FRINK Linked Data Fragments server

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2591538880> ?p ?o ?g. }

• W2591538880 abstract "Abstract The Notch1 pathway plays important roles in modulating erythroid and megakaryocyte differentiation. To screen the Notch1-related genes that regulate differentiation fate of K562 and HEL cells, the expression of transient receptor potential ankyrin 1 (TRPA1) was induced by Notch1 receptor intracellular domain (N1IC), the activated form of Notch1 receptor. N1IC and v-ets erythroblastosis virus E26 oncogene homolog 1 (Ets-1) bound to TRPA1 promoter region to regulate transcription in K562 cells. Transactivation of TRPA1 promoter by N1IC depended on the methylation status of TRPA1 promoter. N1IC and Ets-1 suppressed the DNA methyltransferase 3B (DNMT3B) level in K562 cells. Inhibition of TRPA1 expression after Notch1 knockdown could be attenuated by nanaomycin A, an inhibitor of DNMT3B, in K562 and HEL cells. Functionally, hemin-induced erythroid differentiation could be suppressed by TRPA1, and the reduction of erythroid differentiation of both cells by N1IC and Ets-1 occurred via TRPA1. However, PMA-induced megakaryocyte differentiation could be enhanced by TRPA1, and the surface markers of megakaryocytes could be elevated by nanaomycin A. Megakaryocyte differentiation could be reduced by Notch1 or Ets-1 knockdown and relieved by TRPA1 overexpression. The results suggest that Notch1 and TRPA1 might be critical modulators that control the fate of erythroid and megakaryocyte differentiation." @default.
• W2591538880 created "2017-03-03" @default.
• W2591538880 creator A5011337424 @default.
• W2591538880 creator A5038263925 @default.
• W2591538880 creator A5046059278 @default.
• W2591538880 creator A5048320882 @default.
• W2591538880 creator A5054376682 @default.
• W2591538880 creator A5071365301 @default.
• W2591538880 creator A5085484847 @default.
• W2591538880 date "2017-02-21" @default.
• W2591538880 modified "2023-09-29" @default.
• W2591538880 title "Notch1-promoted TRPA1 expression in erythroleukemic cells suppresses erythroid but enhances megakaryocyte differentiation" @default.
• W2591538880 cites W1546796591 @default.
• W2591538880 cites W1571837352 @default.
• W2591538880 cites W1572790640 @default.
• W2591538880 cites W1833855195 @default.
• W2591538880 cites W1900337607 @default.
• W2591538880 cites W1911156364 @default.
• W2591538880 cites W1972561843 @default.
• W2591538880 cites W1977435477 @default.
• W2591538880 cites W1977582022 @default.
• W2591538880 cites W1979193249 @default.
• W2591538880 cites W1981262353 @default.
• W2591538880 cites W1981478519 @default.
• W2591538880 cites W1982631986 @default.
• W2591538880 cites W1984723596 @default.
• W2591538880 cites W1986357027 @default.
• W2591538880 cites W1986370346 @default.
• W2591538880 cites W1990293965 @default.
• W2591538880 cites W1991682939 @default.
• W2591538880 cites W1998467441 @default.
• W2591538880 cites W2000429979 @default.
• W2591538880 cites W2003862811 @default.
• W2591538880 cites W2011350367 @default.
• W2591538880 cites W2011551149 @default.
• W2591538880 cites W2013005430 @default.
• W2591538880 cites W2019600656 @default.
• W2591538880 cites W2019928804 @default.
• W2591538880 cites W2023181335 @default.
• W2591538880 cites W2028472887 @default.
• W2591538880 cites W2032236844 @default.
• W2591538880 cites W2044217732 @default.
• W2591538880 cites W2046083799 @default.
• W2591538880 cites W2046608265 @default.
• W2591538880 cites W2050903730 @default.
• W2591538880 cites W2070412945 @default.
• W2591538880 cites W2070422708 @default.
• W2591538880 cites W2073514136 @default.
• W2591538880 cites W2074029111 @default.
• W2591538880 cites W2075904779 @default.
• W2591538880 cites W2076966192 @default.
• W2591538880 cites W2078469968 @default.
• W2591538880 cites W2079719679 @default.
• W2591538880 cites W2079822043 @default.
• W2591538880 cites W2081646565 @default.
• W2591538880 cites W2082610530 @default.
• W2591538880 cites W2087990669 @default.
• W2591538880 cites W2088681937 @default.
• W2591538880 cites W2090002737 @default.
• W2591538880 cites W2091022798 @default.
• W2591538880 cites W2095474530 @default.
• W2591538880 cites W2095546422 @default.
• W2591538880 cites W2097598334 @default.
• W2591538880 cites W2097673163 @default.
• W2591538880 cites W2105669948 @default.
• W2591538880 cites W2105687173 @default.
• W2591538880 cites W2106050858 @default.
• W2591538880 cites W2107063571 @default.
• W2591538880 cites W2109879418 @default.
• W2591538880 cites W2112315511 @default.
• W2591538880 cites W2112561535 @default.
• W2591538880 cites W2113684190 @default.
• W2591538880 cites W2116102471 @default.
• W2591538880 cites W2118159405 @default.
• W2591538880 cites W2120229762 @default.
• W2591538880 cites W2122398847 @default.
• W2591538880 cites W2126181026 @default.
• W2591538880 cites W2129155568 @default.
• W2591538880 cites W2140921695 @default.
• W2591538880 cites W2141295972 @default.
• W2591538880 cites W2144109577 @default.
• W2591538880 cites W2147229707 @default.
• W2591538880 cites W2147503051 @default.
• W2591538880 cites W2154861644 @default.
• W2591538880 cites W2159197493 @default.
• W2591538880 cites W2164606073 @default.
• W2591538880 cites W2165979821 @default.
• W2591538880 cites W2187743525 @default.
• W2591538880 cites W2294631915 @default.
• W2591538880 cites W2412078964 @default.
• W2591538880 cites W324549396 @default.
• W2591538880 cites W4238758694 @default.
• W2591538880 cites W4244921051 @default.
• W2591538880 doi "https://doi.org/10.1038/srep42883" @default.
• W2591538880 hasPubMedCentralId "https://www.ncbi.nlm.nih.gov/pmc/articles/5318885" @default.
• W2591538880 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/28220825" @default.
• W2591538880 hasPublicationYear "2017" @default.
• W2591538880 type Work @default.
• W2591538880 sameAs 2591538880 @default.
• W2591538880 citedByCount "6" @default.

• next