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Bisphosphonate enhances TRAIL sensitivity to human osteosarcoma cells $via$ death receptor 5 upregulation
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  • Bisphosphonate enhances TRAIL sensitivity to human osteosarcoma cells $via$ death receptor 5 upregulation
  • Bisphosphonate enhances TRAIL sensitivity to human osteosarcoma cells $via$ death receptor 5 upregulation
저자명
Moon. Myung-Hee,Jeong. Jae-Kyo,Seo. Jae-Suk,Seol. Jae-Won,Lee. You-Jin,Xue. Meilang,Jackson. Christopher J.,Park. Sang-Youel
간행물명
Experimental & molecular medicine : EMM
권/호정보
2011년|43권 3호|pp.138-145 (8 pages)
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생화학분자생물학회
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정기간행물|ENG|
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이 논문은 한국과학기술정보연구원과 논문 연계를 통해 무료로 제공되는 원문입니다.
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Tumor necrosis factor (TNF)-related apoptosis-inducing ligand (TRAIL), a member of the TNF superfamily of cytokines, is one of the most promising candidates for cancer therapeutics. However, many osteosarcomas are resistant to TRAIL. Bisphosphonates are very effective in the treatment of bone problems associated with malignancies; the antitumor effects are due to the inhibition of protein prenylation that is essential for cell function and survival. The purpose of this study was to determine the effects of bisphosphonates on TRAIL-resistant MG 63 human osteosarcoma cells. The cells showed no response to TRAIL alone; however, pre-treatment with bisphosphonates significantly increased TRAIL-mediated apoptosis and cellular activation of caspase-3. Bisphosphonates significantly induced mRNA and protein expression of the TRAIL receptor, DR5. Bisphosphonates induced protein unprenylation in MG 63 cells; in addition, co-treatment with TRAIL also significantly increased protein unprenylation. Blocking of protein unprenylation using geranylgeraniol attenuated the cellular responses, including cell apoptosis and protein unprenylation induced by bisphosphonates and TRAIL. This is the first study to demonstrate that bisphosphonates markedly enhanced TRAIL-induced apoptosis in human osteosarcoma cells. These findings suggest that bisphosphonates may be a new and effective anticancer treatment with TRAIL proteins for TRAIL-resistant cancer cells.