Published online Oct 21, 2021. doi: 10.3748/wjg.v27.i39.6522
Peer-review started: March 28, 2021
First decision: June 14, 2021
Revised: June 28, 2021
Accepted: September 22, 2021
Article in press: September 22, 2021
Published online: October 21, 2021
Processing time: 205 Days and 16 Hours
De novo lipogenesis (DNL) plays an important role in the pathogenesis of hepatic steatosis and also appears to be implicated in hepatic inflammation and fibrosis. Accordingly, the inhibition of acetyl-CoA carboxylase, which catalyzes the rate-limiting step of DNL, might represent a useful approach in the management of patients with nonalcoholic fatty liver disease (NAFLD). Animal studies and preliminary data in patients with NAFLD consistently showed an improvement in steatosis with the use of these agents. However, effects on fibrosis were variable and an increase in plasma triglyceride levels was observed. Therefore, more long-term studies are needed to clarify the role of these agents in NAFLD and to determine their risk/benefit profile.
Core Tip: Acetyl-CoA carboxylase inhibitors suppress de novo lipogenesis resulting in improvement in hepatic steatosis in both animal models and in patients with nonal
- Citation: Neokosmidis G, Cholongitas E, Tziomalos K. Acetyl-CoA carboxylase inhibitors in non-alcoholic steatohepatitis: Is there a benefit? World J Gastroenterol 2021; 27(39): 6522-6526
- URL: https://www.wjgnet.com/1007-9327/full/v27/i39/6522.htm
- DOI: https://dx.doi.org/10.3748/wjg.v27.i39.6522
Non-alcoholic fatty liver disease (NAFLD) is the commonest chronic liver disease in high-income countries, affecting 17%-46% of the general population[1]. NAFLD includes non-alcoholic fatty liver, characterized by isolated hepatic steatosis, and non-alcoholic steatohepatitis (NASH), where variable degrees of hepatic inflammation and fibrosis coexist with steatosis[2]. NASH is associated with increased risk for cirrhosis, hepatocellular cancer (HCC) and cardiovascular disease[3,4]. Diet and exercise, aiming at weight loss, is the cornerstone of management of NAFLD, but only a minority of patients achieves and maintains weight loss > 5%, which is essential for improvement in liver histology[2,5]. Several pharmacological agents have been evaluated in patients with NAFLD but none is currently licensed for use in this disease[2]. Therefore, there is an unmet need for safe and effective treatments in patients with NASH.
The pathogenesis of NASH is complex and multiple pathways, including insulin resistance, inflammation, oxidative stress and apoptosis are implicated[6]. De novo lipogenesis (DNL), defined as the synthesis of fatty acids from non-lipid sources, is pivotal in the development and progression of NASH. DNL is increased in patients with NAFLD and appears to be responsible for up to 38% of intrahepatic triglyceride content in this population[7]. In addition to its contribution to the development of hepatic steatosis, DNL also promotes fibrosis by activating hepatic stellate cells (HSC), which are the principal contributors to liver fibrosis[8,9]. Acetyl-CoA carboxylase (ACC) catalyzes the ATP-dependent carboxylation of acetyl-coenzyme A (CoA) to form malonyl-CoA, which is the rate-limiting and key regulatory step in DNL[10]. ACC exists as two isoenzymes that are encoded by two different genes; ACC1 is cytosolic whereas ACC2 is located at the mitochondrial membrane[10].
