LIGHT, a new TNF superfamily member, is essential for memory T helper cell‐mediated activation of dendritic cells

Morel, Yannis; Truneh, Alemseged; Costello, Régis T.; Olive, Daniel

doi:10.1002/eji.200324410

Cited by 19 publications

(18 citation statements)

References 29 publications

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“…1C, 2C, and 7), suggesting that LIGHT expression is regulated at the transcriptional level. Alternatively, intracellular stores of LIGHT have been reported (43), proposing a presynthesized protein pool that can be rapidly transported to the cell surface. Our data indicate that LIGHT induction is actinomycin D and CHX sensitive (Fig.…”

Section: Cd4mentioning

confidence: 99%

“…Furthermore, full-length LIGHT mRNA was not detected in unstimulated T cells (Figs. 5C and 6C), but a variant form of LIGHT has been described that lacks the transmembrane domain and cannot be displayed on the cell surface (29), most likely accounting for intracellular LIGHT detected in resting PB T cells (43). However, a more precise real-time protein-trafficking analysis will be required to exclude intracellular stores of LIGHT as a mechanism for rapid induction and to establish whether signaling activity may be terminated by shedding LIGHT (29).…”

Section: Cd4mentioning

confidence: 99%

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LIGHT Is Constitutively Expressed on T and NK Cells in the Human Gut and Can Be Induced by CD2-Mediated Signaling

Cohavy

Zhou

Ware

et al. 2005

The Journal of Immunology

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The TNF superfamily cytokine, lymphotoxin-like inducible protein that competes with glycoprotein D for binding herpesvirus entry mediator on T cells (LIGHT; TNFSF14), can augment T cell responses inducing IFN-γ production and can drive pathological gut inflammation when expressed as a transgene in mouse T cells. LIGHT expression by human intestinal T cells suggests the possibility that LIGHT may play a key role in regulation of the mucosal immune system. A nonenzymatic method was developed for the isolation of T cells from the human lamina propria, permitting analysis of native cell surface protein expression. Cell surface LIGHT was constitutively expressed on mucosal T and NK cells and a subpopulation of gut-homing CD4+ T cells in the periphery. In addition, CD2-mediated stimulation induced efficient LIGHT expression on intestinal CD4+ T cells, but not on peripheral blood T cells, suggesting a gut-specific, Ag-independent mechanism for LIGHT induction. By contrast, herpesvirus entry mediator expression on gut T cells was unperturbed, implicating the transcriptional regulation of LIGHT as a mechanism modulating signaling activity in the gut. Quantitative analysis of LIGHT mRNA in a cohort of inflammatory bowel disease patients indicated elevated expression in biopsies from small bowel and from inflamed sites, implicating LIGHT as a mediator of mucosal inflammation.

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Section: Cd4mentioning

confidence: 99%

Section: Cd4mentioning

confidence: 99%

LIGHT Is Constitutively Expressed on T and NK Cells in the Human Gut and Can Be Induced by CD2-Mediated Signaling

Cohavy

Zhou

Ware

et al. 2005

The Journal of Immunology

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“…CD40L/CD154, CD134 and CD70. Nonetheless, the TNFR/TNF family has more than 20 members, and our studies [1][2][3] have particularly focused our attention on the herpes virus entry mediator (HVEM) and its ligand LIGHT (homologous to lymphotoxin, inducible expression, competing for GpD of herpes virus, that binds to the HVEM, and is expressed on activated T lymphocytes). The HVEM molecule has a broad expression in hematopoietic cells, i.e.…”

