Find information on thousands of medical conditions and prescription drugs.

Tardive dyskinesia

Tardive dyskinesia is a serious neurological disorder caused by the long-term and/or high-dose use of dopamine antagonists, usually antipsychotics and among them especially the typical antipsychotics. These neuroleptic drugs are generally prescribed for serious psychiatric disorders. The older typical antipsychotics, which appear to cause tardive dyskinesia somewhat more often than the newer atypical antipsychotics, are being prescribed less frequently. There are some new uses, however, such as year-long implants that are being developed using the older typicals, e.g. more...

Home
Diseases
A
B
C
D
E
F
G
H
I
J
K
L
M
N
O
P
Q
R
S
T
Candidiasis
Tachycardia
Taeniasis
Talipes equinovarus
TAR syndrome
Tardive dyskinesia
Tarsal tunnel syndrome
Tay syndrome ichthyosis
Tay-Sachs disease
Telangiectasia
Telangiectasia,...
TEN
Teratoma
Teratophobia
Testotoxicosis
Tetanus
Tetraploidy
Thalassemia
Thalassemia major
Thalassemia minor
Thalassophobia
Thanatophobia
Thoracic outlet syndrome
Thrombocytopenia
Thrombocytosis
Thrombotic...
Thymoma
Thyroid cancer
Tick paralysis
Tick-borne encephalitis
Tietz syndrome
Tinnitus
Todd's paralysis
Topophobia
Torticollis
Touraine-Solente-Golé...
Tourette syndrome
Toxic shock syndrome
Toxocariasis
Toxoplasmosis
Tracheoesophageal fistula
Trachoma
Transient...
Transient Global Amnesia
Transposition of great...
Transverse myelitis
Traumatophobia
Treacher Collins syndrome
Tremor hereditary essential
Trichinellosis
Trichinosis
Trichomoniasis
Trichotillomania
Tricuspid atresia
Trigeminal neuralgia
Trigger thumb
Trimethylaminuria
Triplo X Syndrome
Triploidy
Trisomy
Tropical sprue
Tropophobia
Trypanophobia
Tuberculosis
Tuberous Sclerosis
Tularemia
Tungiasis
Turcot syndrome
Turner's syndrome
Typhoid
Typhus
Tyrosinemia
U
V
W
X
Y
Z
Medicines

, Haldol®, one of the worst offenders when it comes to tardive dyskinesia. Other dopamine antagonists that can cause tardive dyskinesia are drugs for gastrointestinal disorders (for example metoclopramide) and neurological disorders. Some drugs that are not intended to affect dopamine, such as SSRI antidepressants, may also cause tardive dyskinesia. The new generation of atypical antipsychotics appears to cause tardive dyskinesia somewhat less frequently (though they may cause serious metabolic disorders, e.g., diabetes, frequently enough to make them equally dangerous).

The term tardive dyskinesia was introduced in 1964. Dyskinesia means "abnormal movement" and tardive means "late", signifying that the dyskinesia only occurs after some time has elapsed following initial administration of the neuroleptic drug.

Features

Tardive dyskinesia is characterized by repetitive, involuntary, purposeless movements. Features of the disorder may include grimacing, tongue protrusion, lip smacking, puckering and pursing of the lips, and rapid eye blinking. Rapid movements of the arms, legs, and trunk may also occur. Impaired movements of the fingers may appear as though the patient is playing an invisible guitar or piano. Many of the symptoms of tardive dyskinesia appear similar to Parkinson's disease.

Cause

The cause of tardive dyskinesia appears to be related to damage — due to the use of antipsychotic medications — to the system that uses and processes the neurotransmitter dopamine. It is thought that postsynaptic dopaminergic receptors become supersensitive to stimulation during neuroleptic treatment and that this supersensitivity causes the symptoms of tardive dyskinesia. The available research seems to suggest that the concurrent prophylactical use of a neuroleptic and an antiparkinsonian drug is useless to avoid early extrapyramidal side-effects and may render the patient more sensitive to tardive dyskinesia.

Treatment

Primary prevention of tardive dyskinesia is achieved by using the lowest effective dose of a neuroleptic for the shortest time. If tardive dyskinesia is diagnosed, the causative drug should be reduced or discontinued if possible. Tardive dyskinesia may persist after withdrawal of the 'offending neuroleptic' for months, years, or even permanently. There is no known cure for tardive dyskinesia, but preliminary research suggests that the atypical neuroleptic Clozaril (Clozapine®) may improve the state of the patient. Improvements are also seen in some cases, if the high potency benzodiazepines - lorazepam (Ativan®), diazepam (Valium®), or clonazepam (Klonopin®)—are used. The findings about the effects of natural substances, such as vitamin E (Alpha-Tocopherol) or melatonin, are inconclusive. Treatment with adrenergic blocking agents and dopamine agonists like bromocriptin also remains somewhat controversial. There have been some reports of promising effects from the drug tetrabenazine (a different kind of neuroleptic). On the contrary, most antiparkinsonian drugs worsen the state of the patient.

Read more at Wikipedia.org


[List your site here Free!]


