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Case Studies In Hematology And Coagulation Pdf To Doctors
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- Case Studies In Hematology And Coagulation Pdf File University of Delaware - Hematology (Case Studies). Intravascular Coagulation CURRENT STUDIES IN HEMATOLOGY AND BLOOD.
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CASE 1: A 30-old-male of Afro-American descent was treated at the Howard University hospital complaining of extreme tiredness after exercise, occasional dizziness, and shortness of breath. On one occasion he actually fainted on the job. 1. What valuable information can be extracted from this? | 1. The clinical symptoms of extreme tiredness often suggest the presence of an anemia , but there is not enough information to make an assumption of the specific anemia present. |
CASE 1 cont. Initial Laboratory Profile: WBC 10.0X10 9/L (4.8-19)mm3 MCV 79 fl.( 78-96) RBC 5. 0X10 12/L (4.2-5.4) MCH 24 pg (27-31) Hb 13. 9gm/ dL (12-16) MCHC 34 %(32-36) Hct 40 % (37-47) Plt 150X10 9/L (150-450) N 2. What does the evaluation of these routine lab results show? | 2. The hemoglobin(Hb), hematocrit (Hct), and the Red Cell count (RBC) are all below the acceptable reference ranges for the age and sex of the patient, but the hemoglobin is commonly used as the indicator of anemia. A reduced hemoglobin value always suggest Anemia. |
CASE 1 cont: Additional Lab Results: Peripheral smear morphology shows: microcytic, hypochromic erythrocytes, poikilocytosis, occasional target and banana shaped cells. The white blood cells(WBC’s) had fairly normal morphology, and the platelet distribution was slightly increased. 3. Is this smear abnormal and which are the specific abnormalities? 4. What additional testing should be done to make proper identification of the anemia? | 3. The erythrocytes(hypochromic/ microcytic, targets . The banana shaped cells are commonly found in anemia caused by the deficiency of dietary iron. Iron Deficiency Anemia-IDA 4. The following tests are commonly used to differentiate between the microcytic, hypochromic anemia: Serum Iron Serum Ferritin Total Iron Binding Ferritin % Saturation Capacity (TIBC) Bone Marrow Iron Stores |
CASE 1 cont: Patient Test Results Serum Iron Decreased TIBC Increased % Saturation Decreased Iron Stores Decreased 5. What is the correct specific anemia presented here? | |
Iron deficiency anemia is one of the most frequently encounters anemia. This anemia may result from nutritional deficiency, abnormal absorption of iron , increased demand or excessive bone marrow loss. Among all of these nutritional deficiency appears to be the most frequent cause of Iron Deficiency Anemia (IDA). | |
CASE 2: A 26-year-old American female was treated for excessive joint pains, swollen ankles and fever over a period of years with analgesics and other pain therapy. Her physical examination revealed signs of inflammation, splenomegaly, and some bacterial infection. Initial Laboratory Profile: WBC 15.5x 10 9/L (4.8-10.8)N MCV 91fl (80-96)N RBC 3.5 X1012/L (4.2- 5.5) N MCH 29. 8 pg ( 27-32)N Hb 10. 5gm/dl ( 12-16) N MCHC 32. 4% ( 32-36)N Hct 31.6 % (37-47) N Sed Rate 30/ mm/hr (0-20)N 1. What category of anemia is suggested here? | 1. The RBC parameters (Hct, Hb) indicate the presence of anemia, and the MCV suggests a normocytic, normochromic anemia . The MCV is mostly a measure of erythrocyte size. This situation occurs in a specific group of disorders caused by poor utilization of iron. |
CASE 2 cont: Additional Lab Results: Peripheral smear shows normocytic/normochromic, sl. poikilocytosis, and occasional target cells. Some erythrocytes show inclusions in clusters. •Differential: Seg Neut. 80% Lymphs 10% •Monos 6% Eos 3% •Baso 1% 2. What are the inclusions in the erythrocytes? | 2. These are iron deposits seen usually in bunches or clusters and visible on Wright stain also. |
