Addiction Assessment Tools Indian Medical PG Practice Questions and MCQs
Practice Indian Medical PG questions for Addiction Assessment Tools. These multiple choice questions (MCQs) cover important concepts and help you prepare for your exams.
Addiction Assessment Tools Indian Medical PG Question 1: Which of the following is a validated screening tool for alcohol use disorder?
- A. AUDIT
- B. CAGE questionnaire
- C. SADQ
- D. All of the options (Correct Answer)
Addiction Assessment Tools Explanation: ***CAGE questionnaire and AUDIT***
- Both **CAGE** and **AUDIT** are widely validated screening tools specifically designed for alcohol use disorder [1].
- **CAGE** is a brief 4-item tool focusing on **C**ut down, **A**nnoyed, **G**uilty, and **E**ye-opener - ideal for quick screening in clinical settings [1].
- **AUDIT** (Alcohol Use Disorders Identification Test) is a comprehensive 10-item tool assessing consumption patterns, drinking behaviors, and alcohol-related problems.
- AUDIT is considered the **gold standard** for screening and can assess risk levels and severity.
*Why not SADQ alone?*
- **SADQ** (Severity of Alcohol Dependence Questionnaire) is primarily a **severity assessment tool**, not a screening tool.
- It is a 20-item instrument used to measure the **degree of alcohol dependence** in individuals already identified with alcohol problems.
- While valuable for treatment planning, SADQ is more detailed and designed for assessment rather than initial screening [1].
- However, all three tools are validated and used in alcohol use disorder evaluation - CAGE and AUDIT for screening, SADQ for severity assessment.
Addiction Assessment Tools Indian Medical PG Question 2: Which of the following attributes are essential for an ideal screening test?
- A. Safe
- B. Reliable
- C. Valid
- D. All of the options (Correct Answer)
Addiction Assessment Tools Explanation: ***All of the options***
- An ideal screening test must possess **all three essential attributes**: safety, reliability, and validity.
- **Safe**: Minimizes harm to participants and ensures ethical implementation
- **Reliable**: Produces consistent, reproducible results with minimal random error
- **Valid**: Accurately measures what it intends to measure (high sensitivity and specificity)
- These three attributes work together as fundamental requirements for any effective screening program, ensuring that early detection benefits outweigh potential risks.
*Safe (alone)*
- While safety is absolutely essential, it is **not sufficient by itself** to make an ideal screening test.
- A test that is safe but unreliable or invalid would produce inconsistent or inaccurate results, rendering it ineffective for screening purposes.
*Reliable (alone)*
- Reliability ensures consistent results, which is crucial, but **reliability alone is insufficient**.
- A test can be highly reliable (consistently giving the same result) yet completely invalid if it measures the wrong thing or is unsafe.
*Valid (alone)*
- Validity is critical for accurate measurement, but **validity alone does not make a test ideal**.
- Even a valid test must be safe to protect participants and reliable to ensure consistency across different settings and times.
Addiction Assessment Tools Indian Medical PG Question 3: All should be features of a substance to measure GFR, except?
- A. Freely reabsorbed (Correct Answer)
- B. Not secreted by kidney
- C. Freely filtered across the glomerulus membrane
- D. None of the options
Addiction Assessment Tools Explanation: ***Freely reabsorbed***
- A substance used to measure GFR should **not be reabsorbed** by the kidney tubules. If it were reabsorbed, the amount excreted in the urine would be less than the amount filtered, leading to an **underestimation of GFR**.
- The ideal GFR marker is **neither reabsorbed nor secreted**, ensuring that its excretion rate directly reflects the filtration rate.
*Freely filtered across the glomerulus membrane*
- For a substance to accurately measure GFR, it must be **freely filtered** from the blood into the Bowman's capsule, without any restriction due to its size or charge.
- This ensures that its concentration in the glomerular filtrate is the same as in the plasma, allowing for a direct calculation of the filtration rate.
