JP Pretorius

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JP Pretorius

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Title: JP Pretorius

1
PROPHYLACTIC ANTIMICROBIAL THERAPY

JP Pretorius
Principal Specialist Surgeon
Dept of Surgery and Division of Intensive Care
University of Pretoria
Pretoria Academic Hospital

2
Outline Red hot terminology

Classification of wounds
Why is there a need to get it right first time?
Early appropriate therapy
Source control
Definitions and terminology
Surgery and antibiotic prophylaxis
What is collateral damage
Empiric therapy (educated 1st choice)
Directed therapy (MCS results)
De-escalation (adjusted choice)
Stopping / Discontinuing therapy
Community acquired infection
Health Care Associated infection
Nosocomial infection
Changing trends in antibiotic resistance
Choices for empiric therapy
Choices for pathogen defined therapy (directed)
Doses / Duration / Pk / Pd / Efficient
administration

3
INDEPENDENT PREDICTORS OF INFECTION

Preoperative shock
Number of organs injured
Concomitant central nervous system injury

4
Determinants of surgical wound infection
Microbial concentration and virulence
Foreign material
Injury to wound tissues
Resistance to peri-operative ABs
Risk fo surgical wound infection

General/Local host immunity
Peri-operative antibiotics
5
Risk of Surgical Site Infectionand Degree of
wound contamination

Altemeier classes 1 4
Class 1 Clean surgery 1 2 risk
Class 2 Clean contaminated surgery 5 15 risk
(elective colectomy or hysterectomy)
Class 3 Contaminated surgery 15 30 risk
(enterotomy with spillage)
Class 4 Dirty surgery gt 30 risk (established
infection ie intra-abdominal abcess)
Simplistic but still valid!

6
Patient characteristics associated with
increased risk for surgical site infection

7
Patient characteristics associated with increased
risk for surgical site infection

Extremes of age
Diabetes / periopeative hyperglycaemia
Concurrent tobaco use
Remote infection at time of surgery
Obesity
Malnutrition
Low preoperative S-albumin
Concurrent steroid use
Prolonged preoperative stay
Prior site irradiation
Colonization with S aureus

8
Procedural factors associated with increased risk
for surgical site infections
?
9
Procedural factors associated with increased risk
for surgical site infections

No preoperative antiseptic showering
Shaving of site night prior to procedure
Use of razor for hair removal
Improper preop skin preparation
Improper antimicrobial prophylaxis
Delayed redosing of ABs in prolonged cases
Inadequate OR ventilation
Increased OR traffic
Break in sterile technique and asepsis
Perioperative hypothermia / hypoxia
Poor surgical technique

10
Major Pathogens in Surgical Wound Infections
?
11
Major Pathogens in Surgical Wound Infections

S aureus
20 of infections
Coagulase (-) staphylococci 14
Enterococci 12
E coli
8
P aeruginosa 8
Enterobacter spp 7
Proteus mirabilis 3
Klebsiella pneumoniae 3
Other streptococcal spp 3
Minimal infective inoculum - gt 105 organisms
Foreign bodies reduce this by 3 logs

12
Typical Microbiologic Flora at Surgical Sites
S aureus, CoNS S aureus, CoNS S aureus, CoNS S
aureus, CoNS, streptococci S aureus, CoNS,
streptococci, GNR S aureus, CoNS, streptococci,
GNR S aureus, CoNS, strep pneumoniae GNR S
aureus, CoNS GNR, anaerobes GNR, anaerobes GNR,
anaerobes GNR, streps, oropharygeal anaer S
aureus, streps, oroph anaer GNR, enterococ, group
B strep GNR

Placement of prostheses, grafts, implants
Cardiac
Neurosurgery
Breast
Ophthalmic
Orthopaedic
Noncardiac thoracic
Vascular
Appendectomy
Biliary tract
Colorectal
Gastroduodenal
Headneck intraoral
Obstetric Gyneacological
Urologic

13
Antibiotic prophylaxis for longer than 24 hours
not only has no benefit, but is now recognized to
be detrimental
14
Unfortunately.. reducing prophylaxis to less
than 24 hours has not become popular despite
evidence that prolonged prophylaxis increases the
risk of nosocomial bloodstream infections. It is
imperative for surgeons to modify their practices.
15
Current recommendation for all elective surgical
procedures

Single-dose prophylaxis with a first- or second
generation cephalosporin - even in
Cardiac-
Vascular-
Orthopedic-
Neurosurgical procedures (where a 24 hour
regimen has been traditional)

16
EVENa SINGLE dose of antibiotic
administered appropriately, increases the risk of
such nosocomial infections as 1. Pneumonia2.
Antibiotic associated colitis
17
AND Intraoperative redosing is prudent
if1. the operation gt 3hrs2. blood loss gt
1.5L Once the incision is closed, parenteral
antibiotics no longer have an impact on the risk
of infection! Prolonged prophylaxis sets the
stage for emergence of resistant organisms
18
According to reports from the Centers for Disease
Control

Antibiotic prophylaxis may be administered
appropriately based on the patients RISK FACTORS
Abdominal procedure
Any operation gt 2 hrs
Contaminated or dirty field
gt 3 comorbid medical illnesses
Stratification done by
Number of risk factors present
Degree of wound contamination

19
The incidence of wound infection increased
significantly as the number of risk factors
increased

1 risk factor dirty wound 7 wound infection
rate
4 risk factors the same dirty wound 27 wound
infection rate

20
Published Guidelines for Antibiotic Prophylaxis
in Surgical patients

Single dose prophylaxis
1st Generation Cephalosporin (Cefazolin) for most
procedures (Workhorse)
Multiple dosing with Cefazolin
48 hrs in cardiac cases
24 hrs in vascular cases
The AB chosen, must cover the spectrum of
expected organisms. eg Single dose 2nd generation
cephalosporin for abdominal trauma, appendectomy,
colorectal procedures
Anti-MRSA drugs used only for prophylaxis on
documented incidence of surgical site infections
in your hospital (Condon threshold MRSA gt 20 )

21
RECENTLYThe Medical Letter on Drugs and
Therapeutics recommended that multiple doses may
be inappropriate for ANY surgical prophylaxis!!!!
22
eg Prophylaxis of Endocarditis

