Acute schizophrenia is accompanied by reduced T cell and increased B cell immunity

Steiner, Johann; Jacobs, Roland; Panteli, Benjamin; Brauner, Mareike; Schiltz, Kolja; Bahn, Sabine; Herberth, Marlis; Westphal, Sabine; Gos, Tomasz; Walter, Martin; Bernstein, Hans‐Gert; Myint, Aye-Mu; Bogerts, Bernhard

doi:10.1007/s00406-010-0098-x

Cited by 104 publications

(64 citation statements)

References 54 publications

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“…Related to that, Steiner et al [2] describe in their well-designed paper that in acute paranoid schizophrenia, there might well be reduced T-cell defense and a shift toward B-cell immunity, which normalizes in the response to treatment. Importantly, they point out that in addition to the disease stage or subtype of the illness medication, cigarette smoking and stress are important co-factors.…”

Section: Dear Colleaguesmentioning

confidence: 99%

Biomarkers, population-based studies and a proof of principle investigation in pharmacotherapy

Falkai

Möller

2010

Eur Arch Psychiatry Clin Neurosci

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Section: Dear Colleaguesmentioning

confidence: 99%

Biomarkers, population-based studies and a proof of principle investigation in pharmacotherapy

Falkai

Möller

2010

Eur Arch Psychiatry Clin Neurosci

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“…This algorithm was trained to identify molecules associated with schizophrenia and then we were able to identify stable molecular differences in the patient populations. Through studies of first onset patients we have discovered that most patients with schizophrenia have differences in the levels of insulinrelated molecules 28 , other hormones of the diffuse neuroendocrine system 49 , inflammatory factors 5,50 and molecules associated with endothelial cell function 48 . It is anticipated that determination of which of these factors are altered in each subject will be useful for patient stratification prior to antipsychotic treatment.…”

Section: Table 2 Biomarker Tests Used In Other Indicationsmentioning

confidence: 99%

Testes sanguíneos de biomarcadores para diagnóstico e tratamento de desordens mentais: foco em esquizofrenia

Bahn¹,

Schwarz

Harris

et al. 2012

Arch. Clin. Psychiatry (São Paulo)

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A descoberta e a aplicação clínica de biomarcadores para desordens mentais são confrontadas com muitos desafios. Em geral, os atuais métodos de descoberta e validação de biomarcadores não produziram os resultados que foram inicialmente aguardados depois da finalização do Projeto Genoma Humano. Isso se deve principalmente à falta de processos padronizados conectando a descoberta de marcadores com tecnologias para a validação e a tradução para uma plataforma que ofereça precisão e fácil uso em clínica. Como consequência, a maior parte dos psiquiatras e praticantes em geral são relutantes em aceitar que testes de biomarcadores pode suplementar ou substituir os métodos de diagnóstico utilizados baseados em entrevista. Apesar disso, agências regulatórias concordam agora que melhoras nos correntes métodos são essenciais. Além disso, essas agências estipularam que biomarcadores são importantes para o desenvolvimento de futuras drogas e iniciaram esforços no sentido de modernizar métodos e técnicas para suportar esses esforços. Aqui revisamos os desafios encontrados por essa tentativa do ponto de vista de psiquiatras, praticantes em geral, agências reguladoras e cientistas de biomarcadores. Também descrevemos o desenvolvimento de um novo teste sanguíneo molecular para esquizofrenia como um primeiro passo a esse objetivo.

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“…Alterations in cytokine expression patterns 44 , such as increased levels of peripheral blood interleukin-1 receptor antagonist (IL-1RA), soluble interleukin-2 receptor (sIL-2R), and interleukin-6 (IL-6), as well as a shift from T-to B-cell-mediated immunity 45 have been observed. Moreover, several immune-related susceptibility genes for schizophrenia have been identified in the major histocompatibility complex (MHC) region of chromosome 6p21.3-22.1 46 .…”

Section: Potential Links Between S100b and The Pathogenesis Of Schizomentioning

confidence: 99%

Os possíveis papéis da S100B na esquizofrenia

Steiner

Bernstein

Bogerts

et al. 2012

Arch. Clin. Psychiatry (São Paulo)

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Background: Scientific evidence for increased S100B concentrations in the peripheral blood of acutely ill schizophrenia patients is consistent. In the past, this finding was mainly considered to reflect astroglial or blood-brain barrier dysfunction. Methods: Using Entrez, PubMed was searched for articles published on or before June 15, 2011, including electronic early release publications, in order to determine other potential links between S100B and current hypotheses for schizophrenia. Results: S100B is potentially associated with the dopamine and glutamate hypotheses. Supporting the glial hypothesis, an increased expression of S100B has been detected in cortical astrocytes of paranoid schizophrenia cases, while decreased oligodendrocytic expression has been observed in residual schizophrenia. Recently, the neuroinflammation hypothesis of schizophrenia has gained attention. S100B may act as a cytokine after secretion from glial cells, CD8+ lymphocytes and NK cells, activating monocytes and microglial cells. Moreover, S100B exhibits adipokine-like properties and may be dysregulated in schizophrenia due to disturbances in insulin signaling, leading to the increased release of S100B and free fatty acids from adipose tissue. Discussion: Dysregulation of pathways related to S100B appears to play a role in schizophrenia. However, S100B is expressed in different cell types and is involved in many regulatory processes. Currently, "the most important" mechanism related to schizophrenia cannot be determined.

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Acute schizophrenia is accompanied by reduced T cell and increased B cell immunity

Cited by 104 publications

References 54 publications

Biomarkers, population-based studies and a proof of principle investigation in pharmacotherapy

Biomarkers, population-based studies and a proof of principle investigation in pharmacotherapy

Testes sanguíneos de biomarcadores para diagnóstico e tratamento de desordens mentais: foco em esquizofrenia

Os possíveis papéis da S100B na esquizofrenia

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