Given the central role of ACC in DNL and the implication of the latter in the pathogenesis of NAFLD, ACC might represent an attractive therapeutic target in this disease. Indeed, early studies showed that liver-specific, genetic inactivation of ACC protects against the development of hepatic steatosis[11,12]. More recently, several orally available, liver-specific, dual ACC1/ACC2 inhibitors have been developed and are being evaluated in the management of NAFLD (Table 1). Perhaps the most pro
Population | ACC inhibitor | Major findings | Ref. |
Mice with NASH | Firsocostat (GS-0976) | ↓ Hepatic steatosis, inflammation and fibrosis | [13,14] |
High-fructose-fed rats | A structural analog of firsocostat | ↓ Hepatic steatosis; ↓ hepatic insulin resistance | [15] |
Zucker diabetic fatty rats | ND-630 | ↓ Hepatic steatosis | [16] |
Rat model of NASH | PF-05221304 | ↓ Hepatic steatosis, inflammation and fibrosis | [17] |
Rat model of NASH | MK-4074 | No effect on hepatic fibrosis | [21] |
Rat model of NASH | ND-654 | ↓ Hepatic steatosis; Delayed progression of hepatocellular cancer | [22] |
10 patients with NASH | Firsocostat | ↓ Hepatic steatosis and fibrosis | [23] |
126 patients with NASH | Firsocostat | ↓ Hepatic steatosis and tissue inhibitor of metalloproteinase-1 levels | [24] |
392 patients with NASH and bridging fibrosis or compensated cirrhosis (F3-F4) | Firsocostat | ↓ Hepatic steatosis and stiffness | [25] |
Healthy subjects | PF-05221304 | Dose-dependent suppression of de novo lipogenesis | [26] |
Overweight and/or obese adult males | ND-630 | Suppression of de novo lipogenesis | [27] |
30 patients with non-alcoholic fatty liver | MK-4074 | ↓ Hepatic steatosis | [28] |
In addition to the reduction in hepatic steatosis, ACC inhibition also appears to ameliorate hepatic fibrosis (Table 1), which is the strongest predictor of mortality in NASH[18-20]. In recent studies, firsocostat and a structural analog of this agent inhibited the activation of HSCs and reduced hepatic fibrosis both in vitro and in animal models of NASH[9,13,14]. PF-05221304 also prevented the activation of primary HSCs to myofibroblasts in vitro and reduced fibrosis in choline-deficient, high-fat-fed rats[17]. In contrast, MK-4074 did not affect fibrosis in a rat model of NASH, suggesting that the effect of ACC inhibition on fibrosis might be agent-specific[21]. On the other hand, another liver-specific, dual ACC1/ACC2 inhibitor, ND-654, not only reduced hepatic steatosis but also delayed the progression of HCC in a rat model[22].
Preliminary studies suggest that ACC inhibition might also be effective in patients with NAFLD (Table 1). In a pilot, open-label, prospective study in 10 patients with NASH, administration of firsocostat for 12 wk reduced hepatic steatosis, assessed with magnetic resonance imaging (MRI), and fibrosis, assessed with both magnetic re
Other ACC inhibitors also showed promising results in pilot clinical studies (Table 1). In healthy subjects, PF-05221304 dose-dependently suppressed DNL and was well-tolerated[26]. With doses yielding ≥ 90% DNL inhibition, asymptomatic increases in serum triglyceride levels and declines in platelet count occurred but these were not observed at ≤ 80% DNL inhibition[26]. A single dose of ND-630 was also shown to suppress DNL in overweight and/or obese but otherwise healthy adult males and was well tolerated[27]. Finally, in a randomized study in 30 patients with NAFL, treatment with MK-4074 for 4 wk decreased hepatic fat more than pioglitazone and placebo[28]. However, a 2-fold increase in plasma triglyceride levels was observed in patients treated with MK-4074 and not in the other groups[28]. It was shown that inhibition of ACC results in reduced intrahepatic content of polyunsaturated fatty acids, which in turn activates sterol regulatory element-binding protein-1c that increases hepatic production of very low density lipoprotein and therefore plasma triglyceride levels[28].
In conclusion, ACC inhibitors appear to represent a promising tool for ameliorating hepatic steatosis. The effect of these agents on hepatic fibrosis is less consistent and more studies are needed to assess their impact on NASH. In addition, given the high cardiovascular risk of patients with NASH, the increase in triglyceride levels during treatment with ACC inhibitors is a cause of concern and should be also be factored in the decision to administer them in this population.
Manuscript source: Invited manuscript
Specialty type: Gastroenterology and hepatology
Country/Territory of origin: Greece
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