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结构研究对p53功能的新见解。

New insights into p53 function from structural studies.

作者信息

Arrowsmith C H, Morin P

机构信息

Division of Molecular and Structural Biology, Ontario Cancer Institute, University of Toronto, Canada.

出版信息

Oncogene. 1996 Apr 4;12(7):1379-85.

PMID:8622853
Abstract

Recent structural analysis of p53 has greatly enhanced our understanding of the biochemical activities of this protein by presenting us with a detailed picture of the chemical groups in the protein that are involved in protein stability, conformation and functional interactions. The current structures form the basis for the design of potential therapeutics which could, for example, revert a DNA-binding mutant back to a DNA-binding competent conformation. The structure of the tet domain forms the basis for designing an active therapeutic p53 with an oligomerization domain which would not cross react with a DNA-binding mutant p53. However, as useful as these structures have been in providing insight into the structure/function relationship for p53, a complete understanding of this protein awaits more detailed information on the full-length protein. In this respect, one of the most useful roles for future structural studies will be to help identify the nature of the conformational transition between latent and active p53, and how it can be modulated.

摘要

最近对p53的结构分析,通过向我们展示该蛋白质中参与蛋白质稳定性、构象和功能相互作用的化学基团的详细情况,极大地增进了我们对这种蛋白质生化活性的理解。目前的结构为潜在治疗药物的设计奠定了基础,例如,这些药物可以使DNA结合突变体恢复到具有DNA结合能力的构象。四聚结构域的结构为设计一种带有寡聚化结构域的活性治疗性p53奠定了基础,该寡聚化结构域不会与DNA结合突变体p53发生交叉反应。然而,尽管这些结构在深入了解p53的结构/功能关系方面很有用,但要全面了解这种蛋白质,还需要有关全长蛋白质的更详细信息。在这方面,未来结构研究最有用的作用之一将是帮助确定潜伏型和活性p53之间构象转变的性质,以及如何对其进行调控。

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