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Characterization of Cre recombinase models for the study of adipose tissue

机译:用于研究脂肪组织的Cre重组酶模型的表征

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摘要

The study of adipose tissue in vivo has been significantly advanced through the use of genetic mouse models. While the aP2-CreBI and aP2-CreSalk lines have been widely used to target adipose tissue, the specificity of these lines for adipocytes has recently been questioned. Here we characterize Cre recombinase activity in multiple cell populations of the major adipose tissue depots of these and other Cre lines using the membrane-Tomato/membrane-GFP (mT/mG) dual fluorescent reporter. We find that the aP2-CreBI and aP2-CreSalk lines lack specificity for adipocytes within adipose tissue, and that the aP2-CreBI line does not efficiently target adipocytes in white adipose depots. Alternatively, the Adiponectin-CreERT line shows high efficiency and specificity for adipocytes, while the PdgfRα-CreERUCL and PdgfRα-CreERJHU lines do not efficiently target adipocyte precursor cells in the major adipose depots. Instead, we show that the PdgfRα-Cre line is preferable for studies targeting adipocyte precursor cells in vivo.
机译:通过使用遗传小鼠模型,体内脂肪组织的研究已得到显着进展。尽管aP2-Cre BI 和aP2-Cre Salk 系已广泛用于靶向脂肪组织,但近来人们质疑这些系对脂肪细胞的特异性。在这里,我们使用膜-番茄/膜-GFP(mT / mG)双荧光报告基因表征这些和其他Cre系的主要脂肪组织贮库的多个细胞群体中的Cre重组酶活性。我们发现aP2-Cre BI 和aP2-Cre Salk 品系对脂肪组织内的脂肪细胞缺乏特异性,而aP2-Cre BI 品系不能有效地靶向白色脂肪库中的脂肪细胞。或者,脂联素-CreERT系对脂肪细胞显示出高效率和特异性,而PdgfRα-CreERUCL和PdgfRα-CreERJHU系不能有效地靶向主要脂肪库中的脂肪细胞前体细胞。相反,我们显示PdgfRα-Cre系对于靶向体内脂肪细胞前体细胞的研究更可取。

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