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SRX4704234: RNA-Seq of Mus musculus: adult female tumor associated macrophages isolated from CT26-Sg-Con tumors
1 BGISEQ (BGISEQ-500) run: 24.1M spots, 1.2G bases, 701.7Mb downloads

Design: For RNA sequencing, libraries were prepared using an MGIEasy mRNA kit and sequenced by a BGISEQ-500 instrument. Upon sequencing, raw FASTQ files were aligned using a HISAT aligner with default parameters. Aligned fragments were then counted and annotated using the Bowtie2 transcript database. Normalized RSEM were obtained.
Submitted by: Xinqiao hospitao, Chongqing,China
Study: Intracellular activation of complement C3 modulates tumor-associated macrophages polarization
show Abstracthide Abstract
Mounting evidence has highlighted the importance of complement in the construction of an immunosuppressive tumor microenvironment (TME). Tumor cell-derived C3 has been previously reported, however, whether and how it acts on anti-tumor immunity remains to be elucidated. Here, we describe a unique role of tumor cell-derived C3 in suppressing anti-tumor immunity. Tumor cell-derived C3 was activated intracellularly, which results in generation of C3a. C3a could modulate tumor-associated macrophages (TAMs) via C3a-C3aR-PI3K? signaling, thereby repressing anti-tumor immunity. More importantly, deletion of C3 in tumor cells with high C3 expression is sufficient to enhance the efficacy of ?PD-L1 treatment. Collectively, our present results suggest tumor cell derived C3 may serve as a novel target in cancer immunotherapy, specifically targeting C3 in tumor cells to enhance anti-tumor immunity.
Sample: Tumor asscociated macrophage_2
SAMN10075464 • SRS3790204 • All experiments • All runs
Organism: Mus musculus
Library:
Name: TAM_B
Instrument: BGISEQ-500
Strategy: RNA-Seq
Source: TRANSCRIPTOMIC
Selection: PCR
Layout: SINGLE
Runs: 1 run, 24.1M spots, 1.2G bases, 701.7Mb
Run# of Spots# of BasesSizePublished
SRR785357824,090,0671.2G701.7Mb2018-09-17

ID:
6370512

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