8-Methoxypsoralen induces apoptosis by upregulating p53 and inhibits metastasis by downregulating MMP-2 and MMP-9 in human gastric cancer cells

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dc.contributor.authorEun Kyoung Choi-
dc.contributor.authorHae Dong Kim-
dc.contributor.authorEun Jung Park-
dc.contributor.authorSeuk Young Song-
dc.contributor.authorT T Phan-
dc.contributor.authorM Nam-
dc.contributor.authorM Kim-
dc.contributor.authorDong Uk Kim-
dc.contributor.authorK L Hoe-
dc.date.accessioned2023-02-27T16:32:59Z-
dc.date.available2023-02-27T16:32:59Z-
dc.date.issued2023-
dc.identifier.issn1976-9148-
dc.identifier.urihttps://oak.kribb.re.kr/handle/201005/31123-
dc.description.abstractFuranocoumarin 8-methoxypsoralen (8-MOP) is the parent compound that naturally occurs in traditional medicinal plants used historically. 8-MOP has been employed as a photochemotherapeutic component of Psoralen + Ultraviolet A (PUVA) therapy for the treatment of vitiligo and psoriasis. Although the role of 8-MOP in PUVA therapy has been studied, little is known about the effects of 8-MOP alone on human gastric cancer cells. In this study, we observed anti-proliferative effect of 8-MOP in several human cancer cell lines. Among these, the human gastric cancer cell line SNU1 is the most sensitive to 8-MOP. 8-MOP treated SNU1 cells showed G1-arrest by upregulating p53 and apoptosis by activating caspase-3 in a dose-dependent manner, which was confirmed by loss-of-function analysis through the knockdown of p53-siRNA and inhibition of apoptosis by Z-VAD-FMK. Moreover, 8-MOPinduced apoptosis is not associated with autophagy or necrosis. The signaling pathway responsible for the effect of 8-MOP on SNU1 cells was confirmed to be related to phosphorylated PI3K, ERK2, and STAT3. In contrast, 8-MOP treatment decreased the expression of the typical metastasis-related proteins MMP-2, MMP-9, and Snail in a p53-independent manner. In accordance with the serendipitous findings, treatment with 8-MOP decreased the wound healing, migration, and invasion ability of cells in a dose-dependent manner. In addition, combination treatment with 8-MOP and gemcitabine was effective at the lowest concentrations. Overall, our findings indicate that oral 8-MOP has the potential to treat early human gastric cancer, with fewer side effects.-
dc.publisherKorea Soc-Assoc-Inst-
dc.title8-Methoxypsoralen induces apoptosis by upregulating p53 and inhibits metastasis by downregulating MMP-2 and MMP-9 in human gastric cancer cells-
dc.title.alternative8-Methoxypsoralen induces apoptosis by upregulating p53 and inhibits metastasis by downregulating MMP-2 and MMP-9 in human gastric cancer cells-
dc.typeArticle-
dc.citation.titleBiomolecules & Therapeutics-
dc.citation.number2-
dc.citation.endPage226-
dc.citation.startPage219-
dc.citation.volume31-
dc.contributor.affiliatedAuthorEun Kyoung Choi-
dc.contributor.affiliatedAuthorHae Dong Kim-
dc.contributor.affiliatedAuthorEun Jung Park-
dc.contributor.affiliatedAuthorSeuk Young Song-
dc.contributor.affiliatedAuthorDong Uk Kim-
dc.contributor.alternativeName최은경-
dc.contributor.alternativeName김해동-
dc.contributor.alternativeName박은정-
dc.contributor.alternativeName송석영-
dc.contributor.alternativeNamePhan-
dc.contributor.alternativeName남미영-
dc.contributor.alternativeName김민정-
dc.contributor.alternativeName김동욱-
dc.contributor.alternativeName허광래-
dc.identifier.bibliographicCitationBiomolecules & Therapeutics, vol. 31, no. 2, pp. 219-226-
dc.identifier.doi10.4062/biomolther.2023.004-
dc.subject.keyword8-Methoxypsoralen-
dc.subject.keywordApoptosis-
dc.subject.keywordGastric cancer-
dc.subject.keywordMetastasis-
dc.subject.keywordMMP-2-
dc.subject.keywordp53-
dc.subject.local8-methoxypsoralen-
dc.subject.local8-Methoxypsoralen-
dc.subject.localApoptosis-
dc.subject.localapoptosis-
dc.subject.localGastric cancer-
dc.subject.localGastric cancer (GC)-
dc.subject.localgastric cancer-
dc.subject.localGastric Cancer-
dc.subject.localmetastasis-
dc.subject.localMetastasis-
dc.subject.localMMP-2-
dc.subject.localMMP2-
dc.subject.localP53-
dc.subject.localp53-
dc.description.journalClassY-
Appears in Collections:
Division of A.I. & Biomedical Research > Digital Biotech Innovation Center > 1. Journal Articles
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