Step 1 Antibiotics

Question 1

Penicillin mechanism

Answer 1

binds to penicillin binding proteins in peptidoglycan (blocks transpeptidase crosslinking); activates autolytic enzymes

Question 2

penicillin use

Answer 2

gram positives and syphilis

Question 3

penicillin toxicity

Answer 3

hypersensitivity reactions, hemolytic anemia

Question 4

penicillinase resistant penicillins

Answer 4

methicillin, nafcillin, dicloxacillin

Question 5

penicillinase resistant penicillin use

Answer 5

Staph aureus

Question 6

penicillinase resistant penicillin toxicity

Answer 6

hypersensitivity; methicillin: interstitial nephritis

Question 7

aminopenicillins

Answer 7

ampicillin, amoxacillin

Question 8

aminopenicillin mechanism

Answer 8

same as penicillin but wider spectrum

Question 9

aminopenicillin use

Answer 9

select gram positive and negative bacteria–H flu, E coli, Listeria, Proteus, Salmonella, enterococci

Question 10

aminopenicillin toxicity

Answer 10

hypersensitivity, ampicillin rash, pseudomembranous colitis

Question 11

antipseudomonal drugs

Answer 11

ticarcillin, piperacillin, carbenicillin

Question 12

antipseudomonal mechanism

Answer 12

same as penicillin; wider spectrum

Question 13

antipseudomonal use

Answer 13

Pseudomonas and gram negative rods

Question 14

antipsuedomonal toxicity

Answer 14

hypersensitivity reaction

Question 15

beta lactamase inhibitor mechanism

Answer 15

inhibit beta lactamase (protects penicillins from destruction)

Question 16

beta lacatamase drugs

Answer 16

clavulanic acid, sulbactam, tazobactam

Question 17

bacteriostatic antibiotics

Answer 17

erythromycin, clindamycin, sulfamethoxazole, trimethoprim, tetracycline, chloramphenicol

Question 18

bactericidal antibiotics

Answer 18

vancomycin, fluoroquinolones, penicillin, aminoglycosides, cephalosporins, metronidazole

Question 19

1st generation cephalosporins

Answer 19

cefazolin, cephalexin

Question 20

1st generation cephalosporin coverage

Answer 20

gram positive cocci, Proteus, E coli, Klebsiella

Question 21

cephalosporin mechanism

Answer 21

beta lactams; inhibit cell wall synthesis but less susceptible to penicillinases

Question 22

2nd generation cephalosporins

Answer 22

cefoxitin, cefaclor, cefuroxime

Question 23

2nd generation cephalosporin coverage

Answer 23

same as 1st plus H flu, enterobacter, Neisseria, Serratia

Question 24

3rd generation cephalosporins

Answer 24

ceftriaxone, ceftazidime, cefotaxime

Question 25

3rd generation cephalosporin coverage

Answer 25

serious gram negative infections; ceftriaxone: Neisseria, ceftazidime: pseudomonas

Question 26

4th generation cephalosporins

Answer 26

cefepime

Question 27

cephalosporin toxicity

Answer 27

hypersensitivity, vitamin K deficiency, cross-hypersensitivity with penicillins, increase nephrotoxicity of aminoglycosides, reaction with alcohol

Question 28

aztreonam mechanism

Answer 28

beta lactamase resistant monobactam; binds penicillin binding protein

Question 29

aztreonam use

Answer 29

gram negative rods only

Question 30

aztreonam toxicity

Answer 30

occasional GI upset

Question 31

imipenem/cilastin mechanism

Answer 31

beta-lactamase resistant carbapenem; cilastin is a renal dihydropeptidase 1 (to decrease renal inactivation)

Question 32

imipenem use

Answer 32

broad spectrum; gram + cocci, gram - rods and anaerobes (use limited to life-threatening or refractory infections because of side effects)

