Chromatin structure of the regulatory regions of pS2 and cathepsin D genes in hormone-dependent and -independent breast cancer cell lines

被引:44
作者
Giamarchi, C
Solanas, M
Chailleux, C
Augereau, P
Vignon, F
Rochefort, H
Richard-Foy, H
机构
[1] CNRS, Lab Biol Mol Eucaryote, F-31062 Toulouse, France
[2] Univ Autonoma Barcelona, Fac Med, Dept Biol Cellular & Fisiol, E-08193 Barcelona, Spain
[3] INSERM, U148, Unite Hormones & Canc, F-34090 Montpellier, France
关键词
breast cancer; chromatin; pS2; cathepsin D; estrogens; IGFI;
D O I
10.1038/sj.onc.1202317
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
We have compared the DNase I hypersensitivity of the regulatory region of two estrogen-regulated genes, pS2 and cathepsin D in hormone-dependent and -independent breast carcinoma cell lines. This strategy allowed the identification of two important control regions, one in pS2 and the other in cathepsin D genes, In the hormone-dependent MCF7 cell line within the pS2 gene 5'-flanking region, we detected two major DNase I hypersensitive sites, induced by estrogens and/or IGFI: pS2-HS1, located in the proximal promoter and pS2-HS4, located -10.5 Kb from the CAP site, within a region that has not been cloned. The presence of these two DNase I hypersensitive sites correlates with pS2 expression. Interestingly in MCF7 cells, estrogens and IGFI induced indistinguishable chromatin structural changes over the pS2 regulatory region, suggesting that the two transduction-pathways converge to a unique chromatin target, In two cell lines that do not express pS2, MDA MB 231, a hormone-independent cell line that lacks the estrogen receptor alpha, and HE5, a cell line derived from MDA MB 231 by transfection that expresses estrogen receptor alpha, there was only one hormone-independent DNase I hypersensitive site. This site, pS2-HS2, was located immediately upstream of pS2-HS1, In MCF7 cells, two major DNase I hypersensitive sites were present in the 5'-flanking sequences of the cathepsin D gene, which is regulated by estrogens in these cells. These sites, catD-HS2 and catD-HS3, located at positions -2.3 Kb and -3.45 Kb, respectively, were both hormone-independent. A much weaker site, catD-HS1, covered the proximal promoter. In MDA MB 231 cells, that express cathepsin D constitutively we detected an additional strong hormone-independent DNase I hypersensitive site, catD-HS4, located at position -4.3 Kb, This region might control the constitutive over-expression of cathepsin D in hormone-independent breast cancer cells, All together, these data demonstrate that a local reorganization of the chromatin structure over pS2 and cathepsin D promoters accompanies the establishment of the hormone-independent phenotype of the cells.
引用
收藏
页码:533 / 541
页数:9
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