Chronometric Administration of Cyclophosphamide and a Double-Stranded DNA-Mix at Interstrand Crosslinks Repair Timing, Called “Karanahan” Therapy, Is Highly Efficient in a Weakly Immunogenic Lewis Carcinoma Model

Background and Aims: A new technology based on the chronometric administration of cyclophosphamide and complex composite double-stranded DNA-based compound, which is scheduled in strict dependence on interstrand crosslinks repair timing, and named “Karanahan”, has been developed. Being applied, this...

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Autores principales: Ruzanova, Vera, Proskurina, Anastasia, Efremov, Yaroslav, Kirikovich, Svetlana, Ritter, Genrikh, Levites, Evgenii, Dolgova, Evgenia, Potter, Ekaterina, Babaeva, Oksana, Sidorov, Sergey, Taranov, Oleg, Ostanin, Alexandr, Chernykh, Elena, Bogachev, Sergey
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2022
Materias:
Pathology and Oncology Archive
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9185167/
https://www.ncbi.nlm.nih.gov/pubmed/35693632
http://dx.doi.org/10.3389/pore.2022.1610180
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author Ruzanova, Vera
Proskurina, Anastasia
Efremov, Yaroslav
Kirikovich, Svetlana
Ritter, Genrikh
Levites, Evgenii
Dolgova, Evgenia
Potter, Ekaterina
Babaeva, Oksana
Sidorov, Sergey
Taranov, Oleg
Ostanin, Alexandr
Chernykh, Elena
Bogachev, Sergey
author_facet Ruzanova, Vera
Proskurina, Anastasia
Efremov, Yaroslav
Kirikovich, Svetlana
Ritter, Genrikh
Levites, Evgenii
Dolgova, Evgenia
Potter, Ekaterina
Babaeva, Oksana
Sidorov, Sergey
Taranov, Oleg
Ostanin, Alexandr
Chernykh, Elena
Bogachev, Sergey
author_sort Ruzanova, Vera
collection PubMed
description Background and Aims: A new technology based on the chronometric administration of cyclophosphamide and complex composite double-stranded DNA-based compound, which is scheduled in strict dependence on interstrand crosslinks repair timing, and named “Karanahan”, has been developed. Being applied, this technology results in the eradication of tumor-initiating stem cells and full-scale apoptosis of committed tumor cells. In the present study, the efficacy of this novel approach has been estimated in the model of Lewis carcinoma. Methods: To determine the basic indicative parameters for the approach, the duration of DNA repair in tumor cells, as well as their distribution along the cell cycle, have been assessed. Injections were done into one or both tumors in femoral region of the engrafted mice in accordance with the developed regimen. Four series of experiments were carried out at different periods of time. The content of poorly differentiated CD34(+)/TAMRA+ cells in the bone marrow and peripheral blood has been determined. Immunostaining followed by the flow cytometry was used to analyze the subpopulations of immune cells. Results: The high antitumor efficacy of the new technology against the developed experimental Lewis carcinoma was shown. It was found that the therapy efficacy depended on the number of tumor growth sites, seasonal and annual peculiarities. In some experiments, a long-term remission has been reached in 70% of animals with a single tumor and in 60% with two tumors. In mice with two developed grafts, mobilization capabilities of both poorly differentiated hematopoietic cells of the host and tumor stem-like cells decrease significantly. Being applied, this new technology was shown to activate a specific immune response. There is an increase in the number of NK cell populations in the blood, tumor, and spleen, killer T cells and T helper cells in the tumor and spleen, CD11b+Ly-6C+ and CD11b+Ly-6G+ cells in the tumor. A population of mature dendritic cells is found in the tumor. Conclusion: The performed experiments indicate the efficacy of the Karanahan approach against incurable Lewis carcinoma. Thus, the discussed therapy is a new approach for treating experimental neoplasms, which has a potential as a personalized anti-tumor therapeutic approach in humans.
