1. Plan
GRADE background
certainty in evidence (quality, confidence evidence)
evidence profiles
strength of recommendation
exercises in applying GRADE

2. experience participating guideline panels?
clin epi methodology course?
is grading recommendations a good idea? If so, why?
experience with grading
systems used?

3. Grading good idea, but which grading system to use?
many available
Australian National and MRC
Oxford Center for Evidence-based Medicine
Scottish Intercollegiate Guidelines (SIGN)
US Preventative Services Task Force
American professional organizations
AHA/ACC, ACCP, AAP, Endocrine society, etc....
cause of confusion, dismay

5. Common international grading system?
GRADE (Grades of recommendation, assessment, development and evaluation)
international group
Australian NMRC, SIGN, USPSTF, WHO, NICE, Oxford CEBM, CDC, CC
~ 35 meetings over last 14 years
(~10 – 70 attendants)

6. GRADE GUIDANCE 2004 BMJ, first description 2008 BMJ six part series
for guideline users
, 21 part series, 15 published
for systematic review authors, HTA practitioners, guideline developers

7. Grading system – for what?
interventions
management strategy 1 versus 2
what grade is not about
individual studies (body of evidence)

8. What GRADE is not primarily about
diagnostic accuracy questions
in patients with a sore leg, what is the accuracy of a blood test (D-Dimer) in sorting out whether a deep venous thrombosis is the cause of the pain
prognosis
what it is about: diagnostic impact
are patients better off (improved outcomes) when doctors use the d-dimer test

9. 80+ Organizations
2005
2006
2007
2008
2009
2010
2011 9 9

10. GRADE uptake

11. What are we grading? two components
certainty in estimate of effect adequate to support decision (quality of body of evidence)
high, moderate, low, very low

12. Likelihood of and confidence in an outcome
We can look at this as depicted in this cartoon. The likelihood of and the confidence in an outcome. In the cartoon one meteorologist is saying to another, I figure there is a 40% chance of showers and a 10% chance we know what we are talking about. Once again, this expresses our confidence in an estimate of effect and the likelihood that it actually occurs. For instance, the confidence intervals around the 404 chance of showers estimate may be very tight. They may in fact be based on modeling that has come up with confidence intervals that range from 35 – 45 %. However, the development of the model or the application of the model from one setting to another may leave us with very little confidence that the estimate is actually correct for the particular setting. Just imagine that model being developed in Australia and applied to North America. Once again, this is similar to how we look at the confidence in evidence in the GRADE approach. 12

13. Semantic Issue: Label for trustworthiness
Quality
Initial choice, defined as confidence
natural to clinicians, but confusion with risk of bias
Confidence
what we actually mean, but confusion with confidence intervals, and experts always confident
Certainty
avoids confusion of others, experts might acknowledge uncertainty - Current preferred term

14. What are we grading? two components
certainty in evidence adequate to support decision (quality of body of evidence)
high, moderate, low, very low
strength of recommendation
strong and weak
weak alternatives
conditional, contingent, discretionary

15. Generate an estimate of effect for each outcome
Studies S1 S2 S3 S4 S5
Health Care Question
(PICO)
Systematic reviews
Outcomes
OC1
OC2
OC3
OC4
Important
outcomes
OC1
OC2
Critical
outcomes
OC3
OC4
Generate an estimate of effect for each outcome
Rate the quality of evidence for each outcome, across studies
RCTs start high, observational studies start low
(-)
Study limitations
Imprecision
Inconsistency of results
Indirectness of evidence
Publication bias likely
Final rating of quality for each outcome: high, moderate, low, or very low
(+)
Large magnitude of effect
Dose response
Plausible confounders would ↓ effect when an effect is present or ↑ effect if effect is absent
Rate overall quality of evidence
(lowest quality among critical outcomes)
Decide on the direction (for/against) and grade strength (strong/weak*) of the recommendation considering:
Quality of the evidence
Balance of desirable/undesirable outcomes
Values and preferences
Decide if any revision of direction or strength is necessary considering: Resource use
*also labeled “conditional”
or “discretionary” 15

16. Structured question patients: intervention, testosterone
Males over 50 presenting with fatigue, malaise and erecticle dysfunction with laboratory evidence of decreased testosterone
intervention, testosterone
comparator no testosterone
outcomes?

