Open AccessComplex Glycerol Kinase Deficiency and Adrenocortical Insufficiency in Two Neonates
Author(s) -
Sabriye Korkut,
Osman Baştuğ,
Margarita Raygada,
Nihal Hatipoğlu,
Selim Kurtoğlu,
Mustafa Kendırcı,
Charalampos Lyssikatos,
Constantine A. Stratakis
Publication year - 2016
Publication title -
journal of clinical research in pediatric endocrinology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 0.566
H-Index - 35
eISSN - 1308-5735
pISSN - 1308-5727
DOI - 10.4274/jcrpe.2539
Subject(s) - adrenal insufficiency , medicine , primary adrenal insufficiency , endocrinology , context (archaeology) , creatine kinase , glycerol kinase , hypertriglyceridemia , triglyceride , cholesterol , gene , genetics , biology , paleontology
Contiguous gene deletions of chromosome Xp21 can lead to glycerol kinase deficiency and severe adrenocortical insufficiency (AI) in a male newborn among other problems. We describe our experience with two such patients who presented with dysmorphic facies, AI, and pseudo-hypertriglyceridemia. Both infants had normal serum 17-hidroxyprogesterone levels, and adrenal glands could not be observed with ultrasonography. Creatine kinase and triglyceride levels were measured to elucidate the etiology of adrenal hypoplasia and were above normal limits in both cases. Both patients required steroid and salt supplementation. They were both found to have Xp21.2 deletions (DMD, NR0B1, GK, IL1RAPL1). We conclude that AI in the context of other genetic abnormalities should prompt chromosomal investigations in the absence of another unifying explanation.
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