Prevalent Variants in the LDLR Gene Impair Responsiveness to Rosuvastatin among Family Members of Patients with Premature Myocardial Infarction

Nguyen Trung Kien; Tran Tin Nghia; Nguyen Minh Hoang; Tran Nguyen Trong Phu; Pham Thi Ngoc Nga; Ha Thi Thao Mai; J. Luis Espinoza

doi:10.3390/jpm13121725

Journal of Personalized Medicine (Dec 2023)

Prevalent Variants in the LDLR Gene Impair Responsiveness to Rosuvastatin among Family Members of Patients with Premature Myocardial Infarction

Nguyen Trung Kien,
Tran Tin Nghia,
Nguyen Minh Hoang,
Tran Nguyen Trong Phu,
Pham Thi Ngoc Nga,
Ha Thi Thao Mai,
J. Luis Espinoza

Affiliations

Nguyen Trung Kien: Faculty of Medicine, Can Tho University of Medicine and Pharmacy, Can Tho 900000, Vietnam
Tran Tin Nghia: Faculty of Medicine, Can Tho University of Medicine and Pharmacy, Can Tho 900000, Vietnam
Nguyen Minh Hoang: Tra Vinh General Hospital, Tra Vinh 940000, Vietnam
Tran Nguyen Trong Phu: Faculty of Medicine, Can Tho University of Medicine and Pharmacy, Can Tho 900000, Vietnam
Pham Thi Ngoc Nga: Faculty of Medicine, Can Tho University of Medicine and Pharmacy, Can Tho 900000, Vietnam
Ha Thi Thao Mai: Faculty of Medicine, Can Tho University of Medicine and Pharmacy, Can Tho 900000, Vietnam
J. Luis Espinoza: Faculty of Health Sciences, Kanazawa University, Kanazawa 920-0942, Ishikawa, Japan

DOI: https://doi.org/10.3390/jpm13121725
Journal volume & issue: Vol. 13, no. 12
p. 1725

Abstract

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Background: Familial hypercholesterolemia (FH) is an inherited metabolic disorder characterized by high levels of low-density lipoprotein cholesterol (LDL-c) from birth. About 85% of all FH cases are caused by pathogenic variants in the LDLR gene. Individuals with FH have increased cardiovascular risk, including a high risk of premature myocardial infarction (PMI). Methods: We conducted an opportunistic exome screening to identify variants in the LDLR gene among Vietnamese patients with PMI treated at a general hospital in southern Vietnam. A cascade testing for LDLR variants was conducted in their relatives within three generations, and the effects of the LDLR variant on the response to rosuvastatin treatment were also studied using a comparative before-and-after study design on those who were eligible. Results: A total of 99 participants from the three generations of four PMI patients were recruited, mean age 37.3 ± 18.5 years, 56.6% males. Sanger sequencing revealed two variants in the LDLR gene: variant rs577934998 (c.664T>C), detected in 17 individuals within one family, and variant rs12710260 (c.1060+10G>C), found in 32 individuals (49.5%) in the other three families tested. Individuals harboring the variant c.664T>C had significantly higher baseline LDL-c and total cholesterol levels compared to those with variant c.1060+10G>C (classified as benign) or those without LDLR variants, and among the 47 patients subjected to a 3-month course of rosuvastatin therapy, those with variant c.664T>C had a significantly higher risk of not achieving the LDL-c target after the course of treatment compared to the c.1060+10G>C carriers. Conclusions: These findings provide evidence supporting the existence of pathogenic LDLR variants in Vietnamese patients with PMI and their relatives and may indicate the need for personalizing lipid-lowering therapies. Further studies are needed to delineate the extent and severity of the problem.

Published in Journal of Personalized Medicine

ISSN: 2075-4426 (Online)
Publisher: MDPI AG
Country of publisher: Switzerland
LCC subjects: Medicine
Website: http://www.mdpi.com/journal/jpm

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