Olanzapine and trihexyphenidyl-induced tardive dyskinesia
From Indian Journal of Pharmacology, 7/1/05 by D. Mendhekar

Byline: D. Mendhekar, A. Aggarwal

Olanzapine, a thienobenzodiazepine derivative, is a second generation (atypical) antipsychotic agent, which has been proven efficient against the positive and negative symptoms of schizophrenia, with a low propensity to induce tardive dyskinesia (TD). Compared with typical antipsychotics, it has a greater affinity for serotonin 5-HT2A than dopamine D2 receptors. Olanzapine is thought to have preferential action at mesolimbic over nigrostriatal dopaminergic pathways and therefore associated with a very low incidence of extrapyramidal side effects (EPS) than observed with typical antipsychotic drugs.[1] Furthermore, a retrospective analysis of controlled multicentric trials and numerous case reports of patients with psychotic disorders including schizophrenia suggested that olanzapine even improves pre-existing symptoms of tardive movements.[1] Till now, very few reports of olanzapine-related TD are available in the existing literature. [2],[3],[4],[5],[6] The essential features of antipsychotic-induced TD are abnormal, involuntary movements of the tongue, jaw, trunk or extremities that develop in association with the use of antipsychotic medications. We wish to report another case of TD, which developed after 6 months of treatment with olanzapine.

Mr. A, 30 years old, married, male was suffering from schizophrenia (DSM-IV criteria) for the last 2 years. His sister and brother were both taking treatment for seizure disorder. For the first time in April 2001, the patient was treated with trifluoperazine 20 mg, Chlorpromazine 400 mg, and trihexyphenidyl 2 mg daily for 6 months without any evidence of movement disorders. In October 2001, all the medications mentioned earlier were stopped because he was not showing adequate response, and olanzapine, 5 mg per day was started which was gradually increased to 20 mg per day over a period of 6 weeks. Subsequently, at day 7 of olanzapine 20 mg per day therapy, he exhibited EPS in the form of bradykinesia, tremors, rigidity, and salivation for which, trihexyphenidyl 4 mg per day was added and successful amelioration of EPS occurred. Trihexyphenidyl was not stopped or tapered because of the risk of reemergence of extrapyramidal symptoms. In March 2002, during follow-up, while the patient was on olanzapine 20 mg and trihexyphenidyl 4 mg per day for nearly 6 months, he exhibited moderate severity of stereotypic movements of fingers of both the hands as if he was playing the piano. These movements would be more prominent on distracting his attention from them. A diagnosis of olanzapine and trihexyphenidyl induced TD was made after conducting relevant investigations, including CT Head and electroencephalograph, which were within normal limits. His routine biochemical profile was also within normal limits. He scored 7 on the Abnormal Involuntary Movement Scale. Subsequently, olanzapine was replaced by clozapine 25 mg daily, which was increased to 100 mg per day over a period of 5 weeks. The patient showed complete recovery of the abnormal movements within 2 months of clozapine therapy. The patient is presently maintained on clozapine 100 mg per day without any reemergence of TD.

Mr. A, developed TD while he was on olanzapine and trihexyphenidyl. Our report suggests that past history of antipsychotic-induced EPS and family history of neurological disorder such as seizure disorder may be important risk factors for developing TD with atypical antipsychotics, although evidence is inconsistent even with typical antipsychotic drugs. In this report, it needs to be acknowledged that there was a past history of neuroleptic exposure and this could complicate the clinical picture, because the neuroleptic used was a high potency typical antipsychotic.

In this report, one may consider the possibility of drug-withdrawal dyskinesia, which typically begins within a few days after an abrupt dosage decrease and becomes worse as the neuroleptic is withdrawn. A clinical examination cannot distinguish between withdrawal dyskinesia and other involuntary movements, as they are same as other varieties of TD. In our case, neither the dose of olanzapine was reduced nor stopped before the appearance of dyskinetic movements. Although withdrawal emergent dyskinesia with typical neuroleptics is a well-known entity, here trifluperazine was stopped completely 6 months before the onset of TD. Hence, there was no temporal correlation between withdrawal of typical neuroleptic drug and emergence of dyskinetic movements. One of the striking features of this report was that Mr. A developed EPS with olanzapine therapy when treated with trihexyphenidyl. It is known that severe EPS requiring medication intervention is rare with olanzapine, though not impossible.[7] As seen in our case report, clozapine has been used successfully in olanzapine-induced TD.[4],[5] However, more data is required to know the typical characteristics and risk factors associated with olanzapine induced TD.

References

1. Bhana N, Foster RH, Onley R, Plosker GL. Olanzapine: An updated review. Drugs 2001;61:111-61.

2. Ananth J, Kenan J. Tardive dyskinesia associated with olanzapine monotherapy. J Clin Psychiatry 1999;60:870.

3. Bella VL, Piccoli F. Olanzapine-induced tardive dyskinesia. Br J Psychiatry 2003;182:81-2.

4. Dunayyevich E, Strakawsk SM. Olanzapine-induced tardive dyskinesia. Am J Psychiatry 1999;156:1662.

5. Herran A, Vazquez-Barquero JL. Tardive dyskinesia associated with olanzapine. Ann Intern Med 1999;131:72.

6. Bhanji NH, Margolese HC. Tardive dyskinesia associated with olanzapine in a neuroleptic-naive patient with schizophrenia. Can J Psychiatry 2004;49:343.

7. Richelson E. Receptor pharmacology of neuroleptics: Relation to clinical effects. J Clin Psychiatry 1999;60: 5-14.

COPYRIGHT 2005 Medknow Publications
COPYRIGHT 2005 Gale Group

Return to Tardive dyskinesia
Home Contact Resources Exchange Links ebay