Transcriptome Analysis of K-877 (a Novel Selective PPARα Modulator (SPPARMα))-Regulated Genes in Primary Human Hepatocytes and the Mouse Liver

Raza-Iqbal, Sana; Tanaka, Toshiya; Anai, Motonobu; Inagaki, Takeshi; Matsumura, Yoshihiro; Ikeda, Kaori; Taguchi, Azuma; Gonzalez, Frank J.; Sakai, Juro; Kodama, Tatsuhiko

doi:10.5551/jat.28720

Cited by 88 publications

(87 citation statements)

References 58 publications

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“…Based on a previous report, 8‐week‐old male WT mice were fed a moderate‐fat (MF) diet containing 0.2% (w/w) Feno or 0.001% (w/w) K‐877 for 6 days. Although the dose of K‐877 was 200‐fold lower than that of Feno, compared with no treatment, K‐877 and Feno significantly reduced plasma TG levels, and tended to reduce TC and NEFA levels (Figure a), and the effects of both agonists were blunted in Ppara −/− mice (Figure a).…”

Section: Resultsmentioning

confidence: 99%

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Selective peroxisome proliferator‐activated receptor‐α modulator K‐877 efficiently activates the peroxisome proliferator‐activated receptor‐α pathway and improves lipid metabolism in mice

Takei

Han

Murayama

et al. 2017

J of Diabetes Invest

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Aims/IntroductionPeroxisome proliferator‐activated receptor‐α (PPARα) is a therapeutic target for hyperlipidemia. K‐877 is a new selective PPARα modulator (SPPARMα) that activates PPARα transcriptional activity. The aim of the present study was to assess the effects of K‐877 on lipid metabolism in vitro and in vivo compared with those of classical PPARα agonists.Materials and MethodsTo compare the effects of K‐877 on PPARα transcriptional activity with those of the classical PPARα agonists Wy14643 (Wy) and fenofibrate (Feno), the cell‐based PPARα transactivation luciferase assay was carried out. WT and Ppara −/− mice were fed with a moderate‐fat (MF) diet for 6 days, and methionine–choline‐deficient (MCD) diet for 4 weeks containing Feno or K‐877.ResultsIn luciferase assays, K‐877 activated PPARα transcriptional activity more efficiently than the classical PPARα agonists Feno and Wy. After being fed MF diet containing 0.001% K‐877 or 0.2% Feno for 6 days, mice in the K‐877 group showed significant increases in the expression of Ppara and its target genes, leading to marked reductions in plasma triglyceride levels compared with those observed in Feno‐treated animals. These K‐877 effects were blunted in Ppara −/− mice, confirming that K‐877 activates PPARα. In further experiments, K‐877 (0.00025%) and Feno (0.1%) equally improved the pathology of MCD diet‐induced non‐alcoholic fatty liver disease, with increased expression of hepatic fatty acid oxidation genes.ConclusionsThe present data show that K‐877 is an attractive PPARα‐modulating drug and can efficiently reduce plasma triglyceride levels, thereby alleviating the dysregulation of lipid metabolism.

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Section: Resultsmentioning

confidence: 99%

“…Therefore, a potent and selective PPARα agonist is required for patients with metabolic syndrome. K‐877 is a novel selective PPARα modulator (SPPARMα) that enhances PPARα activity; it also elicits higher PPARα activation than other fibrates, with lower EC 50 values and higher PPAR subtype selectivity.…”

Section: Introductionmentioning

confidence: 99%

Selective peroxisome proliferator‐activated receptor‐α modulator K‐877 efficiently activates the peroxisome proliferator‐activated receptor‐α pathway and improves lipid metabolism in mice

Takei

Han

Murayama

et al. 2017

J of Diabetes Invest

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“…SPPARMS are thought to interact with the large binding pocket of PPARα to induce a different co-factor recruitment, resulting in higher potency and fewer adverse side effects than the original fibrate compounds (Fruchart, 2013). LY518674 and K-877 are currently in phase II trials with promising results in treating dyslipidemia (Ishibashi et al, 2016; Raza-Iqbal et al, 2015). These compounds may prove to be more efficacious candidates for smoking cessation therapy; however, preclinical studies are imperative to investigate this hypothesis.…”

