Part A_EIP OMB 2018 Revision_20180926 ICRO revised

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Emerging Infections Program

OMB: 0920-0978

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Emerging Infections Program (0920-0978)

Revision

Exp. Date 5/31/2021



SUPPORTING STATEMENT PART A: Justification

January 24, 2019


















Lee Samuel

Centers for Disease Control and Prevention

National Center for Emerging and Zoonotic Infectious Diseases

Office of the Director

1600 Clifton Rd

Atlanta GA 30333

404-718-1616

[email protected]




List of Attachments

  1. Authorizing Regulations_T42 section 241

  2. 60-Day Federal Register Notice

  3. ABCs – 2018 Active Bacterial Core Surveillance Case Report Form

  4. ABCs – 2018 H. Influenzae Neonatal Sepsis Expanded Surveillance Form (HiNSES)

  5. ABCs – Invasive Pneumococcal Disease in Children Surveillance

  6. ABCs – Neonatal Infection Expanded Tracking Form

  7. ABCs – Severe GAS Infection Supplemental Form

  8. FoodNet – Active Surveillance - Variable List

  9. FoodNet – Hemolytic Uremic Syndrome (HUS) Surveillance Case Report Form

  10. FoodNet – Clinical Laboratory Practices and Testing Volume Surveillance Data Elements (New)

  11. FluSurv-NET Influenza Hospitalization Surveillance Case Report Form

  12. FluSurv-NET - Consent Form English

  13. FluSurv-NET - Consent Form Spanish

  14. FluSurv-NET - Provider Vaccination History Fax Form

  15. FluSurv-NET – Vaccination Phone Script

  16. FluSurv-NET – Laboratory Survey (New)

  17. HAIC - C. difficile Infection (CDI) Surveillance Case Report Form

  18. HAIC – Annual Survey of Laboratory Testing Practices for C. difficile Infection (New)

  19. HAIC – CDI Annual Surveillance Officer Survey (New)

  20. HAIC – Emerging Infections Program C. difficile Surveillance Nursing Home Telephone Survey (LTCF) (New)

  21. HAIC - Multi-site Gram-Negative Surveillance Initiative (MuGSI-CRE/CRAB)

  22. HAIC - Multi-site Gram-Negative Surveillance Initiative – Extended-Spectrum Beta-Lactamase-Producing Enterobacteriaceae (MuGSI-ESBL)

  23. HAIC - Invasive Methicillin-resistant Staphylococcus aureus (MRSA) Surveillance

  24. HAIC - Invasive Methicillin-sensitive Staphylococcus aureus (MSSA) Surveillance

  25. HAIC Invasive Staphylococcus aureus Annual Laboratory Survey (New)

  26. HAIC – Invasive Staphylococcus aureus Annual Surveillance Officer Survey (New)

  27. HAIC – Candidemia Case Report Form

  28. HAIC – Candidemia Periodic Laboratory Survey (New)

  29. PIA – HAIC

  30. PIA – FoodNet

  31. PIA – ABCs

  32. PIA – Flu

  33. Non-research determination



Shape1

  • Emerging Infection Program (EIP): Population-based surveillance via active, laboratory case finding is used for detecting, identifying, and monitoring emerging pathogens. The estimates of the infection incidence generated by this collection provide the foundation for a variety of epidemiologic studies to explore risk factors, spectrum of disease, and prevention strategies.

  • This ICR includes four collections:

    • Active Bacterial Core surveillance (ABCs): active population-based laboratory surveillance for invasive bacterial diseases;

    • Foodborne Diseases Active Surveillance Network (FoodNet): active population-based laboratory surveillance to monitor the incidence of select enteric diseases;

    • Influenza: active population-based surveillance for laboratory confirmed influenza-related hospitalizations; and

    • Healthcare Associated Infections-Community Interface (HAIC): active population-based surveillance for healthcare associated pathogens and infections (including Clostridium difficile infection).

  • Data collection is done through the EIP network, which comprises a catchment area of approximately 44 million people, though this varies by project. The total EIP population is roughly comparable to the demographic characteristics of the US population based on the distribution of age, gender, race, and urban residence, as well as population density and percent at or below the poverty level.

  • The methods used to collect data will vary depending on the specific core EIP activity and how the EIP site determines their catchment area (e.g. some activities use stratified random sampling however some will use no sampling at all).

  • This revision package will enhance the previous submission by improving surveillance through new forms and minor revised language to improve clarity.



  1. Justification


  1. Circumstances Making the Collection of Information Necessary

A three-year OMB clearance revision is requested for “Emerging Infections Program (EIP) OMB No. 0920-0978.”

A revision is being submitted to make existing collection instruments clearer and to add several new forms specifically surveying laboratory practices. These forms will allow the EIP to better detect, identify, and track changes in laboratory testing methodology, gather information about laboratory utilization in the EIP catchment area to ensure that all cases are being captured, and survey EIP staff to evaluate program quality. The new collection instruments include the following:

  • FoodNet-Clinical Laboratory Practices and Testing Volume Surveillance Data Elements (Att 10)

  • FluSurv-NET Laboratory Survey (Att 16)

  • HAIC Annual Survey of Laboratory Testing Practices for C. difficile Infection (Att 18)

  • CDI Annual Surveillance Officers Survey (Att 19)

  • Emerging Infections Program C. difficile Surveillance Nursing Home Telephone Survey (Att 20)

  • HAIC Staphylococcus aureus Laboratory Survey: Use of Nucleic Acid Amplification Testing (NAAT) (Att 25)

  • Invasive Staphylococcus aureus Supplemental Surveillance Officers Survey (Att 26)

  • Candidemia Periodic Laboratory Survey (Att 28)

The estimates of the infection incidence generated by this collection provide the foundation for a variety of epidemiologic studies to explore risk factors, spectrum of disease, and prevention strategies.

The Emerging Infections Programs (EIPs) are population-based centers of excellence established through a network of state health departments collaborating with academic institutions; local health departments; public health and clinical laboratories; infection control professionals; and healthcare providers. EIPs assist in local, state, and national efforts to prevent, control, and monitor the public health impact of infectious diseases. Clearance approval for 3 years is sought under this request.

Activities of the EIPs fall into the following general categories: (1) active surveillance; (2) applied public health epidemiologic and laboratory activities; (3) implementation and evaluation of pilot prevention/intervention projects; and (4) flexible response to public health emergencies.

Activities of the EIPs are designed to: (1) address issues that the EIP network is particularly suited to investigate; (2) maintain sufficient flexibility for emergency response and new problems as they arise; (3) develop and evaluate public health interventions to inform public health policy and treatment guidelines; (4) incorporate training as a key function; and (5) prioritize projects that lead directly to the prevention of disease.

Activities in the EIP Network to which all applicants must participate are:

  • Active Bacterial Core surveillance (ABCs): active population-based laboratory surveillance for invasive bacterial diseases.

  • Foodborne Diseases Active Surveillance Network (FoodNet): active population-based laboratory surveillance to monitor the incidence of select enteric diseases.

  • Influenza: active population-based surveillance for laboratory confirmed influenza-related hospitalizations.

  • Healthcare-Associated Infections-Community Interface (HAIC) surveillance: active population-based surveillance for healthcare-associated pathogens and infections.


Table A.1 Listing of all Activities and subprojects included in this ICR package


Activity

Surveillances/Projects

ABCs

ABCs Surveillance

ABCs H. Influenzae Neonatal Sepsis Expanded Surveillance (HiNSES)

ABCs Invasive Pneumococcal Disease in Children Surveillance

ABCs Neonatal Infection Expanded Tracking

ABCs Surveillance Non-Invasive Pneumococcal Pneumonia Surveillance (SNiPP)

ABCs Severe GAS Infection Form


FoodNet

FoodNet Active Surveillance

Hemolytic Uremic Syndrome (HUS) Surveillance

Influenza


Influenza Hospitalization Surveillance Network (FluSurv-NET)

HAIC

C. difficile Infection (CDI) Surveillance

Invasive Candida Infections Surveillance

Invasive Methicillin-resistant Staphylococcus aureus (MRSA) Surveillance

Invasive Methicillin-sensitive Staphylococcus aureus (MSSA)

Multi-site Gram-Negative Surveillance Initiative (MuGSI-CRE/CRAB)

Multi-site Gram-Negative Surveillance Initiative – Extended-Spectrum Beta-Lactamase-Producing Enterobacteriaceae (MuGSI-ESBL)


Information in Identifiable Form (IIF) will be collected by each EIP site, and selected identifiers (such as name or medical record number) will be removed prior to its transmission of data to CDC. Please refer to section A.10 for further description of the process for removing selected identifiers from data. Other information that may be collected could include hospitalization history, lab test results and culture information, symptoms, discharge diagnosis, antimicrobial treatments, ICD-9 or ICD-10 codes, healthcare worker status, influenza vaccination status, and underlying medical conditions. Information transmission occurs via a secure CDC website. The case report form does not involve web-based data collection methods, although case report form data are entered into a CDC-developed, approved web-based data management system for some activities, and does not refer respondents to websites.