The less is more trend reflected by the AHA
recommendations
Most cases of endocarditis are not attributable
to an invasive procedure
Cardiac conditions are stratified in relation to
endocarditis risk as high / moderate /negligible
Overall fewer procedures require prophylaxis
When using prophylaxis, prescribe fewer
antibiotics and for shorter terms

23
Timing of prophylaxis

Burke 1961 the surgical wound is best protected
when antibiotics are administered before the
incision is made.
Classen 1992 30 yrs later timelines for
administration - still a major problem!!!!
New York States peer-review programme 1996
only 86 received ABs although indicated
44 different ABs used for 2256 patients
Nichols 1972 some standardization for colon
preparation pre-op oral neomycin, erythromycin
or metronidazole
lt 2/3 received either oral or timely parenteral
AB before elective colon surgery

24
Timing continued -

Liberal definition of TIMELY 2 hrs up to the
time of the skin incision
NY State study only 61 received timely AB
prophylaxis
In 26 ABs were administered prematurely
Adequate tissue concentrations of ABs at time of
skin incision 46 of aortic surgery patients
- 73 of colectomy patients
- 60 of hip surgery patients

25
Penicillin Allergy

Serious penicillin allergy is less common than
medical records portray
Uncritical history taking, labels patients who
are not penicillin allergic
Epidemiologic studies show incidence of 7/1000 of
general population (anaphylactic allergy to
penicillin)
First reaction is worst
Cross-reactivity between ceph and pen allergy is
only about 5. Thus can give ceph, provided it is
not an anaphylactoid reaction
Childhood pen allergies can be outgrown
Critically ill patients may be anergic and unable
to react

26
Hospital Infection Control Practices Advisory
CommitteeRecommendations for Surgical
Antimicrobial prophylaxis

Administer AB only when indicated select based
on published recommendations for a specific
operation. Assure efficacy against most common
pathogens
Administer AB intravenously, timed to ensure
bactericidal serum and tissue concentrations when
the incision is made
Maintain therapeutic concentrations during
operation and, at most, a few hours after closure
Elective colorectal operations mechanical
preparation with enemas, cathartic agents,
non-absorbable oral ABs the day before surgery
in addition to timely IV antimicrobial drugs.
High risk caesarean section patients, administer
IV ABs immediately after cord is clamped

27
The keys to rational antibiotic prophylaxis in
surgical patients include1. Timely and
accurate diagnosis2. Rapid and definitive
therapy3. Astute differentiation of infection
from contamination and sterile inflammation
28
Definitions as an aid to planning prophylaxis

Contamination presence of pathogenic
microorganisms on normally sterile tissue without
an inflammatory response requires only a single
dose off antibiotic for prophylaxis
Infection invasion of a pathogenic microorganism
into normally sterile tissue with a local
inflammatory host response necessitates
therapeutic antibiotics
Antibiotics are NOT APPROPRIATE for sterile
inflammation due to a noninfectious trigger, such
as severe tissue injury

29
Thank you !
30
Example Endocarditis Prophylaxis

Negligible mitral valve prolapse with
midsystolic click, no regurgitation, no thickened
leaflets
- implanted non-valve devices (pacemakers and
defibrillators)
Moderate single dose ampicillin
High ampicillin with gentamycin
Avoid broad-spectrum agents eg 3rd generation
Cephalosporins!!!!!!

31
Example Endocarditis ProphylaxisGastrointestinal
and Genitourinary procedures

Moderate risk single oral dose of amoxicillin or
IV ampicillin
High risk an aminopenicillin with gentamycin 30
minutes before surgery
another dose of ampicillin alone 6 hrs
thereafter
AIM maximal coverage against enterococci, the
major pathogens in endocarditis folowing GI/GU
surgery.

32
Optimising Antibiotic Treatment in Serious
Infections
33
Intra-abdominal InfectionTHE PROBLEM

Important cause of ICU morbidity and mortality.
ICU admission for IAI 30 succumb.
Tertiary peritonitis gt50 mortality.
Association between progressive organ dysfunction
and occult intraperitoneal infection.
Marshall JC CCM 2003

34
2. Intra-abdominal Infection.THE PERITONEAL
CAVITY

Normally lt100ml of fluid, with scattered
macrophages and lymphocytes.
Diaphragmatic movement / contraction generates
negative pressures.
Peritoneal fluid moves upward towards specialized
fenestrae in diaphragmatic peritoneum, draining
into the lymphatic system.
Vigorous inflammatory response
increased vascular permeability
protein-rich exudate
cytokines and chemokines
influx of monocytes and neutrophils

35
3. Intra-abdominal InfectionTHE INFLAMMATORY
RESPONSE

Tissue factor expression of peritoneal
macrophages.
Coagulation cascade is activated.
Accelerated generation of fibrin.
Fibrin polymerizes to form adhesions and capsules
of abscesses.
Rich somatic nerve supply thus severe pain.
Pain localises to area of maximal inflammation.
Normal innate immune response is rapid and
effective
a) Neutrophil phagocytosis is impaired
by complicated peritonitis.
b) Fibrin deposition can impede
microbial clearance.

36
4. Intra-abdominal InfectionPATHOGENESIS

Disruption of adjacent GIT
Spillage of complex indigenous flora.
Stomach and Duodenum
Sterile
Sparse gm-positive organisms,
lactobacilli and
occasionally Candida.
Proximal small bowel.
Gm-negative organisms
Distal small bowel and colon
Anaerobes
Importance in stable patterns of
intestinal colonization.
(Colonization resistance)
CANDIDA.???

37
5. Intra-abdominal InfectionPATHOGENESIS cont.

In the critically ill normal colonization
resistance is disrupted over time.
Due to anti-anaerobic antibiotics
Leads to colonization by Candida and
vancomycin-resistant Enterococci.
Explains the typical flora of tertiary
peritonitis.
Enterococci more often in post op peritonitis
Nasal MRSA colonization risk factor for MRSA
peritonitis.

38
6. Intra-abdominal InfectionPATHOGENESIS
SUMMARY.

