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• W1490666291 abstract "Role of basal ganglia: Vesalius and Piccolomini distinguished subcortical nuclei from cortex and white matter in the 16th century. Willis' mistaken concept in the late 17th century that the corpus striatum was the seat of motor power persisted for 200 years and formed the basis of mid-19th-century localizations of movement disorders to the striatum (chorea by Broadbent and Jackson, and athetosis by Hammond). By the late 19th century, many movement disorders were described but for most no pathologic correlate was known. Tremor: Descriptions of tremors progressed from Galen's definition in the 2nd century; to Galileo's physiologic tremor in 1610; separation of involuntary movements during action and at rest in the 17th and 18th centuries by de la Boë Sylvius and van Sweiten; description of Parkinson's disease by Parkinson, discrimination of the rest tremor of Parkinson's disease from the intention tremor of multiple sclerosis by Charcot, and recognition of familial action tremors by Dana and others in the late 19th century; and recognition of autosomal dominant essential tremor in the mid-20th century. Parkinsonism: Pathologic changes in Parkinson's disease were recognized in the substantia nigra by Blocq and Marinescu in the late 19th century, and around 1920 Trértiakoff established Lewy bodies in the substantia nigra as a pathologic hallmark while the Vogts instead emphasized pathologic changes in the striatum; it was only in the mid-1960s that a nigrostriatal dopaminergic pathway was demonstrated and found to be critical to pathogenesis. Early treatment approaches with anticholinergic medications or crude neurosurgical ablation procedures were eclipsed in the 1960s by the advent of L-DOPA therapy due to the work of Carlsson and colleagues, Birkmayer and Hornykiewicz, Barbeau, and Cotzias. Later progress in understanding and treating Parkinson's disease included recognition of neuroleptic-induced parkinsonism beginning in the 1950s, development of dopamine agonists and elaboration of different dopamine receptors beginning in the 1960s, recognition of MPTP-induced parkinsonism in 1982 and subsequent development of experimental models of MPTP-induced parkinsonism. Since the 1980s, stereotactic neurosurgical ablation procedures such as stereotactic pallidotomy were revisited and improved, and stimulation or ablation procedures that modulate subthalamic nucleus activity were developed. Since 1990, rare genetic forms of Parkinson's disease were discovered, which accelerated progress in understanding pathogenesis, and established roles for alpha synuclein and the ubiquitin-proteasome proteolytic system. Separation of atypical forms of parkinsonism (e.g. Wilson's disease, multisystem atrophy, progressive supranuclear palsy, and corticobasal degeneration) from Parkinson's disease in the 20th century also led to important discoveries of basal ganglia function, and in the case of Wilson's disease to recognition of genetic mutations and effective treatments. Choreoathetosis: Since the middle ages, the term chorea has been used to describe both organic and psychological disorders of motor control. Paracelcus introduced the concept of chorea as an organic medical condition in the 16th century. Sydenham's description of childhood chorea (1686) was followed by recognition in the 19th and 20th centuries that Sydenham's chorea was a manifestation of rheumatic fever; by the 1930s, rheumatic fever was recognized as a sequel of group A streptococcal pharyngitis, which could be effectively prevented with sulfonamides. Athetosis was described by Hammond (1871) and later linked by him to a malignant growth in the contralateral corpus striatum; nevertheless, athetosis has been controversial and often dismissed as a form of post-hemiplegic chorea or part of a continuum between chorea and dystonia. Huntington's classic description of adult-onset hereditary chorea (1872) was followed a century later by demonstration that Huntington's disease is caused by an unstable CAG trinucleotide repeat expansion in the Huntington disease gene on chromosome 4; this triggered a surge in research, development of various animal models, and numerous important discoveries of cell function and disease pathogenesis. Hemiballismus and the subthalamic nucleus: The relationship between a lesion of the subthalamic nucleus of Luys and contralateral hemiballismus was first convincingly demonstrated by Martin in 1927; this led 20 years later to development of an animal model by