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Antibacterial agents(1)

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Kelvin Mulenga
Kelvin Mulenga

antibacterial agents

Saúde e medicina
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ANTIBACTERIAL AGENTS kelvin
Introduction • The ability to direct therapy specifically at a disease-causing infectious agent is unique to the management of infectious diseases. • Its initial success depends on exploiting differences between our own makeup and metabolism and that of the microorganism in question. • The mode of action of antimicrobials on bacteria and viruses is the focus of this chapter. • The continued success of antibacterial and antiviral agents depends on whether the organisms to which the agent was originally directed develop resistance.
GENERAL CONSIDERATIONS • Clinically effective antimicrobial agents all exhibit selective toxicity toward the parasite rather than the host, a characteristic that differentiates them from the disinfectants • In most cases, selective toxicity is explained by action on microbial processes or structures that differ from those of mammalian cells. • For example, some agents act on bacterial cell wall synthesis, and others on functions of the 70 S bacterial ribosome but not the 80 S eukaryotic ribosome.
Definitions •Antibiotic—antimicrobials of microbial origin, most of which are produced by fungi or by bacteria of the genus Streptomyces. •Antimicrobial—any substance with sufficient antimicrobial activity that it can be used in the treatment of infectious diseases. •Bactericidal—an antimicrobial that not only inhibits growth but is lethal to bacteria. •Bacteriostatic—an antimicrobial that inhibits growth but does not kill the organisms
Definitions • Chemotherapeutic—a broad term that encompasses antibiotics, antimicrobials, and drugs used in the treatment of cancer. • In the context of infectious diseases, it implies the agent is not an antibiotic. •Minimal inhibitory concentration (MIC)—a laboratory term that defines the lowest concentration ( g/mL) able to inhibit growth of the microorganism. •Resistant—organisms that are not inhibited by clinically achievable concentrations of a antimicrobial agent
Definitions • Sensitive—term applied to microorganisms indicating that they will be inhibited by concentrations of the antimicrobic that can be achieved clinically. • Spectrum—an expression of the categories of microorganisms against which an antimicrobial is typically active • A narrow-spectrum agent has activity against only a few organisms. • A broad-spectrum agent has activity against organisms of diverse types (eg, Gram-positive and Gram-negative bacteria). • Susceptible—term applied to microorganisms indicating that they will be inhibited by concentrations of the antimicrobic that can be achieved clinically.
General considerations • Some antimicrobial agents, such as penicillin, are essentially nontoxic to the host, unless hypersensitivity has developed. • For others, such as the aminoglycosides, the effective therapeutic dose is relatively close to the toxic dose; as a result, control of dosage and blood level must be much more precise • Ideally, selective toxicity is based on the ability of an antimicrobial agent to attack a target present in bacteria but not humans
Sources of Antimicrobial Agents • Antibiotics are synthesized by molds or bacteria • Production in quantity is by industrial fermentation • Chemicals with antibacterial activity are discovered by chance or as the result of screening programs • Naturally occurring antimicrobics can be chemically modified
Spectrum of Action • Spectrum is the range of bacteria against which the agent is typically active • Some antibacterial antimicrobics are known as narrow- spectrum agents; for example, benzyl penicillin is highly active against many Gram-positive and Gram-negative cocci but has little activity against enteric Gram-negative bacilli • Broad-spectrum agents inhibit both Gram-positive and Gram negative species
Selected antibacterial antimicrobials • Antimicrobics That Act on Cell Wall Synthesis • Cross-linking of peptidoglycan is the target of β-lactams and glycopeptides
β-Lactam Antimicrobials • The β -lactam antimicrobics comprise the penicillins, cephalosporins, carbapenems and monobactams. • A β-lactam ring is part of the structure of all β -lactam antimicrobics • Their name derives from the presence of a β -lactam ring in their structure; this ring is essential for antibacterial activity. • Penicillin, the first member of this class, was derived from molds of the genus Penicillium, and later natural β -lactams were derived from both molds and bacteria of the genus Streptomyces.
