Schlingmann Karl P, Cassar Walburga, Konrad Martin
Department of General Pediatrics, University Children's Hospital, Münster, Germany.
Department of Pediatrics, Bruneck Hospital, Bruneck, Italy.
Bone Rep. 2018 Jun 21;9:42-46. doi: 10.1016/j.bonr.2018.06.005. eCollection 2018 Dec.
The term Idiopathic infantile hypercalcemia (IIH) was first introduced almost 70 years ago when symptomatic hypercalcemia developed in children after receiving high doses of vitamin D for the prevention of rickets. The underlying pathophysiology remained unknown until recessive mutations in encoding Vitamin D-24-hydroxylase were discovered. The defect in vitamin D degradation leads to an accumulation of active 1,25(OH)D with subsequent hypercalcemia. Enhanced renal calcium excretions lead to hypercalciuria and nephrocalcinosis. Meanwhile, the phenotypic spectrum associated with mutations has significantly broadened. Patients may present at all age groups with symptoms originating from increased serum calcium levels as well as from increased urinary calcium excretions, i.e. kidney stones. Possible long term sequelae comprise chronic renal failure as well as cardiovascular disease. Here, we present a family with two affected siblings with differing clinical presentation as an example for the phenotypic variability of CYP24A1 defects.
特发性婴儿高钙血症(IIH)这一术语最早于近70年前提出,当时儿童在接受高剂量维生素D预防佝偻病后出现了症状性高钙血症。在编码维生素D-24-羟化酶的隐性突变被发现之前,其潜在的病理生理学机制一直不明。维生素D降解缺陷导致活性1,25(OH)D积累,继而引发高钙血症。肾脏钙排泄增加导致高钙尿症和肾钙质沉着症。与此同时,与该突变相关的表型谱已显著拓宽。患者可能在各个年龄组出现症状,这些症状源于血清钙水平升高以及尿钙排泄增加,即肾结石。可能的长期后遗症包括慢性肾衰竭以及心血管疾病。在此,我们展示一个有两名患病兄弟姐妹且临床表现不同的家庭,作为CYP24A1缺陷表型变异性的一个例子。
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