Form 1 Draft 2450 r4. Post-TED form

Stem Cell Therapeutic Outcomes Database

Draft 2450 r4. Post-TED form

Stem Cell Therapeutic Outcomes Database (Post-Trans)

OMB: 0915-0310

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PowerPlusWaterMarkObject357831064 CIBMTR Center Number: ___ ___ ___ ___ ___ CIBMTR Research ID: ___ ___ ___ ___ ___ ___ ___ ___ ___ ___


R

OMB No: 0915-0310

Expiration Date:


Public Burden Statement: An agency may not conduct or sponsor, and a person is not required to respond to, a collection of information unless it displays a currently valid OMB control number. The OMB control number for this project is 0915-0310. Public reporting burden for this collection of information is estimated to average 1.25 hours per response when collected at 100 days post-transplant, 1.15 hours per response when collected at 6 and 12 months post-transplant, and 1.15 hours per response annually thereafter, including the time for reviewing instructions, searching existing data sources, and completing and reviewing the collection of information. Send comments regarding this burden estimate or any other aspect of this collection of information, including suggestions for reducing this burden, to HRSA Reports Clearance Officer, 5600 Fishers Lane, Room 10-33, Rockville, Maryland, 20857.


egistry Use Only

Sequence Number:









Date Received:





CIBMTR Center Number: ___ ___ ___ ___ ___

CIBMTR Research ID: ___ ___ ___ ___ ___ ___ ___ ___ ___ ___

Event date: ___ ___ ___ ___ - ___ ___ - ___ ___

YYYY MM DD

HCT type: (check all that apply)

Autologous

Allogeneic, unrelated

Allogeneic, related

Product type: (check all that apply)

Bone marrow

PBSC

Single cord blood unit

Multiple cord blood units

Other product

Specify: ____________________________________

Visit:

100 day

6 months

1 year

2 years

>2 years,

Specify: ___ ___











Survival

  1. Date of actual contact with the recipient to determine medical status for this follow-up report: ___ ___ ___ ___ — ___ ___ — ___ ___

  2. Specify the recipient’s survival status at the date of last contact:

Alive - Answers to subsequent questions should reflect clinical status since the date of last report.- Go to question 7

Dead - Answers to subsequent questions should reflect clinical status between the date of last report and immediately prior to death - Go to question 3

  1. Primary cause of death

Recurrence / persistence / progression of disease for which the HCT or cellular therapy was performed – Go to question 5

Acute GVHD – Go to question 5

Chronic GVHD – Go to question 5

 Graft rejection or failure – Go to question 5

Cytokine release syndrome – Go to question 5

Infection

 Infection, organism not identified – Go to question 5

 Bacterial infection – Go to question 5

 Fungal infection – Go to question 5

 Viral infection – Go to question 5

 Protozoal infection – Go to question 5

 Other infection – Go to question 4

Pulmonary

Idiopathic pneumonia syndrome (IPS) – Go to question 5

Pneumonitis due to Cytomegalovirus (CMV)– Go to question 5

 Pneumonitis due to other virus – Go to question 5

Other pulmonary syndrome (excluding pulmonary hemorrhage) – Go to question 4

Diffuse alveolar damage (without hemorrhage) – Go to question 5

Adult respiratory distress syndrome (ARDS) (other than IPS) – Go to question 5

Organ failure (not due to GVHD or infection)

Liver failure (not VOD) – Go to question 5

Veno-occlusive disease (VOD) / sinusoidal obstruction syndrome (SOS) – Go to question 5

Cardiac failure – Go to question 5

 Pulmonary failure– Go to question 5

 Central nervous system (CNS) failure – Go to question 5

 Renal failure – Go to question 5

Gastrointestinal (GI) failure (not liver) – Go to question 5

Multiple organ failure – Go to question 4

Other organ failure – Go to question 4

Malignancy

New malignancy (post-HCT or post-cellular therapy) – Go to question 5

Prior malignancy (malignancy initially diagnosed prior to HCT or cellular therapy, other than the malignancy for which the HCT or cellular therapy was performed) – Go to question 5