β-Lactam Antimicrobials • It is possible to synthesize β -lactams, but most are derived from semisynthetic processes involving the chemical modification of the products of fermentation • Interfere with peptidoglycan cross-linking by binding to transpeptidases called PBPs • Penicillins, cephalosporins, monobactams, and carbapenems differ in terms of the structures fused to the β- Lactam ring • β -Lactam antimicrobics kill growing bacteria killed by lysing weakened cell walls
β-Lactam Antimicrobics • Penicillins • Penicillins differ primarily in their spectrum of activity against Gram negative bacteria and resistance to staphylococcal penicillinase. • This penicillinase is one of a family of bacterial enzymes called β -lactamases that inactivate β -lactam antimicrobics • Penicillin G is active primarily against Gram-positive organisms, Gram-negative cocci, and some spirochetes, including the spirochete of syphilis.
β-Lactam Antimicrobics • Penicillins • Penicillin G is the least toxic and least expensive of all the penicillins. Its modification as penicillin V confers acid stability, so it can be given orally. • Resistance to staphylococcal and Gram-negative - lactamases determines spectrum • Penetration of outer membrane is often limited
β-Lactam Antimicrobics • The penicillinase-resistant penicillins (methicillin, nafcillin, oxacillin) also have narrow spectra, but are active against penicillinase-producing S. aureus • The broader spectrum penicillins owe their expanded activity to the ability to traverse the outer membrane of some Gram- negative bacteria. • Some, such as ampicillin, have excellent activity against a range of Gram-negative pathogens but not P. aeruginosa, an important opportunistic pathogen. • Broad-spectrum penicillins penetrate the outer membrane of some Gram-negative bacteria
β-Lactam Antimicrobics • Others, such as carbenicillin and ticarcillin, are active against Pseudomonas when given in high dosage but are less active than ampicillin against some other Gram- negative organisms. • The penicillins with a Gram-negative spectrum are slightly less active than penicillin G against Gram-positive organisms and are inactivated by staphylococcal penicillinase. • Some penicillins are inactivated by staphylococcal penicillinase
β-Lactam Antimicrobics • Cephalosporins • Some penicillins are inactivated by staphylococcal penicillinase • Cephalosporins are penicillinase resistant • Shifting between first- and third generation cephalosporins gives a wider Gram-negative spectrum • Second- and third-generation cephalosporins have less activity against Gram-positive bacteria
β-Lactam Antimicrobics • Cephalosporins • First-generation cephalosporins inhibit Gram-positive bacteria and a few Enterobacteriaceae • cefazolin and cephalexin Second-generation cephalosporins are also active against anaerobes • cefoxitin and cefaclor • Second generation-cephalosporins are also active against anaerobes • Third-generation cephalosporins have increasing potency against Gram-negative organisms • ceftriaxone, cefotaxime, and ceftazidime • Ceftriaxone and cefotaxime are preferred for meningitis • Ceftazidime is used for Pseudomonas
β-Lactam Antimicrobics • Fourth-generation cephalosporins have enhanced ability to penetrate outer membrane of Gram negative bacteria and resistance to many Gram-negative β-Lactamases. • Cefepime (example) • They have activity against an even wider spectrum of Enterobacteriaceae as well as P. aeruginosa. • These cephalosporins retain the high affinity of third generation drugs and activity against Neisseria and H. influenzae.
β-Lactam Antimicrobics • Carbapenems • The carbapenems (imipenem & meropenem) have the broadest spectrum of all β-lactam antibiotics. • This fact appears to be due to the combination of easy • penetration of Gram-negative and Gram-positive bacterial cells and high level of resistance to β-Lactamases • Carbapenems are very broad spectrum • Monobactams (Aztreonam) • Activity is primarily against Gram-negatives
β-Lactam Antimicrobics • β-Lactamase Inhibitors • β -lactamase inhibitors are β -lactams that bind β – lactamases and inhibit their activity • Other β -lactams are enhanced in the presence of β - lactamase inhibitors
Glycopeptide Antimicrobics • The agents include vancomycin and teicoplanin. • Each of these antimicrobics inhibit assembly of the linear peptidoglycan molecule by binding directly to the terminal amino acids of the peptide side chains. • The effect is the same as with β -lactams, prevention of peptidoglycan cross-linking. • Both agents are bactericidal, but are primarily active only against Gram-positive bacteria.