17. Rating certainty
Where to start RCTs and observational studies (High, moderate, low, very low)?
Recall antioxidant vitamins
Observational studies less cancer, CV outcomes
RCTs no difference
Result observed repeatedly
What went wrong?

18. Determinants of confidence
RCTs start high
observational studies start low
what can lower confidence?
risk of bias
inconsistency
indirectness
imprecision
publication bias

19. Risk of Bias - RCTs what to consider? well established more recent
concealment
intention to treat principle observed
blinding
completeness of follow-up
more recent
selective outcome reporting bias
Stopping early for benefit

20. RoB – Observational Studies
what to consider?
accurate assessment of exposure
adjusted analysis for all important prognostic factors, accurately measures
accurate assessment of outcome
completeness of follow-up

21. Risk of Bias differs – what to do?
6 studies, 100 patients each
3 studies low risk of bias, 3 high
rate down for risk of bias?

22. Consistency

23. Consistency

24. Consistency of results
How did you decide?
Similarity of point estimates
less similar, less happy
Overlap of confidence intervals
less overlap, less happy

25. -40
-24 -8 8 24 40 56
RRR (95% CI)

26. Homogenous test for heterogeneity what is the p-value?
what is the null hypothesis
for the test for heterogeneity?
Ho: RR1 = RR2 = RR3 = RR4
p=0.99 for heterogeneity

27. Heterogeneous test for heterogeneity what is the p-value?
p-value for heterogeneity < 0.001
p-value for heterogeneity < 0.001

28. Only a little concerned
I2 Interpretation
100%
Why are we pooling?
75%
Very concerned
25%
Only a little concerned
50%
Getting concerned 0%
No worries

29. Homogenous
What is the I2 ?
p=0.99 for heterogeneity
I2=0%

30. Heterogeneous What is the I2 ? I2=89%
p-value for heterogeneity < 0.001
I2=89%

31. Relative Risk with 95% CI for Vitamin D Non-vertebral Fractures

32. Relative Risk with 95% CI for Vitamin D
(Non-Vertebral Fractures, Dose >400)

33. Relative Risk with 95% CI for Vitamin D
(Non-Vertebral Fractures, Dose = 400)

34. Should we believe sub-group analysis?
within-study comparison? No
unlikely chance Yes, p = 0.006
consistent across studies Yes
one of small number a priori hypothesis with direction Yes
biologically compelling Yes
shall we believe sub-group analysis?

35. Credibility of sub-group analysis
no way
sure thing
100

36. Confidence judgments: Directness
populations
older, sicker or more co-morbidity
interventions
warfarin in trials vs clinical practice
outcomes
important versus surrogate outcomes
glucose control versus CV events

37. Hierarchy of outcomes according to their patient-importance effect of phosphate lowering drugs in patients with renal failure and hyperphophatemia
Importance
of endpoints
Surrogates of declining importance
Mortality 9
Critical
for decision making
Important,
but not critical for
decision making
Of low patient-
importance
Coronary
calcification
Ca2+/P-
Product
Myocardial infarction 8
Bone
density
Ca2+/P-
Product
Fractures
Pain due to soft tissue
Calcification / function 6
Soft tissue calcification
Ca2+/P-
Product 5 4
Lower by one level for indirectness 3
Flatulence 2
Lower by two levels for indirectness 1

38. Directness Alendronate Risedronate Placebo interested in A versus B
available data A vs C, B vs C
Alendronate
Risedronate
Placebo

39. Imprecision small sample size wide confidence intervals
small number of events
wide confidence intervals
uncertainty about magnitude of effect
how do you decide what is too wide?
primary criterion:
would decisions differ at ends of CI

40. Precision atrial fib at risk of stroke
warfarin increases serious gi bleeding
3% per year
1,000 patients 1 less stroke
30 more bleeds for each stroke prevented
1,000 patients 100 less strokes
3 strokes prevented for each bleed
where is your threshold?
how many strokes in 100 with 3% bleeding?

