Lecture 12: Leukocyte Disorders Part 1

Question 1

What is a bone marrow biopsy/aspiration?

Answer 1

Drilling a hole into bone to obtain cellular contents of bone marrow.

Question 2

What are CIs of bone marrow biopsy?

Answer 2

Severe bleeding disorders (DIC, hemophilia)
Thrombocytopenia is a relative CI.
(it actually says that thrombocytopenia is not a CI but if they are <20,000 platelets then may want to consider infusion before obtaining biopsy)

Question 3

What can we test with a bone marrow biopsy?

Answer 3

Histology
Cytogenetic testing (testing for chromosome abnormality)
Flow-cytometry (analyzes cells for abnormalities)

Question 4

What are the indications of a bone marrow biopsy?

Answer 4

Diagnosing, staging and therapeutic monitoring of bone marrow disorders

Unecplained elevation or decreased in any hematopoietic cell line

Lymphoma/solid tumors

Evaluation of iron metabolism and stores when routine iron testing is inadequate

FUO

Unexplained slenomegaly

Question 5

Where do we NOT perform a bone marrow biopsy?

Answer 5

Areas with signs of infection, injury, or excess overlying adipose tissue (NO FATTY AREAS)

Question 6

What is the preferred site for a BM biopsy/aspiration?

Answer 6

Posterior iliac crest

Alt is anterior iliac crest

Question 7

What is the preferred site for a BM aspiration only?

Answer 7

Tibia (under general anesthesia, used for infants <1yo)

Sternum (2nd and 3rd ICS, older than 12yo + morbid obese)

Question 8

What is the main cause of acute lymphoblastic leukemia (ALL)?

Answer 8

Chromosomal translocation

Question 9

What is ALL?

Answer 9

Malignant disorder that originates in a single lymphocyte, resulting from an abnormal expression of genes.

It is the cell immediately after the common lymphoid progenitor.

Question 10

What 4 things does ALL result in?

Answer 10

Rapid cell proliferation/self-renewal
Reduction in normal cell proliferation
Block in cell differentiation
Increased resistance in cell apoptosis.

Essentially, it stays as an immature lymphoblast, making more of itself. Since it stays immature, it does not enter apotosis easily.

Question 11

How does ALL impair hematopoiesis?

Answer 11

Accumulation of the lymphoblasts within the bone marrow suppresses the normal hematopoiesis since there is limited room.

Once it builds up, the bone marrow releases the lymphoblasts elsewhere to other organs.

Question 12

How likely is ALL due to genetics vs environment?

Answer 12

Genetics are only 5% of cases.

95% are due to environmental factors.

Question 13

What are the environmental factors associated with ALL?

Answer 13

In utero radiation exposure.
Chemicals
High birth weight (increase insulin-like growth factor 1)
LACK OF EXPOSURE to infections in the first few weeks of life.

Question 14

Who is ALL MC in ?

Answer 14

Children, usually DXd prior to 15yo.

Question 15

What gender is ALL MC in?

Answer 15

Males by a little.

Question 16

What is the MC symptom in ALL?

Answer 16

FUO (fever of unknown origin)

Question 17

What 3 hematologic conditions are common in ALL?

Answer 17

Neutropenia
Anemia
Thrombocytopenia

Question 18

What is the main cause of all the S/S in ALL?

Answer 18

The direct infiltration of marrow or other organs by leukemic cells.

Question 19

When does most deaths due to ALL occur?

Answer 19

In adults.

Question 20

What are significant S/S of ALL?

Answer 20

LAN (often all lymph nodes, not specific)
Bone pain (a deep pain at night that wakes them)
Early satiety (splenomegaly bc stomach is compressed)
Mediastinal mass
Painless testicular swelling/mass

Question 21

What is leukostasis?

Answer 21

Hyperleukocytosis, aka WBCs > 100k

Leads to inadequate circulation.

Question 22

How emergent is leukostasis?

Answer 22

Very!

Risk of ICH, that lasts even 1 week after reduction.
40% mortality in 2 days if not treated.

