Drug Summary: Antibiotics (PDF)

Summary

This document summarizes different classes of antibiotics, including their therapeutic actions, indications, pharmacokinetics, contraindications, adverse effects, and drug interactions. It covers Aminoglycosides, Carbapenems, and Cephalosporins, providing crucial information for medical professionals.

Full Transcript

ANTIBIOTICS
AMINOGLYCOSIDES GENTAMICIN
Def: bactericidal used to treat serious infections caused by Gram-negative aerobic bacilli

THERAPEUTIC ACTIONS Inhibit protein synthesis in Gram-negative bacteria
Irreversibly bind to unit of bacteria ribosomes, leading to misreading of the genetic code & cell death.

INDICATIONS For pseudomonas infections and a wide variety of gram-negative infections

PHARMACOKINETICS Through IM, IV; rapid onset
Peak of 30-90 mins; HL of 2-3 hrs, metabolized in the liver

CONTRAINDICATIONS & C/Is: Known allergy to aminoglycosides; renal/hepatic dse; preexisting hearing loss; active herpes or mycobacterial infections;
CAUTION
myasthenia gravis or parkinsonism; lactation.
Administer w/ caution during pregnancy, benefits must be weighed against potential adverse effects on the fetus. Frequent urine
function tests are necessary because drugs depend on the kidney for excretion.
Potential for nephrotoxicity & ototoxicity with amikacin is very high, used only if absolutely necessary
Streptomycin, reserved for use in special situations (very toxic to the eighth cranial nerve and kidney.

ADVERSE EFFECTS Sinusitis, dizziness, rash, fever, risk of nephrotoxicity

DRUG-DRUG Have synergistic bactericidal effects when given with penicillins or cephalosporins. Avoid combining w/ potent diuretics (increases
INTERACTIONS
AEs). If given w/ anesthetics, nondepolarizing neuromuscular blockers, succinylcholine, or citrate anticoagulated blood, increased
neuromuscular blockade with paralysis is possible.
If given to patient for surgery, indicate in chart & provide extended monitoring and support after surgery

CARBAPENEMS ERTAPENEM

THERAPEUTIC ACTIONS Bactericidal that inhibit cell membrane synthesis in susceptible bacteria, leading to cell death
INDICATIONS Treatment of community-acquired pneumonia, complicated GU infections, complicated intra-abdominal infections, skin-and-skin
structure infections, and acute pelvic infections caused by susceptible bacteria

PHARMACOKINETICS Given IV or IM, once a day for 5 to 14 days, depending on the infection.
Rapid onset
Peak of 30-120 mins.
HL 4 hrs, excreted unchanged in urine

CONTRAINDICATIONS & C/Is: Known allergy, seizure disorders, meningitis, lactation
CAUTION
Use caution during pregnancy. Test urine function regularly (depend on kidney for excretion & toxic to kidney).
Ertapenem & meropenem-vaborbactam - not recommended in patients younger than 18 years of age.

ADVERSE EFFECTS Headache, dizziness, nausea, vomiting, pseudomembranous colitis, rash, pain at injection site

DRUG-DRUG Consider an alternative treatment if patient is on valproic acid. Combination of these drugs can cause serum valproic acid levels
INTERACTIONS
to fall and increase the risk of seizures.

CEPHALOSPORINS CEFACLOR

THERAPEUTIC ACTIONS Inhibits the synthesis of bacterial cell walls, causing cell death in susceptible bacteria

INDICATIONS For respiratory tract infections, skin infections (dermatologic), UTI, otitis media (middle ear), typhoid fever, anthrax exposure

PHARMACOKINETICS Via oral, peak of 20-60 mins, duration of 8-10 hrs
HL of 30-60 mins, excreted unchanged in urine

CONTRAINDICATIONS & C/Is: Allergies to cephalosporins or penicillins because cross-sensitivity is common.
CAUTION
Cautions: Hepatic or renal impairment - cephalosporins are toxic to kidneys & could interfere w/ metabolism & excretion.
Pregnant or lactation – potential effects on fetus/infant not known; use only if benefits outweigh risk.
ADVERSE EFFECTS Nausea, vomiting, diarrhea, rash, superinfections, bone marrow depression, risk for pseudomonas colitis