Glycopeptide Antimicrobics • Their main use has been against multiresistant Gram-positive infections including those caused by strains of staphylococci that are resistant to the penicillinase-resistant penicillins and cephalosporins. • Neither agent is absorbed by mouth, although both have been used orally to treat Clostridium difficile infections of the bowel • Glycopeptide antimicrobics bind directly to amino acid side chains
Aminoglycosides • Aminoglycosides are bactericidal • These include: Streptomycin, gentamicin, tobramycin, amikacin and neomycin • Aminoglycosides must be transported into cell by oxidative metabolism • Not active against anaerobes • Ribosome binding disrupts initiation complexes • binding destabilizes the ribosomes, blocks initiation complexes, and thus prevents elongation of polypeptide chains. • distortion of the site of attachment of mRNA, mistranslation of codons, and failure to produce the correct amino acid sequence in proteins.
Aminoglycosides • Streptomycin binds to the 30S ribosomal subunit but newer and more active aminoglycosides bind to multiple sites on both 30S and 50S subunits. • No entry into human cells • Spectrum includes P. aeruginosa • Broad spectrum and slow development of resistance enhance their use and often combined with β-lactam antimicrobics • Renal and vestibular toxicity must be monitored
Tetracyclines • Tetracyclines include tetracycline, minocycline and doxycycline. • The tetracyclines inhibit protein synthesis by binding to the 30S ribosomal subunit at a point that blocks attachment of aminoacyl- tRNA to the acceptor site on the mRNA ribosome complex • Block tRNA attachment • Activity is bacteriostatic • Broad spectrum includes some intracellular bacteria • Chlamydia, rickettsia and mycoplasma • Orally absorbed but chelated by some foods • Dental staining limits use in children
Chloramphenicol • It influences protein synthesis by binding to the 50S ribosomal subunit and blocking the action of peptidyl transferase, which prevents formation of the peptide bond essential for extension of the peptide chain. • Chloramphenicol blocks peptidyl transferase • Its action is bacteriostatic. • It has little effect on eukaryotic ribosomes, which explains its selective toxicity. • Diffusion into body fluid compartments occurs readily • Marrow suppression and aplastic anemia are serious toxicities and thus use is sharply restricted
Macrolides • The macrolides include erythromycin, azithromycin, and clarithromycin • They affect protein synthesis at the ribosomal level by binding to the 50S subunit and blocking the translocation reaction. • Ribosomal binding blocks translocation • Their effect is primarily bacteriostatic. • Macrolides, which are concentrated in phagocytes and other cells, are effective against some intracellular pathogens • Erythromycin is active against Gram-positives
Macrolides • The Gram-negative spectrum includes Neisseria, Bordetella, Campylobacter, and Legionella, but not the Enterobacteriaceae. • Erythromycin is also effective against Chlamydia and Mycoplasma • Azithromycin and clarithromycin have enhanced Gram- negative spectrum • Borrelia burgdorferi (Lyme disease) and Toxoplasma gondii
Clindamycin & Oxazolidinones • Clindamycin • Spectrum is similar to macrolides with addition of anaerobes • Oxazolidinones (Linezolid) • Activity against Gram-positive bacteria resistant to other agents
Streptogramins • Quinupristin and dalfopristin are used in a fixed combination known as quinupristin-dalfopristin in a synergistic ratio. • They inhibit protein synthesis by binding to different sites on the 50S bacterial ribosome • quinupristin inhibits peptide chain elongation • dalfopristin interferes with peptidyl transferase. • Their clinical use has been limited to treatment of vancomycin-resistant enterococci.
