Your search keyword '"constitutively active mutation"' showing total 4 results

1. An in vitro carcinogenesis model for cervical cancer harboring episomal form of HPV16.

Author

Wongjampa, Weerayut, Nakahara, Tomomi, Tanaka, Katsuyuki, Yugawa, Takashi, Ekalaksananan, Tipaya, Kleebkaow, Pilaiwan, Goshima, Naoki, Kiyono, Tohru, and Pientong, Chamsai

Subjects

CERVICAL cancer, GENE expression, ONCOGENES, VIRAL genomes, HUMAN papillomavirus, CARCINOGENESIS, HELA cells

Abstract

Deregulated expression of viral E6 and E7 genes often caused by viral genome integration of high-risk human papillomaviruses (HR-HPVs) into host DNA and additional host genetic alterations are thought to be required for the development of cervical cancer. However, approximately 15% of invasive cervical cancer specimens contain only episomal HPV genomes. In this study, we investigated the tumorigenic potential of human cervical keratinocytes harboring only the episomal form of HPV16 (HCK1T/16epi). We found that the HPV16 episomal form is sufficient for promoting cell proliferation and colony formation of parental HCK1T cells. Ectopic expression of host oncogenes, MYC and PIK3CAE545K, enhanced clonogenic growth of both early- and late-passage HCK1T/16epi cells, but conferred tumor-initiating ability only to late-passage HCK1T/16epi cells. Interestingly, the expression levels of E6 and E7 were rather lower in late-passage than in early-passage cells. Moreover, additional introduction of a constitutively active MEK1 (MEK1DD) and/or KRASG12V into HCK1T/16epi cells resulted in generation of highly potent tumor-initiating cells. Thus an in vitro model for progression of cervical neoplasia with episomal HPV16 was established. In the model, constitutively active mutation of PIK3CA, PIK3CAE545K, and overexpression of MYC, in the cells with episomal HPV16 genome were not sufficient, but an additional event such as activation of the RAS-MEK pathway was required for progression to tumorigenicity. [ABSTRACT FROM AUTHOR]

Published

2023

2. Susceptibility of Human Head and Neck Cancer Cells to Combined Inhibition of Glutathione and Thioredoxin Metabolism.

Author

Sobhakumari, Arya, Love-Homan, Laurie, Fletcher, Elise V. M., Martin, Sean M., Parsons, Arlene D., Spitz, Douglas R., Knudson, C. Michael, and Simons, Andrean L.

Subjects

HEAD & neck cancer, CANCER cells, GLUTATHIONE, THIOREDOXIN, METABOLISM

Abstract

Increased glutathione (GSH) and thioredoxin (Trx) metabolism are mechanisms that are widely implicated in resistance of cancer cells to chemotherapy. The current study determined if simultaneous inhibition of GSH and Trx metabolism enhanced cell killing of human head and neck squamous cell carcinoma (HNSCC) cells by a mechanism involving oxidative stress. Inhibition of GSH and Trx metabolism with buthionine sulfoximine (BSO) and auranofin (AUR), respectively, induced significant decreases in clonogenic survival compared to either drug alone in FaDu, Cal-27 and SCC-25 HNSCC cells in vitro and in vivo in Cal-27 xenografts. BSO+AUR significantly increased glutathione and thioredoxin oxidation and suppressed peroxiredoxin activity in vitro. Pre-treatment with N-acetylcysteine completely reversed BSO+AUR-induced cell killing in FaDu and Cal-27 cells, while catalase and selenium supplementation only inhibited BSO+AUR-induced cell killing in FaDu cells. BSO+AUR decreased caspase 3/7 activity in HNSCC cells and significantly reduced the viability of both Bax/Bak double knockout (DKO) and DKO-Bax reconstituted hematopoietic cells suggesting that necrosis was involved. BSO+AUR also significantly sensitized FaDu, Cal-27, SCC-25 and SQ20B cells to cell killing induced by the EGFR inhibitor Erlotinib in vitro. These results support the conclusion that simultaneous inhibition of GSH and Trx metabolism pathways induces oxidative stress and clonogenic killing in HNSCCs and this strategy may be useful in sensitizing HNSCCs to EGFR inhibitors. [ABSTRACT FROM AUTHOR]

Published

2012

3. Mediator Subunit 12 Is Required for Neutrophil Development in Zebrafish.

Author

Keightley, Maria-Cristina, Layton, Judith E., Hayman, John W., Heath, Joan K., and Lieschke, Graham J.

Subjects

NEUTROPHILS, ZEBRA danio, HEMATOPOIESIS, STEM cells, PROGENITOR cells, TRANSCRIPTION factors, RNA polymerases, MISSENSE mutation

Abstract

Hematopoiesis requires the spatiotemporal organization of regulatory factors to successfully orchestrate diverse lineage specificity from stem and progenitor cells. Med12 is a regulatory component of the large Mediator complex that enables contact between the general RNA polymerase II transcriptional machinery and enhancer bound regulatory factors. We have identified a new zebrafish med12 allele, syr, with a single missense mutation causing a valine to aspartic acid change at position 1046. Syr shows defects in hematopoiesis, which predominantly affect the myeloid lineage. Syr has identified a hematopoietic cell-specific requirement for Med12, suggesting a new role for this transcriptional regulator. [ABSTRACT FROM AUTHOR]

Published

2011

4. Regulation of the Actin Cytoskeleton by an Interaction of IQGAP Related Protein GAPA with Filamin and Cortexillin I.

Author

Mondal, Subhanjan, Burgute, Bhagyashri, Rieger, Daniela, Müller, Rolf, Rivero, Francisco, Jan Faix, Schleicher, Michael, and Noegel, Angelika A.

Subjects

DICTYOSTELIUM discoideum, PROTEIN crosslinking, CYTOPLASM, CELL division, ACTIN, ACTOMYOSIN, CYTOPLASMIC filaments, CYTOKINESIS, CYTOSKELETON

Abstract

Filamin and Cortexillin are F-actin crosslinking proteins in Dictyostelium discoideum allowing actin filaments to form three-dimensional networks. GAPA, an IQGAP related protein, is required for cytokinesis and localizes to the cleavage furrow during cytokinesis. Here we describe a novel interaction with Filamin which is required for cytokinesis and regulation of the F-actin content. The interaction occurs through the actin binding domain of Filamin and the GRD domain of GAPA. A similar interaction takes place with Cortexillin I. We further report that Filamin associates with Rac1a implying that filamin might act as a scaffold for small GTPases. Filamin and activated Rac associate with GAPA to regulate actin remodelling. Overexpression of filamin and GAPA in the various strains suggests that GAPA regulates the actin cytoskeleton through interaction with Filamin and that it controls cytokinesis through association with Filamin and Cortexillin. [ABSTRACT FROM AUTHOR]

Published

2010