BBS-Induced Ciliary Defect Enhances Adipogenesis, Causing Paradoxical Higher-Insulin Sensitivity, Glucose Usage, and Decreased Inflammatory Response

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• 作者：Vincent Marion ; Ana?s Mockel ; Charlie De?Melo ; Cathy Obringer ; Aur¨¦lie Claussmann ; Alban Simon ; Nadia Messaddeq ; Myriam Dur ; Luc Dupuis ; Jean-Philippe Loeffler ; Peter King ; Catherine Mutter-Schmidt ; Nikolai Petrovsky ; Corinne Stoetzel ; H¨¦l¨¨ne Dollfus
• 刊名：Cell Metabolism
• 出版年：2012
• 出版时间：5 September, 2012
• 年：2012
• 卷：16
• 期：3
• 页码：363-377
• 全文大小：2653 K

文摘

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Summary

Studying ciliopathies, like the Bardet-Biedl syndrome (BBS), allow the identification of signaling pathways potentially involved in common diseases, sharing phenotypic features like obesity or type 2 diabetes. Given the close association between obesity and insulin resistance, obese BBS patients would be expected to be insulin resistant. Surprisingly, we found that a majority of obese BBS patients retained normal glucose tolerance and insulin sensitivity. Patient¡¯s adipose tissue biopsies revealed upregulation of adipogenic genes and decrease of inflammatory mediators. In?vitro studies on human primary mesenchymal stem cells (MSCs) showed that BBS12 inactivation facilitated adipogenesis, increased insulin sensitivity, and glucose utilization. We generated a Bbs12^?/? mouse model to assess the impact of Bbs12 inactivation on adipocyte biology. Despite increased obesity, glucose tolerance was increased with specific enhanced insulin sensitivity in the fat. This correlated with an active recruitment of MSCs resulting in adipose tissue hyperplasia and decreased in inflammation.