*Not secreted by kidney*
- An ideal GFR marker should **not be secreted** by the renal tubules, as active secretion would add to the amount excreted in the urine, leading to an **overestimation of GFR**.
- This property, along with not being reabsorbed, ensures that the amount of the substance appearing in the urine solely reflects the amount filtered.
*None of the options*
- This option is incorrect because there is a definitive feature listed among the choices that is *not* a characteristic of an ideal GFR marker. The ability to be "freely reabsorbed" is a disqualifying trait.
Addiction Assessment Tools Indian Medical PG Question 4: Which of the following is true regarding nicotine substitution therapy?
- A. Preferably given by gastrointestinal route.
- B. Varenicline comes with a black box warning of cardiovascular death
- C. There should be a 15-minute gap between nicotine gum and coffee/soda/acidic food as they decrease its absorption (Correct Answer)
- D. Nicotine chewing gum is better for constant use as it gives 25% higher blood level than lozenges
Addiction Assessment Tools Explanation: ***There should be a 15-minute gap between nicotine gum and coffee/soda/acidic food as they decrease its absorption***
- **Acidic beverages** like coffee, soda, and fruit juices can alter the pH of the mouth and stomach, which significantly **reduces the absorption of nicotine** from gum.
- This recommendation ensures optimal **nicotine delivery** and effectiveness of the therapy in reducing withdrawal symptoms.
*Preferably given by gastrointestinal route*
- Nicotine has poor bioavailability when taken orally due to **extensive first-pass metabolism** in the liver.
- Nicotine substitution therapies are therefore preferentially administered via **transdermal**, **buccal** (gum, lozenges), or **nasal routes** to bypass first-pass metabolism and achieve therapeutic blood levels more effectively.
*Varenicline comes with a black box warning of cardiovascular death*
- Varenicline (Chantix) previously had a black box warning for **neuropsychiatric side effects**, including suicidal ideation and depression, which has since been removed due to further studies.
- It does not carry a black box warning specifically for **cardiovascular death**, though cardiovascular events have been a subject of study, particularly in patients with pre-existing cardiovascular conditions.
*Nicotine chewing gum is better for constant use as it gives 25% higher blood level than lozenges*
- While both nicotine gum and lozenges are effective, the **blood levels achieved are comparable**, and the choice often depends on patient preference and proper technique.
- Nicotine gum is best used with a **"chew and park" technique** to allow buccal absorption, and constant chewing can lead to excessive swallowing of nicotine, causing gastrointestinal upset.
Addiction Assessment Tools Indian Medical PG Question 5: Which of the following statements about testicular feminizing syndrome is incorrect?
- A. Absent vagina (Correct Answer)
- B. Absent ovary
- C. Chromosome pattern 46 x Y
- D. Absent uterus
Addiction Assessment Tools Explanation: ### Absent vagina
- This statement is incorrect. In **complete androgen insensitivity syndrome (CAIS)**, formerly known as testicular feminizing syndrome, individuals develop a **blind-ending vagina** that is typically shorter than normal, but it is not entirely absent.
- The external genitalia are unambiguously female, leading to a female appearance, but the presence of testes and lack of a uterus/fallopian tubes are key features.
*Absent ovary*
- This statement is correct. Individuals with **complete androgen insensitivity syndrome (CAIS)** are **genetically male (46,XY)** and have **testes**, not ovaries.
- The testes are usually undescended (intra-abdominal or inguinal) and produce androgens, but the body's cells are unresponsive to these hormones.
*Chromosome pattern 46 x Y*
- This statement is correct. **Complete androgen insensitivity syndrome (CAIS)** is characterized by a **46,XY karyotype**, meaning individuals are genetically male [1].
- Despite the male genotype, the inability to respond to androgens leads to female external phenotypic development.
*Absent uterus*
- This statement is correct. In **complete androgen insensitivity syndrome (CAIS)**, the **testes produce anti-Müllerian hormone (AMH)**, which causes the regression of the Müllerian ducts.
