Literature DB >> 36131298

Letter to the editor on a paper by Kaivola et al. (2020): carriership of two copies of C9orf72 hexanucleotide repeat intermediate-length alleles is not associated with amyotrophic lateral sclerosis or frontotemporal dementia.

Sterre C M de Boer1,2, Lauren Woolley3, Merel O Mol4, Maria Serpente5, Lianne M Reus6,7,8, Rick van Minkelen9, Joke F A van Vugt10, Federica Sorrentino5,11, Jan H Veldink10, Harro Seelaar4, Daniela Galimberti5,11, Fred van Ruissen12, Simon Mead3, Ekaterina Rogaeva13, Yolande A L Pijnenburg6,7, Sven J van der Lee6,7,14.   

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Year:  2022        PMID: 36131298      PMCID: PMC9494883          DOI: 10.1186/s40478-022-01438-0

Source DB:  PubMed          Journal:  Acta Neuropathol Commun        ISSN: 2051-5960            Impact factor:   7.578


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Sir/madam, Pathological hexanucleotide (G4C2)n-repeat expansion in C9orf72 is the most common genetic cause of amyotrophic lateral sclerosis (ALS), as well as frontotemporal dementia (FTD) and FTD-ALS. Since the discovery of the C9orf72 repeat expansion as cause for ALS/FTD, there have been several contradicting reports whether intermediate repeat lengths are associated with FTD and/or ALS [1-3]. The definition of intermediate repeat length relies on the lower limit for pathological expansions, which has not been well-established. The most studies are using the initially suggested cutoff of 30 repeats [4, 5]. Recently, Kaivola et al. added to the existing literature that carriership of two copies of intermediate-length alleles is a strong risk factor for ALS [6]. Given the prior conflicting evidence, their finding warrants replication and as there is considerable overlap of FTD and ALS, we hypothesized that two copies of the C9orf72 intermediate-length alleles might also be associated with an increased risk of FTD. In cohorts independent from Kaivola et al., we studied the association of carriership of two intermediate-length hexanucleotide C9orf72 repeats with ALS, FTD and a range of other neurodegenerative diseases, including primary progressive aphasia (PPA), corticobasal syndrome (CBS), progressive supranuclear palsy (PSP), Parkinson’s disease (PD) and Alzheimer’s disease (AD). In summary, we did not find evidence for an association of the carriership of two C9orf72 repeat intermediate-length with any of the neurodegenerative diseases. We collected data from six different cohorts studying neurodegenerative diseases (total n = 15,021) [7-12]. The C9orf72 lengths in each cohort were measured using comparable PCR or whole genome sequence methods (Additional file 1: Table S1). We excluded participants with a C9orf72 repeat expansion (using a ≥ 45 repeats threshold following methods of Kaivola et al. [6], n = 295), with an unknown allele length (n = 21), with an unknown phenotype (n = 28) and the phenotypes vascular dementia, mixed dementia and psychiatric diagnoses (n = 593). The remaining 14,084 participants were included for the analysis. We compared controls (n = 9,497) with five different disease classes: (a) ALS (n = 2,054), (b) FTD (n = 1,016), (c) FTD spectrum (FTD, ALS, PPA = 208, PSP/CBS = 8), (d) PD (n = 315), and (e) AD (n = 986). Statistical power and minimal detectable effect sizes (odds ratio’s) were calculated using the Genetic Association Study (GAS) Power Calculator (e.g. the sample size for power calculations of ALS was 11,551 with a case rate of 17.8%, alpha was 0.05). Expected effect sizes were derived from Kaivola et al. [6]. Disease allele frequencies were derived from our control group (Additional File 1: Table S2, Additional File 1: Table S3). We associated the intermediate-length allele thresholds described by Kaivola et al. [6]: (1) ≥ 7/ ≥ 7 repeats, (2) ≥ 7–16/7–16, and (3) ≥ 7/ ≥ 17–45 units. We fitted separate logistic regression models to study the association of traits with each of the three different intermediate-length threshold groups, adjusting for cohort origin. In addition, we performed analysis within region of origin (North-American, United Kingdom, Northern Europe and Southern Europe) followed by a fixed-effects inverse variance meta-analysis. Statistical analyses were performed using RStudio (version 3.5.2, R Development Core team 2010, rmeta package). Power analyses showed that our study has ~ 100% power to detect the reported association in ALS in all intermediate-length threshold groups. We found no significant association of ALS, FTD and the FTD spectrum with carriership of two copies of C9orf72 intermediate-length alleles in all three intermediate-length threshold groups (Table 1). The region of origin analysis (Additional File 1: Table S4) followed by a fixed-effects inverse variance meta-analysis showed similar negative results (Additional File 1: Table S5). We explored the association of AD and PD with carriership of two copies of C9orf72 intermediate-length alleles. No significant association was found. However, sample size was limited in these groups.
Table 1

