Emerging Infections Program (EIP)
Non-substantive Change Request
January 2015
Amy McMillen, MPH
Centers for Disease Control and Prevention
National Center for Emerging and Zoonotic Infectious Diseases
Office of the Director
1600 Clifton Rd
Atlanta GA 30333
404-639-1045
Background
The National Center for National Center for Emerging and Zoonotic Infectious Diseases (NCEZID) of the Centers for Disease Control and Prevention (CDC) is requesting approval of a non-substantive change to the approved package under OMB no. 0920-0978; expiration date 8/31/2016.
These forms are used to conduct surveillance to determine the incidence and epidemiologic characteristics of invasive disease due to Haemophilus influenzae, Neisseria meningitidis, group A Streptococcus, group B Streptococcus, and Streptococcus pneumoniae., specific foodborne diseases that is captured within FoodNet, and Influenza (specifically for the All Age Influenza Hospitalization Surveillance (Flu Hosp) project).
The forms for which approval for changes and additions are being sought include:
2015 ABCs Case Report Form — (Attachment 1)
2015 ABCs Neonatal Infection Expanded Tracking Form — (Attachment 2 )
New Form: 2014 ABCs Non Bacteremic Pneumococcal Disease— (Attachment 3)
2015 FoodNet Variable list — (Attachment 4)
2014-2015 FluSurv-NET Influenza Surveillance Project Case Report Form — (Attachment 5)
2014-2015 FluSurv-NET Influenza Surveillance Project Vaccination History Telephone Survey — (Attachment 6)
2014-2015 FluSurv-NET Influenza Surveillance Project Vaccination History Telephone Survey (Spanish) — (Attachment 7)
2014-2015 FluSurv-NET Influenza Surveillance Project Consent Form — (Attachment 8)
2014-2015 FluSurv-NET Influenza Surveillance Project Consent Form (Spanish) — (Attachment 9)
The changes in this package are minor, do not change the scope of a collection, and does not greatly impact the burden. The following will detail the changes to the EIP surveillance tools including description and crosswalk of changes.
Active Bacterial Core surveillance (ABCs) - Active population-based laboratory surveillance for invasive bacterial diseases
Detailed Description of Changes
2015 ABCs Case Report Form
There is no impact on burden due to the changes on this form. The changes include:
Question 32, Receipt of pneumococcal vaccine
Directions below checkboxes will be changed to ‘If between ≥ 3 months and <5 years of age and an isolate is available for serotyping, please complete the Invasive Pneumococcal Disease in Children expanded form’
2015 ABCs Invasive Pneumococcal Disease in Children Case Report Form
Burden is decreasing as data elements have been removed from the data collection tool
These changes include:
Removed capture of manufacturer and vaccine name for Diptheria/Tetanus/Pertussis (DTP or DTaP)
Removed capture of manufacturer and vaccine name for Haemophilis influenza type B (Hib)
Removed rows capturing influenza immunizations
Added section on data sources for vaccination history, including
What information source was used to identify the health provider
How many health providers were contacted
What information sources were used to obtain vaccination history
2015 ABCs Non-Bacteremic Case Report Form Active Bacterial Core surveillance (ABCs), a part of the Emerging Infections Program (EIP) network, is an active, laboratory, and population-based surveillance system. It is used to determine the incidence and epidemiological characteristics of invasive disease due to group A Streptococcus (GAS), group B Streptococcus (GBS), Streptococcus pneumoniae, Haemophilus influenzae, and Neisseria meningitidis, at 10 sites located throughout the United States. Since ABCs surveillance began in 1995, a case of invasive bacterial disease has been defined as isolation from culture of one of these pathogens from a normally sterile site in a resident of the surveillance area. Data from ABCs have been used to inform the development of vaccines, to inform the Advisory Committee on Immunization Practices (ACIP) recommendations for their use and to evaluate their effectiveness after recommendations for use are in place.
On August 13, 2014, ACIP recommended routine use of 13-valent pneumococcal conjugate vaccine (PCV13) among adults aged ≥65 years in series with the 23-valent pneumococcal polysaccharide vaccine (PPSV23).1 Both vaccines have demonstrated efficacy against invasive pneumococcal disease (IPD) in placebo-controlled trials. One of the determining factors for recommending PCV13 to adults aged ≥65 years was its demonstrated 45% efficacy (95% confidence interval=14-65%) against vaccine-type non-bacteremic (i.e. non-invasive) pneumococcal pneumonia (NBPP) in a placebo-controlled trial conducted in the Netherlands.2 Evidence is less clear as to whether PPSV23 is effective against NBPP. The incidence of NBPP and the effectiveness of PCV13 vaccine against NBPP have a major influence on determining which vaccine or combination of vaccines would provide the greatest health benefits at the lowest costs. Given these and other considerations, ABCs Non-Bacteremic surveillance responds to the ACIP recommendations for the need to re-evaluate the pneumococcal vaccine policy for adults in 2018.
