Overview of antibiotic therapy

Last updated: June 5, 2023

Summary

Antibiotics are a class of drugs employed mainly against bacterial infections. Some antibiotics are also used against parasitic infections. Antibiotics can have bacteriostatic (i.e., stopping bacterial reproduction), bactericidal (i.e., killing bacteria), or both mechanisms of action. Antibiotics are effective against either a small group of bacteria (narrow-spectrum) or a wide range of pathogens (broad-spectrum). Most antibiotics work by inhibiting cell wall synthesis, protein synthesis, or certain enzymes (e.g., THF, RNA-polymerase) in bacteria. Common side effects of antibiotic treatment include hypersensitivity reactions, as well as nephrotoxic and hepatotoxic effects. Many antibiotics are contraindicated in certain patient groups (e.g., children, pregnant and/or breastfeeding women). In the case of severe infection, one or more antibiotics may be initiated without waiting for a microbiological confirmation (empiric antibiotic therapy) to target the most likely pathogens. Antibiotics are widely used because they are instrumental in the management of infectious diseases; however, use of antibiotics without valid indications and with inappropriate dosages and timing has led to the emergence of antibiotic-resistant pathogens (e.g., MRSA, Pseudomonas).

Overview

Definitions

Antibiotics: antimicrobial drugs effective against bacteria
Bactericidal drug: a substance that kills bacteria (e.g., β-lactams, glycopeptides, epoxides)
- Some antibiotics are only effective if used:
  - In combination (e.g., sulfonamides combined with diaminopyrimidine; streptogramin A combined with streptogramin B
  - Against certain pathogens (e.g., oxazolidinones are only bactericidal against Streptococci)
  - In higher concentrations (e.g., amphenicols)
Bacteriostatic drug: a substance that slows bacterial growth or stops bacterial reproduction (e.g., tetracyclines, glycylcyclines, macrolides)
- Some antibiotics are bacteriostatic only against certain pathogens (e.g., glycopeptides against C. difficile).
- Some antibiotics can be both bactericidal and bacteriostatic (e.g., dapsone ).
- Antibiotics that are interfering with bacterial protein synthesis target the subunits (30S and 50S) of bacterial ribosomes (70S) and do not affect human ribosomes (80S).

As a general rule, agents that inhibit cell wall synthesis are bactericidal (except ethambutol), while those that inhibit protein synthesis are bacteriostatic (except rifamycins, and aminoglycosides).

Overview ^[1]^[2]

Overview of antibiotics
Antibacterial classes		Examples	Mechanism of action	Bacteriostatic/bactericidal	Mechanisms of resistance
Inhibition of cell wall synthesis
β-lactams	Penicillins	Natural penicillins (penicillin G and penicillin V) Anti-staphylococcal penicillins (e.g., oxacillin, nafcillin, dicloxacillin) Aminopenicillins (amoxicillin, ampicillin) Antipseudomonal penicillins (e.g., piperacillin, ticarcillin)	Bind to penicillin-binding proteins (PBPs) → ↓ crosslinking of peptidoglycan layer	Bactericidal	Cleavage of β-lactam ring by β-lactamases (penicillinases) PBP mutations (e.g., MRSA)
	Cephalosporins	1^st generation (e.g., cephalexin) 2^nd generation (e.g., cefaclor) 3^rd generation (e.g., cefixime) 4^th generation (e.g., cefepime) 5^th generation (ceftaroline)			Cleavage of β-lactam ring by β-lactamases (cephalosporinases) PBP mutations
	Carbapenems	Imipenem Meropenem Ertapenem Doripenem			Cleavage of β-lactam ring by β-lactamases (carbapenemases)
	Monobactams	Aztreonam			Cleavage by β-lactamases (less suceptible than other ß-lactams)
Glycopeptides		Vancomycin Bacitracin Teicoplanin Telavancin Dalbavancin Oritavancin	Bind to D-alanyl-D-alanine section of peptidoglycan precursor → inhibited peptidoglycan synthesis	Bactericidal Bacteriostatic against C. difficile	Reduced penetration in gram-negative bacteria Change in peptidoglycan precursor structure D-alanyl-D-alanine → D-alanyl-D-lactate Glycopeptides do not bind to the altered precursor.
Epoxides		Fosfomycin	Inactivate enolpyruvate transferase (MurA) → inhibition of N-acetylmuramic acid formation → disruption of peptidoglycan synthesis ^[3]	Bactericidal	Reduced penetration Enzyme gene overexpression Enzymatic inactivation
Disruption of cell membrane integrity
Lipopeptides		Daptomycin	Lipid portion binds to bacterial cytoplasmic membrane → formation of ion-conducting channels → intracellular K⁺ efflux → bacterial cell membrane depolarization	Bactericidal	Not fully understood Altered cell membrane potential
Polymyxins		Polymyxin E (colistin) Polymyxin B	Cationic detergents (polypeptides) bind to outer cell membrane (phospholipids on gram-negative bacteria) → ↑ permeability → bacterial lysis Bind to and inhibit lipopolysaccharides → ↓ effect of bacterial endotoxins	Bactericidal	Not fully understood Altered lipid A portion of lipopolysaccharides (LPSs) Efflux pumps
Inhibition of protein synthesis - 30S ribosomal subunit
Aminoglycosides		Gentamicin Amikacin Tobramycin Streptomycin Neomycin	Inhibit initiation complex → protein mistranslation	Bactericidal	Inactivating enzymes (via e.g., acetylation, phosphorylation, adenylation) Removal by efflux pumps Mutation of the bacterial ribosome binding site Reduced penetration Anaerobic bacteria Acidic environment
Tetracyclines		Tetracycline Doxycycline Minocycline Eravacycline Sarecycline Omadacycline	Block incoming aminoacyl-tRNA with amino acids → ↓ protein synthesis	Bacteriostatic	Reduced cell wall penetration Removal by efflux pumps (plasmid-encoded) Production of a protein that protects ribosome
Glycylcyclines (tetracyclin derivative)		Tigecycline		Bacteriostatic	Designed to overcome the resistance of tetracycline (e.g., efflux pumps, ribosomal protection) ^[4]
Inhibition of protein synthesis - 50S ribosomal subunit
Macrolides and ketolides		Erythromycin Clarithromycin Azithromycin	Bind to 23S rRNA → inhibition of transpeptidation, translocation, and chain elongation → ↓ protein synthesis	Bacteriostatic	Reduced penetration Efflux pumps Methylation of 23S rRNA binding site → inhibits binding of macrolides Cross-resistance with clindamycin and streptogramins Mutation of bacterial ribosome binding site
Lincosamides		Clindamycin	Impair transpeptidation → inhibition of chain elongation → ↓ protein synthesis Increase opsonization and phagocytosis Inhibit alpha toxin expression	Bacteriostatic	Reduced penetration Mutation of bacterial ribosome binding site
Streptogramins		Quinupristin-dalfopristin	Dalfopristin binds to 23S portion of the 50S subunit → conformation change → facilitation of binding of quinupristin Quinupristin binds to and blocks 50S subunit → inhibition of polypeptide elongation → ↓ protein synthesis ^[5]	Bactericidal when used in combination Bacteriostatic when used separately	Alteration of bacterial ribosome binding site Enzyme-mediated methylation Efflux pumps
Oxazolidinones		Linezolid	Prevent association of 50S with 30S subunit → impairment of initiation complex formation → early interruption of protein synthesis	Bacteriostatic Only bactericidal against Streptococci	Point mutation of the 23S rRNA
Amphenicols		Chloramphenicol	Prevent binding of amino acid-containing aminoacyl-tRNA → inhibition of peptidyltransferase → ↓ protein synthesis	Bacteriostatic Bactericidal in higher concentrations	Reduced penetration Enzymatic inactivation by acetyltransferase (plasmid-encoded)
DNA gyrase inhibition
Fluoroquinolones		Norfloxacin Moxifloxacin Gemifloxacin Ciprofloxacin Ofloxacin Levofloxacin Enoxacin	Inhibit prokaryotic topoisomerase II (DNA gyrase) and topoisomerase IV → inhibited DNA synthesis	Bacteriostatic and bactericidal	Mutations (chromosome-encoded) in DNA gyrase and topoisomerase IV ↓ Cell wall permeability Efflux pumps (plasmid-encoded resistance)
Disruption of DNA integrity
Nitroimidazoles		Metronidazole Tinidazole	Prodrug ^[6] Free radical formation → single-strand breaks in DNA molecules	Bactericidal (and antiprotozoal)	Reduced activation due to decreased enzymatic activity
Inhibition of folic acid synthesis and reduction
Sulfonamides and diaminopyrimidines		Trimethoprim-sulfamethoxazole Sulfadiazine and pyrimethamine Sulfisozaxole	Prevent bacterial tetrahydrofolate formation (THF) → ↓ DNA methylation Synergistic effect Sulfamethoxazole inhibits THF Trimethoprim inhibits dihydrofolate reductase (DHFR).	Bactericidal (sulfamethoxazole) Bacteriostatic (trimethoprim)	Overproduction of para-aminobenzoate (PABA) Decreased uptake Structural changes on target enzymes (e.g., dihydropteroate synthase) Efflux pumps
Antimycobacterial drugs
Rifamycins		Rifampin Rifabutin Rifaximin	Block mRNA synthesis via inhibition of bacterial DNA-dependent RNA-polymerase → ↓ protein synthesis	Bacteriostatic and bactericidal	Mutated RNA-polymerase → ↓ binding of rifamycins
Hydrazides		Isoniazid	Prodrug Inhibits mycolic acid synthesis → ↓ cell wall synthesis	Bactericidal	Mutation causing ↓ KatG → ↓ expression of catalase-peroxidase
Nicotinamides		Pyrazinamide	Prodrug Not completely understood	Bacteriostatic	Mutations in RpsA gene coding for ribosomal protein S1
Ethylenediamine derivates		Ethambutol	Inhibits arabinosyltransferase → ↓ cell wall synthesis	Bacteriostatic	Mutations in EmbCAB gene coding for arabinosyltransferase → inability of the drug to inhibit the enzyme
Sulfones		Dapsone	Competitive antagonism of para-aminobenzoic acid → inhibited dihydrofolic acid synthesis	Bacteriostatic and bactericidal	Mutations in folP1 gene coding for dihydropteroate synthase → ↓ expression of dihydropteroate synthase
Others
Nitrofurans		Nitrofurantoin	Prodrug Bind to bacterial ribosomes → inhibtion of DNA, RNA, (cell wall) and protein synthesis ^[7]^[8]	Bacteriostatic Bactericidal in higher concentrations	Enzyme-mediated reduction Efflux pumps

AcTions at 30, CELebrationS at 50: Aminoglycosides and Tetracyclines are 30S inhibitors; Chloramphenicol/Clindamycin, macrolides (e.g., Erythromycin), Linezolid, and Streptogramin are 50S inhibitors.

