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基于表面等离子体共振的肿瘤抑制因子 p53 网络中生物识别相互作用的传感研究。

Surface Plasmon Resonance Sensing of Biorecognition Interactions within the Tumor Suppressor p53 Network.

机构信息

Biophysics & Nanoscience Centre, DEB, Università della Tuscia, Largo dell'Università, 01100 Viterbo, Italy.

出版信息

Sensors (Basel). 2017 Nov 20;17(11):2680. doi: 10.3390/s17112680.

Abstract

Surface Plasmon Resonance (SPR) is a powerful technique to study the kinetics of biomolecules undergoing biorecognition processes, particularly suited for protein-protein interactions of biomedical interest. The potentiality of SPR was exploited to sense the interactions occurring within the network of the tumor suppressor p53, which is crucial for maintaining genome integrity and whose function is inactivated, mainly by down regulation or by mutation, in the majority of human tumors. This study includes p53 down-regulators, p53 mutants and also the p53 family members, p63 and p73, which could vicariate p53 protective function. Furthermore, the application of SPR was extended to sense the interaction of p53 with anti-cancer drugs, which might restore p53 function. An extended review of previous published work and unpublished kinetic data is provided, dealing with the interaction between the p53 family members, or their mutants and two anticancer molecules, Azurin and its cell-penetrating peptide, p28. All the kinetic results are discussed in connection with those obtained by a complementary approach operating at the single molecule level, namely Atomic Force Spectroscopy and the related literature data. The overview of the SPR kinetic results may significantly contribute to a deeper understanding of the interactions within p53 network, also in the perspective of designing suitable anticancer drugs.

摘要

表面等离子体共振(SPR)是研究生物分子发生生物识别过程的动力学的强大技术,特别适合于具有医学意义的蛋白质-蛋白质相互作用。SPR 的潜力被开发用于检测肿瘤抑制因子 p53 网络内发生的相互作用,这对于维持基因组完整性至关重要,其功能主要通过下调或突变失活,在大多数人类肿瘤中失活。本研究包括 p53 下调因子、p53 突变体以及 p53 家族成员 p63 和 p73,它们可以替代 p53 的保护功能。此外,SPR 的应用还扩展到检测 p53 与抗癌药物的相互作用,这可能恢复 p53 的功能。提供了对以前发表的工作和未发表的动力学数据的扩展综述,涉及 p53 家族成员或其突变体与两种抗癌分子(天青蛋白及其穿透细胞肽 p28)之间的相互作用。所有动力学结果都与在单分子水平上进行的互补方法(原子力光谱学)获得的结果以及相关文献数据进行了讨论。SPR 动力学结果的概述可能会极大地有助于深入了解 p53 网络内的相互作用,也有助于设计合适的抗癌药物。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/8433/5713020/590893e8b8f5/sensors-17-02680-g001.jpg

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