FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W4387012956> ?p ?o ?g. }

• W4387012956 abstract "Osteoporosis is not well treated due to the difficulty of finding commonalities between the various types of it. Iron homeostasis is a vital component in supporting biochemical functions, and iron overload is recognized as a common risk factor for osteoporosis. In this research, we found that there is indeed evidence of iron accumulation in the bone tissue of patients with osteoporosis and REPIN1, as an origin specific DNA binding protein, may play a key role in this process. We revealed that sh-Repin1 therapy can rescue bone loss in an iron-overload-induced osteoporosis mouse model. Knockdown of Repin1 can inhibit apoptosis and enhance the resistance of osteoblasts to iron overload toxicity. REPIN1 promoted apoptosis by regulating iron metabolism in osteoblasts. Mechanistically, knockdown of Repin1 decreased the expression of Lcn2, which ameliorated the toxic effects of intracellular iron overload. The anti-iron effect of lentivirus sh-Repin1 was partially reversed or replicated by changing LCN2 expression level via si-RNA or plasmid, which indirectly verified the key regulatory role of LCN2 as a downstream target. Furthermore, the levels of BCL2 and BAX, which play a key role in the mitochondrial apoptosis pathway, were affected. In summary, based on the results of clinical specimens, animal models and in vitro experiments, for the first time, we proved the key role of REPIN1 in iron metabolism-related osteoporosis." @default.
• W4387012956 created "2023-09-26" @default.
• W4387012956 creator A5001664082 @default.
• W4387012956 creator A5028990061 @default.
• W4387012956 creator A5029422969 @default.
• W4387012956 creator A5036424197 @default.
• W4387012956 creator A5042318166 @default.
• W4387012956 creator A5049167024 @default.
• W4387012956 creator A5053581326 @default.
• W4387012956 creator A5053718537 @default.
• W4387012956 date "2023-09-25" @default.
• W4387012956 modified "2023-10-17" @default.
• W4387012956 title "REPIN1 regulates iron metabolism and osteoblast apoptosis in osteoporosis" @default.
• W4387012956 cites W105666515 @default.
• W4387012956 cites W1516581822 @default.
• W4387012956 cites W1536179852 @default.
• W4387012956 cites W1567961394 @default.
• W4387012956 cites W1570067866 @default.
• W4387012956 cites W1577617596 @default.
• W4387012956 cites W1588950918 @default.
• W4387012956 cites W1913925361 @default.
• W4387012956 cites W1940781876 @default.
• W4387012956 cites W1945304539 @default.
• W4387012956 cites W1953570789 @default.
• W4387012956 cites W1969506378 @default.
• W4387012956 cites W1975883416 @default.
• W4387012956 cites W1983048889 @default.
• W4387012956 cites W1991103673 @default.
• W4387012956 cites W1999321565 @default.
• W4387012956 cites W2011035317 @default.
• W4387012956 cites W2011735860 @default.
• W4387012956 cites W2018851450 @default.
• W4387012956 cites W2023958098 @default.
• W4387012956 cites W2026568210 @default.
• W4387012956 cites W2028638897 @default.
• W4387012956 cites W2030184781 @default.
• W4387012956 cites W2030951335 @default.
• W4387012956 cites W2033508977 @default.
• W4387012956 cites W2034160485 @default.
• W4387012956 cites W2036124167 @default.
• W4387012956 cites W2037382204 @default.
• W4387012956 cites W2037556998 @default.
• W4387012956 cites W2053023199 @default.
• W4387012956 cites W2055829911 @default.
• W4387012956 cites W2059652841 @default.
• W4387012956 cites W2070000741 @default.
• W4387012956 cites W2110843283 @default.
• W4387012956 cites W2114015514 @default.
• W4387012956 cites W2123346255 @default.
• W4387012956 cites W2134076305 @default.
• W4387012956 cites W2134472554 @default.
• W4387012956 cites W2139470181 @default.
• W4387012956 cites W2145294892 @default.
• W4387012956 cites W2146209894 @default.
• W4387012956 cites W2152863656 @default.
• W4387012956 cites W2153500348 @default.
• W4387012956 cites W2158562886 @default.
• W4387012956 cites W2159182678 @default.
• W4387012956 cites W2170344626 @default.
• W4387012956 cites W2170885365 @default.
• W4387012956 cites W2214440891 @default.
• W4387012956 cites W2263859327 @default.
• W4387012956 cites W2464723783 @default.
• W4387012956 cites W2527347986 @default.
• W4387012956 cites W2541295351 @default.
• W4387012956 cites W2592014417 @default.
• W4387012956 cites W2597818558 @default.
• W4387012956 cites W2612933061 @default.
• W4387012956 cites W2737451753 @default.
• W4387012956 cites W2888091897 @default.
• W4387012956 cites W2901776842 @default.
• W4387012956 cites W2970391745 @default.
• W4387012956 cites W2976802669 @default.
• W4387012956 cites W2980622391 @default.
• W4387012956 cites W3084317629 @default.
• W4387012956 cites W3157282498 @default.
• W4387012956 cites W3196191694 @default.
• W4387012956 cites W3211818783 @default.
• W4387012956 cites W3215602721 @default.
• W4387012956 cites W3217099983 @default.
• W4387012956 cites W4210805057 @default.
• W4387012956 cites W4283318993 @default.
• W4387012956 doi "https://doi.org/10.1038/s41419-023-06160-w" @default.
• W4387012956 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/37749079" @default.
• W4387012956 hasPublicationYear "2023" @default.
• W4387012956 type Work @default.
• W4387012956 citedByCount "0" @default.
• W4387012956 crossrefType "journal-article" @default.
• W4387012956 hasAuthorship W4387012956A5001664082 @default.
• W4387012956 hasAuthorship W4387012956A5028990061 @default.
• W4387012956 hasAuthorship W4387012956A5029422969 @default.
• W4387012956 hasAuthorship W4387012956A5036424197 @default.
• W4387012956 hasAuthorship W4387012956A5042318166 @default.
• W4387012956 hasAuthorship W4387012956A5049167024 @default.
• W4387012956 hasAuthorship W4387012956A5053581326 @default.
• W4387012956 hasAuthorship W4387012956A5053718537 @default.
• W4387012956 hasBestOaLocation W43870129561 @default.
• W4387012956 hasConcept C104317684 @default.
• W4387012956 hasConcept C126322002 @default.
• W4387012956 hasConcept C127561419 @default.

• next