Individuals with two C9orf72 intermediate-length alleles in ALS, FTD, FTD spectrum, PD and AD patients, and controls after exclusion of expansion carriers

TraitShorter/longer alleleControls with longer alleles (%)Cases with longer alleles (%)p-valueOR [95% CI]
ALS < 7/ < 7 vs. = > 7/ = > 7546 (5.7%)132 (6.4%)0.970.99 [0.76–1.31]
 < 7/ < 7 vs. 7–16/7–16500 (5.3%)121 (5.9%)0.880.98 [0.74–1.30]
 < 7/ < 7 vs. = > 7/ = > 17–4546 (0.5%)11 (0.5%)0.601.28 [0.51–3.23]
FTD < 7/ < 7 vs. = > 7/ = > 7546 (5.7%)71 (7%)0.991.00 [0.72–1.39]
 < 7/ < 7 vs. 7–16/7–16500 (5.3%)64 (6.3%)0.960.99 [0.70–1.40]
 < 7/ < 7 vs. = > 7/ = > 17–4546 (0.5%)7 (0.7%)0.861.09 [0.40–3.00]
FTD spectrum < 7/ < 7 vs. = > 7/ = > 7546 (5.7%)217 (6.6%)0.860.98 [0.79–1.22]
 < 7/ < 7 vs. 7–16/7–16500 (5.3%)199 (6.1%)0.810.97 [0.78–1.22]
 < 7/ < 7 vs. = > 7/ = > 17–4546 (0.5%)18 (0.5%)0.901.05 [0.50–2.20]
PD < 7/ < 7 vs. = > 7/ = > 7546 (5.7%)22 (7%)0.941.02 [0.59–1.76]
 < 7/ < 7 vs. 7–16/7–16500 (5.3%)21 (6.7%)0.731.10 [0.63–1.94]
 < 7/ < 7 vs. = > 7/ = > 17–4546 (0.5%)1 (0.3%)0.410.41 [0.05–3.50]
AD < 7/ < 7 vs. = > 7/ = > 7546 (5.7%)67 (6.8%)0.480.88 [0.60–1.27]
 < 7/ < 7 vs. 7–16/7–16500 (5.3%)60 (6.1%)0.450.86 [0.58–1.27]
 < 7/ < 7 vs. = > 7/ = > 17–4546 (0.5%)7 (0.7%)0.991.00 [0.33–3.02]

ALS Amyotrophic lateral sclerosis, FTD Frontotemporal dementia, FTD spectrum includes bvFTD, primary progressive aphasia, corticobasal degeneration and progressive supra nuclear palsy, PD Parkinson’s disease, AD Alzheimer’s disease OR Odds ratio, CI Confidence interval, N.A not applicable