Whittier and Mettler, who produced experimental hemichorea-hemiballismus in monkeys by lesioning the contralateral subthalamic nucleus. Since the late 1980s, the neurochemistry and neurophysiology of the subthalamic nucleus have been substantially revised with the demonstration that the subthalamic nucleus is not fundamentally inhibitory but instead provides excitatory glutaminergic inputs to the globus pallidus, and appreciation that the subthalamic nucleus serves an important role in both hyperkinetic and hypokinetic movement disorders. Dystonia: Dystonias were often interpreted in psychological or psychiatric terms since the original descriptions of generalized dystonia by Barraquer Roviralta (1897), and familial forms of generalized primary tortion dystonia by Schwalbe (1908) and Oppenheim (1911). Although Oppenheim had first insisted that dystonia was an organic disease, it was only in the late-20th century that an organic framework was firmly established with the identification of genetic mutations in some families with dystonia and with the demonstration that the basal ganglia were often damaged contralateral to acquired hemidystonia. Focal and segmental forms of dystonia, including writer's cramp, other occupational dystonias, and torticollis, were also recognized in the 19th century. Writer's cramp was clearly described in the 1830s by Bell and Kopp, and increasingly recognized in the late 19th century due in part to Solly's influential lectures on scriviner's palsy in the 1860s, and to increasing prevalence because of the increase in writing using primitive writing instruments. Myoclonus: In 1903, Lundborg proposed a classification of myoclonus that remains in use, with primary (essential), epileptic, and secondary or symptomatic categories: essential myoclonus was described by Friedrich in 1881; forms of myoclonic epilepsy were described beginning in the late 19th century by West (1861), Unverricht (1891), and Lundberg (1903); and secondary multifocal myoclonus was recognized in a wide variety of disorders beginning in the 1920s. Asterixis was described in patients with hepatic encephalopathy by Adams and Foley in 1949 and found to result from electrically silent pauses in muscle activity, which led to the concept of negative myoclonus in the 1980s. Posthypoxic action myoclonus (Lance-Adams syndrome) was described by Lance and Adams in 1963 and found to incorporate both positive and negative components. Startle syndromes: Early descriptions of pathologic startle syndromes included Beard's description of the jumping Frenchmen of Maine (1878) and Hammond's description of miryachit (1884), both of which may have had psychological origins. In contrast, hyperekplexia or startle disease was described in the late 1950s and early 1960s, and genetic forms were later found to result from various mutations affecting glycinergic synapses. Tics: Tic disorders were described by Itard (1825) and Trousseau (1873), but only gained wider recognition in the late 19th century after Charcot presented cases before his classroom audiences and after Gilles de la Tourette's classic description in 1885. Gilles de la Tourette and Charcot initially considered tic disorders and startle syndromes to be similar if not identical, but these disorders were later recognized as distinct. Psychodynamic and psychological theories or etiology gave way in the 1960s to biological theories supporting an important role for dopamine in pathogenesis, particularly with the discovery that neuroleptic medications could be useful in treatment.In the last two centuries, neuroscientists and clinicians contributed greatly to our understanding of basal ganglia anatomy and physiology, as well as to movement disorder semiology, pathophysiology, treatment, and prevention. The development of animal models, and the increasing use of genetic and molecular biological techniques will lead to further advances in the coming years." @default.
• W1490666291 created "2016-06-24" @default.
• W1490666291 creator A5001877625 @default.
• W1490666291 date "2009-01-01" @default.
• W1490666291 modified "2023-10-02" @default.
• W1490666291 title "Chapter 33 The history of movement disorders" @default.
• W1490666291 cites W109017489 @default.
• W1490666291 cites W1182971956 @default.
• W1490666291 cites W132345155 @default.
• W1490666291 cites W143547764 @default.
• W1490666291 cites W1483198065 @default.
• W1490666291 cites W1483459119 @default.
• W1490666291 cites W1499794939 @default.
• W1490666291 cites W1512808451 @default.
• W1490666291 cites W1527671059 @default.
