Association Between Early-Onset Parkinson Disease and 22q11.2 Deletion Syndrome
Identifieur interne : 000E45 ( Main/Exploration ); précédent : 000E44; suivant : 000E46Association Between Early-Onset Parkinson Disease and 22q11.2 Deletion Syndrome
Auteurs : Nancy J. Butcher ; Tim-Rasmus Kiehl ; Lili-Naz Hazrati ; Eva W. C. Chow ; Ekaterina Rogaeva ; Anthony E. Lang ; Anne S. BassettSource :
- JAMA neurology [ 2168-6149 ] ; 2013.
English descriptors
- KwdEn :
- Adult, Age of Onset, Aged, Brain (metabolism), Brain (pathology), Canada, Chromosome Deletion, DNA-Binding Proteins (metabolism), DiGeorge Syndrome (complications), DiGeorge Syndrome (genetics), DiGeorge Syndrome (pathology), Female, Genetic Testing, Humans, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2, Male, Middle Aged, Mutation (genetics), Neurologic Examination, Observational Studies as Topic, Parkinson Disease (complications), Parkinson Disease (genetics), Parkinson Disease (pathology), Protein-Serine-Threonine Kinases (genetics), Severity of Illness Index, Tyrosine 3-Monooxygenase, Young Adult, alpha-Synuclein (metabolism).
- MESH :
- chemical , genetics : Protein-Serine-Threonine Kinases.
- chemical , metabolism : DNA-Binding Proteins, alpha-Synuclein.
- complications : DiGeorge Syndrome, Parkinson Disease.
- genetics : DiGeorge Syndrome, Mutation, Parkinson Disease.
- metabolism : Brain.
- pathology : Brain, DiGeorge Syndrome, Parkinson Disease.
- Adult, Age of Onset, Aged, Canada, Chromosome Deletion, Female, Genetic Testing, Humans, Leucine-Rich Repeat Serine-Threonine Protein Kinase-2, Male, Middle Aged, Neurologic Examination, Observational Studies as Topic, Severity of Illness Index, Tyrosine 3-Monooxygenase, Young Adult.
Abstract
Clinical case reports of parkinsonism co-occurring with hemizygous 22q11.2 deletions and the associated multisystem syndrome, 22q11.2 deletion syndrome (22q11.2DS), suggest that 22q11.2 deletions may lead to increased risk of early-onset Parkinson disease (PD). The frequency of PD and its neuropathological presentation remain unknown in this common genetic condition.
To evaluate a possible association between 22q11.2 deletions and PD.
An observational study of the occurrence of PD in the world’s largest cohort of well-characterized adults with a molecularly confirmed diagnosis of 22q11.2DS (n = 159 [6 with postmortem tissue]; age range, 18.1–68.6 years) was conducted in Toronto, Ontario, Canada. Rare postmortem brain tissue from individuals with 22q11.2DS and a clinical history of PD was investigated for neurodegenerative changes and compared with that from individuals with no history of a movement disorder.
A clinical diagnosis of PD made by a neurologist and neuropathological features of PD.
Adults with 22q11.2DS had a significantly elevated occurrence of PD compared with standard population estimates (standardized morbidity ratio = 69.7; 95% CI, 19.0–178.5). All cases showed early onset and typical PD symptom pattern, treatment response, and course. All were negative for family history of PD and known pathogenic PD-related mutations. The common use of antipsychotics in patients with 22q11.2DS to manage associated psychiatric symptoms delayed diagnosis of PD by up to 10 years. Postmortem brain tissue revealed classic loss of midbrain dopaminergic neurons in all 3 postmortem 22q11.2DS-PD cases. Typical α-synuclein–positive Lewy bodies were present in the expected distribution in 2 cases but absent in another.