Question 33

imipenem toxicity

Answer 33

GI distress, skin rash, CNS toxicity (seizures) at high plasma levels

Question 34

vancomycin mechanism

Answer 34

inhibits cell wall mucopeptide formation by binding D ala D ala portion of cell wall precursors

Question 35

vancomycin use

Answer 35

gram + only; use reserved for resistant infections–Staph aureus, enterococci, C diff

Question 36

vancomycin toxicity

Answer 36

nephrotoxicity, ototoxicity, thrombophlebitis, red man syndrome, but well-tolerated in general

Question 37

resistance to vancomycin

Answer 37

amino acid change from D-ala D-ala to D-ala D-lac

Question 38

30s ribosomal inhibitors

Answer 38

tetracyclins, aminoglycosides

Question 39

50s ribosomal inhibitors

Answer 39

clindamycin, chloramphenicol, erythromycin, linezolid, lincomycin

Question 40

aminoglycoside drugs

Answer 40

gentamicin, neomycin, amikacin, tobramycin, streptomycin

Question 41

aminoglycoside mechanism

Answer 41

inhibit formation of the initiation complex and cause misreading of mRNA; require O2 for uptake

Question 42

aminoglycoside use

Answer 42

no anaerobe coverage; severe gram - rod infections; synergistic with beta lactams; neomycin for bowel surgery

Question 43

aminoglycoside toxicity

Answer 43

nephrotoxicity (esp with cephalosporins), ototoxicity (esp with loop diuretics), teratogen

Question 44

aminoglycoside resistance

Answer 44

drug modification via transferases

Question 45

tetracycline mechanism

Answer 45

binds to 30s and prevents attachment of amino-acyl tRNA; limited CNS penetration

Question 46

tetracycline use

Answer 46

borrelia burgdorferi, H. pylori, Mycoplasma. Rickettsia, Chlamydia (accumulates intercellularly); demeclocycline is ADH antagonist so used in SIADH

Question 47

tetracycline administration consideration

Answer 47

absorption inhibited by milk, antacids, iron preparations; can be used in patients with renal failure because fecally eliminated

Question 48

tetracycline toxicity

Answer 48

GI distress, teeth discoloration, inhibition of bone growth in children, photosensitivity

Question 49

tetracycline resistance

Answer 49

decreased uptake or increased efflux

Question 50

macrolide drugs

Answer 50

erythromycin, azithromycin, clarithromycin

Question 51

macrolide mechanism

Answer 51

binds to 50s subunit and blocks translocation (binds to 23s RNA)

Question 52

macrolide use

Answer 52

atypical pneumonias (mycoplasma, chlamydia, legionella), URIs, STDs, gram positive cocci (in pts allergic to penicillin), Neisseria

Question 53

macrolide toxicity

Answer 53

prolonged QT, GI discomfort, acute cholestatic hepatitis, eosinophilia, skin rashes, increases serum concentration of theophyllines and oral anticoagulants

Question 54

macrolide resistance

Answer 54

methylation of 23s binding site

Question 55

chloramphenicol mechanism

Answer 55

binds to 50s ribosome, inhibits peptidyltransferase activity

Question 56

chloramphenicol use

Answer 56

meningitis (H flu, Neisseria meningitis, Strep pneumo)

Question 57

clindamycin mechanism

Answer 57

binds to the 50 S ribosome, blocks peptide bond formation (bacteriostatic)

Question 58

clindamycin use

Answer 58

anaerobic infections in aspiration pneumonia or lung abscesses

Question 59

clindamycin toxicity

Answer 59

psuedomembranous colitis, fever, diarrhea

Question 60

sulfonamide mechanism

Answer 60

PABA antimetabolites inhibit dihydropteroate synthetase; inhibit bacterial folic acid production (bacteriostatic)

Question 61

sulfonamide use

Answer 61

gram positive, gram negative, Nocardia, chlamydia, simple UTI, also opportunistic infection prophylaxis in HIV patients

Question 62

sulfonamide toxicity

Answer 62

hypersensitivity reactions, hemolysis in G6PD deficiency, nephrotoxicity, photosensitivity, kernicterus in infants, displaces warfarin and other drugs from albumin binding

