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髓鞘非依赖性的犬胶质限制前体细胞在脱髓鞘疾病小鼠模型中的治疗潜力。

Myelin-Independent Therapeutic Potential of Canine Glial-Restricted Progenitors Transplanted in Mouse Model of Dysmyelinating Disease.

机构信息

NeuroRepair Department, Mossakowski Medical Research Institute, Polish Academy of Sciences, 02-106 Warsaw, Poland.

Medical Research Agency, 02-106 Warsaw, Poland.

出版信息

Cells. 2021 Nov 1;10(11):2968. doi: 10.3390/cells10112968.

Abstract

BACKGROUND

Dysfunction of glia contributes to the deterioration of the central nervous system in a wide array of neurological disorders, thus global replacement of glia is very attractive. Human glial-restricted precursors (hGRPs) transplanted intraventricularly into neonatal mice extensively migrated and rescued the lifespan in half of the studied mice, whereas mouse GRPs (mGRPs) presented no therapeutic benefit. We studied in the same experimental setting canine GRPs (cGRP) to determine whether their therapeutic potential falls between hGRPs and mGRPs. Additional motivation for the selection of cGRPs was a potential for use in veterinary medicine.

METHODS

cGRPs were extracted from the brain of dog fetuses. The cells were transplanted into the anterior or posterior aspect of the lateral ventricle (LV) of neonatal, immunodeficient, dysmyelinated mice (, KO; shiv/rag2). Outcome measures included early cell biodistribution, animal survival and myelination assessed with MRI, immunohistochemistry and electron microscopy.

RESULTS

Grafting of cGRP into posterior LV significantly extended animal survival, whereas no benefit was observed after anterior LV transplantation. In contrast, myelination of the corpus callosum was more prominent in anteriorly transplanted animals.

CONCLUSIONS

The extended survival of animals after transplantation of cGRPs could be explained by the vicinity of the transplant near the brain stem.

摘要

背景

神经胶质功能障碍导致广泛的神经退行性疾病的中枢神经系统恶化,因此,胶质细胞的全面替代非常有吸引力。人类神经胶质限制前体细胞(hGRPs)被移植到新生小鼠的侧脑室中,广泛迁移并挽救了一半研究小鼠的寿命,而鼠 GRPs(mGRPs)则没有治疗益处。我们在相同的实验环境中研究犬 GRPs(cGRPs),以确定它们的治疗潜力是否介于 hGRPs 和 mGRPs 之间。选择 cGRPs 的另一个动机是它们有可能在兽医医学中使用。

方法

从犬胎脑提取 cGRPs。将细胞移植到新生、免疫缺陷、脱髓鞘小鼠(, KO;shiv/rag2)的侧脑室(LV)前或后角。观察指标包括早期细胞分布、动物存活和 MRI、免疫组织化学和电子显微镜评估的髓鞘形成。

结果

cGRP 移植到后 LV 显著延长了动物的存活时间,而前 LV 移植则没有益处。相比之下,在前向移植的动物中,胼胝体的髓鞘形成更为明显。

结论

cGRPs 移植后动物存活时间的延长可以用移植靠近脑干的位置来解释。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1b0d/8616327/ef1664f1b957/cells-10-02968-g001.jpg

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