美国印第安人左心室尺寸和质量的遗传力：强心研究

Heritability of left ventricular dimensions and mass in American Indians: The Strong Heart Study.

作者信息

Bella Jonathan N, MacCluer Jean W, Roman Mary J, Almasy Laura, North Kari E, Best Lyle G, Lee Elisa T, Fabsitz Richard R, Howard Barbara V, Devereux Richard B

机构信息

Weill Medical College of Cornell University, New York, New York, USA.

出版信息

J Hypertens. 2004 Feb;22(2):281-6. doi: 10.1097/00004872-200402000-00011.

DOI:10.1097/00004872-200402000-00011

PMID:15076185

Abstract

OBJECTIVE

We sought to determine the heritability of left ventricular dimensions and mass in adult American Indians.

METHODS

Echocardiograms were analysed in 1373 American Indian participants, from 445 families, in the Strong Heart Study (SHS) to determine the heritability of left ventricular dimensions and mass. Heritability calculations were performed using variance component analysis in SOLAR, a computer analysis program.

RESULTS

The SHS participants analysed in this study included 1305 relative pairs, predominantly (n = 1077) sib-pairs. After simultaneously adjusting for sex, age and centre, the proportion of the residual phenotypic variance due to additive genetic effects or heritability (h2) of left ventricular mass was 0.27 (SE = 0.08, P < 0.001). Addition of body weight, height, systolic blood pressure, heart rate, medications and diabetes into the polygenic model attenuated the residual h2 of left ventricular mass to 0.17 (SE = 0.09, P < 0.05). The residual h2 for left ventricular end-diastolic chamber diameter (LVID), after simultaneously adjusting for sex, age and centre was 0.36 (SE = 0.08, P < 0.001) for the analysed families. The residual h2 for interventricular septal wall thickness was 0.26 (SE = 0.07), while that of left ventricular posterior wall thickness was 0.19 (SE = 0.08, both P < 0.001). While adjustment for body weight, height, systolic blood pressure, heart rate, medications and diabetes reduced the h2 of LVID to 0.33 (SE = 0.09, P < 0.001), the h2 of septal (0.12, SE = 0.10) and posterior wall thickness (0.09, SE = 0.09) were no longer significant after similar adjustment. The residual h2 for relative wall thickness, a measure of left ventricular geometry, was 0.22 (SE = 0.07, P < 0.001) after adjusting for sex, age and centre, and 0.17 (SE = 0.08, P < 0.05) after additional adjustment for body weight, height, systolic blood pressure, heart rate, medications and diabetes.

CONCLUSIONS

A substantial proportion of the variance of left ventricular dimensions and mass can be explained by heredity, independent of the effects of sex, age, body size, blood pressure, heart rate, medications and diabetes. Identification of genes influencing left ventricular size and geometry may provide mechanistic and therapeutic targets to prevent left ventricular hypertrophy.

摘要

目的

我们试图确定成年美国印第安人左心室尺寸和质量的遗传度。

方法

在强心脏研究（SHS）中，对来自445个家庭的1373名美国印第安参与者的超声心动图进行分析，以确定左心室尺寸和质量的遗传度。使用计算机分析程序SOLAR中的方差成分分析进行遗传度计算。

结果

本研究中分析的SHS参与者包括1305对亲属，主要是（n = 1077）同胞对。在同时调整性别、年龄和中心因素后，左心室质量的加性遗传效应或遗传度（h2）导致的残余表型方差比例为0.27（SE = 0.08，P < 0.001）。将体重、身高、收缩压、心率、药物和糖尿病纳入多基因模型后，左心室质量的残余h2降至0.17（SE = 0.09，P < 0.05）。在对分析的家庭同时调整性别、年龄和中心因素后，左心室舒张末期内径（LVID）的残余h2为0.36（SE = 0.08，P < 0.001）。室间隔厚度的残余h2为0.26（SE = 0.07），而左心室后壁厚度的残余h2为0.19（SE = 0.08，均P < 0.001）。虽然调整体重、身高、收缩压、心率、药物和糖尿病后LVID的h2降至0.33（SE = 0.09，P < 0.001），但类似调整后，室间隔（0.12，SE = 0.10）和后壁厚度（0.09，SE = 0.09）的h2不再显著。在调整性别、年龄和中心因素后，左心室几何形状指标相对壁厚度的残余h2为0.22（SE = 0.07，P < 0.001），在进一步调整体重、身高、收缩压、心率、药物和糖尿病后为0.17（SE = 0.08，P < 0.05）。