Title: L-arginine administration ameliorates serum and pulmonary cytokine response after gut ischemia-reperfusion in immature rats
Abstract: AIM: Small intestinal ischemia-reperfusion (IR) has been demonstrated to result in both local mucosal injury and systemic injuries. The exact role of nitric oxide (NO) in intestinal IR is unclear. We propose that NO and some other cytokines change in the reperfusion period and these changes are associated with lung injury. The aim of this study was to determine the effect of supplementing NO substrate, L-arginine (L-arg), on serum and pulmonary cytokine production during small intestinal IR in immature rats.METHODS: Immature rats underwent 60 min. of superior mesenteric artery occlusion followed by 90 min of reperfusion. L-arg (250 mg/kg) was given intravenously to the experimental group (IR+L-arg) which received L-arg after 45 min of intestinal ischemia. Serum and lung endothelin-1 (ET-1), NO, malondialdehyde (MDA), and tumor necrosis factor α (TNFα) were measured. Sham operation (SHAM) and intestinal IR (IR) groups were performed as control. The lavage fluid of the lung was collected by bronchoalveolar lavage (BAL) and white blood cells and polymorphonuclear cells (PMNs) were immediately counted to identify lung damage.RESULTS: When L-arg was given during small intestinal IR, serum NO concentration increased significantly in IR+L-arg group (162.17±42.93 μmol/L) when compared with IR group (87.57±23.17 μmol/L, t= 3.190, P = 0.008<0.01). Serum MDA reduced significantly in IR+L-arg group (8.93±1.50 nmol/L) when compared with SHAM(23.78±7.81 nmol/L, t = 3.243, P = 0.007<0.01) and IR (25.54±9.32 nmol/L, t = 3.421, P = 0.006<0.01).ET-1 level in lung tissues was significantly lower in IR+L-arg group (13.81±7.84 pg/mL) than that in SHAM(35.52±10.82 pg/mL, t = 2.571, P= 0.03<0.05) and IR(50.83±22.05 pg/mL, t = 3.025, P = 0.009<0.01) groups.MDA contents in lung tissues were significantly lower in IR+L-arg group (10.73±1.99 nmol/L) than in SHAM(16.62±2.28 nmol/L, t = 3.280, P = 0.007<0.01) and IR(21.90±4.82 nmol/L, t= 3.322, P= 0.007<0.01)groups.Serum and lung TNFα concentrations were not sig
Publication Year: 2005
Publication Date: 2005-01-01
Language: en
Type: article
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