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Getting Evidence into
Infection Control Practice
Mary Ann D. Lansang, MD, FPCP, FPSMID
PHICS Convention
May 29, 2015
Outline
• What is Evidence-based Practice (EBP)?
• Introduction to key concepts in EBP
o 6 A’s
o PICOT
o RAMBO
• Practice scenario on infection control & prevention
• The X factor
• Evaluation and quality improvement
What is Evidence-Based Practice?
• The application of the best available research
results (EVIDENCE) when making decisions about
health care (from: Agency for Effective Healthcare Research &
Quality, USA)
• Evidence is used alongside clinical expertise and
patient preferences
• Local/population context is also important
• Origins from “Evidence-Based Medicine” (Sackett et
al. British Medical Journal, 1996)
Dr David Sackett: father of EBM
(1934 – 2015)
What is Evidence-based Practice?
http://www.cebm.net/
What is Evidence Based Practice?
http://www.cebm.net/
Focus of EBP
• Focus on outcomes and costs:
o Reduce unnecessary variations in practice
o Close the gap between evidence and practice
o Enable systematic management of information
overload
• Interventions based on evidence have
better outcomes
EBP improves patient outcomes
EBM/EBP Key Concepts
• ‘PICOT’
• Patient/s
• Intervention/s
• Comparison
• Outcome/s
• Time
• 6 A’s
1. ASK
2. ACCESS
3. APPRAISE
4. AGGREGATE
5. APPLY
6. AUDIT
• RAMBO
• Recruitment
• Allocation
• Maintenance
• Measurements
• Blind, or
• Objective
measure-
ments &
processes
©
The 6 A’s -steps of Evidence-Based Practice
1. ASK a focused question
2. ACCESS - search for epidemiological evidence to help
answer question
3. APPRAISE the evidence for its validity, effect size,
precision)
4. AGGREGATE the evidence using the triangle,circle,box,x
FRAMEWORK
5. APPLY your decision integrating the aggregated evidence
into the trade-off of (i) benefits versus harms;(ii) patient
values and preferences, (iii) cost –effectiveness and cost-
equity,to make an evidence-based decision
6. AUDIT your practice (i.e. check your actual practice
against evidence-based practice on a regular basis)].
Key: Formulate an answerable question from a
patient’s (or hospital’s) problem (1)
Problem:
• 39 y.o. male is admitted to the hospital for intermittent high-
grade fever and chills since 3 weeks prior to admission
• Hemiplegic, with complete spinal cord injury at C6 from a
diving injury in May 2011
• Has had multiple pressure sores in sacral area, and healed
with unrecalled antibiotics
• 2 days prior to admission: developed a tender, swollen,
fluctuant mass at right gluteal area
• Wound C/S showed: MRSA sensitive to clindamycin,
levofloxacin, linezolid and vancomycin; resistant to oxacillin
Key: Formulate an answerable question from a
patient’s (or hospital’s) problem (2)
Problem (cont’d):
•The Hospital Infection Control Unit has instituted contact
precautions and advised daily bathing/wipes with 2%
chlorhexidine
•The patient’s wife asks you: Are these really necessary? Do I
have to wear gowns and gloves all the time? And do we really
have to wipe him with chlorhexidine, which is expensive? Isn’t
soap and water not enough?
•You, as the healthcare worker, secretly agree yourself that all
these procedures are too tedious and labor-intensive, and also
costs the hospital too much.
•YOU LOOK FOR THE EVIDENCE ON THE EFFECTIVENESS OF THESE
INTERVENTIONS – e.g., contact precautions
EBP Step 1: ASK - turn your question
into 5 parts (PICOT)
1. Participants (patient(s) you want to treat)
2. Intervention( or ‘Exposure’ if no intervention )
3. Comparison (there is always an alternative! - another
therapy, nothing …
4. Outcome (MCID [Minimal Clinically Important Difference] in the Humanly
Important Outcome [Distress, Disability, Dysfunction, Death]
5. Time frame (over which you expect a result)
Participants
Intervention Group Comparison Group
Outcomes
Time
P
I C
O
T
PICOT:
the 5 parts of every epidemiological study
OUR PICOT QUESTION
1. Participants (patient(s) you want to treat)
2. Intervention( or ‘Exposure’ if no intervention )
3. Comparison (there is always an alternative! - another
therapy, nothing …)
4. Outcome ( MCID [Minimal Clinically Important Difference] in the
Humanly Important Outcome [Distress,Disability,Dysfunction,Death] )
5. Time frame (over which you expect a result)
Among patients with MRSA infections,
are contact precautions more effective than
standard precautions in
preventing health-care associated infections
over the period of a patient’s hospital stay?
