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载西维来司他纳米胶束的酶靶向递释抑制实验性关节炎的严重程度。

Enzyme targeted delivery of sivelestat loaded nanomicelle inhibits arthritic severity in experimental arthritis.

机构信息

Department of Chemical Biology, Institute of Nano Science and Technology, Sector 81, Knowledge city, Sahibzada Ajit Singh Nagar, Mohali, Punjab 140306, India.

Centre for Pharmaceutical Nanotechnology, Department of Pharmaceutics, National Institute of Pharmaceutical Education and Research, S.A.S Nagar, Sector 67, Mohali, Punjab 160062, India.

出版信息

Life Sci. 2023 Dec 1;334:122206. doi: 10.1016/j.lfs.2023.122206. Epub 2023 Oct 23.

Abstract

AIMS

Rheumatoid arthritis (RA) is chronic inflammatory disorder mainly affects the lining of articular cartilage of synovial joints characterized by severe inflammation and joint damage. The expression of proteolytic enzymes like MMP-2 and Neutrophil Elastase (NE) worsens the RA condition. To address this concern, we have synthesized dual enzyme targeted chlorotoxin conjugated nanomicelles loaded with sivelestat as broad spectrum treatment for RA.

MATERIALS AND METHODS

Conjugation of the chlorotoxin over nanomicelle and incorporation of sivelestat in nanomicelle provide it dual targeting potential. The sivelestat loaded nanomicelle (SLM) evaluated for the drug release and in-vitro cytocompatibility. Further, investigated its in-vivo anti-arthritic potential on collagen-induced arthritis in wistar rats.

KEY FINDINGS

The microscopic observation of SLM showed spherical ball like appearance with size ranging from 190 to 230 nm. SLM showed good drug loading and encapsulation efficiency along with no cytotoxicity against healthy cell lines. In-vivo therapeutic assessment on collagen induced arthritis rat model showed potential chondroprotection. The microscopic visualization of articular cartilage by staining showed that it restores the cartilage integrity and lowers the expression of pro-inflammatory enzymes showed by Immunohistochemistry and Immunofluorescence. We observed that, it restrain the mediators of synovial inflammation by simultaneous inhibition of the proteolytic enzymes involved in swelling, cartilage destruction and joint damage which provides strong chondroprotection.

SIGNIFICANCE

We report that significant alleviation of inflammation and inhibition of proteolytic enzymes together might provide enhanced potential for the treatment and management of RA.

摘要

目的

类风湿关节炎(RA)是一种慢性炎症性疾病,主要影响滑膜关节的关节软骨衬里,其特征为严重的炎症和关节损伤。蛋白水解酶如 MMP-2 和中性粒细胞弹性蛋白酶(NE)的表达使 RA 病情恶化。为了解决这一问题,我们合成了双重酶靶向氯毒素偶联纳米胶束,负载西维来司他,作为 RA 的广谱治疗药物。

材料和方法

氯毒素在纳米胶束上的偶联和西维来司他在纳米胶束中的掺入为其提供了双重靶向潜力。对载有西维来司他的纳米胶束(SLM)进行了药物释放和体外细胞相容性评价。进一步研究了其在胶原诱导性关节炎大鼠体内的抗关节炎潜力。

主要发现

SLM 的显微镜观察显示出球形球状物,大小在 190 到 230nm 之间。SLM 表现出良好的药物负载和包封效率,同时对健康细胞系无细胞毒性。在胶原诱导性关节炎大鼠模型中的体内治疗评估显示出潜在的软骨保护作用。通过染色对关节软骨进行微观可视化显示,它恢复了软骨的完整性,并降低了免疫组织化学和免疫荧光显示的促炎酶的表达。我们观察到,它通过同时抑制参与肿胀、软骨破坏和关节损伤的蛋白水解酶,抑制滑膜炎症的介质,从而提供强有力的软骨保护。

意义

我们报告说,炎症的显著减轻和蛋白水解酶的抑制可能共同为 RA 的治疗和管理提供增强的潜力。

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