Term
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Definition
-inhibit transpeptidation enzymes involved in cell wall synthesis
-active against gram positive and gram negative
-B lactam ring structure inactivated by B-lactamases (penicillinases) |
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Term
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Definition
-cell wall synthesis inhibitors
-inhibit the transpeptidation enzymes involved in cell wall synthesis
-active against gram positive and gram negative
-have a B lactam ring structure that is inactivated by some B lactamases
-frequently used to treat patients allergic to penicillins |
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Term
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Definition
-inhibit transpeptidation enzymes involved in cell wall synthesis
-B-lactam ring fused to a 5 carbon ring
-resistant to B lactamases |
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Term
| Protein Synthesis inhibitors include... |
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Definition
-aminoglycosides, macrolides, lincomycins, and tetracyclines
-known as broad-spectrum antibiotics
-require bacterial growth to be effective |
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Term
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Definition
-include streptomycin, neomycin, kanamycin, and gentamicin
-bactericidal for gram negative bacteria
-bind to 30S ribosomal subunit
-Require O2 for uptake, not active against anaerobes or intracellular bacteria
-may irreversibily block initiation of translation or cause mRNA misreading
-narrow effective concentration range, Nephrotoxicity and 8th cranial nerve damage (hearing loss/ Ototoxicity especially wen used with loop diuretics). Teratogen. |
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Term
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Definition
MAO: Inhibits 50S peptidyltransferase activity (peptide bond formation). Bacteriostatic
Use: meningitis (H. influenzae, N. meningitidis, S. pneumoniae) Conservative use due to toxicities.
Toxicity: anemia (dose dependent), aplastic anemia (dose independant), gray baby syndrome (in premature infants because they lack liver UDP-glucuronyl transferase). |
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Term
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Definition
Griseofulvin
MOA: Interferes with microtubule function; disrupts mitosis. Deposits in keratin-containing tissues (nails)
Use: Oral treatment of superficial infections; inhibits growth of dermatophytes (tinea, ringworm)
Toxicity: teratogenic, carcinogenic, confusion, headaches, increases/induces P-450 and warfarin metabolism |
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Term
| Drugs in the Macrolides class |
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Definition
-include erythromycin, azithromycin, clarithromycin |
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Term
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Definition
MOA: inhibit protein synthesis by blocking translocation, bind to 23S rRNA of the 50S ribosomal subunit
-Bacteriostatic
USE: URI, pneumonias, STD (gram positive cocci), streptococcal infections in pts allergic to penicillin. Used to treat Mycoplasma, Legionella, Chlamydia, Neisseria. |
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Term
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Definition
Toxicity: GI discomfort (most common cause of noncompliance), acute cholestatic hepatitis, eosinophilia, skin rashes.
-Increase serum concentrations of theophyllines, oral anticoagulants |
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Term
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Definition
MAO: Block peptide bond formation at 50S ribosomal subunit. Bacteriostatic
USE: Treat anaerobic infections above the diaphragm (Bacteroides fragilis, Clostridium perfringes)
Toxicity: Pseudomembranous colitis (C. difficile overgrowth), fever, diarrhea |
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Term
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Definition
MOA: Viral DNA polymerase inhibitor that binds to the pyrophosphate-binding site of the enzyme. Does not require activation by viral kinase.
Use: CMV retinitis in immunocompromised patients when Ganciclovir fails, Acyclovir-resistant HSV.