DRUG-DRUG Cephalosporins with aminoglycosides increases the risk for nephrotoxicity. Frequently monitor patients receiving this
INTERACTIONS
combination, & evaluate serum blood urea nitrogen (BUN) & creatinine levels.
Oral anticoagulants + cephalosporins - may increase bleeding. Monitor blood loss (e.g., bleeding gums, easy bruising), may
reduce anticoagulant dose.
Avoid alcohol for up to 72 hours after discontinuation the drug to prevent a disulfiram-like reaction, which results in unpleasant
symptoms such as flushing, throbbing headache, nausea and vomiting, chest pain, palpitations, dyspnea, syncope, vertigo,
blurred vision, and, in extreme reactions, cardiovascular collapse, convulsions, or even death.

FLUOROQUINOLONES CIPROFLOXACIN

THERAPEUTIC ACTIONS Interferes with DNA replication in susceptible Gram-negative bacteria, preventing cell reproduction

INDICATIONS Treatment of respiratory, dermatological, UTI, ear, eye, bone and joint infection; treatment after anthrax exposure, typhoid fever,
plague

PHARMACOKINETICS ORAL - onset varies, peak of 60-90 min, duration of 4-5 hrs
IV - onset in 10 mins, peak of 30 mins, duration of 4-5 hrs
HL of 3.5-4 hrs, metabolized in the liver, excreted via bile and urine

CONTRAINDICATIONS & C/Is: Allergy to drug, pregnancy, lactation.
CAUTION
Cautions: presence of renal dysfunction (could interfere w/ metabolism & excretion of drug), & seizures (exacerbated by drugs’
effects on cell membrane channels).
Not recommended for use in patients younger than 18 (drug is associated with lesions in developing cartilage).

ADVERSE EFFECTS Headache, dizziness, hypotension nausea, vomiting, diarrhea, fever, rash
DRUG-DRUG Effect decreased if taken concurrently w/ iron salts, sucralfate, mineral supplements, or antacids.
INTERACTIONS
If drug combination is necessary, administer 2 agents by at least 4 hours apart.
Fluoroquinolones taken w/ drugs that increase the QTc interval- severe- to-fatal cardiac reactions are possible & should be
avoided, but if used, patients should be hospitalized with continual cardiac monitoring.
Fluoroquinolones w/ theophylline leads to increased theophylline levels coz 2 drugs use similar metabolic pathways. Theophylline
dose should be decreased by one-half and serum theophylline levels monitored carefully.
Fluoroquinolones w/ nonsteroidal antiinflammatory drugs- increased risk of CNS stimulation is possible. closely monitor patients,
especially those who have a history of seizures or CNS problems.
Fluoroquinolone with corticosteroids- can increase risk of tendonitis & tendon rupture. Instruct patient to report any tendon pain or
weakness.

PENICILLINS AND AMOXICILLIN
PENICILLINASE-RESISTANT
ANTIBIOTICS

THERAPEUTIC ACTIONS Inhibits synthesis of the cell wall in susceptible bacteria, causing cell death

INDICATIONS For infections caused by susceptible strains of bacteria; treatment of helicobacter infections as part of combination therapy. Tow
off label uses include post exposure prophylaxis for anthrax and endocarditis

PHARMACOKINETICS Oral, reaching peak levels in 1 hour. Sensitive to gastric acid levels in stomach & should be taken on empty stomach to ensure
adequate absorption. Onset varies. Peak of 1hr, duration of 6-8 hrs
Excreted unchanged in urine, making renal function an important factor in safe use of the drug, HL of 1-1.4 hrs

CONTRAINDICATIONS & C/Is: allergies to penicillin or cephalosporins or other allergens.
CAUTION
Cautions: renal disease (lowered doses are necessary because excretion is reduced). Although there’s no adequate studies of
use during pregnancy, use in patients who are Use in pregnant or lactating mothers- only when benefit is clear. Diarrhea &
superinfections may occur in the infant. Perform culture and sensitivity tests

ADVERSE EFFECTS Nausea, vomiting, diarrhea, glossitis, stomatitis, bone marrow suppression, rash, fever, superinfections, lethargy
DRUG-DRUG Combinations that should be avoided:
INTERACTIONS
Penicillins & penicillinase-resistant antibiotics with tetracyclines- will decrease penicillin’s effectiveness. Penicillin doses should be
raised if cannot be avoided, which could increase the occurrence of adverse effects.
Parenteral forms of penicillins & penicillinase- resistant drugs with any of the parenteral aminoglycosides, inactivation of the
aminoglycosides occurs.