- As a result, structures derived from the Müllerian ducts, such as the **uterus** and fallopian tubes, are absent.
Addiction Assessment Tools Indian Medical PG Question 6: What are nitrergic neurons?
- A. Postganglionic neurons releasing nitric oxide.
- B. First-order neurons releasing nitric oxide. (Correct Answer)
- C. Postganglionic neurons releasing substance P.
- D. First-order neurons releasing calcitonin gene-related peptide.
Addiction Assessment Tools Explanation: **Nitrergic neurons** are a specific class of neurons that utilize **Nitric Oxide (NO)** as their primary neurotransmitter. Unlike classical neurotransmitters stored in vesicles, NO is a gaseous molecule synthesized on demand by the enzyme **Neuronal Nitric Oxide Synthase (nNOS)** [1].
**Why Option B is Correct:**
In the context of the autonomic and enteric nervous systems, nitrergic neurons are typically **first-order neurons** (primary neurons) that release NO to mediate physiological functions. In the gastrointestinal tract, they are the principal inhibitory neurons of the myenteric plexus, responsible for the relaxation of smooth muscles (e.g., the Lower Esophageal Sphincter and the Sphincter of Oddi) [2].
**Analysis of Incorrect Options:**
* **Option A:** While some postganglionic parasympathetic fibers (like those in the corpora cavernosa) release NO, the term "nitrergic neuron" fundamentally refers to the primary/first-order signaling unit in the inhibitory pathways of the enteric nervous system.
* **Option C & D:** Substance P and Calcitonin Gene-Related Peptide (CGRP) are neuropeptides associated with **peptidergic neurons**, primarily involved in pain transmission (nociception) and vasodilation, not nitrergic signaling [2].
**High-Yield Clinical Pearls for NEET-PG:**
* **Achalasia Cardia:** This condition results from the selective **loss of nitrergic neurons** in the myenteric (Auerbach's) plexus, leading to the failure of the Lower Esophageal Sphincter (LES) to relax.
* **Erectile Dysfunction:** NO released from nitrergic nerves in the penis activates guanylyl cyclase, increasing cGMP and causing vasodilation [1]. Sildenafil works by preventing the breakdown of this cGMP.
* **Infantile Hypertrophic Pyloric Stenosis:** Also associated with a deficiency of nNOS and nitrergic innervation at the pylorus.
Addiction Assessment Tools Indian Medical PG Question 7: Punctate yellow exudates in the colon, found on endoscopic examination, are indicative of which of the following?
- A. Balantidium coli
- B. Ulcerative colitis
- C. Antibiotic-associated colitis (Correct Answer)
- D. Gluten-induced enteropathy
Addiction Assessment Tools Explanation: ### **Explanation**
The correct answer is **Antibiotic-associated colitis (Pseudomembranous colitis)**.
**1. Why the Correct Answer is Right:**
Antibiotic-associated colitis, most commonly caused by **_Clostridioides difficile_ (C. diff)** toxins, is characterized by the formation of **pseudomembranes**. On endoscopic examination (sigmoidoscopy or colonoscopy), these appear as classic **punctate yellow-white exudates** or plaques scattered over the colonic mucosa [1]. These plaques are composed of fibrin, inflammatory cells (neutrophils), and necrotic debris. As the disease progresses, these small punctate spots can coalesce to form larger membranes.
**2. Why the Incorrect Options are Wrong:**
* **Balantidium coli:** This parasitic infection typically causes **flask-shaped ulcers** (similar to Amoebiasis) rather than yellow exudative plaques.
* **Ulcerative colitis:** Endoscopy typically reveals continuous mucosal inflammation starting from the rectum, characterized by **loss of vascular markings, friability, and "lead-pipe" appearance** in chronic cases [1]. It does not present with punctate yellow exudates.
* **Gluten-induced enteropathy (Celiac Disease):** This primarily affects the **small intestine** (duodenum/jejunum). Endoscopic findings include scalloping of folds, fissuring, and a mosaic pattern, not colonic exudates.
