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结旁连接的形成和精子发生需要硫糖脂。

Paranodal junction formation and spermatogenesis require sulfoglycolipids.

作者信息

Honke Koichi, Hirahara Yukie, Dupree Jeffrey, Suzuki Kinuko, Popko Brian, Fukushima Kikuro, Fukushima Junko, Nagasawa Takashi, Yoshida Nobuaki, Wada Yoshinao, Taniguchi Naoyuki

机构信息

Department of Biochemistry, Osaka University Medical School, 2-2 Yamadaoka, Suita, Osaka 565-0871, Japan.

出版信息

Proc Natl Acad Sci U S A. 2002 Apr 2;99(7):4227-32. doi: 10.1073/pnas.032068299. Epub 2002 Mar 26.

Abstract

Mammalian sulfoglycolipids comprise two major members, sulfatide (HSO3-3-galactosylceramide) and seminolipid (HSO3-3-monogalactosylalkylacylglycerol). Sulfatide is a major lipid component of the myelin sheath and serves as the epitope for the well known oligodendrocyte-marker antibody O4. Seminolipid is synthesized in spermatocytes and maintained in the subsequent germ cell stages. Both sulfoglycolipids can be synthesized in vitro by using the isolated cerebroside sulfotransferase. To investigate the physiological role of sulfoglycolipids and to determine whether sulfatide and seminolipid are biosynthesized in vivo by a single sulfotransferase, Cst-null mice were generated by gene targeting. Cst(-/-) mice lacked sulfatide in brain and seminolipid in testis, proving that a single gene copy is responsible for their biosynthesis. Cst(-/-) mice were born healthy, but began to display hindlimb weakness by 6 weeks of age and subsequently showed a pronounced tremor and progressive ataxia. Although compact myelin was preserved, Cst(-/-) mice displayed abnormalities in paranodal junctions. On the other hand, Cst(-/-) males were sterile because of a block in spermatogenesis before the first meiotic division, whereas females were able to breed. These data show a critical role for sulfoglycolipids in myelin function and spermatogenesis.

摘要

哺乳动物的硫苷脂包含两个主要成员,硫脂(硫酸根-3-半乳糖神经酰胺)和半乳糖脑苷脂(硫酸根-3-单半乳糖烷基酰基甘油)。硫脂是髓鞘的主要脂质成分,也是著名的少突胶质细胞标记抗体O4的表位。半乳糖脑苷脂在精母细胞中合成,并在随后的生殖细胞阶段得以维持。两种硫苷脂都可以通过使用分离的脑苷脂磺基转移酶在体外合成。为了研究硫苷脂的生理作用,并确定硫脂和半乳糖脑苷脂是否在体内由单一的磺基转移酶生物合成,通过基因靶向产生了Cst基因敲除小鼠。Cst(-/-)小鼠脑内缺乏硫脂,睾丸中缺乏半乳糖脑苷脂,这证明单个基因拷贝负责它们的生物合成。Cst(-/-)小鼠出生时健康,但在6周龄时开始表现出后肢无力,随后出现明显震颤和进行性共济失调。尽管致密髓鞘得以保留,但Cst(-/-)小鼠在结旁连接中表现出异常。另一方面,Cst(-/-)雄性小鼠由于在第一次减数分裂前精子发生受阻而不育,而雌性小鼠能够繁殖。这些数据表明硫苷脂在髓鞘功能和精子发生中起关键作用。

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