This program is authorized under the Public Health Service Act Sections 301(a)[42 U.S.C. 241(a)], 317(k)(1)[42 U.S.C. 247b(k)(1)], and 317(k)(2)[42 U.S.C. 247b(k)(2)], as amended (Attachment 1).


  1. Purpose and Use of Information Collection

ABCs data is critical for documenting disease burden, describing the epidemiology of these bacterial pathogens, detecting emerging infections and epidemics, tracking trends in antimicrobial resistance, contributing to the development and evaluation of new vaccines, developing and assessing public health prevention measures, and improving overall public health practice. ABCs is currently being used to evaluate the effectiveness of meningococcal and pneumococcal vaccines. ABCs data is also used to develop ACIP recommendations for use of bacterial vaccines in children, adolescents and adults. Surveillance data from ABCs is also used to evaluate non-vaccine interventions for invasive bacterial disease. Continuation of these activities is essential to reduce the burden of invasive disease due to these pathogens.


The Foodborne Diseases Active Surveillance Network (FoodNet) is the principal foodborne disease component of the Centers for Disease Control and Prevention’s (CDC) Emerging Infections Program. FoodNet is a collaborative project among CDC, ten state health departments, the Food Safety and Inspection Service of the United States Department of Agriculture (USDA), and the Center for Food Safety and Applied Nutrition and Center for Veterinary Medicine of the United States Food and Drug Administration (FDA).


The objectives of FoodNet are to determine the burden of foodborne diseases in the United States; monitor trends in the burden of specific foodborne illnesses over time; attribute the burden of foodborne illnesses to specific foods and settings; and disseminate information that can lead to improvements in public health practice and the development of interventions to reduce the burden of foodborne illness. FoodNet was established in 1996 in five sites: Minnesota, Oregon, and selected counties in California, Connecticut, and Georgia. By 2004, the FoodNet surveillance area had expanded to include 10 sites; Connecticut, Georgia, Maryland, Minnesota, New Mexico, Oregon, and Tennessee, and selected counties in California, Colorado, and New York. In 2018, the surveillance area included 49 million persons (15% of the U.S. population).


FoodNet conducts population-based active surveillance for laboratory-based infections of select pathogens and a condition commonly transmitted through food: including Campylobacter, Cyclospora, Listeria monocytogenes, Salmonella, Shiga toxin-producing Escherichia coli (STEC), Shigella, Vibrio, Yersinia and hemolytic uremic syndrome (HUS) in residents of the FoodNet surveillance area.


In 2018, Cryptosporidium surveillance was suspended.


In 2019, a pilot for surveillance of Enterotoxigenic E. coli (ETEC) will be conducted in select sites. FoodNet collects standardized data elements from Connecticut, Georgia, Maryland, Minnesota, New Mexico, Oregon, and Tennessee and selected counties within California, Colorado, and New York. The majority of data elements that are transmitted to the FoodNet program at CDC are collected as part of routine public health follow up at the state. Information is collected through electronic laboratory records, chart review, patient interview, or directly from providers or clinical laboratories. In addition, laboratory practices and testing volume are assessed for clinical laboratories within the surveillance area. FoodNet collects standard data elements for the 7 pathogens (Attachment 8), and for one additional pathogen, Norovirus, as part of clinical laboratory surveillance, and has a case report form for HUS (Attachment 9). All information is housed at the state level in state-specific data systems. An extract of the active laboratory-based surveillance data is made monthly and transmitted to CDC. Data elements for clinical laboratory practices and testing volume are submitted to CDC annually. HUS data is either directly entered or imported into a centralized database and data is reviewed annually. No individually identifiable information is collected at CDC, data are only identifiable at the state level.


The Centers for Disease Control (CDC), National Center for Immunization and Respiratory Diseases (NCIRD) is committed to achieving the “Healthy People 2020” goals of increasing immunization rates and reducing preventable infectious diseases. The Influenza Hospitalization Surveillance Network (FluSurv-NET) aligns with these goals and plays an integral role in protecting America’s health. FluSurv-NET is used to obtain population-based surveillance data about laboratory-confirmed influenza-associated hospitalizations in children and adults. These data are used to estimate the national burden of and risk factors for influenza-associated hospitalizations in the United States. The results from this data collection assist the Influenza Division and the CDC in determining which groups are at increased risk for severe outcomes of influenza and in guiding public health interventions and vaccine recommendations. The data are also used to determine the averted burden of influenza through vaccination.


The need for data on influenza impact in children was first highlighted during the 2003-2004 season when anecdotal reports of influenza-associated pediatric deaths and severe complications in otherwise healthy children emerged. When CDC launched an emergency response in December 2003, no systems were in place that could substantiate these anecdotal reports in a timely manner. To address this need, the available surveillance infrastructure of the Emerging Infections Program (EIP) was used to commence FluSurv-NET. In 2005, adult influenza surveillance was added to this platform. In 2006, data from FluSurv-NET were used by the Advisory Committee on Immunization Practices (ACIP) in its decision to expand the ages for which it recommended influenza vaccination from 6-23 month olds to 6- 59 month olds, and to evaluate influenza vaccine effectiveness based on these recommendations. FluSurv-NET data were used by the ACIP in its decision to expand influenza vaccination recommendations for all persons aged 6 months or older. The utility of these data was further underscored during the 2009 H1N1 pandemic. FluSurv-NET data were used to identify groups at highest risk for influenza-associated hospitalizations (e.g., pregnant women during the 2009 H1N1 pandemic), mathematically model the morbidity and mortality burden of the influenza pandemic, and provide data for several peer-reviewed journal articles describing seasonal and pandemic influenza among high risk groups in the population. The data collection network is part of the Emerging Infections Program (EIP), an established CDC-state-academic institution collaborative network which includes the states of California, Colorado, Connecticut, Georgia, Maryland, Minnesota, New Mexico, New York, Oregon, and Tennessee. Upon verification of an influenza positive laboratory result and confirmation of residence within the pre-defined FluSurv-NET catchment area, each FluSurv-NET site conducts data abstraction of the medical chart and laboratory report to complete the project’s standardized case report form. Influenza vaccination status is an important piece of information that is used to evaluate the influenza vaccine program. To obtain as complete an influenza vaccine history as possible sites will use the following sources to collect this information: 1) review the patient’s medical chart, 2) consult the state vaccination registry, 3) contact the patient’s provider via fax or telephone and/or 4) contact the patient or their proxy. If providers and/or patients or proxies need to be contacted, a Consent Form and Provider Vaccination History Fax Form will be used to obtain influenza vaccination history.


The Healthcare-Associated Infections/Community Interface (HAIC) activity was launched in 2009. The HAIC projects include large-scale projects involving all 10 EIP sites that have their own OMB numbers as well as smaller-scale projects involving fewer than 10 EIP sites. The HAIC activity is a collaboration between CDC and the 10 state health departments and academic partners of the EIP network, in California, Colorado, Connecticut, Georgia, Maryland, Minnesota, New Mexico, New York, Oregon, and Tennessee. Healthcare-associated infections (HAIs) are major threats to patient safety and public health in the United States. Elimination of HAIs is a U.S. public health priority. The HAIC activity contributes to the goal of eliminating HAIs through its mission to promote patient safety and healthcare quality by critically evaluating the epidemiology and public health impact of HAIs to understand emerging pathogens and populations-at-risk and to inform prevention interventions. The HAIC activity conducts population-based surveillance for urgent threats to patient safety, including Clostridioides difficile infection (CDI), antibiotic-resistant Gram-negative bacilli, invasive Candida infections, and invasive Staphylococcus aureus infections.


The HAIC activity also conducts periodic HAI and antimicrobial use prevalence surveys under 0920-0852 (hospital survey, expiration 12/31/2019) and 0920-1165 (nursing home survey, expiration 02/29/2020)—these projects are not population-based surveillance, are methodologically distinct from 0920-0978, and were therefore not incorporated into 0920-0978 and will maintain their own OMB control numbers.


For HAIC activities included in 0920-0978, upon verification of a positive laboratory result, each EIP site conducts data abstraction of the medical chart and laboratory report to complete the standardized case report forms. HAIC data collection forms are used by sites during review of medical records to collect demographic and clinical information on laboratory-confirmed cases of CDI, resistant Gram-negative bacilli, invasive S. aureus infection, and invasive Candida infections. Each participating EIP site will destroy identifiers at the earliest opportunity, unless there is a public health or research justification for retaining the identifiers or they are required to by law. For CDI, invasive S. aureus infections and invasive Candida infections, surveys are administered annually to the laboratories reporting surveillance cases. These surveys are being included in this package. For resistant Gram-negative bacilli surveillance, a formal laboratory survey is not conducted. Instead, the sites are instructed to speak with the laboratories serving the EIP catchment area that are reporting cases and determine if any changes have been made to the lab’s automated testing instrument (ATI) (including, but not limited to, changes in software or card types or introduction of new technology into the laboratory), what antimicrobial susceptibility breakpoints the laboratory is using for the carbapenem antibiotics and if the laboratory is conducting any confirmatory testing for carbapenemases. The CDI and invasive S. aureus surveillance activities annually survey the EIP program staff to evaluate program quality. Lastly, the CDI program provides a tool for EIP sites to use to gather information about laboratory utilization among long term care facilities (LTCFs) in the EIP catchment areas.


