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How can we mitigate against non-causal associations in design and analysis?

How can we mitigate against non-causal associations in design and analysis?. Epidemiology matters: a new introduction to methodological foundations Chapter 10. Seven steps. Define the population of interest Conceptualize and create measures of exposures and health indicators

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How can we mitigate against non-causal associations in design and analysis?

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  1. How can we mitigate against non-causal associations in design and analysis? Epidemiology matters: a new introduction to methodological foundations Chapter 10

  2. Seven steps • Define the population of interest • Conceptualize and create measures of exposures and health indicators • Take a sample of the population • Estimate measures of association between exposures and health indicators of interest • Rigorously evaluate whether the association observed suggests a causal association • Assess the evidence for causes working together • Assess the extent to which the result matters, is externally valid, to other populations Epidemiology Matters – Chapter 1

  3. Randomization • Matching • Stratification • Sources of non-comparability • Summary Epidemiology Matters – Chapter 10

  4. Randomization • Matching • Stratification • Sources of non-comparability • Summary Epidemiology Matters – Chapter 10

  5. Comparability • Exposed and unexposed should be comparable on all factors associated with the disease other than the exposure • One way to ensure this comparability is to randomize the exposure Epidemiology Matters – Chapter 10

  6. Comparability What is wrong with non-comparability? Consider an example: • Study: 5,000 smokers and 5,000 non-smokers are followed for 10 years • After 10 years, the smokers have 3.0 times the risk of motor vehicle crash fatality compared with non-smokers • Are you comfortable reporting that smoking causes motor vehicle crash fatality? Epidemiology Matters – Chapter 10

  7. Comparability, an example • Study: 5,000 smokers and 5,000 non-smokers are followed for 10 years • After 10 years, the smokers have 3.0 times the risk of motor vehicle crash fatality compared with non-smokers • Are you comfortable reporting that smoking causes motor vehicle crash fatality? • Individuals who choose to smoke are more likely to engage in other behaviors with adverse consequences for health Epidemiology Matters – Chapter 10

  8. Randomization • Creates comparability between groups • Removes individual’s ability to choose exposure status Epidemiology Matters – Chapter 10

  9. Randomized Control Trial,RCT • Sample from population (purposive) • Assign individuals to be exposed or unexposed • Follow population forward to determine who develops outcome Epidemiology Matters – Chapter 10

  10. The goal of RCT • We want our comparison groups to be • “different” on just our main exposure that we are studying in relation to some outcome AND • the “same” on all the other important covariates Epidemiology Matters – Chapter 10

  11. Why does randomization control for non-comparability? Example • Two investigators conduct two separate studies • Exploring effects of regular cardiovascular exercise on incidence of cardiovascular disease • Population is post-menopausal women • Hypothesis: exercise is protective against cardiovascular disease Epidemiology Matters – Chapter 10

  12. Example, study 1 • Purposive sample of 80 post-menopausal women with no history of cardiovascular disease • Asks women if they engage in ≥ 30 minutes of regular cardiovascular exercise ≥ 3 times/week (regular exercise compared to non-regular exercise) • Follows groups for five years • Count women in each group who have a cardiovascular event • Assume no losses to follow-up Epidemiology Matters – Chapter 10

  13. Non-diseased Diseased Non-exposed Exposed Epidemiology Matters – Chapter 10

  14. Study 1 Epidemiology Matters – Chapter 10

  15. Study 1, interpretation Those who exercise have approximately 0.5 times the risk of cardiovascular disease compared with those who do not exercise. There are approximately 20 fewer cases of cardiovascular disease per every 100 people who exercise compared with those who do not exercise. Epidemiology Matters – Chapter 10

  16. Study 1,validity • Women who choose to exercise regularly may be more likely to be non-smokers, eat a more healthy diet, take multivitamins, etc. • We do not know whether the exercise had any causal effect on their cardiovascular health • In fact, the women who exercise had much lower average daily saturated fat intake than the non-exercisers Epidemiology Matters – Chapter 10

  17. Impact of saturated fat intake Exerciser without high saturated fat intake Exerciser with high saturated fat intake Non-exerciser without high saturated fat intake Non-exerciser with high saturated fat intake Epidemiology Matters – Chapter 10