CASE 2 cont: 3. What would you expect to find on a bone marrow iron stain? 4. What is serum iron and TIBC values for this group of anemia? | 3. The bone marrow (iron stain) should show increased iron storage in 30-50% of the normoblasts (multiple dark inclusions) sideroblasts. 4. The Serum Iron and TIBC values can be normal or increased. |
CASE 2 cont: 5. This anemia is most likely called what? | |
Anemia of chronic disorders is produced by blockage of iron release from the storage areas (macrophage) and availability to be used in the synthesis of heme in the hemoglobin molecule. Current concept suggest a deficiency of an enzyme essential the iron transfer process. This anemia is usually associated with chronic conditions, eg. rheumatoid arthritis, chronic liver disease, rheumatic fever, lupus erythematous, and other related to the inflammatory response. | |
CASE 3: A 24-year-old female on her first visit to her physician complained of weakness and being continually tired. She also stated that she had lost an appreciable amount of weight . There was no family history of anemia, but evidence was produced that she had abused the use of alcohol by consuming several quarts weekly, and neglected having a normal diet for several years. Initial Laboratory Profile RBC 3.0 X 10 12/L ( 4.2-4.5) N MCV 92 fl (78-96) N WBC 9.7 X 10 9/ L ( 4.8-10.8) N MCH 30.9 (27-32) N Hct 26.9 % ( 37-47) N MCHC 33.5 ( 32-36) N Hb 9.0 gm/dL ( 12-14) N RDW 15.0 (11.5-14.5) N 1. What is the category of this anemia? | 1. The MCV suggests a normocytic/ normochromic anemia, which includes the hemolytic anemias. |
CASE 3 cont: Additional Lab Results: Differential Seg Neutrophil 71% Lymphs 5% Bands 5% Monos 11% Lymphs 5 % Eos 3% Peripheral blood morphology shows hypochromic/ microcytic and normochromic/ normocytic RBC with basophilic stippling in some erythrocytes. 2. Explain the discrepancy suggested here? | 2. The hematocrit and hemoglobin suggest iron deficiency anemia, the MCV suggests a hemolytic anemia, but the dimorphism found in the erythrocytes and the basophilic stippling are indicative of a Iron deficiency Anemia associated with increased iron storage. |
CASE 3 cont: Additional Lab Results: This smear represents the bone marrow iron content: 3. Which morphological features are significant in the diagnosis of this anemia? | 3. The presence of increased iron stores, sideroblasts and ringed sideroblasts. |
CASE 3 cont: 4. What are the expected values for the following chemistry tests?. Serum Iron? TIBC? Serum transferrin? Serum B12? | •Serum Iron Increased •TIBC Normal/decreased •Serum Transferrin Increased •Serum Folate Normal |
CASE 3 cont: 5. What is the etiology of this anemia? | 5. This anemia is caused by poor utilization of iron associated with defective heme synthesis. |
CASE 3 cont: 6. What is the diagnosis of this anemia? | |
Sideroblastic anemia is generally produced by the deficiency of the enzyme delta-ALA synthetase enzyme which causes accumulation of nonferritin iron around the nucleus of the immature erythroblast ( metarubricyte stage) cell. This forms the ringed sideroblast which a diagnostic feature of this anemia | |
CASE 4: 23 year old male. Over the past week noted increasing fatigue, sore throat, earaches, headaches, and episodic fever and chills. Unable to run his customary 25 miles per week. Physical Exam: Erythematous throat and tonsils. Swollen cervical lymph nodes. CBC (with microscopic differential) RBC 5.25 x 1012/L HGB 15.4 g/dL HCT 46.1 % MCV 87.9 fL MCH 29.3 pg MCHC 33.4 g/dL RDW 12.2 WBC 12.9 x 109/L N 24 % L (shown) 73 M 0 E 3 B 0 PLT 333 x 109/L Morphologic Alterations Results of the blood smear exam were: RBC morphology: Normocytic, normochromic WBC morphology: Most of the lymphocytes are reactive. They are large cells with a smudged chromatin pattern and abundant cytoplasm with radial and/or peripheral basophilia. Some of the larger cells have finer chromatin and nucleoli. PLT morphology: Within normal limits 1. What further laboratory studies, if any, are indicated? | Further Laboratory Studies Heterophil antibody screen: positive |
