Effectiveness and safety of carboplatin-containing antitumor therapy regimens in a model of coexistance of lung carcinoma and tuberculosis

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Abstract

Introduction. Treatment of the coexistent pathology of lung cancer and tuberculosis remains the prerogative of experimental research, since the optimal treatment strategy for the coexistence of these two diseases has not yet been developed. The purpose was to study the effectiveness and safety of carboplatin-containing antitumor therapy regimens in combination with anti-tuberculosis chemotherapy.

Material and methods. The study was conducted on 64 C57BL/6 mice aged two months with a previously modeled coexistant pathology of lung carcinoma and tuberculosis. Depending on the therapy, 4 groups were formed: 1 – control without treatment (n=16), 2 – antitumor (carboplatin + paclitaxel) + antituberculosis therapy (n=16), 3 – antitumor (carboplatin + pemetrexed) + antituberculosis therapy (n=16), 4 – antitumor (carboplatin + gemcitabine) + anti-tuberculosis therapy (n=16). The anti-tuberculosis therapy regimen included the administration of isoniazid, rifampicin, pyrazinamide and ethambutol. The antitumor effect (tumor growth index, tumor growth inhibition), antituberculosis effect (CFU per lung weight), toxicity (clinical blood test parameters, biometric indicators of internal organs), and survival were assessed. Statistical processing was carried out using non-parmetric statistics methods.

Results. The lowest average body weight was recorded in group 4 from 7 to 21 days. The greatest differences between groups in the volume of the tumor node were observed from 12 to 16 days of the experiment under the influence of antitumor drugs. At the same time, the greatest inhibition of tumor growth was observed in group 4. On day 9 in group 2 there were signs of the myelo-immunosuppressive effect of antitumor therapy in the form of a decrease in the concentration of leukocytes, lymphocytes and monocytes. In the study groups, there were no statistically significant differences in the survival rate of the experimental and control groups. In all experimental groups, significantly lower spleen MC values were recorded, and in group 4, significantly lower liver MC values were also recorded. The highest level of mycobacterial load was recorded in the control group. The lowest CFU per lung weight was found in the carboplatin and gemcitabine treatment group.

Conclusion. Carboplatin-containing chemotherapy regimens for lung carcinoma in tuberculosis-infected mice have both antitumor and antituberculosis effects. The most pronounced antimycobacterial activity was recorded when using a combination of antituberculosis therapy with carboplatin and gemcitabine.

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About the authors

Grigorii G. Kudriashov

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Healthcare of the Russian Federation

Author for correspondence.
Email: dr.kudriashov.gg@yandex.com

Leading Research Associate, Head of the Department of Pulmonology and Thoracic Surgery

Russian Federation, St. Petersburg

Yuliya G. Zmitrichenko

N.N. Petrov National Medicine Research Center of oncology

Email: zmitrichenko@gmail.com

Research Associate, Scientific Laboratory of Cancer Chemoprophylaxis and Oncopharmacology

Russian Federation, St. Petersburg

Tatiana I. Vinogradova

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Healthcare of the Russian Federation

Email: ti.vinogradova@spbniif.ru

Project Leader, MD, PhD, Dr. Sci. (Med.)

Russian Federation, St. Petersburg

Marine Z. Dogonadze

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Healthcare of the Russian Federation

Email: marine-md@mail.ru

Senior Research Associate, MD, PhD

Russian Federation, St. Petersburg

Natalia V. Zabolotnyh

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Healthcare of the Russian Federation

Email: info@spbniif.ru

Leading Research Associate, MD, PhD, Dr. Sci. (Med.)

Russian Federation, St. Petersburg

Marina E. Dyakova

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Healthcare of the Russian Federation

Email: marinadyakova@yandex.ru

Senior Research Associate, PhD, Dr. Sci.

Russian Federation, St. Petersburg

Dilyara S. Esmedlyaeva

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Healthcare of the Russian Federation

Email: diljara-e@yandex.ru

Senior Research Associate, PhD

Russian Federation, St. Petersburg

Grigorii V. Tochilnikov

N.N. Petrov National Medicine Research Center of oncology

Email: gr75@mail.ru

Head of the Scientific Laboratory of Cancer Chemoprophylaxis and Oncopharmacology, MD, PhD

Russian Federation, St. Petersburg

Andrey O. Nefedov

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Healthcare of the Russian Federation

Email: herurg78@mail.ru

Senior Research Associate, Head of the Department of Thoracic Oncology, MD, PhD

Russian Federation, St. Petersburg

Yulia S. Krylova

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Healthcare of the Russian Federation

Email: emerald2008@mail.ru

Senior Research Associate, Center for Molecular Biomedicine, MD, PhD

Russian Federation, St. Petersburg

Piotr K. Yablonskii

Saint-Petersburg State Research Institute of Phthisiopulmonology of the Ministry of Healthcare of the Russian Federation; Federal State Budgetary Educational Institution of Higher Education «Saint-Petersburg State University»

Email: glhirurgb2@mail.ru

Director, MD, PhD, Dr. Sci. (Med.), professor

Russian Federation, St. Petersburg; St. Petersburg

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Supplementary files

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2. Fig. 1. Median body weight of animals in the experiment

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3. Fig. 2. Survival rate of C57BL/6 mice in the study groups

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4. Fig. 3. Mass coefficients (MC) of organs in the studied groups

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5. Fig. 4. CFU per lung weight in study groups

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