2014
DOI: 10.1007/s00401-014-1286-y
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C9orf72 hypermethylation protects against repeat expansion-associated pathology in ALS/FTD

Abstract: Hexanucleotide repeat expansions of C9orf72 are the most common genetic cause of amyotrophic lateral sclerosis and frontotemporal degeneration. The mutation is associated with reduced C9orf72 expression and the accumulation of potentially toxic RNA and protein aggregates. CpG methylation is known to protect the genome against unstable DNA elements and to stably silence inappropriate gene expression. Using bisulfite cloning and restriction enzyme-based methylation assays on DNA from human brain and peripheral b… Show more

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Cited by 167 publications
(207 citation statements)
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“…39 Alternatively, or in combination, epigenetic modifications, such as hypermethylation of CpG islands juxtaposing the repeats or binding of trimethylated histones, may underlie decreased abundance of C9orf72 transcripts. 24,31,[38][39][40] At the immunohistochemical level, C9-L antibody showed a diffuse labeling in the cytoplasm of cerebellar Purkinje cells, with a striking labeling of numerous speckles that were observed both in the neuronal perikarya and dendritic processes. The identity of these speckles remains unknown, and it should be noted that they were observed in both c9-ALS and non-c9-ALS cases.…”
Section: Figurementioning
confidence: 98%
See 1 more Smart Citation
“…39 Alternatively, or in combination, epigenetic modifications, such as hypermethylation of CpG islands juxtaposing the repeats or binding of trimethylated histones, may underlie decreased abundance of C9orf72 transcripts. 24,31,[38][39][40] At the immunohistochemical level, C9-L antibody showed a diffuse labeling in the cytoplasm of cerebellar Purkinje cells, with a striking labeling of numerous speckles that were observed both in the neuronal perikarya and dendritic processes. The identity of these speckles remains unknown, and it should be noted that they were observed in both c9-ALS and non-c9-ALS cases.…”
Section: Figurementioning
confidence: 98%
“…24 Haploinsufficiency was initially suggested as a disease mechanism owing to the decreased abundance of V2 and V3 transcripts in c9-ALS cases, and consistent with this hypothesis, reduced expression of selected or total C9orf72 transcripts in C9orf72 repeat expansion carrier-derived cells or tissues have been widely reported. 1,[24][25][26][27][28][29][30][31] Although there is little known about the effects of C9orf72 haploinsufficiency, the development of motor phenotypes in zebrafish and Caenorhabditis elegans owing to downregulation of C9orf72 orthologues supports its role as a disease pathomechanism. 30,32 It has been predicted that C9orf72 proteins may belong to the DENN-like protein family and play roles in Rabmediated cellular trafficking; however, the precise functions and properties of C9orf72 protein are largely unknown owing to a lack of specific antibodies.…”
mentioning
confidence: 99%
“…Возросший интерес к этой области науки при БАС и ЛВД связан с возможностью иссле-дования новых теорий развития заболевания, что мо-жет обеспечить понимание механизмов этих 2 леталь-ных патологий. Существуют противоречивые данные о том, что эпигенетическая модификация гена C9orf72 посредством гиперметилирования значимо коррели-рует с более быстрым течением заболевания, однако в других исследованиях показан нейропротективный эффект для этой категории пациентов [14][15][16][17]. Гипер-метилирование CpG-островков 5' -промоторной области гена C9orf72 продемонстрировано различными группами исследователей и встречается примерно в 10-30 % случаев среди пациентов с экспансией в ге-не C9orf72 [14,17], вероятно, приводя к снижению уровня экспрессии C9orf72.…”
Section: оригинальные исследованияunclassified
“…Изменение клинического фенотипа у нашего пациента может быть результатом снижения уровня экспрессии патологического аллеля вследствие метилирования 5' -промоторной области гена C9orf72, что может способствовать уменьшению токсического эффекта экспансии. По данным других исследований, четкой корреляции статуса метилирова-ния с фенотипическим вариантом нейродегенератив-ного процесса либо продолжительностью заболевания не выявлено [14][15][16][17]. Для поиска и анализа более де-тальных клинико-эпигенетических корреляций необ-ходимы дальнейшие исследования на большей когорте пациентов с БАС и другой C9orf72-ассоциированной нейродегенеративной патологией.…”
Section: том 8 Volunclassified
“…62,68,[80][81][82] There are 2 cytosine-phosphate-guanine (CpG) islands flanking the C9orf72 repeat locus. The CpG island upstream of the repeat has been found to have increased methylation in a subset of expanded repeat carriers, 62,68,81 while the CpG island downstream of the repeat is unmethylated. The expanded repeat itself is not apparently hypermethylated.…”
Section: Histone and Dna Methylationsmentioning
confidence: 99%