Dopaminergic stimulation leads B-cell infiltration into the central nervous system upon autoimmunity

Prado, Carolina; Osorio‐Barrios, Francisco; Espinoza, Alexandra; Sáez, Juan José; Yuseff, María Isabel; Pacheco, Rodrigo

doi:10.21203/rs.3.rs-41605/v1

Cited by 1 publication

(2 citation statements)

References 49 publications

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“…These results suggest that TCRαβ + T-cells present in the colonic epithelium during the peak of EAE manifestation leave the gut mucosa to reach the CNS during the recovery stage of the disease (25 dpi). Since the chemokine receptor CXCR3 has been involved in lymphocyte in ltration into the CNS upon neuroin ammation [37][38][39][40][41][42], we determined the dynamics of the expression of this receptor on TCRαβ + T-cells obtained from the colonic epithelium and CNS during different stages of EAE development. Interestingly, we observed a signi cant increase of CXCR3 + TCRαβ + T-cells in the colonic epithelium at 15 dpi, followed by a substantial decrease at 25 dpi (Fig.…”

Section: T-cells In Ltrate the Colon Before Reaching The Cns Upon Eae...mentioning

confidence: 99%

“…7A). Since CXCL11-mediated stimulation of CXCR3 has been consistently involved in the lymphocyte in ltration into the CNS in mice and humans upon CNSautoimmunity [37][38][39][40][41][42], we next addressed the question of whether propionate-mediated GPR43 stimulation was able to affect the CXCL11-CXCR3 migration of IEL TCRαβ + T-cells. For this purpose, we treated IEL with or without propionate for 1 h and then placed them on the top chamber to determine the extent of TCRαβ + T-cells migration towards CXCL11 into the bottom transwell chamber.…”

Section: Gpr43 Stimulation Retains Tcrαβ T-cells In the Colonic Epith...mentioning

confidence: 99%

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GPR43 stimulation on TCRαβ+ intraepithelial colonic lymphocytes inhibits the recruitment of encephalitogenic T-cells into the central nervous system and attenuates the development of autoimmunity

Prado

Espinoza

Martínez-Hernández

et al. 2022

Preprint

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Introduction Gut microbiota plays a critical role in the regulation of immune homeostasis. Accordingly, several autoimmune disorders have been associated with dysbiosis in the gut microbiota. Notably, the dysbiosis associated with central nervous system (CNS) autoimmunity involves a substantial reduction of bacteria belonging to Clostridia clusters IV and XIVa, which constitute major producers of short-chain fatty acids (SCFA). Here we addressed the role of the surface receptor-mediated effects of SCFA on mucosal T-cells in the development of CNS autoimmunity. Methods To induce CNS autoimmunity we used the mouse model of experimental autoimmune encephalomyelitis (EAE) induced by immunization with the myelin oligodendrocyte glycoprotein (MOG)-derived peptide (MOG35 − 55 peptide). To address the effects of GPR43 stimulation on colonic TCRαβ+ T-cells upon CNS autoimmunity, mucosal lymphocytes were isolated and stimulated with a selective GPR43 agonist ex vivo and then transferred into congenic mice undergoing EAE. Several subsets of lymphocytes infiltrating the CNS or those present in the gut epithelium and gut lamina propria were analysed by flow cytometry. In vitro migration assays were conducted with mucosal T-cells using transwells. Results Our results show a sharp and selective reduction of intestinal propionate at the peak of EAE development, accompanied by increased IFN-γ and decreased IL-22 in the colonic mucosa. Further analyses indicated that GPR43 was the primary SCFA receptor expressed on T-cells, which was downregulated on colonic TCRαβ+ T-cells upon CNS autoimmunity. The pharmacologic stimulation of GPR43 increased the anti-inflammatory function and reduced the pro-inflammatory features in several TCRαβ+ T-cell subsets in the colonic mucosa upon EAE development. Furthermore, GPR43 stimulation induced the arrest of CNS-autoreactive T-cells in the colonic lamina propria, thus avoiding their infiltration into the CNS and dampening the disease development. Mechanistic analyses revealed that GPR43-stimulation on mucosal TCRαβ+ T-cells inhibits their CXCR3-mediated migration towards CXCL11, which is released from the CNS upon neuroinflammation. Conclusions These findings provide a novel mechanism involved in the gut-brain axis by which bacterial-derived products secreted in the gut mucosa might control the CNS tropism of autoreactive T-cells. Moreover, this study shows GPR43 expressed on T-cells as a promising therapeutic target for CNS autoimmunity.

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Section: T-cells In Ltrate the Colon Before Reaching The Cns Upon Eae...mentioning

confidence: 99%

Section: Gpr43 Stimulation Retains Tcrαβ T-cells In the Colonic Epith...mentioning

confidence: 99%

GPR43 stimulation on TCRαβ+ intraepithelial colonic lymphocytes inhibits the recruitment of encephalitogenic T-cells into the central nervous system and attenuates the development of autoimmunity

Prado

Espinoza

Martínez-Hernández

et al. 2022

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

Dopaminergic stimulation leads B-cell infiltration into the central nervous system upon autoimmunity

Cited by 1 publication

References 49 publications

GPR43 stimulation on TCRαβ+ intraepithelial colonic lymphocytes inhibits the recruitment of encephalitogenic T-cells into the central nervous system and attenuates the development of autoimmunity

GPR43 stimulation on TCRαβ+ intraepithelial colonic lymphocytes inhibits the recruitment of encephalitogenic T-cells into the central nervous system and attenuates the development of autoimmunity

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