B cell–based therapy produces antibodies that inhibit glioblastoma growth
Si Wang, … , Mariafausta Fischietti, Catalina Lee-Chang
Si Wang, … , Mariafausta Fischietti, Catalina Lee-Chang
Published August 29, 2024
Citation Information: J Clin Invest. 2024;134(20):e177384. https://doi.org/10.1172/JCI177384.
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Research Article Immunology Oncology

B cell–based therapy produces antibodies that inhibit glioblastoma growth

Abstract

Glioblastoma (GBM) is a highly aggressive and malignant brain tumor with limited therapeutic options and a poor prognosis. Despite current treatments, the invasive nature of GBM often leads to recurrence. A promising alternative strategy is to harness the potential of the immune system against tumor cells. Our previous data showed that the BVax (B cell–based vaccine) can induce therapeutic responses in preclinical models of GBM. In this study, we aimed to characterize the antigenic reactivity of BVax-derived Abs and evaluate their therapeutic potential. We performed immunoproteomics and functional assays in murine models and samples from patients with GBM. Our investigations revealed that BVax distributed throughout the GBM tumor microenvironment and then differentiated into Ab-producing plasmablasts. Proteomics analyses indicated that the Abs produced by BVax had unique reactivity, predominantly targeting factors associated with cell motility and the extracellular matrix. Crucially, these Abs inhibited critical processes such as GBM cell migration and invasion. These findings provide valuable insights into the therapeutic potential of BVax-derived Abs for patients with GBM, pointing toward a novel direction for GBM immunotherapy.

Authors

Si Wang, Brandyn A. Castro, Joshua L. Katz, Victor Arrieta, Hinda Najem, Gustavo I. Vazquez-Cervantes, Hanxiao Wan, Ian E. Olson, David Hou, Mark Dapash, Leah K. Billingham, Tzu-yi Chia, Chao Wei, Aida Rashidi, Leonidas C. Platanias, Kathleen McCortney, Craig M. Horbinski, Roger Stupp, Peng Zhang, Atique U. Ahmed, Adam M. Sonabend, Amy B. Heimberger, Maciej S. Lesniak, Cécile Riviere-Cazaux, Terry Burns, Jason Miska, Mariafausta Fischietti, Catalina Lee-Chang

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Figure 3

Production of BVax-derived Igs in patients with GBM.

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Production of BVax-derived Igs in patients with GBM. (A) Schema of the e...
(A) Schema of the ex vivo generation of GBM patient BVax-derived Abs. (B) Dot plots of flow cytometric analysis of CD20 and CD38 expression during different stages in the BVax activation protocol to generate GBM patient–derived Abs ex vivo. (C) Box-and-whisker plot of the percentage of plasmablasts generated at day 10 of BVax/BNaive activation in patients with GBM (n = 5 for each group). (D) Western blot confirming the presence of Abs in the media during various stages of the ex vivo BVax activation protocol for patients with GBM. EM, expansion medium; BCS, B cell supplement. Data in C are the mean ± SD and were analyzed by 2-tailed Student’s t test.