Data collected through HAIC population-based surveillance have utility for the government, public health officials, healthcare facilities, and the public. These data have served as the foundation for several important public health reports, including the major national CDC report entitled “Antibiotic Resistance Threats in the United States, 2013” (http://www.cdc.gov/drugresistance/threat-report-2013/index.html), an MMWR on invasive MRSA among people who inject drugs (https://www.cdc.gov/mmwr/volumes/67/wr/mm6722a2.htm), and CDC Vital Signs reports on CDI (http://www.cdc.gov/mmwr/preview/mmwrhtml/mm6109a3.htm) and), Candida ( http://www.life-worldwide.org/assets/uploads/files/Cleveland%20candidemia%20Atlanta%20Baltimore%20Clin%20Infect%20Dis%202012.pdf ) and carbapenem-resistant Enterobacteriaceae (http://www.cdc.gov/mmwr/preview/mmwrhtml/mm6209a3.htm). HAIC surveillance is unique in that it collects detailed data on all cases in the population under surveillance, including cases not associated with hospitalizations or other healthcare exposures, and because isolates of the pathogens under surveillance are submitted to CDC for molecular characterization that contributes to enhanced understanding of resistance and transmission.


  1. Use of Improved Information Technology and Burden Reduction

For ABCs case report forms will be entered and maintained at each surveillance area. CDC will provide to each EIP site a Microsoft Access database that mirrors the data collection forms. Surveillance staff at each participating EIP site will enter data from the data collection form into the database. The computerized databases, with personal identifiers removed, will be transmitted to CDC by the fifth of every month. All of the forms included in this package will be submitted to CDC electronically. All data transfers to CDC take place via a secure CDC SAMS (secure access management services).


For FoodNet, data are housed in an electronic database at each site and an extract is transmitted to CDC once a month or as needed through CDC’s secure access management file transfer. In 2018, FoodNet began piloting a standardized message mapping guide (attached) transitioning data collection to an HL7 format is underway. This will allow for more automated and timely data transmission while reducing staff burden at the sites. FoodNet data elements are incorporated into state case report forms. FoodNet collects standard data elements. FoodNet does not require states to administer a separate standardized questionnaires for routine surveillance data. It is up to the states to decide how best to collect the information required. Sites do complete a standardized case report form for HUS surveillance.


For all laboratory-confirmed influenza cases, a standardized case report form is completed by surveillance officers using data obtained from medical record review. Due to the varied sizes of site catchment areas and differences in health care facilities’ electronic reporting capabilities, it is not feasible to have an electronic reporting form at each site under surveillance. Therefore, data are often obtained from manually reviewing medical and laboratory charts. If influenza vaccine history is not noted in the medical chart or state vaccination registry, telephone and facsimile equipment will be used to contact primary care providers, and if necessary, the patient and/or proxy, to obtain vaccination information.


CDC provides each FluSurv-NET site a Microsoft Access database that mirrors the case report form. Surveillance staff at each participating EIP site enters data from the case report form into the database and submit the complete database, stripped of identifiers, to CDC weekly. Sites that do not use the CDC Access database use local systems which are modeled after the CDC Access database or adapted to meet CDC requirements for data collection and delivery. All data transfers to CDC take place via a secure CDC SAMS or CDC FTP site. At CDC, data from all sites will be concatenated and exported into SAS.


HAIC data for CDI, resistant Gram-negative bacilli, invasive Candida infections, and invasive S. aureus infections are collected by EIP site personnel on paper case report forms (Attachments 16-22). Case tracking information is entered into secure locally-housed case tracking systems for CDI and resistant Gram-negative bacilli; identifiable data (such as name, street address, medical record number) entered into these local systems are not shared with CDC. Case information (without identifiers such as name, medical record number, street address, etc.) from these local systems is then imported or transmitted via a secure web service into CDC-approved, web-based data management systems (including .NET and REDCap systems). Other case report form data for CDI, resistant Gram-negative bacilli, and invasive Candida infections are entered directly by EIP site personnel into these secure web-based systems. The databases used by EIP site personnel for capturing these surveillance data (including ESBLs) have Certification and Accreditation by the Office of the CDC Chief Information Security Officer (OCISO) for compliance with current information technology security policies and procedures. Data on case patient census tracts are uploaded by EIP site personnel to site-specific, encrypted, secure CDC Secure Access Management Services (SAMS) or CDC File Transfer Protocol (FTP) sites for analysis by CDC project staff. For invasive S. aureus, case report forms are entered and maintained in each EIP site. CDC provides each EIP site with a Microsoft Access database that mirrors the data collection forms. Surveillance staff at each participating EIP site enter data from the data collection forms into the Access database. The databases, with personal identifiers such as name and medical record number removed, are transmitted to CDC by sites on a regular basis. All data from forms included in this package are submitted to CDC electronically. All data transfers to CDC take place via a secure CDC SAMS or CDC FTP site.

The HAIC Annual Survey of Laboratory Testing Practices for C. difficile Infection, the HAIC Annual- Invasive Staphylococcus aureus Laboratory Survey: Use of Nucleic Acid Amplification Testing (NAAT), and HAIC Candidemia Periodic Laboratory Survey are collected through a REDCap web-based data management system. For each laboratory that responds to these survey, a staff member at the EIP site enters the response into the system using a unique identifier that CDC cannot link to the identity of the responding laboratory. The data is exported out from REDCap by CDC staff for review and analysis. The CDI and the invasive S. aureus surveillance officer’s surveys are completed by an EIP staff member and collected in a Microsoft Word document and emailed to CDC. The data collected in these surveys is for the purpose of program evaluation and it does not contain identifying facility or laboratory information. EIP sites typically share the data elements obtained from the CDI LTCF survey with CDC through Microsoft Excel spreadsheets. No facility specific information or laboratory information is shared with CDC. A site reports the data elements identified during the LTCF survey in aggregate.

  1. Efforts to Identify Duplication and Use of Similar Information

ABCs is the gold standard for the collection of population- and laboratory-based invasive bacterial disease data in the U.S. No other nationwide surveillance systems which monitor these diseases exist. While similar information may be collected on a sample basis or from a particular area of the country, for most diseases, sampling would not be sufficient for the states’ need of conducting prevention or control programs. ABCs collect data from EIP sites in a uniform manner.


ABCs staff routinely attends local, national, and international conferences relevant to the pathogens of interest and communicates frequently with non-federal colleagues at universities and health departments, as well as colleagues within the government in order to prevent duplication of effort.


Much of the information collected by FoodNet (e.g. patient demographics and laboratory data) is already being collected as part of routine public health surveillance at the state level. FoodNet assembles this information in order to describe it on a national level and to assess changes in incidence over time. We allow sites to use their existing structure and databases to avoid duplicate data entry. All analyses of multi-site data must be proposed and approved by the FoodNet steering committee to avoid duplication of publications.


CDC epidemiologists conduct literature reviews continually to stay informed of the current knowledge-base of influenza. CDC staff also attends local, national, and international conferences relevant to the topic, and communicate frequently with non-federal colleagues at universities and health departments as well as colleagues within the government.


FluSurv-NET provides a unique information collection mechanism. No other system exists in which the breadth of demographic, medical, laboratory and epidemiologic are collected for hospitalized patients with laboratory-confirmed influenza. FluSurv-NET provides a critical set of data that are used to make influenza vaccination recommendations, mathematically model the overall burden of influenza morbidity and mortality, and enhance the understanding of severe influenza.


Due to the uniqueness of this system, the questions contained in the standardized case report form have not been taken directly from another survey. The demographic, clinical and epidemiologic information is characteristic of the data routinely collected through public health surveillance.


HAIC surveillance for CDI, resistant Gram-negative bacilli, invasive Candida infections, and invasive S. aureus infections provides unique information not available through other systems, including detailed clinical and demographic data on all cases of infection, not limited to healthcare or hospital-associated cases, and isolates of the pathogens under surveillance for testing and molecular characterization. The National Healthcare Safety Network (NHSN, 0920-0666) receives data from U.S. healthcare facilities on CDI, and on selected infections due to S. aureus, Candida, and resistant Gram-negative bacilli. Data received by the NHSN are collected by healthcare facility staff rather than trained epidemiologists and are limited to healthcare-associated cases (i.e., community-associated infections and other infections not requiring hospitalization are generally not included). Unlike HAIC, NHSN does not have an isolate submission component, and patient-level data reported to NHSN are limited (e.g., no information on underlying conditions).


