协调先天免疫反应的基因多态性对肾移植后细小病毒B19复制动力学的影响。
Impact of polymorphisms in genes orchestrating innate immune responses on replication kinetics of Torque teno virus after kidney transplantation.
作者信息
Redondo Natalia, Rodríguez-Goncer Isabel, Parra Patricia, Albert Eliseo, Giménez Estela, Ruiz-Merlo Tamara, López-Medrano Francisco, San Juan Rafael, González Esther, Sevillano Ángel, Andrés Amado, Navarro David, Aguado José María, Fernández-Ruiz Mario
机构信息
Unit of Infectious Diseases, Hospital Universitario '12 de Octubre', Instituto de Investigación Sanitaria Hospital '12 de Octubre' (imas12), Madrid, Spain.
Centro de Investigación Biomédica en Red de Enfermedades Infecciosas (CIBERINFEC), Instituto de Salud Carlos III, Madrid, Spain.
出版信息
Front Genet. 2022 Nov 22;13:1069890. doi: 10.3389/fgene.2022.1069890. eCollection 2022.
Torque teno virus (TTV) DNAemia has been proposed as a surrogate marker of immunosuppression after kidney transplantation (KT), under the assumption that the control of viral replication is mainly exerted by T-cell-mediated immunity. However, Tthe impact on post-transplant TTV kinetics of single genetic polymorphisms (SNPs) in genes orchestrating innate responses remains unknown. We aimed to characterize the potential association between 14 of these SNPs and TTV DNA levels in a single-center cohort of KT recipients. Plasma TTV DNAemia was quantified by real-time PCR in 221 KT recipients before transplantation (baseline) and regularly through the first 12 post-transplant months. We performed genotyping of the following SNPs: (rs5742909, rs231775), (rs3775291), (rs5743836, rs352139), (rs735240, rs4804803), (rs12979860, rs8099917), (rs1800629), (rs1878672, rs1800872), (rs3212227) and (rs2275913). The presence of the minor G allele of (rs4804803) in the homozygous state was associated with undetectable TTV DNAemia at the pre-transplant assessment (adjusted odds ratio: 36.96; 95% confidence interval: 4.72-289.67; -value = 0.001). After applying correction for multiple comparisons, no significant differences across SNP genotypes were observed for any of the variables of post-transplant TTV DNAemia analyzed (mean and peak values, areas under the curve during discrete periods, or absolute increments from baseline to day 15 and months 1, 3, 6 and 12 after transplantation). The minor G allele of (rs4804803) seems to exert a recessive protective effect against TTV infection in non-immunocompromised patients. However, no associations were observed between the SNPs analyzed and post-transplant kinetics of TTV DNAemia. These negative results would suggest that post-transplant TTV replication is mainly influenced by immunosuppressive therapy rather than by underlying genetic predisposition, reinforcing its clinical application as a biomarker of adaptive immunity.
有人提出,在肾移植(KT)后,细小病毒B19(TTV)血症可作为免疫抑制的替代标志物,其假设是病毒复制的控制主要由T细胞介导的免疫发挥作用。然而,协调先天性反应的基因中的单基因多态性(SNP)对移植后TTV动力学的影响仍不清楚。我们旨在在一个单中心的KT受者队列中,描述其中14个SNP与TTV DNA水平之间的潜在关联。通过实时聚合酶链反应(PCR)对221名KT受者移植前(基线)的血浆TTV血症进行定量,并在移植后的前12个月定期进行检测。我们对以下SNP进行基因分型:(rs5742909,rs231775)、(rs3775291)、(rs5743836,rs352139)、(rs735240,rs4804803)、(rs12979860,rs8099917)、(rs1800629)、(rs1878672,rs1800872)、(rs3212227)和(rs2275913)。在移植前评估中,纯合状态下(rs4804803)的次要G等位基因的存在与无法检测到的TTV血症相关(调整后的优势比:36.96;95%置信区间:4.72 - 289.67;P值 = 0.001)。在应用多重比较校正后,对于分析的移植后TTV血症的任何变量(平均值和峰值、离散期曲线下面积或从基线到移植后第15天以及第1、3、6和12个月的绝对增量),未观察到SNP基因型之间的显著差异。(rs4804803)的次要G等位基因似乎对非免疫受损患者的TTV感染具有隐性保护作用。然而,在所分析的SNP与移植后TTV血症动力学之间未观察到关联。这些阴性结果表明,移植后TTV复制主要受免疫抑制治疗的影响,而非潜在的遗传易感性,这加强了其作为适应性免疫生物标志物的临床应用。
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