NEET-PG 2012 — Pharmacology

93 Questions — Page 7 of 10

Q61

Which steroid has the maximum mineralocorticoid activity?

Q62

Which statin is considered most potent based on mg-to-mg LDL reduction capability?

Q63

Which of the following antiepileptic drugs is most classically associated with causing hirsutism?

Q64

What is the iodine content percentage in amiodarone?

Q65

Which of the following medications is known to cause increased renin levels with prolonged use?

Q66

Which of the following is NOT caused by Prostaglandin E2 (PGE2)?

Q67

Extrapyramidal syndrome-like side effects are seen in which of the following medications?

Q68

Which of the following is a selective progesterone receptor modulator?

Q69

Finasteride is classified as a:

Q70

What is the drug of choice for listeria meningitis?

NEET-PG 2012 - Pharmacology NEET-PG Practice Questions and MCQs

Question 61: Which steroid has the maximum mineralocorticoid activity?

A. Fludrocortisone (Correct Answer)
B. DOCA
C. Prednisolone
D. Triamcinolone

Explanation: ***Fludrocortisone*** - **Fludrocortisone** is a synthetic corticosteroid specifically designed to have potent **mineralocorticoid activity**, with significant sodium-retaining properties. - Its high affinity for **mineralocorticoid receptors** distinguishes it from other steroids and makes it effective in treating conditions like **Addison's disease** and **postural orthostatic tachycardia syndrome (POTS)** due to its ability to retain sodium and water. *DOCA (Deoxycorticosterone acetate)* - While **DOCA** does possess significant **mineralocorticoid activity** and was historically used for this purpose, **fludrocortisone** is generally considered to have a stronger and more sustained effect in clinical practice. - **DOCA's** mineralocorticoid potency is substantial but slightly less than that of **fludrocortisone** when compared on a weight basis for equivalent sodium retention. *Prednisolone* - **Prednisolone** is primarily a **glucocorticoid** with potent anti-inflammatory and immunosuppressive effects. - It has minimal to negligible **mineralocorticoid activity** and is not used for salt retention purposes. *Triamcinolone* - **Triamcinolone** is a potent **glucocorticoid** with a long duration of action and is known for its strong anti-inflammatory properties. - It has virtually no **mineralocorticoid activity**, making it unsuitable for conditions requiring sodium retention.

Question 62: Which statin is considered most potent based on mg-to-mg LDL reduction capability?

A. Simvastatin
B. Pravastatin
C. Rosuvastatin (Correct Answer)
D. Atorvastatin

Explanation: ***Rosuvastatin*** - **Rosuvastatin** is known for its high potency, achieving significant **LDL-C reduction** at relatively low doses. - It is often considered the most potent statin on a **milligram-to-milligram basis**. *Simvastatin* - **Simvastatin** is a moderate-intensity statin, not as potent as rosuvastatin or atorvastatin in reducing LDL-C. - While effective, it typically requires higher doses to achieve comparable **LDL-C reductions** seen with high-potency statins. *Pravastatin* - **Pravastatin** is a hydrophilic statin, generally considered to be of lower potency compared to other statins like rosuvastatin and atorvastatin. - It is often used in patients with **hepatic dysfunction** due to its different metabolic profile but offers less aggressive **LDL-C reduction**. *Atorvastatin* - **Atorvastatin** is a high-intensity statin, very effective in reducing LDL-C, and often used for aggressive lipid lowering. - While highly potent, **atorvastatin** is generally considered slightly less potent than **rosuvastatin** on a mg-to-mg basis, though both are used for high-intensity lipid therapy.

Question 63: Which of the following antiepileptic drugs is most classically associated with causing hirsutism?

A. Phenytoin (Correct Answer)
B. Valproate
C. Carbamazepine
D. Phenobarbitone

Explanation: ***Phenytoin*** - **Phenytoin** is the **most classically associated** antiepileptic drug with **hirsutism**, which is abnormal/excessive growth of hair [1]. - The mechanism involves changes in **androgen metabolism** and stimulation of hair follicle growth. - Other cosmetic side effects include **gingival hyperplasia** and **coarsening of facial features** [1].*Valproate* - Valproate can paradoxically cause both **hair loss (alopecia)** and **hirsutism**, particularly in women and children. - However, phenytoin has a **stronger and more classical association** with hirsutism. - Valproate is also known for **weight gain**, **hepatotoxicity**, **pancreatitis**, and **teratogenicity**.*Carbamazepine* - Carbamazepine's common side effects include **drowsiness**, **dizziness**, **diplopia**, and **hyponatremia**. - It is not classically linked to **hirsutism** as a prominent adverse effect. - Can cause **agranulocytosis** and **Stevens-Johnson syndrome** in rare cases.*Phenobarbitone* - Phenobarbitone is an older antiepileptic drug associated with **sedation**, **cognitive impairment**, and **dependence**. - It does not commonly cause **hirsutism**. - Also causes **enzyme induction** leading to multiple drug interactions.

