ClinVar Genomic variation as it relates to human health
NM_000311.3(PRNP):c.[385A>G;532G>A]
Germline
Classification
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The aggregate germline classification for this variant, typically for a monogenic or Mendelian disorder as in the ACMG/AMP guidelines, or for response to a drug. This value is calculated by NCBI based on data from submitters. Read our rules for calculating the aggregate classification.
(2)
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Stars represent the aggregate review status, or the level of review supporting the aggregate germline classification for this VCV record. This value is calculated by NCBI based on data from submitters. Read our rules for calculating the review status. The number of submissions which contribute to this review status is shown in parentheses.
Pathogenic
2
no assertion criteria provided
Somatic
No data submitted for somatic clinical impact
Somatic
No data submitted for oncogenicity
Variant Details
This haplotype includes the following variants
NM_000311.4(PRNP):c.[385A>G;532G>A]
- Other names
-
PRNP, ASP178ASN AND MET129VAL
PRNP, ASP178ASN AND MET129
- Functional consequence
- -
- Links
- ClinGen: CA034774
- OMIM: 176640.0007
- OMIM: 176640.0010
Genes
| Gene | OMIM | ClinGen Gene Dosage Sensitivity Curation |
Variation Viewer
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Links to Variation Viewer, a genome browser to view variation data from NCBI databases. |
Related variants | ||
|---|---|---|---|---|---|---|
| HI score
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The haploinsufficiency score for the gene, curated by ClinGen’s Dosage Sensitivity Curation task team. |
TS score
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The triplosensitivity score for the gene, curated by ClinGen’s Dosage Sensitivity Curation task team. |
Within gene
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The number of variants in ClinVar that are contained within this gene, with a link to view the list of variants. |
All
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The number of variants in ClinVar for this gene, including smaller variants within the gene and larger CNVs that overlap or fully contain the gene. |
|||
| PRNP | - | - |
GRCh38 GRCh37 |
171 | 206 | |
Conditions - Germline
| Condition
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The condition for this variant-condition (RCV) record in ClinVar. |
Classification
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The aggregate germline classification for this variant-condition (RCV) record in ClinVar. The number of submissions that contribute to this aggregate classification is shown in parentheses. (# of submissions) |
Review status
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The aggregate review status for this variant-condition (RCV) record in ClinVar. This value is calculated by NCBI based on data from submitters. Read our rules for calculating the review status. |
Last evaluated
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The most recent date that a submitter evaluated this variant for the condition. |
Variation/condition record
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The RCV accession number, with most recent version number, for the variant-condition record, with a link to the RCV web page. |
|---|---|---|---|---|
| Pathogenic (1) |
no assertion criteria provided
|
Nov 26, 2008 | RCV000014336.33 | |
| Pathogenic (1) |
no assertion criteria provided
|
Nov 26, 2008 | RCV000014337.34 |
Submissions - Germline
| Classification
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The submitted germline classification for each SCV record. (Last evaluated) |
Review status
Help
Stars represent the review status, or the level of review supporting the submitted (SCV) record. This value is calculated by NCBI based on data from the submitter. Read our rules for calculating the review status. This column also includes a link to the submitter’s assertion criteria if provided, and the collection method. (Assertion criteria) |
Condition
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The condition for the classification, provided by the submitter for this submitted (SCV) record. This column also includes the affected status and allele origin of individuals observed with this variant. |
Submitter