These findings suggest that 22q11.2 deletions represent a novel genetic risk factor for early-onset PD with variable neuropathological presentation reminiscent of
Url:
DOI: 10.1001/jamaneurol.2013.3646
PubMed: 24018986
PubMed Central: 4464823
Affiliations:
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Le document en format XML
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Chow</name></author><author><name sortKey="Rogaeva, Ekaterina" sort="Rogaeva, Ekaterina" uniqKey="Rogaeva E" first="Ekaterina" last="Rogaeva">Ekaterina Rogaeva</name></author><author><name sortKey="Lang, Anthony E" sort="Lang, Anthony E" uniqKey="Lang A" first="Anthony E." last="Lang">Anthony E. Lang</name></author><author><name sortKey="Bassett, Anne S" sort="Bassett, Anne S" uniqKey="Bassett A" first="Anne S." last="Bassett">Anne S. 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Butcher</name></author><author><name sortKey="Kiehl, Tim Rasmus" sort="Kiehl, Tim Rasmus" uniqKey="Kiehl T" first="Tim-Rasmus" last="Kiehl">Tim-Rasmus Kiehl</name></author><author><name sortKey="Hazrati, Lili Naz" sort="Hazrati, Lili Naz" uniqKey="Hazrati L" first="Lili-Naz" last="Hazrati">Lili-Naz Hazrati</name></author><author><name sortKey="Chow, Eva W C" sort="Chow, Eva W C" uniqKey="Chow E" first="Eva W. C." last="Chow">Eva W. C. Chow</name></author><author><name sortKey="Rogaeva, Ekaterina" sort="Rogaeva, Ekaterina" uniqKey="Rogaeva E" first="Ekaterina" last="Rogaeva">Ekaterina Rogaeva</name></author><author><name sortKey="Lang, Anthony E" sort="Lang, Anthony E" uniqKey="Lang A" first="Anthony E." last="Lang">Anthony E. Lang</name></author><author><name sortKey="Bassett, Anne S" sort="Bassett, Anne S" uniqKey="Bassett A" first="Anne S." last="Bassett">Anne S. Bassett</name></author></analytic><series><title level="j">JAMA neurology</title><idno type="ISSN">2168-6149</idno><idno type="eISSN">2168-6157</idno><imprint><date when="2013">2013</date></imprint></series></biblStruct></sourceDesc></fileDesc><profileDesc><textClass><keywords scheme="KwdEn" xml:lang="en"><term>Adult</term><term>Age of Onset</term><term>Aged</term><term>Brain (metabolism)</term><term>Brain (pathology)</term><term>Canada</term><term>Chromosome Deletion</term><term>DNA-Binding Proteins (metabolism)</term><term>DiGeorge Syndrome (complications)</term><term>DiGeorge Syndrome (genetics)</term><term>DiGeorge Syndrome (pathology)</term><term>Female</term><term>Genetic Testing</term><term>Humans</term><term>Leucine-Rich Repeat Serine-Threonine Protein Kinase-2</term><term>Male</term><term>Middle Aged</term><term>Mutation (genetics)</term><term>Neurologic Examination</term><term>Observational Studies as Topic</term><term>Parkinson Disease (complications)</term><term>Parkinson Disease (genetics)</term><term>Parkinson Disease (pathology)</term><term>Protein-Serine-Threonine Kinases (genetics)</term><term>Severity of Illness Index</term><term>Tyrosine 3-Monooxygenase</term><term>Young Adult</term><term>alpha-Synuclein (metabolism)</term></keywords><keywords scheme="MESH" type="chemical" qualifier="genetics" xml:lang="en"><term>Protein-Serine-Threonine Kinases</term></keywords><keywords scheme="MESH" type="chemical" qualifier="metabolism" xml:lang="en"><term>DNA-Binding Proteins</term><term>alpha-Synuclein</term></keywords><keywords scheme="MESH" qualifier="complications" xml:lang="en"><term>DiGeorge Syndrome</term><term>Parkinson Disease</term></keywords><keywords scheme="MESH" qualifier="genetics" xml:lang="en"><term>DiGeorge Syndrome</term><term>Mutation</term><term>Parkinson Disease</term></keywords><keywords scheme="MESH" qualifier="metabolism" xml:lang="en"><term>Brain</term></keywords><keywords scheme="MESH" qualifier="pathology" xml:lang="en"><term>Brain</term><term>DiGeorge Syndrome</term><term>Parkinson Disease</term></keywords><keywords scheme="MESH" xml:lang="en"><term>Adult</term><term>Age of Onset</term><term>Aged</term><term>Canada</term><term>Chromosome Deletion</term><term>Female</term><term>Genetic Testing</term><term>Humans</term><term>Leucine-Rich Repeat Serine-Threonine Protein Kinase-2</term><term>Male</term><term>Middle