TRIP13 modulates protein deubiquitination and accelerates tumor development and progression of B cell malignancies
Can Li, … , Ivana Frech, Fenghuang Zhan
Can Li, … , Ivana Frech, Fenghuang Zhan
Published June 1, 2021
Citation Information: J Clin Invest. 2021;131(14):e146893. https://doi.org/10.1172/JCI146893.
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TRIP13 modulates protein deubiquitination and accelerates tumor development and progression of B cell malignancies

Abstract

Multiple myeloma (MM), a terminally differentiated B cell malignancy, remains difficult to cure. Understanding the molecular mechanisms underlying the progression of MM may identify therapeutic targets and lead to a fundamental shift in treatment of the disease. Deubiquitination, like ubiquitination, is a highly regulated process, implicated in almost every cellular process. Multiple deubiquitinating enzymes (DUBs) have been identified, but their regulation is poorly defined. Here, we determined that TRIP13 increases cellular deubiquitination. Overexpression of TRIP13 in mice and cultured cells resulted in excess cellular deubiquitination by enhancing the association of the DUB USP7 with its substrates. We show that TRIP13 is an oncogenic protein because it accelerates B cell tumor development in transgenic mice. TRIP13-induced resistance to proteasome inhibition can be overcome by a USP7 inhibitor in vitro and in vivo. These findings suggest that TRIP13 expression plays a critical role in B cell lymphoma and MM by regulating deubiquitination of critical oncogenic (NEK2) and tumor suppressor (PTEN, p53) proteins. High TRIP13 identifies a high-risk patient group amenable to adjuvant anti-USP7 therapy.

Authors

Can Li, Jiliang Xia, Reinaldo Franqui-Machin, Fangping Chen, Yanjuan He, Timothy Cody Ashby, Feixiang Teng, Hongwei Xu, Dingxiao Liu, Dongzheng Gai, Sarah K. Johnson, Frits van Rhee, Siegfried Janz, John D. Shaughnessy Jr., Guido Tricot, Ivana Frech, Fenghuang Zhan

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Figure 2

TRIP13 enhances cellular protein deubiquitination.

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TRIP13 enhances cellular protein deubiquitination. (A–C) Representationa...
(AC) Representational and pathway analysis of approximately 1900 differentially expressed genes in B cells from Eμ-Myc/Trip13TG versus Eμ-Myc/Trip13WT mice (P < 0.001) displayed in volcano plot (A) and bar graphs of GO terms (B) and KEGG pathways (C). Ubiquitin-related (Ub-related) and proteasome-related terms or pathways are indicated by red arrows. (D) Western blot analysis of Ub, TRIP13, and β-actin in EV and TRIP13-OE ARP1 cells treated overnight with or without 10 nM BTZ. (E) Western blot analysis of Ub, TRIP13, and GAPDH in ARP1 cells transfected with a doxycycline-inducible (DOX-inducible) TRIP13 shRNA, treated with or without DOX for 72 hours, followed by treatment with or without 10 nM BTZ. (F) Western blot analysis of Ub, Trip13, and Gapdh in thymus (T) and spleen (S) from Trip13TG and Trip13WT mice.