共查询到18条相似文献,搜索用时 109 毫秒
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内质网应激(endoplasmic reticulum stress,ERs)是内质网腔内错误折叠蛋白聚积的一种适应性反应,适度ERs通过激活未折叠蛋白反应起适应性的细胞保护作用,而过高和持久的ERs则通过诱导转录因子CHOP表达、激活caspase-12和c—Jun氨基末端激酶(JNK)等导致细胞凋亡。近年来,越来越多的研究提示内质网应激是神经退行性病变、2型糖尿病以及肥胖等疾病发生过程中的重要环节。对内质网应激的细胞效应分子机制进行综述。随着对ERs机制理解的深入,有可能会发现新的分子标志物或新的诊疗策略。 相似文献
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内质网是蛋白质折叠、转录后修饰和转运的重要细胞器,对维持细胞稳态具有重要作用。多种内外环境刺激能够引起内质网内错误折叠或未折叠蛋白的积累,即形成内质网应激。内质网应激激活未折叠蛋白反应(unfolded protein response,UPR),进而启动一系列下游信号以维持内质网稳态。但持续或过度的内质网应激激活的UPR最终导致细胞凋亡和疾病。近年来,大量研究证据表明,内质网应激参与多种心血管疾病(cardiovascular disease, CVD)的发生和发展,包括缺血性心脏病、糖尿病性心肌病、心力衰竭、动脉粥样硬化、血管钙化、高血压和主动脉瘤等,是治疗多种CVD的重要靶点。本文就内质网应激激活UPR在多种常见CVD中的调控机制以及内质网应激与CVD关系的研究进展作一简要综述。 相似文献
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内质网(Endoplasmic reticulum,ER)是真核细胞细胞器的重要组成部分,主要负责蛋白质合成和翻译后修饰等过程,还参与调控了钙离子储存和脂类合成,具有重要生理功能。冠状病毒感染细胞后,在复制其遗传信息的同时也在合成大量病毒蛋白,造成未折叠/错误折叠蛋白堆积,进而增加内质网工作负担,诱发内质网应激(Endoplasmic reticulum stress,ERS),激活未折叠蛋白反应(Unfolded protein response,UPR),引起一系列信号级联反应,如诱导细胞凋亡等,进而影响病毒复制。本文就冠状病毒感染与ERS及UPR信号通路的研究进展做一综述,为新型抗冠状病毒药物的研发提供新视角。 相似文献
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内质网应激与帕金森病 总被引:1,自引:0,他引:1
内质网是细胞内最重要的细胞器之一,内质网功能与细胞状态密切相关。异常蛋白在内质网的堆积、胆固醇代谢异常、钙代谢紊乱等均能引起内质网应激。内质网应激在细胞生理病理中发挥重要作用。研究表明:内质网应激与神经退行性疾病,如帕金森病密切相关。该文简单概述了内质网应激与帕金森病之间的关系。 相似文献
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肝脏是机体物质代谢的中心,也是胰岛素作用的重要靶器官。肝脏胰岛素抵抗会影响糖脂代谢,机体出现血糖升高、肝内脂质沉积等症状,从而进一步加重胰岛素抵抗,二者形成恶性循环。内质网是蛋白质合成、折叠、加工及其质量监控的重要场所,广泛分布于真核细胞中。当机体出现生理性应激(如蛋白质分泌量增加)或病理性应激(如内质网中存在大量无法正确折叠的突变蛋白质)时,会导致蛋白质折叠需求与内质网蛋白质折叠能力之间的不平衡,从而引起内质网应激。内质网应激与肝脏胰岛素抵抗密切相关。近年来,大量研究发现,内质网应激不仅能直接破坏胰岛素信号传导通路,还可以通过多种方式作用于靶组织进一步促进胰岛素抵抗(尤其在肝脏)。 相似文献
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内质网是蛋白质合成与折叠、维持Ca2+动态平衡及合成脂类和固醇的场所。遗传或环境损伤引起内质网功能紊乱导致内质网应激,激活未折叠蛋白反应。未折叠蛋白反应是一种细胞自我保护性措施,但是内质网应激过强或持续时间过久可引起细胞凋亡。因此,内质网应激与众多人类疾病的发生发展密切相关。最近研究证明,癌症、炎症性疾病、代谢性疾病、骨质疏松症及神经退行性疾病等有内质网应激信号传递参与。然而内质网应激作为一个有效靶点参与各种疾病发挥作用的功能和机制仍然有待进一步研究。在近年来发表的文献基础上对内质网应激与疾病的关系,以及其可能的作用机制进行综述。 相似文献
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糖尿病肾病(diabetic nephropathy,DN)是糖尿病最常见的微血管并发症,是导致终末期肾脏疾病(end-stage renal disease,ESRD)的继发性肾脏疾病的主要病因之一。多种因素如缺氧、氧化应激、病毒感染、遗传突变等,可导致内质网内稳态失衡,大量未折叠蛋白和错误折叠引起蛋白堆积,即形成内质网应激(endoplasmic reticulum stress, ERS),从而激活未折叠蛋白反应(unfolded protein response, UPR)介导的三条经典的细胞适应性应答通路以恢复内质网稳态和细胞活性。但如果刺激过强或持续存在,便会启动细胞凋亡信号通路。大量研究表明ERS与DN的发生发展相关,并参与不同类型肾细胞损伤的过程,因此ERS作为治疗DN的有效靶点具有很重要的研究前景,调控ERS可为DN的治疗提供新的理论支持。从ERS相关信号通路及其在DN中的作用和新进展领域作一综述,以期为DN的治疗研究提供参考。 相似文献
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近年来,由于内质网应激/未折叠蛋白反应可影响物质代谢途径中的许多环节,故在非酒精性脂肪性肝病中起的作用越来越受到重视。现就内质网应激/未折叠蛋白反应在非酒精性脂肪性肝病中的作用和影响作一综述。 相似文献
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The redox homeostasis of the endoplasmic reticulum lumen is characteristically different from that of the other subcellular compartments. The concerted action of membrane transport processes and oxidoreductase enzymes maintain the oxidized state of the thiol-disulfide and the reducing state of the pyridine nucleotide redox systems, which are prerequisites for the normal functions of the organelle. The powerful thiol-oxidizing machinery allows oxidative protein folding but continuously challenges the local antioxidant defense. Alterations of the cellular redox environment either in oxidizing or reducing direction affect protein processing and may induce endoplasmic reticulum stress and unfolded protein response. The activated signaling pathways attempt to restore the balance between protein loading and processing and induce apoptosis if the attempt fails. Recent findings strongly support the involvement of this mechanism in brain ischemia, neuronal degenerative diseases and traumatic injury. The redox changes in the endoplasmic reticulum are integral parts of the pathomechanism of neurological diseases, either as causative agents, or as complications. 相似文献
