Antimicrobial stewardship Antimicrobial stewardship
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Mar 07, 2025
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About This Presentation
Antimicrobial stewardship
Slide Content
Antimicrobial Stewardship (Section 2)
Empiric vs. targeted therapy.
How to choose the right antimicrobial agent (AMA).
De-escalation Definition.
De-escalation strategies.
Empiric vs. targeted therapy.
How to choose the right antimicrobial agent (AMA).
De-escalation Definition.
De-escalation strategies.
How are antimicrobials used?
Antimicrobials could be used as empirical therapy or pathogen-directed therapy or
prophylaxis.
Empirical therapy : is treatment for a possible or likely infection before laboratory
results become available, or when they are impossible to obtain. Empirical choices
may have to be made on the basis of microscopy, without the benefit of culture
and sensitivity data. This type of use is most common in low resource settings and
in community or outpatient care. However, it is strongly recommended that the
use of antibiotics is reviewed if and when laboratory data are available.
Antimicrobials could be used as empirical therapy or pathogen-directed therapy or
prophylaxis.
Empirical therapy : is treatment for a possible or likely infection before laboratory
results become available, or when they are impossible to obtain. Empirical choices
may have to be made on the basis of microscopy, without the benefit of culture
and sensitivity data. This type of use is most common in low resource settings and
in community or outpatient care. However, it is strongly recommended that the
use of antibiotics is reviewed if and when laboratory data are available.
Pathogen-directed therapy :is antibiotic treatment guided by the results of
microbiological investigations, with choices determined by specific
sensitivity/resistance data.
Prophylaxis : is use of antibiotics to prevent infection. Generally used just prior to
surgery or other invasive procedures, it must target the microorganisms most likely
to cause infections following the procedure (e.g., colo-rectal surgery, prevention of
sub acute bacterial endocarditis, use in prolonged ruptured membranes prior to
delivery). It can also be applied to prevent infections in immunocompromised
patients (e.g., AIDS, cancer patients, transplants) and contacts of known infected
cases (e.g., meningococcal meningitis, TB). Prophylaxis must be used for the
shortest possible time and given when antibiotics are likely to be most effective.
microbiological investigations, with choices determined by specific
sensitivity/resistance data.
Prophylaxis : is use of antibiotics to prevent infection. Generally used just prior to
surgery or other invasive procedures, it must target the microorganisms most likely
to cause infections following the procedure (e.g., colo-rectal surgery, prevention of
sub acute bacterial endocarditis, use in prolonged ruptured membranes prior to
delivery). It can also be applied to prevent infections in immunocompromised
patients (e.g., AIDS, cancer patients, transplants) and contacts of known infected
cases (e.g., meningococcal meningitis, TB). Prophylaxis must be used for the
shortest possible time and given when antibiotics are likely to be most effective.
Choice of An Antimicrobial
Before prescribing an AMA….
Assess patient condition
Is it an infection that can be treated? Is it bacterial?
Can it resolve on its own or with local measures only?
Then
Choose an appropriate AMA from a large number available depend on
some factors.
Before prescribing an AMA….
Assess patient condition
Is it an infection that can be treated? Is it bacterial?
Can it resolve on its own or with local measures only?
Then
Choose an appropriate AMA from a large number available depend on
some factors.
