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Urine Interleukin-8 as a Marker of Vesicoureteral Reflux in Infants

机译:尿白介素8作为婴儿血管输尿管反流的标志物

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OBJECTIVE. Vesicoureteral reflux (VUR) is a common finding in children presenting with urinary tract infection (UTI) and prenatally diagnosed urinary tract dilatation and in relatives of index patients. Children with VUR are at risk for ongoing renal damage with subsequent infections. Detecting VUR and renal scarring currently depends on imaging modalities with associated problems of radiation, invasiveness, and expense. Noninvasive methods would greatly facilitate diagnosis and would also help in identifying relatives of index cases who should be screened. Interleukin-8 (IL-8) is produced by epithelial cells of the renal tract in response to inflammatory stimuli and has been shown to increase during acute UTI. The objective of this study was to assess the urine levels of IL-8 as a noninvasive marker of VUR in infants in the absence of a recent UTI episode.METHODS. We evaluated urine concentrations of IL-8 in 59 infants aged 1 month to 2 years. All infants were free of UTI for a minimum of 3 weeks before IL-8 evaluation. Infants were divided into 3 groups: group A, subjects with proven VUR (24 infants aged 0.15–1.95 years, median 0.43); group B, subjects with a history of UTI but negative investigation for VUR (14 infants aged 0.32–1.95 years, median 0.57); and group C, subjects without any history of acute or chronic condition that might impair renal function (21 infants aged 0.08–1.92 years, median 0.33). IL-8 concentrations were determined by a commercially available quantitative enzyme-linked immunosorbent assay. To avoid dilution effects, urinary levels of IL-8 were expressed as the ratio of cytokine-to-urinary creatinine.RESULTS. Results were presented as medians and ranges. The Kruskal-Wallis test, the Mann-Whitney rank sum U test, and the Spearman rank order correlation test were performed for the univariate analysis. Two-tailed P values were calculated and the conventional level of significance P .05 was applied in all cases. Infants in groups A and B had been free of UTI for a period of 3 to 52 weeks (median, 5.0 weeks) and 3 to 78 weeks (median, 4.5 weeks), respectively, before IL-8 determination. No significant difference was noted in the length of the UTI-free period between groups A and B ( P = .469). Urine creatinine concentrations did not differ among groups A, B, and C (medians 1.15, 2.25, and 1.15 μmol/mL, respectively; P = .080). The median urine IL-8/creatinine concentrations (pg/μmol) were 40.5 (range, 2.04–3874) in group A, 1.91 (range, 0.001–386) in group B, and 2.47 (range, 0.002–55.6) in group C. Urine IL-8/creatinine concentrations were significantly higher in group A than both in group B ( P = .0003) and in group C ( P .0001). No significant difference was observed between groups B and C ( P = .749). In group A, no significant correlation was shown between IL-8/creatinine concentrations and the presence of renal parenchymal damage ( P = .506), reflux grade ( P = .770), or time from UTI ( P = .155). A receiver-operator characteristic curve was constructed by plotting the sensitivity versus the specificity for different cutoff concentrations of IL-8/creatinine. With