首页> 外文期刊>The Journal of Organic Chemistry >A Selective Carborane-Functionalized Gastrin-Releasing Peptide Receptor Agonist as Boron Delivery Agent for Boron Neutron Capture Therapy
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A Selective Carborane-Functionalized Gastrin-Releasing Peptide Receptor Agonist as Boron Delivery Agent for Boron Neutron Capture Therapy

机译:一种选择性碳硼烷官能化的胃泌素释放肽受体激动剂作为硼中子捕获治疗的硼递送剂

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摘要

Boron neutron capture therapy (BNCT) allows the selective elimination of malignant tumor cells without affecting healthy tissue. Although this binary radiotherapy approach has been known for decades, BNCT failed to reach the daily clinics to date. One of the reasons is the lack of selective boron delivery agents. Using boron loaded peptide conjugates, which address G protein-coupled receptors overexpressed on tumor cells allow the intracellular accumulation of boron. The gastrin-releasing peptide receptor (GRPR) is a well-known target in cancer diagnosis and can potentially be used for BNCT. Here, we present the successful introduction of multiple bis-deoxygalactosyl-carborane building blocks to the GRPR-selective ligand [D-Phe(6), beta-Ala(11)) Ala(13), Nle(14)]Bn(6-14) (sBB2L) generating peptide conjugates with up to 80 boron atoms per molecule. Receptor activation was retained, metabolic stability was increased, and uptake into PC3 cells was proven without showing any intrinsic cytotoxicity. Furthermore, undesired uptake into liver cells was suppressed by using L-deoxygalactosyl modified carborane building blocks. Due to its high boron loading and excellent GRPR selectivity, this conjugate can be considered as a promising boron delivery agent for BNCT.
机译:硼中子捕获疗法(BNCT)允许选择性消除恶性肿瘤细胞而不影响健康组织。虽然这种二进制放射治疗方法已经已知几十年来,但BNCT迄今未能达到日常诊所。其中一个原因是缺乏选择性硼递送剂。使用硼加载的肽缀合物,其地址在肿瘤细胞上过表达的G蛋白偶联受体允许细胞内积聚硼。胃泌素释放肽受体(GRPR)是癌症诊断中的众所周知的靶标,可能用于BNCT。在这里,我们向GRPR选择性配体[D-PHE(6),β-ALA(11))ALA(13),NLE(14)] BN(6,我们展示了多个双脱氧糖基 - 碳硼烷基建筑块-14)(SBB2L)每分子产生高达80个硼原子的肽缀合物。保留受体激活,增加代谢稳定性,并经过证明在不显示任何内在细胞毒性的情况下被证明进入PC3细胞。此外,通过使用L-脱氧酰亚乳糖基改性的碳硼结构块抑制了不希望的吸收肝细胞。由于其高硼负载和优异的GRPR选择性,该缀合物可以被认为是BNCT的有前途的硼递送剂。

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