Faculty Bibliography

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Movement disorders. 1989:4(4):363-70.DOI: 10.1002/mds.870040414

Case 1, 1989: juvenile-onset parkinsonism, dystonia, and pyramidal tract signs [Case Report]

Kang, U J; Fahn, S; Schwarz, H; Shoulson, I; Vallejos, H; Goldman, J
PMID: 2530440
ISSN: 0885-3185
CID: 3697622
Rational drug therapy. 1988:22(8):1-7.DOI:

Management of tardive dyskinesia

Kang, U J; Fahn, S
PMID: 3064135
ISSN: 0031-7020
CID: 3651622
Current opinion in neurology & neurosurgery. 1988:1:316-318.DOI:

RECOGNIZING AKATHISIA AS A MOVEMENT DISORDER

BURKE, RE; KANG, UJ
ISI:A1988Q677700014
ISSN: 0951-7383
CID: 3696852
Advances in neurology. 1988:49:199-210.DOI:

Tardive dystonia: clinical aspects and treatment

Burke, R E; Kang, U J
PMID: 3278541
ISSN: 0091-3952
CID: 3651632
Advances in neurology. 1988:50:415-29.DOI:

Tardive dystonia

Kang, U J; Burke, R E; Fahn, S
We retrospectively reviewed the clinical course and response to treatment of 67 patients with tardive dystonia. The age at onset ranged from 13 to 72 years without predilection to any particular age group or sex. Patients developed tardive dystonia even after relatively short duration of exposure to dopamine antagonists (21% within 1 year). Five of 42 patients withdrawn from these drugs remitted. Overall clinical improvement occurred in 52% of patients. Tetrabenazine and reserpine were most effective (greater than 50% response rate) in controlling dystonia. Anticholinergic drugs diminished dystonia in 46% of patients. In conclusion, this review supports our original concept of tardive dystonia as a subtype of tardive dyskinesia, which is quite disabling, usually persistent, and difficult to treat. Although anticholinergics and dopamine-depleting drugs frequently improved symptoms, treatment with them only rarely led to a remission or satisfactory control of symptoms. The difficulty of treating this condition necessitates reemphasis of one important observation of this study, that this condition may develop early in the course of dopamine antagonist treatment; there is no minimum period of exposure which can be considered safe. These drugs must therefore be used only for correct medical indications, and every attempt should be made to withdraw them at the first sign of dyskinesia, particularly of the dystonic type.
PMID: 3400500
ISSN: 0091-3952
CID: 3733812
Journal of neurology neurosurgery & psychiatry. 1986:49(9):1087-8.DOI: 10.1136/jnnp.49.9.1087

A case of parkinsonism following striatal lacunar infarction [Letter]

Friedman, A; Kang, U J; Tatemichi, T K; Burke, R E
PMCID:1029022
PMID: 3760901
ISSN: 0022-3050
CID: 3733822
Neurology. 1986:36:121-121.DOI:

NATURAL-HISTORY AND TREATMENT OF TARDIVE DYSTONIA [Meeting Abstract]

KANG, UJ; BURKE, RE; FAHN, S
ISI:A1986A889100153
ISSN: 0028-3878
CID: 3651832
Movement disorders. 1986:1(3):193-208.DOI: 10.1002/mds.870010305

Natural history and treatment of tardive dystonia

Kang, U J; Burke, R E; Fahn, S
We retrospectively reviewed the clinical course and response to treatment of 67 patients with tardive dystonia. The age at onset ranged from 13 to 72 years without predilection to any particular age group or sex. Patients developed tardive dystonia even after relatively short duration of exposure to dopamine antagonists (21% within one year). Five of 42 patients withdrawn from these drugs remitted. Overall clinical improvement occurred in 52% of patients. Tetrabenazine and reserpine were most effective (greater than 50% response rate) in controlling dystonia. Anticholinergic drugs diminished dystonia in 46% of patients.
PMID: 2904118
ISSN: 0885-3185
CID: 3651602