Alcohol Metabolism Indian Medical PG Practice Questions and MCQs
Practice Indian Medical PG questions for Alcohol Metabolism. These multiple choice questions (MCQs) cover important concepts and help you prepare for your exams.
Alcohol Metabolism Indian Medical PG Question 1: All are true regarding methanol poisoning except.
- A. High anion gap metabolic acidosis is seen in severe cases
- B. Visual disturbances are commonly seen
- C. Hemodialysis is not required in methanol poisoning. (Correct Answer)
- D. Fomepizole acts by inhibiting alcohol dehydrogenase
Alcohol Metabolism Explanation: ***Hemodialysis is not required in methanol poisoning.***
- This statement is **false**, as hemodialysis is often a critical intervention in severe methanol poisoning to actively remove methanol and its toxic metabolites from the body, especially in cases of severe acidosis or organ damage [1].
- Due to the **small molecular size** of methanol and formic acid, **hemodialysis** is highly effective and recommended for rapid clearance.
*High anion gap metabolic acidosis is seen in severe cases*
- This statement is **true**; methanol is metabolized into **formic acid**, which accumulates and causes a characteristic **high anion gap metabolic acidosis** [2], [3].
- The acidosis is directly responsible for many of the severe clinical manifestations and is a key diagnostic feature [4].
*Visual disturbances are commonly seen*
- This statement is **true**; methanol poisoning frequently leads to **visual disturbances**, including blurred vision, photophobia, and even **permanent blindness**, due to the toxic effect of formic acid on the **optic nerve** [2], [4].
- Funduscopic examination may reveal **optic disc hyperemia** or edema in severe cases [4].
*Fomepizole acts by inhibiting alcohol dehydrogenase*
- This statement is **true**; **fomepizole** is the antidote for methanol poisoning and works by competing with methanol for the enzyme **alcohol dehydrogenase** [2], [3].
- By inhibiting alcohol dehydrogenase, fomepizole prevents the metabolism of methanol into its toxic metabolites, **formaldehyde** and **formic acid**, thus reducing toxicity [3].
Alcohol Metabolism Indian Medical PG Question 2: What is the mechanism of metabolism for alcohol, aspirin, and phenytoin at high doses?
- A. First pass kinetics
- B. First order kinetics
- C. Zero order kinetics (Correct Answer)
- D. Second order kinetics
Alcohol Metabolism Explanation: ***Zero order kinetics***
- This mechanism occurs when the **metabolic enzymes become saturated at high drug concentrations**, leading to a constant amount (not a constant percentage) of drug being eliminated per unit time.
- Alcohol, aspirin, and phenytoin are examples of drugs that exhibit **saturable metabolism**, transitioning from first-order to zero-order kinetics at higher doses.
*First pass kinetics*
- This describes the **metabolism of a drug by the liver or gut wall enzymes before it reaches systemic circulation** after oral administration.
- While relevant to the oral bioavailability of these drugs, it does not describe the specific mechanism of elimination at high doses.
*First order kinetics*
- In this mechanism, a **constant fraction or percentage of the drug is eliminated per unit of time**, meaning the rate of elimination is directly proportional to the drug concentration.
- Most drugs follow first-order kinetics at therapeutic doses because metabolizing enzymes are not saturated.
*Second order kinetics*
- This is a **less common pharmacokinetic model** where the rate of elimination is proportional to the square of the drug concentration or involves two reactants.
- It does not typically describe the common elimination patterns of most drugs, including alcohol, aspirin, and phenytoin.
Alcohol Metabolism Indian Medical PG Question 3: In a patient with chronic alcoholism, which nutrient deficiency is most likely to cause neurological symptoms?
- A. Vitamin B6
- B. Thiamine (Correct Answer)
- C. Folate
- D. Vitamin B12
Alcohol Metabolism Explanation: ***Thiamine***
- **Thiamine (Vitamin B1)** deficiency is extremely common in chronic alcoholism due to poor nutrition and impaired absorption, leading to neurological disorders like **Wernicke-Korsakoff syndrome** [1].
