| Literature DB >> 33223332 |
Yaming Yang1, Yongheng Fan1, Haipeng Zhang1, Qi Zhang2, Yannan Zhao2, Zhifeng Xiao2, Wenbin Liu2, Bing Chen2, Lin Gao1, Zheng Sun1, Xiaoyu Xue1, Muya Shu1, Jianwu Dai3.
Abstract
Complete spinal cord injury (SCI) leads to cell death, interruption of axonal connections and permanent functional impairments. In the development of SCI treatments, cell transplantation combined with biomaterial-growth factor-based therapies have been widely studied. Another avenue worth exploring is the generation of neurons from endogenous neural stem cells (NSCs) or reactive astrocytes activated by SCI. Here, we screened a combination of four small molecules, LDN193189, SB431542, CHIR99021 and P7C3-A20, that can increase neuronal differentiation of mouse and rat spinal cord NSCs. Moreover, the small molecules loaded in an injectable collagen hydrogel induced neurogenesis and inhibited astrogliogenesis of endogenous NSCs in the injury site, which usually differentiate into astrocytes under pathological conditions. Meanwhile, induced neurons migrated into the non-neural lesion core, and genetic fate mapping showed that neurons mainly originated from NSCs in the parenchyma, but not from the central canal of the spinal cord. The neuronal regeneration in the lesion sites resulted in some recovery of locomotion. Our findings indicate that the combined treatment of small molecules and collagen hydrogel is a potential therapeutic strategy for SCI by inducing in situ endogenous NSCs to form neurons and restore damaged functions.Entities:
Keywords: Collagen hydrogel; Complete spinal cord injury; In vivo; Migration; Neural stem cells; Neurogenesis; Small molecules
Year: 2020 PMID: 33223332 DOI: 10.1016/j.biomaterials.2020.120479
Source DB: PubMed Journal: Biomaterials ISSN: 0142-9612 Impact factor: 12.479