Question 64: What is the iodine content percentage in amiodarone?

A. 10 - 20%
B. 20 - 40% (Correct Answer)
C. 40 - 60%
D. 60 - 80%

Explanation: ***20 - 40%*** - **Amiodarone** is highly lipophilic and contains a significant amount of **iodine**, typically comprising around **37.5%** of its molecular weight. - This high iodine content is responsible for many of its **adverse effects**, particularly those related to thyroid dysfunction. *10 - 20%* - This range is too low; the actual iodine content in **amiodarone** is considerably higher, making it a prominent feature of the drug's chemical structure. - A lower iodine percentage would likely result in fewer **thyroid-related side effects**. *40 - 60%* - While amiodarone has a high iodine content, 40-60% is slightly above the generally accepted range. - Iodine constitutes a substantial but not an overwhelming majority of the drug's molecular mass. *60 - 80%* - This range is significantly higher than the actual iodine content in **amiodarone**. - Such a high percentage would imply an even greater propensity for **iodine-induced adverse effects**.

Question 65: Which of the following medications is known to cause increased renin levels with prolonged use?

A. Clonidine
B. Enalapril (Correct Answer)
C. Methyldopa
D. Propranolol

Explanation: ***Enalapril*** - **Enalapril** is an **ACE inhibitor** which blocks the conversion of angiotensin I to angiotensin II, leading to decreased levels of angiotensin II [1]. - Reduced angiotensin II levels remove the **negative feedback** on renin release from the juxtaglomerular cells, thus increasing renin secretion [1], [2]. *Clonidine* - Clonidine is a **central alpha-2 adrenergic agonist** that reduces sympathetic outflow from the central nervous system. - This reduction in sympathetic activity leads to a **decrease in renin release**, as sympathetic stimulation normally promotes renin secretion [3]. *Methyldopa* - Methyldopa is a **central alpha-2 adrenergic agonist** that works similarly to clonidine by reducing sympathetic tone. - It consequently causes a **decrease in plasma renin activity** due to reduced sympathetic stimulation of the juxtaglomerular apparatus [3]. *Propranolol* - Propranolol is a **non-selective beta-blocker** that blocks beta-1 receptors in the juxtaglomerular cells of the kidney. - This blockade **inhibits the release of renin** stimulated by sympathetic activity, leading to reduced renin levels [3].

Question 66: Which of the following is NOT caused by Prostaglandin E2 (PGE2)?

A. None of the options (Correct Answer)
B. Water retention
C. Flushing
D. Uterine contraction

Explanation: ***None of the options*** - All three listed effects (water retention, uterine contraction, and flushing) **ARE caused by Prostaglandin E2 (PGE2)**, making this the correct answer to the question asking what is NOT caused by PGE2. - Since PGE2 actually causes all the listed effects, "None of the options" is the accurate response. *Water retention* - PGE2 **stimulates ADH (vasopressin) release** from the posterior pituitary gland. - PGE2 also **enhances ADH action** on renal collecting ducts, promoting water reabsorption. - While PGE2 has complex renal effects including natriuresis, its net effect includes **promoting water retention** through the ADH mechanism. - This is an important effect of PGE2 on fluid balance. *Uterine contraction* - PGE2 is a **potent stimulator of uterine smooth muscle contraction**. - It is used clinically for **labor induction** and **cervical ripening** (dinoprostone). - PGE2 plays a crucial role in **parturition** and is involved in **dysmenorrhea**. *Flushing* - PGE2 causes **peripheral vasodilation**, particularly in cutaneous blood vessels. - This vasodilatory effect leads to **increased skin blood flow**, manifesting as **flushing** and warmth. - This is commonly seen as part of the **inflammatory response** and contributes to erythema.

Question 67: Extrapyramidal syndrome-like side effects are seen in which of the following medications?

A. Haloperidol (Correct Answer)
B. Clozapine
C. Tetracycline
D. Ketoconazole

Explanation: ***Haloperidol*** - **Haloperidol** is a **typical antipsychotic** known for its potent **dopamine D2 receptor blockade**. - This strong blockade in the **nigrostriatal pathway** often leads to **extrapyramidal symptoms (EPS)** such as dystonia, akathisia, and parkinsonism. *Clozapine* - **Clozapine** is an **atypical antipsychotic** that has a lower propensity for causing **extrapyramidal symptoms (EPS)** due to its weaker D2 receptor antagonism and potent serotonin 5-HT2A receptor blockade. - While it can cause other severe side effects, such as **agranulocytosis** and **myocarditis**, EPS are less common compared to typical antipsychotics. *Tetracycline* - **Tetracycline** is an **antibiotic** primarily used to treat bacterial infections. - Its mechanism of action involves inhibiting bacterial protein synthesis, and it is not associated with **neurological side effects** like **extrapyramidal symptoms**. *Ketoconazole* - **Ketoconazole** is an **antifungal medication** that works by inhibiting ergosterol synthesis in fungi. - It is known for potential **hepatotoxicity** and **endocrine dysfunction**, but not for causing **extrapyramidal symptoms**.