- **Wernicke-Korsakoff syndrome** manifests with symptoms such as **ataxia**, **ophthalmoplegia**, **confusion**, and **memory impairment** [2].
*Vitamin B6*
- While **Vitamin B6 (pyridoxine)** deficiency can occur in alcoholism, it is more commonly associated with peripheral neuropathy rather than the extensive neurological picture seen with thiamine deficiency.
- Severe B6 deficiency can cause **seizures** and **encephalopathy**, but these are less common as primary neurological manifestations in typical chronic alcoholics compared to Wernicke-Korsakoff syndrome.
*Folate*
- **Folate deficiency** is very common in chronic alcoholism and primarily leads to **macrocytic anemia**.
- While it can indirectly contribute to neurological issues due to anemia, it does not directly cause the classic acute neurological syndromes seen with thiamine deficiency.
*Vitamin B12*
- **Vitamin B12 deficiency** can cause neurological symptoms, including **peripheral neuropathy**, **ataxia**, and **cognitive impairment**, but it is less directly associated with alcoholism compared to thiamine deficiency.
- B12 deficiency is more commonly seen in strict vegetarians, pernicious anemia, or malabsorption conditions involving the ileum.
Alcohol Metabolism Indian Medical PG Question 4: In chronic alcoholism and its complications, which of the following is seen?
- A. Wernicke's syndrome
- B. Delirium tremens
- C. Korsakoff psychosis
- D. All of the options (Correct Answer)
Alcohol Metabolism Explanation: ***All of the options***
- **Wernicke's syndrome**, **Delirium tremens**, and **Korsakoff psychosis** are all well-recognized neurological and psychiatric complications associated with **chronic alcoholism**
- Chronic alcohol abuse leads to nutritional deficiencies (especially **thiamine deficiency**) and neurotoxicity, predisposing individuals to these distinct but related conditions
*Wernicke's syndrome*
- Acute neurological disorder caused by **thiamine deficiency**
- Characterized by classic triad: **ataxia**, **ophthalmoplegia**, and **confusion**
- If untreated, can progress to **Korsakoff psychosis**
*Delirium tremens*
- Severe form of **alcohol withdrawal** in individuals with long history of heavy drinking
- Symptoms include **delirium**, **severe agitation**, **tremors**, **hallucinations**, and autonomic hyperactivity (**tachycardia**, **hypertension**, **fever**)
- Medical emergency requiring prompt treatment
*Korsakoff psychosis*
- Occurs due to chronic **thiamine deficiency**, often following Wernicke's encephalopathy
- Characterized by severe **anterograde and retrograde amnesia**, **confabulation**, and relative preservation of other cognitive functions
- Often results in permanent cognitive impairment
Alcohol Metabolism Indian Medical PG Question 5: Which of these is the best for management of methanol poisoning?
- A. Fomepizole (Correct Answer)
- B. Naltrexone
- C. Disulfiram
- D. Acamprosate
Alcohol Metabolism Explanation: ***Fomepizole***
- **Fomepizole** is a competitive inhibitor of **alcohol dehydrogenase**, the enzyme responsible for metabolizing methanol into toxic metabolites like formic acid.
- By inhibiting this enzyme, it prevents the formation of these toxic metabolites, thereby reducing organ damage and metabolic acidosis in methanol poisoning.
*Naltrexone*
- **Naltrexone** is an **opioid receptor antagonist** used in the treatment of alcohol and opioid dependence.
- It does not have any direct action on the metabolism of methanol or its toxic byproducts.
*Disulfiram*
- **Disulfiram** inhibits **aldehyde dehydrogenase**, leading to an unpleasant reaction when alcohol is consumed (flushing, nausea, vomiting).
- It is used for alcohol cessation and has no role in the management of methanol poisoning.
