Exploration
Accueil
Racine
Exploration
Accueil
Racine

Serveur d'exploration sur la maladie de Parkinson

Attention, ce site est en cours de développement !
Attention, site généré par des moyens informatiques à partir de corpus bruts.
Les informations ne sont donc pas validées.

parkin mutation analysis in clinic patients with early‐onset Parkinson's disease

Identifieur interne : 001556 ( Main/Exploration ); précédent : 001555; suivant : 001557

parkin mutation analysis in clinic patients with early‐onset Parkinson's disease

Auteurs : P. Poorkaj [États-Unis] ; J. G. Nutt [États-Unis] ; D. James [États-Unis] ; S. Gancher [États-Unis] ; T. D. Bird [États-Unis] ; E. Steinbart [États-Unis] ; G. D. Schellenberg [États-Unis] ; Haydeh Payami [États-Unis]

Source :

RBID : ISTEX:C49F41D98A0EE576F34000686751C924A267D3F4

English descriptors

Abstract

parkin mutations are the most common identified cause of Parkinson's disease (PD). It has been suggested that patients with young‐onset PD be screened for parkin mutations as a part of their clinical work‐up. The aim of this study was to assess parkin mutation frequency in a clinical setting, correlate genotype with phenotype, and evaluate the current justification for clinical parkin testing. Patients were selected from a movement disorder clinic based on diagnosis of PD and onset age ≤40 years. parkin was genotyped by sequence and dosage analysis for all 12 exons. Key relatives and controls were screened for identified mutations. Mutations were found in 7/39 patients. Two patients were compound heterozygous; five were heterozygous. Mutations included deletions in exons 2, 3, and 8, duplications in exons 2–4, and 9, and P437L substitution. Seventy‐eight percent of mutations were deletions/multiplications. A novel substitution (R402W) was found in one patient and in one control. None of the point mutations found in patients were detected in 96 controls. parkin phenotypes were consistent with idiopathic PD. In conclusion, parkin mutations are common in the clinic setting: 10% of PD patients had early‐onset and 18% of them had parkin mutations. However, if parkin is recessive, only 5% of early‐onset cases who had compound mutations could be attributed to this locus. Mutation frequency was 0.12 (95% CI 0.04–0.19). parkin cases can present as typical idiopathic PD, distinguishable only by molecular testing. Seventy percent of parkin cases were heterozygous. It is unclear whether heterozygous mutations are pathogenic. parkin‐based diagnosis and counseling require a better understanding of the mode of inheritance, penetrance, and carrier frequencies. © 2004 Wiley‐Liss, Inc.

Url:
DOI: 10.1002/ajmg.a.30157


Affiliations:

Links toward previous steps (curation, corpus...)

