Protein Synthesis Inhibitors Classification and Mechanisms

Phloston
Protein synthesis inhibitors

30S and 50S inhibitors

30S = aminoglycosides + tetracyclines

30S = aminoglycosides + tetracyclines 50S = chloramphenicol + clindamycin + macrolides
(and linezolid = lower-yield, but in FA)

(and linezolid = lower-yield, but in FA) Knowing the above classifications is mandatory.

(and linezolid = lower-yield, but in FA) Knowing the above classifications is mandatory. However the USMLE is going to throw buzz words at you for these, so you need to know their individual MOAs.

Before I get into the specifics of each drug, here are the
buzz words you need to associate with the 50S drugs:

buzz words you need to associate with the 50S drugs: Macrolides = BLOCK TRANSLOCATION STEP via binding to the 23S rRNA of the 50S subunit.

buzz words you need to associate with the 50S drugs: Macrolides = BLOCK TRANSLOCATION STEP via binding to the 23S rRNA of the 50S subunit. FA says chloramphenicol and clindamycin both block peptide bond formation, but in terms of the USMLE, theyre going to want you to know that chloramphenicol more specifically blocks peptidyl transferase. For clindamycin, it blocks peptide bond formation. Thats how its seen in questions.

For the 30S buzzwords:

Aminoglycosides = disrupt initiation complex and
cause misreading of mRNA.

Aminoglycosides = disrupt initiation complex and
cause misreading of mRNA. Tetracyclines = prevent attachment of aminoacyltRNA to the A-site on the 30S.
Aminoglycosides vs macrolides (names)

Gentamycin, neomycin, amikacin, tobramycin,
steptomycin (highest-yield ones) = AMINOGLYCOSIDES

steptomycin (highest-yield ones) = AMINOGLYCOSIDES Erythromycin, azithromycin, clarithromycin = MACROLIDES

steptomycin (highest-yield ones) = AMINOGLYCOSIDES Erythromycin, azithromycin, clarithromycin = MACROLIDES When you see these drug names enough through doing lots of practice questions, you soon wont have to think twice about their classifications, but at the very minimum, dont screw these up. I had an easy question my real deal where I had to pick out the aminoglycoside, and they had also listed a macrolide.
Bactericidal vs bacteristatic
Youve gotta know which protein synthesis inhibitors
are bactericidal vs static.
are bactericidal vs static. The 50S ones alone are BACTERISTATIC. That means the macrolides and chloramphenicol + clindamycin are BACTERISTATIC.
are bactericidal vs static. The 50S ones alone are BACTERISTATIC. That means the macrolides and chloramphenicol + clindamycin are BACTERISTATIC. Of the 30S, tetracyclines are BACTERISTATIC, but aminoglycosides are BACTERICIDAL.
are bactericidal vs static. The 50S ones alone are BACTERISTATIC. That means the macrolides and chloramphenicol + clindamycin are BACTERISTATIC. Of the 30S, tetracyclines are BACTERISTATIC, but aminoglycosides are BACTERICIDAL. Tangential: TMP and SMX, individually, are bacteristatic. But TOGETHER THEY ARE BACTERICIDAL.
Aminoglycosides
As said before, these inhibit formation of the
initiation complex and cause misreading of the mRNA.
Aminoglycosides
initiation complex and cause misreading of the mRNA. Target AEROBIC GRAM-NEGATIVE RODS.
Aminoglycosides
initiation complex and cause misreading of the mRNA. Target AEROBIC GRAM-NEGATIVE RODS. Therefore require O2 for uptake.
Aminoglycosides
initiation complex and cause misreading of the mRNA. Target AEROBIC GRAM-NEGATIVE RODS. Therefore require O2 for uptake. Synergistic with beta-lactams (beta-lactams permit the aminoglycoside to enter the cell)
Aminoglycosides

initiation complex and cause misreading of the mRNA. Target AEROBIC GRAM-NEGATIVE RODS. Therefore require O2 for uptake. Synergistic with beta-lactams (beta-lactams permit the aminoglycoside to enter the cell) Neomycin is used for bowel surgery
Aminoglycosides
Nephrotoxic with cephalosporins and ototoxic with
loop diuretics. I remembered this through ALOe. I thought of aloe vera Aminoglycosides, Loops, Ototoxicity; so that leaves nephrotoxicity for cephs + aminos.
Aminoglycosides
Nephrotoxic with cephalosporins and ototoxic with
loop diuretics. I remembered this through ALOe. I thought of aloe vera Aminoglycosides, Loops, Ototoxicity; so that leaves nephrotoxicity for cephs + aminos. FA also mentions that its a teratogen. USMLE wants you to know that aminoglycosides can cause congenital deafness. FA (in the embryo chapter) mentions CNVIII toxicity for aminoglycosides.
Aminoglycosides
Resistance is via acetylation, phosphorylation,
adenylation. Sounds low-yield, but its in FA, and Ive seen it in two practice questions (perfect example of a 260+ question bc most people wont make the effort to remember that).
Aminoglycosides (beyond FA)

