109 Zina Pitcher Place 2057 Biomedical Sciences Research Building
Ann Arbor, MI 48109
Available to mentor
Dr. Lumeng is the Frederick G.L. Huetwell Professor for the Cure and Prevention of Birth Defects and Professor in Pediatrics and Molecular and Integrative Physiology and Director of the Division of Pediatric Pulmonary Medicine at the University of Michigan. He is a member of the Graduate Program in Immunology, the Cellular and Molecular Biology Graduate Program at the University of Michigan Medical School, and the Associate Director of the Michigan MSTP Program. The research focus of the Lumeng Laboratory is on immunometabolism and the mechanisms by which inflammation contributes to obesity-associated diseases such as type 2 diabetes and is funded by the NIH and foundations such as the American Diabetes Association.
Dr Lumeng is a graduate of Princeton University (A.B. in Molecular Biology) and received his PhD in Human Genetics and MD from the University of Michigan MSTP Program. He completed residency training in Pediatrics in the Boston Combined Pediatrics Residency Program at Boston Children’s Hospital and Boston Medical Center and completed fellowship training in Pediatric Pulmonology at the University of Michigan. Dr. Lumeng is board certified in Pediatric Pulmonology and was appointed in 2007 as faculty in the Department of Pediatrics at UM.
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Postdoctoral Research FellowUniversity of Michigan Medical School, Cellular and Molecular Biology, 2008
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Pediatric Pulmonology FellowshipUniversity of Michigan Medical School, Pediatrics, 2006
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Pediatric ResidencyBoston Childrens Hospital, Boston, 2003
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Pediatric ResidencyBoston Medical Center, Pediatrics, 2003
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MDUniversity of Michigan Medical School, Ann Arbor, 2000
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PhDUniversity of Michigan Medical School, Ann Arbor, 2000
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Center MemberSamuel and Jean Frankel Cardiovascular Center
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Center MemberCaswell Diabetes Institute
My research program centers on understanding the mechanisms by which obesity negatively impacts health. My laboratory strives to improve the understanding of the links between obesity and disease to enable the design of novel strategies to disrupt these connections. Work from my lab has helped contribute to the new field of immunometabolism which is focused on understanding the intersection between pathways that regulate immune responses and those that control nutrient metabolism. Towards this end, we have focused on understanding how the innate and adaptive immune system respond to dietary excess and contribute to metabolic dysfunction such as insulin resistance that are major risk factors for cardiovascular disease.
Current projects in the lab focus on numerous aspects of adipose tissue immune network in health and disease. Projects focus on the regulation of adipose tissue macrophages in obesity and understanding how macrophage proliferation contributes to their regulation and polarization state. Antigen presenting cells in adipose tissue is also a focus of the lab as a link between innate and adaptive immune regulation. Translational research studies have identified novel genetic pathways relevant to metabolically unhealthy obesity phenotypes by collaborations with bariatric surgery to obtain omental and subcutaneous adipose samples. Recent efforts in the lab are using single cell and nuclear RNA sequencing approaches to delineate cellular diversity in adipose tissue in humans and mice in a team science approach with surgeons, bioinformaticians, and biologists.
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Jacks RD, Lumeng CN. Nat Rev Endocrinol, 2024 Jan; 20 (1): 50 - 61.Journal ArticleMacrophage and T cell networks in adipose tissue.
DOI:10.1038/s41574-023-00908-2 PMID: 37872302 -
Nance SA, Muir L, Delproprosto J, Lumeng CN. Sci Rep, 2023 Feb 14; 13 (1): 2651Journal ArticleMSR1 is not required for obesity-associated inflammation and insulin resistance in mice.
DOI:10.1038/s41598-023-29736-0 PMID: 36788340 -
Heindel JJ, Alvarez JA, Atlas E, Cave MC, Chatzi VL, Collier D, Corkey B, Fischer D, Goran MI, Howard S, Kahan S, Kayhoe M, Koliwad S, Kotz CM, La Merrill M, Lobstein T, Lumeng C, Ludwig DS, Lustig RH, Myers P, Nadal A, Trasande L, Redman LM, Rodeheffer MS, Sargis RM, Stephens JM, Ziegler TR, Blumberg B. Am J Clin Nutr, 2023 Jul; 118 (1): 329 - 337.Journal ArticleObesogens and Obesity: State-of-the-Science and Future Directions Summary from a Healthy Environment and Endocrine Disruptors Strategies Workshop.
DOI:10.1016/j.ajcnut.2023.05.024 PMID: 37230178 -
Jacks R, Lumeng CN. The Journal of Immunology, 2023 May 1; 210 (1_Supplement): 228.05 - 228.05.Journal ArticleRapid adipose tissue expansion induces proliferation of memory adipose tissue T cells
DOI:10.4049/jimmunol.210.supp.228.05 -
Ky A, McCoy AJ, Flesher CG, Friend NE, Li J, Akinleye K, Patsalis C, Lumeng CN, Putnam AJ, O'Rourke RW. Adipocyte, 2023 Dec; 12 (1): 2268261Journal ArticleMatrix density regulates adipocyte phenotype.
DOI:10.1080/21623945.2023.2268261 PMID: 37815174 -
Nance SA, Muir L, Lumeng C. Mol Metab, 2022 Dec; 66: 101642Journal ArticleAdipose tissue macrophages: Regulators of adipose tissue immunometabolism during obesity.
DOI:10.1016/j.molmet.2022.101642 PMID: 36402403 -
Bodur C, Kazyken D, Huang K, Tooley AS, Cho KW, Barnes TM, Lumeng CN, Myers MG, Fingar DC. Diabetes, 2022 Nov 1; 71 (11): 2297 - 2312.Journal ArticleTBK1-mTOR Signaling Attenuates Obesity-Linked Hyperglycemia and Insulin Resistance.
DOI:10.2337/db22-0256 PMID: 35983955 -
Zhang P, Chen Z, Kuang H, Liu T, Zhu J, Zhou L, Wang Q, Xiong X, Meng Z, Qiu X, Jacks R, Liu L, Li S, Lumeng CN, Li Q, Zhou X, Lin JD. Cell Metab, 2022 Sep 6; 34 (9): 1359 - 1376.e7.Journal ArticleNeuregulin 4 suppresses NASH-HCC development by restraining tumor-prone liver microenvironment.
DOI:10.1016/j.cmet.2022.07.010 PMID: 35973424