FAT10 Combined with Miltefosine Inhibits Mitochondrial Apoptosis and Energy Metabolism in Hypoxia-Induced H9C2 Cells by Regulating the PI3K/AKT Signaling Pathway

Yao, Yi; Jia, Weikun; Zeng, Xiaofei; Wang, Yali; Hu, Qiuxia; Yu, Shiran; He, Dongsheng; Li, Ying

doi:10.1155/2022/4388919

Cited by 1 publication

(1 citation statement)

References 45 publications

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“…This suggested that the activation of FAT10-mTORC1 signaling pathway caused by loss of Celf2 is independent to the MA9-DOT1L signaling pathway. FAT10 belongs to the ubiquitin-like protein family and was demonstrated to be able to increase AKT phosphorylation, and thereby activate the mTORC1 signaling pathway [43][44][45][46]. In Yan's study, FAT10 was shown to activate AKT signaling by stabilizing EGFR in bladder cancer cells [44].…”

Section: Discussionmentioning

confidence: 99%

Loss of RNA-binding protein CELF2 promotes acute leukemia development via FAT10-mTORC1

Guo,

Wang,

Sun

et al. 2024

Oncogene

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RNA-binding proteins (RBPs) are critical regulators for RNA transcription and translation. As a key member of RBPs, ELAV-like family protein 2 (CELF2) has been shown to regulate RNA splicing and embryonic hematopoietic development and was frequently seen dysregulated in acute myeloid leukemia (AML). However, the functional role(s) of CELF2 in hematopoiesis and leukemogenesis has not been fully elucidated. In the current study, we showed that Celf2 deficiency in hematopoietic system led to enhanced HSCs self-renewal and differentiation toward myeloid cells in mice. Loss of Celf2 accelerated myeloid cell transformation and AML development in MLL-AF9-induced AML murine models. Gene expression profiling integrated with RNA immunoprecipitation sequencing (RIP-Seq), together with biochemical experiments revealed that CELF2 deficiency stabilizes FAT10 mRNA, promotes FAT10 translation, thereby increases AKT phosphorylation and mTORC1 signaling pathway activation. Notably, combination therapy with a mTORC1 inhibitor (Rapamycin) and a MA9/DOTL1 inhibitor (EPZ-5676) reduced the leukemia burden in MLL-AF9 mice lacking Celf2 in vivo. Our study elucidated a novel mechanism by which the CELF2/FAT10-AKT/mTORC1 axis regulates the proliferation of normal blood cells and the development of AML, thus providing potential therapeutic targets for myeloid leukemia suppression.

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