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Potent and broad HIV-neutralizing antibodies in memory B cells and plasma.记忆B细胞和血浆中强效且广谱的HIV中和抗体。
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Deep Sequencing of T-cell Receptor DNA as a Biomarker of Clonally Expanded TILs in Breast Cancer after Immunotherapy.深度测序 T 细胞受体 DNA 作为免疫治疗后乳腺癌中克隆扩增 TIL 的生物标志物。
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Tumor- and Neoantigen-Reactive T-cell Receptors Can Be Identified Based on Their Frequency in Fresh Tumor.肿瘤和新抗原反应性T细胞受体可根据其在新鲜肿瘤中的频率来识别。
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基于前哨淋巴结中的克隆频率鉴定乳腺癌中的肿瘤反应性 B 细胞和系统性 IgG。

Identification of tumor-reactive B cells and systemic IgG in breast cancer based on clonal frequency in the sentinel lymph node.

机构信息

Department of Chemical Engineering, The University of Texas at Austin, Austin, TX, USA.

Department of Surgery, Vermont Cancer Center, University of Vermont Larner College of Medicine, 89 Beaumont Avenue, Given Medical Building, Burlington, VT, 05405, USA.

出版信息

Cancer Immunol Immunother. 2018 May;67(5):729-738. doi: 10.1007/s00262-018-2123-2. Epub 2018 Feb 9.

DOI:10.1007/s00262-018-2123-2
PMID:29427082
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC6368991/
Abstract

A better understanding of antitumor immune responses is the key to advancing the field of cancer immunotherapy. Endogenous immunity in cancer patients, such as circulating anticancer antibodies or tumor-reactive B cells, has been historically yet incompletely described. Here, we demonstrate that tumor-draining (sentinel) lymph node (SN) is a rich source for tumor-reactive B cells that give rise to systemic IgG anticancer antibodies circulating in the bloodstream of breast cancer patients. Using a synergistic combination of high-throughput B-cell sequencing and quantitative immunoproteomics, we describe the prospective identification of tumor-reactive SN B cells (based on clonal frequency) and also demonstrate an unequivocal link between affinity-matured expanded B-cell clones in the SN and antitumor IgG in the blood. This technology could facilitate the discovery of antitumor antibody therapeutics and conceivably identify novel tumor antigens. Lastly, these findings highlight the unique and specialized niche the SN can fill in the advancement of cancer immunotherapy.

摘要

更好地了解抗肿瘤免疫反应是推进癌症免疫治疗领域的关键。癌症患者的内源性免疫,如循环抗癌抗体或肿瘤反应性 B 细胞,在历史上得到了描述,但并不完全。在这里,我们证明肿瘤引流(哨兵)淋巴结(SN)是肿瘤反应性 B 细胞的丰富来源,这些 B 细胞产生在乳腺癌患者血液中循环的全身性 IgG 抗癌抗体。我们使用高通量 B 细胞测序和定量免疫蛋白质组学的协同组合,描述了基于克隆频率的肿瘤反应性 SN B 细胞的前瞻性鉴定,并且还证明了 SN 中亲和力成熟的扩增 B 细胞克隆与血液中的抗肿瘤 IgG 之间存在明确的联系。该技术可以促进抗肿瘤抗体治疗药物的发现,并可以设想鉴定新的肿瘤抗原。最后,这些发现强调了 SN 在癌症免疫治疗进展中可以填补的独特和专门的利基。