Targeted drug-loaded PLGA-PCL microspheres for specific and localized treatment of triple negative breast cancer

PLGA公司 体内 紫杉醇 三阴性乳腺癌 细胞毒性 神童素 离体 乳腺癌 药品 癌症研究 药理学 靶向给药 癌症 化学 流式细胞术 药物输送 医学 体外 免疫学 内科学 生物 生物化学 有机化学 大肠杆菌 基因 粘质沙雷氏菌 生物技术
作者
Chukwudalu C. Nwazojie,John D. Obayemi,Ali A. Salifu,Sandra M. Borbor-Sawyer,Vanessa O. Uzonwanne,Chinyerem E. Onyekanne,Udom M. Akpan,Killian Onwudiwe,Josephine C. Oparah,Olushola S. Odusanya,Y. Danyuo
出处
期刊:Journal of Materials Science: Materials in Medicine [Springer Science+Business Media]
卷期号:34 (8)
标识
DOI:10.1007/s10856-023-06738-y
摘要

Abstract The paper presents the results of the experimental and analytical study of targeted drug-loaded polymer-based microspheres made from blend polymer of polylactic-co-glycolic acid and polycaprolactone (PLGA-PCL) for targeted and localized cancer drug delivery. In vitro sustained release with detailed thermodynamically driven drug release kinetics, over a period of three months using encapsulated targeted drugs (prodigiosin-EphA2 or paclitaxel-EphA2) and control drugs [Prodigiosin (PGS), and paclitaxel (PTX)] were studied. Results from in vitro study showed a sustained and localized drug release that is well-characterized by non-Fickian Korsmeyer–Peppas kinetics model over the range of temperatures of 37 °C (body temperature), 41 °C, and 44 °C (hyperthermic temperatures). The in vitro alamar blue, and flow cytometry assays in the presence of the different drug-loaded polymer formulations resulted to cell death and cytotoxicity that was evidence through cell inhibition and late apoptosis on triple negative breast cancer (TNBC) cells (MDA-MB 231). In vivo studies carried out on groups of 4-week-old athymic nude mice that were induced with subcutaneous TNBC, showed that the localized release of the EphA2-conjugated drugs was effective in complete elimination of residual tumor after local surgical resection. Finally, ex vivo histopathological analysis carried out on the euthanized mice revealed no cytotoxicity and absence of breast cancer metastases in the liver, kidney, and lungs 12 weeks after treatment. The implications of the results are then discussed for the development of encapsulated EphA2-conjugated drugs formulation in the specific targeting, localized, and sustain drug release for the elimination of local recurred TNBC tumors after surgical resection. Graphical Abstract

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