Introduction

Dominantly inherited spinocerebellar ataxias (SCA), a group of neurodegenerative diseases affecting the cerebellum and/or its afferent/efferent tracts, are characterized by genetic and clinical heterogeneity. The mutations remain unknown in 20–60% of cases, depending on their geographical origin. Seven SCAs (1–3, 6, 7, 17, DRPLA) share a common mutational mechanism, abnormal Cytosine, Adenine, Guanine (CAG) repeat expansions in genes encoding proteins containing polyglutamine tracts (polyQ‐SCAs), but also features such as anticipation and multisystem involvement. Natural histories show that polyQ‐SCAs have distinguishing features; SCA6, in particular, has later onset and slower progression. In other SCAs, point mutations (SCA5, 11, 13, 14, 15/16, 19/22, 21, 23, 28, 35, and 38), rearrangements (15/16, 20) or non‐coding repeat expansions (8, 10, 31, and 36) are found. The pathological mechanisms are mostly unknown and each subtype is very rare. In this study, we analyzed survival and severity in 446 families with polyQ‐SCAs and other mutations.

Patients and Methods

Between 1991 and 2013, we identified 446 index cases with known SCA mutations and 509 affected relatives at the Pitié‐Salpêtrière University Hospital in Paris and through the SPATAX network (spatax.wordpress.com). Molecular analyses were performed in the Neurogenetics Unit of the Pitié‐Salpêtrière University Hospital, the Brain and Spine Institute (ICM) and collaborating centers. All participants signed informed consent forms (RBM 01‐29, RBM 03‐48).

We determined age at onset, age when help was needed walking or a wheelchair in 446 index cases and 509 relatives. Age at death, however, was determined in 332 parents of the index cases to limit the bias introduced by index cases still alive, and to include later ages at death. The transmitting parents and their age at death were reported by the index cases; 16% (n = 63) were examined. In 45/114, information concerning the parents was obtained through registers in their place of birth, but remained unknown for 53 transmitting parents. Survival was determined with the Kaplan–Meier estimator.

Causes of death were presumed to be related to the disease, but we cannot exclude that a limited number of other pathologies were responsible. Missing ages when aid walking or wheelchair use where needed were estimated by multiple imputations using the Markov Chain Monte Carlo method. Imputed data were determined as a function of the gene involved and, for the polyQ‐SCAs, the length of the CAG repeat, and analyzed using Cox models. The null hypothesis was rejected for P < 0.05. Statistical analysis was performed with SAS software (version 9.3; SAS Institute, Cary, NC). Data are expressed as the mean ± SD [minimum–maximum].

Results

Index cases were divided into two groups: polyQ‐SCAs and other known SCAs (Table ); 46% were women in both groups. Among the polyQ group, SCA1 (n = 166), SCA2 (n = 173), SCA3 (n = 301), SCA6 (n = 33) and SCA7 (n = 132) were distinguished. Index cases with polyQ‐SCAs (38.4 ± 13.2 [3–78] years, n = 381/392 with information) tended to be older than the others, but not significantly (37.0 ± 16.6 [1–63] years, n = 51/54, P = 0.51); if affected relatives were included in the calculation, however, polyQ‐SCA patients were significantly older (36.7 ± 13.6 [0–78] (n = 790/814) versus 33.3 ± 16.3 [1–63] (n = 129/141), P = 0.024) (Table ).

Discussion

PolyQ‐SCAs stand out among the dominant cerebellar ataxias because of their high frequency and highly variable clinical features. Based on daily clinical observations, we determined that severity was greater and survival shorter in patients with polyglutamine expansions than in cerebellar ataxias due to other mutations. Survival could not be determined in the other SCAs because of their heterogeneity and rarity. We are aware that distinguishing polyQ‐SCAs from the others might appear artificial. Our aim, however, was to determine specifically the characteristics of the polyQ‐SCA subgroup.

Survival rates according to the SCA genotype revealed that polyQ‐SCA patients have shorter survival, both as a group and individually. We could not correlate survival with CAG repeat number, since it was determined by the age of death of the transmitting parent for whom CAG repeat numbers were not always available. However, since age at onset and severity are dependent on CAG repeat length, survival probably is as well. Because polyQ‐SCAs are more frequent than other SCAs in most countries, published survival or mortality rates are often restricted to the former; for example, SCA3. In our cohort, mean disease duration until death was 19.3 ± 9.7 years in polyQ‐SCAs, which is comparable to previous reports.

