| Literature DB >> 28664270 |
Yangxue Zhang1, Qian Yang1, Chenyang Li1, Mengmeng Ding1, Xueyan Lv1, Chengqiu Tao1, Hongwu Yu1, Fang Chen1, Ying Xu2.
Abstract
A novel type I ribosome-inactivating protein (RIP), designated as curcin C, was purified from Jatropha curcas, an important feedback source of bio-fuel. Molecular mass and isoelectric point of curcin C were 31.398 kDa and 7.12 as detected by MALTI-TOF assay and capillary electrophoresis assay, respectively. N-terminal sequence and LC-MS/MS analyses confirmed that curcin C is a type I RIP having high homology, but not the exactly the same with curcin, another type 1 RIP isolated from the endosperm of J. curcas. It exhibited N-glycosidase activity and in vitro translation inhibition activity. Moreover, curcin C displayed a strong selectively anti-tumor activity on human cancer cells. Its cytotoxicity against osteosarcoma cell line U20S is even higher than that of Paclitaxel with IC50 of 0.019 μM. Purification and identification of curcin C not only suggested its potential in natural anticancer drug development, but also provide chance to understanding different cytotoxic action among different RIPs.Entities:
Keywords: Anti-tumor; Curcin C; Cytotoxicity; Jatropha curcas; N-Glycosidase; Ribosome-inactivating protein
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Year: 2017 PMID: 28664270 DOI: 10.1007/s00726-017-2456-8
Source DB: PubMed Journal: Amino Acids ISSN: 0939-4451 Impact factor: 3.520