Question 63

sulfonamide resistance

Answer 63

altered bacterial dihydropteroate synthetase, decreased uptake or increased PABA synthesis

Question 64

trimethoprim mechanism

Answer 64

inhibits bacterial dihydrofolate reductase (bacteriostatic)

Question 65

trimethoprim use

Answer 65

used in combo with sulfamethoxazole for recurrent UTI’s, Shigella. Salmonella, pneumocystis

Question 66

trimethoprim toxicity

Answer 66

megaloblastic anemia, leukopenia, granulocytopenia; lurcovorin rescue to supplement with folinic acid

Question 67

fluoroquinolone mechanism

Answer 67

inhibit bacterial DNA gyrase (bactericidal)

Question 68

sulfonamide drugs

Answer 68

sulfamethoxazole, sulfisoxazole, sulfadiazine

Question 69

fluoroquinolone drugs

Answer 69

ciprofloxacin, norfloxacin, ofloxacin, sparfloxacin, moxifloxacin, gatifloxacin, enxoxacin, nalidixic acid (a quinolone)

Question 70

fluoroquinolone use

Answer 70

gram negative rods of urinary and GI tracts, Neisseria, some gram positive, also has action vs. psuedomonas

Question 71

fluoroquinolone toxicity

Answer 71

GI upset, rash, superinfection, headache, dizziness; contraindicated in pregnant women because of risk or cartilage damage, tendonitis and tendon rupture in adults, legs cramps and myalgias in kids; do not take with antacids

Question 72

fluoroquinolone resistance

Answer 72

chromosomal DNA gyrase mutation

Question 73

metronidazole mechanism

Answer 73

forms free radical toxic metabolites in bacterial cell that damages DNA; bactericidal and anti-protozoal

Question 74

metronidazole use

Answer 74

anaerobes, giardia, entamoeba histolytica, trichomonas, gardnerella vaginalis; used in H. pylori triple therapy

Question 75

metronidazole toxicity

Answer 75

disulfuram like reaction with alcohol; headache; metallic taste

Question 76

polymixin drugs

Answer 76

polymixin B, colistimethate

Question 77

polymixin mechanism

Answer 77

bind to cell membranes of bacteria and disrupt osmotic properties; cationic and basic proteins that act as detergents

Question 78

polymixin toxicity

Answer 78

neurotoxicity, acute renal tubular necrosis

Question 79

polymixin use

Answer 79

resistant gram - infections

Question 80

TB treatments

Answer 80

rifampin, isoniazide, ethambutol, pyrazinamide (isoniazid is prophylaxis)

Question 81

Mycobacterium avium treatment

Answer 81

azithromycin, rifampin, ethambutol, streptomycin

Question 82

mycobacterium leprae treatment

Answer 82

rifampin, dapsone, clofazimine

Question 83

ethambutol toxicity

Answer 83

optic neuropathy

Question 84

pyrazinamide toxicity

Answer 84

hepatotoxicity

Question 85

ethambutol mechanism

Answer 85

blocks arabinosyltransferase to decrease carbohydrate polymerization of cell wall

Question 86

isoniazid mechanism

Answer 86

decreases synthesis of mycolic acids; need bacterial catalase peroxidase to convert isoniazid to active metabolite

Question 87

clinical use of isoniazid

Answer 87

TB

Question 88

isoniazid toxicity

Answer 88

neurotoxicity, hepatotoxicity, lupus, pyradoxime (B6) deficiency–supplementation can prevent neurotoxicity and maybe lupus