41. 1.0%

42. 1.0%

43. 1.0%

44. 1.0%

45. Example: clopidogrel or ASA?
pts with threatened stroke
RCT of clopidogrel vs ASA
19,185 patients
ischaemic stroke, MI, or vascular death compared
939 events (5·32%) clopidogrel
1021 events (5·83%) with aspirin
RR 0.91 (95% CI 0.83 – 0.99) (p=0·043)
rate down for precision?

46. Clopidogrel or ASA for threatened vascular events
RCT 19,185 patients
1.7% – 0.1%
RR 0.91 (95% CI 0.83 – 0.99)
1.0%

47. Non-inferiority

48. Non-inferiority

49. Non-inferiority

50. small trials, large effect analogy to stopping early
likely to be overestimate
analogy to stopping early
lack of prognostic balance
solution: optimal information size
# of pts from conventional sample size calculation
specify control group risk, α, β, Δ

51. Fluoroquinolone prophylaxis in neutropenia:
infection-related mortality
Total number of events: 47

52. sample size 1,002 α 0.05, β 0.20, Δ 0.25 RRR, CER 7% N = 6,000
Fluoroquinolone prophylaxis in neutropenia:
infection-related mortality
sample size 1,002
α 0.05, β 0.20, Δ 0.25 RRR, CER 7%
N = 6,000

53. Publication bias high likelihood could lower quality when to suspect
number of small studies
industry sponsored

56. Funnel Plot Fish oil on mortality

57. What can raise confidence?
What do you do high certainty, no RCTs?
common criteria
everyone used to do badly
almost everyone does well
quick action
insulin for diabetic ketoacidosis?
thyroxine for thyroid deficiency?
hydrocortisone for adrenal insufficiency?

58. Dose-response gradient
childhood lymphoblastic leukemia
risk for CNS malignancies 15 years after cranial irradiation
no radiation: 1% (95% CI 0% to 2.1%)
12 Gy: 1.6% (95% CI 0% to 3.4%)
18 Gy: 3.3% (95% CI 0.9% to 5.6%).

59. Cetainty assessment criteria

60. Overall level of evidence
What to do when certainty differs across outcomes?
options
ignore all but primary
previous approach
least certainty of any outcome
some blended approach
least certainty of critical outcomes

61. Trading off desirable and undersirable
what do patients/clinicians need to know
relative risk reduction?
absolute risk difference?
Toxic treatment, 50% RRR mortality? OK?
1% to 1/2% OK?
40% to 20%, OK?
body of evidence
how do we get risk difference?

62. How to get absolute? meta-analysis get pooled relative risk
obtain baseline risk and multiply
BR 10%, RRR 50%, RD 5%
why not get risk difference directly?

63. RR 0.67
RD 10%
RR 0.67
RD 3.3%
RR 0.67
RD 1%

65. High versus low PEEP in ALI and ARDS
Population
No. of participants (trials) †
Higher PEEP
Lower PEEP
Adjusted Relative Risk (95% CI; P-value) ‡
Adjusted Absolute Risk Difference (95% CI)
Quality
Patients with ARDS
1892 (3)
324/951 (34.1%)
368/941 (39.1%)
0.90 (0.81 to 1.00; 0.049)
-3.9% (-7.4% to -0.04%)
High
Patients without ARDS
404 (3)
50/184 (27.2%)
41/220 (18.6%)
1.37 (0.98 to 1.92; 0.065)
6.9% (-0.4% to 17.1%)
Moderate
(imprecision)

66. Strength of Recommendation
strong recommendation
benefits clearly outweigh risks/hassle/cost
risk/hassle/cost clearly outweighs benefit
what can downgrade strength?
low confidence in estimates
close balance between up and downsides

