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首页> 外文期刊>Journal of Animal Science >Genetic relationships of antibody response, viremia level, and weight gain in pigs experimentally infected with porcine reproductive and respiratory syndrome virus
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Genetic relationships of antibody response, viremia level, and weight gain in pigs experimentally infected with porcine reproductive and respiratory syndrome virus

机译:用猪生殖和呼吸综合征病毒实验感染猪抗体反应,病毒血症水平和体重增加的遗传关系

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Genetic and antigenic variability between Porcine Reproductive and Respiratory Syndrome Virus (PRRSV) isolates has encumbered vaccine development. Here, the genetic basis of PRRSV antibody response was assessed using data from experimental infection trials of commercial crossbred weaner pigs across with one of two distinct PRRSV isolates, NVSL-97-7895 (similar to 750 pigs) and KS-2006-72109 (similar to 450 pigs). Objectives were to estimate the genetic parameters of antibody response, measured as the sample to positive ratio (S:P) of PRRSV N-protein specific IgG in serum at 42 d post infection (dpi); assess the relationship of S: P at 42 dpi with serum viremia and growth under infection; and identify genomic regions associated with S: P at 42 dpi. Estimates of heritability of S: P at 42 dpi for NVSL and KS06 were 0.31 +/- 0.09 and 0.40 +/- 0.10 and appeared to be under similar genetic control (genetic correlation 0.73 +/- 0.39). Estimates of genetic correlations of S: P were generally weak with viral load (NVSL: -0.20 +/- 0.18; KS06: -0.69 +/- 0.20), measured as area under the curve of log 10 serum viremia from 0 to 21 dpi, and with weight gain (WG) from 0 to 42 dpi (NVSL: -0.38 +/- 0.19; KS06: -0.08 +/- 0.25). However, genetic correlations of S:P at 42 dpi with daily serum viremia and with 3-d WG revealed dynamic relationships, with S: P at 42 dpi having the strongest negative genetic correlations with daily viremia when IgG production starts (10-20 dpi), and negative genetic correlations with WG early after infection but positive later on. This suggests that animals that placed more emphasis on immune response early in infection reaped benefits of that later in infection by more effectively clearing the virus. The WUR10000125 SNP on SSC4, previously associated with response to PRRSV, did not have a significant effect on S: P at 42 dpi (P 0.05) but genotype-specific genetic correlations of S: P with daily viremia and 3-d WG suggested that the lower WG of pigs with the unfavorable AA WUR10000125 genotype may be due to their utilization of a more energetically costly host response compared to pigs with the favorable genotype. Genome-wide association studies identified three SNPs in the Major Histocompatibility Complex associated with S: P that explained similar to 10 (NVSL) and 45% (KS06) of the genetic variance but were not associated with viremia or WG. In conclusion, antibody response to PRRSV infection is a possible biomarker for improved host response to PRRSV infection.
机译:猪繁殖与呼吸综合征病毒(PRRSV)之间的基因和抗原变异株已拖累疫苗开发。这里,PRRSV抗体应答的遗传基础横跨使用从商业杂种断奶猪的实验性感染试验中的数据进行了评估具有两个不同PRRSV分离物的一个,NVSL-97-7895(类似于750个猪)和KS-2006-72109(类似于到450个猪)。目标是估计抗体应答的遗传参数,如样品阳性率测量:在42 d感染后(dpi)的血清中PRRSV的N-蛋白特异性IgG的(S P);评估S的关系:在42 dpi的分辨率下感染血清病毒血症和生长P:在42 DPI,P:和识别与S相关的基因组区域。 S的遗传力的估计值:在42 DPI为NVSL和KS06 P含量0.31 +/- 0.09和0.40 +/- 0.10和似乎是相似的遗传控制(遗传相关0.73 +/- 0.39)下。 S的遗传相关的估计:P总体上与病毒载量弱(NVSL:-0.20±0.18; KS06:-0.69 +/- 0.20),为区域日志10血清病毒血症的曲线下测量从0到21 dpi的和与体重增加(WG)0至42 DPI(NVSL:-0.38 +/- 0.19; KS06:-0.08 +/- 0.25)。然而,S的遗传相关:在42 dpi的每日血清病毒血症,并用3-d WG P揭示的动态关系,其中S:具有与日常病毒血症最强负遗传相关p在42 DPI时IgG产生开始(10-20 dpi的),以及感染,但对积极后来经过年初WG负遗传相关。这表明,动物在感染的早期感染放在免疫反应更强调的是获得收益以后通过更有效地清除病毒。在WUR10000125 SNP上SSC4,先前响应于PRRSV相关联,并没有对S上显著效果:在42 dpi的P(P> 0.05)S的但基因型特异性遗传相关:P每日病毒血症和3- d WG建议与不利AA基因型WUR10000125猪的下WG可能是由于它们的更大力昂贵的宿主反应的利用率相比具有有利的基因型猪。全基因组关联研究中鉴定的主要组织相容性复合物与S相关三个位:P讲解类似于遗传变异的10(NVSL)和45%(KS06),但没有用病毒血症或WG相关联。总之,为了PRRSV感染的抗体应答是针对改进的宿主响应于PRRSV感染的可能的生物标志物。

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