FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2930693194> ?p ?o ?g. }

• W2930693194 endingPage "298" @default.
• W2930693194 startingPage "298" @default.
• W2930693194 abstract "Transforming growth factor-β receptor II (TGFBR2), the type II receptor of the TGF-β/SMA- and MAD-related protein (SMAD) signaling pathway, plays a crucial role in TGF-β signal transduction and is regulated by multiple factors. Nevertheless, the modulation of the non-coding RNA involved in the process of TGFBR2 expression in ovaries is not well studied. In our study, we isolated and characterized the 3′-untranslated region (UTR) of the porcine TGFBR2 gene and microRNA-1306 (miR-1306) was identified as the functional miRNA that targets TGFBR2 in porcine granulosa cells (GCs). Functional analysis showed that miR-1306 promotes apoptosis of GCs as well as attenuating the TGF-β/SMAD signaling pathway targeting and impairing TGFBR2 in GCs. Moreover, we identified the miR-1306 core promoter and found three potential SMAD4-binding elements (SBEs). Luciferase and chromatin immunoprecipitation (ChIP) assays revealed that the transcription factor SMAD4 directly binds to the miR-1306 core promoter and inhibits its transcriptional activity. Furthermore, the TGF-β/SMAD signaling pathway is modulated by SMAD4 positive feedback via inhibition of miR-1306 expression in GCs. Collectively, our findings provide evidence of an epigenetic mechanism that modulates as well as mediates the feedback regulation of the classical TGF-β/SMAD signaling pathway in GCs from porcine ovaries." @default.
• W2930693194 created "2019-04-11" @default.
• W2930693194 creator A5016485685 @default.
• W2930693194 creator A5040424674 @default.
• W2930693194 creator A5049264813 @default.
• W2930693194 creator A5053196971 @default.
• W2930693194 creator A5072173677 @default.
• W2930693194 creator A5073365708 @default.
• W2930693194 date "2019-03-31" @default.
• W2930693194 modified "2023-10-17" @default.
• W2930693194 title "miR-1306 Mediates the Feedback Regulation of the TGF-β/SMAD Signaling Pathway in Granulosa Cells" @default.
• W2930693194 cites W1487581481 @default.
• W2930693194 cites W1963767618 @default.
• W2930693194 cites W1975725727 @default.
• W2930693194 cites W1976591615 @default.
• W2930693194 cites W1979524576 @default.
• W2930693194 cites W1980107542 @default.
• W2930693194 cites W1985851879 @default.
• W2930693194 cites W1988613013 @default.
• W2930693194 cites W2006291194 @default.
• W2930693194 cites W2030486257 @default.
• W2930693194 cites W2035653659 @default.
• W2930693194 cites W2055902335 @default.
• W2930693194 cites W2066556833 @default.
• W2930693194 cites W2074629755 @default.
• W2930693194 cites W2078442918 @default.
• W2930693194 cites W2092513068 @default.
• W2930693194 cites W2093932304 @default.
• W2930693194 cites W2101579992 @default.
• W2930693194 cites W2103807535 @default.
• W2930693194 cites W2109731329 @default.
• W2930693194 cites W2110410340 @default.
• W2930693194 cites W2111357931 @default.
• W2930693194 cites W2124185811 @default.
• W2930693194 cites W2133968430 @default.
• W2930693194 cites W2152966647 @default.
• W2930693194 cites W2168486358 @default.
• W2930693194 cites W2418363013 @default.
• W2930693194 cites W2481611869 @default.
• W2930693194 cites W2516648208 @default.
• W2930693194 cites W2534535096 @default.
• W2930693194 cites W2537136911 @default.
• W2930693194 cites W2550547921 @default.
• W2930693194 cites W2560615789 @default.
• W2930693194 cites W2571961634 @default.
• W2930693194 cites W2587726300 @default.
• W2930693194 cites W2588906225 @default.
• W2930693194 cites W2595226293 @default.
• W2930693194 cites W2598669299 @default.
• W2930693194 cites W2610781950 @default.
• W2930693194 cites W2613723788 @default.
• W2930693194 cites W2647212460 @default.
• W2930693194 cites W2765610314 @default.
• W2930693194 cites W2766001918 @default.
• W2930693194 cites W2770715352 @default.
• W2930693194 cites W2774226220 @default.
• W2930693194 cites W2783456236 @default.
• W2930693194 cites W2790459826 @default.
• W2930693194 cites W2790602792 @default.
• W2930693194 cites W2791445933 @default.
• W2930693194 cites W2793437300 @default.
• W2930693194 cites W2800064828 @default.
• W2930693194 cites W2801804032 @default.
• W2930693194 cites W2802733018 @default.
• W2930693194 cites W2807907278 @default.
• W2930693194 cites W2884189559 @default.
• W2930693194 cites W2885922308 @default.
• W2930693194 cites W2890654351 @default.
• W2930693194 cites W2891730522 @default.
• W2930693194 cites W2897635947 @default.
• W2930693194 cites W2901441090 @default.
• W2930693194 cites W2904729986 @default.
• W2930693194 doi "https://doi.org/10.3390/cells8040298" @default.
• W2930693194 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6523565" @default.
• W2930693194 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/30935128" @default.
• W2930693194 hasPublicationYear "2019" @default.
• W2930693194 type Work @default.
• W2930693194 sameAs 2930693194 @default.
• W2930693194 citedByCount "21" @default.
• W2930693194 countsByYear W29306931942019 @default.
• W2930693194 countsByYear W29306931942020 @default.
• W2930693194 countsByYear W29306931942021 @default.
• W2930693194 countsByYear W29306931942022 @default.
• W2930693194 crossrefType "journal-article" @default.
• W2930693194 hasAuthorship W2930693194A5016485685 @default.
• W2930693194 hasAuthorship W2930693194A5040424674 @default.
• W2930693194 hasAuthorship W2930693194A5049264813 @default.
• W2930693194 hasAuthorship W2930693194A5053196971 @default.
• W2930693194 hasAuthorship W2930693194A5072173677 @default.
• W2930693194 hasAuthorship W2930693194A5073365708 @default.
• W2930693194 hasBestOaLocation W29306931941 @default.
• W2930693194 hasConcept C101762097 @default.
• W2930693194 hasConcept C104317684 @default.
• W2930693194 hasConcept C105580179 @default.
• W2930693194 hasConcept C118131993 @default.
• W2930693194 hasConcept C125555471 @default.
• W2930693194 hasConcept C134320426 @default.
• W2930693194 hasConcept C145059251 @default.

• next