Activation of PERK Contributes to Apoptosis and G<sub>2</sub>/M Arrest by Microtubule Disruptors in Human Colorectal Carcinoma Cells

Activation of PERK Contributes to Apoptosis and G<sub>2</sub>/M Arrest by Microtubule Disruptors in Human Colorectal Carcinoma Cells

Microtubule-targeting agents (MTAs) are widely used in cancer chemotherapy, but the therapeutic responses significantly vary among different tumor types. Protein kinase RNA-like endoplasmic reticular (ER) kinase (PERK) is an ER stress kinase, and the role of PERK in the anticancer effects of MTAs is...

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Main Authors: Ming-Shun Wu, Chih-Chiang Chien, Ganbolor Jargalsaikhan, Noor Andryan Ilsan, Yen-Chou Chen
Format: Article
Language:English
Published: MDPI AG 2019-12-01
Series:Cancers
Subjects:
protein kinase rna-like endoplasmic reticular kinase
microtubule disrupters
taxol
nocodazole
human colon carcinoma cells
Online Access:https://www.mdpi.com/2072-6694/12/1/97
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spelling doaj-26bdf40e1c1941c4bcc12f80505d00512020-11-25T02:19:36ZengMDPI AGCancers2072-66942019-12-011219710.3390/cancers12010097cancers12010097Activation of PERK Contributes to Apoptosis and G<sub>2</sub>/M Arrest by Microtubule Disruptors in Human Colorectal Carcinoma CellsMing-Shun Wu0Chih-Chiang Chien1Ganbolor Jargalsaikhan2Noor Andryan Ilsan3Yen-Chou Chen4Division of Gastroenterology, Department of Internal Medicine, Wan Fang Hospital, Taipei Medical University, Taipei 11031, TaiwanDepartment of Nephrology, Chi-Mei Medical Center, Tainan City 710, TaiwanInternational MS/PhD Program in Medicine, College of Medicine, Taipei Medical University, Taipei 11031, TaiwanInternational MS/PhD Program in Medicine, College of Medicine, Taipei Medical University, Taipei 11031, TaiwanInternational MS/PhD Program in Medicine, College of Medicine, Taipei Medical University, Taipei 11031, TaiwanMicrotubule-targeting agents (MTAs) are widely used in cancer chemotherapy, but the therapeutic responses significantly vary among different tumor types. Protein kinase RNA-like endoplasmic reticular (ER) kinase (PERK) is an ER stress kinase, and the role of PERK in the anticancer effects of MTAs is still undefined. In the present study, taxol (TAX) and nocodazole (NOC) significantly induced apoptosis with increased expression of phosphorylated PERK (pPERK; Tyr980) in four human colon cancer cell lines, including HCT-15, COLO205, HT-20, and LOVO cells. Induction of G<sub>2</sub>/M arrest by TAX and NOC with increases in phosphorylated Cdc25C and cyclin B1 protein were observed in human colon cancer cells. Application of the c-Jun N-terminal kinase (JNK) inhibitors SP600125 (SP) and JNK inhibitor V (JNKI) significantly reduced TAX- and NOC-induced apoptosis and G<sub>2</sub>/M arrest of human colon cancer cells. Interestingly, TAX- and NOC-induced pPERK (Tyr980) protein expression was inhibited by adding the JNK inhibitors, SP and JNKI, and application of the PERK inhibitor GSK2606414 (GSK) significantly reduced apoptosis and G<sub>2</sub>/M arrest by TAX and NOC, with decreased pPERK (Tyr980) and pJNK, phosphorylated Cdc25C, and Cyc B1 protein expressions in human colon cancer cells. Decreased viability by TAX and NOC was inhibited by knockdown of PERK using PERK siRNA in COLO205 and HCT-15 cells. Disruption of the mitochondrial membrane potential and an increase in B-cell lymphoma-2 (Bcl-2) protein phosphorylation (pBcl-2; Ser70) by TAX and NOC were prevented by adding the PERK inhibitor GSK and JNK inhibitor SP and JNKI. A cross-activation of JNK and PERK by TAX and NOC leading to anti-CRC actions including apoptosis and G<sub>2</sub>/M arrest was first demonstrated herein.https://www.mdpi.com/2072-6694/12/1/97protein kinase rna-like endoplasmic reticular kinasemicrotubule disrupterstaxolnocodazolehuman colon carcinoma cells
collection DOAJ
language English
format Article
sources DOAJ
author Ming-Shun Wu
Chih-Chiang Chien
Ganbolor Jargalsaikhan
Noor Andryan Ilsan
Yen-Chou Chen
spellingShingle Ming-Shun Wu
Chih-Chiang Chien
