Multiple system atrophy: A review of 203 pathologically proven cases
Identifieur interne : 005300 ( Main/Exploration ); précédent : 005299; suivant : 005301Multiple system atrophy: A review of 203 pathologically proven cases
Auteurs : Wenning [Royaume-Uni, Autriche] ; F. Tison [Royaume-Uni] ; Y. Ben Shlomo [Royaume-Uni] ; S. E. Daniel [Royaume-Uni] ; N. P. Quinn [Royaume-Uni]Source :
- Movement Disorders [ 0885-3185 ] ; 1997-03.
English descriptors
- KwdEn :
- Aged, Brain (pathology), Clinicopathological features, Corpus Striatum (pathology), Female, Humans, Male, Middle Aged, Multiple system atrophy, Nerve Degeneration (physiology), Neurologic Examination, Olivopontocerebellar Atrophies (diagnosis), Olivopontocerebellar Atrophies (pathology), Parkinson Disease, Secondary (diagnosis), Parkinson Disease, Secondary (pathology), Shy-Drager Syndrome (diagnosis), Shy-Drager Syndrome (pathology), Shy‐Drager syndrome, Spinal Cord (pathology), Striatonigral degeneration, Substantia Nigra (pathology), olivopontocerebellar atrophy.
- MESH :
- diagnosis : Olivopontocerebellar Atrophies, Parkinson Disease, Secondary, Shy-Drager Syndrome.
- pathology : Brain, Corpus Striatum, Olivopontocerebellar Atrophies, Parkinson Disease, Secondary, Shy-Drager Syndrome, Spinal Cord, Substantia Nigra.
- physiology : Nerve Degeneration.
- Aged, Female, Humans, Male, Middle Aged, Neurologic Examination.
Abstract
We report the clinicopathological features of 203 cases of pathologically proven multiple system atrophy (MSA) from 108 publications up to February 1995. The majority of patients showed symptoms in their early fifties, and men were more commonly affected than women (ratio of 1.3:1). Most patients suffered from some degree of autonomic failure (74%). Parkinsonism was the most common motor disorder (87%), followed by cerebellar ataxia (54%) and pyramidal signs (49%). The response to levodopa was poor in most patients, but there was a subgroup with a good response, who also often developed axial levodopa‐induced dyskinesias. Other characteristic features included severe dysarthria, stridor, and, in a few patients, contractures and dystonia (antecollis). Mild or moderate intellectual impairment occurred in some cases, but severe dementing illness was most unusual. The main pathological change comprised cell loss and gliosis in the putamen, caudate nucleus, external pallidum, substantia nigra, locus ceruleus, inferior olives, pontine nuclei, cerebellar Purkinje cells, and intermediolateral cell columns of the spinal cord. However, other neuronal populations were also involved to varying degrees, such as the thalamus, vestibular nucleus, dorsal vagal nucleus, corticospinal tracts, and anterior horn cells. Characteristic glial and/or neuronal cytoplasmic inclusions were identified in all cases in which they were sought, irrespective of clinical presentation. Akinesia correlated with the degree of nigral and putaminal cell loss, whereas rigidity was related only to the latter. Tremor was unrelated to cell loss at any site. Ataxia correlated with the degree of olivopontocerebellar atrophy. Pyramidal signs were associated with pyramidal tract pallor. Our analysis also confirmed an association of postural hypotension with intermediolateral cell column degeneration.
Url:
DOI: 10.1002/mds.870120203
Affiliations:
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Daniel</name><affiliation wicri:level="3"><country>Royaume-Uni</country><placeName><settlement type="city">Londres</settlement><region type="country">Angleterre</region><region type="région" nuts="1">Grand Londres</region></placeName><wicri:orgArea>Parkinson's Disease Society Brain Bank, Institute of Neurology</wicri:orgArea></affiliation></author><author><name sortKey="Quinn, N P" sort="Quinn, N P" uniqKey="Quinn N" first="N. P." last="Quinn">N. P. Quinn</name><affiliation wicri:level="3"><country>Royaume-Uni</country><placeName><settlement type="city">Londres</settlement><region type="country">Angleterre</region><region type="région" nuts="1">Grand Londres</region></placeName><wicri:orgArea>University Department of Clinical Neurology, Institute of Neurology</wicri:orgArea></affiliation></author></analytic><monogr></monogr><series><title level="j">Movement Disorders</title><title level="j" type="abbrev">Mov. Disord.