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通过移植正常和Gsα突变的骨骼祖细胞嵌合体在免疫受损小鼠中重现人类骨纤维发育不良

Reproduction of human fibrous dysplasia of bone in immunocompromised mice by transplanted mosaics of normal and Gsalpha-mutated skeletal progenitor cells.

作者信息

Bianco P, Kuznetsov S A, Riminucci M, Fisher L W, Spiegel A M, Robey P G

机构信息

Department of Experimental Medicine, L'Aquila 67100; University "La Sapienza," Rome 00161, Italy.

出版信息

J Clin Invest. 1998 Apr 15;101(8):1737-44. doi: 10.1172/JCI2361.

Abstract

We have isolated progenitor cells from the stromal system of the fibrous dysplastic marrow of patients with McCune-Albright Syndrome. Analysis of the Gsalpha gene from individual colonies provided direct evidence for the presence of two different genotypes within single fibrous dysplastic lesions: marrow stromal cells containing two normal Gsalpha alleles, and those containing one normal allele and an allele with an activating mutation. Transplantation of clonal populations of normal cells into the subcutis of immunocompromised mice resulted in normal ossicle formation. In contrast, transplantation of clonal populations of mutant cells always led to the loss of transplanted cells from the transplantation site and no ossicle formation. However, transplantation of a mixture of normal and mutant cells reproduced an abnormal ectopic ossicle recapitulating human fibrous dysplasia and providing an in vivo cellular model of this disease. These results provide experimental evidence for the necessity of both normal and mutant cells in the development of McCune-Albright Syndrome fibrous dysplastic lesions in bone.

摘要

我们已经从患有McCune - Albright综合征患者的纤维发育异常骨髓的基质系统中分离出祖细胞。对单个集落的Gsalpha基因分析提供了直接证据,表明在单个纤维发育异常病变中存在两种不同的基因型:含有两个正常Gsalpha等位基因的骨髓基质细胞,以及含有一个正常等位基因和一个具有激活突变等位基因的细胞。将正常细胞的克隆群体移植到免疫受损小鼠的皮下,导致正常小骨形成。相反,突变细胞的克隆群体移植总是导致移植细胞从移植部位丢失,且无小骨形成。然而,正常细胞和突变细胞的混合物移植再现了异常的异位小骨,重现了人类纤维发育异常,并提供了该疾病的体内细胞模型。这些结果为正常细胞和突变细胞在McCune - Albright综合征骨纤维发育异常病变发展中的必要性提供了实验证据。

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