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首页> 外文期刊>The Journal of biological chemistry >Molecular Mechanisms of the Cytotoxicity of Human α-Lactalbumin Made Lethal to Tumor Cells (HAMLET) and Other Protein-Oleic Acid Complexes
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Molecular Mechanisms of the Cytotoxicity of Human α-Lactalbumin Made Lethal to Tumor Cells (HAMLET) and Other Protein-Oleic Acid Complexes

机译:人α-乳白蛋白的细胞毒性对肿瘤细胞(哈姆雷特)和其他蛋白质 - 油酸复合物的分子机制

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摘要

Although HAMLET (human α-lactalbumin made lethal to tumor cells), a complex formed by human α-lactalbumin and oleic acid, has a unique apoptotic activity for the selective killing of tumor cells, the molecular mechanisms of expression of the HAMLET activity are not well understood. Therefore, we studied the molecular properties of HAMLET and its goat counterpart, GAMLET (goat α-lactalbumin made lethal to tumor cells), by pulse field gradient NMR and 920-MHz two-dimensional NMR techniques. We also examined the expression of HAMLET-like activities of complexes between oleic acid and other proteins that form a stable molten globule state. We observed that both HAMLET and GAMLET at pH 7.5 were heterogeneous, composed of the native protein, the monomeric molten globule-like state, and the oligomeric species. At pH 2.0 and 50 °C, HAMLET and GAMLET appeared in the monomeric state, and we identified the oleic acid-binding site in the complexes by two-dimensional NMR. Rather surprisingly, the binding site thus identified was markedly different between HAMLET and GAMLET. Furthermore, canine milk lysozyme, apo-myoglobin, and β2-microglobulin all formed the HAMLET-like complex with the anti-tumor activity, when the protein was treated with oleic acid under conditions in which their molten globule states were stable. From these results, we conclude that the protein portion of HAMLET, GAMLET, and the other HAMLET-like protein-oleic acid complexes is not the origin of their cytotoxicity to tumor cells and that the protein portion of these complexes plays a role in the delivery of cytotoxic oleic acid molecules into tumor cells across the cell membrane.
机译:虽然哈姆雷特(人α-乳白催眠使致命肿瘤细胞),但是由人α-乳白蛋白和油酸形成的复合物具有独特的凋亡活性,用于选择性杀死肿瘤细胞,哈姆雷特活性的表达的分子机制不是完全了解。因此,我们研究了哈姆雷特及其山羊对应物的分子特性,通过脉冲场梯度NMR和920-MHz二维NMR技术,通过脉冲场梯度NMR和920-MHz二维NMR技术。我们还检查了油酸和其他蛋白质之间的堆积米氏菌的表达式,其形成稳定的熔甘细胞状态。我们观察到,在pH7.5的哈姆雷特和发泡丸中均为异质的,由天然蛋白质,单体熔母状状态和低聚物种组成。在pH 2.0和50℃下,在单体状态下出现毛茸茸的毛茸茸,并且我们通过二维NMR鉴定了复合物中的油酸结合位点。如此鉴定的结合位点在哈姆雷特和GAMLLET之间具有明显不同。此外,犬牛奶溶菌酶,apo-myoglobin和β2-微球蛋白全部与抗肿瘤活性形成哈姆雷特状复合物,当蛋白质在其熔融球液稳定的条件下用油酸处理蛋白质。从这些结果来,我们得出结论,哈姆雷特,小族族样蛋白 - 油酸复合物的蛋白质部分不是它们对肿瘤细胞的细胞毒性的起源,并且这些配合物的蛋白质部分在交付中发挥作用细胞毒性油酸分子进入细胞膜肿瘤细胞。

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