Acute loss of integrity of gut wall acute
spillage with generalized peritonitis.
Slow leakage of gut content inflammatory
response with abscess formation.
After both vigorous systemic response leading
to acute organ system dysfunction.

39
Proportions of Bacterial Isolates ()in
Community-acquired Peritonitis
Dupont H. Antimicrob Agents Chemother
2000442028-33 Roehrborn A. Clin Infect Dis
2001331513-9
40
Proportions of Bacterial Isolates () in
Nosocomial or Postoperative Infections
Montravers P et al. Clin Infect Dis.
199623486-494 Dupont H. Antimicrob Agents
Chemother 2000442028-33 Roehrborn A. Clin
Infect Dis 2001331513-9
41
Microbiology

Gram negative aerobic organisms are associated
with acute lethality
Anaerobic organisms predispose to abscesses
Onderdonk Infect Immunol 1997
Eradication of anaerobes predisposes to
overgrowth of E.coli and colonization with
Candida spp and VRE
Berg Infect Immunol 1981

Thomakos
Chemotherapy 2003

Donskey NEJM 2000

42
Classification of Peritonitis

Primary peritonitis
Primary bacterial peritonitis in nephrotic or
cirrhotic patients, primary pneumococcal,
streptococcal peritonitis
Granulomatous peritonitis (Mycobacterium spp.,
Histoplasma spp.)
Secondary peritonitis
Perforation of the GIT postoperative,
spontaneous or traumatic
Infection of pelvic or intraabdominal viscus with
peritoneal involvement
Bowel wall necrosis
Continuous ambulatory peritoneal dialysis
Tertiary peritonitis
Peritonitis in critically ill patients that
persists or recurs at least 48hrs after
apparently adequate surgical management.
Differentiated by more resistant organisms and
poor response to surgery and antibiotics

Wittmann DH. World J Surg 199014145-7
Marshall CCM 2003
43
Classification of peritonitis

Severity
Outcome is determined by age, delay in diagnosis
and therapy, inappropriate therapy, APACHE,
anatomic source of infection, presence of
resistant pathogens
Barie
Curr Opin Crit Care 2001
Published trials of antibiotic therapy have
enrolled patients with a mean APACHE of 8

Barie Arch
Surg 1997
Severe infection may reasonably be defined as an
APACHE 15

44
Microbiology of Peritonitis
Primary Peritonitis Secondary Peritonitis Tertiary Peritonitis
Gm-negative bacteria Gm-negative bacteria Gm-negative bacteria
Eschecheri coli E. coli 32-61 Pseudomonas
Klebsiella Enterobacter 8-26 Enterobacter
Klebsiella 6-26 Acinetobacter
Proteus 4-23
Gm-positive bacteria Gm-positive bacteria Gm-positiv bacteria
S. aureus (MRSA) Enterococci 18-24 Enterococci
Enterococci Streptococci 6-55 Coagulase-negative
Pneumococci Staphylococc 6-16 Staphylococci
Anaerobic bacteria
Bacteroides 25-80
Clostridium 5-18
Fungi 2-15 Fungi Candida
45
Tertiary Peritonitis THE DANGER

Unsatisfactory response to both antibiotics and
surgical source control measures.
Flora similar to flora of upper GIT of the
critically ill.
Flora common causes of nosocomial ICU acquired
infections.
? Role for translocation.
? Antibiotic pressure
Mortality gt 50
No optimal therapeutic strategy

46
The Microbiology of Tertiary Peritonitis

Most surgeons do not dare to leave these patients
without antibiotics before the decision to
reoperate
These interval antibiotics may have a major
impact on the microbiology and the efficacy of
subsequent treatment. (Although many other
factors contribute to survival)
The microbiology of postoperative peritonitis
differs significantly from that of
community-acquired disease, and specific
antibiotic therapy is required, DESPITE the
doubtful impact on survival.
The treatment of CAIAI by 3rd generation
cephalosporins and metronidazole is not adequate
for tertiary peritonitis because
gm() bacteria are not covered
gm() bacteria outnumber gm(-) bacteria
Enterobacter which is most threatening, is
also not sufficiently covered.
Roehrborn A, CID 2001

47
Intra-abdominal InfectionDIAGNOSIS

Difficult in the critically ill.
History unobtainable.
Level of conciousness masks physical examination.
Important Clinical setting
Unexplained signs of sepsis
Unexplained organ
dysfunction
Radiographic studies the
whole range.

48
Appropriate Treatment
Goal directed resuscitation and organ
support Early appropriate parenteral
antibiotic Surgical procedure that controls the
source of infection Avoid or minimize blood
transfusion Glucose control, steroids, ARDS-NET
ventilation Early enteral nutrition Xigris /
Immunomodulation Monitoring Mazuski JE.
Surgical infections 20023161-173

Van den Berghe NEJM 2002
Rivers
NEJM 2001
Annane JAMA2002

ARDS NET
Marik CCM 2002

Chang Vox Sang 2000

Bernard NEJM 2001
49
Appropriate TreatmentSource Control

Drainage (open vs percutaneous)
Debridement (early vs. delayed)
Diversion of bowel content.
Restore intestinal continuity.
Open abdomen techniques.
Intra-abdominal pressures.
Planned relaparotomy.
Marshall JC, CCM 2003 3182228

50
Appropriate TreatmentSelecting an Antibiotic
Regimen

Consider patient specific toxicity.
Cost.
Local microbiological surveillance for resistance
patterns
? Duration of treatment
Adequate source control adjuvant
treatment for
5 - 7 days.
? Role of anti-enterococcal therapy
? Role of antifungal therapy
? Role of antibiotic therapy in tertiary
peritonitis does it
contribute.
Resistance to common empiric regimens.
Narrow spectrum agents according to MCS
Avoid anti-anaerobic activity.

