Abstract

Ovarian and pancreatic cancers are two of the most aggressive and lethal cancers, whose management faces only limited therapeutic options. Typically, these tumors spread insidiously accompanied first with atypical symptoms, and usually shift to a drug resistance phenotype with the current pharmaceutical armamentarium. Thus, the development of new drugs acting via a different mechanism of action represents a clear priority. Herein, we are reporting for the first time that the aminosteroid derivative RM-133, developed in our laboratory, displays promising activity on two models of aggressive cancers, namely ovarian (OVCAR-3) and pancreatic (PANC-1) cancers. The IC50 value of RM-133 was 0.8 μM and 0.3 μM for OVCAR-3 and PANC-1 cell lines in culture, respectively. Based on pharmacokinetic studies on RM-133 using 11 different vehicles, we selected two main vehicles: aqueous 0.4% methylcellulose:ethanol (92:8) and sunflower oil:ethanol (92:8) for in vivo studies. Using subcutaneous injection of RM-133 with the methylcellulose-based vehicle, growth of PANC-1 tumors xenografted to nude mice was inhibited by 63%. Quite interestingly, RM-133 injected subcutaneously with the methylcellulose-based or sunflower-based vehicles reduced OVCAR-3 xenograft growth by 122% and 100%, respectively. After the end of RM-133 treatment using the methylcellulose-based vehicle, OVCAR-3 tumor growth inhibition was maintained for ≥ 1 week. RM-133 was also well tolerated in the whole animal, no apparent sign of toxicity having been detected in the xenograft studies.

Highlights

  • As a major public health concern worldwide, cancer is responsible for one in four deaths in the USA and Canada [1,2]

  • We report pharmacokinetic studies on RM-133 involving various vehicles, as well as its antitumor activity in models of ovarian and pancreatic cancers, namely the OVCAR-3 and PANC-1 tumors xenografted into nude mice

  • To evaluate the effect of RM-133 on the proliferation of OVCAR-3 and PANC-1 cancer cells, the latter were incubated with increasing concentrations of RM-133 for 72 h, and the IC50 of the drug measured

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Summary

Introduction

As a major public health concern worldwide, cancer is responsible for one in four deaths in the USA and Canada [1,2]. Ovarian cancer is a heterogeneous disease that afflicts yearly 225,000 women worldwide [3,4,5]. It is the most lethal among the gynecologic malignancies, due to its asymptomatic nature in its early etiology, and the lack of efficient diagnostic tools [2,5]. 75% of women already present themselves with advanced stages of ovarian cancer (stages III- IV of the International Federation of Gynecology and Obstetrics classification).

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