Exploring the potential of cell-free tumor DNA in bronchoscopic diagnosis of peripheral lung lesions-the DRILL study.

IF 1.8 Q3 RESPIRATORY SYSTEM
European Clinical Respiratory Journal Pub Date : 2025-03-07 eCollection Date: 2025-01-01 DOI:10.1080/20018525.2025.2474277
Amanda Juul, Arman Arshad, Alice V Christophersen, Julie Gellert Larsen, Alexis Pulga, Pernille Kristiansen, Torben Riis Rasmussen, Søren Helbo Skaarup, Ole Hilberg, Christian B Laursen
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引用次数: 0

Abstract

Background: Small lung lesions can represent early-stage lung cancer but are difficult to diagnose. The bronchoscopic approach has the lowest risk of complications; however, the diagnostic yield is generally lower compared to trans-thoracic biopsies. Cell-free tumor DNA (cftDNA) is fragmented DNA stemming from a tumor. CftDNA in the form of methylated HOXA9 has previously been detected in bronchial lavage (BL) and has been proposed as an adjunct to conventional biopsies to improve diagnostic yield. The aim of this study was to assess whether methylated HOXA in BL could be utilized as an add-on diagnostic modality for bronchoscopic tissue sampling.

Method: The study was conducted as a prospective diagnostic accuracy study in accordance with STARD guidelines. Patients undergoing bronchoscopy for diagnosing peripheral lung lesions were included. During bronchoscopy, BL samples were collected before and after biopsy. The samples were analyzed for methylated HOXA using a predefined cutoff and compared to histopathology or the result of CT surveillance.

Results: One hundred seventy-two patients were included, with samples collected from 155 patients. A definite diagnosis was obtained from bronchoscopic biopsies in 47.1%. The sensitivity and specificity of methylated HOXA9 in BL were 68.0 (58.0-76.8) and 76.3 (59.8-88.6), respectively. The positive likelihood ratio of methylated HOXA9 in patients with a non-diagnostic biopsy was 2.11.

Conclusion: The diagnostic accuracy of methylated HOXA9 in BL was too low to confirm or refute malignancy following an inconclusive biopsy; however, BL was superior to blood samples.

探讨无细胞肿瘤DNA在支气管镜诊断肺周围病变中的潜力- DRILL研究。
背景:小的肺病变可以代表早期肺癌,但很难诊断。支气管镜入路并发症风险最低;然而,与经胸活检相比,诊断率通常较低。无细胞肿瘤DNA (cftDNA)是来自肿瘤的片段化DNA。甲基化HOXA9形式的CftDNA先前在支气管灌洗(BL)中被检测到,并被提议作为常规活检的辅助手段来提高诊断率。本研究的目的是评估甲基化HOXA在BL中是否可以作为支气管镜组织取样的附加诊断方式。方法:本研究是根据STARD指南进行的前瞻性诊断准确性研究。接受支气管镜检查诊断周围肺病变的患者也包括在内。在支气管镜检查中,活检前后分别采集BL样本。使用预定义的截止值对样品进行甲基化HOXA分析,并与组织病理学或CT监测结果进行比较。结果:纳入172例患者,从155例患者中采集样本。47.1%的患者通过支气管镜活检得到明确诊断。甲基化HOXA9在BL中的敏感性和特异性分别为68.0(58.0 ~ 76.8)和76.3(59.8 ~ 88.6)。非诊断性活检患者的甲基化HOXA9阳性似然比为2.11。结论:在不确定的活检后,甲基化HOXA9在BL中的诊断准确性太低,无法证实或驳斥恶性肿瘤;但BL优于血液样本。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
CiteScore
3.80
自引率
0.00%
发文量
15
审稿时长
16 weeks
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