Patient Factors
Age
•Chloramphenicol͢͢͢͢͢͢͢͢͢GrayBabySyndrome
•Sulfonamides ͢͢͢Kernicterusinneonates
•Tetracycline's͢͢͢Discolorationanddeformedteethinchildren
•Aminoglycosides͢͢͢Nervetoxicityintheelderly
Age
•Chloramphenicol͢͢͢͢͢͢͢͢͢GrayBabySyndrome
•Sulfonamides ͢͢͢Kernicterusinneonates
•Tetracycline's͢͢͢Discolorationanddeformedteethinchildren
•Aminoglycosides͢͢͢Nervetoxicityintheelderly
Patient Factors
Patient Factors
Local Factors
• Presence of pus or secretions
• Presence of necrotic material or foreign body
• Hematomas
• Low pH at site of infections
• Penetration barriers at certain sites
Local Factors
• Presence of pus or secretions
• Presence of necrotic material or foreign body
• Hematomas
• Low pH at site of infections
• Penetration barriers at certain sites
Patient Factors
Drug Allergy
History of previous intake of AMAs must be obtained before
administering any treatment to determine drug allergy
• Beta lactam drugs
• Sulfonamides }Frequently cause drug allergy
• Fluoroquinolones
Drug Allergy
History of previous intake of AMAs must be obtained before
administering any treatment to determine drug allergy
• Beta lactam drugs
• Sulfonamides }Frequently cause drug allergy
• Fluoroquinolones
Patient Factors
Impaired Host Defense
• NeutropenicPatients
• AIDS
• Impaired Cell-mediated Immunity
* Intensive cidaltherapy is needed in those with impaired host defense
even then, complete eradication of organism may not occur
Impaired Host Defense
• NeutropenicPatients
• AIDS
• Impaired Cell-mediated Immunity
* Intensive cidaltherapy is needed in those with impaired host defense
even then, complete eradication of organism may not occur
Patient Factors
Pregnancy
• ALL AMAs SHOULD BE AVOIDED IN PREGNANCY DUE TO RISK TO THE FETUS
• Penicillins, many cephalosporinsand erythromycin are said to be safe
Genetic Factors
• Primaquine
• Nitrofurantoin
• Sulfonamides } RISK OF CAUSING HAEMOLYSIS IN G-6-PD DEFIENCY
• Chloramphenicol
• Fluoroquinolones
Pregnancy
• ALL AMAs SHOULD BE AVOIDED IN PREGNANCY DUE TO RISK TO THE FETUS
• Penicillins, many cephalosporinsand erythromycin are said to be safe
Genetic Factors
• Primaquine
• Nitrofurantoin
• Sulfonamides } RISK OF CAUSING HAEMOLYSIS IN G-6-PD DEFIENCY
• Chloramphenicol
• Fluoroquinolones
Organism-Related Factors
Clinical Diagnosis Directs the Choice of AMA
• Syphilis ͢͢͢BenzathinePenicillin
• Tuberculosis ͢͢͢ AntitubercularDrugs
• Leprosy ͢͢͢Dapsone, Rifampicin
• Amoebiasis ͢͢͢Metronidazole
• Herpes Simplex ͢͢͢͢͢͢Acyclovir
Clinical Diagnosis Directs the Choice of AMA
• Syphilis ͢͢͢BenzathinePenicillin
• Tuberculosis ͢͢͢ AntitubercularDrugs
• Leprosy ͢͢͢Dapsone, Rifampicin
• Amoebiasis ͢͢͢Metronidazole
• Herpes Simplex ͢͢͢͢͢͢Acyclovir
Organism-Related Factors
A Good Guess can be Made from Clinical Features
• Tonsillitis
• Otitis Media
• Vaginitis
• Urethritis
* Gram stain smear of infected material suffices to make a choice
A Choice to be Based on Bacteriological Examination
• Meningitis
• Osteomyelitis
• UTI
• Wound infection
* But sensitivity testing may not always be possible
A Good Guess can be Made from Clinical Features
• Tonsillitis
• Otitis Media
• Vaginitis
• Urethritis
* Gram stain smear of infected material suffices to make a choice
A Choice to be Based on Bacteriological Examination
• Meningitis
• Osteomyelitis
• UTI
• Wound infection
* But sensitivity testing may not always be possible
Organism-Related Factors
a) Bacteriological services not available
• Empirical therapy to be started with broad spectrum antibiotics
• Therapy is modified on the basis of clinical response
b) Bacteriological services available but treatment cannot be delayed
• Empirical therapy to be started
• AMA should be changed later in the light of bacteriological findings
c) Bacteriological services available and treatment can be delayed
Chronic UT
a) Bacteriological services not available
• Empirical therapy to be started with broad spectrum antibiotics
• Therapy is modified on the basis of clinical response
b) Bacteriological services available but treatment cannot be delayed
• Empirical therapy to be started
• AMA should be changed later in the light of bacteriological findings
c) Bacteriological services available and treatment can be delayed
Chronic UT
Minimum Inhibitory Concentration (MIC)
•The lowest concentration of an antibiotic which prevents visible growth
of a
•bacterium after 24 hours incubation in a microwellculture plate using
serial dilutions of the antibiotic
Minimum Bactericidal Concentration (MBC)
• The concentration of an antibiotic which kills 99.9% of the bacteria
determined by subculturingfrom tubes with no visible growth.