All of the following has rocked up in questions:

Can only be given PARENTERALLY

Can only be given PARENTERALLY Can also be given with nafcillin for MRSA endocarditis
(remember beta-lactam synergy?)

Can only be given PARENTERALLY Can also be given with nafcillin for MRSA endocarditis
(remember beta-lactam synergy?) Neomycin for bowel surgery, right? Well it also kills urease(+) organisms decreased NH3 production decreased NH3 absorption = Tx for hyperammonaemia. FA mentions lactulose for NH3 and the gut, but they dont mention neomycin.

Contraindicated in myasthenia gravis because it can
cause excessive neuromuscular blockade when used with curariform drugs (curare is a neuromuscular blocking agent at nAChR).

cause excessive neuromuscular blockade when used with curariform drugs (curare is a neuromuscular blocking agent at nAChR). Any kidney damage via aminoglycosides, in terms of USMLE questions, is ATN. They might try to trick you with tubulointerstitial nephritis, but its always ATN.

cause excessive neuromuscular blockade when used with curariform drugs (curare is a neuromuscular blocking agent at nAChR). Any kidney damage via aminoglycosides, in terms of USMLE questions, is ATN. They might try to trick you with tubulointerstitial nephritis, but its always ATN. Ampicillin + gentamycin = 1st-line Tx for severe pyelonephritis.
Tetracyclines
Like aminoglycosides, 30S, and as said before, they
prevent aminoacyl-tRNA binding to the A-site.
Tetracyclines
prevent aminoacyl-tRNA binding to the A-site. Doxycycline is eliminated through feces. Good in pts with renal insufficiency. Theyll ask you that. They also want you to know that its ideal Tx for Lyme disease.
Tetracyclines
prevent aminoacyl-tRNA binding to the A-site. Doxycycline is eliminated through feces. Good in pts with renal insufficiency. Theyll ask you that. They also want you to know that its ideal Tx for Lyme disease. Cant take tetracyclines with antacids. The same thing goes for fluoroquinolones. Ive seen both in questions.
Tetracyclines
Causes teeth discoloration IN CHILDREN and
photosensitivity IN ADULTS. guy gets sunburn while on vacation, which drug.. or girl gets sunburn/blisters while being treated for STD (gotta know Chlamydia)
Tetracyclines
photosensitivity IN ADULTS. guy gets sunburn while on vacation, which drug.. or girl gets sunburn/blisters while being treated for STD (gotta know Chlamydia) VACUUM THe BedRoom vibrio, acne, chlamydia, ureaplasma urealyticum, mycoplasma, tularaemia, H. pylori, Borellia (Lyme disease), Rickettsia rickettsii.
Tetracyclines
photosensitivity IN ADULTS. guy gets sunburn while on vacation, which drug.. or girl gets sunburn/blisters while being treated for STD (gotta know Chlamydia) VACUUM THe BedRoom vibrio, acne, chlamydia, ureaplasma urealyticum, mycoplasma, tularaemia, H. pylori, Borellia (Lyme disease), Rickettsia rickettsii. Resistance mechanism is increased efflux or reduced influx. Contrast with aminoglycosides.
Tetracyclines (beyond FA)

MINOCYCLINE, like doxycycline, is also fecally
eliminated. Minocycline, like HIPP, can cause SLElike syndrome.

eliminated. Minocycline, like HIPP, can cause SLElike syndrome. Tetracyclines can cause pill-induced esophagitis.

