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主动点击加载法制备的载多西紫杉醇-谷胱甘肽脂质体的治疗指数提高。

Improved therapeutic index of the liposomal docetaxel-glutathione prepared by active click loading.

机构信息

Clinical Medical College and The First Affiliated Hospital of Chengdu Medical College, Chengdu, China.

The Second Affiliated Hospital of Chengdu Medical College, China National Nuclear Corporation 416 Hospital, China.

出版信息

Eur J Pharm Biopharm. 2024 Oct;203:114435. doi: 10.1016/j.ejpb.2024.114435. Epub 2024 Aug 3.

DOI:10.1016/j.ejpb.2024.114435
PMID:39103002
Abstract

The clinical usage of docetaxel (DTX) is severely hindered by the dose-limiting neutropenia and peripheral neurotoxicity of polysorbate 80-solubilized DTX injection, and there are no alternative formulations until now. In this study, we developed a new liposomal formulation of DTX to reduce its toxicities, accompanying with the greatly improved antitumor activity. The DTX was encapsulated into liposomes in the form of hydrophilic glutathione (GSH)-conjugated prodrugs using a click drug loading method, which achieved a high encapsulation efficiency (∼95 %) and loading capacity (∼30 % wt). The resulting liposomal DTX-GSH provided a sustained and efficient DTX release (∼50 % within 48 h) in plasma, resulting in a greatly improved antitumor activities as compared with that of polysorbate 80-solubilized DTX injection in the subcutaneous and orthotopic 4T1 breast tumor bearing mice. Even large tumors > 500 mm could be effectively inhibited and shrunk after the administration of liposomal DTX-GSH. More importantly, the liposomal DTX-GSH significantly decreased the neutropenia and peripheral neurotoxicity as compared with that of polysorbate 80-solubilized DTX injection at the equivalent dose. These data suggested that the liposomal DTX-GSH might become a superior alternative formulation to the commercial DTX injection.

摘要

多西紫杉醇(DTX)的临床应用受到聚山梨酯 80 增溶 DTX 注射液引起的剂量限制性中性粒细胞减少症和周围神经毒性的严重阻碍,到目前为止还没有替代制剂。在本研究中,我们开发了一种新的多西紫杉醇脂质体制剂,以降低其毒性,同时大大提高抗肿瘤活性。多西紫杉醇采用点击药物加载方法以亲水性谷胱甘肽(GSH)缀合前药的形式包封到脂质体中,实现了高包封效率(约 95%)和载药量(约 30%wt)。所得的脂质体 DTX-GSH 在血浆中提供了持续有效的多西紫杉醇释放(48 小时内约 50%),与聚山梨酯 80 增溶的 DTX 注射液相比,在皮下和原位 4T1 乳腺癌荷瘤小鼠中表现出大大提高的抗肿瘤活性。即使是>500mm 的大肿瘤,在给予脂质体 DTX-GSH 后也能有效抑制和缩小。更重要的是,与聚山梨酯 80 增溶的 DTX 注射液相比,脂质体 DTX-GSH 在等效剂量下显著降低了中性粒细胞减少症和周围神经毒性。这些数据表明,脂质体 DTX-GSH 可能成为商业 DTX 注射液的一种优越替代制剂。

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