イタバシ ミチオ   Itabashi Michio
  板橋 道朗
   所属   医学部 医学科
   職種   特任教授
論文種別 原著
言語種別 英語
査読の有無 査読なし
表題 Feasibility of Pooled One-Step Nucleic Acid Amplification for Molecular Staging of Pathologically Node-Negative Colon Cancer: A Prospective Multicenter Study.
掲載誌名 正式名:Annals of surgical oncology
略  称:Ann Surg Oncol
ISSNコード:15344681/10689265
掲載区分国外
巻・号・頁 28(13),pp.8804-8812
著者・共著者 TANI Kimitaka†, ITABASHI Michio, OKUYA Koichi, TAKEMASA Ichiro, TOMITA Naohiro, OGAWA Shimpei, NAGASHIMA Yoji, YAMAMOTO Masakazu
担当区分 2nd著者
発行年月 2021/12
概要 BACKGROUND:Although conventional one-step nucleic acid amplification (OSNA) is a useful molecular-staging method, its complexity hinders its use in clinical practice. A pooled approach for OSNA (pOSNA) has been evaluated for its feasibility in pathologically node-negative colon cancer (pNNCC) for molecular staging of lymph node metastasis in clinical practice.METHODS:Subjects were patients diagnosed with clinical stage II-IIIA colon cancer between January 2017 and September 2018. pOSNA involved harvesting pericolic lymph nodes from fresh surgical specimens, cutting them in half, placing 50% of the nodes in a single test tube, and performing the OSNA assay. The remaining halved pericolic, intermediate, and main lymph nodes were submitted for histopathologic examination, with metastasis determined by hematoxylin and eosin staining of a cut surface of each node.RESULTS:Of the 98 enrolled patients, 92 formed the analysis set. The mean number of harvested lymph nodes per case was 24.3 (range 5-66) and the mean number of lymph nodes used for pOSNA analysis was 6.9 (range 1-35). The concordance rate, sensitivity, and specificity between methods were 89.1%, 84.6% (95% confidence interval [CI] 0.80-0.91), and 90.9% (95% CI 0.88-0.94), respectively. The pOSNA upstaging rate for node-negative patients was 9.1% (6/66), and pOSNA returned false-negative results in 15.4% of node-positive cases (4/26).CONCLUSIONS:pOSNA demonstrated an upstaging rate for pNNCC equivalent to that in previous studies, suggesting its feasibility for molecular staging of pNNCC in clinical practice.
DOI 10.1245/s10434-021-10140-9
PMID 34086123