Animal models of human lipid metabolism

Suckling, Keith E.; Jackson, Brian

doi:10.1016/0163-7827(93)90002-e

Cited by 55 publications

(43 citation statements)

References 226 publications

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“…This discrepancy may have resulted from the differences in the diet composition, especially dietary cholesterol and fat levels, bile acid supplementation, and the time of BBR administration between the present study and previous studies [13,26,42,43]. It could also be due to the differences in cholesterol metabolism between humans and animal species [44][45][46]. In addition, it should be noted that the effect of BBR on blood cholesterol in rats was previously examined only in disease models such as diabetes or nephritis [42,43,47].…”

Section: Discussioncontrasting

confidence: 63%

Co-administration of berberine and plant stanols synergistically reduces plasma cholesterol in rats

Xiao-ming¹,

Chen

Zidichouski³

et al. 2008

Atherosclerosis

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The objective of the present study was to determine the beneficial effects and the safety of oral administration of the combination of berberine (BBR) and plant stanols (PS) on plasma lipid profiles in male Sprague-Dawley rats. Four groups of animals were fed a cornstarch-casein-sucrose-based high-cholesterol (2%, w:w) and high-fat (27.5%) diet. Three treatment groups were supplemented with either BBR (100 mg kg −1 body weight d −1 ), PS (1% in diet, w:w), or the combination of both (BBRPS). After 6 wk, animals were sacrificed and followed immediately with the collection of blood and organ samples. Lipid analysis revealed that PS lowered plasma total cholesterol (T-C) by 18% (p = 0.067) and non-HDL-cholesterol (non-HDL-C) by 29% (p = 0.013) as compared with the control, while BBR had no effect on both T-C and non-HDL-C. The combination treatment of BBRPS reduced plasma T-C by 41% (p = 0.0002) and non-HDL-C by 59% (p < 0.0001) compared to the control group. BBR reduced plasma TG levels by 31% at a marginal significance relative to the control (p = 0.054), whereas PS had no effect. BBRPS showed an additive effect of BBR and PS on plasma TAG. PS and BBRPS both decreased liver cholesterol (p = 0.0027 and 0.0002, respectively). BBR and PS, either alone or in combination, did not show any toxic effects as assessed by plasma concentration of hepatic biochemical parameters. These results demonstrate that BBR and PS, when combined, synergistically lower plasma cholesterol levels and significantly reduce liver cholesterol, without the observation of any toxic effects. Crown

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Section: Discussioncontrasting

confidence: 63%

Co-administration of berberine and plant stanols synergistically reduces plasma cholesterol in rats

Xiao-ming¹,

Chen

Zidichouski³

et al. 2008

Atherosclerosis

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“…The phenotype should resemble the human physiological condition as closely as possible in both the normal and diseased state (Moghadasian et al, 2001). There are additional practical issues to consider such as the size of the animal and housing requirements, generation times, and the specific cost of overall maintenance, including food, daily care, and experimental treatment (Moghadasian et al, 2001;Suckling, & Jackson, 1993). These concerns become especially important with the development of transgenic models, in that the associated investment costs are much higher than with traditional animal studies.…”

Section: Animal Models Of Atherogenesis 41 Mammalsmentioning

confidence: 99%

“…Subsequently, over 600 human LDLR gene mutations similar to FH that trigger varying degrees of hypercholesterolemia have been identified (Goldstein & Brown, 2001). In addition, hamsters, rabbits and primates have repeatedly shown reduced functional capacity of hepatic receptors in response to a high fat (Suckling & Jackson, 1993) diet. Individual LDLR activity varied in response to dietary fat and cholesterol because primates, like humans, dogs, and rabbits can be hypo-or hyperresponsive to diet (Goldstein & Brown, 2001;Moghadasian et al, 2001;Overturf et al, 1990;Stein et al, 2002), with some individuals demonstrating unique resistance.…”

Section: Animal Models Of Atherogenesis 41 Mammalsmentioning

confidence: 99%

“…Selected disease characteristics in animal models with their relationship to the human atherosclerosis are presented in Table 1. Animal lipid metabolism studies become complicated because the majority of circulating cholesterol is in HDL (Suckling & Jackson, 1993) for most species except humans who utilize LDL (Garcia et al, 2001). For example, a decrease in plasma HDL has been associated with a reduced risk of atherosclerosis in mice (Breslow, 2000).…”

Section: Animal Models Of Atherogenesis 41 Mammalsmentioning

confidence: 99%

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Spontaneous Atherosclerosis in Pigeons: A Good Model of Human Disease

Anderson¹,

Smith²,

Taylor³

2012

Atherogenesis

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“…Rat hepatocytes have been used to study the effects of CAMP on cholesterol and bile acid synthesis [13--15], but it has become recognised recently that the hamster may be a better model for cholesterol metabolism in the human in a number of important respects [16]. Cell-permeable CAMP analgues have been developed to facilitate studies with intact cells, and many of these compounds have the additional advantage that they bind preferentially to a specific binding site on the CAMP-dependent protein kinase and are often more potent than the parent compound [17].…”

Section: Introductionmentioning

confidence: 99%

The effect of cyclic AMP analogues and glucagon on cholesteryl ester synthesis and hydrolysis in cultured hamster hepatocytes

et al. 1993

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Two cyclic AMP analogues, l-chloro cyclic AMP and 8-(4 chlorophenyltbio) cyclic AMP, were found to increase the incorporation of rHJoleate into cholereryl ester in cultured hamster hapatocytes (30-40%), while incorporation into triacylglycerol was unaffected. An increase of a similar magnitude was observed in the presence of glucagon and the phosphodiesterase inhibitor, theophylline. The cyclic AMP analogues also stimulated the activity of neutral cholesteryl ester hydrolase in the cells, and this effect was mimicked by glucagon and theophylline. These results show that cyclic AMP can affect the cholesteryl ester cycle in hamster hepatocytes, and support the idea that the enzymes involved may be co-ordinately regulated.

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Animal models of human lipid metabolism

Cited by 55 publications

References 226 publications

Co-administration of berberine and plant stanols synergistically reduces plasma cholesterol in rats

Co-administration of berberine and plant stanols synergistically reduces plasma cholesterol in rats

Spontaneous Atherosclerosis in Pigeons: A Good Model of Human Disease

The effect of cyclic AMP analogues and glucagon on cholesteryl ester synthesis and hydrolysis in cultured hamster hepatocytes

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