Cancer Science Institute of Singapore, National University of, Singapore, 117599, Singapore.
Department of Tumor Immunology, Aichi Medical University School of Medicine, Nagakute, 480-1195, Japan.
Leukemia. 2022 Sep;36(9):2293-2305. doi: 10.1038/s41375-022-01655-5. Epub 2022 Jul 30.
Adult T-cell leukemia/lymphoma (ATL) is a genetically complex hematological malignancy derived from mature T cells. Using an integrative approach, we previously identified genes recurrently associated with super-enhancers in ATL. One of those genes was TP73, a TP53 family gene; however, the roles and function of TP73 and its super-enhancer in ATL pathogenesis are poorly understood. Our study demonstrates that TP73 is highly activated under the control of a super-enhancer in ATL cells but not in normal T cells or other hematological malignancies examined. Full-length TP73 is required for ATL cell maintenance in vitro and in vivo via the regulation of cell proliferation and DNA damage response pathways. Notably, recurrent deletions of TP73 exons 2-3 were observed in a fraction of primary ATL cases that harbored the super-enhancer, while induction of this deletion in cell lines further increased proliferation and mutational burden. Our study suggests that formation of the TP73 intragenic super-enhancer and genetic deletion are likely sequentially acquired in relation to intracellular state of ATL cells, which leads to functional alteration of TP73 that confers additional clonal advantage.
成人 T 细胞白血病/淋巴瘤 (ATL) 是一种源自成熟 T 细胞的遗传复杂的血液恶性肿瘤。我们之前采用整合方法鉴定了与 ATL 中超增强子反复相关的基因,其中一个基因是 TP73,即 TP53 家族基因;然而,TP73 及其在 ATL 发病机制中的超增强子的作用和功能还知之甚少。我们的研究表明,在 ATL 细胞中,TP73 受超增强子的控制而高度激活,但在正常 T 细胞或其他检查的血液恶性肿瘤中则不然。全长 TP73 通过调节细胞增殖和 DNA 损伤反应途径,体外和体内维持 ATL 细胞的存活。值得注意的是,在存在超增强子的一部分原发性 ATL 病例中观察到 TP73 外显子 2-3 的反复缺失,而在细胞系中诱导这种缺失进一步增加了增殖和突变负担。我们的研究表明,TP73 基因内超增强子的形成和遗传缺失可能与 ATL 细胞的细胞内状态相关,这导致了 TP73 的功能改变,赋予了额外的克隆优势。
