TYK2 a
Janus
kinase, contains a
C-terminal protein tyrosine kinase
catalytic
domain and has no
N-
terminal signal peptide or transmembrane
domain,
of coding regions of exons and the adjacent intronic
DNA sequences,
identical to
tyk2 of mutant
Tyk2 forms deleted at the N terminus locus:19p13.2 [
§§], a human
mRNA (rs2304256) exon¤ encoding a
non-receptor protein
tyrosine kinase, the Tyk2
deficiency is likely to account for the
phenotype by
preventing* Tyk2
tyrosine phosphorylation for interferon (
IFN) responses and Stat
activation. STAT1 and STAT3 translocated to the nucleus following
PAF
(platelet-activating factor) stimulation in the presence of TYK2 in
controlling responses to multiple cytokines
IFNAR1 (the Tyr-based
endocytic motif within) or
PLAUR (a UPA receptor)
urokinase signaling complex
uPA containing TYK2 and phosphatidylinositol
3-kinase
PI3K stabilized at the cell surface are downstream
events
binding to the
type I IFN receptor complex a pathway that
supplements ISGF3/interferon-stimulated response element, and
IRF5 a
regulator. (IFNaR1) domain (dimerized) is required to induce
phosphorylation
of binding
helical
bundled cytokines
and TYK2
phenotypes
ability at binding and signal transduction to the
nucleus for the acquisition of
DNA binding activity, and modulates uPAR dependent functional responses in upregulation of
C5aR* expression.
Mutations in TYK2 and STAT3 mostly impair
IL-6R* responses, and
polymorphisms¤.
Phenylephrine ‡ induced
tyrosine phosphorylation of Jak2, Tyk2, and STAT1. TYK2, has an SH2
domain that contains a
histidine instead of arginine (semi- vs essential amino acid) it may have
lost the
ability on
ligand-induced signaling to bind
phosphotyrosine at a neutral pH of 7. Either of the
two Src homology 2(
SH2)
p85 domains binds the
pseudokinase domain (a
hypothetical masking complex) of TYK2 directly.
 |
| 3lnx light Magneta,
3nzo by chain colors CHNOS, 1bf5-1ynl cartoon Hidden MM prediction model
all centered on 1bf5 DNA of binding helical bundled cytokines and TYK2
of coding regions of exons and the adjacent intronic DNA sequences by
3nzo unspecified 3nxo ligands GBR in foreground. |
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