Lab of Normal and Malignant Hematopoiesis, Center for Medical Genetics, Department of Biomolecular Medicine, Ghent University, 9000 Ghent, Belgium.
Cancer Research Institute Ghent (CRIG), Ghent University, 9000 Ghent, Belgium.
Sci Adv. 2024 Nov;10(44):eado6765. doi: 10.1126/sciadv.ado6765. Epub 2024 Nov 1.
T cell acute lymphoblastic leukemia (T-ALL) is an aggressive hematological malignancy. Current intensified therapeutic protocols coincide with severe side effects, and no salvage therapy is available for primary therapy-resistant or relapsed patients. This highlights the need to identify new therapeutic targets in T-ALL. PSIP1, dispensable for normal hematopoiesis, is a dependency factor in -rearranged myeloid leukemia. Nonetheless, loss-of-function mutations suggest a tumor suppressor role for PSIP1 in T-ALL. Here, we demonstrate that the loss of accelerates T-ALL initiation in mice which we correlated with reduced H3K27me3 binding. Contrastingly, loss of PSIP1 impaired cell proliferation in several T-ALL cell lines. In cell lines, PSIP1 down-regulation leads to a reduction of COX20, an assembly factor of the cytochrome c oxidase in the mitochondria, and to a reduction in mitochondrial respiration. This indicates that PSIP1 can exert a dual role in the context of T-ALL, either as a tumor suppressor gene during tumor initiation or as a dependency factor in tumor maintenance.
T 细胞急性淋巴细胞白血病(T-ALL)是一种侵袭性血液系统恶性肿瘤。目前强化的治疗方案与严重的副作用一致,对于原发性治疗耐药或复发的患者没有挽救疗法。这凸显了在 T-ALL 中确定新的治疗靶点的必要性。PSIP1 对正常造血是可有可无的,是重排髓系白血病的依赖因素。尽管如此,功能丧失突变表明 PSIP1 在 T-ALL 中起肿瘤抑制作用。在这里,我们证明了缺失可加速小鼠 T-ALL 的起始,我们将其与 H3K27me3 结合减少相关联。相比之下,PSIP1 的缺失会损害几种 T-ALL 细胞系的细胞增殖。在细胞系中,PSIP1 的下调导致细胞色素 c 氧化酶组装因子 COX20 的减少,以及线粒体呼吸的减少。这表明 PSIP1 在 T-ALL 中可以发挥双重作用,即在肿瘤起始时作为肿瘤抑制基因,或在肿瘤维持时作为依赖性因子。
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