Which of the following is the most sensitive and specific test during antenatal check-up for a pregnant lady with family history of Thalassemia?

High performance liquid chromatography

P. smear and reticulocyte count

Which of the following statements about sickle cell anemia is false?

Ringed sideroblasts are associated with sickle cell anemia.

Sickle cells are present in sickle cell anemia.

Target cells are commonly seen in sickle cell anemia.

Howell Jolly bodies can be found in sickle cell anemia.

A 59-year-old male came with Hb 18.0 gm/dl on three occasions. The resident doctor wants to exclude Polycythemia Vera. Which of the following is the most relevant investigation :

Serum erythropoietin (EPO) levels

Which of the following statements about sickle cell disease is true?

Fetal hemoglobin inhibits sickling.

Sickling is completely reversible with oxygenation, making it clinically insignificant.

Sickling leads to a significant increase in overall MCHC levels in the blood.

Sickling occurs exclusively in the homozygous state and never in the heterozygous state.

Diagnosis of beta thalassemia is established by what?

Presence of target cells in blood smear

Which of the following is the recommended treatment for iron poisoning in a 4-year-old child?

Deferoxamine IV at a dose of 15 mg/kg/hour

Observation and supportive care

A 5-year-old boy presents with petechial bleeding and bruising on his torso and limbs. He has no other signs or symptoms and does not appear ill. His mother reports a gastrointestinal infection several weeks prior to the onset of petechiae and bruising. Complete blood count reveals thrombocytopenia (<20 x 10^9/L), with other parameters within the expected range for his age. Prothrombin time, partial thromboplastin time, and metabolic panels are all within the reference range. What is the expected outcome of this blood disorder?

Complete resolution is expected.

Survival rate is up to 70% depending on risk stratification.

Lifelong disease dependent on factor VIII substitution.

Lifelong disease dependent on factor IX substitution.

Hemoglobinopathies for NEET-PG: High-Yield Pediatrics Lessons

Hemoglobinopathies - Basics & Blood Bonds

Hemoglobinopathies: Genetic disorders affecting hemoglobin (Hb) structure or synthesis.
- Qualitative: Abnormal globin chain structure (e.g., Sickle Cell Disease).
- Quantitative: Reduced synthesis of normal globin chains (e.g., Thalassemia).
Normal Adult Hemoglobins:
- HbA ($α_2β_2$): >95%
- HbA2 ($α_2δ_2$): 1.5-3.5%
- HbF ($α_2γ_2$): <1-2% (higher in infants)
Inheritance: Most are Autosomal Recessive.

⭐ HbF is the predominant hemoglobin during fetal life, which gradually decreases after birth as HbA production increases.

Sickle Cell Syndromes - Crescent Calamity

Autosomal recessive; β-globin gene mutation (GAG→GTG; Glu→Val at codon 6) → HbS.
Pathophysiology: Deoxygenation → HbS polymerization → RBC sickling → microvascular occlusion, hemolysis.

Clinical Features:
- Vaso-occlusive crisis (VOC): Severe pain.
- Acute Chest Syndrome (ACS): Fever, cough, chest pain, hypoxia.
- Splenic sequestration (infants) → autosplenectomy (adults) → ↑ risk: encapsulated organisms (S. pneumo, H. flu, N. menin).
- Aplastic crisis (Parvovirus B19).
- Dactylitis (hand-foot syndrome; often 1st sign).
- Stroke, priapism, avascular necrosis.
Diagnosis:
- Newborn screening.
- Hb electrophoresis/HPLC: HbS predominant, ↑ HbF, no HbA (in HbSS).
- Peripheral smear: Sickled cells, Howell-Jolly bodies.
Management:
- Hydroxyurea: ↑ HbF, ↓ VOCs.
- Folic acid supplementation.
- Vaccinations (Pneumococcal, etc.).
- Pain control, hydration.
- Transfusions.
- Stem cell transplant (curative).

⭐ Howell-Jolly bodies on peripheral smear indicate splenic dysfunction/asplenia.

Thalassemias - Chain Chain Woes

Quantitative defect in globin chain synthesis (α or β). Results in microcytic hypochromic anemia.