Question 23

How would someone would ALL potentially describe their symptoms?

Answer 23

Deep aching pains at night
Getting full very easily
Dysphagia, persistent chest pain
General swelling of lymph nodes

Question 24

What would an initial workup of ALL be?

Answer 24

CBC
CMP
Blood cultures
CXR
CT/MRI Brain (WITHOUT contrast)

Question 25

What would I expect on a CBC of an ALL patient?

Answer 25

Decreased RBC, platelets, and neutrophils.
WBC could be low, normal, or high.

Question 26

Why do we order a CXR for an ALL patient?

Answer 26

R/o pneumonia
Check mediastinal mass

Question 27

Why do we order a brain MRI/CT?

Answer 27

Neurologic s/s
Leukostasis suspected

Question 28

Case Study:

Further history reveals the patient has multiple febrile illness recently but no specific cause was identified. Mother has noticed that he has been less energetic than usual. On exam, you note the child has lost 5 lbs since last visit 6 mo ago. He has cervical, axillary, and inguinal LAN throughout, measuring 1.5-2.0cm.

What do these symptoms suggest? What are the key symptoms?

Answer 28

Febrile illness without cause = FUO.

Less energetic = possible anemia.

Lost 5 lbs = loss of appetite, early satiety

Generalized LAN = concern for systemic infection.

Question 29

When are blood cultures generally ordered?

Answer 29

Signs of infection.

Question 30

What are additional lab tests we could order to work-up ALL?

Answer 30

Peripheral smears
LDH
CT Chest with Contrast
CSF
flow cytometry
Bone marrow biopsy

Question 31

What would I typically see on a smear for an ALL pt?

Answer 31

Pancytopenia with circulating lymphoblasts.

Question 32

Why does LDH elevate in ALL?

Answer 32

Tissue destruction.

Question 33

When would I order an LP for ALL? What am I looking for?

Answer 33

All patients with suspected ALL to check for CNS involvement.

+ Lymphoblast cells in CSF.

Question 34

What would show up in a flow-cytometry test for an ALL patient?

Answer 34

ALL cells will express CD19 antigens and potentially CD10 antigens.

Lack of mature T-cell markers as well. (CD3, CD4, or CD8)

Question 35

What would show up in a bone marrow aspiration & biopsy for an ALL pt?

Answer 35

> 20% lymphoblasts per the WHO.

This is the definitive diagnostic method for ALL.

Question 36

What are the two treatments for ALL patients?

Answer 36

Induction chemotherapy
CNS prophylaxis

Question 37

What is the goal of induction chemotherapy?

Answer 37

Remission induction via multi-drug chemotherapy.

Question 38

How is CNS prophylaxis administered?

Answer 38

Intrathecal therapy at all stages.

Question 39

What is intrathecal therapy?

Answer 39

Direct administration of chemotherapy via administration directly into the EPIDURAL space.

Question 40

What should we do if ALL is highly suspect?

Answer 40

Refer to heme onc.

Question 41

What is the goal of post-remission therapy in young ALL pts able to tolerate chemo?

Answer 41

Readministration of the induction regimen in order to increase the time of remission.

Either intensified therapy or maintenance therapy.
Maintenance lasts 2-3 years, much longer.

Question 42

When can an ALL pt undergo intensified post-remission therapy?

Answer 42

They must have normal hematopoiesis.

Lasts 4-8 months.

Question 43

What is the post-remission therapy for older ALL pts who cannot withstand chemo?

Answer 43

Allogeneic stem cell transplant.

AKA all patients that are matching donors.

Question 44

How is an allogeneic stem cell transplant given?

Answer 44

Person undergoes massive, intensive chemo to irradiate all their bone marrow.

They are then transfused with the donor stem cells over an hour.

Question 45

How do we manage leukostasis in ALL pts?

Answer 45

Prophylaxis for tumor lysis syndrome via IV hydration and hypouricemia agents.

Emergent chemo and leukapheresis if leukostasis present.

Question 46

Why is tumor lysis syndrome so dangerous?

