Use of genome‐wide DNA methylation analysis to identify prognostic CpG site markers associated with longer survival time in dogs with multicentric high‐grade B‐cell lymphoma

Author:

Teoh Yong Bin12ORCID,Ishizaki Teita3,Kagawa Yumiko3,Yokoyama Shoko12,Jelinek Jaroslav4,Matsumoto Yuki5,Tomiyasu Hirotaka6,Tsujimoto Hajime7ORCID,Takiguchi Mitsuyoshi28ORCID,Yamazaki Jumpei12

Affiliation:

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

2. One Health Research Center Hokkaido University Sapporo Hokkaido Japan

3. North Lab Sapporo Hokkaido Japan

4. Coriell Institute for Medical Research Camden New Jersey USA

5. Anicom Specialty Medical Institute Inc Tokyo Japan

6. Laboratory of Veterinary Internal Medicine University of Tokyo Tokyo Japan

7. Japan Animal Referral Medical Center (JARMeC) Kawasaki Kanagawa Japan

8. Laboratory of Veterinary Internal Medicine Hokkaido University Sapporo Hokkaido Japan

Abstract

AbstractBackgroundDNA methylation analysis might identify prognostic CpG sites in CHOP‐treated dogs with multicentric high‐grade B‐cell lymphoma (MHGL) with heterogenous prognosis.ObjectiveTo identify prognostic CpG sites of MHGL through genome‐wide DNA methylation analysis with pyrosequencing validation.AnimalsTest group: 24 dogs. Validation group: 100 dogs. All client‐owned dogs were diagnosed with MHGL and treated with CHOP chemotherapy.MethodsCohort study. DNA was extracted from lymph node samples obtained via FNA. Genome‐wide DNA methylation analysis using Digital Restriction Enzyme Analysis of Methylation (DREAM) was performed on the test group to identify differentially methylated CpG sites (DMCs). Bisulfite pyrosequencing was used to measure methylation status of candidate DMCs in the validation group. Median survival times (MST) were analyzed using Kaplan‐Meier (log‐rank) product limit method.ResultsDREAM analyzed 101 576 CpG sites. Hierarchical clustering of 16 262 CpG sites in test group identified group with better prognosis (MST = 55‐477 days vs 10‐301 days, P = .007). Volcano plot identified 1371 differentially methylated CpG sites (DMCs). DMC near the genes of FAM213A (DMC‐F) and PHLPP1 (DMC‐P) were selected as candidates. Bisulfite‐pyrosequencing performed on validation group showed group with methylation level of DMC‐F < 40% had favorable prognosis (MST = 11‐1072 days vs 8‐1792 days, P = .01), whereas group with the methylation level combination of DMC‐F < 40% plus DMC‐P < 10% had excellent prognosis (MST = 18‐1072 days vs 8‐1792 days, P = .009).Conclusion and Clinical ImportanceMethylation status of prognostic CpG sites delineate canine MGHL cases with longer MST, providing owners with information on expectations of potential improved treatment outcomes.

Funder

Japan Society for the Promotion of Science

Publisher

Wiley

Subject

General Veterinary

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