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spelling pubmed-91851672022-06-11 Chronometric Administration of Cyclophosphamide and a Double-Stranded DNA-Mix at Interstrand Crosslinks Repair Timing, Called “Karanahan” Therapy, Is Highly Efficient in a Weakly Immunogenic Lewis Carcinoma Model Ruzanova, Vera Proskurina, Anastasia Efremov, Yaroslav Kirikovich, Svetlana Ritter, Genrikh Levites, Evgenii Dolgova, Evgenia Potter, Ekaterina Babaeva, Oksana Sidorov, Sergey Taranov, Oleg Ostanin, Alexandr Chernykh, Elena Bogachev, Sergey Pathol Oncol Res Pathology and Oncology Archive Background and Aims: A new technology based on the chronometric administration of cyclophosphamide and complex composite double-stranded DNA-based compound, which is scheduled in strict dependence on interstrand crosslinks repair timing, and named “Karanahan”, has been developed. Being applied, this technology results in the eradication of tumor-initiating stem cells and full-scale apoptosis of committed tumor cells. In the present study, the efficacy of this novel approach has been estimated in the model of Lewis carcinoma. Methods: To determine the basic indicative parameters for the approach, the duration of DNA repair in tumor cells, as well as their distribution along the cell cycle, have been assessed. Injections were done into one or both tumors in femoral region of the engrafted mice in accordance with the developed regimen. Four series of experiments were carried out at different periods of time. The content of poorly differentiated CD34(+)/TAMRA+ cells in the bone marrow and peripheral blood has been determined. Immunostaining followed by the flow cytometry was used to analyze the subpopulations of immune cells. Results: The high antitumor efficacy of the new technology against the developed experimental Lewis carcinoma was shown. It was found that the therapy efficacy depended on the number of tumor growth sites, seasonal and annual peculiarities. In some experiments, a long-term remission has been reached in 70% of animals with a single tumor and in 60% with two tumors. In mice with two developed grafts, mobilization capabilities of both poorly differentiated hematopoietic cells of the host and tumor stem-like cells decrease significantly. Being applied, this new technology was shown to activate a specific immune response. There is an increase in the number of NK cell populations in the blood, tumor, and spleen, killer T cells and T helper cells in the tumor and spleen, CD11b+Ly-6C+ and CD11b+Ly-6G+ cells in the tumor. A population of mature dendritic cells is found in the tumor. Conclusion: The performed experiments indicate the efficacy of the Karanahan approach against incurable Lewis carcinoma. Thus, the discussed therapy is a new approach for treating experimental neoplasms, which has a potential as a personalized anti-tumor therapeutic approach in humans. Frontiers Media S.A. 2022-05-27 /pmc/articles/PMC9185167/ /pubmed/35693632 http://dx.doi.org/10.3389/pore.2022.1610180 Text en Copyright © 2022 Ruzanova, Proskurina, Efremov, Kirikovich, Ritter, Levites, Dolgova, Potter, Babaeva, Sidorov, Taranov, Ostanin, Chernykh and Bogachev. https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Pathology and Oncology Archive
Ruzanova, Vera
Proskurina, Anastasia
Efremov, Yaroslav
Kirikovich, Svetlana
Ritter, Genrikh
Levites, Evgenii
Dolgova, Evgenia
Potter, Ekaterina
Babaeva, Oksana
Sidorov, Sergey
Taranov, Oleg
Ostanin, Alexandr
Chernykh, Elena
Bogachev, Sergey
Chronometric Administration of Cyclophosphamide and a Double-Stranded DNA-Mix at Interstrand Crosslinks Repair Timing, Called “Karanahan” Therapy, Is Highly Efficient in a Weakly Immunogenic Lewis Carcinoma Model
title Chronometric Administration of Cyclophosphamide and a Double-Stranded DNA-Mix at Interstrand Crosslinks Repair Timing, Called “Karanahan” Therapy, Is Highly Efficient in a Weakly Immunogenic Lewis Carcinoma Model
title_full Chronometric Administration of Cyclophosphamide and a Double-Stranded DNA-Mix at Interstrand Crosslinks Repair Timing, Called “Karanahan” Therapy, Is Highly Efficient in a Weakly Immunogenic Lewis Carcinoma Model
title_fullStr Chronometric Administration of Cyclophosphamide and a Double-Stranded DNA-Mix at Interstrand Crosslinks Repair Timing, Called “Karanahan” Therapy, Is Highly Efficient in a Weakly Immunogenic Lewis Carcinoma Model
title_full_unstemmed Chronometric Administration of Cyclophosphamide and a Double-Stranded DNA-Mix at Interstrand Crosslinks Repair Timing, Called “Karanahan” Therapy, Is Highly Efficient in a Weakly Immunogenic Lewis Carcinoma Model
title_short Chronometric Administration of Cyclophosphamide and a Double-Stranded DNA-Mix at Interstrand Crosslinks Repair Timing, Called “Karanahan” Therapy, Is Highly Efficient in a Weakly Immunogenic Lewis Carcinoma Model
title_sort chronometric administration of cyclophosphamide and a double-stranded dna-mix at interstrand crosslinks repair timing, called “karanahan” therapy, is highly efficient in a weakly immunogenic lewis carcinoma model
topic Pathology and Oncology Archive
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC9185167/
https://www.ncbi.nlm.nih.gov/pubmed/35693632
http://dx.doi.org/10.3389/pore.2022.1610180
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