Drugs and the Blood (plus additional reading)

Question 1

What are 3 presentations (drug characteristics) that may result in changes in protein binding to a drug?

Answer 1

1. Highly protein bound (ceftriazone, phenytoin)
2. High clearance drugs (particularly those cleared by glomerular filtration)
3. Drugs in which dosing is not titrated to effect (or half-life; i.e. antibiotics)

Question 2

What is most affected by changes in the concentration of the protein-bound fraction of a drug?

Answer 2

The unbound drug concentration

For instance: if the protein-bound drug changes from 99% to 95%, the [unbound] just increased 5 fold

Question 3

Which has a greater effect: a change from 98% to 94% [protein-bound drug] or from 5% to 1% [protein-bound drug]?

Answer 3

98% to 95%
(a change in concentration for a minimally bound drug hardly affects the conc, dist, clearance or pharmacokin of the unbound portion)

Question 4

What is most affected by changes in the concentration of the unbound fraction of a drug?

Answer 4

changes in pharmacokinetics

Question 5

What are 3 ways in which neonatal drug-protein binding varies from adult?

Answer 5

A larger amount of drug remains unbound due to the lower blood concentration of plasma proteins

Question 6

How will administering a second drug with greater protein affinity affect a previously administered drug?

Answer 6

The second drug will displace the first (which will then alter the balance of bound versus unbound drug)

Question 7

Why are antibiotics as risk of significant changes in drug pharmacokinetics?

Answer 7

They have multiple half-lives within a single dosing interval

Question 8

In high clearance drugs, what is most affected by changes in protein binding?

Answer 8

Clearance

Distribution/Vd

Question 9

What is the most common adverse clinical consequence of G6PD deficiency?

Answer 9

drug-induced hemolysis

-NADPH is not regenerated, thus glutathione is not reduced; reactive O intermediate cannot be removed

Question 10

What is the function of G6PD?

Answer 10

Protect RBC from oxidative damage

Question 11

Medications that are contraindicated in G6PD deficiency:

Answer 11

Pegloticase
Quinine
Rasburicase
Sulfamethoxazole

(Did he say we needed to know this?)

Question 12

What is eryptosis?

Answer 12

suicidal erythrocyte death

Question 13

How does Ca affect the cell (intracellularly)?

Answer 13

1. Activation of Ca-permeable, non-selective cation channels results in increased cytosolic Ca activity
2. (Inside the cell) Ca activates Ca-sensitive K channels –> K exits, and the cell becomes hyperpolarized –> Cl exits
3. Loss of KCl = loss of water, cell shrinks

Question 14

How does Ca affect the cell membrane?

Answer 14

Ca stimulates cell membrane scrambling (via inhibition of “scramblase”), which results in breakdown of phospholipid asymmetry and phosphatidylserine exposure at surface

Question 15

How is Ca involved in eryptosis?

Answer 15

Acts directly on RBC to promote Ca entry via ion channel

Question 16

What factors can cause a low platelet count?

Answer 16

1. Bone marrow doesn’t make enough
2. Bone marrow makes enough, but the body destroys them
3. Spleen holds on to too many platelets
   (or a combination of these factors)

Question 17

What is the primary manifestation in HIT?

Answer 17

thrombocytopenia

Question 18

6 risk factors for HIT:

Answer 18

1. Female sex
2. IV administration of heparin (versus subcut)
3. Bovine heparine (versus porcine)
4. Post-op patients (worse for ortho srx)
5. Heparin exposure for >4 days
6. Exposure to unfractioned heparin (versus low-mol-weight)

Question 19

By what mechanism does HIT occur?

Answer 19

1. Heparin/PD4 binds with anti-heparin/PD4-IgG
   (drug joins glycoprotein and CDR on antibody)
2. Immune complex binds to Fc receptor on surface of resting platelet, activating it
3. Activated platelet deposits onto subendothelial matrix

Question 20

In HIT, what may be variable among patients?

Answer 20

severity

timing of onset after heparin

Question 21

How does non-immune HIT differ from immune HIT?

Answer 21

1. Milder
2. No antibodies
3. Low thrombosis risk
4. Onset occurs <5 days after exposure
5. Treated via observation (rather than discontinuation of heparin)

Question 22

What may induce an earlier onset of HIT?

Answer 22

administration of heparin in the past 1-3 months

Question 23

What may cause a delayed onset of HIT?

