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低粘附支架胶原蛋白(LASCol)通过自发形成球体减少髓核切除术引起的椎间盘破裂。

Reduced nucleotomy-induced intervertebral disc disruption through spontaneous spheroid formation by the Low Adhesive Scaffold Collagen (LASCol).

作者信息

Takeoka Yoshiki, Yurube Takashi, Morimoto Koichi, Kunii Saori, Kanda Yutaro, Tsujimoto Ryu, Kawakami Yohei, Fukase Naomasa, Takemori Toshiyuki, Omae Kaoru, Kakiuchi Yuji, Miyazaki Shingo, Kakutani Kenichiro, Takada Toru, Nishida Kotaro, Fukushima Masanori, Kuroda Ryosuke

机构信息

Department of Orthopaedic Surgery, Kobe University Graduate School of Medicine, 7-5-1 Kusunoki-cho, Chuo-ku, Kobe, 650-0017, Japan.

Department of Genetic Engineering, Faculty of Biology-Oriented Science and Technology, Kindai University, 930 Nishimitani, Kinokawa, Wakayama, 649-6493, Japan.

出版信息

Biomaterials. 2020 Mar;235:119781. doi: 10.1016/j.biomaterials.2020.119781. Epub 2020 Jan 11.

Abstract

Back pain is a global health problem with a high morbidity and socioeconomic burden. Intervertebral disc herniation and degeneration are its primary cause, further associated with neurological radiculopathy, myelopathy, and paralysis. The current surgical treatment is principally discectomy, resulting in the loss of spinal movement and shock absorption. Therefore, the development of disc regenerative therapies is essential. Here we show reduced disc damage by a new collagen type I-based scaffold through actinidain hydrolysis-Low Adhesive Scaffold Collagen (LASCol)-with a high 3D spheroid-forming capability, water-solubility, and biodegradability and low antigenicity. In human disc nucleus pulposus and annulus fibrosus cells surgically obtained, time-dependent spheroid formation with increased expression of phenotypic markers and matrix components was observed on LASCol but not atelocollagen (AC). In a rat tail nucleotomy model, LASCol-injected and AC-injected discs presented relatively similar radiographic and MRI damage control; however, LASCol, distinct from AC, decelerated histological disc disruption, showing collagen type I-comprising LASCol degradation, aggrecan-positive and collagen type II-positive endogenous cell migration, and M1-polarized and also M2-polarized macrophage infiltration. Reduced nucleotomy-induced disc disruption through spontaneous spheroid formation by LASCol warrants further investigations of whether it may be an effective treatment without stem cells and/or growth factors for intervertebral disc disease.

摘要

背痛是一个全球性的健康问题,发病率高,社会经济负担重。椎间盘突出和退变是其主要原因,还会进一步引发神经型神经根病、脊髓病和瘫痪。目前的手术治疗主要是椎间盘切除术,会导致脊柱运动和减震功能丧失。因此,椎间盘再生疗法的发展至关重要。在此,我们展示了一种新型的基于I型胶原蛋白的支架——经猕猴桃蛋白酶水解的低粘附性支架胶原蛋白(LASCol),它具有高3D球状体形成能力、水溶性、生物降解性和低抗原性,可减少椎间盘损伤。在手术获取的人椎间盘髓核和纤维环细胞中,在LASCol上观察到了随时间的球状体形成,且表型标记物和基质成分的表达增加,而在去端胶原蛋白(AC)上则未观察到。在大鼠尾椎核切除术模型中,注射LASCol和AC的椎间盘在影像学和MRI损伤控制方面表现相对相似;然而,与AC不同的是,LASCol减缓了组织学上的椎间盘破坏,表现为包含LASCol降解的I型胶原蛋白、聚集蛋白聚糖阳性和II型胶原蛋白阳性的内源性细胞迁移,以及M1极化和M2极化的巨噬细胞浸润。LASCol通过自发球状体形成减少核切除诱导的椎间盘破坏,这使得有必要进一步研究它是否可能是一种无需干细胞和/或生长因子即可有效治疗椎间盘疾病的方法。

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