All protein synthesis inhibitors are bacteriostatic, except aminoglycosides (bactericidal) and linezolid (can be either bactericidal or bacteriostatic depending on concentration).

Mechanism of action: antibiotics Mechanisms of action of antibiotics on the bacterial ribosome Antibiotics interfering with folate/tetrahydrofolate synthesis

Beta-lactam antibiotics

Beta-lactams

Definition: : a group of antibiotics that contains beta-lactam ring in their molecular structure; and includes penicillins, carbapenems, monobactams, and cephalosporins
Mechanism of action
- Inhibit cell wall synthesis by blocking peptidoglycan crosslinking
  - β-lactam mimics the D-ala-D-ala structure of bacterial peptidoglycan residue.
  - β-lactam irreversibly binds to penicillin-binding proteins (PBPs) which act as transpeptidases → stalled cross-linking of peptidoglycan in cell wall; (β-lactam cannot be cleaved) → inability to synthesize new cell wall during replication → bacterial death (bactericidal effect)
- Activate autolytic enzymes ^[9]
CNS penetration
- Only when meninges are inflamed
- Exceptions: ceftriaxone and aztreonam always have good CNS penetration.
Route of elimination
- Primarily renal (via tubular secretion)
- Exceptions
  - Primarily biliary: nafcillin
  - Both renal and biliary: other anti-staphylococcal penicillins (e.g., oxacillin, dicloxacillin), ceftriaxone
General adverse effects
- Jarisch-Herxheimer reaction (e.g., in treatment of syphilis)
- Hypersensitivity reactions

Beta-lactamase inhibitors

β-lactamases
- Are usually produced by gram-negative and anaerobic organisms
- Can split the β-lactam ring and render certain β-lactam antibiotics ineffective
β-lactamase inhibitors
- Prevent the destruction of β-lactam antibiotics by β-lactamases and increase the spectrum of the antibiotic activity.
- Can be coadministered with β-lactamase-sensitive penicillins in order to treat β-lactamase-producing organisms
Examples
- Clavulanate (combined with amoxicillin)
- Avibactam (combined with ceftazidime)
- Sulbactam (combined with ampicillin)
- Tazobactam (combined with piperacillin)

CATS: Clavulanate, Avibactam, Tazobactam, Sulbactam are β-lactamase inhibitors.

Penicillins

Natural penicillins (prototype beta-lactam antibiotics)

Examples
- Penicillin G (benzylpenicillin)
  - IV: crystalline penicillin G
  - IM: procaine penicillin G, benzathine penicillin G
- Oral: penicillin V (phenoxymethylpenicillin)
Clinical use
- Gram-positive aerobes (esp. Streptococcus pyogenes, Streptococcus pneumoniae)
- Gram-negative cocci (esp. Neisseria meningitidis)
- Spirochetes (esp. Treponema pallidum)
- Branching gram-positive anaerobes (especially Actinomyces)
Adverse effects
- Hypersensitivity reactions
- Hemolytic anemia positive direct Coombs test
- Drug-induced interstitial nephritis
- Seizures ^[10]
Mechanisms of resistance
- Cleavage of the β-lactam ring by β-lactamases (penicillinases)
- PBP mutations

Penicillinase-resistant penicillins

Examples (oral or IV)
- Nafcillin
- Dicloxacillin
- Oxacillin
- Floxacillin
- Methicillin
Special characteristics: intrinsically β-lactamase resistant through the addition of bulky side chains (e.g., isoxazolyl), which prevent bacterial β-lactamase from hydrolyzing the β-lactam ring
Clinical use: narrow spectrum
- Gram-positive aerobes; , especially S. aureus (non-MRSA)
- Penicillinase-resistant penicillins are not effective against Streptococcus viridans, Enterococci, or Listeria.
Adverse effects
- Interstitial nephritis (esp. associated with methicillin use)
- Hypersensitivity reactions
Mechanism of resistance: alteration of PBP binding site; → reduced affinity → pathogen is not bound or inactivated by β-lactam (an altered PBP target site is one of the main virulence factors of MRSA)

Use NAF (nafcillin) for STAPH (S. aureus).

Aminopenicillins (penicillinase-sensitive penicillins)

Examples
- Oral or IV: amoxicillin (combined with clavulanate; )
- IV or IM: ampicillin (with or without sulbactam)
Special characteristics
- The molecular structure is similar to penicillin and therefore susceptible to degradation by β-lactamase (β-lactamase sensitive).
- Oral bioavailability of amoxicillin is greater than that of ampicillin
Clinical use: broader spectrum of activity than penicillin (extended-spectrum penicillin)
- Gram-positive aerobes
- Gram-negative rods (not effective against Enterobacter spp.)
- Most effective against:
Adverse effects
- Diarrhea
- Pseudomembranous colitis
- Hypersensitivity reactions
- Drug-induced rash
- Possibly acute interstitial nephritis
Mechanisms of resistance: cleavage of the β-lactam ring by penicillinases

AmOxicillin is administered Orally, while amPicillin is administered by a Prick!

Aminopenicillin therapy HHEELPSSS against H. influenzae, H. pylori, E. coli, Enterococci, Listeria monocytogenes, Proteus mirabilis, Salmonella, Shigella, Spirochetes.

Aminopenicillin-related exanthem in infectious mononucleosis

Antipseudomonal penicillins

Examples
- IV ureidopenicillins: piperacillin (combined with tazobactam) , mezlocillin
- IV carboxypenicillins (e.g., ticarcillin)
- PO carbenicillin
Clinical use: extended spectrum but penicillinase-sensitive
- Gram-negative rods, especially Pseudomonas
- Also effective against anaerobes (e.g., Bacteroides fragilis)
- Gram-positive aerobes: not effective against S. viridans
Adverse effects: hypersensitivity reactions

The PIPER in his CAR full of TICks ran over Pseudomonas: PIPERacillin, CARbenicillin, and TICarcillin are antipseudomonals.

Carbapenems

Examples
- IV imipenem (combined with cilastatin)
- IV meropenem
- IV ertapenem
- IV doripenem
Special characteristics
- Imipenem is always given with cilastatin, which inhibits human dehydropeptidase I (a renal tubular enzyme that breaks down imipenem).
- Meropenem is stable to dehydropeptidase I.
Clinical use
- Last-resort drugs (used only in life-threatening infections or after other antibiotics have failed) because of the significant adverse effects
- Broad-spectrum antibiotics with intrinsic beta-lactamase resistance
  - Gram-positive cocci; (except for MRSA and Enterococcus faecalis and Enterococcus faecium, which are intrinsically resistant)
  - Gram-negative rods, including Pseudomonas aeruginosa (except ertapenem which has limited activity against Pseudomonas)
  - Anaerobes
Adverse effects
- Secondary fungal infections ^[11]
- CNS toxicity: can lower seizure threshold at high serum concentrations
  - Highest risk: imipenem
  - Lowest risk: meropenem
- Gastrointestinal upset
- Rash
- Thrombophlebitis ^[12]
Mechanism of resistance: inactivation by carbapenemase
- A type of β-lactamase
- Produced by carbapenemase-producing Enterobacteriaceae (e.g., E. coli, K. pneumoniae, K. aerogenes)

Get a kill that is lastin' with imipenem plus cilastatin.

don't DIe on ME: Doripenem, lmipenem, Meropenem, and Ertapenem are carbapenems and used in life-threatening infections.

Monobactams

Examples: : IV aztreonam
Special characteristics:
- Specifically binds to PBP3: inhibits peptidoglycan cross-linking ^[13]
- Less susceptible to β-lactamases
Clinical use
- Effective against gram-negative bacteria only , including nosocomial Pseudomonas, H. influenzae, and N. meningitidis
- Not effective against gram-positive rods or anaerobes
- Alternative for penicillin-allergic patients (no cross-sensitivity with penicillins)
- Can be used as an alternative to aminoglycosides for patients with renal insufficiency because it is synergistic with aminoglycosides
- Broad-spectrum coverage in combination with vancomycin or clindamycin
Adverse effects: rare
- GI upset
- Injection reactions
- Rash

Cephalosporins

Overview of clinical use of cephalosporins
	1^st generation cephalosporins	2^nd generation cephalosporins	3^rd generation cephalosporins	4^th generation cephalosporins	5^th generation cephalosporins
Examples	Oral: cephalexin IV, IM: cefazolin	Oral: cefaclor, cefuroxime IV: cefuroxime, cefoxitin, cefotetan	Oral: cefixime, cefpodoxime, cefdinir IV: ceftriaxone, cefotaxime, ceftazidime IM: ceftriaxone	IV cefepime	IV ceftaroline
Microbial coverage
Activity against gram-positive bacteria	Highly active	Less active than 1^st generation	Least active among all cephalosporins	Highly active	Highly active
Gram-negative bacteria coverage	Proteus mirabilis E. coli Klebsiella pneumoniae	Proteus mirabilis E. coli Klebsiella pneumoniae H. influenzae Klebsiella aerogenes (previously known as Enterobacter aerogenes) Neisseria Serratia marcescens	Extended-spectrum	Extended-spectrum	Extended-spectrum
MRSA	No	No	No	No	Yes
Listeria	No	No	No	No	Yes
Pseudomonas	No	No	Yes (ceftazidime and cefoperazone)	Yes	No
Enterococcus	No	No	No	No	Yes (only E. faecalis)
Atypicals (Chlamydia, Mycoplasma, Legionella)	No	No	No	No	No
Special clinical considerations	Cefazolin for perioperative wound infection prophylaxis (covers S. aureus)	N/A	Perioperative wound infection (S. aureus) prophylaxis Ceftriaxone specifically Has good CNS penetrance: used to treat meningitis Also used for gonorrhea and disseminated Lyme disease	Used for severe life-threatening infections (including nosocomial)	N/A

Special characteristics: less susceptible to penicillinases
Adverse effects
- Potential cross-reactivity in patients with penicillin allergies (the rate is low even in patients with allergy to penicillin)
- Autoimmune hemolytic anemia (AIHA) ^[14]
- Vitamin K deficiency, which increases the risk of bleeding ^[15]^[16]
- Disulfiram-like reaction, especially when consumed with alcohol (flushing, tachycardia, hypotension)
- Increases nephrotoxic effect of aminoglycosides when administered together with cephalosporins
- Neurotoxicity (can lower seizure threshold) ^[17]
- In neonates: hyperbilirubinemia (ceftriaxone)
Mechanisms of resistance
- Inactivation by cephalosporinase (a type of β-lactamase)
- Change in transpeptidase (PBP) structure

1 PEcK: 1^st generation cephalosporins cover Proteus mirabilis, E. coli, Klebsiella pneumoniae.
2 HENS PEcK: 2^nd generation cephalosporins cover H. influenzae, Enterobacter aerogenes (now Klebsiella aerogenes), Neisseria, Serratia marcescens, Proteus mirabilis, E. coli, Klebsiella pneumoniae.

