Camptothecin induces mitotic arrest through Mad2-Cdc20 complex by activating the JNK-mediated Sp1 pathway

Matharage Gayani Dilshara; Rajapaksha Gedara Prasad Tharanga Jayasooriya; Wisurumuni Arachchilage Hasitha Maduranga Karunarathne; Yung Hyun Choi; Gi-Young Kim

doi:10.1016/j.fct.2019.03.026

Camptothecin induces mitotic arrest through Mad2-Cdc20 complex by activating the JNK-mediated Sp1 pathway

Food Chem Toxicol. 2019 May:127:143-155. doi: 10.1016/j.fct.2019.03.026. Epub 2019 Mar 15.

Authors

Matharage Gayani Dilshara¹, Rajapaksha Gedara Prasad Tharanga Jayasooriya², Wisurumuni Arachchilage Hasitha Maduranga Karunarathne¹, Yung Hyun Choi³, Gi-Young Kim⁴

Affiliations

¹ Department of Marine Life Science, Jeju National University, Jeju, 63243, Republic of Korea.
² Department of Bioprocess Technology, Faculty of Technology, Rajarata University of Sri Lanka, Mihintale, 50300, Sri Lanka.
³ Department of Biochemistry, College of Oriental Medicine, Dong-Eui University, Busan, 47227, Republic of Korea.
⁴ Department of Marine Life Science, Jeju National University, Jeju, 63243, Republic of Korea. Electronic address: immunkim@jejunu.ac.kr.

PMID: 30885713
DOI: 10.1016/j.fct.2019.03.026

Abstract

Camptothecin (CPT) is a popular therapeutic agent that targets topoisomerase I. Our findings demonstrated that CPT-induced microtubule polymerization results in markedly increased histone H3 phosphorylation. CPT also enhanced interactions between the mitotic checkpoint proteins, Mad2 and Cdc20, and thereby increased mitotic arrest. Transient knockdown of Mad2 completely restored cell cycle progression from CPT-induced mitotic arrest, while simultaneously reduced cyclin B1 and Cdk1 expression. Moreover, we found that c-Jun N-terminal kinase (JNK) acts upstream of Sp1, which upregulates p21-mediated mitotic arrest in response to CPT; furthermore, knockdown of p21 restored cell cycle progression, while inhibition of Cdks completely restored cell cycle progression from CPT-induced mitotic arrest. We hypothesized that, during mitotic arrest in response to CPT, cell survival signaling blocks apoptosis, thereby enhancing mitotic arrest. As expected, a caspase-9 inhibitor, z-LEHD-FMK, and an autophagy inhibitor, 3-methyladenine (3 MA), significantly diminished CPT-induced mitotic arrest. On the other hand, when Mad2 was depleted, z-LEHD-FMK and 3 MA markedly increased apoptosis, and restored cell cycle progression. Taken together, these results suggest that CPT decodes the action of topoisomerase I-mediated tubulin targeting drugs, leading to mitotic arrest by upregulating Mad2 through the JNK-mediated Sp1 pathway and autophagy formation from tubulin polymerization.

Keywords: Camptothecin; Mad2; Mitotic arrest; Topoisomerase I; Tubulin.

MeSH terms

Autophagy
CDC2 Protein Kinase / metabolism
Camptothecin / pharmacology*
Cdc20 Proteins / metabolism*
Cell Line, Tumor
Cyclin B1 / metabolism
Humans
MAP Kinase Signaling System*
Mad2 Proteins / metabolism*
Mitosis / drug effects*
Phosphorylation
Polymerization
Sp1 Transcription Factor / metabolism*
Tubulin / metabolism
Up-Regulation / drug effects

Substances

CCNB1 protein, human
Cdc20 Proteins
Cyclin B1
MAD2L1 protein, human
Mad2 Proteins
Sp1 Transcription Factor
SP1 protein, human
Tubulin
CDC20 protein, human
CDC2 Protein Kinase
CDK1 protein, human
Camptothecin