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The submitting organization for this submitted (SCV) record. This column also includes the SCV accession and version number, the date this SCV first appeared in ClinVar, and the date that this SCV was last updated in ClinVar. |
More information
Help
This column includes more information supporting the classification, including citations, the comment on classification, and detailed evidence provided as observations of the variant by the submitter. |
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Pathogenic
(Nov 26, 2008)
|
no assertion criteria provided
Method: literature only
|
CREUTZFELDT-JAKOB DISEASE
Affected status: not provided
Allele origin:
germline
|
OMIM
Accession: SCV000034585.2
First in ClinVar: Apr 04, 2013 Last updated: Oct 11, 2015 |
Comment on evidence:
In a Finnish family with Creutzfeldt-Jakob disease (CJD; 123400), Goldfarb et al. (1991) identified a G-to-A transition in the PRNP gene, resulting in an asp178-to-asn … (more)
In a Finnish family with Creutzfeldt-Jakob disease (CJD; 123400), Goldfarb et al. (1991) identified a G-to-A transition in the PRNP gene, resulting in an asp178-to-asn (D178N) substitution. Nieto et al. (1991) found that the D178N mutation was the cause of transmissible CJD in an American family of Dutch descent, an American family of Hungarian descent, and a French family from Brittany. The Finnish family was the only familial CJD identified in that country (Haltia et al., 1991). The pedigree included 15 affected members in 4 generations in a pattern consistent with autosomal dominant inheritance. The mean age at onset was 47, periodic EEG activity was not observed, and the mean duration of illness of 27.5 months was longer than usual in either familial or sporadic CJD. Neuropathologic examination of brain biopsy and autopsy specimens showed spongiform change without amyloid plaques, and brain tissue from 1 patient transmitted disease to a capuchin monkey. Goldfarb et al. (1992) identified the D178N mutation in 7 unrelated families of western European origin, among which a total of 65 members were known to have died from CJD. The mutation was detected in each of 17 tested patients, including at least 1 affected member of each family, and in 16 of 36 of their first-degree relatives, but not in affected families with other mutations, patients with the nonfamilial form of the disease, or 83 healthy control persons. Linkage analysis in informative families yielded a lod score of 5.30, which, because no recombinants were found, strongly suggested that the codon 178 mutation was the cause of the disease. Brown et al. (1992) compared a group of 43 patients from 7 families affected by CJD caused by the D178N mutation to a group of 211 patients with the sporadic form of the disease. In general, the patients with the codon 178 mutation had an earlier age of onset of illness, almost always presenting as an insidious loss of memory, a longer duration of illness, and an absence of periodic EEG activity. Transmission of the disease to primates was accomplished using brain tissue homogenates from 6 of 10 patients, resulting in significantly shorter incubation periods than those due to sporadic CJD inocula. These findings were interpreted as indicating an accelerated induction of polymerized amyloid protein by its mutationally altered template precursor. Brown et al. (1992) suggested that the earlier age of onset in patients with the codon 178 mutation than in the sporadic patient group may reflect differing rates at which normal host precursor protein is converted into amyloid polymer. If one accepts that an altered protein molecule may serve as a nucleating template to initiate and sustain the conversion process, a 1-per-million probability of its random occurrence would equal the worldwide incidence of sporadic CJD. Precursor protein that has a primary structure already altered by the codon 178 mutation can be presumed to have a correspondingly altered 3-dimensional structure, and this structure may facilitate by a million-fold its conversion to the beta-pleated sheet configuration of amyloid fibrils. An exception to the phenotypic rule of early onset found by Brown et al. (1992) was described by Laplanche et al. (1992) in a man with the D178N mutation who was well and professionally active until the age of 57 years when he had onset of loss of memory, vertigo, and disorientation, leading to professional disability 9 months later. The presence of