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基于多孔硅的眼内药物输送平台,用于双重药物加载和控制释放,实现协同治疗。

Porous silicon based intravitreal platform for dual-drug loading and controlled release towards synergistic therapy.

机构信息

a Department of Chemistry and Biochemistry , University of California , San Diego , CA , USA.

b Department of Ophthalmology , Jacobs Retina Center at Shiley Eye Institute, University of California , San Diego , CA , USA.

出版信息

Drug Deliv. 2018 Nov;25(1):1537-1545. doi: 10.1080/10717544.2018.1486474.

Abstract

The number of blind and low vision persons in the US is projected to increase to 5.68 million by 2020. The eye diseases causing loss of vision are life-long, chronic, and often need protracted presence of therapeutics at the disease site to keep the disease in remission. In addition, multiple pathologies participate in the disease process and a single therapy seems insufficient to bring the disease under control and prevent vision loss. This study demonstrates the use of porous silicon (pSi) particles sequentially loaded with daunorubicin (DNR) and dexamethasone (DEX) to create a synergistic intravitreally injectable dual-drug delivery system. DEX targets chronic inflammation while DNR inhibits excessive cell proliferation as well as suppresses hypoxia-inducible factor 1 to reduce scarring. This pSi-based delivery system releases therapeutic concentrations of DNR for 100 days and DEX for over 165 days after a single dose. This intravitreal dual-drug delivery system is also well tolerated after injection into the rabbit eye model, attested by ocular biomicroscopy, ocular tonometry, electroretinography, and histology. This novel dual-drug delivery system opens an attractive modality for combination therapy to manage refractory chorioretinal diseases and further preclinical studies are warranted to evaluate its efficacy.

摘要

到 2020 年,美国的盲人和低视力患者人数预计将增加到 568 万。导致视力丧失的眼部疾病是终身的、慢性的,并且往往需要在疾病部位长期存在治疗药物来使疾病缓解。此外,多种病理学参与疾病过程,单一疗法似乎不足以控制疾病并防止视力丧失。本研究展示了多孔硅 (pSi) 颗粒依次装载柔红霉素 (DNR) 和地塞米松 (DEX) 以创建协同性眼内注射双药物递送系统的用途。DEX 靶向慢性炎症,而 DNR 抑制过度细胞增殖并抑制缺氧诱导因子 1 以减少瘢痕形成。这种基于 pSi 的递药系统在单次注射后可释放 100 天的 DNR 和超过 165 天的 DEX 的治疗浓度。这种眼内双药物递送系统在注射到兔眼模型后也具有良好的耐受性,通过眼生物显微镜、眼内压测量、视网膜电图和组织学得到证实。这种新型双药物递送系统为联合治疗提供了一种有吸引力的方式来治疗难治性脉络膜视网膜疾病,进一步的临床前研究是评估其疗效的必要条件。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/6ffa/6058705/d0fdf76a162e/IDRD_A_1486474_F0001_C.jpg

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