• W1490666291 cites W1545162411 @default.
• W1490666291 cites W1550876205 @default.
• W1490666291 cites W1599267686 @default.
• W1490666291 cites W175006040 @default.
• W1490666291 cites W1768450208 @default.
• W1490666291 cites W17925877 @default.
• W1490666291 cites W1850908299 @default.
• W1490666291 cites W1877873625 @default.
• W1490666291 cites W1888190124 @default.
• W1490666291 cites W1956187157 @default.
• W1490666291 cites W1963579110 @default.
• W1490666291 cites W1963626598 @default.
• W1490666291 cites W1963912731 @default.
• W1490666291 cites W1964512750 @default.
• W1490666291 cites W1964611988 @default.
• W1490666291 cites W1965271056 @default.
• W1490666291 cites W1965398181 @default.
• W1490666291 cites W1966151464 @default.
• W1490666291 cites W1967063692 @default.
• W1490666291 cites W1967633967 @default.
• W1490666291 cites W1967733235 @default.
• W1490666291 cites W1969800514 @default.
• W1490666291 cites W1970614181 @default.
• W1490666291 cites W1970855336 @default.
• W1490666291 cites W1971259313 @default.
• W1490666291 cites W1971630141 @default.
• W1490666291 cites W1972853510 @default.
• W1490666291 cites W1973055895 @default.
• W1490666291 cites W1974246224 @default.
• W1490666291 cites W1974873885 @default.
• W1490666291 cites W1976813386 @default.
• W1490666291 cites W1977090877 @default.
• W1490666291 cites W1978252125 @default.
• W1490666291 cites W1978883722 @default.
• W1490666291 cites W1979098045 @default.
• W1490666291 cites W1979523206 @default.
• W1490666291 cites W1979786105 @default.
• W1490666291 cites W1980071867 @default.
• W1490666291 cites W1980777453 @default.
• W1490666291 cites W1981823905 @default.
• W1490666291 cites W1982063599 @default.
• W1490666291 cites W1982279196 @default.
• W1490666291 cites W1982827121 @default.
• W1490666291 cites W1983149784 @default.
• W1490666291 cites W1985474993 @default.
• W1490666291 cites W1986042913 @default.
• W1490666291 cites W1986059795 @default.
• W1490666291 cites W1986245765 @default.
• W1490666291 cites W1986594553 @default.
• W1490666291 cites W1986988644 @default.
• W1490666291 cites W1987316957 @default.
• W1490666291 cites W1989848310 @default.
• W1490666291 cites W1989999317 @default.
• W1490666291 cites W1990080997 @default.
• W1490666291 cites W1990280414 @default.
• W1490666291 cites W1991004208 @default.
• W1490666291 cites W1991589426 @default.
• W1490666291 cites W1992583421 @default.
• W1490666291 cites W1993068285 @default.
• W1490666291 cites W1993177176 @default.
• W1490666291 cites W1993191686 @default.
• W1490666291 cites W1993470377 @default.
• W1490666291 cites W1994285647 @default.
• W1490666291 cites W1994893290 @default.
• W1490666291 cites W1995366178 @default.
• W1490666291 cites W1995597202 @default.
• W1490666291 cites W1996001974 @default.
• W1490666291 cites W1996679986 @default.
• W1490666291 cites W1996971698 @default.
• W1490666291 cites W1996993939 @default.
• W1490666291 cites W1997720284 @default.
• W1490666291 cites W1998453312 @default.
• W1490666291 cites W1999540740 @default.
• W1490666291 cites W1999893655 @default.
• W1490666291 cites W2000535168 @default.
• W1490666291 cites W2000705315 @default.
• W1490666291 cites W2000821135 @default.
• W1490666291 cites W2000893321 @default.
• W1490666291 cites W2002023508 @default.
• W1490666291 cites W2002216331 @default.
• W1490666291 cites W2002763309 @default.
• W1490666291 cites W2002867487 @default.
• W1490666291 cites W2004434463 @default.

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