Alpha (α) Thalassemia: Due to gene deletions on chromosome 16 (αα/αα).
- 1-2 deletions (-α/αα or -α/-α or --/αα): Silent carrier or α-thalassemia trait. Usually asymptomatic or mild microcytic anemia.
- 3 deletions (--/-α): HbH disease. Excess β chains form HbH (β4). Chronic hemolytic anemia, jaundice, splenomegaly. Golf ball inclusions (Heinz bodies) with supravital stain.
- 4 deletions (--/--): Hb Barts. Excess γ chains form Hb Barts (γ4). Severe intrauterine hypoxia, hydrops fetalis. Usually fatal.
- Diagnosis: Genetic testing. Hb electrophoresis shows HbH or Hb Barts.
Beta (β) Thalassemia: Due to point mutations in β-globin gene on chromosome 11.
- β-Thalassemia Minor (Trait): Heterozygous (β/β⁰ or β/β⁺). Mild asymptomatic anemia. ↑HbA2 (>3.5%), sometimes ↑HbF.
- β-Thalassemia Intermedia: Homozygous mild or compound heterozygous moderate mutations. Variable severity, may not require regular transfusions.
- β-Thalassemia Major (Cooley's Anemia): Homozygous (β⁰/β⁰) or severe compound heterozygous (β⁰/β⁺). Severe transfusion-dependent anemia by 4-6 months. Massive hepatosplenomegaly, bone marrow expansion (frontal bossing, chipmunk facies, "crew-cut" on X-ray), iron overload.
- Diagnosis: Hb electrophoresis (↓/absent HbA, ↑↑HbF, variable ↑HbA2).
Management (Moderate/Severe):
- Regular packed RBC transfusions (maintain Hb >9-10 g/dL).
- Iron chelation therapy (e.g., Deferoxamine, Deferasirox, Deferiprone) to prevent iron overload complications.
- Folic acid supplementation.
- Splenectomy (if hypersplenism).
- Allogeneic hematopoietic stem cell transplantation (HSCT) is curative.

Pathogenesis of Beta Thalassemia

⭐ Target cells (codocytes) are a characteristic, though not specific, finding on peripheral smear in thalassemias due to relative membrane redundancy.

Diagnostic Approach & Other Variants - Spotting the Suspects

Screening: CBC (↓Hb, abnormal MCV/MCH), Retic count, Peripheral Smear (RBC morphology: target cells, sickled cells, crystals).
Confirmation: HPLC (gold standard), Hb Electrophoresis. Genetic tests for unclear/atypical cases.
Newborn Screening (NBS): Crucial for early detection (SCA, β-Thal Major), allows timely intervention.

Hemoglobinopathies: Genotype, Phenotype, Sickling

Key Variants:
- HbC: Mild hemolysis, target cells, HbC crystals (rod-like).
- HbE: SE Asia; mild microcytic anemia; HbE co-migrates with HbA2.
- HbD-Punjab: Often asymptomatic; co-migrates with HbS (differentiate via solubility test - HbD is soluble).

⭐ On alkaline electrophoresis (pH 8.6), Hb migration: A > F > S/D/G > E/O/C (Anode to Cathode). 📌 Mnemonic: All Fine Sick Doctors Go East Or Centre.

High‑Yield Points - ⚡ Biggest Takeaways

Sickle Cell Anemia (SCA): HbS (β-globin Glu→Val), autosomal recessive. Features vaso-occlusive crises; hydroxyurea ↑HbF.

β-Thalassemia Major: Absent/reduced β-globin chains cause severe microcytic hypochromic anemia; transfusion-dependent with iron chelation.

α-Thalassemia: α-globin gene deletions lead to Hb Bart's (hydrops fetalis) or HbH disease.

Diagnosis: HPLC is gold standard. Newborn screening is key.

SCA Complications: Aplastic crisis (Parvovirus B19), risk of sepsis (prophylaxis needed).

HbE Trait/Disease: Common in NE India/SE Asia; often mild. HbE/β-thalassemia is severe_._

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