Question 68: Which of the following is a selective progesterone receptor modulator?

A. Onapristone
B. Ulipristal (Correct Answer)
C. Nomegestrol
D. Toremifene

Explanation: ***Ulipristal*** - **Ulipristal acetate** is a **selective progesterone receptor modulator (SPRM)** that acts as a progesterone receptor agonist/antagonist. - It is primarily used for **emergency contraception** and for the pre-operative treatment of **uterine fibroids**. *Onapristone* - **Onapristone** is an **antiprogestin** and a **progesterone receptor antagonist**, not a selective modulator. - It has been primarily investigated for its potential role in **breast cancer** treatment but is not approved for general clinical use. *Nomegestrol* - **Nomegestrol** is a **synthetic progestin** used in hormonal contraception. - It functions as a **progesterone receptor agonist** and does not exhibit selective modulation properties. *Toremifene* - **Toremifene** is a **selective estrogen receptor modulator (SERM)**, not a progesterone receptor modulator. - It is used in the treatment of **estrogen receptor-positive metastatic breast cancer** in postmenopausal women.

Question 69: Finasteride is classified as a:

A. 5-alpha reductase inhibitor (Correct Answer)
B. Phosphodiesterase inhibitor
C. Alpha-1 blocker
D. Androgen receptor antagonist

Explanation: ### ***5-alpha reductase inhibitor*** - **Finasteride** specifically inhibits the enzyme **5-alpha reductase**, preventing the conversion of **testosterone** to **dihydrotestosterone (DHT)** [2], [4]. - This reduction in DHT is clinically useful for treating conditions like **benign prostatic hyperplasia (BPH)** and **androgenetic alopecia** [4]. ### *Phosphodiesterase inhibitor* - **Phosphodiesterase inhibitors** (e.g., sildenafil) typically work by increasing levels of **cyclic GMP**, leading to **vasodilation** and are used for **erectile dysfunction** [3]. - Their mechanism of action is distinct from finasteride's effect on **hormone metabolism**. ### *Alpha-1 blocker* - **Alpha-1 blockers** (e.g., tamsulosin) primarily relax **smooth muscle** in the prostate and bladder neck, improving **urine flow** in BPH [3], [5]. - They act on **adrenergic receptors** and do not affect **hormone synthesis** or **metabolism** [3]. ### *Androgen receptor antagonist* - **Androgen receptor antagonists** (e.g., flutamide) directly block the binding of **androgens** (like testosterone and DHT) to their receptors [1], [4]. - While they also affect androgen action, their mechanism is different from finasteride's **enzyme inhibition** [4].

Question 70: What is the drug of choice for listeria meningitis?

A. Ampicillin (Correct Answer)
B. Cefotaxime
C. Ciprofloxacin
D. Ceftriaxone

Explanation: ***Ampicillin*** - **Ampicillin** is the **drug of choice** for *Listeria monocytogenes* meningitis due to its excellent in vitro activity and good central nervous system penetration. - It is often used in combination with an **aminoglycoside** (e.g., gentamicin) for synergistic bactericidal activity, especially in severe cases, though gentamicin does not penetrate the CSF well. *Cefotaxime* - **Third-generation cephalosporins** like cefotaxime have poor activity against *Listeria monocytogenes* due to the organism's intrinsic resistance to these agents. - While effective against many other bacterial causes of meningitis (e.g., *S. pneumoniae*, *N. meningitidis*), it is not appropriate for *Listeria*. *Ceftriaxone* - Similar to cefotaxime, **ceftriaxone** is a third-generation cephalosporin and is **ineffective** against *Listeria monocytogenes* due to the lack of penicillin-binding protein (PBP) affinity. - Its use for *Listeria* meningitis would lead to treatment failure. *Ciprofloxacin* - **Ciprofloxacin**, a fluoroquinolone, is generally **not recommended** as a first-line treatment for *Listeria* meningitis, despite some in vitro activity. - Its use is typically reserved for patients with severe allergies to penicillins, and even then, **trimethoprim-sulfamethoxazole** is usually preferred as an alternative to ampicillin.