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Characterization of two polymorphic sites in the human kinin B1 receptor gene: altered frequency of an allele in patients with a history of end-stage renal failure.

D R Bachvarov, M Landry, I Pelletier, M Chevrette, C Betard, I Houde, J Bergeron, M Lebel and F Marceau
JASN April 1998, 9 (4) 598-604;
D R Bachvarov
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M Landry
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I Pelletier
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M Chevrette
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C Betard
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I Houde
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J Bergeron
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M Lebel
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F Marceau
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Abstract

On the basis of the genomic structure of the human B1 receptor (B1R) for kinins, the presence of possible allelic polymorphisms of this gene was investigated using restriction fragment-length polymorphism and single-strand conformation polymorphism. The frequencies of the found alleles were determined in healthy volunteers and in patients with a history of end-stage renal failure, because there is evidence for a nephroprotective action of the kallikrein-kinin system. An A1098-->G polymorphism has been identified in exon 3 in a minority of volunteer blood donors, and is located 35 nucleotides downstream from the stop codon and 14 nucleotides upstream from the polyadenylation signal. The frequency of the G allele is 4.4% in the control sample and not significantly altered in patients with a history of end-stage renal failure. A second and more frequent polymorphism (18.1% of the alleles in the control group, prevalence of 33.3%) consists of a single base substitution (G-699-->C) in the putative promoter region. This polymorphism is significantly less frequent in the population of renal failure patients (prevalence of 20.6%) and determines an increased activity of the promoter function in constructions involving a reporter gene. The altered prevalence of this allele was also found in some etiologic subgroups of uremic patients. This study confirms the mapping of the B1R gene to 14q32. Other investigators have mapped the bradykinin B2 receptor (B2R) gene to a close site on human chromosome 14. A previously described B2R polymorphism (exon 2, C181-->T) had an allele frequency of 9.7% in the control sample and appears to be clinically neutral. The polymorphism of the B1R promoter may be a marker of prognostic significance for the preservation of renal function in diseased individuals.

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Journal of the American Society of Nephrology
Vol. 9, Issue 4
1 Apr 1998
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Characterization of two polymorphic sites in the human kinin B1 receptor gene: altered frequency of an allele in patients with a history of end-stage renal failure.
D R Bachvarov, M Landry, I Pelletier, M Chevrette, C Betard, I Houde, J Bergeron, M Lebel, F Marceau
JASN Apr 1998, 9 (4) 598-604;

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Characterization of two polymorphic sites in the human kinin B1 receptor gene: altered frequency of an allele in patients with a history of end-stage renal failure.
D R Bachvarov, M Landry, I Pelletier, M Chevrette, C Betard, I Houde, J Bergeron, M Lebel, F Marceau
JASN Apr 1998, 9 (4) 598-604;
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Cited By...

  • Balance between the two kinin receptors in the progression of experimental focal and segmental glomerulosclerosis in mice
  • In vivo DNase I-mediated footprinting analysis along the human bradykinin B1 receptor (BDKRB1) gene promoter: evidence for cell-specific regulation
  • International Union of Pharmacology. XLV. Classification of the Kinin Receptor Family: from Molecular Mechanisms to Pathophysiological Consequences
  • Induction of Functional Bradykinin B1-Receptors in Normotensive Rats and Mice Under Chronic Angiotensin-Converting Enzyme Inhibitor Treatment
  • The Human B1 Bradykinin Receptor Exhibits High Ligand-independent, Constitutive Activity: ROLES OF RESIDUES IN THE FOURTH INTRACELLULAR AND THIRD TRANSMEMBRANE DOMAINS
  • Effect of Allelic Polymorphism of the B1 and B2 Receptor Genes on the Contractile Responses of the Human Umbilical Vein to Kinins
  • The B1 Receptors for Kinins
  • The Human B1 Bradykinin Receptor Exhibits High Ligand-independent, Constitutive Activity: ROLES OF RESIDUES IN THE FOURTH INTRACELLULAR AND THIRD TRANSMEMBRANE DOMAINS
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