2^nd graders wear fake fox fur to tea parties: 2^nd generation cephalosporins include cefaclor, cefoxitin, cefuroxime, and cefotetan.

Cephalosporins are LAME: 1^st–4^th generation cephalosporins do not act against Listeria, Atypical organisms (e.g., Chlamydia, Mycoplasma), MRSA, and Enterococci (with the exception of ceftaroline, which does act against MRSA).

Glycopeptides

Examples
- Oral or IV vancomycin, teicoplanin
- Topical bacitracin
Mechanism of action
- Bind terminal D-ala-D-ala of cell-wall precursor peptides → inhibition of cell wall synthesis (peptidoglycan formation) → bacterial death (bactericidal effect against most gram-positive bacteria)
- Bacteriostatic against C. difficile
CNS penetration: only when there is increased permeability of the meningeal vessels (i.e., with meningeal inflammation)
Route of elimination: renal (via glomerular filtration)
Clinical use: especially effective against multidrug-resistant organisms
- Is effective against a wide range of gram-positive bacteria only
- MRSA
- S. epidermidis
- Enterococci (if not vancomycin resistant enterococci)
- C. difficile (causing pseudomembranous colitis): administered orally
Adverse effects
- Intravenous administration
  - Nephrotoxicity
  - Ototoxicity/vestibular toxicity
  - Thrombophlebitis
  - Vancomycin flushing reaction: an anaphylactoid reaction caused by rapid infusion of vancomycin
    - Nonspecific mast cell degranulation → rapid release of histamine
    - Symptoms
      - Diffuse flushing of the skin, pruritus mainly of the upper body
      - Muscle spasms and pain in the back and chest
      - Possible hypotension and dyspnea ^[18]
    - Can be prevented by slowing the rate of infusion and pretreating with antihistamines
  - DRESS syndrome ^[19]
  - Neutropenia ^[20]
  - Dysgeusia and gastrointestinal side effects (e.g., nausea, vomiting, abdominal pain)
- Oral administration: predominantly dysgeusia and gastrointestinal side effects
Contraindications: Consider use in pregnant women only if the benefits outweigh the risks. ^[21]
Mechanisms of resistance
- Modification of amino acid D-Ala-D-Ala to D-Ala-D-Lac: occurs mainly in Enterococcus (e.g., E. faecium, less in E. faecalis)
- Beta-lactamase resistant

The vancomycin van carries a TON of flashy DRESSes: the side effects of vancomycin are Thrombophlebitis, Ototoxicity, Nephrotoxicity, vancomycin flushing reaction, and DRESS syndrome.

The fine for VANdalism is one DALlAr in LACjac: VANcomycin resistance is caused by amino acid modification (D-Ala-D-Ala to D-Ala-D-Lac).

Vancomycin flushing reaction

Epoxides

Examples: : oral and IV fosfomycin
Mechanism of action: : inhibits enolpyruvate transferase (MurA) → no formation of N-acetylmuramic acid; (a component of bacterial cell wall) → inhibition of cell wall synthesis → cell death (bactericidal effect) ^[22]
Route of elimination: renal
Clinical use: : women with uncomplicated urinary tract infections (e.g., cystitis due to E. coli or E. faecalis) ^[3]^[23]
Adverse effects
- Mild electrolyte imbalances (e.g., hypernatremia, hypokalemia)
- Diarrhea ^[3]
Contraindications: hypersensitivity
Mechanisms of resistance: MurA mutations ^[24]

Lipopeptides

Examples: daptomycin
Mechanism of action: incorporate K⁺ channels into the cell membrane of gram-positive bacteria → rapid membrane depolarization; → loss of membrane potential → inhibition of synthesis of DNA, RNA, and proteins → cell death (bactericidal effect) ^[25]
Route of elimination: renal
Clinical use
- Gram-positive bacteria
- S. aureus, especially MRSA
- Mainly used in skin and skin structure infections, bacteremia, and endocarditis
- Vancomycin-resistant Enterococci (VRE)
- Not used in pneumonia (daptomycin is bound and inactivated by surfactant) ^[25]
Adverse effects
- Reversible myopathy
- Rhabdomyolysis
- Allergic pneumonitis ^[26]
Contraindications: hypersensitivity
Mechanisms of resistance: repulsion of daptomycin molecules due to the change in the bacterial surface charge ^[27]

Dap-to-my-cin is good to my skin: daptomycin is used to treat skin infections.

Polymyxins

Examples
- IV or IM polymyxin B
- IV or IM polymyxin E (colistin) ^[28]
Mechanism of action
- A cationic detergent (polypeptides) molecule that binds to phospholipids of the cytoplasmic membrane of gram-negative bacteria → increased membrane permeability→ leakage of cell contents → cell death (bactericidal effect)
- Binds to and inactivates endotoxins
CNS penetration: poor
Route of elimination: mostly renal
Clinical use: severe infections caused by multidrug-resistant gram-negative bacteria
- Effective only against gram-negative bacteria including P. aeruginosa, K. pneumoniae, E. coli, Acinetobacter baumannii, and Enterobacteriaceae spp.
- Not effective against gram-positive bacteria
- Topical antibiotics: triple antibiotic ointment; (bacitracin, neomycin, and polymyxin B) for superficial skin infections
- Oral polymyxin B may be used to disinfect the bowel to prevent ICU infections
Adverse effects
- Nephrotoxicity
- Neurotoxicity; (e.g., paresthesias, weakness, speech disorders, neuromuscular blockage)
- Urticaria, eosinophilia, and/or anaphylactoid reactions ^[29]
- Respiratory failure
Contraindications:
- Hypersensitivity to polymyxins
- Cautious use in patients with renal dysfunction

Aminoglycosides

Examples
- IV or IM gentamicin
- IV or IM amikacin
- IV or IM tobramycin
- IV or IM streptomycin
- Oral neomycin
- Capreomycin
- Kanamycin
Mechanism of action
- Bind to 30S subunit of the bacterial ribosome → irreversible inhibition of initiation complex → inhibition of bacterial protein synthesis → cell death (bactericidal effect)
- Misreading of mRNA
- Blockage of translocation
- Synergistic effect when combined with β-lactam antibiotics: β-lactams inhibit cell wall synthesis → facilitated entry of aminoglycoside drugs into the cytoplasm
CNS penetration: poor
Route of elimination: renal (via glomerular filtration)
Clinical use ^[30]
- Severe gram-negative rod infections
- Not effective against anaerobes (aminoglycosides require oxygen to be absorbed by cells)
- Neomycin, which is not absorbed systemically, is administered orally to prepare the gut for bowel surgery.
- Streptomycin is used as a second-line treatment for Mycobacterium tuberculosis and M. avium-intracellulare
Adverse effects
- Nephrotoxicity
- Ototoxicity and vestibulotoxicity (risk of ototoxicity is higher when used concurrently with loop diuretics) resulting in:
  - Tinnitus
  - Ataxia
  - Vertigo
- Neuromuscular blockade
- Teratogenicity
Contraindications
- Myasthenia gravis
- Botulism
- Pregnancy
- Cautious use in patients with renal dysfunction
Mechanisms of resistance: inactivation via acetylation, phosphorylation, and/or adenylation by secreted bacterial transferase enzymes

Me and my NEw AMIgA are taking GENeral STEPs to AMeliorate our TOBacco intake but are still unsuccessful: NEomycin, AMIkAcin, GENtamicin, STrEPtomycin AMinoglycosides, and TOBramycin are unsuccessful in killing anaerobes.

Ah, MI(y) NEPHew's OTter keeps TERrorizing our block: the side effects of AMInoglycosides include NEPHrotoxicity, OTotoxicity, TERatogenicity, and neuromuscular blockade.

Mechanisms of action of antibiotics on the bacterial ribosome

Tetracyclines

Examples
- Oral or IV minocycline
- Oral or IV tetracycline
- Oral doxycycline
- Oral demeclocycline
Mechanism of action: bind 30S subunit → aminoacyl-tRNA is blocked from binding to ribosome acceptor site → inhibition of bacterial protein synthesis (bacteriostatic effect)
CNS penetration: poor
Route of elimination
- Renal
- Doxycycline: only gastrointestinal elimination (doxycycline is the only tetracycline that is not contraindicated in patients with renal failure)
Clinical use
- Bacteria that lack a cell wall (e.g, Mycoplasma pneumoniae, Ureaplasma)
- Intracellular bacteria, such as Rickettsia, Chlamydia, or Anaplasma ; (tetracyclines accumulate intracellularly and are, therefore, effective against intracellular pathogens)
- Borrelia burgdorferi
- Other: Ehrlichia, Vibrio cholerae, Francisella tularensis
- Cutibacterium acnes (topical tetracycline is used to treat acne) ^[31]
- Community-acquired MRSA (doxycycline)
Special considerations
- Oral tetracyclines should not be taken with substances that contain large amounts of Ca²⁺, Mg²⁺, or Fe²⁺ (e.g., milk, antacids, iron supplements, respectively) because divalent cations inhibit the intestinal absorption of tetracyclines.
- CNS penetration is limited
Adverse effects
- Hepatotoxicity
- Deposition in bones and teeth; → inhibition of bone growth (in children) and discoloration of teeth
- Damage to mucous membranes (e.g., esophagitis, GI upset)
- Photosensitivity: drug or metabolite in the skin absorbs UV radiation → photochemical reaction → formation of free radicals → damage to cellular components → inflammation (sunburn-like) ^[32]
- Degraded tetracyclines are associated with Fanconi syndrome. ^[33]
- Rarely: pseudotumor cerebri ^[34]
Contraindications
- Children < 8 years of age (except doxycycline) ^[35]
- Pregnant women
- Breastfeeding women
- Patients with renal failure (except doxycycline)
- Cautious use in patients with hepatic dysfunction
Mechanisms of resistance: Plasmid-encoded transport pumps increase efflux out of the bacterial cell and decrease uptake of tetracyclines.

Teethracyclines: teeth discoloration is a side effect of tetracyclines.