SULFONAMIDES COTRIMOXAZOLE

THERAPEUTIC ACTIONS Blocks two consecutive steps in protein and nucleic acid production, leading to inability for cells to multiply

INDICATIONS For UTI, acute otitis media in children, exacerbations of chronic bronchitis in adults, traveler’s diarrhea in adults, pneumocystis
jiroveci pneumonia when caused by susceptible strains of bacteria

PHARMACOKINETICS Combination of sulfamethoxazole & trimethoprim. Orally, rapidly absorbed; peak: 1-4 hrs.
Half-life: 8-10 hrs, excreted in urine

CONTRAINDICATIONS & C/Is: allergy to: Any sulfonamide, Sulfonylureas, Thiazide diuretics (due to cross-sensitivities). Pregnancy (risk of birth defects
CAUTION
and kernicterus). Lactation (risk of kernicterus, diarrhea, and rash in the infant
Cautions: Renal disease or history of kidney stones (risk of increased toxic effects) Elderly (increased incidence of CNS effects
and safety concerns)

ADVERSE EFFECTS GIT: Nausea, vomiting, diarrhea, hepatocellular necrosis, hematouria, bone marrow suppression, rash, urticaria, photophobia,
fever and chills

DRUG-DRUG Antidiabetic Agents- increased risk of hypoglycemia when combined with: Tolbutamide, tolazamide, glyburide, glipizide,
INTERACTIONS
chlorpropamide. Requires monitoring and possible dose adjustment of the antidiabetic agent during and after sulfonamide
therapy.
Cyclosporine- increased risk of nephrotoxicity. Requires close monitoring; D/C sulfonamide if renal dysfunction occurs.
TETRACYCLINE TETRACYCLINE

THERAPEUTIC ACTIONS Inhibit protein synthesis in bacteria; Prevent bacteria from multiplying; Potential toxicity to humans at high concentrations due to
similarity to human proteins.

INDICATIONS For infections caused by susceptible strains of bacteria, acne, and when penicillin is contraindicated for eradication of susceptible
organisms

PHARMACOKINETICS Oral - onset varies, peak of 2-4 hrs
Topical - minimal absorption occurs, peak of 2-4 hrs
HL of 6-12 hrs, excreted unchanged in urine

CONTRAINDICATIONS & C/Is: Allergy to tetracyclines or tartrazine. Pregnancy & lactation (due to effects on developing bones and teeth).
CAUTION
Ophthalmic preparation in patients with fungal, mycobacterial, or viral ocular infections (risk of exacerbating infection by
disrupting normal flora)
Cautions: Children younger than 8 years of age (potential damage to developing bones and teeth). Patients with hepatic or renal
dysfunction (due to concentration in bile and excretion in urine).

ADVERSE EFFECTS Nausea, vomiting, diarrhea, glossitis, discoloring and inadequate calcification of primary teeth of fetus or secondary teeth in
children, bone marrow suppression, photosensitivity, superinfections, rash, local irritation (topical)

DRUG-DRUG Effectiveness of penicillin G decreases when taken with tetracyclines. Increase the dose of penicillin G if used in combination with
INTERACTIONS
tetracyclines.
Digoxin toxicity rises when tetracyclines are taken concurrently.
Administer on an empty stomach 1 hour before or 2 to 3 hours after any meal or other medication.

ANTIMYCOBACTERIALS ISONIAZID

THERAPEUTIC ACTIONS Interferes with lipid and nucleic acid synthesis in actively growing tubercle bacilli

INDICATIONS Treatment of TB as part of combination therapy, prophylactic treatment of household members of pt diagnosed with TB
PHARMACOKINETICS Well absorbed from the GI tract when taken orally, onset varies, peak of 1-2 hrs, duration of 24 hrs
Metabolized in the liver and excreted in the urine with HL of 1-4 hrs

CONTRAINDICATIONS & Contraindicated for patients with known allergies to these agents.
CAUTION
Not recommended for those with severe renal or hepatic failure or severe CNS dysfunction.
Pregnancy is a caution due to potential adverse effects on the fetus; if necessary, a regimen of isoniazid, ethambutol, and
rifampin is considered safest.

