Miscellaneous

Question 1

Lab features of factor XI deficiency and diagnosis

Answer 1

• Prolonged aPTT, which corrects with mixing study
• confirmation by factor XI activity

Question 2

Factor XI clinical features

Answer 2

• Bleeding phenotype highly variable
• NO spontaneous bleeding, hemarthrosis, or muslce hematomas
• Bleeding typically in setting of trauma or surgery - “injury-related bleeding disorder”

Question 3

Factor XI deficiency management

Answer 3

• if significant bleeding history, factor XI replacement
• IF significant bleeding and inhibitor present, recombinant factor VIIa

Question 4

PCH diagnosis

Answer 4

clinical/laboratory
- clinical context of hemolysis precipitated by the cold
- Coombs/DAT + complement (C3) (but can be negative in kids), negative for IgG or IgM
- ideally Donath-landsteiner antibody (But insensitive and can rapidly become negative)

Question 5

Deauville X meaning

Answer 5

New areas of uptake unlikely to be related to lymphoma

Question 6

Deauville 5 meaning

Answer 6

Uptake markedly higher than liver (2-3x) and/or new lesions

Question 7

Deauville 4 meaning

Answer 7

Uptake moderately more than liver uptake, at any site

Question 8

Deauville 3 meaning

Answer 8

Uptake greater than mediastinal blood pool but less than liver

Question 9

Deauville 1 meaning

Answer 9

No uptake

Question 10

Deauville 2 meaning

Answer 10

Uptake less than mediastinal blood pool

Question 11

Morphine IV to PO conversion

Answer 11

1 mg IV = 3 mg PO

Question 12

Niraparib dosing based on weight and plt count

Answer 12

Patients <77 kg or with a platelet count <150,000/mm3: Oral: 200 mg once daily

Patients ≥77 kg and with a platelet count ≥150,000/mm3: Oral: 300 mg once daily

Question 13

Cryoprecipitate components

Answer 13

• Fibrinogen
• Factor XIII
• Von willebrand factor
• Fibronectin

Question 14

VITT presentation

Answer 14

*Strongly mimics HIT
1) vaccine type – J&J, Astra Zeneca
2) timeframe – typically in a narrow window 5 to 10 days post-vaccination, leading to identification of cases typically between 5 to 30 days post-vaccination (so 5-30 currently used as interval)
3) thrombosis – (most commonly in cerebral veins (including intracranial hemorrhage), deep veins of the leg, pulmonary arteries, and splanchnic vessels). Both arterial + venous.
*But can have thrombosis without thrombocytopenia or thrombocytopenia without thrombosis.
4) Platelet count nadir – between 10,000 and 100,000/microL, with a median platelet count of 47k
5) High frequency of DIC.

Question 15

VITT diagnosis

Answer 15

Positive PF4 antibody + appropriate clinical context (post-COVID vaccine thrombosis and/or thrombocytopenia)

Question 16

VITT management

Answer 16

• ***High dose IVIG 1 gm/kg (based on actual body weight) daily for 2 days (reduce VITT antibody-induced platelet activation)
• anticoagulation (DOAC preferred)

Question 17

Duration of anticoagulation for VITT

Answer 17

IF thrombosis → Anticoagulation for minimum 3 months after normalization of the platelet count, as long as no further thrombosis occurs
IF NO thrombosis –> anticoagulation until platelet count recovery and perhaps longer if tolerated (four to six weeks after platelet count recovery)

Question 18

Porphyria mechanism generally

Answer 18

• Porphyrias are caused by alterations in the enzymes of heme biosynthesis. Heme is essential in the function of many hemoproteins, including hemoglobin and hepatic cytochrome P450 enzymes.