Toxicity: Nephrotoxicity
Mech of Resistance: Mutated DNA polymerase |
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Term
| MOA of these drugs is that they block cell wall synthesis by inhibition of peptidoglycan cross-linking |
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Definition
| Penicillin, ampicillin, ticarcillin, piperacillin, imipenem, aztreonam, cephalosporins |
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Term
| MOA is block protein synthesis at 30S ribosomal subunit |
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Definition
Aminoglycosides and tetracyclines
Aminoglycosides (gentamicin, neomycin, amikacin, tobramycin, streptomycin Mean GNATS canNOT kill anaerobes)
Tetracyclines (tetracycline, doxycycline, demeclocycline) |
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Term
| MOA: Block peptidoglycan synthesis |
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Definition
| Bacitracin and Vancomycin |
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Term
| Drug that disrupt bacterial cell membranes |
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Definition
Polymyxins
MOA: bind to cell membranes of bacteria and disrupt their osmotic properties. Are cationic, basic proteins that act like detergents
Use: Resistant gram-negative infections
Toxicity: Neurotoxicity, acute renal tubular necrosis |
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Term
| Block nucleotide synthesis |
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Definition
| Sulfonamides and Trimethoprim |
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Term
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Definition
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Term
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Definition
MOA: Inhibits DNA- dependent RNA polymerase
Use: Mycobacterium tuberculosis; delays resistance to dapsone when used for leprosy. Used for meningococcal prophylaxis and chemoprophylaxis in context of children with Haemophilus influenzae type B
Toxicity: minor hepatotoxicity and drug interactions. Increase P-450. Orange body fluids (nonhazardous) |
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Term
| Bacteriostatic Antibiotics |
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Definition
Erythromycin, Clindamycin, Sulfamethoxazole, Trimethoprim, Tetracyclines, Chloramphenicol
Stop bacterial growth
ECSTaTiC about bacteriostatics |
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Term
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Definition
Vancomycin, Fluoroquinolones, Penicillin, Aminoglycosides, Cephalosporins, Metronidazole
Very Finely Proficient At Cell Murder |
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Term
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Definition
MOA: Bind penicillin binding proteins, block transpeptidase cross-linking of cell wall, activate autolytic enzymes
Use: Bactericidal for gram positive cocci, gram positive rods, gram negative cocci, and spirochetes. Not penicillinase resistant
Toxicity: Hypersensitivity reactions, hemolytic anemia |
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Term
Methicillin, Nafcillin, Dicloxacillin
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Definition
(penicillinase-resistant penicillins)
MOA: Bind penicillin binding proteins, block transpeptidase cross-linking of cell wall, activate autolytic enzymes. Pencillinase resistant b/c of bulkier R group.
Use: S. aureus (except MRSA which is resistant b/c of altered penicillin-binding protein target site)
Toxicity: Hypersensitivity reactions, methicillin - interstitial nephritis |
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Term
| Ampicillin, amoxicillin (aminopenicillins) |
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Definition
MOA: Bind penicillin binding proteins, block transpeptidase cross-linking of cell wall, activate autolytic enzymes. Wider spectrum than penicillin. Pencillinase sensitive.
Use: Extended spectrum penicillin - certain gram positive bacteria and gram negative rods (H. influenzae, E. coli, Listeria monocytogenes, Proteus mirabilis, Salmonella, enterococci)
Toxicity: Hypersensitive reactions, ampicillin rash; pseudomembranous colitis. |
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Term
| Ticarcillin, Carbenicillin, Piperacillin |
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Definition
(antipseudomonals)
MOA: Bind penicillin binding proteins, block transpeptidase cross-linking of cell wall, activate autolytic enzymes. Extended spectrum
USE: Pseudomonas species and gram negative rods; penicillanse susceptible, use with clavulanic
Toxicity: Hypersensitivity reactions |
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Term
| 1st Generation Cephalosporins |
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Definition
Cefazolin and Cephalexin
MOA: B lactam drugs that inhibit cell wall synthesis but are less susceptible to penicillinases. Bactericidal
