Evaluation of CRP SNV rs2808630 and acute proinflammatory biomarkers in patients with CKD and PLHIV with CKD: a case-control study.

IF 2.2 4区 医学 Q2 UROLOGY & NEPHROLOGY
Andrea Torres-Rojas, Luz Alicia González-Hernández, Karina Sánchez-Reyes, Jonathan Samuel Chávez-Iñiguez, Jorge Fernando Topete-Reyes, Jaime Federico Andrade-Villanueva, Pedro Martínez-Ayala, Adriana Valle-Rodriguez, Vida Verónica Ruiz-Herrera, Jorge Hernández-Bello, Zyanya Reyes-Castillo, Monserrat Álvarez-Zavala
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引用次数: 0

Abstract

Background: The CKD in PLHIV is highly prevalent in Jalisco. Despite its control with ART, HIV is characterized by generating low-grade inflammation events that contribute to the development and progression of CKD. Considering the importance of hs-CRP in the context of CKD, various genetic predisposition studies have been conducted to search for variants of the CRP gene, among which the SNV rs2808630 has been associated with serum hs-CRP concentrations and progression of CKD. Due to the above, there is interest in studying this SNV, addressing the limited information available on this topic in Mexico.

Methods: The case-control study included 163 patients with CKD, 102 PLHIV with CKD under ART with undetectable viral loads from the Hospital Civil of Guadalajara "Fray Antonio Alcalde" and 115 controls. Clinical assessment and general laboratory studies were carried out. Also, serum quantification of inflammatory biomarkers was performed by ELISA method. The determination of CRP SNV rs2808630 by qPCR and the association with inflammatory biomarkers was evaluated. Statistical analysis was carried out considering significant values p < 0.05.

Results: Lower prevalence of CC genotype was shown in our population. Of the 358 samples, 221 (61.7%) present the wild-type genotype. The results analyzed correspond with what has been reported worldwide in studies of CRP SNV rs2808630 in the development of CKD without having a relationship with inflammatory and kidney function biomarkers. However, higher creatinine and IL-6 concentrations were observed in the group with the CC genotype. A significant correlation between IL-6 and eGFR was identified in CKD patients, but not for PLHIV with CKD, highlighting a potential difference in inflammatory dynamics between these groups. Importantly, in PLHIV with CKD, we found a strong correlation between hs-CRP and IL-8, suggesting a possible association with a higher proportion of the inflammatory isoform of hs-CRP, which may have implications for disease progression and cardiovascular risk.

Conclusions: The presence of the CRP SNV does not appear to contribute to the development of CKD and has no association with inflammatory biomarkers. Though, genetically independent manner, hs-CRP levels are slightly different between groups and are underrated when related to the CKD stage in PLHIV. Also, high IL-6 concentrations are related to CKD progression, while IL-8 seems to have a better relation to CKD in PLHIV.

CKD和PLHIV合并CKD患者CRP SNV rs2808630和急性促炎生物标志物的评估:一项病例对照研究
背景:PLHIV患者CKD在哈利斯科州非常普遍。尽管通过ART进行控制,HIV的特点是产生低度炎症事件,促进CKD的发展和进展。考虑到hs-CRP在CKD中的重要性,人们开展了各种遗传易感性研究来寻找CRP基因的变异,其中SNV rs2808630与血清hs-CRP浓度和CKD进展有关。由于上述原因,人们有兴趣研究这一SNV,以解决墨西哥关于这一主题的有限信息。方法:病例-对照研究纳入来自瓜达拉哈拉“Fray Antonio Alcalde”市立医院的163例CKD患者,102例接受抗逆转录病毒治疗且病毒载量无法检测的PLHIV合并CKD患者和115例对照组。进行了临床评估和一般实验室研究。同时,采用ELISA法对血清炎症标志物进行定量分析。评价qPCR检测CRP SNV rs2808630及其与炎症生物标志物的相关性。结果:我们人群中CC基因型的患病率较低。在358份样本中,221份(61.7%)为野生型基因型。分析的结果与世界范围内报道的CRP SNV rs2808630在CKD发展中的研究一致,而与炎症和肾功能生物标志物无关。然而,CC基因型组肌酐和IL-6浓度较高。在CKD患者中发现了IL-6和eGFR之间的显著相关性,但在PLHIV合并CKD中没有发现,这突出了这两组之间炎症动力学的潜在差异。重要的是,在伴有CKD的PLHIV中,我们发现hs-CRP和IL-8之间存在很强的相关性,这可能与hs-CRP的炎症亚型比例较高有关,这可能与疾病进展和心血管风险有关。结论:CRP SNV的存在似乎与CKD的发展无关,也与炎症生物标志物无关。尽管hs-CRP水平与基因无关,但两组之间略有不同,并且在与PLHIV的CKD阶段相关时被低估。此外,高IL-6浓度与CKD进展有关,而IL-8似乎与PLHIV患者的CKD有更好的关系。
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来源期刊
BMC Nephrology
BMC Nephrology UROLOGY & NEPHROLOGY-
CiteScore
4.30
自引率
0.00%
发文量
375
审稿时长
3-8 weeks
期刊介绍: BMC Nephrology is an open access journal publishing original peer-reviewed research articles in all aspects of the prevention, diagnosis and management of kidney and associated disorders, as well as related molecular genetics, pathophysiology, and epidemiology.
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