Expression of the cytoskeletal proteins – cytokeratins and beta-III tubulin in human melanoma cell lines from the collection of N. N. Blokhin National Medical Research Center of Oncology

Q4 Pharmacology, Toxicology and Pharmaceutics

Uspehi Molekularnoj Onkologii Pub Date : 2023-10-09 DOI:10.17650/2313-805x-2023-10-3-82-89

T. A. Bogush, I. E. Mizaeva, A. A. Basharina, A. N. Grishanina, M. A. Baryshnikova, O. S. Burova, A. A. Rudakova, V. S. Kosorukov

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Abstract

Introduction. Despite advances in the treatment of melanoma, the results of therapy cannot be considered satisfactory, and the search for new drugs and effective combinations of medicine continues. The drugs are being developed aimed at reducing the metastatic tumor potential – migrastatics. The targets of the drugs can be cytoskeletal proteins of tumor cells – cytokeratin (CK) intermediate filaments and microtubule protein beta-III tubulin (TUBB3). Aim. To estimate of the CK and TUBB3 expression in melanoma cell lines to form an informative in vitro cell model for screening and studying migrastatics. Materials and methods. The molecular phenotype of 21 human melanoma cell lines from the collection of N. N. Blokhin National Medical Research Center of Oncology, and 18 of which were isolated from tumor metastases in the lymph nodes, soft tissues or subcutaneously. The level of TUBB3 expression and de novo expression of CKs in vimentin-expressing cells (CK + Vim) were assessed by an immunofluorescent method and flow cytometry. Results. Beta-III tubulin expression was detected in all cultures studied, de novo expression of CKs was found in 20 / 21 lines. The exception was primary uveal melanoma 92-1, that did not express CK + Vim. Both parameters significantly differed between the cells of the studied panel: CK + Vim co-expression – from 0 to 91 %, TUBB3 – from 18 to 86 %. No correlation was found between the expression level of TUBB3 and CK + Vim (Pearson’s correlation coefficient r = 0.11; p = 0.65). Three groups of the cell lines with different ratio of TUBB3 expression and CK + Vim co-expression were identified: 1) similar level of expression of both markers; 2) the level of co-expression of CK + Vim more or less high than the index for TUBB3; 3) the level of TUBB3 expression more or less high than the index for CK + Vim co-expression. Conclusion. A panel of 21 human melanoma cell lines was formed with quantitatively estimated expression of cytoske-letal proteins responsible for the migration activity of tumor cells – CKs and TUBB3. Groups of the lines with different expression ratio of the markers can be used for screening and preclinical evaluation potential migrastatics that reduce the metastatic potential of melanoma and may reduce resistance to taxanes.

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N. N. Blokhin国家肿瘤医学研究中心收集的人黑色素瘤细胞系中细胞骨架蛋白-细胞角蛋白和β - iii微管蛋白的表达

介绍。尽管在黑素瘤的治疗方面取得了进展，但治疗的结果不能令人满意，对新药和有效药物组合的研究仍在继续。目前正在开发的药物旨在降低转移性肿瘤的可能性。药物的作用靶点可以是肿瘤细胞的细胞骨架蛋白-细胞角蛋白(CK)中间丝和微管蛋白β - iii微管蛋白(TUBB3)。的目标。估计CK和TUBB3在黑色素瘤细胞系中的表达，为筛选和研究迁移性提供体外细胞模型。材料和方法。从N. N. Blokhin国家肿瘤医学研究中心收集的21株人黑色素瘤细胞株的分子表型，其中18株来自淋巴结、软组织或皮下肿瘤转移。采用免疫荧光法和流式细胞术检测vimentin表达细胞(CK + Vim)中TUBB3的表达水平和CK的新生表达水平。结果。β - iii微管蛋白在所有培养物中均有表达，在20 / 21株培养物中有新生表达。唯一的例外是原发性葡萄膜黑色素瘤92-1，它不表达CK + Vim。这两个参数在研究小组的细胞之间有显著差异:CK + Vim共表达-从0到91%，TUBB3 -从18%到86%。TUBB3表达水平与CK + Vim无相关性(Pearson相关系数r = 0.11;P = 0.65)。对TUBB3和CK + Vim共表达比例不同的三组细胞系进行了鉴定:1)两种标记物的表达水平相近;2) CK + Vim的共表达水平高于或低于TUBB3的指数;3) TUBB3表达水平高于或低于CK + Vim共表达指数。结论。21个人类黑色素瘤细胞系组成了一个小组，定量估计了负责肿瘤细胞迁移活性的细胞骨架蛋白- ck和TUBB3的表达。标记物表达比例不同的细胞系组可用于筛选和临床前评估潜在的迁移抑制剂，降低黑色素瘤的转移潜力，并可能降低对紫杉烷类药物的耐药性。

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来源期刊

Uspehi Molekularnoj Onkologii Pharmacology, Toxicology and Pharmaceutics-Pharmacology, Toxicology and Pharmaceutics (miscellaneous)

CiteScore

0.40

自引率

0.00%

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审稿时长

8 weeks