Answer 46

Spillage of tumor contents can cause massive electrolyte abnormalities.

Question 47

What is leukapheresis?

Answer 47

Removal of whole blood to remove the WBCs.

The blood is then retransfused into the patient.

Question 48

What is the cure rate of ALL in children vs adults?

Answer 48

90% in children.

50% in adults.

Question 49

If a patient with ALL relapses, when is it most likely to occur?

Answer 49

Within first 2 years.

Reappearance of leukemic cells at any site.

Question 50

Where is the MC site of relapse for an ALL pt?

Answer 50

CNS.

Hence why we do intrathecal chemo.

Question 51

What falls under good prognostic criteria for ALL?

Answer 51

1. No chromosomal abnormalities
2. Younger than 39
3. WBC < 30k
4. Complete remission within 4 weeks.

Question 52

Damage to what cell is the cause of Chronic Lymphocytic Leukemia? (CLL)

Answer 52

B cells

Question 53

What is the etiology of CLL?

Answer 53

Malignant lymphoid neoplasm characterized by accumulation of long-lived, functionally incompetent, small mature B cells.

Results in dysfunction in the maturation of B cells.

Question 54

What are the B cells of CLL unable to do?

Answer 54

They DO NOT RESPOND to immunologic stimulation.

Question 55

What are the epidemiology stats of CLL?

Answer 55

MC form of leukemia in the US!!

MC in elderly, 90% occur after age 50.

MC in white males.

Question 56

How does CLL commonly present?

Answer 56

LAN (MC finding)
Recurrent infections (Pneumonia, HSV, HZV)
HSM (early satiety)
S/S of anemia/thrombocytopenia in advanced CLL.

Question 57

How does a CBC of CLL appear?

Answer 57

WBC > 20k
Isolated absolute lymphocytosis is the HALLMARK SIGN.

+/- decreased RBC, platelets

Question 58

Bonus: What is normal WBC range?

Answer 58

5k-10k

Question 59

How does a peripheral smear of CLL appear?

Answer 59

Small mature lymphocytes.

+ Smudge cells
Prolymphocyte (precursor to a small lymphocyte)

Question 60

What does flow-cytometry reveal in a CLL patient?

Answer 60

Abnormal B-lymphocyte surface antigens

Generally used to confirm the diagnosis of CLL.

Question 61

Is a bone marrow biopsy/aspiration required to diagnose CLL?

Answer 61

NO!

It may still be performed.

Question 62

What is the difference in lymphocytes in ALL vs CLL?

Answer 62

ALL has lymphoBLASTS

CLL has MATURE lymphocytes.

ALL is also more common in children.

CLL is more common in elderly.

Question 63

What does low-risk/stage 0 CLL present as?

Answer 63

Lymphocytosis aline.

Lymphocyte >15k and > 40% lymphocytes in bone marrow.

Question 64

What does stage 1 CLL look like?

Answer 64

Lymphocytosis with enlarged node in any site.

Moderate risk.

Question 65

What does stage 2 CLL look like?

Answer 65

Splenomegaly or hepatomegaly or both.

Moderate risk.

Question 66

What does stage 3 CLL look like?

Answer 66

Anemia (Hgb < 11)

High risk

Question 67

What does stage 4 CLL look like?

Answer 67

Thrombocytopenia (< 100k)
High risk

Question 68

Modified Rai clinical system for staging CLL (Picture)

Answer 68

Question 69

What is the management for low-risk CLL?

Answer 69

Observation

Question 70

What are the treatment options for moderate-high risk CLL?

Answer 70

Multidrug chemo
Allogeneic stem cell transplant (uncontrolled on chemo)

Splenectomy (refractory splenomegaly and pancytopenia)

Question 71

Which of the treatment options for CLL is considered curative?

Answer 71

Allogeneic stem cell transplant.

Question 72

What is included in chemotherapy for CLL to decrease the duration of neutropenia?

Answer 72

Growth factors.

Question 73

What are the complications of CLL?

Answer 73

Obstructive LAN

Aggressive Large cell lymphoma (Richter syndrome)

AIHA or thrombocytopenia.

