Bacteria‐derived ferrichrome inhibits tumor progression in sporadic colorectal neoplasms and colitis‐associated cancer

Author:

Iwama Takuya,Fujiya MikihiroORCID,Konishi Hiroaki,Tanaka Hiroki,Murakami Yuki,Kunogi Takehito,Sasaki Takahiro,Takahashi Keitaro,Ando Katsuyoshi,Ueno Nobuhiro,Kashima Shin,Moriichi Kentaro,Tanabe Hiroki,Okumura Toshikatsu

Abstract

Abstract Background Colorectal cancers develop through several pathways, including the adenoma–carcinoma sequence and colitis-associated carcinogenesis. An altered intestinal microflora has been reported to be associated with the development and progression of colorectal cancer via these pathways. We identified Lactobacillus casei-derived ferrichrome as a mediator of the bacterial anti-tumor effect of colorectal cancer cells through the upregulation of DDIT3. In this study, we investigated the anti-tumor effects of ferrichrome on precancerous conditions and cancer cells associated with sporadic as well as colitis-associated colorectal cancer. Methods SRB and MTT assays were performed to assess growth inhibition in vitro. Eighteen organoids were prepared from biopsy specimens obtained by colonoscopy. An AOM-DSS carcinogenesis model and xenograft model of colorectal cancer cells were generated for the assessment of the tumor suppressive effect of ferrichrome in vivo. Results Ferrichrome inhibited the cell growth of colorectal cancer cells in vitro and in in vivo xenograft models. Ferrichrome exerted a strong tumor-suppressive effect that was superior to that of currently available anti-tumor agents, including 5-FU and cisplatin, both in vitro and in vivo. The tumor-suppressive effect of the combination of ferrichrome and 5-FU was superior to that of single treatment with either drug. The tumor suppressive effects of ferrichrome were confirmed through the upregulation of DDIT3 in patient-derived organoids of adenoma and carcinoma. Ferrichrome inhibited the tumor progression in the AOM-DSS model while exhibiting no anti-inflammatory effect in the DSS-colitis model, suggesting that ferrichrome inhibited cancer cells, but not a precancerous condition, via the colitis-associated pathway. Conclusions Ferrichrome exerts a tumor suppressive effect on precancerous conditions and cancer cells associated with sporadic as well as colitis-associated colorectal cancer. The anti-tumor effect of ferrichrome was mediated by the upregulation of DDIT3, and was superior to that of 5-FU or cisplatin. These results suggest that Lactobacillus brevis-derived ferrichrome may be a candidate anti-tumor drug for the treatment of colorectal neoplasms.

Funder

Yakult Honsha

EA Pharma Co., Ltd.

Nippon Kayaku Co., Ltd

Novartis Pharmaceuticals Corporation

Boehringer Ingelheim

Technical Informaition Insititute Co., Ltd

Pfizer Japan

Takeda Pharmaceutical Company

Daiichi-Sankyo

Shionogi

Olympus

Janssen Pharmaceuticals

KYORIN Pharmaceutical Co., Ltd.

Taisho Toyama Pharmaceutical Company

AstraZeneca

Tomakomai Minpo Co.,Ltd

Meiji Seika Pharma

Mochida Pharmaceutical Company

Astellas Pharma

Mitsubishi Tanabe Pharma Corporation

Baxter International

Bristol-Myers Squibb

Chugai Pharmaceutical

MSD K.K.

Otsuka Pharmaceutical

Kyowa Hakko Kirin

Taiho Pharmaceutical

ZERIA Pharmaceutical Co.,Ltd.

Alexion Pharmaceuticals

Ajinomoto Pharmaceuticals

Asahi Kasei Pharma Corporation

Sapporo Breweries LTD

Eisai

GlaxoSmithKline

AbbVie

Dainippon Sumitomo Pharma

ASKA Pharmaceutical Co., Ltd.

Boston Scientific Corporation

Kamui Pharma. Inc

Japanese Grants-in-Aid for Scientific Research

Development and Intractable Disease Health and Labour Sciences Research Grants from the Ministry of Health, Labour and Welfare

a patent Intestinal Protectant

Translational Research Network Program of Japan Agency for Medical Research and Development

Takeda Science Foundation

Publisher

Springer Science and Business Media LLC

Subject

Cancer Research,Genetics,Oncology

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