Hemorrhage

Pulmonary hemorrhage – Go to question 5

Diffuse alveolar hemorrhage (DAH) – Go to question 5

Intracranial hemorrhage – Go to question 5

Gastrointestinal hemorrhage – Go to question 5

Hemorrhagic cystitis – Go to question 5

Other hemorrhage – Go to question 4

Vascular

Thromboembolic – Go to question 5

Disseminated intravascular coagulation (DIC) – Go to question 5

Thrombotic microangiopathy (TMA) (Thrombotic thrombocytopenic purpura (TTP)/Hemolytic Uremic Syndrome (HUS))– Go to question 5

Other vascular - Go to question 4

Other

Accidental death – Go to question 5

Suicide – Go to question 5

Other cause - Go to question 4

  1. Specify:

  2. Contributing cause of death

Recurrence / persistence / progression of disease for which the HCT or cellular therapy was performed – Go to question 7

Acute GVHD – Go to question 7

Chronic GVHD – Go to question 7

Graft rejection or failure – Go to question 7

Cytokine release syndrome – Go to question 7

Infection

 Infection, organism not identified – Go to question 7

 Bacterial infection – Go to question 7

 Fungal infection – Go to question 7

 Viral infection – Go to question 7

 Protozoal infection – Go to question 7

 Other infection – Go to question 6

Pulmonary

Idiopathic pneumonia syndrome (IPS) – Go to question 7

Pneumonitis due to Cytomegalovirus (CMV) – Go to question 7

 Pneumonitis due to other virus – Go to question 7

Other pulmonary syndrome (excluding pulmonary hemorrhage) – Go to question 6

Diffuse alveolar damage (without hemorrhage) – Go to question 7

Adult respiratory distress syndrome (ARDS) (other than IPS) – Go to question 7

Organ failure (not due to GVHD or infection)

Liver failure (not VOD) – Go to question 7

Veno-occlusive disease (VOD) / sinusoidal obstruction syndrome (SOS) – Go to question 7

Cardiac failure – Go to question 7

 Pulmonary failure– Go to question 7

 Central nervous system (CNS) failure – Go to question 7

 Renal failure – Go to question 7

Gastrointestinal (GI) failure (not liver) – Go to question 7

Multiple organ failure – Go to question 6

Other organ failure – Go to question 6

Malignancy

New malignancy (post-HCT or post-cellular therapy) – Go to question 7

Prior malignancy (malignancy initially diagnosed prior to HCT or cellular therapy, other than the malignancy for which the HCT or cellular therapy was performed) – Go to question 7

Hemorrhage

Pulmonary hemorrhage – Go to question 7

Diffuse alveolar hemorrhage (DAH) – Go to question 7

Intracranial hemorrhage – Go to question 7

Gastrointestinal hemorrhage – Go to question 7

Hemorrhagic cystitis – Go to question 7

Other hemorrhage – Go to question 6

Vascular

Thromboembolic – Go to question 7

Disseminated intravascular coagulation (DIC) – Go to question 7

Thrombotic microangiopathy (TMA) (Thrombotic thrombocytopenic purpura (TTP)/Hemolytic Uremic Syndrome (HUS)) – Go to question 7

Other vascular - Go to question 6

Other

Accidental death – Go to question 7

Suicide – Go to question 7

Other cause - Go to question 6

  1. Specify:_______________________________________________________________________

If reporting more than one contributing cause of death, copy questions 5-6 and complete for each contributing cause.



Subsequent Transplant

  1. Did the recipient receive a subsequent HCT since the date of last report?

 Yes – Go to question 8

 No - Go to question 12

  1. Date of subsequent HCT: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD

  1. What was the indication for subsequent HCT?

Graft failure / insufficient hematopoietic recovery - Allogeneic HCTs Complete a Pre-TED Form 2400 for the subsequent HCTGo to question 11

Persistent primary disease – Complete a Pre-TED Form 2400 for the subsequent HCTGo to question 11

Recurrent primary disease – Complete a Pre-TED Form 2400 for the subsequent HCTGo to question 11

Planned second HCT, per protocol – Complete a Pre-TED Form 2400 for the subsequent HCTGo to question 11

New malignancy (including PTLD and EBV lymphoma) – Complete a Pre-TED Form 2400 for the subsequent HCTGo to question 11

Insufficient chimerism – Complete a Pre-TED Form 2400 for the subsequent HCT Go to question 11

Other – Complete a Pre-TED Form 2400 for the subsequent HCT Go to question 10

  1. Specify other indication: ___________________

  2. Source of HSCs:

Allogeneic, related - Allogeneic HCTs Complete a Pre-TED Form 2400 for the subsequent HCT

