An effective way for targeting EGFR-mediated carcinogenesis: an in vitro study

Q3 Pharmacology, Toxicology and Pharmaceutics Research Results in Pharmacology Pub Date : 2024-06-12 DOI:10.18413/rrpharmacology.10.453
Viktoria A. Pakina, Evgeniya Z. Iksanova, Evgeniya V. Shih, O. Tumutolova, Karen K. Arutiunian, I V Kargina, K. Blinov, Fedor P. Pilgaev, A. Epishkina, D. Blinov, E. V. Grebenkin, E. Blinova
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Abstract

Introduction: EGFR-activating overexpression or somatic mutations are common in different human cancers. In this regard, the search for promising ways to control the carcinogenic transformation of tumor cells and the progression of malignant tumors expressing EGFR seems to be one of the most promising and developing areas of modern molecular pathology and pharmacology. Material and Methods: An antitumor activity of a novel compound, a pyridine carboxylic acid derivative LHT-17-19, was studied. The molecule was developed and synthesized at the Department of Chemistry, Drug Design and Technology of All-Russian Research Center for Biological Active Compounds Safety (Russia). The study was carried out in cell cultures of stomach cancer (Hs746T, AGS and MKN1) and patient-derived organoid (PDO) model of breast cancer (BC) expressing wild-type EGFR. Results: It was shown that LHT-17-19 induced concentration-dependent cytotoxicity of EGFR-expressing gastric cancer cells of all the aforementioned cultures. Pathomorphological, immunohistochemical and molecular validation of BC organoids derived from ductal breast carcinoma cells of a 68-year-old patient was done. PDOs were established as ER-negative, PR-negative, Her2/neu-negative, EGFR-positive with 35% of the Ki-67 expression index. In addition, the tumor cells translocation was resulted in a loss of ER expression and PDOs molecular pattern conversion towards a more aggressive triple negative type. PDOs incubation with 0.5-60.0 µM LHT-17-19 was accompanied not only by inhibition of their growth and proliferation, but also by significant cytoreduction. Conclusion: Thus, in two-dimensional and three-dimensional tumor cell cultures, the possibility of controlling the oncogenic expression of EGFR with the acridone compound 9-ammonium-3,3-dimethyl-3,4-dihydroacridine-1(2H)-OH L-2-hydroxybutanedivacate (LHT-17-19) was shown.
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针对表皮生长因子受体介导的癌变的有效方法:体外研究
导言:表皮生长因子受体(EGFR)激活过表达或体细胞突变在不同的人类癌症中很常见。因此,寻找有希望的方法来控制肿瘤细胞的癌变和表达表皮生长因子受体的恶性肿瘤的进展,似乎是现代分子病理学和药理学最有希望和最有发展前景的领域之一:研究了一种新型化合物--吡啶甲酸衍生物 LHT-17-19 的抗肿瘤活性。该分子由全俄生物活性化合物安全研究中心(俄罗斯)化学、药物设计和技术部开发合成。研究在胃癌(Hs746T、AGS和MKN1)细胞培养物和表达野生型表皮生长因子受体(EGFR)的乳腺癌(BC)患者衍生有机体(PDO)模型中进行:结果表明,LHT-17-19能诱导上述所有培养物中表达表皮生长因子受体的胃癌细胞产生浓度依赖性细胞毒性。对从一名 68 岁患者的乳腺导管癌细胞中提取的 BC 有机体进行了病理形态学、免疫组化和分子验证。PDOs被确定为ER阴性、PR阴性、Her2/neu阴性、表皮生长因子受体(EGFR)阳性,Ki-67表达指数为35%。此外,肿瘤细胞易位导致ER表达丧失,PDOs分子模式向更具侵袭性的三阴型转化。用 0.5-60.0 µM LHT-17-19 培养 PDOs 不仅能抑制其生长和增殖,还能显著减少细胞减少:因此,在二维和三维肿瘤细胞培养中,吖啶酮化合物 9-铵-3,3-二甲基-3,4-二氢吖啶-1(2H)-OH L-2-hydroxybutanedivacate (LHT-17-19) 可以控制表皮生长因子受体的致癌表达。
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来源期刊
Research Results in Pharmacology
Research Results in Pharmacology Medicine-Pharmacology (medical)
CiteScore
1.50
自引率
0.00%
发文量
32
审稿时长
12 weeks
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