* A small difference between MIC and MBC indicates that an antibiotic
is cidal!
* MBC is not used to guide selection of therapy
•The lowest concentration of an antibiotic which prevents visible growth
of a
•bacterium after 24 hours incubation in a microwellculture plate using
serial dilutions of the antibiotic
Minimum Bactericidal Concentration (MBC)
• The concentration of an antibiotic which kills 99.9% of the bacteria
determined by subculturingfrom tubes with no visible growth.
* A small difference between MIC and MBC indicates that an antibiotic
is cidal!
* MBC is not used to guide selection of therapy
Post Antibiotic Effect (PAE)
• The lag period in growth resumption after an exposed organism is
placed in an antibiotic-free medium… time required to regain
logarithmic growth
• Lag period depends on the antibiotic and on the type of organism
• Drugs with a long PAE has been noted with fluoroquinolones,
aminoglycosides and rifampicin
• The lag period in growth resumption after an exposed organism is
placed in an antibiotic-free medium… time required to regain
logarithmic growth
• Lag period depends on the antibiotic and on the type of organism
• Drugs with a long PAE has been noted with fluoroquinolones,
aminoglycosides and rifampicin
Drug Factors
Spectrum of Activity
• Definitive Therapy → Narrow spectrum drugs concerned with the
causative organism
• Empirical Therapy→ broad spectrum drugs used to cover all likely
pathogens
Spectrum of Activity
• Definitive Therapy → Narrow spectrum drugs concerned with the
causative organism
• Empirical Therapy→ broad spectrum drugs used to cover all likely
pathogens
Drug Factors
Type of Activity
BACTERIOSTATIC OR BACTERICIDAL
• Most infections resolve faster with cidalrather than static
• Cidaldrugs usually have a prolonged post-antibiotic effect preferred in
impaired host defenceand life threatening infections
• With static drugs, bacteria may quickly start multiplying when drug level
falls below MIC→ relapse of infection
Type of Activity
BACTERIOSTATIC OR BACTERICIDAL
• Most infections resolve faster with cidalrather than static
• Cidaldrugs usually have a prolonged post-antibiotic effect preferred in
impaired host defenceand life threatening infections
• With static drugs, bacteria may quickly start multiplying when drug level
falls below MIC→ relapse of infection
Drug Factors
Relative Toxicity
• A LESS TOXIC ANTIBIOTIC IS ALWAYS PREFERRED … OBVIOUSLY!!!
• Beta lactam drugs over aminoglycosides
• Erythromycin over clindamycin
Relative Toxicity
• A LESS TOXIC ANTIBIOTIC IS ALWAYS PREFERRED … OBVIOUSLY!!!
• Beta lactam drugs over aminoglycosides
• Erythromycin over clindamycin
Drug Factors
Route of Administration
• Many AMAs can be given both orally or parenterally
• Few like aminoglycosides, Penicillin G, Vancomycinare given by
injection ONLY
• Oral antibiotics are preferred for less severe infections
• Parenteral antibiotics are preferred in more severe infections
Route of Administration
• Many AMAs can be given both orally or parenterally
• Few like aminoglycosides, Penicillin G, Vancomycinare given by
injection ONLY
• Oral antibiotics are preferred for less severe infections
• Parenteral antibiotics are preferred in more severe infections
Drug Factors
Evidence of Clinical Efficacy
• The value of various AMAs in therapy is based on comparative clinical
trials
• Optimum dosages and duration of treatment are determined based
on studies
•Reliable clinical trial data is the best guide for choice of an antibiotic!
