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细胞动力学塑造冠状病毒的重组频率。

Cellular dynamics shape recombination frequency in coronaviruses.

机构信息

Department of Pathology, Microbiology, and Immunology, University of California Davis School of Veterinary Medicine, Davis, California, United States of America.

出版信息

PLoS Pathog. 2024 Sep 27;20(9):e1012596. doi: 10.1371/journal.ppat.1012596. eCollection 2024 Sep.

Abstract

Coronavirus genomes have evolutionary histories shaped extensively by recombination. Yet, how often recombination occurs at a cellular level, or the factors that regulate recombination rates, are poorly understood. Utilizing experimental co-infections with pairs of genetically distinct coronaviruses, we found that recombination is both frequent and rare during coinfection. Recombination occurred in every instance of co-infection yet resulted in relatively few recombinant RNAs. By integrating a discrete-time Susceptible-Infected-Removed (SIR) model, we found that rates of recombination are determined primarily by rates of cellular co-infection, rather than other possible barriers such as RNA compartmentalization. By staggering the order and timing of infection with each virus we also found that rates of co-infection are themselves heavily influenced by genetic and ecological mechanisms, including superinfection exclusion and the relative fitness of competing viruses. Our study highlights recombination as a potent yet regulated force: frequent enough to ensure a steady influx of genetic variation but also infrequent enough to maintain genomic integrity. As recombination is thought to be an important driver of host-switching and disease emergence, our study provides new insights into the factors that regulate coronavirus recombination and evolution more broadly.

摘要

冠状病毒基因组的进化历史受到广泛重组的影响。然而,细胞水平上重组发生的频率以及调节重组率的因素还了解甚少。利用两对遗传上不同的冠状病毒的实验性共同感染,我们发现,在共感染过程中重组既频繁又罕见。重组发生在每次共感染中,但导致的重组 RNA 相对较少。通过整合离散时间的易感染-感染-清除(SIR)模型,我们发现,重组率主要由细胞共感染率决定,而不是 RNA 区隔等其他可能的障碍。通过错开每种病毒的感染顺序和时间,我们还发现,共感染率本身也受到遗传和生态机制的严重影响,包括超感染排斥和竞争病毒的相对适应性。我们的研究强调了重组是一种强大但受调控的力量:它的频率足以确保持续不断的遗传变异输入,但又不足以维持基因组的完整性。由于重组被认为是宿主转换和疾病出现的重要驱动因素,因此我们的研究为更广泛地调节冠状病毒重组和进化的因素提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/748c/11463787/12fd4621ef8d/ppat.1012596.g001.jpg

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