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随机键动力学促进疟原虫在入侵时于红细胞膜上的定位。

Stochastic bond dynamics facilitates alignment of malaria parasite at erythrocyte membrane upon invasion.

机构信息

Theoretical Physics of Living Matter, Institute of Biological Information Processing and Institute for Advanced Simulation, Forschungszentrum Jülich, Jülich, Germany.

出版信息

Elife. 2020 May 18;9:e56500. doi: 10.7554/eLife.56500.

Abstract

Malaria parasites invade healthy red blood cells (RBCs) during the blood stage of the disease. Even though parasites initially adhere to RBCs with a random orientation, they need to align their apex toward the membrane in order to start the invasion process. Using hydrodynamic simulations of a RBC and parasite, where both interact through discrete stochastic bonds, we show that parasite alignment is governed by the combination of RBC membrane deformability and dynamics of adhesion bonds. The stochastic nature of bond-based interactions facilitates a diffusive-like re-orientation of the parasite at the RBC membrane, while RBC deformation aids in the establishment of apex-membrane contact through partial parasite wrapping by the membrane. This bond-based model for parasite adhesion quantitatively captures alignment times measured experimentally and demonstrates that alignment times increase drastically with increasing rigidity of the RBC membrane. Our results suggest that the alignment process is mediated simply by passive parasite adhesion.

摘要

疟原虫在疾病的血液阶段侵入健康的红细胞(RBC)。尽管寄生虫最初以随机方向附着在 RBC 上,但它们需要将其顶端朝向膜,以便开始入侵过程。通过使用红细胞和寄生虫的流体动力学模拟,其中两者通过离散的随机键相互作用,我们表明寄生虫的排列受 RBC 膜的可变形性和粘附键动力学的组合控制。基于键的相互作用的随机性促进了寄生虫在 RBC 膜上的扩散样再取向,而 RBC 变形则通过膜对寄生虫的部分包裹来帮助建立顶端-膜接触。这种基于键的寄生虫粘附模型定量地捕获了实验测量的排列时间,并表明随着 RBC 膜刚性的增加,排列时间急剧增加。我们的结果表明,排列过程仅通过被动寄生虫附着来介导。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/333f/7269671/224a4c7a3248/elife-56500-fig1.jpg

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