periodic EEG activity also distinguished him from others carrying this mutation. Multiple genetic or environmental factors may modulate the clinical presentation of CJD associated with the codon 178 mutation. On the basis of scrutiny of the NMR structure of the complete 208-residue polypeptide chain of mouse Prnp, Riek et al. (1998) pointed to the hydrogen bond between residues 128 and 178 as providing a structural basis for the observed highly specific influence of the polymorphism at position 129 in human PRNP on the disease phenotype that segregates with the D178N mutation. Familial CJD was first described in the Backer family living in northern Germany (Meggendorfer, 1930). Further clinical and neuropathologic details were reported by others. Autopsies were performed on 3 members of this family in the 1920s and 1940s. Kretzschmar et al. (1995) presented DNA sequencing data from brain tissue that had been embedded in celloidin 72 years previously. PCR amplification of DNA showed the D178N mutation. Goldfarb et al. (1992) demonstrated that the D178N mutation in conjunction with the met129 polymorphism on the same allele (176640.0005) was responsible for fatal familial insomnia (FFI; 600072). They found that CJD was associated with val129 in all 15 affected members of 6 kindreds, whereas met129 was associated with FFI in all 15 affected members of 5 kindreds. Analysis of the PRNP region by Dagvadorj et al. (2002) in 13 families and 2 sporadic patients with either CJD caused by D178N and 129V or FFI caused by D178N and 129M (176640.0010) showed that the D178N chromosomes had independent origins in each affected pedigree or patient. In addition, a de novo spontaneous PRNP mutation was observed in 1 family. Noting that the mutation involving codon 178 occurred at a CpG dinucleotide motif that is considered to be a hotspot for spontaneous human mutations, Dagvadorj et al. (2002) concluded that cases associated with the D178N mutation result from multiple recurrent mutational events. Zarranz et al. (2005) reported 23 patients from 13 Spanish families with prion disease. Nine families were of Basque origin, 6 of which were genetically related by haplotype analysis. They identified 2 patients who were D178N and val/met129 heterozygous with fatal familial insomnia (FFI; 600072). One patient was sporadic, and 1 patient had a relative with the same genotype who presented with CJD. PrPSc isotype analysis was not informative. The largest family had 5 affected individuals. The genotype in all 5 family members was D178N and met129 homozygous (176640.0010) but only 2 presented with FFI. The 3 other family members presented with CJD, 2 with ataxia and 1 with acalculia, aphasia and dementia. In another family with D178N and met129 homozygous, 1 patient had classic FFI presenting with insomnia, 1 had FFI presenting with depression, apathy, and autonomic dysfunction, and 2 other family members presented with CJD. Overall, 7 patients with D178N and met129 homozygous had a clinical and neuropathologic profile compatible with CJD. Zarranz et al. (2005) concluded that there must be other environmental or genetic factors that influence the phenotypic expression of the D178N mutation, and that FFI and CJD due to this genotype are extremes of a phenotypic spectrum rather than 2 discrete entities. Dossena et al. (2008) generated a transgenic mouse model expressing the mouse homolog of the D178N/M129V mutation. These mice developed clinical and pathologic features reminiscent of CJD, including motor dysfunction, memory impairment, cerebral prion protein deposition, and gliosis. Other features included EEG abnormalities and severe alterations of sleep-wake patterns similar to those observed in human patients. Neurons from the mutant mice showed swelling of the endoplasmic reticulum (ER) with intracellular retention of mutant prion protein, suggesting that ER dysfunction could contribute to the pathology of CJD. The mutant protein was protease-resistant and formed aggregations. (less)
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Pathogenic
(Nov 26, 2008)
|
no assertion criteria provided
Method: literature only
|
FATAL FAMILIAL INSOMNIA
Affected status: not provided
Allele origin:
germline
|
OMIM
Accession: SCV000034586.2
First in ClinVar: Apr 04, 2013 Last updated: Oct 11, 2015 |
Comment on evidence:
In a Finnish family with Creutzfeldt-Jakob disease (CJD; 123400), Goldfarb et al. (1991) identified a G-to-A transition in the PRNP gene, resulting in an asp178-to-asn … (more)
