首页> 美国卫生研究院文献>Journal of the Endocrine Society >Neonatal Hypo-Ketotic Hypoglycemia Secondary to Transient Hyperinsulinism: Diazoxide Responsiveness and Experience With Fasting Test After Treatment Withdrawal
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Neonatal Hypo-Ketotic Hypoglycemia Secondary to Transient Hyperinsulinism: Diazoxide Responsiveness and Experience With Fasting Test After Treatment Withdrawal

机译:新生儿的乳腺癌二血糖二生虫素:治疗后禁食试验的二氧化物反应性和经验

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摘要

Introduction:: Transient neonatal hyperinsulinism (TNH) is frequently reported in neonates with stress factors (intrauterine growth restriction (IUGR), large for gestational age (LGA), perinatal asphyxia, infants of diabetic mother, etc.). Early recognition and treatment are prioritary to avoid neurological morbidity. Objective: Clinical, molecular characterization and treatment response in neonates with hypoglycemia due to transient hyperinsulinism admitted to a tertiary hospital Neonatal Unit from January 2015 to August 2020. Materials and Methods: Prospective cohort study. Newborns older than 7 days of age, with diagnostic criteria of hyperinsulinism: non ketotic hypoglycemia with detectable insulin, low free fatty acids, glucose infusion rate > 10mg/kg/min, and positive response to glucagon test, were recruited. Results: Out of 5374 patients admitted, 46 (0.85%) presented hypoglycemia secondary to TNH (57% males and 43% females). 78% were delivered by Cesarean section, 59% were European, 17% Latino-Americans, 11% Asians, 9% Africans, and 4% Arabs. 78% were preterm newborns (median 33 weeks gestational age), 70% had birth weights or heights <-1.6 SDS (medians: -1.8 SDS and -2 SDS, respectively). Median age at diagnosis was 22 days (IQE 10–29 days), and feeding was exclusively enteral. Median blood glucose at diagnosis was 37mg/dl (IQE 31-44mg/dl), median insulin: 3mu/ml, median ketonemia: 0.2mmol/L, GH: 15 ng/ml, Cortisol: 16 ug/dl and AAL: 75mg/dl. 90% received diazoxide (dose ranged between 5-10mg/kg/day), presenting as most prevalent side effects hypertrichosis (80%) and edema (13%). Diazoxide median treatment duration was 83 days (IQE 41–110). Response was positive in 100%, with fasting tests response yielding a glycemia > 60mg / dl after 10 hours of fasting post treatment withdrawal. Molecular analysis was carried out with help of a custom NGS panel (MonDIAB.V3; 385 genes) in 80% of the patients. No mutations were identified in known genes implicated in the etiology of congenital hyperinsulinism (ABCC8, KCNJ11, HNF4A, GLUD1, HADH, SLC16A1, GCK, UCP2, HNF1A, AKT2, INSR, CACNA1D), however, predicted deleterious variants were found in other candidate genes such as G6PC2, TH, PMM2, and APPL1, implicated in insulin secretion or glycemic homeostasis. Conclusions: TNH is a prevalent entity to be considered in neonates with risk factors. In our series, TNH is also present in term newborns (22% of patients) and in newborns with weight and/or height appropriate for gestational age (30%). Treatment with diazoxide at low doses is effective in the resolution of these hypoglycemias. The fasting test could be useful for a safe treatment withdrawal when resolution is suspected. No monogenic cause explaining the TNH was identified. Most of the cases molecularly examined presented with 2 or more predicted deleterious variants, suggesting a multifactorial genetic component.
机译:介绍::瞬态新生儿高胰岛素素(TNH)经常用压力因子(宫内生长限制(IUGR),胎儿症,蛇形肾脏,糖尿病母亲的婴儿等大肿瘤。)。早期识别和治疗良好是避免神经系统发病率。目的:从2015年1月到2020年1月入院的瞬态高胰岛素中的新生儿患者患有低血糖的临床,分子表征和治疗响应。材料与方法:预期队列研究。新生儿超过7天的年龄,具有诊断性高胰岛素中的标准:具有可检测的胰岛素,低离去脂肪酸,葡萄糖输注速率> 10mg / kg / min的非酸钠低血糖,以及对胰高血糖素测试的阳性反应。结果:5374名患者入院中,46名(0.85%)呈现次级血糖继发于TNH(57%的男性和43%的女性)。 78%的剖宫产分为78%,59%是欧洲,17%的拉丁裔美国人,11%的亚洲人,9%的非洲人和4%阿拉伯人。 78%是早产新生儿(中位数33周的孕龄),70%出生体重或高度<-1.6 sds(中位数:-1.8 sds和-2 sds)。诊断的中位年龄为22天(IQE 10-29天),喂养完全是肠内。诊断中的中位血糖是37mg / dl(IQe 31-44mg / dl),中位胰岛素:3mu / ml,中位数酮血症:0.2mmol / L,GH:15ng / ml,皮质醇:16 ug / dl和aal:75mg / dl。 90%接受二氮氧化物(剂量范围为5-10mg / kg /天),呈现为最普遍的副作用Hypertrichosis(80%)和水肿(13%)。二酰氧化物中值治疗持续时间为83天(IQE 41-110)。响应在100%的阳性下呈阳性,禁食试验响应在禁食后处理后10小时后产生糖血症> 60mg / dl。在80%的患者中,通过定制NGS面板(MondiaB.V3; 385基因)的帮助进行分子分析。在与先天性含硫素(ABCC8,KCNJ11,HNF4A,GLUD1,HANF4A,GLUD1,HNF4A,SLC16A1,GCK,UCP2,HNF1A,AKT2,INSR,CACNA1D)中没有鉴定突变,然而,在其他候选人中发现了预测的有害变体基因如G6PC2,Th,PMM2和Appl1,涉及胰岛素分泌或血糖性稳态。结论:TNH是在新生儿的危险因素中考虑的普遍存在。在我们的系列中,TNH还在新生儿(22%的患者)和新生儿中,其重量和/或高度适合于孕龄(30%)。在低剂量下用二氧芳氧化物治疗在这些低血糖的分辨率下是有效的。在怀疑分辨率时,禁食测试可用于安全处理。鉴定了未解释TNH的单体原因。大多数病例分子检查呈现出2个或更多的预测有害变体,表明多因素遗传组分。

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