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首页> 外文期刊>Dalton transactions: An international journal of inorganic chemistry >Towards translation of ~(212)Pb as a clinical therapeutic; Getting the lead in!
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Towards translation of ~(212)Pb as a clinical therapeutic; Getting the lead in!

机译:致力于〜(212)Pb的翻译作为临床治疗药物;抢先一步!

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Targeted α-particle therapy offers the potential for more specific tumor cell killing with less damage to surrounding normal tissue than β-emitters because of the combination of short path length (50-80 μm) with the high linear energy transfer (100 keV μm~(-1)) of this emission. These physical properties offer the real possibility of targeted (pre-targeted) α-therapy suitable for the elimination of minimal residual or micrometastatic disease. Targeted and pre-targeted radioimmunotherapy (RIT) using α-emitters such as ~(212)Bi (T_(1/2) = 1.01 h) and ~(212)Pb (T_(1/2) = 10.6 h) has demonstrated significant utility in both in vitro and in vivo model systems. ~(212)Pb, a promising α-particle emitting source, is the longer-lived parent nuclide of ~(212)Bi, and serves as an in vivo generator of ~(212)Bi. The radionuclide has been successfully used in RIT and pre-targeted RIT and demonstrated an enhanced therapeutic efficacy in combination with chemotherapeutics, such as gemcitabine and paclitaxel. The following perspective addresses the modes of radionuclide production, radiolabelling and chelation chemistry, as well as the application of ~(212)Pb to targeted and pre-targeted radiation therapy.
机译:靶向性的α粒子疗法具有短路径长度(50-80μm)和高线性能量传递(100 keVμm〜)的组合,提供了比β-发射体更特异性地杀死肿瘤细胞,对周围正常组织的伤害较小的潜力。 (-1))。这些物理特性为靶向(预靶向)α治疗提供了真正的可能性,适合消除最小的残留或微转移性疾病。已证明使用〜(212)Bi(T_(1/2)= 1.01 h)和〜(212)Pb(T_(1/2)= 10.6 h)等α发射体进行靶向和预靶向放射免疫治疗(RIT)在体外和体内模型系统中都有重要的用途。 〜(212)Pb是一种有前途的α粒子发射源,是〜(212)Bi寿命更长的母核,并充当〜(212)Bi的体内生成物。放射性核素已成功用于RIT和预靶向RIT中,并与吉西他滨和紫杉醇等化学治疗剂结合使用,显示出增强的治疗功效。以下观点介绍了放射性核素的产生,放射性标记和螯合化学的模式,以及〜(212)Pb在靶向和预靶向放射治疗中的应用。

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