Section: Introductionmentioning

confidence: 99%

LIGHT costimulates CD40 triggering and induces immunoglobulin secretion; a novel key partner in T cell‐dependent B cell terminal differentiation

et al. 2004

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The T cell-dependent differentiation and function of B lymphocytes are tightly regulated by TNF ligands (L) and receptors interactions, such as CD40/CD40L, CD27/CD70 and CD134/ CD314L. The LIGHT/HVEM system [homologous to lymphotoxin, inducible expression, competing for GpD of herpes virus, that binds to the herpes virus entry mediator (HVEM), and is expressed on activated T lymphocytes) focused our attention since HVEM has a large distribution that, in addition to T cells, DC or NK, includes tumor and normal B lymphocytes. HVEM was expressed on memory and naive B cells from peripheral blood or tonsils, but not on germinal center (GC) B cells. Costimulation by CD40L+LIGHT induced LIGHT expression at the B lymphocyte surface by a transcriptional mechanism since we detected de novo expression of LIGHT-specific mRNA. LIGHTexpression was further enhanced by triggering of surface IgM, a stimulus that mimics a normal step of B cell physiology, i.e. specific antigen encounter. Stimulation by LIGHT increased the B cell proliferation induced by CD40L, and induced IgG and IgM (but not IgA) secretion. We conclude that LIGHT costimulation, that mimics the B cell encounter with activated LIGHT-expressing T lymphocytes, enhances both B cell proliferation and Ig production, and thus has a central importance for humoral immunity development.

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“…O aumento da população de dendróci-tos dérmicos Fator XIIIa+, observado após o tratamento com a PTX, poderia ser explicado, então, pela manutenção do estímulo tecidual para sinalização e migração de precursores de células dendríticas, uma vez que os processos etiopatogenéticos não seriam afetados pela droga. 24,[33][34][35][36][37][38][39][40] O questionamento sobre o aumento do núme-ro de mastócitos e sua degranulação na placa psoriá-sica após o tratamento, sem a repercussão clínica de prurido e histaminemia, ainda está para ser respondido. Seriam os mecanismos fisioimunopatogênicos da degranulação causada pela imunomodulação diferentes daquele que ocorre na reação de hipersensibilidade do tipo I?…”

Section: Discussionunclassified

Ação da pentoxifilina nos dendrócitos dérmicos FXIIIa de placas de psoríase

Carneiro

Medeiros²,

Magalhães³

et al. 2005

An. Bras. Dermatol.

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FUNDAMENTOS: Não há consenso sobre o papel dos dendrócitos dérmicos (DD) nos eventos fisiopatológicos nos períodos de exacerbação e de acalmia da doença. A pentoxifilina (PTX) é uma metilxantina que inibe vários mecanismos inflamatórios. OBJETIVO: Estudar os efeitos da PTX sobre os dendróticos dérmicos de placas de psoríase com técnicas imuno-histoquímicas. MATERIAL E MÉTODOS: Trinta biópsias de placas de psoríase antes e após oito semanas de uso oral diário de 1.200mg de PTX foram incubadas com anticorpo primário de coelho antiFator XIIIa e anticorpo de ligação conjugado com fosfatase alcalina. RESULTADOS: As células imunomarcadas Fator XIIIa+ foram proeminentes com morfologia dendrítica arborescente na derme papilar formando linha celular logo abaixo da epiderme e exibindo arranjo nodular ao redor dos vasos. Após tratamento, as células apresentaram-se com morfologia dendrítica e fusiforme, distribuídas ao redor dos vasos da derme papilar e predominantemente fusiformes dispostas paralelamente à junção dermoepidérmica retificada. CONCLUSÕES: A PTX promove aumento do fluxo sangüíneo e diminuição da adesividade endotelial, com aumento dos mastócitos e DD FXIIIa. A PTX inibe o TNF-alfa, que implica a diminuição da expressão de receptores pelos DDs, como CCR7 e a manutenção do estímulo tecidual para sinalização e migração dos precursores, uma vez que os processos etiopatogenéticos não são afetados pela droga.

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LIGHT, a new TNF superfamily member, is essential for memory T helper cell‐mediated activation of dendritic cells

Cited by 19 publications

References 29 publications

LIGHT Is Constitutively Expressed on T and NK Cells in the Human Gut and Can Be Induced by CD2-Mediated Signaling

LIGHT Is Constitutively Expressed on T and NK Cells in the Human Gut and Can Be Induced by CD2-Mediated Signaling

LIGHT costimulates CD40 triggering and induces immunoglobulin secretion; a novel key partner in T cell‐dependent B cell terminal differentiation

Ação da pentoxifilina nos dendrócitos dérmicos FXIIIa de placas de psoríase

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