Targeting N-linked Glycosylation for the Therapy of Aggressive Lymphomas.

Sebastian Scheich ,Hang Nguyen ,Björn Häupl ,Jiamin Liu ,Thomas Oellerich ,Hong Zhao ,Sean Corcoran ,Tony Hsiao ,Frank Schnütgen ,Xin Yu ,Yanlong Ji ,Da Wei Huang ,Jaewoo Choi ,Weihong Xu ,Arnold Bolomsky ,Boya Wang ,Craig J Thomas ,Michele Ceribelli ,Kuan‐Ting Pan ,Ryan M Young ,George W Wright ,Henning Urlaub ,Jiji Chen ,James D Phelan ,Vivian Morris ,Yandan Yang ,Julius C Enßle ,Jagan R Muppidi ,Louis M Staudt

doi:10.1158/2159-8290.cd-22-1401

Abstract

DLBCL depends on constitutive BCR activation and signaling. There are currently no therapeutics that target the BCR directly and attenuate its pathologic signaling. Here, we unraveled a therapeutically exploitable, OST-B-dependent glycosylation pathway that drives BCR organization and proximal BCR signaling. This article is highlighted in the In This Issue feature, p. 1749.

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