CASE 4 cont: 2. What is the most likely diagnosis? | |
CASE 5: 70 year old female. Symptoms of dyspnea on exertion, easy fatigability, and lassitude for past 2 to 3 months. Denied hemoptysis, GI, or vaginal bleeding. Claimed diet was good, but appetite varied. Physical Exam: Other than pallor, no significant physical findings were noted. Occult blood was negative. CBC (with microscopic differential) RBC 3.71 x 1012/L HGB 5.9 g/dL HCT 20.9 % MCV 56.2 fL MCH 15.9 pg MCHC 28.3 g/dL RDW 20.2 WBC 5.9 x 109/L N 82 % L 13 M 1 E 4 B 0 PLT 383 x 109/L Results of the blood smear exam were: RBC morphology: 2+ hypochromasia 3+ microcytosis 2+ anisocytosis 2+ elliptocytes and target cells occ teardrops and fragments WBC morphology: Within normal limits (one lymphocyte shown here) PLT morphology: Within normal limits 1. What further laboratory studies, if any, are indicated? | Further Laboratory Studies Iron studies were performed, and results were: serum ferritin <10 ng/mL (RI 12-86) serum iron 24 µg/dL (RI 65-175) TIBC 729 µg/dL (RI 250-410) saturation 3 % (RI 20-55) |
CASE 5 cont: 2. What is the most likely diagnosis? | |
CASE 6: 51 year old male. Seen by local physician for routine preoperative exam prior to dental surgery. Found to have low hemoglobin and a large left upper quadrant mass. Physical Exam Marked splenomegaly (subsequently confirmed by CT scan) extending from the left costal margin to just above the iliac crest. No other organomegaly. CBC (with microscopic differential) RBC 3.36 x 1012/L HGB 10.9 g/dL HCT 31.2 % MCV 92.8 fL MCH 32.4 pg MCHC 34.9 g/dL WBC 9.3 x 109/L N 14 % L 15 abnormal cells 71 (shown) PLT 59 x 109/L Morphologic Alterations Results of the blood smear exam were: RBC morphology: Normocytic, normochromic WBC morphology: The abnormal cells have round or indented nuclei with a fairly coarse chromatin pattern. They have variable amounts of grainy blue-gray cytoplasm with irregular ragged borders and numerous projections. PLT morphology: Within normal limits 1. What further laboratory studies, if any, are indicated? | Further Laboratory Studies Bone marrow biopsy: Aspirate: Marrow was difficult to obtain. A small amount of fluid was aspirated, and the differential showed 78.1% abnormal cells similar to those in the blood. Sections: Hypocellular with a diffuse loosely structured infiltrate of mononuclear cells. Increased areas of fibrosis. Cytochemistry: Tartrate resistant acid phosphatase (TRAP) stain of abnormal cells: positive Immunophenotyping: Not done. |
CASE 6 cont: 2. What is the most likely diagnosis? | |
CASE 7: 25 year old male. Recurrent upper respiratory infections with fever, nausea, and submandibular swelling for several months prior to admission. Noted that cuts on his hands did not heal well. Physical Exam Submandibular adenopathy. No other organomegaly. CBC (with microscopic differential) RBC 2.70 x 1012/L HGB 9.9 g/dL HCT 28.7 % MCV 106.3 fL MCH 36.9 pg MCHC 34.8 g/dL WBC 7.9 x 109/L N 4 % L 16 M 1 E 0 B 0 abnormal cells 79 (shown) PLT 50 x 109/L Morphologic Alterations Results of the blood smear exam were: RBC morphology: Normochromic 1+ polychromasia 1+ macrocytosis WBC morphology: The abnormal cells are medium-sized blasts. The nuclei are often irregular in shape, and some have invaginations or deep clefts. Most have a fine chromatin pattern and one or more prominent nucleoli. The cytoplasm is basophilic, and thin Auer rods are seen. PLT morphology: Within normal limits 1. What further laboratory studies, if any, are indicated? | Further Laboratory Studies Bone marrow biopsy: Aspirate: The differential showed 93.6% blasts similar to those in the blood. Dyserythropoiesis was not seen in the red cell precursors. Sections: Markedly hypercellular. Cytochemistry: Myeloperoxidase: positive Sudan black B: positive Non-specific esterase: negative Immunophenotyping: Not done. Cytogenetics: Not done. |
