S. E. Naumenko scite author profile

S. E. Naumenko

5Publications

31Citation Statements Received

84Citation Statements Given

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Affiliations

Institute of Physiology and Basic Medicine, Research Institute of Physiology and Fundamental Medicine of the Siberian Branch of the Russian Academy of Medical Sciences, Russian Academy of Sciences

Publications

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The Haemonetics(R) Cell Saver 5 washing properties: effect of different washing pump and centrifuge speeds

Naumenko¹,

Kim²,

Черканова³

et al. 2008

Interactive CardioVascular and Thoracic Surgery

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This study evaluated the effect of different washing and centrifuge rates of the Cell Saver 5 on the quality of processed autologous blood. Autologous blood was washed with 1000 ml of sterile normal saline at centrifuge speed of 5650 revolutions per minute (rpm) (group I) or 4350 rpm (group II) with different washing pump speeds--500, 800 and 1000 ml/min. Hemoglobin, free hemoglobin, hematocrit, erythrocytes, leukocytes, platelets, and protein were measured before and after processing. The highest values of hemoglobin, hematocrit and erythrocytes were achieved using 800 and 1000 ml/min pump speeds in group I and 500 ml/min speed in group II. Red blood cells concentration was higher in group I. There were no significant changes of free hemoglobin removal within group I. In group II the lowest free hemoglobin was achieved when 1000 ml/min rate was used. Platelets and protein did not depend on wash pump speeds in both groups. Platelet recovery in group I was higher than in group II at all washing pump speeds. Leukocytes were not adequately removed at all pump speeds. The Cell Saver 5 produces optimum results when the high wash pump speeds (800 and 1000 ml/min) and standard centrifuge speed are used.

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Cardioprotective Effect of Resveratrol and Resveratroloside

Naumenko¹,

Латышева²,

Gilinsky³

et al. 2014

CHAMC

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Cardioprotective effect of resveratrol and resveratroloside was determined in ischemia-reperfusion experiments on rats. It was found that single intraperitoneal administration of any compound (10 mg/kg) followed by 30-min ischemia and 120-min reperfusion resulted in statistically significant decrease of myocardial infarct area (55.0±4.0% for control group; 40.7±4.4% for the group 1 received resveratrol; 41.6±4.8% for the group 2 received resveratroloside). The cardioprotective effect of resveratroloside was detected for the first time.

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Norvaline Reduces Blood Pressure and Induces Diuresis in Rats with Inherited Stress‐Induced Arterial Hypertension

Gilinsky

Polityko

et al. 2020

BioMed Research International

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Growing evidence suggests that increased arginase activity affects vital bioprocesses in various systems and universally mediates the pathogenesis of numerous metabolic diseases. The adverse effects of arginase are associated with a severe decline in L-arginine bioavailability, which leads to nitric oxide synthase substrate insufficiency, uncoupling, and, eventually, superoxide anion generation and substantial reduction of nitric oxide (NO) synthesis. In cooperation, it contributes to chronic oxidative stress and endothelial dysfunction, which might lead to hypertension and atherosclerosis. Recent preclinical investigations point arginase as a promising therapeutic target in ameliorating metabolic and vascular dysfunctions. In the present study, adult rats with inherited stress-induced arterial hypertension (ISIAH) were used as a model of hypertension. Wistar rats served as normotensive controls. Experimental animals were intraperitoneally administered for seven days with nonproteinogenic amino acid L-norvaline (30 mg/kg/day), which is a potent arginase inhibitor, or with the vehicle. Blood pressure (BP), body weight, and diuresis were monitored. The changes in blood and urine levels of creatinine, urea, and NO metabolites were analyzed. We observed a significant decline in BP and induced diuresis in ISIAH rats following the treatment. The same procedure did not affect the BP of control animals. Remarkably, the treatment had no influence upon glomerular filtration rate in two experimental groups, just like the daily excretion of creatinine and urea. Conversely, NO metabolite levels were amplified in normotonic but not in hypertensive rats following the treatment. The data indicate that L-norvaline is a potential antihypertensive agent and deserves to be clinically investigated. Moreover, we suggest that changes in blood and urine are causally related to the effect of L-norvaline upon BP regulation.

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Inhibition of Norepinephrine Reuptake and Size of Myocardial Infarction during Focal Ischemia and after Preconditioning

Naumenko¹,

Latysheva²,

Gilinskii³

2010

Bull Exp Biol Med

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Methylated arginine analogues: their potential role in atherosclerosis and cognition using the poloxamer-407-induced mouse model of dyslipidemia

Gilinsky

Johnston

Zhukova

et al. 2016

Can. J. Physiol. Pharmacol.

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and anxiety relative to controls. Passive/avoidance testing to assess learning and memory provided suggestive evidence that poloxamer-treated mice could potentially be characterized as having undergone a disruption in the process of forgetting about an aversive event; specifically, a foot shock, when compared to control mice. Thus, it is also suggested that the increase in both plasma monomethylarginine and asymmetric dimethylarginine in poloxamer-407-treated mice may somehow influence learning and memory, since endothelial dysfunction caused by reduced nitric oxide availability has been hypothesized to negatively influence cognitive function.

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S. E. Naumenko

The Haemonetics(R) Cell Saver 5 washing properties: effect of different washing pump and centrifuge speeds

Cardioprotective Effect of Resveratrol and Resveratroloside

Norvaline Reduces Blood Pressure and Induces Diuresis in Rats with Inherited Stress‐Induced Arterial Hypertension

Inhibition of Norepinephrine Reuptake and Size of Myocardial Infarction during Focal Ischemia and after Preconditioning

Methylated arginine analogues: their potential role in atherosclerosis and cognition using the poloxamer-407-induced mouse model of dyslipidemia

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