Question 74

What are the symptoms of richter syndrome?

Answer 74

Weight loss, fevers, night sweats, muscle wasting, increasing HSM, and LAN.

Question 75

What is acute myelogenous leukemia?

Answer 75

AML is a malignant disease of the bone marrow resulting from an arrest in the early development of myeloid precursors.

Question 76

What are the 4 pathophysiology concerns of AML?

Answer 76

Rapid proliferation of myeloblast WITHOUT DIFFERENTIATION into mature cells.

Abnormal myeloblasts are resistant to apoptosis

Accumulation of myeloblasts in marrow, blood, spleen, liver

Reduction of normal hematopoiesis due to marrow accumulation

Question 77

What are myeloblasts?

Answer 77

The precursor to all the granulocytes and monocytes.

Question 78

What is the pathogenesis of AML?

Answer 78

Chromosomal translocation and other genetic mutations.

Question 79

What are the main etiologies of AML?

Answer 79

Myelodysplastic syndrome (MC risk factor)

Trisomy 21, Bloom’s syndrome, Fanconi anemia

Environment

Chemotherapy

Question 80

What is MDS/myelodysplastic syndrome?

Answer 80

A bone marrow disease of unknown etiology that causes progressive cytopenia over years.

MC in older pts.

Question 81

What are the epidemiology stats of AML?

Answer 81

70 y/o median onset.

MC in white males in developed countries.

Question 82

What does a CBC of AML look like?

Answer 82

Decreased RBC, platelet and neutrophils.

WBC can be anything.

Question 83

What does a peripheral smear of AML look like?

Answer 83

Mostly myeloblasts.
Auer rods (CONFIRMATIVE DIAGNOSTIC)

Question 84

What is an Auer Rod?

Answer 84

Eosinophilic needle-like inclusion in the cytoplasm of myeloblasts.
It is a unique finding of abnormal fusion of primary granules.

Question 85

What lab test can distinguish AML from ALL?

Answer 85

Flow cytometry.

Myeloid antigens will appear in AML.

Question 86

When is an LP indicated for AML?

Answer 86

Symptomatic patients only.

CNS infiltration is typically RARE.

Question 87

When is a brain MRI/CT indicated for AML?

Answer 87

Leukostasis/neurologic symptoms.

Question 88

How do we manage AML?

Answer 88

Induction chemotherapy
Post-remission therapy (more chemo and/or stem cell trans)
CNS involvement will use intrathecal chemo.
Leukostasis will require leukapheresis and other tx.

Question 89

What are the two types of stem-cell replacement therapies for post-remission AML?

Answer 89

You can use allogeneic or autologous stem cell transplant for AML post-remission.

It is preferred to use ALLOgeneic stem cells.

Question 90

What are the good prognosis factors for AML?

Answer 90

Age < 60
Remission induction after first chemo.

Question 91

What is chronic myeloid leukemia? (CML)

Answer 91

Disorder characterized by dysregulated production and uncontrolled proliferation of mature and maturing granulocytes with NORMAL DIFFERENTATION.

Question 92

What is the cause of CML?

Answer 92

Translocation of the philadelphia chromosome, aka 9 to 22.

Question 93

How does translocation of 9 to 22 cause CML?

Answer 93

Genetic defect known as bcr/abl occurs.

bcr/abl produces a protein that has overactive tyrosine kinase activity.

Question 94

What does tyrosine kinase do?

Answer 94

Controls cell growth, differentation, metabolism, and apoptosis.

Question 95

When does CML usually occur?

Answer 95

55 y/o

Question 96

What is the only etiology of CML?

Answer 96

Increased risk with exposure to ionized radiation (DOSE RELATED)

Question 97

What are the 3 phases of CML?

Answer 97

1. Chronic: WBCs proliferate
2. Accelerated: Additional cytogenetic abnormalities occur
3. Terminal blast crisis: immature myeloid cells rapidly proliferate (FATAL)

Question 98

In what phase are most CML diagnoses made?

