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袋獾与一种传染性癌症之间协同进化的基因组间特征

Intergenomic signatures of coevolution between Tasmanian devils and an infectious cancer.

作者信息

Gallinson Dylan G, Kozakiewicz Christopher P, Rautsaw Rhett M, Beer Marc A, Ruiz-Aravena Manuel, Comte Sebastien, Hamilton David G, Kerlin Douglas H, McCallum Hamish I, Hamede Rodrigo, Jones Menna E, Storfer Andrew, McMinds Ryan, Margres Mark J

机构信息

Department of Integrative Biology, University of South Florida, Tampa, FL 33620.

College of Public Health, University of South Florida, Tampa, FL 33620.

出版信息

Proc Natl Acad Sci U S A. 2024 Mar 19;121(12):e2307780121. doi: 10.1073/pnas.2307780121. Epub 2024 Mar 11.

Abstract

Coevolution is common and frequently governs host-pathogen interaction outcomes. Phenotypes underlying these interactions often manifest as the combined products of the genomes of interacting species, yet traditional quantitative trait mapping approaches ignore these intergenomic interactions. Devil facial tumor disease (DFTD), an infectious cancer afflicting Tasmanian devils (), has decimated devil populations due to universal host susceptibility and a fatality rate approaching 100%. Here, we used a recently developed joint genome-wide association study (i.e., co-GWAS) approach, 15 y of mark-recapture data, and 960 genomes to identify intergenomic signatures of coevolution between devils and DFTD. Using a traditional GWA approach, we found that both devil and DFTD genomes explained a substantial proportion of variance in how quickly susceptible devils became infected, although genomic architectures differed across devils and DFTD; the devil genome had fewer loci of large effect whereas the DFTD genome had a more polygenic architecture. Using a co-GWA approach, devil-DFTD intergenomic interactions explained ~3× more variation in how quickly susceptible devils became infected than either genome alone, and the top genotype-by-genotype interactions were significantly enriched for cancer genes and signatures of selection. A devil regulatory mutation was associated with differential expression of a candidate cancer gene and showed putative allele matching effects with two DFTD coding sequence variants. Our results highlight the need to account for intergenomic interactions when investigating host-pathogen (co)evolution and emphasize the importance of such interactions when considering devil management strategies.

摘要

协同进化很常见,并且常常决定宿主与病原体相互作用的结果。这些相互作用背后的表型通常表现为相互作用物种基因组的组合产物,但传统的数量性状定位方法忽略了这些基因组间的相互作用。袋獾面部肿瘤病(DFTD)是一种感染袋獾的传染性癌症,由于宿主普遍易感性和接近100%的死亡率,已经使袋獾种群数量大幅减少。在这里,我们使用了最近开发的全基因组联合关联研究(即共GWAS)方法、15年的标记重捕数据以及960个基因组,来识别袋獾和DFTD之间协同进化的基因组间特征。使用传统的全基因组关联方法,我们发现袋獾和DFTD的基因组都解释了易感袋獾感染速度差异的很大一部分方差,尽管袋獾和DFTD的基因组结构不同;袋獾基因组中具有较大效应的位点较少,而DFTD基因组具有更多的多基因结构。使用共GWAS方法,袋獾 - DFTD基因组间的相互作用解释的易感袋獾感染速度差异比单独任何一个基因组多约3倍,并且顶级的基因型 - 基因型相互作用在癌症基因和选择特征方面显著富集。一个袋獾调控突变与一个候选癌症基因的差异表达相关,并与两个DFTD编码序列变体表现出假定的等位基因匹配效应。我们的结果强调了在研究宿主 - 病原体(协同)进化时考虑基因组间相互作用的必要性,并强调了在考虑袋獾管理策略时这种相互作用的重要性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ebb0/10962979/eabe9f8d7928/pnas.2307780121fig01.jpg

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