Question 19

Treatment for AIP

Answer 19

hemin

Question 20

1) Diagnosis of AIP 2) confirmatory testing specific for AIP

Answer 20

1) elevated plasma and urinary ALA and PGB above baseline (>10 mg/L or >10mg/g)
2) normal or slightly elevated total plasma porphyrins
3) normal or slightly increased stool porphyrins
Confirmatory testing:
1) ***low erythrocyte PBGD activity (deficient enzyme in AIP)
2) genetic testing

Question 21

AIP clinical features

Answer 21

• develop over hours to days + insomnia as early symptom + persist for days to weeks + unexplained acute abdominal pain (85-95%, poorly localized) + unexplained psychiatric symptoms + peripheral neuropathy + vomiting + muscle weakness + pain in limbs/head/neck/chest + bladder dysfunction + dark or reddish-brown urine

Question 22

AIP pathophysiology

Answer 22

Inherited deficiency of porphobilinogen deaminase (PBGD; also called hydroxymethylbilane synthase [HMBS]), the third enzyme in the heme biosynthetic pathway

Question 23

Chronic granulomatous disease diagnosis

Answer 23

• undergo neutrophil-function testing (cytochrome c reduction assay, chemiluminescence, nitroblue tetrazolium (NBT) reduction test, and dihydrorhodamine (DHR) 123 oxidation test (preferred))
• Positive findings should be confirmed by genotyping

Question 24

CGD clinical features

Answer 24

• recurrent, life-threatening bacterial and fungal infections + granuloma formation

Question 25

CGD mechanism

Answer 25

defects in the phagocyte nicotinamide adenine dinucleotide phosphate (NADPH) oxidase complex

Question 26

MBL diagnostic criteria

Answer 26

1) monoclonal B cell population (flow cytometry preferred) 2) <5000 cells/microL 3) >3 months 4) no other features of a b cell lymphoproliferative disorder (lymphadenopathy, organomegaly, cytopenias, or extramedullary involvement) or autoimmune disorder or infectious disease

Question 27

X-linked sideroblastic anemia (XLSA) clinical features

Answer 27

- young boy presenting with hgb of 7 with microcytosis and no evidence of iron deficiency

Question 28

XLSA treatment

Answer 28

B6

Question 29

1) 2 categories of sideroblastic anemias 2) causes in second category

Answer 29

1) clonal sideroblastic anemias, which are stem cell disorders (MDS, MPN) 2) sideroblastic anemia attributed to copper deficiency, certain medications, or excessive alcohol use

Question 30

Settings in which copper deficiency develops

Answer 30

1) malabsorption 2) prolonged parenteral nutrition 3) zinc ingestion

Question 31

Work up for ring sideroblast detected on bone marrow aspirate

Answer 31

Review for history of excessive alcohol use Test for copper deficiency Review medications for drug-induced sideroblastic anemia IF above nondiagnostic, genetic testing: ALAS2 (female only), SF3B1 and JAK2

Question 32

Primary complication of sideroblastic anemia to be aware of

Answer 32

- iron overload (ineffective erythropoiesis leads to increased iron absorption)

Question 33

What is Heyde syndrome?

Answer 33

VWF is thought to suppress angiogenesis. Patients with aortic stenosis or severe MR have been found to have increased GI angiodysplasia (Heyde syndrome) thought secondary to acquired VWS and VWF deficiency

Question 34

Brodifacoum is

Answer 34

superwarfarin, used as rodenticide, common cause of toxic ingestion leading to coagulopathy

Question 35

1) Management of toxic ingestion of anticoagulant rodenticides 2) management of associated severe bleeding

Answer 35

- Activated charcoal (assuming normal mental status and no aspiration risk and can be given within 2 hrs) - IF normal coags 48h after ingestion, no treatment - IF INR less than 4.5 and no bleeding, monitor - IF INR greater than 4.5 and no bleeding, oral vitamin K with INR monitoring - IF minor bleeding, oral vitamin K - IF life threatening bleeding, 4-factor PCC, then FFP by rapid infusion + IV vitamin K

