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Bone-Targeted Drug Delivery Systems and Strategies for Treatment of Bone Metastasis

机译:骨靶向药物递送系统和治疗骨转移的策略

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摘要

Bone metastases can cause high morbidity and mortality, often developing as they advance, especially in patients with prostate and breast cancers. Most drugs are rarely distributed to the bone and are hence pharmacologically ineffective in treating bone metastases. The development of drug targeting technologies is required for the efficient treatment of bone metastases. To date, numerous bone-targeting ligands, including tetracyclines, bisphosphonates, aspartic acid, and aptamers have been developed and used for bone-targeted delivery of anti-tumor drugs, peptide/protein drugs, nucleic acid drugs, and diagnostic imaging agents. The conjugates of drugs with bone-targeting ligands were first developed in the field of bone drug targeting systems; macromolecular carriers and nanoparticles modified with these bone-targeting ligands have also been developed. Additionally, antibodies to prostate-specific membrane antigen (PSMA) and human epidermal growth factor receptor 2 (HER2) are used in active targeting bone metastatic prostate cancer and breast cancer, respectively. Some conjugates using antibodies to PSMA and HER2 were developed and used in clinical trials. In this review, recent challenges in the development of bone-targeted delivery systems and strategies for the treatment of bone metastasis have been summarized. Future development of novel drug formulations in order to optimize targeted drug delivery in the treatment of bone metastasis have also been discussed.
机译:骨转移可引起高发病率和死亡率,通常正在发展,特别是在前列腺和乳腺癌的患者中。大多数药物很少分布于骨骼,因此在治疗骨转移方面是药理学上有效。药物靶向技术的发展是有效治疗骨转移的。迄今为止,已经开发了许多骨靶向配体,包括四环素,双膦酸盐,天冬氨酸和适体,并用于骨靶向抗肿瘤药物,肽/蛋白质药物,核酸药物和诊断成像剂。用骨靶向配体的药物的缀合物首先在骨药物靶向系统领域中开发;还开发了用这些骨靶向配体改性的大分子载体和纳米颗粒。另外,对前列腺特异性膜抗原(PSMA)和人表皮生长因子受体2(HER2)的抗体分别用于活性靶向骨转移前列腺癌和乳腺癌。开发并用于临床试验中使用对PSMA和HER2的抗体的一些缀合物。在本综述中,总结了近期骨头递送系统和治疗骨转移策略的挑战。还讨论了新型药物配方的未来发展,以优化靶向药物递送在治疗骨转移中。

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