*Acamprosate*
- **Acamprosate** is a medication used to reduce alcohol cravings in individuals recovering from alcohol dependence, possibly by modulating **glutamate neurotransmission**.
- It does not directly affect the metabolism of methanol or mitigate its toxic effects.
Alcohol Metabolism Indian Medical PG Question 6: A 25-year-old male flushes and feels ill after drinking small amounts of ethanol in alcoholic beverages. This is due to a genetic variation in an enzyme that metabolizes a liver metabolite of alcohol. Which metabolite accumulates?
- A. Methanol
- B. Acetone
- C. Acetaldehyde (Correct Answer)
- D. Hydrogen peroxide
Alcohol Metabolism Explanation: ***Acetaldehyde***
- The flushing and illness after consuming alcohol are characteristic symptoms of **acetaldehyde accumulation**.
- This occurs due to a genetic polymorphism (often seen in individuals of East Asian descent) in **aldehyde dehydrogenase (ALDH2)**, which is responsible for converting acetaldehyde to acetate.
*Methanol*
- **Methanol** is metabolized to **formaldehyde** and then to **formic acid**, which are highly toxic and cause severe symptoms like metabolic acidosis, blindness, and death.
- Methanol poisoning typically results from ingestion of denatured alcohol or adulterated spirits, not small amounts of ethanol-containing beverages.
*Acetone*
- **Acetone** is a ketone body produced during fat metabolism and is not a direct liver metabolite of ethanol.
- While it can be found in the body, its metabolism is primarily via different pathways and does not cause the "alcohol flush reaction."
*Hydrogen peroxide*
- **Hydrogen peroxide** is a reactive oxygen species involved in oxidative stress and is not a direct metabolite of alcohol in the liver associated with flushing and illness from alcohol consumption.
- It is primarily catabolized by **catalase** and **glutathione peroxidase**.
Alcohol Metabolism Indian Medical PG Question 7: Which of the following statements about methyl alcohol poisoning is incorrect?
- A. Effects are due to formic acid
- B. Metabolic acidosis
- C. Blindness
- D. Fomepizole competitively inhibits aldehyde dehydrogenase (Correct Answer)
Alcohol Metabolism Explanation: ***Fomepizole competitively inhibits aldehyde dehydrogenase***
- **Fomepizole** acts as a competitive inhibitor of **alcohol dehydrogenase**, not aldehyde dehydrogenase.
- By inhibiting alcohol dehydrogenase, fomepizole prevents the metabolism of methanol into toxic metabolites like formic acid.
*Effects are due to formic acid*
- This statement is correct. The primary toxicity of methanol poisoning is due to its metabolism into **formic acid** by alcohol and aldehyde dehydrogenases.
- Formic acid is responsible for the **metabolic acidosis** and **ocular toxicity** observed.
*Metabolic acidosis*
- This statement is correct. Methanol poisoning leads to severe **anion gap metabolic acidosis** due to the accumulation of formic acid.
- The acidosis contributes significantly to the overall toxicity and clinical manifestations.
*Blindness*
- This statement is correct. **Blindness** is a classic and feared complication of methanol poisoning.
- **Formic acid** specifically targets the **optic nerve** and retina, leading to **optic neuropathy** and permanent vision loss.
Alcohol Metabolism Indian Medical PG Question 8: Elimination of alcohol follows
- A. Zero order kinetics (Correct Answer)
- B. Third Order kinetics
- C. First order kinetics
- D. Second order kinetics
Alcohol Metabolism Explanation: ***Zero order kinetics***
- Alcohol is metabolized at a **constant rate** (approximately 7-10 grams per hour) regardless of its concentration in the body.
- This occurs because the metabolic enzymes like **alcohol dehydrogenase (ADH)** become **saturated** at blood alcohol concentrations typically achieved during drinking.
- A **fixed amount** of alcohol is eliminated per unit of time, not a fixed percentage.
- **Clinical significance**: This explains why you cannot speed up alcohol elimination by drinking coffee or taking cold showers.
