Zheng Ma scite author profile

SummaryMultiple myeloma (MM) evolves from a highly prevalent premalignant condition termed MGUS. The factors underlying the malignant transformation of MGUS are unknown. We report a MGUS/MM phenotype in transgenic mice with Eμ-directed expression of the XBP-1 spliced isoform (XBP-1s), a factor governing unfolded protein/ER stress response and plasma-cell development. Eμ-XBP-1s elicited elevated serum Ig and skin alterations. With age, Eμ-xbp-1s transgenics develop features diagnostic of human MM, including bone lytic lesions and subendothelial Ig deposition. Furthermore, transcriptional profiles of Eμ-xbp-1s lymphoid and MM cells show aberrant expression of known human MM dysregulated genes. The similarities of this model with the human disease, coupled with documented frequent XBP-1s overexpression in human MM, serve to implicate XBP-1s dysregulation in MM pathogenesis.

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Full-Duplex Device-to-Device Aided Cooperative Non-Orthogonal Multiple Access

Zhang

Xiao

et al. 2016

IEEE Trans. Veh. Technol.

295

265

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Targeting the β-catenin/TCF transcriptional complex in the treatment of multiple myeloma

Sukhdeo

Mani²,

Zhang³

et al. 2007

Proc. Natl. Acad. Sci. U.S.A.

201

200

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Zheng Ma

6G Wireless Networks: Vision, Requirements, Architecture, and Key Technologies

The Differentiation and Stress Response Factor XBP-1 Drives Multiple Myeloma Pathogenesis

Full-Duplex Device-to-Device Aided Cooperative Non-Orthogonal Multiple Access

Targeting the β-catenin/TCF transcriptional complex in the treatment of multiple myeloma

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