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用于测量肿瘤组织中程序性死亡配体-1表达的免疫组织化学检测方法原型的开发。

Development of a Prototype Immunohistochemistry Assay to Measure Programmed Death Ligand-1 Expression in Tumor Tissue.

作者信息

Dolled-Filhart Marisa, Locke Darren, Murphy Tiffany, Lynch Frank, Yearley Jennifer H, Frisman Dennis, Pierce Robert, Weiner Russell, Wu Dianna, Emancipator Kenneth

机构信息

From the Departments of Molecular Biomarkers and Diagnostics (Drs Dolled-Filhart, Pierce, Weiner, Wu, and Emancipator) and Profiling and Expression (Dr Yearley), Merck & Co, Inc, Kenilworth, New Jersey; the Departments of Early Clinical & Translational Research, Clinical Histochemistry (Dr Locke), Research and Clinical Client Services (Dr Murphy), and Operations and Client Services (Dr Lynch), QualTek Molecular Laboratories, Newtown, Pennsylvania; and the Department of Pathology, Eisenhower Medical Center, Rancho Mirage, California (Dr Frisman). Dr Locke is now with Bristol-Myers Squibb, Princeton, New Jersey; Dr Pierce is now with OncoSec Medical, Inc, San Diego, California; Dr Weiner is now with Daiichi Sankyo, Edison, New Jersey; and Dr Wu is currently at Janssen Research & Development, Spring House, Pennsylvania.

出版信息

Arch Pathol Lab Med. 2016 Nov;140(11):1259-1266. doi: 10.5858/arpa.2015-0544-OA.

DOI:10.5858/arpa.2015-0544-OA
PMID:27788043
Abstract

CONTEXT

  • With the abundance of therapeutics targeted against programmed death receptor-1 and its ligand (PD-L1) that are currently approved or in clinical development, there is interest in identifying those patients most likely to respond to these drugs. Expression of PD-L1 may be an indicator of an initial and robust inflammatory response to the presence of tumor cells. Therefore, tumors that express PD-L1 may be the most likely to respond to therapies that interrupt the negative feedback mechanism that leads to PD-L1 upregulation.

OBJECTIVE

  • To develop a prototype immunohistochemistry assay using the anti-PD-L1 antibody clone 22C3.

DESIGN

  • The assay was developed and optimized using commercially available reagents and archival tumor-bank tissue.

RESULTS

  • The optimized immunohistochemistry method had high precision and reproducibility. Using the prototype assay in 142 non-small cell lung cancer and 79 melanoma archival tumor-bank tissue samples, PD-L1 staining was observed at the plasma membrane of nucleated tumor and nontumor cells and, in some cases, as a distinct lichenoid pattern at the tumor-stroma border. Using a preliminary scoring method, 56% (80 of 142) of non-small cell lung cancer and 53% (42 of 79) of melanoma samples were defined as PD-L1 based on a modified H-score of 1 or more or the presence of a distinctive staining pattern at the tumor-stroma interface.

CONCLUSIONS

  • The immunohistochemistry assay using the anti-PD-L1 antibody 22C3 merits further investigation in clinical trials and prevalence assessments to further understand the prognostic and predictive value of PD-L1 expression in cancer.
摘要

背景

  • 鉴于目前已获批或正在临床开发的大量针对程序性死亡受体-1及其配体(PD-L1)的治疗药物,人们对确定最有可能对这些药物产生反应的患者很感兴趣。PD-L1的表达可能是对肿瘤细胞存在的初始且强烈炎症反应的一个指标。因此,表达PD-L1的肿瘤可能最有可能对中断导致PD-L1上调的负反馈机制的治疗产生反应。

目的

  • 开发一种使用抗PD-L1抗体克隆22C3的免疫组织化学检测原型。

设计

  • 使用市售试剂和存档肿瘤库组织开发并优化该检测方法。

结果

  • 优化后的免疫组织化学方法具有高精确度和可重复性。在142例非小细胞肺癌和79例黑色素瘤存档肿瘤库组织样本中使用该检测原型,在有核肿瘤细胞和非肿瘤细胞的质膜上观察到PD-L1染色,在某些情况下,在肿瘤-基质边界呈现出独特的苔藓样模式。使用初步评分方法,基于改良的H评分1或更高或肿瘤-基质界面存在独特染色模式,142例非小细胞肺癌样本中的56%(80例)和79例黑色素瘤样本中的53%(42例)被定义为PD-L1阳性。

结论

  • 使用抗PD-L1抗体22C3的免疫组织化学检测在临床试验和患病率评估中值得进一步研究,以进一步了解PD-L1表达在癌症中的预后和预测价值。

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