Illumina HiSeq 2500 sequencing; GSM1923445: Single_cell_RNA-seq_NKT0_1; Mus musculus; RNA-Seq

Single_cell_RNA-seq_NKT0_1

Natural killer T (NKT) cells have immune stimulatory or inhibitory effects on the immune response that are context-dependent.  This may be attributed in part to the existence of functional NKT cell subsets; however, these functional subsets have only been characterized on the basis of differential expression of a few transcription factors and cell surface molecules.  Here we have analyzed purified populations of thymic NKT cell subsets at both the transcriptomic and epigenomic levels, and by single-cell RNA sequencing.  Our data indicate that despite their similar antigen specificity, the functional NKT cell subsets are highly divergent populations characterized by many gene expression and epigenetic differences.  Therefore the thymus imprints innate-like NKT cells with novel combinations of properties, including differences in proliferative capacity, homing, and effector functions that were not previously anticipated. Overall design: Analysis of single cell transcriptomic heterogeneity in mouse Va14 iNKT thymocyte subsets (NKT1, NKT2, NKT17 and NKT0). Samples were generated from individual experiment using a pool of thymocytes prepared from five five-week old C57BL/6J females. NKT cells subtypes were isolated from thymuses and directly sorted by flow cytometry into lysis buffer (96 well plate single cell sort). The preparation of samples occurred in 2 different batches (both having a equal representation of the different cell populations).

Innate-like functions of natural killer T cell subsets result from highly divergent gene programs [single_cell_RNA-seq]

Submitted by Gene Expression Omnibus on 19-APR-2016

For RNA isolation from thymic iNKT cell subsets, thymus cell suspensions were enriched for iNKT cells by negative selection of cells expressing CD8b.2, CD19 or TER-119 via magnetic selection utilizing reagents and equipment from Stem Cell Technologies. The remaining cells were then stained using an 11-parameter panel of reagents that included tetramers of CD1d loaded with either aGalcer or PBS57 combined with streptavidin-brilliant violet (BV)421 (produced in-house or obtained from the NIH Tetramer Core Facility), anti-CD44-V500 (BD Biosciences #56780), live/dead yellow (ThermoFisher Scientific #L34959), anti-CD4-Qdot 605 (ThermoFisher Scientific #Q10092), anti-CD103-FITC (Affymetrix #11-1031), anti-CD24-PerCPCy5.5 (Affymetrix #45-0242), anti-CD27-APC (Affymetrix #E07114), anti-CD8a-AF700 (Biolegend 100730), anti-TCRb-APC-eF780 (Affymetrix #47-5961), anti-CCR6-PE (Biolegend #129803), and anti-NK1.1-PE-Cy7 (BD Biosciences #552878).  iNKT subsets were sorted using a FACSaria III (BD Biosciences). Single cell RNAseq was perfromed as described in Picelli et al.Nat Protoc. 2014, PMID:24385147. We performed 22 cycles of amplification. Single cell RNAseq was perfromed as described in Picelli et al.Nat Protoc. 2014, PMID:24385147. Barcoded Illumina sequencing libraries (Nextera XT library preparation kit, Illumina) Whole Transcriptome Amplification (SmartSeq2 - Picelli et al.2014); Libraries were sequenced on the HiSeq2500 Illumina platform to obtain 50-bp single end reads (TruSeqÂ® Rapid Kit, Illumina).

Innate-like functions of natural killer T cell subsets result from highly divergent gene programs [single_cell_RNA-seq]

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