Healthcare facilities participating in NHSN complete an annual survey that provides information to CDC. Data elements that are collected in part of this survey include facility characteristics, microbiology laboratory practices, infection control practices, antibiotic stewardship practices, and facility water management. Questions asked about antifungal susceptibility testing (e.g. Candida) and methods used to detect C. difficile are similar to the EIP Candida and CDI lab survey, however, provide far less detail. There are not specific questions on the NHSN survey that ask about MRSA/MSSA laboratory methods about laboratory testing practices. The HAIC laboratory surveys for Candida, CDI and invasive S. aureus surveillance are conducted and the questions are are designed to capture changes in trends in the testing methodology for these pathogens over time and to monitor how these changes could impact surveillance. In addition, laboratories that are not targeted by the NHSN survey (e.g. commercial, outpatient, laboratories serving long-term care facilities) participate in the EIP surveys. Lastly, for the EIP laboratories surveys, laboratories are approached based on whether or not they server the EIP catchment area. For NHSN the laboratory is approached if it is in an acute care hospital and that hospital is participating in NHSN


CDC’s Antibiotic Laboratory Network (AR Lab Network) provides nationwide laboratory capacity through state and regional laboratories to rapidly detect antibiotic resistance in healthcare, food, and the community and to inform local response to prevent spread and protect people. The AR Lab Network currently collects isolates of C. difficile, patient samples to determine colonization with Candida, and isolates of resistant Gram-negative bacilli (e.g., CRE). The AR Lab Network’s collection of C. difficile isolates and specimens to detect Candida colonization do not overlap with or duplicate EIP HAIC activities. C. difficile isolate testing is only conducted at a single AR Lab Network regional laboratory: the Minnesota Department of Health Public Health Laboratory. This laboratory is only testing C. difficile isolates for special projects, and currently there is no overlap with HAIC CDI surveillance. For Candida, AR Lab Network testing is only conducted to identify colonization, whereas EIP HAIC surveillance is focused on collection of isolates from invasive infections. The collection of CRE isolates through the AR Lab Network could in some instances overlap with CRE isolate collection through the EIP. CDC staff are working to minimize or eliminate potentially duplicative efforts in state or regional laboratories and ensure that EIP HAIC and AR Lab Network isolate activities are complementary. The AR Lab Network does not collect epidemiological data on the isolates that are collected, and therefore the extensive medical record review that is collected through the EIP is unique.

The EIP HAI and antimicrobial use prevalence surveys (0920-0852, 0920-1165) are cross-sectional “snapshots” of all HAIs attributable to acute care hospitals or nursing homes (not limited to specific types of infections reported to NHSN through prospective HAI surveillance or specific laboratory-identified pathogens reported through HAIC population-based surveillance). The surveys are conducted intermittently (e.g., approximately every 4 years in a specific healthcare setting). The survey is conducted throughout the entire facility in all eligible units, rather than being limited to specific unit types within the facility (as in NHSN), with a goal of defining the overall burden of HAIs as well as antimicrobial drug use in that specific healthcare setting.


  1. Impact on Small Businesses or Other Small Entities

For all activities, the data collection itself will not impact small businesses because the burden of completing the case report form rests with the surveillance officers appointed by the states, not the hospitals or other healthcare facilities where the cases are identified. However, in some sites, data collection is performed in cooperation with on-site medical personnel (e.g., Infection Control Practitioners or Medical Records Personnel). The impact on these facilities should be minimal, since the hospital has entered into an agreement with the State health department.



  1. Consequences of Collecting the Information Less Frequently

For ABCs and FoodNet, partnering state health departments submit data collection forms or standardized data elements to CDC on a monthly basis. Prompt notification to CDC allows for timely data analysis, tracking of the effects of prevention measures, and policy development. Collecting data less frequently would result in a delay in analysis and subsequent reports and publications.


Respondents are required to submit FluSurv-NET data to the CDC on a weekly basis during influenza season (October 1-April 30). However, reporting frequency may vary, as some weeks during the seven-month influenza season might not include any influenza cases. It would not be appropriate to collect influenza surveillance data less frequently than weekly because the first step in the control of a given disease is its rapid identification followed by notification to the local health authority that a case of disease exists within a particular jurisdiction. In general, case reports are submitted as soon as possible after the investigation of a case. Prompt notification to CDC allows for identification of epidemics and outbreaks, so that immediate prevention measures can be taken. In order to lessen the burden of weekly reporting, respondents are required to submit as soon as possible data for only five variables on the case report form during influenza season. CDC requests the remaining variables to be completed and submitted by September 30.


HAIC EIP personnel will complete data collection on cases as they are identified from laboratory reports on an ongoing basis. Performing data collection on cases as they are identified (versus on a quarterly or annual basis) will allow for rapid classification of cases into epidemiologic categories (e.g. community-associated) and identification of epidemiologic changes, including rates and severity of disease in geographically diverse patient population segments over time. Linking these epidemiological changes to several important determinants of disease, including host susceptibility, practices in prescribing antimicrobials, infection control practices, or the emergence of more virulent strains, requires timely and consistent data collection.


Collection of the laboratory survey data less than annually would prevent our programs from documenting testing method changes that are important to the interpretation of EIP HAIC data. The surveying of HAIC surveillance officers less than once annually would prevent us from ensuring high quality data are being collected and would prevent us from identifying any issues that are ongoing that might need to be addressed. These surveys are important to maintaining high quality data collection for the HAIC program. The LTCF survey is conducted annually across all HAIC pathogens, as part of our surveillance protocols. The CDI program has provided sites with a script to guide them in conducting these calls. It is has been demonstrated that LTCFs can change the laboratories that they contract with frequently, and therefore to assure complete case capture, these providers need to be surveyed annually.


There are no legal obstacles to reduce the burden.


  1. Special Circumstances Relating to the Guidelines of 5 CFR 1320.5

For the reasons described in A.6 above, respondents are required to report information more often than quarterly (monthly). FluSurv-NET requires weekly reporting during the influenza season (October 1- April 30); however, reporting frequency will vary as some weeks during the influenza season might not include influenza cases. Surveillance reports are requested on a periodic basis to permit timely data analysis and prompt initiation of prevention and control measures.


As stated in A.6., delays in reporting could result in serious public health consequences. There are no other special circumstances relating to the guidelines of CFR 1320.5.

  1. Comments in Response to the Federal Register Notice and Efforts to Consult Outside the Agency

  1. A 60-day Federal Register Notice was published in the Federal Register on November 15, 2018, Volume 83, No. 221, p. 57489. No comments were received.


B. ABCs and FoodNet are the gold standards for the collection of population- and laboratory-based bacterial disease data in the U.S. CDC conducts a conference call with site surveillance officers to discuss surveillance-related issues monthly. CDC conducts conference calls with ABCs and FoodNet Principle Investigators to discuss bi-monthly and quarterly, respectively. . CDC also organizes the annual ABCs and FoodNet Steering Committee meetings with each site’s Principle Investigators in attendance and an annual Site coordinator meeting which includes representatives from all sites. These meetings offer the opportunity to discuss ongoing projects and plan for future priorities.

Since FluSurv-NET’s inception, consultation with sites has taken place at an annual meeting to address information collection activities. Additionally, monthly conference calls are held with site personnel to ensure that data collection is standardized, efficient and relevant.

CDC staff involved in the HAIC activity conducts quarterly conference calls with EIP site HAIC principal investigators and hold an annual in-person meeting at CDC with the principal investigators and other key participants to discuss progress and scientific direction for the activity. Regular calls are also held with EIP site and CDC project leads and coordinators to discuss progress and challenges for individual projects.

  1. Explanation of Any Payment or Gift to Respondents

No payments or gifts will be provided to respondents. EIP sites, at their discretion, may provide resources to catchment area laboratories or healthcare facilities, for example, to enable or enhance isolate collection and submission.


  1. Protection of the Privacy and Confidentiality of Information Provided by Respondents

This submission has been reviewed by NCEZID who determined that the Privacy Act does not apply.

As a measure of EIP’s data protection plan, the ABCs, FoodNet, FluSurv-NET, and HAIC activity utilize data transfer methods that are password protected in order to protect the data. In addition to using the CDC FTP platform to transmit data, CDC and EIP sites also have the option to utilize the CDC SAMS platform to transmit data. CDC SAMS is a federal information technology system that gives authorized personnel secure access to non-public CDC applications through a highly secure and password protected and encrypted portal. The SAMS partner portal is a website designed to provide centralized access to public health information and computer applications operated by the CDC. Through this portal EIP sites and CDC are able to transfer data in a secure portal to keep data protected.

Names or other direct personal identifiers (such as address, medical record number, social security number, etc.) may be collected by the EIP site to assist in managing case information, but they are not shared with CDC. There are no direct personal identifiers in the data submitted to CDC for any of the forms included in this package. Patient information that is collected and shared with CDC include date of birth, age, sex, race, ethnicity, census tract, and clinical dates (e.g., dates of admission and discharge).

In the September 2018 change request, ABCs requested an addition of a Patient ID to their 2019 ABCs Case Report form. This addition complies with the statement that CDC is not collecting personal identifiers. All of the EIP activities (ABCs, FoodNet, FluSurv-NET, and HAIC) have a documented PIA and have been submitted as a part of this revision.