EBP Step 2: ACCESS - search for the
best evidence to answer your question/s
Use the PICOT components to choose search terms
1. Patient(s): MRSA infections
2. Intervention: Contact precautions
3. Comparison: Standard precautions
4. Outcome Prevention of HAI/nosocomial infections
5. Time Period of hospital stay
Among patients with MRSA infections,
are contact precautions more effective than hand hygiene
in preventing healthcare associated infections
over the period of a patient’s hospital stay?
Levels of Evidence
Level 1: Systematic
review of
randomized trials
Level 2: Randomized trial
or observational study w/
dramatic effect
Level 3: Nonrandomized controlled
cohort/follow-up study
Level 4: Case series, case-control studies
Level 5: Mechanism-based reasoning; expert opinion
Evidence Hierarchy for
Environmental Infection Control
- from: McDonald & Arduino, CID Jan 2013
Good Resource for systematic reviews:
Special Collections: Cochrane Library
P
I C
O
T
• P
• I
• C
• O
• T
• Recruitment
• Allocation
• Maintenance
• Measurements
• Blind or
• Objective
measurements &
processes
EBP Step 3: Appraise the evidence
using RAMBO on the PICOT frame
Participants
Intervention Group &
Comparison Group
Outcomes
Time
QUESTION: VALIDITY: RAMBO
Measurement of outcomes?
P
IG CG
O
T
DESIGN:
Selection?
Allocation?
Maintenance of allocation?
+ -
+
-
A B
C D
Representative?
Allocation?
- Randomized?
- Comparable
groups?
Maintenance?
- Treated equally?
- Compliant?
Measurements:
- Blind?
- Objective?
Participants
Intervention Group &
Comparison Group
Outcomes
Time
QUESTION: VALIDITY:
Measurement of outcomes?
P
IG CG
O
T
DESIGN:
Selection?
Allocation?
Maintenance of allocation?
+ -
+
-
A B
C D
1. Fair start?
1. Few drop-out’s?
1. Fair finish?
Participants
Intervention Group (IG) &
Comparison Group (CG)
Outcome
I
G
C
G
+ -
+
- DC
BA
Allocation?
Selection?
Maintenance of allocation?
QUESTION:
Measurement of outcomes?
DESIGN: VALIDITY
1. Fair start?
2. Few drop outs?
3. Fair finish?
Participants
Intervention Group (IG) &
Comparison Group (CG)
Outcome
I
G
C
G
+ -
+
- DC
BA
Allocation?
Selection?
Maintenance of allocation?
QUESTION:
Measurement of outcomes?
DESIGN: VALIDITY
1. Fair start?
2. Few drop outs?
3. Fair finish?
ts
n Group (IG) &
Group (CG)
I
G
C
G
+ -
+
- DC
BA
Allocation?
Selection?
Maintenance of allocation?
N:
Measurement of outcomes?
DESIGN: VALIDITY
1. Fair start?
2. Few drop outs?
3. Fair finish?
What about readily accessible practice
guidelines?
• From local medical/specialist societies locally and
abroad. Examples:
• PHICS
• Philippine Society for Microbiology & Infectious Diseases (PSMID)
• Asia Pacific Soceity of Infection Control (APSIC)
• Society for Healthcare Epidemiology in America (SHEA)
• Databases and general resources. Examples:
• Agency for Healthcare Research and Quality (USA): National
Guideline Clearinghouse (www.guideline.gov)
• National Institute for Health and Care Excellence (UK): Guidances
(www.nice.org.uk/guidance)
• U.S. Centers for Disease Control
• World Health Organization
Caution:
Not all guidelines are evidence-based.
Six domains:
1. Scope and purpose
2. Stakeholder involvement
3. Rigor of development
4. Clarity of presentation
5. Applicability
6. Editorial independence
Example: SHEA guidelines – are they evidence based?