67. Risk/Benefit tradeoff
aspirin after myocardial infarction
25% reduction in relative risk
side effects minimal, cost minimal
benefit obviously much greater than risk/cost
warfarin in low risk atrial fibrillation
warfarin reduces stroke vs ASA by 50%
but if risk only 1% per year, ARR 0.5%
increased bleeds by 1% per year
Reason for clear recommendations in first example is that benefits moderate to large and risk or costs are minimal
Reson that equivocal in second is that benefits slightly smaller, risks greater, and costs greater; means that close call (or at least some might think so)

68. Strength of Recommendations
Aspirin after MI – do it
Warfarin rather than ASA in Afib
-- probably do it
-- probably don’t do it

72. Significance of strong vs weak
variability in patient preference
strong, almost all same choice (> 90%)
weak, choice varies appreciably
interaction with patient
strong, just inform patient
weak, ensure choice reflects values
use of decision aid
strong, don’t bother; weak, use the aid
quality of care criterion
strong, consider; weak, don’t consider

73. When evidence is low confidence
choice more preference dependent
risk aversion
steroids for pulmonary fibrosis
low quality evidence in support of benefit
high quality evidence of toxicity

74. When confidence is low recommendation to the hopeful patient
I’m likely to deteriorate
if something might work, let’s try it
damn the torpedoes
recommendation to the fearful patient
doctor, you mean you know it’s toxic
diabetes, skin changes, body habitus, infection, osteoporosis
you don’t know for sure it works? are you crazy?
weak recommendation mandated

75. Presentation strong weak never “we suggest…”
“we recommend”…
weak
“we suggest…”
never
we recommend (or suggest) you consider…

76. Challenge Comparator often not clear
Children with suspected or confirmed tuberculous meningitis should be treated with a four-drug regimen (HRZE) for 2 months, followed by a two-drug regimen (HR) for 10 months
Offer and promote postpartum and post-abortion contraception to adolescents through multiple home visits and/or clinic visits 76

77. Strong recommendations, Low certainty: Discordant recs
Experts use often
Why? What are the possibilities?

78. Why all the inappropriate strong recommendations?
panels don’t believe their own confidence ratings
personal conviction trumps evidence
believe weak recommendations ignored
influence funders

79. Discordant recommendations: What are the possibilities?
good practice
mistaken judgment
inappropriate
exceptional situation they got it right

80. Good Practice Statements
For patients with congenital adrenal hyperplasia, we recommend monitoring patients for signs of glucocorticoid excess
Wealth of indirect linked evidence
High confidence in net benefit
Benefit clear
Minimal harms or costs
Poor use of guideline panel time effort summarize

81. Summarizing evidence poor use of time
symptoms and signs appear not infrequently
Collect cohort studies of incidence
Studies of accuracy of symptoms and signs
patients suffer if clinicians fail to recognize
Reports of untreated glucocorticoid excess
clinical action can ameliorate the problem
Evidence supporting therapy
describe how evidence is linked

82. Questions panels considering good practice statement should ask
Is the statement clear and actionable?
Is the message really necessary?
Is the net benefit large and unequivocal?
Is the evidence difficult to collect and summarize?
If a public health guideline, are there specific issues that should be considered (e.g. equity)
Have you made the rationale explicit?
Is this better to be formally GRADEd?

83. Clear and actionable
For patients with congenital adrenal hyperplasia, we recommend monitoring patients for signs of glucocorticoid excess
Monitor how often?
Nature of monitoring
What to do if signs of excess found

84. Really necessary?
For patients with congenital adrenal hyperplasia, we recommend monitoring patients for signs of glucocorticoid excess
Really plausible that clinicians won’t monitor?
If not, not necessary

85. Provide Rationale relevant symptoms and signs appear not infrequently
patients will suffer if clinicians fail to recognize these signs
clinical action can ameliorate the problem.

