An esterase-responsive ibuprofen nano-micelle pre-modified embryo derived nucleus pulposus progenitor cells promote the regeneration of intervertebral disc degeneration

一种酯酶响应性布洛芬纳米胶束预修饰的胚胎来源髓核祖细胞可促进椎间盘退变的再生。

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作者:Kai-Shun Xia ,Dong-Dong Li ,Cheng-Gui Wang ,Li-Wei Ying ,Jing-Kai Wang ,Biao Yang ,Jia-Wei Shu ,Xian-Peng Huang ,Yu-Ang Zhang ,Chao Yu ,Xiao-Peng Zhou ,Fang-Cai Li ,Nigel K H Slater ,Jian-Bin Tang ,Qi-Xin Chen ,Cheng-Zhen Liang

Abstract

Stem cell-based transplantation is a promising therapeutic approach for intervertebral disc degeneration (IDD). Current limitations of stem cells include with their insufficient cell source, poor proliferation capacity, low nucleus pulposus (NP)-specific differentiation potential, and inability to avoid pyroptosis caused by the acidic IDD microenvironment after transplantation. To address these challenges, embryo-derived long-term expandable nucleus pulposus progenitor cells (NPPCs) and esterase-responsive ibuprofen nano-micelles (PEG-PIB) were prepared for synergistic transplantation. In this study, we propose a biomaterial pre-modification cell strategy; the PEG-PIB were endocytosed to pre-modify the NPPCs with adaptability in harsh IDD microenvironment through inhibiting pyroptosis. The results indicated that the PEG-PIB pre-modified NPPCs exhibited inhibition of pyroptosis in vitro; their further synergistic transplantation yielded effective functional recovery, histological regeneration, and inhibition of pyroptosis during IDD regeneration. Herein, we offer a novel biomaterial pre-modification cell strategy for synergistic transplantation with promising therapeutic effects in IDD regeneration.

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