综合功能基因组分析确定了欧洲海鲈抗病性主要数量性状位点潜在的调控变异。

Integrated functional genomic analysis identifies regulatory variants underlying a major QTL for disease resistance in European sea bass.

作者信息

Mukiibi Robert, Ferraresso Serena, Franch Rafaella, Peruzza Luca, Dalla Rovere Giulia, Babbucci Massimiliano, Bertotto Daniela, Toffan Anna, Pascoli Francesco, Faggion Sara, Peñaloza Carolina, Tsigenopoulos Costas S, Houston Ross D, Bargelloni Luca, Robledo Diego

机构信息

The Roslin Institute and Royal (Dick), University of Edinburgh, Edinburgh, EH25 9RG, UK.

Department of Comparative Biomedicine and Food Science, University of Padova, Legnaro, 35020, Italy.

出版信息

BMC Biol. 2025 Mar 11;23(1):75. doi: 10.1186/s12915-025-02180-4.

DOI:10.1186/s12915-025-02180-4

PMID:40069747

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC11899128/

Abstract

BACKGROUND

Viral nervous necrosis (VNN) is an important viral disease threatening global aquaculture sustainability and affecting over 50 farmed and ecologically important fish species. A major QTL for resistance to VNN has been previously detected in European sea bass, but the underlying causal gene(s) and mutation(s) remain unknown. To identify the mechanisms and genetic factors underpinning resistance to VNN in European sea bass, we employed integrative analyses of multiple functional genomics assays in European sea bass.

RESULTS

The estimated heritability of VNN resistance was high (h ~ 0.40), and a major QTL explaining up to 38% of the genetic variance of the trait was confirmed on chromosome 3, with individuals with the resistant QTL genotype showing a 90% survivability against a VNN outbreak. Whole-genome resequencing analyses narrowed the location of this QTL to a small region containing 4 copies of interferon alpha inducible protein 27-like 2A (IFI27L2A) genes, and one copy of the interferon alpha inducible protein 27-like 2 (IFI27L2) gene. RNA sequencing revealed a clear association between the QTL genotype and the expression of two of the IFI27L2A genes, and the IFI27L2 gene. Integration with chromatin accessibility and histone modification data pinpointed two SNPs in active regulatory regions of two of these genes (IFI27L2A and IFI27L2), and transcription factor binding site gains for the resistant alleles were predicted. These alleles, particularly the SNP variant CHR3:10,077,301, exhibited higher frequencies (0.55 to 0.77) in Eastern Mediterranean Sea bass populations, which show considerably higher levels of resistance to VNN, as compared to susceptible West Mediterranean and Atlantic populations (0.15-0.25).

CONCLUSIONS

The SNP variant CHR3:10,077,301, through modulation of IFI27L2 and IFI27L2A genes, is likely the causative mutation underlying resistance to VNN in European sea bass. This is one of the first causative mutations discovered for disease resistance traits in fish and paves the way for marker-assisted selection as well as biotechnological approaches to enhance resistance to VNN in European sea bass and other susceptible species.

摘要

背景

病毒性神经坏死（VNN）是一种重要的病毒性疾病，威胁着全球水产养殖的可持续性，影响着50多种养殖和具有生态重要性的鱼类。先前在欧洲海鲈中检测到一个抗VNN的主要数量性状基因座（QTL），但其潜在的因果基因和突变仍不清楚。为了确定欧洲海鲈抗VNN的机制和遗传因素，我们对欧洲海鲈进行了多种功能基因组学分析的综合研究。

结果

VNN抗性的估计遗传力较高（h约为0.40），并且在3号染色体上确认了一个主要QTL，该QTL解释了该性状高达38%的遗传变异，具有抗性QTL基因型的个体在VNN爆发时显示出90%的存活率。全基因组重测序分析将该QTL的位置缩小到一个小区域，该区域包含4个干扰素α诱导蛋白27样2A（IFI27L2A）基因拷贝和1个干扰素α诱导蛋白27样2（IFI27L2）基因拷贝。RNA测序揭示了QTL基因型与两个IFI27L2A基因和IFI27L2基因的表达之间存在明显关联。与染色质可及性和组蛋白修饰数据的整合确定了其中两个基因（IFI27L2A和IFI27L2）的活性调控区域中的两个单核苷酸多态性（SNP），并预测了抗性等位基因的转录因子结合位点增加。这些等位基因，特别是SNP变体CHR3:10,077,301，在地中海东部海鲈种群中表现出较高的频率（0.55至0.77），与易感的西地中海和大西洋种群（0.15 - 0.25）相比，它们对VNN的抗性水平要高得多。