In a Finnish family with Creutzfeldt-Jakob disease (CJD; 123400), Goldfarb et al. (1991) identified a G-to-A transition in the PRNP gene, resulting in an asp178-to-asn (D178N) substitution. Nieto et al. (1991) found that the D178N mutation was the cause of transmissible CJD in an American family of Dutch descent, an American family of Hungarian descent, and a French family from Brittany. The Finnish family was the only familial CJD identified in that country (Haltia et al., 1991). The pedigree included 15 affected members in 4 generations in a pattern consistent with autosomal dominant inheritance. The mean age at onset was 47, periodic EEG activity was not observed, and the mean duration of illness of 27.5 months was longer than usual in either familial or sporadic CJD. Neuropathologic examination of brain biopsy and autopsy specimens showed spongiform change without amyloid plaques, and brain tissue from 1 patient transmitted disease to a capuchin monkey. Goldfarb et al. (1992) identified the D178N mutation in 7 unrelated families of western European origin, among which a total of 65 members were known to have died from CJD. The mutation was detected in each of 17 tested patients, including at least 1 affected member of each family, and in 16 of 36 of their first-degree relatives, but not in affected families with other mutations, patients with the nonfamilial form of the disease, or 83 healthy control persons. Linkage analysis in informative families yielded a lod score of 5.30, which, because no recombinants were found, strongly suggested that the codon 178 mutation was the cause of the disease. Brown et al. (1992) compared a group of 43 patients from 7 families affected by CJD caused by the D178N mutation to a group of 211 patients with the sporadic form of the disease. In general, the patients with the codon 178 mutation had an earlier age of onset of illness, almost always presenting as an insidious loss of memory, a longer duration of illness, and an absence of periodic EEG activity. Transmission of the disease to primates was accomplished using brain tissue homogenates from 6 of 10 patients, resulting in significantly shorter incubation periods than those due to sporadic CJD inocula. These findings were interpreted as indicating an accelerated induction of polymerized amyloid protein by its mutationally altered template precursor. Brown et al. (1992) suggested that the earlier age of onset in patients with the codon 178 mutation than in the sporadic patient group may reflect differing rates at which normal host precursor protein is converted into amyloid polymer. If one accepts that an altered protein molecule may serve as a nucleating template to initiate and sustain the conversion process, a 1-per-million probability of its random occurrence would equal the worldwide incidence of sporadic CJD. Precursor protein that has a primary structure already altered by the codon 178 mutation can be presumed to have a correspondingly altered 3-dimensional structure, and this structure may facilitate by a million-fold its conversion to the beta-pleated sheet configuration of amyloid fibrils. An exception to the phenotypic rule of early onset found by Brown et al. (1992) was described by Laplanche et al. (1992) in a man with the D178N mutation who was well and professionally active until the age of 57 years when he had onset of loss of memory, vertigo, and disorientation, leading to professional disability 9 months later. The presence of periodic EEG activity also distinguished him from others carrying this mutation. Multiple genetic or environmental factors may modulate the clinical presentation of CJD associated with the codon 178 mutation. On the basis of scrutiny of the NMR structure of the complete 208-residue polypeptide chain of mouse Prnp, Riek et al. (1998) pointed to the hydrogen bond between residues 128 and 178 as providing a structural basis for the observed highly specific influence of the polymorphism at position 129 in human PRNP on the disease phenotype that segregates with the D178N mutation. Familial CJD was first described in the Backer family living in northern Germany (Meggendorfer, 1930). Further clinical and neuropathologic details were reported by others. Autopsies were performed on 3 members of this family in the 1920s and 1940s. Kretzschmar et al. (1995) presented