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c-Src使表皮生长因子受体的酪氨酸845位点发生磷酸化。

c-Src phosphorylates epidermal growth factor receptor on tyrosine 845.

作者信息

Sato K, Sato A, Aoto M, Fukami Y

机构信息

Laboratory of Molecular Biology, Kobe University, Japan.

出版信息

Biochem Biophys Res Commun. 1995 Oct 24;215(3):1078-87. doi: 10.1006/bbrc.1995.2574.

Abstract

In the previous study [Sato et al. (1995) Biochem. Biophys. Res. Commun. 210, 844-851], we found that c-Src was associated with epidermal growth factor (EGF) receptor and activated upon EGF treatment in A431 cells. In the present study, we investigated the phosphorylation of EGF receptor by c-Src in the c-Src-EGF receptor complex. We have focused our attention to tyrosine residue 845 (Y845) of EGF receptor as a candidate for the phosphorylation site. A synthetic peptide containing Y845, named Y845 peptide, which corresponds to residue 837 to 856 of EGF receptor, was found to be phosphorylated by c-Src and used to provide the standard phosphopeptide. In addition to the autophosphorylated peptide of 25 kDa, a phosphopeptide of 7 kDa was detected in the cyanogen bromide-digested fragments of the c-Src-associated EGF receptor phosphorylated in vitro in an EGF-dependent manner. In phosphopeptide mapping, tryptic digest of the 7-kDa phosphopeptide was shown to co-migrate with that of the phosphorylated Y845 peptide. The 7-kDa phosphopeptide was found to be phosphorylated exclusively on tyrosine. These results suggest that c-Src can phosphorylate EGF receptor on Y845 in an EGF-dependent manner. Furthermore, we confirmed that the same site of the c-Src-associated EGF receptor was phosphorylated in EGF-treated A431 cells.

摘要

在先前的研究中[Sato等人(1995年),《生物化学与生物物理学研究通讯》210卷,844 - 851页],我们发现c-Src与表皮生长因子(EGF)受体相关联,并在A431细胞中经EGF处理后被激活。在本研究中,我们研究了c-Src-EGF受体复合物中c-Src对EGF受体的磷酸化作用。我们将注意力集中在EGF受体的酪氨酸残基845(Y845)上,将其作为磷酸化位点的候选者。一种包含Y845的合成肽,名为Y845肽,它对应于EGF受体的837至856位残基,被发现可被c-Src磷酸化,并用作标准磷酸肽。除了25 kDa的自身磷酸化肽外,在以EGF依赖性方式体外磷酸化的c-Src相关EGF受体的溴化氰消化片段中检测到一种7 kDa的磷酸肽。在磷酸肽图谱分析中,7 kDa磷酸肽的胰蛋白酶消化产物显示与磷酸化的Y845肽的消化产物迁移情况相同。发现7 kDa磷酸肽仅在酪氨酸上被磷酸化。这些结果表明,c-Src可以以EGF依赖性方式使EGF受体的Y845位点磷酸化。此外,我们证实,在经EGF处理的A431细胞中,c-Src相关EGF受体的同一位点也被磷酸化。

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