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Aligning physics and physiology: Engineering antibodies for radionuclide delivery

机译:协调物理学和生理学:放射性核素递送的工程抗体

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摘要

The exquisite specificity of antibodies and antibody fragments renders them excellent agents for targeted delivery of radionuclides. Radiolabeled antibodies and fragments have been successfully used for molecular imaging and radioimmunotherapy (RIT) of cell-surface targets in oncology and immunology. Protein engineering has been employed for antibody humanization essential for clinical applications, as well as optimization of important characteristics including pharmacokinetics, biodistribution, and clearance. Although intact antibodies have high potential as imaging and therapeutic agents, challenges include long circulation time in blood, which leads to later imaging time points post-injection and higher blood absorbed dose that may be disadvantageous for RIT. Utilizing engineered fragments may address these challenges, as size reduction and removal of Fc function decreases serum half-life. Radiolabeled fragments and pretargeting strategies can result in high contrast images within hours to days, and a reduction of RIT toxicity in normal tissues. Additionally, fragments can be engineered to direct hepatic or renal clearance, which may be chosen based on the application and disease setting. This review discusses aligning the physical properties of radionuclides (positron, gamma, beta, alpha, and Auger-emitters) with antibodies and fragments, and highlights recent advances of engineered antibodies and fragments in preclinical and clinical development for imaging and therapy.
机译:抗体和抗体片段的精湛特异性使其成为放射性核素靶向输送的极佳试剂。放射性标记的抗体和片段已成功用于肿瘤和免疫学领域中细胞表面靶标的分子成像和放射免疫治疗(RIT)。蛋白质工程已被用于临床应用中必不可少的抗体人源化以及重要特性(包括药代动力学,生物分布和清除)的优化。尽管完整的抗体作为成像和治疗剂具有很高的潜力,但挑战包括血液中较长的循环时间,这会导致注射后成像时间点较晚,以及更高的血液吸收剂量,这可能对RIT不利。利用工程片段可能会解决这些挑战,因为尺寸减小和Fc功能去除会降低血清半衰期。放射性标记的片段和预靶向策略可在数小时至数天内产生高对比度的图像,并减少正常组织中RIT的毒性。另外,可以对片段进行工程改造以指导肝脏或肾脏清除,这可以根据应用和疾病情况进行选择。这篇综述讨论了将放射性核素(正电子,γ,β,α和俄歇发射体)的物理特性与抗体和片段对齐的方法,并重点介绍了工程化抗体和片段在成像和治疗的临床前和临床开发中的最新进展。

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  • 期刊名称 other
  • 作者

    Wen-Ting K. Tsai; Anna M. Wu;

  • 作者单位
  • 年(卷),期 -1(61),9
  • 年度 -1
  • 页码 693–714
  • 总页数 33
  • 原文格式 PDF
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