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Inheritance of porcine receptors for enterotoxigenic Escherichia coli with 1 fimbriae F4ad and their relation to other F4 receptors 2

机译:带有1个菌毛F4ad的肠毒素大肠杆菌的猪受体的遗传及其与其他F4受体的关系2

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摘要

Enteric Escherichia coli infections are a highly relevant cause of disease and death in young pigs. Breeding genetically resistant pigs is an economical and sustainable method of prevention. Resistant pigs are protected against colonization of the intestine through the absence of receptors for the bacterial fimbriae, which mediate adhesion to the intestinal surface. The present work aimed at elucidation of the mode of inheritance of the F4ad receptor which according to former investigations appeared quite confusing. Intestines of 489 pigs of an experimental herd were examined by a microscopic adhesion test modified in such a manner that four small intestinal sites instead of one were tested for adhesion of the fimbrial variant F4ad. Segregation analysis revealed that the mixed inheritance model explained our data best. The heritability of the F4ad phenotype was estimated to be 0.7±0.1. There are no relations to the strong receptors for variants F4ab and F4ac. Targeted matings allowed the discrimination between two F4ad receptors, that is, a fully adhesive receptor (F4adRFA) expressed on all enterocytes and at all small intestinal sites, and a partially adhesive receptor (F4adRPA) variably expressed at different sites and often leading to partial bacterial adhesion. In pigs with both F4ad receptors, the F4adRPA receptor is masked by the F4adRFA. The hypothesis that F4adRFA must be encoded by at least two complementary or epistatic dominant genes is supported by the Hardy-Weinberg equilibrium statistics. The F4adRPA receptor is inherited as a monogenetic dominant trait. A comparable partially adhesive receptor for variant F4ab (F4abRPA) was also observed but the limited data did not allow a prediction of the mode of inheritance. Pigs were therefore classified into one of eight receptor phenotypes: A1 (F4abRFA/F4acR+/F4adRFA); A2 (F4abRFA/F4acR+/F4adRPA); B (F4abRFA/F4acR+/F4adR-); C1 (F4abRPA/F4acR-/F4adRFA); C2 (F4abRPA/F4acR-/F4adRPA); D1 (F4abR-/F4acR-/F4adRFA); D2 (F4abR-/F4acR-/F4adRPA); E (F4abR-/F4acR-/F4adR-).
机译:肠道大肠杆菌感染是幼猪疾病和死亡的高度相关原因。育种具有遗传抗性的猪是一种经济,可持续的预防方法。通过不存在介导与肠道表面粘附的细菌菌毛受体,可以保护抗性猪免受肠道定植。目前的工作旨在阐明F4ad受体的遗传模式,根据以前的研究,该模式似乎很令人困惑。通过显微镜粘附试验对489只实验猪群的肠进行了检查,该试验经改良,其方式是测试四个小肠部位而不是一个小肠部位对纤维变异体F4ad的粘附性。隔离分析显示,混合继承模型可以最好地解释我们的数据。 F4ad表型的遗传力估计为0.7±0.1。与变体F4ab和F4ac的强受体无关。有针对性的交配可以区分两种F4ad受体,即在所有肠细胞和所有小肠部位表达的完全粘附受体(F4adRFA)和在不同部位变异表达的部分粘附受体(F4adRPA),通常导致部分细菌附着力。在同时具有两个F4ad受体的猪中,F4adRPA受体被F4adRFA掩盖。 Hardy-Weinberg平衡统计数据支持F4adRFA必须由至少两个互补或上位性显性基因编码的假设。 F4adRPA受体作为单基因显性性状遗传。还观察到了类似的部分F4ab的部分粘附受体(F4abRPA),但有限的数据无法预测遗传方式。因此,猪被分为八种受体表型之一:A1(F4abRFA / F4acR + / F4adRFA); A2(F4abRFA / F4acR + / F4adRPA); B(F4abRFA / F4acR + / F4adR-); C1(F4abRPA / F4acR- / F4adRFA); C2(F4abRPA / F4acR- / F4adRPA); D1(F4abR- / F4acR- / F4adRFA); D2(F4abR- / F4acR- / F4adRPA); E(F4abR- / F4acR- / F4adR-)。

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