Department of Medicine, Division of Pulmonary, Allergy and Critical Care, Duke University, Durham, NC.
Department of Medicine, Division of Medical Oncology, Duke University, Durham, NC.
Chest. 2023 Jul;164(1):252-261. doi: 10.1016/j.chest.2023.01.019. Epub 2023 Jan 21.
Pleural cytology is currently used to assess targetable mutations in patients with advanced lung adenocarcinoma. However, it is fraught with low diagnostic yield.
Can pleural cell-free DNA (cfDNA) be used to assess targetable mutations in lung adenocarcinoma patients with malignant pleural effusions (MPE)?
Patients with lung adenocarcinoma MPE were recruited prospectively between January 2017 and September 2021. Oncogenic mutations were assessed by treating providers using pleural fluid cytology or lung cancer biopsies. Pleural and plasma cfDNA were used to assess the mutations using next-generation sequencing (NGS).
Fifty-four pleural fluid samples were collected from 42 patients. The diagnostic yield to detect oncogenic mutations for pleural cfDNA, pleural cytology, biopsy, and plasma cfDNA was 49/54 (90.7%), 16/33 (48.5%), 22/25 (88%), and 24/32 (75%), respectively, P < .001. The agreement of mutations in positive samples between pleural cfDNA and pleural cytology was 100%, whereas the agreement of pleural cfDNA with biopsies was 89.4%. The median concentration (interquartile range) of pleural cfDNA was higher than plasma: 28,444 (4,957-67,051) vs 2,966.5 (2,167-5,025) copies of amplifiable DNA per mL, P < .01. Median of 5 mL (interquartile range, 4.5-5) of pleural fluid supernatant was adequate for cfDNA testing.
The diagnostic yield of pleural cfDNA NGS for oncogenic mutations in lung adenocarcinoma patients is comparable to tumor biopsies and higher than pleural cytology and plasma cfDNA. The pleural cfDNA can be longitudinally collected, can be readily incorporated in clinical workflow, and may decrease the need for additional biopsies.
胸膜细胞学目前用于评估晚期肺腺癌患者的可靶向突变。然而,其诊断率较低。
胸腔细胞游离 DNA(cfDNA)能否用于评估恶性胸腔积液(MPE)肺腺癌患者的可靶向突变?
2017 年 1 月至 2021 年 9 月,前瞻性招募 MPE 肺腺癌患者。采用胸腔积液细胞学或肺癌活检治疗提供者评估致癌突变。使用下一代测序(NGS)检测胸腔和血浆 cfDNA 以评估突变。
42 例患者共采集 54 份胸腔液样本。胸腔 cfDNA、胸腔细胞学、活检和血浆 cfDNA 检测致癌突变的诊断率分别为 49/54(90.7%)、16/33(48.5%)、22/25(88%)和 24/32(75%),P<0.001。胸腔 cfDNA 与胸腔细胞学阳性样本中突变的一致性为 100%,而与活检的一致性为 89.4%。胸腔 cfDNA 的中位数(四分位距)高于血浆:28444(4957-67051)比 2966.5(2167-5025)拷贝/ml 可扩增 DNA,P<0.01。5ml(四分位距,4.5-5)胸腔液上清即可满足 cfDNA 检测要求。
肺腺癌患者胸腔 cfDNA NGS 检测致癌突变的诊断率与肿瘤活检相当,高于胸腔细胞学和血浆 cfDNA。胸腔 cfDNA 可以进行纵向采集,可轻松纳入临床工作流程,可能减少对额外活检的需求。
