Kluger Rainer, Huber Klaus R, Seely Philipp G, Berger Christian E, Frommlet Florian
Department of Orthopedics, SMZOst Donauspital, Vienna, Austria.
Institute of Laboratory Medicine, SMZOst Donauspital, Vienna, Austria.
Am J Sports Med. 2017 Nov;45(13):2955-2964. doi: 10.1177/0363546517729810. Epub 2017 Sep 27.
Several single-nucleotide polymorphisms (SNPs) in the TNC gene have recently been found to be associated with degenerative rotator cuff tears.
Exonic SNPs in the TNC gene are related to the risk for a failure to heal after rotator cuff repair.
Case-control study; Level of evidence, 3.
A total of 302 patients from the Vienna area and European Caucasian ancestry underwent mini-open rotator cuff repair for a full-thickness superior or posterosuperior tear and were assessed for the integrity of the repair 1 year postoperatively with a real-time 7.5- to 10-MHz ultrasound linear array transducer. Outcomes were classified as intact (complete footprint coverage), small (<200 mm), or large (≥200 mm) recurrent defect. Patients were genotyped for 15 previously identified risk SNPs within a 49-kbp segment of the TNC gene with the KASP genotyping technology or the Ion-Torrent Personal Genome Machine System.
All recurrent defects were atraumatic failures, and the overall failure rate was 39.7%. Of the traditional risk factors, only the initial tear size was significantly associated with a failure to heal. In a multinomial logistic regression model, the T allele at rs1138545 [C>T] was protective for a large recurrent defect (odds ratio = 0.16; 95% CI, 0.09-0.31). The role of rs1138545 was further backed by haplotype analysis, which showed that the combination of the C allele at rs1138545 [C>T], the A allele at rs2104772 [A>T], and the G allele at rs10759752 [A>G] formed the risk-related haplotype [CAG]. The CAG haplotype was associated with large recurrent defects ( P < .0001; haplotype frequency, 0.394; haplotype score, 4.518). Exonic marker rs1138545 transcribed into all isoforms of the TNC protein, whereas exonic marker rs2104772, which has been associated with Achilles tendinopathy before, transcribed only into large isoforms of the TNC protein.
Recurrent defects after rotator cuff repairs are clinically relevant, and a heritable component of the disorder is plausible on the basis of a genetic association with 8 TNC variants. Characterization of TNC sequences that favor tendon healing will help engineer new products in regenerative medicine.
最近发现腱生蛋白C(TNC)基因中的几个单核苷酸多态性(SNP)与退行性肩袖撕裂有关。
TNC基因的外显子SNP与肩袖修复后愈合失败的风险相关。
病例对照研究;证据等级,3级。
共有302名来自维也纳地区、具有欧洲高加索血统的患者接受了小切口肩袖修复术,修复的是全层的上方或后上方撕裂,并在术后1年使用7.5至10MHz实时超声线性阵列换能器评估修复的完整性。结果分为完整(完全覆盖足迹)、小(<200mm)或大(≥200mm)复发性缺损。使用竞争性等位基因特异性PCR(KASP)基因分型技术或Ion-Torrent个人基因组机器系统对患者TNC基因49kbp片段内先前确定的15个风险SNP进行基因分型。
所有复发性缺损均为非创伤性失败,总体失败率为39.7%。在传统风险因素中,只有初始撕裂大小与愈合失败显著相关。在多项逻辑回归模型中,rs1138545 [C>T]处的T等位基因对大的复发性缺损具有保护作用(优势比=0.16;95%可信区间,0.09-0.31)。单倍型分析进一步支持了rs1138545的作用,该分析表明rs1138545 [C>T]处的C等位基因、rs2104772 [A>T]处的A等位基因和rs10759752 [A>G]处的G等位基因组合形成了与风险相关的单倍型[CAG]。CAG单倍型与大的复发性缺损相关(P <.0001;单倍型频率,0.394;单倍型评分,4.518)。外显子标记rs1138545转录到TNC蛋白的所有异构体中,而外显子标记rs2104772(之前已与跟腱病相关)仅转录到TNC蛋白的大型异构体中。
肩袖修复术后的复发性缺损具有临床相关性,基于与8个TNC变体的基因关联,该疾病的遗传成分似乎是合理的。确定有利于肌腱愈合的TNC序列特征将有助于再生医学领域开发新产品。
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