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47?Pathologists enhance interpretation of automated multiplex immunohistochemistry assays in cancer immunotherapy trials

机译:47?病理学家提高癌症免疫治疗试验中自动多重免疫组织化学分析的解释

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Background Multiplex fluorescence immunohistochemistry (mFIHC) enables simultaneous detection of multiple biomarkers on a single tissue section. Spatial patterns and differential expression of immune- and tumor cell biomarkers serve as powerful predictors of immunotherapies. In a recent meta-analyses of 8135 patients treated with PD1/L1 pathway blockers, mFIHC was found to provide highest predictive power (P0.05) amongst commonly utilized biomarker modalities, namely, PD-L1 IHC, Tumor Mutation Burden and Gene Expression Profiling alone. [Lu et al ., JAMA Oncol 2019]. As biomarkers in mFIHC assays are read by computer-aided algorithms, the role of pathologists in the digital workflow has been debated. Utilizing clinical cases representing multiple tumor indications, we illustrate the critical collaboration between pathologists (human intelligence, HI) and computer workflows (artificial intelligence, AI) required for accurate interpretation of mFIHC assays in cancer immunotherapy trials. Methods In our clinical trial laboratory, pathologists are involved in pre-analytical, analytical and post-analytical phases of clinical trial sample testing. In the pre-analytical phase, pathologist(s) perform histological examination of H&E stained tissue sections to annotate and confirm tissue types, diagnosis, tissue integrity and acceptance (including viable tumor component), followed by determination of Region of Interest (ROI) for subsequent analysis by computerized programs. In the analytical phase, pathologists identify specific areas of biological and/or clinical interest within ROI (tumor, non-tumor, invasive margin, and tumor-stromal interphase) in the computer scans, as well as exclude ROI containing necrosis, hemorrhage, blood vessels, and autofluorescence. Those pathologist-selected images are then quantified by digital pathology software such as Automated QUantitative Analyses (AQUA?) technology. Finally, pathologists also provide interpretation and summarize findings relevant to the clinical study during the post-analytical phase. Results Case studies representing distinct malignancies, such as melanoma, non-small cell lung cancer, squamous cell carcinoma of head and neck and diffuse large B-cell lymphoma, illustrating the role of pathologists and especially in rescuing challenging cases and interpreting biomarkers scores from mFIHC assays will be presented. Conclusions With the advancement in technologies to detect increasing number of biomarkers in a single tissue section and accompanied growth of mFIHC assays in immuno-oncology studies, there is a clear transition from conventional pathology (HI) to computer-aided pathology (AI HI) that will ultimately ensure greater accuracy, reproducibility and standardization of clinical trial testing, and enable approval of more effective therapies and better patient care.
机译:背景技术多重荧光免疫组织化学(MFIHC)能够在单个组织部分上同时检测多个生物标志物。免疫和肿瘤细胞生物标志物的空间模式和差异表达作为免疫疗法的强大预测因子。在最近对PD1 / L1途径阻滞剂处理的8135名患者的荟萃分析中,发现MFIHC在常用的生物标志物型号中提供最高的预测力(P <0.05),即PD-L1 IHC,肿瘤突变负担和基因表达分析独自的。 [Lu等人,Jama Oncol 2019]。随着MFIHC测定中的生物标志物被计算机辅助算法读取,病理学家在数字工作流中的作用已经讨论。利用代表多种肿瘤适应症的临床病例,我们说明了准确地解释癌症免疫治疗试验中的MFIHC测定所需的病理学家(人类智能,HI)和计算机工作流程(人工智能,AI)之间的关键合作。方法在我们的临床试验实验室中,病理学家参与了临床试验样品测试的预分析,分析和分析阶段。在预分析阶段,病理学家对H&E的组织学检查进行H&E染色的组织切片,以注释和确认组织类型,诊断,组织完整性和验收(包括活肿瘤组分),然后测定感兴趣区域(ROI)通过计算机化程序进行后续分析。在分析阶段,病理学医生在计算机扫描中识别ROI(肿瘤,非肿瘤,侵袭性余量和肿瘤 - 基质间相互作用)的特定生物和/或临床兴趣区域,以及含有坏死,出血,血液的ROI血管和自发荧光。然后通过数字病理软件(如自动定量分析(AQUA)技术)量化这些病理学家的图像。最后,病理学家还提供了与分析后阶段临床研究相关的解释和总结结果。结果案例研究代表不同的恶性肿瘤,如黑素瘤,非小细胞肺癌,头部和颈部鳞状细胞癌,弥漫性大B细胞淋巴瘤,说明了病理学家的作用,特别是在救援挑战性案件和解释来自MFIHC的生物标志物分数分析将被提出。结论,在免疫肿瘤学研究中检测单个组织切片中的越来越多的生物标志物的推进,以及伴随免疫肿瘤学研究中的MFIHC测定的增长,从常规病理学(HI)到计算机辅助病理(AI HI),有明显的转变最终将确保更高的准确性,可重复性和标准化的临床试验,并能够批准更有效的疗法和更好的患者护理。
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