Your search keyword '"Kuan-Ting Pan"' showing total 2 results

1. Rewiring of B cell receptor signaling by Epstein–Barr virus LMP2A.

Author

Fish, Kamonwan, Comoglio, Federico, Shaffer III, Arthur L., Yanlong Ji, Kuan-Ting Pan, Scheicha, Sebastian, Oellerich, Angelika, Doebele, Carmen, Masato Ikeda, Schaller, Samantha J., Hang Nguyen, Muppidi, Jagan, Wright, George W., Urlaub, Henning, Serve, Hubert, Staudt, Louis M., Longnecker, Richard, and Oellerich, Thomas

Subjects

B cell receptors, TUMOR suppressor proteins, EPSTEIN-Barr virus, B cells, MEMBRANE proteins

Abstract

Epstein–Barr virus (EBV) infects human B cells and reprograms them to allow virus replication and persistence. One key viral factor in this process is latent membrane protein 2A (LMP2A), which has been described as a B cell receptor (BCR) mimic promoting malignant transformation. However, how LMP2A signaling contributes to tumorigenesis remains elusive. By comparing LMP2A and BCR signaling in primary human B cells using phosphoproteomics and transcriptome profiling, we identified molecular mechanisms through which LMP2A affects B cell biology. Consistent with the literature, we found that LMP2A mimics a subset of BCR signaling events, including tyrosine phosphorylation of the kinase SYK, the calcium initiation complex consisting of BLNK, BTK, and PLCγ2, and its downstream transcription factor NFAT. However, the majority of LMP2A-induced signaling events markedly differed from those induced by BCR stimulation. These included differential phosphorylation of kinases, phosphatases, adaptor proteins, transcription factors such as nuclear factor κB (NF-κB) and TCF3, as well as widespread changes in the transcriptional output of LMP2Aexpressing B cells. LMP2A affected apoptosis and cell-cycle checkpoints by dysregulating the expression of apoptosis regulators such as BCl-xL and the tumor suppressor retinoblastoma-associated protein 1 (RB1). LMP2A cooperated with MYC and mutant cyclin D3, two oncogenic drivers of Burkitt lymphoma, to promote proliferation and survival of primary human B cells by counteracting MYCinduced apoptosis and by inhibiting RB1 function, thereby promoting cell-cycle progression. Our results indicate that LMP2A is not a pure BCR mimic but rather rewires intracellular signaling in EBVinfected B cells that optimizes cell survival and proliferation, setting the stage for oncogenic transformation. [ABSTRACT FROM AUTHOR]

Published

2020

2. Elucidation of tonic and activated B-cell receptor signaling in Burkitt's lymphoma provides insights into regulation of cell survival.

Author

Corso, Jasmin, Kuan-Ting Pan, Walter, Roland, Doebele, Carmen, Mohr, Sebastian, Bohnenberger, Hanibal, Ströbel, Philipp, Lenz, Christof, Slabicki, Mikolaj, Hüllein, Jennifer, Comoglio, Federico, Rieger, Michael A., Zenz, Thorsten, Wienands, Jürgen, Engelke, Michael, Serve, Hubert, Urlaub, Henning, and Oellerich, Thomas

Subjects

*CELL receptors, *B cells, *BURKITT'S lymphoma, *CELLULAR control mechanisms, *PHOSPHORYLATION, *THERAPEUTICS

Abstract

Burkitt's lymphoma (BL) is a highly proliferative B-cell neoplasm and is treated with intensive chemotherapy that, because of its toxicity, is often not suitable for the elderly or for patients with endemic BL in developing countries. BL cell survival relies on signals transduced by B-cell antigen receptors (BCRs). However, tonic as well as activated BCR signaling networks and their relevance for targeted therapies in BL remain elusive. We have systematically characterized and compared tonic and activated BCR signaling in BL by quantitative phosphoproteomics to identify novel BCR effectors and potential drug targets. We identified and quantified ∼16,000 phospho-sites in BL cells. Among these sites, 909 were related to tonic BCR signaling, whereas 984 phospho-sites were regulated upon BCR engagement. The majority of the identified BCR signaling effectors have not been described in the context of B cells or lymphomas yet. Most of these newly identified BCR effectors are predicted to be involved in the regulation of kinases, transcription, and cytoskeleton dynamics. Although tonic and activated BCR signaling shared a considerable number of effector proteins, we identified distinct phosphorylation events in tonic BCR signaling. We investigated the functional relevance of some newly identified BCR effectors and show that ACTN4 and ARFGEF2, which have been described as regulators of membrane-trafficking and cytoskeletonrelated processes, respectively, are crucial for BL cell survival. Thus, this study provides a comprehensive dataset for tonic and activated BCR signaling and identifies effector proteins that may be relevant for BL cell survival and thus may help to develop newBL treatments. [ABSTRACT FROM AUTHOR]

Published

2016