eliminated. Minocycline, like HIPP, can cause SLElike syndrome. Tetracyclines can cause pill-induced esophagitis. Not good for meningitis because they dont cross the BBB (FA vaguely mentions limited CNS penetration)

eliminated. Minocycline, like HIPP, can cause SLElike syndrome. Tetracyclines can cause pill-induced esophagitis. Not good for meningitis because they dont cross the BBB (FA vaguely mentions limited CNS penetration) Demeclocycline causes diabetes insipidus (FA says it probably in the renal chapter but not in the micro chapter, although its ridiculously high-yield)
Macrolides
Once again, they block translocation via binding to
the 23S rRNA. (elaborate)
Macrolides
the 23S rRNA. (elaborate) Ultra-high-yield: Tx for ATYPICAL PNEUMONIAS.
Macrolides
the 23S rRNA. (elaborate) Ultra-high-yield: Tx for ATYPICAL PNEUMONIAS. Prolongs the QT-interval (FA says erythromycin)
Macrolides
the 23S rRNA. (elaborate) Ultra-high-yield: Tx for ATYPICAL PNEUMONIAS. Prolongs the QT-interval (FA says erythromycin) DOC for pneumonia in penicillin-allergenic pts keep in mind we have aztreonam, so why use a macrolide?
Macrolides

the 23S rRNA. (elaborate) Ultra-high-yield: Tx for ATYPICAL PNEUMONIAS. Prolongs the QT-interval (FA says erythromycin) DOC for pneumonia in penicillin-allergenic pts keep in mind we have aztreonam, so why use a macrolide? GI-discomfort, cholestatic hepatitis, eosinophilia/rash; inhibits P-450. bleeding diathesis in heart valve pt.
Macrolides
Resistance is alteration of the 23S rRNA binding site
Macrolides (beyond FA)

The reason erythromycin causes acute cholestatic
hepatitis is because its the only macrolide eliminated through bile (USMLE would simply ask you for the mechanism of elimination, but if you remember it causes cholestatic hepatitis, it would be easy).

hepatitis is because its the only macrolide eliminated through bile (USMLE would simply ask you for the mechanism of elimination, but if you remember it causes cholestatic hepatitis, it would be easy). Because erythromycin is eliminated through bile, it also is the only macrolide that doesnt require dosage adjustment in renal failure pts.

hepatitis is because its the only macrolide eliminated through bile (USMLE would simply ask you for the mechanism of elimination, but if you remember it causes cholestatic hepatitis, it would be easy). Because erythromycin is eliminated through bile, it also is the only macrolide that doesnt require dosage adjustment in renal failure pts. Macrolides are DOC if pt also has post-operative ileus because they are agonists at the motilin receptor (MMCs).

Ive seen in a practice question where they wanted to
know which drug was most injurious to myocytes. Macrolides was the answer (although protein synthesis inhibitors in general would also be correct). The rationale is that although eukaryotes have 40S/60S (80S) ribosomes, because mitochondria are derived from prokaryotes, they have 30S/50S (70S) ribosomal systems, so muscle, which is heavily mitochondriadependent, can theoretically be injured by protein synthesis inhibitors.
Macrolides vs tetracyclines
I had seen in a practice question that a pt had an
atypical pneumonia and then developed severe sunburn on vacation. They had asked which drug was used. Youve gotta know that atypical pneumonias are classically mycoplasma, chlamydia or legionella. And youve gotta remember that despite macrolides serving as the 1st-line Tx for atypical pneumonias, tetracyclines treat chlamydia, so in this case, the guy had had an atypical chlamydial pneumonia treated with a tetracycline, and he developed photosensitivity.
Chloramphenicol
Blocks peptide bond formation, but if you see it in a
question, they want you to know that it knocks out peptidyl transferase.
Chloramphenicol
question, they want you to know that it knocks out peptidyl transferase. In turn, resistance is via a plasmid-encoded acetyltransferase that inactivates the drug (FA says this, but on the USMLE, theyll reword it as bacterial enzymatic acetylation to see if you actually know what acetyltransferase means).
Chloramphenicol
question, they want you to know that it knocks out peptidyl transferase. In turn, resistance is via a plasmid-encoded acetyltransferase that inactivates the drug (FA says this, but on the USMLE, theyll reword it as bacterial enzymatic acetylation to see if you actually know what acetyltransferase means). Causes aplastic anaemia and grey baby syndrome
Chloramphenicol
Used commonly to treat meningitis in the third-
world because of its cheap cost
Chloramphenicol (beyond FA)

Kaplan liked chloramphenicol as Tx for Lyme disease
in early pregnancy > doxycycline. However, if near term, doxy is > chloramphenicol. Both drugs carry fetal risks.
Chloramphenicol (beyond FA)

