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T regulatory cells as a potential therapeutic target in psychosis? Current challenges and future perspectives

Many studies have reported that patients with psychosis, even before drug treatment, have mildly raised levels of blood cytokines relative to healthy controls. In contrast, there is a remarkable scarcity of studies investigating the cellular basis of immune function and cytokine changes in psychosis...

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Autores principales: Corsi-Zuelli, Fabiana, Deakin, Bill, de Lima, Mikhael Haruo Fernandes, Qureshi, Omar, Barnes, Nicholas M., Upthegrove, Rachel, Louzada-Junior, Paulo, Del-Ben, Cristina Marta
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Elsevier 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7611834/
https://www.ncbi.nlm.nih.gov/pubmed/34661175
http://dx.doi.org/10.1016/j.bbih.2021.100330
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author Corsi-Zuelli, Fabiana
Deakin, Bill
de Lima, Mikhael Haruo Fernandes
Qureshi, Omar
Barnes, Nicholas M.
Upthegrove, Rachel
Louzada-Junior, Paulo
Del-Ben, Cristina Marta
author_facet Corsi-Zuelli, Fabiana
Deakin, Bill
de Lima, Mikhael Haruo Fernandes
Qureshi, Omar
Barnes, Nicholas M.
Upthegrove, Rachel
Louzada-Junior, Paulo
Del-Ben, Cristina Marta
author_sort Corsi-Zuelli, Fabiana
collection PubMed
description Many studies have reported that patients with psychosis, even before drug treatment, have mildly raised levels of blood cytokines relative to healthy controls. In contrast, there is a remarkable scarcity of studies investigating the cellular basis of immune function and cytokine changes in psychosis. The few flow-cytometry studies have been limited to counting the proportion of the major classes of monocyte and lymphocytes without distinguishing their pro- and anti-inflammatory subsets. Moreover, most of the investigations are cross-sectional and conducted with patients on long-term medication. These features make it difficult to eliminate confounding of illness-related changes by lifestyle factors, disease duration, and long exposure to antipsychotics. This article focuses on regulatory T cells (Tregs), cornerstone immune cells that regulate innate and adaptive immune forces and neuroimmune interactions between astrocytes and microglia. Tregs are also implicated in cardio-metabolic disorders that are common comorbidities of psychosis. We have recently proposed that Tregs are hypofunctional (‘h-Tregs’) in psychosis driven by our clinical findings and other independent research. Our h-Treg-glial imbalance hypothesis offers a new account for the co-occurrence of systemic immune dysregulation and mechanisms of psychosis development. This article extends our recent review, the h-Treg hypothesis, to cover new discoveries on Treg-based therapies from pre-clinical findings and their clinical implications. We provide a detailed characterisation of Treg studies in psychosis, identifying important methodological limitations and perspectives for scientific innovation. The outcomes presented in this article reaffirms our proposed h-Treg state in psychosis and reveals emerging preclinical research suggesting the potential benefit of Treg-enhancing therapies. There is a clear need for longitudinal studies conducted with drug-naïve or minimally treated patients using more sophisticated techniques of flow-cytometry, CyTOF expression markers, and in vitro co-culture assays to formally test the suppressive capacity of Tregs. Investment in Treg research offers major potential benefits in targeting emerging immunomodulatory treatment modalities on person-specific immune dysregulations.
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spelling pubmed-76118342021-11-02 T regulatory cells as a potential therapeutic target in psychosis? Current challenges and future perspectives Corsi-Zuelli, Fabiana Deakin, Bill de Lima, Mikhael Haruo Fernandes Qureshi, Omar Barnes, Nicholas M. Upthegrove, Rachel Louzada-Junior, Paulo Del-Ben, Cristina Marta Brain Behav Immun Health Articles from the Special Issue on Emerging PNI research: future leaders in focus; Edited by Amanda Kentner, Lois Harden, Denis de Melo Soares and Christoph Rummel Many studies have reported that patients with psychosis, even before drug treatment, have mildly raised levels of blood cytokines relative to healthy controls. In contrast, there is a remarkable scarcity of studies investigating the cellular basis of immune function and cytokine changes in psychosis. The few flow-cytometry studies have been limited to counting the proportion of the major classes of monocyte and lymphocytes without distinguishing their pro- and anti-inflammatory subsets. Moreover, most of the investigations are cross-sectional and conducted with patients on long-term medication. These features make it difficult to eliminate confounding of illness-related changes by lifestyle factors, disease duration, and long exposure to antipsychotics. This article focuses on regulatory T cells (Tregs), cornerstone immune cells that regulate innate and adaptive immune forces and neuroimmune interactions between astrocytes and microglia. Tregs are also implicated in cardio-metabolic disorders that are common comorbidities of psychosis. We have recently proposed that Tregs are hypofunctional (‘h-Tregs’) in psychosis driven by our clinical findings and other independent research. Our h-Treg-glial imbalance hypothesis offers a new account for the co-occurrence of systemic immune dysregulation and mechanisms of psychosis development. This article extends our recent review, the h-Treg hypothesis, to cover new discoveries on Treg-based therapies from pre-clinical findings and their clinical implications. We provide a detailed characterisation of Treg studies in psychosis, identifying important methodological limitations and perspectives for scientific innovation. The outcomes presented in this article reaffirms our proposed h-Treg state in psychosis and reveals emerging preclinical research suggesting the potential benefit of Treg-enhancing therapies. There is a clear need for longitudinal studies conducted with drug-naïve or minimally treated patients using more sophisticated techniques of flow-cytometry, CyTOF expression markers, and in vitro co-culture assays to formally test the suppressive capacity of Tregs. Investment in Treg research offers major potential benefits in targeting emerging immunomodulatory treatment modalities on person-specific immune dysregulations. Elsevier 2021-08-19 /pmc/articles/PMC7611834/ /pubmed/34661175 http://dx.doi.org/10.1016/j.bbih.2021.100330 Text en © 2021 The Authors https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Articles from the Special Issue on Emerging PNI research: future leaders in focus; Edited by Amanda Kentner, Lois Harden, Denis de Melo Soares and Christoph Rummel
Corsi-Zuelli, Fabiana
Deakin, Bill
de Lima, Mikhael Haruo Fernandes
Qureshi, Omar
Barnes, Nicholas M.
Upthegrove, Rachel
Louzada-Junior, Paulo
Del-Ben, Cristina Marta
T regulatory cells as a potential therapeutic target in psychosis? Current challenges and future perspectives
title T regulatory cells as a potential therapeutic target in psychosis? Current challenges and future perspectives
title_full T regulatory cells as a potential therapeutic target in psychosis? Current challenges and future perspectives
title_fullStr T regulatory cells as a potential therapeutic target in psychosis? Current challenges and future perspectives
title_full_unstemmed T regulatory cells as a potential therapeutic target in psychosis? Current challenges and future perspectives
title_short T regulatory cells as a potential therapeutic target in psychosis? Current challenges and future perspectives
title_sort t regulatory cells as a potential therapeutic target in psychosis? current challenges and future perspectives
topic Articles from the Special Issue on Emerging PNI research: future leaders in focus; Edited by Amanda Kentner, Lois Harden, Denis de Melo Soares and Christoph Rummel
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7611834/
https://www.ncbi.nlm.nih.gov/pubmed/34661175
http://dx.doi.org/10.1016/j.bbih.2021.100330
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