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分子动力学模拟捕捉到了牛朊病毒蛋白在酸性pH值下的错误折叠。

Molecular dynamics simulations capture the misfolding of the bovine prion protein at acidic pH.

作者信息

Cheng Chin Jung, Daggett Valerie

机构信息

Department of Bioengineering, University of Washington, Seattle WA 98195-5013, USA.

出版信息

Biomolecules. 2014 Feb 10;4(1):181-201. doi: 10.3390/biom4010181.

Abstract

Bovine spongiform encephalopathy (BSE), or mad cow disease, is a fatal neurodegenerative disease that is transmissible to humans and that is currently incurable. BSE is caused by the prion protein (PrP), which adopts two conformers; PrPC is the native innocuous form, which is α-helix rich; and PrPSc is the β-sheet rich misfolded form, which is infectious and forms neurotoxic species. Acidic pH induces the conversion of PrPC to PrPSc. We have performed molecular dynamics simulations of bovine PrP at various pH regimes. An acidic pH environment induced conformational changes that were not observed in neutral pH simulations. Putative misfolded structures, with nonnative β-strands formed in the flexible N-terminal domain, were found in acidic pH simulations. Two distinct pathways were observed for the formation of nonnative β-strands: at low pH, hydrophobic contacts with M129 nucleated the nonnative β-strand; at mid-pH, polar contacts involving Q168 and D178 facilitated the formation of a hairpin at the flexible N-terminus. These mid- and low pH simulations capture the process of nonnative β-strand formation, thereby improving our understanding of how PrPC misfolds into the β-sheet rich PrPSc and how pH factors into the process.

摘要

牛海绵状脑病(BSE),即疯牛病,是一种致命的神经退行性疾病,可传染给人类且目前无法治愈。BSE由朊病毒蛋白(PrP)引起,该蛋白有两种构象;PrPC是天然无害形式,富含α-螺旋;而PrPSc是富含β-折叠的错误折叠形式,具有传染性并形成神经毒性物质。酸性pH会诱导PrPC转化为PrPSc。我们在不同pH条件下对牛PrP进行了分子动力学模拟。酸性pH环境诱导了在中性pH模拟中未观察到的构象变化。在酸性pH模拟中发现了推定的错误折叠结构,在柔性N端结构域形成了非天然β链。观察到形成非天然β链有两条不同途径:在低pH下,与M129的疏水接触使非天然β链成核;在中等pH下,涉及Q168和D178的极性接触促进了柔性N端发夹结构的形成。这些中等和低pH模拟捕捉了非天然β链形成过程,从而增进了我们对PrPC如何错误折叠成富含β-折叠的PrPSc以及pH如何影响这一过程的理解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/2aa1/4030982/ac6c2774824a/biomolecules-04-00181-g001.jpg

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