Impaired Platelet Function among Platelet Donors

Jilma‐Stohlawetz, Petra; Hergovich, Nicole; Homoncik, Monika; Dzirlo, Larisa; Horvath, Michaela; Janisiw, Michael; Panzer, Simon; Jilma, Bernd

doi:10.1055/s-0037-1616146

Cited by 65 publications

(71 citation statements)

References 34 publications

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“…It is also well known that EPO can cause thrombosis and therefore tissue injury (40). Even a single exposure of normal humans to EPO causes a dose-dependent increase in E-selectin within 2 days, which is consistent with significant endothelial cell activation (41). Similar responses have also been documented for other markers associated with thrombosis, e.g., P-selectin, and in vitro studies confirm direct and rapid prothrombotic effects of EPO on the endothelium (42).…”

Section: Discussionsupporting

confidence: 64%

A nonerythropoietic derivative of erythropoietin protects the myocardium from ischemia–reperfusion injury

Fiordaliso

Chimenti

Staszewsky

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

201

134

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The cytokine erythropoietin (EPO) protects the heart from ischemic injury, in part by preventing apoptosis. However, EPO administration can also raise the hemoglobin concentration, which, by increasing oxygen delivery, confounds assignment of cause and effect. The availability of EPO analogs that do not bind to the dimeric EPO receptor and lack erythropoietic activity, e.g., carbamylated EPO (CEPO), provides an opportunity to determine whether EPO possesses direct cardioprotective activity. In vivo, cardiomyocyte loss after experimental myocardial infarction (MI) of rats (40 min of occlusion with reperfusion) was reduced from Ϸ57% in MI-control to Ϸ45% in animals that were administered CEPO daily for 1 week (50 g͞kg of body weight s.c.) with the first dose administered intravenously 5 min before reperfusion. CEPO did not increase the hematocrit, yet it prevented increases in left ventricular (LV) end-diastolic pressure, reduced LV wall stress in systole and diastole, and improved LV response to dobutamine infusion compared with vehicle-treated animals. In agreement with the cardioprotective effect observed in vivo, staurosporineinduced apoptosis of adult rat or mouse cardiomyocytes in vitro was also significantly attenuated (Ϸ35%) by CEPO, which is comparable with the effect of EPO. These data indicate that prevention of cardiomyocyte apoptosis, in the absence of an increase in hemoglobin concentration, explains EPO's cardioprotection. Nonerythropoietic derivatives such as CEPO, devoid of the undesirable effects of EPO, e.g., thrombogenesis, could represent safer and more effective alternatives for treatment of cardiovascular diseases, such as MI and heart failure. Furthermore, these findings expand the activity spectrum of CEPO to tissues outside the nervous system. apoptosis ͉ cardioprotection ͉ cytokine ͉ tissue injury E rythropoietin (EPO) protects the brain and the spinal cord from ischemic and traumatic injury (1, 2), the peripheral nerve from diabetic damage (3), the kidney from ischemic (4, 5) or toxic insults (6), and the heart from acute ischemia, either permanent (7-9) or with reperfusion (10). Current data suggest that the observed protective effects of EPO depend on an antiapoptotic effect of this cytokine (7, 10). In the brain, EPO also greatly reduces the inflammatory response after ischemiareperfusion (11). It is notable that in several acute models, e.g., brain ischemia, a single dose of EPO that does not increase the Hb concentration nevertheless confers neuroprotection. However, in other in vivo injury models, including cardiac ischemia with reperfusion and diabetic neuropathy, injury develops gradually, and multiple doses of EPO appear superior but also increase the Hb concentration. The possibility that part of the benefit obtained with EPO in these models may depend on the increased oxygen-carrying capacity of the blood cannot be excluded. However, cardiac protection has clearly been demonstrated after only a single dose (8, 10) when evaluated 1-3 days after infarction before any increase i...

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Section: Discussionsupporting

confidence: 64%

A nonerythropoietic derivative of erythropoietin protects the myocardium from ischemia–reperfusion injury

Fiordaliso

Chimenti

Staszewsky

et al. 2005

Proc. Natl. Acad. Sci. U.S.A.