DNA sequencing data from brain tissue that had been embedded in celloidin 72 years previously. PCR amplification of DNA showed the D178N mutation. Goldfarb et al. (1992) demonstrated that the D178N mutation in conjunction with the met129 polymorphism on the same allele (176640.0005) was responsible for fatal familial insomnia (FFI; 600072). They found that CJD was associated with val129 in all 15 affected members of 6 kindreds, whereas met129 was associated with FFI in all 15 affected members of 5 kindreds. Analysis of the PRNP region by Dagvadorj et al. (2002) in 13 families and 2 sporadic patients with either CJD caused by D178N and 129V or FFI caused by D178N and 129M (176640.0010) showed that the D178N chromosomes had independent origins in each affected pedigree or patient. In addition, a de novo spontaneous PRNP mutation was observed in 1 family. Noting that the mutation involving codon 178 occurred at a CpG dinucleotide motif that is considered to be a hotspot for spontaneous human mutations, Dagvadorj et al. (2002) concluded that cases associated with the D178N mutation result from multiple recurrent mutational events. Zarranz et al. (2005) reported 23 patients from 13 Spanish families with prion disease. Nine families were of Basque origin, 6 of which were genetically related by haplotype analysis. They identified 2 patients who were D178N and val/met129 heterozygous with fatal familial insomnia (FFI; 600072). One patient was sporadic, and 1 patient had a relative with the same genotype who presented with CJD. PrPSc isotype analysis was not informative. The largest family had 5 affected individuals. The genotype in all 5 family members was D178N and met129 homozygous (176640.0010) but only 2 presented with FFI. The 3 other family members presented with CJD, 2 with ataxia and 1 with acalculia, aphasia and dementia. In another family with D178N and met129 homozygous, 1 patient had classic FFI presenting with insomnia, 1 had FFI presenting with depression, apathy, and autonomic dysfunction, and 2 other family members presented with CJD. Overall, 7 patients with D178N and met129 homozygous had a clinical and neuropathologic profile compatible with CJD. Zarranz et al. (2005) concluded that there must be other environmental or genetic factors that influence the phenotypic expression of the D178N mutation, and that FFI and CJD due to this genotype are extremes of a phenotypic spectrum rather than 2 discrete entities. Dossena et al. (2008) generated a transgenic mouse model expressing the mouse homolog of the D178N/M129V mutation. These mice developed clinical and pathologic features reminiscent of CJD, including motor dysfunction, memory impairment, cerebral prion protein deposition, and gliosis. Other features included EEG abnormalities and severe alterations of sleep-wake patterns similar to those observed in human patients. Neurons from the mutant mice showed swelling of the endoplasmic reticulum (ER) with intracellular retention of mutant prion protein, suggesting that ER dysfunction could contribute to the pathology of CJD. The mutant protein was protease-resistant and formed aggregations. (less)
|
Citation text
Meggendorfer, F. Klinische und genealogische Beobachtungen bei einem Fall von spastischer Pseudosklerose Jakobs. Z. Ges. Neurol. Psychiat. 128: 337-341, 1930.
Citation text
Goldfarb, L. G., Petersen, R. B., Tabaton, M., Brown, P., LeBlanc, A. C., Montagna, P., Cortelli, P., Julien, J., Vital, C., Pendelbury, W. W., Haltia, M., Wills, P. R., Hauw, J. J., McKeever, P. E., Monari, L., Schrank, B., Swergold, G. D., Autilio-Gambetti, L., Gajdusek, D. C., Lugaresi, E., Gambetti, P. Fatal familial insomnia and familial Creutzfeldt-Jakob disease: disease phenotype determined by a DNA polymorphism. Science 258: 806-808, 1992.
Citation text
Meggendorfer, F. Klinische und genealogische Beobachtungen bei einem Fall von spastischer Pseudosklerose Jakobs. Z. Ges. Neurol. Psychiat. 128: 337-341, 1930.
Citation text
Goldfarb, L. G., Petersen, R. B., Tabaton, M., Brown, P., LeBlanc, A. C., Montagna, P., Cortelli, P., Julien, J., Vital, C., Pendelbury, W. W., Haltia, M., Wills, P. R., Hauw, J. J., McKeever, P. E., Monari, L., Schrank, B., Swergold, G. D., Autilio-Gambetti, L., Gajdusek, D. C., Lugaresi, E., Gambetti, P. Fatal familial insomnia and familial Creutzfeldt-Jakob disease: disease phenotype determined by a DNA polymorphism. Science 258: 806-808, 1992.
