3.8 Article

Comparative Pre-clinical Efficacy of Chinese and Indian Cultivars of Bitter Melon (Momordica charantia) against Pancreatic Cancer

Journal

JOURNAL OF CANCER PREVENTION
Volume 26, Issue 4, Pages 266-276

Publisher

KOREAN SOC CANCER PREVENTION
DOI: 10.15430/JCP.2021.26.4.266

Keywords

Pancreatic neoplasms; Bitter melon; Apoptosis; Angiogenesis; Natural/dietary agents

Categories

Funding

  1. National Institutes of Health/National Cancer Institute [R01CA195708]
  2. National Institutes of Health Office of Dietary Supplements [R01CA195708-02S1]
  3. office of the Associate Dean for Research and Graduate Education (ADR), School of Pharmacy, UC AMC

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Comparative pre-clinical studies showed that Chinese and Indian bitter melon varieties exhibit comparable efficacy in inhibiting pancreatic cancer cell proliferation, inducing cell death, suppressing tumor growth, and decreasing angiogenesis. The geographical availability of a particular cultivar should not be a limiting factor in selecting a variant for clinical trials.
Given the high rates of incidence and mortality associated with pancreatic cancer (PanC), there is a need to develop alternative strategies to target PanC. Recent studies have demonstrated that fruits of bitter melon (Momordica charantia) exhibit strong anticancer efficacy against PanC. However, the comparative effects of different bitter melon varieties have not been investigated. This has important implications, given that several bitter melon cultivars are geographically available but their differential effects are not known; and that on a global level, individuals could consume different bitter melon varieties sourced from different cultivars for anti-PanC benefits. Considering these shortcomings, in the present study, comparative pre-clinical anti-PanC studies have been conducted using lyophilized-juice and aqueous-methanolic extracts of the two most widely consumed but geographically diverse bitter melon varieties (Chinese [bitter melon juice; BMJ] and Indian [bitter melon extract; BME] variants). We observed that both BMJ and BME possess comparable efficacy against PanC growth and progression; specifically, these preparations have the potential to (a) inhibit PanC cell proliferation and induce cell death; (b) suppress PanC tumor growth, proliferation, and induce apoptosis; (c) restrict capillary tube formation by human umbilical vein endothelial cells, and decrease angiogenesis in PanC tumor xenografts. Thus, given the comparable pre-clinical anti-PanC efficacy of bitter melon cultivars, the geographical non-availability of a certain cultivar should not be a limiting factor in selecting a variant for moving forward for future clinical use/clinical trials either as a preventive or a therapeutic alternative for targeting PanC.

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