A nontumorigenic variant of FGF19 treats cholestatic liver diseases

Luo, Jian; Ko, Brian; Elliott, Michael R.; Zhou, Mei; Lindhout, Darrin A.; Trung, Phùng Văn; To, Carmen; Learned, R. Marc; Tian, Hui; DePaoli, Alex M.; Ling, Lei

doi:10.1126/scitranslmed.3009098

Cited by 143 publications

(136 citation statements)

References 54 publications

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“…Based on these findings, a number of studies were performed to generate mutant FGF19 variants that should lack these pro-tumorigenic properties but retain the beneficial metabolic effects (for review see [54] ). In this regard, the variant M70 (or NGM282) has recently been described as a 'biased ligand' for FGFR4, which lacks tumor-promoting features, but is still able to suppress CYP7A1 activity in vitro and in vivo [63,64] . Clinical phase II trials are currently performed to investigate the potential of this drug to improve metabolic parameters in patients with T2D and NASH (NCT01943045 and NCT02443116).…”

Section: The Intestinal Hormone Fgf19 Contributes To the Pharmacologimentioning

confidence: 99%

Non-Alcoholic Steatohepatitis: From Pathophysiology to Novel Therapies

Jahn

Rau

Wohlfahrt

et al. 2016

Dig Dis

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Non-alcoholic fatty liver (NAFL) disease is defined by an accumulation of liver fat exceeding 5% of its weight in the absence of significant alcoholic intake. In 5-20%, there is a progression from NAFL to non-alcoholic steatohepatitis (NASH). Until now, it is not well understood why only some patients develop NASH, and currently, no drugs are licensed for this indication. Different T-cell populations such as T-regulatory, Th1 and Th17 cells play a central role in the immunopathogenesis of fatty liver disease and open the option of future interleukin (IL)-17-based therapeutics. The inflammatory process underlying NASH is furthermore characterized by elevated expression of pro-inflammatory cytokines such as TNFα and IL-1β. Anakinra, a recombinant version of IL-1Ra shows promising metabolic effects with improved hyperglycemia and beta-cell secretory function in a double-blind placebo controlled randomized trial in type 2 diabetic patients but such studies are still in their preliminary stages for NASH. Several studies point out that bile acid farnesoid X receptor (FXR)-mediated signals (such as the enterohepatic hormone fibroblast growth factor 15/19) are involved in the regulation of triglyceride and glucose metabolism. Recent clinical trials have revealed a beneficial impact of the FXR agonist obeticholic acid on body weight, insulin sensitivity and liver histology in patients with NASH. Further potential novel therapeutic targets in NASH are currently in phase II clinical development.

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Section: The Intestinal Hormone Fgf19 Contributes To the Pharmacologimentioning

confidence: 99%

Non-Alcoholic Steatohepatitis: From Pathophysiology to Novel Therapies

Jahn

Rau

Wohlfahrt

et al. 2016

Dig Dis

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“…As a potential therapeutic strategy for cholestatic liver disease, FGF15/19 has the disadvantage that it needs to be injected instead of oral treatment. However, FGF19 derivative NGM282 with UDCA has been tested for clinical trial phase II in PBC patients (Luo et al 2014). Given that FGF15/19 is a mitogenic peptide, the carcinogenic properties of FGF15/19 should be carefully considered for the clinical purpose.…”

Section: Clinical Effects Of Fxr-fgf19 Signaling Axismentioning

confidence: 99%

Essential roles of bile acids and their nuclear receptors, FXR and PXR, in the cholestatic liver disease

Han

Kim

et al. 2016

Animal Cells and Systems

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Bile acids (BAs) are steroid acids found predominantly in the bile of mammals and other vertebrates. Though BAs have been known as digestive juice, recent studies have revealed that BAs act as signaling molecules to control metabolism and inflammation. Today, BAs are considered as potential therapeutic molecules for treatment of complex metabolic liver disease. However, the detergent properties of BAs lead to hepatic injury and intrahepatic cholestasis when BAs are accumulated in the liver with impaired bile flow into gall bladder. Cholestasis is a pathological condition of hepatic retention of cytotoxic bile acids. To date, hydrophilic ursodeoxycholic acid has been currently used to treat cholestasis, but the efficacy of UDCA for cholestasis is still limited. Given that BAs are endogenous ligands of several nuclear receptors, including Farnesoid X receptor and Pregnane X receptor, novel synthetic ligands for those nuclear receptors are promising for the treatment of cholestatic liver diseases. ARTICLE HISTORY

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“…This hormone, when released from the gut, binds to the tyrosine kinase receptor FGF receptor 4/β-Klotho on hepatocytes, which activates the jun N-terminal kinase 1/2 signaling pathway [53]. Intestinal FXR activation [54] and the FGF19 mimetic M70 [55,56] dampen cholestatic liver injury by strongly reducing hepatic bile acid synthesis and the circulating bile acid pool. So, mouse studies clearly show hepatoprotection through (gut-specific) FGF15/19 signaling, primarily by reducing bile acid pools, sharing its mode of action with ASBT-inhibition.…”

Section: Inhibition Of Bile Acid Uptake To Ameliorate Cholestatic LIVmentioning

confidence: 99%

Bile Acid Uptake Transporters as Targets for Therapy

Slijepćević¹,

Graaf²

2017

Dig Dis

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Background: Bile acids are potent signaling molecules that regulate glucose, lipid and energy homeostasis predominantly via the bile acid receptors farnesoid X receptor (FXR) and transmembrane G protein-coupled receptor 5 (TGR5). The sodium taurocholate cotransporting polypeptide (NTCP) and the apical sodium dependent bile acid transporter (ASBT) ensure an effective circulation of (conjugated) bile acids. The modulation of these transport proteins affects bile acid localization, dynamics and signaling. The NTCP-specific pharmacological inhibitor myrcludex B inhibits hepatic uptake of conjugated bile acids. Multiple ASBT-inhibitors are already in clinical trials to inhibit intestinal bile acid uptake. Here, we discuss current insights into the consequences of targeting bile acid uptake transporters on systemic and intestinal bile acid dynamics and discuss the possible therapeutic applications that evolve as a result.

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A nontumorigenic variant of FGF19 treats cholestatic liver diseases

Cited by 143 publications

References 54 publications

Non-Alcoholic Steatohepatitis: From Pathophysiology to Novel Therapies

Non-Alcoholic Steatohepatitis: From Pathophysiology to Novel Therapies

Essential roles of bile acids and their nuclear receptors, FXR and PXR, in the cholestatic liver disease

Bile Acid Uptake Transporters as Targets for Therapy

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