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Cloning and sequence analysis of a rat liver cDNA coding for a phenobarbital-inducible microheterogenous cytochrome P-450 variant: regulation of its messenger level by xenobiotics
Authors:I R Phillips  E A Shephard  A Ashworth  B R Rabin
Institution:Department of Biochemistry, University College London, Gower Street, London, WC1E 6BT U.K. Tel. (01) 387-7050, Ext. 290
Abstract:A rat liver cDNA library was prepared from total polyribosomal poly(A)+ RNA extracted from phenobarbital-treated animals. A cDNA clone coding for a phenobarbital-inducible cytochrome P-450 (PB P-450) was identified by differential colony hybridization to cDNAs synthesized from liver poly(A)+RNAs isolated from phenobarbital-treated rats for positive selection and cDNAs from either untreated rats or beta-naphthoflavone-treated rats as negative controls, followed by hybrid-selected translation and analysis of the translation products by immunoprecipitation. As the cloning and screening strategies involve no prior enrichment for specific mRNAs, they also permit the identification of sequences coding for phenobarbital-induced proteins other than cytochromes P-450. This relatively straightforward approach is generally applicable to the molecular cloning of sequences coding for other inducible cytochromes P-450. Nucleic acid sequencing data indicated that the cloned PB P-450 cDNA codes for a cytochrome P-450 variant designated P-450e(U.C.)] that is very similar, but not identical, to P-450e. Sequence analysis of the section of cDNA specifying the 3'-non-coding region of the mRNA revealed that it lacked the usual poly(A) addition site signal sequence but contained three inverted repeat structures. Solution hybridization analysis demonstrated that PB P-450 mRNA is increased 20-fold by phenobarbital treatment and decreased 3-fold by beta-naphthoflavone treatment.
Keywords:Recombinant DNA  mRNA induction  drug metabolizing proteins  nucleic acid hybridization  immunoprecipitation  poly(A)-addition site signal sequence  inverted repeats  bp  base pairs  cDNA  DNA complementary to mRNA  EtBr  ethidium bromide  kb  kilobase pairs  PB P-450  P-450e(U  C  )  a microheterogeneous variant of cytochrome P-450e present in Sprague-Dawley rats of the University College London animal facility  mol of ribonucleotides × s × I?1  SDS  sodium dodecyl sulphate  SSC  0  15 M NaCl  0  015 M sodium citrate (pH 7  5)  SSPE  0  18 M NaCl  10 mM sodium phosphate (pH 7  7)  l mM EDTA  TEN  100 mM NaCl  l mM EDTA  20 mM Tris · HCl (pH 9  0)
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