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首页> 外文期刊>Scientific reports. >Oncogenic Mutations Differentially Affect Bax Monomer, Dimer, and Oligomeric Pore Formation in the Membrane
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Oncogenic Mutations Differentially Affect Bax Monomer, Dimer, and Oligomeric Pore Formation in the Membrane

机译:致癌突变差异地影响膜中的Bax单体,二聚体和低聚孔形成

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Dysfunction of Bax, a pro-apoptotic regulator of cellular metabolism is implicated in neurodegenerative diseases and cancer. We have constructed the first atomistic models of the Bax oligomeric pore consisting with experimental residue-residue distances. The models are stable, capturing well double electron-electron resonance (DEER) spectroscopy measurements and provide structural details in line with the DEER data. Comparison with the latest experimental results revealed that our models agree well with both Bax and Bak pores, pointed to a converged structural arrangement for Bax and Bak pore formation. Using multi-scale molecular dynamics simulations, we probed mutational effects on Bax transformation from monomer?→?dimer?→?membrane pore formation at atomic resolution. We observe that two cancer-related mutations, G40E and S118I, allosterically destabilize the monomer and stabilize an off-pathway swapped dimer, preventing productive pore formation. This observation suggests a mechanism whereby the mutations may work mainly by over-stabilizing the monomer?→?dimer transformation toward an unproductive off-pathway swapped-dimer state. Our observations point to misfolded Bax states, shedding light on the molecular mechanism of Bax mutation-elicited cancer. Most importantly, the structure of the Bax pore facilitates future study of releases cytochrome C in atomic detail.
机译:Bax的功能障碍,细胞代谢的促细胞凋亡调节剂涉及神经变性疾病和癌症。我们构建了由实验残留物残留距离组成的Bax低聚孔的第一原子模型。该模型是稳定的,捕获双电子谐振(鹿)光谱测量的稳定性,并根据鹿数据提供结构细节。与最新实验结果的比较透露,我们的模型与Bax和Bak孔隙吻合良好,指向Bax和Bak孔形成的融合结构安排。采用多尺度分子动力学模拟,我们探测了对单体α→二聚体的Bax转化的突变效应?→α→膜孔形成以原子分辨率。我们观察到两种癌症相关的突变,G40E和S118i,体变得破坏性地稳定单体并稳定偏移型交换二聚体,防止生产孔隙形成。该观察表明该突变可以主要通过过度稳定单体α→α→二聚体转化朝向非生产性脱离途径交换二聚体状态的机制。我们的观察结果指出了错误的Bax状态,脱落在Bax突变引发癌症的分子机制上。最重要的是,Bax孔的结构促进了未来对原子细节中释放细胞色素C的研究。

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