| Literature DB >> 32640012 |
Zhi Wen1, Adhithi Rajagopalan1, Evan D Flietner2, Grant Yun1, Marta Chesi3, Quinlan Furumo4, Robert T Burns4, Athanasios Papadas5, Erik A Ranheim2, Adam C Pagenkopf5, Zachary T Morrow5, Remington Finn1, Yun Zhou1, Shuyi Li1, Xiaona You1, Jeffrey Jensen5, Mei Yu6, Alexander Cicala5, James Menting5, Constantine S Mitsiades7, Natalie S Callander5, P Leif Bergsagel3, Demin Wang4,6, Fotis Asimakopoulos5, Jing Zhang1.
Abstract
NRAS Q61 mutations are prevalent in advanced/relapsed multiple myeloma (MM) and correlate with poor patient outcomes. Thus, we generated a novel MM model by conditionally activating expression of endogenous NrasQ61R and an MYC transgene in germinal center (GC) B cells (VQ mice). VQ mice developed a highly malignant MM characterized by a high proliferation index, hyperactivation of extracellular signal-regulated kinase and AKT signaling, impaired hematopoiesis, widespread extramedullary disease, bone lesions, kidney abnormalities, preserved programmed cell death protein 1 and T-cell immunoreceptor with immunoglobulin and immunoreceptor tyrosine-based inhibition motif domain immune-checkpoint pathways, and expression of human high-risk MM gene signatures. VQ MM mice recapitulate most of the biological and clinical features of human advanced/high-risk MM. These MM phenotypes are serially transplantable in syngeneic recipients. Two MM cell lines were also derived to facilitate future genetic manipulations. Combination therapies based on MEK inhibition significantly prolonged the survival of VQ mice with advanced-stage MM. Our study provides a strong rationale to develop MEK inhibition-based therapies for treating advanced/relapsed MM.Entities:
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Year: 2021 PMID: 32640012 PMCID: PMC7808014 DOI: 10.1182/blood.2020007156
Source DB: PubMed Journal: Blood ISSN: 0006-4971 Impact factor: 25.476