ADVERSE EFFECTS Peripheral neuropathies, nausea, vomiting, hepatitis, bone marrow suppression, fever, local irritation at injection sites,
gynecomastia, lupus syndrome

DRUG-DRUG Increased risk of toxic liver reactions when rifampin and INH are combined. Decreased effectiveness due to increased
INTERACTIONS
metabolism when rifampin or rifabutin is combined with various other drugs (e.g., quinidine, metoprolol, oral contraceptives).
Bedaquiline users should avoid other drugs that prolong the QTc interval.
Close monitoring and dose adjustments required for patients on these drug combinations.

KETOLIDES TELITHROMYCIN

THERAPEUTIC ACTIONS Binds to bacterial ribosomes, altering protein function and leading to bacterial cell death

INDICATIONS Effective against several resistant strains, including: S. pneumoniae (including multidrug-resistant strains), H. influenzae, M.
catarrhalis, Chlamydophila pneumoniae, & M. pneumoniae.
Approved for treating mild to moderate community-acquired pneumonia

PHARMACOKINETICS Oral, rapid onset, peak at 0.5-4 hrs
HL of 10 hours, metabolized in the liver, excreted in feces and urine

CONTRAINDICATIONS & Contraindicated with:
CAUTION
Allergy to the drug or macrolide antibiotics. Known congenital prolonged QT interval, bradycardia, or proarrhythmic conditions
(e.g., hypokalemia). Concurrent use of pimozide, cardiac antiarrhythmics, simvastatin, atorvastatin, or lovastatin. Myasthenia
 gravis (due to risk of respiratory failure, black box warning).
Use with caution in: Renal or hepatic impairment. Pregnant and lactating patients

ADVERSE EFFECTS Headache, dizziness, nausea, vomiting, pseudomembranous colitis, superinfections

DRUG-DRUG Avoid combinations with: Pimozide, simvastatin, lovastatin, atorvastatin (risk of serious adverse effects).
INTERACTIONS
Monitor closely if combined with: Digoxin and metoprolol (risk of increased serum levels).
Avoid or substitute other antibiotics if combined with: Rifampin, phenytoin, carbamazepine, or phenobarbital (risk of decreased
telithromycin levels).
Separate doses by at least 1 hour if combined with theophylline (risk of increased GI toxicity).

LINCOSAMIDES CLINDAMYCIN

THERAPEUTIC ACTIONS Target bacterial protein synthesis, similar to other antibiotics.

INDICATIONS For infections caused by bacteria (anaerobes); useful in septicemia and chronic bone and joint infections

PHARMACOKINETICS Oral - onset varies, peak of 1-2 hrs, duration 8-12 hrs
IM - onset within 20-30 mins, peak of 1-3 hrs, same duration
IV - immediate onset, peak in minutes, same duration
Topical - minimal absorption
HL of 2 to 3 hours, metabolized in the liver, excreted in the urine and feces

CONTRAINDICATIONS & Use with caution in patients with hepatic or renal impairment.
CAUTION
Use during pregnancy and lactation only if the benefits outweigh the risks.

ADVERSE EFFECTS Nausea, vomiting, diarrhea, pseudomembranous colitis, bone marrow suppression

DRUG-DRUG None mentioned
INTERACTIONS
LIPOGLYCOPEPTIDES TELEVANCIN

THERAPEUTIC ACTIONS Affects bacterial cell wall synthesis, leading to disruption of cell membrane function and bacterial cell death

INDICATIONS Treatment of complicated skin and skin structure infections

PHARMACOKINETICS Available as IV. rapid onset, peak at the end of infusion
8-9.5 hrs HL, unknown site of metabolism, excreted via urine

CONTRAINDICATIONS & Contraindicated with known allergy to the drug.
CAUTION
Not recommended for pregnant or lactating patients due to potential toxic effects.
Telavancin has a black box warning for serious fetal risk; contraceptive measures are urged.
Culture and sensitivity testing is necessary to ensure appropriate use.

ADVERSE EFFECTS Nausea, vomiting, diarrhea, taste alterations, QT prolongation, nephrotoxicity, foamy urine

DRUG-DRUG Increased risk of prolonged QT interval and arrhythmias when combined with other QTprolonging drugs; ECG monitoring
INTERACTIONS
recommended.
Increased risk of nephrotoxicity when combined with nephrotoxic drugs; renal function should be monitored.

