Gemcitabine eliminates double minute chromosomes from human ovarian cancer cells.

Double minute chromosomes are cytogenetic manifestations of gene amplification frequently seen in cancer cells. Genes amplified on double minute chromosomes include oncogenes and multi-drug resistant genes. These genes encode proteins which contribute to cancer formation, cancer progression, and dev...

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Main Authors: Lisa Yu, Yan Zhao, Chao Quan, Wei Ji, Jing Zhu, Yun Huang, Rongwei Guan, Donglin Sun, Yan Jin, Xiangning Meng, Chunyu Zhang, Yang Yu, Jing Bai, Wenjing Sun, Songbin Fu
Format: Article
Language:English
Published: Public Library of Science (PLoS) 2013-01-01
Series:PLoS ONE
Online Access:http://europepmc.org/articles/PMC3750019?pdf=render
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spelling doaj-75326fbaa09c4aeb84b9e28de2da5b0a2020-11-25T01:54:09ZengPublic Library of Science (PLoS)PLoS ONE1932-62032013-01-0188e7198810.1371/journal.pone.0071988Gemcitabine eliminates double minute chromosomes from human ovarian cancer cells.Lisa YuYan ZhaoChao QuanWei JiJing ZhuYun HuangRongwei GuanDonglin SunYan JinXiangning MengChunyu ZhangYang YuJing BaiWenjing SunSongbin FuDouble minute chromosomes are cytogenetic manifestations of gene amplification frequently seen in cancer cells. Genes amplified on double minute chromosomes include oncogenes and multi-drug resistant genes. These genes encode proteins which contribute to cancer formation, cancer progression, and development of resistance to drugs used in cancer treatment. Elimination of double minute chromosomes, and therefore genes amplified on them, is an effective way to decrease the malignancy of cancer cells. We investigated the effectiveness of a cancer drug, gemcitabine, on the loss of double minute chromosomes from the ovarian cancer cell line UACC-1598. Gemcitabine is able to decrease the number of double minute chromosomes in cells at a 7500X lower concentration than the commonly used cancer drug hydroxyurea. Amplified genes present on the double minute chromosomes are decreased at the DNA level upon gemcitabine treatment. Gemcitabine, even at a low nanomolar concentration, is able to cause DNA damage. The selective incorporation of double minutes chromatin and γ-H2AX signals into micronuclei provides a strong link between DNA damage and the loss of double minute chromosomes from gemcitabine treated cells. Cells treated with gemcitabine also showed decreased cell growth, colony formation, and invasion. Together, our results suggest that gemcitabine is effective in decreasing double minute chromosomes and this affects the biology of ovarian cancer cells.http://europepmc.org/articles/PMC3750019?pdf=render
collection DOAJ
language English
format Article
sources DOAJ
author Lisa Yu
Yan Zhao
Chao Quan
Wei Ji
Jing Zhu
Yun Huang
Rongwei Guan
Donglin Sun
Yan Jin
Xiangning Meng
Chunyu Zhang
Yang Yu
Jing Bai
Wenjing Sun
Songbin Fu
spellingShingle Lisa Yu
Yan Zhao
Chao Quan
Wei Ji
Jing Zhu
Yun Huang
Rongwei Guan
Donglin Sun
Yan Jin
Xiangning Meng
Chunyu Zhang
Yang Yu
Jing Bai
Wenjing Sun
Songbin Fu
Gemcitabine eliminates double minute chromosomes from human ovarian cancer cells.
PLoS ONE
author_facet Lisa Yu
Yan Zhao
Chao Quan
Wei Ji
Jing Zhu
Yun Huang
Rongwei Guan
Donglin Sun
Yan Jin
Xiangning Meng
Chunyu Zhang
Yang Yu
Jing Bai
Wenjing Sun
Songbin Fu
author_sort Lisa Yu
title Gemcitabine eliminates double minute chromosomes from human ovarian cancer cells.
title_short Gemcitabine eliminates double minute chromosomes from human ovarian cancer cells.
title_full Gemcitabine eliminates double minute chromosomes from human ovarian cancer cells.
title_fullStr Gemcitabine eliminates double minute chromosomes from human ovarian cancer cells.
title_full_unstemmed Gemcitabine eliminates double minute chromosomes from human ovarian cancer cells.
title_sort gemcitabine eliminates double minute chromosomes from human ovarian cancer cells.
publisher Public Library of Science (PLoS)
series PLoS ONE
issn 1932-6203
publishDate 2013-01-01
description Double minute chromosomes are cytogenetic manifestations of gene amplification frequently seen in cancer cells. Genes amplified on double minute chromosomes include oncogenes and multi-drug resistant genes. These genes encode proteins which contribute to cancer formation, cancer progression, and development of resistance to drugs used in cancer treatment. Elimination of double minute chromosomes, and therefore genes amplified on them, is an effective way to decrease the malignancy of cancer cells. We investigated the effectiveness of a cancer drug, gemcitabine, on the loss of double minute chromosomes from the ovarian cancer cell line UACC-1598. Gemcitabine is able to decrease the number of double minute chromosomes in cells at a 7500X lower concentration than the commonly used cancer drug hydroxyurea. Amplified genes present on the double minute chromosomes are decreased at the DNA level upon gemcitabine treatment. Gemcitabine, even at a low nanomolar concentration, is able to cause DNA damage. The selective incorporation of double minutes chromatin and γ-H2AX signals into micronuclei provides a strong link between DNA damage and the loss of double minute chromosomes from gemcitabine treated cells. Cells treated with gemcitabine also showed decreased cell growth, colony formation, and invasion. Together, our results suggest that gemcitabine is effective in decreasing double minute chromosomes and this affects the biology of ovarian cancer cells.
url http://europepmc.org/articles/PMC3750019?pdf=render
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