We hypothesized that the true effect is smaller than reported by Kaivola et al. Therefore, we calculated the minimum odds ratio that we have 90% power for in our sample. For the ≥ 7/17–45 intermediate-length threshold, our study has 90% power to detect odds larger than 2.12 for ALS and 2.77 for FTD. Individuals with two C9orf72 intermediate-length alleles in ALS, FTD, FTD spectrum, PD and AD patients, and controls after exclusion of expansion carriers ALS Amyotrophic lateral sclerosis, FTD Frontotemporal dementia, FTD spectrum includes bvFTD, primary progressive aphasia, corticobasal degeneration and progressive supra nuclear palsy, PD Parkinson’s disease, AD Alzheimer’s disease OR Odds ratio, CI Confidence interval, N.A not applicable Several suggestions may explain the discrepancy between Kaivola’s strong positive findings and our negative results. First, the higher prevalence of the intermediate-length alleles in Finland [13] versus the non-Finnish Europeans and North Americans represented in our cohort, could have resulted in the Finnish study to have increased power. Second, there could be another, Finland-specific, pathological variant present on the haplotype with the intermediate length allele that associates with ALS. Likewise, there are sub-haplotypes with an increased ‘base’ repeat-length, predisposing to pathological repeat expansions [10]. Third, the genotyping in the Finnish study and in our study, was not done at one site. This may have resulted in batch or laboratory effects. In our study, we corrected for batch or laboratory effects by adjusting for cohort of origin in our logistic regression models and observed no effects. Still, we cannot fully rule out false negative findings due to cohort or technical biases. In support of the association, a Belgian study showed that lengths of ≥ 7–24 are almost exclusively present on the chromosome 9 risk haplotype tagged by the rs2814707 T-allele and that homozygous carriership of the T-allele is associated with disease (OR = 1.8, p = 0.04) [2]. Homozygous carriership of this T-allele was associated with ALS and FTD-ALS (OR = 2.08, p = 0.04) in the non-expansion group [1]. We also made an interesting observation when reviewing the clinical records of carriers of two copies of repeat intermediate-length in one cohort. These patients showed a bvFTD phenotype with noteworthy co-symptoms of PSP and ALS. A co-existence that, based on clinicopathology, is not to be expected and as far as we are aware, has not previously been associated with C9orf72 repeat intermediate-length [14]. Altogether, in this multinational cohort we could not confirm an association of carriership of two copies of C9orf72 repeat intermediate-length alleles with ALS or FTD. Additional file 1. Additional file 2.
  14 in total

1.  Analysis of C9orf72 Intermediate Alleles in a Retrospective Cohort of Neurological Patients: Risk Factors for Alzheimer's Disease?

Authors:  Maria Serpente; Chiara Fenoglio; Andrea Arighi; Giorgio G Fumagalli; Marina Arcaro; Federica Sorrentino; Caterina Visconte; Elio Scarpini; Daniela Galimberti
Journal:  J Alzheimers Dis       Date:  2021-04-28       Impact factor: 4.472

2.  Population based epidemiology of amyotrophic lateral sclerosis using capture-recapture methodology.

Authors:  Mark H B Huisman; Sonja W de Jong; Perry T C van Doormaal; Stephanie S Weinreich; H Jurgen Schelhaas; Anneke J van der Kooi; Marianne de Visser; Jan H Veldink; Leonard H van den Berg
Journal:  J Neurol Neurosurg Psychiatry       Date:  2011-05-27       Impact factor: 10.154

3.  Length of normal alleles of C9ORF72 GGGGCC repeat do not influence disease phenotype.

Authors:  Nicola J Rutherford; Michael G Heckman; Mariely Dejesus-Hernandez; Matt C Baker; Alexandra I Soto-Ortolaza; Sruti Rayaprolu; Heather Stewart; Elizabeth Finger; Kathryn Volkening; William W Seeley; Kimmo J Hatanpaa; Catherine Lomen-Hoerth; Andrew Kertesz; Eileen H Bigio; Carol Lippa; David S Knopman; Hans A Kretzschmar; Manuela Neumann; Richard J Caselli; Charles L White; Ian R Mackenzie; Ronald C Petersen; Michael J Strong; Bruce L Miller; Bradley F Boeve; Ryan J Uitti; Kevin B Boylan; Zbigniew K Wszolek; Neill R Graff-Radford; Dennis W Dickson; Owen A Ross; Rosa Rademakers
Journal:  Neurobiol Aging       Date:  2012-07-26       Impact factor: 4.673

4.  Underlying genetic variation in familial frontotemporal dementia: sequencing of 198 patients.

Authors:  Merel O Mol; Jeroen G J van Rooij; Tsz H Wong; Shamiram Melhem; Annemieke J M H Verkerk; Anneke J A Kievit; Rick van Minkelen; Rosa Rademakers; Cyril Pottier; Laura Donker Kaat; Harro Seelaar; John C van Swieten; Elise G P Dopper
Journal:  Neurobiol Aging       Date:  2020-07-30       Impact factor: 4.673