Kaplan liked chloramphenicol as Tx for Lyme disease
in early pregnancy > doxycycline. However, if near term, doxy is > chloramphenicol. Both drugs carry fetal risks. USMLE will ask you to pick out the most lipophilic drug of the bunch. Chloramphenicol, bc its great for meningitis due to its BBB penetration, is heavily lipophilic.
Clindamycin
Blocks peptide bond formation
Clindamycin
Anaerobic infections ABOVE the diaphragm
(metronidazole is below)
Clindamycin
(metronidazole is below) Good for lung abscesses or aspiration pneumonia
Clindamycin
(metronidazole is below) Good for lung abscesses or aspiration pneumonia Causes pseudomembranous colitis bc it allows for C. difficile overgrowth
Clindamycin
Only real thing Ive found outside FA for this drug is
that it can also treat MRSA. Or theyll make pseudomembranous colitis apparent then ask you for the AB-toxin test or MOA of C. difficile-mediated necrosis.
Linezolid
For this drug, you only need to remember two things:
Linezolid
1) it acts on the 50S subunit (binds to 23S of 50S
subunit - same as macrolides/clindamycin)
Linezolid
subunit - same as macrolides/clindamycin) 2) Side-effects are HOT:
Linezolid
subunit - same as macrolides/clindamycin) 2) Side-effects are HOT: H = High risk of serotonin syndrome
Linezolid
subunit - same as macrolides/clindamycin) 2) Side-effects are HOT: H = High risk of serotonin syndrome O = optic neuritis
Linezolid
subunit - same as macrolides/clindamycin) 2) Side-effects are HOT: H = High risk of serotonin syndrome O = optic neuritis T = thrombocytopenia
Linezolid
subunit - same as macrolides/clindamycin) 2) Side-effects are HOT: H = High risk of serotonin syndrome O = optic neuritis T = thrombocytopenia
Linezolid
I had only ever encountered one question on this drug,
and it was a vignette of someone with serotonin syndrome (flushing, diarrhea, sweating, hyperthermia, agitation, etc.) and blurry vision, and then they wanted to know the drug that caused the Sx.
Sulfonamides vs trimethoprim
Sulfonamides vs trimethoprim
Sulfadiazine + pyrimethamine used to Tx
toxoplasmosis are analogous. So if they ask you for the MOA of pyrimethamine, you know its like trimethoprim.
Sulfonamides
Dihydropteroate synthase inhibitors (PABA analogues)
Sulfonamides
Simple UTIs
Sulfonamides
Simple UTIs Can treat Nocardia (SNAP)
Sulfonamides
Can treat Chlamydia, as per FA, but Ive never seen this
in a practice question
Sulfonamides
in a practice question Can cause hypersensitivity rxns (tubulointersititial nephritis; in contrast to aminoglycosides ATN)
Sulfonamides
in a practice question Can cause hypersensitivity rxns (tubulointersititial nephritis; in contrast to aminoglycosides ATN) Haemolysis in G6PD-deficiency (ISPAIN)
Sulfonamides
in a practice question Can cause hypersensitivity rxns (tubulointersititial nephritis; in contrast to aminoglycosides ATN) Haemolysis in G6PD-deficiency (ISPAIN) Displaces drugs from albumin kernicterus
Sulfonamides (beyond FA)

So if a pregnant woman takes a drug and the baby has
jaundice kernicterus sulfonamide.
Sulfonamides (beyond FA)

So if a pregnant woman takes a drug and the baby has
jaundice kernicterus sulfonamide. Because the bilirubin is displaced from albumin, it can cross the BBB kernicterus
Trimethoprim
Inhibits dihydrofolate reductase
Trimethoprim
Once again, sulfonamides and trimethoprim are both
BACTERISTATIC, but if combined (TMP-SMX), they are BACTERICIDAL.
Trimethoprim
BACTERISTATIC, but if combined (TMP-SMX), they are BACTERICIDAL. Highest-yield for TMP-SMX is Pneumocystis jiroveci pneumonia. If high-yield were diarrhea, it would be explosive here.
Trimethoprim
BACTERISTATIC, but if combined (TMP-SMX), they are BACTERICIDAL. Highest-yield for TMP-SMX is Pneumocystis jiroveci pneumonia. If high-yield were diarrhea, it would be explosive here. Can Tx SALMONELLA and SHIGELLA
Trimethoprim
BACTERISTATIC, but if combined (TMP-SMX), they are BACTERICIDAL. Highest-yield for TMP-SMX is Pneumocystis jiroveci pneumonia. If high-yield were diarrhea, it would be explosive here. Can Tx SALMONELLA and SHIGELLA May cause megaloblastic anaemia or (or any penia).
Trimethoprim
May alleviate TMP-induced megaloblastic anaemia
with leucovorin rescue folinic acid
Trimethoprim
May alleviate TMP-induced megaloblastic anaemia
with leucovorin rescue folinic acid As stated before, remember the pyrimethamine for toxoplasmosis has same MOA
Fluoroquinolones
-floxacin drugs; inhibit bacterial topoisomerase II
(aka DNA gyrase) very very high-yield
Fluoroquinolones
(aka DNA gyrase) very very high-yield Like tetracyclines, cannot be taken with antacids
Fluoroquinolones
(aka DNA gyrase) very very high-yield Like tetracyclines, cannot be taken with antacids Can treat a range of organisms (mostly gram(-) rods)
Fluoroquinolones
(aka DNA gyrase) very very high-yield Like tetracyclines, cannot be taken with antacids Can treat a range of organisms (mostly gram(-) rods) Can cause cartilage damage or tendon rupture
Fluoroquinolones

