UCL School of Pharmacy, 29-39 Brunswick Square, London WC1N 1AX, United Kingdom; National Institute for Health Research (NIHR) Biomedical Research Centre at Moorfields Eye Hospital NHS Foundation Trust and UCL Institute of Ophthalmology, London EC1V 9EL, United Kingdom.
UCL School of Pharmacy, 29-39 Brunswick Square, London WC1N 1AX, United Kingdom; National Institute for Health Research (NIHR) Biomedical Research Centre at Moorfields Eye Hospital NHS Foundation Trust and UCL Institute of Ophthalmology, London EC1V 9EL, United Kingdom.
Eur J Pharm Biopharm. 2020 Aug;153:130-149. doi: 10.1016/j.ejpb.2020.05.005. Epub 2020 May 21.
The majority of blinding conditions arise due to chronic pathologies in the retina. During the last two decades, antibody-based medicines administered by intravitreal injection directly into the back of the eye have revolutionised the treatment of chronic retinal diseases characterised by uncontrolled blood vessel growth, e.g. wet age-related macular degeneration (wAMD), diabetic retinopathy (DR) and choroidal neovascularisation (CNV). Although intravitreal injections have become a commonly performed ophthalmic procedure that provides a reproducible dose to maximise drug exposure in the back of the eye, there is a need to minimise the frequency and cumulative number of intravitreal injections. Developing longer acting intraocular therapies is one key strategy that is being pursued. Pharmaceutical preclinical development of intraocular medicines is heavily reliant on the use of animal models to determine ocular tolerability, pharmacokinetics, biodistribution and drug stability. Animal eyes are different from human eyes, such as the anatomy, organisation of vitreous macromolecular structure, aqueous outflow and immune response; all which impacts the ability to translate preclinical data into a clinical product. The development of longer acting protein formulations using animals is also limited because animals reject human proteins. Preclinical strategies also do not account for differences in the vitreous due to ageing and whether a vitrectomy has been performed. Intraocular formulations must reside and clear from the vitreous body, so there is a need for the formulation scientist to have knowledge about vitreous structure and physiology to facilitate preclinical development strategies. Preclinical pharmaceutical development paradigms used to create therapies for other routes of administration (e.g. oral, subcutaneous, pulmonary and intravenous) are grounded on the use of preclinical in vitro models. Analogous pharmaceutical strategies with appropriately designed in vitro models that can account for intraocular mass transfer to estimate pharmacokinetic profiles can be used to develop in vitro-in vivo correlations (IVIVCs) to accelerate the preclinical optimisation of long-acting intraocular formulations. Data obtained can then inform preclinical in vivo and clinical studies. With the now widespread use of intravitreal injections, it is also important during early preclinical studies to ensure there is a viable regulatory pathway for new therapies. Knowledge of the physiological, pharmaceutical and regulatory factors will help in the development of long-acting intravitreal medicines, which is rapidly evolving into a distinct pharmaceutical discipline.
大多数致盲情况是由于视网膜的慢性病变引起的。在过去的二十年中,通过玻璃体内注射直接向眼后给药的抗体药物治疗已经彻底改变了慢性视网膜疾病的治疗方法,这些疾病的特征是血管生长失控,例如湿性年龄相关性黄斑变性(wAMD)、糖尿病性视网膜病变(DR)和脉络膜新生血管化(CNV)。虽然玻璃体内注射已经成为一种常见的眼科手术,可提供可重复的剂量以最大限度地提高眼后药物暴露,但仍需要尽量减少玻璃体内注射的频率和累积次数。开发更长效的眼内治疗方法是正在追求的关键策略之一。眼科药物的药物临床前开发严重依赖于使用动物模型来确定眼内耐受性、药代动力学、生物分布和药物稳定性。动物眼睛与人类眼睛不同,例如解剖结构、玻璃体大分子结构、房水流出和免疫反应;所有这些都影响将临床前数据转化为临床产品的能力。由于动物排斥人类蛋白质,使用动物开发更长效的蛋白质制剂也受到限制。临床前策略也没有考虑到由于年龄增长和是否进行玻璃体切割而导致的玻璃体差异。眼内制剂必须在玻璃体中停留并清除,因此制剂科学家需要了解玻璃体的结构和生理学知识,以促进临床前开发策略。用于创建其他给药途径(例如口服、皮下、肺和静脉内)治疗方法的临床前药物开发范例基于使用临床前体外模型。可以使用具有适当设计的、能够考虑眼内质量转移以估计药代动力学特征的类似药物策略来开发体外-体内相关性(IVIVC),以加速长效眼内制剂的临床前优化。然后可以将获得的数据用于临床前体内和临床研究。随着玻璃体内注射的广泛应用,在早期临床前研究中确保新疗法有可行的监管途径也很重要。对生理、药物和监管因素的了解将有助于开发长效眼内药物,这正在迅速发展成为一门独特的药物学科。