Cost
•LESS EXPENSIVE DRUGS ARE PREFERRED …. AGAIN… OBVIOUSLY!!!
Evidence of Clinical Efficacy
• The value of various AMAs in therapy is based on comparative clinical
trials
• Optimum dosages and duration of treatment are determined based
on studies
•Reliable clinical trial data is the best guide for choice of an antibiotic!
Cost
•LESS EXPENSIVE DRUGS ARE PREFERRED …. AGAIN… OBVIOUSLY!!!
Combined Use of Antimicrobials
One is good, two should be better three should cure
• Frequently used
• Should only be administered when there is a specific purpose
• Objectives to use combinations:
1. To achieve synergism → Cotrimoxazole
2. To reduce severity or incidence of Side Effects → Streptomycin + Pen G in SABE
3. To prevent emergence of resistance → TB, Leprosy, HIV, H. pylori, Malaria
4. To broaden spectrum →treatment of mixed infections, severe infections, topical
One is good, two should be better three should cure
• Frequently used
• Should only be administered when there is a specific purpose
• Objectives to use combinations:
1. To achieve synergism → Cotrimoxazole
2. To reduce severity or incidence of Side Effects → Streptomycin + Pen G in SABE
3. To prevent emergence of resistance → TB, Leprosy, HIV, H. pylori, Malaria
4. To broaden spectrum →treatment of mixed infections, severe infections, topical
What is de-escalation?
•De-escalation is when we switch to a narrower-spectrum antibiotic to
target the causative pathogen(s) identified on culture.
Key Points: Switching to narrower spectrum antibiotics when
clinically indicated can prevent adverse reactions and reduce
antibiotic resistance.
•De-escalation is when we switch to a narrower-spectrum antibiotic to
target the causative pathogen(s) identified on culture.
Key Points: Switching to narrower spectrum antibiotics when
clinically indicated can prevent adverse reactions and reduce
antibiotic resistance.
What is my role in de-escalation?
•Every day, review all patients on broad-spectrum antibiotics in your
patient care area and identify those with positive cultures. Review
these patients using the 6-step process to determine whether a
narrower antibiotic would optimize therapy. If you feel a change in
therapy is needed, work with the prescribing provider and
recommend an alternate therapy. This process is designed for
patients with positive cultures only!
key Point: The goal of de-escalation is to determine whether a
narrower antibiotic would be more appropriate for each patient.
•Every day, review all patients on broad-spectrum antibiotics in your
patient care area and identify those with positive cultures. Review
these patients using the 6-step process to determine whether a
narrower antibiotic would optimize therapy. If you feel a change in
therapy is needed, work with the prescribing provider and
recommend an alternate therapy. This process is designed for
patients with positive cultures only!
key Point: The goal of de-escalation is to determine whether a
narrower antibiotic would be more appropriate for each patient.
How we do the de-escalation strategies?
For every patient on broad-spectrum antibiotics with a positive culture,
review the 6-steps to determine whether de-escalation is appropriate.
For every patient on broad-spectrum antibiotics with a positive culture,
review the 6-steps to determine whether de-escalation is appropriate.
Step 1 :Evaluate the source
•Where was the positive culture obtained? Positive cultures in sites
considered sterile need to be taken very seriously. For positive
cultures taken from non-sterile sites, use your clinical judgment to
determine whether the culture represents an infection or colonization
(step 2). Review the type, source, and status of the culture.
Key Point:
• Sterile sites: blood, CSF, bone, pleural fluid, synovial fluid, and
other deep surgical sites.
• Non-sterile sites: urine, skin, wounds, sputum, etc.
