肺癌类癌小活检组织中 Ki-67 和 OTP 的预后免疫组化:Ki-67指数可预测无进展生存期和非典型组织学。

Julia R Naso, Sarah M Jenkins, Anja C Roden, Euhee S Yi, Ying-Chun Lo, Melanie C Bois, Joseph J Maleszewski, Marie Christine Aubry, Jennifer M Boland
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摘要

将肺类癌分为 "典型 "和 "非典型 "两类进行预后分层需要对大量组织进行检查。然而,我们需要能为小型活检样本提供类似预后信息的工具。Ki-67和OTP免疫组化在切除的肺类癌研究中显示出良好的预后价值,但使用活检/细胞学标本的预后价值尚不明确。对肺类癌的小型活检/细胞学标本(n=139)进行了 Ki-67 免疫组化,并通过至少 500 个细胞的自动图像分析对标记指数进行评分。对70例有足够组织的病例进行了OTP免疫组化,并按阳性或阴性(20%肿瘤核染色)进行评分。Ki-67指数越高,疾病特异性无进展生存期(ds-PFS)越差,3%和4%阈值与ds-PFS的关系同样密切(P<0.001,危险比≥11)。Ki-67 <3%患者的三年ds-PFS为98%,Ki-67≥3%患者的三年ds-PFS为89%(P=0.0006)。预测随后切除的典型类癌组织学与非典型类癌组织学的最佳Ki-67阈值为3.21(AUC为0.68)。OTP染色阴性与不典型类癌组织学的关系接近显著性(P=0.06),但与ds-PFS的关系不显著(P=0.24,危险比=3.45),尽管样本量有限。我们建议,Ki-67免疫组化可有助于根据小型活检样本对类癌患者进行风险分层。值得注意的是,3%热点Ki-67阈值是预测ds-PFS的最佳阈值,因为3%的Ki-67阈值目前用于胃肠道神经内分泌肿瘤的分层,允许考虑跨器官系统的统一分类系统。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Prognostic Immunohistochemistry for Ki-67 and OTP on Small Biopsies of Pulmonary Carcinoid Tumors: Ki-67 Index Predicts Progression-free Survival and Atypical Histology.
Prognostic stratification of pulmonary carcinoids into "typical" and "atypical" categories requires examination of large tissue volume. However, there is a need for tools that provide similar prognostic information on small biopsy samples. Ki-67 and OTP immunohistochemistry have shown promising prognostic value in studies of resected pulmonary carcinoids, but prognostic value when using biopsy/cytology specimens is unclear. Ki-67 immunohistochemistry was performed on small biopsy/cytology specimens from pulmonary carcinoid tumors (n=139), and labeling index was scored via automated image analysis of at least 500 cells. OTP immunohistochemistry was performed on 70 cases with sufficient tissue and scored as positive or negative (<20% tumor nuclei staining). Higher Ki-67 index was associated with worse disease-specific progression-free survival (ds-PFS), with 3% and 4% thresholds having similarly strong associations with ds-PFS (P<0.001, hazard ratio ≥11). Three-year ds-PFS was 98% for patients with Ki-67 <3% and 89% for patients with Ki-67≥3% (P=0.0006). The optimal Ki-67 threshold for prediction of typical versus atypical carcinoid histology on subsequent resection was 3.21 (AUC 0.68). Negative OTP staining approached significance with atypical carcinoid histology (P=0.06) but not with ds-PFS (P=0.24, hazard ratio=3.45), although sample size was limited. We propose that Ki-67 immunohistochemistry may contribute to risk stratification for carcinoid tumor patients based on small biopsy samples. Identification of a 3% hot-spot Ki-67 threshold as optimal for prediction of ds-PFS is notable as a 3% Ki-67 threshold is currently used for gastrointestinal neuroendocrine tumor stratification, allowing consideration of a unified classification system across organ systems.
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