生物
巨噬细胞
细胞生物学
细胞
计算生物学
遗传学
体外
作者
Laura Amaya,Brian T. Abe,Deyong Xiao,Feifei Zhao,Wenyan Lucy Zhang,Robert Chen,Rui Li,Steven Wang,Roarke A. Kamber,Miao-Chih Tsai,Michael C. Bassik,Ravindra Majeti,Howard Y. Chang
出处
期刊:Molecular Cell
[Elsevier]
日期:2024-05-17
卷期号:84 (11): 2104-2118.e6
标识
DOI:10.1016/j.molcel.2024.04.022
摘要
Circular RNAs (circRNAs) are stable RNAs present in cell-free RNA, which may comprise cellular debris and pathogen genomes. Here, we investigate the phenomenon and mechanism of cellular uptake and intracellular fate of exogenous circRNAs. Human myeloid cells and B cells selectively internalize extracellular circRNAs. Macrophage uptake of circRNA is rapid, energy dependent, and saturable. CircRNA uptake can lead to translation of encoded sequences and antigen presentation. The route of internalization influences immune activation after circRNA uptake, with distinct gene expression programs depending on the route of RNA delivery. Genome-scale CRISPR screens and chemical inhibitor studies nominate macrophage scavenger receptor MSR1, Toll-like receptors, and mTOR signaling as key regulators of receptor-mediated phagocytosis of circRNAs, a dominant pathway to internalize circRNAs in parallel to macropinocytosis. These results suggest that cell-free circRNA serves as an "eat me" signal and danger-associated molecular pattern, indicating orderly pathways of recognition and disposal.
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