Diverse genome‐wide DNA methylation alterations in canine hepatocellular tumours

Author:

Asari Yu1,Yamazaki Jumpei234ORCID,Thandar Oo1,Suzuki Tamami5,Aoshima Keisuke45ORCID,Takeuchi Kyosuke2,Kinoshita Ryohei24,Kim Sangho46ORCID,Hosoya Kenji46,Ishizaki Teita257,Kagawa Yumiko7,Jelinek Jaroslav8,Yokoyama Shoko234,Sasaki Noboru1ORCID,Ohta Hiroshi1,Nakamura Kensuke1,Takiguchi Mitsuyoshi1

Affiliation:

1. Laboratory of Veterinary Internal Medicine, Graduate School of Veterinary Medicine Hokkaido University Sapporo Japan

2. Veterinary Teaching Hospital Graduate School of Veterinary Medicine Hokkaido University Sapporo Japan

3. Translational Research Unit, Veterinary Teaching Hospital, Graduate School of Veterinary Medicine Hokkaido University Sapporo Japan

4. One Health Research Center, Cancer Research Unit Hokkaido University Sapporo Japan

5. Laboratory of Comparative Pathology, Graduate School of Veterinary Medicine Hokkaido University Sapporo Japan

6. Laboratory of Veterinary Surgery, Graduate School of Veterinary Medicine Hokkaido University Sapporo Japan

7. North Lab Sapporo Japan

8. Coriell Institute for Medical Research Camden New Jersey USA

Abstract

AbstractBackgroundCanine hepatocellular tumours (HCTs) are common primary liver tumours. However, the exact mechanisms of tumourigenesis remain unclear. Although some genetic mutations have been reported, DNA methylation alterations in canine HCT have not been well studied.ObjectivesIn this study, we aimed to analyse the DNA methylation status of canine HCT.MethodsTissues from 33 hepatocellular carcinomas, 3 hepatocellular adenomas, 1 nodular hyperplasia, 21 non‐tumour livers from the patients and normal livers from 5 healthy dogs were used. We analysed the DNA methylation levels of 72,367 cytosine–guanine dinucleotides (CpG sites) in all 63 samples.Results and conclusionsAlthough a large fraction of CpG sites that were highly methylated in the normal liver became hypomethylated in tumours from most patients, we also found some patients with less remarkable change or no change in DNA methylation. Hierarchical clustering analysis revealed that 32 of 37 tumour samples differed from normal livers, although the remaining 5 tumour livers fell into the same cluster as normal livers. In addition, the number of hypermethylated genes in tumour livers varied among tumour cases, suggesting various DNA methylation patterns in different tumour groups. However, patient and clinical parameters, such as age, were not associated with DNA methylation status. In conclusion, we found that HCTs undergo aberrant and diverse patterns of genome‐wide DNA methylation compared with normal liver tissue, suggesting a complex epigenetic mechanism in canine HCT.

Funder

Japan Society for the Promotion of Science

Publisher

Wiley

Subject

General Veterinary

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