Urinary soluble CD163 is a putative non-invasive biomarker for primary sclerosing cholangitis

IF 2.8 4区 医学 Q2 PATHOLOGY Experimental and molecular pathology Pub Date : 2024-05-09 DOI:10.1016/j.yexmp.2024.104900
Tanja Elger , Tanja Fererberger , Muriel Huss , Stefanie Sommersberger , Patricia Mester , Petra Stoeckert , Stefan Gunawan , Gerhard Liebisch , Johanna Loibl , Arne Kandulski , Martina Müller , Christa Buechler , Hauke Christian Tews
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Abstract

Soluble CD163 (sCD163) is a selective marker of macrophages whose circulating levels have been found to be induced in patients with active inflammatory bowel disease (IBD). Urinary proteins are emerging as non-invasive diagnostic biomarkers, and here, sCD163 levels were measured in the urine of 18 controls and 63 patients with IBD by enzyme-linked immunosorbent assay. Urinary sCD163 levels did, however, not differentiate IBD patients from controls. Analysis of sCD163 in the serum of 51 of these patients did not show higher levels in IBD. Primary sclerosing cholangitis (PSC) is often associated with IBD, and sCD163 was higher in the urine of the 21 patients and in the serum of the 13 patients with PSC compared to patients with IBD. Of clinical relevance, urinary sCD163 levels were higher in PSC patients compared to those with other chronic liver diseases (n = 16), while serum sCD163 levels were comparable between the two groups. Serum sCD163 of IBD and PSC patients positively correlated with serum C-reactive protein. Serum creatinine and glomerular filtration rate, surrogate markers for renal function, did not significantly correlate with urinary or serum sCD163 levels in IBD or PSC patients. Moreover, urinary sCD163 was not related to fecal calprotectin levels whereas serum sCD163 of IBD patients showed a positive trend. PSC associated with IBD and PSC without underlying IBD had similar levels of urinary sCD163 while serum sCD163 tended to be higher in the latter group. In PSC patients, urinary sCD163 did not correlate with serum aminotransferase levels, gamma glutamyl transferase, alkaline phosphatase, bilirubin or the Model for End Stage Liver Disease score. Ursodeoxycholic acid was prescribed to our PSC patients and fecal levels of ursodeoxycholic acid and its conjugated forms were increased in PSC compared to IBD patients. Otherwise, fecal bile acid levels of IBD and PSC patients were almost identical, and were not correlated with urinary and serum sCD163 in PSC. In summary, our study identified urinary sCD163 as a potential biomarker for PSC.

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尿液可溶性 CD163 是原发性硬化性胆管炎的一种假定非侵入性生物标记物
可溶性 CD163(sCD163)是巨噬细胞的一种选择性标记物,其循环水平在活动性炎症性肠病(IBD)患者中被诱导。尿液蛋白正逐渐成为非侵入性诊断生物标志物,本研究采用酶联免疫吸附法测定了 18 名对照组和 63 名 IBD 患者尿液中的 sCD163 水平。然而,尿液中的 sCD163 水平并不能将 IBD 患者与对照组区分开来。对其中 51 名患者血清中的 sCD163 进行分析,也未发现 IBD 患者血清中的 sCD163 含量更高。原发性硬化性胆管炎(PSC)通常与 IBD 相关,与 IBD 患者相比,21 名 PSC 患者尿液中的 sCD163 含量更高,13 名 PSC 患者血清中的 sCD163 含量更高。具有临床意义的是,与其他慢性肝病患者(16 人)相比,PSC 患者尿液中的 sCD163 水平更高,而两组患者血清中的 sCD163 水平相当。IBD 和 PSC 患者的血清 sCD163 与血清 C 反应蛋白呈正相关。血清肌酐和肾小球滤过率作为肾功能的替代指标,与 IBD 和 PSC 患者的尿液或血清 sCD163 水平无明显相关性。此外,尿液中的 sCD163 与粪便钙蛋白水平无关,而 IBD 患者血清中的 sCD163 则呈正相关趋势。伴有 IBD 的 PSC 和没有潜在 IBD 的 PSC 的尿 sCD163 水平相似,而后者的血清 sCD163 水平更高。在 PSC 患者中,尿 sCD163 与血清转氨酶水平、γ 谷氨酰转移酶、碱性磷酸酶、胆红素或终末期肝病模型评分没有相关性。我们为 PSC 患者开具了熊去氧胆酸处方,与 IBD 患者相比,PSC 患者粪便中熊去氧胆酸及其共轭形式的含量有所增加。除此之外,IBD 和 PSC 患者粪便中胆汁酸的水平几乎相同,并且与 PSC 患者尿液和血清中的 sCD163 无关。总之,我们的研究发现尿液中的sCD163是PSC的潜在生物标志物。
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来源期刊
CiteScore
8.90
自引率
0.00%
发文量
78
审稿时长
11.5 weeks
期刊介绍: Under new editorial leadership, Experimental and Molecular Pathology presents original articles on disease processes in relation to structural and biochemical alterations in mammalian tissues and fluids and on the application of newer techniques of molecular biology to problems of pathology in humans and other animals. The journal also publishes selected interpretive synthesis reviews by bench level investigators working at the "cutting edge" of contemporary research in pathology. In addition, special thematic issues present original research reports that unravel some of Nature''s most jealously guarded secrets on the pathologic basis of disease. Research Areas include: Stem cells; Neoangiogenesis; Molecular diagnostics; Polymerase chain reaction; In situ hybridization; DNA sequencing; Cell receptors; Carcinogenesis; Pathobiology of neoplasia; Complex infectious diseases; Transplantation; Cytokines; Flow cytomeric analysis; Inflammation; Cellular injury; Immunology and hypersensitivity; Athersclerosis.
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