Zosterabisphenone B, a new diarylheptanoid heterodimer from the seagrass Zostera marina, induces apoptosis cell death in colon cancer cells and reduces tumour growth in mice

Author:

Cacciola Nunzio Antonio1,De Cicco Paola2ORCID,Amico Rebecca2,Sepe Fabrizia3,Li Yan4,Grauso Laura5,Nanì Maria Francesca2,Scarpato Silvia2,Zidorn Christian6,Mangoni Alfonso2,Borrelli Francesca2ORCID

Affiliation:

1. Department of Veterinary Medicine and Animal Production University of Naples Federico II Naples Italy

2. Department of Pharmacy, School of Medicine and Surgery University of Naples Federico II Naples Italy

3. Institute of Experimental Endocrinology and Oncology “G. Salvatore” (IEOS) National Research Council (CNR) Naples Italy

4. Key Lab of Separation Science for Analytical Chemistry Dalian Institute of Chemical Physics, Chinese Academy of Sciences Dalian China

5. Department of Agricultural Sciences University of Naples Federico II Naples Italy

6. Pharmazeutisches Institut, Abteilung Pharmazeutische Biologie Christian‐Albrechts‐Universität zu Kiel Kiel Germany

Abstract

AbstractColorectal cancer (CRC) is one of the most common malignant tumours worldwide. Diarylheptanoids, secondary metabolites isolated from Zostera marina, are of interest in natural products research due to their biological activities. Zosterabisphenone B (ZBP B) has recently been shown to inhibit the viability of CRC cells. The aim of this study was to investigate the therapeutic potential of ZBP B for targeting human CRC cells. Cell viability was determined using the MTT assay. Flow cytometry and Western blot analyses were used to assess apoptosis and autophagy. A CRC xenograft model was used to evaluate the in vivo effect of ZBP B. No cytotoxic effect on HCEC cells was observed in the in vitro experiments. ZBP B caused morphological changes in HCT116 colon cancer cells due to an increase in early and late apoptotic cell populations. Mechanistically, ZBP B led to an increase in cleaved caspase‐3, caspase‐8, caspase‐9, PARP and BID proteins and a decrease in Bcl‐2 and c‐Myc proteins. In the xenograft model of CRC, ZBP B led to a reduction in tumour growth. These results indicate that ZBP B exerts a selective cytotoxic effect on CRC cells by affecting apoptotic signalling pathways and reducing tumour growth in mice. Taken together, our results suggest that ZBP B could be a lead compound for the synthesis and development of CRC drugs.

Funder

Regione Campania

Publisher

Wiley

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