Each participating EIP site will destroy identifiers at the earliest opportunity, unless there is a public health or research justification for retaining the identifiers or are required to by law. Project paperwork maintained by each participating site will never be submitted to CDC and will remain in a locked, secure location, available only to a minimum number of local project staff, and will not be reused or disclosed to any other person or entity except as required by law, for authorized oversight of the research project, or for other research for which the use or disclosure of protected health information would be permitted.

FoodNet surveillance is conducted by state health departments as part of routine public health surveillance and, as such, personnel at the state health departments collect personal identifiers (name, address, phone number) in order to conduct appropriate public health follow up of cases. Date of birth and a coded FoodNet ID field are transmitted to CDC; however, names, addresses and phone numbers are not. The code linking the FoodNet ID field to other personal identifier is maintained confidentially and securely with the state health department that reported the case; it is not shared with CDC. When surveillance data are requested for analysis by persons at CDC, state or federal partners (e.g. FDA or USDA), or others (e.g. students) an analytic dataset is provided that includes only the minimum number of variables required for the specified analysis; it does not include the FoodNet ID field and certain fields are often aggregated into groups to minimize the ability to link to other data sources to identify a person

There are no personal identifiers in the database submitted to CDC in the data collected for FluSurv-NET. Thus, the patients whose charts are reviewed will not be able to be identified through data submitted to CDC; only the FluSurv-NET site collecting the case information will be able to link personal identifiers with case information. Additionally, CDC will not have identifying information on patient health care providers. Each hospital where charts are abstracted will be given a numerical ID that can be linked to hospital name only by staff within individual surveillance areas.

Each participating FluSurv-NET site will destroy identifiers at the earliest opportunity, unless there is a public health or research justification for retaining the identifiers or they are required to by law. Project paperwork maintained by each participating site will never be submitted to CDC and will remain in a locked, secure location, available only to a minimum number of local project staff, and will not be reused or disclosed to any other person or entity except as required by law, for authorized oversight of the research project, or for other research for which the use or disclosure of protected health information would be permitted.

The HAIC activity conducts population-based surveillance for urgent threats to patient safety, including CDI, resistant Gram-negative bacilli, invasive Candida infections, and invasive S. aureus infections. As with ABCs surveillance described above, upon verification of a positive laboratory result and confirmation of residence within the pre-defined EIP catchment area, each EIP site conducts data abstraction of the medical chart and laboratory report to complete the standardized case report forms. HAIC data collection forms (previously approved data collection) are used by sites to review medical records and collect demographic and clinical information on laboratory-confirmed cases.

Each participating EIP site will destroy identifiers at the earliest opportunity, unless there is a public health or research justification for retaining the identifiers or they are required to by law.

Information in Identifiable Form (IIF) will be collected by each EIP site. Other information that may be collected could include hospitalization history, lab test results and culture information, symptoms, discharge diagnosis, antimicrobial treatments, ICD-9 and/or ICD-10 codes, healthcare worker status, influenza vaccination status, and underlying medical conditions. Information transmission occurs via a secure CDC website. The case report form does not involve web-based data collection methods, although case report form data are entered into a CDC-developed, approved web-based data management system for some activities, and does not refer respondents to websites.

For HAIC projects, personally identifying information such as names and addresses are not shared with CDC. Date of birth, race, ethnicity, gender, hospitalization dates and census tract information are shared with CDC. Only the EIP site collecting the case information will be able to link personal identifiers with case information. Each participating EIP site will destroy identifiers at the earliest opportunity, unless there is a public health or research justification for retaining the identifiers or are required to by law. Project paperwork maintained by each participating site will not be submitted to CDC and will remain in a locked, secure location, available only to a minimum number of local project staff, and will not be reused or disclosed to any other person or entity except as required by law, for authorized oversight of the research project, or for other research for which the use or disclosure of protected health information would be permitted.


Data collection for HAIC CDI cases (previously approved data collection) includes state and county of residence, age, gender, date of birth, race/ethnicity, date of stool collection positive for C. difficile, location of stool collection (i.e. hospital inpatient, long term acute care hospital, long term care/skilled nursing facility, emergency room, or outpatient setting), hospitalization and date of admission, residency prior to stool collection (i.e. hospital inpatient, long term acute care hospital, long term care/skilled nursing facility, emergency room, or outpatient setting), hospital admission due to CDI, presence of other enteric pathogens in stool tested for CDI, exposures to healthcare (i.e. chronic hemodialysis, surgical procedure in the 12 weeks prior to stool collection, or emergency room visit in the 12 weeks prior to stool collection), patient outcome (patient survived and date of discharge or patient died and date of death), colectomy and date of procedure, intensive care unit (ICU) admission and date, CDI recurrence, radiographic findings (including toxic megacolon and ileus), presence of pseudomembranous colitis, clinical findings (including diarrhea and white blood cell counts), Charlson co-morbidity index components, medication used in the 14 days prior to illness onset (including antimicrobial therapy use, immunosuppressive therapy use, and use of proton pump inhibitors or H2 blockers), and CDI treatment information (previously approved data collection). Healthcare facilities are identified by facility identification codes. These facility identification codes are assigned by EIP sites. Local data collectors at participating healthcare facilities and EIP personnel will need to collect information in identifiable form (IIF) for patients within their own facility or catchment area, such as patient name, address, telephone number, date of birth, and medical record number. With the exception of date of birth, this information will not be transmitted to CDC. CDI cases are also geocoded and census tract numbers are assigned; EIP site personnel strip out geocoded data (e.g., address, latitude, longitude), and the census tract number is shared with CDC. Unique identification codes not containing any patient identifiers are assigned by EIP sites to patients; CDC does not have access to linkages between patient name and patient identification code. EIP sites also collect data from participating laboratories annually and submit the information to CDC: frequency of line lists, if isolates are being collected from the laboratory, what health care facilities are being served by the laboratory being surveyed, and detailed information about laboratory practices (Attachment 18, 19, 20, 25, 26, 28). The Annual CDI Surveillance Officer Survey collects data on laboratory participation, practices and auditing (case identification methodology, current laboratory participation, are specimen collection counts changing, understanding specimen shipping procedures), data edits, information about assurance of case ascertainment, geocoding and facility information. The LTCF survey gathers information about where facilities send samples for testing, and the tool included in this package is a script used to guide calls with the local LTCFs (Attachment 20). After this survey is conducted CDC receives the following data elements: unique provider/ facility ID (this is a number that is assigned by the EIP site and does not contain facility identifying information), CMS classification of the facility that was surveyed, documentation if the facility contacted as part of the survey process, and a list of laboratory ids for the laboratories that serve the LTCF (the laboratory ids are set by the site and do not contain identifying information).


Data collected for the HAIC resistant Gram-negative bacilli surveillance (previously approved data collection) are similar to those collected for CDI cases, and include variables such as state, county of residence, age, gender, date of birth, race/ethnicity, weight and height or body mass index, date of collection of specimens positive for resistant Gram-negative bacilli, types of specimens, location of specimen collection, results of testing performed on the specimen (including pathogens isolated and antimicrobial susceptibility test results), residency prior to specimen collection, hospitalization data (including dates), underlying conditions, healthcare exposures and other risk factors for infection, signs and symptoms of infection, and patient outcome. For patients with the ESBLs selected resistant organisms, data collection, prior medications are also collected. As with CDI surveillance, healthcare facilities are identified by facility identification codes in the data collection forms. Local data collectors and EIP personnel will need to collect information in identifiable form (including information such as patient name, address, telephone numbers, date of birth, and medical record number), but this information (with the exception of date of birth) is not transmitted to CDC. Cases may also be geocoded and census tract numbers assigned; EIP sites will strip other data (e.g., address, latitude, longitude), and the census tract number will be shared with CDC. Unique identification codes not containing identifiers are assigned by EIP sites to patients; CDC does not have access to any linkages between patient name and patient identification code.as described above for CDI.). For resistant Gram-negative bacilli surveillance, a formal laboratory survey is not conducted. Instead the sites are instructed to speak with the laboratories serving the EIP catchment area that are reporting cases and determine if any changes have been made to the lab’s automated testing instrument (ATI) (including, but not limited to, changes in software or card types or introduction of new technology into the laboratory), what breakpoints the laboratory is using for the carbapenem antibiotics and if the laboratory is conducting any confirmatory testing for carbapenemases. The MuGSI program will encourage sites to work with their CDI staff when surveying LTCFs to ask about testing methodology around gram-negative organisms.

