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Parkin mutations are frequent in patients with isolated early‐onset parkinsonism

Identifieur interne : 000179 ( France/Analysis ); précédent : 000178; suivant : 000180

Parkin mutations are frequent in patients with isolated early‐onset parkinsonism

Auteurs : Magali Periquet ; Morwena Latouche ; Ebba Lohmann ; Nina Rawal ; Giuseppe De Michele ; Sylvain Ricard ; He Lio Teive ; Vale Rie Fraix ; Marie Vidailhet ; David Nicholl ; Paolo Barone ; Nick W. Wood ; Salmo Raskin ; Jean-Franc Ois Deleuze ; Yves Agid [France] ; Alexandra Du Rr ; Alexis Brice

Source :

RBID : ISTEX:DEB4706B4634B67E45513FF14DEA841395194611

English descriptors

Abstract

Parkin gene mutations are reported to be a major cause of early‐onset parkinsonism (age at onset ≤45 years) in families with autosomal recessive inheritance and in isolated juvenile‐onset parkinsonism (age at onset <20 years). However, the precise frequency of parkin mutations in isolated cases is not known. In order to evaluate the frequency of parkin mutations in patients with isolated early‐onset parkinsonism according to their age at onset, we studied 146 patients of various geographical origin with an age at onset ≤45 years. All were screened for mutations in the parkin gene using semi‐quantitative polymerase chain reaction combined with sequencing of the entire coding region. We identified parkin mutations in 20 patients including three new exon rearrangements and two new missense mutations. These results, taken in conjunction with those of our previous study (Lücking et al., 2000) show that parkin mutations account for at least 15% (38 out of 246) of our early‐onset cases without family history, but that the proportion decreases significantly with increasing age at onset. There were no clinical group differences between parkin cases and other patients with early‐onset parkinsonism. However, a single case presenting with cerebellar ataxia several years before typical parkinsonism extends the spectrum of parkin related‐disease.

Url:
DOI: 10.1093/brain/awg136


Affiliations:


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ISTEX:DEB4706B4634B67E45513FF14DEA841395194611

Le document en format XML

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<term>Abbreviations: PCR = polymerase chain reaction</term>
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<div type="abstract" xml:lang="en">Parkin gene mutations are reported to be a major cause of early‐onset parkinsonism (age at onset ≤45 years) in families with autosomal recessive inheritance and in isolated juvenile‐onset parkinsonism (age at onset <20 years). However, the precise frequency of parkin mutations in isolated cases is not known. In order to evaluate the frequency of parkin mutations in patients with isolated early‐onset parkinsonism according to their age at onset, we studied 146 patients of various geographical origin with an age at onset ≤45 years. All were screened for mutations in the parkin gene using semi‐quantitative polymerase chain reaction combined with sequencing of the entire coding region. We identified parkin mutations in 20 patients including three new exon rearrangements and two new missense mutations. These results, taken in conjunction with those of our previous study (Lücking et al., 2000) show that parkin mutations account for at least 15% (38 out of 246) of our early‐onset cases without family history, but that the proportion decreases significantly with increasing age at onset. There were no clinical group differences between parkin cases and other patients with early‐onset parkinsonism. However, a single case presenting with cerebellar ataxia several years before typical parkinsonism extends the spectrum of parkin related‐disease.</div>
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