Liver fat reduction with niacin is influenced by DGAT-2 polymorphisms in hypertriglyceridemic patients

Hu, Miao; Chu, Winnie C.W.; Yamashita, Shizuya; Yeung, D.; Shi, Liming; Wang, Defeng; Masuda, Daisuke; Yang, Ya‐Ling; Tomlinson, Brian

doi:10.1194/jlr.p023614

Cited by 65 publications

(69 citation statements)

References 33 publications

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“…In order to extend the use of niacin for other indications, we recently showed that niacin prevented the accumulation of fat in liver and regressed pre-existing hepatic steatosis in high-fat fed rat model of NAFLD [16]. In support of our study in experimental NAFLD model, Hu et al in a small uncontrolled study in 39 patients recently showed that niacin therapy (2 g/day) significantly reduced liver fat content in Chinese patients with hypertriglyceridemia [17]. However, hepatocellular mechanisms of action of niacin on pathophysiological events involved in NAFLD are not known.…”

supporting

confidence: 86%

“…Although increased levels of alanine aminotransferase and/or aspartate aminotransferase were observed in some patients taking higher concentrations of niacin as compared to placebo, the levels of these enzymes were not greater than 3 times the upper limit in majority of the patients [57,60]. In fact, in a recent uncontrolled study in dyslipidemic patients with steatosis, niacin administration (2 g/day for 16 weeks) improved liver enzymes including alanine aminotransferase, gammaglutamyl transferase, and alkaline phosphatase [17]. These initial clinical observations are consistent with the potentially beneficial effect of niacin on fat accumulation and antioxidant effects as suggested in this and our original report in a rat NAFLD model [16].…”

Section: Discussionmentioning

confidence: 84%

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Niacin inhibits fat accumulation, oxidative stress, and inflammatory cytokine IL-8 in cultured hepatocytes: Impact on non-alcoholic fatty liver disease

2015

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supporting

confidence: 86%

Section: Discussionmentioning

confidence: 84%

Niacin inhibits fat accumulation, oxidative stress, and inflammatory cytokine IL-8 in cultured hepatocytes: Impact on non-alcoholic fatty liver disease

2015

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“…It is now evident that by inhibiting DGAT2, niacin would prevent hepatic steatosis associated with endogenous synthesis of fatty acids. Interestingly, the efficacy of niacin as an agent against fatty liver is dependent on DGAT2 polymorphisms of the individuals studied [94], confirming the central role of the enzyme in determining the rate of de novo TAG synthesis and, in turn, of the absolute rates of net de novo TAG synthesis by the liver.…”

Section: Implications Of the Sequential Action Of Dgat2 And Dgat1mentioning

confidence: 93%

Hepatic triacylglycerol synthesis and secretion: DGAT2 as the link between glycaemia and triglyceridaemia

Zammit

2013

Biochemical Journal

102

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lThe liver regulates both glycaemia and triglyceridaemia. Hyperglycaemia and hypertriglyceridaemia are both characteristic of (pre)diabetes. Recent observations on the specialised role of DGAT2 (diacylglycerol acyltransferase 2) in catalysing the de novo synthesis of triacylglycerols from newly synthesized fatty acids and nascent diacylglycerols identifies this enzyme as the link between the two. This places DGAT2 at the centre of carbohydrate-induced hypertriglyceridaemia and hepatic steatosis. This function is complemented, but not substituted for, by the ability of DGAT1 to rescue partial glycerides from complete hydrolysis. In peripheral tissues not normally considered to be lipogenic, synthesis of triacylglycerols may largely bypass DGAT2 except in hyperglycaemic/hyperinsulinaemic conditions, when induction of de novo fatty acid synthesis in these tissues may contribute towards increased triacylglycerol secretion (intestine) or insulin resistance (adipose tissue, and cardiac and skeletal muscle).

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“…In Chinese patients with hypertriglyceridemia extended-release niacin induced a reduction of liver fat content (Hu et al 2012). A polymorphism of DGAT-2 influenced the strength of this effect which demonstrates the significance of DGAT-2 modification within the action of niacin.…”

Section: Mechanisms Of Action Of Niacinmentioning

confidence: 98%

Niacin as antidyslipidemic drug

Julius

2015

Can. J. Physiol. Pharmacol.

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Niacin is an important vitamin (B3) that can be used in gram doses to positively modify pathogenetically relevant lipid disorders: elevated LDL cholesterol, elevated non-HDL cholesterol, elevated triglycerides, elevated lipoprotein(a), and reduced HDL cholesterol. This review reports the latest published findings with respect to niacin's mechanisms of action on these lipids and its anti-inflammatory and anti-atherosclerotic effects. In the pre-statin era, niacin was shown to have beneficial effects on cardiovascular end-points; but in recent years, two major studies performed in patients whose LDL cholesterol levels had been optimized by a statin therapy did not demonstrate an additional significant effect on these end-points in the groups where niacin was administered. Both studies have several drawbacks that suggest that they are not representative for other patients. Thus, niacin still plays a role either as an additive to a statin or as a substitute for a statin in statin-intolerant patients. Moreover, patients with elevated triglyceride and low HDL cholesterol levels and patients with elevated lipoprotein(a) concentrations will possibly benefit from niacin, although currently the study evidence for these indications is rather poor. Niacin may be useful for compliant patients, however possible side effects (flushing, liver damage) and contraindications should be taken into consideration.

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Liver fat reduction with niacin is influenced by DGAT-2 polymorphisms in hypertriglyceridemic patients

Cited by 65 publications

References 33 publications

Niacin inhibits fat accumulation, oxidative stress, and inflammatory cytokine IL-8 in cultured hepatocytes: Impact on non-alcoholic fatty liver disease

Niacin inhibits fat accumulation, oxidative stress, and inflammatory cytokine IL-8 in cultured hepatocytes: Impact on non-alcoholic fatty liver disease

Hepatic triacylglycerol synthesis and secretion: DGAT2 as the link between glycaemia and triglyceridaemia

Niacin as antidyslipidemic drug

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