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European Society for Paediatric Endocrinology/Lawson Wilkins Pediatric Endocrine Society Consensus Statement on Diabetic Ketoacidosis in Children and Adolescents

机译:欧洲儿科内分泌学会/ Lawson Wilkins儿科内分泌社会对儿童和青少年糖尿病酮症性症的共识陈述

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Diabetic ketoacidosis (DKA) is the leading cause of morbidity and mortality in children with type 1 diabetes mellitus (TIDM). Mortality is predominantly related to the occurrence of cerebral edema; only a minority of deaths in DKA are attributed to other causes. Cerebral edema occurs in ~0.3% to 1% of all episodes of DKA, and its etiology, pathophysiology, and ideal method of treatment are poorly understood. There is debate as to whether physicians treating DKA can prevent or predict the occurrence of cerebral edema and the appropriate site(s) for children with DKA to be managed. There is agreement that prevention of DKA and reduction of its incidence should be a goal in managing children with diabetes.To explore these issues, the Lawson Wilkins Pediatric Endocrine Society (LWPES) and the European Society for Pediatric Endocrinology (ESPE) convened a panel‖ of expert physicians for a consensus conference. The meeting was chaired by Mark A. Sperling, MD, representing LWPES, and David B. Dunger, MD, representing ESPE. The Consensus statement was developed with close partnership between the ESPE and LWPES and the International Society for Pediatric and Adolescent Diabetes, all 3 organizations being represented by members who participated in the writing process. The statement also was endorsed by related organizations; the Juvenile Diabetes Research Foundation International, the World Federation of Pediatric Intensive and Critical Care Societies, the European Society for Pediatric Critical Care, the European Society of Pediatric and Neonatal Intensive Care, and the Australian Pediatric Endocrine Group were represented by invited participants.Each of the major topics had a presenter and recorder, responsible for review of the literature and providing evidence-based recommendations according to criteria used by the American Diabetes Association (see Appendix; levels of evidence are indicated in capital letters, in parentheses).1 Type 2 diabetes was not considered. All participants contributed … Address correspondence to David B. Dunger, Department of Paediatrics, University of Cambridge, Addenbrooke’s Hospital, Level 8, Box 116, Cambridge CB2 2QQ, United Kingdom. E-mail: dbd25{at}cam.ac.uk; or Mark A. Sperling, Department of Pediatrics/Endocrinology, Children’s Hospital of Pittsburgh, 3705 Fifth Ave, Pittsburgh, PA 15213. E-mail: masp{at}pitt.edu
机译:糖尿病酮症症(DKA)是1型糖尿病(TIDM)的儿童发病率和死亡率的主要原因。死亡率主要与脑水肿的发生相关; DKA中只有少数死亡归因于其他原因。脑水肿发生在DKA所有发作的〜0.3%至1%中,其病因,病理生理学和理想的治疗方法知之甚少。辩论是否治疗DKA的医生是否可以预防或预测脑水肿的发生以及用于管理DKA儿童的适当部位。有一致认为,预防DKA和减少其发病率应该是管理糖尿病儿童的目标。探讨这些问题,劳动威尔金斯儿科内分泌会(LWPE)和欧洲儿科内分泌学(ESPE)召集了一个面板专家医师达成共识会议。会议由Mark A. Sperling,MD,代表LWPES和David B. Dunger,MD主持,代表ESPE。所有3个组织由参加写作进程的成员代表,在ESPE和LWPES和国际儿科和青少年糖尿病协会之间以及国际儿科和青少年协会之间制定了共识声明。该陈述也由相关组织认可;少年糖尿病研究基金会国际,世界儿科密集型和关键护理社联联合会,欧洲儿科批判性护理社会,欧洲儿科和新生儿重症监护人员和澳大利亚儿科内分泌小组由邀请参与者代表。主要主题有一个主题和录音机,负责根据美国糖尿病协会使用的标准审查文献和提供的基于证据的建议(见附录;证据水平以大写字母,括号中指示).1类型2糖尿病没有考虑。所有参与者贡献了......与David B. Dunger,剑桥大学,Addenbroke的医院,8级,Box 116,英国剑桥CB2 2QQ,剑桥CB2 2 Q级达迪瓦议员的通信。电子邮件:DBD25 {AT} Cam.ac.uk;或Mark A. Sperling,儿科/内分泌科,匹兹堡儿童医院,3705 Fifth Ave,Pittsburgh,PA 15213.电子邮件:MASP {AT} Pitt.edu

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