USE: gram positive cocci, Proteus mirabilis, E.coli, Klebsiella pneumoniae
Toxicity: Hypersensitivity reactions, cross hypersensitivity with penicillins in 5-10% people, nephrotoxicity of aminoglycosides, disulfiram like reaction with ethanol |
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Term
CEPHALOSPORINS
2ND GENERATION |
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Definition
Cefoxitin, Cefaclor, Cefuroxime
MAO: B lactam drugs that inhibit cell wall synthesisi but are less susceptible to penicillinases. Bactericidal
USE: Gram positive cocci, H. influenzae, Enterobacter aerogenes, Neisseria spp., Proteus mirabilis, E.coli, Klebsiella pneumoniae, Serratia marcescens
TOXICITY: Hypersensitivity reactions, cross hypersensitivity with penicillins in 5-10% people, nephrotoxicity of aminoglycosides, disulfiram like reaction with ethanol |
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Term
Cephalosporins
3rd generation |
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Definition
Ceftriaxone, Cefotaxime, Ceftazidime
MOA: B lactam drugs that inhibit cell wall synthesis but are less susceptible to penicillinases. Bactericidal
USE: Serious gram-negative infections resistant to other B lactams, meningitis. Ceftazidime for Pseudomonas. Ceftriaxone for gonorrhea
TOXICITY: Hypersensitivity reactions, cross hypersensitivity with penicillins in 5-10% people, nephrotoxicity of aminoglycosides, disulfiram like reaction with ethanol |
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Term
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Definition
MOA: A monobactam resistant to B-lactamases. Inhibits cell wall synthesis (binds to PBP3). Synergistic with aminoglycosides
Use: gram-negative rods: Klebsiella species, Pseudomonas species, Serratia species. No activity against gram positives or anaerobes
Toxicity: occasional GI upset |
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Term
| Imipenem/ Cilastatin, Meropenem |
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Definition
MOA: Imipenem is a broad-spectrum, B lactamase resistant carbapenem. always given with cilastatin (inhibitor of renal dihydropeptidase I) to decrease inactivation in renal tubules
Use: Gram positive cocci, gram negative rods, and anaerobes. Drug of choice for Enterobacter. Limit use to life threatening infections b/c of significant side effects. Meropenem has reduced risk of seizures and is stable to dihydropeptidase I
Toxicity: GI distress, skin rash, and CNS toxicity (seizures) at high plasma levels. |
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Term
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Definition
Vancomycin
MOA: Inhibits cell wall mucopeptide formation by binding D-ala D-ala portion of cell wall precursors. Bactericidal. Resistance occurs with amino acid change of D-ala D-ala to D-ala D-lac
Use: serious gram positive multidrug resistant organisms including S. aureus, S. epidermidis, and Clostridium difficile.
Toxicity: Nephrotoxicity, Ototoxicity, Thromboplebitis, diffuse flushing ("red man syndrome" prevent by pretreatment with antihistamines and slow infusion rate) Well-tolerated in general. |
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Term
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Definition
MOA: decreases synthesis of mycolic acids
Use: Mycobacterium tuberculosis. Only agent used as solo prophylaxis against TB
Tox: Neurotoxicity, hepatotoxicity. Pyridoxine (Vit 6) supplementation can prevent neurotoxicity. |
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Term
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Definition
Metronidazole- Bactericidal and antiprotozoal.
MOA: forms toxic metabolites in the bacterial cell that damage DNA.
Use: Treats Giardia, Entamoeba, Trichomonas, Gardnerella vaginalis, Anaerobes (bacteroides, clostridium). Used with bismuth and amoxicillin or tetracycline for "triple therapy" against H. Pylori. GET GAP on the Metro
Used for Anaerobic infection below the diaphragm & Clindamycin for anaerobes above the diaphragm
Toxicity: Disulfiram like reaction with alcohol (also seen in Cephalosporins with methylthiotetraole group like cefamandole), headache, metallic taste |
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Term
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Definition
Sulfonamides- sulfamethoxazole (SMX), sulfisoxazole, and sulfadiazine
MOA: PABA antimetabolites that inhibit dihydropteroate synthetase. Bacteriostatic
Use: Gram positive, gram negative, Nocardia, Chlamydia, Triple sulfas or SMX for simple UTI
Toxicity: Hypersensitivity reactions, hemolysis if G6PD deficient, nephrotoxicity (tubulointerstitial nephritis), photosensitivity, kernicterus in infants, displace other drugs from albumin like warfarin. |
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Term
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Definition
MOA: inhibits DNA synthesis by conversion to 5-fluorouracil blocking synthesis of pyrimidine precursors.
