Matrix Gla protein polymorphism rs1800802 is associated with atheroma plaque progression and with cardiovascular events in a chronic kidney disease cohort

NDT Plus Pub Date : 2023-10-10 DOI:10.1093/ckj/sfad257
Serafí Cambray, Marcelino Bermúdez-López, Alicia Garcia-Carrasco, Jose M Valdivielso, Ma José Aladrén Regidor, Jaume Almirall, Esther Ponz, Jesús Arteaga Coloma, Ma Auxiliadora Bajo Rubio, Raquel Díaz, Montserrat Belart Rodríguez, Antonio Gascón, Jordi Bover Sanjuan, Josep Bronsoms Artero, Juan B Cabezuelo Romero, Salomé Muray Cases, Jesús Calviño Varela, Pilar Caro Acevedo, Jordi Carreras Bassa, Aleix Cases Amenós, Elisabet Massó Jiménez, Rosario Moreno López, Secundino Cigarrán Guldris, Saray López Prieto, Lourdes Comas Mongay, Isabel Comerma, Ma Teresa Compte Jové, Marta Cuberes Izquierdo, Fernando de Álvaro, Covadonga Hevia Ojanguren, Gabriel de Arriba de la Fuente, Ma Dolores del Pino y Pino, Rafael Diaz-Tejeiro Izquierdo, Francisco Ahijado Hormigos, Marta Dotori, Verónica Duarte, Sara Estupiñan Torres, Ma José Fernández Reyes, Ma Loreto Fernández Rodríguez, Guillermina Fernández, Antonio Galán Serrano, Cesar García Cantón, Antonio L García Herrera, Mercedes García Mena, Luis Gil Sacaluga, Maria Aguilar, José Luis Górriz, Emma Huarte Loza, José Luis Lerma, Antonio Liebana Cañada, Jesús Pedro Marín Álvarez, Nàdia Martín Alemany, Jesús Martín García, Alberto Martínez Castelao, María Martínez Villaescusa, Isabel Martínez, Iñigo Moina Eguren, Silvia Moreno Los Huertos, Ricardo Mouzo Mirco, Antonia Munar Vila, Ana Beatriz Muñoz Díaz, Juan F Navarro González, Javier Nieto, Agustín Carreño, Enrique Novoa Fernández, Alberto Ortiz, Beatriz Fernandez, Vicente Paraíso, Miguel Pérez Fontán, Ana Peris Domingo, Celestino Piñera Haces, Ma Dolores Prados Garrido, Mario Prieto Velasco, Carmina Puig Marí, Maite Rivera Gorrín, Esther Rubio, Ruiz Pilar, Mercedes Salgueira Lazo, Ana Isabel Martínez Puerto, José Antonio Sánchez Tomero, José Emilio Sánchez, Ramon Sans Lorman, Ramon Saracho, Maria Sarrias, Daniel Serón, María José Soler, Clara Barrios, Fernando Sousa, Daniel Toran, Fernando Tornero Molina, José Javier Usón Carrasco, Ildefonso Valera Cortes, Ma Merce Vilaprinyo del Perugia, Rafael C Virto Ruiz, Vicente Pallarés Carratalá, Miguel Artigao, Inés Gil, Francisco Adan, Emilio García Criado, Rafael Durá Belinchón
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Abstract

ABSTRACT Background Chronic kidney disease (CKD) is associated with increased atherosclerotic burden and higher risk for cardiovascular events (CVE). Atherosclerosis has a significant genetic component and, in CKD, it is influenced by mineral metabolism alterations. Therefore, genetic modifications of mineral metabolism–related proteins could affect atherosclerosis in CKD patients. In the present study we investigated the role of single nucleotide polymorphisms (SNPs) of the matrix gamma-carboxy glutamic acid protein (MGP) on atherosclerosis progression and CVE in a CKD cohort. Methods A total of 2187 CKD patients from the Observatorio Nacional de Aterosclerosis en Nefrologia (NEFRONA) study were genotyped for SNPs present in the matrix gamma-carboxy glutamic acid (Gla) protein (MGP) gene. Atheromatosis was detected by vascular ultrasound. Progression of atheromatosis, defined as an increase in territories with plaque, was assessed after 24 months. Patients were followed for 48 months for CVE. Association of SNPs with plaque progression was assessed by logistic regression and their capacity to predict CVE by Cox regression. Results Three SNPs of the MGP gene were analyzed. No association of the rs4236 or the rs1800801 SNPs was detected with any of the outcomes. However, patients homozygotes for the minor allele of the rs1800802 SNP showed higher adjusted risk for plaque progression [odds ratio 2.3 (95% confidence interval 1.06–4.9)] and higher risk of suffering a CVE [hazard ratio 2.16 (95% confidence interval 1.13–4.12)] compared with the rest of genotypes. No association of the SNP with total or dp-ucMGP levels was found in a subsample. Conclusions The rs1800802 polymorphism of MGP is associated with plaque progression and CVE in CKD patients.
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在慢性肾病队列中,基质Gla蛋白多态性rs1800802与动脉粥样硬化斑块进展和心血管事件相关
背景:慢性肾脏疾病(CKD)与动脉粥样硬化负担增加和心血管事件(CVE)风险升高相关。动脉粥样硬化具有重要的遗传成分,在CKD中,它受矿物质代谢改变的影响。因此,矿物质代谢相关蛋白的遗传修饰可能影响CKD患者的动脉粥样硬化。在本研究中,我们研究了基质γ -羧基谷氨酸蛋白(MGP)的单核苷酸多态性(snp)在CKD队列中动脉粥样硬化进展和CVE中的作用。方法对来自国家NEFRONA (Observatorio Nacional de Aterosclerosis en Nefrologia)研究的2187例CKD患者进行基质γ -羧基谷氨酸(Gla)蛋白(MGP)基因snp分型。血管超声检查动脉粥样硬化。动脉粥样硬化的进展,定义为斑块区域的增加,在24个月后进行评估。CVE随访48个月。通过逻辑回归评估snp与斑块进展的关系,并通过Cox回归评估其预测CVE的能力。结果分析了MGP基因的3个snp。没有检测到rs4236或rs1800801 snp与任何结果的关联。然而,与其他基因型相比,rs1800802 SNP小等位基因的纯合子患者斑块进展的调整风险更高[优势比2.3(95%置信区间1.06-4.9)],患CVE的风险更高[风险比2.16(95%置信区间1.13-4.12)]。在子样本中未发现SNP与总或dp-ucMGP水平的关联。结论MGP rs1800802多态性与CKD患者斑块进展和CVE相关。
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