Ganbolor Jargalsaikhan
Noor Andryan Ilsan
Yen-Chou Chen
Activation of PERK Contributes to Apoptosis and G<sub>2</sub>/M Arrest by Microtubule Disruptors in Human Colorectal Carcinoma Cells
Cancers
protein kinase rna-like endoplasmic reticular kinase
microtubule disrupters
taxol
nocodazole
human colon carcinoma cells
author_facet Ming-Shun Wu
Chih-Chiang Chien
Ganbolor Jargalsaikhan
Noor Andryan Ilsan
Yen-Chou Chen
author_sort Ming-Shun Wu
title Activation of PERK Contributes to Apoptosis and G<sub>2</sub>/M Arrest by Microtubule Disruptors in Human Colorectal Carcinoma Cells
title_short Activation of PERK Contributes to Apoptosis and G<sub>2</sub>/M Arrest by Microtubule Disruptors in Human Colorectal Carcinoma Cells
title_full Activation of PERK Contributes to Apoptosis and G<sub>2</sub>/M Arrest by Microtubule Disruptors in Human Colorectal Carcinoma Cells
title_fullStr Activation of PERK Contributes to Apoptosis and G<sub>2</sub>/M Arrest by Microtubule Disruptors in Human Colorectal Carcinoma Cells
title_full_unstemmed Activation of PERK Contributes to Apoptosis and G<sub>2</sub>/M Arrest by Microtubule Disruptors in Human Colorectal Carcinoma Cells
title_sort activation of perk contributes to apoptosis and g<sub>2</sub>/m arrest by microtubule disruptors in human colorectal carcinoma cells
publisher MDPI AG
series Cancers
issn 2072-6694
publishDate 2019-12-01
description Microtubule-targeting agents (MTAs) are widely used in cancer chemotherapy, but the therapeutic responses significantly vary among different tumor types. Protein kinase RNA-like endoplasmic reticular (ER) kinase (PERK) is an ER stress kinase, and the role of PERK in the anticancer effects of MTAs is still undefined. In the present study, taxol (TAX) and nocodazole (NOC) significantly induced apoptosis with increased expression of phosphorylated PERK (pPERK; Tyr980) in four human colon cancer cell lines, including HCT-15, COLO205, HT-20, and LOVO cells. Induction of G<sub>2</sub>/M arrest by TAX and NOC with increases in phosphorylated Cdc25C and cyclin B1 protein were observed in human colon cancer cells. Application of the c-Jun N-terminal kinase (JNK) inhibitors SP600125 (SP) and JNK inhibitor V (JNKI) significantly reduced TAX- and NOC-induced apoptosis and G<sub>2</sub>/M arrest of human colon cancer cells. Interestingly, TAX- and NOC-induced pPERK (Tyr980) protein expression was inhibited by adding the JNK inhibitors, SP and JNKI, and application of the PERK inhibitor GSK2606414 (GSK) significantly reduced apoptosis and G<sub>2</sub>/M arrest by TAX and NOC, with decreased pPERK (Tyr980) and pJNK, phosphorylated Cdc25C, and Cyc B1 protein expressions in human colon cancer cells. Decreased viability by TAX and NOC was inhibited by knockdown of PERK using PERK siRNA in COLO205 and HCT-15 cells. Disruption of the mitochondrial membrane potential and an increase in B-cell lymphoma-2 (Bcl-2) protein phosphorylation (pBcl-2; Ser70) by TAX and NOC were prevented by adding the PERK inhibitor GSK and JNK inhibitor SP and JNKI. A cross-activation of JNK and PERK by TAX and NOC leading to anti-CRC actions including apoptosis and G<sub>2</sub>/M arrest was first demonstrated herein.
topic protein kinase rna-like endoplasmic reticular kinase
microtubule disrupters
taxol
nocodazole
human colon carcinoma cells
url https://www.mdpi.com/2072-6694/12/1/97
work_keys_str_mv AT mingshunwu activationofperkcontributestoapoptosisandgsub2submarrestbymicrotubuledisruptorsinhumancolorectalcarcinomacells
AT chihchiangchien activationofperkcontributestoapoptosisandgsub2submarrestbymicrotubuledisruptorsinhumancolorectalcarcinomacells
AT ganbolorjargalsaikhan activationofperkcontributestoapoptosisandgsub2submarrestbymicrotubuledisruptorsinhumancolorectalcarcinomacells
AT noorandryanilsan activationofperkcontributestoapoptosisandgsub2submarrestbymicrotubuledisruptorsinhumancolorectalcarcinomacells
AT yenchouchen activationofperkcontributestoapoptosisandgsub2submarrestbymicrotubuledisruptorsinhumancolorectalcarcinomacells
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