DCAF13 inhibits the p53 signaling pathway by promoting p53 ubiquitination modification in lung adenocarcinoma

Wei, Shan; Xing, Jing; Chen, Jia; Chen, Liping; Lv, Jiapei; Chen, Xiaofei; Li, Tang; Yu, Tao; Wang, Huaying; Wang, Kai; Yu, Wanjun

doi:10.1186/s13046-023-02936-2

Cited by 3 publications

(1 citation statement)

References 62 publications

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“… 21 And DCAF13 is reported to be involved in the regulation of p53-related pathways and is associated with lung cancer development. 22 In breast cancer, DCAF13 is also associated with poor prognosis. 23 However, how STAT5B and DCAF13 regulate p53/xCT ferroptosis and the impact of this mechanism on MCL still needs to be explored.…”

Section: Introductionmentioning

confidence: 99%

STAT5B Suppresses Ferroptosis by Promoting DCAF13 Transcription to Regulate p53/xCT Pathway to Promote Mantle Cell Lymphoma Progression

Zhang,

Hu,

Guo

et al. 2024

BTT

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Section: Introductionmentioning

confidence: 99%

STAT5B Suppresses Ferroptosis by Promoting DCAF13 Transcription to Regulate p53/xCT Pathway to Promote Mantle Cell Lymphoma Progression

Zhang,

Hu,

Guo

et al. 2024

BTT

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AOP report: Development of an adverse outcome pathway for deposition of energy leading to learning and memory impairment

Sleiman,

Miller,

Flores

et al. 2024

Environ and Mol Mutagen

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Understanding radiation‐induced non‐cancer effects on the central nervous system (CNS) is essential for the risk assessment of medical (e.g., radiotherapy) and occupational (e.g., nuclear workers and astronauts) exposures. Herein, the adverse outcome pathway (AOP) approach was used to consolidate relevant studies in the area of cognitive decline for identification of research gaps, countermeasure development, and for eventual use in risk assessments. AOPs are an analytical construct describing critical events to an adverse outcome (AO) in a simplified form beginning with a molecular initiating event (MIE). An AOP was constructed utilizing mechanistic information to build empirical support for the key event relationships (KERs) between the MIE of deposition of energy to the AO of learning and memory impairment through multiple key events (KEs). The evidence for the AOP was acquired through a documented scoping review of the literature. In this AOP, the MIE is connected to the AO via six KEs: increased oxidative stress, increased deoxyribonucleic acid (DNA) strand breaks, altered stress response signaling, tissue resident cell activation, increased pro‐inflammatory mediators, and abnormal neural remodeling that encompasses atypical structural and functional alterations of neural cells and surrounding environment. Deposition of energy directly leads to oxidative stress, increased DNA strand breaks, an increase of pro‐inflammatory mediators and tissue resident cell activation. These KEs, which are themselves interconnected, can lead to abnormal neural remodeling impacting learning and memory processes. Identified knowledge gaps include improving quantitative understanding of the AOP across several KERs and additional testing of proposed modulating factors through experimental work. Broadly, it is envisioned that the outcome of these efforts could be extended to other cognitive disorders and complement ongoing work by international radiation governing bodies in their review of the system of radiological protection.

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USP36 promotes colorectal cancer progression through inhibition of p53 signaling pathway via stabilizing RBM28

Xu,

Wang,

Nie

et al. 2024

Oncogene

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Colorectal cancer (CRC) stands as the second most common cause of cancer-related mortality globally and p53, a widely recognized tumor suppressor, contributes to the development of CRC. Ubiquitin-specific protease 36 (USP36), belonging to the deubiquitinating enzyme family, is involved in tumor progression across multiple cancers. However, the underlying molecular mechanism in which USP36 regulates p53 signaling pathway in CRC is unclear. Here, our study revealed that USP36 was increased in CRC tissues and associated with unfavorable prognosis. Functionally, elevated USP36 could promote proliferation, migration, and invasion of CRC cells in vitro and in vivo. Mechanistically, USP36 could interact with and stabilize RBM28 via deubiquitination at K162 residue. Further, upregulated RBM28 could bind with p53 to suppress its transcriptional activity and therefore inactivate p53 signaling pathway. Collectively, our investigation identified the novel USP36/RBM28/p53 axis and its involvement in promoting cell proliferation and metastasis in CRC, which presents a promising therapeutic strategy for CRC treatment.

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DCAF13 inhibits the p53 signaling pathway by promoting p53 ubiquitination modification in lung adenocarcinoma

Cited by 3 publications

References 62 publications

STAT5B Suppresses Ferroptosis by Promoting DCAF13 Transcription to Regulate p53/xCT Pathway to Promote Mantle Cell Lymphoma Progression

STAT5B Suppresses Ferroptosis by Promoting DCAF13 Transcription to Regulate p53/xCT Pathway to Promote Mantle Cell Lymphoma Progression

AOP report: Development of an adverse outcome pathway for deposition of energy leading to learning and memory impairment

USP36 promotes colorectal cancer progression through inhibition of p53 signaling pathway via stabilizing RBM28

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