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外周神经系统髓鞘中糖蛋白合成的酶促调节。

Enzymatic regulation of glycoprotein synthesis in peripheral nervous system myelin.

作者信息

Smith M E, Somera F P, Sims T J

出版信息

J Neurochem. 1985 Oct;45(4):1205-12. doi: 10.1111/j.1471-4159.1985.tb05543.x.

DOI:10.1111/j.1471-4159.1985.tb05543.x
PMID:4031886
Abstract

The enzyme UDP-N-acetylglucosamine: dolichyl phosphate, N-acetylglucosamine-1-phosphate transferase initiates the synthesis of the oligosaccharide chain of complex-type glycoproteins. In view of the high content of glycoprotein in peripheral nerve myelin, the properties of this enzyme, its changes with age, and the effect of the specific inhibitor tunicamycin were investigated. The enzyme activity in rat peripheral nerve homogenate was completely dependent on the presence of exogenous dolichyl phosphate as well as Mg2+ and a detergent (Triton X-100) and was also greatly stimulated by a high salt concentration (0.4 M KCl) and AMP. The highest specific activity was present in the postmitochondrial membranes. The specific activity in postmitochondrial membranes in the presence of exogenous dolichyl phosphate reached a maximum at 17 days and remained relatively high throughout development, up to 2 years of age, but the activity was much lower when dolichyl phosphate was not added. This indicates that the enzyme level does not decrease with age, but that the content of the lipid cofactor may limit glycoprotein synthesis in vivo. Tunicamycin (5 micrograms) was injected intraneurally into 24-day-old rat sciatic nerve, and the enzyme was assayed from 1 to 24 days after injection. The specific activity of the transferase remained at low levels (5-40% of the level in control nerve) in most injected nerves assayed throughout this postinjection period. A protein previously identified as the unglycosylated P0 protein was synthesized in vitro by the tunicamycin-injected nerve and could be demonstrated to be incorporated into myelin in large amounts at 2 days and in small amounts at 6 days after injection.(ABSTRACT TRUNCATED AT 250 WORDS)

摘要

UDP-N-乙酰葡糖胺:磷酸多萜醇N-乙酰葡糖胺-1-磷酸转移酶启动了复合型糖蛋白寡糖链的合成。鉴于周围神经髓鞘中糖蛋白含量很高,对该酶的特性、其随年龄的变化以及特异性抑制剂衣霉素的作用进行了研究。大鼠周围神经匀浆中的酶活性完全依赖于外源性磷酸多萜醇以及Mg2+和一种去污剂(曲拉通X-100)的存在,并且也受到高盐浓度(0.4M KCl)和AMP的极大刺激。最高比活性存在于线粒体后膜中。在线粒体后膜中,在外源性磷酸多萜醇存在的情况下,比活性在17天时达到最大值,并在整个发育过程中,直至2岁时都保持相对较高,但不添加磷酸多萜醇时活性要低得多。这表明酶水平不会随年龄降低,但脂质辅因子的含量可能会限制体内糖蛋白的合成。将衣霉素(5微克)经神经内注射到24日龄大鼠的坐骨神经中,并在注射后1至24天对酶进行测定。在整个注射后的这段时间内,大多数被测注射神经中转移酶的比活性保持在低水平(为对照神经水平的5-40%)。衣霉素注射的神经在体外合成了一种先前被鉴定为未糖基化P0蛋白的蛋白质,并且可以证明在注射后2天大量并入髓鞘,在6天时少量并入。(摘要截短于250字)

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