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非胰腺性高胰脂酶血症:一种令人费解的临床病症。

Non-pancreatic hyperlipasemia: A puzzling clinical entity.

机构信息

Division of Gastroenterology, Department of Internal Medicine, Faculty of Medicine, University of Debrecen, Debrecen H-4032, Hajdu-Bihar, Hungary.

Kalman Laki Doctoral School of Biomedical and Clinical Sciences, Faculty of Medicine, University of Debrecen, Debrecen H-4032, Hungary.

出版信息

World J Gastroenterol. 2024 May 21;30(19):2538-2552. doi: 10.3748/wjg.v30.i19.2538.

Abstract

BACKGROUND

Increased lipase level is a serological hallmark of the diagnosis of acute pancreatitis (AP) but can be detected in various other diseases associated with lipase leakage due to inflammation of organs surrounding the pancreas or reduced renal clearance and/or hepatic metabolism. This non-pancreatic hyperlipasemia (NPHL) is puzzling for attending physicians during the diagnostic procedure for AP. It would be clinically beneficial to identify the clinical and laboratory variables that hinder the accuracy of lipase diagnosis with the aim of improve it. A more precise description of the NPHL condition could potentially provide prognostic factors for adverse outcomes which is currently lacking.

AIM

To perform a detailed clinical and laboratory characterization of NPHL in a large prospective patient cohort with an assessment of parameters determining disease outcomes.

METHODS

A Hungarian patient cohort with serum lipase levels at least three times higher than the upper limit of normal (ULN) was prospectively evaluated over 31 months. Patients were identified using daily electronic laboratory reports developed to support an ongoing observational, multicenter, prospective cohort study called the EASY trial (ISRCTN10525246) to establish a simple, easy, and accurate clinical scoring system for early prognostication of AP. Diagnosis of NPHL was established based on ≥ 3 × ULN serum lipase level in the absence of abdominal pain or abdominal imaging results characteristic of pancreatitis.

RESULTS

A total of 808 patients [male, = 420 (52%); median age (IQR): 65 (51-75) years] were diagnosed with ≥ 3 × ULN serum lipase levels. A total of 392 patients had AP, whereas 401 had NPHL with more than 20 different etiologies. Sepsis and acute kidney injury (AKI) were the most prevalent etiologies of NPHL (27.7% and 33.2%, respectively). The best discriminative cut-off value for lipase was ≥ 666 U/L (sensitivity, 71.4%; specificity, 88.8%). The presence of AKI or sepsis negatively affected the diagnostic performance of lipase. NPHL was associated with a higher in-hospital mortality than AP (22.4% 5.1%, < 0.001). In multivariate binary logistic regression, not lipase but increased amylase level (> 244 U/L) and neutrophil-to-lymphocyte ratio (NLR) (> 10.37, OR: 3.71, 95%CI: 2.006-6.863, < 0.001), decreased albumin level, age, and presence of sepsis were independent risk factors for in-hospital mortality in NPHL.

CONCLUSION

NPHL is a common cause of lipase elevation and is associated with high mortality rates. Increased NLR value was associated with the highest mortality risk. The presence of sepsis/AKI significantly deteriorates the serological differentiation of AP from NPHL.

摘要

背景

胰酶水平升高是诊断急性胰腺炎(AP)的血清学标志,但由于胰腺周围器官炎症导致的胰酶漏出,或由于肾脏清除率降低和/或肝脏代谢减少,也可在各种其他与胰酶漏出相关的疾病中检测到。这种非胰腺性高胰酶血症(NPHL)在 AP 的诊断过程中给主治医生带来了困惑。如果能识别出影响胰酶诊断准确性的临床和实验室变量,并以此来提高其准确性,这将具有临床意义。更详细地描述 NPHL 状况可能为不良预后提供潜在的预后因素,而目前这方面的信息还很缺乏。

目的

对一个大的前瞻性患者队列进行详细的临床和实验室特征描述,并评估确定疾病结局的参数。

方法

前瞻性评估了 31 个月期间血清脂肪酶水平至少比正常值上限(ULN)高 3 倍的匈牙利患者队列。使用每日电子实验室报告来识别患者,该报告是为支持一项正在进行的观察性、多中心、前瞻性队列研究而开发的,该研究名为 EASY 试验(ISRCTN10525246),旨在建立一种简单、易用、准确的临床评分系统,以便早期预测 AP 的预后。根据血清脂肪酶水平≥3×ULN 且无腹痛或腹部成像结果符合胰腺炎的情况下,诊断为 NPHL。

结果

共有 808 名患者[男性占 420 名(52%);中位年龄(IQR):65(51-75)岁]被诊断为血清脂肪酶水平≥3×ULN。共有 392 名患者患有 AP,而 401 名患者患有 NPHL,其病因超过 20 种。脓毒症和急性肾损伤(AKI)是 NPHL 最常见的病因(分别为 27.7%和 33.2%)。胰酶的最佳鉴别截断值为≥666 U/L(敏感性为 71.4%,特异性为 88.8%)。AKI 或脓毒症的存在会降低胰酶的诊断性能。与 AP 相比,NPHL 院内死亡率更高(22.4% 比 5.1%,<0.001)。在多变量二项逻辑回归中,不是胰酶,而是升高的淀粉酶水平(>244 U/L)和中性粒细胞与淋巴细胞比值(NLR)(>10.37,OR:3.71,95%CI:2.006-6.863,<0.001)、白蛋白水平降低、年龄和脓毒症的存在是 NPHL 院内死亡的独立危险因素。

结论

NPHL 是胰酶升高的常见原因,与高死亡率相关。升高的 NLR 值与最高的死亡风险相关。脓毒症/AKI 的存在显著降低了 AP 与 NPHL 的血清学鉴别诊断。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/943a/11135416/42ba55903101/WJG-30-2538-g001.jpg

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