Immunophenotyping of Synovial Tissue in Adolescents Undergoing ACL Reconstruction: What Is the Role of Synovial Inflammation in Arthrofibrosis?

Sarah M. Romereim, Matthew R. Smykowski, Elaina K. Ball, Edward Grant Carey, Mario Cuadra, Alicia Williams, Kate Hickson, Kara Haim, Meera Sumith, Ziqing Yu, Guangxu Jin, David Foureau, Nury Steuerwald, Susan Odum, Bailey V. Fearing, Jonathan C. Riboh
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Abstract

Background:Loss of motion and arthrofibrosis after anterior cruciate ligament (ACL) reconstruction (ACLR) can be devastating complications for athletes. The cellular and molecular pathogenesis of arthrofibrosis is poorly understood, limiting prevention and treatment options. Synovial inflammation may contribute to post-ACLR arthrofibrosis.Hypothesis:Higher synovial immune cell infiltration and inflammatory/catabolic gene expression patterns at the time of ACLR would correlate with poorer motion-related outcomes.Study Design:Case series; Level of evidence, 4.Methods:Patients aged 10 to 18 years undergoing primary ACLR were enrolled in a prospective pilot study, and synovial tissue biopsy specimens were obtained during ACLR. Flow cytometry and single-cell RNA sequencing explored synovial cell types/frequencies and gene expression. Principal component analysis was performed, followed by clustering which grouped patients into distinct immunophenotypes based on their synovial cell composition. Clinical follow-up data with knee range of motion (ROM), need for lysis of adhesions, and patient-reported outcome measures were collected and compared between immunophenotypes.Results:Enrolled patients (n = 17) underwent ACLR at a median of 37 days after injury. Analysis revealed 3 distinct immunophenotypes. Type 1 consisted of patients with the longest time between injury and surgery and the lowest hematopoietic and T-cell infiltration. Types 2 and 3 had similar times between injury and surgery; type 2 had intermediate while type 3 had the highest hematopoietic and T-cell percentages. Type 3 was associated with worse ROM at 2 and 6 weeks postoperatively; T-cell prevalence and ROM were inversely correlated at those time points. The only patient requiring lysis of adhesions for arthrofibrosis had a type 3 immunophenotype.Conclusion:Synovial immune infiltration after ACL injury shows variability between patients that clusters into 3 immunophenotypes correlating with early ROM and the risk of arthrofibrosis. T-cell recruitment and infiltration were the strongest factors correlated with ROM outcomes and present an exciting venue for future research on post-ACLR arthrofibrosis.
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青少年前交叉韧带重建中滑膜组织的免疫表型分析:滑膜炎症在关节纤维化中的作用?
背景:前交叉韧带(ACL)重建(ACLR)后运动能力丧失和关节纤维化对运动员来说是毁灭性的并发症。关节纤维化的细胞和分子发病机制尚不清楚,这限制了预防和治疗的选择。滑膜炎症可能导致aclr后关节纤维化。假设:ACLR时较高的滑膜免疫细胞浸润和炎症/分解代谢基因表达模式与较差的运动相关结果相关。研究设计:病例系列;证据等级,4级。方法:年龄在10 - 18岁的原发性ACLR患者被纳入前瞻性先导研究,并在ACLR期间获得滑膜组织活检标本。流式细胞术和单细胞RNA测序研究滑膜细胞类型/频率和基因表达。进行主成分分析,然后进行聚类,根据滑膜细胞组成将患者分组为不同的免疫表型。收集了膝关节活动范围(ROM)、粘连溶解需求和患者报告的结果测量的临床随访数据,并在免疫表型之间进行了比较。结果:纳入的患者(n = 17)在受伤后中位时间37天接受ACLR。分析显示3种不同的免疫表型。1型患者损伤至手术时间最长,造血和t细胞浸润最低。2型和3型在受伤和手术之间的时间相似;2型患者造血和t细胞百分比居中,而3型患者造血和t细胞百分比最高。3型患者术后2周和6周ROM恶化;在这些时间点,t细胞患病率与ROM呈负相关。唯一需要解除关节纤维化粘连的患者为3型免疫表型。结论:前交叉韧带损伤后的滑膜免疫浸润在患者之间存在差异,聚集成3种免疫表型,与早期ROM和关节纤维化的风险相关。t细胞募集和浸润是与ROM预后相关的最强因素,为aclr后关节纤维化的未来研究提供了一个令人兴奋的领域。
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