Clinical and Etiological Profile of Tropical Ataxic Neuropathy in Kerala, South India

Madhusudanan, M; Menon, Murali Krishna; Ummer, Karaden; Radhakrishnanan, Kurupath

doi:10.1159/000127975

Cited by 34 publications

(18 citation statements)

References 24 publications

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“…10,11 Further susceptibility to neurotoxicity may be associated with certain micronutrient deficiencies, which needs to be explored. 12,13 Based on these findings in a small group, it may be difficult to make significant suggestions. It would be pertinent to asssess the possibility of enhanced genetic or environmental susceptibility of Indian children to the neurotoxic effects of vincristine in a larger study.…”

Section: Discussionmentioning

confidence: 99%

Vincristine induced neurotoxicity in cancer patients

2009

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Ten out of 20 children, treated with usual doses of vincristine for various types of childhood cancers, developed neurotoxicity during treatment. Peripheral neurotoxicity (mixed motor-sensory 4/10, pure motor 3/10, pure sensory 3/10) was seen in the form of weakness of lower limbs, areflexia, neuropathic pain, or sensory loss. Autonomic neuropathy presented as constipation and urinary retention in 2 children, while 2 children developed encephalopathy in form of seizures, confusion, aphasia, and transient blindness. In children with severe neuropathy, vincristine administration was withheld/dose reduced till clinical improvement started, which took about 2-3 weeks time. Nerve conduction velocity showed motor-sensory axonal polyneuropathy. Electrophysiological abnormalities were found to persist even six months after clinical recovery in children with neurotoxicity. We found a relatively higher incidence of vincristine induced neuropathy in Indian children, which was probably due to coexistence of severe malnutrition in them.

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Section: Discussionmentioning

confidence: 99%

Vincristine induced neurotoxicity in cancer patients

2009

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“…First, the above-mentioned disorders e.g. konzo and TAN consistently share common etiological factors including poor nutrition and cassava cyanogenic toxicity (Banea-Mayambu et al, 1997, Oluwole et al, 2000, Madhusudanan et al, 2008). Second, key biomarkers e.g.…”

Section: Introductionmentioning

confidence: 99%

Determinants of cognitive performance in children relying on cyanogenic cassava as staple food

et al. 2014

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Background While risk factors for konzo are known, determinants of cognitive impairment in konzo-affected children remain unknown. Method We anchored cognitive performance (KABC-II scores) to serum levels of free-thyroxine (free-T4), thyroid-stimulating hormone (TSH), albumin, and motor proficiency (BOT-2 scores) in 40 children including 21 with konzo (median age: 9 years) and 19 without konzo (median age: 8 years). A multiple regression model was used to determine variables associated with changes in KABC-II scores. Results Age (β: − 0.818, 95%CI: − 1.48, − 0.152) (p=0.018), gender (β: − 5.72; 95% CI: − 9.87, −1.57 for females) (p=0.009), BOT-2 score (β: 0.390; 95% CI: 0.113, 0.667) (p=0.008), and free-T4 (β: 1.88; 95% CI: 0.009, 3.74) (p=0.049) explained 61.1% of variation in KABC-II scores. Subclinical hypothyroidism was not associated with poor cognition. A crude association was found between serum albumin and KABC-II scores (β: 1.26; 95% CI: 0.136, 2.39) (p=0.029). On spot urinary thiocyanate reached 688 μmol/l in children without konzo and 1032 μmol/L in those with konzo. Conclusion Female gender and low serum albumin are risk factors common to cognitive and proportionally associated motor deficits in children exposed to cassava cyanogens. The two types of deficits may share common mechanisms.

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“…Cassava consumption causes neuropathies, widely reported from African continent, Tanzania and Zaire designation as Konzo [5][6][7] and Epidemic spastic paraparesis or Mantekassa in Mozambique, tropical ataxic neuropathy in Nigeria [4]. Recently tropical ataxic neuropathy was also reported from Kerala, India [8]. Various nutritional causes of cyanide poisoning including cassava have been elaborated in a recent review [9,10].…”

Section: Introductionmentioning

confidence: 99%

Effect of Alpha-Ketoglutarate on Neurobehavioral, Neurochemical and Oxidative Changes Caused by Sub-Chronic Cyanide Poisoning in Rats

et al. 2010

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Recent studies revealed that alpha-ketoglutarate (A-KG) alone or with sodium thiosulfate (STS) provide significant protection against acute and sub-acute cyanide poisoning in rodents. This study addresses the protective effect of A-KG and/or STS in sub-chronic (90 days) cyanide poisoning. Wistar rats were divided into seven groups (n = 10): Control animals, potassium cyanide (KCN) A-KG, STS, KCN ? A-KG, KCN ? STS and KCN ? A-KG ? STS. Spontaneous motor activity and motor coordination were recorded every 15th day. Lipid peroxidation (LPO), reduced glutathione (GSH), glutathione peroxidase (GPx), superoxide dismutase (SOD) and catalase (CAT) in blood, brain, liver and kidney, and glutamate, aspartate and dopamine in discrete regions of brain were measured following 90 days exposure. Cyanide significantly decreased motor coordination, accompanied by increase in LPO (blood, brain and liver) and dopamine (corpus striatum and cerebral cortex) levels, and depletion in GSH (blood, brain and liver), GPx (brain and liver), SOD (brain and liver), and CAT (blood and brain) levels. Although treatment of A-KG and STS alone significantly blunted the toxicity of KCN, concomitant use of both afforded the maximum protection. This study shows a promising role of A-KG and STS as treatment regime for long term cyanide exposure.

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Clinical and Etiological Profile of Tropical Ataxic Neuropathy in Kerala, South India

Cited by 34 publications

References 24 publications

Vincristine induced neurotoxicity in cancer patients

Vincristine induced neurotoxicity in cancer patients

Determinants of cognitive performance in children relying on cyanogenic cassava as staple food

Effect of Alpha-Ketoglutarate on Neurobehavioral, Neurochemical and Oxidative Changes Caused by Sub-Chronic Cyanide Poisoning in Rats

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