Caught with their PAMPs down? The extracellular signalling actions of molecular chaperones are not due to microbial contaminants

Henderson, Brian E.; Calderwood, Stuart K.; Coates, Anthony R. M.; Cohen, Irun R.; Eden, Willem van; Lehner, Thomas; Pockley, A. Graham

doi:10.1007/s12192-009-0137-6

Cited by 97 publications

(77 citation statements)

References 128 publications

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“…8), similarly to what has previously been proposed [61]. In line with these observations, we demonstrated that doxorubicin treatment increased the level of p21, a key factor capable of orchestrating cellular senescence [62]. Moreover, the decrease of the intracellular levels of the chaperonin may lead to a decrease in its extracellular release.…”

Section: Discussionsupporting

confidence: 90%

Doxorubicin anti-tumor mechanisms include Hsp60 post-translational modifications leading to the Hsp60/p53 complex dissociation and instauration of replicative senescence

et al. 2017

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a b s t r a c tThe chaperone Hsp60 is pro-carcinogenic in certain tumor types by interfering with apoptosis and with tumor cell death. In these tumors, it is not yet known whether doxorubicin anti-tumor effects include a blockage of the pro-carcinogenic action of Hsp60. We found a doxorubicin dose-dependent viability reduction in a human lung mucoepidermoid cell line that was paralleled by the appearance of cell senescence markers. Concomitantly, intracellular Hsp60 levels decreased while its acetylation levels increased. The data suggest that Hsp60 acetylation interferes with the formation of the Hsp60/p53 complex and/or promote its dissociation, both causing an increase in the levels of free p53, which can then activate the p53-dependent pathway toward cell senescence. On the other hand, acetylated Hsp60 is ubiquitinated and degraded and, thus, the anti-apoptotic effect of the chaperonin is abolished with subsequent tumor cell death. Our findings could help in the elucidation of the molecular mechanisms by which doxorubicin counteracts carcinogenesis and, consequently, it would open new roads for the development of cancer treatment protocols targeting Hsp60.

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Section: Discussionsupporting

confidence: 90%

Doxorubicin anti-tumor mechanisms include Hsp60 post-translational modifications leading to the Hsp60/p53 complex dissociation and instauration of replicative senescence

et al. 2017

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“…The function of Hsp70 as a potential proinflammatory cytokine capable of inducing innate immunity (9) has long been considered controversial because it has been shown that the presence of endotoxin contaminants was most likely responsible for the observed effects (25). However, Hsp70 purified from nonbacterial origins was shown to be able to moderately stimulate macrophages as well as monocytes (21,22).…”

Section: Discussionmentioning

confidence: 99%

Inducible Heat Shock Protein 70 Reduces T Cell Responses and Stimulatory Capacity of Monocyte-derived Dendritic Cells

Stocki

Wang²,

Dickinson³

2012

Journal of Biological Chemistry

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Background: An increased presence of Hsp70 has been observed in many clinical conditions; however, its role remains elusive. Results: Hsp70 reduces the stimulatory capacity of dendritic cells and T cell responses in an in vitro experimental setup. Conclusion: Hsp70 might moderate inflammatory reactions mediated by the immune system. Significance: Provides additional insight into the role of Hsp70 in autoimmune diseases, transplantation, and cancer.

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“…In addition to playing important roles in maintaining the integrity of cellular proteins and a cell's response to proteotoxic stress, HSPs also function in inflammation, immune signaling, and antigen presentation Henderson et al 2010). The gastric pathogen H. pylori, the primary cause of chronic gastritis, peptic ulcer, MALT, and gastric cancer, has been demonstrated to down-modulate host-cell HSP expression upon infection (Axsen et al 2009;Baek et al 2004;Konturek et al 2001;Pierzchalski et al 2006;Targosz et al 2006;Yeo et al 2004).…”

Section: Discussionmentioning

confidence: 99%

The Helicobacter pylori cytotoxin CagA is essential for suppressing host heat shock protein expression

Lang

Gorrell

Tafreshi

et al. 2016

Cell Stress and Chaperones

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Bacterial infections typically elicit a strong Heat Shock Response (HSR) in host cells. However, the gastric pathogen Helicobacter pylori has the unique ability to repress this response, the mechanism of which has yet to be elucidated. This study sought to characterize the underlying mechanisms by which H. pylori down-modulates host HSP expression upon infection. Examination of isogenic mutant strains of H. pylori defective in components of the type IV secretion system (T4SS), identified the secretion substrate, CagA, to be essential for down-modulation of the HSPs HSPH1 (HSP105), HSPA1A (HSP72), and HSPD1 (HSP60) upon infection of the AGS gastric adenocarcinoma cell line. Ectopic expression of CagA by transient transfection was insufficient to repress HSP expression in AGS or HEK293T cells, suggesting that additional H. pylori factors are required for HSP repression. RT-qPCR analysis of HSP gene expression in AGS cells infected with wild-type H. pylori or isogenic cagA-deletion mutant found no significant change to account for reduced HSP levels. In summary, this study identified CagA to be an essential bacterial factor for H. pylori-mediated suppression of host HSP expression. The novel finding that HSPH1 is down-modulated by H. pylori further highlights the unique ability of H. pylori to repress the HSR within host cells. Elucidation of the mechanism by which H. pylori achieves HSP repression may prove to be beneficial in the identification of novel mechanisms to inhibit the HSR pathway and provide further insight into the interactions between H. pylori and the host gastric epithelium.

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Caught with their PAMPs down? The extracellular signalling actions of molecular chaperones are not due to microbial contaminants

Cited by 97 publications

References 128 publications

Doxorubicin anti-tumor mechanisms include Hsp60 post-translational modifications leading to the Hsp60/p53 complex dissociation and instauration of replicative senescence

Doxorubicin anti-tumor mechanisms include Hsp60 post-translational modifications leading to the Hsp60/p53 complex dissociation and instauration of replicative senescence

Inducible Heat Shock Protein 70 Reduces T Cell Responses and Stimulatory Capacity of Monocyte-derived Dendritic Cells

The Helicobacter pylori cytotoxin CagA is essential for suppressing host heat shock protein expression

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