CD248 promotes insulin resistance by binding to the insulin receptor and dampening its insulin-induced autophosphorylation

Patricia O. Benedet; Nooshin S. Safikhan; Maria J. Pereira; Bryan M. Lum; José Diego Botezelli; Cheng Hsiang Kuo; Hua Lin Wu; Barbara P. Craddock; W. Todd Miller; Jan W. Eriksson; Jessica T.Y. Yue; Edward M. Conway

doi:10.1016/j.ebiom.2023.104906

CD248 promotes insulin resistance by binding to the insulin receptor and dampening its insulin-induced autophosphorylation

Patricia O. Benedet
, Nooshin S. Safikhan
, Maria J. Pereira
, Bryan M. Lum
, José Diego Botezelli
, Cheng Hsiang Kuo
, Hua Lin Wu
, Barbara P. Craddock
, W. Todd Miller
, Jan W. Eriksson
, Jessica T.Y. Yue
, Edward M. Conway

University of British Columbia
Uppsala University
University of Alberta
National Cheng Kung University
Stony Brook University

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

6 Scopus citations

Abstract

Background: In spite of new treatments, the incidence of type 2 diabetes (T2D) and its morbidities continue to rise. The key feature of T2D is resistance of adipose tissue and other organs to insulin. Approaches to overcome insulin resistance are limited due to a poor understanding of the mechanisms and inaccessibility of drugs to relevant intracellular targets. We previously showed in mice and humans that CD248, a pre/adipocyte cell surface glycoprotein, acts as an adipose tissue sensor that mediates the transition from healthy to unhealthy adipose, thus promoting insulin resistance. Methods: Molecular mechanisms by which CD248 regulates insulin signaling were explored using in vivo insulin clamp studies and biochemical analyses of cells/tissues from CD248 knockout (KO) and wild-type (WT) mice with diet-induced insulin resistance. Findings were validated with human adipose tissue specimens. Findings: Genetic deletion of CD248 in mice, overcame diet-induced insulin resistance with improvements in glucose uptake and lipolysis in white adipose tissue depots, effects paralleled by increased adipose/adipocyte GLUT4, phosphorylated AKT and GSK3β, and reduced ATGL. The insulin resistance of the WT mice could be attributed to direct interaction of the extracellular domains of CD248 and the insulin receptor (IR), with CD248 acting to block insulin binding to the IR. This resulted in dampened insulin-mediated autophosphorylation of the IR, with reduced downstream signaling/activation of intracellular events necessary for glucose and lipid homeostasis. Interpretation: Our discovery of a cell-surface CD248-IR complex that is accessible to pharmacologic intervention, opens research avenues toward development of new agents to prevent/reverse insulin resistance. Funding: Funded by Canadian Institutes of Health Research (CIHR), Natural Sciences and Engineering Research Council of Canada (NSERC), Canada Foundations for Innovation (CFI), the Swedish Diabetes Foundation, Family Ernfors Foundation and Novo Nordisk Foundation.

Original language	English
Article number	104906
Journal	EBioMedicine
Volume	99
DOIs	https://doi.org/10.1016/j.ebiom.2023.104906
State	Published - Jan 2024

Keywords

Adipocyte
CD248
Glucose
Insulin receptor
Insulin resistance
Lipid
Metabolism
Obesity

Access to Document

10.1016/j.ebiom.2023.104906

Cite this

Benedet, P. O., Safikhan, N. S., Pereira, M. J., Lum, B. M., Botezelli, J. D., Kuo, C. H., Wu, H. L., Craddock, B. P., Miller, W. T., Eriksson, J. W., Yue, J. T. Y., & Conway, E. M. (2024). CD248 promotes insulin resistance by binding to the insulin receptor and dampening its insulin-induced autophosphorylation. EBioMedicine, 99, Article 104906. https://doi.org/10.1016/j.ebiom.2023.104906

