The multistep hypothesis of ALS revisited

Author:

Chiò Adriano,Mazzini Letizia,D'Alfonso Sandra,Corrado Lucia,Canosa Antonio,Moglia Cristina,Manera Umberto,Bersano Enrica,Brunetti Maura,Barberis Marco,Veldink Jan H.,van den Berg Leonard H.,Pearce Neil,Sproviero William,McLaughlin Russell,Vajda Alice,Hardiman Orla,Rooney James,Mora Gabriele,Calvo Andrea,Al-Chalabi Ammar

Abstract

ObjectiveAmyotrophic lateral sclerosis (ALS) incidence rates are consistent with the hypothesis that ALS is a multistep process. We tested the hypothesis that carrying a large effect mutation might account for ≥1 steps through the effect of the mutation, thus leaving fewer remaining steps before ALS begins.MethodsWe generated incidence data from an ALS population register in Italy (2007–2015) for which genetic analysis for C9orf72, SOD1, TARDBP, and FUS genes was performed in 82% of incident cases. As confirmation, we used data from ALS cases diagnosed in the Republic of Ireland (2006–2014). We regressed the log of age-specific incidence against the log of age with least-squares regression for the subpopulation carrying disease-associated variation in each separate gene.ResultsOf the 1,077 genetically tested cases, 74 (6.9%) carried C9orf72 mutations, 20 (1.9%) had SOD1 mutations, 15 (1.4%) had TARDBP mutations, and 3 (0.3%) carried FUS mutations. In the whole population, there was a linear relationship between log incidence and log age (r2 = 0.98) with a slope estimate of 4.65 (4.37–4.95), consistent with a 6-step process. The analysis for C9orf72-mutated patients confirmed a linear relationship (r2 = 0.94) with a slope estimate of 2.22 (1.74–2.29), suggesting a 3-step process. This estimate was confirmed by data from the Irish ALS register. The slope estimate was consistent with a 2-step process for SOD1 and with a 4-step process for TARDBP.ConclusionThe identification of a reduced number of steps in patients with ALS with genetic mutations compared to those without mutations supports the idea of ALS as a multistep process and is an important advance for dissecting the pathogenic process in ALS.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Neurology (clinical)

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