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Autologous Platelet-Rich Plasma Preparations

机译:自体富血小板血浆制剂

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Background Autologous platelet-rich plasma (PRP) has been widely used for the treatment of sports injuries. It has been associated with improved healing and regeneration of soft tissues in elite athletes. Athletes are commonly receiving nonsteroidal anti-inflammatory drugs (NSAIDs). As yet, the effect of these drugs on platelet function in PRP formulations has not been taken into consideration. Hypothesis The function of platelets in PRP produced under the influence of NSAIDs is inhibited and may lessen a possible healing effect on the site of injury. Study Design Controlled laboratory study. Methods PRP was collected from patients receiving NSAIDs after elective orthopaedic surgery, and platelet function was evaluated using light transmission aggregometry (LTA). Results were compared with those obtained from healthy volunteers without a history of NSAID intake during the previous 2 weeks. Two different systems for blood collection and PRP production (Arthrex ACP double-syringe system and standard 4.5-mL sodium citrate blood collection tubes) were used and compared regarding the quality of PRP that was produced. Results For both groups, the baseline platelet counts of whole blood and the platelet counts of PRP formulations were found to be in the normal range. Both collection systems for PRP produced comparable results without significant differences between the groups. Platelet function testing with LTA revealed significantly impaired platelet aggregation in both PRP preparations, obtained from patients taking NSAIDs, irrespective of the type of NSAID ( P < .001). All subjects from the control group showed normal platelet aggregation patterns when tested with LTA. Conclusion Autologous PRP produced from subjects after NSAID medication shows significantly impaired platelet function and may result in lower quality regarding the content of bioactive compounds. Clinical Relevance If required, the administration of NSAIDs should be performed after blood collection for preparation of autologous PRP; otherwise, the therapeutic effect may be limited.
机译:背景自体富血小板血浆(PRP)已被广泛用于运动损伤的治疗。它与改善精英运动员软组织的愈合和再生有关。运动员通常会接受非甾体抗炎药(NSAIDs)。迄今为止,尚未考虑这些药物对PRP制剂中血小板功能的影响。假设抑制了在NSAIDs的作用下产生的PRP中的血小板功能,并可能减少了在受伤部位的可能的愈合作用。研究设计受控的实验室研究。方法从整形外科接受整形外科手术的NSAID患者中收集PRP,并通过光透射聚集法(LTA)评估血小板功能。将结果与在过去2周内无NSAID摄入史的健康志愿者的结果进行比较。使用了两种不同的采血和PRP生产系统(Arthrex ACP双注射器系统和标准的4.5 mL柠檬酸钠采血管),并比较了所生产PRP的质量。结果两组的全血基线血小板计数和PRP制剂的血小板计数均在正常范围内。两种PRP收集系统均产生了可比的结果,两组之间没有显着差异。用LTA进行的血小板功能测试表明,从服用NSAID的患者中获得的两种PRP制剂中的血小板聚集均显着受损,而与NSAID的类型无关(P <.001)。用LTA测试时,对照组的所有受试者均显示正常的血小板聚集模式。结论NSAID药物治疗后受试者体内产生的自体PRP表现出明显的血小板功能受损,并可能导致生物活性化合物含量降低。临床相关性如果需要,应在采血后进行NSAIDs的给药以制备自体PRP。否则,治疗效果可能会受到限制。

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