86. 1 2 3 4 5 LQE in a life-threatening situation
Fresh frozen plasma and intracranial bleed 2
LQoE benefit and HQoE suggests harm
Head-to-toe CT/MRI screening for cancer. 3
LQoE suggests equivalence, HQoE less harm for one alternative
Helicobacter pylori eradication early stage gastric MALT lymphoma 4
HQoE suggests equivalence, LQoE suggests harm in one alternative
ACEI in hypertension in women planning conception and in pregnancy. 5
HQoE suggests benefit in one outcome, LQoE suggests harm in more highly valued
outcome
Testosterone in males with or at risk of prostate cancer 86

87. 1 2 3 4 5 LQE in a life-threatening situation
Fresh frozen plasma and intracranial bleed 2
LQoE benefit and HQoE suggests harm
Head-to-toe CT/MRI screening for cancer. 3
LQoE suggests equivalence, HQoE less harm for one alternative
Helicobacter pylori eradication early stage gastric MALT lymphoma 4
HQoE suggests equivalence, LQoE suggests harm in one alternative
ACEI in hypertension in women planning conception and in pregnancy. 5
HQoE suggests benefit in one outcome, LQoE suggests harm in more highly valued
outcome
Testosterone in males with or at risk of prostate cancer 87

88. 1 2 3 4 5 LQE in a life-threatening situation
Fresh frozen plasma and intracranial bleed 2
LQoE benefit and HQoE suggests harm
Head-to-toe CT/MRI screening for cancer. 3
LQoE suggests equivalence, HQoE less harm for one alternative
Helicobacter pylori eradication early stage gastric MALT lymphoma 4
HQoE suggests equivalence, LQoE suggests harm in one alternative
ACEI in hypertension in women planning conception and in pregnancy. 5
HQoE suggests benefit in one outcome, LQoE suggests harm in more highly valued
outcome
Testosterone in males with or at risk of prostate cancer 88

89. 1 2 3 4 5 LQE in a life-threatening situation
Fresh frozen plasma and intracranial bleed 2
LQoE benefit and HQoE suggests harm
Head-to-toe CT/MRI screening for cancer. 3
LQoE suggests equivalence, HQoE less harm for one alternative
Helicobacter pylori eradication early stage gastric MALT lymphoma 4
HQoE suggests equivalence, LQoE suggests harm in one alternative
ACEI in hypertension in women planning conception and in pregnancy. 5
HQoE suggests benefit in one outcome, LQoE suggests harm in more highly valued
outcome
Testosterone in males with or at risk of prostate cancer 89

90. 1 2 3 4 5 LQE in a life-threatening situation
Fresh frozen plasma and intracranial bleed 2
LQoE benefit and HQoE suggests harm
Head-to-toe CT/MRI screening for cancer. 3
LQoE suggests equivalence, HQoE less harm for one alternative
Helicobacter pylori eradication early stage gastric MALT lymphoma 4
HQoE suggests equivalence, LQoE suggests harm in one alternative
ACEI in hypertension in women planning conception and in pregnancy. 5
HQoE suggests benefit in one outcome, LQoE suggests harm in more highly valued
outcome
Testosterone in males with or at risk of prostate cancer 90

91. Methods
systematic survey of all published ES guidelines between 2005 and 2011
screening and extraction in duplicate
for each recommendation: confidence in estimates, strength of recommendation
strong recommendations based on LQE taxonomy for paradigmatic recommendations applied

92. If they did not fit one of 5 paradigms
Condition
Example 1
Best practice statements
For patients with Congenital Adrenal Hyperplasia, we recommend monitoring patients for signs of glucocorticoid excess 2
Additional research
We recommend additional investigation using rodents and primates to further define the specific targets of androgen action 3
Mistaken judgment
For overweight and obese children and adolescents, intensive lifestyle modification for the patient and entire family 4
Inappropriate strong recommendation
In patients with primary aldosteronism who are unable or unwilling to undergo laparascopic adrenalectomy, we recommend medical treatment with mineralocorticoids

93. Guidelines Strenght and Confidence
Strong recommendations (n=206):
n (%)
Weak recommendations (n=151):
High/moderate confidence in estimates 85
(41%)
High/moderate confidence in estimates 16
(8%)
Very low/low confidence in estimates
121
(59%)
Very low/ low confidence in estimates
135
(92%)
Totals (%)
206
(100%)
151 93

