Telmo A Catarino, Ivette Pacheco-Leyva, Marina Baessa, João L Pereira, Nuno R Dos Santos
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引用次数: 0
摘要
前 T 细胞受体(TCR)和 TCR 复合物经常在 T 细胞急性淋巴细胞白血病(T-ALL)中表达,T-ALL 是一种侵袭性 T 细胞前体恶性肿瘤。虽然 TCR 成分的突变在 T-ALL 中并不常见,但早期研究表明,小鼠 T 细胞前体中转基因 αβ TCR 的表达促进了 T-ALL 的发展。然而,我们最近发现,刺激 TCR 在 T-ALL 中的信号传导可诱导白血病细胞凋亡并抑制白血病。我们的目的是阐明特定的 αβ TCR 复合物在白血病发生中是否具有双重作用,这取决于刺激的性质。我们证明,转基因表达对主要组织相容性复合体 II 类呈现的 H-Y 雄性抗原特异的 Marilyn αβ TCR 只在雌性小鼠中引发 T-ALL 的发生。这种 T-ALL 表现出 Notch1 突变、Cdkn2a 拷贝数丢失、免疫表型不成熟,并浸润淋巴和非淋巴器官。此外,白血病细胞表达表面 CD5,这是强直性 TCR 信号转导的标志物。在Rag2缺陷的Marilyn转基因雌鼠中,T-ALL有效地发展,这表明Rag2介导的重组与这种T-ALL模型无关。在OT-I TCR转基因小鼠模型中也观察到了T-ALL的发生,但当通过β2-微球蛋白的基因失活来消除MHC I类时,T-ALL并没有发生。值得注意的是,将玛丽莲雌性T-ALL细胞暴露于雄性受体小鼠的内源性激动剂抗原或雌性受体小鼠的外源性多肽会导致T-ALL细胞凋亡并延长小鼠存活时间。这些发现强调了同一 αβ TCR 复合物在 T-ALL 中的双重作用,即强刺激可致白血病,而强刺激可抑制白血病。
Transgenic αβ TCR tonic signaling is leukemogenic while strong stimulation is leukemia-suppressive.
The pre-T cell receptor (TCR) and TCR complexes are frequently expressed in T-cell acute lymphoblastic leukemia (T-ALL), an aggressive T cell precursor malignancy. Although mutations in TCR components are infrequent in T-ALL, earlier research indicated that transgenic αβ TCR expression in mouse T cell precursors promoted T-ALL development. However, we recently found that stimulation of TCR signaling in T-ALL induced leukemic cell apoptosis and suppressed leukemia. Our aim was to elucidate if a given αβ TCR complex has a dual role in leukemogenesis depending on the nature of the stimulus. We demonstrate that transgenic expression of the Marilyn αβ TCR, specific for the H-Y male antigen presented by major histocompatibility complex class II, triggers T-ALL development exclusively in female mice. This T-ALL exhibited Notch1 mutations, Cdkn2a copy number loss, immature immunophenotype and infiltrated both lymphoid and non-lymphoid organs. Furthermore, leukemic cells expressed surface CD5, a marker of tonic TCR signaling. T-ALL efficiently developed in Rag2-deficient Marilyn transgenic females, indicating that Rag2-mediated recombination is not implicated in this T-ALL model. T-ALL development was also observed in the OT-I TCR transgenic mouse model, but it did not occur when MHC class I was abrogated through genetic inactivation of β2-microglobulin. Remarkably, exposure of Marilyn female T-ALL cells to endogenous agonist antigen in male recipient mice or exogenous peptide in female recipient mice resulted in T-ALL apoptosis and prolonged mouse survival. These findings underscore the dual role of the same αβ TCR complex in T-ALL, where tonic stimulation is leukemogenic, while strong stimulation suppresses leukemia.
期刊介绍:
JLB is a peer-reviewed, academic journal published by the Society for Leukocyte Biology for its members and the community of immunobiologists. The journal publishes papers devoted to the exploration of the cellular and molecular biology of granulocytes, mononuclear phagocytes, lymphocytes, NK cells, and other cells involved in host physiology and defense/resistance against disease. Since all cells in the body can directly or indirectly contribute to the maintenance of the integrity of the organism and restoration of homeostasis through repair, JLB also considers articles involving epithelial, endothelial, fibroblastic, neural, and other somatic cell types participating in host defense. Studies covering pathophysiology, cell development, differentiation and trafficking; fundamental, translational and clinical immunology, inflammation, extracellular mediators and effector molecules; receptors, signal transduction and genes are considered relevant. Research articles and reviews that provide a novel understanding in any of these fields are given priority as well as technical advances related to leukocyte research methods.