Glycylcyclines

Examples: tigecycline
Mechanism of action ^[36]
- Tetracycline derivate ^[4]
- Bind to 30S subunit ; → blockage of entry of amino-acyl tRNA into ribosomal A site → inhibition of protein synthesis (bacteriostatic effect) ^[4]
CNS penetration: poor
Route of elimination: mostly biliary
Clinical use
- Gram-positive aerobes (not effective against S. viridans or Enterococci; limited efficacy against MSSA)
- MRSA
- VRE
- Anaerobes (broad spectrum)
- Partially effective against gram-negative aerobes (no effect against Proteus species)
- Gram-intermediate bacteria: Borrelia, Mycoplasma, Rickettsia, Chlamydia ^[37]^[38]
Special considerations
- Good soft tissue penetration: effective for treating deep tissue infections
- Glycylcyclines should not be taken with milk, antacids, or iron supplements because divalent cations inhibit the absorption of glycylcyclines in the intestines.
Adverse effects ^[4]
- GI upset (nausea, vomiting)
- Hepatotoxicity
- Deposition in bones and teeth
- Photosensitivity
Contraindications ^[39]
- Children < 8 years of age
- Pregnant women
- Breastfeeding women
- Cautious use in patients with hepatic dysfunction

Macrolides

Examples
- Oral or IV: erythromycin, azithromycin, clarithromycin
- Oral: Roxithromycin
Mechanism of action: bind to 23S ribosomal RNA molecule of the 50S subunit → blockage of translocation → inhibition of bacterial protein synthesis; (bacteriostatic effect)
CNS penetration: poor
Route of elimination: biliary
Clinical use
- Atypical pneumonia caused by:
- Bordetella pertussis
- STIs caused by Chlamydia
- Gram-positive cocci especially for the treatment of streptococcal infection in patients who are allergic to penicillin)
- Neisseria spp.
  - Second-line prophylaxis for N. meningitidis
  - Dual therapy with ceftriaxone for N. gonorrhoeae (azithromycin)
- Mycobacterium avium
  - Prophylaxis: azithromycin
  - Treatment: azithromycin, clarithromycin
- H. pylori (clarithromycin is the part of triple therapy )
- Ureaplasma urealyticum
- Babesia spp. (azithromycin in combination with atovaquone)
Adverse effects
- Increased intestinal motility → GI upset
- QT-interval prolongation; , arrhythmia
- Acute cholestatic hepatitis
- Eosinophilia
- Rash
- Increased risk of hypertrophic pyloric stenosis (erythromycin and azithromycin) in infants up to 6 weeks of age ^[40]
Drug interactions
- Erythromycin enhances the effect of oral anticoagulants (e.g., warfarin).
- Erythromycin and clarithromycin
  - Increased theophylline serum concentrations ^[41]
  - CYP3A4 inhibition (cytochrome P450 inhibitors)
Special considerations
- All macrolides (except azithromycin) have a short half-life.
- Erythromycin is used off-label for the treatment of gastroparesis because it increases GI motility.
Contraindications ^[42]^[43]^[44]
- Erythromycin estolate and clarithromycin are contraindicated in pregnant women (potentially hazardous to the fetus)
  - Erythromycin estolate use in pregnant women during the first trimester is associated with an increased risk of hepatic failure in the women.
  - All the other forms of erythromycin (e.g., ethyl succinate, stearate, etc.) can be safely used.
- Azithromycin and clarithromycin are contraindicated in patients with hepatic failure (erythromycin should be used cautiously).
- Consider use of erythromycin in children < 12 years of age only if benefits outweigh the risks, as safety in this population has not been established.
- Consider use of clarithromycin and azithromycin in children < 6 months of age only if benefits outweigh the risks, as safety in this population has not been established.
- Cautious use in breastfeeding women
- Cautious use of clarithromycin in patients with renal failure
Mechanisms of resistance: Methylation of the binding site of 23S rRNA prevents the macrolide from binding to rRNA.

Macroslides: macrolides inhibit translocation during protein synthesis, in which ribosomes slide along mRNA.

The adverse effects of MACROlides include gastrointestinal Motility issues, Arrhythmia (due to prolonged QT interval), acute Cholestatic hepatitis, Rash, and eOsinophilia.

Lincosamides

Examples: clindamycin
Mechanism of action: binds to 50S subunit → blockage of peptide translocation (transpeptidation) → inhibition of peptide chain elongation →inhibition of bacterial protein synthesis (bacteriostatic effect)
CNS penetration: poor
Route of elimination: both renal and biliary
Clinical use
- Anaerobes, such as Clostridium perfringens, Bacteroides spp. (clindamycin is less effective against Bacteroides than other anaerobic species)
  - Aspiration pneumonia
  - Lung abscesses
  - Oral infections
- Group A streptococcus: especially invasive infections
- Partially effective against gram-positive aerobes
  - Can be used in MRSA infections
  - Not effective against Enterococci
- Babesia (together with quinine) ^[45]
Special considerations: cross-resistance with macrolides
Adverse effects
- GI upset (e.g., diarrhea)
- Pseudomembranous colitis
- Fever
- Teratogenicity ^[46]
Contraindications: cautious use in pregnant patients during the 1^st trimester and in breastfeeding patients ^[47]

Learn Clindamycin Faster with Picmonic (USMLE, Step 1, Step 2 CK)

Streptogramin

Examples: IV quinupristin-dalfopristin
Mechanism of action ^[48]
- Synergistic effect
  - Dalfopristin
    - Inhibits the early phase of protein synthesis
    - Binds to 23S portion of 50S subunit → change of conformation → enhanced binding of quinupristin
    - Inhibits peptidyl transferase
  - Quinupristin
    - Inhibits the late phase of protein synthesis
    - Binds to 50S subunit → elongation of polypeptide is prevented → release of incomplete chains ^[5]
- Bacteriostatic when used separately, but bactericidal when used in combination ^[49]
Route of elimination: biliary and renal ^[50]
Clinical use
- Skin and skin structure infection with:
  - S. aureus (methicillin-susceptible and resistant)
  - S. pyogenes
  - Vancomycin-resistant E. faecium
- Not effective against E. faecalis ^[5]^[51]^[52]
Special considerations: inhibits CYP3A4 ^[52]
Adverse effects
- Nausea, vomiting
- Diarrhea
- Headache
- Arthralgia, myalgia
- Thrombophlebitis
- Rash, pruritus
- Pseudomembranous colitis
Contraindications: consider use in the following populations only if benefits outweigh the risks, as safety in these has not been established ^[52]
- Pregnant and/or breastfeeding women
- Children < 16 years of age
Mechanisms of resistance
- Modification of bacterial ribosome binding site
- Enzyme-mediated methylation
- Efflux pumps ^[50]

Oxazolidinones

Examples: linezolid
Mechanism of action
- Binds to 50S subunit of bacterial ribosome; → inhibition of initiation complex formation → inhibition of bacterial protein synthesis (bacteriostatic effect)
- Nonselective monoamine oxidase inhibition (MAOI) ^[53]
- Bactericidal against streptococci
CNS penetration: good
Route of elimination: both biliary and renal elimination after hepatic metabolism
Clinical use: multidrug-resistant gram-positive bacteria (VRE, MRSA)
Adverse effects
- GI upset
- Pancytopenia (especially thrombocytopenia) due to bone marrow suppression
- Peripheral neuropathy
- Serotonin syndrome: Linezolid partially inhibits monoamine oxidase, which is responsible for the break down of neurotransmitters like serotonin.
Contraindications
- Concurrent use with MAOIs and selective serotonin reuptake inhibitors (SSRIs)
- Consider use in pregnant women only if benefits outweigh the risks, as safety in this population has not been established.
Mechanism of resistance: point mutation of 23S rRNA ^[54]

Amphenicols

Examples: chloramphenicol
Mechanism of action: bind 50S subunit → blockage of peptidyltransferase → inhibition of bacterial protein synthesis (bacteriostatic effect) ^[55]
CNS penetration: good
Route of elimination: renal elimination after hepatic metabolism
Clinical use
- Meningitis caused by H. influenzae, N. meningitidis, and/or S. pneumoniae
- Rickettsia infections (e.g., Rocky Mountain spotted fever caused by Rickettsia rickettsii)
Special considerations
- Potent inhibitory effect on cytochrome P450 isoforms CYP2C19 and CYP3A4 ^[55]
- Rare in the US due to adverse effects
- Most commonly used in resource-limited countries due to low drug costs
Adverse effects
- Dose-dependent bone marrow suppression: aplastic anemia, leukopenia, and/or thrombocytopenia
- Gray baby syndrome
  - Occurs mainly in premature infants because of develomental lack of UDP-glucuronyltransferase
  - Symptoms: cyanosis, vomiting, flaccidity, hypothermia, shock
Contraindications
- Infancy
- Pregnancy
- Cautious use in patients with renal and/or hepatic dysfunction
Mechanisms of resistance: drug inactivation via plasmid-encoded acetyltransferase

Fluoroquinolones

Examples
- 1^st generation: nalidixic acid (oral)
- 2^nd generation: norfloxacin, ciprofloxacin, ofloxacin; (oral), enoxacin (oral or IV)
- 3^rd generation: levofloxacin (oral or IV)
- 4^th generation: moxifloxacin, gemifloxacin, gatifloxacin (oral)
- Levofloxacin, moxifloxacin, and gemifloxacin are respiratory fluoroquinolones.
Mechanism of action: inhibition of prokaryotic topoisomerase II (DNA gyrase) and topoisomerase IV; → DNA supercoiling → formation of double-stranded breaks → inhibition of DNA replication and transcription (bactericidal effect) ^[56]
CNS penetration: good ^[57]
Route of elimination
- Primarily renal (via glomerular filtration and tubular secretion)
- Moxifloxacin undergoes biliary excretion.
- Absorption is reduced when coadministered with polyvalent cations (e.g., magnesium, calcium, iron).
Clinical use
- Norfloxacin, ciprofloxacin, and ofloxacin
  - Gram-negative rods causing urinary and gastrointestinal infections
  - Some gram-positive pathogens
  - Genitourinary infections caused by Neisseria gonorrhoeae, Chlamydia trachomatis, and/or Ureaplasma urealyticum
  - Ciprofloxacin: Pseudomonas aeruginosa (e.g., malignant otitis externa)
- Levofloxacin, moxifloxacin, and gemifloxacin:
  - Atypical bacteria (e.g., Legionella spp., Mycoplasma spp., Chlamydophila pneumoniae)
  - Also effective against anaerobes
  - Gemifloxacin is highly potent against penicillin-resistant pneumococci.
  - Moxifloxacin: 2nd-line treatment of tuberculosis in patients who cannot tolerate antitubercular drugs and in multidrug resistant tuberculosis
Adverse effects
- GI upset
- Neurological symptoms
  - Mild headache
  - Dizziness
  - Mood changes
  - Peripheral neuropathy
  - Can lower seizure threshold (increased risk in patients taking NSAIDs and those with a previous history of epilepsy)
- Hyperglycemia/hypoglycemia
- QT prolongation
- Photosensitivity
- Skin rash
- Superinfection (most commonly with gram-positive pathogens) ^[58]^[59]
- Potentially life-threatening exacerbations in patients with myasthenia gravis ^[60]
- In children: potential damage to growing cartilage → reversible arthropathy
- Muscle ache, leg cramps, tendinitis, tendon rupture, especially of the Achilles tendon (the risk of tendon rupture is higher for individuals over 60 years of age and for individuals on steroid therapy)
Special considerations: : increased risk for drug interactions as ciprofloxacin inhibits cytochrome P450
Contraindications
- Children and teenagers < 18 years of age
- Patients > 60 years of age and those taking cortisol
- Pregnant women
- Breastfeeding women
- Epilepsy, stroke, CNS lesions/inflammation
- QT prolongation
- Myasthenia gravis
- Cautious use in patients with:
  - Renal failure
  - Hepatic failure
  - Antacid use ^[61]
  - Known aortic aneurysm or increased risk of aneurysms (e.g., Marfan syndrome, Ehlers-Danlos syndrome, advanced age, peripheral atherosclerotic disease, hypertension)
Mechanism of resistance
- Chromosome-encoded mutation in DNA gyrase and topoisomerase IV enzymes
- Altered cell wall permeability
- Plasmid-encoded mutations in efflux pump proteins

