危重症患儿新发中枢性尿崩症的诊断和处理在儿科重症医学和儿科内分泌临床医生之间存在差异

IF 0.5 Q4 PEDIATRICS Journal of Pediatric Intensive Care Pub Date : 2022-09-14 DOI:10.1055/s-0042-1756309
R. B. Hunter, Herodes Guzman, Jessica M Winters, K. Lord, M. Kirschen, V. Srinivasan
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引用次数: 0

摘要

危重患儿中枢性尿崩症的诊断和处理不规范。我们的目的是表征儿科重症监护医学(PCCM)和儿科内分泌学(PE)临床医生在儿科重症监护病房新发CDI的诊断和管理方面的差异。我们还试图描述普通儿科(GP)居民的知识差距。这是一项基于场景的调查,旨在评估新发CDI的诊断和管理模式,该调查分发给在一家城市儿童医院工作的PCCM、PE和GP临床医生。在接受调查的275名PCCM、PE和GP临床医生中,158名(57%)做出了回应。PCCM临床医生比PE临床医生更多地依赖血清钠水平(96%比75%,p <0.01), PE临床医生比PCCM临床医生更多地依赖血清渗透压(91%比40%,p < 0.001)进行诊断。与PE临床医生相比,较少的PCCM倾向于将静脉输液限制在维持率的三分之二(4比37%,p <0.001)。与PE临床医生相比,更多的PCCM临床医生倾向于静脉输注抗利尿激素的起始剂量为0.5毫单位/千克/小时(76比53%,p = 0.048)。PCCM临床医生比PE临床医生更倾向于每20分钟滴注一次血管加压素(24比2%,p = 0.02),而PE临床医生比PCCM临床医生更倾向于每60分钟滴注一次(38比14%,p = 0.03)。接受培训较早的全科医生自我报告的知识差距更大。我们观察到PCCM、PE和GP临床医生对危重儿童新发CDI的诊断和管理存在很大差异。对这些病人的护理需要更大程度的标准化。
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Diagnosis and Management of New-Onset Central Diabetes Insipidus in Critically Ill Children Varies between Pediatric Critical Care Medicine and Pediatric Endocrinology Clinicians
The diagnosis and management of central diabetes insipidus in critically ill children is not standardized. Our objective was to characterize differences between Pediatric Critical Care Medicine (PCCM) and Pediatric Endocrinology (PE) clinicians in the diagnosis and management of new-onset CDI in the pediatric intensive care unit. We also sought to characterize knowledge gaps among general pediatrics (GP) residents. This is a scenario-based survey to assess patterns of diagnosis and management of new-onset CDI that was distributed to PCCM, PE, and GP clinicians who work in a quaternary care urban children's hospital. Of 275 PCCM, PE, and GP clinicians surveyed, 158 (57%) responded. More PCCM than PE clinicians relied on serum sodium levels (96 vs. 75%, p <0.01) and more PE than PCCM clinicians relied on serum osmolality (91 vs. 40%, p < .001) for diagnosis. Fewer PCCM than PE clinicians favored restricting IV fluids to two-thirds maintenance rate (4 vs. 37%, p <0.001). More PCCM than PE clinicians favored a starting dose of 0.5 milli-units/kg/h for IV vasopressin infusion (76 vs. 53%, p = 0.048). More PCCM clinicians than PE clinicians favored titrating the IV vasopressin infusion every 20 minutes (24 vs. 2%, p = 0.02), whereas more PE clinicians than PCCM clinicians favored titration every 60 minutes (38 vs. 14%, p = 0.03). GP residents earlier in training had greater self-reported gaps in knowledge. We observed substantial variability in the diagnosis and management of new-onset CDI in critically ill children among PCCM, PE, and GP clinicians. There is a need for greater standardization in care of these patients.
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