Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
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Target Concepts:
Gene/Protein
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Query: UMLS:C0039483 (
giant cell arteritis
)
3,204
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Nearly 1 million Alu elements in human DNA were inserted by an RNA-mediated retroposition-amplification process that clearly decelerated about 30 million years ago. Since then, Alu sequences have proliferated at a lower rate, including within the human genome, in which Alu mobility continues to generate genetic variability. Initially derived from 7SL RNA of the signal recognition particle (SRP), Alu became a dominant retroposon while retaining secondary structures found in 7SL RNA. We previously identified a human Alu RNA-binding protein as a homolog of the 14-kDa Alu-specific protein of SRP and have shown that its expression is associated with accumulation of 3'-processed Alu RNA. Here, we show that in early anthropoids, the gene encoding
SRP14
Alu RNA-binding protein was duplicated and that
SRP14
-homologous sequences currently reside on different human chromosomes. In anthropoids, the active
SRP14
gene acquired a
GCA
trinucleotide repeat in its 3'-coding region that produces
SRP14
polypeptides with extended C-terminal tails. A C-->G substitution in this region converted the mouse sequence CCA
GCA
to
GCA
GCA
in prosimians, which presumably predisposed this locus to
GCA
expansion in anthropoids and provides a model for other triplet expansions. Moreover, the presence of the trinucleotide repeat in
SRP14
DNA and the corresponding C-terminal tail in
SRP14
are associated with a significant increase in
SRP14
polypeptide and Alu RNA-binding activity. These genetic events occurred during the period in which an acceleration in Alu retroposition was followed by a sharp deceleration, suggesting that Alu repeats coevolved with C-terminal variants of
SRP14
in higher primates.
...
PMID:A trinucleotide repeat-associated increase in the level of Alu RNA-binding protein occurred during the same period as the major Alu amplification that accompanied anthropoid evolution. 753 78