Use: systemic fungal infections (Candida, Cryptococcus) in combination with amphotericin B.
Tox: Nausea, vomiting, diarrhea, bone marrow suppression. |
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Term
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Definition
MOA: Inhibits DNA-dependent RNA polymerase
Use: TB. Delays resistance to dapsone when used for leprosy. used for meningococcal prophylaxis and chemoprophylaxis in contacts of children with H. influenzae type B.
Tox: Minor hepatotoxicity and drug interactions (↑ P-450); orange body fluids (nonhazerous side effect) |
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Term
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Definition
MOA: binds ergosterol; forms membrane pores that allow leakage of electrolytes
Use: systemic mycoses: cryptococcus, blastomyces, coccidiodes, aspergillus, histoplasma, candida, mucor. does not cross blood-brain barrier
Toxicity: Fever/chills ("shake and bake"), hypotension, nephrotoxicity, arrhythmias, anemia, IV phlebitis. Hydration reduces nephrotoxicity. Liposomal amphotericin reduces toxicity |
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Term
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Definition
MOA: binds to ergosterol, disrupting fungal membranes. Too toxic for systemic use.
Use: "swish and swallow" for oral candidias (thrush); topical for diaper rash or vaginal candidias |
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Term
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Definition
fluconazole, ketoconazole, clotrimazole, miconazole, itraconazole, voriconazole
MOA: inhibit fungal sterol (ergosterol) synthesis
Use: systemic mycosis. Fluconazole for cryptooccal meningitis in AIDS patients b/c can cross blood-brain barrier and candidial infections. Clotrimazole and miconazole for topical fungal infections.
Tox: hormone synthesis inhibition (gynecomastia). Liver dysfunction b/c inhibits cytochrome P-450 |
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Term
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Definition
MOA: inhibits fungal enzyme squalene epoxidase
--> ultimately causing ↓ synthesis of ergosterol
Use: used to treat dermatophytes (especially onychomycosis b/c accumulates in skin and nails) |
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Term
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Definition
MOA: blocks viral penetration/uncoating (M2 protein), may buffer pH of endosomes. Also causes release of dopamine from intact nerve terminal. Blocks influenza A and rubellA and causes problems with the cerebellA.
Use: Prophylaxis and treatment for influenza A; parkinson disease
Tox: Ataxia, dizziness, and slurred speech
Rimantidine is a derivative with fewer CNS side effects b/c does not cross blood brain barrier.
Mech of resistance: Mutated M2 protein. 90% of all influenza A strains are resistant to amantadine so not used. |
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Term
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Definition
MOA: Inhibit influenza neuraminidase, decreasing the release of progeny virus
Use: Both influenza A and influenza B
They are sialic acid analogue inhibitors of influenza A & B |
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Term
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Definition
MOA: Inhibits synthesis of guanine nucleotides by competitively inhibiting IMP dehydrogenase.
Use: RSV, chronic hepatitis C
Tox: Hemolytic anemia and Severe teratogen |
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Term
| Acyclovir, Valacyclovir, Famciclovir |
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Definition
MOA: Guanosine analog. Monophosphorylated by HSV/VZV thymidine kinase. Triphosphate formed by host cellular enzymes. Preferentially inhibits viral DNA polymerase by chain termination.
Use: HSV, VZV, EBV. Most effective for HSV and VZV then EBV and CMV. Used for HSV induced mucocutaneous and genital lesions as well as encephalitis. Prophylaxis in immunocompromised pts. Herpes zoster use famciclovir.
Resistance: lack of thymidine kinase |
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Term
| Ganciclovir and Valganciclovir |
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Definition
MOA: Guanosine analog. 5-monophosphate formed by a CMV viral kinase or HSV/VZV thymidine kinase. Triphosphate formed by cellular kinases. Preferentially inhibits viral DNA polymerase
Use: CMV, espicially in immunocompromised pts
Tox: leukopenia, neutropenia, thrombocytopenia, renal toxicity. More toxic to host enzymes than acyclor. bone marrow suppression and renal impairment.
