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Joost Willebrords Michaël Maes Isabel Veloso Alves Pereira Tereza Cristina da Silva Veronica Mollica Govoni Valéria Veras Lopes Sara Crespo Yanguas Valery I. Shestopalov Marina Sayuri Nogueira Inar Alves de Castro Anwar Farhood Inge Mannaerts Leo van Grunsven Jephte Akakpo Margitta Lebofsky Hartmut Jaeschke Bruno Cogliati Mathieu Vinken 《生物化学与生物物理学报:疾病的分子基础》2018,1864(3):819-830
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目的:在建立高纯度小鼠肝血窦内皮细胞的体外培养的基础上研究γ分泌酶抑制剂(DAPT)对肝血窦内皮细胞活性的影响.方法:首先通过胶原酶灌注消化、percoll梯度离心和选择性贴壁分离得到高纯度、可在体外条件下培养的肝血窦内皮细胞,其次用不同浓度的DAPT(15 μmol/L、45 μmol/L、75 μmol/L)处理细胞,然后通过MTT检测细胞增殖情况、Real time PCR检测相关分子改变.结果:在体外条件下DAPT对肝血窦内皮细胞的增殖起到促进作用,这种促进作用随着DAPT浓度的增加相应的增加;DAPT能够导致肝血窦内皮细胞Notch信号下游分子Hes1表达下调,VEGF信号中VEGFR1表达下调,VEGFR2表达上调.结论:γ分泌酶抑制剂(DAPT)通过抑制肝血窦内皮细胞Notch信号,引起肝血窦内皮细胞表面VEGFR1表达下调,VEGFR2 表达上调显著增加肝血窦内皮细胞的活性. 相似文献
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Foteini Kiagiadaki Marilena Kampa Argyro Voumvouraki Elias Castanas Elias Kouroumalis George Notas 《生物化学与生物物理学报:疾病的分子基础》2018,1864(3):891-899
Background & aims
TGFβ superfamily member Activin-A is a multifunctional hormone/cytokine expressed in multiple tissues and cells, where it regulates cellular differentiation, proliferation, inflammation and tissue architecture. High activin-A levels have been reported in alcoholic cirrhosis and non-alcoholic steatohepatitis (NASH). Our aim was to identify the cell types involved in the fibrotic processes induced by activin-A in liver and verify the liver diseases that this molecule can be found increased.Methods
We studied the effect of activin-A on mouse primary Kupffer cells (KCs) and Hepatic Stellate cells (HSCs) and the levels of activin-A and its inhibitor follistatin in the serum of patients from a large panel of liver diseases.Results
Activin-A is expressed by mouse hepatocytes, HSCs and Liver Sinusoid Endothelial cells but not KCs. Each cell type expresses different activin receptor combinations. HSCs are unresponsive to activin-A due to downregulation/desensitization of type-II activin receptors, while KCs respond by increasing the expression/production of TNFα και TGFβ1. In the presence of KCs or conditioned medium from activin-A treated KCs, HSCs switch to a profibrogenic phenotype, including increased collagen and αSMA expression and migratory capacity. Incubation of activin-A treated KC conditioned medium with antibodies against TNFα and TGFβ1 partially blocks its capacity to activate HSCs. Only patients with alcoholic liver diseases and NASH cirrhosis have significantly higher activin-A levels and activin-A/follistatin ratio.Conclusions
Activin-A may induce fibrosis in NASH and alcoholic cirrhosis via activation of KCs to express pro-inflammatory molecules that promote HSC-dependent fibrogenesis and could be a target for future anti-fibrotic therapies. 相似文献4.
Clathrin-coated vesicles form a unique net-like structure in liver sinusoidal endothelial cells by assembling along undisrupted microtubules 总被引:1,自引:0,他引:1
Falkowska-Hansen B Falkowski M Metharom P Krunic D Goerdt S 《Experimental cell research》2007,313(9):1745-1757
Liver sinusoidal endothelial cells (LSECs) are highly active professional scavenger cells using clathrin-mediated endocytosis to clear the blood from macromolecular waste products. Using confocal microscopy, we observed a remarkable net-like distribution of clathrin heavy chain (CHC) in LSECs while all other cell types examined including various primary endothelial cells and cell lines showed the well-known punctuate staining pattern representing clathrin-coated vesicles (CCV). The net-like distribution of CHC in LSECs co-localized fully with microtubules, but not with actin. Upon 3D imaging, the net-like distribution of CHC resolved into numerous CCVs organized along the microtubules. The CCVs only partially co-localized with early endosome antigen 1 (EEA1) and adaptor protein 2 (AP-2). Endocytic vesicles containing ligand destined for degradation (FITC-AHGG) were organized along the clathrin/tubulin net-like structures, whereas transferrin-containing recycling vesicles co-localized to a much lower extent. Disruption of the microtubules by nocodazole treatment caused a collapse of the net-like organization of CCVs as well as a profound redistribution of EEA1, AP-2 and FITC-AHGG-containing vesicles, while transferrin internalization and recycling remained unaffected. 相似文献
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《Cell reports》2023,42(8):112836
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