Scientific validation and mechanistic evaluation of chuntaivatral chooranam in DMH-induced gastrointestinal cancer: An in vivo study

Antitumor efficacy of Chuntaivatral chooranam on lipid peroxidation in control and Experimental animals

Authors

  • Muninathan Natarajan Associate Professor and Scientist
  • Vadivel Mani Assistant Professor, Department of Biochemistry, Konaseema Institute of Medical Sciences and Research Foundation, Amalapuram, East Godavari - 533201, Andhra Pradesh, India.
  • Beula Christina W Phd Scholar
  • Poongkuzhali S Phd Scholar
  • Arumugam Suresh Scientist
  • Priyanka G Assistant Professor

DOI:

https://doi.org/10.56042/ijtk.v25i6.24114

Keywords:

Chemoprotection, Chuntai vatral chooranam, Colon cancer, Di methyl hydrazine, Oxidative stress markers, Phase I enzymes

Abstract

Colorectal cancer is one of the leading causes of cancer-related morbidity and mortality worldwide, ranking third among males and second among females in industrialized countries. Its incidence is also rapidly increasing in developing nations, including India, largely due to changing dietary habits and lifestyle factors. 1,2-Dimethylhydrazine (DMH), a potent alkylating agent, is widely used to induce experimental colon carcinogensis. Chuntaivatral chooranam (CVC), a traditional Siddha polyherbal formulation, is commonly prescribed for gastrointestinal disorders such as piles, indigestion, and irritable bowel syndrome. However, its potential anticancer properties remain largely unexplored. The present study aimed to evaluate the chemopreventive efficacy of Chuntaivatral chooranam against DMH-induced colon cancer in Wistar rats.A total of 42 male Wistar rats were divided into nine groups, each consisting of six animals. Colon carcinogenesis was induced using DMH, and treatment groups received Chuntaivatral chooranam at different doses, either alone or in combination with 5-Fluorouracil. At the end of the experimental period, animals were sacrificed, and blood and tissue samples were collected for biochemical and molecular analyses. The results demonstrated that DMH administration significantly increased oxidative stress markers, tumor markers, and Phase I enzyme activities while decreasing antioxidant enzyme levels and membrane-bound ATPase activities. Treatment with Chuntaivatral chooranam, particularly in combination with 5-Fluorouracil, significantly reversed these alterations (p<0.001), reduced tumor incidence, and improved biochemical parameters. In conclusion, Chuntaivatral chooranam exhibited significant chemoprotective and antitumor activity against DMH-induced colon cancer, suggesting its potential as a complementary therapeutic agent in the management of colorectal cancer.

Author Biographies

  • Muninathan Natarajan, Associate Professor and Scientist

    Central Research Laboratory, Meenakshi Medical College Hospital and Research Institute, Meenakshi Academy of Higher Education and Research, Kanchipuram, Tamil Nadu, India.

  • Beula Christina W, Phd Scholar

     Central Research Laboratory, Meenakshi Medical College Hospital and Research Institute, Meenakshi Academy of Higher Education and Research, Kanchipuram, Tamil Nadu, India.

  • Poongkuzhali S, Phd Scholar

    Central Research Laboratory, Meenakshi Medical College Hospital and Research Institute, Meenakshi Academy of Higher Education and Research, Kanchipuram, Tamil Nadu, India.

  • Arumugam Suresh, Scientist

    Central Research Laboratory, Meenakshi Medical College Hospital and Research Institute, Meenakshi Academy of Higher Education and Research, Kanchipuram, Tamil Nadu, India.

  • Priyanka G, Assistant Professor

    Department of Physiology, Sree Balaji Medical College and Hospital, Chromepet, Chennai -600044, Tamil Nadu, India

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Published

2026-06-25

How to Cite

Scientific validation and mechanistic evaluation of chuntaivatral chooranam in DMH-induced gastrointestinal cancer: An in vivo study: Antitumor efficacy of Chuntaivatral chooranam on lipid peroxidation in control and Experimental animals. (2026). Indian Journal of Traditional Knowledge (IJTK), 25(6), 557-565. https://doi.org/10.56042/ijtk.v25i6.24114

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