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先前与前交叉韧带损伤风险相关的胶原基因变异也与关节松弛有关。

Collagen gene variants previously associated with anterior cruciate ligament injury risk are also associated with joint laxity.

机构信息

Department of Kinesiology, University of North Carolina at Greensboro, Greensboro, North Carolina.

出版信息

Sports Health. 2012 Jul;4(4):312-8. doi: 10.1177/1941738112446684.

Abstract

BACKGROUND

Genetic association studies demonstrate a relationship between several collagen gene variants and anterior cruciate ligament (ACL) injury, yet the mechanism of these relationships is still unclear. Joint laxity is a heritable trait; increased magnitudes of anterior knee laxity (AKL), genu recurvatum (GR), and general joint laxity (GJL) have been consistently associated with a greater risk of ACL injury. Joint laxity may constitute an important intermediate phenotype for the genetic association with ACL injury that can be measured clinically.

HYPOTHESIS

To determine if genetic variants within the COL1A1, COL5A1, and COL12A1 genes, previously associated with ACL injury, were also associated with greater magnitudes of AKL, GR, and GJL.

STUDY DESIGN

Descriptive laboratory study.

METHODS

Blood samples and measures of AKL, GR, and GJL were obtained from 124 (50 male, 74 female) healthy, recreationally active subjects. Genomic DNA was extracted from the blood samples and genotyped for single-nucleotide polymorphisms previously examined relative to ACL injury. Univariate analyses of variance compared the magnitude of each laxity variable across the 3 genotypes for each single-nucleotide polymorphism in both sex-combined and sex-specific models.

RESULTS

Specific genotypes were associated with greater GR in all subjects. Some genotypes were associated with greater magnitudes of GR, AKL, and GJL in females only.

CONCLUSIONS

Gene variants previously associated with ACL injury risk were in large part also associated with joint laxity. Sex-specific genetic associations with joint laxity were consistent with those previously reported for ACL injury.

CLINICAL RELEVANCE

These data provide insight into potential pathways through which genotypic variants in collagen genes have the potential to alter ligament structure and behavior and, thus, ACL injury risk.

摘要

背景

遗传关联研究表明,几个胶原基因变异与前交叉韧带(ACL)损伤之间存在关系,但这些关系的机制仍不清楚。关节松弛是一种遗传性特征;前膝松弛(AKL)、膝反屈(GR)和一般关节松弛(GJL)的程度增加与 ACL 损伤的风险增加密切相关。关节松弛可能是与 ACL 损伤的遗传关联的重要中间表型,可以通过临床测量。

假设

确定以前与 ACL 损伤相关的 COL1A1、COL5A1 和 COL12A1 基因中的遗传变异是否也与更大程度的 AKL、GR 和 GJL 相关。

研究设计

描述性实验室研究。

方法

从 124 名(50 名男性,74 名女性)健康、有规律运动的受试者中获得血液样本和 AKL、GR 和 GJL 的测量值。从血液样本中提取基因组 DNA,并对以前相对于 ACL 损伤进行检查的单核苷酸多态性进行基因分型。在男女混合和性别特异性模型中,对每个单核苷酸多态性的每个松弛变量的幅度,在 3 个基因型之间进行单变量方差分析。

结果

特定基因型与所有受试者的 GR 程度增加有关。一些基因型与女性中更大程度的 GR、AKL 和 GJL 相关。

结论

以前与 ACL 损伤风险相关的基因变异在很大程度上也与关节松弛相关。与关节松弛相关的性别特异性遗传关联与以前报告的 ACL 损伤一致。

临床相关性

这些数据提供了深入了解胶原基因中基因型变异如何潜在改变韧带结构和行为,从而改变 ACL 损伤风险的潜在途径的见解。

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