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A structural gene (Hdc-s) for mouse kidney histidine decarboxylase
Authors:S A M Martin  Grahame Bulfield
Institution:(1) Department of Genetics, University of Edinburgh, West Mains Road, EH9 3JN Edinburgh, U.K.;(2) Genetics Group, Agricultural and Food Research Council's Poultry Research Centre, EH25 9PS Roslin, Midlothian, U.K.
Abstract:The concentration of mouse kidney histidine decarboxylase (HDC) is modulated by estrogen, testosterone, and thyroxine in a tissue-specific manner. Variation in HDC levels between strains of mice can be used to investigate the genetic regulation of (i) enzyme structure, (ii) tissue specific expression, and (iii) induction and repression by hormones. Variation in the structure of HDC between different inbred strains of mice affecting its K m for the cofactor pyridoxal-5prime-phosphate (PLP) and its heat stability has been discovered. The alternative phenotypes are additively inherited in crosses and the heat stability difference is due to alleles of a single structural gene, Hdc-s, which segregate among the BXD and BXH recombinant inbred strains. The allele Hdc-s b determines the heat-stable phenotype (C57BL substrains), and the allele Hdc-s d the heat-labile phenotype (DBA/2 and C3H/He strains). The alleles of the structural gene cosegregate with alleles of a regulatory gene previously named Hdc (determining kidney enzyme concentration); there were no recombinants among 38 RI strains. Therefore the two loci are less than 0.685 cM apart and comprise part of the HDC gene complex, Hdc], on chromosome 2 of the mouse.This work was supported in part by an SERC studentship to S.A.M. and an MRC project grant to G.B.
Keywords:mouse  kidney  histidine decarboxylase  structural gene
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