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小鼠酸不稳定亚基基因的失活导致出生后生长轻度迟缓,尽管循环胰岛素样生长因子系统受到严重破坏。

Inactivation of the acid labile subunit gene in mice results in mild retardation of postnatal growth despite profound disruptions in the circulating insulin-like growth factor system.

作者信息

Ueki I, Ooi G T, Tremblay M L, Hurst K R, Bach L A, Boisclair Y R

机构信息

Department of Animal Science, Cornell University, Ithaca, NY 14853, USA.

出版信息

Proc Natl Acad Sci U S A. 2000 Jun 6;97(12):6868-73. doi: 10.1073/pnas.120172697.

Abstract

Insulin-like growth factors (IGFs) I and II are important regulators of cell proliferation and differentiation. After birth, plasma IGFs, representing mostly liver-derived IGFs, circulate in ternary complexes of 150 kDa consisting of one molecule each of IGF, IGF-binding protein (IGFBP) 3, and an acid labile subunit (ALS). Onset of ALS synthesis after birth is the primary factor driving the formation of ternary complexes. Capture of IGFs by ALS is thought to allow the development of a plasma reservoir without negative effects such as hypoglycemia and cell proliferation. To evaluate the importance of ALS and ternary complexes, we have created mice in which the ALS gene has been inactivated. The mutation was inherited in a Mendelian manner, without any effects on survival rates and birth weights. A growth deficit was observed in null mice after 3 weeks of life and reached 13% by 10 weeks. This modest phenotype was observed despite reductions of 62 and 88% in the concentrations of plasma IGF-I and IGFBP-3, respectively. Increased turnover accounted for these reductions because indices of synthesis in liver and kidney were not decreased. Surprisingly, absence of ALS did not affect glucose and insulin homeostasis. Therefore, ALS is required for postnatal accumulation of IGF-I and IGFBP-3 but, consistent with findings supporting a predominant role for locally produced IGF-I, is not critical for growth. This model should be useful to determine whether presence of ALS is needed for other actions of liver-derived IGF-I and for maintenance of homeostasis in presence of high circulating levels of IGF-II.

摘要

胰岛素样生长因子(IGFs)I和II是细胞增殖和分化的重要调节因子。出生后,血浆中的IGFs主要来源于肝脏,以150 kDa的三元复合物形式循环,该复合物由一个IGF分子、一个胰岛素样生长因子结合蛋白(IGFBP)3分子和一个酸性不稳定亚基(ALS)组成。出生后ALS合成的开始是驱动三元复合物形成的主要因素。ALS对IGFs的捕获被认为有助于形成血浆储备,而不会产生低血糖和细胞增殖等负面影响。为了评估ALS和三元复合物的重要性,我们培育了ALS基因被灭活的小鼠。该突变以孟德尔方式遗传,对存活率和出生体重没有任何影响。在出生3周后的基因敲除小鼠中观察到生长缺陷,到10周时达到13%。尽管血浆IGF-I和IGFBP-3的浓度分别降低了62%和88%,但仍观察到这种适度的表型。周转率增加导致了这些降低,因为肝脏和肾脏中的合成指标并未下降。令人惊讶的是,ALS的缺失并不影响葡萄糖和胰岛素的稳态。因此,ALS是出生后IGF-I和IGFBP-3积累所必需的,但与支持局部产生的IGF-I起主要作用的研究结果一致,对生长并不关键。该模型对于确定肝脏来源的IGF-I的其他作用以及在循环中IGF-II水平较高时维持稳态是否需要ALS应该是有用的。

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