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Antibiotic therapy Vaccines for healthcare worker

Antibiotic therapy Vaccines for healthcare worker. Key points. Introduction Choice of the proper antibiotic Antimicrobial combinations Choice of the route and efficacy assessment. Sir A. Fleming: discoverer of Penicillin. Noble prize 1945. Antibiotics. PCNs Cephalosporins Carbapenem

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Antibiotic therapy Vaccines for healthcare worker

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  1. Antibiotic therapyVaccines for healthcare worker

  2. Key points • Introduction • Choice of the proper antibiotic • Antimicrobial combinations • Choice of the route and efficacy assessment

  3. Sir A. Fleming: discoverer of Penicillin Noble prize 1945

  4. Antibiotics • PCNs • Cephalosporins • Carbapenem • Monobactams • Glycopeptide • Aminoglycoside • Fluroquinolone

  5. PCN • PCN G • PCN V • Amoxicillin • Cloxacillin • Oxacillin • Ampicillin • Piperacillin • Methicillin

  6. Choice of the proper agent • Identification of the organism • Antimicrobial susceptibility • The narrowest effective spectrum • Host factors (Allergy, Age, renal and liver, site of infection, pregnancy, metabolic abnormalities)

  7. Identification of the organism • Gram stain (CSF, Pleural, synovial, peritoneal, urine, sputum) • ELISA / latex agglutination • PCR • CULTURE (best if before Abx) • Bacteriologic statistics (the application of knowledge of the organisms most likely to cause infection in a given clinical sitting)

  8. Antimicrobial susceptibility • Disk diffusion method • Epsilometer (E-test) • Minimum inhibitory conc. (MIC) • Minimum bactercidal conc. (MBC) • Specialized testing for: fastidious organisms (obligate anaerobes), Haemophilus spp, pneumococci, MRSA • Resistance mechanism of the bacteria: • eg: Staph. aureus, E. coli, Enterbacter …..

  9. Pharmacodynamic profile • Area under the curve / time curve to MIC (AUC / MIC) • Maximal serum conc. / MIC (C max / MIC) • Time during dosing interval that plasma conc. exceed the MIC (t / MIC)

  10. Conc. & Time dependent dosing • Conc. dependent (FQ, Ag)  increase in conc leads to a more rapid rate of bacterial death (i.e. large dose at long intervals) • Time dependent (-lactams, vancomycin) reduction in bacterial density is proportional to the time that the conc. exceeds MIC (i.e. sufficient dose at appropriate intervals to keep conc. above MIC)

  11. Organism A Concentration Time Organism B Organism C A : resistant; B : moderately susceptible; C very susceptible

  12. Resistance selection days Antibiotic X Antibiotic X

  13. Published data • Manuals • eg:Sanford’s • Medical letter on drugs and therapeutics • (nb: use this information within its context)

  14. Host factors • Previous history of adverse reactions • Neutrophil function  neutropenic are treated aggressively • CLL, Multiple Myeloma, asplenia  treated empirically

  15. Age • Renal function (impaired physiologic function) • Absorption • Tetracyclines • INH hepatotoxicity • Nephrotoxicity • Ag and cochlear toxicity

  16. Genetic / metabolic • Hemolysis in G6PD deficiency • DM : sulfa drugs can potentiate the sulfonylurea hypoglycemic agents • - Dextrose load • - Poor IM absorption (use IV route)

  17. Pregnancy • Safe : PCN, cephalosporin, erythromycin • Dangerous: tetracyclines (hepatic toxicity, dental discoloration) • ? metronidazole • FQ  Contrindicated • ?? rifampin, Ag, azithromyccin, clindamycin, imipenem,vancomycin, TMP • Abx dose needs to be increased?

