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重症病患之抗生素使用原則 財團法人為恭紀念醫院 感染科  曾政尹 醫師 C.Y.T.
抗生素使用 ,[object Object],[object Object],[object Object],[object Object],[object Object]
抗生素一般使用原則 ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Choice of proper antimicrobial agent ,[object Object],[object Object],[object Object],[object Object],C.Y.T.
Golden Triangle Antimicrobial  agent Microorganism Host Immune system Microbiological profile Pharmacokinetics C.Y.T.
Host factors ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Initial Selection of Antibiotics SUSPECTED  DIAGNOSIS CLINICAL EVALUATION (site of infection, host, lab. data) C.Y.T.
Initial Selection of Penicillin-G ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Third  Generation Cephalosporins ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Indications of Third-generation Cephalosporins ,[object Object],[object Object],[object Object],[object Object],C.Y.T.
Extended-spectrum   -lactamase (ESBL)  ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],Antimicrobial Agents And Chemotherapy 1131-1136, 1989 C.Y.T.
抗生素使用 ,[object Object],[object Object],[object Object],[object Object],[object Object]
Getting It Right From Start To Finish The Role of  De-escalation Therapy C.Y.T.
De-escalation therapy ( 降階治療 ) ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
De-escalation therapy ( 降階治療 ) ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Initial Appropriate Therapy ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Local microbiological data
De-escalate ,[object Object],[object Object],C.Y.T.
Choose broad-spectrum, empiric treatment regimen based on   clinical symptoms   and   unit-specific   antibiogram data   and   guidelines .  Obtain culture prior  to antibiotic administration. Obtain and analyze microbiological data Modify regimen accordingly Reassess patient Process for Initial Appropriate Therapy C.Y.T.
Factors in Selecting Initial Appropriate Therapy ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Indications for Combination ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Initial Empiric Antibiotic Therapy ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],Am J Respir Crit Care Med, Vol. 171; 388-416, 2005 C.Y.T.
Initial Inadequate Therapy ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],1 Kollef  MH et al.  Chest  1999;115:462-474. 2 Ibrahim EH et al.  Chest  2000;118:146-155 . C.Y.T.
Appropriate Therapy Leads to Lower Mortality in Gram-Negative Sepsis <0.001 49% (47-51%) 28% (22-32%) Total <0.001 29% (23-31%) 10% (0-13%) Non-fatal <0.001 67% (63-72%) 42% (39-45%) Ultimately fatal NS 85% (71-100%) 84% (80-86%) Rapidly fatal P-value Mortality without appropriate therapy Combined data (range) Mortality with appropriate therapy Combined data (range)  Underlying Disease Bochud P-Y et al.  Intensive Care Med  2001;27:S33-S48. C.Y.T.
Mortality Associated With Initial Inadequate Therapy In Critically Ill Patients With Serious Infections in the ICU 0% 20% 40% 60% 80% 100 % Luna, 1997 Ibrahim, 2000 Kollef, 1998 Kollef, 1999 Rello, 1997 Alvarez-Lerma,1996 Initial appropriate therapy Initial inadequate therapy *Mortality refers to crude or infection-related mortality Alvarez-Lerma F et al.  Intensive Care Med  1996;22:387-394. Ibrahim EH et al.  Chest  2000;118L146-155. Kollef MH et al.  Chest  1999; 115:462-474 Kollef  MH et al.  Chest  1998;113:412-420. Luna CM et al.  Chest  1997;111:676-685. Rello J et al.  Am J Resp Crit Care Med  1997;156:196-200. Mortality* C.Y.T.
Reassess therapy when ,[object Object],[object Object],C.Y.T.
抗生素使用 ,[object Object],[object Object],[object Object],[object Object],[object Object]
Empirical Broad-Spectrum  Antimicrobial Therapy ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Hospital acquired infection  - 定義 ,[object Object],[object Object],[object Object],C.Y.T.
Patients With VAP Suffer Excess Morbidity and Mortality ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],Heyland DK.  Am J Respir Crit Care Med  1999;159:1249-1256.   C.Y.T.
Spectrum of Potential Pathogens in Hospital-Acquired Pneumonia* Based on Severity of Illness Campbell GD et al.  Am J Respir Crit Care Med  1996;153:1711-1725  * Excludes patients with immunosuppression. ** Includes severe HAP without risk factors (early onset) *** Severe HAP with risk factors (onset any time) or severe HAP without unusual risk factors (late onset) Mild-to-Moderate (With risk factors) Severe*** Core Organisms Enteric GNB Core Organisms,  Plus Anaerobes Core Organisms , Plus P. aeruginosa (Non-pseudomonal) (recent abdominal •  Enterobacter surgery; witnessed Acinetobacter •  E. coli aspiration) species •  Klebsiella •  Proteus Consider MRSA •  Serratia marcescens Haemophilus influenzae S. aureus (including MRSA if coma, head trauma, DM, renal failure) Methicillin-sensitive Legionella Staphylococcus aureus (high-dose steroids) Streptococcus pneumoniae P. aeruginosa (prolonged ICU, steroids, antibiotics) structural lung disease, Mild-to-Moderate (No unusual risks)**  C.Y.T.
