Future aspects of CDK5 in prostate cancer: From pathogenesis to therapeutic implications

Muhammet Oner; Eugene Lin; Mei Chih Chen; Fu Ning Hsu; G. M. Shazzad Hossain Prince; Kun Yuan Chiu; Chieh Lin Jerry Teng; Tsung Ying Yang; Hsin Yi Wang; Chia Herng Yue; Ching Han Yu; Chih Ho Lai; Jer Tsong Hsieh; Ho Lin

doi:10.3390/ijms20163881

Future aspects of CDK5 in prostate cancer: From pathogenesis to therapeutic implications

Muhammet Oner, Eugene Lin, Mei Chih Chen, Fu Ning Hsu, G. M. Shazzad Hossain Prince, Kun Yuan Chiu, Chieh Lin Jerry Teng, Tsung Ying Yang, Hsin Yi Wang, Chia Herng Yue, Ching Han Yu, Chih Ho Lai, Jer Tsong Hsieh, Ho Lin

Research output: Contribution to journal › Review article › peer-review

18 Scopus citations

Abstract

Cyclin-dependent kinase 5 (CDK5) is a unique member of the cyclin-dependent kinase family. CDK5 is activated by binding with its regulatory proteins, mainly p35, and its activation is essential in the development of the central nervous system (CNS) and neurodegeneration. Recently, it has been reported that CDK5 plays important roles in regulating various biological and pathological processes, including cancer progression. Concerning prostate cancer, the androgen receptor (AR) is majorly involved in tumorigenesis, while CDK5 can phosphorylate AR and promotes the proliferation of prostate cancer cells. Clinical evidence has also shown that the level of CDK5 is associated with the progression of prostate cancer. Interestingly, inhibition of CDK5 prevents prostate cancer cell growth, while drug-triggered CDK5 hyperactivation leads to apoptosis. The blocking of CDK5 activity by its small interfering RNAs (siRNA) or Roscovitine, a pan-CDK inhibitor, reduces the cellular AR protein level and triggers the death of prostate cancer cells. Thus, CDK5 plays a crucial role in the growth of prostate cancer cells, and AR regulation is one of the important pathways. In this review paper, we summarize the significant studies on CDK5-mediated regulation of prostate cancer cells. We propose that the CDK5–p35 complex might be an outstanding candidate as a diagnostic marker and potential target for prostate cancer treatment in the near future.

Original language	English (US)
Article number	3881
Journal	International journal of molecular sciences
Volume	20
Issue number	16
DOIs	https://doi.org/10.3390/ijms20163881
State	Published - Aug 2 2019

Keywords

Androgen receptor (AR)
Cyclin-dependent kinase 5 (CDK5)
P35
Prostate cancer

ASJC Scopus subject areas

Catalysis
Molecular Biology
Spectroscopy
Computer Science Applications
Physical and Theoretical Chemistry
Organic Chemistry
Inorganic Chemistry

Access to Document

10.3390/ijms20163881

Cite this

Oner, M., Lin, E., Chen, M. C., Hsu, F. N., Shazzad Hossain Prince, G. M., Chiu, K. Y., Teng, C. L. J., Yang, T. Y., Wang, H. Y., Yue, C. H., Yu, C. H., Lai, C. H., Hsieh, J. T., & Lin, H. (2019). Future aspects of CDK5 in prostate cancer: From pathogenesis to therapeutic implications. International journal of molecular sciences, 20(16), Article 3881. https://doi.org/10.3390/ijms20163881

@article{6ca1438df087472ebc1a4d5874a8ace1,

title = "Future aspects of CDK5 in prostate cancer: From pathogenesis to therapeutic implications",

abstract = "Cyclin-dependent kinase 5 (CDK5) is a unique member of the cyclin-dependent kinase family. CDK5 is activated by binding with its regulatory proteins, mainly p35, and its activation is essential in the development of the central nervous system (CNS) and neurodegeneration. Recently, it has been reported that CDK5 plays important roles in regulating various biological and pathological processes, including cancer progression. Concerning prostate cancer, the androgen receptor (AR) is majorly involved in tumorigenesis, while CDK5 can phosphorylate AR and promotes the proliferation of prostate cancer cells. Clinical evidence has also shown that the level of CDK5 is associated with the progression of prostate cancer. Interestingly, inhibition of CDK5 prevents prostate cancer cell growth, while drug-triggered CDK5 hyperactivation leads to apoptosis. The blocking of CDK5 activity by its small interfering RNAs (siRNA) or Roscovitine, a pan-CDK inhibitor, reduces the cellular AR protein level and triggers the death of prostate cancer cells. Thus, CDK5 plays a crucial role in the growth of prostate cancer cells, and AR regulation is one of the important pathways. In this review paper, we summarize the significant studies on CDK5-mediated regulation of prostate cancer cells. We propose that the CDK5–p35 complex might be an outstanding candidate as a diagnostic marker and potential target for prostate cancer treatment in the near future.",

