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Literature DB >> 23192980

A novel adipose-specific gene deletion model demonstrates potential pitfalls of existing methods.

Shannon E Mullican¹, Takuya Tomaru, Christine A Gaddis, Lindsey C Peed, Anand Sundaram, Mitchell A Lazar.

Abstract

Adipose-specific gene deletion in mice is crucial in determining gene function in adipocyte homeostasis and the development of obesity. We noted 100% mortality when the Hdac3 gene was conditionally deleted using Fabp4-Cre mice, the most commonly used model of adipose-targeted Cre recombinase. However, this surprising result was not reproduced using other models of adipose targeting of Cre, including a novel Retn-Cre mouse. These findings underscore the need for caution when interpreting data obtained using Fabp4-Cre mice and should encourage the use of additional or alternative adipose-targeting Cre mouse models before drawing conclusions about in vivo adipocyte-specific functions.

Entities: Disease Gene Species

Mesh：

Substances：

Year: 2012 PMID： 23192980 PMCID： PMC3545212 DOI： 10.1210/me.2012-1267

Source DB: PubMed Journal: Mol Endocrinol ISSN： 0888-8809

47 in total

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7. Ectopic recombination in the central and peripheral nervous system by aP2/FABP4-Cre mice: implications for metabolism research.

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51 in total

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Review 3. Mitochondrial homeostasis in adipose tissue remodeling.

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4. P65 inactivation in adipocytes and macrophages attenuates adipose inflammatory response in lean but not in obese mice.

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6. A PRDM16-Driven Metabolic Signal from Adipocytes Regulates Precursor Cell Fate.

Authors: Wenshan Wang; Jeff Ishibashi; Sophie Trefely; Mengle Shao; Alexis J Cowan; Alexander Sakers; Hee-Woong Lim; Sean O'Connor; Mary T Doan; Paul Cohen; Joseph A Baur; M Todd King; Richard L Veech; Kyoung-Jae Won; Joshua D Rabinowitz; Nathaniel W Snyder; Rana K Gupta; Patrick Seale
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