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antibiotic principles.ppt

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Jigar Mehta
Jigar Mehta

antibiotic

Health & Medicine
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PRINCIPLES OF ANTIBIOTIC THERAPY Dr jigar mehta
Causative agent host environment INFECTION/ DISEASE •Age •prior illness •level of nutrition •pregnancy •coexisting illness,immunoc ompromised state •Community acquired: environment,geography •Hospital acquired Evolution of variety of antiobiotics/AMAs to kill/supress the causative agents. The problem of antibiotic resistance
Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
Principles of Antibiotic prescribing……. Fever may not always indicate infection • Infections- bacterial,viral, fungal,protozoal • collagen vascular diseases • malignancies • a stressful event- – CVA, AMI, PE – Post operative surgical stress – thrombophlebitis – hemorrhage- GI,Brain • others- – LCF, CAH, thyroiditis, FMF – Drug fever, factitious fever
Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
Principles of Antibiotic prescribing……. Community or Hospital acquired Epidemiology of ICU Nis. Infection site FOLEYS CATHETER (95%) Main Nis. UTI 31% Pathogen distributn Fungal:candida MECHANICAL VENTILATION (86%) Pneumonia 27% G-ve aerobic 64% Staphylococci 20% CVP (87%) Blood stream infection (19%) CoNS 36% Enterococci (16% Staph aureus13% Fungus 12%
Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
Principles of Antibiotic prescribing……. Status of host • Immunocompromised patient – Severe underlying illness – Malnutrition – DM – Repeated hospitalisations – HIV, others • Use of devices Such patients are colonized with resistant organisms due to prior antibiotic use
Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
• Use newer antibiotics when absolutely necessary and only when indicated WHY? BECAUSE OF THE GROWING PROBLEM OF ANTIBIOTIC RESISTANCE Principles of Antibiotic prescribing
“we know everything about antibiotics except how much to give” Maxwell Finland (The 500 mg 6hrly era) Bacterial Killing is a function of drug concentration and time of exposure Concentration independent Killing Concentration dependant Killing Optimal Dose
Time dependant killing • B lactams • Clindamycin Dose more frequently rather than increasing single dose (or continuous infusion) Ceftriaxone 1 gm as good as higher dose for most community acquired respiratory, uti, abdominal infections
Optimal Duration • Most antibiotics are being given for far too long • Stop antimicrobial treatment: • -When infection is cured. (if patient is afebrile & well for 48hrs) • -When cultures are negative and infection is unlikely.
OPTIMAL SELECTION Presumed Site of infection (e.g. respiratory tract, urinary tract, a subdiaphragmatic collection, or whatever) address any surgically remediable pathology right away
Community Acquired v/s hospital acquired Community acquired usually sensitive (even if severe) Hospital acquired likely to be caused by resistant bugs (even if mild) e.g. pneumonia, abdominal infections, skin & soft tissue infections
Optimal antibiotic Selection Always culture Start antibiotics immediately Hit Hard & high De escalate
History Penicillin - first antibiotic 1929, Alexander Flemming late ‘40’s and early 50”s (golden age of discovery) streptomycin, chloramphenicol, tetracycline,sulfonamides 80% staph aureus resistant PRSP 1953 - Shigella outbreak in Japan 1950’s - Mycobacterium tuberculosis largely resistant to streptomycin
IT IS A GLOBAL PROBLEM THE BUGS HAVE BEEN THERE EVER SINCE AND THEY ARE GETTING CLEVERER BY THE MINUTE
Factors in Antimicrobial Resistance in hospitalised patients Cross transmission Lack of Asepsis Unwashed hands Care of devices Level of crowding Transfer of critically ill patients from other facilities Host defense Immunocompromised patient Severe underlying illness Malnutrition DM Repeated hospitalisations HIV, others Use of devices Antimicrobial use ANTIMICROBIAL RESISTANCE
Antimicrobial Use • Direct, consistent correlation between antibiotic use and resistance patterns • development of resistance is correlated with level of antibiotic use – overuse has increased the incidence of and selection for resistance-conferring mutations – McGowan et al Rev. Inf. Dis 1983 – Ballow C.H., Schentag J.J. - National Nosocomial Resistance Surveillance Group 1992 – Fridkin S.K. et al Antimicrobial Resistance in ICU’s, Clinics in Chest Medicine 1999
Evolution of Antimicrobial Resistance in Gram-Positive Cocci S. aureus Penicillin [1940s] Penicillin-resistant S. aureus Methicillin [1960s] Methicillin-resistant S. aureus (MRSA) Vancomycin-resistant enterococcus (VRE) Vancomycin [1997] Vancomycin (glycopeptide) intermediate-resistant S. aureus Vancomycin- resistant S. aureus Ciprofloxacin 1987 [2002] Adapted from: CDC. Prevent Antimicrobial Resistance: A Campaign for Clinicians. April 2002.
