徐祥祐

Hi, I’m Frank Hsu. I graduated from NYCU with a bachelor degree in Molecular Medicine and Bioengineering, and continue to pursue my doctoral degree in same field. My main research interest is the pathogenic mechanisms of cancer. I am currently studying the effects of DEAD-box helicase 3 X-linked (DDX3X) on metabolic reprogramming in Hepatocellular carcinoma (HCC). Hoping my research could provide novel therapeutic strategy for patients suffering from cancer.

Sumoylation Participates in the Regulation of YB-1-mediated Mismatch Repair Deficiency and Alkylator Tolerance

Hsiang-Yu Hsu (徐祥祐)1,2, Yu-Chin Kao2,3, Yi Cheng1,2, and Ru-Tsun Mai2,3

1Institute of Molecular Medicine and Bioengineering, College of Biological Science and Technology, National Yang Ming Chiao Tung University

2Center for Intelligent Drug Systems and Smart Bio-devices (IDS2B), National Yang Ming Chiao Tung University

3Department of Biological Science and Technology, College of Biological Science and Technology, National Yang Ming Chiao Tung University

Numerous reports indicate that enhanced expression of Y-box binding protein-1 (YB-1) in tumor cells is strongly associated with tumorigenesis, aggressiveness, drug resistance, as well as poor prognosis in several types of cancers, and YB-1 is considered to be an oncogene. The molecular mechanism contributing to the regulation of the biological activities of YB-1 remains obscure. Sumoylation, a post-translational modification involving the covalent conjugation of small ubiquitin-like modifier (SUMO) proteins to a target protein, plays key roles in the modulation of protein functions. In this study, our results revealed that YB-1 is sumoylated and that Lys26 is a critical residue for YB-1 sumoylation. Moreover, YB-1 was found to directly interact with SUMO proteins, and disruption of the SUMO-interacting motif (SIM) of YB-1 not only interfered with this interaction but also diminished YB-1 sumoylation. The subcellular localization, protein stability, and transcriptional regulatory activity of YB-1 were not significantly affected by sumoylation. However, decreased sumoylation disrupted the interaction between YB-1 and PCNA as well as YB-1-mediated inhibition of the MutSα/PCNA interaction and MutSα mismatch binding activity, indicating a functional role of YB-1 sumoylation in inducing DNA mismatch repair (MMR) deficiency and spontaneous mutations. The MMR machinery also recognizes alkylator-modified DNA adducts to signal for cell death. We further demonstrated that YB-1 sumoylation is crucial for the inhibition of SN1-type alkylator MNNG-induced cytotoxicity, G2/M-phase arrest, apoptosis, and the MMR-dependent DNA damage response. Collectively, these results provide molecular explanations for the impact of YB-1 sumoylation on MMR deficiency and alkylator tolerance, which may provide insight for designing therapeutic strategies for malignancies and alkylator-resistant cancers associated with YB-1 overexpression.

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