SHEA guideline update 2014:
Strategies to prevent transmission and infection
in acute care hospitals
Quick access and appraisal results (1)
• Jain R et al. NEJM 2011; 364:
1419+: Veterans Affairs
initiative to prevent MRSA
infections
• Before – after observational
study (Oct 2007-June 2010)
o I: “MRSA bundle”: universal nasal
surveillance for MRSA, contact
precautions for pts colonized/infected
with MRSA, hand hygiene, institution-wide
effort (1.9 M admissions; 8.3 M pt-days)
o C: period before Oct 2007
• Significant decrease of 62%
from pre-intervention
infection rates (1.62 MRSA
infections per 1,000 pt days)
to the MRSA intervention
period (0.62 infections per
1,000 pt days)
• Huskins WC et al. NEJM
2011; 364: 1407+: The STAR-
ICU Trial
• A cluster-randomized
controlled trial
o I: surveillance for MRSA and VRE
colonization + contact precautions
(5,434 admissions in 10 ICUs)
o C: existing hospital practice, which
could include contact precautions
for MRSA-infected pts (3,705
admission in 8 ICUs)
• 6 months study period
• No significant difference in
mean ICU level of incidence
of col’n or infection with
MRSA/VRE per 1000 pt-days
at risk (40.3 vs 35.6 events)
Quick access and appraisal results (2)
• Jain R et al. NEJM 2011; 364:
1419+: Veterans Affairs
initiative to prevent MRSA
infections
• All acute care units (except
psychiatry
• Inherent limitations of an
uncontrolled before-and-
after study
o VA system had introduced new
VAP and CLBSI guidelines the
previous year
o Issued a new guidance
document on MRSA
decolonization 6 months after
start of intervention
o More awareness and
education during the
intervention period:
“institutional cultural change”
as part of the MRSA bundle
• Huskins WC et al. NEJM
2011; 364: 1407+: The STAR-
ICU Trial
• Limited to ICUs
• Median compliance to
contact precautions:
o Gloves: 82%
o Gowns: 77%
o Hand hygiene: 69%
• Median compliance to
standard precautions:
o Gloves: 72%
o Hand hygiene: 62%
Quick access and appraisal results (1)
• Jain R et al. NEJM 2011; 364:
1419+: Veterans Affairs
initiative to prevent MRSA
infections
• Before – after observational
study (Oct 2007-June 2010)
o I: “MRSA bundle”: universal nasal
surveillance for MRSA, contact
precautions for pts colonized/infected
with MRSA, hand hygiene, institution-wide
effort (1.9 M admissions; 8.3 M pt-days)
o C: period before Oct 2007
• Significant decrease of 62%
from pre-intervention
infection rates (1.62 MRSA
infections per 1,000 pt days)
to the MRSA intervention
period (0.62 infections per
1,000 pt days)
• Huskins WC et al. NEJM
2011; 364: 1407+: The STAR-
ICU Trial
• A cluster-randomized
controlled trial
o I: surveillance for MRSA and VRE
colonization + contact precautions
(5,434 admissions in 10 ICUs)
o C: universal gloving until
surveillance cultures negative (3,705
admission in 8 ICUs)
• 6 months study period
• No significant difference in
mean ICU level of incidence
of col’n or infection with
MRSA/VRE per 1000 pt-days
at risk (40.3 vs 35.6 events)
