Gut-associated IgA+ immune cells regulate obesity-related insulin resistance

Helen Luck; Saad Khan; Justin H. Kim; Julia K. Copeland; Xavier S. Revelo; Sue Tsai; Mainak Chakraborty; Kathleen Cheng; Yi Tao Chan; Mark K. Nøhr; Xavier Clemente-Casares; Marie Christine Perry; Magar Ghazarian; Helena Lei; Yi Hsuan Lin; Bryan Coburn; Allan Okrainec; Timothy Jackson; Susan Poutanen; Herbert Gaisano; Johane P. Allard; David S. Guttman; Margaret E. Conner; Shawn Winer; Daniel A. Winer

doi:10.1038/s41467-019-11370-y

Gut-associated IgA⁺ immune cells regulate obesity-related insulin resistance

Helen Luck, Saad Khan, Justin H. Kim, Julia K. Copeland, Xavier S. Revelo, Sue Tsai, Mainak Chakraborty, Kathleen Cheng, Yi Tao Chan, Mark K. Nøhr, Xavier Clemente-Casares, Marie Christine Perry, Magar Ghazarian, Helena Lei, Yi Hsuan Lin, Bryan Coburn, Allan Okrainec, Timothy Jackson, Susan Poutanen, Herbert GaisanoJohane P. Allard, David S. Guttman, Margaret E. Conner, Shawn Winer, Daniel A. Winer

Physiology

Research output: Contribution to journal › Article › peer-review

121 Scopus citations

Abstract

The intestinal immune system is emerging as an important contributor to obesity-related insulin resistance, but the role of intestinal B cells in this context is unclear. Here, we show that high fat diet (HFD) feeding alters intestinal IgA⁺ immune cells and that IgA is a critical immune regulator of glucose homeostasis. Obese mice have fewer IgA⁺ immune cells and less secretory IgA and IgA-promoting immune mediators. HFD-fed IgA-deficient mice have dysfunctional glucose metabolism, a phenotype that can be recapitulated by adoptive transfer of intestinal-associated pan-B cells. Mechanistically, IgA is a crucial link that controls intestinal and adipose tissue inflammation, intestinal permeability, microbial encroachment and the composition of the intestinal microbiome during HFD. Current glucose-lowering therapies, including metformin, affect intestinal-related IgA⁺ B cell populations in mice, while bariatric surgery regimen alters the level of fecal secretory IgA in humans. These findings identify intestinal IgA⁺ immune cells as mucosal mediators of whole-body glucose regulation in diet-induced metabolic disease.

Original language	English (US)
Article number	3650
Journal	Nature communications
Volume	10
Issue number	1
DOIs	https://doi.org/10.1038/s41467-019-11370-y
State	Published - Dec 1 2019

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Publisher Copyright:
© 2019, The Author(s).

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Luck, H., Khan, S., Kim, J. H., Copeland, J. K., Revelo, X. S., Tsai, S., Chakraborty, M., Cheng, K., Tao Chan, Y., Nøhr, M. K., Clemente-Casares, X., Perry, M. C., Ghazarian, M., Lei, H., Lin, Y. H., Coburn, B., Okrainec, A., Jackson, T., Poutanen, S., ... Winer, D. A. (2019). Gut-associated IgA⁺ immune cells regulate obesity-related insulin resistance. Nature communications, 10(1), Article 3650. https://doi.org/10.1038/s41467-019-11370-y

Luck, H, Khan, S, Kim, JH, Copeland, JK, Revelo, XS, Tsai, S, Chakraborty, M, Cheng, K, Tao Chan, Y, Nøhr, MK, Clemente-Casares, X, Perry, MC, Ghazarian, M, Lei, H, Lin, YH, Coburn, B, Okrainec, A, Jackson, T, Poutanen, S, Gaisano, H, Allard, JP, Guttman, DS, Conner, ME, Winer, S & Winer, DA 2019, 'Gut-associated IgA⁺ immune cells regulate obesity-related insulin resistance', Nature communications, vol. 10, no. 1, 3650. https://doi.org/10.1038/s41467-019-11370-y

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abstract = "The intestinal immune system is emerging as an important contributor to obesity-related insulin resistance, but the role of intestinal B cells in this context is unclear. Here, we show that high fat diet (HFD) feeding alters intestinal IgA+ immune cells and that IgA is a critical immune regulator of glucose homeostasis. Obese mice have fewer IgA+ immune cells and less secretory IgA and IgA-promoting immune mediators. HFD-fed IgA-deficient mice have dysfunctional glucose metabolism, a phenotype that can be recapitulated by adoptive transfer of intestinal-associated pan-B cells. Mechanistically, IgA is a crucial link that controls intestinal and adipose tissue inflammation, intestinal permeability, microbial encroachment and the composition of the intestinal microbiome during HFD. Current glucose-lowering therapies, including metformin, affect intestinal-related IgA+ B cell populations in mice, while bariatric surgery regimen alters the level of fecal secretory IgA in humans. These findings identify intestinal IgA+ immune cells as mucosal mediators of whole-body glucose regulation in diet-induced metabolic disease.",

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