Allogeneic, unrelated – Complete a Pre-TED Form 2400 for the subsequent HCT

 Autologous

  1. Has the recipient received a cellular therapy since the date of last report? (e.g. DCI)

Yes – Go to question 13– Also complete Cellular Therapy Essential Data Pre-Infusion Form 4000

No – Go to question 14

  1. Date of cellular therapy: ___ ___ ___ ___ - ___ ___ - ___ ___

Initial ANC Recovery

  1. Was there evidence of initial hematopoietic recovery?

Yes (ANC ≥ 500/mm3 achieved and sustained for 3 lab values) – Go to question 15

No (ANC ≥ 500/mm3 was not achieved) – Go to question 16

Not applicable (ANC never dropped below 500/mm3 at any time after the start of the preparative regimen) – Go to question 16

Previously reported (recipient’s initial hematopoietic recovery was recorded on a previous report) – Go to question 16

  1. Date ANC ≥ 500/mm3 (first of 3 lab values): ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD

  1. Did late graft failure occur?

Yes

No



Initial Platelet Recovery

(Optional for Non-U.S. Centers)

  1. Was an initial platelet count ≥ 20 x 109/L achieved?

Yes – Go to question 18

No – Go to question 19

Not applicable - Platelet count never dropped below 20 x 109/L – Go to question 19

Previously reported - ≥ 20 x 109/L was achieved and reported previously – Go to question 19

  1. Date platelets ≥ 20 x 109/L: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD



Graft vs. Host Disease

This section is for allogeneic HCTs only. If this was an autologous HCT, continue to Liver Toxicity Prophylaxis.

  1. Did acute GVHD develop since the date of last report?

Yes– Go to question 20

No – Go to question 21

Unknown – Go to question 21

  1. Date of acute GVHD diagnosis: ___ ___ ___ ___ — ___ ___ — ___ ___ - Go to question 22

YYYY MM DD

  1. Did acute GVHD persist since the date of last report?

Yes– Go to question 29

No – Go to question 31

Unknown – Go to question 31

  1. Overall grade of acute GVHD at diagnosis:

I - Rash on ≤ 50% of skin, no liver or gut involvement

II - Rash on > 50% of skin, bilirubin 2-3 mg/dL, or diarrhea 500 – 1000 mL/day or persistent nausea

III - Bilirubin 3-15 mg/dL, or gut stage 2-4 diarrhea > 1000 mL/day or severe abdominal pain with or without ileus

IV - Generalized erythroderma with bullous formation, or bilirubin >15 mg/dL

Not applicable (acute GVHD present but grade is not applicable)

List the stage for each organ at diagnosis of acute GVHD:

  1. Skin:

Stage 0 – no rash, no rash attributable to acute GVHD

Stage 1 – maculopapular rash, < 25% of body surface

Stage 2 – maculopapular rash, 25–50% of body surface

Stage 3 – generalized erythroderma, > 50% of body surface

Stage 4 – generalized erythroderma with bullae formation and/or desquamation

  1. Lower intestinal tract: (use mL/day for adult recipients and mL/m2/day for pediatric recipients)

Stage 0 – no diarrhea, no diarrhea attributable to acute GVHD / diarrhea < 500 mL/day (adult), or < 10 mL/kg/day (pediatric)

Stage 1 – diarrhea 500 - 1000 mL/day (adult), or 10 - 19.9 mL/kg/day (pediatric)

Stage 2 – diarrhea 1001 - 1500 mL/day (adult), or 20 - 30 mL/kg/day (pediatric)

Stage 3 – diarrhea > 1500 mL/day (adult), or > 30 mL/kg/day (pediatric)

Stage 4 – severe abdominal pain, with or without ileus, and/or grossly bloody stool

  1. Upper intestinal tract:

Stage 0 – no persistent nausea or vomiting

Stage 1 – persistent nausea or vomiting

  1. Liver:

Stage 0 – No liver acute GVHD / bilirubin < 2.0 mg/dL (< 34 μmol/L)

Stage 1 – bilirubin 2.0–3.0 mg/dL (34–52 μmol/L)

Stage 2 – bilirubin 3.1–6.0 mg/dL (53–103 μmol/L)

Stage 3 – bilirubin 6.1–15.0 mg/dL (104–256 μmol/L)