(aka DNA gyrase) very very high-yield Like tetracyclines, cannot be taken with antacids Can treat a range of organisms (mostly gram(-) rods) Can cause cartilage damage or tendon rupture Leg cramps + myalgias in kids (as per FA, but Ive never seen this in a practice question)
Fluoroquinolones
Bacterial resistance is via chromosome-mediated
mutation in DNA gyrase. FA mentions this, but its not minutiae. Ive seen in a couple questions where they want you to know that bacterial resistance is ALMOST ALWAYS plasmid-mediated, but fluoros are the exception because theyre chromosomal.
Fluoroquinolones (beyond FA)

First-line Tx for diarrhea due to Shigella + travelers
diarrhea

diarrhea Ciprofloxacin is DOC for UTIs in pts with sulfa allergy. If pt has sulfa allergy and has GERD nitrofurantoin

diarrhea Ciprofloxacin is DOC for UTIs in pts with sulfa allergy. If pt has sulfa allergy and has GERD nitrofurantoin Kaplan liked that H. influenzae can also be treated by fluoros.

diarrhea Ciprofloxacin is DOC for UTIs in pts with sulfa allergy. If pt has sulfa allergy and has GERD nitrofurantoin Kaplan liked that H. influenzae can also be treated by fluoros. GOOD ORAL BIOAVAILABILITY. That rocked up on an NBME exam (Gd knows why), which means it was once (or still is) floating around on the real deal.

Gatifloxacin causes dysglycaemia (rocked up in GT)

Moxifloxacin causes heart conduction abnormalities

Moxifloxacin causes heart conduction abnormalities USMLE might try to re-word the MOA as that which
affects the DNA nicking process
Metronidazole
Forms toxic metabolites that damage DNA
Metronidazole
GET GAP Tx for Giardia, Entamoeba, Trichomonas,
Gardnerella vaginalis, Anaerobes, H. pylori
Metronidazole
GET GAP Tx for Giardia, Entamoeba, Trichomonas,
Gardnerella vaginalis, Anaerobes, H. pylori USMLE will literally give you a classic vignette / presentation of one of the above organisms, then ask for the Tx. They might tell you clue cells, for instance, then ask for the Tx, or theyll tell you a guy went swimming in a lake and now has steatorrhoea, then ask for the Tx, etc.
Metronidazole
Disulfiram-like rxn with EtOH headache /
metallic taste in the mouth
Metronidazole
Disulfiram-like rxn with EtOH headache /
metallic taste in the mouth Once again, clindamycin = anaerobes ABOVE diaphragm; metronidazole = BELOW
Metronidazole (beyond FA)

FA doesnt say it for metro at the end of the micro
chapter, although it does under C. difficile, but metronidazole is a TREATMENT FOR pseudomembranous colitis. Vancomycin and metro are both Txs for it, but if a question has both as answer choices, metro is always correct > vancomycin because of the scare of vancomycin-resistant organisms. Another thing: vanco is always given IV (poor oral bioavailability), but for pseudomembranous colitis, ITS GIVEN ORALLY (makes sense bc it stays confined to the gut).
Metronidazole (beyond FA)

