Cell Cycle Arrest and Cytotoxic Effects of SAHA and RG7388 Mediated through p21<sup>WAF1/CIP1</sup> and p27<sup>KIP1</sup> in Cancer Cells

Cell Cycle Arrest and Cytotoxic Effects of SAHA and RG7388 Mediated through p21<sup>WAF1/CIP1</sup> and p27<sup>KIP1</sup> in Cancer Cells

<i>Background and Objective</i>: Alterations in gene expressions are often due to epigenetic modifications that can have a significant influence on cancer development, growth, and progression. Lately, histone deacetylase inhibitors (HDACi) such as suberoylanilide hydroxamic acid (SAHA, o...

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Main Authors: Umamaheswari Natarajan, Thiagarajan Venkatesan, Vijayaraghavan Radhakrishnan, Shila Samuel, Periannan Rasappan, Appu Rathinavelu
Format: Article
Language:English
Published: MDPI AG 2019-01-01
Series:Medicina
Subjects:
SAHA
RG7388
MDM2
p53
p21
cell cycle arrest
cell death
Online Access:https://www.mdpi.com/1010-660X/55/2/30
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spelling doaj-4e4c55f08dc845328efa2a964e036fa02020-11-24T21:36:16ZengMDPI AGMedicina1010-660X2019-01-015523010.3390/medicina55020030medicina55020030Cell Cycle Arrest and Cytotoxic Effects of SAHA and RG7388 Mediated through p21<sup>WAF1/CIP1</sup> and p27<sup>KIP1</sup> in Cancer CellsUmamaheswari Natarajan0Thiagarajan Venkatesan1Vijayaraghavan Radhakrishnan2Shila Samuel3Periannan Rasappan4Appu Rathinavelu5Rumbaugh-Goodwin Institute for Cancer Research, Nova Southeastern University, Fort Lauderdale, FL 33314, USARumbaugh-Goodwin Institute for Cancer Research, Nova Southeastern University, Fort Lauderdale, FL 33314, USAVRR Institute of Biomedical Science, Kattupakkam, Chennai 600056, IndiaVRR Institute of Biomedical Science, Kattupakkam, Chennai 600056, IndiaVRR Institute of Biomedical Science, Kattupakkam, Chennai 600056, IndiaRumbaugh-Goodwin Institute for Cancer Research, Nova Southeastern University, Fort Lauderdale, FL 33314, USA<i>Background and Objective</i>: Alterations in gene expressions are often due to epigenetic modifications that can have a significant influence on cancer development, growth, and progression. Lately, histone deacetylase inhibitors (HDACi) such as suberoylanilide hydroxamic acid (SAHA, or vorinostat, MK0683) have been emerging as a new class of drugs with promising therapeutic benefits in controlling cancer growth and metastasis. The small molecule RG7388 (idasanutlin, R05503781) is a newly developed inhibitor that is specific for an oncogene-derived protein called MDM2, which is also in clinical trials for the treatment of various types of cancers. These two drugs have shown the ability to induce p21 expression through distinct mechanisms in MCF-7 and LNCaP cells, which are reported to have wild-type TP53. Our understanding of the molecular mechanism whereby SAHA and RG7388 can induce cell cycle arrest and trigger cell death is still evolving. In this study, we performed experiments to measure the cell cycle arrest effects of SAHA and RG7388 using MCF-7 and LNCaP cells. <i>Materials and Methods</i>: The cytotoxicity, cell cycle arrest, and apoptosis/necroptosis effects of the SAHA and RG7388 treatments were assessed using the Trypan Blue dye exclusion (TBDE) method, 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) assay, fluorescence assay with DEVD-<i>amc</i> substrate, and immunoblotting methods. <i>Results:</i> The RG7388 treatment was able to induce cell death by elevating p21<sup>WAF1/CIP1</sup> through inhibition of MDM2 in LNCaP, but not in MCF-7 cells, even though there was evidence of p53 elevation. Hence, we suspect that there is some level of uncoupling of p53-mediated transcriptional induction of p21<sup>WAF1/CIP1</sup> in MCF-7 cells. <i>Conclusion</i>: Our results from MCF-7 and LNCaP cells confirmed that SAHA and RG7388 treatments were able to induce cell death via a combination of cell cycle arrest and cytotoxic mechanisms. We speculate that our findings could lead to the development of newer treatments for breast and prostate cancers with drug combinations including HDACi.https://www.mdpi.com/1010-660X/55/2/30SAHARG7388MDM2p53p21cell cycle arrestcell death
