Down-regulation of HSP60 expression by RNAi increases lipopolysaccharide- and cerulein-induced damages on isolated rat pancreatic tissues

Li, Yongyu; Lü, Shuai; Li, Kun; Feng, Jia-yan; Li, Yanna; Gao, Zhen; Chen, Changjie

doi:10.1007/s12192-010-0207-9

Cited by 13 publications

(16 citation statements)

References 28 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…Studies have shown that the ordered synthesis, transport, modi cation and secretion of pancreatic enzymes are closely related to Hsp60 [3,13]. And there are reports to reveal the protective effects of Hsp60 on AP, that is, water immersion stress induced Hsp60 expression protects against pancreatitis in rats [14], and down-regulation of Hsp60 worsen the injuries of isolated rat pancreatic tissues [5]. However, few studies have observed the protective effect of Hap60 on AP in mice, and the mechanism of Hsp60 in the pathogenesis and protection of AP need further investigation [15].…”

Section: Discussionmentioning

confidence: 99%

“…Heat shock protein 60 (Hsp60), known as molecular chaperonin, is a member of heat shock protein family which functions in protein folding, transmembrane translocation, assembly, and disassembly. In pancreas, there is evidence that Hsp60 coexists with pancreatic zymogen granules along the exocrine secretion pathway in pancreatic acinar cells [3], and studies suggest that the decreased expression of Hsp60 in pancreas may correlate with the occurrence of AP in rat [4,5]. The protective effect of HSP60 on AP is to be discussed further.…”

Section: Introductionmentioning

confidence: 95%

See 1 more Smart Citation

Pre-inhalation of Hydrogen-rich Gases Protect Against Caerulein-induced Mouse Acute Pancreatitis While Enhance the Pancreatic Hsp60 Protein Expression

Yin²,

Yi³

et al. 2020

Preprint

Self Cite

View full text Add to dashboard Cite

Background: Acute pancreatitis (AP) lacks targeted prevention and treatment measures. Some key points in the pathogenesis of AP remain unclear, such as early activation of pancreatic enzymes. Several recent reports have shown the protective effect of hydrogen on several AP animal models, and the mechanism is related to antioxidant activity. Heat shock protein 60 (Hsp60) is known to accompany pancreatic enzymes synthesis and secretion pathway of in pancreatic acinar cells, while role of hsp60 in AP remains a topic. The aim of this study was to investigate effect of hydrogen pretreatment on experimental AP mice, as well as the possible mechanisms, focusing on antioxidant and Hsp60 expression alteration mechanisms.Methods: 80 mice were randomly assigned into four groups: HAP group, AP group, HNS group, and NS group and each group were set 3 observation time point as 1h, 3h and 5h (n=6- 8). Mouse AP model was induced by intraperitoneal injection of 50μg/kg caerulein per hour for 6 injections both in AP and HAP groups, and mice in NS group and HNS group given normal saline (NS) injections at the same way as control respectively. Mice in HAP group and HNS group were treated with hydrogen-rich gases inhalation for 3 days before the first injection of caerulein or saline, while mice in AP group and NS group in normal air condition. Histopathology of pancreatic tissue, plasma amylase and lipase, plasma IL-1 and IL-6, pancreatic glutathione (GSH) and malondialdehyde (MDA), and Hsp60 mRNA and protein expression were investigated. Comparisons were made by one-way analysis of variance.Results: The pancreatic pathological changes, plasma amylase and lipase activity, and the increase of plasma IL-1 and IL-6 levels in AP mice were significantly improved by the hydrogen-rich gases pretreatment, Meanwhile, the pancreatic GSH content increased and the pancreatic MDA content decreased. And, the hydrogen-rich gases pretreatment improved the Hsp60 protein expression in pancreatic tissues of AP mice at 1h and 5h. Conclusions: Pre-inhalation of hydrogen-rich gases have a good protective effect on AP mice, and the possible mechanisms of reduced oxidative stress and the early increased pancreatic Hsp60 protein deserve attention.

show abstract

Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 95%

Pre-inhalation of Hydrogen-rich Gases Protect Against Caerulein-induced Mouse Acute Pancreatitis While Enhance the Pancreatic Hsp60 Protein Expression

Yin²,

Yi³

et al. 2020

Preprint

Self Cite

View full text Add to dashboard Cite

show abstract

“…This expression of HSP60 in pancreatic tissues has been decreased with prolonged stimulation with LPS [64]. Ohashi et al [14] claimed that TLR4 mediates HSP60 signaling, as a putative endogenous ligand of the TLR4 complex.…”

Section: Discussionmentioning

confidence: 99%

Long-Lasting Effect of Infant Rats Endotoxemia on Heat Shock Protein 60 in the Pancreatic Acinar Cells: Involvement of Toll-Like Receptor 4