Fluoroquinolones hurt the attachments to your bones.

Nitroimidazoles

Examples
- Oral or IV metronidazole
- Oral or IV tinidazole
Mechanism of action: creates free radicals within the bacterial cell → DNA-strand breaks; → cell death (bactericidal and antiprotozoal effect)
CNS penetration: good
Route of elimination: renal
Clinical use
- Certain protozoa (e.g., Entamoeba histolytica, Giardia, Trichomonas)
- Anaerobes(e.g., C. difficile, Bacteroides spp.) ^[62]
- Facultative anaerobes
  - Gardnerella vaginalis
  - Helicobacter pylori in place of amoxicillin (e.g., in case of penicillin allergy) as part of a triple therapy regimen
- Not effective against aerobes
Adverse effects
- Headache ^[63]
- Disulfiram-like reaction: Nitroimidazoles are no longer believed to cause disulfiram-like reactions. ^[47]
  - Despite case reports suggesting that concomitant metronidazole and alcohol intake can trigger a disulfiram-like reaction, evidence of an association is lacking. ^[47]
  - Metronidazole does not inhibit acetaldehyde dehydrogenase and therefore does not increase blood acetaldehyde concentrations. ^[64]
  - Possible explanations behind the reaction involve metronidazole-induced changes in the gut flora and histamine reactions. ^[64]
- Metallic taste
- Peripheral neuropathy; (particularly with prolonged use), vestibular dysfunction
Contraindications
- Consider use in the following populations, if benefits outweigh the risks, as safety in this populations has not been established.
  - Breastfeeding women ^[65]
  - Pregnant women
  - Children
- Cautious use in patients with hepatic dysfunction

Take the Metro To lonG BEaCH: Metronidazole treats Trichomonas, Giardia/Gardnerella, Bacteroides, Entamoeba, Clostridium, and H. pylori.

Sulfonamides and diaminopyrimidine

Drug classes
- Diaminopyrimidine derivatives: trimethoprim (TMP), pyrimethamine
- Sulfonamides
  - Antibiotics: sulfamethoxazole (SMX), sulfadiazine, sulfisoxazole
  - Nonantibiotic sulfonamides
    - Diuretics: thiazides, furosemide, acetazolamide
    - Anti-inflammatory drugs: sulfasalazine, celecoxib
    - Sulfonylureas
    - Probenecid
Examples
- Oral or IV cotrimoxazole (TMP/SMX)
- Oral sulfadiazine in combination with pyrimethamine
- Oral sulfisoxazole
Mechanism of action
- Inhibition of bacterial folic acid synthesis
  - Sulfonamides inhibit dihydropteroate synthase.
  - Diaminopyrimidine derivatives inhibit dihydrofolate reductase (DHFR).
    - DHFR uses NADPH to reduce dihydrofolic acid to tetrahydrofolic acid (THF).
    - THF can be converted to methylene-THF.
    - Methylene-THF is an important cofactor for thymidylate synthetase, which catalyzes the conversion of deoxyuridine monophosphate (dUMP) to deoxythymidine monophosphate (dTMP).
- Both are bacteriostatic but become bactericidal when combined (sequential block of folate synthesis)
CNS penetration: good
Route of elimination: primarily renal (via tubular secretion)
Clinical use: Common indications include UTIs and acute otitis media.
- Sulfisoxazole
  - Gram-positive bacteria and gram-negative bacteria
  - N. meningitidis
  - Chlamydia trachomatis
  - Nocardia asteroides
  - Toxoplasma gondii
  - Plasmodia spp. ^[66]
- TMP/SMX
  - Shigella
  - Salmonella
  - Empiric treatment for simple UTI
  - Prophylaxis and treatment of P. jirovecii
  - Prophylaxis of toxoplasmosis
Adverse effects of sulfonamides
- Drug interactions due to CYP450 inhibition
- Displacement of other drugs (e.g., warfarin) from albumin
- Kernicterus in infancy
- Nephrotoxicity (especially acute tubulointerstitial nephritis) ^[67]
- GI upset
- Hyperkalemia ^[68]
- Agranulocytosis
- Aplastic anemia, thrombocytopenia, and pancytopenia ^[69]
- Triggers hemolytic anemia in G6PD-deficient patients
- Stevens-Johnson syndrome
- Hypersensitivity reactions (especially urticaria and hives) ^[70]
- Photosensitivity
- Fever
Adverse effects of diaminopyrimidine derivatives
- Megaloblastic anemia
- Leukopenia, granulocytopenia (can be prevented with concomitant administration of folinic acid)
- Hyperkalemia
  - Caused by competitive inhibition of ENaC channels in the distal convoluted tubule → ↓ Na⁺reabsorption → ↓ K⁺secretion ^[71]
  - Patients with HIV are commonly affected because they often take higher doses of trimethoprim. ^[68]
- Increased creatinine ^[71]
  - Caused by decreased tubular secretion
  - GFR is unchanged.
Contraindications
- Pregnant women
- Children < 2 months of age
- Breastfeeding women
- Cautious use in people with
  - Hepatic failure
  - Renal failure
Mechanisms of resistance
- Sulfonamides
  - Mutation in bacterial dihydropteroate synthase
  - Decreased uptake of sulfonamide
  - Increased para-aminobenzoate (PABA) synthesis

TMP Treats Marrow Poorly.

ROCk, PAper, SCiSSors: the most important sulfa drugs are fuROsemide, (hydro)Chlorthalidone, Probenecid, Acetazolamide, Sulfamethoxazole/Sulfadiazine, Celecoxib, Sulfasalazine, and Sulfonylureas).

Antibiotics interfering with folate/tetrahydrofolate synthesis

Nitrofurans

Examples: nitrofurantoin
Mechanism of action: : reduced by bacterial nitroreductases to reactive metabolites → bind to bacterial ribosomes → impaired metabolism, impaired synthesis of protein, DNA, and RNA → cell death (bactericidal effect)^[7]^[8]
Route of elimination: : primarily renal , small amounts in feces
Clinical use
- Urinary tract pathogens
  - Gram-positive: Enterococci, Staphylococcus saprophyticus, group B streptococcus, Staphylococcus aureus, Staphylococcus epidermidis
  - Gram-negative: E. coli, Enterobacter spp., Shigella spp., Salmonella spp., Citrobacter spp, Neisseria spp, Bacteroides spp., Klebsiella spp.
- Not effective against Pseudomonas and/or Proteus
- Clinical indications include:
  - Treatment and prophylaxis of acute uncomplicated UTIs (e.g., urethritis, cystitis)
  - Asymptomatic bacteriuria or symptomatic UTI in pregnant women
  - Should not be used in (suspected) pyelonephritis because nitrofurantoin does not achieve adequate concentration in renal tissue
Adverse effects
- Nitrofurantoin-induced lung disease (NILD) ^[72]
  - Types
    - Acute NILD: a hypersensitivity reaction that usually occurs approximately nine days after the first exposure
    - Chronic NILD: a cell-mediated or toxic reaction that usually occurs ∼ 6 months after initiation of the drug
  - Clinical features
    - Acute NILD: fever, dyspnea, cough, and rash
    - Chronic NILD: manifests gradually with cough and dyspnea and can lead to permanent pulmonary fibrosis
  - Diagnostics
    - Presence of characteristic clinical and diagnostic features with nitrofurantoin exposure
    - Chest x-ray: reticular shadowing, bilateral alveolar or interstitial infiltrates, pleural effusion
    - PFT: restrictive pattern, ↓ DLCO
    - Eosinophilia may be present in serum or bronchoalveolar lavage sample.
  - Differential diagnoses: heart failure, infection, and ARDS
  - Treatment: cessation of nitrofurantoin
- Pulmonary fibrosis (see “Chronic NILD”)
- Hemolytic anemia in patients with G6PD deficiency
- GI upset
- Reversible peripheral neuropathy
Contraindications
- Children < 1 month of age
- Breastfeeding women
- Women at 38–42 weeks' gestation or during delivery
- Hepatic dysfunction ^[73]
- Renal dysfunction with a creatinine clearance < 60 mL/min

Antimycobacterial drugs

See “Treatment” in “Tuberculosis.”

