SemOpenAlex |

SemOpenAlex

Matches in SemOpenAlex for { <https://semopenalex.org/work/W2130301032> ?p ?o ?g. }

Showing items 1 to 100 of ±128 with 100 items per page.

W2130301032 endingPage "15614" @default.
W2130301032 startingPage "15608" @default.
W2130301032 abstract "The ubiquitin-activating enzyme E1 exists as two isoforms, E1a (117 kDa) and E1b (110 kDa). E1a is phosphorylated, whereas E1b is not. In the present study we have demonstrated the cell cycle dependence of E1a phosphorylation: a 2-fold increase in the specific phosphorylation of E1a in G2 compared with the basal level of phosphorylation in the other stages of the cell cycle. Two-dimensional gel electrophoresis resolved E1 into the two isoforms E1a and E1b; E1a resolved further as three phosphorylated forms and one nonphosphorylated form, while E1b resolved as one nonphosphorylated form. E1a is found predominantly in the phosphorylated forms. However, the distribution of E1a among these different phosphorylated forms was not cell cycle-dependent. We next evaluated the enzymatic activity of E1 as well as its subcellular localization throughout the cell cycle. 32P-Pyrophosphate exchange activity of E1 did not vary along the cell cycle; however, the amount of ubiquitin-protein conjugates decreased by 50% in G2. Nuclear and cytosolic fractionation of cells revealed the nuclear to cytosolic ratio of phosphorylated E1a was 3-fold greater in G2 compared with the other stages of the cell cycle. Finally, purified nuclear extracts supported E1-dependent ubiquitin conjugation of exogenous substrates as did purified cytosol. However, in nuclear extracts but not in cytosol the amount of E1 activity was rate-limiting. Thus we establish nuclear E1-dependent protein ubiquitination and propose that an increase in phosphorylation of E1a in G2 functions to increase the import and/or retention of E1a in the nucleus and may modulate nuclear protein ubiquitination. The ubiquitin-activating enzyme E1 exists as two isoforms, E1a (117 kDa) and E1b (110 kDa). E1a is phosphorylated, whereas E1b is not. In the present study we have demonstrated the cell cycle dependence of E1a phosphorylation: a 2-fold increase in the specific phosphorylation of E1a in G2 compared with the basal level of phosphorylation in the other stages of the cell cycle. Two-dimensional gel electrophoresis resolved E1 into the two isoforms E1a and E1b; E1a resolved further as three phosphorylated forms and one nonphosphorylated form, while E1b resolved as one nonphosphorylated form. E1a is found predominantly in the phosphorylated forms. However, the distribution of E1a among these different phosphorylated forms was not cell cycle-dependent. We next evaluated the enzymatic activity of E1 as well as its subcellular localization throughout the cell cycle. 32P-Pyrophosphate exchange activity of E1 did not vary along the cell cycle; however, the amount of ubiquitin-protein conjugates decreased by 50% in G2. Nuclear and cytosolic fractionation of cells revealed the nuclear to cytosolic ratio of phosphorylated E1a was 3-fold greater in G2 compared with the other stages of the cell cycle. Finally, purified nuclear extracts supported E1-dependent ubiquitin conjugation of exogenous substrates as did purified cytosol. However, in nuclear extracts but not in cytosol the amount of E1 activity was rate-limiting. Thus we establish nuclear E1-dependent protein ubiquitination and propose that an increase in phosphorylation of E1a in G2 functions to increase the import and/or retention of E1a in the nucleus and may modulate nuclear protein ubiquitination." @default.
W2130301032 created "2016-06-24" @default.
W2130301032 creator A5070024846 @default.
W2130301032 creator A5070862606 @default.
W2130301032 creator A5075580325 @default.
W2130301032 creator A5087180436 @default.
W2130301032 date "1996-06-01" @default.
W2130301032 modified "2023-10-17" @default.
W2130301032 title "The Ubiquitin-activating Enzyme E1 Is Phosphorylated and Localized to the Nucleus in a Cell Cycle-dependent Manner" @default.