What should we do? Prevent overuse /misuse Optimize use of antimicrobial agents Prevent cross-transmission
Examples of overuse/misuse “DOES MY PATIENT NEED AN ANTIBIOTIC?” • prophylactic use after elective surgery • empiric use (no known etiologic agent) • increased use of broad spectrum agents • antibiotics in animal feeds • pediatric use for viral infections • patients who do not complete course (TB,AIDS)
Prevent cross transmission • Hand washing • Gloves • Gowns • Face masks • Patient isolation or cohorting • Traffic control
Other Strategies • New Drugs – currently about 100 antibiotics on market – three main mechanisms of action • inhibition of protein synthesis • inhibition of cell wall synthesis/maintenance • inhibition of DNA replication
New Antibiotics • Cell Wall inhibitors - based on beta lactam skeleton – carbapenems - broad spectrum • imipenem usually given with cilastatin (prevents degradation by renal enzymes) • meropenem - enhaced anti-Pseudomonas activity • ertapenem – monobactams - beta lactamase stable • Aztreonam • Moxalactam
New Antibiotics • Betalactamase inhibitors – clavulanate – sulbactam – tazobactam • piperacillin/tazobactam • ticarcillin/clavulanate • do not penetrate meninges thus may not potentiate the action of extended spectrum penicillins. • Fourth generation cephalosporins
New Antibiotics • New Quinolones – gatifloxacin – moxifloxacin – trovafloxacin – gemifloxacin – sitafloxacin – Clinafloxacin • isolates of S.pneumoniae less resistant to these as compared to penicillin,amox-clav, cefuroxime, erythromycin • very effective against L.pneumophilia,M. catarrhalis, H influenzae.
New Antibiotics- enhanced activity against GPC Sr.No Class examples activity versus VRE MRSA PRSP 1 GLYCOPEPTIDES BI- 397, LY333328 + + + 2 EVERNINOMICINS Ziracin + + + 3 LIPOPEPTIDES daptomycin + + + 4 OXAZOLIDINONES linezolid + + + 5 STREPTOGRANINS quinupristin/ dalfopristin + + + 6
3rd Gen Cephalosporins Enterococcus Klebsiella sp E coli/enterobacteriaceae with ESBL’s Vancomycin Meropenem Imipenem/Cilastatin Acinetobacter Fungi, Yeast VRE Overuse Resistance Overgrowth Escalating drug therapy and its hazards Piperacillin/tazobactam ticarcillin/clavulanate
Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
Skin, soft tissue infections • Amoxycillin/clavulanate + cefoxitin/cloxacillin or • Clinda or Metro + amoxy/amoxycillin- clavulanate + Genta • * Penicillin treatment alone carries 30 - 50% mortality
Bone infections • Oxacillin, nafcillin, cephalosporin like cefpirome or glycopeptide like vanco` or teicoplanin to cover Staph aureus well • If Gram -ve org are suspected - 3rd gen cephalosporin or aminoglycoside or fluoroquinolone is added • For P. aeruginosa :Aminglycoside like Tobramycin + ticarcillin-clavulanate /ceftazidime /fluoroquinolone • Duration of therapy - 6 weeks
