posted on 2024-09-04, 07:41authored bySean R. Corcoran, James D. Phelan, Jaewoo Choi, Galina Shevchenko, Rachel E. Fenner, Xin Yu, Sebastian Scheich, Tony Hsiao, Vivian M. Morris, Evangelia K. Papachristou, Kamal Kishore, Clive S. D’Santos, Yanlong Ji, Stefania Pittaluga, George W. Wright, Henning Urlaub, Kuan-Ting Pan, Thomas Oellerich, Jagan Muppidi, Daniel J. Hodson, Louis M. Staudt
Knockout of Klhl6 in mouse germinal center B cells increases surface BCR expression
Funding
Cancer Research UK (CRUK)
Wellcome - MRC Cambridge Stem Cell Institute, University of Cambridge
Cancer Research UK Cambridge Institute, University of Cambridge (CRUK CI)
NIHR Cambridge Biomedical Research Centre (NIHR Cambridge BRC)
Intramural Research Program (IRP)
Deutsche Forschungsgemeinschaft (DFG)
History
ARTICLE ABSTRACT
Polatuzumab vedotin (Pola-V) is an antibody–drug conjugate directed to the CD79B subunit of the B-cell receptor (BCR). When combined with conventional immunochemotherapy, Pola-V improves outcomes in diffuse large B-cell lymphoma (DLBCL). To identify determinants of Pola-V sensitivity, we used CRISPR-Cas9 screening for genes that modulated Pola-V toxicity for lymphomas or the surface expression of its target, CD79B. Our results reveal the striking impact of CD79B glycosylation on Pola-V epitope availability on the lymphoma cell surface and on Pola-V toxicity. Genetic, pharmacological, and enzymatic approaches that remove sialic acid from N-linked glycans enhanced lymphoma killing by Pola-V. Pola-V toxicity was also modulated by KLHL6, an E3 ubiquitin ligase that is recurrently inactivated in germinal center derived lymphomas. We reveal how KLHL6 targets CD79B for degradation in normal and malignant germinal center B cells, thereby determining expression of the surface BCR complex. Our findings suggest precision medicine strategies to optimize Pola-V as a lymphoma therapeutic.Significance: These findings unravel the molecular basis of response heterogeneity to Pola-V and identify approaches that might be deployed therapeutically to enhance the efficacy of CD79B-specific tumor killing. In addition, they reveal a novel post-translational mechanism used by normal and malignant germinal center B cells to regulate expression of the BCR.See related commentary by Leveille, p. 1577See related article by Meriranta et al.