2016
DOI: 10.1007/s12192-015-0659-z
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Tolerization against atherosclerosis using heat shock protein 60

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Cited by 37 publications
(28 citation statements)
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“…Finally, another immune cell type involved in atheroprogression (albeit to a lesser degree) are T-regulatory cells, which mediate atheroprotection by amplifying the release of IL-10, thereby resulting in immune suppression ( 139 142 ). However, the role of HSP27 in T-regulatory function during atheroprogression is uncertain ( 143 ). Mast cells, a key cell type that populates atherosclerotic plaque, are classically known to react immediately to allergens via cross-linking of cell surface IgE resulting in degranulation, histamine release, and synthesis of arachidonic acid metabolites, which can activate stress-signaling and pro-apoptotic pathways ( 144 ).…”
Section: Hsp27 In Atherosclerosismentioning
confidence: 99%
“…Finally, another immune cell type involved in atheroprogression (albeit to a lesser degree) are T-regulatory cells, which mediate atheroprotection by amplifying the release of IL-10, thereby resulting in immune suppression ( 139 142 ). However, the role of HSP27 in T-regulatory function during atheroprogression is uncertain ( 143 ). Mast cells, a key cell type that populates atherosclerotic plaque, are classically known to react immediately to allergens via cross-linking of cell surface IgE resulting in degranulation, histamine release, and synthesis of arachidonic acid metabolites, which can activate stress-signaling and pro-apoptotic pathways ( 144 ).…”
Section: Hsp27 In Atherosclerosismentioning
confidence: 99%
“…It is thought that T-cell reactivity to Hsp60 is less prominent in men age 50 and over because the majority of the T-cells have already formed from blood to the site of inflammation in atherosclerotic plaques and lymphocytes from peripheral blood may no longer present the specific antigen repertoire of cells in vessel walls [ 55 ]. This T-cell reactivity to Hsp60 is capable of triggering both innate and adaptive immune responses that initiate the earliest inflammatory stage of atherosclerosis, and mitochondrial Hsp60 is increasingly being recognised as a key autoantigen at the sites of endothelial inflammation [ 56 , 57 ]. However, the mechanisms leading to expression of Hsp60 during the initiation of arteriosclerosis due to T-cell reactivity to Hsp60 are still not well understood.…”
Section: Hsp60 and Inflammationmentioning
confidence: 99%
“…It has been reported that administration route of HSP60 immunization could affect the progression of atherosclerosis [31]. The current understanding is that HSP60 oral administration protects from atherosclerosis due to the HSP60-induced mucosal immune tolerance, whereas subcutaneous injection promotes atherosclerosis progression [12,[31][32][33]. Oral administrations of HSP60 increase MSDCs (myeloid derived suppressor cells) that suppress the progression of atherosclerosis [31].…”
Section: Plos Onementioning
confidence: 99%