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Ronald C. Kessler, Ph.D. Department of Health Care Policy Harvard Medical School March 6, 2008

Comorbidity of Anxiety Disorders in the National Comorbidity Survey Adolescent Supplement (NCS-A). Ronald C. Kessler, Ph.D. Department of Health Care Policy Harvard Medical School March 6, 2008. NCS-A study design. Nationally representative sample of n = 10,200 adolescents

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Ronald C. Kessler, Ph.D. Department of Health Care Policy Harvard Medical School March 6, 2008

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  1. Comorbidity of Anxiety Disorders in the National Comorbidity Survey Adolescent Supplement (NCS-A) Ronald C. Kessler, Ph.D. Department of Health Care Policy Harvard Medical School March 6, 2008

  2. NCS-A study design • Nationally representative sample of n = 10,200 adolescents • Sampled from a nationally representative sample of 230 schools • All respondents were ages 13 – 17, English-speaking, and students • Face-to-face interviews with respondents • Self-administered questionnaires with parents

  3. The NCS-A instruments • Adolescent version of WHO CIDI – 3.0 with adolescents • Informant version of CIDI with parents • School survey focused on mental health resources with school Principals and mental health coordinators

  4. DSM-IV anxiety disorders assessed • Panic disorder with or without agoraphobia • Agoraphobia without a history of panic disorder • Specific phobia • Social phobia • Generalized anxiety disorder • Post-traumatic stress disorder • Obsessive-compulsive disorder • Separation anxiety disorder

  5. Other DSM-IV disorders assessed • Mood disorders (MDD, dysthymic disorder, BPD) • Externalizing disorders (ADHD, ODD, CD, IED, eating disorders) • Substance disorders (alcohol and drug abuse-dependence)

  6. Concordance of DSM-IV diagnoses based on the CIDI and the K-SADS SensSpecAUC

  7. DSM-IV/CIDI lifetime prevalence estimates of anxiety disorders %(se)

  8. Age of onset distributions for anxiety disorders

  9. Age of onset distributions for mood disorders

  10. Age of onset distributions for externalizing disorders

  11. Age of onset distributions for substance disorders

  12. Age of onset distributions for each class of disorders

  13. Rotated (promax) factor loadings (standardized regression coefficients) of lifetime DSM-IV/CIDI diagnoses at the level of the person-year

  14. Rotated (promax) factor loadings (standardized regression coefficients) of lifetime DSM-IV/CIDI diagnoses at the level of the person-year

  15. Discrete-time survival analysis of associations between temporally primary disorders and the subsequent onset of secondary disorders • Person-year data array

  16. Discrete-time survival analysis of associations between temporally primary disorders and the subsequent onset of secondary disorders • Person-year data array • Temporally primary disorders are treated as time-varying covariates

  17. Discrete-time survival analysis of associations between temporally primary disorders and the subsequent onset of secondary disorders • Person-year data array • Temporally primary disorders are treated as time-varying covariates • A series of models was estimated to evaluate the effects of primary disorders on onset of secondary disorders

  18. Survival analysis summary of results • Everything predicts everything in bivariate models

  19. Survival analysis summary of results • Everything predicts everything in bivariate models • Many sign flips in additive multivariate models

  20. Survival analysis summary of results • Everything predicts everything in bivariate models • Many sign flips in additive multivariate models • Marginal effects stabilize in a simple global interactions model

  21. Survival analysis summary of results • Everything predicts everything in bivariate models • Many sign flips in additive multivariate models • Marginal effects stabilize in a simple global interactions model • Global interactions are significant and consistently sub-additive

  22. Survival analysis summary of results • Everything predicts everything in bivariate models • Many sign flips in additive multivariate models • Marginal effects stabilize in a simple global interactions model • Global interactions are significant and consistently sub-additive • More complex interaction models find no evidence of domain-specific effects

  23. Survival analysis summary of results • Everything predicts everything in bivariate models • Many sign flips in additive multivariate models • Marginal effects stabilize in a simple global interactions model • Global interactions are significant and consistently sub-additive • More complex interaction models find no evidence of domain-specific effects • Marginal effects show some evidence of domain specificity, but domain-specific effects do not account for all significant associations

  24. Survival analysis summary of results regarding marginal effects • There are 240 logically possible time-lagged associations among 16 disorders

  25. Survival analysis summary of results regarding marginal effects • There are 240 logically possible time-lagged associations among 16 disorders • But some of these do not exist by definition (e.g., BPD predicting MDD)

  26. Survival analysis summary of results regarding marginal effects • There are 240 logically possible time-lagged associations among 16 disorders • But some of these do not exist by definition (e.g., BPD predicting MDD) • Others had too few cases for analysis (e.g., drug disorders predicting ADHD, as onset of ADHD occurs so much earlier than onset of drug abuse)