*Third Order kinetics*
- This kinetic order is **not typically observed** for drug elimination in biological systems.
- It would imply an extremely complex relationship between concentration and elimination rate that is not seen in clinical pharmacology.
*First order kinetics*
- Most drugs follow **first-order kinetics**, where a **constant fraction** (percentage) of the drug is eliminated per unit of time.
- This occurs when enzyme systems are **not saturated**, which is **not the case** with alcohol at typical intoxicating doses.
- At very low blood alcohol concentrations (below enzyme saturation), alcohol may exhibit first-order kinetics.
*Second order kinetics*
- **Second-order kinetics** means the elimination rate is proportional to the **square of the drug concentration**.
- This type of kinetics is **rarely relevant** for drug elimination in pharmacology.
Alcohol Metabolism Indian Medical PG Question 9: A middle-aged male presented with a history of fatigue and tiredness. On investigation, he had a hemoglobin level of 8 g/dL and a mean corpuscular volume (MCV) of 110 fl, with the peripheral smear showing macrocytes and hypersegmented neutrophils. Which of the following is the most likely cause of these findings in this patient?
- A. Chronic alcohol use (Correct Answer)
- B. Ancylostoma duodenale infection
- C. Chronic kidney disease
- D. Colorectal cancer
Alcohol Metabolism Explanation: ***Chronic alcoholism***
- **Macrocytic anemia** with a **hemoglobin level of 8 g/dL** is commonly seen in chronic alcoholism due to impaired erythropoiesis and folate deficiency. [1]
- The **peripheral smear** showing **hypersegmented neutrophils** is indicative of megaloblastic anemia, often linked to **alcoholism**. [1]
*Chronic renal failure*
- Typically causes **normocytic anemia** due to inadequate erythropoietin production, not macrocytic anemia. [2]
- While uremic effects can impact erythropoiesis, they usually do not produce **hypersegmented neutrophils** found in megaloblastic anemia.
*Colon cancer*
- More commonly causes **microcytic anemia** due to **iron deficiency** from chronic blood loss rather than macrocytic anemia. [2]
- **Macrocytic anemia** with hypersegmented neutrophils would not be expected in most cases of colon cancer.
*Ancylostoma duodenale infestation*
- This hookworm infection typically leads to **microcytic anemia** due to **iron deficiency**, not macrocytic. [2]
- The presence of **macrocytes** and **hypersegmented neutrophils** does not correlate with this type of anemia.
Alcohol Metabolism Indian Medical PG Question 10: Which of the following enzymes is not classified as an oxidoreductase?
- A. Alcohol dehydrogenase
- B. Catalase
- C. Peroxidase
- D. Glucokinase (Correct Answer)
Alcohol Metabolism Explanation: ***Glucokinase***
- **Glucokinase** is a **transferase** enzyme that catalyzes the transfer of a phosphate group from ATP to glucose, forming glucose-6-phosphate.
- Its function is primarily in **glucose metabolism** and **insulin secretion**, not in oxidation or reduction reactions.
*Catalase*
- **Catalase** is an **oxidoreductase** that catalyzes the decomposition of **hydrogen peroxide** into water and oxygen.
- This reaction involves the **oxidation and reduction** of substrates, fitting the definition of an oxidoreductase.
*Alcohol dehydrogenase*
- **Alcohol dehydrogenase** is an **oxidoreductase** that catalyzes the interconversion between alcohols and aldehydes or ketones with the concomitant reduction and oxidation of **NAD+** to **NADH**.
- This enzyme is crucial in **detoxifying alcohol** by oxidizing it and is a classic example of an oxidoreductase.
*Peroxidase*
- **Peroxidase** is an **oxidoreductase** that catalyzes the oxidation of a substrate by **hydrogen peroxide**.
- Peroxidases work by using hydrogen peroxide to accept electrons from another molecule, thereby **oxidizing** that molecule.
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