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用于退变椎间盘的半合成可降解脊索细胞衍生基质水凝胶:初步体外表征。

Semi-synthetic degradable notochordal cell-derived matrix hydrogel for use in degenerated intervertebral discs: Initial in vitro characterization.

机构信息

Orthopaedic Biomechanics, Department of Biomedical Engineering, Eindhoven University of Technology, Eindhoven, The Netherlands.

SyMO-Chem BV, Eindhoven, The Netherlands.

出版信息

J Biomed Mater Res A. 2023 Dec;111(12):1903-1915. doi: 10.1002/jbm.a.37594. Epub 2023 Aug 4.

Abstract

Low back pain is the leading cause of disability worldwide, but current therapeutic interventions are palliative or surgical in nature. Loss of notochordal cells (NCs) and degradation of the healthy matrix in the nucleus pulposus (NP), the central tissue of intervertebral discs (IVDs), has been associated with onset of degenerative disc changes. Recently, we established a protocol for decellularization of notochordal cell derived matrix (NCM) and found that it can provide regenerative cues to nucleus pulposus cells of the IVD. Here, we combined the biologically regenerative properties of decellularized NCM with the mechanical tunability of a poly(ethylene glycol) hydrogel to additionally address biomechanics in the degenerate IVD. We further introduced a hydrolysable PEG-diurethane crosslinker for slow degradation of the gels in vivo. The resulting hydrogels were tunable over a broad range of stiffness's (0.2 to 4.5 kPa), matching that of NC-rich and -poor NP tissues, respectively. Gels formed within 30 min, giving ample time for handling, and remained shear-thinning post-polymerization. Gels also slowly released dNCM over 28 days as measured by GAG effusion. Viability of encapsulated bone marrow stromal cells after extrusion through a needle remained high. Although encapsulated NCs stayed viable over two weeks, their metabolic activity decreased, and their phenotype was lost in physiological medium conditions in vitro. Overall, the obtained gels hold promise for application in degenerated IVDs but require further tuning for combined use with NCs.

摘要

下背痛是全球导致残疾的主要原因,但目前的治疗干预措施要么是姑息性的,要么是手术性的。脊索细胞(NCs)的丧失和椎间盘(IVD)中央组织髓核中健康基质的降解,与退行性椎间盘变化的发生有关。最近,我们建立了一种脱细胞脊索细胞衍生基质(NCM)的方案,发现它可以为 IVD 的髓核细胞提供再生线索。在这里,我们将脱细胞 NCM 的生物再生特性与聚乙二醇(PEG)水凝胶的机械可调性相结合,以进一步解决退变 IVD 的生物力学问题。我们进一步引入了一种可水解的 PEG-二异氰酸酯交联剂,以在体内缓慢降解凝胶。所得水凝胶的弹性模量可在较宽的范围内(0.2 至 4.5 kPa)进行调节,分别与富含 NC 和 NC 较少的 NP 组织相匹配。凝胶在 30 分钟内形成,有足够的时间进行处理,并且在聚合后仍保持剪切变稀。凝胶还可以在 28 天内缓慢释放 dNCM,通过 GAG 渗出来测量。通过针头挤出后,包封的骨髓基质细胞的活力仍然很高。尽管包封的 NC 在两周内保持存活,但它们的代谢活性下降,并且在体外生理条件下其表型丧失。总的来说,所获得的凝胶有望应用于退变的 IVD,但需要进一步调整以与 NC 联合使用。

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