L25 Medicinal Chemisty of Antihypertensives

Description

PHCY310 Quiz on L25 Medicinal Chemisty of Antihypertensives, created by Mer Scott on 14/04/2019.
Mer Scott
Quiz by Mer Scott, updated more than 1 year ago
Mer Scott
Created by Mer Scott over 5 years ago
6
0

Resource summary

Question 1

Question
The drugs that are Angiotensin II ‘blockers’ are thought to be AT1R antagonists.
Answer
  • True
  • False

Question 2

Question
Peptides are usually very specific and have [blank_start]high[blank_end] affinity for the target, but have [blank_start]poor[blank_end] chemical and biological stability, and so a [blank_start]short[blank_end] half life. They also have [blank_start]poor[blank_end] oral bioavailability.
Answer
  • high
  • low
  • poor
  • good
  • short
  • long
  • poor
  • good

Question 3

Question
Captopril was the first orally available ACE inhibitor. It was well known to cause taste disturbances. It contains a [blank_start]proline[blank_end] amino acid, and has two S [blank_start]stereocentres[blank_end], the same stereochemistry as the endogenous peptide. It contains a thiol because ACE is a zinc metalloenzyme, and the thiol group [blank_start]chelates[blank_end] very well to zinc. Multiple daily [blank_start]dosing[blank_end] requirements and side effects due to thiol drove further drug discovery.
Answer
  • proline
  • stereocentres
  • chelates
  • dosing

Question 4

Question
Enalaprilat was made when the sulfhydryl part of captopril was replaced with something else that fits well into the ACE ligand [blank_start]binding[blank_end] site and can chelate to a [blank_start]zinc[blank_end] ion. Enalaprilat is 10-fold more [blank_start]potent[blank_end] than captopril. To overcome the [blank_start]poor[blank_end] oral bioavailability of enalaprilat, the prodrug enalapril was made. Enalaprilat is converted by [blank_start]esterases[blank_end] (mostly in the liver) to enalaprilat.
Answer
  • binding
  • zinc
  • potent
  • poor
  • esterases

Question 5

Question
Most other carboxylate-based ACE inhibitors (e.g Cilazapril, perindopril, quinapril) also are prodrugs that have an ester which is hydrolysed to the active drug.
Answer
  • True
  • False

Question 6

Question
Using the endogenous ligand angiotensin as the structural starting point, angiotensin II receptor blockers were made. They are [blank_start]small molecules[blank_end] with similar key ligand-receptor contacts. They [blank_start]compete[blank_end] with angiotensin II and blocks it’s action. An example is [blank_start]losartan[blank_end]. An analogue prodrug of this is [blank_start]candesartan[blank_end] cilexetil. It is activated by [blank_start]ester[blank_end] hydrolysis which occurs during [blank_start]absorption[blank_end] from the GI tract. It is long [blank_start]acting[blank_end] –because of [blank_start]tight[blank_end] binding to AT1R and [blank_start]slow[blank_end] dissociation from the receptor.
Answer
  • small molecules
  • compete
  • losartan
  • candesartan
  • ester
  • absorption
  • acting
  • tight
  • slow

Question 7

Question
Calcium channel blockers act at L-type [blank_start]voltage[blank_end]-gated calcium channels. L-type are [blank_start]long[blank_end]-lasting, and large, and located in skeletal, cardiac and smooth muscle. The blockers [blank_start]bind[blank_end] to the α1 subunit. Most calcium channel blockers are dihydropyridines which have: - [blank_start]Phenyl ring[blank_end] at C4 - [blank_start]Esters[blank_end] at C3 and C5 - [blank_start]Electron withdrawing[blank_end] group Those funded in NZ are amlodipine, felodipine, isradipine, nifedipine, and nimodipine. All racemic except nifedapine.
Answer
  • long
  • voltage
  • bind
  • Phenyl ring
  • Esters
  • Electron withdrawing

Question 8

Question
Drugs that block the binding of adrenalin and noradrenalin to the adrenoceptors and do not act as agonists are AR blockers. - ‘First generation’ ARBs are non selective, acting on [blank_start]beta[blank_end] adrenoceptors, designed via [blank_start]chain[blank_end] extension of the endogenous agonist catecholamines. The catechol is [blank_start]replaced[blank_end] with an extended structure to reduce COMT metabolism. There is a [blank_start]linker/spacer[blank_end] added between the Ar and alcohol. A short length [blank_start]bulky[blank_end] group is added to the amine. An example is propanolol. - The 'second generation’ are [blank_start]selective[blank_end] for β1AR. All have functional groups off the phenyl ring, capable of [blank_start]hydrogen[blank_end] bonding. An example is metoprolol. - There are also α1-AR blockers indicated for hypertension, like prazosin. They have an [blank_start]extended[blank_end] chain with an [blank_start]Ar[blank_end] group.
Answer
  • beta
  • chain
  • replaced
  • linker/spacer
  • bulky
  • selective
  • hydrogen
  • extended
  • Ar

Question 9

Question
Thiazide diuretics block the Na+Cl- symporter, disallowing Na+ reabsorption and increasing urine output. They also cause arteriolar vasodilation. Structural requirements of the drugs: - [blank_start]electron withdrawing[blank_end] group at C-6 (ie Cl, CF3) - C-7 must be [blank_start]sulfonamide[blank_end] - C-3 [blank_start]lipophilic[blank_end] group, to increase in potency and duration of action (ie benzyl)
Answer
  • electron withdrawing
  • sulfonamide
  • lipophilic

Question 10

Question
Loop diuretics inhibit NKCC2 (the [blank_start]luminal[blank_end] Na/K/2Cl co-transporter) and cause a strong diuresis. They are meta-substituted sulfamoylbenzoic acids, meaning there is a [blank_start]sulfamoyl or sulfonamide[blank_end] group on one meta position of a ring and a [blank_start]benzoic[blank_end] acid on the opposite meta position. Note: [blank_start]Bumetanide[blank_end] is more potent than [blank_start]furosemide[blank_end].
Answer
  • luminal
  • sulfamoyl or sulfonamide
  • benzoic
  • Bumetanide
  • furosemide
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