Germline Functional Evidence
| There is no functional evidence in ClinVar for this variation. If you have generated functional data for this variation, please consider submitting that data to ClinVar. |
Citations for germline classification of this variant
Help| Title | Author | Journal | Year | Link |
|---|---|---|---|---|
| Genetic Prion Disease. | Adam MP | - | 2021 | PMID: 20301407 |
| Genetic Creutzfeldt-Jakob disease. | Ladogana A | Handbook of clinical neurology | 2018 | PMID: 29887139 |
| Towards authentic transgenic mouse models of heritable PrP prion diseases. | Watts JC | Acta neuropathologica | 2016 | PMID: 27350609 |
| Quantifying prion disease penetrance using large population control cohorts. | Minikel EV | Science translational medicine | 2016 | PMID: 26791950 |
| The Features of Genetic Prion Diseases Based on Chinese Surveillance Program. | Shi Q | PloS one | 2015 | PMID: 26488179 |
| Disease-associated mutations in the prion protein impair laminin-induced process outgrowth and survival. | Machado CF | The Journal of biological chemistry | 2012 | PMID: 23132868 |
| Discordant clinicopathologic phenotypes in a Japanese kindred of fatal familial insomnia. | Saitoh Y | Neurology | 2010 | PMID: 20038778 |
| A novel protective prion protein variant that colocalizes with kuru exposure. | Mead S | The New England journal of medicine | 2009 | PMID: 19923577 |
| Mutant prion protein expression causes motor and memory deficits and abnormal sleep patterns in a transgenic mouse model. | Dossena S | Neuron | 2008 | PMID: 19038218 |
| A novel PRNP-P105S mutation associated with atypical prion disease and a rare PrPSc conformation. | Tunnell E | Neurology | 2008 | PMID: 18955686 |
| Defective retrotranslocation causes loss of anti-Bax function in human familial prion protein mutants. | Jodoin J | The Journal of neuroscience : the official journal of the Society for Neuroscience | 2007 | PMID: 17494694 |
| [Fatal familiar insomnia: clinical, neurophysiological and histopathological study of two cases]. | Ayuso Blanco T | Neurologia (Barcelona, Spain) | 2006 | PMID: 17013786 |
| Prion protein (PRNP) genotypes in frontotemporal lobar degeneration syndromes. | Rohrer JD | Annals of neurology | 2006 | PMID: 16969862 |
| Complete sequence data support lack of balancing selection on PRNP in a natural Chinese population. | Zan Q | Journal of human genetics | 2006 | PMID: 16565881 |
| Prion disease genetics. | Mead S | European journal of human genetics : EJHG | 2006 | PMID: 16391566 |
| Prion protein codon 129 genotype prevalence is altered in primary progressive aphasia. | Li X | Annals of neurology | 2005 | PMID: 16315279 |
| Polymorphism at residue 129 modulates the conformational conversion of the D178N variant of human prion protein 90-231. | Apetri AC | Biochemistry | 2005 | PMID: 16313190 |
| Phenotypic variability in familial prion diseases due to the D178N mutation. | Zarranz JJ | Journal of neurology, neurosurgery, and psychiatry | 2005 | PMID: 16227536 |
| Phenotypic variability in familial prion diseases due to the D178N mutation. | Zarranz JJ | Journal of neurology, neurosurgery, and psychiatry | 2005 | PMID: 16227536 |
| Association of sporadic Creutzfeldt-Jakob disease with homozygous genotypes at PRNP codons 129 and 219 in the Korean population. | Jeong BH | Neurogenetics | 2005 | PMID: 16217673 |
| The prion gene is associated with human long-term memory. | Papassotiropoulos A | Human molecular genetics | 2005 | PMID: 15987701 |
| Human prion protein with valine 129 prevents expression of variant CJD phenotype. | Wadsworth JD | Science (New York, N.Y.) | 2004 | PMID: 15539564 |
| Prion protein codon 129 polymorphism and risk of Alzheimer disease. | Riemenschneider M | Neurology | 2004 | PMID: 15277640 |
| Polymorphisms in the prion protein gene and in the doppel gene increase susceptibility for Creutzfeldt-Jakob disease. | Croes EA | European journal of human genetics : EJHG | 2004 | PMID: 14970845 |