Stage 4 – bilirubin > 15.0 mg/dL (> 256 μmol/L)



  1. Other site(s) involved with acute GVHD

Yes – Go to question 28

No – Go to question 29

  1. Specify other site(s):



Specify the maximum overall grade of acute GVHD since the date of last report

  1. Maximum overall grade of acute GVHD:

I - Rash on ≤ 50% of skin, no liver or gut involvement

II - Rash on > 50% of skin, bilirubin 2-3 mg/dL, or diarrhea 500 – 1000 mL/day or persistent nausea

III - Bilirubin 3-15 mg/dL, or gut stage 2-4 diarrhea > 1000 mL/day or severe abdominal pain with or without ileus

IV - Generalized erythroderma with bullous formation, or bilirubin >15 mg/dL

Not applicable (acute GVHD present but cannot be graded)

  1. Date maximum overall grade of acute GVHD: ___ ___ ___ ___ - ___ ___ - ___ ___

YYYY MM DD



  1. Did chronic GVHD develop since the date of last report?

Yes – Go to questions 32

No - Go to question 33

Unknown – Go to question 33

  1. Date of chronic GVHD diagnosis: ___ ___ ___ ___ — ___ ___ — ___ ___ Date estimated Go to questions 34

YYYY MM DD

  1. Did chronic GVHD persist since the date of last report?

Yes – Go to questions 34

No - Go to question 37

Unknown Go to question 37

Specify the maximum grade of chronic GVHD since the date of last report:

  1. Maximum grade of chronic GVHD: (according to best clinical judgment)

Mild

Moderate

Severe

Unknown

  1. Specify if chronic GVHD was limited or extensive:

Limited - localized skin involvement and/or liver dysfunction

Extensive – one or more of the following:

– generalized skin involvement; or,

– liver histology showing chronic aggressive hepatitis, bridging necrosis or cirrhosis; or,

– involvement of eye: Schirmer’s test with < 5 mm wetting; or

– involvement of minor salivary glands or oral mucosa demonstrated on labial biopsy; or

– involvement of any other target organ

  1. Date of maximum grade of chronic GVHD: ___ ___ ___ ___ - ___ ___ - ___ ___

YYYY MM DD

  1. Is the recipient still taking systemic steroids? (Do not report steroids for adrenal insufficiency, ≤10 mg/day for adults, <0.1 mg/kg/day for children)

Yes

No

Not applicable

 Unknown

  1. Is the recipient still taking (non-steroid) immunosuppressive agents (including PUVA) for GVHD?

Yes

No

Not applicable

 Unknown



Liver Toxicity Prophylaxis

  1. Was specific therapy used to prevent liver toxicity?

Yes – Go to question 40

No – Go to question 46

  1. Defibrotide

Yes

No

  1. N-acetylcysteine

Yes

No

  1. Tissue plasminogen activator (TPA)

Yes

No

  1. Ursodiol

Yes

No

  1. Other therapy

Yes – Go to question 45

No – Go to question 46

  1. Specify other therapy: ______________________________________



Veno-occlusive disease (VOD) / Sinusoidal obstruction syndrome (SOS)



Specify if the recipient developed VOD / SOS since the date of last report:

  1. Did veno-occlusive disease (VOD) / sinusoidal obstruction syndrome (SOS) develop since the date of last report?

 Yes – Go to question 47

No – Go to question 48

  1. Date of diagnosis: ___ ___ ___ ___ - ___ ___ - ___ ___ - Go to question 49

  2. Did veno-occlusive disease (VOD) / sinusoidal obstruction syndrome (SOS) persist or recur since the date of last report?

Yes

No



New Malignancy, Lymphoproliferative or Myeloproliferative Disease /Disorder

Report new malignancies that are different than the disease/disorder for which HCT was performed. Do not include relapse, progression or transformation of the same disease subtype.

  1. Did a new malignancy, myelodysplastic, myeloproliferative, or lymphoproliferative disease/disorder occur that is different from the disease/disorder for which the HCT or cellular therapy was performed? (include clonal cytogenetic abnormalities, and post-transplant lymphoproliferative disorders)

Yes – Go to question 50

No – Go to question 57



Copy and complete questions 50-56 to report each new malignancy diagnosed since the date of last report. The submission of a pathology report or other supportive documentation for each reported new malignancy is strongly recommended.

