Lecture 13: Leukocyte Disorders Part 2 Flashcards

Question 1

Q

Where are the extranodal lymph sites?

Answer

A

Skin
GI tract & liver
Bone marrow
Testicles

Question 2

Q

What are the lymph node sizes in children

Answer

A

Largest are anterior cervical <= 2cm
Smallest are axillary <= 1cm
Inguinal Nodes are<=1.5

Question 3

Q

What lymph nodes should I palpate on children vs adults?

Answer

A

Anterior cervical, axillary, and inguinal are the best for children.

Adults can be palpated at any lymph node site. (<1cm)

Question 4

Q

When does lymph node atrophy begin?

Answer

A

Early adolescence, so adult lymph nodes are expected to be smaller than children.

Question 5

Q

What should you note regarding the physical characteristics of a lymph node?

Answer

A

Size
Location
Consistency
Tenderness
Fixation

Question 6

Q

What do hard lymph nodes suggest?

Answer

A

Fibrotic cancers

Question 7

Q

What do firm and rubbery nodes suggest?

Answer

A

Lymphomas
Chronic leukemia

Question 8

Q

What do softer lymph nodes suggest?

Answer

A

Acute leukemia
Inflammation

Question 9

Q

What does tenderness in a lymph node suggest?

Answer

A

Acute enlargement would suggest an inflammatory process.

Question 10

Q

What does lack of tenderness in a lymph node suggest?

Answer

A

Malignancy

Question 11

Q

Are lymph nodes normally fixed or mobile? What does it suggest if they aren’t?

Answer

A

Mobile is NORMAL.

Fixed suggests malignancy or inflammation.

Question 12

Q

How do we describe lymph nodes combining?

Question 13

Q

How do we manage isolated LAN in children?

Answer

A

Depending on area, we treat empirically for a short time.

High CA-MRSA prevalence = clindamycin.
Low CA-MRSA prevalence = keflex or augmentin
Cat/kittens (B. henselae) = add azithromycin.
f/u in 2-4 wks.

This is NOT recommended for adults.

CA-MRSA = community acquired MRSA.

Question 14

Q

How do we manage isolated LAN in adults?

Answer

A

Work up to r/o malignancy.
Refer for possible biopsy

DO NOT TREAT empirically.

Question 15

Q

What is non-hodgkin’s lymphoma?

Answer

A

The MC lymphoma.

A malignant overgrowth of the lymphocyte or its precursor within the lymphatic tissue.

MC site: lymph nodes

Question 16

Q

What is the pathophysiology of Non-hodgkin’s lymphoma?

Answer

A

Monoclonal proliferation of lymphocytic cells.

All 3 cells can be affected. Mainly B-cells (85%)

Question 17

Q

What are the etiologies of Non-hodgkin’s lymphoma?

Answer

A

Chromosomal translocations
Infections (EBV, Hep B/C, H. pylori, Kaposi sarcoma Herpes Virus)
Environmental factors
Immunodeficiency states
Chronic inflammation (autoimmune)

Question 18

Q

What is the MC demographic of Non-hodgkin’s lymphoma?

Answer

A

50-60yo
White males

Question 19

Q

What are the two ways non-hodgkin’s lymphoma presents clinically?

Answer

A

Indolent (slow-growing) but often disseminated by time of Dx.

Aggressive

Question 20

Q

How does indolent non-hodgkin’s lymphoma present?

Answer

A

PAINLESS and SLOW growing LAN. (can be local or generalized)
HSM
Cytopenias

Note:
Lymph nodes can swell and regress periodically.

Question 21

Q

How does aggressive non-hodgkin’s lymphoma present?

Answer

A

PAINLESS and FAST GROWING LAN.
Usually progresses fast enough to cause compression of nearby vessels.

B-symptoms in advanced stage.
HSM
Abd/testicular mass
Symptoms of disseminated disease (vertebra, GI, BM, CNS)

Question 22

Q

What are the B-symptoms of aggressive Non-hodgkin’s lymphoma?

Answer

A

Unexplained weight loss > 10% in past 6 months.
Unexplained fever > 38C
DRENCHING night sweats.

Also known as constitutional symptoms.

