FERROCHELATASE STRUCTURAL MUTANT (FECH(M1PAS)) IN THE HOUSE MOUSE

被引：64

作者：

BOULECHFAR, S

LAMORIL, J

MONTAGUTELLI, X

GUENET, JL

DEYBACH, JC

NORDMANN, Y

DAILEY, H

GRANDCHAMP, B

DEVERNEUIL, H

机构：

[1] UNIV BORDEAUX 2,DEPT BIOCHIM MED & BIOL MOLEC,146 RUE LEO SAIGNAT,F-33076 BORDEAUX,FRANCE

[2] UNIV PARIS 07,FAC X BICHAT,GENET MOLEC LAB,F-75018 PARIS,FRANCE

[3] HOP LOUIS MOURIER,CTR FRANCAIS PORPHYRIES,SERV BIOCHIM,F-92701 COLOMBES,FRANCE

[4] INST PASTEUR,UNITE GENET MAMMIFERES,F-75724 PARIS 15,FRANCE

[5] UNIV GEORGIA,DEPT MICROBIOL,ATHENS,GA 30602

来源：

GENOMICS | 1993年 / 16卷 / 03期

关键词：

D O I：

10.1006/geno.1993.1242

中图分类号：

Q81 [生物工程学（生物技术）]; Q93 [微生物学];

学科分类号：

071005 ; 0836 ; 090102 ; 100705 ;

摘要：

The molecular basis of an inherited defect of ferrochelatase in mouse (Fechm1Pas/Fechm1Pas, described by Tutois et al., 1991, J. Clin. Invest. 88: 1730-1736) was investigated. cDNA clones encoding ferrochelatase, isolated by amplification of the mRNA from the liver of a mutant mouse using the polymerase chain reaction, were sequenced by the dideoxynucleotide chain-termination method. All the clones carried a T to A transversion at nucleotide 293, leading to a methionine to lysine substitution at position 98 in the protein (mutation M98K). Hybridization with allele-specific oligonucleotides (ASOs) confirmed the mutation at the cDNA and genomic levels. Finally, expression of the mutant ferrochelatase protein in E. coli demonstrated a marked deficiency in activity in agreement with the activity of the deficient enzyme in vivo. This Fechm1Pas/Fechm1Pas mutant mouse represents a useful model for studying the pathophysiological feature of the human disease and the first accessible model for gene therapy in the field of porphyrias. © 1993 Academic Press. All rights reserved.

引用

页码：645 / 648

页数：4

共 18 条

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