module 7 hemolytic anemia

Question 1

signs increased RBC production:

Answer 1

RPI >2, inceased IRF, leukocytosis, nucleated RBCs, polychromasia of RBCs, normoblastic erythroid hyperplasia.

Question 2

signs increased RBC destruction

Answer 2

Anemia, schistocytes, spherocytes, positive DAT, decreased haptoglobin andhemopoexin, increased billirubin and urobillinogen, increased serum LD, increased CO.

Question 3

Signs increased IV hemolysis

Answer 3

hemoglobinemia and uria, hemosiderinuria, methemoglobinemia

Question 4

clinical findings HA

Answer 4

jaundice, gallstones, dark or red urine in IV hemolysis, anemia, thinning cortical bone, Extramedullary hematopoeisis, splenomegaly.

Question 5

loss of vertical interactions

Answer 5

cause microvessicles and spherocytes (ankyrin, band 4 protein 4.2)

Question 6

loss of horizontal interactions leads to

Answer 6

poikilocytes (spectrin, actin, protein 4.1, GPC)

Question 7

acanthocyte

Answer 7

spiked membrane, excess in outer layer

Question 8

stomatocyte

Answer 8

looks like kissing lips or coffee bean,

Question 9

lipid composition defects characterized by

Answer 9

acanthocytes

Question 10

Hereditary spherocytosis

Answer 10

deficient in membrane proteins, permeable monovalent cations. Often combined spectrin ankyrin deficiency. Membrane loss causes decreased SA to volume ratio and spherocyte. More permeable to Na, causing pumps to work harder expend more glucose. Can be well compensated. Can have aplastic crisis after viral infection.

Question 11

HS LAB RESULTS

Answer 11

Reticulocyte count > 8%. MCHC increased. MCV decreased. increased billirubin, increased LD.

Question 12

Osmotic fragility test

Answer 12

incubate in varying NaCl solutions. HS hemolyze at higher salt concentrations than normal. Little water can be absorbed before lysis. If < 2% spherocytes, incubate overnight at 37C before addition to NaCl. Increases SA loss and spherocyte formation.

Question 13

Target cells and thalassemia in osmotic fragility test

Answer 13

target cells such as those in thalassemia shift to right because lysis occurs at lower NaCl concentration due to increased SA to volume ratio.

Question 14

Autohemolysis test

Answer 14

incubate cells at 37C. Increased hemolyisis due to membrane chages. corrected by addition of glucose. Autohemolyisis increases in immunue hemoluytic anemia, but glucose does not correct.

Question 15

HS and HE shape acquired

Answer 15

in the circulation, not created with misshape.

Question 16

HE defect

Answer 16

horizontal interactions, such as: defective spetrin chains decrease dimer : tetramer ratio, band 4.1 defect, , abnormal GPC/ band 3.

Question 17

HE clinical findings

Answer 17

hemolysis mild and well compensated. Membrane more rigid, may provide malaria defense.

Question 18

HE lab findings

Answer 18

> 25 % elliptocytes. Osmotic fragility positive but not necessary as picture is obvious. Responds well to splenectomy.

Question 19

HPP defect

Answer 19

disintegrate at 45-46C unlike normal at 50C. or >37C for 6 hours. Due to inheritance of both a mutant spectrin and a decreased expression spectrin gene. Disruption membrane, fragmentation, poikilocytosis.

Question 20

HPP clinical and lab finding

Answer 20

exchange transfuion needed. bizarre shapes. Extreme microcytosis 25-55 fL MCV. Osmotic fragility abnormal after incubation and heat. Autohemolysis not corrected by glucose. SPlenectomy.

Question 21

Overhydragted hereitary stomatocytosis

Answer 21

Gain of Na+ which exceeds K+ loss. Water enters cell, causes formation of stomatocyte.

Question 22

dehydrated hereditary spherocytosis

Answer 22

Loss of K+ which exceeds Na gain. water leaves cell, becomes targeted.

Question 23

HSS clinical and lab findings

Answer 23

abnormal cation permeability. mild to moderate anemia, 10-50% stomatocytes. osmotic fragility and autohemolysis increased, partially corrected by glucose.

