首页> 外文期刊>European journal of pharmaceutics and biopharmaceutics: official journal of Arbeitsgemeinschaft fuer Pharmazeutische Verfahrenstechnik e.V >Development of controlled drug delivery systems for bone fracture-targeted therapeutic delivery: A review
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Development of controlled drug delivery systems for bone fracture-targeted therapeutic delivery: A review

机译:骨折针对性治疗交付控制药物递送系统的开发:综述

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Impaired fracture healing is a major clinical problem that can lead to patient disability, prolonged hospitalization, and significant financial burden. Although the majority of fractures heal using standard clinical practices, approximately 10% suffer from delayed unions or non-unions. A wide range of factors contribute to the risk for nonunions including internal factors, such as patient age, gender, and comorbidities, and external factors, such as the location and extent of injury. Current clinical approaches to treat nonunions include bone grafts and low intensity pulsed ultrasound (LIPUS), which realizes clinical success only to select patients due to limitations including donor morbidities (grafts) and necessity of fracture reduction (LIPUS), respectively. To date, therapeutic approaches for bone regeneration rely heavily on protein-based growth factors such as INFUSE, an FDA-approved scaffold for delivery of bone morphogenetic protein 2 (BMP-2). Small molecule modulators and RNAi therapeutics are under development to circumvent challenges associated with traditional growth factors. While preclinical studies has shown promise, drug delivery has become a major hurdle stalling clinical translation. Therefore, this review overviews current therapies employed to stimulate fracture healing pre-clinically and clinically, including a focus on drug delivery systems for growth factors, parathyroid hormone (PTH), small molecules, and RNAi therapeutics, as well as recent advances and future promise of fracture-targeted drug delivery.
机译:骨折愈合受损是一种主要的临床问题,可导致患者残疾,长期住院,以及重大的金融负担。虽然大多数骨折使用标准临床实践愈合,但大约10%的人遭受了延迟的工会或非工会。广泛的因素有助于非官量的风险,包括内部因素,例如患者年龄,性别和合并症,以及外部因素,如伤害的位置和程度。治疗非源性的当前临床方法包括骨移植和低强度脉冲超声(LIPUS),其仅实现临床成功,仅针对包括供体病症(移植物)的限制和骨折减少(LIPUS)的必要性。迄今为止,骨再生的治疗方法严重依赖于基于蛋白质的生长因子,例如注入,用于递送骨形态发生蛋白2(BMP-2)的FDA批准的支架。小分子调节剂和RNAi治疗方法正在开发中以规避与传统生长因素相关的挑战。虽然临床前研究表明了承诺,但药物递送已成为一个主要的障碍临床翻译。因此,本综述概述了在临床和临床上刺激骨折愈合的当前疗法,包括关注生长因子的药物递送系统,甲状旁腺激素(PTH),小分子和RNAi治疗,以及最近的进步和未来承诺骨折靶向药物递送。

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