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在一个类似于鼠 ALCL 的模型中存在重编程的淋巴瘤干细胞。

Existence of reprogrammed lymphoma stem cells in a murine ALCL-like model.

机构信息

Department of Medicine I, Medical Center-University of Freiburg, Faculty of Medicine, University of Freiburg, 79106, Freiburg, Germany.

German Cancer Consortium (DKTK) and German Cancer Research Center (DKFZ), 69120, Heidelberg, Germany.

出版信息

Leukemia. 2020 Dec;34(12):3242-3255. doi: 10.1038/s41375-020-0789-x. Epub 2020 Mar 17.

Abstract

While cancer stem cells are well established in certain hematologic and solid malignancies, their existence in T cell lymphoma is unclear and the origin of disease is not fully understood. To examine the existence of lymphoma stem cells, we utilized a mouse model of anaplastic large cell lymphoma. Established NPM-ALK lymphomas contained heterogeneous cell populations ranging from mature T cells to undifferentiated hematopoietic stem cells. Interestingly, CD4/CD8 double negative (DN) lymphoma cells aberrantly expressed the T cell receptor α/β chain. Serial transplantation of sorted CD4/CD8 and DN lymphoma subpopulations identified lymphoma stem cells within the DN3/DN4 T cell population, whereas all other subpopulations failed to establish serial lymphomas. Moreover, transplanted lymphoma DN3/DN4 T cells were able to differentiate and gave rise to mature lymphoma T cells. Gene expression analyses unmasked stem-cell-like transcriptional regulation of the identified lymphoma stem cell population. Furthermore, these lymphoma stem cells are characterized by low CD30 expression levels, which might contribute to limited long-term therapeutic success in patients treated with anti-CD30-targeted therapies. In summary, our results highlight the existence of a lymphoma stem cell population in a NPM-ALK-driven CD30 mouse model, thereby giving the opportunity to test innovative treatment strategies developed to eradicate the origin of disease.

摘要

虽然癌症干细胞在某些血液系统和实体恶性肿瘤中已经得到很好的确立,但它们在 T 细胞淋巴瘤中的存在尚不清楚,疾病的起源也不完全清楚。为了研究淋巴瘤干细胞的存在,我们利用了一种间变性大细胞淋巴瘤的小鼠模型。已建立的 NPM-ALK 淋巴瘤包含从成熟 T 细胞到未分化造血干细胞的异质细胞群体。有趣的是,CD4/CD8 双阴性(DN)淋巴瘤细胞异常表达 T 细胞受体 α/β 链。对分选的 CD4/CD8 和 DN 淋巴瘤亚群进行连续移植,鉴定出 DN3/DN4 T 细胞群内的淋巴瘤干细胞,而其他所有亚群均未能建立连续淋巴瘤。此外,移植的淋巴瘤 DN3/DN4 T 细胞能够分化,并产生成熟的淋巴瘤 T 细胞。基因表达分析揭示了鉴定的淋巴瘤干细胞群体中具有干细胞样转录调控。此外,这些淋巴瘤干细胞的特征是低 CD30 表达水平,这可能导致接受抗 CD30 靶向治疗的患者的长期治疗效果有限。总之,我们的结果强调了 NPM-ALK 驱动的 CD30 小鼠模型中存在淋巴瘤干细胞群体,从而为测试旨在根除疾病起源的创新治疗策略提供了机会。

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