The Role of Mitochondrial Genes in Hypertension

	Associate Provost for Research Boston University Medical Campus
NIA - National Institute on Aging	Research Resources

Abstract

Grant Number:	5R01AG018412-05
PI Name:	SCHWARTZ, FAINA
PI Email:	fschw@bu.edu
PI Title:	ASSISTANT PROFESSOR
Project Title:	The Role of Mitochondrial Genes in Hypertension

Abstract: DESCRIPTION (provided by applicant): This competitive renewal application will further challenge our hypothesis that mitochondrial (mtDNA) defects are important contributors to hypertension (HTN). During the present funding period, we developed a novel method for the detection of mitochondrial involvement in complex disorders and applied it to the hypertension data set from 350 Caucasian and 98 African American pedigrees ascertained through the HTN clinics at Boston Medical Center and collaborating clinical sites. Remarkably, we found the fraction of families potentially due to mtDNA mutations to be approximately 55% (95% Cl, 45%-65%). Sequence analysis of the entire mitochondrial genome in 10 African American and 10 Caucasian hypertensive probands from families with suspected mitochondrial involvement led to the identification of several novel, as well as previously reported, mutations with a likely pathogenic effect. Molecular biological characterization of two mutations, T3308C in the ND1 gene and T5655C in the tRNA-Ala gene, detected in African Americans of Lib haplogroup, revealed a reduced Complex I activity in the mitochondrial cybrids containing these mutations. Preliminary data from case-control association study of another mutation, the A10398G in the ND3 gene, conducted in 700 unrelated individuals provided evidence for association of the 10398G allele with HTN. In the present application, we seek to confirm our findings in an independent cohort and to further assess the role of mtDNA variants in blood pressure (BP) homeostasis. Our specific aims are: 1) confirm maternal effect on BP inheritance in Framingham Heart Study participants using existing clinical and genetic data sets from 330 largest Framingham families; 2) identify rare mtDNA variants with potential effects on BP by sequencing the mitochondrial genome from individuals with extreme systolic (n=50) and diastolic (n=50) BP phenotypes; 3) test the association of selected mtDNA variants with HTN and related BP phenotypes by case-control and quantitative association analyses.

Thesaurus Terms:
cardiovascular disorder epidemiology, family genetics, gene mutation, hypertension, mitochondrial DNA, mitochondrial disease /disorder
African American, caucasian American, familial hypertension, genetic polymorphism, genetic susceptibility, racial /ethnic difference
clinical research, computer assisted sequence analysis, genetic mapping, human data, human genetic material tag, polymerase chain reaction

Institution: BOSTON UNIVERSITY MEDICAL CAMPUS

715 ALBANY ST, 560

BOSTON, MA 021182394

Fiscal Year: 2006

Department: MEDICINE

Project Start: 01-AUG-2000

Project End: 31-JUL-2010

ICD: NATIONAL INSTITUTE ON AGING

IRG: HM

Boston, Tue, 23 Jan 2007 16:35:13 EST

Institution:	BOSTON UNIVERSITY MEDICAL CAMPUS
	715 ALBANY ST, 560
	BOSTON, MA 021182394
Fiscal Year:	2006
Department:	MEDICINE
Project Start:	01-AUG-2000
Project End:	31-JUL-2010
ICD:	NATIONAL INSTITUTE ON AGING
IRG:	HM