Phenotypic heterogeneity and genetic modification of P102L inherited prion disease in an international series

MD Geshwind; AH Nemeth; S Wroe; J Collinge; S Mead; S Brandner; S Pal; D Siddique; JD Wadsworth; S Joiner; K Alner; C Peterson; S Hampson; C Rhymes; C Treacy; E Storey; TE Webb; M Poulter; J Beck; J Uphill; G Adamson; T Campbell; J Linehan; C Powell

doi:10.1093/brain/awn202

Phenotypic heterogeneity and genetic modification of P102L inherited prion disease in an international series

MD Geshwind, AH Nemeth, S Wroe, J Collinge, S Mead, S Brandner, S Pal, D Siddique, JD Wadsworth, S Joiner, K Alner, C Peterson, S Hampson, C Rhymes, C Treacy, E Storey, TE Webb, M Poulter, J Beck, J UphillG Adamson, T Campbell, J Linehan, C Powell

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

Abstract

The largest kindred with inherited prion disease P102L, historically Gerstmann-Straussler-Scheinker syndrome, originates from central England, with emigres now resident in various parts of the English-speaking world. We have collected data from 84 patients in the large UK kindred and numerous small unrelated pedigrees to investigate phenotypic heterogeneity and modifying factors. This collection represents by far the largest series of P102L patients so far reported. Microsatellite and genealogical analyses of eight separate European kindreds support multiple distinct mutational events at a cytosine-phosphate diester-guanidine dinucleotide mutation hot spot. All of the smaller P102L kindreds were linked to polymorphic human prion protein gene codon 129M and were not connected by genealogy or microsatellite haplotype background to the large kindred or each other. While many present with classical Gerstmann-Straussler-Scheinker syndrome, a slowly progressive cerebellar ataxia with later onset cognitive impairment, there is remarkable heterogeneity. A subset of patients present with prominent cognitive and psychiatric features and some have met diagnostic criteria for sporadic Creutzfeldt-Jakob disease. We show that polymorphic human prion protein gene codon 129 modifies age at onset: the earliest eight clinical onsets were all MM homozygotes and overall age at onset was 7 years earlier for MM compared with MV heterozygotes (P = 0.02). Unexpectedly, apolipoprotein E4 carriers have a delayed age of onset by 10 years (P = 0.02). We found a preponderance of female patients compared with males (54 females versus 30 males, P = 0.01), which probably relates to ascertainment bias. However, these modifiers had no impact on a semi-quantitative pathological phenotype in 10 autopsied patients. These data allow an appreciation of the range of clinical phenotype, modern imaging and molecular investigation and should inform genetic counselling of at-risk individuals, with the identification of two genetic modifiers.

Original language	English
Pages (from-to)	2632-2646
Journal	Brain
Volume	131
DOIs	https://doi.org/10.1093/brain/awn202
Publication status	Published - 2008

Bibliographical note

Note: Funding: Medical Research Council; Department of Health's NIHR Biomedical Research Centres, Department of Health.

Keywords

Pre-clinical and human biological sciences

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10.1093/brain/awn202

http://dx.doi.org/10.1093/brain/awn202

Cite this

Geshwind, MD., Nemeth, AH., Wroe, S., Collinge, J., Mead, S., Brandner, S., Pal, S., Siddique, D., Wadsworth, JD., Joiner, S., Alner, K., Peterson, C., Hampson, S., Rhymes, C., Treacy, C., Storey, E., Webb, TE., Poulter, M., Beck, J., ... Powell, C. (2008). Phenotypic heterogeneity and genetic modification of P102L inherited prion disease in an international series. Brain, 131, 2632-2646. https://doi.org/10.1093/brain/awn202

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title = "Phenotypic heterogeneity and genetic modification of P102L inherited prion disease in an international series",

abstract = "The largest kindred with inherited prion disease P102L, historically Gerstmann-Straussler-Scheinker syndrome, originates from central England, with emigres now resident in various parts of the English-speaking world. We have collected data from 84 patients in the large UK kindred and numerous small unrelated pedigrees to investigate phenotypic heterogeneity and modifying factors. This collection represents by far the largest series of P102L patients so far reported. Microsatellite and genealogical analyses of eight separate European kindreds support multiple distinct mutational events at a cytosine-phosphate diester-guanidine dinucleotide mutation hot spot. All of the smaller P102L kindreds were linked to polymorphic human prion protein gene codon 129M and were not connected by genealogy or microsatellite haplotype background to the large kindred or each other. While many present with classical Gerstmann-Straussler-Scheinker syndrome, a slowly progressive cerebellar ataxia with later onset cognitive impairment, there is remarkable heterogeneity. A subset of patients present with prominent cognitive and psychiatric features and some have met diagnostic criteria for sporadic Creutzfeldt-Jakob disease. We show that polymorphic human prion protein gene codon 129 modifies age at onset: the earliest eight clinical onsets were all MM homozygotes and overall age at onset was 7 years earlier for MM compared with MV heterozygotes (P = 0.02). Unexpectedly, apolipoprotein E4 carriers have a delayed age of onset by 10 years (P = 0.02). We found a preponderance of female patients compared with males (54 females versus 30 males, P = 0.01), which probably relates to ascertainment bias. However, these modifiers had no impact on a semi-quantitative pathological phenotype in 10 autopsied patients. These data allow an appreciation of the range of clinical phenotype, modern imaging and molecular investigation and should inform genetic counselling of at-risk individuals, with the identification of two genetic modifiers.",

keywords = "Pre-clinical and human biological sciences",

author = "MD Geshwind and AH Nemeth and S Wroe and J Collinge and S Mead and S Brandner and S Pal and D Siddique and JD Wadsworth and S Joiner and K Alner and C Peterson and S Hampson and C Rhymes and C Treacy and E Storey and TE Webb and M Poulter and J Beck and J Uphill and G Adamson and T Campbell and J Linehan and C Powell",

