Expression of the Carboxy-Terminal Portion of MUC16/CA125 Induces Transformation and Tumor Invasion | Zendy

Thapi D. Rao | Zendy; Huasong Tian | Zendy; Xun Ma | Zendy; Xiujun Yan | Zendy; Sahityasri Thapi | Zendy; Nikolaus Schultz | Zendy; Néstor Rosales | Zendy; Sébastien Monette | Zendy; Amy Wang | Zendy; David M. Hyman | Zendy; Douglas A. Levine | Zendy; David B. Solit | Zendy; David R. Spriggs | Zendy

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Expression of the Carboxy-Terminal Portion of MUC16/CA125 Induces Transformation and Tumor Invasion

Author(s) -

Thapi D. Rao,

Huasong Tian,

Xun Ma,

Xiujun Yan,

Sahityasri Thapi,

Nikolaus Schultz,

Néstor Rosales,

Sébastien Monette,

Amy Wang,

David M. Hyman,

Douglas A. Levine,

David B. Solit,

David R. Spriggs

Publication year - 2015

Publication title -

plos one

Language(s) - English

Resource type - Journals

SCImago Journal Rank - 0.99

H-Index - 332

ISSN - 1932-6203

DOI - 10.1371/journal.pone.0126633

Subject(s) - biology , ectodomain , cancer research , mmp2 , transfection , matrigel , ovarian cancer , carcinogenesis , pten , microbiology and biotechnology , metastasis , cell culture , cancer , pi3k/akt/mtor pathway , signal transduction , receptor , biochemistry , angiogenesis , genetics

The CA125 antigen is found in the serum of many patients with serous ovarian cancer and has been widely used as a disease marker. CA125 has been shown to be an independent factor for clinical outcome in this disease. In The Cancer Genome Atlas ovarian cancer project, MUC16 expression levels are frequently increased, and the highest levels of MUC16 expression are linked to a significantly worse survival. To examine the biologic effect of the proximal portion of MUC16/CA125, NIH/3T3 (3T3) fibroblast cell lines were stably transfected with the carboxy elements of MUC16. As few as 114 amino acids from the carboxy-terminal portion of MUC16 were sufficient to increase soft agar growth, promote matrigel invasion, and increase the rate of tumor growth in athymic nude mice. Transformation with carboxy elements of MUC16 was associated with activation of the AKT and ERK pathways. MUC16 transformation was associated with up-regulation of a number of metastases and invasion gene transcripts, including IL-1β, MMP2, and MMP9. All observed oncogenic changes were exclusively dependent on the extracellular “ectodomain” of MUC16. The biologic impact of MUC16 was also explored through the creation of a transgenic mouse model expressing 354 amino acids of the carboxy-terminal portion of MUC16 (MUC16 c354 ). Under a CMV, early enhancer plus chicken β actin promoter (CAG) MUC16 c354 was well expressed in many organs, including the brain, colon, heart, kidney, liver, lung, ovary, and spleen. MUC16 c354 transgenic animals appear to be viable, fertile, and have a normal lifespan. However, when crossed with p53-deficient mice, the MUC16 c354 :p53 +/- progeny displayed a higher frequency of spontaneous tumor development compared to p53 +/- mice alone. We conclude that the carboxy-terminal portion of the MUC16/CA125 protein is oncogenic in NIH/3T3 cells, increases invasive tumor properties, activates the AKT and ERK pathways, and contributes to the biologic properties of ovarian cancer.

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