@article{b9d74e8edffc4a7fa44aeaebcf8eb8db,

title = "CD248 promotes insulin resistance by binding to the insulin receptor and dampening its insulin-induced autophosphorylation",

abstract = "Background: In spite of new treatments, the incidence of type 2 diabetes (T2D) and its morbidities continue to rise. The key feature of T2D is resistance of adipose tissue and other organs to insulin. Approaches to overcome insulin resistance are limited due to a poor understanding of the mechanisms and inaccessibility of drugs to relevant intracellular targets. We previously showed in mice and humans that CD248, a pre/adipocyte cell surface glycoprotein, acts as an adipose tissue sensor that mediates the transition from healthy to unhealthy adipose, thus promoting insulin resistance. Methods: Molecular mechanisms by which CD248 regulates insulin signaling were explored using in vivo insulin clamp studies and biochemical analyses of cells/tissues from CD248 knockout (KO) and wild-type (WT) mice with diet-induced insulin resistance. Findings were validated with human adipose tissue specimens. Findings: Genetic deletion of CD248 in mice, overcame diet-induced insulin resistance with improvements in glucose uptake and lipolysis in white adipose tissue depots, effects paralleled by increased adipose/adipocyte GLUT4, phosphorylated AKT and GSK3β, and reduced ATGL. The insulin resistance of the WT mice could be attributed to direct interaction of the extracellular domains of CD248 and the insulin receptor (IR), with CD248 acting to block insulin binding to the IR. This resulted in dampened insulin-mediated autophosphorylation of the IR, with reduced downstream signaling/activation of intracellular events necessary for glucose and lipid homeostasis. Interpretation: Our discovery of a cell-surface CD248-IR complex that is accessible to pharmacologic intervention, opens research avenues toward development of new agents to prevent/reverse insulin resistance. Funding: Funded by Canadian Institutes of Health Research (CIHR), Natural Sciences and Engineering Research Council of Canada (NSERC), Canada Foundations for Innovation (CFI), the Swedish Diabetes Foundation, Family Ernfors Foundation and Novo Nordisk Foundation.",

keywords = "Adipocyte, CD248, Glucose, Insulin receptor, Insulin resistance, Lipid, Metabolism, Obesity",

author = "Benedet, \{Patricia O.\} and Safikhan, \{Nooshin S.\} and Pereira, \{Maria J.\} and Lum, \{Bryan M.\} and Botezelli, \{Jos{\'e} Diego\} and Kuo, \{Cheng Hsiang\} and Wu, \{Hua Lin\} and Craddock, \{Barbara P.\} and Miller, \{W. Todd\} and Eriksson, \{Jan W.\} and Yue, \{Jessica T.Y.\} and Conway, \{Edward M.\}",

note = "Publisher Copyright: {\textcopyright} 2023 The Author(s)",

year = "2024",

month = jan,

doi = "10.1016/j.ebiom.2023.104906",

language = "English",

volume = "99",

journal = "EBioMedicine",

issn = "2352-3964",

}

TY - JOUR

T1 - CD248 promotes insulin resistance by binding to the insulin receptor and dampening its insulin-induced autophosphorylation

AU - Benedet, Patricia O.

AU - Safikhan, Nooshin S.

AU - Pereira, Maria J.

AU - Lum, Bryan M.

AU - Botezelli, José Diego

AU - Kuo, Cheng Hsiang

AU - Wu, Hua Lin

AU - Craddock, Barbara P.

AU - Miller, W. Todd

AU - Eriksson, Jan W.

AU - Yue, Jessica T.Y.

AU - Conway, Edward M.

