O'Driscoll Shane, Piggott Carolyn, Benton Sally C
NHS Bowel Cancer Screening Programme Southern Hub, Royal Surrey County Hospital, England.
Berkshire and Surrey Pathology Services, Royal Surrey County Hospital, England.
Ann Clin Biochem. 2025 Jan;62(1):67-70. doi: 10.1177/00045632241273266. Epub 2024 Aug 14.
Faecal calprotectin is an inflammatory marker used to triage patients for further investigation with suspected inflammatory bowel disease (IBD). Our current method requires faecal samples be sent to the laboratory, where calprotectin is extracted before analysis. This is a time-consuming, potential bottleneck in the pathway. We have recently evaluated the OC-SENSOR PLEDIA fCAL method that uses the same sampling device as used in some bowel cancer screening and symptomatic colorectal cancer programmes that detect faecal haemoglobin. The below study is a comparison of the OC-FCa method with the BÜHLMANN fCAL Turbo which is used routinely within BSPS.
150 homogenised and 110 non-homogenised faecal samples were loaded into OC-Sampling Bottle 3 and BÜHLMANN CALEX cap sampling devices. The samples were then analysed on their respective systems according to manufacturer's instructions.
The OC-FCa assay had a mean positive bias of 67.3% (homogenised) and 88.4% (non-homogenised). Homogenised samples showed substantial agreement between the methods for normal (<50 µg/g) and elevated (150+µg/g) risk categories (k = 0.794, k = 0.788, respectively) and moderate agreement for borderline (51-150 µg/g) (k = 0.25) according to the current Berkshire and Surrey Pathology Service (BSPS) guidelines. Non-homogenised samples had none to slight agreement for normal and borderline values (k = 0.02 for both) and moderate agreement for elevated (k = 0.596).
The OC-FCa method is a viable alternative for faecal calprotectin testing, but requires an adjustment to clinical cut-off values due to the lack of standardisation and strong positive bias. A clinical comparative study is required to assess the impact of patients collecting their own samples into the devices, as this may negate any potential degradation samples may exhibit during transit to the laboratory.
粪便钙卫蛋白是一种炎症标志物,用于对疑似炎症性肠病(IBD)患者进行分流以便进一步检查。我们目前的方法需要将粪便样本送到实验室,在那里提取钙卫蛋白后进行分析。这是该流程中耗时且可能成为瓶颈的环节。我们最近评估了OC-SENSOR PLEDIA fCAL方法,该方法使用的采样装置与一些检测粪便血红蛋白的肠癌筛查和有症状结直肠癌项目中使用的相同。以下研究是将OC-FCa方法与BSPS常规使用的BÜHLMANN fCAL Turbo方法进行比较。
将150份匀浆粪便样本和110份未匀浆粪便样本装入OC采样瓶3和BÜHLMANN CALEX帽式采样装置中。然后根据制造商的说明在各自的系统上对样本进行分析。
OC-FCa检测在匀浆样本中的平均正偏差为67.3%,在未匀浆样本中为88.4%。根据目前伯克希尔和萨里病理服务(BSPS)指南,匀浆样本在正常(<50μg/g)和高风险(150μg/g及以上)类别中两种方法之间显示出实质性一致性(分别为k = 0.794,k = 0.788),在临界值(51 - 150μg/g)时为中等一致性(k = 0.25)。未匀浆样本在正常和临界值时一致性为无至轻微(两者k = 0.02),在高风险时为中等一致性(k = 0.596)。
OC-FCa方法是粪便钙卫蛋白检测的一种可行替代方法,但由于缺乏标准化和强烈的正偏差,需要调整临床临界值。需要进行一项临床比较研究,以评估患者自行将样本采集到这些装置中的影响,因为这可能消除样本在运往实验室途中可能出现的任何潜在降解。
