Father-to-offspring transmission of extremely long NOTCH2NLC repeat expansions with contractions: genetic and epigenetic profiling with long-read sequencing

Fukuda, Hiromi; Yamaguchi, Daisuke; Nyquist, Kristofor; Yabuki, Yasushi; Miyatake, Satoko; Uchiyama, Yuri; Hamanaka, Kohei; Saida, Ken; Koshimizu, Eriko; Tsuchida, Naomi; Fujita, Atsushi; Mitsuhashi, Satomi; Ohbo, Kazuyuki; Satake, Yuki; Sone, Jun; Doi, Hiroshi; Morihara, Keisuke; Okamoto, Tomoko; Takahashi, Yūji; Wenger, Aaron M.; Shioda, Norifumi; Tanaka, Fumiaki; Matsumoto, Naomichi; Mizuguchi, Takeshi

doi:10.1186/s13148-021-01192-5

Cited by 23 publications

(24 citation statements)

References 32 publications

(43 reference statements)

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Another advantage of the approach demonstrated hereby is that PCR-free analysis potentially allows the direct assessment of DNA methylation, as already reported for other repeat-linked diseases (Fukuda et al 2021;Giesselmann et al 2019). This can provide additional information concerning the impact of expansions on the functionality of the CNBP gene.…”

Section: Discussionmentioning

confidence: 73%

Characterization of full-length CNBP expanded alleles in myotonic dystrophy type 2 patients by Cas9-mediated enrichment and nanopore sequencing

Alfano

Antoni

Centofanti

et al. 2022

Preprint

View full text Add to dashboard Cite

Myotonic dystrophy type 2 (DM2) is caused by CCTG repeat expansions in the CNBP gene, comprising 75 to >11,000 units and featuring extensive mosaicism, making it challenging to sequence fully-expanded alleles. To overcome these limitations, we used PCR-free Cas9-mediated nanopore sequencing to characterize CNBP repeat expansions at the single-nucleotide level in nine DM2 patients. The length of normal and expanded alleles can be assessed precisely using this strategy, agreeing with traditional methods, and revealing the degree of mosaicism. We also sequenced an entire ∼50-kbp expansion, which has not been achieved previously for DM2 or any other repeat-expansion disorders. Our approach precisely counted the repeats and identified the repeat pattern for both short interrupted and uninterrupted alleles. Interestingly, in the expanded alleles, only two DM2 samples featured the expected pure CCTG repeat pattern, while the other seven presented also TCTG blocks at the 3′ end, which have not been reported before in DM2 patients, but confirmed hereby with orthogonal methods. The demonstrated approach simultaneously determines repeat length, structure/motif and the extent of somatic mosaicism, promising to improve the molecular diagnosis of DM2 and achieve more accurate genotype– phenotype correlations for the better stratification of DM2 patients in clinical trials.

show abstract

Section: Discussionmentioning

confidence: 73%

Characterization of full-length CNBP expanded alleles in myotonic dystrophy type 2 patients by Cas9-mediated enrichment and nanopore sequencing

Alfano

Antoni

Centofanti

et al. 2022

Preprint

View full text Add to dashboard Cite

show abstract

“…), there are only few examples of anticipation reported in NIID and OPDM families, and a limited correlation between the size of CGG expansions and the age of onset in OPDM1 and OPDM2, with a r 2 of 0.188 and 0.158, respectively, ( Kumutpongpanich et al, 2021 ; Xi et al, 2021 ). On the contrary, there are increasing reports of individuals carrying large CGG expansions (>200–300 repeats) in the NOTCH2NLC , GIPC1, and LRP12 genes and who are free of overt clinical manifestations ( Deng et al, 2020 ; Ogasawara et al, 2020 ; Deng et al, 2021 ; Fukuda et al, 2021 ; Kumutpongpanich et al, 2021 ; Yu et al, 2021 ). Molecular analyses indicate that these individuals present DNA hypermethylation associated to promoter silencing and loss of expression of the allele carrying these large CGG expansions.…”

Section: Expansion Without Anticipation In Niid and Opdm?mentioning

confidence: 99%

“…Second, these data also provide some molecular bases to the complex pedigree observed in these diseases, with increasing reports of asymptomatic ascendants who nevertheless carry the causative mutation, but of longer size (over 200–300 CGG repeats) compared to their affected descendants who typically carry an allele with 60 to 200–300 CGG repeats. Interestingly, of the ∼10 currently reported examples of asymptomatic individuals with large expansions and who have transmitted shorter repeats to their NIID or OPDM-affected descendants, all were father to infant transmission cases, suggesting a bias of expansions contraction in male germinal cells ( Deng et al, 2020 ; Deng et al, 2021 ; Fukuda et al, 2021 ; Kumutpongpanich et al, 2021 ; Yu et al, 2021 ). Of interest, a similar bias of transmission was observed in carriers of the FMR1 CGG repeat premutation where contraction occurred more often in paternal than in maternal transmission ( Nolin et al, 2019 ).…”

Section: Expansion Without Anticipation In Niid and Opdm?mentioning

confidence: 99%

Trinucleotide CGG Repeat Diseases: An Expanding Field of Polyglycine Proteins?

