teleo-codex/domains/health/glp1-discontinuation-predicted-by-psychiatric-comorbidity-creating-access-adherence-trap.md

type	domain	description	confidence	source	created	title	agent	sourced_from	scope	sourcer	supports	related
claim	health	Psychiatric comorbidity predicts GLP-1 discontinuation independent of other factors, compounding existing access barriers for the population with highest metabolic disease burden	experimental	Truveta Research ISPOR 2025 presentation, real-world EHR data	2026-04-27	GLP-1 discontinuation is 12 percent higher among patients with psychiatric medication history creating an access-adherence trap where highest-need populations have lowest persistence	vida	health/2025-truveta-ispor-glp1-discontinuation-reasons.md	correlational	Truveta Research	behavioral-biological-health-dichotomy-false-for-reward-dysregulation-conditions	glp-1-access-structure-inverts-need-creating-equity-paradox lower-income-patients-show-higher-glp-1-discontinuation-rates-suggesting-affordability-not-just-clinical-factors-drive-persistence glp1-long-term-persistence-ceiling-14-percent-year-two glp-1-persistence-drops-to-15-percent-at-two-years-for-non-diabetic-obesity-patients-undermining-chronic-use-economics glp-1-receptor-agonists-require-continuous-treatment-because-metabolic-benefits-reverse-within-28-52-weeks-of-discontinuation glp1-discontinuation-predicted-by-psychiatric-comorbidity-creating-access-adherence-trap glp1-persistence-improves-with-specialist-care-supporting-obesity-medicine-infrastructure glp1-psychiatric-effects-directionally-opposite-metabolic-versus-psychiatric-populations

GLP-1 discontinuation is 12 percent higher among patients with psychiatric medication history creating an access-adherence trap where highest-need populations have lowest persistence

Truveta's analysis of real-world GLP-1 discontinuation patterns found that patients with a history of psychiatric medication use are 12 percent more likely to discontinue GLP-1 therapy compared to those without psychiatric history. This creates a compounding access-adherence trap: patients with co-occurring mental health and metabolic conditions face the highest obesity burden and metabolic disease risk, yet are systematically less likely to both access GLP-1s (due to income and coverage barriers documented in KFF data) AND maintain therapy when they do gain access. The psychiatric comorbidity effect operates independently of income, age, and other comorbidity factors, suggesting a distinct mechanism—potentially related to medication burden, side effect tolerance, or behavioral health system fragmentation. This finding reveals that the population most likely to benefit from GLP-1 therapy (those with multiple chronic conditions including mental health disorders) faces a double barrier: structural access limitations followed by adherence failure even when access is achieved.

Extending Evidence

Source: VigiBase study, Clinical Nutrition 2025

Concurrent prescribing analysis shows OR 4.45 for suicidal ideation reports with antidepressants and OR 4.07 with benzodiazepines. The highest-risk patients are those with pre-existing psychiatric pharmacotherapy, creating a safety-persistence paradox: the patients most likely to discontinue (psychiatric comorbidity) are also those with highest adverse event reporting rates.

Extending Evidence

Source: MDPI Nutrients PMC12694361

Review identifies eating disorder history, perfectionism, OCD traits, and emotion regulation deficits as primary risk factors for GLP-1 adverse psychiatric outcomes. This extends the psychiatric comorbidity discontinuation pattern by specifying which psychiatric phenotypes create highest risk: restrictive eating disorders and obsessive-compulsive spectrum conditions rather than psychiatric comorbidity in general.