**3. High-Yield Clinical Pearls for NEET-PG:**
* **Risk Factor:** Most common after the use of **Clindamycin**, Fluoroquinolones, or 3rd generation Cephalosporins [1].
* **Diagnosis:** The gold standard for diagnosis is the detection of **C. diff toxin A and B** in the stool via PCR or EIA [1].
* **Histology:** Look for the characteristic **"Volcano lesion"** (an eruption of fibrin and PMNs from an ulcerated crypt).
* **Treatment:** First-line treatment is oral **Vancomycin** or **Fidaxomicin**. Metronidazole is now reserved for non-severe cases where other options are unavailable.
Addiction Assessment Tools Indian Medical PG Question 8: A person has a history of steatorrhea of long duration. D-xylose testing was performed. A 5-hour urine sample showed <4.5 g excretion after a 25g D-xylose load. What is/are the probable diagnosis?
- A. Celiac disease (Correct Answer)
- B. Pancreatitis
- C. Blind loop syndrome
- D. Heal disease
Addiction Assessment Tools Explanation: The **D-xylose absorption test** is a classic diagnostic tool used to differentiate between **malabsorption** (mucosal disease) and **maldigestion** (pancreatic insufficiency). D-xylose is a monosaccharide that is absorbed in the proximal small intestine by passive diffusion and does not require pancreatic enzymes for digestion [1].
1. **Why Celiac Disease is Correct:** In Celiac disease, there is diffuse mucosal damage and blunting of the villi in the small intestine. This leads to impaired absorption of D-xylose [1]. A 5-hour urinary excretion of **<4.5 g** (after a 25g oral load) indicates intestinal mucosal dysfunction, confirming malabsorption.
2. **Why Pancreatitis is Incorrect:** In chronic pancreatitis, steatorrhea occurs due to a lack of lipase (maldigestion) [1]. However, the intestinal mucosa remains intact. Therefore, D-xylose is absorbed normally, and urinary excretion will be **>4.5 g** (Normal).
3. **Why Blind Loop Syndrome is Incorrect:** While Small Intestinal Bacterial Overgrowth (SIBO) can sometimes cause a false positive D-xylose test (as bacteria may metabolize the sugar), it is not the primary diagnosis associated with classic mucosal malabsorption in standard NEET-PG scenarios.
4. **Why Ileal Disease is Incorrect:** D-xylose is primarily absorbed in the **duodenum and jejunum**. Disease localized strictly to the terminal ileum (like Crohn’s) typically results in a normal D-xylose test but abnormal Vitamin B12 absorption (Schilling test).
**High-Yield Clinical Pearls for NEET-PG:**
* **Normal D-xylose test:** Points toward Pancreatic Insufficiency.
* **Abnormal D-xylose test:** Points toward Mucosal Disease (Celiac, Tropical Sprue, Whipple’s) [1].
* **False Positives:** Can occur in patients with renal failure, ascites, or delayed gastric emptying.
* **Gold Standard for Celiac:** Small bowel biopsy showing villous atrophy and crypt hyperplasia.
Addiction Assessment Tools Indian Medical PG Question 9: A moderate increase in serum aminotransferases with AST/ALT > 3 is suggestive of which of the following?
- A. Acute viral hepatitis
- B. Prolonged hypotension
- C. Alcoholic liver disease (Correct Answer)
- D. Drug hepatotoxicity
Addiction Assessment Tools Explanation: In alcoholic liver disease (ALD), the ratio of **AST to ALT is typically >2:1**, and a ratio **>3:1** is highly suggestive of the diagnosis.
### Why Alcoholic Liver Disease is Correct
The biochemical basis for this ratio lies in two factors:
1. **Pyridoxal-5'-phosphate (Vitamin B6) Deficiency:** Chronic alcohol consumption leads to a deficiency of Vitamin B6, which is a required co-factor for ALT synthesis. Consequently, ALT levels remain relatively low even during liver injury.