201

134

View full text Add to dashboard Cite

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“…EPO is a potent cytokine with stimulatory effects on vascular endothelium, 43 smooth muscle cells, 44,45 and platelets. 46 EPO administration induces a release of vasoactive factors such as monocyte chemoattractant protein-1, 45,47 endothelin-1, 48 thromboxane A2, and selectin. 46,49 It can also induce endothelial dysfunction by inhibiting dimethylarginine dimethylaminohydrolase, thereby increasing asymmetric dimethyl arginine.…”

Section: Role Of Epo Inflammation and Vascular Injurymentioning

confidence: 99%

“…46 EPO administration induces a release of vasoactive factors such as monocyte chemoattractant protein-1, 45,47 endothelin-1, 48 thromboxane A2, and selectin. 46,49 It can also induce endothelial dysfunction by inhibiting dimethylarginine dimethylaminohydrolase, thereby increasing asymmetric dimethyl arginine. 50 Furthermore, EPO is a potent stimulant of endothelial and progenitor cell proliferation, 51,52 as well as wound-healing responses 53 that are reminiscent of histologic 45,47 might also contribute to the fibrogenesis seen in NSF.…”

Section: Role Of Epo Inflammation and Vascular Injurymentioning

confidence: 99%

New Insights into Nephrogenic Systemic Fibrosis

Swaminathan

Shah

2007

Journal of the American Society of Nephrology

110

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“…We determined prothrombin fragment (F 1 + 2 ) by an enzyme immunoassay (Behring, Marburg, Germany) to examine whether the blockade of IL-8 inhibits thrombin formation. We measured serum thromboxane B 2 levels as previously described (10), to evaluate if the accumulation of the reparixin metabolite ibuprofen (C ss= 4mg/L) is sufficient to inhibit the cyclooxygenase pathway. Blood counts were performed with a cell counter (Sysmex, Milton Keynes, UK).…”

Section: Analyses Ofsoluble Parametersmentioning

confidence: 99%

Reparixin, a Specific Interleukin-8 Inhibitor, Has No Effects on Inflammation during Endotoxemia

Leitner

Mayr

Firbas

et al. 2007

Int J Immunopathol Pharmacol

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Reparixin antagonizes interleukin-8 (IL-8) on the level of signal transduction in vitro. We hypothesized that IL-8 mediates some of the reactions occurring during acute inflammation and specifically that IL-8 may be a mediator of endotoxin induced neutrophilia. We therefore tested the effects of reparixin on humoral and cellular parameters in LPS-induced acute systemic inflammation. The study is a randomized (3:2 active:placebo), double-blind, placebo-controlled parallel group trial. Twenty healthy male volunteers randomly received either reparixin (12) or placebo (8) intravenously. One hour after the start ofreparixin/placebo infusion a bolus of2 ng/kg endotoxin was infused over t-2 min. Blood samples were obtained over 24 h. Reparixin, being metabolized to ibuprofen, suppressed serum thromboxane 82 levels by 78% compared to baseline and control at 8 h. LPS-induced neutrophilia was not significantly affected by reparixin in human volunteers. Consistently, reparixin did not alter the lymphocyte or monocyte counts and had no effect on LPS-induced systemic inflammation as measured by tumor necrosis factor alpha (TNF-a) or interleukin-6 (IL-6) release. Regulation of IL-8 receptors CXCRt and 2 and the degranulation marker CDllb showed the expected kinetics. Reparixin had no effect on thrombin formation as measured by prothrombin fragment (F 1 + 2 ) . In conclusion, our study showed that reparixin was safe but had no impact on endotoxin induced inflammation. In contrast to previous studies with its metabolite ibuprofen, reparixin does not enhance inflammation in this model.Reparixin is a small molecule, which is structurally related to the known anti-inflammatory drug ibuprofen. It was developed as a novel, potent and specific inhibitor of the chemokine interleukin-8 (IL-8) on the level of intracellular signal transduction (1). Reparixin acts as a noncompetitive allosteric inhibitor of IL-8 receptors (CXCRI/2) which, by locking CXCR1I2 in an inactive conformation, prevents receptor signalling and human polymorphonuclear leukocyte (PMN) chemotaxis. IL-8 is responsible for several reactions occurring during acute inflammation and is able to induce neutrophilia (2-3). In particular, IL-8 infusion markedly increases neutrophil counts in non-human primates (2). Interleukin-8 induced neutrophilia results from demargination or by a release of neutrophils from bone marrow (3). In circulating monocytes, IL-6 and IL-8 induce tissue factor

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Impaired Platelet Function among Platelet Donors

Cited by 65 publications

References 34 publications

A nonerythropoietic derivative of erythropoietin protects the myocardium from ischemia–reperfusion injury

A nonerythropoietic derivative of erythropoietin protects the myocardium from ischemia–reperfusion injury

New Insights into Nephrogenic Systemic Fibrosis

Reparixin, a Specific Interleukin-8 Inhibitor, Has No Effects on Inflammation during Endotoxemia

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