Answer 98

Chronic phase, phase 1.

85% of diagnoses are found incidentally and patients tend to stay in it for 3-5 years.

Question 99

What is the MC first symptoms noted by CML patients?

Answer 99

Fatigue and weight loss.

Question 100

What is the cause of pruritis, diarrhea, flushing, and GI ulcers in CML?

Answer 100

Overproduction of HISTAMINE by basophils.

Pruritis = histamine binding to nerves?
Diarrhea = irritation
Flushing = vasodilation
GI ulcers = histamine releases gastric acid

Question 101

How does the accelerated phase of CML present?

Answer 101

FUO
Bone pain
Marked splenomegaly
Acute leukemia signs: anemia, neutropenia, thrombocytopenia

Question 102

What is the most common PE finding in CML?

Answer 102

Splenomegaly.

You can also see hepatomegaly and LAN.

Question 103

How does a CBC for a CML patient in the chronic phase present?

Answer 103

WBC in the 100k-150k range.

Granulocytosis with marked increase in mature neutrophils, with a mild increase in basophils and eosinophils.

Question 104

Why do we not immediately treat a WBC of >100k for leukostasis?

Answer 104

We need symptoms to be sure.

CML presents with hyperleukocytosis with no neurologic symptoms.

Question 105

How does a CBC for a CML patient in the accelerated phase present?

Answer 105

Reduced platelets, RBC, increase in myeloblasts.

Question 106

How does a peripheral smear for a CML patient in accelerated phase present?

Answer 106

Peripheral blast cells and promyelocytes

Question 107

What is leukocyte alkaline phosphatase?

Answer 107

LAP is found in leukocytes.

We will see LOW LAP because the granulocytes are RESISTANT to apoptosis.

AKA cells aren’t dying, so they don’t release LAP.

Question 108

How does a bone marrow aspiration/biopsy present for a CML patient?

Answer 108

Hypercellular with increased granulocytes and progenitors.

> 20% blasts means they are in blast phase.

Question 109

What is a PCR used for in CML patients?

Answer 109

Identifying the bcr/abl segment within the philly chromsome.

Question 110

What is the standard therapy for a CML patient in phase 1/chronic phase?

Answer 110

SINGLE DRUG CHEMO.

Tyrosine kinase inhibitor, inhibiting the cells addiction to tyrosine kinase.

Targets CML death more than regular cells.

Question 111

What are the types of remission we can see in standard therapy for CML?

Answer 111

1. Hematologic remission within 3 months. Normal CBC/PE.
2. Cytogenetic remission within 6 months. Normal chromsone with < 10% philly cells.
3. Molecular remission within 1 year. Negative PCR for bcr/abl segment.

Question 112

How long do we continue therapy for CML after we reach molecular remission?

Answer 112

2 years!

Question 113

How do we treat the accelerated/blast phase of CML?

Answer 113

TKI + multidrug chemo

Consider allogeneic stem cell transplant. Also indicated if TKI doesn’t work.

TKI = tyrosine kinase inhibitor.

Question 114

What should we be monitoring for CML patients in regards to phase transition between chronic to accelerated?

Answer 114

Progressive splenomegaly
Inadequate decreases in granulocytes with standard therapy.
Blast cells and promyelocytes in peripheral smear
Anemia, Basophilia, and thrombocytopenia.
New cytogenetic abnormalities or myelofibrosis in BM biopsy.

Question 115

What is the prognosis for CML?

Answer 115

100% survival rate at 9 years if they responded to the TKI.

Question 116

What is multiple myeloma?

Answer 116

MM is a neoplastic proliferation of plasma cells overproducing a nonfunctional, monoclonal immunoglobulins.

Question 117

What is the pathogenesis of MM?

Answer 117

Preceded by a premalignant plasma cell proliferative disorder known as monoclonal gammopathy of undetermined significance. (MUGS)

Question 118

What does MUGS come from?

Answer 118

Abnormal plasma cell response to antigenic stimulation.

Question 119

What are the epidemiology stats of MM?

