基层医疗中色素沉着性皮肤病变的皮肤镜检查准确性:一种新诊断算法的开发与验证
Accuracy of SIAscopy for pigmented skin lesions encountered in primary care: development and validation of a new diagnostic algorithm.
作者信息
Emery Jon D, Hunter Judith, Hall Per N, Watson Anthony J, Moncrieff Marc, Walter Fiona M
机构信息
General Practice, School of Primary, Aboriginal and Rural Health Care, University of Western Australia, 328 Stirling Highway, Claremont, WA 6010, Australia.
出版信息
BMC Dermatol. 2010 Sep 25;10:9. doi: 10.1186/1471-5945-10-9.
BACKGROUND
Diagnosing pigmented skin lesions in general practice is challenging. SIAscopy has been shown to increase diagnostic accuracy for melanoma in referred populations. We aimed to develop and validate a scoring system for SIAscopic diagnosis of pigmented lesions in primary care.
METHODS
This study was conducted in two consecutive settings in the UK and Australia, and occurred in three stages: 1) Development of the primary care scoring algorithm (PCSA) on a sub-set of lesions from the UK sample; 2) Validation of the PCSA on a different sub-set of lesions from the same UK sample; 3) Validation of the PCSA on a new set of lesions from an Australian primary care population. Patients presenting with a pigmented lesion were recruited from 6 general practices in the UK and 2 primary care skin cancer clinics in Australia. The following data were obtained for each lesion: clinical history; SIAscan; digital photograph; and digital dermoscopy. SIAscans were interpreted by an expert and validated against histopathology where possible, or expert clinical review of all available data for each lesion.
RESULTS
A total of 858 patients with 1,211 lesions were recruited. Most lesions were benign naevi (64.8%) or seborrhoeic keratoses (22.1%); 1.2% were melanoma. The original SIAscopic diagnostic algorithm did not perform well because of the higher prevalence of seborrhoeic keratoses and haemangiomas seen in primary care. A primary care scoring algorithm (PCSA) was developed to account for this. In the UK sample the PCSA had the following characteristics for the diagnosis of 'suspicious': sensitivity 0.50 (0.18-0.81); specificity 0.84 (0.78-0.88); PPV 0.09 (0.03-0.22); NPV 0.98 (0.95-0.99). In the Australian sample the PCSA had the following characteristics for the diagnosis of 'suspicious': sensitivity 0.44 (0.32-0.58); specificity 0.95 (0.93-0.97); PPV 0.52 (0.38-0.66); NPV 0.95 (0.92-0.96). In an analysis of lesions for which histological diagnosis was available (n = 111), the PCSA had a significantly greater Area Under the Curve than the 7-point checklist for the diagnosis of melanoma (0.83; 95% CI 0.71-0.95 versus 0.61; 95% CI 0.44-0.78; p = 0.02 for difference).
CONCLUSIONS
The PCSA could have a useful role in improving primary care management of pigmented skin lesions. Further work is needed to develop and validate the PCSA in other primary care populations and to evaluate the cost-effectiveness of GP management of pigmented lesions using SIAscopy.
背景
在全科医疗中诊断色素沉着性皮肤病变具有挑战性。皮肤镜检查已被证明可提高转诊人群中黑色素瘤的诊断准确性。我们旨在开发并验证一种用于基层医疗中色素沉着性病变皮肤镜诊断的评分系统。
方法
本研究在英国和澳大利亚连续两个地点进行,分三个阶段:1)根据英国样本中的一部分病变开发基层医疗评分算法(PCSA);2)在英国样本的另一部分不同病变上验证PCSA;3)在澳大利亚基层医疗人群的一组新病变上验证PCSA。从英国的6家全科诊所和澳大利亚的2家基层医疗皮肤癌诊所招募有色素沉着性病变的患者。为每个病变获取以下数据:临床病史;皮肤镜扫描;数码照片;以及数码皮肤镜检查。皮肤镜扫描由一名专家进行解读,并尽可能对照组织病理学进行验证,或对每个病变的所有可用数据进行专家临床审查。
结果
共招募了858例患者,有1211个病变。大多数病变为良性痣(64.8%)或脂溢性角化病(22.1%);1.2%为黑色素瘤。由于在基层医疗中脂溢性角化病和血管瘤的患病率较高,最初的皮肤镜诊断算法表现不佳。为此开发了一种基层医疗评分算法(PCSA)。在英国样本中,PCSA诊断“可疑”病变具有以下特征:敏感性0.50(0.18 - 0.81);特异性0.84(0.78 - 0.88);阳性预测值0.09(0.03 - 0.22);阴性预测值0.98(0.95 - 0.99)。在澳大利亚样本中,PCSA诊断“可疑”病变具有以下特征:敏感性0.44(0.32 - 0.58);特异性0.95(0.93 - 0.97);阳性预测值0.52(0.38 - 0.66);阴性预测值0.95(0.92 - 0.96)。在对有组织学诊断的病变(n = 111)进行分析时,PCSA的曲线下面积显著大于黑色素瘤诊断的7分检查表(0.83;95%可信区间0.71 - 0.95 vs 0.61;95%可信区间0.44 - 0.78;差异p = 0.02)。
结论
PCSA在改善色素沉着性皮肤病变的基层医疗管理方面可能发挥有益作用。需要进一步开展工作,在其他基层医疗人群中开发并验证PCSA,并评估使用皮肤镜检查的全科医生对色素沉着性病变管理的成本效益。
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