51
Principles of Antibiotic Therapy

Initiated as soon as the diagnosis established
and surgery planned
Early administration
Parenteral route
AB must differ from antibiotic prophylaxis used
in the unit

Mazuski Surgical
infections 2003

AB must target Enterobacteriaceae and anaerobes
directly responsible for the immediate prognosis
and development of abscesses
Bartlett JG. Med Clin North Am. 199579599-617
AB should also target ß- lactam susceptible gram
pos cocci
Solomkin IDSA Guidelines CID 2003
52
Defining Appropriate Therapy
Considerations in determining appropriate therapy

Site of perforation
Dose and dosing frequency( PK/PD)
Prior antibiotic treatment
Nosocomial / Health Care Associated / Community
Acquired.
Prevalent pathogens (ESBL, acinetobacter)
Severity

Raymond DP et al. Surg Infect 2002 Kollef MH.
Clin Infect Dis 200031(Suppl 4)
53
Appropriate versus Inappropriate Empiric Therapy
for IAI Mortality
In a retrospective analysis, mortality was
substantially higher for IAI patients who receive
inappropriate versus appropriate therapy.
Bare M, et al. Presented at the 12th European
Congress of Clinical Microbiology and Infectious
Diseases, Milan, Italy 2002.
54
Effect of Inappropriate Initial Antibiotic Therapy
Retrospective study (1999-2001) 20 hospitals in
Germany Assessment of appropriateness of initial
AB and outcome
5 11 27 57
4 3 12 81
Resolved with initial or stepdown therapy
Resolved with second-line therapy
Resolved after reoperation
Increased length of stay 14.4 versus 16.8 days
Appropriate
Inappropriate
Death
Sendt W. et al. IDSA 2002. P 566
55
Appropriate Versus Inappropriate Therapy Cost
of Hospital Stay
Appropriately treated IAI patients incurred
significantly lower hospitalization costs versus
inappropriately treated patients 348 patients
from three Scottish hospitals from 1993 to 1997
Davey P, et al. Presented at the International
Society of Pharmacoeconomics and Outcomes
Research Sixth Annual International Meeting May,
2001.
56
Kollef MH, et al. Chest. 1999115462.
Inadequate Antimicrobial Treatment Effect on
Mortality

Prospective cohort study by Kollef et al
2000 patients admitted over an 8-month period to
a 19-bed medical ICU and an 18-bed surgical ICU
Study aim to determine if inadequate empiric
antibiotic therapy is a risk factor for mortality
Sponsors CDC, Bayer

57
Definitions

Inadequate antibiotic therapy was defined at the
time culture and susceptibility reports became
available
Absence of antimicrobial agents directed at a
specific type of organism (eg, absence of
antifungal agents for Candidemia)
Administration of an antibiotic to which the
organism was resistant (eg, use of ceftazidime
for Klebsiella with ceftazidime MIC gt256)

58
Impact of Inadequate Empiric Choice
Antimicrobial Treatment Mortality
Inadequate 52
Adequate 12
RR 4.3 (95 CI, 3.5 to 5.2 p lt0.001)

Multivariate analysis inadequate antibiotic
treatment was the most important independent risk
factor for death

Kollef MH, et al. Chest. 1999115462.
59
More Evidence

At least 5 other studies have shown comparable
findings
Delays in receipt of appropriate therapy have
also been associated with excess hospital
mortality
These concepts have been incorporated into the
official statement of ATS and IDSA on management
of hospital-acquired pneumonia (Am J Respir Crit
Care Med. 2005171388)

60
Why do we get empiric therapy wrong?

The most frequent reason is resistance to the
antibiotic chosen

61
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62
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63
Recent Publications confirm resistance linked to
overuse of traditional antibiotics
Neither third-generation cephalosporins nor
quinolones appear suitable for sustained use in
hospitals as workhorse antibiotic therapy.
64
What is collateral damage?

Adverse effects of antibiotics on ecology of
normal flora of gut or skin
Selection of drug-resistant organisms
Unwanted colonization or infection with MDRs
Third generation cephalosporins and quinolones
are the most frequently implicated (VRE, C
difficile, ESBL K pneumoniae, beta-lactam
resistant Acinetobacter spp)
Quinolones (MRSA, resistant Ps aeruginosa
Neither 3rd generation cephalosporins nor
quinolones appear suitable as workhorse
antibiotics in hospitals.

65
How do we get resistant organisms in a hospital?
Horizontal Transfer Via hands
Transfer of Patient from Another facility
Resistant Organisms Selected By antibiotics
Transfer of Resistance Genes
66
The Growing Resistance Problem
67
The Growing Resistance ProblemMechanisms of
resistance

Altered balance of accumulation (impermeability
and efflux)
Loss of porin protein channels in outer
membrane (All ABs except aminoglycocides)
Acquired efflux pumps to eject antibiotics (may
be broad or narrow spectrum)
Enzymic inactivation
Beta-lactamases (pen, ceph, carba)
Aminoglycocide modifying enzymes
Alteration of target
Penicillin-binding proteins (beta-lactams)
Ribosomal methylation (Macrolides)
DNA gyrase mutation (Floroquinolones)

68
The Growing Resistance Problem

Well documented and increasing
Restrict treatment options
Result in clinical failures
Some encoded by chromosomally located genes
limiting potential for spread to other bacteria
Some encoded by plasmids and transposons
facilitating spread to other bacterial species
Induction a reversible regulatory process due
to an inducer initiating eg enzyme synthesis
(AmpC beta lactamase in Enterobacter spp)
Selection an irreversible process individuals
within a mixed population (eg spontaneous mutants
producing the same AmpC beta lactamase) increase

69
Resistance Due to Selection
Spontaneous mutation occurs in the absence of
drug selection in a sensitive population
Sanders CC, Sanders WE. J Infect Dis
1986154792-800
70
ESBLs

Extended
Spectrum
Beta-
Lactamases

71
ESBLs

First described in Klebsiella
10-30 of most enteric Gram negative bacilli are
now ESBL producers
Leads to resistance to third generation
cephalosporins plus many other classes
Biggest risk factor is third generation
cephalosporin use