Data collected for the HAIC invasive S. aureus surveillance (previously approved data collection) are similar to those collected for CDI cases, and include variables such as state, county of residence, age, gender, date of birth, race/ethnicity, weight and height or body mass index, date of collection of specimens positive for S. aureus, types of positive specimens, location of initial specimen collection, results of antimicrobial susceptibility testing performed on the specimen, residency prior to specimen collection, hospitalization and ICU admission data (including date of hospital and ICU admissions), underlying conditions, type of infection associated with the culture, healthcare exposures and other risk factors for infection, and patient outcome. As with CDI surveillance, healthcare facilities are identified in the data collection forms by facility identification codes. Local data collectors and EIP personnel will need to collect information in identifiable form (including information such as patient name, address, telephone numbers, date of birth, and medical record number), but this information (with the exception of date of birth) is not transmitted to CDC. Cases may also be geocoded and census tract numbers assigned; EIP sites will strip other data (e.g., address, latitude, longitude), and the census tract number will be shared with CDC. Unique identification codes not containing identifiers are assigned by EIP sites to patients; CDC does not have access to any linkages between patient name and patient identification code. The invasive S. aureus program collects data from participating laboratories annually, the EIP site staff collect information the type of laboratory being surveyed, current testing methods for S. aureus, the use of culturing techniques and if culture independent diagnostic tests (CIDTs) are being utilized at the laboratory. The Annual invasive S. aureus Surveillance Officer Survey collects data on surveillance area characteristics (including is the pathogen reportable locally, are isolates collected and submitted to CDC for testing, what parts of the invasive S. aureus program the site is participating in, does the site have access to their states’ NHSN S. aureus data, and if so how are those data being used locally), laboratory participation and case finding (including the number and types of laboratories that are serving the catchment area, culture sources from which S. aureus is being identified form, case finding methods, how laboratory data is being share with the EIP site staff, have laboratories stopped participating in surveillance), data edits (including information if a site edits there data beyond the required CDC data edits), ascertainment of surveillance area and case audits (including how an audit case is defined and how these types of cases are contributing to case counts, what auditing methods are being used, how case ascertainment is being conducted), geocoding, and feedback on CDC staffs performance.

Data collected for the HAIC Candidemia program (previously approved data collection) are similar to those collected for CDI cases, and include variables such as state, county of residence, age, gender, date of birth, race/ethnicity, date of collection of specimens positive for resistant Gram-negative bacilli, types of specimens, location of specimen collection, results of testing performed on the specimen (including Candida species and antimicrobial susceptibility test results), residency prior to specimen collection, hospitalization data (including dates), underlying conditions, healthcare exposures and other risk factors for infection, signs and symptoms of infection, and patient outcome. As with CDI surveillance, healthcare facilities are identified in the data collection forms by facility identification codes. Local data collectors and EIP personnel will need to collect information in identifiable form (including information such as patient name, address, telephone numbers, date of birth, and medical record number), but this information (with the exception of date of birth) is not transmitted to CDC. Cases may also be geocoded and census tract numbers assigned; EIP sites will strip other data (e.g., address, latitude, longitude), and the census tract number will be shared with CDC. Unique identification codes not containing identifiers are assigned by EIP sites to patients; CDC does not have access to any linkages between patient name and patient identification code. The Candidemia Periodic Laboratory Survey collects the following information: the type of laboratory being surveyed, the types of facilities that the laboratory serves, is mycology testing capabilities, capacity and testing methodology.

Privacy Impact Assessment Information

  1. Respondents are informed about the voluntary nature of their response.

  1. For FluSurv-NET, consent forms are obtained from patients undergoing telephone interview for influenza vaccination history. Copies of the consent form will be retained at the participating site and will not be submitted to CDC. CDC only receives vaccine status information and does not receive any personally identifiable information.

For the medical review component of HAIC, consent is not applicable as EIP personnel perform review of existing medical record data in participating facilities or via remote access and submit these data to CDC in a secure manner, as described previously, without having any interaction with individual patients. Information received by CDC are stored in secure databases (certification and accreditation at appropriate level according to current information security procedures and standards) or will be uploaded by EIP site personnel to site-specific encrypted, secure CDC FTP sites or other secure sites meeting current information security requirements. Case-specific information received by CDC will be provided only to those individuals at CDC with a need to know.


  1. Project case report forms maintained by each participating site will not be submitted to CDC, and will remain in a locked, secure location, available only to a minimum number of local project staff, and will not be reused or disclosed to any other person or entity except as required by law, for authorized oversight of the surveillance project, or for other research for which the use or disclosure of protected health information would be permitted. Each participating EIP site will destroy identifiers at the earliest opportunity, unless there is a public health justification for retaining the identifiers or are required to by law.

  2. This submission has been reviewed by NCEZID who determined that the Privacy Act does not apply.

To comply with OMB’s terms of clearance from the September 13, 2018 change request, four Privacy Impact Assessments (Atts. 29, 30, 31, and 32)—one for each of the four activities—are included with this submission.

  1. Institutional Review Board (IRB) and Justification for Sensitive Questions

IRB Approval

The data collection forms included in this package constitute public health surveillance and are not considered human subjects research (Attachment 33). Therefore the protocols associated with the forms included in this package are not subject to IRB review.

Justification for Sensitive Questions

For ABCs, epidemiological characteristics such as age, race, sex, geographic location, etc., are collected only when these factors may produce health problems. Clinical and laboratory data are collected and analyzed with the purpose of contributing valuable knowledge to the field of public health.

For FoodNet, clinical and laboratory data are collected and analyzed with the purpose of contributing valuable knowledge to the field of public health. Data collected for FoodNet surveillance are not considered sensitive. However, persons can refuse to provide any information that they consider to be sensitive.

In FluSurv-NET, age and variables related to documentation of laboratory-confirmed influenza-associated hospitalization are of central importance to this study. Additional clinical and, underlying health conditions, influenza vaccination status, diagnosis with secondary bacterial co-infections, and ICU admission are necessary for determining rates of influenza-associated complications and factors associated with these complications. Questions about pregnancy, past medical history or chronic conditions are asked to clarify any risk factors for influenza or assess confounding factors of illness. Questions about race and ethnicity are asked in order to clarify risk factors for influenza and evaluate race and ethnicity in the context of influenza infection. All race and ethnicity questions meet OMB’s minimum standards for collecting race and ethnicity information.

For HAIC surveillance, demographic and clinical data (including information on the presence of HIV/AIDS and other chronic conditions, smoking, drug and alcohol use, and incarceration) are collected from medical records and analyzed to describe risk factors for infection with important healthcare-associated and antimicrobial-resistant pathogens.

  1. Estimates of Annualized Burden Hours and Costs

For this revision, the total estimated burden is 40,601 hours. The previous approval (non-substantive change request approved 9/13/2018) was for an estimated annual burden of 39,989 hours.


  1. ABCs: The total burden estimate for the ABCs collection activity is 3,320 hours and is shown in Table A.12-A1. A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.



  1. FoodNet: The total burden estimate for the FoodNet collection activity is 7,887 hours and is shown in Table A.12-A1. The FoodNet Clinical Laboratory Practices and Testing Volume is a new collection instrument with 233 hours of total burden. The changes made for this collection helps further characterize and determine the burden of foodborne illness.



  1. FluSurv-NET: The total burden estimate for the Influenza FluSurv-NET collection activity is 5,039 hours and is shown in Table A.12-A1. The number of responses varies by influenza season and the current burden estimates are based on previous experience and feedback from stakeholders using these instruments. Burden changes include an increase in the burden hours by 38 hours to reflect a laboratory survey administered to laboratories that serve FluSurv-NET facilities, which assess laboratory testing practices.



  1. HAIC: The total burden estimate for HAIC collection activity is 24,355 hours and is shown in Table A.12-A1. Six new HAIC collection instruments are being added with a total of 130 burden hours; Three collection tools that are used for surveying the clinical laboratories that serve the defined project catchment areas and two tools are used to survey EIP surveillance officers, and one survey that is used to collect information from LTCFs about clinical laboratory utilization. The purpose of the laboratory survey data collection is to track laboratory testing practices that are important for interpreting changes in surveillance data. As changes occur in testing methodologies, this could affect how cases are identified. The purpose of surveying the EIP site’s Surveillance Officers, is to ensure that sites are following current protocols, to ensure data quality and to validate surveillance practices. Lastly, the purpose of conducting a LTCF survey is to ensure that each EIP site is working with all laboratories that serve the catchment area and therefore ensuring complete case capture. To account for the possibility that more sites may conduct invasive S. aureus surveillance in the future, we have opted to leave this surveillance in this package, but we anticipate that the total number of respondents will remain at 7 for 2019. The changes made for this collection helps further characterize and determine the burden of hospital-associated infections.

