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January 2026

PTSD

What January 2026's 5 new studies found, synthesized from the papers below. All PTSD research →

The synthesis

Synthesized from 5 studies in the library · AI-generated, grounded in the abstracts below

Found by searching the library for PTSD, post-traumatic stress disorder, traumatic stress, then ranked by relevance.

Research on PTSD in January 2026 found that a large randomized trial showed no overall benefit of ketamine over placebo, though DNA methylation patterns may predict which individuals respond. Naturalistic survey data indicate that difficult psychedelic experiences can lead to PTSD symptoms in a subset of users, and case reports suggest both potential adverse effects (e.g., new-onset OCD after MDMA-assisted therapy) and possible benefits of oral glutamatergic augmentation. Overall, findings are preliminary and based on small or single studies, with no large-scale definitive results.

Confidence in the evidence

Low
  • Only one large RCT (CAP-ketamine) found null overall results, but its subgroup analysis is exploratory.
  • The survey study on psychedelic-related PTSD is cross-sectional with convenience sampling, limiting causal inference.
  • Case reports (n=4 and n=1) provide very weak evidence for treatment effects or adverse outcomes.
  • The biomarker study (copeptin) is exploratory with a small transdiagnostic sample.
  • No meta-analyses or large-scale replication studies were provided.
How we rate confidence

Confidence reflects the strength of the underlying evidence, not whether the result is favorable. It weighs the number and size of studies, their design (randomized trials count for more than observational or single-case work), how consistently they point the same way, and their risk of bias.

Tiers run from Insufficient to High. High is rare in this field: small, early, or open-label studies land lower even when their direction is encouraging.

Evidence by study

Direction is each study's finding relative to your question: Supports, Opposes, No effect, Mixed, or Unclear.

Ketamine showed no overall benefit over placebo, but a DNA methylation-based model predicted treatment response with 92.9% accuracy.

RCT (subgroup analysis with machine learning)

Participants with MDE+PTSD had lower baseline copeptin levels and blunted post-ketamine copeptin reduction compared to MDE-only, but copeptin was unrelated to symptom severity.

observational

31.3% of participants met DSM-5 criteria for PTSD following a difficult psychedelic experience, with avoidance predicting greater symptoms.

observational (survey) Sample size: 243

All four patients showed clinically meaningful symptom improvement within days to weeks on an oral glutamatergic protocol.

case series Sample size: 4

A patient developed new-onset OCD following MDMA-assisted psychotherapy, with symptoms persisting over a year.

case report Sample size: 1

Points of agreement

  • Ketamine and related glutamatergic agents are being explored for PTSD, but efficacy may be limited to subgroups.
  • Psychedelic and MDMA-assisted therapies carry potential risks, including adverse psychiatric outcomes.
  • Biomarker and genetic approaches may help identify treatment responders.

Conflicts

  • The large CAP-ketamine trial found no overall benefit of ketamine, while a case series reported rapid improvement with an oral glutamatergic protocol.
  • MDMA-assisted therapy is reported as effective in reducing PTSD symptoms in one case, but also linked to new-onset OCD in another.

Gaps

  • No large-scale replication of DNA methylation prediction models for ketamine response.
  • Durability of treatment effects and long-term outcomes are not addressed.
  • Blinding and control conditions are lacking in survey and case studies.
  • Populations studied are heterogeneous; no standardized dosing or protocols.
  • Mechanisms linking psychedelic experiences to PTSD symptoms are not established.
Browse these studies in the library