SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4313637574> ?p ?o ?g. }

Showing items 1 to 100 of ±144 with 100 items per page.

W4313637574 endingPage "164" @default.
W4313637574 startingPage "150" @default.
W4313637574 abstract "Uric acid (UA) accumulation triggers endothelial dysfunction, oxidative stress, and inflammation. Histone deacetylase (HDAC) plays a vital role in regulating the pathological processes of various diseases. However, the influence of HDAC inhibitor on UA-induced vascular endothelial cell injury (VECI) remains undefined. Hence, this study aimed to investigate the effect of HDACs inhibition on UA-induced vascular endothelial cell dysfunction and its detailed mechanism. UA was used to induce human umbilical vein endothelial cell (HUVEC) injury. Meanwhile, potassium oxonate-induced and hypoxanthine-induced hyperuricemia mouse models were also constructed. A broad-spectrum HDAC inhibitor trichostatin A (TSA) or selective HDAC6 inhibitor TubastatinA (TubA) was given to HUVECs or mice to determine whether HDACs can affect UA-induced VECI. The results showed pretreatment of HUVECs with TSA or HDAC6 knockdown-attenuated UA-induced VECI and increased FGF21 expression and phosphorylation of AKT, eNOS, and FoxO3a. These effects could be reversed by FGF21 knockdown. In vivo, both TSA and TubA reduced inflammation and tissue injury while increased FGF21 expression and phosphorylation of AKT, eNOS, and FoxO3a in the aortic and renal tissues of hyperuricemia mice. Therefore, HDACs, especially HDAC6 inhibitor, alleviated UA-induced VECI through upregulating FGF21 expression and then activating the PI3K/AKT pathway. This suggests that HDAC6 may serve as a novel therapeutic target for treating UA-induced endothelial dysfunction." @default.
W4313637574 created "2023-01-07" @default.
W4313637574 creator A5001070148 @default.
W4313637574 creator A5010511860 @default.
W4313637574 creator A5031879809 @default.
W4313637574 creator A5066068373 @default.
W4313637574 creator A5075149466 @default.
W4313637574 creator A5077096394 @default.
W4313637574 creator A5090789649 @default.
W4313637574 date "2023-02-01" @default.
W4313637574 modified "2023-09-30" @default.
W4313637574 title "HDAC Inhibitors Alleviate Uric Acid–Induced Vascular Endothelial Cell Injury by Way of the HDAC6/FGF21/PI3K/AKT Pathway" @default.
W4313637574 cites W1519326211 @default.
W4313637574 cites W1977871132 @default.
W4313637574 cites W1981944929 @default.
W4313637574 cites W1985749449 @default.
W4313637574 cites W2015650304 @default.
W4313637574 cites W2015769719 @default.
W4313637574 cites W2026138134 @default.
W4313637574 cites W2029245566 @default.
W4313637574 cites W2043787407 @default.
W4313637574 cites W2053645334 @default.
W4313637574 cites W2098584422 @default.
W4313637574 cites W2104705785 @default.
W4313637574 cites W2105202257 @default.
W4313637574 cites W2113056756 @default.
W4313637574 cites W2141040456 @default.
W4313637574 cites W2141653683 @default.
W4313637574 cites W2169881448 @default.
W4313637574 cites W2327015076 @default.
W4313637574 cites W2334719620 @default.
W4313637574 cites W2347124890 @default.
W4313637574 cites W2396184091 @default.
W4313637574 cites W2408620991 @default.
W4313637574 cites W2440658907 @default.
W4313637574 cites W2470634927 @default.
W4313637574 cites W2525149912 @default.
W4313637574 cites W2568049857 @default.
W4313637574 cites W2587085370 @default.
W4313637574 cites W2587560805 @default.
W4313637574 cites W2729790472 @default.
W4313637574 cites W2732681243 @default.
W4313637574 cites W2772221901 @default.
W4313637574 cites W2775102598 @default.
W4313637574 cites W2798054067 @default.
W4313637574 cites W2804847406 @default.
W4313637574 cites W2809841075 @default.
W4313637574 cites W2900601576 @default.
W4313637574 cites W2921829590 @default.
W4313637574 cites W2953536521 @default.
W4313637574 cites W2957527083 @default.
W4313637574 cites W2966010975 @default.
W4313637574 cites W2981648727 @default.
W4313637574 cites W2985580063 @default.
W4313637574 cites W2990498378 @default.
W4313637574 cites W3006078128 @default.
W4313637574 cites W3012420683 @default.
W4313637574 cites W3013426744 @default.
W4313637574 cites W3015051404 @default.
W4313637574 cites W3093680583 @default.
W4313637574 cites W3126857982 @default.
W4313637574 cites W3133054349 @default.
W4313637574 cites W3137996165 @default.
W4313637574 cites W3181252977 @default.
W4313637574 cites W3216190396 @default.
W4313637574 cites W438790120 @default.
W4313637574 doi "https://doi.org/10.1097/fjc.0000000000001372" @default.
W4313637574 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/36607630" @default.
W4313637574 hasPublicationYear "2023" @default.
W4313637574 type Work @default.
W4313637574 citedByCount "1" @default.
W4313637574 countsByYear W43136375742023 @default.
W4313637574 crossrefType "journal-article" @default.
W4313637574 hasAuthorship W4313637574A5001070148 @default.
W4313637574 hasAuthorship W4313637574A5010511860 @default.
W4313637574 hasAuthorship W4313637574A5031879809 @default.
W4313637574 hasAuthorship W4313637574A5066068373 @default.
W4313637574 hasAuthorship W4313637574A5075149466 @default.
W4313637574 hasAuthorship W4313637574A5077096394 @default.
W4313637574 hasAuthorship W4313637574A5090789649 @default.
W4313637574 hasBestOaLocation W43136375741 @default.
W4313637574 hasConcept C104317684 @default.
W4313637574 hasConcept C11960822 @default.
W4313637574 hasConcept C126322002 @default.
W4313637574 hasConcept C185592680 @default.
W4313637574 hasConcept C202751555 @default.
W4313637574 hasConcept C2777411675 @default.
W4313637574 hasConcept C2777622882 @default.
W4313637574 hasConcept C2778305200 @default.
W4313637574 hasConcept C2778326061 @default.
W4313637574 hasConcept C502942594 @default.
W4313637574 hasConcept C519581460 @default.
W4313637574 hasConcept C55493867 @default.
W4313637574 hasConcept C62478195 @default.
W4313637574 hasConcept C64927066 @default.
W4313637574 hasConcept C71924100 @default.
W4313637574 hasConcept C75217442 @default.
W4313637574 hasConcept C86554907 @default.