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通过脂肪酰化作用将癌蛋白靶向至细胞膜。

Targeting of oncoproteins to membranes by fatty acylation.

作者信息

Magee A I, Gutierrez L, Marshall C J, Hancock J F

机构信息

National Institute for Medical Research, Laboratory of Cell Surface Interactions, London, UK.

出版信息

J Cell Sci Suppl. 1989;11:149-60. doi: 10.1242/jcs.1989.supplement_11.12.

Abstract

Post-translational modification of proteins with hydrophobic lipid-derived substituents is increasingly becoming recognized as a major route for targeting proteins to membranes. Glycosylphosphatidylinositol (GPI) anchors are found at the C terminus of a wide range of cell surface proteins, and may endow the cell with the ability to release them in a controlled fashion via specific phospholipases. We have concentrated on the direct attachment (acylation) of long-chain fatty acids (myristate, C14:0 and palmitate, C16:0) to proteins associated with the cytoplasmic face of cellular membranes. Two such proteins, the products of the src and ras oncogenes, require acylation respectively with myristate and palmitate for their membrane association and biological activity, including transformation. N-terminal myristoylation of p60src seems to be a cotranslational stable modification. However, our recent results show that post-translational modification of p21ras is a complex cascade of events involving proteolysis, methylation and thioesterification of palmitate. This last acylation event is dynamic in vivo and may regulate ras function. Enzymological studies of these modification events are in progress. A better understanding of acylation may provide targets for future pharmacological intervention.

摘要

用疏水脂质衍生取代基对蛋白质进行翻译后修饰,日益被认为是将蛋白质靶向细胞膜的主要途径。糖基磷脂酰肌醇(GPI)锚定在多种细胞表面蛋白的C末端,并且可能赋予细胞通过特定磷脂酶以可控方式释放它们的能力。我们专注于将长链脂肪酸(肉豆蔻酸,C14:0和棕榈酸,C16:0)直接连接(酰化)到与细胞膜胞质面相关的蛋白质上。两种这样的蛋白质,即src和ras癌基因的产物,分别需要肉豆蔻酸和棕榈酸酰化才能实现其膜结合和生物学活性,包括转化。p60src的N末端肉豆蔻酰化似乎是一种共翻译稳定修饰。然而,我们最近的结果表明,p21ras的翻译后修饰是一个复杂的事件级联,涉及棕榈酸的蛋白水解、甲基化和硫酯化。最后这个酰化事件在体内是动态的,可能调节ras功能。对这些修饰事件的酶学研究正在进行中。对酰化的更好理解可能为未来的药物干预提供靶点。

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