Question 89

rifampin mechanism

Answer 89

inhibits DNA-dependent RNA polymerase

Question 90

rifampin use

Answer 90

TB, delays dapsone resistance in leprosy, Neisseria and H.flu prophylaxis

Question 91

rifampin toxicity

Answer 91

minor hepatotoxicity, P450 inducer, orange body fluids

Question 92

rifampin resistance

Answer 92

mutation in RNA polymerase

Question 93

meningococcal prophylaxis

Answer 93

rifampin, minocycline

Question 94

gonorrhea prophylaxis

Answer 94

ceftriaxone

Question 95

syphylis prophylaxis

Answer 95

penicillin G

Question 96

recurrent UTI prophylaxis

Answer 96

TMP-SMX

Question 97

pneumocystis prophylaxis

Answer 97

TMP-SMX, aerosolized pentamidine

Question 98

endocarditis prophylaxis in surgical/dental procedures

Answer 98

penicillins

Question 99

mycobacterium avium prophylaxis

Answer 99

azithromycin

Question 100

amphotericin B mechanism

Answer 100

binds ergosterol in fungal membrane and forms pores that allow leakage of electrolytes; does not cross BBB

Question 101

amphotericin B use

Answer 101

serious systemic mycoses (crypococcus, blastomyces, coccidiodes, aspergillus, histoplasma, candida)

Question 102

amphotericin B toxicity

Answer 102

fever/chills, hypotension, nephrotoxicity, arrhythmias, anemia, IV phlebitis; liposomal amphotericin reduces toxicity

Question 103

nystatin mechanism

Answer 103

binds ergosterol in fungal membrane and forms pores that allow leakage of electrolytes

Question 104

nystatin use

Answer 104

topical only because too toxic for systemic use; “swish and swallow” for oral thrush, topical for diaper rash or vaginal candidiasis

Question 105

nystatin toxicity

Answer 105

too toxic for systemic use but not absorbed in GI tract

Question 106

azole drugs

Answer 106

fluconazole, ketoconazole, clotrimazole, miconazole, itraconazole, voriconazole

Question 107

azole mechanism

Answer 107

inhibit ergosterol synthesis by inhibiting the P450 enzyme that converts lanosterol to ergosterol

Question 108

azole use

Answer 108

systemic mycoses

Question 109

fluconazole use

Answer 109

cryptococcal meningitis in AIDS patients (can cross BBB), candidal infections

Question 110

ketoconazole use

Answer 110

blastomyces, histoplasma, coccidiodes, candida, hypercortisolism

Question 111

clotrimazole, miconazole use

Answer 111

for topical fungal infections

Question 112

azole toxicity

Answer 112

hormone synthesis inhibition (gynecomastia) liver dysfunction, CYP 450 inhibitor, fever, chills

Question 113

flucytosine mechanism

Answer 113

inhibits DNA synthesis by conversion to 5-FU

Question 114

flucytosine use

Answer 114

systemic fungal infections in combo with amphotericin B (candida, crypto)

Question 115

flucytosine toxicity

Answer 115

nausea, vomiting, diarrhea, bone marrow suppression

Question 116

caspofungin mechanism

Answer 116

inhibits cell wall synthesis by inhibiting synthesis of beta glucan

Question 117

caspofungin use

Answer 117

invasive aspergillosis

Question 118

caspofungin toxicity

Answer 118

GI upset, flushing

Question 119

terbinafine mechanism

Answer 119

inhibits fungal squalene epoxidase (preventing the production of ergosterol)

Question 120

terbinafine use

Answer 120

dermatophytoses (especially onychomycosis)

Question 121

griseofulvin mechanism

Answer 121

interferes with microtubule function; disrupts mitosis; deposits in keratin-containing tissues

Question 122

griseofulvin use

Answer 122

oral treatment of superficial infections; dermatophytes (tinea, ringworm)

Question 123

griseofulvin toxicity

Answer 123

P450 inducer (increases warfarin metabolism), teratogenic, carcinogenic, confusion, headaches

Question 124

pyrimethamine mechanism

Answer 124

selectively inhibits plasmodial dihydrofolate reductase (best for . falciparum)

