Publication | Closed Access
Molecular Analysis of the Hotspot of Recombination in the Murine Major Histocompatibility Complex
154
Citations
34
References
1986
Year
HistocompatibilityGeneticsHla ImmunogeneticsImmunologyMolecular BiologyAntigen ProcessingMolecular GeneticsDna SequencesImmunogeneticsMolecular AnalysisKnockout MouseE Beta GeneGene ExpressionFunctional GenomicsCell BiologyNatural SciencesSerological AssaysImmunoglobulin ERecombination DynamicMedicine
Biological and serological assays have been used to define four subregions for the I region of the major histocompatibility complex (MHC) in the order I-A, I-B, I-J, and I-E. The I-J subregion presumably encodes the I-J polypeptide of the elusive T-cell suppressor factors. Restriction enzyme site polymorphisms and DNA sequence analyses of the I region from four recombinant mouse strains were used to localize the putative I-B and I-J subregions to a 1.0-kilobase (kb) region within the E beta gene. Sequencing this region from E beta clones derived from the two mouse strains: B10.A(3R), I-Jb and B10.A(5R), I-Jk initially used to define the I-J subregion revealed that these regions are identical, hence the distinct I-Jb and I-Jk molecules cannot be encoded by this DNA. In addition, the DNA sequence data also refute the earlier mapping of the I-B subregion. Analysis of the DNA sequences of three parental and four I region recombinants reveals that the recombinant events in three of the recombinant strains occurred within a 1-kb region of DNA, supporting the proposition that a hotspot for recombination exists in the I region. The only striking feature of this hotspot is a tetramer repeat (AGGC)n that shows 80 percent homology to the minisatellite sequence which may facilitate recombination in human chromosomes.
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