Leiter E H, Kintner J, Flurkey K, Beamer W G, Naggert J K
The Jackson Laboratory, Bar Harbor, ME 04609-1500, USA.
Endocrine. 1999 Feb;10(1):57-66. doi: 10.1385/endo:10:1:57.
The fat gene in mice represents a recessive mutation at the carboxypeptidase E (Cpe) locus. The mutant allele (Cpe(fat)) encodes a highly unstable enzyme and produces an obesity phenotype characterized by attenuated processing of prohormones such as proinsulin that require this exopeptidase for full maturation. This article presents a preliminary physiologic and endocrinologic characterization of the stock of C57BLKS/LtJ-Cpe(fat)/Cpe(fat) mice at the backcross generation (N10) currently distributed by The Jackson Laboratory. Although previously reported not to be diabetogenic at N5, an additional five backcrosses to the C57BLKS/J background resulted in a male-biased development of both obesity and diabetes. Major differences distinguishing this mutant stock from the phenotypes produced by either the diabetes (Lepr(db)) or obese (Lep(ob)) mutations on the same inbred strain background are lack of hyperphagia and hypercorticism, sensitivity of diabetic males to exogenous insulin, and a milder and male-biased diabetes syndrome that is not associated with widespread beta-cell necrosis and islet atrophy, and that often remits with age.
小鼠中的肥胖基因代表羧肽酶E(Cpe)位点的隐性突变。突变等位基因(Cpe(fat))编码一种高度不稳定的酶,并产生肥胖表型,其特征是前激素(如胰岛素原)的加工过程减弱,而胰岛素原需要这种外肽酶才能完全成熟。本文介绍了杰克逊实验室目前分发的回交世代(N10)的C57BLKS/LtJ-Cpe(fat)/Cpe(fat)小鼠品系的初步生理和内分泌特征。尽管之前报道在N5时不会致糖尿病,但与C57BLKS/J背景再进行五次回交后,肥胖和糖尿病在雄性中更易发生。该突变品系与同一近交系背景下糖尿病(Lepr(db))或肥胖(Lep(ob))突变产生的表型的主要区别在于,缺乏食欲亢进和高皮质醇血症,糖尿病雄性对外源胰岛素敏感,以及糖尿病综合征较轻且在雄性中更易发生,该综合征与广泛的β细胞坏死和胰岛萎缩无关,且常随年龄缓解。