Answer 23

formation of heparin-independent antibodies (drug acts as an intermediate in an otherwise weak reaction)

Question 24

T?F: Heparin is the only drug capable of inducing immune thrombocytopenia.

Answer 24

F (penicillin, quinine, NSAIDs, abciximab, l-dopa, etc)

Question 25

What is the most common cause of peripheral blood cytopenias in the industrial world?

Answer 25

myelosuppression

Question 26

What dose-limiting side effect is caused by cytotoxic agents?

Answer 26

myelosuppression

Question 27

T/F: Myelosuppression can be an idiosyncratic drug reaction.

Answer 27

T

Question 28

How do drugs cause peripheral cytopenias?

Answer 28

shortening the survival of blood cells (does NOT affect marrow cell production)

Question 29

What are 2 disorders related to drug-induced myelosuppression?

Answer 29

Autoimmune hemolytic anemia

Immune Thrombocytopenia

Question 30

What glycoproteins are available for therapeutic use?

Answer 30

G-CSF
GM-CSF
EPO (human recombinant)

Question 31

What are non-cytotoxic mechanisms that induce myelosuppression?

Answer 31

1. defects in hematopoietic stem cells
2. damage to stroma (marrow)
3. inhibition of production/release of hematopoietic growth factors
4. Immunosuppression of marrow cells

Question 32

T/F: The immune system plays an important role in immunosuppression via B-cell mediated activity.

Answer 32

F: T cell mediated

Question 33

What are 6 classes of drugs associated with iosyncratic myelosuppression?

Answer 33

1. antimicrobials
2. antirheumatics
3. antithyroid
4. anticonvulsants
5. psychotropic agents
6. cardiovascular drugs

Question 34

The incidence of severe or opportunistic infections increase as _____ levels decrease.

Answer 34

neutrophil

Question 35

What is the best immediate treatment of neutropenic, febrile patients?

Answer 35

empirical therapy with broad spectrum antibiotics (IV)

Question 36

What are 4 causes of agranulocytosis?

Answer 36

1. certain drugs (e.g. antithyroid)
2. Hypoplastic BM (does not produce cells)
3. Anti-neutrophil antibodies
   (“immuno-allergic”)
4. Toxicity to myeloid precursors
   (ATP depletion, reduce glutathione)

Question 37

What are 2 factors considered when a patient has developed agranulocytosis due to treatment with a particular drug?

Answer 37

• Duration of drug exposure prior to onset of acute agranulocytosis
• Time between onset of acute agranulocytosis and neut count normalization

Question 38

When giving drugs that are known to induce agranulocytosis, what should you do as a physician to prevent harm to the patient (and you…)?

Answer 38

follow with blood counts

*this won’t occur in every patient

Question 39

How do aspirin and NSAIDs differ in their anti-platelet activity?

Answer 39

• Aspirin irreversibly acetylates platelets, rendering it nonfunctional (thromboxane)
• NSAIDs are reversible
• Clopidogrel act on ADP receptors

Question 40

How does clopidogrel affect platelets?

Answer 40

Antagonizes ADP receptors

Question 41

Anti-platelet drugs inhibit:

Answer 41

platelet aggregation

Question 42

How does warfarin inhibit coagulation?

Answer 42

inhibits vitamin K dependent activation of clotting factors II (thrombin), VII, IX, X

Question 43

How does heparin inhibit coagulation?

Answer 43

catalyzes inactivation of clotting factors II and X

low molecular weight heparin = only X

Question 44

How does dabigatran inhibit coagulation?

Answer 44

inhibits thrombin

Question 45

Why must warfarin be monitored closely?

Answer 45

response to dosing rate will be pharmacogenomically determined

Question 46

What stimulates EPO synthesis? Where?

Answer 46

Hypoxia, kidneys

Question 47

Why does renal failure cause anemia?

Answer 47

decreased EPO production

Question 48

How does EPO affect cancer growth?

Answer 48

Increases metastasis, resistance to chemo and evasion of apoptosis
(*related to increased cancer risk)

Question 49

How does folic acid deficiency result in glossitis?

Answer 49

Inadequate DNA synthesis (which affects rapidly growing tissues such as tongue)

Question 50

How does folic acid deficiency result in megaloblastic anemia?

Answer 50

Reduced DNA synthesis relative to RNA synthesis, causing unbalanced cell growth and omitted cell divisions during erythropoiesis

Question 51

How does cobalamin deficiency cause neuro disease and degeneration?

Answer 51

Causes demyelination

Question 52

What cytokine plays a role in asthma?

