ผลต่างระหว่างรุ่นของ "หน้าหลัก"
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| − | + | Ained bioavailable in plasma. Conversely, RBC MP {levels|ranges|amounts|stages | |
| − | + | Ained bioavailable in plasma. Conversely, RBC MP stages ended up greater in continual state SCD MP, with enhanced imply fluorescence intensities (MFI), but identical sizing vs. controls. SCD MP bore far more PS available to annexin-A5 at their area plus the equilibrium concerning PS and annexin-A5 was compromised. In VOC, MP levels were being greater even even more and bore cytotoxic heme and CD235a. We nonetheless observed practically no ligand-free annexin-A5.This advised that endogenous annexin-A5 could possibly be consumed by surplus PS externalization in SCD, and insufficient to neutralize the substantial levels of PS' MP made by RBC through hemolysis. In SCD, the therapeutic utilization of recombinant annexin-A5 may so aid compensate the imbalance involving PS' MP and annexin-A5.PT2.Exosomes launched from sulforaphane-treated fibroblasts safeguard the cardiomyocytes from angiotensin II-induced hypertrophy Gaia Papini1, Marco Matteucci1, Enrica Ciofini1,2, Vincenzo Lionetti1,one Scuola Superiore Sant'Anna, Institute of Daily life Sciences, Pisa, Italy; 2Fondazione Toscana ``G. Monasterio'', Pisa, ItalyPT2.An imbalance concerning circulating microparticles and annexin-A5 might market vascular injuries through sickle mobile illness Sihem Sadoudi1, Dominique Charue2, Chantal Boulanger2, Sylvain Le Jeune3 and Olivier Blanc-Brude1 INSERM; 2Institute of Wellness and Clinical Study, Paris, France; 3Assistance Publique-Hopitaux De Paris, Paris, FranceChronic hemolytic anemia, like sickle cell illness (SCD) is characterised by painful vaso-occlusive crises (VOC), vascular injury, red blood cell (RBC) aggregation and vesiculation, and intravascular hemolysis. At continuous point out, RBC launch haemoglobin, heme and microparticles (MP) [https://www.ncbi.nlm.nih.gov/pubmed/27907933 PubMed ID:https://www.ncbi.nlm.nih.gov/pubmed/27907933] in plasma. This will increase yet again two-fold through VOC. MP from pressured RBC express phosphatidylserine (PS) at their surface and comprise cytotoxic heme. Alternatively, annexinA5 is really an intracellular protein introduced in plasma throughout mobile worry. Annexin-A5 acts to be a PS inhibitor, neutralizing PS-mediated consequences in stressed cells and MP. We collected plasma from cohorts of SCD people during continuous condition, or VOC, and controls. We designed a novel ELISA-based assay to seize PS' MP using an anti-annexin-A5 antibody. It quantified annexin-A5-covered MP in plasma, but also believed ligand-free functional annexin-A5. We characterised plasma MP by FACS with labelling of ligand-free PS with annexin-Introduction: The interaction among fibroblasts and cardiomyocytes underlies the pathological cardiac hypertrophy induced by angiotensin-II (AngII), which contributes to coronary heart failure. Fibroblastderived exosomes (F-Exo) have been implicated in mediating AngII-induced cardiomyocyte hypertrophy. Having said that, how release of anti-hypertrophic F-Exo is induced, remains an unanswered challenge. Sulforaphane (SFN), a naturally taking place isothiocyanate extracted from cruciferous veggies, attenuates AngII-induced cardiomyocytes hypertrophy. We examined the results of SFN over the release of anti-hypertrophic F-Exo in vitro. Approaches: Murine embryo fibroblasts had been taken care of with non-toxic dose of SFN (3 mM/7 times). Intact F-Exo have been isolated from mobile culture media by differential centrifugation. F-Exo have been quantified by Western blot employing CD63. Hypertrophy of HL-1 cardiomyocytes [https://www.ncbi.nlm.nih.gov/pubmed/17763406 PubMed ID:https://www.ncbi.nlm.nih.gov/pubmed/17763406] was induced by AngII (a hundred nM/12 h). Mobile viability was assessed by MTT assay. Cell surface area location, an indicator of cell hypertrophy, was measured just after 3 or 24 h incubation with 30 mg exosomes isolated from SFN-treated (SFN-F-Exo). | |
