Inheritance of the F4ab, F4ac and F4ad E. coli receptors in swine and examination of four candidate genes for F4acR

• Published in: Journal of animal breeding and genetics (1986) Vol. 122; no. s1; pp. 5 - 14
• Main Authors: Python, P., Jörg, H., Neuenschwander, S., Asai-Coakwell, M., Hagger, C., Bürgi, E., Bertschinger, H.U., Stranzinger, G., Vögeli, P.
• Format: Journal Article
• Language: English
• Published: Berlin, Germany Blackwell Verlag GmbH 01.04.2005; Blackwell Publishing Ltd
• Subjects: Animals; Antigens, Bacterial - genetics; Antigens, Bacterial - metabolism; Bacteria; Bacterial Adhesion - genetics; Base Sequence; Chromosome Mapping - veterinary; Chromosomes, Mammalian - genetics; DNA Primers; DNA, Complementary - genetics; Escherichia coli; Escherichia coli Infections - genetics; Escherichia coli Infections - microbiology; Escherichia coli Infections - veterinary; Escherichia coli Proteins - genetics; Escherichia coli Proteins - metabolism; Fimbriae Proteins - genetics; Fimbriae Proteins - metabolism; Genes; Genetic Predisposition to Disease - genetics; Genotype & phenotype; Heredity; Hogs; Intestines - microbiology; Lod Score; Molecular Sequence Data; Pedigree; Phenotype; Reverse Transcriptase Polymerase Chain Reaction - veterinary; Sequence Analysis, DNA - veterinary; Sus scrofa; Swine; Swine Diseases - genetics; Swine Diseases - microbiology
• ISSN: 0931-2668; 1439-0388
• DOI: 10.1111/j.1439-0388.2005.00490.x

Summary Susceptibility to enterotoxigenic Escherichia coli with fimbriae F4ac is dominantly inherited in the pig. A three‐generation pedigree was created to refine the position of F4acR on chromosome 13 comprising 202 pigs: eight parents, 18 F1 and 176 F2 pigs. The 17‐point analysis indicates that F4acR lies between Sw207 and S0283. Recombinant offspring specify that the most probable order is Sw207–S0075–F4acR–Sw225–S0283. We observed six phenotypes for the three fimbrial variants F4ab, F4ac and F4ad. The two missing phenotypes F4abR−/F4acR+/F4adR+ and F4abR−/F4acR+/F4adR− indicate that pigs susceptible to F4ac are always susceptible to F4ab. Furthermore, a weak and a strong adhesion of F4ab and F4ad bacteria was observed. The weak receptor F4abR (F4abRw) was present only in pigs devoid of the receptor F4acR (F4abR+/F4acR−). In contrast, in pigs with the phenotype F4abR+/F4acR+, F4ab bacteria adhered to the majority of enterocytes. F4abRw constitutes a frequently observed phenotype whose inheritance is still unclear. Strong adhesion of F4ab and F4ac bacteria is most likely influenced by the same receptor that we name F4bcR. The number of F4ad bacteria that adhered to enterocytes was very variable in the adhesion test. Moreover, expression of F4adR was independent of age. Our segregation analyses indicated a dominant inheritance of F4adR, although the number of susceptible pigs was smaller than expected. We examined four genes as candidates for the F4acR locus: the transferrin receptor gene (TFRC) and three genes members of the glucosyl/galactosyltransferase family (B3GnT5, B3GALT3 and B4GALT4). Comparison of sequences from resistant and homozygous susceptible F4ac pigs did not reveal any causative single nucleotide polymorphism in the four genes. Two silent mutations at the positions 295 (C/T) and 313 (T/C) in B3GALT3 were found. Using the somatic cell hybrid panel, B3GnT5 and B3GALT3 were assigned to the chromosomal region SSC13q23‐q41. No mutations were found in the cDNA sequences of these genes associated with the F4acR genotypes.