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对CT引导和支气管镜引导下肺病变活检的临床放射学、组织病理学及免疫组化特征的批判性评估

A critical appraisal of the clinico-radiological, histopathological and immunohistochemical profile of CT-guided and bronchoscopy-guided biopsies in lung lesions.

作者信息

Pujani Mukta, Sachdeva Ruchi Arora, Abbas S Zafar, Agarwal Charu, Bhardwaj Minakshi, Chauhan Varsha, Rajpoot Jyoti, Sidam Dipti, Dey Aniruna

机构信息

Department of Pathology, ESIC Medical College and Hospital, Faridabad, Haryana, India.

Department of Pulmonary Medicine, ESIC Hospital and PGIMSR Basaidarapur, New Delhi, India.

出版信息

Lung India. 2025 May 1;42(3):218-224. doi: 10.4103/lungindia.lungindia_496_24. Epub 2025 Apr 29.

Abstract

BACKGROUND

Lung biopsies are obtained by bronchoscopy or by percutaneous route under image guidance and usually have limited tissue material. It is quite challenging for a pathologist to make an accurate diagnosis of lung cancer using only a limited panel of immunohistochemical markers and mucin stains as well as spare as much tissue for molecular testing.Molecular testing for specific genetic mutations or biomarkers serves as an adjunct for more rational, targeted treatment regimens.

METHODS

All the consecutive image-guided lung biopsies (both computed tomography [CT] guided and bronchoscopy-guided) for a period of 3 years (2021-2024) were included in the study. The clinicopathological data was compiled from the hospital records, and histopathology and immunohistochemistry (IHC) were analysed critically for all lung carcinomas. Sensitivity, specificity, negative predictive value, positive predictive value and diagnostic accuracy were calculated for IHC markers.

RESULTS

There were 127 lung biopsies (117 bronchoscopic and 10 CT-guided biopsies) comprise of adenocarcinoma (30%), squamous cell carcinoma (25.2%), small-cell carcinoma (13.4%) and poorly differentiated carcinoma (6.3%). The concordance between clinico-radiological and pathological diagnosis was 85%. P40 (22/22 cases) and CK5/6 (10/10) were the most sensitive and specific markers for squamous cell carcinoma, while TTF-1 (35/36) and Napsin A (18/22) were the most sensitive IHC markers for adenocarcinoma. The most sensitive markers for small-cell carcinoma lung were synaptophysin (17/17), CD 56, NSE followed by chromogranin A (11/15).

CONCLUSION

Integrating conventional histopathology with IHC results in accurate diagnosis, thereby avoiding a broad diagnosis of non-small-cell lung carcinoma (NSCLC). Subclassification of NSCLC has significant treatment implications, especially for advanced-stage tumours for which chemotherapy or targeted therapy is being considered. The focus should be on the judicious use of IHC based on histological type because of the limited availability of tissues in bronchoscopic and CT-guided biopsy specimens.

摘要

背景

肺活检可通过支气管镜检查或在影像引导下经皮途径获取,通常组织材料有限。对于病理学家而言,仅使用有限的免疫组织化学标志物、黏液染色组合并尽可能保留足够组织用于分子检测来准确诊断肺癌颇具挑战性。针对特定基因突变或生物标志物的分子检测可辅助制定更合理、有针对性的治疗方案。

方法

本研究纳入了连续3年(2021 - 2024年)所有影像引导下的肺活检病例(包括计算机断层扫描[CT]引导和支气管镜引导的活检)。临床病理数据从医院记录中整理得出,对所有肺癌病例进行了严格的组织病理学和免疫组织化学(IHC)分析。计算了IHC标志物的敏感性、特异性、阴性预测值、阳性预测值和诊断准确性。

结果

共有127例肺活检病例(117例支气管镜活检和10例CT引导下活检),包括腺癌(30%)、鳞状细胞癌(25.2%)、小细胞癌(13.4%)和低分化癌(6.3%)。临床放射学诊断与病理诊断的一致性为85%。P40(22/22例)和CK5/6(10/10)是鳞状细胞癌最敏感和特异的标志物,而TTF - 1(35/36)和Napsin A(18/22)是腺癌最敏感的IHC标志物。肺小细胞癌最敏感的标志物是突触素(17/17)、CD56、神经元特异性烯醇化酶,其次是嗜铬粒蛋白A(11/15)。

结论

将传统组织病理学与IHC相结合可实现准确诊断,从而避免对非小细胞肺癌(NSCLC)进行宽泛诊断。NSCLC的亚分类对治疗具有重要意义,尤其是对于正在考虑化疗或靶向治疗的晚期肿瘤。由于支气管镜和CT引导下活检标本中的组织有限,应基于组织学类型谨慎使用IHC。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f93f/12097671/12150a63bef1/LI-42-218-g001.jpg

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