Cytotoxic and cytostatic activity of five new imidazotetrazine derivatives on breast cancer cell cultures MDAMB231, BT474, and MCF-7

Авторы

DOI:

https://doi.org/10.18413/rrpharmacology.10.479

Аннотация

Introduction: The work presents the results of the study of new imidazotetrazine derivatives to establish the possibility of using them as anticancer agents, including for chemotherapy of metastatic breast cancer. The relevance of the work is due to the wide spread of oncological diseases and high cancer mortality, which dictates the need to constantly obtain cell lines and improve cultivation protocols for testing new antitumor drugs. The goal of this study is to check the potential of five new imidazotetrazine derivatives to become new antitumor drugs, in the scope of studying their cytotoxic and cytostatic activities on breast cancer cell cultures.

Materials and Methods: The culturing MCF-7, MDAMB231, BT474, and MCF-10a cells with determining cytotoxic and cytostatic activities of five new azolotetrazine derivatives are base methods used in this study.

Results: For the MCF-7 culture, MCS of comparison drug temozolomide was equal to 2.44 and IC50 was 6.81 mM/L; for other cultures CTA indicators were worse. Imidazotetrazine 2 and imidazotetrazine 3 demonstrated CTA indicators lower than those of temozolomide. IC50 was not achieved, and the MCS value varied between 1.34 and 1.74. These two derivatives were classified as the compounds with an extremely low CTA. Imidazotetrazine 1 and iminothiotriazine 5 showed cytotoxic activity higher than that of the comparison drug and we classified these compounds as the ones with a moderate CTA. Finally, we found imidazotetrazine 4 with IC50 of 0.85 mM/L and CTA of 7.34 as a compound with a potentially strong anticancer effect for further investigation. The cytostatic activity of four of the five azoloazine derivatives studied was in a narrow range corresponding to the survival rate from 0.21 to 0.32, depending on the compound and cell culture. Against this background, imidazotetrazine 4 demonstrated a higher CSA, determined by the survival rate from 0.17 to 0.20.

Conclusion: As a result of an in vitro study, we found that five new azolotriazine derivatives can be evaluated in the ascending order of these properties, as a combination of CTA+CSA in order imidazotetrazine 2, imidazotetrazine 3 < temozolomide < imidazotetrazine 1, iminothiotriazine 5 < imidazotetrazine 4, although the CSA of all the studied compounds turned out to be high. Thus, 3-Cyclohexyl-4-oxoimidazo[5,1-d]-[1,2,3,5]tetrazine-8-N-piperidinyl-carboxamide (imidazotetrazine 4) is an unconditional leader in the tested series of new azoloazine derivatives and we recommend it for further preclinical trials.

Графическая аннотация

Ключевые слова:

breast cancer, imidazotetrazine, cytotoxic activity, cytostatic activity, MCF-7 cell line, MDAMB231 cell line, BT474 cell line, MCF-10a cell line

Библиографические ссылки

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Вклад авторов

Ahmed Hamid Al-Humairi, Volgograd State Medical University

PhD (Pharmacology, Clinical Pharmacology and Oncology, radiation therapy), Lecturer, Department of Disaster Medicine, Volgograd State Medical University of the Ministry of Health of the Russian Federation, Volgograd, Russia; Researcher, Laboratory of Physiology, Molecular and Clinical Pharmacology, Research institute of Pharmacology and Regenerative Medicine named after E.D. Goldberg, Tomsk National Research Medical Center of the Russian Academy of Sciences, Tomsk, Russia; e-mail: ahmed.h.mneahil@gmail.com; ORCID ID https://orcid.org/0000-0001-7545-8567. The author proposed the basic concept, hypothesis of the study and developed its design, performed experiments and collected data, analyzed and interpreted results and edited the text of the article.

Svetlana E. Sitnikova, Volgograd State Medical University

PhD (Economics), Associate Professor, Department of Economics and Management, Institute of Public Health, Volgograd State Medical University of the Ministry of Health of the Russian Federation, Volgograd, Russia; e-mail: sesitnikova@volgmed.ru; ORCID ID https://orcid.org/0000-0002-1394-0734. The author conducted statistical analysis and prepared the draft manuscript.

Valery V Novochadov, Volgograd State University

Doctor Habil. of Sciences (Medicine), Professor, Department of Biology and Bioengineering, Volgograd State University, Volgograd, Russia; e-mail: novochadov.valeriy@volsu.ru; ORCID ID https://orcid.org/0000-0001-6317-7418. The author supervised and managed the study, proposed the basic concept, hypothesis of the study and developed its design, reviewed the results and approved the final version to be published.

Опубликован

09.09.2024

Как цитировать

Al-Humairi AH, Sitnikova SE, Novochadov VV (2024) Cytotoxic and cytostatic activity of five new imidazotetrazine derivatives on breast cancer cell cultures MDAMB231, BT474, and MCF-7. Research Results in Pharmacology 10(3): 33–42. https://doi.org/10.18413/rrpharmacology.10.479

Выпуск

Раздел

Экспериментальная фармакология