Answer 52

GM-CSF

Question 53

What is the function of cytokines?

Answer 53

Control of proliferation of blood components (through signaling and inflammation)

Question 54

What are the major actions of G-CSF?

Answer 54

• Increase neutrophil production
• Increase neutrophil survival/adhesion
• Increased mobilization of blood cells into blood
• Decreased T cell reactivity, with increased Treg production

Question 55

What are the major functions of GM-CSF?

Answer 55

• Maturation of dendritic cells
• Steady-state differentiation of macroph/NK
• Mobilization of myeloid cells into blood
• Survival/activation of macro, neut, eosin

Question 56

Cardiovascular adaptations to chronic anemia:

Answer 56

tachycardia
increased cardiac output
vasodilation

Question 57

Most common cause of chronic anemia:

Answer 57

IRON DEFICIENCY

Question 58

Functions of iron:

Answer 58

iron-porphyrin heme ring (component of Hg)

Question 59

How does iron deficiency affect RBC?

Answer 59

results small hemoglobin-deficient erythrocytes, which causes microcytic hypochromic anemia

Question 60

T/F: The body reclaims Fe, thus only a small amount is lost every day

Answer 60

T

Question 61

What type of iron should be used to treat deficiency?

Answer 61

ferrous salts

Question 62

How many mg of elemental iron should be given daily to correct iron deficiency most quickly?

Answer 62

200-400 mg

Question 63

Why should oral iron should be continued for 3–6 months after correction of the cause of anemia?

Answer 63

1. correct the anemia

2. replenishes iron stores

Question 64

What are the most common toxic effects of iron supplements?

Answer 64

Nausea, epigastric discomfort, abdominal cramps, constipation, and diarrhea

Question 65

How can toxic effects of iron supplements be overcome?

Answer 65

lowering the daily dose of iron or by taking with food

also–trying another salt may help

Question 66

Why may obscure the diagnosis of continued GI blood loss?

Answer 66

Iron supplements turn stool black

Question 67

What conditions may result in inability to correct anemia with oral iron alone (need parenteral)?

Answer 67

• advanced renal disease
• gastrectomy or bowel resections
• inflammatory bowel disease of prox small bowel
• Malabsorption syndrome

Question 68

What treatment challenge is associated with parenteral administration of inorganic free ferric iron?

Answer 68

Dose-dependent toxicity (which limits the dosage that can be given)

Question 69

What is a colloid formulation of iron?

Answer 69

carbohydrate surrounding a core of iron oxyhydroxide

Question 70

What iron formulation is most likely to cause hypersensitivity reactions?

Answer 70

parenteral IV Iron dextran

thus, you should always give a test dose

Question 71

Why should patients on parenteral iron be tested for iron overload?

Answer 71

parenteral route bypasses the absorptive regulatory processes that are involved in oral routes

Question 72

What serum concentrations can be used to determine iron stores?

Answer 72

ferritin

transferrin saturation

Question 73

What is total iron-binding capacity?

Answer 73

Ratio of total serum iron concentration to total iron-binding capacity

Question 74

What condition may be caused by acute iron toxicity in children?

Answer 74

Necrotizing gastroenteritis
(nausea, vomiting, bloody diarrhea, shock; patients will improve initially, then experience metabolic acidosis, coma or death)

Question 75

What are two ways to detoxify a patient with iron overload?

Answer 75

Whole bowel irrigation

Deferoxamine [Desferal] (potent Fe chelator)

Question 76

How is Deferoxamine [Desferal] excreted?

Answer 76

Urine (turns it red)

Bile

Question 77

What is hemochromatosis?

Answer 77

chronic iron toxicity disorder in which excess iron is deposited in heart, liver, pancreas, etc; can lead to organ failure and death

Question 78

Hemochromatosis is most commonly seen in what type of patients?

Answer 78

1. Patients with inherited hemochromatosis (absorb too much Fe)
2. Patients who receive lots of transfusions over time (thalassemia)

Question 79

How is chronic iron overload in the absence of anemia is most efficiently treated?

Answer 79

intermittent phlebotomy (1 unit/week)

Question 80

What serum levels are increased by Deferasirox [Exjade]?

Answer 80

creatinine
hepatic enzymes

*this drug treats chronic iron overload

Question 81

What are common side effects of Deferasirox [Exjade]?

Answer 81

• Diarrhea, nausea, abd pain, headache, pyrexia, cough
• Auditory and visual disturbances

*this drug treats chronic iron overload

Question 82

What are common causes of B12 deficiency?

