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原发性硬化性胆管炎中胆管疾病进展的替代标志物——一项重复进行内镜逆行胰胆管造影检查的前瞻性研究

Surrogate markers of bile duct disease progression in primary sclerosing cholangitis - A prospective study with repeated ERCP examinations.

作者信息

Färkkilä Martti, Åberg Fredrik, Alfthan Henrik, Jokelainen Kalle, Puustinen Lauri, Kautiainen Hannu, Tenca Andrea

机构信息

Helsinki University, Finland.

Department of Gastroenterology, Helsinki University Hospital, Abdominal Center, Helsinki, Finland.

出版信息

JHEP Rep. 2024 Jul 2;6(10):101161. doi: 10.1016/j.jhepr.2024.101161. eCollection 2024 Oct.

Abstract

BACKGROUND & AIMS: Validated prognostic tools for estimating short-term bile duct disease progression in primary sclerosing cholangitis (PSC) are lacking. We evaluated the predictive value of serum and biliary biochemistry for the progression of bile duct disease in PSC using repeated endoscopic retrograde cholangiopancreatography (ERCP) examinations to identify surrogate markers for more personalized surveillance.

METHODS

We conducted a prospective analysis including patients with PSC who underwent ERCP for confirmation of diagnosis, monitoring of disease progression, or dysplasia surveillance. ERCP findings were scored, and dilatation was performed if a dominant stricture was diagnosed or if a cytology brush could not be passed. Bile samples were aspirated for biliary IL8 and calprotectin. We analysed optimal cut-off values and AUCs for 20 laboratory markers and evaluated their association with the time to an ERCP score increase of ≥2 points or first dilatation, whichever came first. Of the 1,002 patients, 653 had ≥2 ERCP examinations and ≥3 years of follow-up. After excluding patients with PSC-overlap syndrome or initial dilatation, 398 patients were included.

RESULTS

Of the patients included, 62% had mild or moderate and 38% had advanced bile duct disease. During follow-up, 41% of patients demonstrated progression of disease. Biliary calprotectin (AUC 0.76; 95% CI 0.69 to 0.82) and IL8 (AUC 0.76; 95% CI 0.69 to 0.84) were the only variables that demonstrated predictive value for disease progression and/or need for dilatation.

CONCLUSIONS

Biliary calprotectin and IL8 are promising surrogate markers for identifying patients with PSC at risk of progression and determining the timing for subsequent imaging. Conventional liver function tests may not be sensitive or specific enough to monitor PSC progression, particularly in the short term.

IMPACT AND IMPLICATIONS

Validated prognostic tools for estimating short-term bile duct disease progression in primary sclerosing cholangitis are lacking. In this prospective study, based on sequential endoscopic retrograde cholangiopancreatography examinations, biliary calprotectin and IL8 levels turned out to be more sensitive for predicting bile duct progression than traditional liver function tests, such as alkaline phosphatase, in the short term. These findings could lead to more personalized patient surveillance and improve clinical practice by providing a more accurate method for monitoring disease progression and treatment responses. Additionally, these markers have potential as surrogate endpoints in clinical drug trials. The limitation is that measurement of biliary IL8 and calprotectin requires endoscopic retrograde cholangiopancreatography with bile sampling.

摘要

背景与目的

目前缺乏用于评估原发性硬化性胆管炎(PSC)短期胆管疾病进展的有效预后工具。我们通过重复进行内镜逆行胰胆管造影(ERCP)检查,评估血清和胆汁生化指标对PSC胆管疾病进展的预测价值,以确定更具个性化监测的替代标志物。

方法

我们进行了一项前瞻性分析,纳入因确诊、监测疾病进展或异型增生监测而接受ERCP的PSC患者。对ERCP检查结果进行评分,若诊断为主要狭窄或细胞刷无法通过,则进行扩张。采集胆汁样本检测胆汁白细胞介素8(IL8)和钙卫蛋白。我们分析了20种实验室指标的最佳截断值和曲线下面积(AUC),并评估它们与ERCP评分增加≥2分或首次扩张时间(以先到者为准)的相关性。1002例患者中,653例进行了≥2次ERCP检查且随访≥3年。排除PSC重叠综合征或初始扩张患者后,纳入398例患者。

结果

纳入患者中,62%患有轻度或中度胆管疾病,38%患有重度胆管疾病。随访期间,41%的患者疾病出现进展。胆汁钙卫蛋白(AUC 0.76;95%置信区间0.69至0.82)和IL8(AUC 0.76;95%置信区间0.69至0.84)是仅有的对疾病进展和/或扩张需求具有预测价值的变量。

结论

胆汁钙卫蛋白和IL8是有前景的替代标志物,可用于识别有疾病进展风险的PSC患者,并确定后续成像检查的时机。传统肝功能检查可能不够敏感或特异,不足以监测PSC进展,尤其是在短期内。

影响与意义

缺乏用于评估原发性硬化性胆管炎短期胆管疾病进展的有效预后工具。在这项前瞻性研究中,基于连续的内镜逆行胰胆管造影检查,结果表明,短期内胆汁钙卫蛋白和IL8水平在预测胆管进展方面比碱性磷酸酶等传统肝功能检查更敏感。这些发现可能带来更具个性化的患者监测,并通过提供更准确的疾病进展和治疗反应监测方法来改善临床实践。此外,这些标志物在临床药物试验中具有作为替代终点的潜力。局限性在于胆汁IL-8和钙卫蛋白的检测需要通过内镜逆行胰胆管造影采集胆汁样本。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0c95/11405802/98ef5a9dc7ec/ga1.jpg

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