MACROLIDES ERYTHROMYCIN

THERAPEUTIC ACTIONS may be bactericidal or bacteriostatic, affecting bacterial protein synthesis by binding to ribosomes.

INDICATIONS For respiratory, dermatological, UTI and GI infections

PHARMACOKINETICS Oral - onset in 1-2 hrs, peak within 1-4 hrs
IV, rapid onset, peak in 1 hr
HL of 3 to 5 hrs, metabolized in the liver, excreted in bile and urine
CONTRAINDICATIONS & Contraindicated in patients with a known allergy to macrolides (cross-sensitivity occurs). Ocular preparations contraindicated for
CAUTION
viral, fungal, or mycobacterial eye infections.
Use with caution in: Patients with hepatic or renal dysfunction; Pregnant and lactating women (macrolides in breast milk can
cause diarrhea and superinfections in infants).

ADVERSE EFFECTS Abdominal cramping, vomiting, diarrhea, rash, superinfections, liver toxicity, pseudomonas colitis, possibly hearing loss

DRUG-DRUG Digoxin: Increased serum levels when taken with macrolides; monitor and adjust dosage.
INTERACTIONS
Oral anticoagulants, theophyllines, carbamazepine, corticosteroids: Effects increase due to metabolic changes in the liver; may
require dose reduction and careful monitoring.
Cycloserine: Increased serum levels, risk of renal toxicity; avoid combination if possible.

DRUG-FOOD Food decreases absorption of oral macrolides.
INTERACTIONS
Take macrolides on an empty stomach with a full glass of water 1 hour before or 2-3 hours after meals.

OXAZOLIDINONES LINEZOLID

THERAPEUTIC ACTIONS Binds to ribosomes within bacterial cell

INDICATIONS For infections caused by resistant strains, pneumonias, skin and skin structure infections, diabetic foot infections

PHARMACOKINETICS Oral and IV, rapid onset, peak in 1-2 hrs (oral) and 90 mins (IV)
HL of 5 hours, metabolized in liver, excreted in urine

CONTRAINDICATIONS & Contraindicated with: Known allergy to the drug or components; Phenylketonuria (with oral suspension of linezolid); Patients on
CAUTION
MAO inhibitors (due to reversible MAO inhibitor effect); Breastfeeding women (drug enters breast milk, can be toxic).
Use with caution in patients with: Hepatic impairment, pheochromocytoma, hypertension, hyperthyroidism, bone marrow
suppression. During pregnancy (effects on fetus unknown).

ADVERSE EFFECTS Headache, dizziness, vomiting, diarrhea, potential for pseudomembranous colitis, thrombocytopenia
DRUG-DRUG Increased risk of hypertension with drugs that raise blood pressure.
INTERACTIONS
Increased risk of bleeding and thrombocytopenia with NSAIDs and platelet inhibitors.
Risk of serotonin syndrome with serotogenic drugs; avoid combination unless necessary.
Serotonergic drugs should be stopped 2 weeks before starting oxazolidinones.

DRUG-FOOD Avoid large amounts of tyramine-containing foods due to the risk of serious or life-threatening hypertension.
INTERACTIONS

MONOBACTAM ANTIBIOTIC AZTREONAM

THERAPEUTIC ACTIONS Effective against Gram-negative enterobacteria. Not effective against Gram-positive or anaerobic bacteria; Disrupts bacterial cell
wall synthesis, causing cell death.

INDICATIONS For lower respiratory, dermatological, UTI, intra-abdominal, gynecological infections

PHARMACOKINETICS IM - onset varies, peak in 60-90 mins, 6-8 hrs duration
IV- immediate onset, 30 mins peak, same duration
HL 1.5 to 2 hrs, excreted unchanged in urine

CONTRAINDICATIONS & Contraindicated in patients with known allergy to aztreonam.
CAUTION
Use with caution in patients with: History of acute allergic reaction to penicillins or cephalosporins (possible cross-reactivity),
Renal or hepatic dysfunction (may interfere with drug clearance and excretion), Pregnant and lactating women (potential adverse
effects on fetus or neonate).

ADVERSE EFFECTS Nausea, vomiting, diarrhea, rash, superinfections, anaphylaxis, local discomfort

DRUG-DRUG Incompatible in solution with nafcillin, cephradine, and metronidazole.
INTERACTIONS