Inhibitors of Nucleic Acid Synthesis • Quinolones • The quinolones have a nucleus of two fused six-member rings that when substituted with fluorine become fluoroquinolones, which are now the dominant quinolones for treatment of bacterial infections. • Fuoroquinolones include ciprofloxacin, norfloxacin and ofloxacin, the addition of a piperazine ring and its methylation alter the activity and pharmacologic properties of the individual compound. • The primary target of all quinolones is DNA topoisomerase (gyrase)
Inhibitors of Nucleic Acid Synthesis - Quinolones • This enzyme is responsible for nicking, supercoiling, and sealing bacterial DNA during replication. • Inhibition of topoisomerase blocks supercoiling • They are bactericidal • The enhanced activity and lower frequency of resistance seen with the fluoroquinolones is attributed to binding at multiple sites on the enzyme. • Fluoroquinolones have a broad spectrum, including Pseudomonas • Well distributed after oral administration
Inhibitors of Nucleic Acid Synthesis Folate - Inhibitors • Agents that interfere with synthesis of folic acid by bacteria have selective toxicity because mammalian cells are unable to accomplish this feat and use preformed folate from dietary sources • Bacteria must synthesize folate that humans acquire in their diet • Sulfonamides • Sulfonamides are structural analogs of PABA and compete with it for the enzyme (dihydropteroate synthetase) that combines PABA and pteridine in the initial stage of folate synthesis. • This blockage has multiple effects on the bacterial cells; the most important of these is disruption of nucleic acid synthesis.
Inhibitors of Nucleic Acid Synthesis - Folate Inhibitors • Competition with PABA disrupts nucleic acids • The effect is bacteriostatic, and the addition of PABA to a medium that contains sulfonamide neutralizes the inhibitory effect and allows growth to resume. • Major use is urinary tract infections • Trimethoprim-Sulfamethoxazole • Trimethoprim acts on the folate synthesis pathway but at a point after sulfonamides • It competitively inhibits the activity of bacterial dihydrofolate reductase, which catalyzes the conversion of folate to its reduced active coenzyme form.
Inhibitors of Nucleic Acid Synthesis - Folate Inhibitors • Trimethoprim-Sulfamethoxazole • When combined with sulfamethoxazole, a sulfonamide, trimethoprim leads to a two-stage blockade of the folate pathway, which often results in synergistic bacteriostatic or bactericidal effects. • This quality is exploited in therapeutic preparations that combine both agents in a fixed proportion designed to yield optimum synergy. • Dihydrofolate reductase inhibition is synergistic with sulfonamides • Activity against common bacteria and some fungi
Inhibitors of Nucleic Acid Synthesis - Metronidazole • Active against bacteria, fungi, and parasites • The antibacterial action requires reduction of the nitro group under anaerobic conditions • The reduction products act on the cell at multiple points • The most lethal of these effects is induction of breaks in DNA strands. • Metronidazole is active against a wide range of anaerobes, including Bacteroides fragilis
Inhibitors of Nucleic Acid Synthesis - Metronidazole • Clinically, it is useful for any infection in which anaerobes may be involved. • Because these infections are typically polymicrobial, a second antimicrobial (eg, β -lactam) is usually added to cover aerobic and facultative bacteria.
Inhibitors of Nucleic Acid Synthesis - Rifampin • Blocking of RNA synthesis occurs by binding to polymerase • Rifampin binds to the β -subunit of DNA-dependent RNA polymerase, which prevents the initiation of RNA synthesis. • This agent is active against most Gram-positive bacteria and selected Gram-negative organisms, including Neisseria and Haemophilus • Not active against members of the Enterobacteriaceae
Inhibitors of Nucleic Acid Synthesis - Rifampin • The most clinically useful property of rifampin is its antimycobacterial activity, which includes Mycobacterium tuberculosis and the other species that most commonly infect humans. • • Resistance by mutation of the polymerase readily occurs
Antimicrobics Acting on the Outer & Cytoplasmic Membranes • The polypeptide antimicrobics polymyxin B and colistin have a cationic detergent-like effect. • They bind to the cell membranes of susceptible Gram- negative bacteria and alter their permeability, resulting in loss of essential cytoplasmic components and bacterial death. • These agents react to a lesser extent with cell membranes of the host, resulting in nephrotoxicity and neurotoxicity.
Antimicrobics Acting on the Outer & Cytoplasmic Membranes • Their spectrum is essentially Gram-negative; they act against P. aeruginosa and other Gram-negative rods. • Although these antimicrobics were used for systemic treatment in the past, their use is now limited to topical applications. • They have an advantage; resistance to them rarely develops.
