Phenotypic variability in ARCA2 and identification of a core ataxic phenotype with slow progression

Cyril Mignot,Marlène Rio,Pascale De Lonlay,Agnès Rötig,Sandrine Canaple,Caroline Moreau,Nathalie Drouot,Elsa Nourisson,Isabelle Desguerre,David Devos,Nadine Kempf,Emmanuelle Apartis,Perrine Charles,Coralie Rastel,Charles Marques Lourenço,Emmanuel Roze,Yves Chaix,Alexis Brice,Mathieu Anheim,Sandra Chantot‐Bastaraud ,C Tranchant ,Alexandra Dürr ,Éric Bieth ,I Bonnet ,Lydie Bürglen ,M Kœnig ,Anne-Sophie Lèbre

doi:10.1186/1750-1172-8-173

Abstract

Autosomal recessive cerebellar ataxia 2 (ARCA2) is a recently identified recessive ataxia due to ubiquinone deficiency and biallelic mutations in the ADCK3 gene. The phenotype of the twenty-one patients reported worldwide varies greatly. Thus, it is difficult to decide which ataxic patients are good candidates for ADCK3 screening without evidence of ubiquinone deficiency. We report here the clinical and molecular data of 10 newly diagnosed patients from seven families and update the disease history of four additional patients reported in previous articles to delineate the clinical spectrum of ARCA2 phenotype and to provide a guide to the molecular diagnosis. First signs occurred before adulthood in all 14 patients. Cerebellar atrophy appeared in all instances. The progressivity and severity of ataxia varied greatly, but no patients had the typical inexorable ataxic course that characterizes other childhood-onset recessive ataxias. The ataxia was frequently associated with other neurological signs. Importantly, stroke-like episodes contributed to significant deterioration of the neurological status in two patients. Ubidecarenone therapy markedly improved the movement disorders, including ataxia, in two other patients. The 7 novel ADCK3 mutations found in the 10 new patients were two missense and five truncating mutations. There was no apparent correlation between the genotype and the phenotype. Our series reveals that the clinical spectrum of ARCA2 encompasses a range of ataxic phenotypes. On one end, it may manifest as a pure ataxia with very slow progressivity and, on the other end, as a severe infantile encephalopathy with cerebellar atrophy. The phenotype of most patients, however, lies in between. It is characterized by a very slowly progressive or apparently stable ataxia associated with other signs of central nervous system involvement. We suggest undergoing the molecular analysis of ADCK3 in patients with this phenotype and in those with cerebellar atrophy and a stroke-like episode. The diagnosis of patients with a severe ARCA2 phenotype may also be performed on the basis of biological data, i.e. low ubiquinone level or functional evidence of ubiquinone deficiency. This diagnosis is crucial since the neurological status of some patients may be improved by ubiquinone therapy.

Highlights

Autosomal recessive cerebellar ataxias (ARCAs) are a group of neurodegenerative disorders defined by a persistent and gradually worsening disorder of gait and balance or with the development over months or years of hypotonia or excessive clumsiness [1]
General data The 10 new patients with ADCK3 mutations identified since the first report were six females and four males, including six individuals from three unrelated sibships and four sporadic cases
The description of the phenotype in the 14 patients reported here together with that of other patients of the literature (Additional file 3: Table S2) allows us to give an accurate picture of the Autosomal recessive cerebellar ataxia 2 (ARCA2) from the first signs to adulthood and throughout adulthood

Summary

Introduction

Autosomal recessive cerebellar ataxias (ARCAs) are a group of neurodegenerative disorders defined by a persistent and gradually worsening disorder of gait and balance or with the development over months or years of hypotonia or excessive clumsiness [1]. ARCA2 is a recently identified entity reported in 21 patients worldwide [2-6]. It is due to recessive mutations in the ADCK3/ CABC1 gene leading to coenzyme Q10 (CoQ10) deficiency, and is known as COQ10D4 and SCAR9 (spinocerebellar ataxia recessive 9, MIM #612016). If the parents of the patient are healthy, the hypothesis of a recessive ataxia is reasonable and molecular studies will be guided by clinical, radiological and biological findings. If variants of unknown significance are identified in ADCK3 with new generation sequencing analyses, the diagnostic process will be guided by their clinical relevance

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