Cross walk of 2015 form changes
2015 ABCs Case Report Form
2014 form |
2015 form |
32. Did the patient receive pneumococcal vaccination? 1 □ Yes 2 □ No 9 □ Unknown
If YES, please note which pneumococcal vaccine was received (Check all that apply) 1 □ Prevnar®, 7-valent Pneumococcal Conjugate Vaccine (PCV7) 1 □ Prevnar-13®, 13-valent Pneumococcal Conjugate Vaccine (PCV13) 1 □ Pneumovax®, 23-valent Pneumococcal Polysaccharide Vaccine (PPV23) 1 □ Vaccine type not specified
If between ≥3 months and <18 years of age and an isolate is available for serotyping, please complete the Invasive Pneumococcal Disease in Children expanded form.
|
32. Did the patient receive pneumococcal vaccination? 1 □ Yes 2 □ No 9 □ Unknown
If YES, please note which pneumococcal vaccine was received (Check all that apply) 1 □ Prevnar®, 7-valent Pneumococcal Conjugate Vaccine (PCV7) 1 □ Prevnar-13®, 13-valent Pneumococcal Conjugate Vaccine (PCV13) 1 □ Pneumovax®, 23-valent Pneumococcal Polysaccharide Vaccine (PPV23) 1 □ Vaccine type not specified
If between ≥ 2 months and <5 years of age and an isolate is available for serotyping, please complete the Invasive Pneumococcal Disease in Children expanded form.
|
2015 ABCs Invasive Pneumococcal Disease Case Report Form
2014 form |
2015 form |
Title: Active Bacterial Core Surveillance (ABCs) Invasive Pneumococcal Disease in Children |
Title: Active Bacterial Core Surveillance (ABCs) Invasive Pneumococcal Disease in Children (aged ≥2 months to <5 years) |
Indicate manufacturer for Diptheria/Tetanus/Pertussis (DTP or DTap) |
Removed |
Indicate vaccine name for Diptheria/Tetanus/Pertussis (DTP or DTap) |
Removed |
Indicate manufacturer for Haemophilus influenzae type B (Hib) |
Removed |
Indicate vaccine name for Haemophilus influenzae type B (Hib) |
Removed |
Indicate dates of immunization for influenza vaccine |
Removed |
Indicate manufacturer for influenza vaccine |
Removed |
Indicate vaccine name for influenza vaccine |
Removed |
|
Was health care provider information available from the following sources?
Medical chart: □ Yes □ No □ Did not check
Vaccine Registry: □ Yes □ No □ Did not check
Parent/Guardian: □ Yes □ No □ Did not check □ Refused |
|
If yes to any sources, how many providers were contacted? |
|
What sources were used for vaccination history?
Medical chart: □ Yes □ No □ Did not check
Vaccine Registry: □ Yes □ No □ Did not check
Primary Care Provider: □ Yes □ No □ Did not check
Other Provider: □ Yes □ No □ Did not check
|
ABCs Change Estimates of Annualized Burden Hours from 2014 to 2015
Table A.1 Estimated Annualized Burden Hours(Highlighted forms below indicate a change in burden hours in 2015)
Type of Respondent |
Form Name |
No. of respondents |
No. of responses per respondent |
Avg. burden per response (in hours) |
2015 Total burden (in hours) |
State Health Department
|
ABCs Case Report Form |
10 |
809 |
20/60 |
2697 |
Invasive Methicillin-resistant Staphylococcus aureus ABCs Case Report Form |
10 |
609 |
20/60 |
2030 |
|
ABCs Invasive Pneumococcal Disease in Children Case Report Form |
10 |
22 |
10/60 |
37 |
|
New Form: ABCs Non-Bacteremic Pneumococcal Disease Case Report Form |
10 |
100 |
10/60 |
167 |
|
Neonatal Infection Expanded Tracking Form |
10 |
37 |
20/60 |
123 |
|
ABCs Legionellosis Case Report Form |
10 |
100 |
20/60 |
333 |
Foodborne Diseases Active Surveillance Network (FoodNet)
Minor revisions have been made to the FoodNet surveillance tool since the last change approval in 2014; however the changes did not result in a change to estimated burden hours for those forms.
