image: (From left) Dr. Wookbong Kwon of DGIST, Seong-Kyoon Choi, Director of the Center for Core Protein Resources at DGIST, Zae Young Ryoo, Professor at Kyungpook National University, and Song Park, Core Protein Resources at DGIST. In their breakthrough research, the team has identified a protein that play critical role in prostate cancer progression and might serve as a potential biomarker. view more
Credit: DGIST
Prostate cancer (PC) is one of the leading causes of global cancer-related deaths among men. While a standard systemic therapy called “androgen deprivation therapy” (ADT) is widely administered to reduce the level of androgen—the male hormone responsible for the development of PC— in the body by surgical or chemical castration, most individuals stop responding to such treatment and experience the emergence of a castration-resistant PC that rapidly progresses into a highly aggressive form with no known effective treatment protocol. A novel biomarker that can predict such a progression effectively is, therefore, highly sought after.
Against this backdrop, researchers led by Dr. Wookbong Kwon, Seong-Kyoon Choi, and Song from Daegu Gyeongbuk Institute of Science and Technology (DGIST), and Prof. Zae Young Ryoo from Kyungpook National University, Korea, addressed this issue in a study recently published in the Journal of Experimental & Clinical Cancer Research, identifying a protein called “zinc finger protein 507” (ZNF507) as the primary contributor to the progression of PC to its aggressive form.
“While working with mice deficient in producing a particular protein named ZNF507, we observed that the animals did not survive beyond the embryonic stage. Interestingly, research has indicated that this very protein also plays an active role in human cancers,” explains Dr. Kwon. “But exactly how it takes part in cancer progression remains unknown. To connect the missing link, we looked into the tissue samples of patients suffering from PC and the data from various human PC database.”
The researchers made an interesting observation. In advanced stage PC tissue, ZNF507 protein was present in a much higher amount compared to that in normal tissue. Next, by a series of cell line-based experiments, the researchers established that ZNF507 accelerated the growth, survival, proliferation, and migration of PC. Prof. Ryoo explains, “ZNF507 increased the expression of other proteins, such as TGFBR1 and MAP3K8, involved in cancer-inducing cross-talk inside the cell. In turn, it influenced the transforming growth factor-β or TGF-β signaling, a protein related to PC progression to malignancy.”
On diminishing the expression of ZNF507 in tumors developed from PC cells in mice, the weight of the tumors reduced dramatically, indicating the effect of the protein in PC.
While these findings do not have immediate practical ramifications, researchers are hopeful they will eventually lead to the development of novel drugs. “Our research findings will serve as the seeds for the development of genetic therapeutics that can specifically treat PC in the future,” concludes Dr. Kwon.
We certainly hope his vision is not too far from being realized!
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Reference
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Authors: |
Wookbong Kwon1,2, Seong-Kyoon Choi1,2*, Daehwan Kim1,2,3, Hyeon-Gyeom Kim1, Jin-Kyu Park4, Jee Eun Han4, Gil-Jae Cho4, Sungho Yun4, Wookyung Yu5, Se-Hyeon Han6,7, Yun-Sok Ha8, Jun Nyung Lee8, Tae Gyun Kwon8, Dong-Hyung Cho3,9, Jun-Koo Yi10, Myoung Ok Kim11, Zae Young Ryoo3* and Song Park1,5*
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Title of original paper: |
ZNF507 affects TGF-β signaling via TGFBR1 and MAP3K8 activation in the progression of prostate cancer to an aggressive state
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Journal: |
Journal of Experimental & Clinical Cancer Research
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DOI: |
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Affiliations: |
1Core Protein Resources Center, Republic of Korea. 2Division of Biotechnology, Republic of Korea. 3Core Protein Resources Center, Republic of Korea. 4Division of Biotechnology, Republic of Korea. 5School of Life Science, Kyungpook National University, Korea. 6College of Veterinary Medicine, Kyungpook National University, Korea. 7Department of Brain and Cognitive Sciences, Republic of Korea. 8School of Media Communication, Hanyang University, South Korea. 9Department of News-team, SBS (Seoul Broadcasting System), South Korea. 10Department of Urology, School of Medicine, Kyungpook National University, Korea. 11Brain Science and Engineering Institute, Kyungpook National University, Republic of Korea. |
*Corresponding author’s email: cskbest@dgist.ac.kr; jaewoong64@knu.ac.kr; cristaling@dgist.ac.kr
About Daegu Gyeongbuk Institute of Science and Technology (DGIST)
Daegu Gyeongbuk Institute of Science and Technology (DGIST) is a well-known and respected research institute located in Daegu, Republic of Korea. Established in 2004 by the Korean Government, the main aim of DGIST is to promote national science and technology, as well as to boost the local economy.
With a vision of “Changing the world through convergence", DGIST has undertaken a wide range of research in various fields of science and technology. DGIST has embraced a multidisciplinary approach to research and undertaken intensive studies in some of today's most vital fields. DGIST also has state-of-the-art-infrastructure to enable cutting-edge research in materials science, robotics, cognitive sciences, and communication engineering.
Website: https://www.dgist.ac.kr/en/html/sub01/010204.html
About the author
The authors are part of a joint research team of DGIST and Kyungpook National University, Korea. The researchers in the team are experts in the life sciences.
Journal
Journal of Experimental & Clinical Cancer Research
Method of Research
Experimental study
Subject of Research
People
Article Title
ZNF507 affects TGF-β signaling via TGFBR1 and MAP3K8 activation in the progression of prostate cancer to an aggressive state
Article Publication Date
18-Sep-2021