END

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Antibacterial agents(1)

  • 2. Introduction • The ability to direct therapy specifically at a disease-causing infectious agent is unique to the management of infectious diseases. • Its initial success depends on exploiting differences between our own makeup and metabolism and that of the microorganism in question. • The mode of action of antimicrobials on bacteria and viruses is the focus of this chapter. • The continued success of antibacterial and antiviral agents depends on whether the organisms to which the agent was originally directed develop resistance.
  • 3. GENERAL CONSIDERATIONS • Clinically effective antimicrobial agents all exhibit selective toxicity toward the parasite rather than the host, a characteristic that differentiates them from the disinfectants • In most cases, selective toxicity is explained by action on microbial processes or structures that differ from those of mammalian cells. • For example, some agents act on bacterial cell wall synthesis, and others on functions of the 70 S bacterial ribosome but not the 80 S eukaryotic ribosome.
  • 4. Definitions •Antibiotic—antimicrobials of microbial origin, most of which are produced by fungi or by bacteria of the genus Streptomyces. •Antimicrobial—any substance with sufficient antimicrobial activity that it can be used in the treatment of infectious diseases. •Bactericidal—an antimicrobial that not only inhibits growth but is lethal to bacteria. •Bacteriostatic—an antimicrobial that inhibits growth but does not kill the organisms
  • 5. Definitions • Chemotherapeutic—a broad term that encompasses antibiotics, antimicrobials, and drugs used in the treatment of cancer. • In the context of infectious diseases, it implies the agent is not an antibiotic. •Minimal inhibitory concentration (MIC)—a laboratory term that defines the lowest concentration ( g/mL) able to inhibit growth of the microorganism. •Resistant—organisms that are not inhibited by clinically achievable concentrations of a antimicrobial agent
  • 6. Definitions • Sensitive—term applied to microorganisms indicating that they will be inhibited by concentrations of the antimicrobic that can be achieved clinically. • Spectrum—an expression of the categories of microorganisms against which an antimicrobial is typically active • A narrow-spectrum agent has activity against only a few organisms. • A broad-spectrum agent has activity against organisms of diverse types (eg, Gram-positive and Gram-negative bacteria). • Susceptible—term applied to microorganisms indicating that they will be inhibited by concentrations of the antimicrobic that can be achieved clinically.
  • 7. General considerations • Some antimicrobial agents, such as penicillin, are essentially nontoxic to the host, unless hypersensitivity has developed. • For others, such as the aminoglycosides, the effective therapeutic dose is relatively close to the toxic dose; as a result, control of dosage and blood level must be much more precise • Ideally, selective toxicity is based on the ability of an antimicrobial agent to attack a target present in bacteria but not humans
  • 8. Sources of Antimicrobial Agents • Antibiotics are synthesized by molds or bacteria • Production in quantity is by industrial fermentation • Chemicals with antibacterial activity are discovered by chance or as the result of screening programs • Naturally occurring antimicrobics can be chemically modified
  • 9. Spectrum of Action • Spectrum is the range of bacteria against which the agent is typically active • Some antibacterial antimicrobics are known as narrow- spectrum agents; for example, benzyl penicillin is highly active against many Gram-positive and Gram-negative cocci but has little activity against enteric Gram-negative bacilli • Broad-spectrum agents inhibit both Gram-positive and Gram negative species
  • 10. Selected antibacterial antimicrobials • Antimicrobics That Act on Cell Wall Synthesis • Cross-linking of peptidoglycan is the target of β-lactams and glycopeptides
  • 11. β-Lactam Antimicrobials • The β -lactam antimicrobics comprise the penicillins, cephalosporins, carbapenems and monobactams. • A β-lactam ring is part of the structure of all β -lactam antimicrobics • Their name derives from the presence of a β -lactam ring in their structure; this ring is essential for antibacterial activity. • Penicillin, the first member of this class, was derived from molds of the genus Penicillium, and later natural β -lactams were derived from both molds and bacteria of the genus Streptomyces.
