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预测跟腱断裂后深静脉血栓形成和愈合结果的新型组织生物标志物候选物。

Novel tissue biomarker candidates to predict both deep venous thrombosis and healing outcome after Achilles tendon rupture.

作者信息

Saarensilta Annukka, Chen Junyu, Reitzner Stefan Markus, Hart David A, Ahmed Aisha S, Ackermann Paul W

机构信息

Department of Molecular Medicine and Surgery, Karolinska Institutet, Stockholm, Sweden.

Department of Molecular Medicine and Surgery, K1 MMK Orthopaedics, Stockholm, 17176, Sweden.

出版信息

Sci Rep. 2025 Mar 1;15(1):7318. doi: 10.1038/s41598-025-91511-0.

Abstract

Deep venous thrombosis (DVT) and poor long-term patient outcomes frequently occur in patients with Achilles tendon rupture (ATR). Biomarkers for DVT and their possible relationship to long-term healing outcomes remain unexplored. To identify DVT biomarkers from proteomic profiles during the inflammatory and proliferative healing stages and assess their associations with one-year healing outcomes after surgical repair of ATR. A cohort of 53 patients undergoing standardized ATR repair from previous clinical trials was investigated. Intraoperative inflammatory-stage tendon biopsies were obtained from 40 patients, and tendon microdialysates from 28 patients were collected two weeks later during the proliferative stage. Liquid chromatography-tandem mass spectrometry proteomic profiles were linked to DVT status at two weeks post-surgery using ultrasonography screening and to patient-reported outcomes at one-year post-surgery. Six candidate DVT biomarkers were identified from tendon biopsies, whereof four (ABI3BP, IGKV2-40/IGKV2D-40, PCYOX1, STIP1) were associated with one-year healing outcomes. In tendon microdialysates, 43 candidate DVT biomarkers were identified, but none were associated with healing outcomes. Bioinformatic analysis revealed pathways related to heat shock response, platelet signaling, collagen and extracellular matrix metabolism, and immunoglobulins. The results support shared inflammatory-stage protein pathways in regulating venous thrombosis and reported healing outcomes, where elements of individual hypoxic tolerance and platelet signaling emerge as potential key links.

摘要

跟腱断裂(ATR)患者常发生深静脉血栓形成(DVT)且长期预后较差。DVT的生物标志物及其与长期愈合结果的可能关系仍未得到探索。旨在从炎症和增殖愈合阶段的蛋白质组学谱中识别DVT生物标志物,并评估它们与ATR手术修复后一年愈合结果的关联。对先前临床试验中53例接受标准化ATR修复的患者队列进行了研究。从40例患者中获取术中炎症期肌腱活检样本,两周后在增殖期从28例患者中收集肌腱微透析液。采用超声检查将液相色谱 - 串联质谱蛋白质组学谱与术后两周的DVT状态相关联,并与术后一年患者报告的结果相关联。从肌腱活检中鉴定出6种候选DVT生物标志物,其中4种(ABI3BP、IGKV2 - 40/IGKV2D - 40、PCYOX1、STIP1)与一年愈合结果相关。在肌腱微透析液中,鉴定出43种候选DVT生物标志物,但均与愈合结果无关。生物信息学分析揭示了与热休克反应、血小板信号传导、胶原蛋白和细胞外基质代谢以及免疫球蛋白相关的途径。结果支持在调节静脉血栓形成和报告的愈合结果方面存在共同的炎症期蛋白质途径,其中个体缺氧耐受性和血小板信号传导的元素成为潜在的关键环节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ca71/11873306/636298f62b04/41598_2025_91511_Fig1_HTML.jpg

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