MAPPING OF AMINOACYLASE-1 AND BETA-GALACTOSIDASE-A TO HOMOLOGOUS REGIONS OF HUMAN-CHROMOSOME 3 AND MOUSE CHROMOSOME-9 SUGGESTS LOCATION OF ADDITIONAL GENES

Abstract

Conserved linkage groups were found on the X and autosomal chromosomes in several mammalian species. The identification of conserved chromosomal regions has potential for predicting gene location in mammals, particularly in humans. The genes for human aminoacylase-1 (ACY1, N-acylamino acid aminohydrolase, EC 3.5.1.14), an enzyme in amino acid metabolism, and .beta.-galactosidase-A (GLB1, EC 3.2.1.23), deficient in GM1-gangliosidosis, were assigned to human chromosome 3. Using human-mouse somatic cell hybrids segregating translocations of human chromosome 3, expression of both ACY1 and GLB1 correlated with the presence of the p21 .fwdarw. q21 region of chromosome 3. In a previous study, assignment of these genes to mouse chromosome 9 used mouse-Chinese hamster somatic cell hybrids, eliminating mouse chromosomes. To approximate the size of the conserved region in the mouse, experiments were performed with recombinant inbred mouse strains. An electrophoretic variant of ACY-1 in mouse strains was used to map the Acy-1 gene 10.7 map U from the .beta.-galactosidase locus. There is evidently a region of homology within the p21 .fwdarw. q21 region of human chromosome 3 and a segment of mouse chromosome 9. Since the mouse transferrin gene (Trf) is closely linked to the aminoacylase and .beta.-galactosidase loci, the human transferrin (TF) gene is on chromosome 3.