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Sandbox GGC16
From Proteopedia
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== Function == | == Function == | ||
| - | <scene name='87/874948/Earpurinerich/2'>Bases at Interface</scene> Within the nucleus, PU.1 activates transcription of lymphoid genes by binding DNA during hematopoiesis. The name PU.1 comes from the protein's binding interactions with a purine-rich DNA sequence. | + | <scene name='87/874948/Earpurinerich/2'>Bases at Interface</scene> Within the nucleus, PU.1 activates transcription of lymphoid genes by binding DNA during hematopoiesis. The name PU.1 comes from the protein's binding interactions with a purine-rich DNA sequence (5'-GAGGAA-3'). |
=== Activation === | === Activation === | ||
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PU.1 can exhibit protein-protein interaction. As a transcription factor, it binds DNA as a monomer. However, it can dimerize on a longer, downstream binding site. Interestingly, other Ets family proteins that a structurally homologous cannot bind DNA in as a 2:1, dimer complex. A study suggested that the 2:1 complex formation could be a mechanism of auto-inhibition.<ref>Esaki, S., Evich, M. G., Erlitzki, N., Germann, M. W., & Poon, G. M. K. (2017). Multiple DNA-binding modes for the ETS family transcription factor PU.1. Journal of Biological Chemistry, 292(39), 16044–16054. https://doi.org/https://doi.org/10.1074/jbc.M117.798207 </ref> | PU.1 can exhibit protein-protein interaction. As a transcription factor, it binds DNA as a monomer. However, it can dimerize on a longer, downstream binding site. Interestingly, other Ets family proteins that a structurally homologous cannot bind DNA in as a 2:1, dimer complex. A study suggested that the 2:1 complex formation could be a mechanism of auto-inhibition.<ref>Esaki, S., Evich, M. G., Erlitzki, N., Germann, M. W., & Poon, G. M. K. (2017). Multiple DNA-binding modes for the ETS family transcription factor PU.1. Journal of Biological Chemistry, 292(39), 16044–16054. https://doi.org/https://doi.org/10.1074/jbc.M117.798207 </ref> | ||
| + | === Other Protein Interactions === | ||
| + | PU.1 can interact with GATA-2, another endothelial transcription factor responsible for leukocyte development. This interaction has been observed | ||
== Disease == | == Disease == | ||
Revision as of 21:46, 27 April 2021
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