COMMUNITY ACQUIRED PNEUMONIAS Out Patients: No Cardiopulmonary Disease, No Modifying Factors Advanced generation macrolide:azithromycin / clarithromycin Or Doxycycline •Strep. Pneumoniae •M.Pneumoniae •Chlamydia pneumoniae •Hemophilus influenzae •Respiratory viruses •Miscellaneous •Legionella spp Therapy Organism
Out Patients: With Cardiopulmonary Disease / Modifying Factors Β-Lactam (oral cefpodoxime, cefuroxime,high-dose amoxicillin/clavulanate; or parenteral ceftriaxone followed by oral cefpodoxime) + Macrolide / Doxyclcline Or Antipneumococcal fluroquinolones (used alone) Add Clindamycin/Metronidazole when anaerobes are suspected •Strep. Pneumoniae(including PRSP) •M.Pneumoniae •Chlamydia pneumoniae •Mixed infection (bacteria plus atyrpical pathogen or virus) •Hemophilus influenzae •Enteric Gram Negatives •Anaerobes • Respiratory viruses •Miscellaneous •Legionella spp Therapy Organism
In Patients: No Cardiopulmonary Disease / Modifying Factors I.V Azithromycin alone If macrolide allergic or intolerant: Doxycycline and a β-lactam Or Monotherpay with an antipneumococcal fluroquinolone •Strep. Pneumoniae •Hemophilus influenzae •M.Pneumoniae •Chlamydia pneumoniae •Mixed infection (bacteria plus atyrpical pathogen) •Viruses •Legionella spp •M.Tuberculosis •Endemic fungi Therapy Organism
In Patients: With Cardiopulmonary Disease / Modifying Factors I.V Β-Lactam (cefotaxime, ceftriaxone, amox-clav) Plus I.V or oral Macrolide / Doxyclcline Or I.V Antipneumococcal fluroquinolones alone Add Clindamycin/Metronidazole when anaerobes are suspected •Strep. Pneumoniae(including DRSP) •Hemophilus influenzae •M.Pneumoniae •Chlamydia pneumoniae •Mixed infection (bacteria plus atyrpical pathogen) •Enteric Gram Negatives •Aspiration (Anaerobes) •Viruses •Staph •Legionella spp Therapy Organism
Urinary infections • Acute uncomplicated cystitis- – cotrimoxazole, norflox/ciplox/oflox • acute urethritis-chlamydial – doxycycline • Complicated urinary infection requires – ampi/sulbactam +/- aminoglycoside – 3rd gen cephalosporin like ceftazidime/ cefoperazone – cefoperazone/sulbactam – piperacillin/tazobactam or ticarcillin/clavulanate • Prolonged duration of therapy usually required 7- 21 days
CNS infections • Meningitis – <1month - Ampi, cefotaxime – 4 -12 weeks - Ampi + 3rd gen ceph. – 3mths - 6yrs - 3rd gen ceph + Vanco – young adult - 3rd gen ceph Cefotaxime or ceftriaxone. – >50yrs - Ampi +3rd gen ceph +/- Vanco – Postneurosurgical - Vanco + ceftazidime+/- intrathecal aminoglycosides +/- rifampin
Sepsis of unkown origin • Broad spectrum cover • HIT HARD HIT FAST especially severe sepsis with septicemic shock • Is host immunocompromised? • What prior antibiotics has he received? • Where was he admitted?-does he have a nosocomial infection • How ill is the patient?