Question 125

pyrimethamine use

Answer 125

for toxoplasmosis with sulfadiazine

Question 126

suramin mechanism

Answer 126

inhibits enzymes involved in energy metabolism; no CNS involvement

Question 127

suramin use

Answer 127

anti-protozoal; blood-borne trypanosoma brucei

Question 128

melarsoprol mechanism

Answer 128

inhibits sulfhydryl groups in parasite enzymes; CNS involvement

Question 129

melarsoprol use

Answer 129

anti-protozoal, CNS penetration of trypanosoma brucei

Question 130

nifurtimox mechanism

Answer 130

forms intracellular oxygen radical that are toxic to the organism

Question 131

sodium stibogluconate mechanism

Answer 131

inhibits glycolysis at PFK reaction

Question 132

nifurtimox use

Answer 132

anti-protozoal, trypanosoma cruzi

Question 133

sodium stibogluconate use

Answer 133

anti-protozoal; leishmania

Question 134

chloroquine mechanism

Answer 134

blocks plasmodium heme polymerase, leading to accumulation of hemoglobin breakdown products that destroy the organism

Question 135

mefloquine mechanism

Answer 135

unknown

Question 136

chloroquine use

Answer 136

malaria

Question 137

mefloquine use

Answer 137

chloroquine resistant malaria

Question 138

quinine mechanism

Answer 138

unknown, maybe blocks protozoal protein/nuclei acid synthesis

Question 139

quinine use

Answer 139

chloroquine resistant malaria when use in combination with pyrimethamine, sulfonamide, babesia

Question 140

mebendazole mechanism

Answer 140

inhibits glucose uptake and microtubule synthesis

Question 141

mebendazole use

Answer 141

anti-helminthic

Question 142

pyrantel pamoate mechanism

Answer 142

stimulates nicotinic receptors at neuromuscular junction; depolarization-induced paralysis; no effect on tapeworms or flukes

Question 143

pyrantel pamoate use

Answer 143

anti-helminthic

Question 144

ivermectin mechanism

Answer 144

intensifies GABA-mediated neurotransmission and causes immobilization; doesn’t cross BBB (so no effect on humans)

Question 145

ivermectin use

Answer 145

anti-helminthic

Question 146

diethylcarbamazine mechanism

Answer 146

unknown

Question 147

diethycarbamazine use

Answer 147

anti-helminthic

Question 148

praziquantel mechanism

Answer 148

increases membrane permeablility to Ca, causing contraction and paralysis in flukes and tapeworms

Question 149

praziquantel use

Answer 149

anti-helminthic

Question 150

primaquine use

Answer 150

plasmodium vivax and ovale

Question 151

amantadine mechanism

Answer 151

blocks viral penetration/uncoating (M2 protein); causes release of dopamine from intact nerve terminals

Question 152

amantidine use

Answer 152

Parkinson’s; prophylaxis and treatment for Influenza A (only A!)

Question 153

amantidine toxicity

Answer 153

ataxia, dizziness, slurred speech

Question 154

amantidine resistance

Answer 154

mutated M2 protein (most Influenza A strains are resistant)

Question 155

zanamivir and oseltamivir mechanism

Answer 155

inhibit influenza neuraminidase, decreases progeny release

Question 156

zanamivir and oseltamivir use

Answer 156

influenza A and B (give early or as prophylaxis!)

Question 157

ribavirin mechanism

Answer 157

inhibits synthesis of guanine nucleosides by competitively inhibiting IMP dephydrogenase

Question 158

ribavirin use

Answer 158

RSV, chronic Hep C

Question 159

ribavirin toxicity

Answer 159

hemolytic anemia; severe teratogen

Question 160

acyclovir mechanism

Answer 160

monophosphorylated by HSV/VZV thymidine kinase; guanosine analog; chain termination of DNA polymerase

Question 161

acyclovir use

Answer 161

HSV (mucocutaneous lesions and encephalitis), VZV, EBV; not effective for latent virus; prophylaxis in immunocompromised patients

