The Contribution of CD40/CD40L Axis in Inflammatory Bowel Disease: An Update

Senhaji, Nezha; Kojok, Kevin; Darif, Youssef; Fadainia, C.; Zaid, Younes

doi:10.3389/fimmu.2015.00529

Cited by 70 publications

(57 citation statements)

References 47 publications

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“…As such, macrophage-associated genes downregulated in response to vedolizumab included the costimulatory molecule CD40,50 chemokines ( CXCL9 , CXCL11 , CXCL13 ), phospholipase A1 member A ( PLA1A1 ), which is increased in expression in CD and contributes to the production of proinflammatory lysophospholipids,51 signalling lymphocytic activation molecule (SLAM/ SLAMF1 ), which contributes to myeloid-derived inflammatory cytokine production,52 and proinflammatory chitinase 3-like-1 ( CHI3L1 ,53) (figure 7G). In contrast, we observed increased expression of ADAMDEC1 , a disintegrin and metalloproteinase (ADAM) family member that inhibits intestinal inflammation54 (figure 7G).…”

Section: Resultsmentioning

confidence: 99%

Vedolizumab is associated with changes in innate rather than adaptive immunity in patients with inflammatory bowel disease

Zeißig

Rosati

Dowds

et al. 2018

Gut

177

180

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ObjectiveVedolizumab, a monoclonal antibody directed against the integrin heterodimer α4β7, is approved for the treatment of Crohn’s disease and ulcerative colitis. The efficacy of vedolizumab has been suggested to result from inhibition of intestinal T cell trafficking although human data to support this conclusion are scarce. We therefore performed a comprehensive analysis of vedolizumab-induced alterations in mucosal and systemic immunity in patients with inflammatory bowel disease (IBD), using anti-inflammatory therapy with the TNFα antibody infliximab as control.DesignImmunophenotyping, immunohistochemistry, T cell receptor profiling and RNA sequencing were performed using blood and colonic biopsies from patients with IBD before and during treatment with vedolizumab (n=18) or, as control, the anti-TNFα antibody infliximab (n=20). Leucocyte trafficking in vivo was assessed using single photon emission computed tomography and endomicroscopy.ResultsVedolizumab was not associated with alterations in the abundance or phenotype of lamina propria T cells and did not affect the mucosal T cell repertoire or leucocyte trafficking in vivo. Surprisingly, however, α4β7 antibody treatment was associated with substantial effects on innate immunity including changes in macrophage populations and pronounced alterations in the expression of molecules involved in microbial sensing, chemoattraction and regulation of the innate effector response. These effects were specific to vedolizumab, not observed in response to the TNFα antibody infliximab, and associated with inhibition of intestinal inflammation.ConclusionOur findings suggest that modulation of innate immunity contributes to the therapeutic efficacy of vedolizumab in IBD.Trial registration numberNCT02694588

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Section: Resultsmentioning

confidence: 99%

Vedolizumab is associated with changes in innate rather than adaptive immunity in patients with inflammatory bowel disease

Zeißig

Rosati

Dowds

et al. 2018

Gut

177

180

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“…The CD154 ligand for CD40R is briefly synthesized on the membrane of activated CD4 + T cells and is also synthesized on immune cells involved in the development of autoimmunity (64, 65). Interactions between CD40R and its ligand CD154 results in movement of CD40R into cholesterol-rich membrane microdomains and the binding of TNFR-associated factors (TRAFs) to its cytoplasmic tail as recently described by Senhaji et al (66) and others (61, 67–71). The CD40R receptor was also shown to directly bind TRAF2, TRAF3, TRAF5, and TRAF6 and to indirectly associate with TRAF1 (61, 68, 72) (Figure 1).…”

Section: The Impact Of DC Costimulation On the Induction Of Iddmmentioning

confidence: 86%

The Role of Dendritic Cell Maturation in the Induction of Insulin-Dependent Diabetes Mellitus

et al. 2017

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Dendritic cells (DCs) are the dominant class of antigen-presenting cells in humans and are largely responsible for the initiation and guidance of innate and adaptive immune responses involved in maintenance of immunological homeostasis. Immature dendritic cells (iDCs) phagocytize pathogens and toxic proteins and in endosomal vesicles degrade them into small fragments for presentation on major histocompatibility complex (MHC) II receptor molecules to naïve cognate T cells (Th0). In addition to their role in stimulation of immunity, DCs are involved in the induction and maintenance of immune tolerance toward self-antigens. During activation, the iDCs become mature. Maturation begins when the DCs cease taking up antigens and begin to migrate from their location in peripheral tissues to adjacent lymph nodes or the spleen where during their continued maturation the DCs present stored antigens on surface MHCII receptor molecules to naive Th0 cells. During antigen presentation, the DCs upregulate the biosynthesis of costimulatory receptor molecules CD86, CD80, CD83, and CD40 on their plasma membrane. These activated DC receptor molecules bind cognate CD28 receptors presented on the Th0 cell membrane, which triggers DC secretion of IL-12 or IL-10 cytokines resulting in T cell differentiation into pro- or anti-inflammatory T cell subsets. Although basic concepts involved in the process of iDC activation and guidance of Th0 cell differentiation have been previously documented, they are poorly defined. In this review, we detail what is known about the process of DC maturation and its role in the induction of insulin-dependent diabetes mellitus autoimmunity.

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“…This crosstalk between hyperactive T cells, B cells and DCs, which is accentuated by CD40L overexpression, constitutes a vicious circle in SLE patients, and ultimately leads to disease flare and end-stage organ damage. Enhanced T cell receptor (TCR)-mediated Ca 2+ influx and CD40L expression have also been reported in IBD and contribute to the development of the disease [5, 15]. …”

Section: Introductionmentioning

confidence: 99%

Nanovesicle-targeted Kv1.3 knockdown in memory T cells suppresses CD40L expression and memory phenotype

Chimote

Hajdú

Kottyan

et al. 2016

Journal of Autoimmunity

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Ca2+ signaling controls activation and effector functions of T lymphocytes. Ca2+ levels also regulate NFAT activation and CD40 ligand (CD40L) expression in T cells. CD40L in activated memory T cells binds to its cognate receptor, CD40, on other cell types resulting in the production of antibodies and pro-inflammatory mediators. The CD40L/CD40 interaction is implicated in the pathogenesis of autoimmune disorders and CD40L is widely recognized as a therapeutic target. Ca2+ signaling in T cells is regulated by Kv1.3 channels. We have developed lipid nanoparticles that deliver Kv1.3 siRNAs (Kv1.3-NPs) selectively to CD45RO+ memory T cells and reduce the activation-induced Ca2+ influx. Herein we report that Kv1.3-NPs reduced NFAT activation and CD40L expression exclusively in CD45RO+ T cells. Furthermore, Kv1.3-NPs suppressed cytokine release and induced a phenotype switch of T cells from predominantly memory to naïve. These findings indicate that Kv1.3-NPs operate as targeted immune suppressive agents with promising therapeutic potentials.

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The Contribution of CD40/CD40L Axis in Inflammatory Bowel Disease: An Update

Cited by 70 publications

References 47 publications

Vedolizumab is associated with changes in innate rather than adaptive immunity in patients with inflammatory bowel disease

Vedolizumab is associated with changes in innate rather than adaptive immunity in patients with inflammatory bowel disease

The Role of Dendritic Cell Maturation in the Induction of Insulin-Dependent Diabetes Mellitus

Nanovesicle-targeted Kv1.3 knockdown in memory T cells suppresses CD40L expression and memory phenotype

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