Novel Insights into Psychosis and Antipsychotic Interventions: From Managing Symptoms to Improving Outcomes

Author:

Sfera Adonis123ORCID,Imran Hassan123,Sfera Dan O.123,Anton Jacob J.4,Kozlakidis Zisis5ORCID,Hazan Sabine6

Affiliation:

1. Patton State Hospital, 3102 Highland Ave., Patton, CA 92369, USA

2. University of California Riverside, Riverside 900 University Ave., Riverside, CA 92521, USA

3. Loma Linda University, 11139 Anderson St., Loma Linda, CA 92350, USA

4. California Baptist University, Riverside, CA 92521, USA

5. International Agency for Research on Cancer, 69372 Lyon, France

6. ProgenaBiome, Ventura, CA 93003, USA

Abstract

For the past 70 years, the dopamine hypothesis has been the key working model in schizophrenia. This has contributed to the development of numerous inhibitors of dopaminergic signaling and antipsychotic drugs, which led to rapid symptom resolution but only marginal outcome improvement. Over the past decades, there has been limited research on the quantifiable pathological changes in schizophrenia, including premature cellular/neuronal senescence, brain volume loss, the attenuation of gamma oscillations in electroencephalograms, and the oxidation of lipids in the plasma and mitochondrial membranes. We surmise that the aberrant activation of the aryl hydrocarbon receptor by toxins derived from gut microbes or the environment drives premature cellular and neuronal senescence, a hallmark of schizophrenia. Early brain aging promotes secondary changes, including the impairment and loss of mitochondria, gray matter depletion, decreased gamma oscillations, and a compensatory metabolic shift to lactate and lactylation. The aim of this narrative review is twofold: (1) to summarize what is known about premature cellular/neuronal senescence in schizophrenia or schizophrenia-like disorders, and (2) to discuss novel strategies for improving long-term outcomes in severe mental illness with natural senotherapeutics, membrane lipid replacement, mitochondrial transplantation, microbial phenazines, novel antioxidant phenothiazines, inhibitors of glycogen synthase kinase-3 beta, and aryl hydrocarbon receptor antagonists.

Publisher

MDPI AG

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