5.  A hexanucleotide repeat expansion in C9ORF72 is the cause of chromosome 9p21-linked ALS-FTD.

Authors:  Alan E Renton; Elisa Majounie; Adrian Waite; Javier Simón-Sánchez; Sara Rollinson; J Raphael Gibbs; Jennifer C Schymick; Hannu Laaksovirta; John C van Swieten; Liisa Myllykangas; Hannu Kalimo; Anders Paetau; Yevgeniya Abramzon; Anne M Remes; Alice Kaganovich; Sonja W Scholz; Jamie Duckworth; Jinhui Ding; Daniel W Harmer; Dena G Hernandez; Janel O Johnson; Kin Mok; Mina Ryten; Danyah Trabzuni; Rita J Guerreiro; Richard W Orrell; James Neal; Alex Murray; Justin Pearson; Iris E Jansen; David Sondervan; Harro Seelaar; Derek Blake; Kate Young; Nicola Halliwell; Janis Bennion Callister; Greg Toulson; Anna Richardson; Alex Gerhard; Julie Snowden; David Mann; David Neary; Michael A Nalls; Terhi Peuralinna; Lilja Jansson; Veli-Matti Isoviita; Anna-Lotta Kaivorinne; Maarit Hölttä-Vuori; Elina Ikonen; Raimo Sulkava; Michael Benatar; Joanne Wuu; Adriano Chiò; Gabriella Restagno; Giuseppe Borghero; Mario Sabatelli; David Heckerman; Ekaterina Rogaeva; Lorne Zinman; Jeffrey D Rothstein; Michael Sendtner; Carsten Drepper; Evan E Eichler; Can Alkan; Ziedulla Abdullaev; Svetlana D Pack; Amalia Dutra; Evgenia Pak; John Hardy; Andrew Singleton; Nigel M Williams; Peter Heutink; Stuart Pickering-Brown; Huw R Morris; Pentti J Tienari; Bryan J Traynor
Journal:  Neuron       Date:  2011-09-21       Impact factor: 17.173

6.  The C9orf72 repeat size correlates with onset age of disease, DNA methylation and transcriptional downregulation of the promoter.

Authors:  I Gijselinck; S Van Mossevelde; J van der Zee; A Sieben; S Engelborghs; J De Bleecker; A Ivanoiu; O Deryck; D Edbauer; M Zhang; B Heeman; V Bäumer; M Van den Broeck; M Mattheijssens; K Peeters; E Rogaeva; P De Jonghe; P Cras; J-J Martin; P P de Deyn; M Cruts; C Van Broeckhoven
Journal:  Mol Psychiatry       Date:  2015-10-20       Impact factor: 15.992

Review 7.  Intermediate C9orf72 alleles in neurological disorders: does size really matter?

Authors:  Adeline S L Ng; Eng-King Tan
Journal:  J Med Genet       Date:  2017-07-08       Impact factor: 6.318

8.  Genome-wide association study of frontotemporal dementia identifies a C9ORF72 haplotype with a median of 12-G4C2 repeats that predisposes to pathological repeat expansions.

Authors:  Lianne M Reus; Iris E Jansen; Merel O Mol; Fred van Ruissen; Jeroen van Rooij; Natasja M van Schoor; Niccolò Tesi; Marcel J T Reinders; Martijn A Huisman; Henne Holstege; Pieter Jelle Visser; Sterre C M de Boer; Marc Hulsman; Shahzad Ahmad; Najaf Amin; Andre G Uitterlinden; Arfan Ikram; Cornelia M van Duijn; Harro Seelaar; Inez H G B Ramakers; Frans R J Verhey; Aad van der Lugt; Jurgen A H R Claassen; Geert Jan Biessels; Peter Paul De Deyn; Philip Scheltens; Wiesje M van der Flier; John C van Swieten; Yolande A L Pijnenburg; Sven J van der Lee
Journal:  Transl Psychiatry       Date:  2021-09-02       Impact factor: 6.222

9.  A pan-European study of the C9orf72 repeat associated with FTLD: geographic prevalence, genomic instability, and intermediate repeats.