  27. Survival analysis summary of results regarding marginal effects • There are 240 logically possible time-lagged associations among 16 disorders • But some of these do not exist by definition (e.g., BPD predicting MDD) • Others had too few cases for analysis (e.g., drug disorders predicting ADHD, as onset of ADHD occurs so much earlier than onset of drug abuse) • As a result, we had a total of 236 time-lagged associations to study

  28. Survival analysis summary of results regarding marginal effects • 91.5% of the 236 survival coefficients were positive

  29. Survival analysis summary of results regarding marginal effects • 91.5% of the 236 survival coefficients were positive • 58.8% of the positive coefficients were statistically significant at the .05 level (two-sided tests)

  30. Survival analysis summary of results regarding marginal effects • 91.5% of the 236 survival coefficients were positive • 58.8% of the positive coefficients were statistically significant at the .05 level (two-sided tests) • None of the negative coefficients was statistically significant

  31. Survival analysis summary of results regarding marginal effects • 91.5% of the 236 survival coefficients were positive • 58.8% of the positive coefficients were statistically significant at the .05 level (two-sided tests) • None of the negative coefficients was statistically significant • The within-domain coefficients were generally larger than the between-domain coefficients

  32. Mean values (and percent statistically significant at the .05 level, two-sided test) of marginal effect survival coefficients within and between domains

  33. Mean values (and percent statistically significant at the .05 level, two-sided test) of marginal effect survival coefficients within and between domains

  34. Mean values of substantively significant odds-ratios within and between domains

  35. Conclusions • It is not entirely clear that it makes sense to speak of a single “domain” of disorders known as “anxiety disorders.” Distinct fear and distress domains clearly exist. The situation with OCD might be part of yet a third domain.

  36. Conclusions The Fear and Distress Disorders Association of America

  37. Conclusions FD2A2

  38. Conclusions • It is not entirely clear that it makes sense to speak of a single “domain” of disorders known as “anxiety disorders.” Distinct fear and distress domains clearly exist. The situation with OCD might be part of yet a third domain. • Fear disorders are the most commonly occurring early-onset mental disorders.

  39. Conclusions • It is not entirely clear that it makes sense to speak of a single “domain” of disorders known as “anxiety disorders.” Distinct fear and distress domains clearly exist. The situation with OCD might be part of yet a third domain. • Fear disorders are the most commonly occurring early-onset mental disorders. • Fear disorders have a very strong pattern of cumulation over time, with the onset of the first strongly predicting the subsequent onset of the second, the second predicting the third, and so forth.

  40. Conclusions (cont.) • Fear disorders also strongly predict the subsequent onset of a wide range of other disorders, the main exception being substance disorders.

  41. Conclusions (cont.) • Fear disorders also strongly predict the subsequent onset of a wide range of other disorders, the main exception being substance disorders. • Social and specific phobias are as important here as panic disorder. This is striking in light of the general perception that child-adolescent phobias are not very “important” in comparison to other commonly occurring early-onset disorders.

  42. Conclusions (cont.) • Fear disorders also strongly predict the subsequent onset of a wide range of other disorders, the main exception being substance disorders. • Social and specific phobias are as important here as panic disorder. This is striking in light of the general perception that child-adolescent phobias are not very “important” in comparison to other commonly occurring early-onset disorders. • It’s not clear that these associations are causal.

  43. Conclusions (cont.) • An impediment to addressing the causality issue is that early-onset fear disorders are under-treated.

  44. Conclusions (cont.) • An impediment to addressing the causality issue is that early-onset fear disorders are under-treated. • We need effectiveness trials that evaluate the effects of timely detection and treatment of early-onset fear disorders on the subsequent onset of other mental disorders.

  45. Conclusions (cont.) • Distress disorders, which include not only depression but also GAD and PTSD, typically have later ages of onset.

  46. Conclusions (cont.) • Distress disorders, which include not only depression but also GAD and PTSD, typically have later ages of onset. • We know that distress disorders are seriously impairing in their own right and greatly increase the severity of comorbid disorders.

  47. Conclusions (cont.) • Distress disorders, which include not only depression but also GAD and PTSD, typically have later ages of onset. • We know that distress disorders are seriously impairing in their own right and greatly increase the severity of comorbid disorders. • It is especially important in light of these other results that distress disorders are quite important in predicting the subsequent onset of diverse secondary disorders.

  48. Conclusions (cont.) • As a result, distress disorders are usually highly comorbid. The vast majority of people with all major distress disorders have a history of other mental disorders.

  49. Conclusions (cont.) • As a result, distress disorders are usually highly comorbid. The vast majority of people with all major distress disorders have a history of other mental disorders. • As with fear disorders, it’s difficult to know what causes what in comorbidities involving distress disorders.

  50. Conclusions (cont.) • An added complication in sorting out causal priorities for distress disorders is that distress disorders have a very protracted risk window compared to fear disorders, as indicated by the wider IQR of the AOO distribution (close to 30 years for distress vs. 7-10 years for fear disorders).

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