Section: Discussionmentioning

confidence: 99%

In vivo interactions between α7 nicotinic acetylcholine receptor and nuclear peroxisome proliferator-activated receptor-α: Implication for nicotine dependence

et al. 2017

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Chronic tobacco use dramatically increases health burdens and financial costs. Limitations of current smoking cessation therapies indicate the need for improved molecular targets. The main addictive component of tobacco, nicotine, exerts its dependency effects via nicotinic acetylcholine receptors (nAChRs). Activation of the homomeric α7 nAChR reduces nicotine's rewarding properties in conditioned place preference (CPP) test and i.v. self-administration models, but the mechanism underlying these effects is unknown. Recently, the nuclear receptor peroxisome proliferator-activated receptor type-α (PPARα) has been implicated as a downstream signaling target of the α7 nAChR in ventral tegmental area dopamine cells. The present study investigated PPARα as a possible mediator of the effect of α7 nAChR activation in nicotine dependence. Our results demonstrate the PPARα antagonist GW6471 blocks actions of the α7 nAChR agonist PNU282987 on nicotine reward in an unbiased CPP test in male ICR adult mice. These findings suggests that α7 nAChR activation attenuates nicotine CPP in a PPARα-dependent manner. To evaluate PPARα activation in nicotine dependence we used the selective and potent PPARα agonist, WY-14643 and the clinically used PPARα activator, fenofibrate, in nicotine CPP and we observed attenuation of nicotine preference, but fenofibrate was less potent. We also studied PPARα in nicotine dependence by evaluating its activation in nicotine withdrawal. WY-14643 reversed nicotine withdrawal signs whereas fenofibrate had modest efficacy. This suggests that PPARα plays a role in nicotine reward and withdrawal and that further studies are warranted to elucidate its function in mediating the effects of α7 nAChRs in nicotine dependence.

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“…K-877 is a SPPAR α M currently being tested in dyslipidemic patients that exhibits higher lipid lowering activity than fibrates and has a favorable risk profile [206, 207]. INT-131, SPPAR γ M, has potent glucose lowering effects not associated with TZD side-effects [208].…”

Section: Perspectives and Conclusionmentioning

confidence: 99%

PPARs and Mitochondrial Metabolism: From NAFLD to HCC

2016

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Metabolic related diseases, such as type 2 diabetes, metabolic syndrome, and nonalcoholic fatty liver disease (NAFLD), are widespread threats which bring about a significant burden of deaths worldwide, mainly due to cardiovascular events and cancer. The pathogenesis of these diseases is extremely complex, multifactorial, and only partially understood. As the main metabolic organ, the liver is central to maintain whole body energetic homeostasis. At the cellular level, mitochondria are the metabolic hub connecting and integrating all the main biochemical, hormonal, and inflammatory signaling pathways to fulfill the energetic and biosynthetic demand of the cell. In the liver, mitochondria metabolism needs to cope with the energetic regulation of the whole body. The nuclear receptors PPARs orchestrate lipid and glucose metabolism and are involved in a variety of diseases, from metabolic disorders to cancer. In this review, focus is placed on the roles of PPARs in the regulation of liver mitochondrial metabolism in physiology and pathology, from NAFLD to HCC.

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Transcriptome Analysis of K-877 (a Novel Selective PPARα Modulator (SPPARMα))-Regulated Genes in Primary Human Hepatocytes and the Mouse Liver

Cited by 88 publications

References 58 publications

Selective peroxisome proliferator‐activated receptor‐α modulator K‐877 efficiently activates the peroxisome proliferator‐activated receptor‐α pathway and improves lipid metabolism in mice

Selective peroxisome proliferator‐activated receptor‐α modulator K‐877 efficiently activates the peroxisome proliferator‐activated receptor‐α pathway and improves lipid metabolism in mice

In vivo interactions between α7 nicotinic acetylcholine receptor and nuclear peroxisome proliferator-activated receptor-α: Implication for nicotine dependence

PPARs and Mitochondrial Metabolism: From NAFLD to HCC

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