Karches Center for Chronic Lymphocytic Leukemia Research, The Feinstein Institute for Medical Research, Manhasset, NY 11030, USA.
Proc Natl Acad Sci U S A. 2013 Apr 16;110(16):E1500-7. doi: 10.1073/pnas.1300616110. Epub 2013 Apr 2.
(Auto)antigen engagement by the B-cell receptor (BCR) and possibly the sites where this occurs influence the outcome of chronic lymphocytic leukemia (CLL). To test if selection for autoreactivity leads to increased aggressiveness and if this selection plays out equally in primary and secondary tissues, we used T-cell leukemia (TCL)1 cells reactive with the autoantigen phosphatidylcholine (PtC). After repeated transfers of splenic lymphocytes from a single mouse with oligoclonal PtC-reactive cells, outgrowth of cells expressing a single IGHV-D-J rearrangement and superior PtC-binding and disease virulence occurred. In secondary tissues, increased PtC-binding correlated with enhanced BCR signaling and cell proliferation, whereas reduced signaling and division of cells from the same clone was documented in cells residing in the bone marrow, blood, and peritoneum, even though cells from the last site had highest surface membrane IgM density. Gene-expression analyses revealed reciprocal changes of genes involved in BCR-, CD40-, and PI3K-signaling between splenic and peritoneal cells. Our results suggest autoantigen-stimulated BCR signaling in secondary tissues promotes selection, expansion, and disease progression by activating pro-oncogenic signaling pathways, and that--outside secondary lymphoid tissues--clonal evolution is retarded by diminished BCR-signaling. This transferrable, antigenic-specific murine B-cell clone (TCL1-192) provides a platform to study the types and sites of antigen-BCR interactions and genetic alterations that result and may have relevance to patients.
(自动)B 细胞受体(BCR)的自身抗原结合,以及可能发生这种结合的部位,影响慢性淋巴细胞白血病(CLL)的结局。为了测试自身反应性选择是否会导致侵袭性增加,以及这种选择是否在原发性和继发性组织中同等发挥作用,我们使用了对自身抗原磷脂酰胆碱(PtC)具有反应性的 T 细胞白血病(TCL)1 细胞。在从单个具有寡克隆 PtC 反应性细胞的小鼠中反复转移脾淋巴细胞后,表达单一 IGHV-D-J 重排的细胞和具有优越的 PtC 结合能力和疾病毒力的细胞出现了生长。在继发性组织中,PtC 结合的增加与 BCR 信号转导和细胞增殖增强相关,而在骨髓、血液和腹膜中相同克隆的细胞的信号转导和分裂减少,尽管最后一个部位的细胞具有最高的表面膜 IgM 密度。基因表达分析显示,参与 BCR、CD40 和 PI3K 信号转导的基因在脾细胞和腹膜细胞之间发生了相反的变化。我们的结果表明,继发性组织中自身抗原刺激的 BCR 信号转导通过激活致癌信号通路促进了选择、扩增和疾病进展,并且在外周淋巴组织之外,克隆进化受到 BCR 信号转导的减弱而受到阻碍。这种可转移的、抗原特异性的小鼠 B 细胞克隆(TCL1-192)为研究导致这种情况的抗原-BCR 相互作用和遗传改变的类型和部位提供了一个平台,并且可能与患者相关。