HAP: risk factors for  resistant pathogens ,[object Object],[object Object],[object Object],[object Object],C.Y.T.
Risk Factors for Resistance in VAP ,[object Object],[object Object],[object Object],1 Trouillet J-L et al.  Am J Respir Crit Care Med  1998;157:531-539. 2 Lautenbach E et al.  Clin Infect Dis  2001;32:1162-1171. C.Y.T.
Risk Factors for Resistance in VAP Adapted from Trouillet J-L et al.  Am J Respir Crit Care Med  1998;157:531-539. MRSA,  P. aeruginosa ,  A. baumannii ,  S. maltophilia More sensitive bacteria than in Group 2 More resistant bacteria than in Group 3 Antibiotic-sensitive organisms (e.g., pneumococci,  H. influenzae ) MV  ≥7 days; prior use of antibiotics MV  ≥7 days; no prior antibiotics MV <7 days; prior use of   antibiotics MV <7 days;  no prior antibiotics Group 4 Group 3 Group 2 Group 1 C.Y.T.
ATS recommendations: I ,[object Object],C.Y.T.
ATS recommendations: II ,[object Object],[object Object],[object Object],C.Y.T.
血流感染 ( Bloodstream Infection) ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],Prevention and Control of Nosocomial Infections, 4 th  ed. P.281-2 C.Y.T.
Resistant Pathogens Account for High Number of Bloodstream and Nosocomial Infections Kollef MH et al.  Clin Inf Dis  2000;31(Suppl. 4):S131-S138. Coagulase-negative Staphylococci P= .001 0 10 20 30 40 50 Bloodstream  infection Nosocomial pneumonia Urinary tract  infection Invasive device present Percentage occurrence P. aeruginosa P= .002 A. baumannii P= .006 E. coli P= .023 C. albicans P= .009 Invasive device absent C.Y.T.
CVC-Associated Bloodstream Infection ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
敗血性休克 (Septic shock) ,[object Object],[object Object],- Prevention and Control of Nosocomial Infections, 3rd ed. P.714 C.Y.T.
抗生素使用 ,[object Object],[object Object],[object Object],[object Object],[object Object]
抗藥性細菌增加的原因 ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
抗生素的抗藥性 (ICU, 2004 NNIS Report)
抗生素的抗藥性 (2004 NNIS Report)
哪些抗生素的附加損害 (collateral damage) 最大 ? ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Collateral damage ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Multidrug-Resistant Organisms (MDROs) ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],- MRSA, VISA, VRSA - MRCNS MDRSP C.Y.T.
Most Frequently Reported Pathogens from ICU Patients with Nosocomial Pneumonia 1.  Pseudomonas aeruginosa 2.  Staphylococcus aureus 3.  Enterobacter  spp. 4.  Klebsiella pneumoniae 5.  Acinetobacter  spp. Richards MJ et al.  Crit Care Med  1999; 887-892. C.Y.T.
95 年 TNIS 加護病房院內感染最常見菌株前三名 ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Preventing the emergence and transmission of MDROs ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],– The prevention and control of MDROs is a national priority. C.Y.T.
[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
抗生素使用 ,[object Object],[object Object],[object Object],[object Object],[object Object]
Summary ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
De-escalation Therapy ,[object Object],[object Object],[object Object],[object Object],C.Y.T.
Considerations for choosing  empirical therapy    In vitro activity of drugs against  likely pathogens    Local  resistance  burden    Pharmacologic and pharmacodynamic properities of  antimicrobials    Safety  and  tolerability C.Y.T.
Major pathway of antibiotic excretions ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Antibiotic Therapy ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Antibiotic Therapy ,[object Object],[object Object],[object Object],[object Object],C.Y.T.
Therapy and Infection Control ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
An Art in Medicine Balance An Evidence-Based Problem: Mortality with Inadequate Therapy A Theoretical Dilemma: Concern of Resistance with Broad-Spectrum Therapy Evans RS et al.  N Engl J Med  1998;338:232-238. Gruson D et al.  Am J Respir Crit Care Med  2000;162:837-843.  Raymond DP et al.  Crit Care Med  2001;29:1101-1108. ⋆  Clinical evidence showing lack of resistance with  heterogeneous use of broad-spectrum therapy C.Y.T.
C.Y.T.
結語 ,[object Object],[object Object],[object Object],[object Object],[object Object],[object Object],C.Y.T.
Thank you for your attention !

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重症病患抗生素使用961113

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  • 5. Golden Triangle Antimicrobial agent Microorganism Host Immune system Microbiological profile Pharmacokinetics C.Y.T.
  • 6.
  • 7. Initial Selection of Antibiotics SUSPECTED DIAGNOSIS CLINICAL EVALUATION (site of infection, host, lab. data) C.Y.T.
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  • 13. Getting It Right From Start To Finish The Role of De-escalation Therapy C.Y.T.
