The past half a decade has witnessed a great progress in the rapidly growing field of ribosomal stress (RS)-, or nucleolar stress (NuS)-RP-MDM2-p53 field. Growing evidence has demonstrated the biological importance of the RS-RP-MDM2-p53 pathway in development of human cancer and genetic diseases, such as 5q syndrome and Diamond Blackfan anemia (DBA). Also, more ribosomal proteins and their nucleolar or nucleoplasmic regulators have been identified in modifying this pathway. The crystal structure of the RPL11-MDM2 complex was just reported, which validated our previous study on the RPL11-MDM2 complex and also offered structural information for better understanding of the underlying mechanisms. Additional studies have shown that the RS responsive p53 activation also involves inhibition of MDMX, an MDM2 analog and partner. While trying to purify our previously proposed sub-ribosome complex that regulates this MDM2-p53 pathway, we identified Spin1 (Spindlin1) and RPL22 as two new regulators of this pathway. Spin 1 is a nucleolar protein that belongs to the tudar family, acts as a histone code ?reader? to stimulate rRNA expression, and promotes genomic instability and cell transformation as a potential oncogenic protein. Interestingly, we showed that Spin1 binds to RPL5, preventing its association with MDM2 and consequently activating MDM2 and inactivating p53. Identification of RPL22 as another regulator is also remarkably significant because 1) knockout of its gene in mice is not lethal and non-essential for ribosome assembly and protein translation, and 2) it is highly mutated human cancers, such as colorectal and endometrial tumors, and/or down-regulated in lung cancer. Since RPL22 is the first RP whose mutations are highly associated with human cancer, our preliminary findings highly suggest that this ribosomal protein might be crucially important for preventing tumorigenesis via the RS- p53 pathway. More interestingly, RPL22 can bind to EBER-1, a short RNA encoded by Epstein-Bar virus (EBV) highly associated with nasopharyngeal and gastric cancers. Therefore, in light of growing evidence recently published in literature as well as our own published and preliminary studies, I hypothesize that the RS-RP- MDM2-p53 pathway is highly regulated by endogenous, such as Spin1, and exogenous, such as EBER-1, molecules, and this regulation is relevant to virus- or non-virus-pertinent cancer development. We will test this hypothesis by addressing four aims: 1) To further characterize the RS-RP-MDM2-p53 pathway biochemically; 2) To determine if dual defects of the MDM2-MDMX-p53 pathways rescues 5q-syndrome in mice; 3) To determine if Spin1 regulates the RPL5-MDM2 pathway; 4) To determine the role of RPL22 in regulation of the MDM2-p53 loop and cancer development. We will employ biochemical, biophysical, X-ray structural, molecular biological, cell biological, and genetic tools as well as recombinant proteins, cell line systems, xenograft, orthotopic tumor, and genetic mouse model systems. Completing these studies would offer new molecular insights into the RS-p53 pathway and its role in the development of genetic diseases and cancer.

Public Health Relevance

Aberrant alterations of the tumor suppressor p53-oncoprotein MDM2 pathway play a crucial role in the development of genetic diseases and cancer, but the underlying molecular mechanisms remain incompletely understood. Studies by others and us reveal that a group of ribosomal proteins can regulate this pathway and might be responsible for part of the alterations. This application is proposed to understand the role and regulation of these ribosomal proteins in the dependent development of genetic disease and cancer, and the underlying mechanisms, in hoping to ultimately identify novel molecules as anti-cancer drug targets.

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA095441-20
Application #
9842400
Study Section
Cancer Molecular Pathobiology Study Section (CAMP)
Program Officer
Watson, Joanna M
Project Start
2019-01-01
Project End
2021-12-31
Budget Start
2020-01-01
Budget End
2020-12-31
Support Year
20
Fiscal Year
2020
Total Cost
Indirect Cost
Name
Tulane University
Department
Biochemistry
Type
Schools of Medicine
DUNS #
053785812
City
New Orleans
State
LA
Country
United States
Zip Code
70118
Fang, Ziling; Cao, Bo; Liao, Jun-Ming et al. (2018) SPIN1 promotes tumorigenesis by blocking the uL18 (universal large ribosomal subunit protein 18)-MDM2-p53 pathway in human cancer. Elife 7:
Cao, Bo; Fang, Ziling; Liao, Peng et al. (2017) Cancer-mutated ribosome protein L22 (RPL22/eL22) suppresses cancer cell survival by blocking p53-MDM2 circuit. Oncotarget 8:90651-90661
Liu, Dai-Chi; Seimetz, Joseph; Lee, Kwan Young et al. (2017) Mdm2 mediates FMRP- and Gp1 mGluR-dependent protein translation and neural network activity. Hum Mol Genet 26:3895-3908
Aydin, Yucel; Chedid, Milad; Chava, Srinivas et al. (2017) Activation of PERK-Nrf2 oncogenic signaling promotes Mdm2-mediated Rb degradation in persistently infected HCV culture. Sci Rep 7:9223
Zhang, Yiwei; Zeng, Shelya X; Hao, Qian et al. (2017) Monitoring p53 by MDM2 and MDMX is required for endocrine pancreas development and function in a spatio-temporal manner. Dev Biol 423:34-45
Shao, Jia; Xu, Linlin; Chen, Limin et al. (2017) Arl13b Promotes Gastric Tumorigenesis by Regulating Smo Trafficking and Activation of the Hedgehog Signaling Pathway. Cancer Res 77:4000-4013
Zhou, Xiang; Cao, Bo; Lu, Hua (2017) Negative auto-regulators trap p53 in their web. J Mol Cell Biol 9:62-68
Liao, Peng; Zeng, Shelya X; Zhou, Xiang et al. (2017) Mutant p53 Gains Its Function via c-Myc Activation upon CDK4 Phosphorylation at Serine 249 and Consequent PIN1 Binding. Mol Cell 68:1134-1146.e6
Lu, Hua (2017) p53 and MDM2: their Yin-Yang intimacy. J Mol Cell Biol 9:1-2
Nguyen, Daniel; Liao, Wenjuan; Zeng, Shelya X et al. (2017) Reviving the guardian of the genome: Small molecule activators of p53. Pharmacol Ther 178:92-108

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