72
Challenges in Clinical Management of
Extended-Spectrum ß-Lactamases (ESBLs) in Enteric
Gram-negative Bacilli

ESBLs
Enzymes capable of hydrolyzing all ß-lactams
(penicillin, cephalosporins, monobactam) except
Carbapenems
Can be produced by all enteric bacilli (GI tract
is common reservoir) especially E.coli and K.
pneumoniae
Risk factors age gt65 prior cephalosporin or
quinolones use healthcare exposure
Often missed in routine in-vitro susceptibility
testing
Rapid wide dissemination horizontal transfer
by plasmids (among gram-negative bacilli) and
between hospitals/communities
Carbapenem is the only reliable and highly
effective agent in treating infections caused by
ESBL-producing Enterobacteriaceae
Many ESBL-producing Enterobacteriaceae are
multi-drug resistant
Fluoroquinolone, aminoglycoside,
trimethroprin-sulfamethoxazole
Treatment failures often observed with
ß-lactam/ß-lactamase inhibitor combination, even
when they are susceptible in-vitro
Carbapenem use independently associated with
decreased mortality

Paterson DL et al Clin Infect Dis 20033931-37
Paterson DL et al. Ann Intern Med
200414026-32 Warren R et al. Clin Micro Infect
2004 10(Suppl3)188 Gold HS et al. NEJM 1996
3351445-1452
73
Patient Selection

Contamination vs. infection may often be a gray
area
For example where there is
Extensive contamination shortly pre-op
Infection of an abdominal viscus removable by
surgery
Antibiotics can be given for 24 hrs or less in
traumatic
perforations with early operation
Fabian Surgery1992

Bozorgzadeh Am J Surg
1999

Kirton J
Trauma 2000
This should be similar with iatrogenic
perforation and also
possibly with early repair of gastro duodenal
perforation
Schein Br J
Surg 1994

74
Patient Selection

Consensus is that treatment is necessary for
Colonic perforation gt 12hrs
Gastro duodenal gt 24hrs
Similarly Class 2 evidence that antibiotics are
necessary for 24hrs or less for acute or
gangrenous appendicitis and cholecystitis without
perforation or infected peritoneal fluid
Andaker Acta Chir Scand !987

Schein Br J Surg 1994

75
Duration of Therapy

5-7 days has been the recommended duration

Bohnen Arch Surg 1992
Protocol directed therapy i.e.2 days for limited
infection
5
days for extensive infection
Have been as successful as historical controls
Andaker Acta Chir Scand
!987
Schein Br J Surg 1994
Therapy directed to clinical response is
successful and limits duration

Lennard Ann
Surg 1982

Smith J hosp Infect 1985

Taylor Am Surg 2000

76
Duration of Therapy

Persistence of signs of sepsis indicates a need
for surgical intervention, not prolonged
antibiotics

Lennard Ann Surg 1982

Lennard Arch Surg
1980
There is limited data that prolonged courses
might work where source control cannot be
achieved
Visser Eur J Surg 1998
High cost in terms of resistance

77
Antibiotic Regimens

Mild to moderate community acquired infection
amoxicillin / clavulanate
cefuroxime ceftriaxone cefotaxime /
metronidazole
Severe community acquired infections or
nosocomial sepsis
amoxicillin / clavulanate aminoglycoside
piperacillin / tazobactam
carbapenems
cefepime metronidazole
cipro -levofloxacin metronidazole
aminoglycoside metronidazole or clindamycin

78
Antibiotic Regimens

There is little guidance in the literature on
which regimen is superior
Antimicrobials have been designed to test
equivalence and most patients entered into
studies have had non-severe community acquired
infections
Since most regimens appear to be equivalent, cost
considerations, toxicity and likely organism are
more important considerations

Solomkin CID 2003 Mazuski Surgical Infections 2002
79
Antibiotic Regimens

The expanded gram negative spectrum of some
agents confers no advantage in CAIAI and may
contribute to increased resistance
Agents routinely used to treat nosocomial sepsis
in the ICU should not be used for CAIAI

Solomkin CID 2003 Mazuski Surgical Infections
2002 Shlaes CID 1997 McGowan New Horiz 1996
80
Antibiotic Therapy

Enterococci controversial
Treatment failure due to enterococci seems more
common in a higher risk group age APACHE, non
appendiceal sepsis, post operative or nosocomial
infection
Mazuski Surgical Infection
2002
Sitges-Serra Br J Surg 2002

Linden
Curr Infect Dis Rep 2003
Routine coverage for enterococci is not necessary
for CAIAI. They should be treated when cultured
from patients in health care settings

Solomkin CID
2003

81
Monotherapy with a Broad-Spectrum Beta-Lactam Is
as Effective as Its Combination with an
Aminoglycoside in Treatment of severe Generalized
Peritonitis a Multicenter Randomized Controlled
Trial.

H. DUPONT, C. CARBON, and J. CARLET for THE
SEVERE GENERALIZED PERITONITIS STUDY GROUP.
Antimicrobial Agents and Chemotherapy, Aug. 2000,
p. 2028-2033.

82
Aminoglycosides in Peritonitis

The 1980s - ? Synergism
- lack of broad spectrum
beta-lactams
Recent literature reviews no clear evidence to
support the use of aminoglycosides for the
treatment of peritonitis.
Aminoglycoside activity is reduced by
intra-abdominal acidosis and hypoxia, and the
presence of drug binding purulent debris.
Despite the marked post-antibiotic effect on
gm(-) bacilli, no study has proven this for
intra-abdominal infection.
Doubt about synergism with beta-lactams the
emergence of resistant strains such as Ps
aeruginosa is not prevented.
Increased incidence of nephrotoxicity.

83
Increasing Antimicrobial Resistance among
Pathogens Causing Hospital-Onset Infections
3rd generation cephalosporin- resistant
Klebsiella pneumoniae
Fluoroquinolone-resistant Pseudomonas aeruginosa
Non-Intensive Care Unit Patients Intensive Care
Unit Patients
Source National Nosocomial Infections
Surveillance (NNIS) System
12 Steps to Prevent Antimicrobial Resistance
Hospitalized Adults
84
Open Management of the Abdomen and Planned
Reoperations in Severe Bacterial Peritonitis.

Despite this approach, mortality continues to be
high, (42 in hospital)
Both short and long term morbidity are
appreciable.
(particularly the number of abdominal wall
defects)
Value of this technique rests on the fact that
other conventional surgical methods often fail to
control severe bacterial peritonitis.

85
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87
Antibiotics and Pancreatic Necrosis

Death from acute severe pancreatitis results from
infection and MODS late in the course of illness.
Necrotising pancreatitis involving at least one
third of the organ, are at highest risk of
secondary infection and death.
Based on recent studies, early antibiotic
prophylaxis in patients with necrotising
pancreatitis has been suggested and most
practitioners use imipenem for this
task.????????????

