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Sweet-P inhibition of glucocorticoid receptor ? as a potential cancer therapy.


ABSTRACT: The need for the development of new cancer therapies and push for the design of new targeting techniques is on the rise, and would be useful for cancers that are resistant to current drug treatments. The understanding of the genome has significantly advanced cancer therapy, as well as prevention and earlier detection. This research highlight discusses a potential new type of cancer-targeting molecule, Sweet-P, which is the first of its kind. Sweet-P specifically targets the microRNA-144 binding site in the 3' untranslated region (3' UTR) of the human glucocorticoid receptor ? (GR?), which has been demonstrated to increase expression. GR? has been shown to be highly expressed in cells from solid tumors of uroepithelial carcinomas, gliomas, osteosarcomas, and hepatocellular carcinomas, as well as in liquid tumor cells from leukemia patients. In non-cancerous diseases, GR? has been shown to be highly expressed in glucocorticoid-resistant asthma. These maladies brought the need for the development of the Sweet-P anti-GR? molecule. Sweet-P was shown to repress the migration of bladder cancer cells, and may serve as a new therapeutic for GR?-related diseases.

SUBMITTER: Nwaneri AC 

PROVIDER: S-EPMC4959805 | biostudies-literature | 2016

REPOSITORIES: biostudies-literature

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Sweet-P inhibition of glucocorticoid receptor β as a potential cancer therapy.

Nwaneri Assumpta C AC   McBeth Lucien L   Hinds Terry D TD  

Cancer cell & microenvironment 20160705 3


The need for the development of new cancer therapies and push for the design of new targeting techniques is on the rise, and would be useful for cancers that are resistant to current drug treatments. The understanding of the genome has significantly advanced cancer therapy, as well as prevention and earlier detection. This research highlight discusses a potential new type of cancer-targeting molecule, Sweet-P, which is the first of its kind. Sweet-P specifically targets the microRNA-144 binding  ...[more]

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