W2130301032 cites W1487877558 @default.
W2130301032 cites W1496897161 @default.
W2130301032 cites W1513849811 @default.
W2130301032 cites W1514253388 @default.
W2130301032 cites W1517718286 @default.
W2130301032 cites W1529476232 @default.
W2130301032 cites W1530194480 @default.
W2130301032 cites W1542081345 @default.
W2130301032 cites W1553060266 @default.
W2130301032 cites W1576686733 @default.
W2130301032 cites W1748894748 @default.
W2130301032 cites W1957935650 @default.
W2130301032 cites W1969336855 @default.
W2130301032 cites W1978186903 @default.
W2130301032 cites W1979438396 @default.
W2130301032 cites W1981772689 @default.
W2130301032 cites W1991101546 @default.
W2130301032 cites W1993243592 @default.
W2130301032 cites W1996015633 @default.
W2130301032 cites W2005717642 @default.
W2130301032 cites W2015997780 @default.
W2130301032 cites W2019894624 @default.
W2130301032 cites W2029761435 @default.
W2130301032 cites W2056453686 @default.
W2130301032 cites W2069355785 @default.
W2130301032 cites W2071191421 @default.
W2130301032 cites W2072389679 @default.
W2130301032 cites W2074126694 @default.
W2130301032 cites W2076217757 @default.
W2130301032 cites W2084343743 @default.
W2130301032 cites W2086192909 @default.
W2130301032 cites W2091403769 @default.
W2130301032 cites W2106869142 @default.
W2130301032 cites W2136776958 @default.
W2130301032 cites W2140182533 @default.
W2130301032 cites W2146437721 @default.
W2130301032 cites W2149244862 @default.
W2130301032 cites W2164931904 @default.
W2130301032 cites W2238296752 @default.
W2130301032 cites W45974969 @default.
W2130301032 doi "https://doi.org/10.1074/jbc.271.26.15608" @default.
W2130301032 hasPubMedId "https://pubmed.ncbi.nlm.nih.gov/8663123" @default.
W2130301032 hasPublicationYear "1996" @default.
W2130301032 type Work @default.
W2130301032 sameAs 2130301032 @default.
W2130301032 citedByCount "51" @default.
W2130301032 countsByYear W21303010322013 @default.
W2130301032 countsByYear W21303010322014 @default.
W2130301032 countsByYear W21303010322015 @default.
W2130301032 countsByYear W21303010322017 @default.
W2130301032 countsByYear W21303010322018 @default.
W2130301032 countsByYear W21303010322020 @default.
W2130301032 countsByYear W21303010322021 @default.
W2130301032 countsByYear W21303010322023 @default.
W2130301032 crossrefType "journal-article" @default.
W2130301032 hasAuthorship W2130301032A5070024846 @default.
W2130301032 hasAuthorship W2130301032A5070862606 @default.
W2130301032 hasAuthorship W2130301032A5075580325 @default.
W2130301032 hasAuthorship W2130301032A5087180436 @default.
W2130301032 hasBestOaLocation W21303010321 @default.
W2130301032 hasConcept C104317684 @default.
W2130301032 hasConcept C11960822 @default.
W2130301032 hasConcept C1491633281 @default.
W2130301032 hasConcept C153911025 @default.
W2130301032 hasConcept C181199279 @default.
W2130301032 hasConcept C185592680 @default.
W2130301032 hasConcept C25602115 @default.
W2130301032 hasConcept C27239569 @default.
W2130301032 hasConcept C2780114586 @default.
W2130301032 hasConcept C2780723820 @default.
W2130301032 hasConcept C29512474 @default.
W2130301032 hasConcept C29537977 @default.
W2130301032 hasConcept C55493867 @default.
W2130301032 hasConcept C86339819 @default.
W2130301032 hasConcept C86803240 @default.
W2130301032 hasConcept C87325107 @default.
W2130301032 hasConcept C95444343 @default.
W2130301032 hasConcept C97029542 @default.
W2130301032 hasConcept C98539663 @default.
W2130301032 hasConceptScore W2130301032C104317684 @default.
W2130301032 hasConceptScore W2130301032C11960822 @default.
W2130301032 hasConceptScore W2130301032C1491633281 @default.
W2130301032 hasConceptScore W2130301032C153911025 @default.
W2130301032 hasConceptScore W2130301032C181199279 @default.
W2130301032 hasConceptScore W2130301032C185592680 @default.
W2130301032 hasConceptScore W2130301032C25602115 @default.
W2130301032 hasConceptScore W2130301032C27239569 @default.
W2130301032 hasConceptScore W2130301032C2780114586 @default.
W2130301032 hasConceptScore W2130301032C2780723820 @default.