| RNA molecules stimulate prion protein conversion. | Deleault NR | Nature | 2003 | PMID: 14562104 |
| Absence of association between codon 129/219 polymorphisms of the prion protein gene and Alzheimer's disease in Japan. | Ohkubo T | Annals of neurology | 2003 | PMID: 14520676 |
| Early cognitive decline is associated with prion protein codon 129 polymorphism. | Croes EA | Annals of neurology | 2003 | PMID: 12891686 |
| Distribution of codon 129 genotype in human growth hormone-treated CJD patients in France and the UK. | Brandel JP | Lancet (London, England) | 2003 | PMID: 12867116 |
| PRNP Val129 homozygosity increases risk for early-onset Alzheimer's disease. | Dermaut B | Annals of neurology | 2003 | PMID: 12601712 |
| Mutations of the prion protein gene phenotypic spectrum. | Kovács GG | Journal of neurology | 2002 | PMID: 12420099 |
| Spontaneous mutations in the prion protein gene causing transmissible spongiform encephalopathy. | Dagvadorj A | Annals of neurology | 2002 | PMID: 12205650 |
| Distribution of the M129V polymorphism of the prion protein gene in a Turkish population suggests a high risk for Creutzfeldt-Jakob disease. | Erginel-Unaltuna N | European journal of human genetics : EJHG | 2001 | PMID: 11840201 |
| Biochemical and structural studies of the prion protein polymorphism. | Petchanikow C | FEBS letters | 2001 | PMID: 11749972 |
| Sporadic Creutzfeldt-Jakob disease in a young Dutch valine homozygote: atypical molecular phenotype. | Head MW | Annals of neurology | 2001 | PMID: 11506411 |
| Increased incidence of sporadic Creutzfeldt-Jakob disease on the island of Crete associated with a high rate of PRNP 129-methionine homozygosity in the local population. | Plaitakis A | Annals of neurology | 2001 | PMID: 11506406 |
| Prion protein gene polymorphism and Alzheimer's disease: one modulatory trait of cognitive decline? | Casadei VM | Journal of neurology, neurosurgery, and psychiatry | 2001 | PMID: 11488277 |
| Polymorphism at codon 129 of the prion protein gene is not associated with sporadic AD. | Combarros O | Neurology | 2000 | PMID: 10953203 |
| Novel twelve-generation kindred of fatal familial insomnia from germany representing the entire spectrum of disease expression. | Harder A | American journal of medical genetics | 1999 | PMID: 10588836 |
| Prominent psychiatric features and early onset in an inherited prion disease with a new insertional mutation in the prion protein gene. | Laplanche JL | Brain : a journal of neurology | 1999 | PMID: 10581230 |
| Prominent psychiatric features and early onset in an inherited prion disease with a new insertional mutation in the prion protein gene. | Laplanche JL | Brain : a journal of neurology | 1999 | PMID: 10581230 |
| The genetics of prions--a contradiction in terms? | Aguzzi A | Lancet (London, England) | 1999 | PMID: 10437852 |
| Familial mutations and the thermodynamic stability of the recombinant human prion protein. | Swietnicki W | The Journal of biological chemistry | 1998 | PMID: 9813003 |
| Phenotype-genotype studies in kuru: implications for new variant Creutzfeldt-Jakob disease. | Cervenáková L | Proceedings of the National Academy of Sciences of the United States of America | 1998 | PMID: 9789072 |
| Prion protein NMR structure and familial human spongiform encephalopathies. | Riek R | Proceedings of the National Academy of Sciences of the United States of America | 1998 | PMID: 9751723 |
| Prion protein NMR structure and familial human spongiform encephalopathies. | Riek R | Proceedings of the National Academy of Sciences of the United States of America | 1998 | PMID: 9751723 |
| Polymorphism of the prion protein is associated with cognitive impairment in the elderly: the EVA study. | Berr C | Neurology | 1998 | PMID: 9748018 |
| Genotype at codon 129 and susceptibility to Creutzfeldt-Jakob disease. | Deslys JP | Lancet (London, England) | 1998 | PMID: 9643750 |
