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Biological Trace Element Research - In persons who had accumulated radiocesium from the fallout of the Chernobyl nuclear reactor accident, the amount of radiocesium and radiopotassium was measured...  相似文献   

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The effects of infant diet (breast milk or formula containing 2, 30 or 60 mg/dl cholesterol) and subsequent dietary cholesterol (0.02, 1.0 or 1.7 mg/kcal) and fat (saturated or unsaturated) on heparin-releasable lipolytic activity from omental adipose tissue was estimated from 99 baboons of 5-8 years of age. This lipase activity was characterized as lipoprotein lipase based on salt inhibition and apolipoprotein C-II activation. Lipoprotein lipase activity released from adipose tissue by heparin was significantly (P less than 0.002) lower in high cholesterol-fed baboons than in those fed low cholesterol. Most of this difference was due to impaired long-term heparin release of lipoprotein lipase. Adipose tissue lipoprotein lipase increased with increasing fat cell size regardless of diet, but there was no effect of diet on adipocyte size. There were no significant effects of infant cholesterol intake nor adult saturated or unsaturated fat on lipoprotein lipase activity. Adult baboons breast fed as infants had lower adipose tissue lipoprotein lipase activity (P less than 0.07) than adults fed formula as infants.  相似文献   

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The objectives of the present paper were to review and quantitatively determine the influence of the nutritional factors on whole body glucose turnover in growing and adult non-productive ruminants. A meta-analysis approach was used. The dietary grain: forage ratio significantly increased the slope of the relationship between glucose turnover and metabolisable energy intake. This effect was probably associated with the inclusion of maize rather than any other grain source in the diet. The analysis pointed out the possible differences in response between growing and adult non-productive animals, and suggested that the performance level of the animals (and their glucose requirements) could contribute to regulating whole body glucose turnover. This aspect would warrant further investigation.  相似文献   

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In 23 patients, the decay curves of serum cholesterol specific activity after a single intravenous dose of radioactive cholesterol were measured for 16-66 wk and were subjected to computerized input-output analysis. Of 17 patients with decay curves followed for longer than 50 wk, a three-exponential curve fit was better in 12, and a two-exponential curve fit in 5, according to computerized F tests. Of six patients with decay curves followed for less than 50 wk, a two-exponential curve fit was better in five and a three-exponential curve fit in one. In the 13 patients who exhibited three-exponential curve fits, the third exponential appeared after 13-43 wk of observation (average, 25 wk). In 12 patients of this group who were followed for 50 wk or more, turnover rates and exchangeable masses of cholesterol were measured at maximum lengths of the curves (50-66 wk), and these parameters were then compared with measurements made with curves successively shortened down to 10-12 wk. The average differences between analyses of the minimum vs. the maximum lengths of the curves were: It (input rate: absorbed dietary plus biosynthesized cholesterol), 14% larger (1.24 vs. 1.09 g/day); M(a) (rapidly exchangeable mass of cholesterol), no change (34 vs. 33 g); M (total exchangeable mass), 26% smaller (67 vs. 91 g); M - M(a) (remaining exchangeable mass), 39% smaller (40 vs. 65 g). Significant differences in It, M, and M - M(a) (minimum vs. maximum curve lengths) were found in both normolipidemic and hypercholesterolemic patients, and the differences were of similar magnitude in the two groups. Since only 12 of 17 patients followed for 50 wk or longer demonstrated three-exponential curve fits, various means were sought by which it might be predicted at the outset whether a given patient must be studied for so long a time; none was found. However, in the group with two exponentials the value of M(a) was significantly larger than those with three-exponential curve fits, and this difference was apparent at as early as 10-12 wk.  相似文献   

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The effects of polyunsaturated, monounsaturated and saturated dietary fat on total and hepatic cholesterol synthesis were studied in the guinea-pig. Male Hartley guinea-pigs were fed semi-synthetic diets containing 7.5% (w/w) of either corn oil (CO), olive oil (OL) or lard for a period of 5 weeks and rates of endogenous cholesterol synthesis were determined from the incorporation of [3H]water into digitonin-precipitable sterols (DPS) and by measurement of sterol balance. In addition, total and expressed 3-hydroxy-3-methylglutaryl coenzyme A (HMG-CoA) reductase activities were determined in hepatic microsomes. Rates of whole body cholesterol synthesis determined by incorporation of [3H]water into DPS were significantly lower for guinea-pigs on the CO diet with values of 18.7 +/- 1.8 mumol/h (n = 4) vs. 26.7 +/- 4.8 and 24.6 +/- 1.8 mumol/h for animals on the OL (n = 4) and lard (n = 3) diets (P less than 0.001), respectively. Hepatic cholesterol synthesis rates were significantly decreased in animals on the OL diet, whether determined from incorporation of [3H]water into DPS or by analysis of HMG-CoA reductase activity. Hepatic total and free cholesterol levels were not different for animals on the three dietary fats; however, cholesteryl ester levels were 35% lower in guinea-pigs fed the lard diet (P less than 0.02). Sterol balance measurements indicated that whole body cholesterol synthesis rates were not affected by dietary fat quality (51.9 +/- 12.2, 42.8 +/- 7.6 and 51.2 +/- 20.2 mg/kg per day for animals on the CO, OL and lard diets, respectively). This is in striking contrast to the observed reduction in cholesterol synthesis rates for animals on the polyunsaturated CO diet as determined by incorporation of [3H]water into DPS. One possible explanation for the discrepancy between the sterol balance and [3H]water incorporation data is a polyunsaturated fat-mediated effect on energy utilization, which affects the equilibration of NADPH with the body water pool such that the [3H]NADPH has a lower specific activity than body [3H]water.  相似文献   

