--- type: source title: "GLP-1 Agonists Are Psychiatric Drugs. Psychiatry Should Start Acting Like It." author: "Dr. Will Sauvé, Dr. Annette Bosworth, Dr. Brittany Albright (Osmind)" url: https://www.osmind.org/blog/glp-1-psychiatry date: 2026-03-17 domain: health secondary_domains: [] format: article status: unprocessed priority: high tags: [glp-1, psychiatry, competency-gap, anhedonia, addiction, dosing] intake_tier: research-task --- ## Content Osmind CMO Dr. Will Sauvé, Dr. Annette Bosworth (internal medicine, developer of Dr. Boz Ratio metabolic monitoring protocol), and addiction psychiatrist Dr. Brittany Albright argue that GLP-1 receptor agonists are functionally psychiatric drugs — engaging VTA, nucleus accumbens, insula, and prefrontal cortex to directly regulate reward pathways and reinforcement learning. **Core argument:** GLP-1 receptors in these brain regions directly regulate reward pathways. These are psychiatric tools, not just metabolic agents. **Competency gap:** Dr. Sauvé (CMO, Osmind): "If our field of psychiatry does not get a hundred percent ahead of how this GLP thing works, then we're going to be left behind." Current problem: psychiatrists managing GLP-1-prescribed patients without understanding central mechanisms, dosing nuances, or psychiatric side effects — drugs prescribed by primary care. **Key clinical evidence cited:** - Hendershot trial (JAMA Psychiatry 2025): Semaglutide in 48 adults with AUD showed effect sizes exceeding naltrexone or acamprosate - Eli Lilly brenipatide Phase 3 trials (RENEW-ALC): 2,200 patients with moderate-to-severe AUD - All of Us observational (March 2026): GLP-1 exposure associated with 75% lower odds of any SUD **Monitoring recommendation (Dr. Bosworth "Dr. Boz Ratio"):** Track blood glucose ÷ blood ketones: >80 = glucose metabolism; 40-80 = moderate ketosis; <40 = deeper therapeutic ketosis. **Low-dose psychiatric protocol:** - Low-dose tirzepatide: 0.6mg weekly (one-quarter standard starting dose) - Paired with ketogenic diet - No emotional blunting reported in ~100 patients per cohort - Dr. Bosworth: structured resistance training + adequate protein (1.6–2.3g/kg/day) prevents lean mass loss **Anhedonia mechanism:** Tonic vs. phasic receptor activation. Natural GLP-1 half-life ~1-2 minutes (phasic). Long-acting GLP-1 agonists: days-long tonic activation → sustained dopaminergic suppression → anhedonia. Dosing strategy — not inherent pharmacology — determines anhedonic outcome. Parallel drawn to ziprasidone: 20mg produces one effect; 120mg the opposite. **Drug specificity:** Tirzepatide (GLP-1+GIP) vs. semaglutide (GLP-1 only) may have different neurochemical profiles because of GIP component. ## Agent Notes **Why this matters:** Single authoritative synthesis from a psychiatric platform (Osmind = psychiatric practice management + TMS/ketamine) arguing directly that GLP-1 is a psychiatric drug class. The competency gap framing and low-dose protocol recommendations are the most concrete clinical guidance for psychiatric prescribers available as of March 2026. **What surprised me:** The Bosworth metabolic ratio monitoring protocol (blood glucose ÷ ketones) is highly specific and operational — more concrete than anything from professional societies. Suggests clinical protocols are being developed in practice before guidelines exist. **What I expected but didn't find:** Specific prevalence data on anhedonia rates in clinical cohorts. The ~100 patient cohorts are real but anecdotal; no formal incidence figures. **KB connections:** - [[human-in-the-loop clinical AI degrades to worse-than-AI-alone]] — the competency gap is structurally similar: a clinical tool being used without the cognitive architecture to govern it safely - [[value-based care transitions stall at the payment boundary]] — Belief 3 parallel: primary care prescribing at weight-loss doses without psychiatric monitoring is a structural misalignment problem, not a knowledge problem - [[GLP-1 receptor agonists are the largest therapeutic category launch in pharmaceutical history]] **Extraction hints:** 1. Claim about prescribing competency gap and how it's being addressed (CME pathway vs formal guidelines) 2. Claim about low-dose tirzepatide psychiatric protocol (0.6mg weekly + ketogenic diet = no anhedonia) 3. The dosing = anhedonia relationship is a distinct claim from the tonic/phasic mechanism ## Curator Notes (structured handoff for extractor) PRIMARY CONNECTION: [[GLP-1 receptor agonists are the largest therapeutic category launch in pharmaceutical history but their chronic use model makes the net cost impact inflationary through 2035]] WHY ARCHIVED: Documents the emerging psychiatric prescribing context and competency gap — a Belief 3 (structural misalignment) instance where a powerful drug is being prescribed without the competency to govern its psychiatric effects EXTRACTION HINT: Focus on (1) the competency gap claim itself, (2) the monitoring protocol specifics, (3) the low-dose protocol — these are three distinct potential claims