CCR5 deficiency impairs CD4+ T-cell memory responses and antigenic sensitivity through increased ceramide synthesis

Ana Martín-Leal; Raquel Blanco; Josefina Casas; María E. Sáez; Elena Rodríguez-Bovolenta; Itziar de Rojas; Carina Drechsler; Luis Miguel Real; Gemma Fabrias; Agustín Ruíz; Mario Castro; Wolfgang W.A. Schamel; Balbino Alarcón; Hisse M. van Santen; Santos Mañes

doi:10.15252/embj.2020104749

CCR5 deficiency impairs CD4⁺ T-cell memory responses and antigenic sensitivity through increased ceramide synthesis

Ana Martín-Leal, Raquel Blanco, Josefina Casas, María E. Sáez, Elena Rodríguez-Bovolenta, Itziar de Rojas, Carina Drechsler, Luis Miguel Real, Gemma Fabrias, Agustín Ruíz, Mario Castro, Wolfgang W.A. Schamel, Balbino Alarcón, Hisse M. van Santen, Santos Mañes

Producción científica: Article › revisión exhaustiva

21 Citas (Scopus)

Resumen

CCR5 is not only a coreceptor for HIV-1 infection in CD4⁺ T cells, but also contributes to their functional fitness. Here, we show that by limiting transcription of specific ceramide synthases, CCR5 signaling reduces ceramide levels and thereby increases T-cell antigen receptor (TCR) nanoclustering in antigen-experienced mouse and human CD4⁺ T cells. This activity is CCR5-specific and independent of CCR5 co-stimulatory activity. CCR5-deficient mice showed reduced production of high-affinity class-switched antibodies, but only after antigen rechallenge, which implies an impaired memory CD4⁺ T-cell response. This study identifies a CCR5 function in the generation of CD4⁺ T-cell memory responses and establishes an antigen-independent mechanism that regulates TCR nanoclustering by altering specific lipid species.

Idioma original	English (US)
Número de artículo	e104749
Publicación	EMBO Journal
Volumen	39
N.º	15
DOI	https://doi.org/10.15252/embj.2020104749
Estado	Published - ago 3 2020
Publicado de forma externa	Sí

ASJC Scopus subject areas

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

Acceder al documento

10.15252/embj.2020104749

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Martín-Leal, A., Blanco, R., Casas, J., Sáez, M. E., Rodríguez-Bovolenta, E., de Rojas, I., Drechsler, C., Real, L. M., Fabrias, G., Ruíz, A., Castro, M., Schamel, W. W. A., Alarcón, B., van Santen, H. M., & Mañes, S. (2020). CCR5 deficiency impairs CD4⁺ T-cell memory responses and antigenic sensitivity through increased ceramide synthesis. EMBO Journal, 39(15), Artículo e104749. https://doi.org/10.15252/embj.2020104749

Martín-Leal, A, Blanco, R, Casas, J, Sáez, ME, Rodríguez-Bovolenta, E, de Rojas, I, Drechsler, C, Real, LM, Fabrias, G, Ruíz, A, Castro, M, Schamel, WWA, Alarcón, B, van Santen, HM & Mañes, S 2020, 'CCR5 deficiency impairs CD4⁺ T-cell memory responses and antigenic sensitivity through increased ceramide synthesis', EMBO Journal, vol. 39, n.º 15, e104749. https://doi.org/10.15252/embj.2020104749

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title = "CCR5 deficiency impairs CD4+ T-cell memory responses and antigenic sensitivity through increased ceramide synthesis",

abstract = "CCR5 is not only a coreceptor for HIV-1 infection in CD4+ T cells, but also contributes to their functional fitness. Here, we show that by limiting transcription of specific ceramide synthases, CCR5 signaling reduces ceramide levels and thereby increases T-cell antigen receptor (TCR) nanoclustering in antigen-experienced mouse and human CD4+ T cells. This activity is CCR5-specific and independent of CCR5 co-stimulatory activity. CCR5-deficient mice showed reduced production of high-affinity class-switched antibodies, but only after antigen rechallenge, which implies an impaired memory CD4+ T-cell response. This study identifies a CCR5 function in the generation of CD4+ T-cell memory responses and establishes an antigen-independent mechanism that regulates TCR nanoclustering by altering specific lipid species.",

keywords = "ccr5[delta]32, humoral response, membrane phase, sphingolipid, T-cell receptor",

author = "Ana Mart{\'i}n-Leal and Raquel Blanco and Josefina Casas and S{\'a}ez, \{Mar{\'i}a E.\} and Elena Rodr{\'i}guez-Bovolenta and \{de Rojas\}, Itziar and Carina Drechsler and Real, \{Luis Miguel\} and Gemma Fabrias and Agust{\'i}n Ru{\'i}z and Mario Castro and Schamel, \{Wolfgang W.A.\} and Balbino Alarc{\'o}n and \{van Santen\}, \{Hisse M.\} and Santos Ma{\~n}es",

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doi = "10.15252/embj.2020104749",

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T1 - CCR5 deficiency impairs CD4+ T-cell memory responses and antigenic sensitivity through increased ceramide synthesis

AU - Martín-Leal, Ana

AU - Blanco, Raquel

AU - Casas, Josefina

AU - Sáez, María E.

AU - Rodríguez-Bovolenta, Elena

AU - de Rojas, Itziar

AU - Drechsler, Carina

AU - Real, Luis Miguel

AU - Fabrias, Gemma

AU - Ruíz, Agustín

AU - Castro, Mario

AU - Schamel, Wolfgang W.A.

AU - Alarcón, Balbino

AU - van Santen, Hisse M.

AU - Mañes, Santos

PY - 2020/8/3

Y1 - 2020/8/3

N2 - CCR5 is not only a coreceptor for HIV-1 infection in CD4+ T cells, but also contributes to their functional fitness. Here, we show that by limiting transcription of specific ceramide synthases, CCR5 signaling reduces ceramide levels and thereby increases T-cell antigen receptor (TCR) nanoclustering in antigen-experienced mouse and human CD4+ T cells. This activity is CCR5-specific and independent of CCR5 co-stimulatory activity. CCR5-deficient mice showed reduced production of high-affinity class-switched antibodies, but only after antigen rechallenge, which implies an impaired memory CD4+ T-cell response. This study identifies a CCR5 function in the generation of CD4+ T-cell memory responses and establishes an antigen-independent mechanism that regulates TCR nanoclustering by altering specific lipid species.

AB - CCR5 is not only a coreceptor for HIV-1 infection in CD4+ T cells, but also contributes to their functional fitness. Here, we show that by limiting transcription of specific ceramide synthases, CCR5 signaling reduces ceramide levels and thereby increases T-cell antigen receptor (TCR) nanoclustering in antigen-experienced mouse and human CD4+ T cells. This activity is CCR5-specific and independent of CCR5 co-stimulatory activity. CCR5-deficient mice showed reduced production of high-affinity class-switched antibodies, but only after antigen rechallenge, which implies an impaired memory CD4+ T-cell response. This study identifies a CCR5 function in the generation of CD4+ T-cell memory responses and establishes an antigen-independent mechanism that regulates TCR nanoclustering by altering specific lipid species.

KW - ccr5[delta]32

KW - humoral response

KW - membrane phase

KW - sphingolipid

KW - T-cell receptor

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