Boivin

Charlet‐Berguerand

2022

Front. Genet.

View full text Add to dashboard Cite

Microsatellites are repeated DNA sequences of 3–6 nucleotides highly variable in length and sequence and that have important roles in genomes regulation and evolution. However, expansion of a subset of these microsatellites over a threshold size is responsible of more than 50 human genetic diseases. Interestingly, some of these disorders are caused by expansions of similar sequences, sizes and localizations and present striking similarities in clinical manifestations and histopathological features, which suggest a common mechanism of disease. Notably, five identical CGG repeat expansions, but located in different genes, are the causes of fragile X-associated tremor/ataxia syndrome (FXTAS), neuronal intranuclear inclusion disease (NIID), oculopharyngodistal myopathy type 1 to 3 (OPDM1-3) and oculopharyngeal myopathy with leukoencephalopathy (OPML), which are neuromuscular and neurodegenerative syndromes with overlapping symptoms and similar histopathological features, notably the presence of characteristic eosinophilic ubiquitin-positive intranuclear inclusions. In this review we summarize recent finding in neuronal intranuclear inclusion disease and FXTAS, where the causing CGG expansions were found to be embedded within small upstream ORFs (uORFs), resulting in their translation into novel proteins containing a stretch of polyglycine (polyG). Importantly, expression of these polyG proteins is toxic in animal models and is sufficient to reproduce the formation of ubiquitin-positive intranuclear inclusions. These data suggest the existence of a novel class of human genetic pathology, the polyG diseases, and question whether a similar mechanism may exist in other diseases, notably in OPDM and OPML.

show abstract

“…Toutefois, dans les maladies causées par des expansions de répétitions CGG situées dans des régions 5'UTR, l'existence d'un mécanisme d'anticipation et/ou une corrélation exacte entre la taille de l'expansion et la sévérité des symptômes ne font pas actuellement consensus [7]. En effet, certains individus étaient porteurs de longues expansions de répétitions CGG dans les gènes LRP12, GIPC1 ou NOTCH2NLC mais ne développaient pas les symptômes de l'OPDM [2,38,39]. Par exemple, dans l'OPDM2, un individu asymptomatique était porteur d'une expansion de plus de 500 répétitions CGG dans le gène GIPC1 alors que ses deux enfants sont porteurs d'expansions de répétitions CGG plus courtes (117 et 113 répétitions) et ont tous deux développé des formes classiques d'OPDM [2].…”

Section: Mécanisme D'anticipation Dans L'opdm ?unclassified

“…De manière similaire, des patients possédant un nombre de répétitions CGG supérieur à 300 ne développent pas de symptômes particuliers contrairement à leurs enfants porteurs d'expansions plus courtes et qui développent une NIID et/ou une OPDM3. Il a été montré récemment que ces longues expansions (200-300 répétitions CGG) conduisent à des modifications épigénétiques du promoteur et donc à une perte d'expression du gène et de la protéine NOTCH2NLC, suggérant ainsi qu'un mécanisme de perte de fonction est peu probable dans la NIID et l'OPDM3 [38]. Ces données sont à mettre en perspective avec la physiopathologie du FXS et du FXTAS.…”

Section: Mécanisme D'anticipation Dans L'opdm ?unclassified

Les myopathies oculo-pharyngo-distales : des nouvelles maladies à expansions de répétitions CGG

et al. 2022

View full text Add to dashboard Cite

La myopathie oculo-pharyngo-distale (OPDM) est une maladie génétique rare de l’adulte affectant les muscles squelettiques du visage, du pharynx et des extrémités des membres. Récemment, des variants dans quatre gènes distincts ont été identifiés comme responsables de cette pathologie. Bien que localisées dans différents gènes, le mécanisme mutationnel est identique, à savoir une expansion de 50 à 200-300 répétitions de triplets de nucléotides CGG. Dans cet article, nous décrivons les aspects cliniques, histopathologiques et génétiques de l’OPDM, ainsi que les mécanismes moléculaires pouvant expliquer la toxicité de ces expansions de répétitions trinucléotidiques.

show abstract

Father-to-offspring transmission of extremely long NOTCH2NLC repeat expansions with contractions: genetic and epigenetic profiling with long-read sequencing

Cited by 23 publications

References 32 publications

Characterization of full-length CNBP expanded alleles in myotonic dystrophy type 2 patients by Cas9-mediated enrichment and nanopore sequencing

Characterization of full-length CNBP expanded alleles in myotonic dystrophy type 2 patients by Cas9-mediated enrichment and nanopore sequencing

Trinucleotide CGG Repeat Diseases: An Expanding Field of Polyglycine Proteins?

Les myopathies oculo-pharyngo-distales : des nouvelles maladies à expansions de répétitions CGG

Contact Info

Product

Resources

About