Martin Colin H, Aifantis Iannis, Scimone M Lucila, von Andrian Ulrich H, Reizis Boris, von Boehmer Harald, Gounari Fotini
Department of Pathology, Harvard Medical School, Dana-Farber Cancer Institute Boston, Massachusetts, 02115, USA.
Nat Immunol. 2003 Sep;4(9):866-73. doi: 10.1038/ni965. Epub 2003 Aug 17.
Using a human CD25 reporter transgene controlled by regulatory sequences from the gene encoding pre-T cell receptor alpha, we identified a common lymphocyte precursor (CLP-2) population that, in contrast to the previously identified CLP-1 population, was c-Kit-B220+. In short-term culture, the CLP-2 could be derived from the CLP-1 subset, and contained cells that in clonogenic assays were assessed to be bipotent precursors of T and B cells. Intravenous injection of bone marrow cells yielded a selective accumulation of CLP-2 thymic immigrants that in thymic organ culture generated mature alphabeta T cells. Although the CLP-2 subset may represent the most differentiated population with T cell potential before commitment to the B cell lineage, other subsets of thymic immigrants capable of generating T cells may exist.
利用由编码前T细胞受体α的基因的调控序列控制的人类CD25报告基因转基因,我们鉴定出了一个常见淋巴细胞前体(CLP-2)群体,与先前鉴定的CLP-1群体不同,该群体是c-Kit+B220+。在短期培养中,CLP-2可源自CLP-1亚群,并且包含在克隆形成试验中被评估为T细胞和B细胞双能前体的细胞。静脉注射骨髓细胞会导致CLP-2胸腺移民的选择性积累,这些移民在胸腺器官培养中产生成熟的αβT细胞。尽管CLP-2亚群可能代表在定向分化为B细胞谱系之前具有T细胞潜能的最分化群体,但可能存在其他能够产生T细胞的胸腺移民亚群。
