Acetyl‐CoA Carboxylase Inhibition Reverses NAFLD and Hepatic Insulin Resistance but Promotes Hypertriglyceridemia in Rodents

Goedeke, Leigh; Bates, Jamie; Vatner, Daniel F.; Perry, Rachel J.; Wang, Ting; Ramírez, Ricardo; Li, Li; Ellis, Matthew W.; Wong, Kari E.; Beysen, Carine; Cline, Gary W.; Ray, Adrian S.; Shulman, Gerald I.

doi:10.1002/hep.30097

Cited by 191 publications

(189 citation statements)

References 44 publications

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“…), and pharmacological inhibition of ACC can decrease hepatic DNL and hepatic steatosis (Goedeke et al . ). This is, however, at the expense of hypertriglyceridaemia (Goedeke et al .…”

Section: Hepatic Lipid and Carbohydrate Handling Hepatic De Novo Lipmentioning

confidence: 97%

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Fructose and metabolic health: governed by hepatic glycogen status?

Hengist

Koumanov

Gonzalez

2019

The Journal of Physiology

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Fructose is a commonly ingested dietary sugar which has been implicated in playing a particularly harmful role in the development of metabolic disease. Fructose is primarily metabolised by the liver in humans, and increases rates of hepatic de novo lipogenesis. Fructose increases hepatic de novo lipogenesis via numerous mechanisms: by altering transcriptional and allosteric regulation, interfering with cellular energy sensing, and disrupting the balance between lipid synthesis and lipid oxidation. Hepatic de novo lipogenesis is also upregulated by the inability to synthesise glycogen, either when storage is inhibited in knock‐down animal models or storage is saturated in glycogen storage disease. Considering that fructose has the capacity to upregulate hepatic glycogen storage, and replenish these stores more readily following glycogen depleting exercise, the idea that hepatic glycogen storage and hepatic de novo lipogenesis are linked is an attractive prospect. We propose that hepatic glycogen stores may be a key factor in determining the metabolic responses to fructose ingestion, and saturation of hepatic glycogen stores could exacerbate the negative metabolic effects of excessive fructose intake. Since physical activity potently modulates glycogen metabolism, this provides a rationale for considering nutrient–physical activity interactions in metabolic health.

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“…), and pharmacological inhibition of ACC can decrease hepatic DNL and hepatic steatosis (Goedeke et al . ). This is, however, at the expense of hypertriglyceridaemia (Goedeke et al .…”

Section: Hepatic Lipid and Carbohydrate Handling Hepatic De Novo Lipmentioning

confidence: 97%

“…This is, however, at the expense of hypertriglyceridaemia (Goedeke et al . ). In human‐derived HEPG2 cells, addition of fructose to glucose does not further upregulate ACC expression (Hirahatake et al .…”

Section: Hepatic Lipid and Carbohydrate Handling Hepatic De Novo Lipmentioning

confidence: 97%

Fructose and metabolic health: governed by hepatic glycogen status?

Hengist

Koumanov

Gonzalez

2019

The Journal of Physiology

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“…These findings have now been validated in a phase II trial of a liver-targeted, allosteric inhibitor of ACC1 and ACC2, which demonstrated reduced hepatic steatosis and improved markers of fibrosis. (5) Hypertriglyceridemia, an unanticipated response to long-term ACC inhibition, has been observed in both rodents (4,6) and humans. (5,6) Goedeke et al (4) as well as Kim et al (6) have now shed light on this phenomenon as a previously unappreciated mechanistic point of control in triglyceride metabolism.…”

Section: See Article On Page 2197mentioning

confidence: 99%

“…Liver-directed inhibition of ACC1 and ACC2 reduces de novo lipogenesis and increases fatty acid β-oxidation. (4,6) Despite reductions in triglycerides content in the liver and improvements in insulin sensitivity, liver-directed inhibition of ACC1 and ACC2 leads to a decrease in polyunsaturated fatty acids and an increase in SREBP1c, GPAT1 expression and VLDL secretion, eventually leading to hypertriglyceridemia. Fibrate drugs decrease plasma triglycerides by enhancing fatty acid oxidation in the liver and by promoting lipoprotein lipase-mediated triglyceride clearance from the plasma.…”

Section: See Article On Page 2197mentioning

confidence: 99%

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Trimming the Fat: Acetyl‐CoA Carboxylase Inhibition for the Management of NAFLD

Imai

Cohen

2018

Hepatology

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Adenosine Triphosphate Citrate Lyase and Fatty Acid Synthesis Inhibition

Lau

Giugliano

2023

JAMA Cardiol

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ImportanceAdenosine triphosphate citrate lyase (ACLY) is a key regulatory enzyme of glucose metabolism, cholesterol and fatty acid synthesis, and the inflammatory cascade. Bempedoic acid, an ACLY inhibitor, significantly reduces atherogenic lipid markers, including low-density lipoprotein cholesterol (LDL-C), non–high-density lipoprotein cholesterol, and apolipoprotein B. Additional effects of ACLY inhibition include antitumor growth; reduction of triglycerides and proinflammatory molecules such as high-sensitivity C-reactive protein; less insulin resistance; reduction of hepatic lipogenesis; and weight loss.ObservationsWhile numerous ACLY inhibitors have been identified, most of the clinical data have focused on bempedoic acid. The Cholesterol Lowering via Bempedoic Acid, an ACL-Inhibiting Regimen (CLEAR) program was a series of phase 3 clinical trials that evaluated its effects on lipid parameters and safety, leading to US Food and Drug Administration approval in 2020. CLEAR Outcomes was a phase 3, double-blind, randomized, placebo-controlled trial in individuals with a history of statin intolerance, serum LDL-C level of 100 mg/dL or higher, and a history of, or at high risk for, cardiovascular disease. Bempedoic acid modestly reduced the primary 4-way cardiovascular composite end point as well as the individual components of myocardial infarction and coronary revascularization but did not reduce stroke, cardiovascular death, or all-cause mortality. Rates of gout and cholelithiasis were higher with bempedoic acid, and small increases in serum creatinine, uric acid, and hepatic-enzyme levels were also observed.Conclusions and relevanceACLY inhibition with bempedoic acid has been established as a safe and effective therapy in high-risk patients who require further LDL-C lowering, particularly for those with a history of statin intolerance. The recently published CLEAR Outcomes trial revealed modest reductions in cardiovascular events with bempedoic acid, proportional to its LDL-C lowering, in high-risk individuals with statin intolerance and LDL-C levels of 100 mg/dL or higher. The additional effects of ACLY inhibition have prompted a more thorough search for novel ACLY inhibitors for conditions such as cancer, hypertriglyceridemia, chronic inflammation, type 2 diabetes, fatty liver disease, obesity, and metabolic syndrome. Similarly, therapies that reduce fatty acid synthesis are being explored for their use in cardiometabolic conditions.

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Acetyl‐CoA Carboxylase Inhibition Reverses NAFLD and Hepatic Insulin Resistance but Promotes Hypertriglyceridemia in Rodents

Cited by 191 publications

References 44 publications

Fructose and metabolic health: governed by hepatic glycogen status?

Fructose and metabolic health: governed by hepatic glycogen status?

Trimming the Fat: Acetyl‐CoA Carboxylase Inhibition for the Management of NAFLD

Adenosine Triphosphate Citrate Lyase and Fatty Acid Synthesis Inhibition

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