Cytokine production by human thymic epithelial cells: control by the immune recognition of the neurohypophysial self-antigen

Martens, Henri; Malgrange, Brigitte; Robert, Françoise; Charlet, C.; Groote, Donat De; Heymann, Dominique; Godard, Alex; Soulillou, Jean‐Paul; Moonen, Gustave; Geenen, Vincent

doi:10.1016/s0167-0115(96)00105-x

Cited by 37 publications

(34 citation statements)

References 37 publications

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“…Our data confirm previous observations that TEC spontaneously produce cytokines in vitro (18,21) and that viruses can modulate the production of cytokines by TEC, without a virusinduced cytopathic effect (31). However, our study is different from those of other investigators, because we report a significantly increased production of IL-6, LIF, and GM-CSF by TEC in response to CVB4 and because CVB4 replication was investigated at the molecular level.…”

supporting

confidence: 92%

Persistent Infection of Human Thymic Epithelial Cells by Coxsackievirus B4

Brilot

Chehadeh

Charlet-Renard

et al. 2002

J Virol

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Persistent replication of coxsackievirus B4 (CVB4) E2 (diabetogenic) and CVB4 JBV (nondiabetogenic)strains in thymic epithelial cell (TEC)-enriched cultures (>95%) was proved by detection of positive-and negative-strand viral RNA by reverse transcription-PCR in extracted RNA from cell cultures, VP1 capsid protein detection by immunofluorescence (IF) staining, and release of infectious particles up to 30 days after infection without obvious cytolysis. By double-IF staining, cytokeratin-containing cells were shown to be susceptible to CVB4. The persistence of CVB4 was associated with a significantly increased rate of TEC proliferation (up to 70%) after 20 days of culture and a significantly increased chronic production of immunoreactive interleukin-6 (IL-6), leukemia inhibitory factor, and granulocyte-macrophage colony-stimulating factor in supernatant after 3 days of culture. The CVB4 replication and the release of cytokines were not restricted to the CVB4 E2 diabetogenic strain and did not depend on the genetic background of the host; however, TEC were more responsive to CVB4 E2 than CVB4 JBV as far as the production of cytokines.

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supporting

confidence: 92%

Persistent Infection of Human Thymic Epithelial Cells by Coxsackievirus B4

Brilot

Chehadeh

Charlet-Renard

et al. 2002

J Virol

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“…The cell feature, morphology, and overall distribution correspond to TEC. This is in accordance with our previous immunocytochemical studies showing that OT and VP are identified in human and murine TEC, including thymic nurse cells (TNC) (Geenen et al, 1988;Martens et al, 1996b;Robert et al, 1991). OT and VP transcription in the thymus is therefore coupled to mRNA translation and precursor processing.…”

Section: Discussionsupporting

confidence: 92%

“…As a source of hypothalamus-specific antigens, OT and VP are also expressed in TEC from different species, although with a dominance of OT at the peptide level. Thymic OT is not secreted but targeted to the outer surface of TEC plasma membrane where it is recognized by specific monoclonal antibodies (mAbs) (Martens et al, 1996b). Specific and functional receptors for these peptides are expressed by human thymocytes and a murine double negative (DN) CD4…”

Section: Introductionmentioning

confidence: 99%

Ontogenesis and functional aspects of oxytocin and vasopressin gene expression in the thymus network

Hansenne¹,

Rasier²,

Péqueux³

et al. 2005

Journal of Neuroimmunology

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Ontogenesis of oxytocin (OT) and vasopressin (VP) gene expression and function were investigated in murine thymus. OT and VP transcripts were detected in the thymus on embryonic days 13 and 15, respectively. Corresponding messenger RNAs were evidenced in thymic epithelial cells by in situ hybridization with a neurophysin probe. From all OT and VP receptors, only OTR was expressed by all Tcell subsets, while V1bR was found in double positive and single positive CD8 cells. In fetal thymic organ cultures, OTR antagonist d [dTyr(Et) 2 , Thr 4 ]OVT increased early apoptosis of CD8 cells, while V1bR antagonist (Sanofi SSR149415) inhibited T-cell differentiation, and favored CD8 T-cell commitment. D

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“…Self-tolerance is initiated in the thymus during T-cell ontogeny [Geenen and Kroemer, 1993;Martens et al, 1996;Geenen et al, 2001], a multi-step process which starts as soon as foetal life. The thymus fulfils this function by two complementary mechanisms: the deletion of T cells directed against self-antigens presented in the thymic cellular environment (thymic epithelial cells, macrophages and dendritic cells) by major histocompatiblity complex (MHC) proteins, and the generation of self-antigen specific regulatory T cells (T REG ).…”

Section: Introductionmentioning

confidence: 99%

Coxsackievirus B4 infection of murine foetal thymus organ cultures

Brilot

Jaïdane

Geenen

et al. 2008

Journal of Medical Virology

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The infection of foetal thymus with coxsackievirus B4 (CV-B4) E2 has been studied ex vivo by using CD-1 mice on foetal day 14, as a ready source of organs for experimentation to investigate the hypothesis of the role of thymic viral infections in the pathogenesis of type 1 diabetes. The replication of CV-B4 E2 in murine foetal thymus organ cultures has been demonstrated by evaluating the levels of positive-and negativestranded viral RNA in cells by using a real-time quantitative RT-PCR method and by determining titres of infectious viral particles in culture supernatants for 7 days post-infection (p.i.). Staining of tissue sections with an anti-cytokeratin antibody and haematoxylin-eosin showed that CV-B4 infection had no visible effect on cell survival and organ integrity. Cell counts in mock-and virus-infected foetal thymus organ cultures increased from day 1 through day 7, and live cell numbers were comparable in both conditions as shown by Trypan blue exclusion test and 7-amino-actinomycin D staining of thymocytes. Compared with controls on day 7 p.i., cytofluorometric analyses on cells from CV-B4 E2-infected foetal thymus organ cultures displayed a marked increase in the percentage of the most immature CD3 À CD4 À CD8 À thymocytes, and a decrease in the percentage of immature CD3 À CD4 þ CD8 þ cells, together with an increase in the percentage of mature CD3 þ CD4 þ and CD3 þ CD8 þ cells. These data show that CV-B4 E2 disturbs T-cell maturation and differentiation processes in infected murine foetal thymus organ cultures and provide evidence of a suitable system to investigate the effect of viruses in T-cell differentiation.

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Cytokine production by human thymic epithelial cells: control by the immune recognition of the neurohypophysial self-antigen

Cited by 37 publications

References 37 publications

Persistent Infection of Human Thymic Epithelial Cells by Coxsackievirus B4

Persistent Infection of Human Thymic Epithelial Cells by Coxsackievirus B4

Ontogenesis and functional aspects of oxytocin and vasopressin gene expression in the thymus network

Coxsackievirus B4 infection of murine foetal thymus organ cultures

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