secretory pathways

分泌途径
  • 文章类型: Journal Article
    BACKGROUND: Systemic multi-organ dysfunction resulting from dysregulated immune responses in the host triggered by microbial infection or other factors is a major cause of death in sepsis, and secretory pathways play an important role in it.
    METHODS: GSE57065, GSE65682, GSE145227, and GSE54514 from Gene Expression Omnibus (GEO) were derived for this study. Secretory pathways single sample gene set enrichment analysis (ssGSEA) scores in sepsis and normal samples were exposed. Gene modules associated with secretory pathways were selected by weighted gene coexpression network analysis (WGCNA) for Protein-Protein Interaction Networks (PPI) assessment, and crossover genes in both were evaluated by eXtreme Gradient Boosting (XGBoost) model in feature selection to identify hub genes in sepsis. In addition, we explored the immune cells and signaling pathways regulated by hub genes.
    RESULTS: Remarkable dysregulation of secretory pathways was demonstrated in sepsis. The secretory pathways-associated gene modules were intimately involved in cytokine and immune responses in infection. Four crossover genes (CD163, FCER1G, C3AR1, ARG1) were present in WGCNA and PPI, and training in the XGBoost model revealed the best diagnostic performance of these 4 genes, meaning that these genes were the hub genes for sepsis. The 4-hub genes showed a significant negative correlation with T cell activity and a significant positive correlation with inflammatory immune cells. In addition, we found that the 4-hub genes markedly positively regulated INFLAMMATORY RESPONSE, IL6 JAK STAT3 SIGNALING.
    CONCLUSIONS: Based on WGCNA, PPI, and XGBoost models, we identified hub genes that play an important regulatory role in sepsis. We also developed novel molecular models for the diagnosis of sepsis.
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  • 文章类型: Journal Article
    黄病毒属含有多种在人类中引起严重疾病的病毒,包括登革热病毒,黄热病病毒,寨卡病毒,西尼罗河病毒,日本脑炎病毒和蜱传脑炎病毒。非结构蛋白1(NS1)是一种糖蛋白,编码352个氨基酸的多肽,分子量为46-55kDa,具体取决于其糖基化状态。NS1在多种黄病毒中高度保守,并以不同的形式发生。包括内质网内的二聚体形式,质膜上的细胞相关形式,或分泌的六聚体形式(sNS1)运输到细胞外基质。细胞内二聚体NS1与其他NS相互作用,参与病毒复制和病毒体成熟,而细胞外sNS1在免疫逃避中起关键作用,黄病毒致病机理和与天然载体的相互作用。在这次审查中,我们概述了黄病毒NS1的最新研究进展,包括结构细节的研究,哺乳动物和蚊子细胞的分泌途径以及病毒复制的多种功能,免疫逃避,发病机理和与自然宿主的相互作用,将以前的数据汇总在一起以确定这种蛋白质的特性。
    The genus Flavivirus contains a wide variety of viruses that cause severe disease in humans, including dengue virus, yellow fever virus, Zika virus, West Nile virus, Japanese encephalitis virus and tick-borne encephalitis virus. Nonstructural protein 1 (NS1) is a glycoprotein that encodes a 352-amino-acid polypeptide and has a molecular weight of 46-55 kDa depending on its glycosylation status. NS1 is highly conserved among multiple flaviviruses and occurs in distinct forms, including a dimeric form within the endoplasmic reticulum, a cell-associated form on the plasma membrane, or a secreted hexameric form (sNS1) trafficked to the extracellular matrix. Intracellular dimeric NS1 interacts with other NSs to participate in viral replication and virion maturation, while extracellular sNS1 plays a critical role in immune evasion, flavivirus pathogenesis and interactions with natural vectors. In this review, we provide an overview of recent research progress on flavivirus NS1, including research on the structural details, the secretory pathways in mammalian and mosquito cells and the multiple functions in viral replication, immune evasion, pathogenesis and interaction with natural hosts, drawing together the previous data to determine the properties of this protein.
