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高胰岛素血症性低血糖和由此导致的婴儿痉挛的临床问题。

The clinical problem of hyperinsulinemic hypoglycemia and resultant infantile spasms.

机构信息

Developmental Endocrinology Research Group, Clinical and Molecular Genetics Unit, Institute of Child Health, University College London, 30 Guilford St, London WC1N 1EH, United Kingdom.

出版信息

Pediatrics. 2010 Nov;126(5):e1231-6. doi: 10.1542/peds.2009-2775. Epub 2010 Oct 18.

Abstract

Hyperinsulinemic hypoglycemia (HH) is a cause of severe hypoglycemia in the newborn and infancy period and is associated with a high risk of neurologic handicap and epilepsy. Infantile spasms after exposure to HH is rare and has been described in only 1 previous report. We report the clinical, biochemical, and neurodevelopmental characteristics of 5 patients with neonatal-onset HH who subsequently developed infantile spasms. All 5 patients had neonatal-onset HH of varying severity and duration. These patients presented with the characteristic ictal pattern of spasms in clusters at a mean age of 6.6 months. Characteristic hypsarrhythmia was noted in only 3 of 5 patients. Structural abnormality was found in only 1 of 4 patients who underwent MRI of the brain. Infantile spasms responded to medical treatment in 3 patients, spasms in 1 patient were refractory to antiepileptic drugs, and treatment duration was insufficient for us to comment on the response in 1 patient. Developmental delay was evident in all of them. In conclusion neonatal HH of varying severity is associated with later (after a latent period) development of infantile spasms. The latent period before the onset of the spasms can be variable; hence, long-term neurodevelopmental follow-up (until 1 year of age) is necessary.

摘要

高胰岛素血症性低血糖(HH)是新生儿和婴儿期严重低血糖的原因,与神经功能障碍和癫痫的高风险相关。HH 暴露后婴儿痉挛很少见,仅在 1 份先前的报告中描述过。我们报告了 5 例新生儿期 HH 后发生婴儿痉挛的患者的临床、生化和神经发育特征。所有 5 例患者均有不同严重程度和持续时间的新生儿期 HH。这些患者以平均 6.6 个月的年龄出现特征性痉挛发作簇的癫痫发作模式。仅 5 例患者中的 3 例出现特征性高波幅失律。仅 4 例接受脑部 MRI 的患者中发现结构异常。3 例患者对药物治疗有反应,1 例患者的痉挛对抗癫痫药物耐药,1 例患者的治疗时间不足,我们无法对其反应进行评论。他们所有人都有明显的发育迟缓。总之,不同严重程度的新生儿 HH 与痉挛的后期(潜伏期后)发展有关。痉挛发作前的潜伏期可能不同;因此,需要进行长期的神经发育随访(直到 1 岁)。

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