Question 162

acyclovir toxicity

Answer 162

generally well-tolerated

Question 163

acyclovir resistance

Answer 163

lack of viral thymidine kinase

Question 164

ganciclovir mechanism

Answer 164

guanosine analog that inhibits viral DNA polymerase (also interferes with human DNA polymerase)

Question 165

ganciclovir use

Answer 165

CMV (esp. in immunocompromised patients)

Question 166

ganciclovir toxicity

Answer 166

leukopenia, neutropenia, thrombocytopenia, renal toxicity

Question 167

ganciclovir resistance

Answer 167

mutated DNA polymerase or lack of viral kinase

Question 168

foscarnet mechanism

Answer 168

viral DNA polymerase inhibitor that binds to pyrophosphate binding site of enzyme; doesn’t need activation

Question 169

foscarnet use

Answer 169

CMV retinitis when ganciclovir fails; also acyclovir resistant HSV

Question 170

foscarnet toxicity

Answer 170

nephrotoxicity

Question 171

foscarnet resistance

Answer 171

mutated DNA polymerase

Question 172

saquinavir class

Answer 172

protease inhibitor

Question 173

ritonavir class

Answer 173

protease inhibitor

Question 174

indinavir class

Answer 174

protease inhibitor

Question 175

nelfinavir class

Answer 175

protease inhibitor

Question 176

amprenavir class

Answer 176

protease inhibitor

Question 177

protease inhibitor mechanism

Answer 177

prevent maturation of new viruses (protease cleaves the polypeptide products of HIV mRNA into functional parts)

Question 178

protease inhibitor toxicity

Answer 178

hyperglycemia, GI intolerance, lipodystrophy, thrombocytopenia

Question 179

zidovudine class

Answer 179

nucleoside reverse transcriptase inhibitor

Question 180

didanosine class

Answer 180

nucleoside reverse transcriptase inhibitor

Question 181

zalcitabine class

Answer 181

NRTI

Question 182

stavudine class

Answer 182

NRTI

Question 183

NRTI mechanism

Answer 183

competitively inhibit nucleotide binding to reverse transcriptase and terminated DNA chain; must be phosphorylated by thymidine kinase

Question 184

zidovudine use

Answer 184

general prophylaxis and during pregnancy to reduce risk of fetal transmission

Question 185

NRTI toxicity

Answer 185

bone marrow suppression (give EPO and G-CSF), peripheral neuropathy, lactic acidosis, rash, megaloblastic anemia

Question 186

nevirapine class

Answer 186

NNRTI

Question 187

efavirenz class

Answer 187

NNRTI

Question 188

delaviridine class

Answer 188

NNRTI

Question 189

NNRTI mechanism

Answer 189

bind to reverse transcriptase at site different from NRTIs; do not need to be phosphorylated for activation

Question 190

NNRTI toxicity

Answer 190

bone marrow suppression (give EPO and G-CSF), peripheral neuropathy, lactic acidosis, rash, megaloblastic anemia

Question 191

enfuviritide class

Answer 191

fusion inhibitor

Question 192

fusion inhibitor mechanism

Answer 192

bind viral gp41 subunit; inhibit conformational change for fusion with CD4 cells; blocks entry and replication

Question 193

enfuvirtide toxicity

Answer 193

hypersensitivity reactions, injection site reaction, increased risk of bacterial pneumonia

Question 194

interferon mechanism

Answer 194

glycoproteins synthesized by virus-infected cells that blocks replication of viruses

Question 195

interferon use

Answer 195

alpha: HBV and HCV, Kaposi’s sarcoma; beta: MS; gamma: NADPH oxidase deficiency

Question 196

interferon toxicity

Answer 196

neuropenia

Question 197

antibiotics to avoid in pregnancy

Answer 197

fluoroquinolones, sulfonamides, aminoglycosides, metronidazole, tetracyclines, ribavirin, griseofulvin, chloramphenicol

Question 198

HAART therapy

Answer 198

2 NRTIs and 1 protease inhibitor or 2 NRTIs and 1 NNRTI