note = "Note: Funding: Medical Research Council; Department of Health's NIHR Biomedical Research Centres, Department of Health.",

year = "2008",

doi = "10.1093/brain/awn202",

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Geshwind, MD, Nemeth, AH, Wroe, S, Collinge, J, Mead, S, Brandner, S, Pal, S, Siddique, D, Wadsworth, JD, Joiner, S, Alner, K, Peterson, C, Hampson, S, Rhymes, C, Treacy, C, Storey, E, Webb, TE, Poulter, M, Beck, J, Uphill, J, Adamson, G, Campbell, T, Linehan, J & Powell, C 2008, 'Phenotypic heterogeneity and genetic modification of P102L inherited prion disease in an international series', Brain, vol. 131, pp. 2632-2646. https://doi.org/10.1093/brain/awn202

TY - JOUR

T1 - Phenotypic heterogeneity and genetic modification of P102L inherited prion disease in an international series

AU - Geshwind, MD

AU - Nemeth, AH

AU - Wroe, S

AU - Collinge, J

AU - Mead, S

AU - Brandner, S

AU - Pal, S

AU - Siddique, D

AU - Wadsworth, JD

AU - Joiner, S

AU - Alner, K

AU - Peterson, C

AU - Hampson, S

AU - Rhymes, C

AU - Treacy, C

AU - Storey, E

AU - Webb, TE

AU - Poulter, M

AU - Beck, J

AU - Uphill, J

AU - Adamson, G

AU - Campbell, T

AU - Linehan, J

AU - Powell, C

N1 - Note: Funding: Medical Research Council; Department of Health's NIHR Biomedical Research Centres, Department of Health.

PY - 2008

Y1 - 2008

N2 - The largest kindred with inherited prion disease P102L, historically Gerstmann-Straussler-Scheinker syndrome, originates from central England, with emigres now resident in various parts of the English-speaking world. We have collected data from 84 patients in the large UK kindred and numerous small unrelated pedigrees to investigate phenotypic heterogeneity and modifying factors. This collection represents by far the largest series of P102L patients so far reported. Microsatellite and genealogical analyses of eight separate European kindreds support multiple distinct mutational events at a cytosine-phosphate diester-guanidine dinucleotide mutation hot spot. All of the smaller P102L kindreds were linked to polymorphic human prion protein gene codon 129M and were not connected by genealogy or microsatellite haplotype background to the large kindred or each other. While many present with classical Gerstmann-Straussler-Scheinker syndrome, a slowly progressive cerebellar ataxia with later onset cognitive impairment, there is remarkable heterogeneity. A subset of patients present with prominent cognitive and psychiatric features and some have met diagnostic criteria for sporadic Creutzfeldt-Jakob disease. We show that polymorphic human prion protein gene codon 129 modifies age at onset: the earliest eight clinical onsets were all MM homozygotes and overall age at onset was 7 years earlier for MM compared with MV heterozygotes (P = 0.02). Unexpectedly, apolipoprotein E4 carriers have a delayed age of onset by 10 years (P = 0.02). We found a preponderance of female patients compared with males (54 females versus 30 males, P = 0.01), which probably relates to ascertainment bias. However, these modifiers had no impact on a semi-quantitative pathological phenotype in 10 autopsied patients. These data allow an appreciation of the range of clinical phenotype, modern imaging and molecular investigation and should inform genetic counselling of at-risk individuals, with the identification of two genetic modifiers.

AB - The largest kindred with inherited prion disease P102L, historically Gerstmann-Straussler-Scheinker syndrome, originates from central England, with emigres now resident in various parts of the English-speaking world. We have collected data from 84 patients in the large UK kindred and numerous small unrelated pedigrees to investigate phenotypic heterogeneity and modifying factors. This collection represents by far the largest series of P102L patients so far reported. Microsatellite and genealogical analyses of eight separate European kindreds support multiple distinct mutational events at a cytosine-phosphate diester-guanidine dinucleotide mutation hot spot. All of the smaller P102L kindreds were linked to polymorphic human prion protein gene codon 129M and were not connected by genealogy or microsatellite haplotype background to the large kindred or each other. While many present with classical Gerstmann-Straussler-Scheinker syndrome, a slowly progressive cerebellar ataxia with later onset cognitive impairment, there is remarkable heterogeneity. A subset of patients present with prominent cognitive and psychiatric features and some have met diagnostic criteria for sporadic Creutzfeldt-Jakob disease. We show that polymorphic human prion protein gene codon 129 modifies age at onset: the earliest eight clinical onsets were all MM homozygotes and overall age at onset was 7 years earlier for MM compared with MV heterozygotes (P = 0.02). Unexpectedly, apolipoprotein E4 carriers have a delayed age of onset by 10 years (P = 0.02). We found a preponderance of female patients compared with males (54 females versus 30 males, P = 0.01), which probably relates to ascertainment bias. However, these modifiers had no impact on a semi-quantitative pathological phenotype in 10 autopsied patients. These data allow an appreciation of the range of clinical phenotype, modern imaging and molecular investigation and should inform genetic counselling of at-risk individuals, with the identification of two genetic modifiers.

KW - Pre-clinical and human biological sciences

UR - http://www.ncbi.nlm.nih.gov/pubmed/18757886

U2 - 10.1093/brain/awn202

DO - 10.1093/brain/awn202

M3 - Article

C2 - 18757886

SN - 0006-8950

VL - 131

SP - 2632

EP - 2646

JO - Brain

JF - Brain

ER -

Phenotypic heterogeneity and genetic modification of P102L inherited prion disease in an international series

Abstract

Bibliographical note

Keywords

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