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Disturbances in proteostasis are observed in many neurodegenerative diseases. This leads to activation of protein quality control to restore proteostasis, with a key role for the removal of aberrant proteins by proteolysis. The unfolded protein response (UPR) is a protein quality control mechanism of the endoplasmic reticulum (ER) that is activated in several neurodegenerative diseases. Recently we showed that the major proteolytic pathway during UPR activation is via the autophagy/lysosomal system. Here we investigate UPR induction if the other major proteolytic pathway of the ER -ER associated degradation (ERAD)-is inhibited. Surprisingly, impairment of ERAD results in decreased UPR activation and protects against ER stress toxicity. Autophagy induction is not affected under these conditions, however, a striking relocalization of the lysosomes is observed. Our data suggest that a protective UPR-modulating mechanism is activated if ERAD is inhibited, which involves lysosomes. Our data provide insight in the cross-talk between proteolytic pathways involved in ER proteostasis. This has implications for neurodegenerative diseases like Alzheimer’s disease where disturbed ER proteostasis and proteolytic impairment are early phenomena in the pathology. 相似文献
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Kubota K Niinuma Y Kaneko M Okuma Y Sugai M Omura T Uesugi M Uehara T Hosoi T Nomura Y 《Journal of neurochemistry》2006,97(5):1259-1268
Endoplasmic reticulum (ER) stress is defined as an accumulation of unfolded proteins in the endoplasmic reticulum. 4-phenylbutyrate (4-PBA) has been demonstrated to promote the normal trafficking of the DeltaF508 cystic fibrosis transmembrane conductance regulator (CFTR) mutant from the ER to the plasma membrane and to restore activity. We have reported that 4-PBA protected against cerebral ischemic injury and ER stress-induced neuronal cell death. In this study, we revealed that 4-PBA possesses chemical chaperone activity in vitro, which prevents the aggregation of denatured alpha-lactalbumin and bovine serum albumin (BSA). Furthermore, we investigated the effects of 4-PBA on the accumulation of Parkin-associated endothelin receptor-like receptor (Pael-R) pathologically relevant to the loss of dopaminergic neurons in autosomal recessive juvenile parkinsonism (AR-JP). Interestingly, 4-PBA restored the normal expression of Pael-R protein and suppressed ER stress induced by the overexpression of Pael-R. In addition, we showed that 4-PBA attenuated the activation of ER stress-induced signal transduction pathways and subsequent neuronal cell death. Moreover, 4-PBA restored the viability of yeasts that fail to induce an ER stress response under ER stress conditions. These results suggest that 4-PBA suppresses ER stress by directly reducing the amount of misfolded protein, including Pael-R accumulated in the ER. 相似文献
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I B Mosbah M A Zaouali C Martel M Bjaoui H B Abdennebi G Hotter C Brenner J Rosell��-Catafau 《Cell death & disease》2012,3(3):e279
Injury due to cold ischemia reperfusion (I/R) is a major cause of primary graft non-function following liver transplantation. We postulated that I/R-induced cellular damage during liver transplantation might affect the secretory pathway, particularly at the endoplasmic reticulum (ER). We examined the involvement of ER stress in organ preservation, and compared cold storage in University of Wisconsin (UW) solution and in Institute Georges Lopez-1 (IGL-1) solution. In one group of rats, livers were preserved in UW solution for 8 h at 4 °C, and then orthotopic liver transplantation was performed according to Kamada''s cuff technique. In another group, livers were preserved in IGL-1 solution. The effect of each preservation solution on the induction of ER stress, hepatic injury, mitochondrial damage and cell death was evaluated. As expected, we found increased ER stress after liver transplantation. IGL-1 solution significantly attenuated ER damage by reducing the activation of three pathways of unfolded protein response and their effector molecules caspase-12, C/EBP homologous protein-10, X-box-binding protein 1, tumor necrosis factor-associated factor 2 and eukaryotic translation initiation factor 2. This attenuation of ER stress was associated with a reduction in hepatic injury and cell death. Our results show that IGL-1 solution may be a useful means to circumvent excessive ER stress reactions associated with liver transplantation, and may optimize graft quality. 相似文献