2. **Mitochondrial Damage:** Alcohol is a mitochondrial toxin [1]. AST exists in both cytosolic and mitochondrial forms; alcohol-induced damage causes the preferential release of mitochondrial AST [1].
In ALD, the absolute values of transaminases are usually only **moderately elevated** (typically <300-500 IU/L). If AST exceeds 500 IU/L or ALT exceeds 300 IU/L, a co-existing cause (like acetaminophen toxicity) should be suspected [1].
### Why Other Options are Incorrect
* **Acute Viral Hepatitis:** Characterized by massive elevations in transaminases (often >1000 IU/L) with an **AST/ALT ratio <1** [2].
* **Prolonged Hypotension (Ischemic Hepatitis):** Causes "shock liver" with rapid, dramatic rises in transaminases (often >5000 IU/L) and LDH.
* **Drug Hepatotoxicity:** Most drugs (except for specific toxins like acetaminophen in the late stage) typically present with an **AST/ALT ratio <1**.
### High-Yield Clinical Pearls for NEET-PG
* **GGT (Gamma-Glutamyl Transferase):** The most sensitive marker for chronic alcohol ingestion, though less specific than the AST/ALT ratio [3].
* **Macrocytosis (High MCV):** Often seen in chronic alcoholics due to direct bone marrow toxicity or folate deficiency [3].
* **Rule of Thumb:** If AST/ALT >2, think Alcohol. If ALT > AST, think Viral or Fatty Liver (NAFLD).
Addiction Assessment Tools Indian Medical PG Question 10: The pathogenesis of hypochromic anemia in lead poisoning is due to which of the following mechanisms?
- A. Inhibition of enzymes involved in heme biosynthesis (Correct Answer)
- B. Binding of lead to transferrin, inhibiting the transport of iron
- C. Binding of lead to the cell membrane of erythroid precursors
- D. Binding of lead to ferritin, inhibiting their breakdown into hemosiderin
Addiction Assessment Tools Explanation: Lead poisoning (Plumbism) causes a microcytic hypochromic anemia primarily by interfering with the enzymatic pathway of heme synthesis.
**1. Why Option A is Correct:**
Lead inhibits two critical enzymes in the heme biosynthetic pathway:
* **Delta-aminolevulinic acid dehydratase (ALAD):** Lead inhibits this enzyme, preventing the conversion of ALA to porphobilinogen [1]. This leads to an accumulation of ALA in the blood and urine.
* **Ferrochelatase:** This enzyme is responsible for incorporating iron into the protoporphyrin ring to form heme [3]. Lead inhibits this step, resulting in an accumulation of **erythrocyte protoporphyrin**.
The lack of heme production results in decreased hemoglobin synthesis, leading to the characteristic **hypochromic anemia**.
**2. Why Other Options are Incorrect:**
* **Option B & D:** Lead does not significantly interfere with iron transport (transferrin) or storage (ferritin/hemosiderin). The iron is available, but the cell cannot utilize it to make heme due to enzyme inhibition.
* **Option C:** While lead does bind to red cell membranes and inhibits the enzyme **5'-nucleotidase** (leading to **basophilic stippling** due to RNA degradation failure) [2], this mechanism contributes to hemolysis rather than the primary defect in hemoglobin synthesis (hypochromia).
**High-Yield Clinical Pearls for NEET-PG:**
* **Basophilic Stippling:** Coarse blue granules in RBCs (retained RNA) is a classic peripheral smear finding [2].
* **Burton’s Line:** Bluish-purple line on the gingival margin [2].
* **Radiology:** "Lead lines" (increased density) at the metaphyses of long bones in children [2].
* **Treatment:** Chelation therapy with **Succimer** (oral, first-line in kids), **Ca-EDTA**, or **Dimercaprol (BAL)** [4].
More Addiction Assessment Tools Indian Medical PG questions available in the OnCourse app. Practice MCQs, flashcards, and get detailed explanations.