keywords = "Androgen receptor (AR), Cyclin-dependent kinase 5 (CDK5), P35, Prostate cancer",

author = "Muhammet Oner and Eugene Lin and Chen, {Mei Chih} and Hsu, {Fu Ning} and {Shazzad Hossain Prince}, {G. M.} and Chiu, {Kun Yuan} and Teng, {Chieh Lin Jerry} and Yang, {Tsung Ying} and Wang, {Hsin Yi} and Yue, {Chia Herng} and Yu, {Ching Han} and Lai, {Chih Ho} and Hsieh, {Jer Tsong} and Ho Lin",

note = "Funding Information: Funding: This study was supported by the Ministry of Science and Technology, Taiwan (106-2320-B-005-002-MY3/108-2911-I-005-509 to H.L.), the grant of NCHU ENABLE Center (108-16 to H.L.), Taichung Veterans General Hospital/National Chung Hsing University Joint Research Program (TCVGH-NCHU-1097615 to H.L.), Tung{\textquoteright}s Taichung Metro Harbor Hospital (TTMHH-NCHULS107004 to H.L.), and National Chung Hsing University/Chung Shan Medical University Joint Research Program (NCHU-CSMU-10710). Funding Information: This study was supported by the Ministry of Science and Technology, Taiwan (106-2320-B-005-002-MY3/108-2911-I-005-509 to H.L.), the grant of NCHU ENABLE Center (108-16 to H.L.), Taichung Veterans General Hospital/National Chung Hsing University Joint Research Program (TCVGH-NCHU-1097615 to H.L.), Tung?s Taichung Metro Harbor Hospital (TTMHH-NCHULS107004 to H.L.), and National Chung Hsing University/Chung Shan Medical University Joint Research Program (NCHU-CSMU-10710). Funding Information: Funding: This study was supported by the Ministry of Science and Technology, Taiwan (106-2320-B-005-002-MY3/108-2911-I-005-509 to H.L.), the grant of NCHU ENABLE Center (108-16 to H.L.), Taichung Veterans General Hospital/National Chung Hsing University Joint Research Program (TCVGH-NCHU-1097615 to H.L.), Publisher Copyright: {\textcopyright} 2019 by the authors. Licensee MDPI, Basel, Switzerland.",

year = "2019",

month = aug,

day = "2",

doi = "10.3390/ijms20163881",

language = "English (US)",

volume = "20",

journal = "International journal of molecular sciences",

issn = "1661-6596",

publisher = "Multidisciplinary Digital Publishing Institute (MDPI)",

number = "16",

}

TY - JOUR

T1 - Future aspects of CDK5 in prostate cancer

T2 - From pathogenesis to therapeutic implications

AU - Oner, Muhammet

AU - Lin, Eugene

AU - Chen, Mei Chih

AU - Hsu, Fu Ning

AU - Shazzad Hossain Prince, G. M.

