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Query: UNIPROT:P20226 (
TATA-binding protein
)
1,297
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
The CT element is a positively acting homopyrimidine tract upstream of the c-myc gene to which the well-characterized transcription factor Spl and heterogeneous nuclear ribonucleoprotein (hnRNP) K, a less well-characterized protein associated with hnRNP complexes, have previously been shown to bind. The present work demonstrates that both of these molecules contribute to CT element-activated transcription in vitro. The pyrimidine-rich strand of the CT element both bound to
hnRNP K
and competitively inhibited transcription in vitro, suggesting a role for
hnRNP K
in activating transcription through this single-stranded sequence. Direct addition of recombinant
hnRNP K
to reaction mixtures programmed with templates bearing single-stranded CT elements increased specific RNA synthesis. If
hnRNP K
is a transcription factor, then interactions with the RNA polymerase II transcription apparatus are predicted. Affinity columns charged with recombinant
hnRNP K
specifically bind a component(s) necessary for transcription activation. The depleted factors were biochemically complemented by a crude TFIID phosphocellulose fraction, indicating that
hnRNP K
might interact with the
TATA-binding protein
(
TBP
)-TBP-associated factor complex. Coimmunoprecipitation of a complex formed in vivo between
hnRNP K
and epitope-tagged
TBP
as well as binding in vitro between recombinant proteins demonstrated a protein-protein interaction between
TBP
and
hnRNP K
. Furthermore, when the two proteins were overexpressed in vivo, transcription from a CT element-dependent reporter was synergistically activated. These data indicate that
hnRNP K
binds to a specific cis element, interacts with the RNA polymerase II transcription machinery, and stimulates transcription and thus has all of the properties of a transcription factor.
...
PMID:Heterogeneous nuclear ribonucleoprotein K is a transcription factor. 862 2
Translation initiation factor eukaryotic translation initiation factor 4E (eIF4E) plays a key role in regulation of cellular proliferation. Its effects on the m7GpppN mRNA cap are critical because overexpression of eIF4E transforms cells, and eIF4E function is rate-limiting for G1 passage. Although we identified eIF4E as a c-Myc target, little else is known about its transcriptional regulation. Previously, we described an element at position -25 (TTACCCCCCCTT) that was critical for eIF4E promoter function. Here we report that this sequence (named 4EBE, for eIF4E basal element) functions as a basal promoter element that binds
hnRNP K
. The 4EBE is sufficient to replace TATA sequences in a heterologous reporter construct. Interactions between 4EBE and upstream activator sites are position, distance, and sequence dependent. Using DNA affinity chromatography, we identified
hnRNP K
as a 4EBE-binding protein. Chromatin immunoprecipitation, siRNA interference, and
hnRNP K
overexpression demonstrate that
hnRNP K
can regulate eIF4E mRNA. Moreover,
hnRNP K
increased translation initiation, increased cell division, and promoted neoplastic transformation in an eIF4E-dependent manner.
hnRNP K
binds the
TATA-binding protein
, explaining how the 4EBE might replace TATA in the eIF4E promoter.
hnRNP K
is an unusually diverse regulator of multiple steps in growth regulation because it also directly regulates c-myc transcription, mRNA export, splicing, and translation initiation.
...
PMID:hnRNP K binds a core polypyrimidine element in the eukaryotic translation initiation factor 4E (eIF4E) promoter, and its regulation of eIF4E contributes to neoplastic transformation. 1602 82
