温血马易碎驹 1 型突变（PLOD1 c.2032G>A）与灾难性衰竭无关，在纯血马品种中的等位基因频率较低。

Warmblood fragile foal syndrome type 1 mutation (PLOD1 c.2032G>A) is not associated with catastrophic breakdown and has a low allele frequency in the Thoroughbred breed.

机构信息

Veterinary Genetics Laboratory, School of Veterinary Medicine, University of California-Davis, Davis, California, USA.

Department of Population Health and Reproduction, School of Veterinary Medicine, University of California-Davis, Davis, California, USA.

出版信息

Equine Vet J. 2020 May;52(3):411-414. doi: 10.1111/evj.13182. Epub 2019 Oct 4.

DOI:10.1111/evj.13182

PMID:31502696

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7062577/

Abstract

BACKGROUND

Catastrophic fractures are among the most common cause of fatalities in racehorses. Several factors, including genetics, likely contribute to increased risk for fatal injuries. A variant in the procollagen-lysine, 2-oxoglutarate 5-dioxygenase1 gene (PLOD1 c.2032G>A) was shown to cause Warmblood fragile foal syndrome type 1 (WFFS), a fatal recessive defect of the connective tissue. Screening of multiple horse breeds identified the presence of the WFFS allele in the Thoroughbred. PLOD1 is involved in cross-linking of collagen fibrils and thus could potentially increase the risk of catastrophic breakdown.

OBJECTIVES

Estimate the frequency of the WFFS allele (PLOD1 c.2032G>A) and determine if it is a risk factor for catastrophic breakdown in the Thoroughbred.

STUDY DESIGN

Case-control genetic study.

METHODS

Genomic DNA from hair and/or tissue samples was genotyped for the WFFS allele. Fisher's Exact tests were performed to compare allele and carrier frequencies between the case cohort (catastrophic breakdown, n = 22) and several cohorts with no record of injury (n = 138 raced/trained at same track and season and n = 185 older than 7 years and raced during same season), nonracers (n = 92), and a random sample without consideration for racing history (n = 279).

RESULTS

The frequency of the PLOD1 c.2032G>A variant in the Thoroughbred breed is low (1.2%). Seventeen of 716 Thoroughbreds tested were carriers (2.4%) and no WFFS homozygotes were detected. Only one catastrophic breakdown case carried the WFFS allele. No statistically significant difference in allele or carrier frequency was identified between case and control cohorts (P>0.05 in all comparisons performed).

MAIN LIMITATIONS

This study evaluated cases from one single track.

CONCLUSIONS

This study demonstrated that the PLOD1 c.2032G>A associated with WFFS is present at very low frequency in Thoroughbreds and is not a genetic risk factor for catastrophic breakdown.

摘要

背景

灾难性骨折是赛马中最常见的致死原因之一。多种因素，包括遗传因素，可能会增加致命性损伤的风险。脯氨酰-赖氨酸，2-氧戊二酸 5-双加氧酶 1 基因（PLOD1 c.2032G>A）的变异可导致温血脆弱驹综合征 1 型（WFFS），这是一种致命的结缔组织隐性缺陷。对多个马品种进行筛查后发现，该突变也存在于纯血马中。PLOD1 参与胶原纤维的交联，因此可能会增加灾难性骨折的风险。

目的

估计 WFFS 等位基因（PLOD1 c.2032G>A）的频率，并确定其是否是纯血马发生灾难性骨折的危险因素。

研究设计

病例对照遗传研究。

方法

从毛发和/或组织样本中提取基因组 DNA，对 WFFS 等位基因进行基因分型。通过 Fisher 精确检验比较病例队列（灾难性骨折，n=22）与无损伤记录的多个队列（在同一赛道和赛季内参赛/训练的 n=138 匹，年龄大于 7 岁且在同一赛季参赛的 n=185 匹，非参赛者 n=92 匹）、随机样本（不考虑参赛历史，n=279 匹）的等位基因和携带者频率。

结果

在纯血马品种中，PLOD1 c.2032G>A 变异的频率较低（1.2%）。在 716 匹纯血马中，17 匹为携带者（2.4%），未检测到 WFFS 纯合子。只有 1 例灾难性骨折病例携带 WFFS 等位基因。在病例和对照组中，等位基因或携带者频率无统计学差异（所有比较 P>0.05）。

主要局限性

本研究仅评估了一个单一赛道的病例。

结论

本研究表明，与 WFFS 相关的 PLOD1 c.2032G>A 变异在纯血马中频率非常低，不是灾难性骨折的遗传危险因素。

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温血马易碎驹 1 型突变（PLOD1 c.2032G>A）与灾难性衰竭无关，在纯血马品种中的等位基因频率较低。

Warmblood fragile foal syndrome type 1 mutation (PLOD1 c.2032G>A) is not associated with catastrophic breakdown and has a low allele frequency in the Thoroughbred breed.

机构信息

Veterinary Genetics Laboratory, School of Veterinary Medicine, University of California-Davis, Davis, California, USA.

Department of Population Health and Reproduction, School of Veterinary Medicine, University of California-Davis, Davis, California, USA.

出版信息

Equine Vet J. 2020 May;52(3):411-414. doi: 10.1111/evj.13182. Epub 2019 Oct 4.

DOI:10.1111/evj.13182

PMID:31502696

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC7062577/

Abstract

BACKGROUND

OBJECTIVES

Estimate the frequency of the WFFS allele (PLOD1 c.2032G>A) and determine if it is a risk factor for catastrophic breakdown in the Thoroughbred.

STUDY DESIGN

Case-control genetic study.

METHODS

RESULTS

MAIN LIMITATIONS

This study evaluated cases from one single track.

CONCLUSIONS

This study demonstrated that the PLOD1 c.2032G>A associated with WFFS is present at very low frequency in Thoroughbreds and is not a genetic risk factor for catastrophic breakdown.

摘要

背景

目的

估计 WFFS 等位基因（PLOD1 c.2032G>A）的频率，并确定其是否是纯血马发生灾难性骨折的危险因素。

研究设计

病例对照遗传研究。

方法

结果

主要局限性

本研究仅评估了一个单一赛道的病例。

结论

本研究表明，与 WFFS 相关的 PLOD1 c.2032G>A 变异在纯血马中频率非常低，不是灾难性骨折的遗传危险因素。

温血马易碎驹 1 型突变（PLOD1 c.2032G>A）与灾难性衰竭无关，在纯血马品种中的等位基因频率较低。

Warmblood fragile foal syndrome type 1 mutation (PLOD1 c.2032G>A) is not associated with catastrophic breakdown and has a low allele frequency in the Thoroughbred breed.

机构信息

出版信息

BACKGROUND

OBJECTIVES

STUDY DESIGN

METHODS

RESULTS

MAIN LIMITATIONS

CONCLUSIONS

背景

目的

研究设计

方法

结果

主要局限性

结论

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温血马易碎驹 1 型突变（PLOD1 c.2032G>A）与灾难性衰竭无关，在纯血马品种中的等位基因频率较低。

Warmblood fragile foal syndrome type 1 mutation (PLOD1 c.2032G>A) is not associated with catastrophic breakdown and has a low allele frequency in the Thoroughbred breed.

机构信息

出版信息

BACKGROUND

OBJECTIVES

STUDY DESIGN

METHODS

RESULTS

MAIN LIMITATIONS

CONCLUSIONS

背景

目的

研究设计

方法

结果

主要局限性

结论