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Potential anticancer activity of a new pro-apoptotic peptide-thioctic acid gold nanoparticle platform

机译:新型促凋亡肽 - 噻吨酸金纳米粒子平台的潜在抗癌活性

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Targeted nanoparticle platforms designed to induce cell death by apoptosis can bypass the resistance mechanisms of cancer cells. With this in mind we have constructed a new cancer-targeting peptide-functionalized nanoparticle using gold nanoparticles (AuNPs) and a thioctic acid-DMPGTVLP peptide (TA-peptide) conjugate. Morphological analysis of the nanoparticles by transmission electron microscopy showed average diameters of about 3.52 nm and 26.2 nm for the AuNP core and shell, respectively. Strong affinity toward the nucleolin receptors of breast cancer cell lines MCF-7 and T47D was observed for the TA-peptide gold nanoparticles (TAP@AuNPs) based on IC50 values. Furthermore, the nanoparticles showed excellent hemocompatibility. Quantitative results of atomic absorption showed improved uptake of TAP@AuNPs. Treatment of the cells with TAP@AuNPS resulted in greater release of cytochrome c following caspase-3/7 activation compared with free TA-peptide. The cytosolic level of adenosine triphosphate for TAP@AuNPs was higher than in controls. Higher anti-tumor efficiency was observed for TAP@AuNPs than TA-peptide compared with phosphate-buffered saline after intratumoral injection in tumor-bearing mice. It can be concluded that the design and development of a receptor-specific peptide-AuNP platform will be valuable for theranostic applications in cancer nanomedicine.
机译:通过凋亡诱导细胞死亡的靶向纳米颗粒平台可以绕过癌细胞的耐药机制。考虑到这一点,我们利用金纳米粒子(AuNPs)和硫辛酸DMPGTVLP肽(TA肽)结合物构建了一种新的癌症靶向肽功能化纳米粒子。通过透射电子显微镜对纳米颗粒进行的形态分析显示,AuNP核和壳的平均直径分别约为3.52 nm和26.2 nm。观察到TA肽金纳米颗粒对乳腺癌细胞系MCF-7和T47D的核仁蛋白受体具有很强的亲和力(TAP@AuNPs)基于IC50值。此外,纳米颗粒显示出良好的血液相容性。原子吸收的定量结果显示,对有机物的吸收有所改善TAP@AuNPs.细胞的化学治疗TAP@AuNPS与游离TA肽相比,caspase-3/7激活后细胞色素c的释放量更大。三磷酸腺苷的胞浆水平TAP@AuNPs高于对照组。观察到的抗肿瘤效率较高TAP@AuNPs在荷瘤小鼠肿瘤内注射TA肽后,与磷酸盐缓冲盐水相比,TA肽的作用更强。可以得出结论,受体特异性肽AuNP平台的设计和开发将对癌症纳米医学的治疗应用具有重要价值。

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