Question 35

Presentation of brodifacoum/superwarfarin toxicity - 1) timeframe 2) sources of rodenticide

Answer 35

- Spontaneous bleeding following toxic ingestion of rodenticide (in cereal bait, pellets, loose grain, paste) - usually 24h delay until bleeding starts - lasts for months (much longer half life)

Question 36

Management of supratherapeutic INR

Answer 36

- Given INR 4.5-10 and no evidence bleeding, no indication for vitamin k (per American Society of Hematology guidelines) - Given INR >10 and patient has no evidence of bleeding, recommend vitamin K 2.5 mg or 5 mg PO (per American Society of Hematology guidelines) - Given bleeding OR urgent surgery/procedure needed, recommend Vitamin K IV 10 mg once, slow infusion 4 Factor-prothrombin complex concentrate (PCC or Kcentra)

Question 37

Management of low or intermediate risk MDS

Answer 37

- essentially observation until they become transfusion dependent

Question 38

Factor dosing calculation in hemophilia B

Answer 38

*Goal is to raise factor levels to 100% initially and then maintain factor levels above 50% by bolus q8-12h or continuous infusion - 1 U/kg raises factor level by 1% (More like 0.75% but can fudge) 100 U/kg raises factor level by 100%

Question 39

venetoclax mechanism

Answer 39

BH3-mimetic.[10] Venetoclax blocks the anti-apoptotic B-cell lymphoma-2 (Bcl-2) protein, leading to programmed cell death of CLL cells.

Question 40

Management of low risk myelofibrosis

Answer 40

- IF asymptomatic, observation - IF symptomatic, start JAKinhibitor *UMass BMT providers had very low threshold to start JAK inhibitors but for boards and by the books, low risk asymptomatic observation is indicated

Question 41

Precipitants of CRS

Answer 41

- CAR-T - BiTe - *post-transplant cytoxan used for prophylaxis of GVHD - *post haplo-HCT

Question 42

Definition of mild CRS

Answer 42

Fever without other systemic symptoms

Question 43

Management of mild CRS

Answer 43

- antihistamines, antipyretics, IV fluids, close monitoring

Question 44

Initial management of severe CRS

Answer 44

STAT tocilizumab one dose (Start w/ toci since you don’t want to theoretically ablate product with steroids - UMass, UTD argues for toci + steroids given more rapid and complete CRS control and ablation is theoretical)

Question 45

Initial management of patient w/ severe CRS and ICANS

Answer 45

- steroids (toci not effective for ICANS)

Question 46

Management of severe bite associated CRS

Answer 46

1) Stop infusion 2) dexamethasone 10 mg up to 4 times/daily (toci less effective than steroids in this setting)

Question 47

Precipitants of atypical HUS

Answer 47

**pregnancy → surgery → autoimmunity → congenital

Question 48

Risk factors for hemolysis with IVIG

Answer 48

- high-dose infusions (1 to 2 grams per kg per day) - high IVIG doses (eg, >100 grams) - female sex, - non-O blood group

Question 49

Presentation of CM TMA postpartum

Answer 49

All CM-TMA features + can see severe AKI postpartum

Question 50

Lab features of immune TTP

Answer 50

(median plt count (10k) almost always <30K) + low grade anemia w/ median hematocrit 21% + reticulocytosis + hemolysis labs (extremely high LDH (around 1000 typically) + indirect hyperbilirubinemia + low haptoglobin) + negative DAT + normal coags + ADAMTS13 <10% (low specificity - many diseases can cause low ADAMTS13)

Question 51

Clinical features of immune TTP

Answer 51

Initial symptoms (fatigue, dyspnea, petechia, abdominal pain/ nausea/vomiting (45%), headache/confusion (20%) - typically mild symptoms at onset) + abnormal or normal (more commonly) kidney function (AKI uncommon), often comorbid autoimmune disorders + typically previously healthy person + median age 40 + females more commonly (75%) + increased frequency in pregnancy