collection DOAJ
language English
format Article
sources DOAJ
author Umamaheswari Natarajan
Thiagarajan Venkatesan
Vijayaraghavan Radhakrishnan
Shila Samuel
Periannan Rasappan
Appu Rathinavelu
spellingShingle Umamaheswari Natarajan
Thiagarajan Venkatesan
Vijayaraghavan Radhakrishnan
Shila Samuel
Periannan Rasappan
Appu Rathinavelu
Cell Cycle Arrest and Cytotoxic Effects of SAHA and RG7388 Mediated through p21<sup>WAF1/CIP1</sup> and p27<sup>KIP1</sup> in Cancer Cells
Medicina
SAHA
RG7388
MDM2
p53
p21
cell cycle arrest
cell death
author_facet Umamaheswari Natarajan
Thiagarajan Venkatesan
Vijayaraghavan Radhakrishnan
Shila Samuel
Periannan Rasappan
Appu Rathinavelu
author_sort Umamaheswari Natarajan
title Cell Cycle Arrest and Cytotoxic Effects of SAHA and RG7388 Mediated through p21<sup>WAF1/CIP1</sup> and p27<sup>KIP1</sup> in Cancer Cells
title_short Cell Cycle Arrest and Cytotoxic Effects of SAHA and RG7388 Mediated through p21<sup>WAF1/CIP1</sup> and p27<sup>KIP1</sup> in Cancer Cells
title_full Cell Cycle Arrest and Cytotoxic Effects of SAHA and RG7388 Mediated through p21<sup>WAF1/CIP1</sup> and p27<sup>KIP1</sup> in Cancer Cells
title_fullStr Cell Cycle Arrest and Cytotoxic Effects of SAHA and RG7388 Mediated through p21<sup>WAF1/CIP1</sup> and p27<sup>KIP1</sup> in Cancer Cells
title_full_unstemmed Cell Cycle Arrest and Cytotoxic Effects of SAHA and RG7388 Mediated through p21<sup>WAF1/CIP1</sup> and p27<sup>KIP1</sup> in Cancer Cells
title_sort cell cycle arrest and cytotoxic effects of saha and rg7388 mediated through p21<sup>waf1/cip1</sup> and p27<sup>kip1</sup> in cancer cells
publisher MDPI AG
series Medicina
issn 1010-660X
publishDate 2019-01-01
description <i>Background and Objective</i>: Alterations in gene expressions are often due to epigenetic modifications that can have a significant influence on cancer development, growth, and progression. Lately, histone deacetylase inhibitors (HDACi) such as suberoylanilide hydroxamic acid (SAHA, or vorinostat, MK0683) have been emerging as a new class of drugs with promising therapeutic benefits in controlling cancer growth and metastasis. The small molecule RG7388 (idasanutlin, R05503781) is a newly developed inhibitor that is specific for an oncogene-derived protein called MDM2, which is also in clinical trials for the treatment of various types of cancers. These two drugs have shown the ability to induce p21 expression through distinct mechanisms in MCF-7 and LNCaP cells, which are reported to have wild-type TP53. Our understanding of the molecular mechanism whereby SAHA and RG7388 can induce cell cycle arrest and trigger cell death is still evolving. In this study, we performed experiments to measure the cell cycle arrest effects of SAHA and RG7388 using MCF-7 and LNCaP cells. <i>Materials and Methods</i>: The cytotoxicity, cell cycle arrest, and apoptosis/necroptosis effects of the SAHA and RG7388 treatments were assessed using the Trypan Blue dye exclusion (TBDE) method, 3-(4,5-dimethylthiazol-2-yl)-2,5-diphenyltetrazolium bromide (MTT) assay, fluorescence assay with DEVD-<i>amc</i> substrate, and immunoblotting methods. <i>Results:</i> The RG7388 treatment was able to induce cell death by elevating p21<sup>WAF1/CIP1</sup> through inhibition of MDM2 in LNCaP, but not in MCF-7 cells, even though there was evidence of p53 elevation. Hence, we suspect that there is some level of uncoupling of p53-mediated transcriptional induction of p21<sup>WAF1/CIP1</sup> in MCF-7 cells. <i>Conclusion</i>: Our results from MCF-7 and LNCaP cells confirmed that SAHA and RG7388 treatments were able to induce cell death via a combination of cell cycle arrest and cytotoxic mechanisms. We speculate that our findings could lead to the development of newer treatments for breast and prostate cancers with drug combinations including HDACi.
topic SAHA
RG7388
MDM2
p53
p21
cell cycle arrest
cell death
url https://www.mdpi.com/1010-660X/55/2/30
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