Question 24

acanthocytosis

Answer 24

increased sphingomyelin secondary to plasma changes. expansion of outer leaflet, decreased deformability. Not due to proteins. Abetalipoproteinemia, spur cell anemia,

Question 25

glucose corrects for autohemolysis test in

Answer 25

HS not IHA.

Question 26

SPUR CELL ANEMIA

Answer 26

type acanthocytosis associated with liver disease.

Question 27

G6PD

Answer 27

first step in Hexose monophosphate shunt for GSH. Therefore responsible for preventing cellular oxidation.

Question 28

Oxidation causes

Answer 28

iron oxidation and sulfahydryl groups of globin. Cannot bind oxygen, heinz bodies. Ion proetins and lipids also need to stay reduced.

Question 29

Bite and Blister cells

Answer 29

G6PD deficiency. Splenic macrophages take bite out of cell. MCV goes down, MCHC goes up. Can cause spherocytes.

Question 30

Detect G6PD deficiency

Answer 30

spectrometry flourescencePCR.

Question 31

Pyruvate Kinase

Answer 31

important in glycolytic pathwy. Deficeincy leads to Echinocytes, target cells, and HJ bodies.

Question 32

Hemolysis in pyruvate kinase often compensated by

Answer 32

2-3 BPG overproduction, decreases oxygen affinity.

Question 33

Micrangiopathy HA (MAHA)

Answer 33

thrombii in circulation. Fibrin deposits in vasculature damages RBC membrane

Question 34

TPP

Answer 34

microclots damage RBCs. Usually follow infection or pregnancy. Similar to HUS.

Question 35

DIC

Answer 35

often from bacterial blood infection, platelets consumed. Clots damage RBCs. Clotting time extended, abnormal bleeding, blood flow impeded to organs. Multiple organ faiilure. Abnormal coagulation tests differentiate it from TTP and HUS.

Question 36

babesia

Answer 36

normally mild anemia like malaria. transmitted by ticks. PCR and serological tests to dif from malaria.

Question 37

complement fixation

Answer 37

recruiting complement by antibodies.

Question 38

IGG

Answer 38

warm reactive

Question 39

IGM

Answer 39

cold reactive

Question 40

Contrast warm and cold acting hemolysis

Answer 40

Splenic macrophages have direct FCrIGG and can EV hemolyze. IGM can be IV through complement, or EV hrough c3b R on macrophages.

Question 41

AlloAb Hem Anemia examples

Answer 41

HDFN, blood transfusions.

Question 42

IGM complement activation

Answer 42

only one molecule of IGG required to activated classical pathway, therefore much more sensitive. 2 in close proximity required for IGG.

Question 43

IGM detection on RBC

Answer 43

antisera can detect IGM on RBC via agglutination in saline. Zeta potential and size of IGG prevents agglutination.

Question 44

Direct Anti human Globulin test (DAT or direct coombs)

Answer 44

Polyspecific AHG is added, agglutination means either the anti IGG or the anti complement antibodies have bridged zeta potential and caused agglutination. Follow with monospecific AHG. If only complement then likely IGM.

Question 45

IAT indirect anti human globulin or indirect coombs

Answer 45

Detects antibody in plasma. Less Ab required. Ab incubated with known antigenic makeup screening cells. Then add AHG positive if agglutination.

Question 46

pathophysiology WAIHA

Answer 46

most auto Ab against Rh antigens. common in CLL, neoplastic syndromes, autoimmune disorders. Most hemolysis EV.

Question 47

Clinical and Lab findings

Answer 47

Splenomegaly common. Positiv DAT, normocytic normochromic. increased LD, billirubin. Decreased haptoglobin. Increased osmotic fragility. Spherocytes, increased RDW compared to HS.

Question 48

Distinguish HS from WAIHA

Answer 48

DAT. Increased RDW.

Question 49

WAIHIA therpay

Answer 49

Alloantibodies make transfusion difficult. Focus is on preventing auto Ab formation: corticosteroids, splenectomy, IVIG \, plamapheresis.

Question 50

Cold Agglutination Syndrome

Answer 50

Mostly IGM against I antigens. Splenomegaly. Often episodic.

Question 51

Raynaud’s phenmomena

Answer 51

pain and cyanosis in extremeties due to cold agglutination of IGM.