  1. Specify the new malignancy:

Acute myeloid leukemia (AML / ANLL) – Go to question 53

Other leukemia – Go to question 53

 Myelodysplastic syndrome (MDS) – Go to question 53

 Myeloproliferative neoplasm (MPN) – Go to question 53

Myelodysplasia / myeloproliferative neoplasm (MDS / MPN)– Go to question 53

 Hodgkin lymphoma – Go to question 52

Non-Hodgkin lymphoma – Go to question 52

Post-transplant lymphoproliferative disorder (PTLD)– Go to question 52

Clonal cytogenetic abnormality without leukemia or MDS – Go to question 53

Uncontrolled proliferation of donor cells without malignant transformation – Go to question 53

 Breast cancer – Go to question 53

 Central nervous system (CNS) malignancy (e.g. glioblastoma, astrocytoma) – Go to question 53

 Gastrointestinal malignancy (e.g. colon, rectum, stomach, pancreas, intestine) – Go to question 53

 Genitourinary malignancy (e.g. kidney, bladder, ovary, testicle, genitalia, uterus, cervix) – Go to question 53

 Lung cancer – Go to question 53

 Melanoma – Go to question 53

 Basal cell skin malignancy – Go to question 53

 Squamous cell skin malignancy – Go to question 53

 Oropharyngeal cancer (e.g. tongue, buccal mucosa) – Go to question 53

 Sarcoma – Go to question 53

 Thyroid cancer – Go to question 53

 Other new malignancy – Go to question 51

  1. Specify other new malignancy: _________________________________ - Go to question 53

  2. Is the tumor EBV positive?

 Yes

 No

  1. Date of diagnosis: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD

  1. Was documentation submitted to the CIBMTR? (e.g. pathology / autopsy report or other documentation)

Yes

No

  1. Was the new malignancy donor / cell product derived?

Yes – Go to question 56

No – Go to question 57

Not done – Go to question 57

  1. Was documentation submitted to the CIBMTR? (e.g. cell origin evaluation (VNTR, cytogenetics, FISH)

Yes

No



Chimerism Studies (Cord Blood Units Only)

This section relates to chimerism studies from allogeneic HCTs using cord blood units only. If this was an autologous HCT, or an allogeneic HCT using a bone marrow or PBSC product, continue to disease assessment.

  1. Were chimerism studies performed since the date of last report?

Yes – Go to question 58

No – Go to question 76

  1. Was documentation submitted to the CIBMTR? (e.g. chimerism laboratory reports)

Yes

No

  1. Were chimerism studies assessed for more than one donor / multiple donors?

Yes

No

Provide date(s), method(s) and other information for all chimerism studies performed since the date of last report.

  1. NMDP donor ID: ___ ___ ___ ___ — ___ ___ ___ ___ — ___

  2. NMDP cord blood unit ID: ___ ___ ___ ___ ___ ___ ___ ___ ___ ___

  3. Non-NMDP unrelated donor ID: ___ ___ ___ ___ ___ ___ ___ ___ ___ ___

  4. Non-NMDP cord blood unit ID: ___ ___ ___ ___ ___ ___ ___ ___ ___ ___ ___ ___ ___ ___ ___

  5. Date of birth: (donor / infant) ___ ___ ___ ___ — ___ ___ — ___ ___ – OR – Age: (donor/infant) ___ ___

YYYY MM DD Months

Years

  1. Sex (Donor / infant)

Male

Female



  1. Date sample collected: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD

  1. Method

Karyotyping for XX/XY– Go to question 69

  • Fluorescent in situ hybridization (FISH) for XX/XY – Go to question 69

Restriction fragment-length polymorphisms (RFLP) – Go to question 69

VNTR or STR, micro or mini satellite (also include AFLP) – Go to question 69

Other – Go to question 68

  1. Specify:

  2. Cell source

Bone marrow

Peripheral blood

  1. Cell type

Unsorted / whole – Go to question 72

Red blood cells – Go to question 74

Hematopoietic progenitor cells (CD34+ cells) – Go to question 74

Total mononuclear cells (lymphs & monos) – Go to question 74

T-cells (includes CD3+, CD4+, and/or CD8+) – Go to question 74

B-cells (includes CD19+ or CD20+) – Go to question 74

Granulocytes (includes CD33+ myeloid cells) – Go to question 74

NK cells (CD56+) – Go to question 74

Other – Go to question 71

  1. Specify:

  2. Total cells examined: ___ ___ ___ ___ ___ ___

  3. Number of donor cells: ___ ___ ___ ___- Go to question 76

  4. Were donor cells detected?

Yes - Go to question 75

No – Go to question 76

  1. Percent donor cells: ___ ___ ___ %

Copy questions 60 – 75 if needed for multiple chimerism studies.



