Expression of Mitochondrial Non-coding RNAs (ncRNAs) Is Modulated by High Risk Human Papillomavirus (HPV) Oncogenes


Autoria(s): Villota, Claudio; Campos, America; Vidaurre, Soledad; Oliveira-Cruz, Luciana; Pierulivo, Enrique Mario Boccardo; Burzio, Veronica A.; Varas, Manuel; Villegas, Jaime; Villa, Luisa Lina; Valenzuela, Pablo D. T.; Socias, Miguel; Roberts, Sally; Burzio, Luis O.
Contribuinte(s)

UNIVERSIDADE DE SÃO PAULO

Data(s)

06/11/2013

06/11/2013

2012

Resumo

The study of RNA and DNA oncogenic viruses has proved invaluable in the discovery of key cellular pathways that are rendered dysfunctional during cancer progression. An example is high risk human papillomavirus (HPV), the etiological agent of cervical cancer. The role of HPV oncogenes in cellular immortalization and transformation has been extensively investigated. We reported the differential expression of a family of human mitochondrial non-coding RNAs (ncRNAs) between normal and cancer cells. Normal cells express a sense mitochondrial ncRNA (SncmtRNA) that seems to be required for cell proliferation and two antisense transcripts (ASncmtRNAs). In contrast, the ASncmtRNAs are down-regulated in cancer cells. To shed some light on the mechanisms that trigger down-regulation of the ASncmtRNAs, we studied human keratinocytes (HFK) immortalized with HPV. Here we show that immortalization of HFK with HPV-16 or 18 causes down-regulation of the ASncmtRNAs and induces the expression of a new sense transcript named SncmtRNA-2. Transduction of HFK with both E6 and E7 is sufficient to induce expression of SncmtRNA-2. Moreover, E2 oncogene is involved in down-regulation of the ASncmtRNAs. Knockdown of E2 in immortalized cells reestablishes in a reversible manner the expression of the ASncmtRNAs, suggesting that endogenous cellular factors(s) could play functions analogous to E2 during non-HPV-induced oncogenesis.

Fondecyt [11090060, 1085210, 1110835]

FONDECYT

Fondef [D04I1338]

Fondef

CCTEPFB16 Program Grant

CCTE-PFB16 Program Grant

Conicyt, Chile

CONICYT, Chile

Universidad Andres Bello, Chile

Universidad Andres Bello, Chile [DI-34-09/R, DI-31-09/R, DI-28-09/R4, DI-06-09/R]

Identificador

JOURNAL OF BIOLOGICAL CHEMISTRY, BETHESDA, v. 287, n. 25, supl. 1, Part 1, pp. 21303-21315, 42156, 2012

0021-9258

http://www.producao.usp.br/handle/BDPI/42451

10.1074/jbc.M111.326694

http://dx.doi.org/10.1074/jbc.M111.326694

Idioma(s)

eng

Publicador

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC

BETHESDA

Relação

JOURNAL OF BIOLOGICAL CHEMISTRY

Direitos

closedAccess

Copyright AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC

Palavras-Chave #DOUBLE-STRANDED-RNA #TRANSGENIC MICE #HUMAN KERATINOCYTES #TUMOR-SUPPRESSOR #E2 PROTEIN #REGULATORY REGION #CANCER-CELLS #TYPE-16 E7 #GENES #TARGETS #BIOCHEMISTRY & MOLECULAR BIOLOGY
Tipo

article

original article

publishedVersion