Inhibition of autophagy exerts anti-colon cancer effects via apoptosis induced by p53 activation and ER stress

Kosuke Sakitani; Yoshihiro Hirata; Yohko Hikiba; Yoku Hayakawa; Sozaburo Ihara; Hirobumi Suzuki; Nobumi Suzuki; Takako Serizawa; Hiroto Kinoshita; Kei Sakamoto; Hayato Nakagawa; Keisuke Tateishi; Shin Maeda; Tsuneo Ikenoue; Shoji Kawazu; Kazuhiko Koike

doi:10.1186/s12885-015-1789-5

Inhibition of autophagy exerts anti-colon cancer effects via apoptosis induced by p53 activation and ER stress

BMC Cancer. 2015 Oct 24:15:795. doi: 10.1186/s12885-015-1789-5.

Authors

Kosuke Sakitani^{1

2}, Yoshihiro Hirata³, Yohko Hikiba⁴, Yoku Hayakawa⁵, Sozaburo Ihara⁶, Hirobumi Suzuki⁷, Nobumi Suzuki⁸, Takako Serizawa⁹, Hiroto Kinoshita¹⁰, Kei Sakamoto¹¹, Hayato Nakagawa¹², Keisuke Tateishi¹³, Shin Maeda¹⁴, Tsuneo Ikenoue¹⁵, Shoji Kawazu¹⁶, Kazuhiko Koike¹⁷

Affiliations

¹ The Institute for Adult Diseases, Asahi Life Foundation, 2-2-6 Bakuro-cho, Nihon-Bashi, Chuo-ku, Tokyo, 113-8655, Japan. sakitani-tky@umin.ac.jp.
² Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. sakitani-tky@umin.ac.jp.
³ Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. hiratay-int@h.u-tokyo.ac.jp.
⁴ The Institute for Adult Diseases, Asahi Life Foundation, 2-2-6 Bakuro-cho, Nihon-Bashi, Chuo-ku, Tokyo, 113-8655, Japan. y.hikiba@gmail.com.
⁵ Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. hayakawayoku@gmail.com.
⁶ Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. sihara-tky@umin.ac.jp.
⁷ Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. suzuhiro817@yahoo.co.jp.
⁸ Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. s_nobu3wall@yahoo.co.jp.
⁹ Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. st8039-fki@umin.ac.jp.
¹⁰ Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. kinosita.hiroto@gmail.com.
¹¹ The Institute for Adult Diseases, Asahi Life Foundation, 2-2-6 Bakuro-cho, Nihon-Bashi, Chuo-ku, Tokyo, 113-8655, Japan. ksakamoto.spvir@gmail.com.
¹² Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. hayaton0120@gmail.com.
¹³ Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. ktate-tky@umin.ac.jp.
¹⁴ Gastroenterology Division, Yokohama City University Graduate School of Medicine, Yokohama, Japan. smaeda@yokohama-cu.ac.jp.
¹⁵ Division of Clinical Genome Research, The Institute of Medical Science, The University of Tokyo, Tokyo, Japan. tikenoue@hotmail.com.
¹⁶ The Institute for Adult Diseases, Asahi Life Foundation, 2-2-6 Bakuro-cho, Nihon-Bashi, Chuo-ku, Tokyo, 113-8655, Japan. skawa@asahi-life.or.jp.
¹⁷ Department of Gastroenterology, Graduate School of Medicine, The University of Tokyo, Tokyo, Japan. kkoike-tky@umin.ac.jp.

Abstract

Background: Although some molecularly targeted drugs for colorectal cancer are used clinically and contribute to a better prognosis, the current median survival of advanced colorectal cancer patients is not sufficient. Autophagy, a basic cell survival mechanism mediated by recycling of cellular amino acids, plays an important role in cancer. Recently, autophagy has been highlighted as a promising new molecular target. The unfolded protein response (UPR) reportedly act in complementary fashion with autophagy in intestinal homeostasis. However, the roles of UPR in colon cancer under autophagic inhibition remain to be elucidated. We aim to clarify the inhibitory effect of autophagy on colon cancer.

Methods: We crossed K19 (CreERT) and Atg5 (flox/flox) mice to generate Atg5 (flox/flox)/K19 (CreERT) mice. Atg5 (flox/flox)/K19 (CreERT) mice were first treated with azoxymethane/dextran sodium sulfate and then injected with tamoxifen to inhibit autophagy in CK19-positive epithelial cells. To examine the anti-cancer mechanisms of autophagic inhibition, we used colon cancer cell lines harboring different p53 gene statuses, as well as small interfering RNAs (siRNAs) targeting Atg5 and immunoglobulin heavy-chain binding protein (BiP), a chaperone to aid folding of unfolded proteins.

Results: Colon tumors in Atg5 (flox/flox)/K19 (CreERT) mice showed loss of autophagic activity and decreased tumor size (the total tumor diameter was 28.1 mm in the control and 20.7 mm in Atg5 (flox/flox)/K19 (CreERT) mice, p = 0.036). We found that p53 and UPR/endoplasmic reticulum (ER) stress-related proteins, such as cleaved caspase 3, and CAAT/enhancer-binding protein homologous protein, are up-regulated in colon tumors of Atg5 (flox/flox)/K19 (CreERT) mice. Although Atg5 and BiP silencing, respectively, increased apoptosis in p53 wild type cells, Atg5 silencing alone did not show the same effect on apoptosis in p53 mutant cells. However, co-transfection of Atg5 and BiP siRNAs led to increased apoptosis in p53 mutant cells.

Conclusions: Blocking autophagy has potential in the treatment of colon cancer by inducing apoptosis via p53 and ER stress, and suppressing the UPR pathway is a valid strategy to overcome resistance to autophagic inhibition.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Apoptosis / physiology*
Autophagy / physiology*
Cell Line, Tumor
Colonic Neoplasms / metabolism*
Colonic Neoplasms / prevention & control*
Endoplasmic Reticulum Stress / physiology*
Genes, p53 / physiology
HCT116 Cells
Humans
Mice
Mice, Inbred C57BL
Mice, Transgenic
Tumor Suppressor Protein p53 / biosynthesis*

Substances

Tumor Suppressor Protein p53