AU - Chiu, Kun Yuan

AU - Teng, Chieh Lin Jerry

AU - Yang, Tsung Ying

AU - Wang, Hsin Yi

AU - Yue, Chia Herng

AU - Yu, Ching Han

AU - Lai, Chih Ho

AU - Hsieh, Jer Tsong

AU - Lin, Ho

N1 - Funding Information: Funding: This study was supported by the Ministry of Science and Technology, Taiwan (106-2320-B-005-002-MY3/108-2911-I-005-509 to H.L.), the grant of NCHU ENABLE Center (108-16 to H.L.), Taichung Veterans General Hospital/National Chung Hsing University Joint Research Program (TCVGH-NCHU-1097615 to H.L.), Tung’s Taichung Metro Harbor Hospital (TTMHH-NCHULS107004 to H.L.), and National Chung Hsing University/Chung Shan Medical University Joint Research Program (NCHU-CSMU-10710). Funding Information: This study was supported by the Ministry of Science and Technology, Taiwan (106-2320-B-005-002-MY3/108-2911-I-005-509 to H.L.), the grant of NCHU ENABLE Center (108-16 to H.L.), Taichung Veterans General Hospital/National Chung Hsing University Joint Research Program (TCVGH-NCHU-1097615 to H.L.), Tung?s Taichung Metro Harbor Hospital (TTMHH-NCHULS107004 to H.L.), and National Chung Hsing University/Chung Shan Medical University Joint Research Program (NCHU-CSMU-10710). Funding Information: Funding: This study was supported by the Ministry of Science and Technology, Taiwan (106-2320-B-005-002-MY3/108-2911-I-005-509 to H.L.), the grant of NCHU ENABLE Center (108-16 to H.L.), Taichung Veterans General Hospital/National Chung Hsing University Joint Research Program (TCVGH-NCHU-1097615 to H.L.), Publisher Copyright: © 2019 by the authors. Licensee MDPI, Basel, Switzerland.

PY - 2019/8/2

Y1 - 2019/8/2

N2 - Cyclin-dependent kinase 5 (CDK5) is a unique member of the cyclin-dependent kinase family. CDK5 is activated by binding with its regulatory proteins, mainly p35, and its activation is essential in the development of the central nervous system (CNS) and neurodegeneration. Recently, it has been reported that CDK5 plays important roles in regulating various biological and pathological processes, including cancer progression. Concerning prostate cancer, the androgen receptor (AR) is majorly involved in tumorigenesis, while CDK5 can phosphorylate AR and promotes the proliferation of prostate cancer cells. Clinical evidence has also shown that the level of CDK5 is associated with the progression of prostate cancer. Interestingly, inhibition of CDK5 prevents prostate cancer cell growth, while drug-triggered CDK5 hyperactivation leads to apoptosis. The blocking of CDK5 activity by its small interfering RNAs (siRNA) or Roscovitine, a pan-CDK inhibitor, reduces the cellular AR protein level and triggers the death of prostate cancer cells. Thus, CDK5 plays a crucial role in the growth of prostate cancer cells, and AR regulation is one of the important pathways. In this review paper, we summarize the significant studies on CDK5-mediated regulation of prostate cancer cells. We propose that the CDK5–p35 complex might be an outstanding candidate as a diagnostic marker and potential target for prostate cancer treatment in the near future.

AB - Cyclin-dependent kinase 5 (CDK5) is a unique member of the cyclin-dependent kinase family. CDK5 is activated by binding with its regulatory proteins, mainly p35, and its activation is essential in the development of the central nervous system (CNS) and neurodegeneration. Recently, it has been reported that CDK5 plays important roles in regulating various biological and pathological processes, including cancer progression. Concerning prostate cancer, the androgen receptor (AR) is majorly involved in tumorigenesis, while CDK5 can phosphorylate AR and promotes the proliferation of prostate cancer cells. Clinical evidence has also shown that the level of CDK5 is associated with the progression of prostate cancer. Interestingly, inhibition of CDK5 prevents prostate cancer cell growth, while drug-triggered CDK5 hyperactivation leads to apoptosis. The blocking of CDK5 activity by its small interfering RNAs (siRNA) or Roscovitine, a pan-CDK inhibitor, reduces the cellular AR protein level and triggers the death of prostate cancer cells. Thus, CDK5 plays a crucial role in the growth of prostate cancer cells, and AR regulation is one of the important pathways. In this review paper, we summarize the significant studies on CDK5-mediated regulation of prostate cancer cells. We propose that the CDK5–p35 complex might be an outstanding candidate as a diagnostic marker and potential target for prostate cancer treatment in the near future.

KW - Androgen receptor (AR)

KW - Cyclin-dependent kinase 5 (CDK5)

KW - P35

KW - Prostate cancer

UR - http://www.scopus.com/inward/record.url?scp=85071280898&partnerID=8YFLogxK

UR - http://www.scopus.com/inward/citedby.url?scp=85071280898&partnerID=8YFLogxK

U2 - 10.3390/ijms20163881

DO - 10.3390/ijms20163881

M3 - Review article

C2 - 31395805

AN - SCOPUS:85071280898

SN - 1661-6596

VL - 20

JO - International journal of molecular sciences

JF - International journal of molecular sciences

IS - 16

M1 - 3881

ER -

Future aspects of CDK5 in prostate cancer: From pathogenesis to therapeutic implications

Abstract

Keywords

ASJC Scopus subject areas

Access to Document

Other files and links

Fingerprint

Cite this