Choi Jene, Nannenga Bonnie, Demidov Oleg N, Bulavin Dmitry V, Cooney Austin, Brayton Cory, Zhang Yongxin, Mbawuike Innocent N, Bradley Allan, Appella Ettore, Donehower Lawrence A
Department of Molecular Virology and Microbiology, Baylor College of Medicine, Houston, Texas 77030, USA.
Mol Cell Biol. 2002 Feb;22(4):1094-105. doi: 10.1128/MCB.22.4.1094-1105.2002.
The Wip1 gene is a serine/threonine phosphatase that is induced in a p53-dependent manner by DNA-damaging agents. We show here that Wip1 message is expressed in moderate levels in all organs, but is present at very high levels in the testes, particularly in the postmeiotic round spermatid compartment of the seminiferous tubules. We have confirmed that Wip1 mRNA is induced by ionizing radiation in mouse tissues in a p53-dependent manner. To further determine the normal biological function of Wip1 in mammalian organisms, we have generated Wip1-deficient mice. Wip1 null mice are viable but show a variety of postnatal abnormalities, including variable male runting, male reproductive organ atrophy, reduced male fertility, and reduced male longevity. Mice lacking Wip1 show increased susceptibility to pathogens and diminished T- and B-cell function. Fibroblasts derived from Wip1 null embryos have decreased proliferation rates and appear to be compromised in entering mitosis. The data are consistent with an important role for Wip1 in spermatogenesis, lymphoid cell function, and cell cycle regulation.
Wip1基因是一种丝氨酸/苏氨酸磷酸酶,在DNA损伤剂作用下以p53依赖的方式被诱导表达。我们在此表明,Wip1信息在所有器官中均以中等水平表达,但在睾丸中表达水平非常高,特别是在生精小管的减数分裂后圆形精子细胞区室。我们已经证实,Wip1 mRNA在小鼠组织中经电离辐射以p53依赖的方式被诱导表达。为了进一步确定Wip1在哺乳动物机体中的正常生物学功能,我们培育出了Wip1基因缺失的小鼠。Wip1基因敲除小鼠能够存活,但表现出多种出生后异常,包括雄性生长迟缓、雄性生殖器官萎缩、雄性生育力下降以及雄性寿命缩短。缺乏Wip1的小鼠对病原体的易感性增加,T细胞和B细胞功能减弱。源自Wip1基因敲除胚胎的成纤维细胞增殖速率降低,进入有丝分裂的能力似乎受损。这些数据表明Wip1在精子发生、淋巴细胞功能和细胞周期调控中发挥重要作用。