Detailed Description of Changes
Expanded the list of responses for ‘AgClinicTestType’ to reflect new tests that are now being used in clinical labs.
Added two new variables related to culture-independent testing for STEC:
DXO157
DXO157TestType
Added the following new variables to capture case exposure information to be used for attribution estimates. These variables were developed by a working group consisting of CDC and state health department sites over a two-year period. Variables were pilot-tested in 4 sites for a three-month period for Salmonella and Campylobacter cases.
Meat and poultry
CEA_Beef
CEA_Beef_grnd
CEA_Beef_out
CEA_Beef_unckgrnd
CEA_Chicken
CEA_Chx_grnd
CEA_Chx_out
CEA_Pork
CEA_Turkey
CEA_Turkey_grnd
CEA_Turkey_out
Fish and seafood
CEA_Fish
CEA_Fish_unck
CEA_Seafd
CEA_Seafd_unck
Dairy
CEA_Dairy
CEA_Milk_raw
CEA_Odairy_raw
CEA_Softcheese
CEA_Softcheese_raw
Eggs
CEA_Eggs
CEA_Eggs_out
CEA_Eggs_unck
Fruits and vegetables
CEA_Berries
CEA_Cantaloupe
CEA_Herbs
CEA_Lettuce
CEA_Spinach
CEA_Sprouts
CEA_Raw_cider
CEA_Tomatoes
CEA_Watermelon
Water
CEA_Ountreat_water
CEA_Sewer_water
CEA_Swim_treat
CEA_Swim_untreat
CEA_Well_water
Person-to-person
CEA_Sick_contact
Environmental
CEA_Bird
CEA_Cat
CEA_Dog
CEA_Farm_ranch
CEA_Live_poultry
CEA_Pig
CEA_Pocketpet
CEA_Reptile_amphib
CEA_Ruminants
CEA_Sick_pet
Influenza - All Age Influenza Hospitalization Surveillance Project
Minor revisions have been made to the FluSurv-NET Influenza Surveillance tool since the last change approval in 2014; however the changes did not result in a change to estimated burden hours for those forms.
Detailed Description of Changes
2014-15 FluSurv-NET Influenza Surveillance Project_Case Report Form
A question was added to capture the type of address provided for the patient.
Additional questions were added to capture additional patient provider contact information.
To better capture information on where the patient resided at the time of, additional residence type options for question C13 were added.
Questions regarding Influenza testing results were updated to include new influenza testing types and corresponding result options.
To better capture information regarding signs/symptoms at the time of admission, question E2 was rephrased to list signs/symptoms as they appear in medical chart – but original intent of question was preserved.
The options for specifying location of consolidation was removed from questionnaire.
The section on vaccination status has now an option to record type of vaccination (injected or nasal spray) for children <9 years of age.
2014-2015 FluSurv-NET Influenza Surveillance Project_Vaccination History Telephone Survey
(Changes Account for the English and Spanish Version)
Addition of a question to capture the type of vaccination (injected or nasal spray) received by patients <9 years of age.
2014-2015 FluSurv-NET Influenza Surveillance Project_Consent Form
(Changes Account for the English and Spanish Version)
Location of reference material for continuation of interview was updated to reflect current location.
