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首页> 外文期刊>Journal of natural products >Grassystatins D-F, Potent Aspartic Protease Inhibitors from Marine Cyanobacteria as Potential Antimetastatic Agents Targeting Invasive Breast Cancer
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Grassystatins D-F, Potent Aspartic Protease Inhibitors from Marine Cyanobacteria as Potential Antimetastatic Agents Targeting Invasive Breast Cancer

机译:蝗虫D-F,来自海洋蓝藻的有效的天冬氨酸蛋白酶抑制剂作为靶向侵入性乳腺癌的潜在抗致抗体剂

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摘要

Three new modified peptides named grassystatins D-F (1-3) were discovered from a marine cyanobacterium from Guam. Their structures were elucidated using NMR spectroscopy and mass spectrometry. The hallmark structural feature in the peptides is a statine unit, which contributes to their aspartic protease inhibitory activity preferentially targeting cathepsins D and E. Grassystatin F (3) was the most potent analogue, with IC50 values of 50 and 0.5 nM against cathepsins D and E, respectively. The acidic tumor microenvironment is known to increase the activation of some of the lysosomal proteases associated with tumor metastasis such as cathepsins. Because cathepsin D is a biomarker in aggressive forms of breast cancer and linked to poor prognosis, the effects of cathepsin D inhibition by 1 and 3 on the downstream cellular substrates cystatin C and PAI-1 were investigated. Furthermore, the functional relevance of targeting cathepsin D substrates was evaluated by examining the effect of 1 and 3 on the migration of MDA-MD-231 cells. Grassystatin F (3) inhibited the cleavage of cystatin C and PAI-1, the activities of their downstream targets cysteine cathepsins and tPA, and the migration of the highly aggressive triple negative breast cancer cells, phenocopying the effect of siRNA-mediated knockdown of cathepsin D.
机译:来自关岛的海洋蓝色的海洋蓝杆菌发现了三种新的改性肽。使用NMR光谱和质谱法阐明了它们的结构。肽中的标志性结构特征是一种诱导肽单元,其促进其优先靶向组织蛋白酶D和E. Grastsstatin F(3)是最有效的类似物,IC50值为50%和0.5nm对抗组织蛋白酶d和0.5nm。 e分别。已知酸性肿瘤微环境,用于增加与肿瘤转移相关的一些溶酶体蛋白酶等组织蛋白酶的活化。由于组织蛋白酶D是乳腺癌侵蚀性形式的生物标志物并与预后差,所研究的表明蛋白酶D抑制在下游细胞底物胱抑素C和PAI-1上的影响。此外,通过检查MDA-MD-231细胞的迁移的效果来评价靶向组织蛋白酶D衬底的功能相关性。蚱蜢F(3)抑制胱抑素C和PAI-1的切割,其下游靶线性半胱氨酸组织蛋白和TPA的活性,以及​​高侵蚀性三重阴性乳腺癌细胞的迁移,杀菌术治疗蛋白的敲低的效果D.

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