CASE 6 cont: 2. What is the most likely diagnosis? | |
CASE 7: 34 year old female. Two day history of ecchymoses, petechiae, and hematuria. She had noted headaches, nausea, and increasing dysphoria over the past week. Physical Exam Mild scleral icterus. Scattered ecchymoses and petechiae. Appeared anxious and agitated. CBC (with microscopic differential) RBC 2.38 x 1012/L HGB 6.6 g/dL HCT 18.4 % MCV 77.5 fL MCH 27.7 pg MCHC 35.8 g/dL RDW 23.8 WBC 16.9 x 109/L N 78 % L 14 M 8 E 0 B 0 PLT 14 x 109/L Morphologic Alterations Results of the blood smear exam were: RBC morphology: normochromic 2+ polychromasia 3+ anisocytosis 3+ fragments 2+ spherocytes WBC morphology: Within normal limits (one lymphocyte shown here) PLT morphology: Within normal limits 1. What further laboratory studies, if any, are indicated? | Further Laboratory Studies Coagulation: PT 12.2 sec (RI 11.0-13.5) PTT 29.2 sec (RI 23-34) TT 22.9 sec (RI 13-18) Fibrinogen 0.43 g/dL (RI 0.17-0.37) FDP 80 µg/mL (RI 0-10) D dimer 2320 ng/mL (RI 0-420) Chemistry: BUN 41 mg/dL (RI 9-23) Creatinine 0.8 mg/dL (RI 0.3-1.0) Bilirubin Conj. 0.5 mg/dL (RI 0.0-0.3) Total 2.8 mg/dL (RI 0.0-1.3) Haptoglobin <5 mg/dL (RI 50-150) Urinalysis: Large amount of blood present Protein positive (100 mg/dL) |
CASE 7 cont: What is the most likely diagnosis? | |
CASE 8: 6 year old male. Well until 3 weeks prior to admission. Developed upper respiratory symptoms, persistent headaches, bone pain, and easy bruising. Physical Exam Adenopathy: submandibular, axillary, and cervical. Hepatosplenomegaly. Petechiae and bruises on trunk and limbs. CBC (with microscopic differential) RBC 3.34 x 1012/L HGB 9.0 g/dL HCT 27.2 % MCV 82.0 fL MCH 27.2 pg MCHC 33.4 g/dL RDW 13.9 WBC 92.4 x 109/L N 4 % L 8 M 1 E 0 B 1 abnormal cells 86 (shown) PLT 18 x 109/L Morphologic Alterations Results of the blood smear exam were: RBC morphology: Normocytic, normochromic WBC morphology: The abnormal cells are small to medium-sized blasts. They have a relatively fine chromatin pattern, one or more indistinct nucleoli, and scanty basophilic cytoplasm. Occasional cells show nuclear clefts. PLT morphology: Within normal limits 1. What further laboratory studies, if any, are indicated? | Further Laboratory Studies Bone marrow biopsy: Aspirate: The differential showed 89.1% blasts similar to those in the blood. Sections: Markedly hypercellular. Cytochemistry: Myeloperoxidase negative Sudan black B negative PAS positive (intensely staining clumps in cytoplasm) Immunophenotyping: TdT positive B precursor markers positive T precursor markers negative Myelomonocytic markers negative Cytogenetics: 46, XY. No numerical or structural abnormalities found. Cerebrospinal fluid analysis: Clear, colorless CSF Glucose 62 mg/dL (RI 50-80) Protein 25 mg/dL (RI 20-60) RBC 85 x 106/L WBC 2 x 106/L Gram stain negative Culture negative |
CASE 8 cont: 2. What is the most likely diagnosis? | B precursor ALL (acute lymphoblastic leukemia), FAB L1 |
CASE 9: 72 year old male. Symptoms of itching, rash, skin discomfort, and malaise increasing over several months. Physical Exam Generalized erythroderma. Skin appeared leathery, cracked, and peeling. Bilateral epitrochlear and inguinal adenopathy. CBC (with microscopic differential) RBC 4.80 x 1012/L HGB 14.2 g/dL HCT 42.4 % MCV 88.3 fL MCH 29.7 pg MCHC 33.6 g/dL WBC 10.8 x 109/L N 35 % L 13 M 8 E 4 B 0 abnormal cells 40 (shown) PLT 158 x 109/L Morphologic Alterations Results of the blood smear exam were: RBC morphology: normocytic, normochromic WBC morphology: The abnormal cells have convoluted cerebriform nuclei. The cytoplasm is basophilic, and occasionally contains small vacuoles. Both small and large cell types are seen. PLT morphology: Within normal limits 1. What further laboratory studies, if any, are indicated? | Further Laboratory Studies Cytochemistry: PAS: many of the abnormal cells show punctate PAS positivity around the nuclei. Immunophenotyping: Elevated CD3 and CD4 positivity consistent with helper T cell phenotype. |