Answer 119

Median onset of 65 yo.
Most common in african american males, rather than white males.

Question 120

What are the 5 pathophysiologies of MM?

Answer 120

1. Proliferation of neoplastic plasma cells in the bone marrow results in DIMINISHED HEMATOPOIESIS.
2. Neoplastic plasma cells are monoclonal, resulting in LACK OF ADEQUATE IMMUNOGLOBULIN RESPONSE to infection.
3. Neoplastic plasma cells increase osteoCLASTIC acitivty, bone tumor formation, and hypercalcemia
4. Neoplastic plasma cells secrete an antibody called myeloma proteins, which are harmful to the KIDNEYS, NERVES, and other organs.
5. Infiltration of plasma cells in tissues, leading to plasmacytomas.

Question 121

How does MM typically present?

Answer 121

MC is skeletal symptoms, esp in the axial skeleton.

Bone pain in the back, hips, and ribs
Spinal cord compression
Pathologic fractures
Hypercalcemia causing skeletal destruction

Question 122

How does MM affect BM?

Answer 122

Anemia
Neutropenia
Thrombocytopenia

Question 123

How does MM affet the kidney?

Answer 123

Reduced kidney function or failure.
PROTEINURIA
Oliguria

Question 124

How does MM present neuro-wise?

Answer 124

Radiculopathy or neuro deficits

Peripheral nerve compression, MC is median nerve (carpal tunnel syndrome)

Question 125

What do plasmacytomas do?

Answer 125

Cause bleeding and obstruction.
Affects many organs.

Question 126

What kind of CBC would I expect in MM?

Answer 126

Pancytopenia

Question 127

What would I see in a smear of a MM patient?

Answer 127

RBC Rouleaux formation.

Question 128

What would I expect in a CMP of a MM patient?

Answer 128

Hypercalcemia
Elevated BUN/Cr

Question 129

What would I expect in a BM biopsy/aspiration of a MM patient?

Answer 129

Infiltration of monoclonal plasma cells by morphologically ABNORMAL cells.

Question 130

What would I see in a protein electrophoresis of MM?

Answer 130

+ Paraprotein (M-protein)

Question 131

What would I see in a urine protein electrophoresis of MM?

Answer 131

+ Bence Jones protein

Question 132

What would I see in a quantitative immunoglobulin level of MM?

Answer 132

Suppression of the NON-myelomatous immunoglobulins (IgG, IgM, IgA)

Question 133

What test do I run for prognostic testing of MM?

Answer 133

Beta-2 microglobulin.

Elevated is directly related to the tumor burden.

Question 134

What am I looking for in an XRAY of MM?

Answer 134

Lytic lesions or pathologic fractures in the skull, spine, or long bones.

Question 135

What is a CT scan used for in MM?

Answer 135

Monitor for neoplastic bone disease.

Question 136

What is a MRI spine used for in MM?

Answer 136

Assess spinal nerve decompression.

Question 137

How do we manage MM?

Answer 137

It is incurable.
The goal is palliative.

Question 138

What is the treatment protocol for MM?

Answer 138

Triple agent chemo for induction.

Autologous stem cell transplant after chemo if pt is younger.

Localized radiation for bone pan related to tumor formation.

Question 139

How do we manage pathologic fractures in MM?

Answer 139

Stabilize bone
Irradiate lesion

Question 140

How do we manage vertebral body collapse in MM?

Answer 140

Spinal ortho for kyphoplasty or vertebroplasty

Question 141

How do we manage spinal cord compression in MM?

Answer 141

IV steroids to reduce swelling.
Radiation therapy
Consult neurosurgery

Question 142

How do we manage bone disease/hypercalcemia in MM?

Answer 142

Bisphosphonates if renal function intact.

Drug: IV Reclast

Question 143

How do we manage anemia in MM?

Answer 143

EPO therapy if persistent and no other possible etiologies.

Question 144

How do we manage renal impairment in MM?

Answer 144

Plasmaphersis to remove M-proteins/paraproteins.

Question 145

What is the median survival rate for MM?

Answer 145

3 years ):