The effect of addition of two targeted vectors, cRGD peptide and folic acid, with the same linker length on the properties of the doxorubicin phospholipid composition: a study of properties in vitro.

Q3 Biochemistry, Genetics and Molecular Biology

Biomeditsinskaya khimiya Pub Date : 2025-02-01 DOI:10.18097/PBMCR1538

L V Kostryukova, Yu A Tereshkina, F N Bedretdinov, A M Gisina

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引用次数: 0

Abstract

Serious side effects of the chemotherapeutic drug doxorubicin prompt researchers to develop systems for its targeted delivery to cells. In this work, we continued the study on the effect of using two vectors in a phospholipid delivery system of doxorubicin (Dox) for targeted therapy of breast cancer. We have obtained a composition NPh-Dox-cRGD-Fol(2.0) with the same linker length for both targeting ligands, cRGD and folic acid (PEG 2000). The resulting composition NPh-Dox-cRGD-Fol(2.0) with a particle size less than 50 nm and with 99% Dox incorporated into nanoparticles in an experiment on drug release at different pH values (5.0 and 7.4) showed a faster release and a high level of Dox compared to the phospholipid nanoform and a composition containing only the cRGD peptide. In vitro experiments on MDA-MB-231 breast cancer cells expressing the folate receptor and integrin αvβ3 demonstrated an increase in the total accumulation and internalization of Dox upon incubation with the dual-vector composition compared to the control samples. On the MCF-7 breast cancer cell line (expressing only the folate receptor), a similar effect was observed upon incubation with the single-vector composition containing folic acid (NPh-Dox-Fol(2.0)). In experiments with normal Wi-38 cell line, the internalization and total accumulation of the drug were comparable for both the free substance and the vector compositions. After 24 h-incubation of MDA-MB-231 cells with Dox-containing (10 μg/ml DOX) samples, the lowest percentage of living cells was observed for the studied dual-vector composition NPh-Dox-cRGD-Fol(2.0). On MCF-7 cells, the cytotoxic effect was manifested equally for the studied samples. The study of the cell death pathway on MDA-MB-231 cells showed the predominance of the apoptotic pathway (late apoptosis), while in the case of MCF-7 the necrosis pathway predominated. The cell cycle study performed using MDA-MB-231 cells (folate receptor (+) and integrin αvβ3 (+)) revealed an increase in the percentage of cells in the G0/G1 phase was noted thus indicating apoptotic cell death during incubation with NPh-Dox-cRGD-Fol(2.0). No differences were found between the samples in experiments performed on MCF-7 cells (folate receptor (+) and integrin αvβ3 (-)).

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连接体长度相同的cRGD肽和叶酸两种靶向载体的加入对阿霉素磷脂组成物性质的影响：体外性质研究

化疗药物阿霉素的严重副作用促使研究人员开发靶向递送到细胞的系统。在这项工作中，我们继续研究了在阿霉素（Dox）磷脂递送系统中使用两种载体对乳腺癌靶向治疗的影响。我们获得了一个NPh-Dox-cRGD-Fol（2.0）的组合物，它具有相同的连接长度，用于靶向配体，cRGD和叶酸（PEG 2000）。在不同pH值（5.0和7.4）的药物释放实验中，所得到的粒径小于50 nm且含有99% Dox的纳米颗粒组合物NPh-Dox-cRGD-Fol（2.0）与磷脂纳米形式和仅含有cRGD肽的组合物相比，释放速度更快，Dox水平较高。在表达叶酸受体和整合素αvβ3的MDA-MB-231乳腺癌细胞的体外实验中，与对照样品相比，双载体组合培养后，Dox的总积累和内化增加。在MCF-7乳腺癌细胞系（仅表达叶酸受体）上，用含有叶酸的单载体组合物（NPh-Dox-Fol(2.0)）孵育后观察到类似的效果。在正常Wi-38细胞系的实验中，游离物质和载体组成的药物内化和总蓄积相当。MDA-MB-231细胞与含DOX （10 μg/ml）的样品孵育24 h后，所研究的双载体组成NPh-Dox-cRGD-Fol（2.0）的活细胞率最低。在MCF-7细胞上，其细胞毒性作用对所研究的样品均有相同的表现。对MDA-MB-231细胞死亡途径的研究显示，凋亡途径（晚期凋亡）占主导地位，而MCF-7则以坏死途径占主导地位。使用MDA-MB-231细胞（叶酸受体（+）和整合素αvβ3(+)）进行的细胞周期研究显示，在NPh-Dox-cRGD-Fol（2.0）孵育期间，注意到G0/G1期细胞百分比的增加，从而表明凋亡细胞死亡。在MCF-7细胞（叶酸受体（+）和整合素αvβ3(-)）上进行的实验中，样品之间没有差异。

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来源期刊

Biomeditsinskaya khimiya Biochemistry, Genetics and Molecular Biology-Biochemistry, Genetics and Molecular Biology (all)

CiteScore

1.30

自引率

0.00%

发文量

期刊介绍： The aim of the Russian-language journal "Biomeditsinskaya Khimiya" (Biomedical Chemistry) is to introduce the latest results obtained by scientists from Russia and other Republics of the Former Soviet Union. The Journal will cover all major areas of Biomedical chemistry, including neurochemistry, clinical chemistry, molecular biology of pathological processes, gene therapy, development of new drugs and their biochemical pharmacology, introduction and advertisement of new (biochemical) methods into experimental and clinical medicine etc. The Journal also publish review articles. All issues of journal usually contain invited reviews. Papers written in Russian contain abstract (in English).