EBP Step 4: AGGREGATE the relevant information &
make an evidence-based decision:’ the X-factor
©
Epidemiologic
evidence
Clinical /
population
health
considerations
Policy issues
Patient / community
preferences
X-factor: making evidence-based decisions
expertise: ‘putting it all together’ the art of
practice
Step 5
APPLY your decision
USE THE ‘GRADE’ Framework
Integrating
• the aggregated evidence
• the trade-off of benefits versus harms
•patient values and preferences
•cost –effectiveness and cost- equity,
to make an evidence-based decision
http://www.gradeworkinggroup.org/publications/index.htm
Step 6: AUDIT –
evaluate & improve performance
1. Determine ‘best’ practice (EBP Steps 1-4)
2. Assess current practice: survey
3. Compare with best practice - is there a gap?
4. Consider reasons for gap, identify processes to
reduce gap & implement
5. Re-survey: is there any improvement?
= quality improvement / audit
Recap
• Evidence-based Practice (EBP)
• Introduction to key concepts in EBP
o 6 A’s
o PICOT
o RAMBO
• Application to an infection control problem: levels
of evidence
• The X factor
• Evaluation and quality improvement
Huge acknowledgments to:
For some EBP slides:
• Professor Peter Tugwell, Center for Global Health,
University of Ontario, Canada
• Carl Heneghan, Center for Evidence Based
Medicine, University of Oxford, UK (www.cebm.net)

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Evidence-based Practice in Infection Control and Prevention

  • 1. Getting Evidence into Infection Control Practice Mary Ann D. Lansang, MD, FPCP, FPSMID PHICS Convention May 29, 2015
  • 2. Outline • What is Evidence-based Practice (EBP)? • Introduction to key concepts in EBP o 6 A’s o PICOT o RAMBO • Practice scenario on infection control & prevention • The X factor • Evaluation and quality improvement
  • 3. What is Evidence-Based Practice? • The application of the best available research results (EVIDENCE) when making decisions about health care (from: Agency for Effective Healthcare Research & Quality, USA) • Evidence is used alongside clinical expertise and patient preferences • Local/population context is also important • Origins from “Evidence-Based Medicine” (Sackett et al. British Medical Journal, 1996)
  • 4. Dr David Sackett: father of EBM (1934 – 2015)
  • 5. What is Evidence-based Practice? http://www.cebm.net/
  • 6. What is Evidence Based Practice? http://www.cebm.net/
  • 7. Focus of EBP • Focus on outcomes and costs: o Reduce unnecessary variations in practice o Close the gap between evidence and practice o Enable systematic management of information overload • Interventions based on evidence have better outcomes
  • 9. EBM/EBP Key Concepts • ‘PICOT’ • Patient/s • Intervention/s • Comparison • Outcome/s • Time • 6 A’s 1. ASK 2. ACCESS 3. APPRAISE 4. AGGREGATE 5. APPLY 6. AUDIT • RAMBO • Recruitment • Allocation • Maintenance • Measurements • Blind, or • Objective measure- ments & processes ©
  • 10. The 6 A’s -steps of Evidence-Based Practice 1. ASK a focused question 2. ACCESS - search for epidemiological evidence to help answer question 3. APPRAISE the evidence for its validity, effect size, precision) 4. AGGREGATE the evidence using the triangle,circle,box,x FRAMEWORK 5. APPLY your decision integrating the aggregated evidence into the trade-off of (i) benefits versus harms;(ii) patient values and preferences, (iii) cost –effectiveness and cost- equity,to make an evidence-based decision 6. AUDIT your practice (i.e. check your actual practice against evidence-based practice on a regular basis)].
  • 11. Key: Formulate an answerable question from a patient’s (or hospital’s) problem (1) Problem: • 39 y.o. male is admitted to the hospital for intermittent high- grade fever and chills since 3 weeks prior to admission • Hemiplegic, with complete spinal cord injury at C6 from a diving injury in May 2011 • Has had multiple pressure sores in sacral area, and healed with unrecalled antibiotics • 2 days prior to admission: developed a tender, swollen, fluctuant mass at right gluteal area • Wound C/S showed: MRSA sensitive to clindamycin, levofloxacin, linezolid and vancomycin; resistant to oxacillin
  • 12. Key: Formulate an answerable question from a patient’s (or hospital’s) problem (2) Problem (cont’d): •The Hospital Infection Control Unit has instituted contact precautions and advised daily bathing/wipes with 2% chlorhexidine •The patient’s wife asks you: Are these really necessary? Do I have to wear gowns and gloves all the time? And do we really have to wipe him with chlorhexidine, which is expensive? Isn’t soap and water not enough? •You, as the healthcare worker, secretly agree yourself that all these procedures are too tedious and labor-intensive, and also costs the hospital too much. •YOU LOOK FOR THE EVIDENCE ON THE EFFECTIVENESS OF THESE INTERVENTIONS – e.g., contact precautions
  • 13. EBP Step 1: ASK - turn your question into 5 parts (PICOT) 1. Participants (patient(s) you want to treat) 2. Intervention( or ‘Exposure’ if no intervention ) 3. Comparison (there is always an alternative! - another therapy, nothing … 4. Outcome (MCID [Minimal Clinically Important Difference] in the Humanly Important Outcome [Distress, Disability, Dysfunction, Death] 5. Time frame (over which you expect a result)
  • 14. Participants Intervention Group Comparison Group Outcomes Time P I C O T PICOT: the 5 parts of every epidemiological study
  • 15. OUR PICOT QUESTION 1. Participants (patient(s) you want to treat) 2. Intervention( or ‘Exposure’ if no intervention ) 3. Comparison (there is always an alternative! - another therapy, nothing …) 4. Outcome ( MCID [Minimal Clinically Important Difference] in the Humanly Important Outcome [Distress,Disability,Dysfunction,Death] ) 5. Time frame (over which you expect a result) Among patients with MRSA infections, are contact precautions more effective than standard precautions in preventing health-care associated infections over the period of a patient’s hospital stay?
