Abnormal modulation of cell protective systems in response to ischemic/reperfusion injury is important in the development of mouse sickle cell hepatopathy

Siciliano, Angela; Malpeli, Giorgio; Platt, Orah S.; Lebouef, Christophe; Janin, Anne; Scarpa, Aldo; Olivieri, Oliviero; Amato, Eliana; Corrocher, Roberto; Beuzard, Yves; Franceschi, Lucia De

doi:10.3324/haematol.2010.028506

Cited by 27 publications

(28 citation statements)

References 43 publications

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“…10 While studying the transgenic mouse model for SCD exposed to ischemia/reperfusion stress, Siciliano et al elucidated additional mechanisms that disrupt NO homeostasis. 4 Their results, published in this month's issue of Haematologica, show that the sickle cell hepatopathy in SAD mice is associated with an imbalance of endothelial/inducible NO synthase and lack of heme oxygenase-1/biliverdin reductase cytoprotection. In addition, up-regulation of phosphodiesterase-4 genes is noted in hepatocytes in response to ischemia/reperfusion stress.…”

Section: Mechanisms Of Vasculopathymentioning

confidence: 99%

“…These and other manifestations result from chronic hemolysis and intermittent episodes of vascular occlusion that cause both acute and chronic tissue injury and organ dysfunction. 2,3 Two articles in this issue of Haematologica explore unique mechanisms leading to organ damage and clinical sequelae in both the transgenic mouse model for SCD (SAD mice) 4 and in children with SCD, 5 exemplifying the advancements in our knowledge achieved over the last 100 years.…”

Section: T His Year Marks the 100mentioning

confidence: 99%

“…Inhibition of phosphodiesterase-4 by rolipram attenuated ischemia/reperfusionrelated vasculopathy and inflammation, while inducing the heme oxygenase-1/biliverdin reductase cytoprotective systems, leading to improved hepatocellular survival. 4 The…”

Section: Mechanisms Of Vasculopathymentioning

confidence: 99%

“…1,2 In the last decade, however, such deaths have been significantly reduced. [2][3][4][5] This improvement has been attributed in part to greater iron chelation options and the ability to recognize pre-clinical cardiac iron deposition by Magnetic Resonance Imaging studies (MRI). Patients with low cardiac T2*, as measured by MRI, have a significant risk of developing overt heart failure over a 12-month period if changes to their chelation regime are not made (Figure 1).…”

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Vascular risk assessment in patients with sickle cell disease

Morris¹

2010

Haematologica

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Section: Mechanisms Of Vasculopathymentioning

confidence: 99%

Section: T His Year Marks the 100mentioning

confidence: 99%

Section: Mechanisms Of Vasculopathymentioning

confidence: 99%

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Vascular risk assessment in patients with sickle cell disease

Morris¹

2010

Haematologica

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“…The lung and liver pathology were analyzed and the liver pathological score, inflammatory cell infiltrate and presence of thrombi were determined by blinded pathologists as previously described. 19,23 Details on the histological analysis are provided in the Online Supplementary Materials and Methods.…”

Section: Histological Analysismentioning

confidence: 99%

Dietary -3 fatty acids protect against vasculopathy in a transgenic mouse model of sickle cell disease

et al. 2015

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The anemia of sickle cell disease is associated with a severe inflammatory vasculopathy and endothelial dysfunction, which leads to painful and life-threatening clinical complications. Growing evidence supports the anti-inflammatory properties of ω-3 fatty acids in clinical models of endothelial dysfunction. Promising but limited studies show potential therapeutic effects of ω-3 fatty acid supplementation in sickle cell disease. Here, we treated humanized healthy and sickle cell mice for 6 weeks with ω-3 fatty acid diet (fish-oil diet). We found that a ω-3 fatty acid diet: (i) normalizes red cell membrane ω-6/ ω-3 ratio; (ii) reduces neutrophil count; (iii) decreases endothelial activation by targeting endothelin-1 and (iv) improves left ventricular outflow tract dimensions. In a hypoxia-reoxygenation model of acute vaso-occlusive crisis, a ω-3 fatty acid diet reduced systemic and local inflammation and protected against sickle cell-related end-organ injury. Using isolated aortas from sickle cell mice exposed to hypoxia-reoxygenation, we demonstrated a direct impact of a ω-3 fatty acid diet on vascular activation, inflammation, and anti-oxidant systems. Our data provide the rationale for ω-3 dietary supplementation as a therapeutic intervention to reduce vascular dysfunction in sickle cell disease. ABSTRACTmice. 16,17 The animal protocol was approved by the Animal Care and Use Committee of the University of Verona (CIRSAL). Twomonth old animals were fed for 6 weeks with either the standard AIN-93M purified rodent diet (soy-diet with n6/n3 ratio of 8:1 -Dyets Inc., Bethlehem, PA, USA), containing 140 g/kg casein, 1.8 g/kg L-cystine, 100 g/kg sucrose, 465.9 g/kg cornstarch, 155 g/kg dextrose, 40 g/kg soybean oil, 0.8 mg/kg t-butylhydroquinone, 50 g/kg cellulose, 35 g/kg mineral mix, 10 g/kg vitamin mix, and 2.5 g/kg choline bitartrate 18 or the ω-3 FD, an AIN-93M-based purified rodent diet in which all of the calories provided by fat (10%) are replaced by 7.9% from HCO and 2.1% from ω-3 oil (Dyets Inc., Bethlehem, PA, USA). At the end of the 6 weeks of FD supplementation, animals were anesthetized with isofluorane, and whole blood was collected from each mouse via retro-orbital venipuncture by heparinized microcapillaries. Mice were euthanized and organs removed immediately. The organs were divided into two and either frozen immediately in liquid nitrogen or fixed in 10% formalin and embedded in paraffin for histology. Whenever indicated, 6-week old mice were exposed to hypoxia (8% oxygen for 10 h) followed by 3 h of reoxygenation (21% oxygen) (H/R stress) to mimic an acute VOC, as previously described.

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