Question 23

Q

What are symptoms of a disseminated disease in the bones?

Answer

A

EX: vertebra would result in bone pain.

BM: deep aching bone pain

Question 24

Q

How does a CBC for non-hodgkin’s lymphoma present?

Answer

A

Normal until the BM is infiltrated, which results in pancytopenia.

Question 25

Q

How does a CBC for non-hodgkin’s lymphoma present?

Question 26

Q

How does a CMP for non-hodgkin’s lymphoma present?

Answer

A

Elevated BUN/Cr in hydronephrosis if ureter compressed.
Elevated LFTs with hepatic involvement
Elevated ALP in liver/Bone involvement

Question 27

Q

When is LDH elevated in non-hodgkin’s lymphoma?

Answer

A

Advanced disease.

Question 28

Q

What viruses would we screen for in non-hodgkin’s lymphoma?

Answer

A

HIV
HCV
HBV

EBV is not tested since most pts have had it.
We can also treat the other viruses.

Question 29

Q

What are we looking for in a CXR or a CT for non-hodgkin’s lymphoma?

Answer

A

CXR: mediastinal nodes/mass

CT w/ contrast:
Neck/chest/abd/pelvis
Evaluate extent of lymph node involvement.
Mainly for staging.

Question 30

Q

What is the diagnostic test for non-hodgkin’s lymphoma?

Answer

A

EXCISIONAL LYMPH NODE BIOPSY.

Question 31

Q

What would we see in a positive lymph node biopsy in non-hodgkin’s lymphoma?

Answer

A

+ for monoclonal lymphocytes.

Indication = if there is a suspicious lymph node. (>2.25cm2 or 2cm diameter)

Question 32

Q

What kind of lymph node do we prefer to biopsy? What is the alternative?

Answer

A

Preferred is a peripheral node.

Alternative is a CT-guided fine needle biopsy.

Question 33

Q

What are bilateral bone marrow biopsies used for in non-hodgkin’s lymphoma?

Answer

A

For staging.

You must have 2 biopsies in 2 different sites.

Question 34

Q

How does a PET scan work? Why can we use it to monitor lymphoma?

Answer

A

PET Scans show areas of HIGH metabolic activity.

Cancers are highly metabolic, so they appear very active via the radioactive tracers. (radioactive glucose)

Often used for metastatic cancers.

Question 35

Q

How do we stage Non-hodgkin’s lymphoma?

Answer

A

Ann Arbor staging system.

Stages 1-4
Subcategory of A or B
A = non-systemic
B = B-symptoms/systemic symptoms.

Question 36

Q

What is required to stage non-hodgkin’s lymphoma?

Answer

A

PET/CT of the neck, chest, abdomen, and pelvis + a bilateral BM biopsy/aspiration.

Question 37

Q

What is stage 1 of non-hodgkin’s lymphoma?

Answer

A

Single lymph node or single extranodal site.

Question 38

Q

What is stage 2 of non-hodgkin’s lymphoma?

Answer

A

2+ lymph node areas on SAME SIDE of diaphragm.

Question 39

Q

What is stage 3 of non-hodgkin’s lymphoma?

Answer

A

Lymph nodes on both sides of diaphragm.

Question 40

Q

What is stage 4 of non-hodgkin’s lymphoma?

Answer

A

Disseminated or multi organ involvement.

Question 41

Q

What are the additional staging modifications (Cotswolds) avaiable for non-hodgkin’s lymphoma?

Answer

A

E = extralymphatic site
S = splenic
P = pulmonary
H = hepatic
M = marrow

Question 42

Q

How is indolent non-hodgkin’s lymphoma treated?

Answer

A

If it is disseminated by the time of diagnosis, it is incurable.

1-2 drug chemo only used for symptomatic treatment.

Question 43

Q

How is aggressive non-hodgkin’s lymphoma treated?

Answer

A

Chemo +/- radiation therapy.
Allogeneic stem cell transplant

Question 44

Q

What is the prognosis of an indolent NHL diagnosis?

Answer

A

10-15 yrs.

Question 45

Q

What are the poor prognosis factors for NHL?