Ive also seen it in a practice question: USMLE likes
metronidazole CREAM as Tx for acne rosacea. But erythromycin CREAM is Tx for acne vulgaris.
Polymyxins
USMLE for some reason likes you to know the
structures/MOA of these drugs really well. Know that they have a long hydrophobic tail and that they are cationic and basic. They act as detergents on the cell membrane and DISRUPT ITS OSMOTIC PROPERTIES.
Polymyxins
USMLE for some reason likes you to know the
structures/MOA of these drugs really well. Know that they have a long hydrophobic tail and that they are cationic and basic. They act as detergents on the cell membrane and DISRUPT ITS OSMOTIC PROPERTIES. Theyre used only when a pt is resistant to practically all other Txs very high neuro- and nephrotoxicity
Polymyxins
Youll find them in the THAYER-MARTIN medium
used to culture N. gonorrhea. TM medium = VPN client = vancomycin (hits gram+), Polymyxin = colistin (hits other gram-), nystatin (hits fungi)
Daptomycin
Dont be fooled by the name. Its not an
aminoglycoside, nor is it a macrolide.
Daptomycin
aminoglycoside, nor is it a macrolide. Youve gotta know that it creates membrane channels that result in depolarization and **disruption of the membrane potential.**
Daptomycin
aminoglycoside, nor is it a macrolide. Youve gotta know that it creates membrane channels that result in depolarization and **disruption of the membrane potential.** Its notable side-effect is myopathy with increased CPK (so contraindicated with statins/fibrates)
Daptomycin
aminoglycoside, nor is it a macrolide. Youve gotta know that it creates membrane channels that result in depolarization and **disruption of the membrane potential.** Its notable side-effect is myopathy with increased CPK (so contraindicated with statins/fibrates) It is only effective against gram(+)s.
Daptomycin
aminoglycoside, nor is it a macrolide. Youve gotta know that it creates membrane channels that result in depolarization and **disruption of the membrane potential.** Its notable side-effect is myopathy with increased CPK (so contraindicated with statins/fibrates) It is only effective against gram(+)s. Cannot be used for pneumonia bc pulmonary surfactant inhibits it.
Anti-TB drugs
Anti-TB drugs
Prophylaxis = isoniazid. High-yield.
Anti-TB drugs
Tx = RIPE = rifampin, isoniazid, pyrazinamide,
ethambutol
Anti-TB drugs
Tx = RIPE = rifampin, isoniazid, pyrazinamide,
ethambutol All are HEPATOTOXIC, except for ethambutol, which causes VISUAL CHANGES.
Rifampin
Inhibits DNA-dependent RNA-polymerase. USMLE
really likes that. And theyll really nail it. Theyll literally list RNA-dependent DNA-polymerase and other types of similar polymerases to trick you, but you need to remember that rifampin inhibits DNAdependent RNA-polymerase. That means it prevents RNA synthesis. The way I remembered this was RDR = rifampin-DNA-RNA. Whatever works for you. Just find a way to remember it.
Rifampin
FA says that rifampin delays resistance to dapsone
when used for leprosy. Ive never actually seen a question on this though.
Rifampin
when used for leprosy. Ive never actually seen a question on this though. As said prior, isoniazid, NOT rifampin, is the prophylaxis for TB. But you need to remember that rifampin is the prophylaxis for N. meningitidis and H. influenzae type-B.
Rifampin
when used for leprosy. Ive never actually seen a question on this though. As said prior, isoniazid, NOT rifampin, is the prophylaxis for TB. But you need to remember that rifampin is the prophylaxis for N. meningitidis and H. influenzae type-B. Ill summarize that last point bc its so important:
TB prophylaxis = isoniazid
TB Tx = rifampin, isoniazid, pyrazinamide, ethambutol N. meningitidis / H. influenzae prophylaxis =
rifampin N. meningitidis Tx = ceftriaxone (FA says ceftriaxone or penicillin G, but in terms of USMLE questions, Ive only ever seen ceftriaxone)
Rifampin (contd)
Upregulates P-450 (very high-yield)
Rifampin (contd)
Upregulates P-450 (very high-yield)
Can cause orange tears/sweat/urine (high-yield);
harmless side-effect, but pt will be concerned
Rifampin (beyond FA)

Since rifampin upregulates P-450, you dont want to
give it to HIV pts on protease inhibitors bc youll increase the rate of the latters degradation, so you instead give rifabutin. USMLE will list both as Txs for TB in the same question, but the answer is rifabutin if the pt is HIV(+) bc you need to assume he/she is on HAART.

give it to HIV pts on protease inhibitors bc youll increase the rate of the latters degradation, so you instead give rifabutin. USMLE will list both as Txs for TB in the same question, but the answer is rifabutin if the pt is HIV(+) bc you need to assume he/she is on HAART. USMLE wants to know WHY rifampin is prophylaxis for N. meningitidis.

give it to HIV pts on protease inhibitors bc youll increase the rate of the latters degradation, so you instead give rifabutin. USMLE will list both as Txs for TB in the same question, but the answer is rifabutin if the pt is HIV(+) bc you need to assume he/she is on HAART. USMLE wants to know WHY rifampin is prophylaxis for N. meningitidis. ..it penetrates the respiratory tract wall and prevents meningococcal pharyngeal colonization.