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  • 19. Choose broad-spectrum, empiric treatment regimen based on clinical symptoms and unit-specific antibiogram data and guidelines . Obtain culture prior to antibiotic administration. Obtain and analyze microbiological data Modify regimen accordingly Reassess patient Process for Initial Appropriate Therapy C.Y.T.
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  • 24. Appropriate Therapy Leads to Lower Mortality in Gram-Negative Sepsis <0.001 49% (47-51%) 28% (22-32%) Total <0.001 29% (23-31%) 10% (0-13%) Non-fatal <0.001 67% (63-72%) 42% (39-45%) Ultimately fatal NS 85% (71-100%) 84% (80-86%) Rapidly fatal P-value Mortality without appropriate therapy Combined data (range) Mortality with appropriate therapy Combined data (range) Underlying Disease Bochud P-Y et al. Intensive Care Med 2001;27:S33-S48. C.Y.T.
  • 25. Mortality Associated With Initial Inadequate Therapy In Critically Ill Patients With Serious Infections in the ICU 0% 20% 40% 60% 80% 100 % Luna, 1997 Ibrahim, 2000 Kollef, 1998 Kollef, 1999 Rello, 1997 Alvarez-Lerma,1996 Initial appropriate therapy Initial inadequate therapy *Mortality refers to crude or infection-related mortality Alvarez-Lerma F et al. Intensive Care Med 1996;22:387-394. Ibrahim EH et al. Chest 2000;118L146-155. Kollef MH et al. Chest 1999; 115:462-474 Kollef MH et al. Chest 1998;113:412-420. Luna CM et al. Chest 1997;111:676-685. Rello J et al. Am J Resp Crit Care Med 1997;156:196-200. Mortality* C.Y.T.
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  • 31. Spectrum of Potential Pathogens in Hospital-Acquired Pneumonia* Based on Severity of Illness Campbell GD et al. Am J Respir Crit Care Med 1996;153:1711-1725 * Excludes patients with immunosuppression. ** Includes severe HAP without risk factors (early onset) *** Severe HAP with risk factors (onset any time) or severe HAP without unusual risk factors (late onset) Mild-to-Moderate (With risk factors) Severe*** Core Organisms Enteric GNB Core Organisms, Plus Anaerobes Core Organisms , Plus P. aeruginosa (Non-pseudomonal) (recent abdominal • Enterobacter surgery; witnessed Acinetobacter • E. coli aspiration) species • Klebsiella • Proteus Consider MRSA • Serratia marcescens Haemophilus influenzae S. aureus (including MRSA if coma, head trauma, DM, renal failure) Methicillin-sensitive Legionella Staphylococcus aureus (high-dose steroids) Streptococcus pneumoniae P. aeruginosa (prolonged ICU, steroids, antibiotics) structural lung disease, Mild-to-Moderate (No unusual risks)** C.Y.T.
  • 32.
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  • 34. Risk Factors for Resistance in VAP Adapted from Trouillet J-L et al. Am J Respir Crit Care Med 1998;157:531-539. MRSA, P. aeruginosa , A. baumannii , S. maltophilia More sensitive bacteria than in Group 2 More resistant bacteria than in Group 3 Antibiotic-sensitive organisms (e.g., pneumococci, H. influenzae ) MV ≥7 days; prior use of antibiotics MV ≥7 days; no prior antibiotics MV <7 days; prior use of antibiotics MV <7 days; no prior antibiotics Group 4 Group 3 Group 2 Group 1 C.Y.T.
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  • 38. Resistant Pathogens Account for High Number of Bloodstream and Nosocomial Infections Kollef MH et al. Clin Inf Dis 2000;31(Suppl. 4):S131-S138. Coagulase-negative Staphylococci P= .001 0 10 20 30 40 50 Bloodstream infection Nosocomial pneumonia Urinary tract infection Invasive device present Percentage occurrence P. aeruginosa P= .002 A. baumannii P= .006 E. coli P= .023 C. albicans P= .009 Invasive device absent C.Y.T.
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  • 48. Most Frequently Reported Pathogens from ICU Patients with Nosocomial Pneumonia 1. Pseudomonas aeruginosa 2. Staphylococcus aureus 3. Enterobacter spp. 4. Klebsiella pneumoniae 5. Acinetobacter spp. Richards MJ et al. Crit Care Med 1999; 887-892. C.Y.T.
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  • 55. Considerations for choosing empirical therapy  In vitro activity of drugs against likely pathogens  Local resistance burden  Pharmacologic and pharmacodynamic properities of antimicrobials  Safety and tolerability C.Y.T.
  • 56.
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  • 60. An Art in Medicine Balance An Evidence-Based Problem: Mortality with Inadequate Therapy A Theoretical Dilemma: Concern of Resistance with Broad-Spectrum Therapy Evans RS et al. N Engl J Med 1998;338:232-238. Gruson D et al. Am J Respir Crit Care Med 2000;162:837-843. Raymond DP et al. Crit Care Med 2001;29:1101-1108. ⋆ Clinical evidence showing lack of resistance with heterogeneous use of broad-spectrum therapy C.Y.T.
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  • 63. Thank you for your attention !