Diagnosis of Familial Dysbetalipoproteinemia Based on the Lipid Abnormalities Driven by APOE2/E2 Genotype

Author:

Bea Ana M1,Cenarro Ana12,Marco-Bened Victoria13,Laclaustra Martn13,Martn Csar456,Ibarretxe Daiana7,Pint Xavier8ORCID,Arrobas Teresa9,Vials Clara101112,Civeira Fernando13ORCID,Olmos Salvador113

Affiliation:

1. Hospital Universitario Miguel Servet, IIS Aragn, CIBERCV , Zaragoza , Spain

2. Molecular Research Laboratory, Instituto Aragones de Ciencias de la Salud (IACS) , Zaragoza , Spain

3. Departamento de Medicina, Psiquiatra y Dermatologa, Universidad de Zaragoza , Zaragoza , Spain

4. Fundacin Biofisika Bizkaia , Leioa , Spain

5. Biofisika Institute (UPV/EHU, CSIC) , Leioa , Spain

6. Department of Biochemistry and Molecular Biology, Universidad del Pas Vasco UPV/EHU , Bilbao , Spain

7. Unitat de Medicina Vascular i Metabolisme (UVASMET) Hospital Universitari Sant Joan, IISPV, CIBERDEM, Universitat Rovira i Virgili , Reus, Tarragona , Spain

8. Unidad de Lpidos, Servicio de Medicina Interna, Hospital Universitario de Bellvitge-Idibell, Universidad de Barcelona, CiberObn , Barcelona , Spain

9. Laboratorio de Nutricin y RCV, Laboratorio de Bioqumica Clnica, Hospital Virgen Macarena , Sevilla , Spain

10. Endocrinology Department, Hospital Clnic de Barcelona , Barcelona , Spain

11. Institut dInvestigacions Biomdiques August Pi i Sunyer (IDIBAPS) , Barcelona , Spain

12. Centro de Investigacin Biomdica en Red Fisiopatologa de la Obesidad y Nutricin (CIBEROBN), Instituto de Salud Carlos III (ISCIII) , Madrid , Spain

13. Aragon Institute of Engineering Research (I3A), Universidad de Zaragoza , Zaragoza , Spain

Abstract

Abstract Background Familial dysbetalipoproteinemia (FDBL) is a monogenic disease due to variants in APOE with a highly variable phenotype. Current diagnostic lipid-based methods have important limitations. The objective is twofold: to define characteristics of dysbetalipoproteinemia (DBL) based on the analysis of APOE in patients from a lipid unit and in a sample from the general population, and to propose a screening algorithm for FDBL. Methods Lipids and APOE genotype from consecutive unrelated subjects from Miguel Servet University Hospital (MSUH) (n 3603), subjects from the general population participants of the Aragon Workers Health Study (AWHS) (n 4981), and selected subjects from external lipid units (Ext) (n 390) were used to define DBL criteria and to train and validate a screening tool. Results Thirty-five subjects from MSUH, 21 subjects from AWHS, and 31 subjects from Ext were APOE2/2 homozygous. The combination of non high-density lipoprotein cholesterol (non-HDLc)/apoB 1.7 plus triglycerides/apoB 1.35, in mg/dL (non-HDLc [mmol/L]/apolipoprotein B (apoB) [g/L] 4.4 and triglycerides [mmol/L]/apoB [g/L] 3.5), provided the best diagnostic performance for the identification of subjects with hyperlipidemia and APOE2/2 genotype (sensitivity 100 in the 3 cohorts, and specificity 92.8 [MSUH], 80.9 [AWHS], and 77.6 [Ext]). This improves the performance of previous algorithms. Similar sensitivity and specificity were observed in APOE2/2 subjects receiving lipid-lowering drugs. Conclusions The combination of non-HDLc/apoB and triglycerides/apoB ratios is a valuable tool to diagnose DBL in patients with hyperlipidemia with or without lipid-lowering drugs. FDBL diagnosis requires DBL and the presence of a compatible APOE genotype. Most adult APOE2/2 subjects express DBL, making FDBL as common as familial hypercholesterolemia in the population.

Publisher

Oxford University Press (OUP)

Subject

Biochemistry (medical),Clinical Biochemistry

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