Rifampin binds the beta-subunit of DNA-dependent
RNA-polymerase. Retarded, but it showed up in a question (lord knows why). This is an example of how everyone needs a little luck on the real deal.

RNA-polymerase. Retarded, but it showed up in a question (lord knows why). This is an example of how everyone needs a little luck on the real deal. USMLE might tell you the pts contact lenses were rusty colored as an indirect reference to the orange tears a little trickier

RNA-polymerase. Retarded, but it showed up in a question (lord knows why). This is an example of how everyone needs a little luck on the real deal. USMLE might tell you the pts contact lenses were rusty colored as an indirect reference to the orange tears a little trickier Why is isoniazid used over rifampin for TB prophylaxis?

RNA-polymerase. Retarded, but it showed up in a question (lord knows why). This is an example of how everyone needs a little luck on the real deal. USMLE might tell you the pts contact lenses were rusty colored as an indirect reference to the orange tears a little trickier Why is isoniazid used over rifampin for TB prophylaxis? ..bc rifampin is way more hepatotoxic.
Isoniazid (INH)
Decreases synthesis of mycolic acids (high-yield)
Isoniazid (INH)
KatG (catalase-peroxidase) needed to convert INH
to active metabolite
Isoniazid (INH)
to active metabolite Although hepatotoxic, USMLE loves that INH is a common cause of vitamin B6 deficiency. Quite HY.
Isoniazid (INH)
to active metabolite Although hepatotoxic, USMLE loves that INH is a common cause of vitamin B6 deficiency. Quite HY. Theyll tell you a person with TB was treated and now has paresthesias (or sometimes seizures) B6 def.
Isoniazid (beyond FA)

KatG needed to convert INH to active metabolite does
so via acyl-carrier and ketoacyl-carrier protein synthesis. So KatG is a catalase-peroxidase enzyme that carries out acyl-carrier and ketoacyl-carrier protein synthesis.

KatG needed to convert INH to active metabolite does
so via acyl-carrier and ketoacyl-carrier protein synthesis. So KatG is a catalase-peroxidase enzyme that carries out acyl-carrier and ketoacyl-carrier protein synthesis. USMLE loves to ask about metabolism of INH. If they show you a bimodal curve of INH metabolism, youve gotta know that people demonstrate phenotypic variation regarding fast vs slow acetylation.

Ive seen a practice question where the hepatotoxicity
of INH was presented as fever, anorexia and nausea, WITHOUT jaundice. Effects can be acute. If they throw neurotoxicity at you, it will be the paresthesias. If its hepatotoxicity, youll get the former Sx (just think, in paracetamol poisoning, does jaundice develop?)

USMLE wants you to know WHY isoniazid causes B6
deficiency.

deficiency. Its bc INH inhibits pyridoxal kinase, so B6 cannot get activated (normally pyridoxine pyridoxal phosphate).

deficiency. Its bc INH inhibits pyridoxal kinase, so B6 cannot get activated (normally pyridoxine pyridoxal phosphate). INH can cause D/NE/E deficiency (secondary to the B6 deficiency)

deficiency. Its bc INH inhibits pyridoxal kinase, so B6 cannot get activated (normally pyridoxine pyridoxal phosphate). INH can cause D/NE/E deficiency (secondary to the B6 deficiency) Seizures secondary to B6 deficiency and INH occur bc of decreased GABA (bc you need B6 to decarboxylate glutamate to GABA!).
Pyrazinamide
Knocks out mycobacterial fatty acid synthase I
Pyrazinamide
Effective in the acidic pH of phagolysosomes
Pyrazinamide
Effective in the acidic pH of phagolysosomes Although it causes hepatotoxicity, it also causes gout
(hyperuricaemia). On my real deal, I was asked the lower-yield side-effect of a drug (hint hint).
Pyrazinamide (beyond FA)

Like INH, pyrazinamide requires activation by TB
Pyrazinamide (beyond FA)