  18. Impact of saturated fat intake • 9 dotted people (high fat consumers) among 40 exercisers • Total prevalence = 22.5% of high fat consumption among the exercisers • 18 dotted people (high fat consumers) among the 40 non-exercisers • Total prevalence = 45%of high fat consumption among the non-exercisers • There is a greater proportion of high fat consumers among the non-exercisers Epidemiology Matters – Chapter 10

  19. Example, study 2 • Purposive sample of 80 post-menopausal women with no history of cardiovascular disease • Randomly assigns women to engage in ≥ 30 minutes of regular cardiovascular exercise ≥ 3 times/week (regular exercise compared to non-regular exercise) • Follows groups for five years • Counts women in each group who have a cardiovascular event • Assume no losses to follow-up or noncompliance Epidemiology Matters – Chapter 10

  20. Study 2 Epidemiology Matters – Chapter 10

  21. Study 2 - interpretation Risk of cardiovascular disease among those randomized to exercise is 14.3% lessthan the risk among those randomized to not exercise. We expect 10 fewer cases per 100 individuals exposed compared with the unexposed. Epidemiology Matters – Chapter 10

  22. Study 1 vs Study 2 • Study 1 risk ratio = 0.5 and risk difference = -0.2 • Study 2 risk ratio = 0.86 and risk difference = -0.1 • Therefore, the effect is weaker in Study 2 than the effect in Study 1. • Why? Epidemiology Matters – Chapter 10

  23. Study 2, impact of saturated fat intake Exerciser without high saturated fat intake Exerciser with high saturated fat intake Non-exerciser without high saturated fat intake Non-exerciser with high saturated fat intake Epidemiology Matters – Chapter 10

  24. Study 2, impact of saturated fat intake • 12 dotted people (high fat consumers) among 40 exercisers • Total prevalence = 30% of high fat consumption among the exercisers • 12 dotted people (high fat consumers) among the 40 non-exercisers • Total prevalence = 30% of high fat consumption among the non-exercisers • There is the same proportion of excess high fat consumers among both groups Epidemiology Matters – Chapter 10

  25. Limitations to randomization • Equipoise and ethics • Complication and intention to treat analysis, • Placebos and placebo effects, and the • Importance of blinding Epidemiology Matters – Chapter 10

  26. Randomization, summary • When randomization works, all factors that would differ between two groups who got to choose their exposure status are, on average, evenly distributed between the groups • This includes all known risk factors for the outcome and a myriad unknown or difficult to measure • Because they are evenly distributed across the groups, factors cannot affect the study estimates • Randomized trials are a powerful way to achieve comparability between exposed and unexposed groups on both known and unknown factors that cause the outcome Epidemiology Matters – Chapter 10

  27. Randomization • Matching • Stratification • Sources of non-comparability • Summary Epidemiology Matters – Chapter 10

  28. Matching • Why and how to match • Analyzing matched pair data Epidemiology Matters – Chapter 10

  29. Matching • Randomization often unethical and infeasible • Matching controls non-comparability where randomization is impossible Epidemiology Matters – Chapter 10

  30. Matching • Participants matched on potential sources of non-comparability • Matching is a common way to control for non-comparability in design stage • In a cohort study, exposed individuals are matched to ≥ 1 unexposed individuals on ≥ 1 factor(s) of interest • In a case control study, diseased individuals are matched to a sample of disease free individuals Epidemiology Matters – Chapter 10

  31. Matching,example • Research question: Is low regular consumption of fish oil associated with development of depression? • Sample • 25 individuals with a first diagnosis of depression recruited from local mental health treatment center • 25 individuals with no history of depression from community surrounding mental health treatment center Epidemiology Matters – Chapter 10

  32. Matching,example • Concerned about sexas a potential source of non-comparability • Women more likely to develop depression compared with men • Women on average have more nutritious diets and more likely to supplement diets with fish oil • Other potential sources of non-comparability to worry about (though we are not necessarily matching on) areage,alcohol and cigarette use, socio-economic factors Epidemiology Matters – Chapter 10

  33. Matching,example Each time we select a case from the treatment center, we select one or more controls of the same sex Epidemiology Matters – Chapter 10