•Where was the positive culture obtained? Positive cultures in sites
considered sterile need to be taken very seriously. For positive
cultures taken from non-sterile sites, use your clinical judgment to
determine whether the culture represents an infection or colonization
(step 2). Review the type, source, and status of the culture.
Key Point:
• Sterile sites: blood, CSF, bone, pleural fluid, synovial fluid, and
other deep surgical sites.
• Non-sterile sites: urine, skin, wounds, sputum, etc.
Step 2: Is an infection present
•Is an infection present? The positive culture may represent any one of the
following:
• Infection: The presence of pathogenic microorganisms that invade a body
part or tissue to cause symptomatic disease.
• Colonizer: The presence of microorganisms in a non-sterile site that is not
causing infection. These are typically commensal organisms belonging to
normal flora and harmless to healthy people; sometimes they perform a vital
function (e.g., gut bacteria aid in digestion).
• Contaminant: The unintentional or accidental introduction of
microorganisms into a culture, either when the culture was obtained or in
the microbiology laboratory.
Key Point for step 2 : If the culture shows a colonizer or a contaminant is
present, suggest that the provider stop or adjust the patient’s
antimicrobials
•Is an infection present? The positive culture may represent any one of the
following:
• Infection: The presence of pathogenic microorganisms that invade a body
part or tissue to cause symptomatic disease.
• Colonizer: The presence of microorganisms in a non-sterile site that is not
causing infection. These are typically commensal organisms belonging to
normal flora and harmless to healthy people; sometimes they perform a vital
function (e.g., gut bacteria aid in digestion).
• Contaminant: The unintentional or accidental introduction of
microorganisms into a culture, either when the culture was obtained or in
the microbiology laboratory.
Key Point for step 2 : If the culture shows a colonizer or a contaminant is
present, suggest that the provider stop or adjust the patient’s
antimicrobials
Step 3: Review culture
•Isthepositiveculturecomplete?Askyourself:
•Istheculturefinalized?Areotherculturespending?
•ArethereotherorganismsontheGramstainthatdidn’tgrow?
•Doestheinfectioussyndromewarrantbroadertherapythantheculturewould
suggest?Doyouneedtocovermorethanjustthepositiveculture?Forexample,
ifthepatienthasanintra-abdominalabscessandthebloodculturegrowsEcoli,
anaerobiccoverageisstillrequiredeventhoughtheculturedidn’tgrow
anaerobes.
•Doesthepatienthaveacomorbidinfectioussyndromethatwarrantsbroader
therapy?
KeyPoint:Ifallculturesaren’tfinal,considerwaitingongivingtheprovidera
recommendationforde-escalation
•Isthepositiveculturecomplete?Askyourself:
•Istheculturefinalized?Areotherculturespending?
•ArethereotherorganismsontheGramstainthatdidn’tgrow?
•Doestheinfectioussyndromewarrantbroadertherapythantheculturewould
suggest?Doyouneedtocovermorethanjustthepositiveculture?Forexample,
ifthepatienthasanintra-abdominalabscessandthebloodculturegrowsEcoli,
anaerobiccoverageisstillrequiredeventhoughtheculturedidn’tgrow
anaerobes.
•Doesthepatienthaveacomorbidinfectioussyndromethatwarrantsbroader
therapy?
KeyPoint:Ifallculturesaren’tfinal,considerwaitingongivingtheprovidera
recommendationforde-escalation
Step 4: Review resistance
•What is the organism’s susceptibility profile?
•Always review the susceptibility profile to determine what antibiotics
will be active. If there is an antibiotic you would like to use that isn’t
listed on the culture, call your microbiology laboratory for more
information.
Key Point: Talk to the microbiological laboratory for more
information.
•What is the organism’s susceptibility profile?
•Always review the susceptibility profile to determine what antibiotics
will be active. If there is an antibiotic you would like to use that isn’t
listed on the culture, call your microbiology laboratory for more
information.
Key Point: Talk to the microbiological laboratory for more
information.
