Neuropathological hallmarks in autopsied cases with mitochondrial diseases caused by the mitochondrial 3243A>G mutation

Hiroaki Miyahara; Chisato Tamai; Masanori Inoue; Kazuhito Sekiguchi; Daisuke Tahara; Nao Tahara; Kazuhiro Takeda; Shusei Arafuka; Hideyuki Moriyoshi; Ryuichi Koizumi; Akio Akagi; Yuichi Riku; Jun Sone; Mari Yoshida; Kenji Ihara; Yasushi Iwasaki

doi:10.1111/bpa.13199

Neuropathological hallmarks in autopsied cases with mitochondrial diseases caused by the mitochondrial 3243A>G mutation

Brain Pathol. 2023 Nov;33(6):e13199. doi: 10.1111/bpa.13199. Epub 2023 Aug 3.

Authors

Affiliations

¹ Department of Neuropathology, Institute for Medical Research of Aging, Aichi Medical University, Aichi, Japan.
² Department of Pediatrics, Oita University Faculty of Medicine, Oita, Japan.

Abstract

The mitochondrial (m.) 3243A>G mutation is known to be associated with various mitochondrial diseases including mitochondrial myopathy, encephalopathy, lactic acidosis, and stroke-like episodes (MELAS). Their clinical symptoms have been estimated to occur with an increased mitochondrial DNA (mtDNA) heteroplasmy and reduced activity of oxidative phosphorylation (OXPHOS) complexes, but their trends in the central nervous system remain unknown. Six autopsied mutant cases and three disease control cases without the mutation were enrolled in this study. The mutant cases had a disease duration of 1-27 years. Five of six mutant cases were compatible with MELAS. In the mutant cases, cortical lesions including a laminar necrosis were frequently observed in the parietal, lateral temporal, and occipital lobes; less frequently in the frontal lobe including precentral gyrus; and not at all in the medial temporal lobe. The mtDNA heteroplasmy in brain tissue samples of the mutant cases was strikingly high, ranging from 53.8% to 85.2%. The medial temporal lobe was preserved despite an inhospitable environment having high levels of mtDNA heteroplasmy and lactic acid. OXPHOS complex I was widely decreased in the mutant cases. The swelling of smooth muscle cells in the vessels on the leptomeninges, with immunoreactivity (IR) against mitochondria antibody, and a decreased nuclear/cytoplasmic ratio of choroidal epithelial cells were observed in all mutant cases but in none without the mutation. Common neuropathological findings such as cortical laminar necrosis and basal ganglia calcification were not always observed in the mutant cases. A high level of mtDNA heteroplasmy was observed throughout the brain in spite of heterogeneous cortical lesions. A lack of medial temporal lesion, mitochondrial vasculopathy in vessels on the leptomeninges, and an increased cytoplasmic size of epithelial cells in the choroid plexus could be neuropathological hallmarks helpful in the diagnosis of mitochondrial diseases.

Keywords: MELAS; choroidal epithelial cell swelling; mitochondrial 3243A>G mutation; mitochondrial vasculopathy; mtDNA heteroplasmy; stroke-like episodes.

Publication types

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

MeSH terms

DNA, Mitochondrial / genetics
Humans
MELAS Syndrome* / complications
MELAS Syndrome* / genetics
MELAS Syndrome* / pathology
Mitochondria / pathology
Mitochondrial Diseases* / genetics
Mutation
Necrosis

Substances

DNA, Mitochondrial