PY - 2024/1

Y1 - 2024/1

N2 - Background: In spite of new treatments, the incidence of type 2 diabetes (T2D) and its morbidities continue to rise. The key feature of T2D is resistance of adipose tissue and other organs to insulin. Approaches to overcome insulin resistance are limited due to a poor understanding of the mechanisms and inaccessibility of drugs to relevant intracellular targets. We previously showed in mice and humans that CD248, a pre/adipocyte cell surface glycoprotein, acts as an adipose tissue sensor that mediates the transition from healthy to unhealthy adipose, thus promoting insulin resistance. Methods: Molecular mechanisms by which CD248 regulates insulin signaling were explored using in vivo insulin clamp studies and biochemical analyses of cells/tissues from CD248 knockout (KO) and wild-type (WT) mice with diet-induced insulin resistance. Findings were validated with human adipose tissue specimens. Findings: Genetic deletion of CD248 in mice, overcame diet-induced insulin resistance with improvements in glucose uptake and lipolysis in white adipose tissue depots, effects paralleled by increased adipose/adipocyte GLUT4, phosphorylated AKT and GSK3β, and reduced ATGL. The insulin resistance of the WT mice could be attributed to direct interaction of the extracellular domains of CD248 and the insulin receptor (IR), with CD248 acting to block insulin binding to the IR. This resulted in dampened insulin-mediated autophosphorylation of the IR, with reduced downstream signaling/activation of intracellular events necessary for glucose and lipid homeostasis. Interpretation: Our discovery of a cell-surface CD248-IR complex that is accessible to pharmacologic intervention, opens research avenues toward development of new agents to prevent/reverse insulin resistance. Funding: Funded by Canadian Institutes of Health Research (CIHR), Natural Sciences and Engineering Research Council of Canada (NSERC), Canada Foundations for Innovation (CFI), the Swedish Diabetes Foundation, Family Ernfors Foundation and Novo Nordisk Foundation.

AB - Background: In spite of new treatments, the incidence of type 2 diabetes (T2D) and its morbidities continue to rise. The key feature of T2D is resistance of adipose tissue and other organs to insulin. Approaches to overcome insulin resistance are limited due to a poor understanding of the mechanisms and inaccessibility of drugs to relevant intracellular targets. We previously showed in mice and humans that CD248, a pre/adipocyte cell surface glycoprotein, acts as an adipose tissue sensor that mediates the transition from healthy to unhealthy adipose, thus promoting insulin resistance. Methods: Molecular mechanisms by which CD248 regulates insulin signaling were explored using in vivo insulin clamp studies and biochemical analyses of cells/tissues from CD248 knockout (KO) and wild-type (WT) mice with diet-induced insulin resistance. Findings were validated with human adipose tissue specimens. Findings: Genetic deletion of CD248 in mice, overcame diet-induced insulin resistance with improvements in glucose uptake and lipolysis in white adipose tissue depots, effects paralleled by increased adipose/adipocyte GLUT4, phosphorylated AKT and GSK3β, and reduced ATGL. The insulin resistance of the WT mice could be attributed to direct interaction of the extracellular domains of CD248 and the insulin receptor (IR), with CD248 acting to block insulin binding to the IR. This resulted in dampened insulin-mediated autophosphorylation of the IR, with reduced downstream signaling/activation of intracellular events necessary for glucose and lipid homeostasis. Interpretation: Our discovery of a cell-surface CD248-IR complex that is accessible to pharmacologic intervention, opens research avenues toward development of new agents to prevent/reverse insulin resistance. Funding: Funded by Canadian Institutes of Health Research (CIHR), Natural Sciences and Engineering Research Council of Canada (NSERC), Canada Foundations for Innovation (CFI), the Swedish Diabetes Foundation, Family Ernfors Foundation and Novo Nordisk Foundation.

KW - Adipocyte

KW - CD248

KW - Glucose

KW - Insulin receptor

KW - Insulin resistance

KW - Lipid

KW - Metabolism

KW - Obesity

UR - https://www.scopus.com/pages/publications/85179006823

U2 - 10.1016/j.ebiom.2023.104906

DO - 10.1016/j.ebiom.2023.104906

M3 - Article

C2 - 38061240

AN - SCOPUS:85179006823

SN - 2352-3964

VL - 99

JO - EBioMedicine

JF - EBioMedicine

M1 - 104906

ER -

CD248 promotes insulin resistance by binding to the insulin receptor and dampening its insulin-induced autophosphorylation

Abstract

Keywords

Access to Document

Other files and links

Fingerprint

Cite this