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骨髓基质细胞作为具有成骨不全表型的转基因小鼠中非造血组织祖细胞的来源。

Marrow stromal cells as a source of progenitor cells for nonhematopoietic tissues in transgenic mice with a phenotype of osteogenesis imperfecta.

作者信息

Pereira R F, O'Hara M D, Laptev A V, Halford K W, Pollard M D, Class R, Simon D, Livezey K, Prockop D J

机构信息

Center for Gene Therapy, Allegheny University of the Health Sciences, Philadelphia, PA 19102-1192, USA.

出版信息

Proc Natl Acad Sci U S A. 1998 Feb 3;95(3):1142-7. doi: 10.1073/pnas.95.3.1142.

Abstract

Marrow stromal cells from wild-type mice were infused into transgenic mice that had a phenotype of fragile bones resembling osteogenesis imperfecta because they expressed a human minigene for type I collagen. In mice that were irradiated with potentially lethal levels (700 cGy) or sublethal levels (350 cGy), DNA from the donor marrow stromal cells was detected consistently in marrow, bone, cartilage, and lung either 1 or 2.5 mo after the infusions. The DNA also was detected but less frequently in the spleen, brain, and skin. There was a small but statistically significant increase in both collagen content and mineral content of bone 1 mo after the infusion. Similar results were obtained with infusion of relatively large amounts of wild-type whole marrow cells into the transgenic mice. In experiments in which male marrow stromal cells were infused into a female osteogenesis imperfecta-transgenic mouse, fluorescense in situ hybridization assays for the Y chromosome indicated that, after 2.5 mo, donor male cells accounted for 4-19% of the fibroblasts or fibroblast-like cells obtained in primary cultures of the lung, calvaria, cartilage, long bone, tail, and skin. In a parallel experiment in which whole marrow cells from a male mouse were infused into a female immunodeficient rag-2 mouse, donor male cells accounted for 4-6% of the fibroblasts or fibroblast-like cells in primary cultures. The results support previous suggestions that marrow stromal cells or related cells in marrow serve as a source for continual renewal of cells in a number of nonhematopoietic tissues.

摘要

将野生型小鼠的骨髓基质细胞注入转基因小鼠体内,这些转基因小鼠由于表达了人I型胶原蛋白小基因而具有类似成骨不全的脆弱骨骼表型。在接受潜在致死剂量(700 cGy)或亚致死剂量(350 cGy)照射的小鼠中,输注后1个月或2.5个月时,在骨髓、骨骼、软骨和肺中均能持续检测到供体骨髓基质细胞的DNA。在脾脏、大脑和皮肤中也检测到了DNA,但频率较低。输注后1个月,骨骼的胶原蛋白含量和矿物质含量均有小幅但具有统计学意义的增加。将相对大量的野生型全骨髓细胞注入转基因小鼠也得到了类似结果。在将雄性骨髓基质细胞注入雌性成骨不全转基因小鼠的实验中,Y染色体的荧光原位杂交分析表明,2.5个月后,供体雄性细胞占肺、颅骨、软骨、长骨、尾巴和皮肤原代培养物中获得的成纤维细胞或成纤维样细胞的4%-19%。在一项平行实验中,将雄性小鼠的全骨髓细胞注入雌性免疫缺陷rag-2小鼠,供体雄性细胞占原代培养物中成纤维细胞或成纤维样细胞的4%-6%。这些结果支持了先前的观点,即骨髓基质细胞或骨髓中的相关细胞是许多非造血组织中细胞持续更新的来源。

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