多中心临床应用 Afirma 基因表达分类器的经验。
Multicenter clinical experience with the Afirma gene expression classifier.
机构信息
Department of Medicine (E.K.A., M.S.), The Brigham and Women's Hospital and Harvard Medical School, Boston, Massachusetts 02115; Department of Medicine (C.K., S.J.M.), Perelman School of Medicine, University of Pennsylvania, Philadelphia, Pennsylvania 19104; Department of Medicine (J.S., F.N.), The Ohio State University College of Medicine, Columbus, Ohio 43210; University of Cincinnati College of Medicine (C.P., D.L.S.), Cincinnati, Ohio 45220; and Department of Medicine (J.K., B.R.H.), University of Colorado School of Medicine, Aurora, Colorado 80045.
出版信息
J Clin Endocrinol Metab. 2014 Jan;99(1):119-25. doi: 10.1210/jc.2013-2482. Epub 2013 Dec 20.
BACKGROUND
Increasingly, patients with thyroid nodule cytology labeled atypical (or follicular lesion) of undetermined significance (AUS/FLUS) or follicular neoplasm (FN) undergo diagnostic analysis with the Afirma gene expression classifier (GEC). No long-term, multisite analysis of Afirma GEC performance has yet been performed.
METHODS
We analyzed all patients who had received Afirma GEC testing at five academic medical centers between 2010 and 2013. Nodule and patient characteristics, fine needle aspiration cytology, Afirma GEC results, and subsequent clinical or surgical follow-up were obtained for 339 patients. Results were analyzed for pooled test performance, impact on clinical care, and site-to-site variation.
RESULTS
Three hundred thirty-nine patients underwent Afirma GEC testing of cytologically indeterminate nodules (165 AUS/FLUS; 161 FN; 13 suspicious for malignancy) and 174 of 339 (51%) indeterminate nodules were GEC benign, whereas 148 GEC were suspicious (44%). GEC results significantly altered care recommendations, as 4 of 175 GEC benign were recommended for surgery in comparison to 141 of 149 GEC suspicious (P<.01). Of 121 Cyto Indeterminate/GEC Suspicious nodules surgically removed, 53 (44%) were malignant. Variability in site-to-site GEC performance was confirmed, as the proportion of GEC benign varied up to 29% (P=.58), whereas the malignancy rate in nodules cytologically indeterminate/GEC suspicious varied up to 47% (P=.11). Seventy-one of 174 GEC benign nodules had documented clinical follow-up for an average of 8.5 months, in which 1 of 71 nodules proved cancerous.
CONCLUSIONS
These multicenter, clinical experience data confirm originally published Afirma GEC test performance and demonstrate its substantial impact on clinical care recommendations. Although nonsignificant site-to-site variation exists, such differences should be anticipated by the practicing clinician. Follow-up of GEC benign nodules thus far confirm the clinical utility of this diagnostic test.
背景
越来越多的甲状腺结节细胞学检查结果为不典型(或滤泡性病变)意义不明(AUS/FLUS)或滤泡性肿瘤(FN)的患者,采用 Afirma 基因表达分类器(GEC)进行诊断分析。目前尚未对 Afirma GEC 的性能进行长期、多地点的分析。
方法
我们分析了 2010 年至 2013 年间在五所学术医疗中心接受 Afirma GEC 检测的所有患者。获取了 339 例患者的结节和患者特征、细针穿刺细胞学检查、Afirma GEC 结果以及随后的临床或手术随访结果。对汇总检测性能、对临床护理的影响以及各检测中心之间的差异进行了分析。
结果
339 例细胞学不确定的结节患者进行了 Afirma GEC 检测(165 例 AUS/FLUS;161 例 FN;13 例可疑恶性),339 例中的 174 例(51%)不确定结节的 GEC 为良性,而 148 例 GEC 为可疑(44%)。GEC 结果显著改变了护理建议,因为与 149 例 GEC 可疑的患者相比,4 例 GEC 良性患者建议手术治疗(P<.01)。在 121 例细胞学不确定/GEC 可疑的结节中,有 53 例(44%)为恶性。各检测中心间 GEC 性能的差异得到了证实,因为 GEC 良性的比例差异高达 29%(P=.58),而细胞学不确定/GEC 可疑的结节的恶性率差异高达 47%(P=.11)。在 174 例 GEC 良性结节中,有 71 例有记录的临床随访,平均随访时间为 8.5 个月,其中 1 例证实为癌症。
结论
这些多中心临床经验数据证实了最初发表的 Afirma GEC 检测性能,并证明了其对临床护理建议的重大影响。尽管存在无统计学意义的检测中心间差异,但临床医生应预料到这种差异。目前对 GEC 良性结节的随访证实了该诊断检测的临床应用价值。
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