Project description:BM-MSC-Derived Migrasomes Reverse Stroke-Induced Thymic Atrophy and Immunosuppression via Pin1 Delivery to Thymic Epithelial Cells

Project description:miRNA microarray was performed for migrasomes and exosomes derived from urine

Project description:Conventional anti-angiogenic drugs (AADs) combined with sorafenib have little success in HCC patients, as the formation of hypoxia areas in tumors and vasculogenic mimicry’s (VM's) non-responsiveness to AADs. Migrasomes are recently discovered extracellular vesicles produced during cell migration. In this study, the results show that hypoxia-induced migrasomes induce the formation of VM and promote the sorafenib resistance. Further studies reveal that hypoxia-induced migrasomes can be taken up by HCC cells via macropinocytosis, which activates PI3K/AKT/TWIST1 signaling. Moreover, CD147 on the surface of hypoxia-induced migrasomes is identified as a key protein in regulating the signaling pathway. Overall, our findings uncover a previously unrecognized mechanism mediated by hypoxia-induced migrasomes and the formation of VM and provide a new method for preventing SFR.

Project description:We report the application of migrasomes in wound healing process. ScRNA-seq was used to compare the differences in ctrl and mig group.

Project description:In the present study, we have documented a previously unrecognized membrane vesicles called “migrasomes” (M-mig) that originate from the filament-like nanotubes of macrophage.To characterize the signatures of macrophage migrasomes (M-mig) gene expression that might underlie M-mig-associated biological function. M0-mig, M1-mig, M2-mig and HG-mig genome-wide expression profiling was carried out by using SurePrint G3 Mouse GE V2.0 8X60K Microarrays (Design ID:074809, Agilent Technologies, USA). Total RNA was quantified by the NanoDrop ND-2000 (Thermo Scientific) and the RNA integrity was assessed using Agilent Bioanalyzer 2100 (Agilent Technologies). The sample labeling, microarray hybridization and washing were performed based on the manufacturer’s standard protocols. Briefly, total RNA was transcribed to double strand cDNA, then synthesized into cRNA and labeled with Cyanine-3-CTP. The labeled cRNAs were hybridized onto the microarray. After washing, the arrays were scanned by the Agilent Scanner G2505C (Agilent Technologies). For data analysis, Feature Extraction software (version10.7.1.1, Agilent Technologies) was used to analyze array images to get raw data. Genespring (version14.9, Agilent Technologies) were employed to finish the basic analysis with the raw data. To begin with, the raw data was normalized with the quantile algorithm. Differentially expressed genes were then identified through fold change. The threshold set for up- and down-regulated genes was a fold change>=2.0. Afterwards, GO analysis and KEGG analysis were applied to determine the roles of these differentially expressed mRNAs.

Project description:Migrasomes are recently identified vesicular organelles that form on retraction fibers behind migrating cells, cellular contents are released from migrasome by a process named migracytosis. The function of migrasomes in living organisms is unknown. Here we show that migrasomes are formed during zebrafish gastrulation, signaling molecules such as chemokines are enriched in migrasomes. Migrasomes are clustered on spatially restricted area in embryo where they provide regional cues for organ morphogenesis. Our study shown migrasome is signaling organelles which integrate spatial and specific biochemical information to coordinate migrating cells in complex biological processes such as morphogenesis.

Project description:Migrasomes are essential intermediates for intercellular communication, involved in critical processes such as embryonic development, angiogenesis, and blood coagulation. So far, a comprehensive understanding of the protein cargoes within migrasomes and their transport mechanisms, which is fundamental to advancing the understanding of migrasomes function, is still lacking. In this study, we investigated the Rab-mediated cargo transport network to migrasomes. Rabs selectively transported proteins to migrasomes that are enriched in intracellular vesicle trafficking pathways. By integrating migrasomes protein profiling and Rab-effectors under various Rab activations, we identified key driving proteins involved in Rab-mediated cargo delivery to migrasomes. Additionally, we uncovered and validated that Rabs transported plasma membrane-localized receptors and matrix metalloproteinase to migrasomes, providing new insights into their in vivo functions. The proteomic dataset and integrated approach can be applied in further investigation of migrasomes in both physiological and disease contexts.

Project description:Neutrophil-derived migrasomes are an essential part of the coagulation system, Tspan9

Project description:Neutrophil-derived migrasomes are an essential part of the coagulation system, human

Project description:Neutrophil-derived migrasomes are an essential part of the coagulation system, mouse.