a cutoff concentration of urinary IL-8/creatinine at 5 pg/μmol, the sensitivity of this marker in diagnosing VUR was 88%, the specificity 69%, the positive prognostic value 66%, and the negative prognostic value 89%. In higher cutoff concentrations, specificity of the marker increased but sensitivity rapidly decreased.CONCLUSIONS. We present evidence that urine IL-8 concentrations remain elevated in infants with VUR even in the absence of UTI and that a cutoff of 5 pg/μmol IL-8/creatinine is of high sensitivity and adequate specificity for diagnosing VUR. Elevated urine IL-8 levels in VUR and renal scarring have already been reported; however, the present study is, to our knowledge, the first to confirm significant differences between infants with VUR and infants with a history of UTI alone and healthy controls, and to suggest a reliable cutoff concentration for diagnosing VUR. Our findings additionally suggest that inflammatory process in VUR is ongoing even after UTI has resolved, pointing against the currently held belief that sterile reflux cannot harm kidneys. The chronic inflammatory cell infiltrate associated with reflux nephropathy rather than VUR itself might offer an explanation for the secretion of IL-8, which may well be independent of reflux grade. Using urine IL-8 for diagnosing VUR is not free of limitations, because IL-8 may be elevated as a result of urinary tract manipulation or undetected UTI. In addition, this study focused on infants and not in older children with longstanding VUR. Increased urine IL-8 concentrations after UTI has resolved is a promising noninvasive marker for an initial screening for VUR in infancy with high sensitivity and adequate specificity.
机译:目的。膀胱输尿管反流(VUR)是患有尿路感染(UTI)和产前诊断为尿路扩张的儿童及其索引亲属的常见发现。患有VUR的儿童有持续性肾损伤和随后感染的风险。目前,检测VUR和肾瘢痕形成取决于成像方式以及相关的放射,侵袭性和费用问题。无创方法将极大地促进诊断,也将有助于确定应筛选的索引病例的亲属。白细胞介素8(IL-8)由肾脏的上皮细胞响应炎症刺激而产生,并已显示在急性UTI期间会增加。这项研究的目的是评估在没有最近的UTI发作的情况下婴儿尿液中IL-8作为VUR的非侵入性标志物的方法。我们评估了59例1个月至2岁婴儿的尿液IL-8浓度。在评估IL-8之前,所有婴儿都至少有3周没有尿路感染。婴儿分为3组:A组,经证实具有VUR的受试者(24名0.15-1.95岁的婴儿,中位值为0.43); B组,有尿路感染史但对VUR检查阴性(14例0.32–1.95岁婴儿,中位数0.57); C组没有急性或慢性病史,可能损害肾功能(21例0.08-1.92岁,中位数0.33)。通过市售的定量酶联免疫吸附测定法确定IL-8浓度。为了避免稀释作用,将尿中IL-8的水平表示为细胞因子与尿中肌酐的比值。结果以中位数和范围表示。对单变量分析进行了Kruskal-Wallis检验,Mann-Whitney秩和U检验和Spearman秩序相关检验。计算了两尾P值,并且在所有情况下均采用了常规的显着性水平P <.05。在测定IL-8之前,A组和B组的婴儿分别在3到52周(中位数为5.0周)和3到78周(中位数为4.5周)内没有尿路感染。在A组和B组之间,无UTI的时间长度没有显着差异(P = .469)。 A,B和C组的尿肌酐浓度没有差异(中位数分别为1.15、2.25和1.15μmol/ mL; P = .080)。 A组尿液IL-8 /肌酐的中位数浓度(pg /μmol)为40.5(范围2.03至3874),B组为1.91(范围为0.001至386)和B组为2.47(范围为0.002至55.6) C. A组的尿液IL-8 /肌酐浓度显着高于B组(P = .0003)和C组(P <.0001)。 B组和C组之间未观察到显着差异(P = .749)。在A组中,IL-8 /肌酐浓度与肾实质损害(P = .506),反流程度(P = .770)或距UTI时间(P = .155)之间无显着相关性。通过绘制IL-8 /肌酐的不同截断浓度的灵敏度与特异性的关系,绘制出接收者-操作者特征曲线。在尿液IL-8 /肌酐的截断浓度为5 pg /μmol时,该标志物诊断VUR的敏感性为88%,特异性为69%,阳性预后值为66%,阴性预后值为89%。在较高的临界浓度下,标记物的特异性增加,但灵敏度迅速降低。我们提供的证据表明,即使在没有UTI的情况下,VUR患儿的尿IL-8浓度仍保持升高,并且5 pg /μmolIL-8 /肌酐的临界值对VUR的诊断具有很高的敏感性和特异性。尿中IL-8水平在VUR和肾脏瘢痕形成方面已有报道。然而,据我们所知,本研究是第一个证实具有VUR的婴儿与有UTI病史的婴儿和健康对照之间的显着差异,并提出了可靠的临界浓度来诊断VUR的研究。我们的发现还表明,即使在UTI消退后,VUR中的炎症过程仍在进行,这与目前认为无菌回流不会损害肾脏的观点背道而驰。与反流性肾病相关的慢性炎性细胞浸润而不是VUR本身可能为IL-8的分泌提供了解释,IL-8的分泌可能与反流程度无关。使用尿液IL-8诊断VUR并非没有局限性,因为尿道操作或未检测到的UTI可能导致IL-8升高。此外,本研究关注的是婴儿,而不是长期存在VUR的较大儿童。 UTI解决后尿液IL-8浓度升高是一种有前途的无创性标志物,可用于婴儿期VUR的初筛,具有高灵敏度和足够的特异性。

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