  • 16. EBP Step 2: ACCESS - search for the best evidence to answer your question/s Use the PICOT components to choose search terms 1. Patient(s): MRSA infections 2. Intervention: Contact precautions 3. Comparison: Standard precautions 4. Outcome Prevention of HAI/nosocomial infections 5. Time Period of hospital stay Among patients with MRSA infections, are contact precautions more effective than hand hygiene in preventing healthcare associated infections over the period of a patient’s hospital stay?
  • 17. Levels of Evidence Level 1: Systematic review of randomized trials Level 2: Randomized trial or observational study w/ dramatic effect Level 3: Nonrandomized controlled cohort/follow-up study Level 4: Case series, case-control studies Level 5: Mechanism-based reasoning; expert opinion
  • 18. Evidence Hierarchy for Environmental Infection Control - from: McDonald & Arduino, CID Jan 2013
  • 19. Good Resource for systematic reviews: Special Collections: Cochrane Library
  • 20. P I C O T • P • I • C • O • T • Recruitment • Allocation • Maintenance • Measurements • Blind or • Objective measurements & processes EBP Step 3: Appraise the evidence using RAMBO on the PICOT frame
  • 21. Participants Intervention Group & Comparison Group Outcomes Time QUESTION: VALIDITY: RAMBO Measurement of outcomes? P IG CG O T DESIGN: Selection? Allocation? Maintenance of allocation? + - + - A B C D Representative? Allocation? - Randomized? - Comparable groups? Maintenance? - Treated equally? - Compliant? Measurements: - Blind? - Objective?
  • 22. Participants Intervention Group & Comparison Group Outcomes Time QUESTION: VALIDITY: Measurement of outcomes? P IG CG O T DESIGN: Selection? Allocation? Maintenance of allocation? + - + - A B C D 1. Fair start? 1. Few drop-out’s? 1. Fair finish? Participants Intervention Group (IG) & Comparison Group (CG) Outcome I G C G + - + - DC BA Allocation? Selection? Maintenance of allocation? QUESTION: Measurement of outcomes? DESIGN: VALIDITY 1. Fair start? 2. Few drop outs? 3. Fair finish? Participants Intervention Group (IG) & Comparison Group (CG) Outcome I G C G + - + - DC BA Allocation? Selection? Maintenance of allocation? QUESTION: Measurement of outcomes? DESIGN: VALIDITY 1. Fair start? 2. Few drop outs? 3. Fair finish? ts n Group (IG) & Group (CG) I G C G + - + - DC BA Allocation? Selection? Maintenance of allocation? N: Measurement of outcomes? DESIGN: VALIDITY 1. Fair start? 2. Few drop outs? 3. Fair finish?
  • 23. What about readily accessible practice guidelines? • From local medical/specialist societies locally and abroad. Examples: • PHICS • Philippine Society for Microbiology & Infectious Diseases (PSMID) • Asia Pacific Soceity of Infection Control (APSIC) • Society for Healthcare Epidemiology in America (SHEA) • Databases and general resources. Examples: • Agency for Healthcare Research and Quality (USA): National Guideline Clearinghouse (www.guideline.gov) • National Institute for Health and Care Excellence (UK): Guidances (www.nice.org.uk/guidance) • U.S. Centers for Disease Control • World Health Organization
  • 24. Caution: Not all guidelines are evidence-based. Six domains: 1. Scope and purpose 2. Stakeholder involvement 3. Rigor of development 4. Clarity of presentation 5. Applicability 6. Editorial independence
  • 25. Example: SHEA guidelines – are they evidence based?