88
There is general agreement that the development
and extent of pancreatic necrosis are the most
important indicators of disease severity
Necrosis correlates with length of
hospitalisation, development of complications,
numeric systems and death.
89

Challenges of caring for the patient with severe
pancreatitis in the critical care environment.
Timing / indications for admission and
monitoring in the Intensive Care or High Care
Unit.
Should patients with SAP receive prophylactic
antibiotics?
The role of nutritional support in the
management of patients with SAP.
What is the role of surgery in the management of
patients with SAP - indications - optimal
timing - less invasive approaches
Interventions for gallstone pancreatitis
Targeting the inflammatory response in patients
with SAP
Nathens CCM 32 (12) 2004

90
Infected Necrosis

Definitions of pancreatic infections
Pancreatic infection
Infected necrosis
Pancreatic abscess
Infected pancreatic pseudocyst
The incidence of infection correlates with the
presence of intra- and extrapancreatic necrosis
General infection rate of pancreatic tissue 7-12
80 of deaths from acute pancreatitis due to
septic complications

91
Diagnosis of infective necrosis

Difficult to distinguish sterile from infected
necrosis
Distinction is important, infected necrosis
without intervention - 100 mortality
CT-guided FNA - sensitivity 90
- specificity 99
continue ...

92
Diagnosis of infective necrosis

FNA is recommended for patients with acute
necrotizing pancreatitis whos clinical
condition
Deteriorate
Fail to improve despite progressive supportive
care
Surveillance aspiration should be repeated when
clinically indicated

93
?-amylase pancreatic lipase CRP, LDH
Ulm Protocol for treatment of AP
MILD AP Intestinal Edematous pancreatitis Daily
CRP US ? Biliary lithiasis Impacted stone ??
EPT After AP Laparoscopic CCE
SEVERE AP Necrotizing Pancreatitis ICU treatment
antibiotic prophylaxis Daily CRP, IL-8,
procalcitonin, Apache II scoring
Increasing severity ? cCT Clinical sepsis
FNA
Negative Sterile necrosis Nonsurgical management
Positive Infected necrosis Surgical management
Responders ? Definitive Conservative treatment
Non responders to ICU Clinical sepsis Surgery
Necrosectomy closed Lavage / open packing
94
QUESTION 2 SHOULD PATIENTS WITH SEVERE ACUTE
PANCREATITIS RECEIVE PROPHYLACTIC
ANTIBIOTICS?Recommendations 1. Do not
administer prophylactic systemic antibacterial
or antifungal agents routinely for patients
with necrotising pancreatitis. 2.
Routine selective decontamination of the gut
should not be used for necrotising
pancreatitis. 3. SDD is promising and further
study is warranted in SAP.
95
How can we get AB Rx right?

The problem -- How to ensure adequate (early
appropriate) yet not excessive use of
antimicrobials.
-- a liberal
protective approach vs restrictive antibiotic
control
High risk patients demand liberal empiric use of
broad-spectrum antimicrobials to reduce the risk
of morbidity and mortality due to nosocomial
infections.
The use and abuse of broad-spectrum agents,
prescribed to treat the critically ill,
dramatically increases the prevalence of MDR
pathogens.
MRSA
VRE
ESBL producers - Ps aeruginosa, Acinetobacter,
Klebsiella, Enterobacter
Candida

96
How can we get ABRx right?

STRATEGISE!!!
Close examination of a unit specific antibiogram
to help devise empiric regimens with the greatest
likelihood of covering the organisms posing the
greatest risk.
Computer-assisted antimicrobial decision-support
systems to
Improve antimicrobial selection
To control costs
To decrease emergence of resistance
A patient specific antibiogram.

97
How can we get ABRx right?

STRATEGISE!!!
CPIS as an objective measure to guide
antimicrobial therapy in patients with pulmonary
infiltrates.
Invasive management or diagnostic strategy based
on bronchoscopic sampling.

98
Ertapenem

The third commercially available carbapenem
Activity similar to imipenem or meropenem except
lacks activity against
Pseudomonas aeruginosa
Acinetobacter
Enterococci
Stenotrophomonas.
Highly active against ESBL producing organisms
Conventional dose is 1 gram q 24 hr IV

99
Carbapenem Classification
GROUP 1 Carbapenems (community acquired infections, early hospital acquired infections, non- pseudomonal infections) GROUP 2 Carbapenems (hospital acquired infections pseudomonas activity) GROUP 3 Carbapenems (hospital acquired infections Pseudomonas and MRSA activity)
INVANZ TIENAM Meropenem Doripenem CS-023 ?

Pseudomonas-sparing carbapenem (INVANZ) is ideal
for most community-acquired polymicrobial
infections
Pseudomonas coverage is not required in most
community-acquired infections
Reduces antibiotic pressure on selecting
MDR-Pseudomonas
Spare the use of anti-pseudomonal carbapenem in
community setting

100
Ertapenem

Activity excellent against Enterobacteriaceae and
other fermenters, anaerobes and ß- lactam
susceptible enterococci Livermore
JAC 2003
Solomkin Ann Surg 2003
633 patients moderate to ? severe peritonitis
50 complicated appendicitis randomized to
receive ertapenem 1g dly vs. tazocin 3.375g 6hrly
This showed equivalence -favourable responses
were seen in 19/26(vs.23/26) patients in whom
pseudomonas was cultured and in 50/56(vs24/37) in
whom enterococci were cultured

