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Inhibitory Growth of Oral Squamous Cell Carcinoma Cancer via Bacterial Prodigiosin.


ABSTRACT: Chemotherapy drugs for oral cancers always cause side effects and adverse effects. Currently natural sources and herbs are being searched for treated human oral squamous carcinoma cells (OSCC) in an effort to alleviate the causations of agents in oral cancers chemotherapy. This study investigates the effect of prodigiosin (PG), an alkaloid and natural red pigment as a secondary metabolite of Serratia marcescens, to inhibit human oral squamous carcinoma cell growth; thereby, developing a new drug for the treatment of oral cancer. In vitro cultured human OSCC models (OECM1 and SAS cell lines) were used to test the inhibitory growth of PG via cell cytotoxic effects (MTT assay), cell cycle analysis, and Western blotting. PG under various concentrations and time courses were shown to effectively cause cell death and cell-cycle arrest in OECM1 and SAS cells. Additionally, PG induced autophagic cell death in OECM1 and SAS cells by LC3-mediated P62/LC3-I/LC3-II pathway at the in vitro level. These findings elucidate the role of PG, which may target the autophagic cell death pathways as a potential agent in cancer therapeutics.

SUBMITTER: Cheng MF 

PROVIDER: S-EPMC5532666 | biostudies-literature | 2017 Jul

REPOSITORIES: biostudies-literature

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Inhibitory Growth of Oral Squamous Cell Carcinoma Cancer via Bacterial Prodigiosin.

Cheng Ming-Fang MF   Lin Chun-Shu CS   Chen Yu-Hsin YH   Sung Ping-Jyun PJ   Lin Shian-Ren SR   Tong Yi-Wen YW   Weng Ching-Feng CF  

Marine drugs 20170715 7


Chemotherapy drugs for oral cancers always cause side effects and adverse effects. Currently natural sources and herbs are being searched for treated human oral squamous carcinoma cells (OSCC) in an effort to alleviate the causations of agents in oral cancers chemotherapy. This study investigates the effect of prodigiosin (PG), an alkaloid and natural red pigment as a secondary metabolite of <i>Serratia marcescens</i>, to inhibit human oral squamous carcinoma cell growth; thereby, developing a n  ...[more]

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