Answer 82

inadequate supply in diet

inadequate absorption

Question 83

What are 3 symptoms of B12 deficiency?

Answer 83

Megaloblastic anemia
Macrocytic anemia
Neurologic syndrome
(paresthesia progressing to ataxia, etc;
B12 halts but not necessarily reverses)

Question 84

What are common causes of B12 deficiency?

Answer 84

Pernicious anemia
Partial or total gastrectomy
Conditions affecting distal ileum
(malabsorption, inflamm bowel, resection)

Question 85

What are rare causes of B12 deficiency in adults?

Answer 85

Bacterial overgrowth in small bowel
Chronic pancreatitis
Thyroid disease

Question 86

What are rare causes of B12 deficiency in children?

Answer 86

1. congenital deficiency of intrinsic factor

2. defective receptor sites for vitamin B12-intrinsic factor complex (in distal ileum)

Question 87

T/F: Most B12 deficiency diseases are resolved with injected B12.

Answer 87

F: “Most patients do not have curable

deficiency syndromes and require lifelong treatment with vitamin B12”

Question 88

Why is hydroxocobalamin preferable to cyanocobalamin?

Answer 88

More highly protein-bound, remains longer in the circulation

Question 89

Folic acid deficiency is most commonly found in (5):

Answer 89

Pregnant women
Malabsorption syndromes
Dialysis patients
Alcoholics
Liver disease

Question 90

Reduced forms of folic acid are precursors for:

Answer 90

synthesis of amino acids, purines, and DNA

Question 91

Folic acid oral absorption is (high/low)

Answer 91

high–even in patients with malabsorption syndrome

Question 92

Trimethoprim and pyrimethamine are (more/less) likely than methotrexate to
produce folate deficiency.

Answer 92

less (they have a greater affinity for bacterial and malarial dihydrofolate reductase)

Question 93

What antimicrobial drug causes folate deficiency?

Answer 93

Trimethoprim

Question 94

What antiseizure drug causes folate deficiency?

Answer 94

Phenytoin

Question 95

What drug rescues cells from the effects of folate antagonists?

Answer 95

LEUCOVORIN

Question 96

T/F: Excessively high folate levels have been linked to depression.

Answer 96

F: low levels

Question 97

Biologically active form of folate in circulation?

Answer 97

Levomefolate

6(S)-5-methyltetrahydrofolate and L-methylfolate

Question 98

What enzyme reduces folate and dihydrofolate?

Answer 98

MTHFR (methylenetetrahydrofolate reductase)

Question 99

How does reduced folate enter cells?

Answer 99

Once converted to levomefolate, transported across cell membranes by receptor-mediated endocytosis

Question 100

What is the function of levomefolate once it crosses the BBB?

Answer 100

modulates formation of monoamines (serotonin, norepinephrine, dopamine)

Question 101

What is the function of epoetin alpha?

Answer 101

Agonizes EPO receptors on RBC progenitors, which stimulates RBC prolif/diff
*causes reticulocyte release from BM

Question 102

What is epoetin alpha used to treat?

Answer 102

1. anemia (esp in chronic renal failure, HIV, cancer)

2. prevent the need for transfusion (elective surgery)

Question 103

What does the prefix “peg-“ mean?

Answer 103

original drug has been reformulated with addition of polyethylene glycol moieties (extends PKs of the drug, less frequent re-dosing)

Question 104

The erythropoietin receptor is a member of what superfamily of cytokine receptors?

Answer 104

JAK/STAT’s

Question 105

What growth factor induces maturation into RBC?

Answer 105

EPO

Question 106

What growth factors induce maturation into granulocytes, eosinophils, basophils?

Answer 106

GM-CSF and C-CSF

Question 107

What growth factors induce maturation into monocytes?

Answer 107

GM-CSF and M-CSF

Question 108

What growth factor induces maturation into megakaryocytes?

Answer 108

CFU-Meg

Question 109

What growth factors induce maturation into platelets?

Answer 109

IL6, IL11, thrombopoietin

Question 110

How is hypoxia related to EPO production?

Answer 110

Gene transcription inversely related to tissue oxygenation levels

Question 111

Severely anemic patients have (high/low) EPO.

Answer 111

high

Question 112

Patients with renal disease (are/aren’t) likely to respond to exogenous EPO.

Answer 112

ARE likely

Question 113

Patients in renal failure have (high/low) EPO.