Authors:  Julie van der Zee; Ilse Gijselinck; Lubina Dillen; Tim Van Langenhove; Jessie Theuns; Sebastiaan Engelborghs; Stéphanie Philtjens; Mathieu Vandenbulcke; Kristel Sleegers; Anne Sieben; Veerle Bäumer; Githa Maes; Ellen Corsmit; Barbara Borroni; Alessandro Padovani; Silvana Archetti; Robert Perneczky; Janine Diehl-Schmid; Alexandre de Mendonça; Gabriel Miltenberger-Miltenyi; Sónia Pereira; José Pimentel; Benedetta Nacmias; Silvia Bagnoli; Sandro Sorbi; Caroline Graff; Huei-Hsin Chiang; Marie Westerlund; Raquel Sanchez-Valle; Albert Llado; Ellen Gelpi; Isabel Santana; Maria Rosário Almeida; Beatriz Santiago; Giovanni Frisoni; Orazio Zanetti; Cristian Bonvicini; Matthis Synofzik; Walter Maetzler; Jennifer Müller Vom Hagen; Ludger Schöls; Michael T Heneka; Frank Jessen; Radoslav Matej; Eva Parobkova; Gabor G Kovacs; Thomas Ströbel; Stayko Sarafov; Ivailo Tournev; Albena Jordanova; Adrian Danek; Thomas Arzberger; Gian Maria Fabrizi; Silvia Testi; Eric Salmon; Patrick Santens; Jean-Jacques Martin; Patrick Cras; Rik Vandenberghe; Peter Paul De Deyn; Marc Cruts; Christine Van Broeckhoven; Julie van der Zee; Ilse Gijselinck; Lubina Dillen; Tim Van Langenhove; Jessie Theuns; Stéphanie Philtjens; Kristel Sleegers; Veerle Bäumer; Githa Maes; Ellen Corsmit; Marc Cruts; Christine Van Broeckhoven; Julie van der Zee; Ilse Gijselinck; Lubina Dillen; Tim Van Langenhove; Stéphanie Philtjens; Jessie Theuns; Kristel Sleegers; Veerle Bäumer; Githa Maes; Marc Cruts; Christine Van Broeckhoven; Sebastiaan Engelborghs; Peter P De Deyn; Patrick Cras; Sebastiaan Engelborghs; Peter P De Deyn; Mathieu Vandenbulcke; Mathieu Vandenbulcke; Barbara Borroni; Alessandro Padovani; Silvana Archetti; Robert Perneczky; Janine Diehl-Schmid; Matthis Synofzik; Walter Maetzler; Jennifer Müller Vom Hagen; Ludger Schöls; Matthis Synofzik; Walter Maetzler; Jennifer Müller Vom Hagen; Ludger Schöls; Michael T Heneka; Frank Jessen; Alfredo Ramirez; Delia Kurzwelly; Carmen Sachtleben; Wolfgang Mairer; Alexandre de Mendonça; Gabriel Miltenberger-Miltenyi; Sónia Pereira; Clara Firmo; José Pimentel; Raquel Sanchez-Valle; Albert Llado; Anna Antonell; Jose Molinuevo; Ellen Gelpi; Caroline Graff; Huei-Hsin Chiang; Marie Westerlund; Caroline Graff; Anne Kinhult Ståhlbom; Håkan Thonberg; Inger Nennesmo; Anne Börjesson-Hanson; Benedetta Nacmias; Silvia Bagnoli; Sandro Sorbi; Valentina Bessi; Irene Piaceri; Isabel Santana; Beatriz Santiago; Isabel Santana; Maria Helena Ribeiro; Maria Rosário Almeida; Catarina Oliveira; João Massano; Carolina Garret; Paula Pires; Giovanni Frisoni; Orazio Zanetti; Cristian Bonvicini; Stayko Sarafov; Ivailo Tournev; Albena Jordanova; Ivailo Tournev; Gabor G Kovacs; Thomas Ströbel; Michael T Heneka; Frank Jessen; Alfredo Ramirez; Delia Kurzwelly; Carmen Sachtleben; Wolfgang Mairer; Frank Jessen; Radoslav Matej; Eva Parobkova; Adrian Danel; Thomas Arzberger; Gian Maria Fabrizi; Silvia Testi; Sergio Ferrari; Tiziana Cavallaro; Eric Salmon; Patrick Santens; Patrick Cras
Journal:  Hum Mutat       Date:  2013-01-04       Impact factor: 4.878

10.  Carriership of two copies of C9orf72 hexanucleotide repeat intermediate-length alleles is a risk factor for ALS in the Finnish population.

Authors:  Hannu Laaksovirta; Pentti J Tienari; Karri Kaivola; Samuli J Salmi; Lilja Jansson; Jyrki Launes; Laura Hokkanen; Anna-Kaisa Niemi; Kari Majamaa; Jari Lahti; Johan G Eriksson; Timo Strandberg
Journal:  Acta Neuropathol Commun       Date:  2020-11-09       Impact factor: 7.578
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