Rabdosianone I, a Bitter Diterpene from an Oriental Herb, Suppresses Thymidylate Synthase Expression by Directly Binding to ANT2 and PHB2.

Motoki Watanabe,Yasumasa Yamada,Mamiko Sukeno,Tomoshi Kameda,Yosuke Iizumi,Toshiyuki Sakai,Yoichi Kurumida,Hideki Takakura,Mahiro Iizuka-Ohashi,Michihiro Mutoh,Yoshihiro Sowa,Shingo Miyamoto

doi:10.3390/cancers13050982

Abstract

Simple SummaryIn the present study, we found the novel pleiotropic regulation of the oncogene product thymidylate synthase (TS) by a chemical biology approach to identify rabdosianone I-binding proteins. Rabdosianone I, which is extracted from a traditional Asian herb Isodon japonicus Hara for longevity, suppressed TS expression at mRNA and protein levels. We immobilized rabdosianone I onto nano-magnetic beads and identified two mitochondrial proteins, adenine nucleotide translocase 2 (ANT2) and prohibitin 2 (PHB2), as the direct targets of rabdosianone I in cancer cells. Mechanistically, the knockdown of ANT2 or PHB2 promoted proteasomal degradation of the TS protein. In addition, PHB2 reduced TS mRNA levels. Thus, we provide previously unknown mechanisms of TS regulation by ANT2 and PHB2 and propose the possibility of rabdosianone I as a promising lead compound for the discovery of a novel TS suppressor.Natural products have numerous bioactivities and are expected to be a resource for potent drugs. However, their direct targets in cells often remain unclear. We found that rabdosianone I, which is a bitter diterpene from an oriental herb for longevity, Isodon japonicus Hara, markedly inhibited the growth of human colorectal cancer cells by downregulating the expression of thymidylate synthase (TS). Next, using rabdosianone I-immobilized nano-magnetic beads, we identified two mitochondrial inner membrane proteins, adenine nucleotide translocase 2 (ANT2) and prohibitin 2 (PHB2), as direct targets of rabdosianone I. Consistent with the action of rabdosianone I, the depletion of ANT2 or PHB2 reduced TS expression in a different manner. The knockdown of ANT2 or PHB2 promoted proteasomal degradation of TS protein, whereas that of not ANT2 but PHB2 reduced TS mRNA levels. Thus, our study reveals the ANT2- and PHB2-mediated pleiotropic regulation of TS expression and demonstrates the possibility of rabdosianone I as a lead compound of TS suppressor.

Highlights

Natural products have been a rich repository of medical supplies [1]
We found that the deletion of adenine nucleotide translocase 2 (ANT2) or prohibitin 2 (PHB2) resulted in the downregulation of thymidylate synthase (TS) at mRNA and protein levels, which is analogous to the mode of action of rabdosianone I
Rabdosianone I is a bitter diterpene isolated from an oriental herb, Isodon japonicus Hara (Figure 1A)

Summary

Introduction

Plant extracts from many types of herbs have been used throughout history. According to legend, Kukai (774–835), one of the most well-known Japanese monks, treated patients using the traditional herb Isodon japonicus Hara during the Heian period in Japan. Isodon japonicus Hara, known as Enmeiso, which means “grass of longevity” in Japanese, has been infused to make tea for health purposes. How Isodon japonicus Hara may contribute to disease prevention and treatment, including anticancer activity, is not well characterized. It was reported that several types of bitter diterpenes (e.g., oridonin, enmein, and rabdosianone I) were extracted from Isodon japonicus Hara [2]. To date, no attempt has been made to demonstrate the anticancer activity of rabdosianone I

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