Human CD206+ macrophages associate with diabetes and adipose tissue lymphoid clusters
Lindsey A. Muir, … , Robert W. O’Rourke, Carey N. Lumeng
Lindsey A. Muir, … , Robert W. O’Rourke, Carey N. Lumeng
Published January 6, 2022
Citation Information: JCI Insight. 2022;7(3):e146563. https://doi.org/10.1172/jci.insight.146563.
View: Text | PDF
Research Article Immunology Metabolism

Human CD206+ macrophages associate with diabetes and adipose tissue lymphoid clusters

Abstract

Increased adipose tissue macrophages (ATMs) correlate with metabolic dysfunction in humans and are causal in development of insulin resistance in mice. Recent bulk and single-cell transcriptomics studies reveal a wide spectrum of gene expression signatures possible for macrophages that depends on context, but the signatures of human ATM subtypes are not well defined in obesity and diabetes. We profiled 3 prominent ATM subtypes from human adipose tissue in obesity and determined their relationship to type 2 diabetes. Visceral adipose tissue (VAT) and s.c. adipose tissue (SAT) samples were collected from diabetic and nondiabetic obese participants to evaluate cellular content and gene expression. VAT CD206+CD11c− ATMs were increased in diabetic participants, were scavenger receptor–rich with low intracellular lipids, secreted proinflammatory cytokines, and diverged significantly from 2 CD11c+ ATM subtypes, which were lipid-laden, were lipid antigen presenting, and overlapped with monocyte signatures. Furthermore, diabetic VAT was enriched for CD206+CD11c− ATM and inflammatory signatures, scavenger receptors, and MHC II antigen presentation genes. VAT immunostaining found CD206+CD11c– ATMs concentrated in vascularized lymphoid clusters adjacent to CD206–CD11c+ ATMs, while CD206+CD11c+ were distributed between adipocytes. Our results show ATM subtype–specific profiles that uniquely contribute to the phenotypic variation in obesity.

Authors

Lindsey A. Muir, Kae Won Cho, Lynn M. Geletka, Nicki A. Baker, Carmen G. Flesher, Anne P. Ehlers, Niko Kaciroti, Stephen Lindsly, Scott Ronquist, Indika Rajapakse, Robert W. O’Rourke, Carey N. Lumeng

×

Figure 6

ATM subtype cytokine secretion and localization.

Options: View larger image (or click on image) Download as PowerPoint
ATM subtype cytokine secretion and localization. (A) Expression of cytok...
(A) Expression of cytokines in NDM and DM obese whole visceral adipose tissue. Data are shown as mean FPKM log2-fold difference. (B) Expression of cytokines in CD206+ and CD11c+ ATMs by RNA-Seq. (C) Baseline cytokine secretion from sorted CD206+ or CD206 VAT ATMs, shown as mean concentration. (D) Cytokine secretion from sorted, LPS-stimulated CD206+ or CD206 VAT ATMs. Each replicate was normalized to baseline, and measures are shown as mean fold over baseline ± SD. (C and D) Replicates: n = 3–4 wells per measure. Raw data were analyzed by 2-way ANOVA with Sidak’s multiple comparison test. (E) Immunostaining for CD206 (green) and CD11c (red) in 2 human visceral adipose tissue samples in obesity. CD206 and CD11c show differential expression in CLS (white arrows) and FALC (orange arrow), but they show coexpress in cells between adipocytes (blue arrows). Blood vessels (blue) were stained with UEA-1 lectin. Scale bar: 100 μm. Row 1: epifluorescence microscopy. Rows 2–4: confocal microscopy.