Phenotypic diversity of less predominant B-lineage clones.

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Pathogenesis beyond the cancer clone(s) in multiple myeloma by Giada Bianchi, and Nikhil C. Munshi Blood Volume 125(20): May 14, 2015 ©2015 by.

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IL32 prompts cell activation and cancer-related pathways.

Tfr cells’ transcriptomic profile distinguishes them from Treg and Tfh cells. Tfr cells’ transcriptomic profile distinguishes them from Treg and Tfh cells.

PD-1–PD-L1 axis is highly expressed and is not IFNγ-dependent in a subcutaneous murine model of PDA. A, experimental design for establishment of subcutaneous.

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Quantification of MHC-I, β2m, and T-cell subsets.

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Changes throughout time in the lineage content of clones regenerated in secondary mice. Changes throughout time in the lineage content of clones regenerated.

Kinetics of clone appearance, size, persistence, and lineage content.

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Relationship between blood cell and plasma miRNA expression among published circulating cancer biomarkers. Relationship between blood cell and plasma miRNA.

The TSDR of ATL cells exhibits Treg-like hypomethylated status or CD4+ conventional T cell–like methylated status. The TSDR of ATL cells exhibits Treg-like.

Frequency and kinetics of killer cell apoptosis are dependent on functional conjugations with multiple NALM-6 tumor cells. Frequency and kinetics of killer.

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Combined BRAFi and anti-CTLA4 administration leads to prolonged antitumor immunity in a patient with metastatic melanoma. Combined BRAFi and anti-CTLA4.

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Phenotypic diversity of individual multiple myeloma clones.

Convergent expansion in less predominant B-lineage clones.

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Immunological effects of anticancer therapy.

Expression of the angiogenic phenotype in the 4-NQO mouse model of HNSCC. A, tissue sections containing areas of normal, hyperkeratosis, dysplasia, and.

Technology schematic for phenotypic tracking of single molecularly defined B-lineage clones. Technology schematic for phenotypic tracking of single molecularly.

Characteristic gene expression patterns distinguish LCH cells from other immune cells present in LCH lesions. Characteristic gene expression patterns distinguish.

Varying the MHC-I affinity, TCR affinity or antigen dose alters the phenotype of CD8 T cells ex vivo. Varying the MHC-I affinity, TCR affinity or antigen.

Phenotyping of T cells. Phenotyping of T cells. Circulating lymphocytes from a tumor-naïve C57BL/6 mice (left column) were compared with those from C57BL/6.

RIL21 and checkpoint blockade restore IFNγ production in Tim-3+PD-1+ intratumoral NK cells from cancer patients. rIL21 and checkpoint blockade restore.

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Presentation transcript:

Phenotypic diversity of less predominant B-lineage clones. Phenotypic diversity of less predominant B-lineage clones. Immune phenotypes of cells of less predominant clones (in black) were visualized. The areas presumably representing physiologic and/or malignant plasma cell phenotypes are circled in blue. While cells of the second predominant clone of multiple myeloma 2 (A) colocalize with normal-phenotype B lymphocytes, cells of the second and third predominant clones in multiple myeloma 3 (B) map to areas that have been shown to be occupied with multiple myeloma cells in Fig. 3. See Supplementary Fig. S6 for detailed immune phenotypes. Leo Hansmann et al. Cancer Immunol Res 2017;5:744-754 ©2017 by American Association for Cancer Research