Study of biological activity of 2-quinoline-2-yl-derivative 1,3-tropolone in experiment

E. Lukbanova, E. Dzhenkova, A. Goncharova, A. Maksimov, E. F. Komarova, V. Minkin, Y. A. Sayapin, E. A. Gusakov, L. Z. Kurbanova, A. Kiblitskaya, E. Zaikina, M. V. Mindar, M. V. Voloshin, A. Shaposhnikov, I. Lysenko, N. Nikolaeva
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Abstract

Purpose of the study. Was to reveal the antitumor effect of 2‑(6,8‑dimethyl‑5‑nitro‑4‑chloroquinoline‑2‑yl)‑5,6,7‑trichloro‑1,3‑tropolone in subcutaneous PDX models of human lung cancer.Material and methods. The studied tropolone was synthesized using a method of expanding the o‑quinone cycle. Assess to it’s toxic effects was given by the survival and changes in the health status of female Balb/c Nude mice. Antitumor tropolone effects were studied in subcutaneous patient‑derived xenograft (PDX) models of human squamous cell lung cancer in Balb/c Nude mice. The average volumes of tumor nodes and tumor growth inhibition (TGI %) rate were taken into account. Biochemical blood tests and histological analysis of the tumor material were performed in recipient mice.Results. An analysis of acute tropolone toxic effects did not reveal the lethal dose. The maximal TGI was observed on day 36 of the experiment in group 5 which have received 2.75 mg/g tropolone and accounted 73.5 % for females and 74.4 % for males. The average tumor volumes in females of this group were 431.3 ± 1,1 mm3 on day 33 of the experiment, in males – 428.9 ± 1,7 mm3 on day 30, and then the tumor volumes declined. The biochemical analysis of blood and histological examination of the tumor tissue of recipient mice reflect the severity of the antitumor effect on the dose of the studied tropolone.Conclusion. The research demonstrated the antitumor activity of 2‑(6,8‑dimethyl‑5‑nitro‑4‑chloroquinoline‑2‑yl)‑5,6,7‑trichloro‑1,3‑tropolone against subcutaneous PDX models of human NSCLC. The revealed tendencies can be used to search for effective modes of the compound application in clinical practice.
2-喹啉-2-酰基衍生物1,3-tropolone生物活性的实验研究
研究目的:目的探讨2 -(6,8 -二甲基- 5 -硝基- 4 -氯喹啉- 2 -基)- 5,6,7 -三氯- 1,3 - tropolone对人肺癌PDX皮下模型的抗肿瘤作用。材料和方法。采用扩大邻醌循环的方法合成了所研究的tropolone。通过雌性Balb/c裸鼠的生存和健康状况的变化来评价其毒性作用。在Balb/c裸鼠人鳞状细胞肺癌皮下患者源异种移植(PDX)模型中研究了tropolone的抗肿瘤作用。考虑肿瘤淋巴结的平均体积和肿瘤生长抑制率(TGI %)。对受体小鼠进行血液生化检查和肿瘤材料的组织学分析。急性tropolone毒性作用分析没有显示致死剂量。试验第36天,注射2.75 mg/g tropolone的第5组TGI达到最大值,雌性占73.5%,雄性占74.4%。实验第33天,实验组女性平均肿瘤体积为431.3±1.1 mm3,第30天,实验组男性平均肿瘤体积为- 428.9±1.7 mm3,之后肿瘤体积逐渐下降。受体小鼠血液生化分析和肿瘤组织组织学检查反映了所研究的tropolone剂量对抗肿瘤作用的严重程度。该研究证实了2 -(6,8 -二甲基- 5 -硝基- 4 -氯喹啉- 2 -基)- 5,6,7 -三氯- 1,3 - tropolone对人NSCLC皮下PDX模型的抗肿瘤活性。揭示的趋势可用于寻找该化合物在临床应用的有效模式。
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