Cross walk of 2015 form changes
2014-15 FluSurv-NET Influenza Surveillance Project_Case Report Form
Question on 2013-14 Form |
Question on 2014-15 Form |
N/A |
A10. Address Type: ___________ |
N/A |
A16. Primary Provider (PCP) Name 2: ______________ |
N/A |
A17. Primary Provider (PCP) Phone 2: ______________ |
N/A |
A18. Primary Provider (PCP) Fax2: ______________ |
E13. Where did patient reside at the time of hospitalization? Private residence Rehabilitation facility Group home/Retirement home Assisted living/Residential care Homeless/Shelter Nursing home Unknown Other, specify: _____________________ |
E13. Where did patient reside at the time of hospitalization? Private residence Alcohol/Drug Abuse Treatment Group home/Retirement home Homeless/Shelter Hospitalized at birth Jail/Prison LTACH/Transitional Care (TCU) Mental Hospital Nursing home Rehabilitation facility Hospice Unknown Other, specify: ___________________ |
D1-4. Test 1-4: Rapid RT-PCR Viral Culture Serology Fluorescent Antibody Method Unknown/Note Only |
D1-4. Test 1-4: Rapid Molecular Assay Viral Culture Serology Fluorescent Antibody Method Unknown/Note Only |
D1a-4a. Result: Flu A (not subtyped) Flu B Flu A & B Flu A/B (Not Distinguished) 2009 H1N1 H1, Seasonal H1, Unspecified H3 Flu A, Unsubtypable Negative Unknown Other, specify: __________________________ |
D1a-4a. Result: Flu A (no subtype) Flu B(no genotype) Flu A & B Flu A/B (Not Distinguished) 2009 H1N1 H1, Unspecified H3 Flu A, Unsubtypable Flu B, Yamagata Flu B, Victoria Negative Unknown Type Other, specify: __________________________ |
E2. Acute conditions at admission (Check all that apply): Acute respiratory illness Asthma and/or COPD exacerbation Fever Pneumonia Other respiratory or cardiac conditions Other, neither respiratory nor cardiac conditions Unknown
|
E2. Acute signs/symptoms at admission [within 2 weeks prior to positive flu test]: Altered mental status/confusion Chest pain Congested/runny nose Conjunctivitis/pink eye Cough Diarrhea Fever/chills Headache Myalgia/muscle aches Nausea/vomiting Rash Seizures Shortness of breath/resp distress Sore throat Wheezing Other, non-respiratory |
E3. Date of onset of acute respiratory symptoms: ____/ ____/ ____ Unknown |
E3. Date of onset of acute respiratory symptoms [within 2 weeks prior to positive flu test]: ____/ ____/ ____ Unknown |
E3a. If no respiratory symptoms, date of onset of acute illness resulting in hospitalization: ____/ ____/ ____ Unknown |
E4. Date of onset of acute condition resulting in current hospitalization: ____/ ____/ ____ Unknown |
E9i. Immunocompromised Condition Yes No/Unknown AIDS or CD4 count < 200 Cancer diagnosis in last 12 months Complement deficiency HIV Infection Immunoglobulin deficiency Immunosuppressive therapy Organ transplant Stem cell transplant (e.g., bone marrow transplant) Steroid therapy (taken within 2 weeks of admission) Other, specify__________________ |
E10i. Immunocompromised Condition Yes No/Unknown AIDS or CD4 count < 200 Cancer: current/in treatment or diagnosed in last 12 months Complement deficiency HIV Infection Immunoglobulin deficiency Immunosuppressive therapy Organ transplant Stem cell transplant (e.g., bone marrow transplant) Steroid therapy (taken within 2 weeks of admission) Other, specify__________________
|
E9k. Other Yes No/Unknown Liver disease (e.g., cirrhosis, chronic hepatitis, hepatitis C) Morbidly obese (ADULTS ONLY) Obese Pregnant If pregnant, specify gestational age in weeks: ________ Unknown gestational age Post-partum (two weeks or less) Other, specify _______________ |
E10k. Other Yes No/Unknown Intravenous drug use Liver disease (e.g., cirrhosis, chronic hepatitis, hepatitis C) Systemic lupus erythematosus/SLE/Lupus Morbidly obese (ADULTS ONLY) Obese Pregnant If pregnant, specify gestational age in weeks: ________ Unknown gestational age Post-partum (two weeks or less) Other, specify _______________ |
H1f. Human metapneumovirus Yes, positive Yes, negative Not tested/Unknown Date: ____/____/____ |
H1f. Parainfluenza 4 Yes, positive Yes, negative Not tested/Unknown Date: ____/____/____ |
H1g. Rhinovirus Yes, positive Yes, negative Not tested/Unknown Date: ____/____/____ |
H1g. Human metapneumovirus Yes, positive Yes, negative Not tested/Unknown Date: ____/____/____ |
H1h. Other, specify: ______________ Yes, positive Yes, negative Not tested/Unknown Date: ____/____/____ |
H1h. Rhinovirus/Enterovirus Yes, positive Yes, negative Not tested/Unknown Date: ____/____/____ |
N/A |
H1i.Coronavirus (type):____________ Yes, positive Yes, negative Not tested/Unknown Date: ____/____/____ |
J2c. Please specify location for bronchopneumonia/pneumonia/consolidation/lobar infiltrate/air space density/opacity: Single lobar Multiple lobar (unilateral) Multiple lobar (bilateral) Unknown |
Removed |
