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A linkage map of mouse Chromosome 1 using an interspecific cross segregating for the gld autoimmunity mutation
Authors:Mark L Watson  Peter D'Eustachio  Beverly A Mock  Alfred D Steinberg  Herbert C Morse III  Rebecca J Oakey  Thad A Howard  Julie M Rochelle  Michael F Seldin
Institution:(1) Department of Medicien and Department of Microbiogy, Duke University, 27710 Durham, North Carolina, USA;(2) Department of Biochemistry and Kaplan Cancer Center, New York University Medical Center, 10016 New York, New York, USA;(3) Laboratory of Genetics, National Cancer Institute, National Institutes of Health, 20892 Bethesda, Maryland, USA;(4) Cellular Immunology Section, National Institute of Arthritis and Musculoskeletal and Skin Diseases, National Institutes of Health, 20892 Bethesda, Maryland, USA;(5) Laboratory of Immunopathology, National Institute of Allergy and Infectious Disease, National Institutes of Health, 20892 Bethesda, Maryland, USA
Abstract:An interspecific backross was used to define a high resolution linkage map of mouse Chromosome (Chr) 1 and to analyze the segregation of the generalized lymphoproliferative disease (gld) mutation. Mice homozygous for gld have multiple features of autoimmune disease. Analysis of up to 428 progeny from the backcross (C3H/HeJ-gld x Mus spretus)F1 x C3H/HeJ-gld] established a map that spans 77.6 cM and includes 56 markers distributed over 34 ordered genetic loci. The gld mutation was mapped to a less than 1 cM segment on distal mouse Chr 1 using 357 gld phenotype-positive backcross mice. A second backcross, between the laboratory strains C57BL/6J and SWR/J, was examined to compare recombination frequency between selected markers on mouse Chr 1. Significant differences in crossover frequency were demonstrated between the interspecific backcross and the inbred laboratory cross for the entire interval studied. Sex difference in meiotic crossover frequency was also significant in the laboratory mouse cross. Two linkage groups known to be conserved between segments of mouse Chr 1 and the long arm of human Chrs 1 and 2 where further defined and a new conserved linkage group was identified that includes markers of distal mouse Chr 1 and human Chr 1, bands q32 to q42.
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