Step 5: Review antibiotic
•What antibiotic is the patient on? Can we go any narrower? After you’ve assessed
the culture and susceptibility profile, ask yourself:
• Is there a narrower antibiotic that will better meet the needs of the patient?
• What exactly should I recommend?
Key Point: When you are ready to make a de-escalation recommendation, be
specific (e.g., include patient specific dosing).
•What antibiotic is the patient on? Can we go any narrower? After you’ve assessed
the culture and susceptibility profile, ask yourself:
• Is there a narrower antibiotic that will better meet the needs of the patient?
• What exactly should I recommend?
Key Point: When you are ready to make a de-escalation recommendation, be
specific (e.g., include patient specific dosing).
Step 6: Assess the patient
•Are there any patient-specific factors we have to consider? Consider
the following patient-specific factors before making your
recommendation:
• Convenience (e.g., dosing interval, IV and PO, side effects, etc.)
• Allergies
• Drug-drug interaction
• IV or oral conversion
Key Point: Individualize your recommendation to the patient.
•Are there any patient-specific factors we have to consider? Consider
the following patient-specific factors before making your
recommendation:
• Convenience (e.g., dosing interval, IV and PO, side effects, etc.)
• Allergies
• Drug-drug interaction
• IV or oral conversion
Key Point: Individualize your recommendation to the patient.
Questions:
1-Empiric antimicrobial therapy:
a. Is given routinely before appropriate microbiological specimens have been
taken
b. Consists usually of a single antimicrobial drug that targets the most likely
pathogen
c.Usually includes several anti-infective drugs that cover the most likely
causative pathogens
d. Is continued even after the definitive cause of the infection is identified.
2-Targeted antimicrobial therapy:
a. Aims to match the antimicrobial given to the specific pathogen-causing
infection
b. Uses broad-spectrum antibiotics to cover all potential pathogens
c. Does not require the collection of appropriate microbiological specimens
d. Usually requires several different antimicrobials to be prescribed
1-Empiric antimicrobial therapy:
a. Is given routinely before appropriate microbiological specimens have been
taken
b. Consists usually of a single antimicrobial drug that targets the most likely
pathogen
c.Usually includes several anti-infective drugs that cover the most likely
causative pathogens
d. Is continued even after the definitive cause of the infection is identified.
2-Targeted antimicrobial therapy:
a. Aims to match the antimicrobial given to the specific pathogen-causing
infection
b. Uses broad-spectrum antibiotics to cover all potential pathogens
c. Does not require the collection of appropriate microbiological specimens
d. Usually requires several different antimicrobials to be prescribed
3-De-escalation of antimicrobial therapy:
a. Means changing the patient’s prescription from a narrow to a broad-spectrum
antimicrobial
b. Is potentially harmful, even if the pathogen is sensitive to a narrow-spectrum
antimicrobial
c. Ensures effective therapy but reduces harmful effects of broad-spectrum
antimicrobials
d. Means that therapy should be stopped or discontinued.
•Mark (True/ False)
1-Minimum inhibitory concentration(MIC) The concentration of an
antibiotic which kills 99.9% of the bacteria determined by sub
culturing from tubes with no visible growth (T/F)
2-If all cultures aren’t final, Not consider waiting on giving the provider
a recommendation for de-escalation (T/F)
a. Means changing the patient’s prescription from a narrow to a broad-spectrum
antimicrobial
b. Is potentially harmful, even if the pathogen is sensitive to a narrow-spectrum
antimicrobial
c. Ensures effective therapy but reduces harmful effects of broad-spectrum
antimicrobials
d. Means that therapy should be stopped or discontinued.
•Mark (True/ False)
1-Minimum inhibitory concentration(MIC) The concentration of an
antibiotic which kills 99.9% of the bacteria determined by sub
culturing from tubes with no visible growth (T/F)
2-If all cultures aren’t final, Not consider waiting on giving the provider
a recommendation for de-escalation (T/F)
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