K2a. If discharged alive, please indicate to where: Home Other hospital Hospice/Home hospice Homeless/Shelter Rehabilitation Facility Group home/Retirement home Assisted living/Residential Care Home with Services Nursing home Unknown Other, specify: _____________________ |
K2a. If discharged alive, please indicate to where: Private residence Alcohol/Drug Abuse Treatment Assisted living/Residential Care Group home/Retirement home Home with Services Homeless/Shelter Jail/Prison LTACH/Transitional Care (TCU) Mental Hospital Nursing home Rehabilitation Facility Hospice Unknown Other, specify: ________________ |
M1. Did patient receive the influenza vaccine for the current influenza season? Yes No Unknown |
Removed |
M2-M6. [vaccination history source] Yes Yes, specific date unknown No Unknown Not Checked |
M1-M4. [vaccination history source] Yes, full date known Yes, specific date unknown No Unknown Not Checked |
N/A |
M1b-M4b. If patient < 9 yrs, specify vaccine type: Injected Vaccine Nasal Spray/FluMist Combination of both Unknown type
|
2014-2015 FluSurv-NET Influenza Surveillance Project_Vaccination History Telephone Survey
Question on 2013-14 Survey |
Question on 2014-15 Survey |
N/A |
1b) What type of flu vaccine did [you / child’s name] receive? Injected Vaccine Nasal Spray/FluMist Combination of both Unknown type
|
2014-2015 FluSurv-NET Influenza Surveillance Project_Consent Form
Question on 2013-14 Consent Form |
Question on 2014-15 Consent Form |
Hello. My name is __________ from the _____[state] Department of Public Health. May I speak to ______ [patient’s name /parent of [child’s name] ] . We are working with the Centers for Disease Control and Prevention and other health departments to learn more about influenza disease or the flu. To do this, we are talking to people who have been in the hospital with the flu. We want to look at things that may affect their illness and whether they were vaccinated against the flu.
Because you/your child [or NAME if speaking with proxy] were in the hospital for the flu beginning on _______[day admitted], I would like to ask you a few questions about whether you/your child [or NAME if speaking with proxy] received the flu vaccine this season. This will take about five minutes. Your participation is voluntary and if you choose to refuse it will not affect any medical care or benefits you receive. All of your responses will be kept confidential as much as the law allows. You may refuse to answer any questions and may stop at any time. This information will help [State/Local Health Department] and CDC better describe influenza-associated hospitalizations. Additionally, this information may help us improve vaccination recommendations for flu and better protect the public’s health. There is no other benefit to you for answering these questions. There is also no risk to you. If you have any questions about the study, you may call _____[state contact] at the Department of Public Health at XXX-XXX-XXXX. Do you have any questions before I begin? May I continue with this interview? □ Yes □ No If YES, go to Appendix F. If NO: Thank you for your time. Have a good day |
Hello. My name is __________ from the _____[state] Department of Public Health. May I speak to ______ [patient’s name /parent of [child’s name] ] . We are working with the Centers for Disease Control and Prevention and other health departments to learn more about influenza disease or the flu. To do this, we are talking to people who have been in the hospital with the flu. We want to look at things that may affect their illness and whether they were vaccinated against the flu.
Because you/your child [or NAME if speaking with proxy] were in the hospital for the flu beginning on _______[day admitted], I would like to ask you a few questions about whether you/your child [or NAME if speaking with proxy] received the flu vaccine this season. This will take about five minutes. Your participation is voluntary and if you choose to refuse it will not affect any medical care or benefits you receive. All of your responses will be kept confidential as much as the law allows. You may refuse to answer any questions and may stop at any time. This information will help [State/Local Health Department] and CDC better describe influenza-associated hospitalizations. Additionally, this information may help us improve vaccination recommendations for flu and better protect the public’s health. There is no other benefit to you for answering these questions. There is also no risk to you. If you have any questions about the study, you may call _____[state contact] at the Department of Public Health at XXX-XXX-XXXX. Do you have any questions before I begin? May I continue with this interview? □ Yes □ No If YES, go to Appendix 7. If NO: Thank you for your time. Have a good day. |
| File Type | application/vnd.openxmlformats-officedocument.wordprocessingml.document |
| Author | CDC User |
| File Modified | 0000-00-00 |
| File Created | 2021-01-20 |