Immunocompromised/Septic host • III/IV gen cephalosporin + Vanco/linezolid +Metro +Antifungal or any other broad spectrum combn • Specific situation may require specific workup and specific drugs
Conclusion • Fever may not always indicate infection • The interaction between host, agent and environment must be understood and targeted in controlling disease • Resistance to antimicrobials is currently and will continue to be a problem • Have an antibiotic policy – To provide the most effective treatment for the individual patient – To advise on rational prescribing – To limit the use of prophylactic antibiotics – To delay the emergence of resistance – To minimise adverse events – To maintain a cost effective strategy
antibiotic principles.ppt

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antibiotic principles.ppt

  • 2. Causative agent host environment INFECTION/ DISEASE •Age •prior illness •level of nutrition •pregnancy •coexisting illness,immunoc ompromised state •Community acquired: environment,geography •Hospital acquired Evolution of variety of antiobiotics/AMAs to kill/supress the causative agents. The problem of antibiotic resistance
  • 3. Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
  • 4. Principles of Antibiotic prescribing……. Fever may not always indicate infection • Infections- bacterial,viral, fungal,protozoal • collagen vascular diseases • malignancies • a stressful event- – CVA, AMI, PE – Post operative surgical stress – thrombophlebitis – hemorrhage- GI,Brain • others- – LCF, CAH, thyroiditis, FMF – Drug fever, factitious fever
  • 5. Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
  • 6. Principles of Antibiotic prescribing……. Community or Hospital acquired Epidemiology of ICU Nis. Infection site FOLEYS CATHETER (95%) Main Nis. UTI 31% Pathogen distributn Fungal:candida MECHANICAL VENTILATION (86%) Pneumonia 27% G-ve aerobic 64% Staphylococci 20% CVP (87%) Blood stream infection (19%) CoNS 36% Enterococci (16% Staph aureus13% Fungus 12%
  • 7. Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
  • 8. Principles of Antibiotic prescribing……. Status of host • Immunocompromised patient – Severe underlying illness – Malnutrition – DM – Repeated hospitalisations – HIV, others • Use of devices Such patients are colonized with resistant organisms due to prior antibiotic use
  • 9. Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
  • 10. • Use newer antibiotics when absolutely necessary and only when indicated WHY? BECAUSE OF THE GROWING PROBLEM OF ANTIBIOTIC RESISTANCE Principles of Antibiotic prescribing
  • 11. “we know everything about antibiotics except how much to give” Maxwell Finland (The 500 mg 6hrly era) Bacterial Killing is a function of drug concentration and time of exposure Concentration independent Killing Concentration dependant Killing Optimal Dose
  • 12.
  • 13. Time dependant killing • B lactams • Clindamycin Dose more frequently rather than increasing single dose (or continuous infusion) Ceftriaxone 1 gm as good as higher dose for most community acquired respiratory, uti, abdominal infections
  • 14. Optimal Duration • Most antibiotics are being given for far too long • Stop antimicrobial treatment: • -When infection is cured. (if patient is afebrile & well for 48hrs) • -When cultures are negative and infection is unlikely.
  • 15. OPTIMAL SELECTION Presumed Site of infection (e.g. respiratory tract, urinary tract, a subdiaphragmatic collection, or whatever) address any surgically remediable pathology right away
  • 16. Community Acquired v/s hospital acquired Community acquired usually sensitive (even if severe) Hospital acquired likely to be caused by resistant bugs (even if mild) e.g. pneumonia, abdominal infections, skin & soft tissue infections
  • 17. Optimal antibiotic Selection Always culture Start antibiotics immediately Hit Hard & high De escalate
  • 18. History Penicillin - first antibiotic 1929, Alexander Flemming late ‘40’s and early 50”s (golden age of discovery) streptomycin, chloramphenicol, tetracycline,sulfonamides 80% staph aureus resistant PRSP 1953 - Shigella outbreak in Japan 1950’s - Mycobacterium tuberculosis largely resistant to streptomycin
  • 19. IT IS A GLOBAL PROBLEM THE BUGS HAVE BEEN THERE EVER SINCE AND THEY ARE GETTING CLEVERER BY THE MINUTE
  • 20. Factors in Antimicrobial Resistance in hospitalised patients Cross transmission Lack of Asepsis Unwashed hands Care of devices Level of crowding Transfer of critically ill patients from other facilities Host defense Immunocompromised patient Severe underlying illness Malnutrition DM Repeated hospitalisations HIV, others Use of devices Antimicrobial use ANTIMICROBIAL RESISTANCE
  • 21. Antimicrobial Use • Direct, consistent correlation between antibiotic use and resistance patterns • development of resistance is correlated with level of antibiotic use – overuse has increased the incidence of and selection for resistance-conferring mutations – McGowan et al Rev. Inf. Dis 1983 – Ballow C.H., Schentag J.J. - National Nosocomial Resistance Surveillance Group 1992 – Fridkin S.K. et al Antimicrobial Resistance in ICU’s, Clinics in Chest Medicine 1999
  • 22. Evolution of Antimicrobial Resistance in Gram-Positive Cocci S. aureus Penicillin [1940s] Penicillin-resistant S. aureus Methicillin [1960s] Methicillin-resistant S. aureus (MRSA) Vancomycin-resistant enterococcus (VRE) Vancomycin [1997] Vancomycin (glycopeptide) intermediate-resistant S. aureus Vancomycin- resistant S. aureus Ciprofloxacin 1987 [2002] Adapted from: CDC. Prevent Antimicrobial Resistance: A Campaign for Clinicians. April 2002.