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  • 文章类型: Journal Article
    重组蛋白的产生会对细胞代谢造成严重的应激,导致滴度和产品质量有限。为了研究与这些限制相关的细胞和代谢特征,我们比较了以不同速率产生促红细胞生成素(EPO)(分泌)或GFP(非分泌)蛋白的HEK293克隆。转录组学和功能分析表明,与亲本和GFP细胞相比,EPO生产者的代谢和氧化磷酸化明显更高。此外,核糖体基因根据重组蛋白和生产率表现出特定的表达模式。在一个显示EPO分泌显著增加的克隆中,我们检测到与内质网(ER)应激负调控相关的较高基因表达,包括ATF6B的上调,其通过过表达或小干扰RNA(siRNA)敲低来帮助在克隆的子集中产生EPO。我们的结果为进一步开发哺乳动物细胞工厂的分泌能力提供了潜在的目标途径和基因。
    Recombinant protein production can cause severe stress on cellular metabolism, resulting in limited titer and product quality. To investigate cellular and metabolic characteristics associated with these limitations, we compare HEK293 clones producing either erythropoietin (EPO) (secretory) or GFP (non-secretory) protein at different rates. Transcriptomic and functional analyses indicate significantly higher metabolism and oxidative phosphorylation in EPO producers compared with parental and GFP cells. In addition, ribosomal genes exhibit specific expression patterns depending on the recombinant protein and the production rate. In a clone displaying a dramatically increased EPO secretion, we detect higher gene expression related to negative regulation of endoplasmic reticulum (ER) stress, including upregulation of ATF6B, which aids EPO production in a subset of clones by overexpression or small interfering RNA (siRNA) knockdown. Our results offer potential target pathways and genes for further development of the secretory power in mammalian cell factories.
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  • 文章类型: Journal Article
    羧肽酶A3(CPA3)是具有可变表达的特异性肥大细胞(MC)蛋白酶。该蛋白酶是分泌组的预先形成的组分之一。在颗粒成熟期间,CPA3成为具有特征性定位的活性酶,决定了MC的细胞学和超微结构表型的特征。CPA3参与特定组织微环境的调节,影响先天免疫的实施,血管生成的机制,细胞外基质的重塑过程,等。CPA3在MC中的表达特征可用于完善MC分类,有助于预后,提高靶向治疗的有效性。
    Carboxypeptidase A3 (CPA3) is a specific mast cell (MC) protease with variable expression. This protease is one of the preformed components of the secretome. During maturation of granules, CPA3 becomes an active enzyme with a characteristic localization determining the features of the cytological and ultrastructural phenotype of MC. CPA3 takes part in the regulation of a specific tissue microenvironment, affecting the implementation of innate immunity, the mechanisms of angiogenesis, the processes of remodeling of the extracellular matrix, etc. Characterization of CPA3 expression in MC can be used to refine the MC classification, help in a prognosis, and increase the effectiveness of targeted therapy.
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  • 文章类型: Journal Article
    Neutrophils sense and migrate towards chemotactic factors released at sites of infection/inflammation and contain the affected area using a variety of effector mechanisms. Aside from these established immune defense functions, neutrophils are emerging as one of the key tumor-infiltrating immune cells that influence cancer progression and metastasis. Neutrophil recruitment to the tumor microenvironment (TME) is mediated by multiple mediators including cytokines, chemokines, lipids, and growth factors that are secreted from cancer cells and cancer-associated stromal cells. However, the molecular mechanisms that underlie the expression and secretion of the different mediators from cancer cells and how neutrophils integrate these signals to reach and invade tumors remain unclear. Here, we discuss the possible role of the epithelial to mesenchymal transition (EMT) program, which is a well-established promoter of malignant potential in cancer, in regulating the expression and secretion of these key mediators. We also summarize and review our current understanding of the machineries that potentially control the secretion of the mediators from cancer cells, including the exocytic trafficking pathways, secretory autophagy, and extracellular vesicle-mediated secretion. We further reflect on possible mechanisms by which different mediators collaborate by integrating their signaling network, and particularly focus on TGF-β, a cytokine that is highly expressed in invasive tumors, and CXCR2 ligands, which are crucial neutrophil recruiting chemokines. Finally, we highlight gaps in the field and the need to expand current knowledge of the secretory machineries and cross-talks among mediators to develop novel neutrophil targeting strategies as effective therapeutic options in the treatment of cancer.
