miR-29b enhances prostate cancer cell invasion independently of MMP-2 expression

被引:23
作者
Ivanovic, Renato F. [1 ]
Viana, Nayara I. [1 ]
Morais, Denis R. [1 ]
Silva, Iran A. [1 ]
Leite, Katia R. [1 ]
Pontes-Junior, Jose [1 ]
Inoue, Gustavo [1 ]
Nahas, William C. [2 ,3 ]
Srougi, Miguel [1 ]
Reis, Sabrina T. [1 ]
机构
[1] Univ Sao Paulo, Med Sch, Urol Dept, Lab Med Invest LIM55, Av Dr Arnaldo 455,2 Floor,Room 2145, BR-01246903 Sao Paulo, Brazil
[2] Univ Sao Paulo, Med Sch, Urol Dept, Urooncol Grp, Sao Paulo, Brazil
[3] ICESP, Sao Paulo, Brazil
基金
巴西圣保罗研究基金会;
关键词
Prostate cancer; Matrix metalloproteinases; Collagen; microRNA; MATRIX METALLOPROTEINASE-2; COLLAGEN PRODUCTION; TUMOR; METASTASIS; GROWTH; TISSUE;
D O I
10.1186/s12935-018-0516-0
中图分类号
R73 [肿瘤学];
学科分类号
100214 ;
摘要
Background: The ability to metastasize is one of the most important characteristics of neoplastic cells. An imbalance between the action of some matrix metalloproteinases (MMPs) and tissue inhibitors of MMPs drives the invasion process. Some studies have suggested that MMP-2 is involved in metastasis, while other studies have reported that collagen production by cancer cells might also contribute to motility. However, decreased expression of microRNA-29b (miR-29b), which may control MMP-2 and collagen gene expression, has been shown in prostate cancer (PCa). The objectives of the present study were to clarify whether MMP-2 as well as collagens I and III (encoded by COL1A1 and COL3A1, respectively) are controlled by miR-29b and to determine whether metastasis is altered by this relationship. Methods: PCa DU145 and PC-3 cells were transfected with 100 mu L of OPTI-MEM I containing 100 nmol of miR-29b (or its inhibitor) along with 1.5 mu L of lipofectamine. Positive and negative controls were prepared using the same protocol. MMP-2, COL1A1 and COL3A1 messenger RNA (mRNA) levels were evaluated via real-time polymerase chain reaction (qRT-PCR). For qRT-PCR, 6 x 10(4) cells were used. Invasion studies were conducted with Matrigel assays, which simulate invasion of the extracellular matrix by neoplastic cells. After transfection of 3 x 10(4) cells, invasion was allowed to proceed for 48 h. Invasive cells were counted under an optical microscope. Each experiment was performed in triplicate. Results: MMP-2 mRNA was not expressed in DU145 cells after transfection with miR-29b. After transfection of cells with the miR-29b inhibitor, COL1A1 (p = 0.02) and COL3A1 (p = 0.06) mRNA expression was increased in DU145 cells, and a large number of transfected DU145 and PC3 cells invaded the Matrigel membrane. Conclusions: In vitro studies showed that reducing the amount of miR-29b may lead to higher PCa cell invasion via a process that is independent of MMP-2. Collagen expression, controlled by miR-29b, may facilitate this motility process. Thus, the present study suggests that collagen production plays an active role in metastasis control and restoration of miR-29b levels may decrease metastasis. Altogether, these findings support further exploration of drug therapy targeting this aspect of the metastasis circuit.
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页数:6
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共 25 条
[1]  
ADAMS AT, 1985, EXP CELL BIOL, V53, P181
[2]   Overexpression of TGF-β by infiltrated granulocytes correlates with the expression of collagen mRNA in pancreatic cancer [J].
Aoyagi, Y ;
Oda, T ;
Kinoshita, T ;
Nakahashi, C ;
Hasebe, T ;
Ohkohchi, N ;
Ochiai, A .
BRITISH JOURNAL OF CANCER, 2004, 91 (07) :1316-1326
[3]   NEOPLASTIC ASSOCIATION OF ENHANCED TYPE-V COLLAGEN PRODUCTION IN RAT FIBROSARCOMA [J].
ASOKAN, R ;
REDDY, GK ;
DHAR, SC .
MOLECULAR AND CELLULAR BIOCHEMISTRY, 1993, 120 (01) :25-32
[4]  
BOSTWICK DG, 1995, ARCH PATHOL LAB MED, V119, P444
[5]   LOX-Mediated Collagen Crosslinking Is Responsible for Fibrosis-Enhanced Metastasis (Publication with Expression of Concern. See vol. 79, pg. 5124, 2019) [J].
Cox, Thomas R. ;
Bird, Demelza ;
Baker, Ann-Marie ;
Barker, Holly E. ;
Ho, Melisa W-Y ;
Lang, Georgina ;
Erler, Janine T. .
CANCER RESEARCH, 2013, 73 (06) :1721-1732
[6]   Remodeling and homeostasis of the extracellular matrix: implications for fibrotic diseases and cancer [J].
Cox, Thomas R. ;
Erler, Janine T. .
DISEASE MODELS & MECHANISMS, 2011, 4 (02) :165-178
[7]   Characterization of reactive stroma in prostate cancer: involvement of growth factors, metalloproteinase matrix, sexual hormones receptors and prostatic stem cells [J].
da Silva Junior, Mauricio Moreira ;
Matheus, Wagner Eduardo ;
Garcia, Patrick Vianna ;
Stopiglia, Rafael Mamprim ;
Billis, Athanase ;
Ferreira, Ubirajara ;
Favaro, Wagner Jose .
INTERNATIONAL BRAZ J UROL, 2015, 41 (05) :849-858
[8]   DESMOPLASIA AND ITS RELEVANCE TO COLORECTAL TUMOR INVASION [J].
HEWITT, RE ;
POWE, DG ;
CARTER, GI ;
TURNER, DR .
INTERNATIONAL JOURNAL OF CANCER, 1993, 53 (01) :62-69
[9]  
Kanoh Y, 2002, ANTICANCER RES, V22, P1813
[10]   Comprehensive Study of Gene and microRNA Expression Related to Epithelial-Mesenchymal Transition in Prostate Cancer [J].
Katz, Betina ;
Reis, Sabrina T. ;
Viana, Nayara I. ;
Morais, Denis R. ;
Moura, Caio M. ;
Dip, Nelson ;
Silva, Iran A. ;
Iscaife, Alexandre ;
Srougi, Miguel ;
Leite, Katia R. M. .
PLOS ONE, 2014, 9 (11)