Cross center single-cell RNA sequencing study of the immune microenvironment in rapid progressing multiple myeloma

被引:17
|
作者
Pilcher, William [1 ,2 ]
Thomas, Beena E. [1 ,3 ]
Bhasin, Swati S. [1 ,3 ]
Jayasinghe, Reyka G. [4 ]
Yao, Lijun [4 ]
Gonzalez-Kozlova, Edgar [5 ,6 ]
Dasari, Surendra [7 ]
Kim-Schulze, Seunghee [5 ,8 ]
Rahman, Adeeb [5 ,6 ]
Patton, Jonathan [1 ]
Fiala, Mark [4 ]
Cheloni, Giulia [9 ]
Kourelis, Taxiarchis [10 ]
Dhodapkar, Madhav V. [11 ,12 ]
Vij, Ravi [13 ]
Mehr, Shaadi [14 ]
Hamilton, Mark [14 ]
Cho, Hearn Jay [5 ,14 ]
Auclair, Daniel [14 ]
Avigan, David E. [9 ]
Kumar, Shaji K. [10 ]
Gnjatic, Sacha [5 ,8 ]
Ding, Li [4 ]
Bhasin, Manoj [1 ,2 ,3 ,12 ,15 ]
机构
[1] Aflac Canc & Blood Disorders Ctr, Atlanta, GA 30322 USA
[2] Emory Univ, Coulter Dept Biomed Engn, Atlanta, GA 30322 USA
[3] Emory Sch Med, Dept Pediat, Atlanta, GA 30307 USA
[4] Washington Univ, Dept Med, Sch Med, St Louis, MO USA
[5] Icahn Sch Med Mt Sinai, Human Immune Monitoring Ctr, New York, NY USA
[6] Icahn Sch Med Mt Sinai, Dept Genet & Genom Sci, New York, NY USA
[7] Mayo Clin, Dept Quantitat Hlth Sci, Div Biomed Stat & Informat, Rochester, MN USA
[8] Icahn Sch Med Mt Sinai, Dept Oncol Sci, New York, NY USA
[9] Harvard Med Sch, Beth Israel Deaconess Med Ctr, Boston, MA USA
[10] Mayo Clin Rochester, Div Hematol, Rochester, MN USA
[11] Emory Univ, Dept Hematol Med Oncol, Sch Med, Atlanta, GA USA
[12] Emory Univ, Winship Canc Inst, Atlanta, GA 30322 USA
[13] Washington Univ, Sch Med, St Louis, MO USA
[14] Multiple Myeloma Res Fdn MMRF, Norwalk, CT USA
[15] Emory Sch Med, Dept Biomed Informat, Atlanta, GA 30307 USA
关键词
BONE-MARROW MICROENVIRONMENT; PLASMA-CELLS; PATHWAY; GROWTH; EXPRESSION; ATACICEPT; ADHESION; BAFF;
D O I
10.1038/s41525-022-00340-x
中图分类号
Q3 [遗传学];
学科分类号
071007 ; 090102 ;
摘要
Despite advancements in understanding the pathophysiology of Multiple Myeloma (MM), the cause of rapid progressing disease in a subset of patients is still unclear. MM's progression is facilitated by complex interactions with the surrounding bone marrow (BM) cells, forming a microenvironment that supports tumor growth and drug resistance. Understanding the immune microenvironment is key to identifying factors that promote rapid progression of MM. To accomplish this, we performed a multi-center single-cell RNA sequencing (scRNA-seq) study on 102,207 cells from 48 CD138(-) BM samples collected at the time of disease diagnosis from 18 patients with either rapid progressing (progression-free survival (PFS) < 18 months) or non-progressing (PFS > 4 years) disease. Comparative analysis of data from three centers demonstrated similar transcriptome profiles and cell type distributions, indicating subtle technical variation in scRNA-seq, opening avenues for an expanded multicenter trial. Rapid progressors depicted significantly higher enrichment of GZMK(+) and TIGIT(+) exhausted CD8(+) T-cells (P = 0.022) along with decreased expression of cytolytic markers (PRF1, GZMB, GNLY). We also observed a significantly higher enrichment of M2 tolerogenic macrophages in rapid progressors and activation of pro-proliferative signaling pathways, such as BAFF, CCL, and IL16. On the other hand, non-progressive patients depicted higher enrichment for immature B Cells (i.e., Pre/Pro B cells), with elevated expression for markers of B cell development (IGLL1, SOX4, DNTT). This multi-center study identifies the enrichment of various pro-tumorigenic cell populations and pathways in those with rapid progressing disease and further validates the robustness of scRNA-seq data generated at different study centers.
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页数:18
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