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  • 文章类型: Journal Article
    Signal peptides (SP) are short peptides located in the N-terminal of proteins, carrying information for protein secretion. They are ubiquitous to all prokaryotes and eukaryotes. SPs have been of special interest in several scientific and industrial fields, including recombinant protein production, disease diagnosis, immunization, and laboratory techniques. Recently, the role of SPs in recombinant protein production has gained too much attention. Herein, several studies have been reviewed to elucidate the precise structure and function of SPs, particularly the optimized ones for recombinant protein production. However, some features of SPs still have remained obscure. In this review, some approaches concerning elucidation and optimization of SPs are discussed, and pragmatic conclusions and suggestions for future studies are also proposed. Moreover, a summary of secretory pathways, evolutionary changes, functions, applications, and different types of SPs is mentioned. At last, current limitations and prospects are discussed.
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  • 文章类型: Journal Article
    Dengue virus nonstructural protein 1 (NS1) is a multifunctional glycoprotein. For decades, the notion in the field was that NS1 is secreted exclusively from vertebrate cells and not from mosquito cells. However, recent evidence shows that mosquito cells also secrete NS1 efficiently. In this review, we discuss the evidence for secretion of NS1 of dengue virus, and of other flaviviruses, from mosquito cells, differences between NS1 secreted from mosquito and NS1 secreted from vertebrate cells, and possible roles of soluble NS1 in the insect flavivirus vector.
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  • 文章类型: Journal Article
    Annexin A1 (ANXA1) is a Ca(2+)-regulated phospholipid-binding protein involved in various cell processes. ANXA1 was initially widely studied in inflammation resolution, but its overexpression was later reported in a large number of cancers. Further in-depth investigations have revealed that this protein could have many roles in cancer progression and act at different levels (from cancer initiation to metastasis). This is partly due to the location of ANXA1 in different cell compartments. ANXA1 can be nuclear, cytoplasmic and/or membrane associated. This last location allows ANXA1 to be proteolytically cleaved and/or to become accessible to its cognate partners, the formyl-peptide receptors. Indeed, in some cancers, ANXA1 is found at the cell surface, where it stimulates formyl-peptide receptors to trigger oncogenic pathways. In the present review, we look at the different locations of ANXA1 and their association with the deregulated pathways often observed in cancers. We have specifically detailed the non-classic pathways of ANXA1 externalization, the significance of its cleavage and the role of the ANXA1-formyl-peptide receptor complex in cancer progression.
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  • 文章类型: Journal Article
    植物分泌体是植物细胞分泌的蛋白质,参与细胞壁结构的维持。宿主和病原体之间的关系,植物中不同细胞之间的交流,等。生物信息学等方法的融合,生物化学,蛋白质组学被用来分离,分类,并通过协调植物系统和体外悬浮培养细胞系统(SSC)来概述分泌组。我们总结并解释了Secretome的含义,本文综述了细胞外空间分泌蛋白的鉴定和分离方法以及分泌蛋白纯度的评价方法。还讨论了两种基于DPAGE方法和基于HPLC的分析方法以及用于预测分泌组蛋白的不同生物信息学工具。分泌组蛋白在不同环境胁迫下的生物学意义,即,盐胁迫,干旱胁迫,氧化应激,等。,还详细解释了防御反应和植物与环境的相互作用。
    Plant secretomes are the proteins secreted by the plant cells and are involved in the maintenance of cell wall structure, relationship between host and pathogen, communication between different cells in the plant, etc. Amalgamation of methodologies like bioinformatics, biochemical, and proteomics are used to separate, classify, and outline secretomes by means of harmonizing in planta systems and in vitro suspension cultured cell system (SSCs). We summed up and explained the meaning of secretome, methods used for the identification and isolation of secreted proteins from extracellular space and methods for the assessment of purity of secretome proteins in this review. Two D PAGE method and HPLC based methods for the analysis together with different bioinformatics tools used for the prediction of secretome proteins are also discussed. Biological significance of secretome proteins under different environmental stresses, i.e., salt stress, drought stress, oxidative stress, etc., defense responses and plant interactions with environment are also explained in detail.
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