Histopathological and epigenetic changes in myocardium associated with cancer therapy-related cardiac dysfunction

Chiyoko-Ikeda Terada; Kenji Onoue; Tomomi Fujii; Hiroe Itami; Kohei Morita; Tomoko Uchiyama; Maiko Takeda; Hitoshi Nakagawa; Tomoya Nakano; Youichirou Baba; Kisaki Amemiya; Yoshihiko Saito; Kinta Hatakeyama; Chiho Ohbayashi

doi:10.1002/ehf2.14034

Histopathological and epigenetic changes in myocardium associated with cancer therapy-related cardiac dysfunction

ESC Heart Fail. 2022 Oct;9(5):3031-3043. doi: 10.1002/ehf2.14034. Epub 2022 Jun 23.

Authors

Affiliations

¹ Department of Diagnostic Pathology, Nara Medical University, 840 Shijo, Kashihara, Nara, 643-8522, Japan.
² Department of Cardiovascular Medicine, Nara Medical University, 840 Shijo, Kashihara, Nara, 634-8522, Japan.
³ Department of Pathology, Suzuka General Hospital, 1275-53 Yasuduka, Suzuka, Mie, 513-8630, Japan.
⁴ Department of Pathology, National Cerebral and Cardiovascular Center, 6-1 Kishibe-Shimmachi, Suita, Osaka, 564-8565, Japan.

Abstract

Aims: Cancer therapy-related cardiac dysfunction (CTRCD) is commonly reported, but its histopathology, mechanisms, and risk factors are not known. We aimed to clarify the histopathology and mechanisms of CTRCD to identify risk factors.

Methods and results: We performed myocardial histopathological studies on 13 endomyocardial biopsies from CTRCD patients, 35 autopsied cancer cases with or without cardiac dysfunction, and controls without cancer (10 biopsies and 9 autopsies). Cardiotoxicity risk scores were calculated based on medication; and patient-related risk factors, fibrosis, and cardiomyocyte changes were scored; and p53 and H3K27ac histone modification were evaluated by histological score (H-score). In the biopsy cases, all histopathological changes and the p53 evaluation were significantly higher in the CTRCD group than in the controls [p53 H-score; 63 (9.109) vs. 33 (5.099), P < 0.05]. In patients with a short time between drug and disease onset (<4.2 years), fibrosis and p53 positively correlated (r = 0.76, P < 0.05), and in those with late onset disease (>4.2 years), cellular abnormalities and p53 trended to a positive correlation and cardiotoxicity risk scores and p53 positively correlated (r = 0.95, P < 0.05). A year after biopsy, the short-term group had significant recovery of ejection fraction compared with the long-term group (P < 0.05). The CTRCD group had a significantly worse overall survival prognosis than the control group [hazard ratio 7.61 (95% confidence interval 1.30-44.6), P < 0.05]. Autopsy cases with cancer treatment also had a high grade of histopathological changes, with even more severe changes in patients with cardiac dysfunction, and had increased p53 and H3K27ac expression levels, compared with controls. H-scores of p53 and H3K27ac showed a positive correlation in the CTRCD group in biopsy cases (r = 0.62, P < 0.05) and a positive correlation in autopsy cases.

Conclusions: Our results indicate distinct morphological characteristics in myocardial histopathology associated with CTRCD. p53 and H3K27ac histone modification could be sensitive markers of CTRCD and suggest a mechanistic involvement of epigenetic changes.

Keywords: endomyocardial biopsy; epigenetics; histone acetylation; oncocardiology; p53.

Publication types

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

MeSH terms

Antineoplastic Agents* / adverse effects
Cardiotoxicity / etiology
Epigenesis, Genetic
Fibrosis
Heart Diseases* / etiology
Humans
Myocardium
Neoplasms* / chemically induced
Neoplasms* / complications
Neoplasms* / drug therapy
Tumor Suppressor Protein p53 / genetics

Substances

Antineoplastic Agents
Tumor Suppressor Protein p53