Le document en format XML

<record>
<TEI wicri:istexFullTextTei="biblStruct">
<teiHeader>
<fileDesc>
<titleStmt>
<title xml:lang="en">parkin mutation analysis in clinic patients with early‐onset Parkinson's disease</title>
<author>
<name sortKey="Poorkaj, P" sort="Poorkaj, P" uniqKey="Poorkaj P" first="P." last="Poorkaj">P. Poorkaj</name>
</author>
<author>
<name sortKey="Nutt, J G" sort="Nutt, J G" uniqKey="Nutt J" first="J. G." last="Nutt">J. G. Nutt</name>
</author>
<author>
<name sortKey="James, D" sort="James, D" uniqKey="James D" first="D." last="James">D. James</name>
</author>
<author>
<name sortKey="Gancher, S" sort="Gancher, S" uniqKey="Gancher S" first="S." last="Gancher">S. Gancher</name>
</author>
<author>
<name sortKey="Bird, T D" sort="Bird, T D" uniqKey="Bird T" first="T. D." last="Bird">T. D. Bird</name>
</author>
<author>
<name sortKey="Steinbart, E" sort="Steinbart, E" uniqKey="Steinbart E" first="E." last="Steinbart">E. Steinbart</name>
</author>
<author>
<name sortKey="Schellenberg, G D" sort="Schellenberg, G D" uniqKey="Schellenberg G" first="G. D." last="Schellenberg">G. D. Schellenberg</name>
</author>
<author>
<name sortKey="Payami, Haydeh" sort="Payami, Haydeh" uniqKey="Payami H" first="Haydeh" last="Payami">Haydeh Payami</name>
</author>
</titleStmt>
<publicationStmt>
<idno type="wicri:source">ISTEX</idno>
<idno type="RBID">ISTEX:C49F41D98A0EE576F34000686751C924A267D3F4</idno>
<date when="2004" year="2004">2004</date>
<idno type="doi">10.1002/ajmg.a.30157</idno>
<idno type="url">https://api.istex.fr/document/C49F41D98A0EE576F34000686751C924A267D3F4/fulltext/pdf</idno>
<idno type="wicri:Area/Main/Corpus">001802</idno>
<idno type="wicri:Area/Main/Curation">001559</idno>
<idno type="wicri:Area/Main/Exploration">001556</idno>
</publicationStmt>
<sourceDesc>
<biblStruct>
<analytic>
<title level="a" type="main" xml:lang="en">parkin mutation analysis in clinic patients with early‐onset Parkinson's disease</title>
<author>
<name sortKey="Poorkaj, P" sort="Poorkaj, P" uniqKey="Poorkaj P" first="P." last="Poorkaj">P. Poorkaj</name>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Geriatric Research Education Clinical Center, Veterans Affairs Puget Sound Health Care System, Seattle Division, Seattle</wicri:cityArea>
</affiliation>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Division of Gerontology and Geriatric Medicine, University of Washington, Seattle</wicri:cityArea>
</affiliation>
</author>
<author>
<name sortKey="Nutt, J G" sort="Nutt, J G" uniqKey="Nutt J" first="J. G." last="Nutt">J. G. Nutt</name>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Oregon</region>
</placeName>
<wicri:cityArea>Department of Neurology, Oregon Health & Science University, Portland</wicri:cityArea>
</affiliation>
</author>
<author>
<name sortKey="James, D" sort="James, D" uniqKey="James D" first="D." last="James">D. James</name>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Oregon</region>
</placeName>
<wicri:cityArea>Department of Neurology, Oregon Health & Science University, Portland</wicri:cityArea>
</affiliation>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">État de New York</region>
</placeName>
<wicri:cityArea>Division of Genetic Disorders, Wadsworth Center, Albany</wicri:cityArea>
</affiliation>
</author>
<author>
<name sortKey="Gancher, S" sort="Gancher, S" uniqKey="Gancher S" first="S." last="Gancher">S. Gancher</name>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Oregon</region>
</placeName>
<wicri:cityArea>Kaiser Permanante, Portland</wicri:cityArea>
</affiliation>
</author>
<author>
<name sortKey="Bird, T D" sort="Bird, T D" uniqKey="Bird T" first="T. D." last="Bird">T. D. Bird</name>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Geriatric Research Education Clinical Center, Veterans Affairs Puget Sound Health Care System, Seattle Division, Seattle</wicri:cityArea>
</affiliation>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Department of Neurology, University of Washington, Seattle</wicri:cityArea>
