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Clinical spectrum of homozygous and heterozygous PINK1 mutations in a large German family with Parkinson disease: role of a single hit?

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Clinical spectrum of homozygous and heterozygous PINK1 mutations in a large German family with Parkinson disease: role of a single hit? / Hedrich, Katja; Hagenah, Johann; Djarmati, Ana; Hiller, Anja; Lohnau, Thora; Lasek, Kathrin; Grünewald, Anne; Hilker, Rüdiger; Steinlechner, Susanne; Boston, Heather; Kock, Norman; Schneider-Gold, Christiane; Kress, Wolfram; Siebner, Hartwig; Binkofski, Ferdinand; Lencer, Rebekka; Münchau, Alexander; Klein, Christine.

in: ARCH NEUROL-CHICAGO, Jahrgang 63, Nr. 6, 6, 2006, S. 833-838.

Publikationen: SCORING: Beitrag in Fachzeitschrift/ZeitungSCORING: ZeitschriftenaufsatzForschungBegutachtung

Harvard

Hedrich, K, Hagenah, J, Djarmati, A, Hiller, A, Lohnau, T, Lasek, K, Grünewald, A, Hilker, R, Steinlechner, S, Boston, H, Kock, N, Schneider-Gold, C, Kress, W, Siebner, H, Binkofski, F, Lencer, R, Münchau, A & Klein, C 2006, 'Clinical spectrum of homozygous and heterozygous PINK1 mutations in a large German family with Parkinson disease: role of a single hit?', ARCH NEUROL-CHICAGO, Jg. 63, Nr. 6, 6, S. 833-838. <http://www.ncbi.nlm.nih.gov/pubmed/16769864?dopt=Citation>

APA

Hedrich, K., Hagenah, J., Djarmati, A., Hiller, A., Lohnau, T., Lasek, K., Grünewald, A., Hilker, R., Steinlechner, S., Boston, H., Kock, N., Schneider-Gold, C., Kress, W., Siebner, H., Binkofski, F., Lencer, R., Münchau, A., & Klein, C. (2006). Clinical spectrum of homozygous and heterozygous PINK1 mutations in a large German family with Parkinson disease: role of a single hit? ARCH NEUROL-CHICAGO, 63(6), 833-838. [6]. http://www.ncbi.nlm.nih.gov/pubmed/16769864?dopt=Citation

Vancouver

Hedrich K, Hagenah J, Djarmati A, Hiller A, Lohnau T, Lasek K et al. Clinical spectrum of homozygous and heterozygous PINK1 mutations in a large German family with Parkinson disease: role of a single hit? ARCH NEUROL-CHICAGO. 2006;63(6):833-838. 6.

Bibtex

@article{28277d28132042b4ab924dd9ad4098bd,
title = "Clinical spectrum of homozygous and heterozygous PINK1 mutations in a large German family with Parkinson disease: role of a single hit?",
abstract = "BACKGROUND: Although homozygous mutations in the PTEN-induced putative kinase 1 (PINK1) gene have been unequivocally associated with early-onset Parkinson disease (PD), the role of single heterozygous PINK1 mutations is less clear. OBJECTIVE: To investigate the role of homozygous and heterozygous PINK1 mutations in a large German pedigree (family W). DESIGN: Mutation analysis of PINK1 and results of standardized neurological and motor examination by 3 independent movement disorder specialists, including blinded video rating. SETTINGS: University of L{\"u}beck. PARTICIPANTS: Twenty family members. MAIN OUTCOME MEASURES: The PINK1 genotype and PD status of all family members. RESULTS: The index patient of family W carried a homozygous nonsense mutation (c.1366C>T; p.Q456X) and presented with a phenotype closely resembling idiopathic PD but with an onset at 39 years of age. The family included a total of 4 affected homozygous members (age, 60-71 years; age at onset, 39-61 years), 6 members with slight or mild signs of PD (affected) and a heterozygous mutation (age, 31-49 years), and 5 unaffected heterozygous mutation carriers (age, 34-44 years). Although none of the heterozygous affected family members was aware of their signs (asymptomatic), the clinical findings were unequivocal and predominantly or exclusively present on their dominant right-hand side, eg, unilaterally reduced or absent arm swing and unilateral rigidity. The heterozygous members were all considerably younger than the affected homozygous mutation carriers. CONCLUSIONS: Heterozygous PINK1 mutations may predispose to PD, as was previously suggested by the presence of dopamine hypometabolism in asymptomatic mutation carriers. Long-term follow-up of our large family W provides an excellent opportunity to further evaluate the role of single heterozygous PINK1 mutations later in life, which will have major implications on genetic counseling.",
author = "Katja Hedrich and Johann Hagenah and Ana Djarmati and Anja Hiller and Thora Lohnau and Kathrin Lasek and Anne Gr{\"u}newald and R{\"u}diger Hilker and Susanne Steinlechner and Heather Boston and Norman Kock and Christiane Schneider-Gold and Wolfram Kress and Hartwig Siebner and Ferdinand Binkofski and Rebekka Lencer and Alexander M{\"u}nchau and Christine Klein",
year = "2006",
language = "Deutsch",
volume = "63",
pages = "833--838",
number = "6",

}

RIS

TY - JOUR

T1 - Clinical spectrum of homozygous and heterozygous PINK1 mutations in a large German family with Parkinson disease: role of a single hit?

