A novel therapy for fracture healing by increasing lymphatic drainage

IF 5.9 1区 医学 Q1 ORTHOPEDICS
Yangkang Zheng , Pengyu Wang , Li Zhao , Lianping Xing , Hao Xu , Ning Li , Yongjian Zhao , Qi Shi , Qianqian Liang , YongJun Wang
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引用次数: 0

Abstract

Background

The musculoskeletal system contains an extensive network of lymphatic vessels. Decreased lymph flow of the draining collecting lymphatics usually occurs in clinic after traumatic fractures. However, whether defects in lymphatic drainage can affect fracture healing is unclear.

Methods

To investigate the effect of lymphatic dysfunction on fracture healing, we used a selective VEGFR3 tyrosine kinase inhibitor to treat tibial fractured mice for 5 weeks versus a vehicle-treated control. To ensure successfully establishing deceased lymphatic drainage model for fractured mice, we measured lymphatic clearance by near infrared indocyanine green lymphatic imaging (NIR-ICG) and the volume of the draining popliteal lymph nodes (PLNs) by ultrasound at the whole phases of fracture healing. In addition, hindlimb edema from day 0 to day 7 post-fracture, pain sensation by Hargreaves test at day 1 post-fracture, bone histomorphometry by micro-CT and callus composition by Alcian Blue-Hematoxylin/Orange G staining at day 14 post-fracture, and bone quality by biomechanical testing at day 35 post-fracture were applied to evaluate fracture healing. To promote fracture healing via increasing lymphatic drainage, we then treated fractured mice with anti-mouse podoplanin (PDPN) neutralizing antibody or isotype IgG antibody for 1 week to observe lymphatic drainage function and assess bone repair as methods described above.

Results

Compared to vehicle-treated group, SAR-treatment group significantly decreased lymphatic clearance and the volume of draining PLNs. SAR-treatment group significantly increased soft tissue swelling, and reduced bone volume (BV)/tissue volume (TV), trabecular number (Tb.N), woven bone and biomechanical properties of fracture callus. In addition, anti-PDPN treated group significantly reduced the number of CD41+ platelets in PLNs and increased the number of pulsatile lymphatic vessels, lymphatic clearance and the volume of PLNs. Moreover, anti-PDPN treated group significantly reduced hindlimb edema and pain sensation and increased BV/TV, trabecular number (Tb.Th), woven bone and biomechanical properties of fracture callus.

Conclusions

Inhibition of proper lymphatic drainage function delayed fracture healing. Use of a anti-PDPN neutralizing antibody reduced lymphatic platelet thrombosis (LPT), increased lymphatic drainage and improved fracture healing.

The translational potential of this article

(1) We demonstrated lymphatic drainage function is crucial for fracture healing. (2) To unblock the lymphatic drainage and prevent the risk of bleeding and mortality by blood thinner, we demonstrated PDPN neutralizing antibody is a novel and safe way forward in the treatment of bone fracture healing by eliminating LPT and increasing lymphatic drainage.

Abstract Image

通过增加淋巴引流促进骨折愈合的新疗法
背景肌肉骨骼系统包含广泛的淋巴管网。临床上,创伤性骨折后通常会出现引流集合淋巴管淋巴流量减少的情况。为了研究淋巴功能障碍对骨折愈合的影响,我们使用一种选择性 VEGFR3 酪氨酸激酶抑制剂治疗胫骨骨折小鼠 5 周,并与用药物治疗的对照组进行比较。为确保成功建立骨折小鼠死亡淋巴引流模型,我们通过近红外吲哚菁绿淋巴成像(NIR-ICG)测量了淋巴清除率,并通过超声波测量了骨折愈合全过程中引流腘淋巴结(PLN)的体积。此外,还采用骨折后第0天至第7天的后肢水肿、骨折后第1天的哈格里夫斯痛觉测试、骨折后第14天的显微CT骨组织形态测量和阿尔新蓝-血红素/橙G染色法胼胝体成分以及骨折后第35天的生物力学测试来评估骨折愈合情况。为了通过增加淋巴引流促进骨折愈合,我们用抗小鼠荚膜磷脂蛋白(PDPN)中和抗体或同种型 IgG 抗体治疗骨折小鼠 1 周,观察淋巴引流功能,并按照上述方法评估骨修复情况。SAR治疗组软组织肿胀明显增加,骨体积(BV)/组织体积(TV)、骨小梁数(Tb.N)、编织骨和骨折胼胝体的生物力学特性降低。此外,抗 PDPN 治疗组明显减少了 PLN 中 CD41+ 血小板的数量,增加了搏动性淋巴管的数量、淋巴清除率和 PLN 的体积。此外,抗 PDPN 治疗组明显减轻了后肢水肿和痛感,增加了 BV/TV、骨小梁数(Tb.Th)、编织骨和骨折胼胝体的生物力学特性。本文的转化潜力(1)我们证明了淋巴引流功能对骨折愈合至关重要。(2)为了疏通淋巴引流,防止血液稀释剂带来的出血和死亡风险,我们证明了 PDPN 中和抗体通过消除 LPT 和增加淋巴引流,是治疗骨折愈合的一条新颖而安全的途径。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Orthopaedic Translation
Journal of Orthopaedic Translation Medicine-Orthopedics and Sports Medicine
CiteScore
11.80
自引率
13.60%
发文量
91
审稿时长
29 days
期刊介绍: The Journal of Orthopaedic Translation (JOT) is the official peer-reviewed, open access journal of the Chinese Speaking Orthopaedic Society (CSOS) and the International Chinese Musculoskeletal Research Society (ICMRS). It is published quarterly, in January, April, July and October, by Elsevier.
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