</affiliation>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Division of Medical Genetics, Department of Medicine, University of Washington, Seattle</wicri:cityArea>
</affiliation>
</author>
<author>
<name sortKey="Steinbart, E" sort="Steinbart, E" uniqKey="Steinbart E" first="E." last="Steinbart">E. Steinbart</name>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Geriatric Research Education Clinical Center, Veterans Affairs Puget Sound Health Care System, Seattle Division, Seattle</wicri:cityArea>
</affiliation>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Department of Neurology, University of Washington, Seattle</wicri:cityArea>
</affiliation>
</author>
<author>
<name sortKey="Schellenberg, G D" sort="Schellenberg, G D" uniqKey="Schellenberg G" first="G. D." last="Schellenberg">G. D. Schellenberg</name>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Geriatric Research Education Clinical Center, Veterans Affairs Puget Sound Health Care System, Seattle Division, Seattle</wicri:cityArea>
</affiliation>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Division of Gerontology and Geriatric Medicine, University of Washington, Seattle</wicri:cityArea>
</affiliation>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Washington (État)</region>
</placeName>
<wicri:cityArea>Departments of Neurology, and Pharmacology, University of Washington, Seattle</wicri:cityArea>
</affiliation>
</author>
<author>
<name sortKey="Payami, Haydeh" sort="Payami, Haydeh" uniqKey="Payami H" first="Haydeh" last="Payami">Haydeh Payami</name>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">Oregon</region>
</placeName>
<wicri:cityArea>Department of Neurology, Oregon Health & Science University, Portland</wicri:cityArea>
</affiliation>
<affiliation wicri:level="2">
<country xml:lang="fr">États-Unis</country>
<placeName>
<region type="state">État de New York</region>
</placeName>
<wicri:cityArea>Division of Genetic Disorders, Wadsworth Center, Albany</wicri:cityArea>
</affiliation>
</author>
</analytic>
<monogr></monogr>
<series>
<title level="j">American Journal of Medical Genetics Part A</title>
<title level="j" type="abbrev">Am. J. Med. Genet.</title>
<idno type="ISSN">1552-4825</idno>
<idno type="eISSN">1552-4833</idno>
<imprint>
<publisher>Wiley Subscription Services, Inc., A Wiley Company</publisher>
<pubPlace>Hoboken</pubPlace>
<date type="published" when="2004-08-15">2004-08-15</date>
<biblScope unit="volume">129A</biblScope>
<biblScope unit="issue">1</biblScope>
<biblScope unit="page" from="44">44</biblScope>
<biblScope unit="page" to="50">50</biblScope>
</imprint>
<idno type="ISSN">1552-4825</idno>
</series>
<idno type="istex">C49F41D98A0EE576F34000686751C924A267D3F4</idno>
<idno type="DOI">10.1002/ajmg.a.30157</idno>
<idno type="ArticleID">AJMG30157</idno>
</biblStruct>
</sourceDesc>
<seriesStmt>
<idno type="ISSN">1552-4825</idno>
</seriesStmt>
</fileDesc>
<profileDesc>
<textClass>
<keywords scheme="KwdEn" xml:lang="en">
<term>Parkinson's disease</term>
<term>clinical testing</term>
<term>gene dosage</term>
<term>parkin</term>
</keywords>
</textClass>
<langUsage>
<language ident="en">en</language>
</langUsage>
</profileDesc>
</teiHeader>
<front>
<div type="abstract" xml:lang="en">parkin mutations are the most common identified cause of Parkinson's disease (PD). It has been suggested that patients with young‐onset PD be screened for parkin mutations as a part of their clinical work‐up. The aim of this study was to assess parkin mutation frequency in a clinical setting, correlate genotype with phenotype, and evaluate the current justification for clinical parkin testing. Patients were selected from a movement disorder clinic based on diagnosis of PD and onset age ≤40 years. parkin was genotyped by sequence and dosage analysis for all 12 exons. Key relatives and controls were screened for identified mutations. Mutations were found in 7/39 patients. Two patients were compound heterozygous; five