The primary objective of Dr. Shulman’s laboratory is to elucidate the cellular and molecular mechanisms responsible for insulin resistance in liver and muscle in patients with type 2 diabetes mellitus.  Recent studies by the Shulman group have demonstrated that alterations in muscle mitochondrial metabolism ( Science 300;1140-1142, 2003, N. Eng. J. Med 664-671, 2004, Science 2005:307;384-387) may be responsible for lipid accumulation in muscle and liver resulting in insulin resistance in these organs.  Available rotation projects for prospective MSTP students which address this theme include (but are not limited to): 1) In vivo and in vitro NMR studies of muscle and liver mitochondrial metabolism in humans and various transgenic and knockout mouse models of type 2 diabetes, 2) molecular and in vivo studies examining the regulation of mitochondrial biogenesis in AMPK, PGC-1 and CaMIV transgenic and knockout mice, 3) In vivo and in vitro regulation of insulin signaling by fatty acids.

Rotation projects: please contact Debbie Mento (ext 5-5447) Or Dr. Shulman. Lab Meeting Dates- Every Wednesday at 3:00 (if you would like to attend)

Kim JK, Kim YJ, Fillmore JJ, Chen Y, Moore I, Lee J, Yuan M, Li ZW, Karin M, Perret P, Shoelson SE, Shulman GI. Prevention of fat-induced insulin resistance by salicylate. J Clin Invest. 2001 Aug 1;108(3):437-446.

Fernandez AM, Kim JK, Yakar S, Dupont J, Hernandez-Sanchez C, Castle AL, Filmore J, Shulman GI, Le Roith D. Functional inactivation of the IGF-I and insulin receptors in skeletal muscle causes type 2 diabetes. Genes Dev. 2001 Aug 1;15(15):1926-34.