  • 12. β-Lactam Antimicrobials • It is possible to synthesize β -lactams, but most are derived from semisynthetic processes involving the chemical modification of the products of fermentation • Interfere with peptidoglycan cross-linking by binding to transpeptidases called PBPs • Penicillins, cephalosporins, monobactams, and carbapenems differ in terms of the structures fused to the β- Lactam ring • β -Lactam antimicrobics kill growing bacteria killed by lysing weakened cell walls
  • 13. β-Lactam Antimicrobics • Penicillins • Penicillins differ primarily in their spectrum of activity against Gram negative bacteria and resistance to staphylococcal penicillinase. • This penicillinase is one of a family of bacterial enzymes called β -lactamases that inactivate β -lactam antimicrobics • Penicillin G is active primarily against Gram-positive organisms, Gram-negative cocci, and some spirochetes, including the spirochete of syphilis.
  • 14. β-Lactam Antimicrobics • Penicillins • Penicillin G is the least toxic and least expensive of all the penicillins. Its modification as penicillin V confers acid stability, so it can be given orally. • Resistance to staphylococcal and Gram-negative - lactamases determines spectrum • Penetration of outer membrane is often limited
  • 15. β-Lactam Antimicrobics • The penicillinase-resistant penicillins (methicillin, nafcillin, oxacillin) also have narrow spectra, but are active against penicillinase-producing S. aureus • The broader spectrum penicillins owe their expanded activity to the ability to traverse the outer membrane of some Gram- negative bacteria. • Some, such as ampicillin, have excellent activity against a range of Gram-negative pathogens but not P. aeruginosa, an important opportunistic pathogen. • Broad-spectrum penicillins penetrate the outer membrane of some Gram-negative bacteria
  • 16. β-Lactam Antimicrobics • Others, such as carbenicillin and ticarcillin, are active against Pseudomonas when given in high dosage but are less active than ampicillin against some other Gram- negative organisms. • The penicillins with a Gram-negative spectrum are slightly less active than penicillin G against Gram-positive organisms and are inactivated by staphylococcal penicillinase. • Some penicillins are inactivated by staphylococcal penicillinase
  • 17. β-Lactam Antimicrobics • Cephalosporins • Some penicillins are inactivated by staphylococcal penicillinase • Cephalosporins are penicillinase resistant • Shifting between first- and third generation cephalosporins gives a wider Gram-negative spectrum • Second- and third-generation cephalosporins have less activity against Gram-positive bacteria
  • 18. β-Lactam Antimicrobics • Cephalosporins • First-generation cephalosporins inhibit Gram-positive bacteria and a few Enterobacteriaceae • cefazolin and cephalexin Second-generation cephalosporins are also active against anaerobes • cefoxitin and cefaclor • Second generation-cephalosporins are also active against anaerobes • Third-generation cephalosporins have increasing potency against Gram-negative organisms • ceftriaxone, cefotaxime, and ceftazidime • Ceftriaxone and cefotaxime are preferred for meningitis • Ceftazidime is used for Pseudomonas
  • 19. β-Lactam Antimicrobics • Fourth-generation cephalosporins have enhanced ability to penetrate outer membrane of Gram negative bacteria and resistance to many Gram-negative β-Lactamases. • Cefepime (example) • They have activity against an even wider spectrum of Enterobacteriaceae as well as P. aeruginosa. • These cephalosporins retain the high affinity of third generation drugs and activity against Neisseria and H. influenzae.
  • 20. β-Lactam Antimicrobics • Carbapenems • The carbapenems (imipenem & meropenem) have the broadest spectrum of all β-lactam antibiotics. • This fact appears to be due to the combination of easy • penetration of Gram-negative and Gram-positive bacterial cells and high level of resistance to β-Lactamases • Carbapenems are very broad spectrum • Monobactams (Aztreonam) • Activity is primarily against Gram-negatives
  • 21. β-Lactam Antimicrobics • β-Lactamase Inhibitors • β -lactamase inhibitors are β -lactams that bind β – lactamases and inhibit their activity • Other β -lactams are enhanced in the presence of β - lactamase inhibitors
  • 22. Glycopeptide Antimicrobics • The agents include vancomycin and teicoplanin. • Each of these antimicrobics inhibit assembly of the linear peptidoglycan molecule by binding directly to the terminal amino acids of the peptide side chains. • The effect is the same as with β -lactams, prevention of peptidoglycan cross-linking. • Both agents are bactericidal, but are primarily active only against Gram-positive bacteria.