CASE 9 cont: 2. What is the most likely diagnosis? | Sezary syndrome (Confirmed by skin and lymph node biopsy.) |
CASE 10: 30 year old male. Almost 4 years prior to admission, he was diagnosed with a malignant brain tumor. It was removed surgically and he received chemotherapy. After about three years, the tumor recurred. He was treated with radiation, and chemotherapy was resumed. During a clinic visit he was found to have a fever of 101°F, WBC of 1.0 x 109/L, and ANC (absolute neutrophil count) of 0 (zero). He was admitted to the hospital and started on IV antobiotics and daily G-CSF injections. This CBC is from the sixth day of growth factor therapy. | CASE 9: CBC & Diff CBC (with microscopic differential) RBC 3.17 x 1012/L HGB 10.4 g/dL HCT 30.0 % MCV 94.7 fL MCH 32.9 pg MCHC 34.7 g/dL RDW 11.9 WBC 23.9 x 109/L N seg 52 % N band 13 N meta 8 N myelo 8 N pro 4 Myeloblast 1 L 8 M 3 E 3 PLT 103 x 109/L |
CASE 9 cont: Morphologic Alterations Results of the blood smear exam were: RBC morphology: normocytic, normochromic 1+ polychromasia WBC morphology: Both mature and immature stages of neutrophils have intense azurophilic granulation. Some bands and segmented forms contain Dohle bodies. Some have bubbly, vacuolated cytoplasm. Neutrophil nuclei are deeply stained, and nuclear projections are seen. Some promyelocytes are extremely large. PLT morphology: Within normal limits 1. What further laboratory studies, if any, are indicated? | |
CASE 9 cont: 2. What is the most likely diagnosis? | Answer: Shift to the left and reactive changes in neutrophils consistent with response to G-CSF or GM-CSF therapy. |
CASE 10: 33 year old female. Immigrated to the United States from Laos four years prior to admission. History obtained through an interpreter. Multiple transfusions and splenectomy two years prior to admission. Reason and/or diagnosis unclear to patient. Presented with flu-like symptoms of fever, malaise, epigastric discomfort and nonproductive cough. | CASE 10: CBC & Diff CBC (with microscopic differential) RBC 4.15 x 1012/L HGB 8.1 g/dL HCT 28.6 % MCV 68.9 fL MCH 19.5 pg MCHC 28.2 g/dL RDW 22.3 WBC (corrected) 8.0 x 109/L N 51 % L 36 M 7 E 4 B 2 NRBC/100 WBC 83 PLT 540 x 109/L |
CASE 10 cont: Morphologic Alterations Results of the blood smear exam were: RBC morphology: 3+ hypochromasia 1+ polychromasia 2+ anisocytosis 3+ target cells occ spherocytes and fragments Howell Jolly bodies present WBC morphology: Within normal limits PLT morphology: Within normal limits 1. What further laboratory studies, if any, are indicated? | Answer: Further Laboratory Studies Hemoglobin electrophoresis: Hemoglobin E 80 % Hemoglobin F 5 % Other hemoglobins* 15 % *Identified as hemoglobin A2, hemoglobin Barts and a hemoglobin H mutant. Iron studies: Serum ferritin 3234 ng/mL (RI 12-86) Serum iron 140 µg/dL (RI 65-175) TIBC 152 µg/dL (RI 250-410) Saturation 92 % (RI 20-55) |
CASE 10 cont: 2. What is the most likely diagnosis? | Answer: Homozygous hemoglobin E disease and alpha thalassemia |
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Case Studies In Hematology And Coagulation Pdf To Docs
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Case Studies In Hematology And Coagulation Pdf To Docx
- All of the following conditions cause an increased (prolonged) thrombin time except
Hypofibrinogenemia
Increased fibrin-degradation products
Heparin therapy
Decreased prothrombin
- The end product of the interaction between platelets and plasma factors, other than fibrinogen, is
Prothrombin
Thrombin
Fibrin
Factor II
- Heparin inhibits the clotting of blood by neutralizing the effect of
Thrombin
Calcium ions
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Platelets
Factor VIII
Factor X
- Defibrinated plasma, in order to clot when mixed with tissue thromboplastin and calcium, requires an outside source of?