Answer

A

Age > 60
Elevated LDH
Poor response to standard therapy
Stage 3-4

Question 46

Q

What is hodgkin’s lymphoma?

Answer

A

A malignancy of the B-LYMPHOCYTES within lymph tissue characterized by Reed-Sternberg cells.

Question 47

Q

What are Reed sternberg cells?

Answer

A

Large, abnormal lymphocytes with more than 1 nucleus.

Question 48

Q

What are the etiologies of Hodgkin’s lymphoma?

Answer

A

EBV and HIV

Question 49

Q

What is the MC demographic of Hodgkin’s lymphoma?

Answer

A

20s or 50s
Males (White and african american are equal, other races less likely)

Question 50

Q

How does hodgkin’s lymphoma present?

Answer

A

PAINLESS mass lymph node, MC in the neck.

Pain after ETOH consumption (specific but infrequent)

B symptoms in 40% of pts.

Generalized pruritis
HSM (possible)
Mediastinal mass (possible)

Question 51

Q

How does a CBC, LDH, ALP, and viral serology present for hodgkin’s lymphoma?

Answer

A

CBC: normal or non-specific
LDH: elevated in advanced disease
ALP: elevated if liver/bone involvement.
Viral serology: HIV, HBV, HCV

Question 52

Q

What is the confirmatory test for hodgkin’s lymphoma? What is the finding?

Answer

A

Lymph node excisional biopsy positive for reed-sternberg cells.

Question 53

Q

What scans do we use to stage hodgkin’s lymphoma?

Answer

A

CXR
CT
PET

Question 54

Q

How do we stage hodgkin’s lymphoma?

Answer

A

Identical to NHL.

Stage 1-4 via ann arbor staging.

Question 55

Q

What is the treatment for stage 1-2 (non-bulky) hodgkin’s lymphoma?

Answer

A

Multi drug chemo +/- field radiation therapy

Question 56

Q

What is the treatment for stage 3 or 4 or bulky stage 2 hodgkin’s lymphoma?

Answer

A

Multi drug chemo

Question 57

Q

What is the treatment for relapsing hodgkin’s lymphoma?

Answer

A

High dose chemo
Autologous stem cell transplant

Question 58

Q

What are the poor prognostic factors for hodgkin’s lymphoma?

Answer

A

Low serum albumin < 4
Low Hgb < 10.5
Male
> 45 yo
Stage 4
High WBC > 15k
Low ALC count < 600, less than 8% of total WBC count, or both.

Question 59

Q

What is polycythemia vera?

Answer

A

An ACQUIRED disorder resulting overproduction of all 3 hematopoietic cell lines.

Mutation of Janus Kinase (JAK2 gene), causing excessive cell growth and division.

Question 60

Q

What is the etiology of polycythemia vera?

Answer

A

Unknown, mainly ionizing radiation and toxins suggested.

Question 61

Q

When is polycythemia vera MC age-wise?

Answer

A

50-70.

No other demographic factors.

Question 62

Q

How does polycythemia vera often present?

Answer

A

Increased blood viscosity (fatigue, HA, dizziness, vertigo, tinnitus, visual disturbances, chest pain, and intermittent claudication)

Generalized pruritis worsened after a hot shower.

Bleeding: epistaxis, bleeding gums, ecchymosis, GI bleeding.

Question 63

Q

What does increased blood viscosity cause?

Answer

A

Impaired O2 delivery to tissues.

Question 64

Q

Why does generalized pruritis occur in polycythemia vera?

Answer

A

Basophilic histamine release

Answer 63

A

Engorged vessels and platelet dysfunction.

Answer 64

A

Ulcer formation from increased gastric acidity due to excessive histamine.

HSM

Answer 65

A

Increased blood viscosity and platelet dysfunction.

Answer 66

A

Splenomegaly

Answer 67

A

Retinal and conjuctival vessels.

Answer 68

A

Excess blood.

Answer 69

A

Elevated RBC, PLT, WBC.

HCT: >54 in males and > 51 in females is the hallmark sign!

Answer 70

A

EPO is low. Because we have an excess, our body thinks we don’t need EPO.