Table A.12-A1. Estimated Annualized Burden Hours


Type of Respondent

Form Name

No. of respondents

No. of responses per respondent

Avg. burden per response (in hours)

Total burden (in hours)

State Health Department


ABCs Case Report Form

10

809

20/60

2697

ABCs Invasive Pneumococcal Disease in Children Case Report Form

10

22

10/60

37

ABCs H.influenzae Neonatal Sepsis Expanded Surveillance Form

10

6

10/60

10

ABCs Severe GAS Infection Supplemental Form

10

136

20/60

453

ABCs Neonatal Infection Expanded Tracking Form

10

37

20/60

123

FoodNet Campylobacter

10

942

21/60

3297

FoodNet Cyclospora

10

163

10/60

272

FoodNet Listeria monocytogenes

10

15

20/60

50

FoodNet Salmonella

10

789

21/60

2761

FoodNet Shiga toxin producing E. coli

10

205

20/60

683

FoodNet Shigella

10

213

10/60

355

FoodNet Vibrio

10

34

10/60

56

FoodNet Yersinia

10

48

10/60

80

FoodNet Hemolytic Uremic Syndrome Case Report Form

10

10

1

100

FoodNet Clinical Laboratory Practices and Testing Volume – NEW

10

70

20/60

233

Influenza Hospitalization Surveillance Network Case Report Form

10

1000

25/60

4167

Influenza Hospitalization Surveillance Project Vaccination Phone Script Consent Form (English/Spanish)

10

333

5/60

278

Influenza Hospitalization Surveillance Project Vaccination Phone Script (English/Spanish)

10

333

5/60

278

Influenza Hospitalization Surveillance Project Provider Vaccination History Fax Form (Children/Adults)

10

333

5/60

278

FluSurv-NET Laboratory Survey – NEW

10

23

10/60

38

HAIC CDI Case Report Form

10

1650

35/60

9625

HAIC CDI Annual Laboratory Survey-NEW

10

16

10/60

27

HAIC CDI Annual Surveillance Officers Survey- NEW

10

1

15/60

3

HAIC CDI LTCF Survey- NEW

10

45

5/60

38

HAIC Multi-site Gram-Negative Bacilli Case Report Form (MuGSI-CRE/CRAB)

10

500

25/60

2083

HAIC Multi-site Gram-Negative Surveillance Initiative – Extended-Spectrum Beta-Lactamase-Producing Enterobacteriaceae (MuGSI-ESBL)

10

1200

25/60

5000

HAIC Invasive Methicillin-resistant Staphylococcus aureus (MRSA)

10

474

25/60

1975

HAIC Invasive Methicillin-sensitive Staphylococcus aureus (MSSA)

10

754

25/60

3142

HAIC Invasive Staphylococcus aureus Annual Laboratory Survey- NEW

10

11

8/60

15

HAIC Invasive Staphylococcus aureus Annual Surveillance Officers Survey- NEW

10

1

10/60

2

HAIC Candidemia Case Report Form

9

800

20/60

2400

HAIC Candidemia Periodic Laboratory Survey- NEW

9

15

20/60

45

Total


40,601


B. The following table shows estimated burden costs associated with each instrument. The mean hourly wage for epidemiologists was used (https://www.bls.gov/oes/current/oes191041.htm).


Type of Respondent

Form Name

Total burden hours

Hourly wage rate

Total respondent costs

State Health Department


ABCs Case Report Form

2697

$36.65

$98845.05

ABCs Invasive Pneumococcal Disease in Children Case Report Form

37

$36.65

$1,356.05

ABCs H.influenzae Neonatal Sepsis Expanded Surveillance Form

10

$36.65

$366.50

ABCs Severe GAS Infection Supplemental Form

453

$36.65

$16,602.45

ABCs Neonatal Infection Expanded Tracking Form

123

$36.65

$4,507.95

FoodNet Campylobacter

3297

$36.65

$120,835.05

FoodNet Cyclospora

272

$36.65

$9,968.80

FoodNet Listeria monocytogenes

50

$36.65

$1,832.50

FoodNet Salmonella

2761

$36.65

$101,190.65

FoodNet Shiga toxin producing E. coli

683

$36.65

$25,031.95

FoodNet Shigella

355

$36.65

$13,010.75

FoodNet Vibrio

56

$36.65

$2,052.40

FoodNet Yersinia

80

$36.65

$2,932.00

FoodNet Hemolytic Uremic Syndrome Case Report Form

100

$36.65

$3,665.00

FoodNet Clinical Laboratory practices and testing volume – NEW

233

$36.65

$8,539.45

Influenza Hospitalization Surveillance Network Case Report Form

4167

$36.65

$152,720.55

Influenza Hospitalization Surveillance Project Vaccination Phone Script Consent Form (English/Spanish)

278

$36.65

$10,188.70

Influenza Hospitalization Surveillance Project Vaccination Phone Script (English/Spanish)

278

$36.65

$10,188.70

Influenza Hospitalization Surveillance Project Provider Vaccination History Fax Form (Children/Adults)

278

$36.65

$10,188.70

FluSurv-NET Laboratory Survey – NEW

38

$36.65

$1,392.70

HAIC CDI Case Report Form

9625

$36.65

$352,756.25

HAIC CDI Annual Laboratory Survey- NEW

27

$36.65

$989.55

HAIC CDI Annual Surveillance Officers Survey- NEW

2

$36.65

$73.30

HAIC CDI LTCF Survey- NEW

38

$36.65

$1,392.70

HAIC Multi-site Gram-Negative Bacilli Case Report Form for Carbapenem-resistant Enterobacteriacaea and Acinetobactoer baumannii (MuGSI-CRE/CRAB)

2083

$36.65

$76,341.95

HAIC Multi-site Gram-Negative Surveillance Initiative – Extended-Spectrum Beta-Lactamase-Producing Enterobacteriaceae (MuGSI-ESBL)

5000

$36.65

$183,250

HAIC Invasive Methicillin-resistant Staphylococcus aureus (MRSA)

1975

$36.65

$72,383.75

HAIC Invasive Methicillin-sensitive Staphylococcus aureus (MSSA)

3142

$36.65

$115,154.30

HAIC Staphylococcus aureus Annual Laboratory Survey-NEW

15

$36.65

$549.75

HAIC Invasive S. aureus Annual Surveillance Officers Survey- NEW

2

$36.65

$73.30

HAIC Candidemia Case Report Form

2400

$36.65

$87,960

HAIC Candidemia Periodic Laboratory Survey- NEW

45

$36.65

$1,649.25

Total


$1,487,990.00


  1. Estimates of Other Total Annual Cost Burden to Respondents or Record Keepers

There are not costs to respondents other than their time.

  1. Annualized Cost to the Federal Government

Estimated cost based on 2017 figures

Active Bacterial Core surveillance (ABCs) - Active population-based laboratory surveillance for invasive bacterial diseases

Table 14-1: Estimates of Annualized Costs to the Federal Government



Expense Type



Expense Explanation


Annual Costs (dollars)

Direct Costs to the Federal Government

CDC Principal Investigator (0.8 FTE); CDC Surveillance Coordinator (0.8 FTE); Program Analyst (1.0 FTE), Data Manager (1.0 FTE)

350,000





Subtotal, Direct Costs to the Government

350,000

Cooperative Agreement Expenses

California Site Cost and Fees

638,409


Colorado Site Cost and Fees

629,781


Connecticut Site Cost and Fees

711,556


Georgia Site Cost and Fees

1,112,959


Maryland Site Cost and Fees

1,226,107


Minnesota Site Cost and Fees

1,384,433


New Mexico Site Cost and Fees

751,779


New York Site Cost and Fees

1,069,299


Oregon Site Cost and Fees

793,550


Tennessee Site Cost and Fees

1,092,127





Subtotal, Contracted Services

9,410,000


TOTAL COST TO THE GOVERNMENT

9,760,000



Foodborne Diseases Active Surveillance Network (FoodNet)

Table 14-2: Estimates of Annualized Costs to the Federal Government

Expense Type

Expense Explanation


Annual Costs (dollars)

Direct Costs to the Federal Government

CDC Principle Investigator (1.0 FTE); CDC Doctoral staff (2.0 FTE); CDC project Coordinator (1.0 FTE); CDC surveillance officers (5.0 FTE); CDC Technical research assistant (1.0 contractor); CDC Programmer (1.0 FTE contractor)

850,000






Subtotal, Direct Costs to the Government

850,000


Cooperative Agreement Expenses

California Site Cost and Fees

582,048


Colorado Site Cost and Fees

543,900


Connecticut Site Cost and Fees

483,861


Georgia Site Cost and Fees

738,442


Maryland Site Cost and Fees

310,893


Minnesota Site Cost and Fees

645,087


New Mexico Site Cost and Fees

332,463


New York Site Cost and Fees

549,537


Oregon Site Cost and Fees

532,946


Tennessee Site Cost and Fees

491,605





Subtotal, Contracted Services

5,210,782


TOTAL COST TO THE GOVERNMENT

6,060,782



Influenza - All Age Influenza Hospitalization Surveillance Network

Table 14-3: Estimates of Annualized Costs to the Federal Government

Expense Type

Expense Explanation


Annual Costs (dollars)

Direct Costs to the Federal Government

CDC Project Officer (1.0 FTE); CDC Principle Investigator (0.8 FTE)

214,500





Subtotal, Direct Costs to the Government

155,500

Cooperative Agreement Expenses

California Site Cost and Fees

601,046


Colorado Site Cost and Fees

307,163


Connecticut Site Cost and Fees

428,671


Georgia Site Cost and Fees

373,245


Maryland Site Cost and Fees

404,000


Minnesota Site Cost and Fees

396,754


New Mexico Site Cost and Fees

374,850


New York Site Cost and Fees

696,142


Oregon Site Cost and Fees

550,673


Tennessee Site Cost and Fees

536,368





Subtotal, Contracted Services

4,668,912


TOTAL COST TO THE GOVERNMENT

4,824,412


Healthcare Associated Infections-Community Interface (HAIC)

