Remediation of ABCG5-Linked Macrothrombocytopenia With Ezetimibe Therapy

To investigate refractory hypercholesterolemia, a female patient and relatives were subjected to whole-genome sequencing. The proband was found to have compound heterozygous substitutions p. Arg446Gln and c.1118+3G>T in ABCG5, one of two genes causing sitosterolemia. When tracing these variants in the full pedigree, all maternally related heterozygotes for the intronic ABCG5 variant exhibited large platelets (over 30 fl), which segregated in an autosomal dominant manner, consistent with macrothrombocytopenia, or large platelet syndrome which may be associated with a bleeding tendency. In vitro cell-line and in vivo rat model experiments supported a pathogenic role for the variant and the macrothrombocytopenia was recapitulated in heterozygous rats and human cell lines exhibiting that single variant. Ezetimibe treatment successfully ameliorated all the symptoms of the proband with sitosterolemia and resolved the macrothrombocytopenia of the treated heterozygote relatives. Subsequently, in follow up these observations, platelet size, and size distribution were measured in 1,180 individuals; 30 were found to be clinically abnormal, three of which carried a single known pathogenic ABCG5 variant (p.Arg446Ter) and two individuals carried novel ABCG5 variants of uncertain significance. In this study, we discovered that identification of large platelets and therefore a possible macrothrombocytopenia diagnosis could easily be inadvertently missed in clinical practice due to variable instrument settings. These findings suggest that ABCG5 heterozygosity may cause macrothrombocytopenia, that Ezetimibe treatment may resolve macrothrombocytopenia in such individuals, and that increased attention to platelet size on complete blood counts can aid in the identification of candidates for ABCG5 genetic testing who might benefit from Ezetimibe treatment.

Predominantly Increased Triglyceride-rich Lipoproteins Induced by Dietary Cholesterol Promoted Atherosclerosis Formation in LDL Receptor Knockout Golden Hamster

Epidemiological investigation showed that triglyceride is an independent risk factor of cardiovascular diseases, but it is difficult to distinguish the effects of different lipoproteins by an experimental system in vivo, the role of triglyceride-rich lipoproteins (TRLs) in atherosclerosis have not been fully understood. Here we found LDL receptor knock-out (LDLR−/−) hamsters have special characteristics of lipid profile for investigating effects of TRLs. Mixed hyperlipidemia in LDLR−/− hamsters after high cholesterol and high fat (HCHF) diet were marked by increasing of chylomicrons, VLDL and their remnants, but not LDL. Ezetimibe treatment significantly decreased these large particles containing ApoB and ApoE without affecting LDL, leading to the dramatic reduction of plasma cholesterol and triglycerides. 40 days of HCHF diet feeding accelerated aortic atherosclerosis accompanied severe fatty liver, and ezetimibe treatment inhibited their development. Also, TRLs lowering inhibited the expression of vascular adhesion factors and lipid uptake of macrophage. Our results suggest that golden hamster is a proper model for studying hypertriglyceridemia related diseases. In LDLR−/− hamster, TRLs showed independent atherogenicity by triggering inflammatory response of endothelial cells and the formation of foam cells from macrophages. And these TRLs clearance is mediated by LDL receptor. TRLs would be an important therapeutic target for atherosclerotic development with postprandial hyperlipidemia.