FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2992185350> ?p ?o ?g. }

• W2992185350 abstract "Background Translocation of miR‐181c into cardiac mitochondria downregulates the mitochondrial gene, mt‐ COX 1. miR‐181c/d −/− hearts experience less oxidative stress during ischemia/reperfusion (I/R) and are protected against I/R injury. Additionally, miR‐181c overexpression can increase mitochondrial matrix Ca 2+ ([Ca 2+ ] m ), but the mechanism by which miR‐181c regulates [Ca 2+ ] m is unknown. Methods and Results By RNA sequencing and analysis, here we show that hearts from miR‐181c/d −/− mice overexpress nuclear‐encoded Ca 2+ regulatory and metabolic pathway genes, suggesting that alterations in miR‐181c and mt‐ COX 1 perturb mitochondria‐to‐nucleus retrograde signaling and [Ca 2+ ] m regulation. Quantitative polymerase chain reaction validation of transcription factors that are known to initiate retrograde signaling revealed significantly higher Sp1 (specificity protein) expression in the miR‐181c/d −/− hearts. Furthermore, an association of Sp1 with the promoter region of MICU 1 was confirmed by chromatin immunoprecipitation‐quantitative polymerase chain reaction and higher expression of MICU 1 was found in the miR‐181c/d −/− hearts. Conversely, downregulation of Sp1 by small interfering RNA decreased MICU 1 expression in neonatal mouse ventricular myocytes. Changes in PDH activity provided evidence for a change in [Ca 2+ ] m via the miR‐181c/ MICU 1 axis. Moreover, this mechanism was implicated in the pathology of I/R injury. When MICU 1 was knocked down in the miR‐181c/d −/− heart by lentiviral expression of a short‐hairpin RNA against MICU 1, cardioprotective effects against I/R injury were abrogated. Furthermore, using an in vitro I/R model in miR‐181c/d −/− neonatal mouse ventricular myocytes, we confirmed the contribution of both Sp1 and MICU 1 in ischemic injury. Conclusions miR‐181c regulates mt‐ COX 1, which in turn regulates MICU 1 expression through the Sp1‐mediated mitochondria‐to‐nucleus retrograde pathway. Loss of miR‐181c can protect the heart from I/R injury by modulating [Ca 2+ ] m through the upregulation of MICU 1." @default.
• W2992185350 created "2019-12-13" @default.
• W2992185350 creator A5003726306 @default.
• W2992185350 creator A5007052382 @default.
• W2992185350 creator A5038709923 @default.
• W2992185350 creator A5042448754 @default.
• W2992185350 creator A5047733660 @default.
• W2992185350 creator A5053313727 @default.
• W2992185350 creator A5061566627 @default.
• W2992185350 creator A5064257229 @default.
• W2992185350 creator A5064259897 @default.
• W2992185350 creator A5073163138 @default.
• W2992185350 creator A5077806459 @default.
• W2992185350 creator A5080198568 @default.
• W2992185350 date "2019-12-17" @default.
• W2992185350 modified "2023-10-18" @default.
• W2992185350 title "miR‐181c Activates Mitochondrial Calcium Uptake by Regulating MICU1 in the Heart" @default.
• W2992185350 cites W1508030134 @default.
• W2992185350 cites W1523821352 @default.
• W2992185350 cites W1546952499 @default.
• W2992185350 cites W1547216871 @default.
• W2992185350 cites W1622243645 @default.
• W2992185350 cites W1965025793 @default.
• W2992185350 cites W1968148259 @default.
• W2992185350 cites W1984661543 @default.
• W2992185350 cites W1986213783 @default.
• W2992185350 cites W1991055482 @default.
• W2992185350 cites W1992901862 @default.
• W2992185350 cites W1999754403 @default.
• W2992185350 cites W2024538200 @default.
• W2992185350 cites W2027851837 @default.
• W2992185350 cites W2028452582 @default.
• W2992185350 cites W2030740999 @default.
• W2992185350 cites W2034819039 @default.
• W2992185350 cites W2036897871 @default.
• W2992185350 cites W2038468721 @default.
• W2992185350 cites W2041639550 @default.
• W2992185350 cites W2045338351 @default.
• W2992185350 cites W2060880575 @default.
• W2992185350 cites W2068048197 @default.
• W2992185350 cites W2073256947 @default.
• W2992185350 cites W2078179312 @default.
• W2992185350 cites W2084824261 @default.
• W2992185350 cites W2094770594 @default.
• W2992185350 cites W2096465161 @default.
• W2992185350 cites W2097167248 @default.
• W2992185350 cites W2107018762 @default.
• W2992185350 cites W2117571600 @default.
• W2992185350 cites W2121711825 @default.
• W2992185350 cites W2122762775 @default.
• W2992185350 cites W2126125281 @default.
• W2992185350 cites W2138207763 @default.
• W2992185350 cites W2142903428 @default.
• W2992185350 cites W2146512944 @default.
• W2992185350 cites W2156007429 @default.
• W2992185350 cites W2157191747 @default.
• W2992185350 cites W2160294830 @default.
• W2992185350 cites W2165573061 @default.
• W2992185350 cites W2166513441 @default.
• W2992185350 cites W2169456326 @default.
• W2992185350 cites W2204029753 @default.
• W2992185350 cites W2225852931 @default.
• W2992185350 cites W2506140674 @default.
• W2992185350 cites W2522797636 @default.
• W2992185350 cites W2593870194 @default.
• W2992185350 cites W2593990129 @default.
• W2992185350 cites W2599820498 @default.
• W2992185350 cites W2606220580 @default.
• W2992185350 cites W2610173397 @default.
• W2992185350 cites W2624937154 @default.
• W2992185350 cites W2750054522 @default.
• W2992185350 cites W2792978395 @default.
• W2992185350 doi "https://doi.org/10.1161/jaha.119.012919" @default.
• W2992185350 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/6951067" @default.
• W2992185350 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/31801413" @default.
• W2992185350 hasPublicationYear "2019" @default.
• W2992185350 type Work @default.
• W2992185350 sameAs 2992185350 @default.
• W2992185350 citedByCount "17" @default.
• W2992185350 countsByYear W29921853502020 @default.
• W2992185350 countsByYear W29921853502021 @default.
• W2992185350 countsByYear W29921853502022 @default.
• W2992185350 countsByYear W29921853502023 @default.
• W2992185350 crossrefType "journal-article" @default.
• W2992185350 hasAuthorship W2992185350A5003726306 @default.
• W2992185350 hasAuthorship W2992185350A5007052382 @default.
• W2992185350 hasAuthorship W2992185350A5038709923 @default.
• W2992185350 hasAuthorship W2992185350A5042448754 @default.
• W2992185350 hasAuthorship W2992185350A5047733660 @default.
• W2992185350 hasAuthorship W2992185350A5053313727 @default.
• W2992185350 hasAuthorship W2992185350A5061566627 @default.
• W2992185350 hasAuthorship W2992185350A5064257229 @default.
• W2992185350 hasAuthorship W2992185350A5064259897 @default.
• W2992185350 hasAuthorship W2992185350A5073163138 @default.
• W2992185350 hasAuthorship W2992185350A5077806459 @default.
• W2992185350 hasAuthorship W2992185350A5080198568 @default.
• W2992185350 hasBestOaLocation W29921853501 @default.
• W2992185350 hasConcept C101762097 @default.
• W2992185350 hasConcept C104317684 @default.
• W2992185350 hasConcept C126322002 @default.

• next