Mechanism of action: antimycobacterial drugs

Rifamycins

Examples
- Oral or IV rifampin (rifampicin)
- Oral rifabutin
- Oral rifaximin
- Oral rifapentine
Mechanism of action: inhibits bacterial DNA-dependent RNA-polymerase → prevention of transcription (mRNA synthesis) → inhibition of bacterial protein synthesis → cell death (bactericidal effect)
Route of elimination: biliary
Clinical use ^[36]
- Mycobacteria
  - Tuberculosis (together with isoniazid, pyrazinamide, and ethambutol)
  - Leprosy
    - Long-term treatment of tuberculoid form: dapsone and rifampin (rifampin delays resistance to dapsone)
    - Long-term treatment of lepromatous form: combination of dapsone, clofazimine, and rifampin
  - M. avium-intracellulare prophylaxis and treatment (rifabutin)
- Meningococcal prophylaxis
- Chemoprophylaxis for people who had contact with children infected with H. influenzae type b
- Rifaximin: second-line therapy in hepatic encephalopathy. ^[74]
Adverse effects
- Harmless red-orange discoloration of body fluids (e.g., urine, tears)
- Flu-like symptoms (fever, arthralgia; in severe cases hemolytic anemia, thrombocytopenia, and renal failure)
- Minor hepatotoxicity
- Cytochrome P450 induction (CYP3A4, CYP2C9)
  - Causes minor drug interactions
  - Rifabutin is preferred for the treatment of mycobacterial infections in patients with HIV because it has a lower potential for CYP induction than rifampin.
- Intermittent therapy is associated with an increased risk of renal failure, so rifamycins should be administered daily ^[75]
- False positive urine opiate screening ^[76]
Contraindications
- Breastfeeding women
- Should be used during pregnancy only if clearly needed
- Cautious use in patients with hepatic dysfunction
Mechanisms of resistance
- RNA polymerase mutations decrease the affinity of rifamycins to RNA polymerase. ^[77]
- Resistance develops rapidly if used as monotherapy.

The 6Rs of Rifampin: Red or orange urine, RNA polymerase Repression, Ramping up of cytochrome P450 activity, and Rapid Resistance development if used alone.

Rifampin really amplifies (induces) cytochrome P450, but rifabutin does not.

Isoniazid (INH)

Mechanism of action
- Isoniazid is a prodrug and needs to be converted into its active metabolite by bacterial catalase-peroxidase (encoded by KatG).
- Prevents cell wall synthesis by inhibiting the synthesis of mycolic acid
CNS penetration: variable
Metabolization: primarily hepatic
- INH is converted into various metabolites (e.g., via acetylation), some of which are hepatotoxic (e.g., hydrazine, acetylhydrazine).
- Main metabolic enzyme: N-acetyltransferase (NAT): involved in metabolite formation and subsequent neutralization
- The rate of NAT acetylation is genetically determined.
  - Individuals with slow acetylation: higher half-life due to lack of hepatic NAT → increased risk of drug-induced toxicity
  - Individuals with fast acetylation: lower half-life of active drug → administration of a higher dose is required for reaching the same blood concentration compared to individuals with slow acetylation ^[78]^[79]
- Inhibits cytochrome P450 isoforms (CYP1A2, CYP2A6, CYP2C19, and CYP3A4) ^[79]
Route of elimination: renal elimination after hepatic metabolism
Clinical use: ^[80]
- Treatment of TB (together with rifampin, pyrazinamide, and ethambutol)
- The only drug that can be used as monoprophylaxis against TB
Adverse effects
- Hepatotoxicity (drug-induced hepatitis)
- Anion gap metabolic acidosis
- Drug-induced lupus erythematosus
- High doses of INH can precipitate benzodiazepine-refractory seizures
- Vitamin B₆ deficiency: INH should be administered with pyridoxine to avoid vitamin B₆ deficiency.
  - Peripheral neuropathy due to S-adenosylmethionine accumulation
  - Sideroblastic anemia, aplastic anemia, thrombocytopenia
  - Pellagra
Contraindications
- Should be used during pregnancy only if clearly needed
- Cautious use in patients with renal and/or hepatic dysfunction
Mechanisms of resistance: mutations causing decreased KatG; → decreased expression of catalase-peroxidase → less/no biologically active INH

INH Is Not Healthy In Neurons and Hepatocytes.

Neurotoxicity may be prevented by supplementing with pyridoxine (vitamin B6).

Pyrazinamide

Mechanism of action
- Not completely understood
  - Prodrug: converted into active form pyrazinoic acid
  - Most effective at acidic pH (e.g., in acidic phagolysosomes)
- Bactericidal effect
CNS penetration: only when meninges are inflamed
Route of elimination: renal elimination after hepatic metabolism
Clinical use: M. tuberculosis
Adverse effects
- Hyperuricemia
- Hepatotoxicity
Contraindications
- Consider use in pregnant and breastfeeding women only if benefits outweigh the risks ^[81]
- Hepatic failure ^[82]
- Acute gout
Mechanisms of resistance: mutations in RpsA gene coding for ribosomal protein S1 ^[83]

Ethambutol

Mechanism of action: inhibits arabinosyltransferase → ↓ carbohydrate polymerization → prevention of mycobacterial cell wall synthesis (bacteriostatic effect)
CNS penetration: only when meninges are inflamed
Route of elimination: primarily renal
Clinical use
- M. tuberculosis therapy (together with isoniazid, rifampin, and pyrazinamide)
- M. avium-intracellulare treatment
  - Together with azithromycin or clarithromycin
  - Ciprofloxacin or rifabutin can be added
Adverse effects
- Optic neuropathy with decreased visual acuity and red-green color blindness which may result in irreversible blindness
- Resistance develops rapidly if used as monotherapy
- Hyperuricemia ^[84]
Contraindications
- Contraindicated in patients who are unable to report visual changes
- Contraindicated in patients with optic neuritis
- Consider use in the following populations only if benefits outweigh the risks, as safety in these has not been established
  - Children < 13 years of age
  - Pregnant women
  - Breastfeeding women ^[85]
Mechanisms of resistance: mutations of EmbCAB gene coding for arabinosyltransferase ^[86]

EYEthambutol: Ethambutol causes optic neuropathy.

Dapsone

Mechanism of action
- Competitive antagonist of para-aminobenzoic acid (PABA) for dihydropteroate synthetase → inhibition of dihydrofolic acid synthesis
- Bacteriostatic and weakly bactericidal effect ^[87]
- Structurally different from sulfonamides but a similar mechanism of action
Route of elimination: mostly renal
Clinical use
- M. leprae: lepromatous and tuberculoid leprosy ^[87]
- P. jiroveci pneumonia
  - Prophylaxis
  - Treatment: used in combination with TMP as an alternative to TMP/SMX
- Dermatitis herpetiformis ^[88]
- Alternative to the combination of sulfadiazine and pyrimethamine for toxoplasmosis
- In combination with pyrimethamine as an alternative for chloroquine-resistant malaria
Adverse effects
- Methemoglobinemia
- Triggers hemolytic anemia in patients with G6PD deficiency
- Agranulocytosis
- GI upset
- Peripheral neuropathy
Contraindications
- G6PD deficiency
- Consider use in pregnant and breastfeeding women only if benefits outweigh the risks
- Cautious use in patients with renal and/or hepatic dysfunction
Mechanism of resistance: mutations of folP1 gene coding for dihydropteroate synthase ^[89]

Antibiotics interfering with folate/tetrahydrofolate synthesis

Contraindications

	Absolute contraindication	Relative contraindication	Safe to use
Children	Tetracyclines: < 8 years old (except doxycycline) Glycylcyclines: < 8 years old Chloramphenicol Fluoroquinolones Sulfonamides and diaminopyrimidines: < 2 years old Nitrofurans: < 1 month old Ethambutol: young children who are unable to report visual changes	Polymyxin: < 2 years old Streptogramin: < 16 years old Nitroimidazole Ethambutol: < 13 years old Macrolides Erythromycin: < 12 years old Clarithromycin and azithromycin: < 6 months old	β-lactams Epoxide Lipopeptide Glycopeptide Aminoglycosides Lincosamides Oxazolidinones Rifamycins Isoniazid Pyrazinamide Dapsone
Pregnant women	Aminoglycosides Tetracyclines Glycylcyclines Chloramphenicol Fluoroquinolones Sulfonamides with diaminopyrimidines Macrolides (clarithromycin and erythromycin estolate )	Lincosamides: 1^st trimester Oxazolidinones Nitrofurans Rifamycins Isoniazid Pyrazinamide Ethambutol Dapsone Glycopeptide Polymyxin Streptogramin Nitroimidazole	β-lactams Epoxide Lipopeptide Macrolides (azithromycin and erythromycin )
Breastfeeding women	Aminoglycosides Tetracyclines Glycylcyclines Lincosamides Chloramphenicol Fluoroquinolones Sulfonamides with diaminopyrimidines Nitrofurans Rifamycins	Macrolides Oxazolidinones Nitroimidazole Pyrazinamide Ethambutol Dapsone Glycopeptide Epoxide Streptogramin	β-lactams Lipopeptide Polymyxin Isoniazid
Individuals with renal failure	Epoxides Aminoglycosides Tetracyclines Sulfonamides with diaminopyrimidines Nitrofurans	Polymyxin Chloramphenicol Fluoroquinolones Isoniazid Dapsone Macrolides (clarithromycin)	β-lactams Glycopeptide Lipopeptide Lincosamides Streptogramin Oxazolidinones Nitroimidazole Rifamycins Pyrazinamide Ethambutol Macrolides (erythromycin and azithromycin)
Individuals with hepatic failure	Tetracyclines Macrolides (azithromycin and clarithromycin) Sulfonamides with diaminopyrimidines Nitrofurans Pyrazinamide	Glycylcyclines Macrolides (erythromycin) Chloramphenicol Fluoroquinolones Nitroimidazole Rifamycins Isoniazid Dapsone	β-lactams Glycopeptide Epoxide Lipopeptide Polymyxin Aminoglycosides Lincosamides Streptogramin Oxazolidinones Ethambutol

For SaFe Children, these Tablets are Contraindicated: Sulfonamides, Fluoroquinolones, Clarithromycin, Tetracyclines, and Chloramphenicol are contraindicated in children.

Cut the Tablets for your Child's SAFety: Chloramphenicol, Tetracyclines, Clarithromycin, Sulfonamides, Aminoglycosides, and Fluoroquinolones are contraindicated in pregnancy.

We list the most important contraindications. The selection is not exhaustive.

Additional considerations

Empiric antibiotic therapy

Empiric antibiotic therapy covers the most probable causative organism(s) before the pattern of resistance and/or causative organism are known.