Mech of resistance: Mutated CMV DNA polymerase or lack of viral kinase |
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Term
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Definition
MOA: Viral DNA polymerase inhibitor that binds to the pyrophophate-binding site of the enzyme. Does not require activation by viral kinase.
Use: CMV retinitis in immunocompromised pts, when ganciclovir fails, acyclovir-resistant HSV.
Tox: Nephrotoxicity
Mech of Resist: Mutated DNA polymerase |
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Term
| Saqinavir, ritonavir, indinavir, nelfinavir, amprenavir |
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Definition
All protease inhibitors end in -navir
MOA: inhibit maturation of new virus by blocking protease in progeny virions
Tox: GI intolerance (nausea, diarrhea), hyperglycemia (insulin resistance), lipodystrophy, thrombocytopenia (indinavir) |
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Term
| Zidovudine, didanosine, zalcitabine, stavudine, lamivudine, abacavir |
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Definition
Nucleoside Reverse transcriptase inhibitors. Must be converted to monophosphate form by cellular thymidine kinase before conversion to triphosphate
MOA: Preferentially inhibit reverse transcriptase of HIV; prevent incorporation of DNA copy of viral genome into host.
Tox: bone marrow suppression in 40% (neutropenia, anemia), peripheral neuropathy, nucleosides cause lactic acidosis. Non-nucleosides cause a rash. Zidovudine causes megaloblastic anemia. GM-CSF and erythropoietin can be used to reduce bone marrow suppression. |
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Term
| Reverse transcriptase inhibitors clinical use |
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Definition
Use: in HAART (highly active antiretroviral therapy) which is combination of therapy with protease inhibitors and reverse transcriptase inhibitors. Initiated when patients have low CD4 counts (less than 500 cells/mm3) or high viral load.
-Zidovudine (nucleoside reverse transcriptase inhibitor) used for general prophylaxis and during pregnancy to reduce risk of fetal transmission. |
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Term
| Nevirapine, Efavirenz, Delavirdine |
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Definition
Never Ever Deliver nucleosides
MOA: Preferentially inhibit reverse transcriptase of HIV; prevent incorporation of DNA copy of viral genome into host.
Tox: bone marrow suppression in 40% (neutropenia, anemia), peripheral neuropathy, nucleosides cause lactic acidosis. Non-nucleosides cause a rash. GM-CSF and erythropoietin can be used to reduce bone marrow suppression.
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Term
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Definition
MOA: Fusion inhibitor. Binds viral gp41 subunit; inhibit conformational change required for fusion with CD4 cells. Therefore block entry and subsequent replication.
Use: In patients with persistent viral replication in spite of antiretrovial therapy. Used in combination with other drugs.
Tox: Hypersensitivity reactions, reactions at subcutaneous injection site, increase risk of bacterial pneumonia. |
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Term
Interferon therapy for what diseases and toxicities
IFN-α
IFN-β
IFN-γ
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Definition
IFN-α- chronic Hep B & C, Kaposi's sarcoma
IFN-β - Multiple Sclerosis
IFN-γ - NADPH oxidase deficiency
Toxicity: neutropnenia |
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Term
| Antibiotics to avoid in pregnancy |
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Definition
SAFE Moms Take Really Good Care
S-sulfonamides- kernicterus
A-aminoglycosides- ototoxicity
F-fluoroquinolones- cartilage damage
E-erythromycin- acute cholestatic hepatitis in mom and clarithromycin- embryotoxic
M-metronidazole- mutagenesis
T- tetracyclines- discolored teeth, inhibition of bone growth
R- ribavirin (antiviral) - teratogenic
G- griseofulvin (antifungal)- teratogenic
C-chloramphenicol- "gray baby" |
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