Bonior

Jaworek

Kot

et al. 2012

International Journal of Inflammation

View full text Add to dashboard Cite

Introduction. Lipopolysaccharide endotoxin (LPS) is responsible for septic shock and multiorgan failure, but pretreatment of rats with low doses of LPS reduced pancreatic acute damage. Aim. We investigated the effects of the endotoxemia induced in the early period of life on Toll-like receptor 4 (TLR4), heat shock protein 60 (HSP60) and proapoptotic Bax, caspase-9 and -3 or antiapoptotic Bcl-2 protein expression in the pancreatic acinar cells of adult animals. Material and Methods. Newborn rats (25 g) were injected with endotoxin (Escherichia coli) for 5 consecutive days. Two months later, pancreatic acinar cells were isolated from all groups of animals and subjected to caerulein stimulation (10−8 M). Protein expression was assessed employing Western blot. For detection of apoptosis we have employed DNA fragmentation ladder assay. Results. Preconditioning of newborn rats with LPS increased TLR4, Caspase-9 and -3 levels, but failed to affect basal expression of HSP60, Bax, and Bcl-2. Subsequent caerulein stimulation increased TLR4, Bcl-2, and caspases, but diminished HSP60 and Bax proteins in pancreatic acinar cells. Endotoxemia dose-dependently increased TLR4, Bax, HSP60, and both caspases protein signals in the pancreatic acini, further inhibiting antiapoptotic Bcl-2. Conclusions. Endotoxemia promoted the induction of HSP60 via TLR4 in the infant rats and participated in the LPS-dependent pancreatic tissue protection against acute damage.

show abstract

“…HSP60 is typically a mitochondrial protein, which together with its co-chaperone HSP10 (also designated HSPE1 in humans, and Hsp10 or Cpn10 in prokaryotes), assists protein folding inside the organelle [12][13][14][15]. The presence and integrity of HSP60 in mitochondria are crucial for cell survival as demonstrated by inducing HSP60 knockdown with siRNA oligonucleotides, which leads to apoptosis [12][13][14][15][16][17][18], and by the occurrence of at least two serious human genetic chaperonopathies associated with mutations of the HSP60 gene [19,20].…”

Section: Hsp60: a Multifunctional Molecule That Interacts With The Immentioning

confidence: 99%

“…Distinctive functional domains in chaperone molecules recognize a polypeptide in need of assistance, build a chaperoning complex, form a network with other chaperoning complexes, or interact with a protein-degrading machine like the ubiquitin-proteasome system. HSP/chaperones also play 'extrachaperoning' roles, namely non-canonical functions, such as participation in IS regulation, cell differentiation, gene expression, DNA replication, signal transduction, programmed cell death, cellular senescence, and carcinogenesis [12][13][14][15][16][17][18].…”

Section: Introductionmentioning

confidence: 99%

HSP60 is a Ubiquitous Player in the Physiological and Pathogenic Interactions between the Chaperoning and the Immune Systems

Gammazza¹,

Bavisotto

David

et al. 2017

CIR

View full text Add to dashboard Cite

HSP60 participates in many interactions between the system integrated by all chaperones and closely associated molecules (chaperoning system or CS) and the immune system (IS). These interactions occur constantly to maintain normal cell physiology but, occasionally, they are perturbed and become mediators of pathologic events that may lead to disease. This switch to pathology may be initiated by various factors, genetic or acquired, which cause qualitative and/or quantitative modifications of HSP60, or immune crossreactivity between the human and microbial chaperonin orthologs, or a break in the balance between the pro-and anti-inflammatory actions of the chaperonin. Thus, autoimmune and chronic inflammatory pathologies may occur. Likewise, a perturbation of the CS-IS interactions, e.g., those that take place during ageing, may favor carcinogenesis. HSP60 may be commandeered by tumor cells to assist its high-rate protein synthesis and, also, to be an emissary among the devices tumor cells utilize to avoid anti-tumor immune reactions. Here, we briefly discuss the canonical and non-canonical functions of HSP/chaperones; and HSP60 as a multifunctional molecule, its migration itinerary, and its possible roles during carcinogenesis and in certain chronic inflammatory and autoimmune diseases. We examine the potential of HSP60 as a biomarker useful for diagnosing and monitoring the progression of the various conditions in which it actively participates. Lastly, we discuss the use HSP60 as target for controlling its activity when it is an etiopathogenic factor, or as a therapeutic agent to correct its deficiency.

show abstract

Down-regulation of HSP60 expression by RNAi increases lipopolysaccharide- and cerulein-induced damages on isolated rat pancreatic tissues

Cited by 13 publications

References 28 publications

Pre-inhalation of Hydrogen-rich Gases Protect Against Caerulein-induced Mouse Acute Pancreatitis While Enhance the Pancreatic Hsp60 Protein Expression

Pre-inhalation of Hydrogen-rich Gases Protect Against Caerulein-induced Mouse Acute Pancreatitis While Enhance the Pancreatic Hsp60 Protein Expression

Long-Lasting Effect of Infant Rats Endotoxemia on Heat Shock Protein 60 in the Pancreatic Acinar Cells: Involvement of Toll-Like Receptor 4

HSP60 is a Ubiquitous Player in the Physiological and Pathogenic Interactions between the Chaperoning and the Immune Systems

Contact Info

Product

Resources

About