Hepatocyte CYR61 polarizes profibrotic macrophages to orchestrate NASH fibrosis

Mooring, Meghan; Yeung, Grace A.; Luukkonen, Panu; Liu, Silvia; Akbar, Muhammad Waqas; Zhang, Gary J.; Balogun, Oluwashanu; Yu, Xuemei; Mo, Rigen; Nejak-Bowen, Kari; Poyurovsky, Masha V.; Booth, Carmen J.; Konnikova, Liza; Shulman, Gerald I.; Yimlamai, Dean

doi:10.1126/scitranslmed.ade3157

Cited by 4 publications

(1 citation statement)

References 81 publications

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“…The fluorescence intensity of CS-NPs/VDGtreated group was even lower than that of control group, which may be explained by that in vitro cultured HSCs would be partially activated when cultured in 10% FBS DMEM. [40] In a further experiment, HSCs-LSECs coculture system was applied to explore the possibility of inhibiting HSCs activation to prevent the loss of fenestrae and phenotype transformation of LSECs (Figure 3G). Immuno-staining of CD31 (a classic marker of capillarized LSECs) showed that HSCs pretreated with TGF-𝛽 and CS-NPs/VDG could reverse LSECs capillarization process.…”

Section: Interruption Of Hscs-lsecs Crosstalk By Cs-nps/vdg In Vitromentioning

confidence: 99%

Vicious Cycle‐Breaking Lipid Nanoparticles Remodeling Multicellular Crosstalk to Reverse Liver Fibrosis

Zhang,

Deng,

Huang

et al. 2024

Advanced Materials

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During liver fibrogenesis, the reciprocal crosstalk among capillarized liver sinusoidal endothelial cells (LSECs), activated hepatic stellate cells (HSCs) and dysfunctional hepatocytes constructs a self‐amplifying vicious cycle, greatly exacerbating the disease condition and weakening therapeutic effect. Limited by the malignant cellular interactions, the previous single‐cell centric treatment approaches showed unsatisfactory efficacy and failed to meet clinical demand. Herein, a vicious cycle‐breaking strategy was proposed to target and repair pathological cells separately to terminate the malignant progression of liver fibrosis. Chondroitin sulfate modified and vismodegib loaded nanoparticles (CS‐NPs/VDG) were designed to efficiently normalize the fenestrae phenotype of LSECs and restore HSCs to quiescent state by inhibiting Hedgehog signaling pathway. In addition, glycyrrhetinic acid modified and silybin loaded nanoparticles (GA‐NPs/SIB) were prepared to restore hepatocytes function by relieving oxidative stress. The results showed successful interruption of vicious cycle as well as distinct fibrosis resolution in two animal models through multi‐regulation of the pathological cells. This work not only highlights the significance of modulating cellular crosstalk but also provides a promising avenue for developing anti‐fibrotic regimens.This article is protected by copyright. All rights reserved

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Section: Interruption Of Hscs-lsecs Crosstalk By Cs-nps/vdg In Vitromentioning

confidence: 99%

Vicious Cycle‐Breaking Lipid Nanoparticles Remodeling Multicellular Crosstalk to Reverse Liver Fibrosis

Zhang,

Deng,

Huang

et al. 2024

Advanced Materials

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Thyroid hormone receptor-beta agonist HSK31679 alleviates MASLD by modulating gut microbial sphingolipids

Zhang,

Xie,

Dai

et al. 2024

Journal of Hepatology

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Cysteine‐rich 61 inhibition attenuates hepatic insulin resistance and improves lipid metabolism in high‐fat diet fed mice and HepG2 cells

Heo,

Park,

Lee

et al. 2024

The FASEB Journal

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Metabolic dysfunction‐associated steatotic liver disease (MASLD) is strongly associated with insulin resistance development. Hepatic lipid accumulation and inflammation are considered the main drivers of hepatic insulin resistance in MASLD. Cysteine‐rich 61 (Cyr61 also called CCN1), a novel secretory matricellular protein, is implicated in liver inflammation, and its role in MASLD is not clearly understood. Therefore, we investigated the role of Cyr61 in hepatic insulin resistance and lipid metabolism as major factors in MASLD pathogenesis. In high‐fat diet (HFD)‐fed C57BL/6J mice, Cyr61 was downregulated or upregulated via viral transduction. Measurements of glucose homeostasis, histological assessment of liver tissues, and gene expression and signaling pathways of lipogenesis, fatty acid oxidation, and inflammation were performed using liver samples from these mice. Cyr61 levels in HepG2 cells were reduced using RNAi‐mediated gene knockdown. Inflammation and insulin resistance were evaluated using real‐time polymerase chain reaction and western blotting. HFD/AAV‐shCyr61 mice exhibited enhanced glucose tolerance via the protein kinase B pathway, reduced hepatic inflammation, decreased lipogenesis, and increased fatty acid oxidation. Notably, HFD/AAV‐shCyr61 mice showed elevated protein expression of sirtuin 6 and phosphorylated‐AMP‐activated protein kinase. In vitro experiments demonstrated that inhibition of Cyr61 downregulated pro‐inflammatory cytokines such as interleukin‐1 beta, IL‐6, and tumor necrosis factor‐alpha via the nuclear factor kappa B/c‐Jun N‐terminal kinase pathway, and alleviated insulin resistance. Cyr61 affected hepatic inflammation, lipid metabolism, and insulin resistance. Inhibition of Cyr61 reduced inflammation, recovered insulin resistance, and altered lipid metabolism in vivo and in vitro. Therefore, Cyr61 is a potential therapeutic target in MASLD.

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Hepatocyte CYR61 polarizes profibrotic macrophages to orchestrate NASH fibrosis

Cited by 4 publications

References 81 publications

Vicious Cycle‐Breaking Lipid Nanoparticles Remodeling Multicellular Crosstalk to Reverse Liver Fibrosis

Vicious Cycle‐Breaking Lipid Nanoparticles Remodeling Multicellular Crosstalk to Reverse Liver Fibrosis

Thyroid hormone receptor-beta agonist HSK31679 alleviates MASLD by modulating gut microbial sphingolipids

Cysteine‐rich 61 inhibition attenuates hepatic insulin resistance and improves lipid metabolism in high‐fat diet fed mice and HepG2 cells

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