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รุ่นแก้ไขเมื่อ 12:47, 20 ตุลาคม 2564
Ained bioavailable in plasma. Conversely, RBC MP {levels|ranges|amounts|stages Ained bioavailable in plasma. Conversely, RBC MP stages ended up greater in continual state SCD MP, with enhanced imply fluorescence intensities (MFI), but identical sizing vs. controls. SCD MP bore far more PS available to annexin-A5 at their area plus the equilibrium concerning PS and annexin-A5 was compromised. In VOC, MP levels were being greater even even more and bore cytotoxic heme and CD235a. We nonetheless observed practically no ligand-free annexin-A5.This advised that endogenous annexin-A5 could possibly be consumed by surplus PS externalization in SCD, and insufficient to neutralize the substantial levels of PS' MP made by RBC through hemolysis. In SCD, the therapeutic utilization of recombinant annexin-A5 may so aid compensate the imbalance involving PS' MP and annexin-A5.PT2.Exosomes launched from sulforaphane-treated fibroblasts safeguard the cardiomyocytes from angiotensin II-induced hypertrophy Gaia Papini1, Marco Matteucci1, Enrica Ciofini1,2, Vincenzo Lionetti1,one Scuola Superiore Sant'Anna, Institute of Daily life Sciences, Pisa, Italy; 2Fondazione Toscana ``G. Monasterio, Pisa, ItalyPT2.An imbalance concerning circulating microparticles and annexin-A5 might market vascular injuries through sickle mobile illness Sihem Sadoudi1, Dominique Charue2, Chantal Boulanger2, Sylvain Le Jeune3 and Olivier Blanc-Brude1 INSERM; 2Institute of Wellness and Clinical Study, Paris, France; 3Assistance Publique-Hopitaux De Paris, Paris, FranceChronic hemolytic anemia, like sickle cell illness (SCD) is characterised by painful vaso-occlusive crises (VOC), vascular injury, red blood cell (RBC) aggregation and vesiculation, and intravascular hemolysis. At continuous point out, RBC launch haemoglobin, heme and microparticles (MP) PubMed ID:https://www.ncbi.nlm.nih.gov/pubmed/27907933 in plasma. This will increase yet again two-fold through VOC. MP from pressured RBC express phosphatidylserine (PS) at their surface and comprise cytotoxic heme. Alternatively, annexinA5 is really an intracellular protein introduced in plasma throughout mobile worry. Annexin-A5 acts to be a PS inhibitor, neutralizing PS-mediated consequences in stressed cells and MP. We collected plasma from cohorts of SCD people during continuous condition, or VOC, and controls. We designed a novel ELISA-based assay to seize PS' MP using an anti-annexin-A5 antibody. It quantified annexin-A5-covered MP in plasma, but also believed ligand-free functional annexin-A5. We characterised plasma MP by FACS with labelling of ligand-free PS with annexin-Introduction: The interaction among fibroblasts and cardiomyocytes underlies the pathological cardiac hypertrophy induced by angiotensin-II (AngII), which contributes to coronary heart failure. Fibroblastderived exosomes (F-Exo) have been implicated in mediating AngII-induced cardiomyocyte hypertrophy. Having said that, how release of anti-hypertrophic F-Exo is induced, remains an unanswered challenge. Sulforaphane (SFN), a naturally taking place isothiocyanate extracted from cruciferous veggies, attenuates AngII-induced cardiomyocytes hypertrophy. We examined the results of SFN over the release of anti-hypertrophic F-Exo in vitro. Approaches: Murine embryo fibroblasts had been taken care of with non-toxic dose of SFN (3 mM/7 times). Intact F-Exo have been isolated from mobile culture media by differential centrifugation. F-Exo have been quantified by Western blot employing CD63. Hypertrophy of HL-1 cardiomyocytes PubMed ID:https://www.ncbi.nlm.nih.gov/pubmed/17763406 was induced by AngII (a hundred nM/12 h). Mobile viability was assessed by MTT assay. Cell surface area location, an indicator of cell hypertrophy, was measured just after 3 or 24 h incubation with 30 mg exosomes isolated from SFN-treated (SFN-F-Exo).
