Allergic Testing Methods Indian Medical PG Practice Questions and MCQs
Practice Indian Medical PG questions for Allergic Testing Methods. These multiple choice questions (MCQs) cover important concepts and help you prepare for your exams.
Allergic Testing Methods Indian Medical PG Question 1: Which test is most useful for initial evaluation of suspected pulmonary sarcoidosis?
- A. Bronchoalveolar lavage (BAL) (Correct Answer)
- B. Cutaneous skin biopsy
- C. Serum angiotensin-converting enzyme (ACE) levels
- D. Chest radiograph (X-ray)
Allergic Testing Methods Explanation: ***Bronchoalveolar lavage (BAL)***
- While other tests provide supportive evidence, **BAL with differential cell count** is crucial for distinguishing sarcoidosis from other interstitial lung diseases by detecting a high CD4/CD8 ratio.
- It allows for direct sampling of inflammatory cells and helps to exclude infections, making it a critical step in confirming the diagnosis, often combined with **transbronchial biopsy**, which can be facilitated through endobronchial ultrasound (EBUS) mapping [2].
*Cutaneous skin biopsy*
- **Skin biopsies** are useful if there are visible skin lesions (seen in ~5% of patients), which can show non-caseating granulomas supporting sarcoidosis [1].
- However, sarcoidosis often presents without skin involvement, and a skin biopsy would not be the **initial diagnostic test** for suspected pulmonary disease.
*Serum angiotensin-converting enzyme (ACE) levels*
- Elevated **serum ACE levels** are found in some sarcoidosis patients and can support the diagnosis or monitor disease activity.
- However, ACE levels are **not specific** to sarcoidosis and can be normal even in active disease, making it a less reliable primary diagnostic tool.
*Chest radiograph (X-ray)*
- A **chest X-ray** is often the first imaging study performed and can show findings like **bilateral hilar lymphadenopathy** or interstitial infiltrates, which are highly suggestive of sarcoidosis [1].
- While important for initial suspicion, a chest X-ray does not provide a definitive diagnosis and requires further investigation to confirm sarcoidosis and rule out other causes.
Allergic Testing Methods Indian Medical PG Question 2: Which type of dermatitis is evaluated through patch testing?
- A. Atopic dermatitis
- B. Irritant contact dermatitis
- C. Discoid eczema
- D. Contact dermatitis due to allergens (Correct Answer)
Allergic Testing Methods Explanation: ***Contact dermatitis due to allergens***
- **Patch testing** is specifically used to identify specific **allergens** that trigger an **allergic contact dermatitis** reaction.
- It involves applying suspected allergens to the skin and observing for a localized inflammatory response, indicating delayed type IV hypersensitivity.
*Atopic dermatitis*
- This is a chronic inflammatory skin condition characterized by **eczematous lesions** and severe **pruritus**, often linked to a genetic predisposition and immune dysfunction.
- While allergy testing (e.g., prick tests, blood tests for IgE) might be used to identify triggers, **patch testing** is not the primary diagnostic tool for atopic dermatitis itself.
*Irritant contact dermatitis*
- This type of dermatitis is caused by direct **damage to the skin barrier** from exposure to caustic substances or irritants, not an immune-mediated allergic reaction.
- Diagnosis is usually based on clinical history of exposure and symptom presentation, and **patch testing** is typically negative in these cases.
*Discoid eczema*
- Also known as **nummular dermatitis**, this condition presents with distinctive **coin-shaped lesions** and is often associated with dry skin or skin trauma.
- Its etiology is generally unknown and not attributable to specific allergens detectable by **patch testing**.
Allergic Testing Methods Indian Medical PG Question 3: Which of the following is the platinum-based chemotherapeutic agent used as first-line treatment for ovarian carcinoma?
- A. Cyclophosphamide
- B. Methotrexate
- C. Cisplatin (Correct Answer)
- D. Dacarbazine
Allergic Testing Methods Explanation: ***Cisplatin***
- **Cisplatin** is a platinum-based chemotherapy drug that forms **DNA cross-links**, inhibiting DNA synthesis and leading to the death of rapidly dividing cells, making it highly effective against **ovarian carcinoma**.
- It is a cornerstone of chemotherapy regimens for ovarian cancer, often used in combination with other agents such as paclitaxel.
*Methotrexate*
- **Methotrexate** is an **antimetabolite** that inhibits dihydrofolate reductase, thereby interfering with DNA synthesis.
- While it is used in various cancers like leukemia, lymphoma, and some solid tumors (e.g., breast cancer, gestational trophoblastic disease), it is **not a primary recommended drug for ovarian carcinoma**.
*Cyclophosphamide*
- **Cyclophosphamide** is an **alkylating agent** that causes DNA damage, leading to cell death.