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Peroxidative stress selectively down-regulates the neuronal stress response activated under conditions of endoplasmic reticulum dysfunction 总被引:5,自引:0,他引:5
Oxidative stress has been implicated in mechanisms leading to neuronal cell injury in various pathological states of the brain. Here, we investigated the effect of peroxide exposure on the expression of genes coding for cytoplasmic and endoplasmic reticulum (ER) stress proteins. Primary neuronal cell cultures were exposed to H(2)O(2) for 6 h and mRNA levels of hsp70, grp78, grp94, gadd153 were evaluated by quantitative PCR. In addition, peroxide-induced changes in protein synthesis and cell viability were investigated. Peroxide treatment of cells triggered an almost 12-fold increase in hsp70 mRNA levels, but a significant decrease in grp78, grp94 and gadd153 mRNA levels. To establish whether peroxide exposure blocks the ER-resident stress response, cells were also exposed to thapsigargin (Tg, a specific inhibitor of ER Ca(2+)-ATPase) which has been shown to elicit the ER stress response. Tg exposure induced 7.2-fold, 3.6-fold and 8.8-fold increase in grp78, grp94 and gadd153 mRNA levels, respectively. However, after peroxide pre-exposure, the Tg-induced effect on grp78, grp94 and gadd153 mRNA levels was completely blocked. The results indicate that oxidative damage causes a selective down-regulation of the neuronal stress response activated under conditions of ER dysfunction. This down-regulation was only observed in cultures exposed to peroxide levels which induced severe suppression of protein synthesis and cell injury, implying a causative link between peroxide-induced down-regulation of ER stress response system and development of neuronal cell injury. These observations could have implications for our understanding of the mechanisms underlying neuronal cell injury in pathological states of the brain associated with oxidative damage, including Alzheimer's disease where the neuronal stress response activated under conditions of ER dysfunction has been shown to be down-regulated. Down-regulation of ER stress response may increase the sensitivity of neurones to an otherwise nonlethal form of stress. 相似文献
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《Biology of the cell / under the auspices of the European Cell Biology Organization》2018,110(9):205-216
Chronic kidney disease (CKD) affects millions of persons worldwide and constitutes a major public health problem. Therefore, understanding the molecular basis of CKD is a key challenge for the development of preventive and therapeutic strategies. A major contributor to chronic histological damage associated with CKD is acute kidney injury (AKI). At the cellular level, kidney injuries are associated with microenvironmental alterations, forcing cells to activate adaptive biological processes that eliminate the stressor and generate alarm signals. These signalling pathways actively participate in tissue remodelling by promoting inflammation and fibrogenesis, ultimately leading to CKD. Many stresses that are encountered upon kidney injury are prone to trigger endoplasmic reticulum (ER) stress. In the kidney, ER stress both participates in acute and chronic histological damages, but also promotes cellular adaptation and nephroprotection. In this review, we will discuss the implication of ER stress in the pathophysiology of AKI and CKD progression, and we will give a critical analysis of the current experimental and clinical evidence that support ER stress as a mediator of kidney damage. 相似文献