Mapping brain-behavior space relationships along the psychosis spectrum

Author:

Ji Jie Lisa12ORCID,Helmer Markus1ORCID,Fonteneau Clara1,Burt Joshua B3,Tamayo Zailyn1,Demšar Jure45,Adkinson Brendan D12ORCID,Savić Aleksandar6,Preller Katrin H7ORCID,Moujaes Flora7,Vollenweider Franz X7ORCID,Martin William J8ORCID,Repovš Grega6,Murray John D129ORCID,Anticevic Alan1210ORCID

Affiliation:

1. Department of Psychiatry, Yale University School of Medicine, New Haven, United States

2. Interdepartmental Neuroscience Program, Yale University School of Medicine, New Haven, United States

3. RBNC Therapeutics, San Francisco, United States

4. Department of Psychology, University of Ljubljana, Ljubljana, Slovenia

5. Faculty of Computer and Information Science, University of Ljubljana, Ljubljana, Slovenia

6. Department of Psychiatry, University of Zagreb, Zagreb, Croatia

7. Department of Psychiatry, Psychotherapy and Psychosomatics, University Hospital for Psychiatry Zurich, Zurich, Switzerland

8. The Janssen Pharmaceutical Companies of Johnson and Johnson, San Francisco, United States

9. Department of Physics, Yale University, New Haven, United States

10. Department of Psychology, Yale University School of Medicine, New Haven, United States

Abstract

Difficulties in advancing effective patient-specific therapies for psychiatric disorders highlight a need to develop a stable neurobiologically grounded mapping between neural and symptom variation. This gap is particularly acute for psychosis-spectrum disorders (PSD). Here, in a sample of 436 PSD patients spanning several diagnoses, we derived and replicated a dimensionality-reduced symptom space across hallmark psychopathology symptoms and cognitive deficits. In turn, these symptom axes mapped onto distinct, reproducible brain maps. Critically, we found that multivariate brain-behavior mapping techniques (e.g. canonical correlation analysis) do not produce stable results with current sample sizes. However, we show that a univariate brain-behavioral space (BBS) can resolve stable individualized prediction. Finally, we show a proof-of-principle framework for relating personalized BBS metrics with molecular targets via serotonin and glutamate receptor manipulations and neural gene expression maps derived from the Allen Human Brain Atlas. Collectively, these results highlight a stable and data-driven BBS mapping across PSD, which offers an actionable path that can be iteratively optimized for personalized clinical biomarker endpoints.

Funder

Heffter Research Institute

Swiss Neuromatrix Foundation

Swiss National Science Foundation

Slovenian Research Agency

National Institutes of Health

Simons Foundation

Publisher

eLife Sciences Publications, Ltd

Subject

General Immunology and Microbiology,General Biochemistry, Genetics and Molecular Biology,General Medicine,General Neuroscience

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