  • 26. SHEA guideline update 2014: Strategies to prevent transmission and infection in acute care hospitals
  • 27. Quick access and appraisal results (1) • Jain R et al. NEJM 2011; 364: 1419+: Veterans Affairs initiative to prevent MRSA infections • Before – after observational study (Oct 2007-June 2010) o I: “MRSA bundle”: universal nasal surveillance for MRSA, contact precautions for pts colonized/infected with MRSA, hand hygiene, institution-wide effort (1.9 M admissions; 8.3 M pt-days) o C: period before Oct 2007 • Significant decrease of 62% from pre-intervention infection rates (1.62 MRSA infections per 1,000 pt days) to the MRSA intervention period (0.62 infections per 1,000 pt days) • Huskins WC et al. NEJM 2011; 364: 1407+: The STAR- ICU Trial • A cluster-randomized controlled trial o I: surveillance for MRSA and VRE colonization + contact precautions (5,434 admissions in 10 ICUs) o C: existing hospital practice, which could include contact precautions for MRSA-infected pts (3,705 admission in 8 ICUs) • 6 months study period • No significant difference in mean ICU level of incidence of col’n or infection with MRSA/VRE per 1000 pt-days at risk (40.3 vs 35.6 events)
  • 28. Quick access and appraisal results (2) • Jain R et al. NEJM 2011; 364: 1419+: Veterans Affairs initiative to prevent MRSA infections • All acute care units (except psychiatry • Inherent limitations of an uncontrolled before-and- after study o VA system had introduced new VAP and CLBSI guidelines the previous year o Issued a new guidance document on MRSA decolonization 6 months after start of intervention o More awareness and education during the intervention period: “institutional cultural change” as part of the MRSA bundle • Huskins WC et al. NEJM 2011; 364: 1407+: The STAR- ICU Trial • Limited to ICUs • Median compliance to contact precautions: o Gloves: 82% o Gowns: 77% o Hand hygiene: 69% • Median compliance to standard precautions: o Gloves: 72% o Hand hygiene: 62%
  • 29. Quick access and appraisal results (1) • Jain R et al. NEJM 2011; 364: 1419+: Veterans Affairs initiative to prevent MRSA infections • Before – after observational study (Oct 2007-June 2010) o I: “MRSA bundle”: universal nasal surveillance for MRSA, contact precautions for pts colonized/infected with MRSA, hand hygiene, institution-wide effort (1.9 M admissions; 8.3 M pt-days) o C: period before Oct 2007 • Significant decrease of 62% from pre-intervention infection rates (1.62 MRSA infections per 1,000 pt days) to the MRSA intervention period (0.62 infections per 1,000 pt days) • Huskins WC et al. NEJM 2011; 364: 1407+: The STAR- ICU Trial • A cluster-randomized controlled trial o I: surveillance for MRSA and VRE colonization + contact precautions (5,434 admissions in 10 ICUs) o C: universal gloving until surveillance cultures negative (3,705 admission in 8 ICUs) • 6 months study period • No significant difference in mean ICU level of incidence of col’n or infection with MRSA/VRE per 1000 pt-days at risk (40.3 vs 35.6 events)
  • 30. EBP Step 4: AGGREGATE the relevant information & make an evidence-based decision:’ the X-factor ©
  • 31. Epidemiologic evidence Clinical / population health considerations Policy issues Patient / community preferences X-factor: making evidence-based decisions expertise: ‘putting it all together’ the art of practice
  • 32. Step 5 APPLY your decision USE THE ‘GRADE’ Framework Integrating • the aggregated evidence • the trade-off of benefits versus harms •patient values and preferences •cost –effectiveness and cost- equity, to make an evidence-based decision http://www.gradeworkinggroup.org/publications/index.htm
  • 33. Step 6: AUDIT – evaluate & improve performance 1. Determine ‘best’ practice (EBP Steps 1-4) 2. Assess current practice: survey 3. Compare with best practice - is there a gap? 4. Consider reasons for gap, identify processes to reduce gap & implement 5. Re-survey: is there any improvement? = quality improvement / audit
  • 34. Recap • Evidence-based Practice (EBP) • Introduction to key concepts in EBP o 6 A’s o PICOT o RAMBO • Application to an infection control problem: levels of evidence • The X factor • Evaluation and quality improvement
  • 35. Huge acknowledgments to: For some EBP slides: • Professor Peter Tugwell, Center for Global Health, University of Ontario, Canada • Carl Heneghan, Center for Evidence Based Medicine, University of Oxford, UK (www.cebm.net)