- It is used in many cancers, including lymphoma, breast cancer, and some leukemias, but it is **not a first-line or primary agent for ovarian carcinoma** in contemporary treatment guidelines.
*Dacarbazine*
- **Dacarbazine** is an **alkylating agent** primarily used in the treatment of **malignant melanoma** and Hodgkin lymphoma.
- It is **not indicated for the treatment of ovarian carcinoma**.
Allergic Testing Methods Indian Medical PG Question 4: AMPLE history involved all except?
- A. Last meal
- B. Pregnancy
- C. Personal history (Correct Answer)
- D. Allergy
Allergic Testing Methods Explanation: ***Personal history***
- The "P" in **AMPLE** stands for **Past medical history**, not Personal history. Personal history (social history) is a broader category that includes elements like smoking, alcohol use, and occupation, which are not specifically covered by the AMIPLE acronym.
- While personal history is important for overall patient assessment, it is not a direct component of the focused **AMPLE** mnemonic used in emergency and critical care settings.
*Last meal*
- The "L" in **AMPLE** stands for **Last meal** (or Last oral intake).
- This information is crucial for assessing aspiration risk, especially before procedures or surgery, and understanding metabolic status.
*Pregnancy*
- The "P" in **AMPLE** stands for **Past medical history or Pregnancy**.
- For female patients of reproductive age, identifying pregnancy status is critical for medication administration, imaging decisions, and overall management.
*Allergy*
- The "A" in **AMPLE** stands for **Allergies**.
- Knowing a patient's allergies is fundamental to prevent adverse reactions to medications, foods, and environmental factors during treatment.
Allergic Testing Methods Indian Medical PG Question 5: Myasthenia gravis is which type of hypersensitivity?
- A. Type IV
- B. Type III
- C. Type II (Correct Answer)
- D. Type I
Allergic Testing Methods Explanation: ***Type II***
- Myasthenia gravis is an **autoimmune disease** where antibodies are directed against the **nicotinic acetylcholine receptors** at the neuromuscular junction [1], [2].
- This **antibody-mediated cytotoxicity** and receptor blockade leading to muscle weakness is characteristic of a **Type II hypersensitivity reaction** [1].
*Type IV*
- Type IV hypersensitivity is a **delayed-type hypersensitivity**, mediated by **T-cells** rather than antibodies.
- Examples include **contact dermatitis** and the tuberculin skin test, which do not involve autoantibodies against receptors.
*Type III*
- Type III hypersensitivity involves the formation of **immune complexes** (antigen-antibody complexes) that deposit in tissues and cause inflammation.
- Conditions like **serum sickness** and **lupus nephritis** are examples, differing from receptor-specific antibody attacks.
*Type I*
- Type I hypersensitivity is an **immediate hypersensitivity** mediated by **IgE antibodies** binding to mast cells and basophils, leading to histamine release.
- This type is responsible for **allergic reactions** like anaphylaxis and asthma, which is distinct from autoimmune receptor blockade.
**References:**
[1] Kumar V, Abbas AK, et al.. Robbins and Cotran Pathologic Basis of Disease. 9th ed. Diseases of the Immune System, pp. 213-214.
[2] Kumar V, Abbas AK, et al.. Robbins and Cotran Pathologic Basis of Disease. 9th ed. Peripheral Nerves and Skeletal Muscles, pp. 1237-1238.
Allergic Testing Methods Indian Medical PG Question 6: Which medium is most commonly used for antibiotic sensitivity testing?
- A. CLED agar
- B. Mueller-Hinton agar (Correct Answer)
- C. Blood agar
- D. MacConkey agar
Allergic Testing Methods Explanation: ***Mueller-Hinton agar***
- It is specifically formulated to provide optimal conditions for bacterial growth and **diffusion of antibiotics**, ensuring accurate and reproducible results for sensitivity testing.
- Its **low concentration of sulfonamide inhibitors (thymidine and thymine)** and proper calcium and magnesium levels are crucial for accurate results for particular antibiotics.
- It is the **gold standard medium** recommended by CLSI (Clinical and Laboratory Standards Institute) for the Kirby-Bauer disk diffusion method.
*Blood agar*
- Blood agar is a **general-purpose enrichment medium** that supports the growth of a wide range of fastidious microorganisms and is used to detect hemolytic reactions.
- While many bacteria grow on blood agar, its composition and opacity can **interfere with precise zone of inhibition measurements** in antibiotic susceptibility testing.
*MacConkey agar*
- MacConkey agar is a **selective and differential medium** used for the isolation of Gram-negative enteric bacteria and differentiation based on lactose fermentation.