Disease Assessment at the Time of Best Response to HCT

  1. Compared to the disease status prior to the preparative regimen, what was the best response to HCT since the date of the last report? (Include response to any therapy given for post-HCT maintenance or consolidation, but exclude any therapy given for relapsed, persistent, or progressive disease)

Continued complete remission (CCR) - Go to question 78

Complete remission (CR) - Go to question 78

Not in complete remission - Go to question 77

Not evaluated - Go to question 99

  1. Specify disease status if not in complete remission:

Disease detected - Go to question 80

No disease detected but incomplete evaluation to establish CR - Go to question 80

  1. Was the date of best response previously reported?

Yes - Go to question 99

No - Go to question 79

  1. Date assessed: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD

Specify the method(s) used to assess the disease status at the time of best response:

  1. Was the disease status assessed by molecular testing (e.g. PCR)?

Yes - Go to questions 81

No - Go to question 83

Not applicable - Go to question 83

  1. Date assessed: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD

  1. Was disease detected?

Yes

No

  1. Was the disease status assessed via flow cytometry?

Yes - Go to question 84

No - Go to question 86

Not applicable - Go to question 86

  1. Date assessed: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD

  1. Was disease detected?

 Yes

 No

  1. Was the disease status assessed by cytogenetic testing (karyotyping or FISH)?

Yes - Go to question 87

No - Go to question 93

Not applicable - Go to question 93

  1. Was the disease status assessed via FISH?

Yes - Go to questions 81

No - Go to question 83

Not applicable - Go to question 83

  1. Date assessed: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD

  1. Was disease detected?

Yes

No

  1. Was the disease status assessed via karyotyping?

Yes - Go to question 91

No - Go to question 93

Not applicable - Go to question 93

  1. Date assessed: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD

  1. Was disease detected?

Yes

No

  1. Was the disease status assessed by radiological assessment? (e.g. PET, MRI, CT)

Yes - Go to question 94

No - Go to question 96

Not applicable - Go to question 96

  1. Date assessed: ___ ___ ___ ___ — ___ ___ — ___ ___

  2. Was disease detected?

 Yes

No

  1. Was the disease status assessed by clinical/hematologic assessment?

Yes - Go to question 97

No - Go to question 99

  1. Date assessed: ___ ___ ___ ___ — ___ ___ — ___ ___

  2. Was disease detected?

 Yes

No

Post-HCT Therapy

Report therapy given since the date of last report to prevent relapse or progressive disease. This may include maintenance and consolidation therapy. Do not report any therapy given for relapsed, persistent, or progressive disease.

  1. Was therapy given since the date of the last report for reasons other than relapse, persistent, or progressive disease? (Include any maintenance and consolidation therapy.)