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Genetic effects on serum high density lipoprotein (HDL) cholesterol concentration and several parameters of a two-pool model of cholesterol metabolism were investigated in 79 baboons, the progeny of 6 sires. Significant differences (P less than 0.05) were observed among the sire progeny groups for HDL cholesterol (HDL-C), cholesterol production rate, cholesterol mass of pool A, and the rate constants KA and KAB. Rank correlations (rs) revealed that the sire progeny group means for HDL-C are closely correlated with those for the cholesterol mass of pool A (rs = 0.89), KA (rs = -0.78), and KAB (rs = -0.94). These strong correlations suggest that pool A, KA, and KAB are influenced to a large degree by the same genes that regulate HDL-C concentration. The strong inverse relationship (rs = -0.78) between HDL-C and KA suggests that the differences among these sire progeny groups for HDL-C are due chiefly to those metabolic processes which regulate cholesterol excretion from pool A. This conclusion is consistent with reports that HDL-C is a preferred precursor for bile acid synthesis.  相似文献   

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A number of studies have been conducted on serum cholesterol disappearance following a single injection of tracer. They have shown 2 or 3 component curves depending on the length of time of observation. They have been interpreted to indicate pools of cholesterol in fast or slow equilibrium with serum and generally depicted as representing groups of tissues. A cholesterol kinetic study was conducted using rats so that each tissue could be analyzed for appearance-disappearance of cholesterol from 30 minutes to 75 days.Serum and liver appeared to die-away for 30 days in a 2 component configuration, then exhibited a repetition of the same curve in the next 30 days. Skeletal muscle and kidney had a slow buildup for 2 weeks, then a plateau for 2 weeks then a 2 component die-away. Adipose showed a high plateau from 30 minutes to 30 days then a 2 component die-away, with specific activity higher than serum at all times.The data are interpreted to indicate that adipose tissue sequestered part of the tracer dose and all tissues reached equilibrium at about 30 days. After that time all tissues had a statistically significant 2 component die-away curve. The mathematical models tested suggest that in the steady state, cholesterol enters and exits the slow pool of serum, kidney, muscle and adipose and in liver enters both pools. Interpretation of the complete die-away is that the tracer dose first equilibrates with membrane free cholesterol, then with the intracellular cholesterol, and finally dies-away at the rate of release by the slow intercellular pool.  相似文献   

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《Autophagy》2013,9(7):1037-1038
In a recent study, we investigated the relationship between inclusion body (IB) formation and the activity of the ubiquitin-

proteasome system (UPS) in a primary neuron model of Huntington disease. We followed individual neurons over the

course of days and monitored the level of mutant huntingtin (htt) (which causes Huntington disease), IB formation, UPS function,

and neuronal toxicity. The accumulation of UPS substrates and neuronal toxicity increased with increasing levels of proteasome

inhibition. The UPS was more impaired in neurons that subsequently formed IBs than in those that did not; however, after IBs

formed, UPS function improved. These findings suggest that IB formation is a protective cellular response mediated in part by

increased degradation of intracellular protein.  相似文献   

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Butyrylcholinesterase (BChE) has proven to be an effective bioscavenger against nerve agents and organophosphates. Phase I safety trials of human BChE are currently being conducted and large-scale production of recombinant BChE is underway. Information on the real-time distribution of BChE from the injection site has not been well characterized. This study utilized the BChE nullizygote (BChE-/-) mouse and tetrameric equine BChE labeled with LI-COR((R)) fluorescent IRDye 800CW to track, quantify and determine the retention time of BChE in vivo following intramuscular injection. In vivo images were acquired with Xenogen's IVIS((R)) 200 imager and the LI-COR Odyssey((R)) Imaging System fitted with the MousePODtrade mark. Plasma and tissues were tested for BChE activity. The 2mg of BChE spread from the injection site to heart, liver, intestine, kidneys, lungs, salivary glands, and muscle, but did not enter the brain or the skin. Fluorescence intensity in organs and BChE activity in plasma peaked on day 1. BChE activity in plasma was undetectable by day 16, at a time when there was still significant fluorescent signal and BChE activity in the liver (0.32units/g), injected quadriceps (0.13units/g) and in most of the organs analyzed. It is concluded that the tetrameric BChE glycoprotein of 340kDa diffuses from the muscle injection site to blood and peripheral organs and has a longer residence time in the organs than in blood.  相似文献   

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