Heparin
Calcium chloride
Barium sulfate
Fibrinogen Print shop press writer download online.
- Serum differs from plasma by the loss of
Factor II
Factor VII
Thromboplastin
Fibrinogen
- The substance necessary to convert fibrinogen to fibrin is
Platelets
Thromboplastin
Thrombin
Prothrombin
- A.
- B.
- C.
- D.
- 8.
- A.
- B.
- C.
- D.
- 9.The substance active in splitting fibrin, fibrinogen and fragments is
Plasminogen
Plasmin
Peptides
Thrombin
- The intrinsic pathway of the coagulation system begins with the activation of
Factor II
Factor I
Factor XII
Factor V
Factor VIII
- A.
- B.
- C.
- D.
- E.
- 12.
- A.
- B.
- C.
- D.
- E.
- 13.The final stage of the coagulation pathway involves the conversion of
Factor I to Ia
Factor II to IIa
Factor V to Va
Factor I to fibrin clot
Factor IX to IXa
- Prothrombin is
A protein formed by the liver in the presence of Vitamin K
An enzyme that converts fibrinogen into fibrin threads
The end product of the reaction between fibrinogen and thrombin
A protein released by platelets during coagulation
- Aspirin ingestion has the following hemostatic effect in a normal person
Prolongs the bleeding time
Prolongs the clotting time
Inhibits factor VIII
Creates a circulating anticoagulant effect
No effect
- Fibrin monomers polymerize to form
Fibrinopeptide A
Fibrinopeptide B
Fibrin polymer
Stable fibrin
- Plasminogen is activated by
Proteolytic enzymes
Plasmin
Fragment X
Fragment Y
- Activated Protein C acts by
Precipitating calcium
Binding calcium
Activating plasmin
Inactivating VIIIa
- Prothrombin is converted to thrombin by
A complex of activated factors IX and VII and calcium ions
Calcium ions only
A complex of phospholipids, factor VII, and calcium ions
A complex of activated factors X and V, platelet factor 3 and calcium
None of the above
- A.
- B.
- C.
- D.
- 21.
- A.
- B.
- C.
- D.
- 22.
- A.
- B.
- C.
- D.
- 23.Which of the following is a source of error that can affect most coagulation procedures?