Indications

A bacterial infection that is potentially life-threatening (e.g., meningitis, sepsis) and/or may result in severe morbidity (e.g., septic arthritis) if treatment is delayed until the causative organism is definitively identified.
Infections that are commonly treated empirically
- Brain: meningitis, brain abscess
- Lung: pneumonia, lung abscess
- Skin: cellulitis, necrotizing fasciitis, surgical site infections
- Bones and/or joints: osteomyelitis, septic arthritis
- Respiratory tract: bacterial rhinosinusitis, tonsillitis, pharyngitis
- Heart: infective endocarditis
- GI tract: dysentery, spontaneous bacterial peritonitis
- Kidney and genital region: urinary tract infections (e.g., pyelonephritis, prostatitis, genital discharge)
- Any cause of sepsis

Choosing empiric antibiotic therapy

Target the most probable causative organism(s) but consider factors which might affect the success of usage of the chosen agent:

Host factors
- Circumstances of infection
  - Community-acquired vs. nosocomial infection
  - If nosocomial: general ward vs. intensive care unit
  - Geographical location
  - Differences among individual hospitals
- Site of infection
  - Specific infections are more commonly caused by certain organisms (e.g., UTIs are most commonly caused by E. coli
  - Certain sites are difficult to reach by antibiotics and require the use of higher/more frequent doses, longer duration of therapy, combinations of antibiotics, and/or the use of antibiotics that cross the blood-brain barrier.
    - Meningitis/encephalitis: blood-brain barrier
    - Chronic prostatitis, intraocular infections: nonfenestrated capillaries
    - Abscesses: thick walls, acidic pH, hydrolyzing enzymes within the abscess cavity
    - Infective endocarditis: poor penetration within vegetations
    - Osteomyelitis: avascular sequestrum
- Relative contraindications (see “Contraindications” above)
  - Children, pregnant women, breastfeeding women
  - Individuals with pre-existing illnesses and/or comorbidities
    - Allergies
    - Immunosuppression
- Previous antibiotic therapy
Drug factors
- Route of administration
- Antibiotic toxicity
- Drug interactions
- Cost of the antibiotic

Other guiding principles

Escalation of antibiotic therapy
- Increasing the spectrum of antibiotic therapy coverage when clinical symptoms do not improve and/or if the causative pathogen persists
- Broad-spectrum antibiotics are effective against both gram-positive bacteria and gram-negative bacteria.
- Examples include:
  - Aminopenicillins with β-lactamase inhibitors
  - Antipseudomonal penicillins
  - Carbapenems
  - 3^rd, 4^th, and 5^th generation cephalosporins
  - 3^rd and 4^th generation fluoroquinolones
  - Tetracyclines
  - Macrolides
  - Chloramphenicol
De-escalation of antibiotic therapy: A more specific narrow-spectrum antibiotic regimen is initiated after the causative organism, as well as its patterns of resistance and sensitivity, are known.

Blood cultures should be taken before initiating empiric antibiotic therapy.

Targeted antibiotic therapy

Targeted antibiotic therapy is chosen based on the results of culture and antibacterial sensitivity testing.
Aims to decrease the risk of treatment toxicity, prevent the development of antimicrobial resistance, and reduce the cost of the treatment
Usually employs narrow-spectrum agents to maximize efficacy and reduce the risk of side effects

Antibiotic prophylaxis

Antibiotics are commonly used for prophylaxis against infections in the following situations:
- Immunocompromised patients (e.g., HIV, immunosupression, neutropenia)
- Infective endocarditis (see “Prophylaxis for endocarditis”)
- Before and/or after surgical procedures (e.g., perioperative cefazolin to prevent surgical site infection)
- Post-exposure prophylaxis (e.g., doxycycline against malaria, rifampin against bacterial meningitis)

Related One-Minute Telegram

One-Minute Telegram 61-2022-3/3: Fluoroquinolones are not associated with increased suicidality

Interested in the newest medical research, distilled down to just one minute? Sign up for the One-Minute Telegram in “Tips and links” below.

