Beta-thalassemia is a modifying factor of the clinical expression of familial hypercholesterolemia.

Sebastiano Calandra, Stefano Bertolini, Giovanni Mario Pes, Luca Deiana, Patrizia Tarugi, Livia Pisciotta, Salvatore Li Volti, Giovanni Li Volti, Carmela Maccarone
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引用次数: 1

Abstract

Familial hypercholesterolemia (FH) is a codominant disorder due to a variety of mutations of the low-density lipoprotein (LDL) receptor gene that result in an elevation of plasma LDL-cholesterol (LDL-C). Plasma levels of LDL-C show large interindividual variation even in subjects carrying the same mutation of the LDL receptor gene. This variability may be due to genetic factors (modifier genes). Several surveys indicate that the overall contribution of common polymorphisms of modifier genes (such as the genes encoding apolipoproteins E and B) to this variability is less than 10%. In contrast, beta-thalassemia has a profound LDL-lowering effect. This was documented in FH patients identified on the island of Sardinia, in Italy, where 12% of the inhabitants are carriers of beta-thalassemia due to a single mutation (Q39X) of the beta-globin gene that abolishes the synthesis of beta-globin chain of hemoglobin (beta(o)-thalassemia). Plasma LDL-C in FH heterozygotes carrying the beta(o)-thalassemia trait is 25% lower than in noncarriers, regardless of the LDL receptor gene mutation. It is likely that this effect is due to two main mechanisms: (1) increased uptake of LDL by the bone marrow to provide cholesterol for the increased proliferation of erythroid progenitor cells and (2) increased production of inflammatory cytokines that reduce the hepatic secretion and increase the catabolism of LDL. In view of its LDL-C-lowering effect, beta-thalassemia trait may protect FH heterozygotes against premature coronary atherosclerosis.

-地中海贫血是家族性高胆固醇血症临床表现的修饰因子。
家族性高胆固醇血症(FH)是一种共显性疾病,由于低密度脂蛋白(LDL)受体基因的多种突变导致血浆LDL-胆固醇(LDL- c)升高。即使在携带相同LDL受体基因突变的受试者中,血浆LDL- c水平也显示出较大的个体差异。这种变异可能是由于遗传因素(修饰基因)。几项调查表明,修饰基因(如编码载脂蛋白E和B的基因)的共同多态性对这种变异的总体贡献小于10%。相反,-地中海贫血具有显著的低密度脂蛋白降低作用。在意大利撒丁岛发现的FH患者中记录了这一点,其中12%的居民是β -地中海贫血的携带者,这是由于β -珠蛋白基因的单一突变(Q39X),该突变消除了血红蛋白-珠蛋白链的合成(β (o)-地中海贫血)。无论LDL受体基因突变如何,携带β (o)-地中海贫血性状的FH杂合子的血浆LDL- c比非携带者低25%。这种影响可能是由于两个主要机制:(1)骨髓对LDL的摄取增加,为红细胞祖细胞的增殖增加提供胆固醇;(2)炎症细胞因子的产生增加,减少肝脏分泌,增加LDL的分解代谢。鉴于其降低ldl - c的作用,β -地中海贫血性状可能保护FH杂合子抗过早冠状动脉粥样硬化。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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