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抗逆转录病毒纳米晶体的配方及其开发成微针给药系统,用于治疗 HIV 相关神经认知障碍 (HAND) 的潜在治疗。

Formulation of antiretroviral nanocrystals and development into a microneedle delivery system for potential treatment of HIV-associated neurocognitive disorder (HAND).

机构信息

School of Pharmacy, Queen's University Belfast, 97 Lisburn Road, BT9 7BL, UK.

出版信息

Int J Pharm. 2023 Jun 10;640:123005. doi: 10.1016/j.ijpharm.2023.123005. Epub 2023 May 2.

DOI:10.1016/j.ijpharm.2023.123005
PMID:37142137
Abstract

HIV/AIDS remains a major global public health issue. While antiretroviral therapy is effective at reducing the viral load in the blood, up to 50% of those with HIV suffer from some degree of HIV-associated neurocognitive disorder, due to the presence of the blood-brain barrier restricting drugs from crossing into the central nervous system and treating the viral reservoir there. One way to circumvent this is the nose-to-brain pathway. This pathway can also be accessed via a facial intradermal injection. Certain parameters can increase delivery via this route, including using nanoparticles with a positive zeta potential and an effective diameter of 200 nm or less. Microneedle arrays offer a minimally invasive, pain-free alternative to traditional hypodermic injections. This study shows the formulation of nanocrystals of both rilpivirine (RPV) and cabotegravir, followed by incorporation into separate microneedle delivery systems for application to either side of the face. Following an in vivo study in rats, delivery to the brain was seen for both drugs. For RPV, a C was seen at 21 days of 619.17 ± 73.32 ng/g, above that of recognised plasma IC90 levels, and potentially therapeutically relevant levels were maintained for 28 days. For CAB, a C was seen at 28 days of 478.31 ± 320.86 ng/g, and while below recognised 4IC90 levels, does indicate that therapeutically relevant levels could be achieved by manipulating final microaaray patch size in humans.

摘要

HIV/AIDS 仍然是一个主要的全球公共卫生问题。虽然抗逆转录病毒疗法能有效降低血液中的病毒载量,但高达 50%的 HIV 患者患有某种程度的 HIV 相关神经认知障碍,这是由于血脑屏障限制了药物进入中枢神经系统并在那里治疗病毒库。一种规避方法是鼻脑途径。该途径也可以通过面部皮内注射进入。某些参数可以通过这种途径增加药物传递,包括使用带有正 zeta 电位和有效直径为 200nm 或以下的纳米颗粒。微针阵列为传统皮下注射提供了一种微创、无痛的替代方案。这项研究展示了利匹韦林(RPV)和卡替拉韦的纳米晶体的配方,然后将其纳入单独的微针传递系统,用于面部两侧的应用。在大鼠体内研究后,两种药物都能递送到大脑。对于 RPV,在 21 天时 C 为 21 天,为 619.17±73.32ng/g,高于公认的血浆 IC90 水平,并且在 28 天内维持潜在的治疗相关水平。对于 CAB,在 28 天时 C 为 28 天,为 478.31±320.86ng/g,虽然低于公认的 4IC90 水平,但表明通过操纵人类最终微阵列贴片的大小可以达到治疗相关水平。

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