| Literature DB >> 29031828 |
Jeff DeFalco1, Michael Harbell1, Amy Manning-Bog1, Gilson Baia1, Alexander Scholz1, Beatriz Millare1, May Sumi1, Danhui Zhang1, Felix Chu1, Christine Dowd1, Patricia Zuno-Mitchell1, Dongkyoon Kim1, Yvonne Leung1, Shuwei Jiang1, Xiaobin Tang1, Kevin S Williamson1, Xiaomu Chen1, Sean M Carroll1, Gregg Espiritu Santo1, Nicole Haaser1, Ngan Nguyen1, Eldar Giladi1, David Minor2, Yann Chong Tan3, Jeremy B Sokolove4, Lawrence Steinman5, Tito A Serafini1, Guy Cavet1, Norman M Greenberg1, Jacob Glanville6, Wayne Volkmuth1, Daniel E Emerling7, William H Robinson8.
Abstract
There is significant debate regarding whether B cells and their antibodies contribute to effective anti-cancer immune responses. Here we show that patients with metastatic but non-progressing melanoma, lung adenocarcinoma, or renal cell carcinoma exhibited increased levels of blood plasmablasts. We used a cell-barcoding technology to sequence their plasmablast antibody repertoires, revealing clonal families of affinity matured B cells that exhibit progressive class switching and persistence over time. Anti-CTLA4 and other treatments were associated with further increases in somatic hypermutation and clonal family size. Recombinant antibodies from clonal families bound non-autologous tumor tissue and cell lines, and families possessing immunoglobulin paratope sequence motifs shared across patients exhibited increased rates of binding. We identified antibodies that caused regression of, and durable immunity toward, heterologous syngeneic tumors in mice. Our findings demonstrate convergent functional anti-tumor antibody responses targeting public tumor antigens, and provide an approach to identify antibodies with diagnostic or therapeutic utility.Entities:
Mesh:
Substances:
Year: 2017 PMID: 29031828 DOI: 10.1016/j.clim.2017.10.002
Source DB: PubMed Journal: Clin Immunol ISSN: 1521-6616 Impact factor: 3.969