Question 52

Major RF's for recurrent VTE

Answer 52

1),Major surgery >30 minutes 2) hospitalization or confined to bed with "bathroom privileges" for ≥3 days due to acute illness 3) CS 4) trauma with *fractures* 5) high estrogen states - estrogen therapy, pregnancy or puerperium

Question 53

Minor RF's for recurrent VTE

Answer 53

Minor surgery <30 minutes, hospitalization <3 days, reduced mobility at home ≥3 days due to acute illness, lower extremity injury without fracture with reduced mobility ≥3 days, long-haul flight

Question 54

When is it appropriate to measure D-dimer to determine risk of recurrent VTE?

Answer 54

female patients with VTE in whom there is uncertainty regarding the appropriateness of extended anticoagulant therapy

Question 55

Paraneoplastic syndromes associated with Hodgkin Lymphoma

Answer 55

1) nephrotic syndrome (minimal change disease or FSGS) 2) Subacute motor neuropathy (Guillain-Barré) (subacute, progressive, painless, and often asymmetric lower motor neuron weakness)

Question 56

Sweet syndrome presentation

Answer 56

abrupt appearance of painful, edematous, and erythematous papules, plaques, or nodules on the skin

Question 57

Paraneoplastic syndromes associated with AML

Answer 57

- Sweet syndrome - erythroderma

Question 58

What is the function of irradiating PRBCs?

Answer 58

Inactivating lymphocytes (Thus, used to prevent ta-GVHD in at-risk individuals)

Question 59

Indications for irradiating PRBCs

Answer 59

1) Congenital immunodeficiencies 2) potent immunosuppressive therapies (*purine analogs, ATG, certain monoclonal antibodies) 3) auto or allo transplant recipients 4) Hodgkin Lymphoma 5) Individuals at risk for partial HLA matching with the donor due to directed donations, HLA-matched products, or genetically homogeneous populations

Question 60

How leukoreduction works

Answer 60

- Each unit of whole blood or packed RBCs contains approximately two to five billion (2 to 5 x 109) leukocytes (white blood cells [WBCs]), which are collected along with the other cellular elements. These leukocytes are thought to contribute to a number of adverse effects including febrile nonhemolytic transfusion reactions (FNHTRs), human leukocyte antigen (HLA) alloimmunization, and transmission of cytomegalovirus - Leukoreduction refers to the selective removal of leukocytes by passing the blood through a leukocyte reduction filter

Question 61

Indications for leukoreduction (by the books)

Answer 61

*essentially all PRBCs are leukoreduced now 1) Chronically transfused patients 2) Previous febrile nonhemolytic transfusion reaction 3) Patients undergoing cardiac surgery 4) All recipients (or potential recipients) of solid organ or hematopoietic cell transplants 5) All individuals with acute leukemia, and probably individuals with other malignancies 6) CMV seronegative at-risk patients for whom seronegative components are not supplied

Question 62

Malignant heme pathologies associated with HTLV-1

Answer 62

Adult T cell leukemia-lymphoma (ATL) (including CTCL)

Question 63

NCCN recommendation for low emetic risk chemo

Answer 63

- single agent: Decadron vs. reglan vs. compazine vs. 5-HT3

Question 64

Blastic plasmacytoid dendritic cell neoplasm clinical features

Answer 64

aggressive + Lymphadenopathy + cutaneous involvement

Question 65

Blastic plasmacytoid dendritic cell neoplasm immunophenotype

Answer 65

CD123 + CD4 + CD56 + TdT + BDCA-2/CD303 *count from 1-6

Question 66

Transplant criteria for amyloidosis

Answer 66

1) Age <70 2) SBP >90 3) NYHA <3 4) No more than 2 organs involved (liver, heart, kidney, or autonomic nerve) 5) Troponin T level <0.06 (high sensitivity troponin T <75 ng/ml) 6) NTproBNP <5 ng/L 7) ECOG 0-1 8) CrCl ?30 mL/minute

