2013
DOI: 10.2217/fnl.12.97
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Diagnosis and Management of Pediatric Peripheral Neuropathies In Resource-Poor Settings

Abstract: The diagnosis of a peripheral neuropathy in a child who resides in the majority of resource-poor settings is based on the history taken and the clinical examination. The majority of children, unless they demonstrate additional clinical markers, will lack a more definitive diagnosis beyond the label ‘peripheral neuropathy’. The treatable, typically acquired conditions, which are prevalent in these settings, are the priority to identify. This would include neuroinfections, neuroinflammation, toxins and vitamin d… Show more

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Cited by 8 publications
(6 citation statements)
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“…17 In the present day, the second largest group of heredodegenerative disorders with peripheral neuropathy can be diagnosed by specific metabolic or genetic testing without the need for a nerve biopsy. But in the absence of availability of these advanced tests, as in most developing countries, 6 nerve biopsy aids in definitive diagnosis, genetic counseling, and prognostication especially in patients with metachromatic leukodystrophy that forms a large proportion of cases in this category.…”
Section: Discussionmentioning
confidence: 99%
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“…17 In the present day, the second largest group of heredodegenerative disorders with peripheral neuropathy can be diagnosed by specific metabolic or genetic testing without the need for a nerve biopsy. But in the absence of availability of these advanced tests, as in most developing countries, 6 nerve biopsy aids in definitive diagnosis, genetic counseling, and prognostication especially in patients with metachromatic leukodystrophy that forms a large proportion of cases in this category.…”
Section: Discussionmentioning
confidence: 99%
“…[3][4][5] Etiologic spectrum of peripheral neuropathies in the pediatric age group differ depending on the settings and the inclusion criteria. 6 In resource-poor settings, acquired causes dominate in contrast to higher prevalence of hereditary neuropathies in high-income countries. [7][8][9] Etiologic categories also differ when peripheral nerve biopsy is used as the entry point for analysis and varies with specific age groups.…”
mentioning
confidence: 99%
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“…Insiden SGB usia 0-15 tahun di Amerika latin, Amerika Serikat, Finlandia, dan Taiwan sebesar 0,34-1,34/100,000 anak. 7 Pada SGB, 90%-95% mengalami pemulihan dalam kurun waktu 6-12 bulan. 7 Sebagian kecil SGB akan berlanjut menjadi CIDP yang dapat mengalami perbaikan klinis yang lambat.…”
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“…7 Pada SGB, 90%-95% mengalami pemulihan dalam kurun waktu 6-12 bulan. 7 Sebagian kecil SGB akan berlanjut menjadi CIDP yang dapat mengalami perbaikan klinis yang lambat. Perjalanan klinis DMD sangat lambat dan menyebabkan kematian di usia sekitar 20 tahun.…”
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