- Its selective agents (bile salts and crystal violet) and pH indicators would **interfere with the standardized conditions** required for accurate antibiotic sensitivity testing.
*CLED agar*
- **Cystine-Lactose-Electrolyte-Deficient (CLED) agar** is primarily used for the isolation and enumeration of urinary tract pathogens, as it prevents the swarming of *Proteus* species and differentiates lactose fermenters from non-fermenters.
- It is **not optimized** for antibiotic diffusion or inhibition of bacterial growth in the same way Mueller-Hinton is.
Allergic Testing Methods Indian Medical PG Question 7: Which of the following are early mediators of allergic rhinitis?
- A. Leukotrienes
- B. Interleukin-4
- C. Interleukin-5
- D. Platelet-activating factor and bradykinin (Correct Answer)
Allergic Testing Methods Explanation: ### Explanation
Allergic rhinitis is a Type I hypersensitivity reaction occurring in two distinct phases: the **Early Phase** (within minutes) and the **Late Phase** (4–8 hours later).
**Why Option D is Correct:**
The early phase is triggered when an allergen cross-links IgE antibodies on the surface of **mast cells**, leading to immediate degranulation. This releases **pre-formed mediators** and rapidly synthesized lipid mediators.
* **Histamine** is the primary mediator.
* **Platelet-activating factor (PAF), Bradykinin, and Prostaglandin D2** are also released during this immediate window, causing vasodilation, increased vascular permeability (edema), and stimulation of sensory nerves (itching/sneezing).
**Why Other Options are Incorrect:**
* **A. Leukotrienes:** While Cysteinyl Leukotrienes (CysLTs) are produced during the early phase, they are most characteristic of the transition to and maintenance of the **Late Phase** response, contributing significantly to prolonged nasal congestion.
* **B & C. Interleukin-4 and Interleukin-5:** These are **cytokines** produced by Th2 lymphocytes. They are involved in the **Late Phase** response. IL-4 promotes IgE isotype switching, while IL-5 is the primary factor for **eosinophil** recruitment and activation.
**NEET-PG High-Yield Pearls:**
1. **Early Phase (Minutes):** Mediated by Mast cells. Key symptoms: Sneezing, itching, rhinorrhea. Key mediator: Histamine.
2. **Late Phase (Hours):** Mediated by Eosinophils, Basophils, and Th2 cells. Key symptom: Nasal congestion.
3. **Gold Standard Diagnosis:** Skin Prick Test (detects specific IgE).
4. **Pharmacology Link:** Antihistamines work best on early-phase symptoms (itch/sneeze), while Intranasal Steroids are the most effective treatment for late-phase symptoms (congestion) because they inhibit cytokine release.
Allergic Testing Methods Indian Medical PG Question 8: Which of the following preformed toxins is involved in the mechanism of allergic rhinitis?
- A. Histamine (Correct Answer)
- B. Leukotriene
- C. TXA2
- D. PGD2
Allergic Testing Methods Explanation: Allergic rhinitis is a **Type I Hypersensitivity reaction** mediated by IgE antibodies. When an allergen cross-links IgE on the surface of mast cells, it triggers **degranulation**, releasing two types of chemical mediators: **Preformed mediators** (stored in granules) and **Newly synthesized mediators** (produced after activation).
### Why Histamine is Correct
**Histamine** is the primary **preformed mediator** stored in the granules of mast cells and basophils. Upon degranulation, it is released immediately (within minutes), causing the "Early Phase" symptoms of allergic rhinitis: vasodilation, increased capillary permeability (edema/nasal block), and stimulation of sensory nerves (itching/sneezing).
### Why Other Options are Incorrect
* **Leukotrienes (B):** These are **newly synthesized** mediators derived from arachidonic acid via the lipoxygenase pathway. While potent (causing mucus secretion and congestion), they are produced *after* mast cell activation and are not pre-stored.
* **TXA2 (Thromboxane A2) (C):** This is a product of the cyclooxygenase pathway primarily involved in platelet aggregation and vasoconstriction; it plays a minimal role in the pathophysiology of allergic rhinitis.
* **PGD2 (Prostaglandin D2) (D):** Like leukotrienes, PGD2 is a **newly synthesized** mediator produced via the cyclooxygenase pathway. It contributes to late-phase inflammation but is not preformed.
### NEET-PG High-Yield Pearls
* **Early Phase Response:** Mediated by **Histamine** (Preformed). Occurs within minutes.
* **Late Phase Response:** Mediated by **Leukotrienes, PGD2, and Cytokines**. Occurs 4–8 hours later; characterized by eosinophil infiltration.
* **Drug of Choice:** Intranasal corticosteroids are the most effective maintenance therapy for allergic rhinitis.