Answer 71

A

Genetic testing for JAK2

Answer 72

A

Therapeutic phleb by heme.
1 unit of whole blood (500mL) weekly until Hct < 45%.
DO NOT TREAT IRON DEFICIENCY FROM THIS.
ONLY TAKE 1 UNIT A WEEK.

81mg asa unless active blood loss.

Answer 73

A

Anything causing O2 impairment.

Smoking cessation
CV Risk factors
Hypoxic conditions (COPD, sleep apnea)

Answer 74

A

Used if the therapeutic phlebotomy is insufficient.

Hydroxyurea is used.
It suppresses BM production by interfering with DNA repair.

Answer 75

A

Severe BM suppression, pregnancy, attempted conception, breast feeding.

Answer 76

A

JAK1/JAK2 inhibitor (Jakafi)
Pemazyre (FGFR inhibitor)

Must have failed HU and phlebotomies.
AND 1 of the following:
Markedly symtomatic splenomegaly.
Severe, protracted pruritis
Post-PV myelofibrosis

Answer 77

A

< 60 yo
No hx of thromboembolism

Answer 78

A

Therapeutic phlebotomies, 81mg asa, and lifestyle modifications.

Answer 79

A

Uncontrolled PV-associated symptoms.
Progressive increase of leukocytes or platelet counts
Symptomatic or progressive splenomegaly
Poor tolerance of phlebotomy.

Answer 80

A

Therapeutic phlebotomy
Low dose ASA
Life-style modifications
Hydroxyurea

Answer 81

A

15 year median survival.
MC of death is thrombosis

Answer 82

A

Myelofibrosis
CML
AML (Rare)

Answer 83

A

Disorder of increased proliferation of the megakaryocytes (platelet precursor)

Cause by JAK2 mainly.
Others include calreticulin (CALR) or myeloproliferative leukemia virus oncogene (MPL)

Answer 84

A

50-60 yo.

Answer 85

A

Microvascular occlusion (finger/toe pain relieved by asa)
Thrombosis
HA
Transient dizziness, unsteadiness, vertigo, syncope
Bleeding (rare)

Answer 86

A

Plts > 2million
Mild leukocytosis

Answer 87

A

large plts

Answer 88

A

Increased megakaryocytes

Answer 89

A

JAK2, CLR, MPL

Answer 90

A

60 YO
HX OF THROMBOSIS
JAK2 MUTATION

plt> 1.5mil
Obesity
CV risk factors
Hypercoagulable state

Answer 91

A

High-risk = Hx of thrombosis and/or >60 + JAK2 mutation.

Intermediate-risk = >60, no JAK2, no hx of thrombosis

Low-risk = <60, JAK2 +, no hx of thrombosis

Very low-risk = <60, no JAK2, no hx of thrombosis

Answer 92

A

Observation and baby asa.
Avoid NSAIDs.

Answer 93

A

HU with target plt count of 100k-400k

Answer 94

A

Thrombosis.

Keep plt < 500k

Answer 95

A

Elevated RBC/Hgb/Hct due to an acquired or congenital disorder.

Answer 96

A

Tissue hypoxia
Decreased renal perfusion
Inappropriate EPO secretion
Testosterone administration

Answer 97

A

NO SPLENOMEGALY

Answer 98

A

Long-term hypoxia

Answer 99

A

Elevated EPO.

Answer 100

A

Treat the underlying condition.

Answer 101

A

Elevated PLT count that develops 2/2 to another disorder.

Answer 102

A

Depends on etiology.

Increased megakaryocyte proliferation/maturation.

Accelerated plt release

Reduced plt sequestration/turnover (asplenia)

Answer 103

A

Increased production of the inflammatory cytokines (Infection, chronic inflammatory processes, or malignancy)

Stimulation of the RBC progenitors leading to plt progenitor increase as well. Caused by anemias (hemorrhage, iron deficiency, and hemolysis)

Answer 104

A

ESR
CRP
ANA
RF

Answer 105

A

Elevated PLTs
Variable RBCs

Answer 106

A

Iron studies
Peripheral Smears
Retic counts

Answer 107

A

Treating the underlying condition.

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Lecture 13: Leukocyte Disorders Part 2 Flashcards

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