首页> 外文期刊>The Tohoku Journal of Experimental Medicine >Late-Onset Glucocorticoid-Responsive Circulatory Collapse in Preterm Infants: Clinical Characteristics of 14 Patients
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Late-Onset Glucocorticoid-Responsive Circulatory Collapse in Preterm Infants: Clinical Characteristics of 14 Patients

机译:早产儿糖皮质激素反应迟缓的循环塌陷:14例患者的临床特征

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Preterm infants may develop acute systemic hypotension that responds to glucocorticoid therapy, but not to volume loading or vasopressors, during the postnatal period. This condition is termed late-onset circulatory collapse (LCC) that develops a few weeks after birth in relatively stable infants. LCC may cause periventricular leukomalacia, periventricular necrosis in the white matter. The aim of this study was to identify the clinical characteristics of LCC. We retrospectively reviewed the clinical data of infants with LCC. Among 41 infants born at < 29 weeks of gestation between 2010 and 2014, we identified 14 infants (median gestational age 25.6 weeks) with LCC. All infants were stable before the acute onset of circulatory collapse at a median age of 21 days, which is characterized by the decreased physical activity, systolic blood pressure (12 mmHg decrease), urine output (76% decrease), and serum sodium level (4 mEq/L decrease), and the increased resistance index in the cerebral and renal arteries on Doppler ultrasonography. Both left ventricular dimension and contraction were well preserved. Three infants developed hyperkalemia. The median time from the initial hydrocortisone dose to improvements was 4 h (interquartile range 3-5 h). Hydrocortisone therapy was effective, but had to be withdrawn slowly to prevent relapse. The median duration of hydrocortisone therapy was 23 days. There was no evidence of periventricular leukomalacia in any of the infants. None of the infants developed adrenal insufficiency during the follow-up period. During the acute stage of LCC, the main priority is the early initiation of glucocorticoid therapy.
机译:早产儿在出生后可能会出现急性全身性低血压,对糖皮质激素治疗有反应,但对容量负荷或升压药无反应。这种情况被称为迟发性循环衰竭(LCC),在相对稳定的婴儿出生后几周发展。 LCC可能引起脑室白细胞软化,脑室周围白质坏死。这项研究的目的是确定LCC的临床特征。我们回顾性地回顾了LCC婴儿的临床资料。在2010年至2014年间,妊娠<29周出生的41例婴儿中,我们鉴定出14例LCC婴儿(中位孕龄25.6周)。所有婴儿在中位年龄为21天的急性循环衰竭之前均处于稳定状态,其特征在于体力活动减少,收缩压降低(降低12 mmHg),尿量(降低76%)和血清钠水平(降低4 mEq / L),并在多普勒超声检查中增加脑和肾动脉的抵抗指数。左心室的尺寸和收缩都得到了很好的保存。三名婴儿出现高钾血症。从氢化可的松初始剂量到改善的中位时间为4小时(四分位间距3-5小时)。氢化可的松疗法有效,但必须缓慢撤药以防止复发。氢化可的松治疗的中位时间为23天。没有任何婴儿脑室周围白细胞减少的证据。在随访期间,没有婴儿出现肾上腺功能不全。在LCC的急性期,主要优先事项是尽早开始糖皮质激素治疗。

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