Your search keyword '"Peng, Meixi"' showing total 15 results

1. A novel LGALS1-depended and immune-associated fatty acid metabolism risk model in acute myeloid leukemia stem cells

Author

Qin, Huanhuan, Peng, Meixi, Cheng, Jingsong, Wang, Zhenyu, Cui, Yinghui, Huang, Yongxiu, Gui, Yaoqi, Sun, Yanni, Xiang, Wenqiong, Huang, Xiaomei, Huang, Ting, Wang, Li, Chen, Jieping, and Hou, Yu

Published

2024

2. Oxidized ATM governs stemness of breast cancer stem cell through regulating ubiquitylation and acetylation switch

Author

Zhou, Xinyue, Liu, Xiaoqi, Wan, Xueying, Xu, Ming, Wang, Rui, Yang, Dan, Peng, Meixi, Jin, Ting, Tang, Rui, Liu, Manran, and Hou, Yixuan

Published

2024

3. Retraction Note: Intracellular citrate accumulation by oxidized ATM-mediated metabolism reprogramming via PFKP and CS enhances hypoxic breast cancer cell invasion and metastasis

Author

Peng, Meixi, Yang, Dan, Hou, Yixuan, Liu, Shuiqing, Zhao, Maojia, Qin, Yilu, Chen, Rui, Teng, Yong, and Liu, Manran

Published

2023

4. Targeted activation of GPER enhances the efficacy of venetoclax by boosting leukemic pyroptosis and CD8+ T cell immune function in acute myeloid leukemia

Author

Ren, Jun, Tao, Yonghong, Peng, Meixi, Xiao, Qiaoling, Jing, Yipei, Huang, Junpeng, Yang, Jing, Lin, Can, Sun, Minghui, Lei, Li, Yang, Zesong, Yang, Zailin, and Zhang, Ling

Published

2022

5. LAPTM4B promotes AML progression through regulating RPS9/STAT3 axis

Author

Huang, Yongxiu, primary, Peng, Meixi, additional, Qin, Huanhuan, additional, Li, Yan, additional, Pei, Li, additional, Liu, Xindong, additional, and Zhao, Xueya, additional

Published

2023

6. Cytoplasmic Expression of TP53INP2 Modulated by Demethylase FTO and Mutant NPM1 Promotes Autophagy in Leukemia Cells

Author

Huang, Junpeng, primary, Sun, Minghui, additional, Tao, Yonghong, additional, Ren, Jun, additional, Peng, Meixi, additional, Jing, Yipei, additional, Xiao, Qiaoling, additional, Yang, Jing, additional, Lin, Can, additional, Lei, Li, additional, Yang, Zailin, additional, and Zhang, Ling, additional

Published

2023

7. Circulating plasma exosomal long non-coding RNAs LINC00265, LINC00467, UCA1, and SNHG1 as biomarkers for diagnosis and treatment monitoring of acute myeloid leukemia

Author

Xiao, Qiaoling, primary, Lin, Can, additional, Peng, Meixi, additional, Ren, Jun, additional, Jing, Yipei, additional, Lei, Li, additional, Tao, Yonghong, additional, Huang, Junpeng, additional, Yang, Jing, additional, Sun, Minghui, additional, Wu, Jing, additional, Yang, Zailin, additional, Yang, Zesong, additional, and Zhang, Ling, additional

Published

2022

8. A Novel Long Non‐Coding RNA lnc030 Maintains Breast Cancer Stem Cell Stemness by Stabilizing SQLE mRNA and Increasing Cholesterol Synthesis

Author

Qin, Yilu, primary, Hou, Yixuan, additional, Liu, Shuiqing, additional, Zhu, Pengpeng, additional, Wan, Xueying, additional, Zhao, Maojia, additional, Peng, Meixi, additional, Zeng, Huan, additional, Li, Qiao, additional, Jin, Ting, additional, Cui, Xiaojiang, additional, and Liu*, Manran, additional

Published

2022

9. Targeting Mitochondrial Oxidative Phosphorylation Eradicates Acute Myeloid Leukemic Stem Cells

Author

Peng, Meixi, primary, Huang, Yongxiu, additional, Zhang, Ling, additional, Zhao, Xueya, additional, and Hou, Yu, additional

Published

2022

10. Mutant NPM1-Regulated FTO-Mediated m6A Demethylation Promotes Leukemic Cell Survival via PDGFRB/ERK Signaling Axis

Author

Xiao, Qiaoling, Lei, Li, Ren, Jun, Peng, Meixi, Jing, Yipei, Jiang, Xueke, Huang, Junpeng, Tao, Yonghong, Lin, Can, Yang, Jing, Sun, Minghui, Tang, Lisha, Wei, Xingyu, Yang, Zailin, and Zhang, Ling

Subjects

Cancer Research, Oncology, N6-methyladenosine, hemic and lymphatic diseases, nucleophosmin 1, PDGFRB, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, acute myeloid leukemia, FTO, ERK cascade, RC254-282

Abstract

Acute myeloid leukemia (AML) with nucleophosmin 1 (NPM1) mutations exhibits distinct biological and clinical features, accounting for approximately one-third of AML. Recently, the N6-methyladenosine (m6A) RNA modification has emerged as a new epigenetic modification to contribute to tumorigenesis and development. However, there is limited knowledge on the role of m6A modifications in NPM1-mutated AML. In this study, the decreased m6A level was first detected and high expression of fat mass and obesity-associated protein (FTO) was responsible for the m6A suppression in NPM1-mutated AML. FTO upregulation was partially induced by NPM1 mutation type A (NPM1-mA) through impeding the proteasome pathway. Importantly, FTO promoted leukemic cell survival by facilitating cell cycle and inhibiting cell apoptosis. Mechanistic investigations demonstrated that FTO depended on its m6A RNA demethylase activity to activate PDGFRB/ERK signaling axis. Our findings indicate that FTO-mediated m6A demethylation plays an oncogenic role in NPM1-mutated AML and provide a new layer of epigenetic insight for future treatments of this distinctly leukemic entity.