Table 14-4: Estimates of Annualized Costs to the Federal Government



Expense Type



Expense Explanation


Annual Costs (dollars)

Direct Costs to the Federal Government

CDC HAIC Director (1.5 FTE), Principal Investigators (3.48 FTE); CDC Surveillance Coordinators (3.37 FTE); Laboratory Scientists (6.3FTE); Data Manager (0.75 FTE); Business Analyst (0.5 FTE)

2,124,107





Subtotal, Direct Costs to the Government

2,124,107

Cooperative Agreement Expenses

California Site Cost and Fees

693,421


Colorado Site Cost and Fees

695,678


Connecticut Site Cost and Fees

1,100,944


Georgia Site Cost and Fees

908,109


Maryland Site Cost and Fees

961,446


Minnesota Site Cost and Fees

1,076,459


New Mexico Site Cost and Fees

362,214


New York Site Cost and Fees

786,703


Oregon Site Cost and Fees

515,751


Tennessee Site Cost and Fees

1,221,964





Subtotal, Contracted Services

8,322,689


TOTAL COST TO THE GOVERNMENT

10,446,796


Annualized Total Cost to the Federal Government

31,091,990


  1. Explanation for Program Changes or Adjustments

This is a request for a revision. The majority of the collection activities remain the same, however, there are a few proposed revisions including minor revised language and rewording to improve clarity and readability of the data collection forms.

CDC is also requesting the use of 8 new forms: FoodNet - Clinical Laboratory Practices and Testing Volume Surveillance Data Elements, FluSurv- NET – Laboratory Survey, HAIC - Annual Survey of Laboratory Testing Practices for C. difficile Infection, CDI Annual Surveillance Officers Survey, Emerging Infections Program C. difficile Surveillance Nursing Home Telephone Survey, Candidemia Periodic Laboratory Survey,- the HAIC Staphylococcus aureus Laboratory Survey: Use of Nucleic Acid Amplification Testing (NAAT) and Invasive Staphylococcus aureus Supplemental Surveillance Officers Survey. These forms will allow the EIP to better detect, identify, track changes in laboratory testing methodology, gather information about laboratory utilization in the EIP catchment area to ensure that all cases are being captured and survey EIP staff to evaluate program quality. Details of each collection instrument for the revision is as follows:

  • ABCs Case Report Form – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • ABCs Invasive Pneumococcal Disease in Children Case Report Form – For this revision, no change to content or burden.

  • ABCs H. influenzae Neonatal Sepsis Expanded Surveillance Form (HiNSES)— A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • ABCs Neonatal Infection Expanded Tracking Form – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • ABCs Severe GAS Infection Supplemental Form – For this revision, no change to content or burden.

  • Legionellosis Expanded Case Report Form – For this revision, no change to content or burden.

  • FoodNet Active Surveillance Data Elements – A non-substantive change request was OMB approved on 05/05/2017. In summary, in January 2018, transmission of Cryptosporidium cases were suspended. In addition, 5 data elements related to case exposure ascertainment were suspended. In this revision, two data elements were added to capture information on homelessness and census tract for sites in which these elements can be mapped and transmitted. The overall increase in burden represents an estimated total of 211 hours.

  • FoodNet Hemolytic Uremic Syndrome Case Report Form – A non-substantive change request was OMB approved on 05/05/2017. In summary, that non-substantive change request added 3 new site-transmitted variables to our HUS case report form. In this revision no changes were made and there is no change to burden.

  • FoodNet Clinical Laboratory Practices and Testing Volume Data Elements — Added to this revision in 2019, in order to collect information on clinical laboratory practices and testing volume to inform changes in trends of enteric disease, 89 data elements were added, of which a subset have been collected since 2012. The increase in burden represents an estimated total of 233 hours.

  • FluSurv-NET – Case Report Form – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • FluSurv- NET – Vaccination Phone Script Consent Form (English/Spanish) – For this revision, no change to content or burden.

  • FluSurv-NET – Vaccination Phone Script (English/Spanish) – For this revision, no change to content or burden.

  • FluSurv-NET Provider Vaccination History Fax Form (Children/Adults) – For this revision, no change to content or burden.

  • FluSurv-NET Laboratory Survey – For this revision, a new form has been added to inform about testing practices for influenza and other respiratory viruses including resulting in an increase of 38 burden hours.

  • C. difficile infection (CDI) Surveillance Case Report Form – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • Annual Survey of Laboratory Testing Practices for C. difficile Infection – This is a new form for total burden of 27 hours.

  • CDI Annual Surveillance Officers Survey – This is a new form with a total of 2 burden hours.

  • Emerging Infections Program C. difficile Surveillance Nursing Home Telephone Survey – This is a new data collection with 38 burden hours.

  • Multi-site Gram-Negative Surveillance Initiative – (MuGSI-CRE/CRAB) – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • Multi-site Gram-Negative Surveillance Initiative – Carbapenem-resistant Pseudomonas aeruginosa (MuGSI-CR-PA) – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • Multi-site Gram-Negative Surveillance Initiative – Extended-Spectrum Beta-Lactamase-Producing Enterobacteriaceae (ESBL) – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • Methicillin-resistant Staphylococcus aureus (MRSA) Case Report Form – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • Methicillin-sensitive Staphylococcus aureus (MSSA) Case Report Form – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • Staphylococcus aureus Laboratory Survey: Use of Nucleic Acid Amplification Testing (NAAT) – This is a new form with a total of 15 burden hours.

  • Invasive Staphylococcus aureus Supplemental Surveillance Officer Survey – This is a new form with a total of 2 burden hours.

  • Candidemia Case Report Form – A non-substantive change request was OMB approved on 9/13/2018. There is no change to the burden for this revision.

  • Candidemia Periodic Laboratory Survey – This is a new form with a total of 45 burden hours.

  1. Plans for Tabulation and Publication and Project Time Schedule

For ABCs, CDC will provide each surveillance area with several forms of feedback including data integrity checks and summary tables. Specifically, data from multiple sites will be concatenated approximately 3 weeks after receipt at CDC. Feedback from sites to local hospitals, laboratories, and other constituents is at the discretion of each site.


CDC generates pathogen-specific ABCs surveillance reports annually in October (http://www.cdc.gov/ncidod/dbmd/abcs/survreports.htm). CDC also summarizes data for presentation in written manuscripts for peer-reviewed journals, and at national and local scientific meetings. These analyses are on-going throughout the calendar year.


For FoodNet, surveillance data are reviewed monthly at CDC, and published yearly in an MMWR and an annual report, and online through a web-based interface (https://wwwn.cdc.gov/foodnetfast/).


For FluSurv-NET, prospective surveillance will be conducted for hospital admissions occurring each influenza season between October 1 and April 30.


Activity

Time Schedule

Begin prospective case finding and chart review

October 1


Weekly: sites send data to CDC

October 1- April 30


End prospective case finding

April 30


Sites submit finalized prospective data to CDC

September 30


Data Analysis

Continuous throughout and following data collection

Presentation of findings

Continuous throughout and following data collection

Manuscript Preparation

Continuous throughout and following data collection


For HAIC, CDC provides each EIP site with several forms of feedback including data integrity checks. HAIC staff members at CDC and in the sites are engaged in an ongoing fashion in data analysis, and it is routine each year (throughout the year) for several abstracts and papers to be presented at national meetings and published in peer-reviewed journals. Feedback from sites to local hospitals, laboratories, and other constituents is at the discretion of each site. CDC also produces an annual report for CDI (https://www.cdc.gov/hai/eip/clostridium-difficile.html) and MRSA (https://www.cdc.gov/hai/eip/saureus.html). HAIC’s Annual Laboratory Surveys for invasive S. aureus and CDI are conducted annually. Laboratory outreach is planned annually for Gram-negative surveillance. The HAIC Candidemia Periodic Laboratory Survey is conducted approximately every three years. The invasive S. aureus and the CDI Annual Surveillance Officers survey is conducted annually. The CDI LTCF survey is also conducted annually. The data collected from these survey tools are used to inform surveillance, to ensure standard data collection practice and data quality. These data are not collected for the sole purpose of publishing, although data elements that are collected could be used to inform data analysis or appear in a publication.


EIP will be developing an approach to (or guidance for) making EIP datasets publicly available, in accordance with recently issued requirements. The policy at CDC (SDAP – Scientific Data Access Project) is still new and precisely what is required and by when appears to be still under discussion. A plan will be forthcoming.


  1. Reasons Display of OMB Expiration Date is Inappropriate

Data collections for ABCs and HAIC forms remain constant from one expiration date to the next. In order to make the most efficient use of the forms that have already been distributed to state health department personnel we request that the OMB expiration date not be printed on these forms. Therefore, the display of the OMB expiration date is not appropriate. For FoodNet and FluSurv-NET the expiration date will be displayed.

  1. Exceptions to Certification for Paperwork Reduction Act Submissions

There are no exceptions to the Paperwork Reduction Act Submission certification.

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