摘要
100多年前,德国医师Paul Ehrlich首先提出了通过靶向剂选择性地向肿瘤提供“魔法子弹”的概念。通常由单克隆抗体或肽组成的抗体 - 药物偶联物(ADC)和肽 - 药物偶联物(PDC)的靶向治疗已被广泛研究了数十年。缀合物能够选择性地将细胞毒性有效载体递送到靶细胞,与传统化疗相比,其导致改善的功效,降低的全身毒性和改善的药代动力学(PK)/药效学(PD)。 PDC和ADC共享类似的概念,但具有非常不同的结构和性质。人源化抗体引入高特异性和延长的半衰期,而小分子量肽表现出更高的药物负载和增强的组织穿透能力,并且柔性线性或环肽更容易修饰。在本次审查中,总结了设计,综合方法和PDCs最新进展的原则。
关键词: 肽 - 药物偶联物(PDC),抗体 - 药物共轭物(ADC),肽,接头,有效载荷,药物设计。
Current Medicinal Chemistry
Title:Peptide-Drug Conjugate: A Novel Drug Design Approach
Volume: 24 Issue: 31
关键词: 肽 - 药物偶联物(PDC),抗体 - 药物共轭物(ADC),肽,接头,有效载荷,药物设计。
摘要: More than 100 years ago, German physician Paul Ehrlich first proposed the concept of selectively delivering “magic bullets” to tumors through targeting agents. The targeting therapy with antibody-drug conjugates (ADCs) and peptide-drug conjugate (PDCs), which are usually composed of monoclonal antibodies or peptides, toxic payloads and cleavage/ noncleavage linkers, has been extensively studied for decades. The conjugates enable selective delivery of cytotoxic payloads to target cells, which results in improved efficacy, reduced systemic toxicity and improved pharmacokinetics (PK)/pharmacodynamics (PD) compared with traditional chemotherapy. PDC and ADC share similar concept, but with vastly different structures and properties. Humanized antibodies introduce high specificity and prolonged half-life, while small molecule weight peptides exhibit higher drug loading and enhanced tissue penetration capacity, and the flexible linear or cyclic peptides are also modified more easily. In this review, the principles of design, synthesis approaches and the latest advances of PDCs are summarized.
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Cite this article as:
Peptide-Drug Conjugate: A Novel Drug Design Approach, Current Medicinal Chemistry 2017; 24 (31) . https://dx.doi.org/10.2174/0929867324666170404142840
DOI https://dx.doi.org/10.2174/0929867324666170404142840 |
Print ISSN 0929-8673 |
Publisher Name Bentham Science Publisher |
Online ISSN 1875-533X |
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