Metabolic alterations, HFE gene mutations and atherogenic lipoprotein modifications in patients with primary iron overload-Reference-Cited by-同舟云学术

Metabolic alterations, HFE gene mutations and atherogenic lipoprotein modifications in patients with primary iron overload

Published:2015-02-11 Issue:9 Volume:128 Page:609-618
ISSN:0143-5221
Container-title:Clinical Science
language:en
Short-container-title:

Author:

Meroño Tomás¹²,Brites Fernando¹,Dauteuille Carolane²,Lhomme Marie²,Menafra Martín¹,Arteaga Alejandra³,Castro Marcelo⁴,Saez María Soledad⁵,Ballerga Esteban González³,Sorroche Patricia⁵,Rey Jorge⁴,Lesnik Philippe²,Sordá Juan Andrés³,Chapman M. John²,Kontush Anatol²,Daruich Jorge³⁶

Affiliation:

1. Laboratory of Lipids and Lipoproteins, School of Pharmacy and Biochemistry, INFIBIOC, University of Buenos Aires, CONICET, Junín 956, 1113 Buenos Aires, Argentina

2. National Institute for Health and Medical Research (INSERM), UMR ICAN 1166, University of Pierre et Marie Curie–Paris 6, AP-HP, Groupe hospitalier Pitié-Salpétrière, ICAN, Paris F-75013, France

3. Hepatology Division, Hospital “José de San Martín”, University of Buenos Aires, Buenos Aires, Argentina

4. Department of Hemotherapy and Immunohematology, Hospital “José de San Martín”, University of Buenos Aires, Buenos Aires, Argentina

5. Central Laboratory, Italian Hospital of Buenos Aires, Buenos Aires, Argentina

6. Diagnostic and Therapeutical Gastroenterology (GEDYT), Buenos Aires, Argentina

Abstract

Iron overload (IO) has been associated with glucose metabolism alterations and increased risk of cardiovascular disease (CVD). Primary IO is associated with mutations in the HFE gene. To which extent HFE gene mutations and metabolic alterations contribute to the presence of atherogenic lipoprotein modifications in primary IO remains undetermined. The present study aimed to assess small, dense low-density lipoprotein (LDL) levels, chemical composition of LDL and high-density lipoprotein (HDL) particles, and HDL functionality in IO patients. Eighteen male patients with primary IO and 16 sex- and age-matched controls were recruited. HFE mutations (C282Y, H63D and S65C), measures of insulin sensitivity and secretion (calculated from the oral glucose tolerance test), chemical composition and distribution profile of LDL and HDL subfractions (isolated by gradient density ultracentrifugation) and HDL functionality (as cholesterol efflux and antioxidative activity) were studied. IO patients compared with controls exhibited insulin resistance (HOMA-IR (homoeostasis model assessment-estimated insulin resistance): +93%, P< 0.001). Metabolic profiles differed across HFE genotypes. C282Y homozygotes (n=7) presented a reduced β-cell function and insulin secretion compared with non-C282Y patients (n=11) (−58% and −73%, respectively, P< 0.05). In addition, C282Y homozygotes featured a predominance of large, buoyant LDL particles (C282Y: 43±5; non-C282Y: 25±8; controls: 32±7%; P< 0.001), whereas non-C282Y patients presented higher amounts of small, dense LDL (C282Y: 23±5; non-C282Y: 39±10; controls: 26±4%; P< 0.01). HDL particles were altered in C282Y homozygotes. However, HDL functionality was conserved. In conclusion, metabolic alterations and HFE gene mutations are involved in the presence of atherogenic lipoprotein modifications in primary IO. To what extent such alterations could account for an increase in CVD risk remains to be determined.

Publisher

Portland Press Ltd.

Subject

General Medicine

Link

https://portlandpress.com/clinsci/article-pdf/128/9/609/446912/cs1280609.pdf

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