References

Cho H, Uehara T, Bernhardt TG. Beta-Lactam Antibiotics Induce a Lethal Malfunctioning of the Bacterial Cell Wall Synthesis Machinery. Cell. 2014; 159 (6): p.1300-1311.doi: 10.1016/j.cell.2014.11.017 . | Open in Read by QxMD
Sutter R, Rüegg S, Tschudin-Sutter S. Seizures as adverse events of antibiotic drugs: A systematic review.. Neurology. 2015.
Krcméry V Jr, Matejicka F, Pichnová E, Jurga L, Sulcova M, Kunová A, West D.. Documented fungal infections after prophylaxis or therapy with wide spectrum antibiotics: relationship between certain fungal pathogens and particular antimicrobials?. Journal of Chemotherapy. 1999.
Peter M Hawkey, David M Livermore. Carbapenem antibiotics for serious infections. The BMJ. 2012.
Tomasz A. Penicillin-Binding Proteins and the Antibacterial Effectiveness of β-Lactam Antibiotics. Clinical Infectious Diseases. 1986; 8 (Supplement_3): p.S260-S278.doi: 10.1093/clinids/8.supplement_3.s260 . | Open in Read by QxMD
George Garratty. Drug-induced immune hemolytic anemia. American Society of Hematology. 2009.
Li-Ju Chen, Fei-Yuan Hsiao, Li-Jiuan Shen, Fe-Lin Lin Wu, Woei Tsay, Chien-Ching Hung, and Shu-Wen Lin. Use of Hypoprothrombinemia-Inducing Cephalosporins and the Risk of Hemorrhagic Events: A Nationwide Nested Case-Control Study. PLOS One. 2016.
Shirakawa H, Komai M, Kimura S.. Antibiotic-induced vitamin K deficiency and the role of the presence of intestinal flora.. International Journal for Vitamin and Nutrition. 1990.
Grill MF, Maganti R.. Cephalosporin-induced neurotoxicity: clinical manifestations, potential pathogenic mechanisms, and the role of electroencephalographic monitoring.. Annals of Pharmacotherapy. 2008.
Peter F Weller, MD, MACP. Vancomycin hypersensitivity. In: Post TW, ed. UpToDate. Waltham, MA: UpToDate. https://www.uptodate.com/contents/vancomycin-hypersensitivity. Last updated: February 9, 2019. Accessed: July 12, 2019.
Blumenthal KG, Patil SU, Long AA.. The importance of vancomycin in drug rash with eosinophilia and systemic symptoms (DRESS) syndrome.. Allergy & Asthma Proceedings. 2012.
Black E, Lau TT, Ensom MH.. Vancomycin-induced neutropenia: is it dose- or duration-related?. Annals of Pharmacotherapy. 2011.
Vancomycin Pregnancy and Breastfeeding Warnings. https://www.drugs.com/pregnancy/vancomycin.html. Updated: March 27, 2019. Accessed: July 29, 2019.
Levofloxacin. https://www.drugbank.ca/drugs/DB01137. Updated: July 13, 2019. Accessed: July 15, 2019.
Nau R, Sörgel F, Eiffert H. Penetration of drugs through the blood-cerebrospinal fluid/blood-brain barrier for treatment of central nervous system infections. Clin Microbiol Rev. 2010; 23 (4): p.858-883.doi: 10.1128/CMR.00007-10 . | Open in Read by QxMD
Quinolones. http://www.antimicrobe.org/new/d17.asp. Updated: February 21, 2017. Accessed: February 21, 2017.
Gordon JJ, Kauffman CA.. Superinfection with Streptococcus pneumoniae during therapy with ciprofloxacin.. The American Journal of Medicine. 1990.
Jones SC, Sorbello A, Boucher RM.. Fluoroquinolone-associated myasthenia gravis exacerbation: evaluation of postmarketing reports from the US FDA adverse event reporting system and a literature review.. Drug Safety. 2011.
Marchbanks CR. Drug-drug interactions with fluoroquinolones.. Pharmacotherapy. 1993.
Sulfisoxazole. https://www.drugbank.ca/drugs/DB00263. Updated: July 24, 2019. Accessed: July 24, 2019.
Kastrup J, Petersen P, Bartram R, Hansen JM. The effect of trimethoprim on serum creatinine. Br J Urol. 1985; 57 (3): p.265-268.
Perazella MA. Trimethoprim-induced hyperkalaemia: clinical data, mechanism, prevention and management. Drug Saf. 2000; 22 (3): p.227-236.
Sultan Ayed Al Qahtani. Drug-induced megaloblastic, aplastic, and hemolytic anemias: current concepts of pathophysiology and treatment. International Journal of Clinical and Experimental Medicine. 2018.
Anthony Montanaro, MD, FAAAAIS. Sulfonamide allergy in HIV-uninfected patients. In: Post TW, ed. UpToDate. Waltham, MA: UpToDate. https://www.uptodate.com/contents/sulfonamide-allergy-in-hiv-uninfected-patients. Last updated: October 10, 2018. Accessed: July 12, 2019.
Masters PA, O’Bryan TA, Zurlo J, Miller DQ, Joshi N. Trimethoprim-Sulfamethoxazole Revisited. Arch Intern Med. 2003; 163 (4): p.402.doi: 10.1001/archinte.163.4.402 . | Open in Read by QxMD
Daptomycin. https://www.drugbank.ca/drugs/DB00080. Updated: July 11, 2019. Accessed: July 12, 2019.
Yoshitsugu Higashi, Shigeki Nakamura, Yasuhiro Tsuji, Chika Ogami, Kaoru Matsumoto, Koyomi Kawago, Kotaro Tokui, Ryuji Hayashi, Ippei Sakamaki, and Yoshihiro Yamamoto. Daptomycin-induced Eosinophilic Pneumonia and a Review of the Published Literature. Internal Medicine Journal. 2018.
Tran TT, Munita JM, Arias CA. Mechanisms of drug resistance: daptomycin resistance. Ann N Y Acad Sci. 2015; 1354 (1): p.32-53.doi: 10.1111/nyas.12948 . | Open in Read by QxMD
Chloramphenicol. https://www.drugbank.ca/drugs/DB00446. Updated: July 16, 2019. Accessed: July 17, 2019.
Johnson BA, Nunley JR. Use of Systemic Agents in the Treatment of Acne Vulgaris. Am Fam Physician. 2000; 62 (8): p.1823-1830.
Paula E Beattie. Drug induced photosensitivity. Medicines Update. 2014.
Mark H. J. Litzinger, Mersedyes D. Boatman, Eugene Talatala, Monica Litzinger. Fanconi Syndrome. NEPHROLOGY. 2011.
Holst AV, Danielsen PL, Romner B. A severe case of tetracycline-induced intracranial hypertension. Dermatology Reports. 2011; 3 (1): p.1.doi: 10.4081/dr.2011.e1 . | Open in Read by QxMD
Todd SR, Dahlgren FS, Traeger MS, et al. No Visible Dental Staining in Children Treated with Doxycycline for Suspected Rocky Mountain Spotted Fever. J Pediatr. 2015; 166 (5): p.1246-1251.doi: 10.1016/j.jpeds.2015.02.015 . | Open in Read by QxMD
Katzung B,Trevor A. Basic and Clinical Pharmacology. McGraw-Hill Education ; 2014
Tigecycline. https://www.drugbank.ca/drugs/DB00560. Updated: July 16, 2019. Accessed: July 17, 2019.
Jonathan Cohen, William G Powderly, Steven M. Opal. Infectious Diseases. Elsevier ; 2016
Nickie D. Greer. Tigecycline (Tygacil): the first in the glycylcycline class of antibiotics. Proceedings (Baylor University Medical Center). 2006.
Briggs GG, Freeman RK, Yaffe SJ. Drugs in Pregnancy and Lactation: A Reference Guide to Fetal and Neonatal Risk. Lippincott Williams & Wilkins ; 2011
Eberly MD, Eide MB, Thompson JL, Nylund CM. Azithromycin in Early Infancy and Pyloric Stenosis. Pediatrics. 2015; 135 (3): p.483-488.doi: 10.1542/peds.2014-2026 . | Open in Read by QxMD
Nahata M. Drug interactions with azithromycin and the macrolides: an overview.. Journal of Antimicrobial Chemotherapy. 1996.
ZITHROMAX. https://www.rxlist.com/zithromax-drug.htm. Updated: March 30, 2020. Accessed: August 21, 2020.
ERYTHROMYCIN. https://www.rxlist.com/erythromycin-drug.htm. Updated: May 20, 2020. Accessed: August 21, 2020.
BIAXIN. https://www.rxlist.com/biaxin-drug.htm. Updated: May 13, 2020. Accessed: August 21, 2020.
Le T, Bayer AS. Combination antibiotic therapy for infective endocarditis. Clin Infect Dis. 2003; 36 (5): p.615-621.doi: 10.1086/367661 . | Open in Read by QxMD
Linezolid. https://www.drugbank.ca/drugs/DB00601. Updated: July 16, 2019. Accessed: July 18, 2019.
Katherine S. Long and Birte Vester. Resistance to Linezolid Caused by Modifications at Its Binding Site on the Ribosome. Antimicrobial Agents and Chemotherapy. 2012.
Hirakawa H, Kurabayashi K, Tanimoto K, Tomita H. Oxygen Limitation Enhances the Antimicrobial Activity of Fosfomycin in Pseudomonas aeruginosa Following Overexpression of glpT Which Encodes Glycerol-3-Phosphate/Fosfomycin Symporter. Frontiers in Microbiology. 2018; 9.doi: 10.3389/fmicb.2018.01950 . | Open in Read by QxMD
Can Fosfomycin Treat Multidrug-Resistant UTIs?. https://www.medscape.com/viewarticle/778281. Updated: January 30, 2013. Accessed: July 11, 2019.
Fosfomycin. https://www.drugbank.ca/drugs/DB00828. Updated: July 8, 2019. Accessed: July 9, 2019.
Castañeda-García A, Blázquez J, Rodríguez-Rojas A. Molecular Mechanisms and Clinical Impact of Acquired and Intrinsic Fosfomycin Resistance. Antibiotics. 2013; 2 (2): p.217-236.doi: 10.3390/antibiotics2020217 . | Open in Read by QxMD
Edouard G. Vannier, PhD, Maria A. Diuk-Wasser, PhD, Choukri Ben Mamoun, PhD, and Peter J. Krause, MD. Babesiosis. Infectious Disease Clinics of North America. 2016.
Clindamycin Pregnancy and Breastfeeding Warnings. https://www.drugs.com/pregnancy/clindamycin.html. Updated: December 14, 2018. Accessed: July 17, 2019.
Workowski KA, Bachmann LH, Chan PA, et al. Sexually Transmitted Infections Treatment Guidelines, 2021. MMWR. Recommendations and Reports. 2021; 70 (4): p.1-187.doi: 10.15585/mmwr.rr7004a1 . | Open in Read by QxMD
Johns Hopkins Antibiotic (ABX) Guide: Bacteroides fragilis. https://www.hopkinsguides.com/hopkins/view/Johns_Hopkins_ABX_Guide/540052/all/Bacteroides_fragilis. Updated: January 30, 2016. Accessed: February 21, 2017.
Metronidazole - Drugs.com. https://www.drugs.com/metronidazole.html. Updated: December 26, 2018. Accessed: July 15, 2019.
Visapää JP, Tillonen JS, Kaihovaara PS, Salaspuro MP. Lack of disulfiram-like reaction with metronidazole and ethanol.. Ann Pharmacother. 2002; 36 (6): p.971-4.doi: 10.1345/aph.1A066 . | Open in Read by QxMD
METRONIDAZOLE. https://www.rxlist.com/metronidazole-drug.htm. Updated: March 8, 2019. Accessed: August 21, 2020.
Maddalena Diana Iadevaia, Anna Del Prete, Claudia Cesaro, Laura Gaeta, Claudio Zulli, and Carmelina Loguercio. Rifaximin in the treatment of hepatic encephalopathy. Hepatic Medicine. 2011.
Muthukumar T, Jayakumar M, Fernando EM, Muthusethupathi MA.. Acute renal failure due to rifampicin: a study of 25 patients.. American Journal of Kidney Diseases. 2002.
Brahm NC, Yeager LL, et al. Commonly prescribed medications and potential false-positive urine drug screens. American Journal of Health-System Pharmacy. 2010; 67 (16): p.1344-1350.doi: 10.2146/ajhp090477 . | Open in Read by QxMD
Xun-Chao Cai, Huan Xi, Li Liang, Jia-Dong Liu, Chang-Hong Liu, Ya-Rong Xue and Xiang-Yang Yu. Rifampicin-Resistance Mutations in the rpoB Gene in Bacillus velezensis CC09 have Pleiotropic Effects. Frontiers in Microbiology. 2017.
Henrik Cordes, Christoph Thiel, Hélène E. Aschmann, Vanessa Baier, Lars M. Blank, Lars Kuepfer. A Physiologically Based Pharmacokinetic Model of Isoniazid and Its Application in Individualizing Tuberculosis Chemotherapy. Antimicrobial Agents and Chemotherapy. 2016.
Isoniazid. https://www.drugbank.ca/drugs/DB00951. Updated: July 21, 2019. Accessed: July 23, 2019.
UpToDate. Isoniazid: Drug Information. In: Post TW, ed. UpToDate. Waltham, MA: UpToDate. https://www.uptodate.com/contents/isoniazid-drug-information. Last updated: January 1, 2018. Accessed: November 12, 2018.
TB Treatment & Pregnancy. https://www.cdc.gov/tb/topic/treatment/pregnancy.htm. Updated: April 5, 2016. Accessed: July 23, 2019.
PYRAZINAMIDE. https://www.rxlist.com/pyrazinamide-drug.htm. Updated: May 13, 2019. Accessed: August 21, 2020.
Zhang Y, Shi W, Zhang W, Mitchison D. Mechanisms of Pyrazinamide Action and Resistance. Microbiology Spectrum. 2014; 2 (4).doi: 10.1128/microbiolspec.mgm2-0023-2013 . | Open in Read by QxMD
Ben Salem C, Slim R, et al. Drug-induced hyperuricaemia and gout. Rheumatology. 2016; 56 (5): p.679-688.doi: 10.1093/rheumatology/kew293 . | Open in Read by QxMD
MYAMBUTOL. https://www.rxlist.com/myambutol-drug.htm. Updated: December 21, 2017. Accessed: August 21, 2020.
Nazir T, Rasool MH, Hameed A, Ahmad B, Qureshi JA. Ethambutol resistance of indigenous Mycobacterium tuberculosis isolated from human patients.. Brazilian journal of microbiology : [publication of the Brazilian Society for Microbiology]. 2010; 41 (4): p.1065-9.doi: 10.1590/S1517-838220100004000026 . | Open in Read by QxMD
Colistin. https://www.drugbank.ca/drugs/DB00803. Updated: July 18, 2019. Accessed: July 19, 2019.
David Landman, Claudiu Georgescu, Don Antonio Martin, and John Quale. Polymyxins Revisited. Clinical Microbiology Reviews. 2008.
Nitrofurantoin. https://www.drugbank.ca/drugs/DB00698. Updated: July 8, 2019. Accessed: July 9, 2019.
Francis J. Squadrito, Daniel del Portal.. Nitrofurantoin. StatPearls. 2019.
Madani Y, Mann B. Nitrofurantoin-induced lung disease and prophylaxis of urinary tract infections. Primary Care Respiratory Journal. 2012; 21 (3): p.337-341.doi: 10.4104/pcrj.2012.00059 . | Open in Read by QxMD
MACROBID. https://www.rxlist.com/macrobid-drug.htm. Updated: August 11, 2020. Accessed: August 21, 2020.
A Parthasarathy. Textbook of Pediatric Infectious Diseases. Jaypee Brothers Medical Publishers ; 2019
Dapsone - Drugbank. https://www.drugbank.ca/drugs/DB00250. Updated: August 21, 2020. Accessed: August 21, 2020.
Gillis TP, Williams DL. Dapsone resistance in Mycobacterium leprae. Lepr Rev. 2000; 71.doi: 10.5935/0305-7518.20000076 . | Open in Read by QxMD
Brunton L. Goodman and Gilman's The Pharmacological Basis of Therapeutics, 13th Edition. McGraw-Hill Education / Medical ; 2017
Hauser AR. Antibiotic Basics for Clinicians. Lippincott Williams & Wilkins ; 2012
Quinupristin. https://www.drugbank.ca/drugs/DB01369. Updated: July 2, 2019. Accessed: July 9, 2019.
Metronidazole - Drugbank. https://www.drugbank.ca/drugs/DB00916. Updated: July 8, 2019. Accessed: July 9, 2019.
Katzung BG, Masters S, Trevor A. Basic and Clinical Pharmacology 12/E. McGraw Hill Professional ; 2012
Cheryle Gurk-Turner. Quinupristin/dalfopristin: the first available macrolide-lincosamide-streptogramin antibiotic. Proceedings (Baylor University. Medical Center)".. 2000.
Ellie Hershberger, Susan Donabedian, Konstantinos Konstantinou, Marcus J. Zervos, George M. Eliopoulos. Quinupristin-Dalfopristin Resistance in Gram-Positive Bacteria: Mechanism of Resistance and Epidemiology. Clinical Infectious Diseases. 2004.
Dalfopristin. https://www.drugbank.ca/drugs/DB01764. Updated: July 13, 2019. Accessed: July 24, 2019.
dalfopristin/quinupristin - Drug Summary. https://www.pdr.net/drug-summary/Synercid-dalfopristin-quinupristin-1492. Updated: January 1, 2019. Accessed: July 25, 2019.
Bennett JE, Dolin R, Blaser MJ. Mandell, Douglas, and Bennett's Principles and Practice of Infectious Diseases. Elsevier Saunders ; 2015

3 free articles remaining

You have 3 free member-only articles left this month. Sign up and get unlimited access.

Have an account? Log In Start free trial

Evidence-based content, created and peer-reviewed by physicians. Read the disclaimer