Question 52

CAS Lab findings

Answer 52

RBC count decreased for hemoglobin, MCV is falsely elevated due to agglutination. Must warm all reagents and bood to 37C. When warm, normocytic normochromic, spherocytes, rolouex, nucleated RBCS. Dat poly and complement positive, IGG negative.

Question 53

Cold agglutinin test

Answer 53

Titer at which cells agglutinate. For benign cold agglutinins 1:50 or less. For CAS 1:1000.

Question 54

CAS therapy

Answer 54

corticosteroids, keep hands warm. Plasma exchange. Splenectomy not effective.

Question 55

Paroxsymal Cold hemoglobinuria

Answer 55

common in children. Generally appears weeks after certain infections, persists month or more. IGG antibody against p antigens. Biphasic, complement fixation. Hemoglobinuria, jaundice, splenomegaly.

Question 56

PCH clinical findings

Answer 56

weak or no DAT to complement. Can be positive for IAT if done at low temperature. HB levels drop following an attack and appear in blood and urine. Classic IV signs and neutropenic shift to left. No therapy, recover after infection.

Question 57

PCH specific test

Answer 57

incubate two tubes one at 37 one at 4C. Then incubate both at 37. Lysis in the 4C tube confirms PCH.

Question 58

Drug dependent and independent antibodies

Answer 58

describes whether the drug presence is required for the antibodies to react.

Question 59

Drug independent Ab mechanism

Answer 59

usually modifies antigens so no longer recognized as self. Drugs can also alter the membrane so that ab can bind non specifically. DAT positive, complement negative.

Question 60

Hemolytic transfusion reaction

Answer 60

Patients alloantibodies destroy donors RBCs. Immediate usually ABO and IGM can be IV. Delayed: previously sensitized but not detectable in lab. usually IGG usually EV.

Question 61

HDNF how it occurs

Answer 61

mother must be previously sensitized to antigen (previous pregnancy or transfusion). Baby must possess antigen. Mother must produce antibodies to this antigen that are capable of crossing placenta. Only IGG can cross placenta.

Question 62

ABO HDNF

Answer 62

An O mother has anti A and Anti B antibodies. A or B blood type in the fetus: IGG can cross placenta and case anemia even in first child,.

Question 63

billirunin in HDNF

Answer 63

mother conjugates and excretes in utero. After birth, remaining maternal antibodies still cause hemolysis. Infant is not efficient at metabolizing, and buildup of unconjugated can cause neurological defects.

Question 64

hdnf CLINICAL LAB FINDINGS

Answer 64

RETICULOCYTES CAN BE AS HIGH AS 60%. CORD BLOOD BILLIRUBIN IS ELEVATED.

Question 65

treatment for HDNF newborns

Answer 65

phototherapy: lowers billirubin in infants born with HDNF. Exchange transfusions: lowers billirubin, removes maternal antibodies, treats anemia.

Question 66

Rh Ig

Answer 66

injection of Rh ijmmunoglobulin prevents maternal immunization.

Question 67

Hemolytic Uremic Syndrome

Answer 67

hemolytic anemia with RBC fragmentation, thrombocytopenia, acute nepropathy renal failure. Seen in children. MOst common cause is from shiga toxin in ecoli. BUN and creatinine levels increased reflecting kidney damage.

Question 68

G6PD deficiency protects against

Answer 68

malaria. Could be more oxidants, early stage parasites more easily phagocytosed.

Question 69

G6PD sequence events pathophys

Answer 69

decreased NADH leads to oxidation of hb, and attachement of heinzbodies to band 3. Splenic macrophages pit and with progressive membrane loss sperocytes are formed. Spherocytes become trapped in the spleen.

Question 70

G6PD hemolysis usually caused by

Answer 70

exposure to oxidant drugs. Fava beans can also trigger. Primaquine (antimalarial).

Question 71

Hereditary non spherocytic anemia

Answer 71

is chronic. well compensated.

Question 72

blister cell

Answer 72

Hb oxidized and on one side of the cell. Indicative of oxidant related HA.

Question 73

Tests for G6PD deficiency

Answer 73

ascorbate cyanide test as screeening, quantitation at 340nm, molecular.

Question 74

PK clinical findings

Answer 74

autohemolysis increased at 48 hours, not corrected by glucose but corrected by ATP. Measure dissapearance of flourescence at 340 NM.