  18. Renal and liver fx • Vancomycin & Aminoglycosides

  19. Site of infection • Optimal therapy requires concentrations > MIC at the site of infection • Meningitis • Endocarditis • Osteomylitis • Chronic prostatitis • Intraocular infections • Abscesses • Foreign body • UTI

  20. Immune system • Abx can cause immune suppression esp. in the immunosuppressed patients • Suppress monocyte transformation, phagocytosis, chemotaxis, antibody production

  21. Combinations • Some physicians use combinations for the sense of security  deleterious effects • Indications: 1) prevention of emergence of resistant bacteria : TB, staph endocarditis • 2) polymicrobial infections : abd. sepsis • 3) initial therapy: eg: Ag + piperacillin • 4)Synergism:…

  22. Synergism • For resistant organisms • Limited data to support their benefit • e.g.: PCN + Ag  Enterococcal endocarditis • Oxacillin + Ag  Staph. endocarditis • Anti-pseudomonal - lactam + Ag  Pseudomonas bacteremia • Impaired host

  23. Antagonism • Too many in vitro reports • Clinically was seen in : PCN + tetracyclines • 2 -lactams  induce  lactamases • More important in immunosuppressed pts

  24. Adverse effects • 5% of pts will have a side effect • Combinations  more cost, more adverse effects

  25. Anaphylaxis • Beta lactams are the most common ABx to cause anaphylaxis • PCN risk of anaphylaxis: 0.01% • Death occurs in 1 / 100,000 courses • 10 - 20% of pts who claim to have an allergy to PCN are truly allergic • 50% of pts with a positive skin test: reaction

  26. Anaphylaxis • PCN cross reaction with Cephalosporins • Minimum cross reaction with carbapenem  1% • No cross reaction with Aztreonam (except ceftazidime)

  27. Route • Oral  stable , mild infection (reliable pts) • IV  serious infections (sepsis) + DM

  28. Monitoring the response • Clinically • Drug levels • Lab tests

  29. Cost • If all other factors are equal, the least expensive drug should be chosen

  30. Needle stick Risk of transmission - Hepatitis B virus 30% - Hepatitis C virus 3% - HIV 0.3%

  31. HBV Vaccinerecommendations • HB vaccine offered for all HCW • Required in US (1991) • Human rights issues (what if they refused ??) • Check response after 1 month • Responders: ….. 10 IU/l • Non responders………. < 10 IU/l

  32. HBV vaccine • Does not transmit the virus • 3 shots at 0, 1, 6 months • The series is administered once • A booster shot can be given in times of outbreak conditions • If you are exposed to HBV immediate vaccination is extremely helpful

  33. HBV vaccine (cont) • You do not need to accept the vaccine • You can decline it and sign a declination form • If you are exposed to HBV or changed your mind, you can still receive it • Your employer might not offer you the vaccine if: • You are vaccinated • Have Antibodies • Contraindicated in your case

  34. HBV (cont)

  35. Response or no ??? • High risk practice • True non response vs. Waning Ab levels • One boost to differentiate • Non response: < 10 IU/l • Responders: > 10 IU/l NEJM Dec 2004

  36. To boost or not to boost ?? • Currently, there is no proof that booster injections are indicated for the first two decades after successful immunization • After 3rd decade: ???? Studies are needed J clini Virology 2003

  37. Influenza vaccine • Annually • In the fall season • even if late • 2 strains of A + 1 strain of B • No protection against other Flu like illnesses like • RSV • Para influenza • Adenovirus

  38. Influenza vaccine • Weak or no association with Guillain Barre syndrome • 1 / million • Contraindication • Previous GB syndrome • ? Egg allergy • Allergic reaction to any component

  39. Prevention - Rubella + Rubella IgG Immune _ Non-Immune MMR (avoid pregnancy x 2 m) 2 months _ _ Check titers Booster Inform patient + Immune

  40. Rubella-risk • Risk of congenital infection • 1 + 2 month: 90% • 3rd month 50% • Termination of pregnancy is usually recommended in Western countries • > 16 weeks negligible • 12 – 16 weeks: deafness can occur

  41. Congenital rubella syndrome: • growth retardation; malformations of the heart, eyes, or brain; deafness; and liver, spleen, and bone marrow problems.

  42. Prevention - Varicella • Varicella • History of chicken pox: … immune • Positive titers ….. . .. . . immune • Absent titers: not immune • Give vaccine: 2 doses, 2 months apart • Postpone pregnancy 2 m after the second dose

  43. Tetanus - Diphtheria vaccine • Once every ten years • Toxoid vaccine

  44. Peneumococcal vaccine • Indicated for all immunocompromised adults • > 65 years • 1 or 2 doses

  45. شكرا

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