Yes - Go to question 100

No - Go to question 162

  1. Systemic therapy

Yes – Go to question 101

No – Go to question 156

  1. Monoclonal antibody (mAb)

Yes - Go to question 102

No - Go to question 111

  1. Alemtuzumab (Campath)

Yes

No

  1. Bispecific mAb

Yes – Go to question 104

No – Go to question 107

  1. Blinatumomab

Yes

No

  1. Other bispecific mAb

Yes

No

  1. Specify other bispecific mAb: _______________________

  2. Gemtuzumab (Mylotarg, anti-CD33)

Yes

No

  1. Rituximab (Rituxan, MabThera)

Yes

No

  1. Other mAb

Yes

No

  1. Specify other mAb:_________________________________

  2. Tyrosine kinase inhibitors (TKI)

Yes – Go to question 112

No – Go to question 118

  1. Bosutinib

Yes

No

  1. Dasatinib (Sprycel)

Yes

No

  1. Imatinib mesylate (Gleevec)

Yes

No

  1. Nilotinib (AMN107, Tasignal)

Yes

No

  1. Other TKI

Yes – Go to question 117

No– Go to question 118

  1. Specify other TKI:_________________________________

  2. FLT3 inhibitors

Yes – Go to question 119

No – Go to question 127

  1. Gilteritinib

Yes

No

  1. Lestaurtinib

Yes

No

  1. Midostaurin

Yes

No

  1. Quizartinib

Yes

No

  1. Sorafenib

Yes

No

  1. Sunitinib

Yes

No

  1. Other FLT3 inhibitor

Yes – Go to question 126

No– Go to question 127

  1. Specify other FLT3 inhibitor:_________________________________

  2. Hypomethylating agents

Yes – Go to question 128

No – Go to question 132

  1. Azacytidine (Vidaza)

Yes

No

  1. Decitabine (Dacogen)

Yes

No

  1. Other hypomethylating agent

Yes – Go to question 131

No– Go to question 132

  1. Specify other hypomethylating agent:_______________________________

  2. Proteasome inhibitors

Yes – Go to question 133

No – Go to question 138

  1. Bortezomib (Velcade)

Yes

No

  1. Carfilzomib

Yes

No

  1. Ixazomib

Yes

No

  1. Other proteasome inhibitor

Yes – Go to question 137

No – Go to question 138

  1. Specify other proteasome inhibitor:_________________________

  2. Immune modulating agents

Yes – Go to question 139

No – Go to question 144

  1. Lenalidomide (Revlimid)

Yes

No

  1. Pomalidomide

Yes

No

  1. Thalidomide (Thalomid)

Yes

No

  1. Other immune modulating agent

Yes – Go to question 143

No – Go to question 144

  1. Specify other immune modulating agent: _____________________

  2. PD1 inhibitor

Yes – Go to question 145

No – Go to question 149

  1. Nivolumab

Yes

No

  1. Pembrolizumab

Yes

No

  1. Other PD1 inhibitor

Yes – Go to question 148

No – Go to question 149

  1. Specify other PD1 inhibitor: _____________________

  2. BTK inhibitors

Yes – Go to question 150

No – Go to question 153

  1. Ibrutinib

Yes

No

  1. Other BTK inhibitor

Yes – Go to question 152

No – Go to question 153

  1. Specify other BTK inhibitor:_______________________________

  2. Chemotherapy

Yes – Go to question 154

No – Go to question 155

  1. Specify chemotherapy drugs: ________________

  2. Other systemic therapy

Yes – Go to question 156

No – Go to question 157

  1. Specify other systemic therapy: ____________________

  2. Radiation

Yes

No

  1. Cellular therapy

Yes

No

  1. Blinded randomized trial

Yes

No

  1. Other therapy

Yes – Go to question 161

No – Go to question 162



  1. Specify other therapy: ____________________________________

Relapse or Progression Post-HCT

Report if the recipient has experienced a clinical/hematologic relapse or progression post-HCT. If the relapse or progression was detected in a previous reporting period indicate that and continue on. If the first clinical/hematologic relapse occurred since the date of last report, indicate the date it was first detected in this reporting period.

  1. Did the recipient experience a clinical/hematologic relapse or progression post-HCT?

Yes - Go to question 163

No - Go to question 165

  1. Was the date of clinical/hematologic relapse or progression previously reported?

Yes - Go to question 165 (only valid >day 100)

No - Go to question 164

  1. Date first seen: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD



Intervention for relapsed disease, persistent disease, progressive disease, or decreased/loss of chimerism

  1. Was intervention given for relapsed, persistent or progressive disease, or decreased/loss of chimerism since the date of last report?

Yes - Go to question 166

No - Go to question 236

  1. Specify reason for which intervention was given:

Persistent disease

Relapsed / progressive disease

Decrease / loss of chimerism



Specify the method(s) of detection for which intervention was given:

  1. Clinical/hematologic

Yes

No

  1. Radiological (e.g. PET, MRI, CT)

Yes

No

  1. Cytogenetic

Yes

No

  1. Flow cytometry

Yes

No

  1. Disease specific molecular marker

Yes

No

  1. Chimerism testing

Yes

No

  1. Date intervention started: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD



Specify intervention(s):