AU - Hedrich, Katja

AU - Hagenah, Johann

AU - Djarmati, Ana

AU - Hiller, Anja

AU - Lohnau, Thora

AU - Lasek, Kathrin

AU - Grünewald, Anne

AU - Hilker, Rüdiger

AU - Steinlechner, Susanne

AU - Boston, Heather

AU - Kock, Norman

AU - Schneider-Gold, Christiane

AU - Kress, Wolfram

AU - Siebner, Hartwig

AU - Binkofski, Ferdinand

AU - Lencer, Rebekka

AU - Münchau, Alexander

AU - Klein, Christine

PY - 2006

Y1 - 2006

N2 - BACKGROUND: Although homozygous mutations in the PTEN-induced putative kinase 1 (PINK1) gene have been unequivocally associated with early-onset Parkinson disease (PD), the role of single heterozygous PINK1 mutations is less clear. OBJECTIVE: To investigate the role of homozygous and heterozygous PINK1 mutations in a large German pedigree (family W). DESIGN: Mutation analysis of PINK1 and results of standardized neurological and motor examination by 3 independent movement disorder specialists, including blinded video rating. SETTINGS: University of Lübeck. PARTICIPANTS: Twenty family members. MAIN OUTCOME MEASURES: The PINK1 genotype and PD status of all family members. RESULTS: The index patient of family W carried a homozygous nonsense mutation (c.1366C>T; p.Q456X) and presented with a phenotype closely resembling idiopathic PD but with an onset at 39 years of age. The family included a total of 4 affected homozygous members (age, 60-71 years; age at onset, 39-61 years), 6 members with slight or mild signs of PD (affected) and a heterozygous mutation (age, 31-49 years), and 5 unaffected heterozygous mutation carriers (age, 34-44 years). Although none of the heterozygous affected family members was aware of their signs (asymptomatic), the clinical findings were unequivocal and predominantly or exclusively present on their dominant right-hand side, eg, unilaterally reduced or absent arm swing and unilateral rigidity. The heterozygous members were all considerably younger than the affected homozygous mutation carriers. CONCLUSIONS: Heterozygous PINK1 mutations may predispose to PD, as was previously suggested by the presence of dopamine hypometabolism in asymptomatic mutation carriers. Long-term follow-up of our large family W provides an excellent opportunity to further evaluate the role of single heterozygous PINK1 mutations later in life, which will have major implications on genetic counseling.

AB - BACKGROUND: Although homozygous mutations in the PTEN-induced putative kinase 1 (PINK1) gene have been unequivocally associated with early-onset Parkinson disease (PD), the role of single heterozygous PINK1 mutations is less clear. OBJECTIVE: To investigate the role of homozygous and heterozygous PINK1 mutations in a large German pedigree (family W). DESIGN: Mutation analysis of PINK1 and results of standardized neurological and motor examination by 3 independent movement disorder specialists, including blinded video rating. SETTINGS: University of Lübeck. PARTICIPANTS: Twenty family members. MAIN OUTCOME MEASURES: The PINK1 genotype and PD status of all family members. RESULTS: The index patient of family W carried a homozygous nonsense mutation (c.1366C>T; p.Q456X) and presented with a phenotype closely resembling idiopathic PD but with an onset at 39 years of age. The family included a total of 4 affected homozygous members (age, 60-71 years; age at onset, 39-61 years), 6 members with slight or mild signs of PD (affected) and a heterozygous mutation (age, 31-49 years), and 5 unaffected heterozygous mutation carriers (age, 34-44 years). Although none of the heterozygous affected family members was aware of their signs (asymptomatic), the clinical findings were unequivocal and predominantly or exclusively present on their dominant right-hand side, eg, unilaterally reduced or absent arm swing and unilateral rigidity. The heterozygous members were all considerably younger than the affected homozygous mutation carriers. CONCLUSIONS: Heterozygous PINK1 mutations may predispose to PD, as was previously suggested by the presence of dopamine hypometabolism in asymptomatic mutation carriers. Long-term follow-up of our large family W provides an excellent opportunity to further evaluate the role of single heterozygous PINK1 mutations later in life, which will have major implications on genetic counseling.

M3 - SCORING: Zeitschriftenaufsatz

VL - 63

SP - 833

EP - 838

IS - 6

M1 - 6

ER -