101
Ertapenem vs. Piperacillin/Tazobactam Over 90
Success Rate at End of IV Therapy
100 80 60 40 20 0
92
Ertapenem 1 g once a day (n203)
88
87
81
Piperacillin/Tazobactam 3.375 g every 6 hours
(n193)
Success rate was defined as clinical and
microbiologic resolution of the index infection
requiring no additional antimicrobial therapy.
Success rate,
Data computed from statistical model adjusted for
strata.
End of IV Therapy (approximately 8 days)
Final Assessment (test of cure, primary endpoint
46 weeks post-therapy)
Solomkin JS et al. Ann Surg 2003237235-245.
102
Ertapenem vs. Piperacillin/Tazobactam High
Per-Pathogen Microbiologic Response Rates at Test
of Cure (46 weeks post-therapy)
Pathogens in the B. fragilis group include B.
caccae, B. distasonis, B. eggerthii, B. merdae,
B. fragilis, B. ovatus, B. thetaiotaomicron, B.
stercoris, B. vulgatus, and B. uniformis. n/N
refers to the number of isolates with a favorable
response/total number of isolates.
103
Ertapenem vs. Piperacillin/Tazobactam Showed
Excellent Efficacy in Microbiologically Evaluable
Subgroup
Piperacillin/Tazobactam 3.375 g every 6 hr
(n/N) n193
Ertapenem 1 g once a day (n/N) n203
Solomkin JS et al. Ann Surg 2003237235-245.
104
Summary of Results
Piperacillin/ tazobactam 3.375 g q6h
Ertapenem 1 g once a day
Generalized peritonitis
74 (39/53)
83 (50/60)
abscesses
50 (2/4)
89 (8/9)
Single abscess
82 (55/67)
90 (53/59)
88 (61/69)
87 (65/75)
Localized disease
105
Success Rate according to Infection Site
106
Ertapenem

Yellin AAC 2002
Ertapenem 1g and 1.5g/day(51) vs. ceftriaxone 2g
daily and metronidazole 500mg 8 hrly (59)
followed by switch to cipro and metronidazole
after 3 days of IVI therapy for complicated IAI
1g group 84 vs. 85 had favourable clinical and
microbial responses
1.5g group 83vs77
Well tolerated ,safe

107
Ertapenem vs. Ceftriaxone plus Metronidazole
High Microbiological and Clinical Success Rates
at Test of Cure
84
85
Clinical and Microbiological Success (46 weeks
post-therapy)
Yellin AE et al. Int J Antimicrob Agents 2002
20165-173.
108
Ertapenem vs. Ceftriaxone plus Metronidazole In
a Clinical Study of Patients with IAI, Ertapenem
Showed High Eradication Rates
Yellin AE et al. Int J Antimicrob Agents 2002
20165-173.
109
Ertapenem vs. Ceftriaxone plus Metronidazole
Conclusions

In patients with IAI
Ertapenem, one gram, one dose, once a day, was
effective compared with 2 g of ceftriaxone
administered once daily plus 500 mg metronidazole
administered in three divided daily doses.
The tolerability of ertapenem was comparable to
ceftriaxone plus metronidazole.

Yellin AE et al. Int J Antimicrob Agents 2002
20165-173.
110

2 separate OASIS trials confirmed that Ertapenem
Reduced ESBL-producing organisms during therapy
Had minimal or no risk of resistance development
during therapy
Stable against ESBLs thus minimal selection for
resistant Enterobacteriaceae
Is Pseudomonas-sparing thus minimal selective
pressure on MDR-Pseudomonas

Baseline
End of therapy and/or test of cure
End of therapy
30
25
20
percent
15
10
5
0
R
R
R
Ertapenem1,2
Piperacillin/tazo1
Ceftriaxone/Met2
1 Friedland I et al. 13th ECCMID, Glasgow, UK,
May 10-13, 2003
2 Friedland I et al. 3rd ACCP, San Margherita,
Italy, October 16-19, 2003 (Poster 57)
111
Ertapenem

Once daily administration and the absence of
activity against Pseudomonas and Acinetobacter
could mean a greater role in community acquired
infections however is the extended gram (-)
spectrum necessary?
Should it be reserved for hospital acquired ESBL
infections exclusively, allowing a reduction in
usage of other carbapenems, reserving these
agents for Acinetobacter and Pseudomonas ?
Should the necessity for appropriate initial
therapy lead us to utilize ertapenem and
de-escalation in community acquired infections.

112
Recent Publications confirm role of carbapenems
in treating ESBL infections
The prevalence of extended-spectrum b-lactamase
(ESBL) production by Klebsiella pneumonia
approaches 50 in some countries in eastern
Europe and Latin America Use of carbapenem
(primarily imipenem) was associated with a
significantly lower 14-day mortality than was use
of other antibiotics active in vitro.
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114
Are we wasting antipseudomonal therapy?

UTI quinolones
CAP quinolones
Aspiration piperacillin/tazobactam
Cellulitis quinolones, piperacillin/tazobactam
Intra-abdominal infections pip./tazobactam

115
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116
Figure. Fluoroquinolone Use and Resistance Rates
in Pseudomonas aeruginosa and Gram-Negative
Bacilli
National fluoroquinolone use data were obtained
from IMS HEALTH Retail and Provider Perspective
(Plymouth Meeting, Pa). The increasing rates of
ciprofloxacin resistance correlate with the
steadily increasing fluoroquinolone use (r
0.976, Plt.001 for P aeruginosa r 0.891, P
.007 for gram-negative bacilli r 0.958, Plt.001
for years of observation). The 1990-1993 data
points represent composite susceptibility3 and
fluoroquinolone use for those 4 years.
117
New antipseudomonal drugs available in the next 5
years
118
Pittsburgh protocol

ICUs antipseudomonal agents unrestricted
(except quinolones)
Outside of ICUs all antipseudomonal drugs need
prior approval

119
Effects of restricting use of antipseudomonal
drugs
Antibiotic Pre-AMP N3532 Post-AMP N1122 Change in S p-value
Amikacin 86.4 89.6 3.2 0.0119
Aztreonam 55.9 57.2 1.4 0.48
Cefepime 80.0 82.2 2.2 0.0985
Cipro. 56.4 68.8 12.2 lt0.0001
Gentamicin 71.4 76.4 5.0 0.0028
Imipenem 79.9 83.6 3.7 0.0120
Levofloxacin 51.0 62.7 11.7 lt0.0001
Tobramycin 81.8 84.0 2.3 0.0849
Pip/Tazo 77.6 79.6 2.0 0.1570
120
Carmeli- Key take aways

Stratification of patients at risk of being
infected with resistant organisms
3 risk groups
Scheme Patients stratified according to 3
domains

No risk for resistant organisms
Risk for resistant Enterobacteriaceae
Risk for non-fermenters
A
B
C
Patient Characteristics
AB treament
Contact with healthcare system

No contact
Contact with health care ( e.g. recent admission,
nursing home, dialysis) without invasive
procedures
Long hospitalisation/ invasive procedures

No treatment
Recent treatment

Young, few co-morbid conditions
Older/ multiple co-morbidities
Cystic fibrosis, structural lung disease,
advanced AIDS, neutropenia, other severe
immunodeficiency disorders

Score of 1 in all 3 domains low risk for
resistant organisms Score of 2 in at least 1
group risk for resistant
enterobacteriaceae Score of 3 in 1 of the groups
risk for infection with nonfermenters
121
It is not rocket science.

