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Characterization and comparison of 5 platelet-rich plasma preparations in a single-donor model

机译:单供体模型中5种富含血小板的血浆制剂的表征和比较

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摘要

Purpose The purpose of this study was to compare the biological characteristics of platelet-rich plasma (PRP) obtained from 4 medical devices and a preparation developed in our laboratory using a single-donor model. Methods Ten healthy persons donated blood that was processed to produce PRP by use of 4 commercial preparation systems and a protocol developed in our laboratory. Volumes and platelet, white blood cell (WBC), and red blood cell concentrations were recorded. The platelet activation status was assessed by flow cytometry. Enzyme-linked immunosorbent assay was used to determine the concentrations of vascular endothelial growth factor, platelet-derived growth factor AB, epidermal growth factor, and transforming growth factor β1. We calculated platelet capture efficiency, relative composition, and increase factors from whole blood in platelets and WBC, as well as platelet and growth factor (GF) doses, provided from each preparation. Results Leukocyte-rich PRP was obtained with RegenPRP (RegenLab, Le Mont-sur-Lausanne, Switzerland) and the Mini GPS III System (Biomet Biology, Warsaw, IN) and provides PRP with higher proportions of red blood cells, WBCs, and neutrophils than leukocyte-poor PRP obtained with the Selphyl System (Selphyl, Bethlehem, PA), Arthrex ACP (Arthrex, Naples, FL), and the preparation developed in our laboratory. The highest platelet and GF concentrations and doses were obtained with the Mini GPS III System and the preparation developed in our laboratory. Different centrifugation protocols did not show differences in the percentages of activated platelets. Finally, a positive correlation between platelet doses and all the GFs studied was found, whereas a positive correlation between WBC doses and GFs was found only for vascular endothelial growth factor and epidermal growth factor. Conclusions In a single-donor model, significant biological variations in PRP obtained from different preparation systems were highlighted. The observed differences suggest different results for treated tissue and could explain the large variability in the clinical benefit of PRP reported in the literature. Clinical Relevance Our findings will help clinicians to choose a system that meets their specific needs for a given indication.
机译:目的本研究的目的是比较从4种医疗设备获得的富血小板血浆(PRP)的生物学特性,以及在我们实验室中使用单供体模型开发的制剂的生物学特性。方法十名健康人捐献的血液经过4种商业制备系统和我们实验室制定的方案处理后产生PRP。记录体积和血小板,白细胞(WBC)和红细胞浓度。通过流式细胞术评估血小板活化状态。酶联免疫吸附法用于测定血管内皮生长因子,血小板衍生生长因子AB,表皮生长因子和转化生长因子β1的浓度。我们计算了血小板和白细胞中全血的血小板捕获效率,相对组成和增加因子,以及每种制剂提供的血小板和生长因子(GF)剂量。结果富含白细胞的PRP是通过RegenPRP(RegenLab,洛桑河畔洛蒙市)和Mini GPS III系统(Biomet Biology,华沙,印第安纳州)获得的,为PRP提供了比例更高的红细胞,白细胞和中性白细胞比通过Selphyl系统(Selphyl,Bethlehem,PA),Arthrex ACP(Arthrex,Naples,FL)获得的贫白细胞PRP,以及在我们实验室开发的制剂。使用Mini GPS III系统和在我们实验室中开发的制剂可获得最高的血小板和GF浓度和剂量。不同的离心方案没有显示出活化血小板百分比的差异。最后,发现血小板剂量与所有研究的GFs之间呈正相关,而WBC剂量与GFs之间仅与血管内皮生长因子和表皮生长因子呈正相关。结论在单供体模型中,强调了从不同制备系统获得的PRP的显着生物学差异。观察到的差异表明治疗组织的结果不同,并且可以解释文献中报道的PRP的临床益处存在较大差异。临床相关性我们的发现将帮助临床医生针对给定适应症选择满足其特定需求的系统。

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