AJOU Open Repository: 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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Cysteine-rich 61 inhibition attenuates hepatic insulin resistance and improves lipid metabolism in high-fat diet fed mice and HepG2 cells

DC Field	Value	Language
dc.contributor.author	Heo, YJ	-
dc.contributor.author	Park, J	-
dc.contributor.author	Lee, N	-
dc.contributor.author	Choi, SE	-
dc.contributor.author	Jeon, JY	-
dc.contributor.author	Han, SJ	-
dc.contributor.author	Kim, DJ	-
dc.contributor.author	Lee, KW	-
dc.contributor.author	Kim, HJ	-
dc.date.accessioned	2024-09-27T00:19:56Z	-
dc.date.available	2024-09-27T00:19:56Z	-
dc.date.issued	2024	-
dc.identifier.issn	0892-6638	-
dc.identifier.uri	http://repository.ajou.ac.kr/handle/201003/32834	-
dc.description.abstract	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.	-
dc.language.iso	en	-
dc.subject.MESH	Animals	-
dc.subject.MESH	Cysteine-Rich Protein 61	-
dc.subject.MESH	Diet, High-Fat	-
dc.subject.MESH	Hep G2 Cells	-
dc.subject.MESH	Humans	-
dc.subject.MESH	Insulin Resistance	-
dc.subject.MESH	Lipid Metabolism	-
dc.subject.MESH	Lipogenesis	-
dc.subject.MESH	Liver	-
dc.subject.MESH	Male	-
dc.subject.MESH	Mice	-
dc.subject.MESH	Mice, Inbred C57BL	-
dc.title	Cysteine-rich 61 inhibition attenuates hepatic insulin resistance and improves lipid metabolism in high-fat diet fed mice and HepG2 cells	-
dc.type	Article	-
dc.identifier.pmid	39082187	-
dc.identifier.url	https://faseb.onlinelibrary.wiley.com/doi/epdf/10.1096/fj.202400860R	-
dc.subject.keyword	AMP-activated protein kinase	-
dc.subject.keyword	Cyr61	-
dc.subject.keyword	inflammation	-
dc.subject.keyword	insulin resistance	-
dc.subject.keyword	lipid metabolism	-
dc.subject.keyword	Sirt6	-
dc.contributor.affiliatedAuthor	Heo, YJ	-
dc.contributor.affiliatedAuthor	Lee, N	-
dc.contributor.affiliatedAuthor	Choi, SE	-
dc.contributor.affiliatedAuthor	Jeon, JY	-
dc.contributor.affiliatedAuthor	Han, SJ	-
dc.contributor.affiliatedAuthor	Kim, DJ	-
dc.contributor.affiliatedAuthor	Lee, KW	-
dc.contributor.affiliatedAuthor	Kim, HJ	-
dc.type.local	Journal Papers	-
dc.identifier.doi	10.1096/fj.202400860R	-
dc.citation.title	FASEB journal	-
dc.citation.volume	38	-
dc.citation.number	15	-
dc.citation.date	2024	-
dc.citation.startPage	e23859	-
dc.citation.endPage	e23859	-
dc.identifier.bibliographicCitation	FASEB journal, 38(15). : e23859-e23859, 2024	-
dc.identifier.eissn	1530-6860	-
dc.relation.journalid	J008926638	-

Appears in Collections:: Journal Papers > School of Medicine / Graduate School of Medicine > Endocrinology & Metabolism
Journal Papers > School of Medicine / Graduate School of Medicine > Physiology

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