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On the Effect of Thermodynamic Equilibrium on the Assembly Efficiency of Complex Multi-Layered Virus-Like Particles (VLP): the Case of Rotavirus VLP

机译:热力学平衡对复杂多层病毒样颗粒(VLP)装配效率的影响:轮状病毒VLP的案例

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Previous studies have reported the production of malformed virus-like-particles (VLP) in recombinant host systems. Here we computationally investigate the case of a large triple-layered rotavirus VLP (RLP). In vitro assembly, disassembly and reassembly data provides strong evidence of microscopic reversibility of RLP assembly. Light scattering experimental data also evidences a slow and reversible assembly untypical of kinetic traps, thus further strengthening the fidelity of a thermodynamically controlled assembly. In silico analysis further reveals that under favourable conditions particles distribution is dominated by structural subunits and completely built icosahedra, while other intermediates are present only at residual concentrations. Except for harshly unfavourable conditions, assembly yield is maximised when proteins are provided in the same VLP protein mass composition. The assembly yield decreases abruptly due to thermodynamic equilibrium when the VLP protein mass composition is not obeyed. The latter effect is more pronounced the higher the Gibbs free energy of subunit association is and the more complex the particle is. Overall this study shows that the correct formation of complex multi-layered VLPs is restricted to a narrow range of association energies and protein concentrations, thus the choice of the host system is critical for successful assembly. Likewise, the dynamic control of intracellular protein expression rates becomes very important to minimize wasted proteins.
机译:先前的研究报告了重组宿主系统中畸形病毒样颗粒(VLP)的产生。在这里,我们通过计算研究大型三层轮状病毒VLP(RLP)的情况。体外组装,拆卸和重新组装数据为RLP组装的微观可逆性提供了有力证据。光散射实验数据还证明了缓慢而可逆的装配是典型的动力学陷阱,因此进一步增强了热力学控制装配的保真度。硅计算机分析进一步表明,在有利条件下,颗粒分布主要由结构亚基和完全建成的二十头蛇组成,而其他中间体仅以残留浓度存在。除了极度不利的条件外,当在相同的VLP蛋白质质量组成中提供蛋白质时,组装产量将最大化。当不遵守VLP蛋白质质量组成时,由于热力学平衡,装配产量突然降低。亚基缔合的吉布斯自由能越高,粒子越复杂,后一种效应越明显。总体而言,这项研究表明,复杂多层VLP的正确形成仅限于窄范围的缔合能和蛋白质浓度,因此宿主系统的选择对于成功组装至关重要。同样,动态控制细胞内蛋白质的表达速度对于减少蛋白质的浪费非常重要。

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