Clean your hands between patients
Beware taking herpes simplex, C. difficile and
MRSA home with you!
Antibiotics are not the answer for every culture
or every fever
Optimize empiric therapy based on local
epidemiology
Find alternatives to antipseudomonal drugs

122
Areas for Future Research

Appropriate specimen processing.
Role of routine Antimicrobial susceptibility
testing.
Definition of appropriate duration of AB therapy.
The impact of prolonged therapy (oral regimens)
Impact of empirical therapy on tertiary
peritonitis.
Confirmation of the pattern of infecting
organisms in tertiary peritonitis.
Solomkin JS, CID 2003

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125
Reasons for exclusion from clinical and
microbiological evaluability
126
Intra-abdominal Infection
Clinical and Microbiologic Response
Ertapenem 1 g
Piperacillin/Tazobactam
Cure Rate
Cure Rate
n/m
Stratum
n/m
Complicated appendicitis All other
diagnoses APACHE II ? 15 APACHE II gt 15 Overall
without generalized peritonitis.
127
Ertapenem

Roy Infect Dis Obstet Gynecol 2003 Acute pelvic
infections

128
Excluded Diagnoses

Traumatic bowel perforation with operation within
12 hours
Perforation of gastroduodenal ulcers operated
upon within 24 hours
Simple cholecystitis
Simple appendicitis
Infected necrotizing pancreatitis
Staged abdominal repair or open abdomen technique

129
Appropiate Treatment

Source control
Resuscitation
Physiological support of organ systems.
Monitoring
Metabolic
Respiratory
Haemodynamic
Nephrological
Intra-abdominal pressures
Antibiotics based on knowledge of the probable
flora.

130
Optimising Antibiotic Treatment in Serious
Infections

D Paterson

131
Hospital-acquired MRSA

ICU vs non-ICU
Proportion of nosocomial S. aureus isolates which
are MRSA in non-ICU areas now approaches
proportion in ICUs
Hospital size
Hospitals with less than 200 beds now have same
proportion of isolates which are MRSA as in
hospitals with more than 500 beds
Source CDC 2004

132
Vancomycin current recommendations

Dose at 1 gram every 12 hours only for wound
infection, cellulitis etc
Give 20-25 mg/kg every 12 hours for endocarditis
and pneumonia (this will often mean 1.5 gram q
12hr IV)
Only check trough levels (no need for peak
levels) aim for 10-20 µg/mL in most patients

133
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134
Linezolid

An oxazolidinone (only member of that class which
is currently available)
Dose is 600mg q12 hr IV or PO
Second-line agent in pneumonia failing to respond
to high-dose vancomycin
Marrow toxicity
Lactic acidosis, peripheral neuropathy and optic
neuritis increasingly recognized

135
Daptomycin

A lipopeptide (the only agent of this class
currently available)
IV formulation only (once per day)
Inactivated by surfactant
Rapidly bactericidal appears at least as good
as vancomycin for bacteremia and endocarditis
Can cause CPK elevations

136
Tigecycline

Glycylcyline (first of this class available)
Synthetic modification of tetracycline
Low blood levels, high tissue levels
Substantial rates of nausea/vomiting
Thus far, only approved for skin/soft tissue and
intra-abdominal infections

137
Despite the availability of new drugs.

Antistaphylococcal penicillins are still the
drugs of choice for methicillin susceptible
Staphylococcus aureus

138
Community-acquired MRSA

MMWR 199948707 Four pediatric deaths from
community-acquired MRSA
MRSA is an emerging community-acquired pathogen
among patients without established risk factors
for MRSA eg, no recent hospitalization, no
recent surgery, no residence in a long-term care
facility and no injecting drug use

139
CA-MRSA (II)

The proportion of all community-acquired
Staphylococcus aureus strains in the US which are
MRSA, ranges from 9-20, depending on the
geographic region
In the U.S., one PFGE type (USA 300 strain) is
found throughout the country
CA-MRSA has smaller resistance gene (SCCmecIV)
CA MRSA has gene for Panton-Valentine leukocidin
(PVL) toxin

140
CA-MRSA (III)

Almost 90 of cases are skin infections, often
first detected as clusters of abscesses (spider
bites) PVL is a necrotizing cytotoxin
Various epidemiologic settings
Sports participants
Jails, military recruits
Men who have sex with men

141
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143
CA-MRSA pneumonia following influenza

17 cases presented by CDC at IDSA 2004
Age range 8 months to 62 years
4/17 had traditional MRSA risk factors
Fever of at least 39o C and hemoptysis were
typical
3/17 had radiologically evident
cavitation/necrosis
13/17 admitted to ICU
5/17 died, with median of 7 days from symptom
onset to death

144
VISA/VRSA

hVISA (heteroVISA)
Typically patients who fail prolonged vancomycin
Rx
Numerous cases, but issues with detection
VISA
13 cases in USA (MIC 8-16)
30 near-VISAs (MIC4)
VRSA
4 cases thus far (MIC 32)

145
VRSA

Four distinct isolates since July 2002
No relationships between the isolates
One patient was never known to have received
vancomycin but had dual VRE and MRSA carriage
Two isolates known to have mecA and vanA together
Enterococcus faecalis is known to be the donor of
vanA in one strain

JP Pretorius - PowerPoint PPT Presentation

JP Pretorius

... and probably increasing Potential source of vancomycin resistance in staphylococci Clostridium difficile Several case ... ertapenem demonstrated a clinical ... – PowerPoint PPT presentation