Original ArticlesEffects of ethnicity on the distribution of clinically relevant endothelial nitric oxide variantsTanus-Santos, Jose E; Desai, Mehul; Flockhart, David AAuthor Information Division of Clinical Pharmacology, Georgetown University Medical Center, Washington, DC, USA Correspondence to Jose E. Tanus-Santos, Division of Clinical Pharmacology, Georgetown University Medical Center, 3900 Reservoir Rd, NW, Washington, DC 20007, USA Fax: +1 202 687 7894; email: [email protected] Dates Received 22 May 2001 Accepted 28 June 2001 Pharmacogenetics: November 2001 - Volume 11 - Issue 8 - p 719-725 Buy Abstract Polymorphisms in the endothelial nitric oxide synthase (eNOS) gene have been associated inconsistently with cardiovascular diseases. A maldistribution of eNOS variants among ethnic groups may explain interethnic differences in nitric oxide (NO)-mediated vasodilation and response to drugs. To test this possibility, we examined the distribution of genetic variants of three clinically relevant eNOS polymorphisms (T−786C in the promoter, the variable number of tandem repeats (VNTR) in intron 4, and the Glu298Asp variant in exon 7) in 305 ethnically well-characterized DNA samples (100 Caucasians, 100 African-Americans, and 105 Asians). We estimated the haplotype frequency, and evaluated associations between these variants. The Asp298 variant was more common in Caucasians (34.5%) than in African-Americans (15.5%) or Asians (8.6%)(P < 0.0001). The C−786 variant was also more common in Caucasians (42.0%) than in African-Americans (17.5%) or Asians (13.8%) (P < 0.0001). The 4a variant in intron 4 was more common in African-Americans (26.5%) than in Caucasians (16.0%) or Asians (12.9%) (P < 0.0001). The most common predicted haplotype in the three groups combined only wild-type variants. Asians had the highest frequency of this haplotype (77% in Asians v. 46% in the other groups). In Caucasians, the Asp298 and C−786variants were associated, and this haplotype was predicted to have a frequency of 24%. In African-Americans, the second most common haplotype included the variant 4a and wild-type variants; the Asp298 and 4a variants were associated negatively in this group. The C−786 and 4a variants were associated in Asians (P < 0.0001). The marked interethnic differences that we found in the distribution of eNOS variants, in the estimated haplotype frequency, and in the association between variants may help us to understand how the combination of these genetic variants may influence cardiovascular diseases. © 2001 Lippincott Williams & Wilkins, Inc.