Study of liposome encapsulated monoacetate glycolysis inhibitor as an antitumor agent in a Lewis lung carcinoma model


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Abstract

Background. Advances in understanding the molecular mechanisms associated with the Warburg effect have become the basis for the creation of new specific anti-glycolytic agents. Despite their successful preclinical trials, many new anticancer agents based on glycolysis inhibitors have failed in clinical trials, demonstrating systemic toxicity. An effective approach to reducing systemic intoxication is targeted drug delivery using liposomes. However, there are technical difficulties in obtaining liposomes for low molecular weight compounds, which include glycolysis inhibitors, as well as the efficiency of delivery to the tumor due to the peculiarities of liposome biodistribution and pharmacokinetics. Aims. To evaluate the antitumor and antimetastatic effects of a monoiodoacetate glycolysis inhibitor immersed in liposomes. Material and methods. The therapeutic effect of antimetabolite was evaluated in C57BL/6j mice using a Lewis lung carcinoma model. Methotrexate was used as a reference preparation. Liposomes were obtained by extrusion. Ready liposomes were purified from the not included component by dialysis methods. Liposomes were injected through the tail vein. Results. The inhibition of the growth of the primary tumor in iodoacetate in an independent form was comparable with the effect of methotrexate, reaching an average of 15%. Treating with liposomal forms of iodoacetate increased the growth inhibition index to 25%. Inhibition of the growth of lung metastases in iodoacetate and methotrexate was stronger than the effect of drugs on the primary tumor. The averages in these treated groups were 65%. The liposomal form of iodoacetate, in contrast to the similar form of methotrexate, did not significantly inhibit the growth of metastases. Conclusions. Liposomal forms of iodoacetate inhibit the growth of the primary focus more strongly in comparison with their independent action, however, as a result of changes in biodistribution, the antimetastatic effect decreases.

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About the authors

E. E Buyko

Tomsk Polytechnic University

Email: buykoevgen@yandex.ru
Post-graduate Student, Research School of Chemistry and Applied Biomedical Sciences Tomsk

D. A Korshunov

Tomsk National Research Medical Center

Email: ieved@ya.ru
Ph.D. (Med.), Research Scientist, Laboratory of Tumor Biochemistry, Cancer Research Institute Tomsk

I. V Kondakova

Cancer Research Institute of National Research Medical Center

Email: kondakova@oncology.tomsk.ru
Dr.Sc. (Med.), Head of Laboratory of Tumor Biochemistry, Cancer Research Institute Tomsk

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