Answer 113

low–kidneys cannot produce the growth factor

Question 114

Black box warning: Patients with what disorder had greater risk of death, stroke or CV problems when taking erythropoiesis-stimulating agents if their hgb>11?

Answer 114

chronic kidney disease

Question 115

Black box warning: Why are erythropoiesis-stimulating agents given in lowest possible dose and used only for anemia from myelosuppressive chemo?

Answer 115

shown to shorten overall survival and/or increase risk of tumor progression in some cancers

Question 116

In patients with cancer, what is prophylactically treated if taking erythropoiesis-stimulating agent?

Answer 116

DVT

Question 117

Why should methoxy polyethylene glycol epoetin beta not be used for treatment of
anemia caused by chemo?

Answer 117

a clinical trial found significantly more deaths among patients receiving this form of erythropoietin

Question 118

What does G-CSF stimulate?

Answer 118

1. proliferation and differentiation of progenitors already committed to the neutrophil lineage
2. Activation of phagocytic activity of mature neutrophils (and prolongs survival)
3. Mobilizes hematopoietic stem cells (increase their concentration in periph blood–use in stem cell transplantation)

Question 119

What toxicities are associated with G-CSF?

Answer 119

bone pain (after discontinued)
splenic rupture (rarely, when used for PBSCs)

Question 120

Which myeloid growth factor is more likely to cause fever: G-CSF or GM-CSF?

Answer 120

GM-CSF (also more likely to cause arthralgia, myalgia, capillary leak syndrome)

Question 121

What myeloid growth factor stimulates T cell proliferation?

Answer 121

GM-CSF (with the help of IL2)

Question 122

What are 3 ways that GM-CSF affects blood cell?

Answer 122

1. stimulates proliferation and differentiation of early and late granulocytic progenitor cells
2. growth factor for erythroid and megakaryocyte progenitors
3. stimulates the function of mature neutrophils

(also mobilizes periph blood cells, but less effectively than G-CSF)

Question 123

Why is G-CSF given after dose-intensive chemo?

Answer 123

Speeds up rate of neutrophil recovery, which reduces episodes of:

 1. febrile neutropenia 
 2. need for broad-spectrum abx
 3. infections
 4. hospital length of stay

Question 124

T/F: G-CSF improves patient survival rates after chemo.

Answer 124

F

Question 125

Explain the benefit of administering G-CSF to a patient that is ABOUT to undergo high-dose chemo.

Answer 125

Because the chemo will induce myelosuppression, patients are given G-CSF (to mobilize peripheral blood stem cells) and stem cells are harvested.

After chemo, patients receive an autologous stem cell transplantation (with the cells that were collected) to counteract chemo’s effects.

Question 126

What is often collected as the hematopoietic preparation for autologous transplantation (instead of BM)?

Answer 126

PBSCs (peripheral blood stem cells)

Question 127

What drug is the long acting form of G-CSF [filgrastim] that is covalently linked to polyethylene glycol?

Answer 127

pegfilgrastim

peg=polyethylene glycol

Question 128

Where does oprelvekin often cause fluid to accumulate?

Answer 128

lungs

Question 129

What does oprelvekin [neumega] stimulate?

Answer 129

megakaryocytopoiesis and thrombopoiesis

*megak maturation results in increased platelet production

Question 130

To which receptor does oprelvekin bind?

Answer 130

IL-11 receptor on megakaryocytes and megakaryocyte progenitor cells
(receptor interactions with signal transducing receptor gp130, whatever that is)

Question 131

What is oprelvekin approved to treat?

Answer 131

prevention of thrombocytopenia in patients receiving

cytotoxic chemo for nonmyeloid cancers

Question 132

Oprelvekin is administered subcut in order to:

Answer 132

increase platelet count to >50,000

Question 133

What toxic CV effects are associated with oprelvekin?

Answer 133

Anemia (due to hemodilution)
Dyspnea (due to fluid accumulation in lungs)
Transient atrial arrhythmias
*all are reversible

Question 134

What are the components of the 2 identical subunits of Romiplostin [Nplate], and what to they do?

Answer 134

1. Peptide sequence: binds/activates TPO receptor

2. Fc: extends half life (remains in circ much longer than endogenous TPO)

Question 135

What removes Romiplostin [Nplate] from circulation?

Answer 135

reticuloendothelial system

Question 136

Most common toxicities related to Oprelvekin; rh-IL-11 [Neumega]:

Answer 136

fatigue, headache, dizziness

less common = hypokalemia