Pre‐clinical evidences for the efficacy of tryptanthrin as a potent suppressor of skin cancer

Author:

Shankar G. Mohan12,Alex Vijai V.1,Nisthul A. Amrutha3,Bava Smitha V.4,Sundaram Sankar5,Retnakumari Archana P.1,Chittalakkottu Sadasivan3,Anto Ruby John1ORCID

Affiliation:

1. Division of Cancer Research Rajiv Gandhi Centre for Biotechnology Thiruvananthapuram Kerala India

2. Research Scholar Manipal Academy of Higher Education Manipal Karnataka India

3. Department of Biotechnology and Microbiology Kannur University Kannur Kerala India

4. Department of Biotechnology University of Calicut Calicut Kerala India

5. Department of Pathology Government Medical College Kottayam Kerala India

Abstract

AbstractObjectiveClinical trials have demonstrated the efficacy of indigo naturalis, a traditional Chinese medicine ingredient, against psoriasis, a skin disease characterized by keratinocyte hyperproliferation and inflammation. The present study investigates the efficacy of tryptanthrin, a bioactive compound in indigo naturalis, against non‐melanoma skin cancer (NMSC) and the signalling events involved.MethodsEfficacy of tryptanthrin against NMSC was assessed using DMBA/PMA‐induced skin carcinogenesis model in Swiss albino mice. Immunostaining for PCNA and ki‐67 was used to mark proliferating cells in tissues. Haematoxylin and eosin staining and toluidine staining were employed to assess inflammation, and TUNEL assay was used to detect apoptosis in tissues. The signalling events were evaluated using Western blot, imunohistochemistry and immunofluorescence staining. MTT assay and clonogenic assay were performed to assess the viability and proliferation of cancer cells, in vitro.ResultsIn mice, topical application of tryptanthrin suppressed skin carcinogenesis. It attenuated inflammation, impeded the proliferation of hair follicle (HF) cells and suppressed the activation of β‐catenin, a major driver of HF cell proliferation. Additionally tryptanthrin suppressed the activation of ERK1/2 and p38, both of which promote β‐catenin activation and lowered the expression of c‐Myc and cyclin‐D1. Tryptanthrin suppressed the proliferation of the human NMSC cell line, A431 and abrogated EGF‐induced activation of β‐catenin and subsequent cytoskeletal rearrangement.ConclusionThe study demonstrates with molecular evidence that tryptanthrin is an effective suppressor of NMSC.

Funder

Department of Biotechnology, Ministry of Science and Technology, India

Indian Council of Medical Research

Publisher

Wiley

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