Amyloid Induced Suicidal Erythrocyte Death

Nicolay, Jan P.; Gatz, Sabine; Liebig, Gerd; Gulbins, Erich; Läng, Florian

doi:10.1159/000099205

Cited by 84 publications

(48 citation statements)

References 60 publications

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“…Some of these diseases may cause eryptosis by stimulating the formation of hemin. Furthermore, several eryptosis-triggering xenobiotics and endogeneous substances have been identified, such as cordycepin [50], methylglyoxal [54], amyloid peptides [53], lipopetides [71] retinoic acid [55], paclitaxel [44], amantadine [23], chlorpromazine [1], ciglitazone [58], cyclosporine [56], Bay-5884 [65], curcumin [4], valinomycin [64], listeriolysin [25], aluminum [57], copper [46], bismuth [13], tin [52], cadmium [68], selenium [67], vanadate [27], gold [69], and arsenic [51]. At least in theory, some of those substances may be effective through stimulation of hemin formation.…”

Section: Discussionmentioning

confidence: 99%

Hemin-induced suicidal erythrocyte death

2009

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Several diseases, such as malaria, sickle cell disease, and ischemia/reperfusion may cause excessive formation of hemin, which may in turn trigger hemolysis. A variety of drugs and diseases leading to hemolysis triggers suicidal erythrocyte death or eryptosis, i.e., cell membrane scrambling and cell shrinkage. Eryptosis is elicited by increased cytosolic Ca 2+ activity and by ceramide. The present study explored whether hemin stimulates eryptosis. Cell membrane scrambling was estimated from annexin Vbinding to phosphatidylserine exposed at the cell surface, cell shrinkage from forward scatter in fluorescence-activated cell sorter analysis, cytosolic Ca 2+ activity from Fluo3 fluorescence and ceramide formation from fluorescencelabeled antibody binding. Exposure to hemin (1-10 μM) within 48 h significantly increased annexin V-binding, decreased forward scatter, increased cytosolic Ca 2+ activity, and stimulated ceramide formation. In conclusion, hemin stimulates suicidal cell death, which may in turn contribute to the clearance of circulating erythrocytes and thus to anemia.

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Section: Discussionmentioning

confidence: 99%

Hemin-induced suicidal erythrocyte death

2009

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“…Eryptosis has been observed in a wide variety of further anemic conditions, including sickle-cell anemia [59,60], beta-thalassemia [55], glucose-6-phosphate dehydrogenase (G6PD)-deficiency [55], phosphate depletion [59], iron deficiency [61], Hemolytic Uremic Syndrome [62], sepsis [63], malaria [64] and Wilson disease [35]. Moreover, enhanced eryptosis could contribute to the anemia following excessive formation, treatment or intoxication with hemolysin Kanagawa [65], listeriolysin [66], PGE 2 [67], lipoxygenase inhibitor Bay-5884 [68], platelet activating factor [69], paclitaxel [70], methylglyoxal [71], chlorpromazine [72], amantadine [73], cyclosporine [34], curcumin [74], amyloid peptides [75], aluminium [34], lead [32], mercury [33] and copper ions [35]. …”

Section: Discussionmentioning

confidence: 99%

Stimulation of Eryptosis by Cadmium Ions

Sopjani

Föller²,

Dreischer

et al. 2008

Cell Physiol Biochem

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Cadmium ions are known to trigger apoptosis. Erythrocytes may similarly undergo suicidal death or eryptosis, which is characterized by exposure of phosphatidylserine at the erythrocyte surface. As macrophages are equipped with phosphatidylserine receptors, they bind, engulf and degrade phosphatidylserine exposing cells. Cellular mechanisms known to trigger cell membrane phospholipid scrambling include increased cytosolic Ca

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“…Ceramide molecules spontaneously aggregate and form small domains that fuse to larger ceramide-enriched membrane platforms that serve to re-organize and cluster receptors and signaling molecules [25, 26]. The generation of ceramide molecules within membranes also changes membrane properties and membrane fluidity [27-31]. The re-organization of receptors and associated signaling molecules mediates many of the cellular effects of ceramides [25].…”

Section: Introductionmentioning

confidence: 99%

Staphylococcus aureus α-Toxin Induces Inflammatory Cytokines via Lysosomal Acid Sphingomyelinase and Ceramides

Gulbins

Edwards

et al. 2017

Cell Physiol Biochem

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Background/Aims: Staphylococcus aureus (S. aureus) infections are a major clinical problem and range from mild skin and soft-tissue infections to severe and even lethal infections such as pneumonia, endocarditis, sepsis, osteomyelitis, and toxic shock syndrome. Toxins that are released from S. aureus mediate many of these effects. Here, we aimed to identify molecular mechanisms how α-toxin, a major S. aureus toxin, induces inflammation. Methods: Macrophages were isolated from the bone marrow of wildtype and acid sphingomyelinase-deficient mice, stimulated with S. aureus α-toxin and activation of the acid sphingomyelinase was quantified. The subcellular formation of ceramides was determined by confocal microscopy. Release of cathepsins from lysosomes, activation of inflammasome proteins and formation of Interleukin-1β (IL-1β) and Tumor Necrosis Factor-α (TNF-α) were analyzed by western blotting, confocal microscopy and ELISA. Results: We demonstrate that S. aureus α-toxin activates the acid sphingomyelinase in ex vivo macrophages and triggers a release of ceramides. Ceramides induced by S. aureus α-toxin localize to lysosomes and mediate a release of cathepsin B and D from lysosomes into the cytoplasm. Cytosolic cathepsin B forms a complex with Nlrc4. Treatment of macrophages with α-toxin induces the formation of IL-1β and TNF-α. These events are reduced or abrogated, respectively, in cells lacking the acid sphingomyelinase and upon treatment of macrophages with amitriptyline, a functional inhibitor of acid sphingomyelinase. Pharmacological inhibition of cathepsin B prevented activation of the inflammasome measured as release of IL-1β, while the formation of TNF-α was independent of cathepsin B. Conclusion: We demonstrate a novel mechanism how bacterial toxins activate the inflammasome and mediate the formation and release of cytokines: S. aureus α-toxin triggers an activation of the acid sphingomyelinase and a release of ceramides resulting in the release of lysosomal cathepsin B and formation of pro-inflammatory cytokines.

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Amyloid Induced Suicidal Erythrocyte Death

Cited by 84 publications

References 60 publications

Hemin-induced suicidal erythrocyte death

Hemin-induced suicidal erythrocyte death

Stimulation of Eryptosis by Cadmium Ions

Staphylococcus aureus α-Toxin Induces Inflammatory Cytokines via Lysosomal Acid Sphingomyelinase and Ceramides

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