The mean age at death in our cohort (66 years [SD 65–67]; median: 68 years [CI 95% 65–70]) is earlier than the mean age at death in the Swedish Registry study (75 [SD 64–82] years) that included unspecified inherited ataxias. This could be due to a smaller proportion of polyQ‐SCA patients in Sweden, as in other Scandinavian countries; the median age at death in other SCAs in our study was 80 [73–84] years (mean: 79 years).

There was a possible bias in favor of later deaths in that only persons with descendents were analyzed, excluding juvenile cases. However, the median age at death in the generation of polyQ‐SCA index patients still being followed was 71 years, i.e., close to the mean age at death of the parents (59 deceased, 119 still alive and 268 censored at last visit, data not shown).

We report, for the first time, that the shortest survival in polyQ‐SCAs is in SCA1. Natural histories and clinical characteristics have been well described for SCA1, 2, 3, 6 and 7, as well as SCA17 and DRPLA. CAG repeat size modulates clinical expression, disease duration and phenotype. It is difficult to distinguish between the different polyQ‐SCAs on clinical grounds, but extreme phenotypes may characterize certain SCAs: motor neuron disease in SCA1, chorea in SCA2 or dystonia and spastic ataxia in SCA3, notably in cases with early onset.

In addition to shorter survival, polyQ‐SCA patients also had a more severe disease than those with other SCA mutations. Severity in polyQ‐SCAs was clearly related to repeat size. The influence of repeat size on age at onset in polyQ‐SCAs is well known. The natural history is also significantly influenced by repeat size: the longer the repeat the faster the disease evolves. In SCA1, SCA2 and SCA3, the evolution of SARA scores was mainly determined by the length of the repeat on the expanded allele, age at onset and disease duration. Most polyQ‐SCAs are multisystem disorders characterized by prominent brainstem atrophy, even before disease onset. This also differentiates polyQ‐SCAs from other SCAs in which isolated cerebellar atrophy is frequent.

In conclusion, we determined survival and severity in a large group of polyQ‐SCA patients and individually in those with SCA1, 2, 3, 6, and 7. Of interest, survival in non‐polyQ‐SCAs was similar to that of the French population in general, and disease progression slower than in polyQ‐SCAs despite an earlier age at onset. This observation has to be confirmed in larger populations of other SCAs. Genetic heterogeneity complicates genetic counseling, since information concerning the more frequent subtypes cannot be extrapolated to rarer forms of the disease. This is important for the understanding of these diseases and could have implications for patient care and the design of treatment trials.

Acknowledgments

Many thanks to the patients and families for their help. We are very grateful to Merle Ruberg for her critical reading of the manuscript. We acknowledge the clinicians of the SPATAX network involved in this study: M. Tchikviladzé, M. Anheim, P. Ribai, I. Leber A. Benomar, S. Medjbeur, E. Ollagnon, V. Meininger, A. Vighetto, J. Pouget, C. Tranchant, H. Aliouche, D. Brassat, A. Destee, A. Toutain, C. Goizet, A. Lannuzel, D. Hannequin, A. Lagueny, P. Damier, C. Delpirou, D. Broglin, G. Ponsot, J. C. Pages, A. Autret, C. Vial, P. Labauge, P. Clavelou, P. Amati‐Bonneau, E. Kaphan, R. Bellance, J. M. Leger, C. Desnuelle, P. Coutinho, J. Melki, Y. Boukhriche, V. Paquis, F. Tison, A. Barois, R. Ghnassia, J. Gayon, J. Julien, M. Abada‐Bendib, M. Clanet, J. Guimaraes, Laurent, P. Desfontaines, E. Bieth, M. L. Klimek, S. Schaeffer, P. Calvas, H. Chneiweiss, Bataillard, B. Fontaine, J. C. Netter, P. Bejani, G. Fenelon, D. Grid, J. M. Vallat, F. Viallet, J. P. Azulay, N. Pageot, I. Ferrer, P. Edery, Foubert, J. L. Gastaut, W. Camu, P. Sarda, S. Brique, D. Devos, I. Vuillaume, E. Roze, G. Castelnovo, D. Malapert, T. Fioretos, J. Honnorat, J. Koht, J. Zlotogora, P. Pollak, A. Megarbane, A. David, F. Durif, Bertrandeau, D. Cherif, Ménage, D. Rochefort, L. Faivre, E. Salort, Soulages, P. Vandebergh, P. Jonveaux.

Conflict of Interest

Dr. Durr reports non‐financial support from INSERM, during the conduct of the study; In addition, has a patent N° 14/308,966 issued.

Dr. Stevanin reports grants from Agence National pour la Recherche, from Verum foundation, during the conduct of the study.