  • 23. What should we do? Prevent overuse /misuse Optimize use of antimicrobial agents Prevent cross-transmission
  • 24. Examples of overuse/misuse “DOES MY PATIENT NEED AN ANTIBIOTIC?” • prophylactic use after elective surgery • empiric use (no known etiologic agent) • increased use of broad spectrum agents • antibiotics in animal feeds • pediatric use for viral infections • patients who do not complete course (TB,AIDS)
  • 25. Prevent cross transmission • Hand washing • Gloves • Gowns • Face masks • Patient isolation or cohorting • Traffic control
  • 26. Other Strategies • New Drugs – currently about 100 antibiotics on market – three main mechanisms of action • inhibition of protein synthesis • inhibition of cell wall synthesis/maintenance • inhibition of DNA replication
  • 27. New Antibiotics • Cell Wall inhibitors - based on beta lactam skeleton – carbapenems - broad spectrum • imipenem usually given with cilastatin (prevents degradation by renal enzymes) • meropenem - enhaced anti-Pseudomonas activity • ertapenem – monobactams - beta lactamase stable • Aztreonam • Moxalactam
  • 28. New Antibiotics • Betalactamase inhibitors – clavulanate – sulbactam – tazobactam • piperacillin/tazobactam • ticarcillin/clavulanate • do not penetrate meninges thus may not potentiate the action of extended spectrum penicillins. • Fourth generation cephalosporins
  • 29. New Antibiotics • New Quinolones – gatifloxacin – moxifloxacin – trovafloxacin – gemifloxacin – sitafloxacin – Clinafloxacin • isolates of S.pneumoniae less resistant to these as compared to penicillin,amox-clav, cefuroxime, erythromycin • very effective against L.pneumophilia,M. catarrhalis, H influenzae.
  • 30. New Antibiotics- enhanced activity against GPC Sr.No Class examples activity versus VRE MRSA PRSP 1 GLYCOPEPTIDES BI- 397, LY333328 + + + 2 EVERNINOMICINS Ziracin + + + 3 LIPOPEPTIDES daptomycin + + + 4 OXAZOLIDINONES linezolid + + + 5 STREPTOGRANINS quinupristin/ dalfopristin + + + 6
  • 31. 3rd Gen Cephalosporins Enterococcus Klebsiella sp E coli/enterobacteriaceae with ESBL’s Vancomycin Meropenem Imipenem/Cilastatin Acinetobacter Fungi, Yeast VRE Overuse Resistance Overgrowth Escalating drug therapy and its hazards Piperacillin/tazobactam ticarcillin/clavulanate
  • 32. Principles of Antibiotic prescribing • Fever may not always indicate infection • Community or Hospital acquired • Status of host • Site of infection • Document reason for starting antibiotics • Obtain microbiological specimens, ask for early Gram stain reports • Gram +ve, Gram -ve, anerobes, fungus? • Use the narrowest spectrum with imp. exceptions • Conform to established treatment guidelines • Use newer antibiotics when absolutely necessary and only when indicated
  • 33. Skin, soft tissue infections • Amoxycillin/clavulanate + cefoxitin/cloxacillin or • Clinda or Metro + amoxy/amoxycillin- clavulanate + Genta • * Penicillin treatment alone carries 30 - 50% mortality
  • 34. Bone infections • Oxacillin, nafcillin, cephalosporin like cefpirome or glycopeptide like vanco` or teicoplanin to cover Staph aureus well • If Gram -ve org are suspected - 3rd gen cephalosporin or aminoglycoside or fluoroquinolone is added • For P. aeruginosa :Aminglycoside like Tobramycin + ticarcillin-clavulanate /ceftazidime /fluoroquinolone • Duration of therapy - 6 weeks