Improper specimen storage
Improperly reconstituting and storing test reagents
Improper temperature of reaction
Improper timing of a test
All of the above
- In specimen collection, leaving a tourniquet on too long immediately prior to doing a venipuncture can result in:
Hemoconcentration
In vivo clotting
The vein collapsing
A hematoma
- The proper proportion (in parts) of blood to anticoagulant in the PTT and Protime is
2:1
3:1
5:1
9:1
- Of the following tests, which one should be drawn last:
EDTA - CBC
Heparin - pH
Citrate - PTT
Clot tube - CK
- If a protime vacutainer was not filled with blood, the results would be
Unaffected
Normal
Shortened
Prolonge
- The reagent used for PTT:
Phospholipid
Tissue thromboplastin
Heparin
Thrombin
- The test that detects the presence of non-specific IgG inhibitaors of phospholipid
Thrombin time
Protime
PTT
Lupus anticoagulants
- The bleeding time test measures:
The ability of platelets to stick together
Platelet adhesion and aggregation on locally injured vascular subendothelium
The quantity and quality of platelets
Antibodies against platelets
Both a and b
- A lower temperature than optimum, when performing a prothrombin time, will result in
Shorter time
Longer time
No effect
- If a protime or PTT cannot be run immediately, it is best to
Wait to centrifuge the whole blood
Refrigerate the whole blood
Centrifuge the whole blood, decant and freeze plasma
Centrifuge the whole blood, then refrigerate
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- The normal value for the protime is
8-10 seconds
11-14 seconds
20-30 seconds
Under 45 seconds
- The partial thromboplastin reagent used in the PTT test is a substitute for
Platelet factor
Calcium chloride
Thrombin
Fibrin
- The PTT is different from the prothrombin time in that it measures the
Extrinsic clotting system
Intrinsic clotting system
Factor VII and platelets
Fibrinogen
- Automated mechanical end-point detection systems rely on the principle of
Clot elasticity
Fibrin adhesion
Conduction or impedance of an electrical current by fibrin
Changes in optical density
None of the above
- When performing a bleeding time, the usual puncture site is the
Finger
Forearm
Heel
Ear lobe
Big toe
- A source of error when using a photo-optical endpoint detection method in coagulation studies can be
Lipemia
Hemolysis
Icterous
A and b
All of the above
- The PTT test is a good measure of quantity and function of which of the following factors except
VIII and IX
VII and XIII
I and II
V and X
- The thrombin test measures
Thrombin
Prothrombin
Fibrinogen
Factor XIII
- The adhesiveness of platelets is measured, in vitro, by their ability to adhere to
Ristocetin
Damaged cells
Glass beads
Polyvinyl tubing
- Hyperfibrinogenemia may develop in
Hemophiliacs
Vitamin K deficiencies
Late stages of pregnancy
Sickle cell anemia
- The following laboratory results were obtained for a patient with an inherited autosomal dominant trait:Platelet adhesiveness - abnormalPT - normalPTT - normalBleeding time - prolongedThese findings are most consistent with
Hemolytic disease of the newborn
Factor X deficiency
Factor XI deficiency
VonWillebrand's disease
- Thrombocytopenia may be associated with the prolongation of all of the following except:
Bleeding time
Ristocetin assay
Platelet aggregometry
PTT
- A defect in factor IX causes which of the following diseases
Hemophilia A
Hemophilia B
Afibrinogenemia
Hypothrombinemia
- Coumadin drugs produce anticoagulation by interfering with the reaction of
Thrombin and fibrinogen
AHG, PTA & XIII
XI & XII
II, VII, IX & X
- The hereditary gene for hemophilia is carried on the
X chromosome of the female
X chromosome of the male
Y chromosome of the male
X & Y chromosomes of the male
- Hemophilia A is a condition which results in a deficiency of factor
I
II
VIII
IX
- A factor deficiency noted by prolongation of the protime and PTT is
VII & IX
VIII & XI
VIII & XII
V & VII
- An elevated FDP (fibrin degradation products) suggest:
Lupus
Cortisone therapy
PA
DIC
- An 'labile' factor is Factor:
I
II
V
VII
- Thrombocytopenia can be caused by
Decreased production
Increased production
Increased utilization
Disorders of distribution
All of the above
- Which of the following tests is (are) usually abnormal in classical Von Willebrand's disease?
Bleeding time
Ristocetin assay
Platelet adhesiveness
Factor VIII assay
All of the above
- LAboratory results in acute disseminated intravascular coagulation reflect abnormalities in which of the following coagulation components.
Platelets
Fibrinolysis
https://luckyharmony.netlify.app/edition-introduction-sixth-sociology-major.html. Thrombin formation
Fibrin formation
All
- Prolonged thrombin times are noted in
Factor II deficiencies
Presence of fibrin-split products
Proteolytic enzyme presence
Patients with hemophilia
- A.
- B.
- C.
- D.
- E.
- 57.Christmas disease is caused by a deficiency in Factor:
VIII
IX
X
XI
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- DIC conditions often times are treated with
Fibrinogen
Heparin
Dicumerol
ACTH