Negative correlation between organ heteroplasmy, particularly hepatic heteroplasmy, and age at death revealed by post-mortem studies of m.3243A > G cases

异质性 医学 相关性 病理 线粒体DNA 生物 遗传学 数学 几何学 基因
作者
Kunimasa Yagi,S. Okazaki,Azusa Ohbatake,Moto Nakaya,Jianhui Liu,Eiko Arite,Yukiko Miyamoto,Naoko Ito,Kaoru Nakano,Naoto Yamaaki,Hisae Honoki,Shiho Fujisaka,Daisuke Chujo,Shinichiro Tsunoda,Kunio Yanagimoto,Tsuyoshi Nozue,Masayo Yamada,Ooe K,Tsutomu Araki,Akikatsu Nakashima,Yasushi Azami,Yukio Sodemoto,Kenichi Tadokoro,Makoto Nagano,Tohru Noguchi,A Nohara,Hideki Origasa,Yo Niida,Hayato Tada
出处
期刊:Molecular Genetics and Metabolism [Elsevier]
卷期号:140 (3): 107691-107691 被引量:1
标识
DOI:10.1016/j.ymgme.2023.107691
摘要

Mitochondrial DNA m.3243A > G mutation causes mitochondrial encephalopathy, lactic acidosis, and stroke-like episodes (MELAS) and its associated multi-organ disorders, including diabetes. To clarify associations between m.3243A > G organ heteroplasmy and clinical phenotypes, including the age at death, we combined genetic and pathological examinations from seven unreported and 36 literature cases of autopsied subjects. Clinical characteristics of subjects were as follows: male, 13; female, 28; unknown, 2; the age at death, 36.9 ± 20.2 [4-82] years; BMI, 16.0 ± 2.9 [13.0-22.3]; diabetes, N = 21 (49%), diabetes onset age 38.6 ± 14.2 years; deafness, N = 27 (63%); stroke-like episodes (StLEp), N = 25 (58%); congestive heart failure (CHF), N = 15 (35%); CHF onset age, 51.3 ± 14.5 years. Causes of death (N = 32) were as follows: cardiac, N = 13 (41%); infection, N = 8 (25%); StLEp, N = 4 (13%); gastrointestinal, N = 4 (13%); renal, N = 2 (6%); hepatic, N = 1 (2%). High and low heteroplasmies were confirmed in non-regenerative and regenerative organs, respectively. Heteroplasmy of the liver, spleen, leukocytes, and kidney for all subjects was significantly associated with the age at death. Furthermore, the age at death was related to juvenile-onset (any m.3243A > G-related symptoms appeared before 20) and stroke-like episodes. Multiple linear regression analysis with the age at death as an objective variable showed the significant contribution of liver heteroplasty and juvenile-onset to the age at death. m.3243A > G organ heteroplasmy levels, particularly hepatic heteroplasmy, are significantly associated with the age at death in deceased cases.
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