细胞生物学
流式细胞术
CD24型
刺激
B细胞
细胞
受体
化学
微泡
胞外囊泡
B细胞受体
CD40
生物
分子生物学
免疫学
微泡
干细胞
细胞毒性T细胞
体外
抗体
生物化学
小RNA
内分泌学
癌症干细胞
基因
作者
Hong‐Dien Phan,Modeline N. Longjohn,Delania J B Gormley,Reilly H. Smith,May Dang-Lawson,Linda Matsuuchi,Michael R. Gold,Sherri L. Christian
出处
期刊:Journal of Immunology
[American Association of Immunologists]
日期:2021-11-12
卷期号:207 (12): 3004-3015
被引量:15
标识
DOI:10.4049/jimmunol.2100025
摘要
Abstract Extracellular vesicles (EVs) are membrane-encapsulated nanoparticles that carry bioactive cargo, including proteins, lipids, and nucleic acids. Once taken up by target cells, EVs can modify the physiology of the recipient cells. In past studies, we reported that engagement of the glycophosphatidylinositol-anchored receptor CD24 on B lymphocytes (B cells) causes the release of EVs. However, a potential function for these EVs was not clear. Thus, we investigated whether EVs derived from CD24 or IgM-stimulated donor WEHI-231 murine B cells can transfer functional cargo to recipient cells. We employed a model system where donor cells expressing palmitoylated GFP (WEHI-231-GFP) were cocultured, after stimulation, with recipient cells lacking either IgM (WEHI-303 murine B cells) or CD24 (CD24 knockout mouse bone marrow B cells). Uptake of lipid-associated GFP, IgM, or CD24 by labeled recipient cells was analyzed by flow cytometry. We found that stimulation of either CD24 or IgM on the donor cells caused the transfer of lipids, CD24, and IgM to recipient cells. Importantly, we found that the transferred receptors are functional in recipient cells, thus endowing recipient cells with a second BCR or sensitivity to anti-CD24–induced apoptosis. In the case of the BCR, we found that EVs were conclusively involved in this transfer, whereas in the case in the CD24 the involvement of EVs is suggested. Overall, these data show that extracellular signals received by one cell can change the sensitivity of neighboring cells to the same or different stimuli, which may impact B cell development or activation.
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