94. Condition N - 35 1 LQE in a life-threatening situation 13
LQoE benefit and HQoE suggests harm or a very high cost 7
LQoE suggests equivalence, HQoE less harm for one of the competing alternatives. 5
HQoE suggests equivalence of two alternatives and LQoE suggests harm in one alternative 9
HQoE suggests modest benefits and LQoE suggests possibility of catastrophic harm

95. Inappropriate strong recommendation
Condition 43
Best practice 5
Mistaken judgment
Additional research 33
Inappropriate strong recommendation

96. Summary majority ES recommendations strong 121 (59%) discordant
35/121 (29%) of discordant appropriate
of 86 inappropriate, 43 (50%) best practice statements
33/86 inappropriate, should have been weak recommendations

97. WHO recommendation mental health guideline 2013
8 of 9 confidence low, strong
“On a number of occasions, the GDG decided to give a strong recommendation despite a GRADE assessment of the available evidence on effect as being of “very low quality”.

98. Why?
“This occurred only when the following conditions applied: (a) there was certainty about the balance of benefits versus harms and burdens; (b) the expected values and preferences were clearly in favour of the recommendation; and (c) there was certainty about the balance between benefits and resources being consumed.”

99. Value and preference statements
underlying values and preferences always present
sometimes crucial
important to make explicit

100. Values and preferences
Stroke guideline: patients with TIA clopidogrel over aspirin (Grade 2B).
Underlying values and preferences: This recommendation to use clopidogrel over aspirin places a relatively high value on a small absolute risk reduction in stroke rates, and a relatively low value on minimizing drug expenditures.

101. Values and preferences
peripheral vascular disease: aspirin be used instead of clopidogrel (Grade 2A).
Underlying values and preferences: This recommendation places a relatively high value on avoiding large expenditures to achieve small reductions in vascular events.

102. Values and preferences
Consider UpToDate style of values and preferences
Weak recommendation low certainty evidence for trial of testosterone in men with apparent testosterone deficiency and cardiovascular disease
Men who place a high value on minimizing risk of an adverse cardiovascular event and a relatively low value in ameliorating the symptoms of testosterone deficiency are likely to choose against testoserone use

103. Flavanoids for Hemorrhoids
venotonic agents
mechanism unclear, increase venous return
popularity
90 venotonics commercialized in France
none in Sweden and Norway
France 70% of world market
possibilities
French misguided
rest of world missing out

104. Systematic Review 14 trials, 1432 patients key outcome
risk not improving/persistent symptoms
11 studies, 1002 patients, 375 events
RR 0.4, 95% CI 0.29 to 0.57
minimal side effects
is France right?
what is the certainty of evidence?

105. What can lower confidence?
risk of bias
lack of detail re concealment
questionnaires not validated
indirectness – no problem
inconsistency, need to look at the results

107. Publication bias? size of studies 40 to 234 patients, most around 100
all industry sponsored

109. What can lower confidence?
risk of bias
lack of detail re concealment
questionnaires not validated
inconsistency
almost all show positive effect, trend
heterogeneity p < 0.001; I2 65.1%
indirectness
imprecision
RR 0.4, 95% CI 0.29 to 0.57
publication bias
40 to 234 patients, most around 100

110. Is France right? recommendation yes no against use strength strong
weak

111. Beta blockers in non-cardiac surgery
Quality Assessment
Summary of Findings
Quality
Relative Effect
(95% CI)
Absolute risk difference
Outcome
Number of participants
(studies)
Risk of Bias
Consistency
Directness
Precision
Publication Bias
Myocardial infarction
10,125
(9)
No serious limitations
No serious imitations
Not detected
High
0.71
(0.57 to 0.86)
1.5% fewer
(0.7% fewer to 2.1% fewer)
Mortality
10,205
(7)
No serious limiations
Imprecise
Moderate
1.23
(0.98 – 1.55)
0.5% more
(0.1% fewer
to 1.3% more)
Stroke
10,889
(5)
No serious limitaions
2.21
(1.37 – 3.55)
(0.2% more to
1.3% more0

112. Where to from here? GRADE values and preferences GRADE diagnosis
Aspirin for primary prevention
Culprit only vs complete revascularization in STEMI
Management of esophageal varices