  1. Systemic therapy

Yes – Go to question 175

No – Go to question 231

  1. Monoclonal antibody (mAb)

Yes – Go to question 176

No – Go to question 185

  1. Alemtuzumab (Campath)

Yes

No

  1. Bispecific mAb

Yes – Go to question 178

No – Go to question 181

  1. Blinatumomab

Yes

No

  1. Other bispecific mAb

Yes

No

  1. Specify other bispecific mAb:__________________

  2. Gemtuzumab (Mylotarg, anti-CD33)

Yes

No

  1. Rituximab (Rituxan, MabThera)

Yes

No

  1. Other mAb

Yes – Go to question 184

No – Go to question 185

  1. Specify other mAb:_________________________________

  2. Tyrosine kinase inhibitors (TKI)

Yes – Go to question 186

No – Go to question 192

  1. Bosutinib

Yes

No

  1. Dasatinib (Sprycel)

Yes

No

  1. Imatinib mesylate (Gleevec)

Yes

No

  1. Nilotinib (AMN107, Tasignal)

Yes

No

  1. Other TKI

Yes – Go to question 191

No – Go to question 192

  1. Specify other TKI:_________________________________

  2. FLT3 inhibitors

Yes – Go to question 193

No – Go to question 201

  1. Gilteritinib

Yes

No

  1. Lestaurtinib

Yes

No

  1. Midostaurin

Yes

No

  1. Quizartinib

Yes

No

  1. Sorafinib

Yes

No

  1. Sunitinib

Yes

No



  1. Other FLT3 inhibitor

Yes – Go to question 200

No – Go to question 201

  1. Specify other FLT3 inhibitor:_________________________________

  2. Hypomethylating agents

Yes – Go to question 202

No – Go to question 206

  1. Azacytidine (Vidaza)

Yes

No

  1. Decitabine (Dacogen)

Yes

No

  1. Other hypomethylating agent

Yes – Go to question 205

No – Go to question 206

  1. Specify other hypomethylating agent:_______________________________

  2. Proteasome inhibitors

Yes – Go to question 207

No – Go to question 212

  1. Bortezomib (Velcade)

Yes

No

  1. Carfilzomib

Yes

No

  1. Ixazomib

Yes

No

  1. Other proteasome inhibitor

Yes – Go to question 211

No – Go to question 212

  1. Specify other proteasome inhibitor:_________________________

  2. Immune modulating agents

Yes – Go to question 213

No – Go to question 218

  1. Lenalidomide (Revlimid)

Yes

No

  1. Pomalidomide

Yes

No

  1. Thalidomide (Thalomid)

Yes

No

  1. Other immune modulating agent

Yes – Go to question 217

No – Go to question 218

  1. Specify other immune modulating agent: _____________________

  2. PD1 inhibitor

Yes – Go to question 219

No – Go to question 223

  1. Nivolumab

Yes

No

  1. Pembrolizumab

Yes

No

  1. Other PD1 inhibitor

Yes – Go to question 222

No – Go to question 223

  1. Specify other PD1 inhibitor: _____________________

  2. BTK inhibitors

Yes – Go to question 225

No – Go to question 227

  1. Ibrutinib

Yes

No

  1. Other BTK inhibitor

Yes – Go to question 226

No – Go to question 227

  1. Specify other BTK inhibitor:_______________________________

  2. Chemotherapy

Yes – Go to question 228

No – Go to question 229

  1. Specify chemotherapy drugs: ___________________

  2. Other systemic therapy

Yes – Go to question 230

No – Go to question 231

  1. Specify other systemic therapy: ____________________

  2. Radiation

Yes

No

  1. Cellular therapy

Yes

No

  1. Blinded randomized trial

Yes

No

  1. Other therapy

Yes – Go to question 235

No – Go to question 236

  1. Specify other therapy: ____________________________________

Current Disease Status

  1. What is the current disease status?

Complete remission (CR) - Go to question 238

Not in complete remission - Go to question 237

Not evaluated - Go to First Name

  1. Specify disease status if not in complete remission:

Disease detected

No disease detected but incomplete evaluation to establish CR

  1. Date of most recent disease assessment

Known – Go to question 239

Unknown – Go to First Name

  1. Date of most recent disease assessment: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD



First Name: ________________________________________________________________________________

Last Name:

E-mail address:

Date: ___ ___ ___ ___ — ___ ___ — ___ ___

YYYY MM DD



CIBMTR Form 2450 revision 4 (page 30 of 30) DRAFT 421-2016<

Internal use: Document number F00486 revision 2 Replaces: F00486 version 1.0 July 2007

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File Title2450r2 Mockup
AuthorRobinette Aley
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