| Identification in Israel of 2 Jewish Creutzfeld-Jakob disease patients with a 178 mutation at their PrP gene. | Rosenmann H | Acta neurologica Scandinavica | 1998 | PMID: 9531435 |
| The D178N (cis-129M) "fatal familial insomnia" mutation associated with diverse clinicopathologic phenotypes in an Australian kindred. | McLean CA | Neurology | 1997 | PMID: 9270595 |
| Codon 178 mutation of the human prion protein gene in a German family (Backer family): sequencing data from 72-year-old celloidin-embedded brain tissue. | Kretzschmar HA | Acta neuropathologica | 1995 | PMID: 7709737 |
| Fatal familial insomnia and familial Creutzfeldt-Jakob disease: different prion proteins determined by a DNA polymorphism. | Monari L | Proceedings of the National Academy of Sciences of the United States of America | 1994 | PMID: 7908444 |
| Fatal familial insomnia and the widening spectrum of prion diseases. | Gambetti P | British medical bulletin | 1993 | PMID: 8137139 |
| Familial Creutzfeldt-Jakob disease in Chile is associated with the codon 200 mutation of the PRNP amyloid precursor gene on chromosome 20. | Brown P | Journal of the neurological sciences | 1992 | PMID: 1469441 |
| Fatal familial insomnia and familial Creutzfeldt-Jakob disease: disease phenotype determined by a DNA polymorphism. | Goldfarb LG | Science (New York, N.Y.) | 1992 | PMID: 1439789 |
| Phenotypic characteristics of familial Creutzfeldt-Jakob disease associated with the codon 178Asn PRNP mutation. | Brown P | Annals of neurology | 1992 | PMID: 1353342 |
| Creutzfeldt-Jakob disease cosegregates with the codon 178Asn PRNP mutation in families of European origin. | Goldfarb LG | Annals of neurology | 1992 | PMID: 1353341 |
| Creutzfeldt-Jakob disease cosegregates with the codon 178Asn PRNP mutation in families of European origin. | Goldfarb LG | Annals of neurology | 1992 | PMID: 1353341 |
| Familial Creutzfeldt-Jakob disease in Finland: epidemiological, clinical, pathological and molecular genetic studies. | Haltia M | European journal of epidemiology | 1991 | PMID: 1684756 |
| Presymptomatic detection or exclusion of prion protein gene defects in families with inherited prion diseases. | Collinge J | American journal of human genetics | 1991 | PMID: 1684089 |
| CJD discrepancy. | Doh-ura K | Nature | 1991 | PMID: 1682813 |
| Homozygous prion protein genotype predisposes to sporadic Creutzfeldt-Jakob disease. | Palmer MS | Nature | 1991 | PMID: 1677164 |
| Codon 178 mutation in ethnically diverse Creutzfeldt-Jakob disease families. | Nieto A | Lancet (London, England) | 1991 | PMID: 1671983 |
| New mutation in scrapie amyloid precursor gene (at codon 178) in Finnish Creutzfeldt-Jakob kindred. | Goldfarb LG | Lancet (London, England) | 1991 | PMID: 1671440 |
| New mutation in scrapie amyloid precursor gene (at codon 178) in Finnish Creutzfeldt-Jakob kindred. | Goldfarb LG | Lancet (London, England) | 1991 | PMID: 1671440 |
| Codon 129 changes in the prion protein gene in Caucasians. | Owen F | American journal of human genetics | 1990 | PMID: 2378641 |
| A codon 129 polymorphism in the PRIP gene. | Owen F | Nucleic acids research | 1990 | PMID: 1971924 |
| Pro----leu change at position 102 of prion protein is the most common but not the sole mutation related to Gerstmann-Sträussler syndrome. | Doh-ura K | Biochemical and biophysical research communications | 1989 | PMID: 2783132 |
| Meggendorfer, F. Klinische und genealogische Beobachtungen bei einem Fall von spastischer Pseudosklerose Jakobs. Z. Ges. Neurol. Psychiat. 128: 337-341, 1930. | - | - | - | - |
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HelpRecord last updated Nov 03, 2024
This date represents the last time this VCV record was updated. The update may be due to an update to one of the included submitted records (SCVs), or due to an update that ClinVar made to the variant such as adding HGVS expressions or a rs number. So this date may be different from the date of the “most recent submission” reported at the top of this page.