Aged</term><term>Neurologic Examination</term><term>Observational Studies as Topic</term><term>Severity of Illness Index</term><term>Tyrosine 3-Monooxygenase</term><term>Young Adult</term></keywords></textClass></profileDesc></teiHeader><front><div type="abstract" xml:lang="en"><sec id="S1"><title>IMPORTANCE</title><p id="P1">Clinical case reports of parkinsonism co-occurring with hemizygous 22q11.2 deletions and the associated multisystem syndrome, 22q11.2 deletion syndrome (22q11.2DS), suggest that 22q11.2 deletions may lead to increased risk of early-onset Parkinson disease (PD). The frequency of PD and its neuropathological presentation remain unknown in this common genetic condition.</p></sec><sec id="S2"><title>OBJECTIVE</title><p id="P2">To evaluate a possible association between 22q11.2 deletions and PD.</p></sec><sec id="S3"><title>DESIGN, SETTING, AND PARTICIPANTS</title><p id="P3">An observational study of the occurrence of PD in the world’s largest cohort of well-characterized adults with a molecularly confirmed diagnosis of 22q11.2DS (n = 159 [6 with postmortem tissue]; age range, 18.1–68.6 years) was conducted in Toronto, Ontario, Canada. Rare postmortem brain tissue from individuals with 22q11.2DS and a clinical history of PD was investigated for neurodegenerative changes and compared with that from individuals with no history of a movement disorder.</p></sec><sec id="S4"><title>MAIN OUTCOMES AND MEASURES</title><p id="P4">A clinical diagnosis of PD made by a neurologist and neuropathological features of PD.</p></sec><sec id="S5"><title>RESULTS</title><p id="P5">Adults with 22q11.2DS had a significantly elevated occurrence of PD compared with standard population estimates (standardized morbidity ratio = 69.7; 95% CI, 19.0–178.5). All cases showed early onset and typical PD symptom pattern, treatment response, and course. All were negative for family history of PD and known pathogenic PD-related mutations. The common use of antipsychotics in patients with 22q11.2DS to manage associated psychiatric symptoms delayed diagnosis of PD by up to 10 years. Postmortem brain tissue revealed classic loss of midbrain dopaminergic neurons in all 3 postmortem 22q11.2DS-PD cases. Typical α-synuclein–positive Lewy bodies were present in the expected distribution in 2 cases but absent in another.</p></sec><sec id="S6"><title>CONCLUSIONS AND RELEVANCE</title><p id="P6">These findings suggest that 22q11.2 deletions represent a novel genetic risk factor for early-onset PD with variable neuropathological presentation reminiscent of <italic>LRRK2</italic>-associated PD neuropathology. Individuals with early-onset PD and classic features of 22q11.2DS should be considered for genetic testing, and those with a known 22q11.2 deletion should be monitored for the development of parkinsonian symptoms. Molecular studies of the implicated genes, including <italic>DGCR8</italic>, may help shed light on the underlying pathophysiology of PD in 22q11.2DS and idiopathic PD.</p></sec></div></front></TEI><affiliations><list></list><tree><noCountry><name sortKey="Bassett, Anne S" sort="Bassett, Anne S" uniqKey="Bassett A" first="Anne S." last="Bassett">Anne S. Bassett</name><name sortKey="Butcher, Nancy J" sort="Butcher, Nancy J" uniqKey="Butcher N" first="Nancy J." last="Butcher">Nancy J. Butcher</name><name sortKey="Chow, Eva W C" sort="Chow, Eva W C" uniqKey="Chow E" first="Eva W. C." last="Chow">Eva W. C. Chow</name><name sortKey="Hazrati, Lili Naz" sort="Hazrati, Lili Naz" uniqKey="Hazrati L" first="Lili-Naz" last="Hazrati">Lili-Naz Hazrati</name><name sortKey="Kiehl, Tim Rasmus" sort="Kiehl, Tim Rasmus" uniqKey="Kiehl T" first="Tim-Rasmus" last="Kiehl">Tim-Rasmus Kiehl</name><name sortKey="Lang, Anthony E" sort="Lang, Anthony E" uniqKey="Lang A" first="Anthony E." last="Lang">Anthony E. Lang</name><name sortKey="Rogaeva, Ekaterina" sort="Rogaeva, Ekaterina" uniqKey="Rogaeva E" first="Ekaterina" last="Rogaeva">Ekaterina Rogaeva</name></noCountry></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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