</title><idno type="ISSN">0885-3185</idno><idno type="eISSN">1531-8257</idno><imprint><publisher>Wiley Subscription Services, Inc., A Wiley Company</publisher><pubPlace>Hoboken</pubPlace><date type="published" when="1997-03">1997-03</date><biblScope unit="vol">12</biblScope><biblScope unit="issue">2</biblScope><biblScope unit="page" from="133">133</biblScope><biblScope unit="page" to="147">147</biblScope></imprint><idno type="ISSN">0885-3185</idno></series><idno type="istex">3A6BF5F6F46F21777C569F9207527A840F759102</idno><idno type="DOI">10.1002/mds.870120203</idno><idno type="ArticleID">MDS870120203</idno></biblStruct></sourceDesc><seriesStmt><idno type="ISSN">0885-3185</idno></seriesStmt></fileDesc><profileDesc><textClass><keywords scheme="KwdEn" xml:lang="en"><term>Aged</term><term>Brain (pathology)</term><term>Clinicopathological features</term><term>Corpus Striatum (pathology)</term><term>Female</term><term>Humans</term><term>Male</term><term>Middle Aged</term><term>Multiple system atrophy</term><term>Nerve Degeneration (physiology)</term><term>Neurologic Examination</term><term>Olivopontocerebellar Atrophies (diagnosis)</term><term>Olivopontocerebellar Atrophies (pathology)</term><term>Parkinson Disease, Secondary (diagnosis)</term><term>Parkinson Disease, Secondary (pathology)</term><term>Shy-Drager Syndrome (diagnosis)</term><term>Shy-Drager Syndrome (pathology)</term><term>Shy‐Drager syndrome</term><term>Spinal Cord (pathology)</term><term>Striatonigral degeneration</term><term>Substantia Nigra (pathology)</term><term>olivopontocerebellar atrophy</term></keywords><keywords scheme="MESH" qualifier="diagnosis" xml:lang="en"><term>Olivopontocerebellar Atrophies</term><term>Parkinson Disease, Secondary</term><term>Shy-Drager Syndrome</term></keywords><keywords scheme="MESH" qualifier="pathology" xml:lang="en"><term>Brain</term><term>Corpus Striatum</term><term>Olivopontocerebellar Atrophies</term><term>Parkinson Disease, Secondary</term><term>Shy-Drager Syndrome</term><term>Spinal Cord</term><term>Substantia Nigra</term></keywords><keywords scheme="MESH" qualifier="physiology" xml:lang="en"><term>Nerve Degeneration</term></keywords><keywords scheme="MESH" xml:lang="en"><term>Aged</term><term>Female</term><term>Humans</term><term>Male</term><term>Middle Aged</term><term>Neurologic Examination</term></keywords></textClass><langUsage><language ident="en">en</language></langUsage></profileDesc></teiHeader><front><div type="abstract" xml:lang="en">We report the clinicopathological features of 203 cases of pathologically proven multiple system atrophy (MSA) from 108 publications up to February 1995. The majority of patients showed symptoms in their early fifties, and men were more commonly affected than women (ratio of 1.3:1). Most patients suffered from some degree of autonomic failure (74%). Parkinsonism was the most common motor disorder (87%), followed by cerebellar ataxia (54%) and pyramidal signs (49%). The response to levodopa was poor in most patients, but there was a subgroup with a good response, who also often developed axial levodopa‐induced dyskinesias. Other characteristic features included severe dysarthria, stridor, and, in a few patients, contractures and dystonia (antecollis). Mild or moderate intellectual impairment occurred in some cases, but severe dementing illness was most unusual. The main pathological change comprised cell loss and gliosis in the putamen, caudate nucleus, external pallidum, substantia nigra, locus ceruleus, inferior olives, pontine nuclei, cerebellar Purkinje cells, and intermediolateral cell columns of the spinal cord. However, other neuronal populations were also involved to varying degrees, such as the thalamus, vestibular nucleus, dorsal vagal nucleus, corticospinal tracts, and anterior horn cells. Characteristic glial and/or neuronal cytoplasmic inclusions were identified in all cases in which they were sought, irrespective of clinical presentation. Akinesia correlated with the degree of nigral and putaminal cell loss, whereas rigidity was related only to the latter. Tremor was unrelated to cell loss at any site. Ataxia correlated with the degree of olivopontocerebellar atrophy. Pyramidal signs were associated with pyramidal tract pallor. Our analysis also confirmed an association of postural hypotension with intermediolateral cell column degeneration.</div></front></TEI><affiliations><list><country><li>Autriche</li><li>Royaume-Uni</li></country><region><li>Angleterre</li><li>Grand Londres</li></region><settlement><li>Londres</li></settlement></list><tree><country name="Royaume-Uni"><region name="Angleterre"><name sortKey="Wenning" sort="Wenning" uniqKey="Wenning" last="Wenning">Wenning</name></region><name sortKey="Ben Shlomo, Y" sort="Ben Shlomo, Y" uniqKey="Ben Shlomo Y" first="Y." last="Ben Shlomo">Y. Ben Shlomo</name><name sortKey="Daniel, S E" sort="Daniel, S E" uniqKey="Daniel S" first="S. E." last="Daniel">S. E. Daniel</name><name sortKey="Quinn, N P" sort="Quinn, N P" uniqKey="Quinn N" first="N. P." last="Quinn">N. P. Quinn</name><name sortKey="Tison, F" sort="Tison, F" uniqKey="Tison F" first="F." last="Tison">F. Tison</name></country><country name="Autriche"><noRegion><name sortKey="Wenning" sort="Wenning" uniqKey="Wenning" last="Wenning">Wenning</name></noRegion></country></tree></affiliations></record>Pour manipuler ce document sous Unix (Dilib)
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