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与含Pro564的HIF-1α的VHL介导的蛋白质破坏基序融合的前半胱天冬酶-3的低氧特异性细胞毒性机制。

Mechanism of hypoxia-specific cytotoxicity of procaspase-3 fused with a VHL-mediated protein destruction motif of HIF-1alpha containing Pro564.

作者信息

Harada Hiroshi, Kizaka-Kondoh Shinae, Hiraoka Masahiro

机构信息

Department of Radiation Oncology and Image-Applied Therapy, Kyoto University Graduate School of Medicine, 54 Kawahara-cho, Shogoin, Sakyo-ku, Kyoto 606-8507, Japan.

出版信息

FEBS Lett. 2006 Oct 16;580(24):5718-22. doi: 10.1016/j.febslet.2006.09.025. Epub 2006 Sep 22.

DOI:10.1016/j.febslet.2006.09.025
PMID:17010341
Abstract

Under normoxic conditions the alpha-subunit of hypoxia-inducible factor (HIF-1alpha) protein is targeted for degradation by the von Hippel-Lindau (VHL) tumor suppressor protein acting as an E3 ubiquitin ligase. Recently, we developed a hypoxia-targeting protein, TOP3, which consisted of procaspase-3 with the VHL-mediated protein destruction motif of HIF-1alpha. This design enables procaspase-3 to be regulated similarly with HIF-1alpha, being degraded under normoxia while stabilized under hypoxia. Furthermore, stabilized TOP3 was cleaved by the hypoxic stress-induced endogenous caspases and thus the procaspase-3 was converted to active caspase-3 specifically under hypoxic conditions. These data demonstrated that the VHL-mediated protein destruction motif of HIF-1alpha endowed procaspase-3 with hypoxia-specific cytotoxicity.

摘要

在常氧条件下,缺氧诱导因子(HIF-1α)蛋白的α亚基会被作为E3泛素连接酶的冯·希佩尔-林道(VHL)肿瘤抑制蛋白靶向降解。最近,我们开发了一种缺氧靶向蛋白TOP3,它由procaspase-3和HIF-1α的VHL介导的蛋白破坏基序组成。这种设计使得procaspase-3能够与HIF-1α受到类似的调控,在常氧条件下被降解,而在缺氧条件下则稳定存在。此外,稳定的TOP3会被缺氧应激诱导的内源性半胱天冬酶切割,因此procaspase-3会在缺氧条件下特异性地转化为活性半胱天冬酶-3。这些数据表明,HIF-1α的VHL介导的蛋白破坏基序赋予了procaspase-3缺氧特异性细胞毒性。

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