Vasoactive intestinal peptide loss leads to impaired CNS parenchymal T-cell infiltration and resistance to experimental autoimmune encephalomyelitis

Abad, Catalina; Tan, Yossan‐Var; Lopez, Robert; Nobuta, Hiroko; Dong, Hongmei; Phu, Phan; Feng, Ji‐Ming; Campagnoni, Anthony T.; Waschek, James A.

doi:10.1073/pnas.1007622107

Cited by 47 publications

(46 citation statements)

References 42 publications

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“…The Vip Ϫ/Ϫ mouse exhibits a number of interesting phenotypes, including disturbances of circadian rhythm (27), impaired or enhanced inflammatory responses (37,38), and dysglycemia with abnormal sweet taste preference (39). Very little is known about the basal intestinal phenotype of Vip Ϫ/Ϫ mice; however, increased small bowel weight and smooth muscle thickening, together with increased villous length and reduced staining of mucus in the small bowel has been described in the Vip Ϫ/Ϫ mouse (36).…”

Section: Discussionmentioning

confidence: 99%

Intestinotrophic Glucagon-Like Peptide-2 (GLP-2) Activates Intestinal Gene Expression and Growth Factor-Dependent Pathways Independent of the Vasoactive Intestinal Peptide Gene in Mice

et al. 2012

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The enteroendocrine and enteric nervous systems convey signals through an overlapping network of regulatory peptides that act either as circulating hormones or as localized neurotransmitters within the gastrointestinal tract. Because recent studies invoke an important role for vasoactive intestinal peptide (VIP) as a downstream mediator of glucagon-like peptide-2 (GLP-2) action in the gut, we examined the importance of the VIP-GLP-2 interaction through analysis of Vip(-/-) mice. Unexpectedly, we detected abnormal villous architecture, expansion of the crypt compartment, increased crypt cell proliferation, enhanced Igf1 and Kgf gene expression, and reduced expression of Paneth cell products in the Vip(-/-) small bowel. These abnormalities were not reproduced by antagonizing VIP action in wild-type mice, and VIP administration did not reverse the intestinal phenotype of Vip(-/-) mice. Exogenous administration of GLP-2 induced the expression of ErbB ligands and immediate-early genes to similar levels in Vip(+/+) vs. Vip(-/-) mice. Moreover, GLP-2 significantly increased crypt cell proliferation and small bowel growth to comparable levels in Vip(+/+) vs. Vip(-/-) mice. Unexpectedly, exogenous GLP-2 administration had no therapeutic effect in mice with dextran sulfate-induced colitis; the severity of colonic injury and weight loss was modestly reduced in female but not male Vip(-/-) mice. Taken together, these findings extend our understanding of the complex intestinal phenotype arising from loss of the Vip gene. Furthermore, although VIP action may be important for the antiinflammatory actions of GLP-2, the Vip gene is not required for induction of a gene expression program linked to small bowel growth after enhancement of GLP-2 receptor signaling.

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Section: Discussionmentioning

confidence: 99%

Intestinotrophic Glucagon-Like Peptide-2 (GLP-2) Activates Intestinal Gene Expression and Growth Factor-Dependent Pathways Independent of the Vasoactive Intestinal Peptide Gene in Mice

et al. 2012

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“…However, in vivo data on the effects of VIP during inflammatory states are not consistent. In a model of EAE (Abad 2010), genetic deletion of VIP resulted in resistance to inflammation with mild or absent clinical signs and lack of CD4 cells infiltration into the brain parenchyma. In another study, VIP −/− mice exhibited resistance to LPS administration with decreased mortality, tissue damage, and pro-inflammatory cytokines (Abad 2012).…”

Section: Discussionmentioning

confidence: 99%

“…The entry of immune cells into mesenteric lymph nodes and Peyer’s patches is regulated by VPAC1 signaling (Von der Weid 2012). Furthermore, in a model of EAE in VIP −/− mice, T-cells and macrophages accumulated in the subarachnoid space but failed to enter the CNS parenchyma (Abad 2010); the levels of chemokine expression in the CNS were significantly lower in EAE-induced VIP −/− mice. Pharmacological inhibition of VIP in our model was effective in inducing resistance to colitis as that observed in VIP −/− mice.…”

Section: Discussionmentioning

confidence: 99%

Inhibition of Vasoactive Intestinal Polypeptide (VIP) Induces Resistance to Dextran Sodium Sulfate (DSS)-Induced Colitis in Mice