Question 67

Difference between 3 and 4 factor PCC

Answer 67

- 3 does not have factor VII

Question 68

What is the mechanism of action of FC fusion protein

Answer 68

Alprolix Coagulation Factor IX (Recombinant), Fc Fusion Protein, is a recombinant DNA derived, coagulation Factor IX concentrate. It temporarily replaces the missing coagulation Factor IX needed for effective hemostasis. Alprolix contains the Fc region of human IgG1, which binds to the neonatal Fc receptor (FcRn). FcRn is part of a naturally occurring pathway that delays lysosomal degradation of immunoglobulins by cycling them back into circulation, and prolonging their plasma half-life.

Question 69

SVT management

Answer 69

IF no VTE RF's but close to deep vein system (within 5 cm), prophylactic NOAC for 45 days IF VTE RF's, then need therapeutic dosing

Question 70

Next step after PVT diagnosed in a young, healthy person

Answer 70

JAK2 mutational analysis

Question 71

High leukocyte alkaline phosphatase score suggests what

Answer 71

Leukemoid reaction

Question 72

Bone marrow findings in CMML

Answer 72

- <20% blasts by definition - dysplasia

Question 73

Key criteria for CMML

Answer 73

***monocytosis accounting for >10% of WBC

Question 74

Avapritinib SE to know

Answer 74

diarrhea

Question 75

HDAC inhibitors

Answer 75

- romidepsin - vorinostat - panobinostat - belinostat

Question 76

Donor type for patients with familial AML

Answer 76

Matched unrelated donor

Question 77

Xa reversal agenet

Answer 77

andexanet alfa

Question 78

benefit of exchange over simple transfusion

Answer 78

less alloimmunization

Question 79

ICANS treatment

Answer 79

- Prophylactic AED w/ keppra 500 mg BID - Dex 10 mg q8h

Question 80

Required prophylaxis with campath

Answer 80

PJP

Question 81

Belzutifan SE's

Answer 81

anemia + hypoxia

Question 82

caplacizumab mechanism

Answer 82

Binds VWD and blocks its interaction with plt glycoprotein Ib-IX-V

Question 83

Drugs known to cause immune TTP

Answer 83

- bactrim - Quetiapine - gemcitabine - oxaliplatin - Quinine

Question 84

Drugs known to cause non-immune TTP

Answer 84

- valproic acid - avastin - velcade - carfilzomib - dasatinib - docetaxel - imatinib - ixazomib - mitomycin - palbociclib - pentostatin - ponatinib - sunitinib - cocaine - oxycontin - cyclosporine - everolimus - inflixmab - sirolimus - tacrolimus

Question 85

Revlimid mechanism of action

Answer 85

- Modulates CRL4 E3 ubiquitin ligase - Induces the ubiquitination of IKZF1 and IKZF3 by CRL4

Question 86

Immunophenotype of Langerhans cell histiocytosis

Answer 86

CD1a+ CD207+

Question 87

angiosarcoma immunophenotype

Answer 87

- CD31+ - CD34+

Question 88

Monomorphic PTLD treatment

Answer 88

Anti-CD20 (rituxan) + CHOP

Question 89

morphology of cells in LGL

Answer 89

large granular lymphocytes

Question 90

Virus associated with ATL

Answer 90

HTLV-1

Question 91

Paraneoplastic syndrome associated with ATL

Answer 91

hypercalcemia

Question 92

mutations to know for T-LGL

Answer 92

STAT3 and STAT5b

Question 93

Relevance of cresyl blue staining

Answer 93

G6PD + Hgh H disease

Question 94

Blood to transfuse HCT recipient that is A+ with a B+ donor

Answer 94

O+ (they will have the blood type of the donor after engraftment BUT a type O pt may have anti-A in their plasma produced by residual lymphocytes either transiently or persistently despite converting to blood type A.