  • 23. Glycopeptide Antimicrobics • Their main use has been against multiresistant Gram-positive infections including those caused by strains of staphylococci that are resistant to the penicillinase-resistant penicillins and cephalosporins. • Neither agent is absorbed by mouth, although both have been used orally to treat Clostridium difficile infections of the bowel • Glycopeptide antimicrobics bind directly to amino acid side chains
  • 24. Aminoglycosides • Aminoglycosides are bactericidal • These include: Streptomycin, gentamicin, tobramycin, amikacin and neomycin • Aminoglycosides must be transported into cell by oxidative metabolism • Not active against anaerobes • Ribosome binding disrupts initiation complexes • binding destabilizes the ribosomes, blocks initiation complexes, and thus prevents elongation of polypeptide chains. • distortion of the site of attachment of mRNA, mistranslation of codons, and failure to produce the correct amino acid sequence in proteins.
  • 25. Aminoglycosides • Streptomycin binds to the 30S ribosomal subunit but newer and more active aminoglycosides bind to multiple sites on both 30S and 50S subunits. • No entry into human cells • Spectrum includes P. aeruginosa • Broad spectrum and slow development of resistance enhance their use and often combined with β-lactam antimicrobics • Renal and vestibular toxicity must be monitored
  • 26. Tetracyclines • Tetracyclines include tetracycline, minocycline and doxycycline. • The tetracyclines inhibit protein synthesis by binding to the 30S ribosomal subunit at a point that blocks attachment of aminoacyl- tRNA to the acceptor site on the mRNA ribosome complex • Block tRNA attachment • Activity is bacteriostatic • Broad spectrum includes some intracellular bacteria • Chlamydia, rickettsia and mycoplasma • Orally absorbed but chelated by some foods • Dental staining limits use in children
  • 27. Chloramphenicol • It influences protein synthesis by binding to the 50S ribosomal subunit and blocking the action of peptidyl transferase, which prevents formation of the peptide bond essential for extension of the peptide chain. • Chloramphenicol blocks peptidyl transferase • Its action is bacteriostatic. • It has little effect on eukaryotic ribosomes, which explains its selective toxicity. • Diffusion into body fluid compartments occurs readily • Marrow suppression and aplastic anemia are serious toxicities and thus use is sharply restricted
  • 28. Macrolides • The macrolides include erythromycin, azithromycin, and clarithromycin • They affect protein synthesis at the ribosomal level by binding to the 50S subunit and blocking the translocation reaction. • Ribosomal binding blocks translocation • Their effect is primarily bacteriostatic. • Macrolides, which are concentrated in phagocytes and other cells, are effective against some intracellular pathogens • Erythromycin is active against Gram-positives
  • 29. Macrolides • The Gram-negative spectrum includes Neisseria, Bordetella, Campylobacter, and Legionella, but not the Enterobacteriaceae. • Erythromycin is also effective against Chlamydia and Mycoplasma • Azithromycin and clarithromycin have enhanced Gram- negative spectrum • Borrelia burgdorferi (Lyme disease) and Toxoplasma gondii
  • 30. Clindamycin & Oxazolidinones • Clindamycin • Spectrum is similar to macrolides with addition of anaerobes • Oxazolidinones (Linezolid) • Activity against Gram-positive bacteria resistant to other agents
  • 31. Streptogramins • Quinupristin and dalfopristin are used in a fixed combination known as quinupristin-dalfopristin in a synergistic ratio. • They inhibit protein synthesis by binding to different sites on the 50S bacterial ribosome • quinupristin inhibits peptide chain elongation • dalfopristin interferes with peptidyl transferase. • Their clinical use has been limited to treatment of vancomycin-resistant enterococci.