  34. Matching to control non-comparability Female low fish oil Male low fish oil Female high fish oil Male high fish oil Epidemiology Matters – Chapter 10

  35. Matching to control non-comparability Female low fish oil Male low fish oil Female high fish oil Male high fish oil Epidemiology Matters – Chapter 10

  36. Matching pairs, sex Female lowfish oil Male lowfish oil Female highfish oil Male highfish oil Each pair is identical with respect to the matched factors Sample had 50 individuals Sample now has 25 matched pairs Epidemiology Matters – Chapter 10

  37. Matching pairs, sex Epidemiology Matters – Chapter 10

  38. Analyzing matched pair data Epidemiology Matters – Chapter 10

  39. Analyzing matched pair, example Interpretation: Individuals who do not consume fish oil are 2.0 times as likely to develop depression as individuals who consume fish oil, controlling for sex. Epidemiology Matters – Chapter 10

  40. Randomization • Matching • Stratification • Sources of non-comparability • Summary Epidemiology Matters – Chapter 10

  41. Controlof non-comparability Design stage • Randomization • Matching Analysis stage • Stratification Epidemiology Matters – Chapter 10

  42. Stratification • Why and how to stratify • Interpreting stratified analyses Epidemiology Matters – Chapter 10

  43. Control of non-comparability in theanalysis stage • Collect data on variables that might contribute to non-comparability • Our ability to control for non-comparability in analysis stage is only as good as the quality of measures of variables contributing to non-comparability Epidemiology Matters – Chapter 10

  44. Control of non-comparability in theanalysis stage Is a potential factor related to non-comparability associated with the exposure and the outcome? Epidemiology Matters – Chapter 10

  45. Stratification Stratification removes effects of non-comparable variable on an exposure-outcome relation by limiting the variance on that outcome Epidemiology Matters – Chapter 10

  46. Stratification, example Examine relation between alcohol consumption and esophageal cancer among two groups Non-smokers • Among individuals who have never smoked a cigarette in their lives, what is the relation between heavy alcohol consumption and esophageal cancer? • Smoking cannot confound the effect estimate because no individual in this subgroup has engaged in any smoking Smokers • Among smokers (presumably around the same duration and average amount), were those who are heavy alcohol consumers more likely to develop esophageal cancer? • Smoking cannot confound the estimate because everyone is a smoker Epidemiology Matters – Chapter 10

  47. Stratificationexamplenon-smokers Conditional probability of esophageal cancer among heavy alcohol consumers =1/6 or 16.7% Conditional probability of esophageal cancer among not heavy alcohol consumers = 1/16 or 6.3% Risk ratio = 16.7/ 6.3 = 2.65 Risk difference = 16.7– 6.3 = 10.4 Interpretation: There is an increased risk of esophageal cancer among heavy alcohol consumers, even in the subpopulation of individuals who do not smoke. Epidemiology Matters – Chapter 10

  48. Stratificationexamplesmokers 31 Conditional probability of esophageal cancer among heavy alcohol consumers =21/31, or 67.7%. Conditional probability of esophageal cancer among not heavy alcohol consumers = 7/27 or 25.9% Risk ratio = 67.7 / 25.9 = 2.61 Risk difference = 67.7 – 25.9 = 41.8 There is an increased risk of esophageal cancer among heavy alcohol consumers, even in the subpopulation of individuals who all smoke. Epidemiology Matters – Chapter 10

  49. Stratification, example • There is an increased risk of esophageal cancer among heavy alcohol consumers, even in the subpopulation of individuals who do not smoke • There is an increased risk of esophageal cancer among heavy alcohol consumers, even in the subpopulation of individuals who all smoke • Therefore, even when we limit variance on the possible source of non-comparability (i.e., smoking) there still remains an increased risk of esophageal cancer among heavy alcohol drinkers Epidemiology Matters – Chapter 10

  50. Non-comparability throughstratification • Careful and rigorous measurement of potential non-comparable variables is key to control for non-comparability in data analysis • Before stratification, always check that potential non-comparable variables are associated with exposure and outcome under study • If a variable is not associated with both exposure and outcome, then stratifying or otherwise controlling for that variable will not change the estimate of the effect of exposure on outcome Epidemiology Matters – Chapter 10

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