  • 35. COMMUNITY ACQUIRED PNEUMONIAS Out Patients: No Cardiopulmonary Disease, No Modifying Factors Advanced generation macrolide:azithromycin / clarithromycin Or Doxycycline •Strep. Pneumoniae •M.Pneumoniae •Chlamydia pneumoniae •Hemophilus influenzae •Respiratory viruses •Miscellaneous •Legionella spp Therapy Organism
  • 36. Out Patients: With Cardiopulmonary Disease / Modifying Factors Β-Lactam (oral cefpodoxime, cefuroxime,high-dose amoxicillin/clavulanate; or parenteral ceftriaxone followed by oral cefpodoxime) + Macrolide / Doxyclcline Or Antipneumococcal fluroquinolones (used alone) Add Clindamycin/Metronidazole when anaerobes are suspected •Strep. Pneumoniae(including PRSP) •M.Pneumoniae •Chlamydia pneumoniae •Mixed infection (bacteria plus atyrpical pathogen or virus) •Hemophilus influenzae •Enteric Gram Negatives •Anaerobes • Respiratory viruses •Miscellaneous •Legionella spp Therapy Organism
  • 37. In Patients: No Cardiopulmonary Disease / Modifying Factors I.V Azithromycin alone If macrolide allergic or intolerant: Doxycycline and a β-lactam Or Monotherpay with an antipneumococcal fluroquinolone •Strep. Pneumoniae •Hemophilus influenzae •M.Pneumoniae •Chlamydia pneumoniae •Mixed infection (bacteria plus atyrpical pathogen) •Viruses •Legionella spp •M.Tuberculosis •Endemic fungi Therapy Organism
  • 38. In Patients: With Cardiopulmonary Disease / Modifying Factors I.V Β-Lactam (cefotaxime, ceftriaxone, amox-clav) Plus I.V or oral Macrolide / Doxyclcline Or I.V Antipneumococcal fluroquinolones alone Add Clindamycin/Metronidazole when anaerobes are suspected •Strep. Pneumoniae(including DRSP) •Hemophilus influenzae •M.Pneumoniae •Chlamydia pneumoniae •Mixed infection (bacteria plus atyrpical pathogen) •Enteric Gram Negatives •Aspiration (Anaerobes) •Viruses •Staph •Legionella spp Therapy Organism
  • 39. Urinary infections • Acute uncomplicated cystitis- – cotrimoxazole, norflox/ciplox/oflox • acute urethritis-chlamydial – doxycycline • Complicated urinary infection requires – ampi/sulbactam +/- aminoglycoside – 3rd gen cephalosporin like ceftazidime/ cefoperazone – cefoperazone/sulbactam – piperacillin/tazobactam or ticarcillin/clavulanate • Prolonged duration of therapy usually required 7- 21 days
  • 40. CNS infections • Meningitis – <1month - Ampi, cefotaxime – 4 -12 weeks - Ampi + 3rd gen ceph. – 3mths - 6yrs - 3rd gen ceph + Vanco – young adult - 3rd gen ceph Cefotaxime or ceftriaxone. – >50yrs - Ampi +3rd gen ceph +/- Vanco – Postneurosurgical - Vanco + ceftazidime+/- intrathecal aminoglycosides +/- rifampin
  • 41. Sepsis of unkown origin • Broad spectrum cover • HIT HARD HIT FAST especially severe sepsis with septicemic shock • Is host immunocompromised? • What prior antibiotics has he received? • Where was he admitted?-does he have a nosocomial infection • How ill is the patient?
  • 42. Immunocompromised/Septic host • III/IV gen cephalosporin + Vanco/linezolid +Metro +Antifungal or any other broad spectrum combn • Specific situation may require specific workup and specific drugs
  • 43. Conclusion • Fever may not always indicate infection • The interaction between host, agent and environment must be understood and targeted in controlling disease • Resistance to antimicrobials is currently and will continue to be a problem • Have an antibiotic policy – To provide the most effective treatment for the individual patient – To advise on rational prescribing – To limit the use of prophylactic antibiotics – To delay the emergence of resistance – To minimise adverse events – To maintain a cost effective strategy