Distribution, type and origin of Parkin mutations: Review and case studies

Katja Hedrich; Cordula Eskelson; Beth Wilmot; Karen Marder; Juliette Harris; Jennifer Garrels; Helen Meija-Santana; Peter Vieregge; Helfried Jacobs; Susan B. Bressman; Anthony E. Lang; Martin Kann; Giovanni Abbruzzese; Paolo Martinelli; Eberhard Schwinger; Laurie J. Ozelius; Peter P. Pramstaller; Christine Klein; Patricia Kramer

doi:10.1002/mds.20234

Distribution, type and origin of Parkin mutations: Review and case studies

Katja Hedrich, Cordula Eskelson, Beth Wilmot, Karen Marder, Juliette Harris, Jennifer Garrels, Helen Meija-Santana, Peter Vieregge, Helfried Jacobs, Susan B. Bressman, Anthony E. Lang, Martin Kann, Giovanni Abbruzzese, Paolo Martinelli, Eberhard Schwinger, Laurie J. Ozelius, Peter P. Pramstaller, Christine Klein, Patricia Kramer

Research output: Contribution to journal › Article › peer-review

189 Scopus citations

Abstract

Early-onset Parkinson's disease (PD) has been associated with different mutations in the Parkin gene (PARK2). To study distribution and type of Parkin mutations, we carried out a comprehensive literature review that demonstrated two prominent types of mutations among 359 unrelated mutation carriers: exon rearrangements involving exon 3, 4, or both, and alterations in exons 2 and 7, suggesting mutational hot spots a founders. To elucidate the origin of 14 recurrent Parkin mutations in our samples, we carried out a detailed haplotype analysis at the PARK2 locus. Thirty-eight mutation-positive individuals, available family members, and 62 mutation-negative individuals were genotyped. We determined allele frequencies and linkage disequilibrium (LD) to evaluate the significance of shared haplotypes. We observed no LD between markers at PARK2. Our data support a common for the most frequent Parkin point mutation (924C>T; exon 7) and indicate a mutational hot spot as cause of a common small deletion (255/256delA; exon 2). Furthermore, the most frequent Parkin exon deletion (Ex4del) arose independently in 2 of our subjects. However, it also occurred as the result of a founder mutation in 2 cases that shared identical deletion break points. This study provides evidence for both mutational hot spots and founder mutations as a source of recurrent mutation in Parkin, regardless of the mutation type.

Original language	English (US)
Pages (from-to)	1146-1157
Number of pages	12
Journal	Movement Disorders
Volume	19
Issue number	10
DOIs	https://doi.org/10.1002/mds.20234
State	Published - Oct 2004

Keywords

Break point analysis
Distribution
Linkage disequilibrium
Origin
Parkin
Recurrent mutations

ASJC Scopus subject areas

Neurology
Clinical Neurology

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10.1002/mds.20234

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Hedrich, K., Eskelson, C., Wilmot, B., Marder, K., Harris, J., Garrels, J., Meija-Santana, H., Vieregge, P., Jacobs, H., Bressman, S. B., Lang, A. E., Kann, M., Abbruzzese, G., Martinelli, P., Schwinger, E., Ozelius, L. J., Pramstaller, P. P., Klein, C., & Kramer, P. (2004). Distribution, type and origin of Parkin mutations: Review and case studies. Movement Disorders, 19(10), 1146-1157. https://doi.org/10.1002/mds.20234

Hedrich, K, Eskelson, C, Wilmot, B, Marder, K, Harris, J, Garrels, J, Meija-Santana, H, Vieregge, P, Jacobs, H, Bressman, SB, Lang, AE, Kann, M, Abbruzzese, G, Martinelli, P, Schwinger, E, Ozelius, LJ, Pramstaller, PP, Klein, C & Kramer, P 2004, 'Distribution, type and origin of Parkin mutations: Review and case studies', Movement Disorders, vol. 19, no. 10, pp. 1146-1157. https://doi.org/10.1002/mds.20234

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abstract = "Early-onset Parkinson's disease (PD) has been associated with different mutations in the Parkin gene (PARK2). To study distribution and type of Parkin mutations, we carried out a comprehensive literature review that demonstrated two prominent types of mutations among 359 unrelated mutation carriers: exon rearrangements involving exon 3, 4, or both, and alterations in exons 2 and 7, suggesting mutational hot spots a founders. To elucidate the origin of 14 recurrent Parkin mutations in our samples, we carried out a detailed haplotype analysis at the PARK2 locus. Thirty-eight mutation-positive individuals, available family members, and 62 mutation-negative individuals were genotyped. We determined allele frequencies and linkage disequilibrium (LD) to evaluate the significance of shared haplotypes. We observed no LD between markers at PARK2. Our data support a common for the most frequent Parkin point mutation (924C>T; exon 7) and indicate a mutational hot spot as cause of a common small deletion (255/256delA; exon 2). Furthermore, the most frequent Parkin exon deletion (Ex4del) arose independently in 2 of our subjects. However, it also occurred as the result of a founder mutation in 2 cases that shared identical deletion break points. This study provides evidence for both mutational hot spots and founder mutations as a source of recurrent mutation in Parkin, regardless of the mutation type.",

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AU - Garrels, Jennifer

AU - Meija-Santana, Helen

AU - Vieregge, Peter

AU - Jacobs, Helfried

AU - Bressman, Susan B.

AU - Lang, Anthony E.

AU - Kann, Martin

AU - Abbruzzese, Giovanni

AU - Martinelli, Paolo

AU - Schwinger, Eberhard

AU - Ozelius, Laurie J.

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AB - Early-onset Parkinson's disease (PD) has been associated with different mutations in the Parkin gene (PARK2). To study distribution and type of Parkin mutations, we carried out a comprehensive literature review that demonstrated two prominent types of mutations among 359 unrelated mutation carriers: exon rearrangements involving exon 3, 4, or both, and alterations in exons 2 and 7, suggesting mutational hot spots a founders. To elucidate the origin of 14 recurrent Parkin mutations in our samples, we carried out a detailed haplotype analysis at the PARK2 locus. Thirty-eight mutation-positive individuals, available family members, and 62 mutation-negative individuals were genotyped. We determined allele frequencies and linkage disequilibrium (LD) to evaluate the significance of shared haplotypes. We observed no LD between markers at PARK2. Our data support a common for the most frequent Parkin point mutation (924C>T; exon 7) and indicate a mutational hot spot as cause of a common small deletion (255/256delA; exon 2). Furthermore, the most frequent Parkin exon deletion (Ex4del) arose independently in 2 of our subjects. However, it also occurred as the result of a founder mutation in 2 cases that shared identical deletion break points. This study provides evidence for both mutational hot spots and founder mutations as a source of recurrent mutation in Parkin, regardless of the mutation type.

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Distribution, type and origin of Parkin mutations: Review and case studies

Abstract

Keywords

ASJC Scopus subject areas

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