were heterozygous. Mutations included deletions in exons 2, 3, and 8, duplications in exons 2–4, and 9, and P437L substitution. Seventy‐eight percent of mutations were deletions/multiplications. A novel substitution (R402W) was found in one patient and in one control. None of the point mutations found in patients were detected in 96 controls. parkin phenotypes were consistent with idiopathic PD. In conclusion, parkin mutations are common in the clinic setting: 10% of PD patients had early‐onset and 18% of them had parkin mutations. However, if parkin is recessive, only 5% of early‐onset cases who had compound mutations could be attributed to this locus. Mutation frequency was 0.12 (95% CI 0.04–0.19). parkin cases can present as typical idiopathic PD, distinguishable only by molecular testing. Seventy percent of parkin cases were heterozygous. It is unclear whether heterozygous mutations are pathogenic. parkin‐based diagnosis and counseling require a better understanding of the mode of inheritance, penetrance, and carrier frequencies. © 2004 Wiley‐Liss, Inc.</div>
</front>
</TEI>
<affiliations>
<list>
<country>
<li>États-Unis</li>
</country>
<region>
<li>Oregon</li>
<li>Washington (État)</li>
<li>État de New York</li>
</region>
</list>
<tree>
<country name="États-Unis">
<region name="Washington (État)">
<name sortKey="Poorkaj, P" sort="Poorkaj, P" uniqKey="Poorkaj P" first="P." last="Poorkaj">P. Poorkaj</name>
</region>
<name sortKey="Bird, T D" sort="Bird, T D" uniqKey="Bird T" first="T. D." last="Bird">T. D. Bird</name>
<name sortKey="Bird, T D" sort="Bird, T D" uniqKey="Bird T" first="T. D." last="Bird">T. D. Bird</name>
<name sortKey="Bird, T D" sort="Bird, T D" uniqKey="Bird T" first="T. D." last="Bird">T. D. Bird</name>
<name sortKey="Gancher, S" sort="Gancher, S" uniqKey="Gancher S" first="S." last="Gancher">S. Gancher</name>
<name sortKey="James, D" sort="James, D" uniqKey="James D" first="D." last="James">D. James</name>
<name sortKey="James, D" sort="James, D" uniqKey="James D" first="D." last="James">D. James</name>
<name sortKey="Nutt, J G" sort="Nutt, J G" uniqKey="Nutt J" first="J. G." last="Nutt">J. G. Nutt</name>
<name sortKey="Payami, Haydeh" sort="Payami, Haydeh" uniqKey="Payami H" first="Haydeh" last="Payami">Haydeh Payami</name>
<name sortKey="Payami, Haydeh" sort="Payami, Haydeh" uniqKey="Payami H" first="Haydeh" last="Payami">Haydeh Payami</name>
<name sortKey="Poorkaj, P" sort="Poorkaj, P" uniqKey="Poorkaj P" first="P." last="Poorkaj">P. Poorkaj</name>
<name sortKey="Schellenberg, G D" sort="Schellenberg, G D" uniqKey="Schellenberg G" first="G. D." last="Schellenberg">G. D. Schellenberg</name>
<name sortKey="Schellenberg, G D" sort="Schellenberg, G D" uniqKey="Schellenberg G" first="G. D." last="Schellenberg">G. D. Schellenberg</name>
<name sortKey="Schellenberg, G D" sort="Schellenberg, G D" uniqKey="Schellenberg G" first="G. D." last="Schellenberg">G. D. Schellenberg</name>
<name sortKey="Steinbart, E" sort="Steinbart, E" uniqKey="Steinbart E" first="E." last="Steinbart">E. Steinbart</name>
<name sortKey="Steinbart, E" sort="Steinbart, E" uniqKey="Steinbart E" first="E." last="Steinbart">E. Steinbart</name>
</country>
</tree>
</affiliations>
</record>

Pour manipuler ce document sous Unix (Dilib)

EXPLOR_STEP=$WICRI_ROOT/Wicri/Sante/explor/ParkinsonV1/Data/Main/Exploration

HfdSelect -h $EXPLOR_STEP/biblio.hfd -nk 001556 | SxmlIndent | more

Ou

HfdSelect -h $EXPLOR_AREA/Data/Main/Exploration/biblio.hfd -nk 001556 | SxmlIndent | more

Pour mettre un lien sur cette page dans le réseau Wicri

{{Explor lien
   |wiki=    Wicri/Sante
   |area=    ParkinsonV1
   |flux=    Main
   |étape=   Exploration
   |type=    RBID
   |clé=     ISTEX:C49F41D98A0EE576F34000686751C924A267D3F4
   |texte=   parkin mutation analysis in clinic patients with early‐onset Parkinson's disease
}}
Wicri

This area was generated with Dilib version V0.6.23.
Data generation: Sun Jul 3 18:06:51 2016. Site generation: Wed Mar 6 18:46:03 2024