  • 32. Inhibitors of Nucleic Acid Synthesis • Quinolones • The quinolones have a nucleus of two fused six-member rings that when substituted with fluorine become fluoroquinolones, which are now the dominant quinolones for treatment of bacterial infections. • Fuoroquinolones include ciprofloxacin, norfloxacin and ofloxacin, the addition of a piperazine ring and its methylation alter the activity and pharmacologic properties of the individual compound. • The primary target of all quinolones is DNA topoisomerase (gyrase)
  • 33. Inhibitors of Nucleic Acid Synthesis - Quinolones • This enzyme is responsible for nicking, supercoiling, and sealing bacterial DNA during replication. • Inhibition of topoisomerase blocks supercoiling • They are bactericidal • The enhanced activity and lower frequency of resistance seen with the fluoroquinolones is attributed to binding at multiple sites on the enzyme. • Fluoroquinolones have a broad spectrum, including Pseudomonas • Well distributed after oral administration
  • 34. Inhibitors of Nucleic Acid Synthesis Folate - Inhibitors • Agents that interfere with synthesis of folic acid by bacteria have selective toxicity because mammalian cells are unable to accomplish this feat and use preformed folate from dietary sources • Bacteria must synthesize folate that humans acquire in their diet • Sulfonamides • Sulfonamides are structural analogs of PABA and compete with it for the enzyme (dihydropteroate synthetase) that combines PABA and pteridine in the initial stage of folate synthesis. • This blockage has multiple effects on the bacterial cells; the most important of these is disruption of nucleic acid synthesis.
  • 35. Inhibitors of Nucleic Acid Synthesis - Folate Inhibitors • Competition with PABA disrupts nucleic acids • The effect is bacteriostatic, and the addition of PABA to a medium that contains sulfonamide neutralizes the inhibitory effect and allows growth to resume. • Major use is urinary tract infections • Trimethoprim-Sulfamethoxazole • Trimethoprim acts on the folate synthesis pathway but at a point after sulfonamides • It competitively inhibits the activity of bacterial dihydrofolate reductase, which catalyzes the conversion of folate to its reduced active coenzyme form.
  • 36. Inhibitors of Nucleic Acid Synthesis - Folate Inhibitors • Trimethoprim-Sulfamethoxazole • When combined with sulfamethoxazole, a sulfonamide, trimethoprim leads to a two-stage blockade of the folate pathway, which often results in synergistic bacteriostatic or bactericidal effects. • This quality is exploited in therapeutic preparations that combine both agents in a fixed proportion designed to yield optimum synergy. • Dihydrofolate reductase inhibition is synergistic with sulfonamides • Activity against common bacteria and some fungi
  • 37. Inhibitors of Nucleic Acid Synthesis - Metronidazole • Active against bacteria, fungi, and parasites • The antibacterial action requires reduction of the nitro group under anaerobic conditions • The reduction products act on the cell at multiple points • The most lethal of these effects is induction of breaks in DNA strands. • Metronidazole is active against a wide range of anaerobes, including Bacteroides fragilis
  • 38. Inhibitors of Nucleic Acid Synthesis - Metronidazole • Clinically, it is useful for any infection in which anaerobes may be involved. • Because these infections are typically polymicrobial, a second antimicrobial (eg, β -lactam) is usually added to cover aerobic and facultative bacteria.
  • 39. Inhibitors of Nucleic Acid Synthesis - Rifampin • Blocking of RNA synthesis occurs by binding to polymerase • Rifampin binds to the β -subunit of DNA-dependent RNA polymerase, which prevents the initiation of RNA synthesis. • This agent is active against most Gram-positive bacteria and selected Gram-negative organisms, including Neisseria and Haemophilus • Not active against members of the Enterobacteriaceae
  • 40. Inhibitors of Nucleic Acid Synthesis - Rifampin • The most clinically useful property of rifampin is its antimycobacterial activity, which includes Mycobacterium tuberculosis and the other species that most commonly infect humans. • • Resistance by mutation of the polymerase readily occurs
  • 41. Antimicrobics Acting on the Outer & Cytoplasmic Membranes • The polypeptide antimicrobics polymyxin B and colistin have a cationic detergent-like effect. • They bind to the cell membranes of susceptible Gram- negative bacteria and alter their permeability, resulting in loss of essential cytoplasmic components and bacterial death. • These agents react to a lesser extent with cell membranes of the host, resulting in nephrotoxicity and neurotoxicity.
  • 42. Antimicrobics Acting on the Outer & Cytoplasmic Membranes • Their spectrum is essentially Gram-negative; they act against P. aeruginosa and other Gram-negative rods. • Although these antimicrobics were used for systemic treatment in the past, their use is now limited to topical applications. • They have an advantage; resistance to them rarely develops.
  • 43. END