* **Gold Standard Test:** Skin Prick Test (SPT) is used to identify specific allergens.
Allergic Testing Methods Indian Medical PG Question 9: A 29-year-old non-smoker man presents with sneezing, post-nasal drip, eye-watering, and an itch of his posterior pharynx. These symptoms tend to be worse in the spring and summer and have been bothering him since mid-April. His past medical history is remarkable only for mild asthma induced by being outdoors. He takes no regular medications but does take diphenhydramine on occasion. What is the most appropriate diagnostic test at this time?
- A. Blood radioallergosorbent test
- B. None, the diagnosis is based solely on the history and physical examination (Correct Answer)
- C. Intradermal testing
- D. Serum protein electrophoresis
Allergic Testing Methods Explanation: **Explanation:**
The patient presents with classic symptoms of **Allergic Rhinitis (AR)**: paroxysmal sneezing, post-nasal drip, ocular symptoms (watering), and palatal itching. The seasonal pattern (spring/summer) and comorbid mild asthma strongly suggest **Seasonal Allergic Rhinitis**.
**1. Why Option B is Correct:**
In clinical practice, the diagnosis of Allergic Rhinitis is primarily **clinical**, based on a characteristic history and physical examination (e.g., pale/bluish nasal mucosa, turbinate hypertrophy). Diagnostic testing is **not mandatory** for initial management. Testing (like Skin Prick Tests) is typically reserved for patients who do not respond to empirical therapy (intranasal corticosteroids/antihistamines) or those being considered for allergen-specific immunotherapy.
**2. Why Other Options are Incorrect:**
* **Option A (RAST):** This measures allergen-specific IgE in the blood. While useful if skin testing is contraindicated (e.g., severe eczema or antihistamine use), it is more expensive and less sensitive than skin testing. It is not the first-line diagnostic step.
* **Option C (Intradermal testing):** This is more sensitive but less specific than the Skin Prick Test (SPT). It carries a higher risk of systemic anaphylaxis and is generally used only if SPT is negative despite a strong clinical suspicion.
* **Option D (Serum protein electrophoresis):** This is used to diagnose plasma cell dyscrasias (like Multiple Myeloma) and has no role in the diagnosis of allergy.
**Clinical Pearls for NEET-PG:**
* **First-line treatment for AR:** Intranasal Corticosteroids (e.g., Fluticasone).
* **Allergic Shiners:** Dark circles under eyes due to venous congestion.
* **Allergic Salute:** Upward rubbing of the nose leading to a **transverse nasal crease**.
* **Gold Standard for identifying allergens:** Skin Prick Test (SPT).
* **Definitive/Disease-modifying treatment:** Immunotherapy (SIT/SLIT).
Allergic Testing Methods Indian Medical PG Question 10: Which of the following is the preformed toxin involved in the mechanism of allergic rhinitis?
- A. Histamine (Correct Answer)
- B. Leukotriene
- C. TXA2
- D. PGD2
Allergic Testing Methods Explanation: ### Explanation
The pathophysiology of Allergic Rhinitis is a **Type I Hypersensitivity reaction** mediated by IgE. When an allergen cross-links IgE antibodies on the surface of mast cells, it triggers **degranulation**, leading to the release of two types of inflammatory mediators:
**1. Why Histamine is Correct:**
Histamine is a **preformed mediator** stored in the granules of mast cells and basophils. Upon activation, it is released immediately (within minutes), causing the "Early Phase" response characterized by sneezing, itching, and rhinorrhea. Because it is synthesized and stored *before* the allergic trigger occurs, it is classified as a preformed toxin/mediator.
**2. Why the Other Options are Incorrect:**
* **Leukotrienes (B), TXA2 (C), and PGD2 (D):** These are **newly synthesized mediators** (lipid-derived). They are not stored in granules but are produced *de novo* from arachidonic acid via the cyclooxygenase (COX) or lipoxygenase (LOX) pathways only after the mast cell is activated. These mediators typically contribute to the "Late Phase" response, leading to nasal congestion and sustained inflammation.
### NEET-PG High-Yield Pearls:
* **Early Phase (Minutes):** Primarily mediated by **Histamine**. Clinical features: Sneezing, itching, watery rhinorrhea.
* **Late Phase (4–8 hours):** Mediated by **Leukotrienes (LTC4, LTD4, LTE4)**, Cytokines, and PGD2. Clinical feature: Nasal congestion (due to cellular infiltration, mainly eosinophils).
* **Gold Standard Investigation:** Skin Prick Test (detects specific IgE).
* **Drug of Choice:** Intranasal Corticosteroids (act on both early and late phases).
* **Mast Cell Stabilizer:** Sodium Cromoglycate (prevents degranulation; used prophylactically).
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