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TREML4 MRNA Expression and Polymorphisms in Blood Leukocytes Are Associated with Atherosclerotic Lesion Extension in Coronary Artery Disease

Overview

Overview

Journal Sci Rep

Specialty Science

Date 2019 May 12

PMID 31076644

Citations 4

Authors

Authors

Victor Hugo Rezende Duarte

Carolinne Thaisa de Oliveira Fernandes Miranda

Marina Sampaio Cruz

Jessica Nayara Goes de Araujo

Mychelle Kytchia Rodrigues Nunes Duarte

Ayda Maria Quirino Silva Dos Santos

Isabelle Cristina Clemente Dos Santos

Jessica Cavalcante Dos Santos

Ananilia Medeiros Gomes da Silva

Juliana Marinho de Oliveira

Maria Sanali Moura de Oliveira Paiva

Marcos Felipe de Oliveira Galvao

Adriana Augusto Rezende

Mario Hiroyuki Hirata

Rosario Dominguez Crespo Hirata

Andre Ducati Luchessi

Vivian Nogueira Silbiger

Affiliations

Affiliations

Soon will be listed here.

Abstract

Members of the triggering receptor expressed on myeloid cells (TREM) family are associated with atherosclerosis risk and progression. TREML4 is upregulated in the early phase of acute coronary syndrome. We investigated the relationship between the mRNA expression of 13 genes in blood leukocytes, TREML4 polymorphisms, and coronary artery lesion extension (Friesinger index) in patients with coronary artery disease (CAD) (n = 137). TREML4 rs2803495 (A > G) and rs2803496 (T > C) variants and leukocyte mRNA expression were analysed by qRT-PCR. TREML4 expression was higher in patients with major coronary artery lesions than in subjects without or with low and intermediate lesions (p < 0.05). However, TREML4 polymorphisms were not associated with coronary lesion extent. Presence of the rs2803495 G allele was not associated with increased TREML4 mRNA expression. Patients carrying the rs2803496 C allele (TC/CC genotypes) were more likely to express TREML4 mRNA than non-C allele carriers (allele C: OR 7.3, and 95% CI 1.9-27.5, p = 0.03). In conclusion, increased TREML4 mRNA expression in blood leukocytes is influenced by gene polymorphisms and is associated with more severe coronary artery lesions, suggesting its potential as a biomarker of the extent of coronary lesions in patients with CAD.

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