Single-cell analysis of neoplastic plasma cells identifies myeloma pathobiology mediators and potential targets

多发性骨髓瘤 等离子体电池 浆细胞肿瘤 癌症研究 医学 浆细胞瘤 免疫学
作者
Luz Yurany Moreno Rueda,Hua Wang,Keiko Akagi,Minghao Dang,Amishi U. Vora,Qin Li,Hans C. Lee,Krina K. Patel,Pei Lin,David E. Mery,Fenghuang Zhan,John D. Shaughnessy,Qing Yi,Song Yang,Bo Jiang,Maura L. Gillison,Sheeba K. Thomas,Donna M. Weber,Lixia Diao,Jing Wang
出处
期刊:Cell reports medicine [Elsevier BV]
卷期号:: 101925-101925
标识
DOI:10.1016/j.xcrm.2024.101925
摘要

Multiple myeloma is a clonal plasma cell (PC) dyscrasia that arises from precursors and has been studied utilizing approaches focused on CD138+ cells. By combining single-cell RNA sequencing (scRNA-seq) with scB-cell receptor sequencing (scBCR-seq), we differentiate monoclonal/neoplastic from polyclonal/normal PCs and find more dysregulated genes, especially in precursor patients, than we would have by analyzing bulk PCs. To determine whether this approach can identify oncogenes that contribute to disease pathobiology, mitotic arrest deficient-2 like-1 (MAD2L1) and S-adenosylmethionine synthase isoform type-2 (MAT2A) are validated as targets with drug-like molecules that suppress myeloma growth in preclinical models. Moreover, functional studies show a role of lysosomal-associated membrane protein family member-5 (LAMP5), which is uniquely expressed in neoplastic PCs, in tumor progression and aggressiveness via interactions with c-MYC. Finally, a monoclonal antibody recognizing cell-surface LAMP5 shows efficacy as an antibody-drug conjugate and in a chimeric antigen receptor-guided T-cell format. These studies provide additional insights into myeloma biology and identify potential targeted therapeutic approaches that can be applied to reverse myeloma progression.
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