Aryl hydrocarbon receptor agonist indigo protects against obesity-related insulin resistance through modulation of intestinal and metabolic tissue immunity

Yi-Hsuan Lin; Helen Luck; Saad Khan; Pierre H H Schneeberger; Sue Tsai; Xavier Clemente-Casares; Helena Lei; Yann-Lii Leu; Yi Tao Chan; Hsing-Yu Chen; Sien-Hung Yang; Bryan Coburn; Shawn Winer; Daniel A Winer

doi:10.1038/s41366-019-0340-1

Aryl hydrocarbon receptor agonist indigo protects against obesity-related insulin resistance through modulation of intestinal and metabolic tissue immunity

Int J Obes (Lond). 2019 Dec;43(12):2407-2421. doi: 10.1038/s41366-019-0340-1. Epub 2019 Apr 3.

Authors

Yi-Hsuan Lin^#^{1

2

3

4}, Helen Luck^#^{4

5}, Saad Khan^{4

5}, Pierre H H Schneeberger^{6

7}, Sue Tsai⁴, Xavier Clemente-Casares⁴, Helena Lei⁴, Yann-Lii Leu^{1

8}, Yi Tao Chan^{4

5}, Hsing-Yu Chen^{1

2

3}, Sien-Hung Yang^{1

2

9}, Bryan Coburn^{6

7}, Shawn Winer^#^{4

7

10}, Daniel A Winer^#^{11

12

13

14

15

16}

Affiliations

¹ Division of Chinese Internal Medicine, Center for Traditional Chinese Medicine, Chang Gung Memorial Hospital, Taoyuan, 33378, Taiwan.
² School of Traditional Chinese Medicine, College of Medicine, Chang Gung University, Taoyuan, 33302, Taiwan.
³ Graduate Institute of Clinical Medical Sciences, College of Medicine, Chang Gung University, Taoyuan, 33302, Taiwan.
⁴ Division of Cellular & Molecular Biology, Diabetes Research Group, Toronto General Research Institute (TGRI), University Health Network, 101 College Street, Toronto, ON, M5G 1L7, Canada.
⁵ Department of Immunology, University of Toronto, 1 King's College Circle, Toronto, ON, M5S 3B3, Canada.
⁶ Department of Medicine, Division of Infectious Diseases, University Health Network, Toronto, Canada.
⁷ Department of Laboratory Medicine and Pathobiology, University of Toronto, Toronto, ON, M5S 1A8, Canada.
⁸ Graduate Institute of Natural Products, College of Medicine, Chang Gung University, Taoyuan, 33302, Taiwan.
⁹ Chang Gung Immunology Consortium, Chang Gung Memorial Hospital and Chang Gung University, Gueishan, Taoyuan, 33302, Taiwan.
¹⁰ Department of Laboratory Medicine, St. Michael's Hospital, Toronto, ON, M5B 1W8, Canada.
¹¹ Division of Cellular & Molecular Biology, Diabetes Research Group, Toronto General Research Institute (TGRI), University Health Network, 101 College Street, Toronto, ON, M5G 1L7, Canada. dan.winer@uhn.ca.
¹² Department of Immunology, University of Toronto, 1 King's College Circle, Toronto, ON, M5S 3B3, Canada. dan.winer@uhn.ca.
¹³ Department of Laboratory Medicine and Pathobiology, University of Toronto, Toronto, ON, M5S 1A8, Canada. dan.winer@uhn.ca.
¹⁴ Department of Pathology, University Health Network, 200 Elizabeth Street, Toronto, ON, M5G 2C4, Canada. dan.winer@uhn.ca.
¹⁵ Buck Institute for Research on Aging, 8001 Redwood Boulevard, Novato, CA, 94945, USA. dan.winer@uhn.ca.
¹⁶ 10-352 Toronto Medical Discovery Tower, 101 College Street, Toronto, ON, M5G 1L7, Canada. dan.winer@uhn.ca.

^# Contributed equally.

Abstract

Background/objectives: Low-grade chronic inflammation in visceral adipose tissue and the intestines are important drivers of obesity associated insulin resistance. Bioactive compounds derived from plants are an important source of potential novel therapies for the treatment of chronic diseases. In search for new immune based treatments of obesity associated insulin resistance, we screened for tissue relevant anti-inflammatory properties in 20 plant-based extracts.

Methods: We screened 20 plant-based extracts to assess for preferential production of IL-10 compared to TNFα, specifically targetting metabolic tissues, including the visceral adipose tissue. We assessed the therapeutic potential of the strongest anti-inflammatory compound, indigo, in the C57BL/6J diet-induced obesity mouse model with supplementation for up to 16 weeks by measuring changes in body weight, glucose and insulin tolerance, and gut barrier function. We also utilized flow cytometry, quantitative PCR, enzyme-linked immunosorbent assay (ELISA), and histology to measure changes to immune cells populations and cytokine profiles in the intestine, visceral adipose tissue (VAT), and liver. 16SrRNA sequencing was performed to examine gut microbial differences induced by indigo supplementation.

Results: We identifed indigo, an aryl hydrocarbon receptor (AhR) ligand agonist, as a potent inducer of IL-10 and IL-22, which protects against high-fat diet (HFD)-induced insulin resistance and fatty liver disease in the diet-induced obesity model. Therapeutic actions were mechanistically linked to decreased inflammatory immune cell tone in the intestine, VAT and liver. Specifically, indigo increased Lactobacillus bacteria and elicited IL-22 production in the gut, which improved intestinal barrier permeability and reduced endotoxemia. These changes were associated with increased IL-10 production by immune cells residing in liver and VAT.

Conclusions: Indigo is a naturally occurring AhR ligand with anti-inflammatory properties that effectively protects against HFD-induced glucose dysregulation. Compounds derived from indigo or those with similar properties could represent novel therapies for diseases associated with obesity-related metabolic tissue inflammation.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Anti-Inflammatory Agents / pharmacology*
Cytokines / metabolism
Diet, High-Fat
Gastrointestinal Microbiome
Indigo Carmine / pharmacology*
Inflammation / metabolism
Insulin Resistance / physiology*
Male
Mice
Mice, Inbred C57BL
Obesity / metabolism*
Plant Extracts / chemistry
Receptors, Aryl Hydrocarbon / agonists*

Substances

Anti-Inflammatory Agents
Cytokines
Plant Extracts
Receptors, Aryl Hydrocarbon
Indigo Carmine

Abstract

Publication types

MeSH terms

Substances

Grants and funding