Integrative Genomic–Epigenomic Analysis of Clozapine-Treated Patients with Refractory Psychosis

Author:

Mayén-Lobo Yerye Gibrán,Martínez-Magaña José JaimeORCID,Pérez-Aldana Blanca Estela,Ortega-Vázquez Alberto,Genis-Mendoza Alma Delia,Dávila-Ortiz de Montellano David JoséORCID,Soto-Reyes ErnestoORCID,Nicolini Humberto,López-López Marisol,Monroy-Jaramillo NancyORCID

Abstract

Clozapine (CLZ) is the only antipsychotic drug that has been proven to be effective in patients with refractory psychosis, but it has also been proposed as an effective mood stabilizer; however, the complex mechanisms of action of CLZ are not yet fully known. To find predictors of CLZ-associated phenotypes (i.e., the metabolic ratio, dosage, and response), we explore the genomic and epigenomic characteristics of 44 patients with refractory psychosis who receive CLZ treatment based on the integration of polygenic risk score (PRS) analyses in simultaneous methylome profiles. Surprisingly, the PRS for bipolar disorder (BD-PRS) was associated with the CLZ metabolic ratio (pseudo-R2 = 0.2080, adjusted p-value = 0.0189). To better explain our findings in a biological context, we assess the protein–protein interactions between gene products with high impact variants in the top enriched pathways and those exhibiting differentially methylated sites. The GABAergic synapse pathway was found to be enriched in BD-PRS and was associated with the CLZ metabolic ratio. Such interplay supports the use of CLZ as a mood stabilizer and not just as an antipsychotic. Future studies with larger sample sizes should be pursued to confirm the findings of this study.

Funder

Consejo Nacional de Ciencia y Tecnología

Publisher

MDPI AG

Subject

Drug Discovery,Pharmaceutical Science,Molecular Medicine

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