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血清蛋白对药物传递的临床影响。

Clinical impact of serum proteins on drug delivery.

机构信息

Tumor Biology Center, Division of Macromolecular Prodrugs, Breisacher Strasse 117, 79106 Freiburg, Germany.

出版信息

J Control Release. 2012 Jul 20;161(2):429-45. doi: 10.1016/j.jconrel.2011.11.028. Epub 2011 Dec 1.

Abstract

Among serum proteins albumin and transferrin have attracted the most interest as drug carriers in the past two decades. Prior to that, their potential use was overshadowed by the advent of monoclonal antibodies that was initiated by Milstein and Koehler in 1975. Meanwhile intensive pursuit of exploiting transferrin, but above all albumin as an exogenous or endogenous carrier protein for treating various diseases, primarily cancer, rheumatoid arthritis, diabetes and hepatitis has resulted in several marketed products and numerous clinical trials. While the use of transferrin has clinically been primarily restricted to immunotoxins, albumin-based drug delivery systems ranging from albumin drug nanoparticles, albumin fusion protein, prodrugs and peptide derivatives that bind covalently to albumin as well as physically binding antibody fragments and therapeutically active peptides are in advanced clinical trials or approved products. For treating diabetes, Levemir and Victoza that are myristic acid derivatives of human insulin or glucagon-like peptide 1 (GLP-1) act as long-acting peptides by binding to the fatty acid binding sites on circulating albumin to control glucose levels. Levemir from Novo Nordisk has already developed into a blockbuster since its market approval in 2004. Abraxane, an albumin paclitaxel nanoparticle as a water-soluble galenic formulation avoiding the use of cremophor/ethanol, transports paclitaxel through passive targeting as an albumin paclitaxel complex to the tumor site and is superior to conventional Taxol against metastatic breast cancer. INNO-206, an albumin-binding doxorubicin prodrug that also accumulates in solid tumors due to the enhanced permeability and retention (EPR) effect but releases the parent drug through acid cleavage, either intra- or extracellularly, is entering phase II studies against sarcoma. An expanding field is the use of albumin-binding antibody moieties which do not contain the fragment crystallizable (Fc) portion of, conventional immunoglobulin G (IgG) but are comprised of monovalent or bivalent light and/or heavy chains and incorporate an additional albumin-binding peptide or antibody domain. The most advanced antibody of this kind is ATN-103 (Ozoralizumab), a trivalent albumin-binding nanobody that neutralizes the pro-inflammatory tumor necrosis factor alpha (TNF-α) as a causative agent for exacerbating rheumatoid arthritis. ATN-103 is currently in multi-center phase II trials against this debilitating disease. In summary, because albumin as the most abundant circulating protein cannot only be used to improve the pharmacokinetic profile of therapeutically relevant peptides and the targeting moiety of antibodies but also for peptide-based targeting as well as low-molecular weight drugs to inflamed or malignant tissue, it is anticipated that R&D efforts of academia and the pharmaceutical industry in this field of drug delivery will prosper.

摘要

在过去的二十年中,血清蛋白白蛋白和转铁蛋白作为药物载体引起了人们的极大兴趣。在此之前,它们的潜在用途被米尔斯坦和科勒于 1975 年开创的单克隆抗体的出现所掩盖。与此同时,人们一直在积极探索转铁蛋白的用途,但最重要的是白蛋白作为治疗各种疾病(主要是癌症、类风湿关节炎、糖尿病和肝炎)的外源性或内源性载体蛋白,已经有几种上市产品和许多临床试验。虽然转铁蛋白的临床应用主要限于免疫毒素,但基于白蛋白的药物递送系统,包括白蛋白药物纳米颗粒、白蛋白融合蛋白、前药和肽衍生物,这些药物通过与白蛋白共价结合以及物理结合抗体片段和治疗活性肽,正在进行高级临床试验或获得批准产品。为了治疗糖尿病,人胰岛素或胰高血糖素样肽 1(GLP-1)的衍生物 Levemir 和 Victoza 通过与循环白蛋白上的脂肪酸结合位点结合,作为长效肽来控制血糖水平。自 2004 年获得批准以来,诺和诺德的 Levemir 已成为一款重磅炸弹药物。白蛋白紫杉醇纳米颗粒 Abraxane 作为一种水溶性的制剂,避免使用聚氧乙烯蓖麻油/乙醇,将紫杉醇作为白蛋白紫杉醇复合物通过被动靶向输送到肿瘤部位,优于传统的紫杉醇治疗转移性乳腺癌。INNO-206 是一种白蛋白结合的多柔比星前药,由于增强的通透性和保留(EPR)效应,也会在实体瘤中积累,但通过酸裂解在细胞内或细胞外释放母体药物,目前正在肉瘤的 II 期研究中。一个不断扩大的领域是使用不包含常规免疫球蛋白 G(IgG)的片段结晶(Fc)部分的白蛋白结合抗体片段,但由单价或二价轻链和/或重链组成,并包含额外的白蛋白结合肽或抗体结构域。这种最先进的抗体是 ATN-103(Ozoralizumab),一种三价白蛋白结合纳米抗体,可中和促炎肿瘤坏死因子-α(TNF-α),作为加重类风湿关节炎的致病因子。ATN-103 目前正在针对这种衰弱性疾病的多中心 II 期试验中。总之,由于白蛋白作为最丰富的循环蛋白,不仅可以用于改善治疗相关肽和抗体的靶向部分的药代动力学特性,还可以用于肽靶向以及针对炎症或恶性组织的低分子量药物,预计学术界和制药行业在药物输送领域的研发工作将蓬勃发展。

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