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Mos在非洲爪蟾卵母细胞中刺激丝裂原活化蛋白激酶,并在体外激活一种丝裂原活化蛋白激酶激酶。

Mos stimulates MAP kinase in Xenopus oocytes and activates a MAP kinase kinase in vitro.

作者信息

Posada J, Yew N, Ahn N G, Vande Woude G F, Cooper J A

机构信息

Fred Hutchinson Cancer Research Center, Seattle, Washington 98104.

出版信息

Mol Cell Biol. 1993 Apr;13(4):2546-53. doi: 10.1128/mcb.13.4.2546-2553.1993.

Abstract

Several protein kinases, including Mos, maturation-promoting factor (MPF), mitogen-activated protein (MAP) kinase, and MAP kinase kinase (MAPKK), are activated when Xenopus oocytes enter meiosis. De novo synthesis of the Mos protein is required for progesterone-induced meiotic maturation. Recently, bacterially synthesized maltose-binding protein (MBP)-Mos fusion protein was shown to be sufficient to initiate meiosis I and MPF activation in fully grown oocytes in the absence of protein synthesis. Here we show that MAP kinase is rapidly phosphorylated and activated following injection of wild-type, but not kinase-inactive mutant, MBP-Mos into fully grown oocytes. MAP kinase activation by MBP-Mos occurs within 20 min, much more rapidly than in progesterone-treated oocytes. The MBP-Mos fusion protein also activates MPF, but MPF activation does not occur until approximately 2 h after injection. Extracts from oocytes injected with wild-type but not kinase-inactive MBP-Mos contain an activity that can phosphorylate MAP kinase, suggesting that Mos directly or indirectly activates a MAPKK. Furthermore, activated MBP-Mos fusion protein is able to phosphorylate and activate a purified, phosphatase-treated, rabbit muscle MAPKK in vitro. Thus, in oocytes, Mos is an upstream activator of MAP kinase which may function through direct phosphorylation of MAPKK.

摘要

当非洲爪蟾卵母细胞进入减数分裂时,包括Mos、成熟促进因子(MPF)、丝裂原活化蛋白(MAP)激酶和MAP激酶激酶(MAPKK)在内的几种蛋白激酶会被激活。孕酮诱导的减数分裂成熟需要从头合成Mos蛋白。最近研究表明,在没有蛋白质合成的情况下,细菌合成的麦芽糖结合蛋白(MBP)-Mos融合蛋白足以在完全成熟的卵母细胞中启动减数分裂I并激活MPF。在此我们发现,将野生型而非激酶失活突变体的MBP-Mos注射到完全成熟的卵母细胞中后,MAP激酶会迅速磷酸化并被激活。MBP-Mos激活MAP激酶的过程在20分钟内发生,比用孕酮处理的卵母细胞快得多。MBP-Mos融合蛋白也能激活MPF,但MPF的激活直到注射后约2小时才会发生。注射野生型而非激酶失活的MBP-Mos的卵母细胞提取物含有一种能够磷酸化MAP激酶的活性,这表明Mos直接或间接激活了一种MAPKK。此外,活化的MBP-Mos融合蛋白能够在体外磷酸化并激活一种纯化的、经磷酸酶处理的兔肌肉MAPKK。因此,在卵母细胞中,Mos是MAP激酶的上游激活剂,可能通过直接磷酸化MAPKK发挥作用。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/5b6d/359584/3e72f1b9acbf/molcellb00016-0580-a.jpg

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