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富血小板纤维蛋白增强的兔前交叉韧带修复中的间隙桥接策略。

Platelet-Rich Fibrin-Augmented Gap-Bridging Strategy in Rabbit Anterior Cruciate Ligament Repair.

机构信息

Department of Orthopedics, Taipei Medical University Shuang Ho Hospital, New Taipei City, Taiwan.

Department of Orthopedics, School of Medicine, College of Medicine, Taipei Medical University, Taipei, Taiwan.

出版信息

Am J Sports Med. 2023 Mar;51(3):642-655. doi: 10.1177/03635465221149993. Epub 2023 Feb 8.

Abstract

BACKGROUND

We assessed the efficacy of a novel platelet-rich fibrin (PRF)-augmented repair strategy for promoting biological healing of an anterior cruciate ligament (ACL) midsubstance tear in a rabbit model. The biological gap-bridging effect of a PRF scaffold alone or in combination with rabbit ligamentocytes on primary ACL healing was evaluated both in vitro and in vivo.

HYPOTHESIS

A PRF matrix can be implanted as a provisional fibrin-platelet bridging scaffold at an ACL defect to facilitate functional healing.

STUDY DESIGN

Controlled laboratory study.

METHODS

The biological effects of PRF on primary rabbit ligamentocyte proliferation, tenogenic differentiation, migration, and tendon-specific matrix production were investigated for treatment of cells with PRF-conditioned medium (PRFM). Three-dimensional (3D) lyophilized PRF (LPRF)-cell composite was fabricated by culturing ligamentocytes on an LPRF patch for 14 days. Cell-scaffold interactions were investigated under a scanning electron microscope and through histological analysis. An ACL midsubstance tear model was established in 3 rabbit groups: a ruptured ACL was treated with isolated suture repair in group A, whereas the primary repair was augmented with LPRF and LPRF-cell composite to bridge the gap between ruptured ends of ligaments in groups B and C, respectively. Outcomes-gross appearance, magnetic resonance imaging, and histological analysis-were evaluated in postoperative weeks 8 and 12.

RESULTS

PRFM promoted cultured ligamentocyte proliferation, migration, and expression of tenogenic genes (type I and III collagen and tenascin). PRF was noted to upregulate cell tenogenic differentiation in terms of matrix production. In the 3D culture, viable cells formed layers at high density on the LPRF scaffold surface, with notable cell ingrowth and abundant collagenous matrix depositions. Moreover, ACL repair tissue and less articular cartilage damage were observed in knee joints in groups B and C, implying the existence of a chondroprotective phenomenon associated with PRF-augmented treatment.

CONCLUSION

Our PRF-augmented strategy can facilitate the formation of stable repair tissue and thus provide gap-bridging in ACL repair.

CLINICAL RELEVANCE

From the translational viewpoint, effective primary repair of the ACL may enable considerable advancement in therapeutic strategy for ACL injuries, particularly allowing for proprioception retention and thus improved physiological joint kinematics.

摘要

背景

我们评估了一种新型富血小板纤维蛋白(PRF)增强修复策略在兔 ACL 中质撕裂模型中的功效,以促进生物愈合。我们评估了 PRF 支架单独或与兔韧带细胞结合对 ACL 愈合的生物学间隙桥接作用,包括体外和体内。

假设

PRF 基质可作为 ACL 缺损处的临时纤维蛋白-血小板桥接支架植入,以促进功能愈合。

研究设计

对照实验室研究。

方法

用 PRF 条件培养基(PRFM)处理细胞,研究 PRF 对原代兔韧带细胞增殖、腱性分化、迁移和腱特异性基质产生的生物学作用。通过在 LPRF 贴片上培养韧带细胞 14 天,制备三维(3D)冻干 PRF(LPRF)-细胞复合物。通过扫描电子显微镜和组织学分析研究细胞-支架相互作用。在 3 组兔中建立 ACL 中质撕裂模型:A 组采用单纯缝线修复撕裂的 ACL,B 组和 C 组分别采用 LPRF 和 LPRF-细胞复合物增强初级修复,以桥接韧带撕裂端之间的间隙。在术后 8 周和 12 周评估了术后外观、磁共振成像和组织学分析。

结果

PRFM 促进了培养的韧带细胞增殖、迁移和腱性基因(I 型和 III 型胶原和腱蛋白)的表达。PRF 被证明可以上调细胞的腱性分化,表现在基质产生方面。在 3D 培养中,活细胞在 LPRF 支架表面高密度形成层,有明显的细胞内陷和丰富的胶原基质沉积。此外,B 组和 C 组膝关节的 ACL 修复组织和较少的关节软骨损伤表明存在与 PRF 增强治疗相关的软骨保护现象。

结论

我们的 PRF 增强策略可以促进稳定修复组织的形成,从而为 ACL 修复提供间隙桥接。

临床相关性

从转化的角度来看,有效的 ACL 初步修复可能会为 ACL 损伤的治疗策略带来重大进展,特别是保留本体感觉,从而改善生理关节运动学。

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