Like INH, pyrazinamide requires activation by TB
FA mentions that pyrazinamide is most effective in the
acidic pH of phagolysosomes, but what this means is that pyrazinamide is the most effective intracellular TB medication thats how theyll ask it. The other drugs still penetrate the cell, but pyrazinamide is simply the best at killing TB that have already been engulfed by macrophages.
Ethambutol
Decreases carbohydrate polymerization of the
mycobacterial cell wall by blocking arabinosyltransferase.
Ethambutol
Decreases carbohydrate polymerization of the
mycobacterial cell wall by blocking arabinosyltransferase. So they want you to know that ethambutol knocks out carbohydrate synthesis but that pyrazinamide knocks out fatty acid synthesis. Isoniazid hits mycolic acid synthesis directly, and rifampin inhibits nucleic acid synthesis.
Ethambutol
Causes optic neuropathy. FA says red-green color
blindness for ethambutol, but Ive seen it in questions as decreased visual acuity and central scotoma.
Ethambutol
blindness for ethambutol, but Ive seen it in questions as decreased visual acuity and central scotoma. Although, of RIPE, RIP are hepatotoxic, ethambutol causes VISUAL PROBLEMS, so if they list hepatotoxicity and central scotoma as two answers, the latter is right, even though FA only says red-green color blindness.
Ethambutol
blindness for ethambutol, but Ive seen it in questions as decreased visual acuity and central scotoma. Although, of RIPE, RIP are hepatotoxic, ethambutol causes VISUAL PROBLEMS, so if they list hepatotoxicity and central scotoma as two answers, the latter is right, even though FA only says red-green color blindness. Tangential: sildenafil instead causes blue-green color blindness.
TB drugs in general
RIPES can also be used instead of RIPE. If they ask
about an aminoglycoside, streptomycin has shown some use against TB.
TB drugs in general
RIPES can also be used instead of RIPE. If they ask
about an aminoglycoside, streptomycin has shown some use against TB. Ive seen in a practice question cycloserine as general TB Tx. It is a broad-spectrum TB drug and can cause CNS effects/seizures.

Protein Synthesis Inhibitors Classification and Mechanisms

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Protein synthesis inhibitors

Protein synthesis inhibitors

Protein synthesis inhibitors

Protein synthesis inhibitors

(and linezolid = lower-yield, but in FA)

Protein synthesis inhibitors

Protein synthesis inhibitors

Protein synthesis inhibitors

buzz words you need to associate with the 50S drugs:

Protein synthesis inhibitors

Protein synthesis inhibitors

Protein synthesis inhibitors

Protein synthesis inhibitors

cause misreading of mRNA.

Protein synthesis inhibitors

Aminoglycosides vs macrolides (names)

steptomycin (highest-yield ones) = AMINOGLYCOSIDES

Aminoglycosides vs macrolides (names)

steptomycin (highest-yield ones) = AMINOGLYCOSIDES Erythromycin, azithromycin, clarithromycin = MACROLIDES

Aminoglycosides vs macrolides (names)

are bactericidal vs static.

initiation complex and cause misreading of the mRNA.

Aminoglycosides (beyond FA)

Aminoglycosides (beyond FA)

Aminoglycosides (beyond FA)

(remember beta-lactam synergy?)

Aminoglycosides (beyond FA)

Aminoglycosides (beyond FA)

Aminoglycosides (beyond FA)

Aminoglycosides (beyond FA)

prevent aminoacyl-tRNA binding to the A-site.

Tetracyclines (beyond FA)

eliminated. Minocycline, like HIPP, can cause SLElike syndrome.

Tetracyclines (beyond FA)

Tetracyclines (beyond FA)

Tetracyclines (beyond FA)

the 23S rRNA. (elaborate)

the 23S rRNA. (elaborate) Ultra-high-yield: Tx for ATYPICAL PNEUMONIAS.

Macrolides (beyond FA)

Macrolides (beyond FA)

Macrolides (beyond FA)

Macrolides (beyond FA)

world because of its cheap cost

Chloramphenicol (beyond FA)

Chloramphenicol (beyond FA)

(metronidazole is below) Good for lung abscesses or aspiration pneumonia

subunit - same as macrolides/clindamycin)

subunit - same as macrolides/clindamycin) 2) Side-effects are HOT:

Sulfonamides (beyond FA)

jaundice kernicterus sulfonamide.

Sulfonamides (beyond FA)

BACTERISTATIC, but if combined (TMP-SMX), they are BACTERICIDAL.

with leucovorin rescue folinic acid

(aka DNA gyrase) very very high-yield

Fluoroquinolones (beyond FA)

Fluoroquinolones (beyond FA)

Fluoroquinolones (beyond FA)

Fluoroquinolones (beyond FA)

Fluoroquinolones (beyond FA)

Fluoroquinolones (beyond FA)

Fluoroquinolones (beyond FA)