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et al. 2014

J Mol Neurosci

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VIP is highly expressed in the colon and regulates motility, vasodilatation, and sphincter relaxation. However, its role in the development and progress of colitis is still controversial. Our aim was to determine the participation of VIP on dextran sodium sulfate (DSS)-induced colonic mucosal inflammation using VIP−/− and WT mice treated with VIP antagonists. Colitis was induced in 32 adult VIP−/− and 14 age-matched WT litter-mates by giving 2.5 % DSS in the drinking water. DSS-treated WT mice were injected daily with VIP antagonists, VIPHyb (n=22), PG 97–269 (n=9), or vehicle (n=31). After euthanasia, colons were examined; colonic cytokines mRNA were quantified. VIP−/− mice were remarkably resistant to DSS-induced colitis compared to WT. Similarly, DSS-treated WT mice injected with VIPHyb (1 μM) or PG 97–269 (1 nM) had significantly reduced clinical signs of colitis. Furthermore, colonic expression of IL-1, TNF-α, and IL-6 was significantly lower in VIP−/− and VIPHyb or PG 97–269 compared to vehicle-treated WT. Genetic deletion of VIP or pharmacological inhibition of VIP receptors resulted in resistance to colitis. These data demonstrate a pro-inflammatory role for VIP in murine colitis and suggest that VIP antagonists may be an effective clinical treatment for human inflammatory bowel diseases.

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“…PACAP-KO mice show higher incidence and severity of experimental autoimmune encephalomyelitis (EAE), increased inflammatory and Th1-encephalitogenic cells, and decreased antigen-specific Treg cells [87]. Interestingly, the response of VIP-KO mice to EAE results in a delayed onset and mild clinical profile [88]. Although VIP-KO mice exhibited robust Th1/Th17 cell inductions and cytokine responses, showing their increased EAE profile, VIP loss seemed to be involved in the immune infiltration of the nervous parenchyma.…”

Section: Functional Neuropeptide Network Is Crucial For Maintaining Amentioning

confidence: 99%

Neuropeptides as Pleiotropic Modulators of the Immune Response

et al. 2011

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Although necessary to eliminate pathogens, inflammation can lead to serious deleterious effects in the host if left unchecked. During the inflammatory response, further damage may arise from potential autoimmune responses occurring when the immune cells and molecules that respond to pathogen-derived antigens also react to self-antigens. In this sense, the identification of endogenous factors that control exacerbated immune responses is a key goal for the development of new therapeutic approaches for inflammatory and autoimmune diseases. Some neuropeptides that are produced during the ongoing inflammatory response have emerged as endogenous anti-inflammatory agents that could collaborate in tuning the balanced steady state of the immune system. These neuropeptides participate in maintaining immune tolerance through two distinct mechanisms: by regulating the balance between pro-inflammatory and anti-inflammatory factors, and by inducing the emergence of regulatory T cells with suppressive activity against autoreactive T cell effectors. Indeed, a functioning neuropeptide system contributes to general health, and alterations in the levels of these neuropeptides and/or their receptors lead to changes in susceptibility to inflammatory and autoimmune diseases. Recently, we found that some neuropeptides also have antimicrobial and antiparasitic actions, suggesting that they could act as primary mediators of innate defense, even in the most primitive organisms. In this review, we use the vasoactive intestinal peptide as example of an immunomodulatory neuropeptide to summarize the most relevant data found for other neuropeptides with similar characteristics, including adrenomedullin, urocortin, cortistatin and ghrelin.

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Vasoactive intestinal peptide loss leads to impaired CNS parenchymal T-cell infiltration and resistance to experimental autoimmune encephalomyelitis

Cited by 47 publications

References 42 publications

Intestinotrophic Glucagon-Like Peptide-2 (GLP-2) Activates Intestinal Gene Expression and Growth Factor-Dependent Pathways Independent of the Vasoactive Intestinal Peptide Gene in Mice

Intestinotrophic Glucagon-Like Peptide-2 (GLP-2) Activates Intestinal Gene Expression and Growth Factor-Dependent Pathways Independent of the Vasoactive Intestinal Peptide Gene in Mice

Inhibition of Vasoactive Intestinal Polypeptide (VIP) Induces Resistance to Dextran Sodium Sulfate (DSS)-Induced Colitis in Mice

Neuropeptides as Pleiotropic Modulators of the Immune Response

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