Unique cerebral dysfunction following triphenyltin acetate poisoning

1 In animal studies, TPTA was found to be neurotoxic. In humans, variable CNS pictures have been described with or without significant EEG findings. Brain CT does not usually reveal any abnormalities. 2 Our patient presented with intermittent unique spontaneous involuntary movement of hands, facial...

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Bibliographic Details
Published in:Human & experimental toxicology 1998-07, Vol.17 (7), p.403-405
Main Authors: Lin, Tzeng-Jih, Hung, Dong-Zong, Kao, Chia-Hung, Hu, Wei-Hsiung, Yang, Dar-Yu
Format: Article
Language:English
Subjects:
Adult
Biological and medical sciences
Brain - drug effects
Brain - pathology
Central Nervous System - drug effects
Chemical and industrial products toxicology. Toxic occupational diseases
Cognition - drug effects
Electroencephalography - drug effects
Female
Fungicides, Industrial - poisoning
Humans
Medical sciences
Metals and various inorganic compounds
Motor Activity - drug effects
Organotin Compounds - poisoning
Suicide, Attempted
Toxicology
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Summary:1 In animal studies, TPTA was found to be neurotoxic. In humans, variable CNS pictures have been described with or without significant EEG findings. Brain CT does not usually reveal any abnormalities. 2 Our patient presented with intermittent unique spontaneous involuntary movement of hands, facial twitching, silly smile and crying. Diplopia, drowsiness, giddiness, vertigo, bidirectional nystagmus, impairment of calculation ability, as well as disorientation to time, people and place also developed. EEG showed mild cortical dysfunction without seizures. MRI and Tc-99m HMPAO brain SPECT revealed no significant findings. TPTA may cause cellular dysfunction of brain without structural damage, which results in variable CNS clinical presentations. 3 Nadir of leucopenia was noted on the sixth day after consumption of TPTA. Liver impairment occurred on the ninth day. Borderline demyelinated neuropathy developed on the fifty-third day. CNS abnormalities, delayed peripheral neuropathy, hepatitis and leucopenia deserve monitoring for a prolonged period, even when the victim initially presents with GI upset only after consumption of TPTA.
ISSN:0960-3271
1477-0903
DOI:10.1177/096032719801700707