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胰岛素样生长因子-I(IGF-I)处理后3T3小鼠成纤维细胞中蛋白激酶C向内核基质转位的免疫细胞化学评估。

Immunocytochemical evaluation of protein kinase C translocation to the inner nuclear matrix in 3T3 mouse fibroblasts after IGF-I treatment.

作者信息

Zini N, Martelli A M, Neri L M, Bavelloni A, Sabatelli P, Santi S, Maraldi N M

机构信息

Institute of Citomorfologia Normale e Patologica, C.N.R., Bologna, Italy.

出版信息

Histochem Cell Biol. 1995 Jun;103(6):447-57. doi: 10.1007/BF01457544.

Abstract

The complex pathway which links the agonist-cell membrane receptor binding to the response at the genome level involves, among other elements, protein kinase C (PKC). Agonists acting at the cell membrane can affect an autonomous nuclear polyphosphoinositide signaling system inducing an activation of nuclear phosphoinositidase activity and a subsequent translocation of PKC to the nuclear region. The fine localization of PKC has been investigated by means of electron microscopy quantitative immunogold labeling in 3T3 mouse fibroblasts, mitogenically stimulated by IGF-I. The enzyme, which in untreated cells is present in the cytoplasm, except for the organelles, and in the nucleoplasm, after IGF-I treatment is reduced in the cytoplasm and almost doubled in the nucleus. The PKC isoform translocated to the nucleus is the alpha isozyme, which is found not only associated with the nuclear envelope but mainly with the interchromatin domains. By using in situ matrix preparations, PKC appears to be retained at the nuclear matrix level, both at the nuclear lamina and at the inner nuclear matrix, suggesting a direct involvement in the phosphorylation of nuclear proteins which are responsible for the regulation of DNA replication.

摘要

将激动剂与细胞膜受体结合与基因组水平的反应联系起来的复杂途径,除其他因素外,还涉及蛋白激酶C(PKC)。作用于细胞膜的激动剂可影响自主的核多磷酸肌醇信号系统,诱导核磷酸肌醇酶活性的激活以及PKC随后向核区域的转位。通过电子显微镜定量免疫金标记,在受IGF-I有丝分裂刺激的3T3小鼠成纤维细胞中研究了PKC的精细定位。该酶在未处理的细胞中存在于细胞质(细胞器除外)和核质中,经IGF-I处理后,在细胞质中减少,在细胞核中几乎增加一倍。转位到细胞核的PKC同工型是α同工酶,它不仅与核膜相关,而且主要与染色质间区域相关。通过使用原位基质制剂,PKC似乎保留在核基质水平,在核纤层和内核基质中均如此,这表明它直接参与了负责DNA复制调控的核蛋白的磷酸化。

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