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Robert V. Farese, Mini P. Sajan, Hong Yang, Pengfei Li, Steven Mastorides, William R. Gower, Sonali Nimal, Cheol Soo Choi, Sheene Kim, Gerald I. Shulman, C. Ronald Kahn, Ursula Braun, Michael Leitges
Published in Volume 117, Issue 8
J Clin Invest. 2007; 117(8):2289–2301 doi:10.1172/JCI31408
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Figure 4
Effects of homozygous and heterozygous muscle-specific KO of PKC-λ on basal and insulin-stimulated activities of aPKC, PKB, IRS-1–dependent PI3K, and IRS-2–dependent PI3K in liver.

Experiments were performed as described in Figure 1, A–D. Insets show representative immunoblots of hepatic aPKC and phosphorylated Ser473-PKB as well as autoradiograms of IRS-1–dependent PI3K activity with or without insulin, i.e., 32P-PI-3-PO4 resolved by thin-layer chromatography. Values are mean ± SEM. n for each group is shown in parentheses. #P < 0.05; ##P < 0.01; ###P < 0.001 versus non–insulin-stimulated group of the same genotype (ANOVA). *P < 0.05 (ANOVA).