Published

2022

11. Targeted Activation of GPER Enhances the Efficacy of Venetoclax by Boosting Leukemic Pyroptosis and Cd8 + T Cell Immune Function in Acute Myeloid Leukemia

Author

Ren, Jun, primary, Tao, Yonghong, additional, Peng, Meixi, additional, Xiao, Qiaoling, additional, Jing, Yipei, additional, Huang, Junpeng, additional, Yang, Jing, additional, Lin, Can, additional, Sun, Minghui, additional, Lei, Li, additional, Yang, Zesong, additional, Yang, Zailin, additional, and Zhang, Ling, additional

Published

2022

12. Oxidized ATM Governs Stemness of Breast Cancer Stem Cell Through Regulating Ubiquitylation and Acetylation Switch

Author

Zhou, Xinyue, primary, Liu, Xiaoqi, additional, Wan, Xueying, additional, Yang, Dang, additional, Peng, Meixi, additional, Wang, Rui, additional, Jin, Ting, additional, Tang, Rui, additional, Liu, Manran, additional, and Hou, Yixuan, additional

Published

2022

13. Tumour‐derived small extracellular vesicles suppress CD8+ T cell immune function by inhibiting SLC6A8‐mediated creatine import in NPM1‐mutated acute myeloid leukaemia

Author

Peng, Meixi, primary, Ren, Jun, additional, Jing, Yipei, additional, Jiang, Xueke, additional, Xiao, Qiaoling, additional, Huang, Junpeng, additional, Tao, Yonghong, additional, Lei, Li, additional, Wang, Xin, additional, Yang, Zailin, additional, Yang, Zesong, additional, Zhan, Qian, additional, Lin, Can, additional, Jin, Guoxiang, additional, Zhang, Xian, additional, and Zhang, Ling, additional

Published

2021

14. Mutant NPM1-Regulated FTO-Mediated m6A Demethylation Promotes Leukemic Cell Survival via PDGFRB/ERK Signaling Axis.

Author

Xiao, Qiaoling, Lei, Li, Ren, Jun, Peng, Meixi, Jing, Yipei, Jiang, Xueke, Huang, Junpeng, Tao, Yonghong, Lin, Can, Yang, Jing, Sun, Minghui, Tang, Lisha, Wei, Xingyu, Yang, Zailin, and Zhang, Ling

Subjects

CELL survival, ACUTE myeloid leukemia, DEMETHYLATION, RNA modification & restriction, ADIPOSE tissues

Abstract

Acute myeloid leukemia (AML) with nucleophosmin 1 (NPM1) mutations exhibits distinct biological and clinical features, accounting for approximately one-third of AML. Recently, the N 6-methyladenosine (m6A) RNA modification has emerged as a new epigenetic modification to contribute to tumorigenesis and development. However, there is limited knowledge on the role of m6A modifications in NPM1-mutated AML. In this study, the decreased m6A level was first detected and high expression of fat mass and obesity-associated protein (FTO) was responsible for the m6A suppression in NPM1-mutated AML. FTO upregulation was partially induced by NPM1 mutation type A (NPM1-mA) through impeding the proteasome pathway. Importantly, FTO promoted leukemic cell survival by facilitating cell cycle and inhibiting cell apoptosis. Mechanistic investigations demonstrated that FTO depended on its m6A RNA demethylase activity to activate PDGFRB/ERK signaling axis. Our findings indicate that FTO-mediated m6A demethylation plays an oncogenic role in NPM1-mutated AML and provide a new layer of epigenetic insight for future treatments of this distinctly leukemic entity. [ABSTRACT FROM AUTHOR]

Published

2022

15. Mutant NPM1-Regulated FTO-Mediated m 6 A Demethylation Promotes Leukemic Cell Survival via PDGFRB/ERK Signaling Axis.

Author

Xiao Q, Lei L, Ren J, Peng M, Jing Y, Jiang X, Huang J, Tao Y, Lin C, Yang J, Sun M, Tang L, Wei X, Yang Z, and Zhang L

Abstract

Acute myeloid leukemia (AML) with nucleophosmin 1 (NPM1) mutations exhibits distinct biological and clinical features, accounting for approximately one-third of AML. Recently, the N 6 -methyladenosine (m 6 A) RNA modification has emerged as a new epigenetic modification to contribute to tumorigenesis and development. However, there is limited knowledge on the role of m 6 A modifications in NPM1-mutated AML. In this study, the decreased m 6 A level was first detected and high expression of fat mass and obesity-associated protein (FTO) was responsible for the m 6 A suppression in NPM1-mutated AML. FTO upregulation was partially induced by NPM1 mutation type A (NPM1-mA) through impeding the proteasome pathway. Importantly, FTO promoted leukemic cell survival by facilitating cell cycle and inhibiting cell apoptosis. Mechanistic investigations demonstrated that FTO depended on its m 6 A RNA demethylase activity to activate PDGFRB/ERK signaling axis. Our findings indicate that FTO-mediated m 6 A demethylation plays an oncogenic role in NPM1-mutated AML and provide a new layer of epigenetic insight for future treatments of this distinctly leukemic entity., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Xiao, Lei, Ren, Peng, Jing, Jiang, Huang, Tao, Lin, Yang, Sun, Tang, Wei, Yang and Zhang.)

Published

2022