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Status | 已發表Published |
A robust luminescent assay for screening alkyladenine DNA glycosylase inhibitors to overcome DNA repair and temozolomide drug resistance | |
Song,Ying Qi1; Li,Guo Dong1; Niu,Dou1; Chen,Feng1; Jing,Shaozhen3; Wai Wong,Vincent Kam4; Wang,Wanhe3; Leung,Chung Hang1,2 | |
2023-04-19 | |
Source Publication | Journal of Pharmaceutical Analysis |
ISSN | 2095-1779 |
Volume | 13Issue:5Pages:514-522 |
Abstract | Temozolomide (TMZ) is an anticancer agent used to treat glioblastoma, typically following radiation therapy and/or surgical resection. However, despite its effectiveness, at least 50% of patients do not respond to TMZ, which is associated with repair and/or tolerance of TMZ-induced DNA lesions. Studies have demonstrated that alkyladenine DNA glycosylase (AAG), an enzyme that triggers the base excision repair (BER) pathway by excising TMZ-induced N3-methyladenine (3meA) and N7-methylguanine lesions, is overexpressed in glioblastoma tissues compared to normal tissues. Therefore, it is essential to develop a rapid and efficient screening method for AAG inhibitors to overcome TMZ resistance in glioblastomas. Herein, we report a robust time-resolved photoluminescence platform for identifying AAG inhibitors with improved sensitivity compared to conventional steady-state spectroscopic methods. As a proof-of-concept, this assay was used to screen 1440 food and drug administration-approved drugs against AAG, resulting in the repurposing of sunitinib as a potential AAG inhibitor. Sunitinib restored glioblastoma (GBM) cancer cell sensitivity to TMZ, inhibited GBM cell proliferation and stem cell characteristics, and induced GBM cell cycle arrest. Overall, this strategy offers a new method for the rapid identification of small-molecule inhibitors of BER enzyme activities that can prevent false negatives due to a fluorescent background. |
Keyword | Alkyladenine Dna Glycosylase Drug Screening Glioblastoma N3-methyladenine Sunitinib Temozolomide |
DOI | 10.1016/j.jpha.2023.04.010 |
URL | View the original |
Indexed By | SCIE |
Language | 英語English |
WOS Research Area | Pharmacology & Pharmacy |
WOS Subject | Pharmacology & Pharmacy |
WOS ID | WOS:001017230700001 |
Publisher | ELSEVIER, RADARWEG 29, 1043 NX AMSTERDAM, NETHERLANDS |
Scopus ID | 2-s2.0-85158889733 |
Fulltext Access | |
Citation statistics | |
Document Type | Journal article |
Collection | DEPARTMENT OF BIOMEDICAL SCIENCES Institute of Chinese Medical Sciences THE STATE KEY LABORATORY OF QUALITY RESEARCH IN CHINESE MEDICINE (UNIVERSITY OF MACAU) |
Corresponding Author | Wang,Wanhe; Leung,Chung Hang |
Affiliation | 1.State Key Laboratory of Quality Research in Chinese Medicine,Institute of Chinese Medical Sciences,University of Macau,999078,Macao 2.Department of Biomedical Sciences,Faculty of Health Sciences,University of Macau,999078,Macao 3.Institute of Medical Research,Northwestern Polytechnical University,Xi'an,710072,China 4.Dr. Neher's Biophysics Laboratory for Innovative Drug Discovery,State Key Laboratory of Quality Research in Chinese Medicine,Macau University of Science and Technology,999078,Macao |
First Author Affilication | Institute of Chinese Medical Sciences |
Corresponding Author Affilication | Institute of Chinese Medical Sciences; Faculty of Health Sciences |
Recommended Citation GB/T 7714 | Song,Ying Qi,Li,Guo Dong,Niu,Dou,et al. A robust luminescent assay for screening alkyladenine DNA glycosylase inhibitors to overcome DNA repair and temozolomide drug resistance[J]. Journal of Pharmaceutical Analysis, 2023, 13(5), 514-522. |
APA | Song,Ying Qi., Li,Guo Dong., Niu,Dou., Chen,Feng., Jing,Shaozhen., Wai Wong,Vincent Kam., Wang,Wanhe., & Leung,Chung Hang (2023). A robust luminescent assay for screening alkyladenine DNA glycosylase inhibitors to overcome DNA repair and temozolomide drug resistance. Journal of Pharmaceutical Analysis, 13(5), 514-522. |
MLA | Song,Ying Qi,et al."A robust luminescent assay for screening alkyladenine DNA glycosylase inhibitors to overcome DNA repair and temozolomide drug resistance".Journal of Pharmaceutical Analysis 13.5(2023):514-522. |
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