Title : Familial lipoprotein lipase deficiency caused by known (G188E) and novel (W394X) LPL gene mutations - Hooper_2008_Ann.Clin.Biochem_45_102 |
Author(s) : Hooper AJ , Crawford GM , Brisbane JM , Robertson K , Watts GF , van Bockxmeer FM , Burnett JR |
Ref : Annals of Clinical Biochemistry , 45 :102 , 2008 |
Abstract :
Lipoprotein lipase (LPL) is the key enzyme in the catabolism of triglyceride-rich lipoproteins in the circulation. Familial LPL deficiency is characterized by hypertriglyceridaemia and absence of LPL activity. We report a case of LPL deficiency in a 43-year-old woman, who initially presented in childhood with chylomicronaemia syndrome. At that time, her plasma triglyceride concentration was approximately 30 mmol/L and post-heparin lipolytic activity was very low. In addition to having the known missense mutation LPL G188E, the patient was also found to have a novel nonsense mutation in exon 8, namely LPL W394X. The novel substitution in exon 8 (c.1262G > A) predicts a truncated protein product of 393 amino acids that lacks the carboxylterminal 12% of the mature LPL. Trp(394) is part of a cluster of exposed tryptophan residues in the carboxyl-terminal domain of LPL important for binding lipid substrate. Of 11 members from her three-generation family, three were heterozygotes for G188E (mean plasma triglyceride, 3.5 +/- 2.0 mmol/L), whereas six were heterozygotes for W394X (triglyceride, 4.3 +/- 1.8 mmol/L). In summary, we describe a case of familial LPL deficiency caused by compound heterozygosity for known (G188E) and novel (W394X) LPL gene mutations. |
PubMedSearch : Hooper_2008_Ann.Clin.Biochem_45_102 |
PubMedID: 18275685 |
Hooper AJ, Crawford GM, Brisbane JM, Robertson K, Watts GF, van Bockxmeer FM, Burnett JR (2008)
Familial lipoprotein lipase deficiency caused by known (G188E) and novel (W394X) LPL gene mutations
Annals of Clinical Biochemistry
45 :102
Hooper AJ, Crawford GM, Brisbane JM, Robertson K, Watts GF, van Bockxmeer FM, Burnett JR (2008)
Annals of Clinical Biochemistry
45 :102