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Translation initiation factor eIF2: Initiation and Recycling
Phosphorylation of eIF2a reduces the concentration of the eIF2-GTP-tRNAMet
eIF2-GTP-tRNAMet
Ternary
eIF2 Complex
b
a
GTP
GTP
g
tRNAMet
40S
40S
eIF2B
eIF2a
kinase
GTP
PO3
GDP
tRNAMet
40S
GTP
5’cap tRNAMet
40S
GTP
tRNAMet
40S
GTP
tRNAMet
AUG
60S
40S
60S
High concentration of eIF2-GTP-tRNAMet
GDP
GTP
Repressed
translation
GDP
40S
40S
40S 40S
GTP
60SuORF
60S
GTP
40S
GTP
GCN4
60SuORF
60S
Low concentration of eIF2-GTP-tRNAMet
GDP
40S
GTP
GTP
60SuORF
40S
40S uORF
40S
GTP
GDP
40S
GTP
Derepressed
translation
GCN4
40S
60S
60S
Selection of alternative in-frame start codons are sensitive to eIF2 alpha phosphorylation
AUG
AUG
eIF2a kinases
Heme deprivation
(disassociation of hemin)
Amino acid deprivation
(binding uncharged tRNAs)
Calcium mobilization
or misfolded proteins
(disassociation of BiP-GRP78)
GCN2
Viral infection
(binding dsRNA)
HRI
PERK
PKR
PO3
b
(-)
Initiation of protein synthesis
a
NRF-2
g eIF2
Transcription
(+)
mRNA specific translation initiation
Activation of PERK via ER stress and loss of ER calcium
Endoplasmic reticulum
Thapsigargin
SERCA
BiP
Ca2+ = 5x10-5M
RyR
Ca2+
IP3R
ATP
Inactive
Activated
PERK
PERK
Repression of global
Adaptation to
protein synthesis
stress or apoptosis
(e.g. activation ATF-4 -> CHOP)
Receptor-mediated generation of IP3 and/or activation of voltage-gated channels
stimulates ER calcium mobilization
Ligand
and activation of PERK
Ca2+
GCPR
Endoplasmic reticulum
SERCA
BiP
Ca2+ = 5x10-5M
IP3
IP3R
Ca2+
RyR
Ca2+
ATP
Inactive
Activated
PERK
PERK
Glucose metabolism increases ER calcium and represses PERK
glucose
....
...
....
exocytosis
VGCC
K+ATP
GLUT2
PMCA
plasma membrane
Ca2+
Ca2+ (10-7M)
K+
Ca2+
IP3R
ATP
Secreted proteins
Secretory machinery
Differentiation factors
Proliferatiaon factors
SERCA
ER
BiP
Ca2+ (5x10-5M)
nucleus
Transcription
factors
Inactive PERK
Activated
dimerized PERK
Translation control of
specific mRNAs
Glucose metabolism generating
driving transient
ATP and
calcium-induced
driving sustainted
calcium
release from
Calcium
uptake
the in
ERthe ER by the SERCA calcium pump ATPase
Glucose
Ca2+
ATP
ATP
Endoplasmic reticulum
SERCA
BiP
Ca2+
Ca2+
RyR
Ca2+
RYR
Ca2+
ATP
Inactive
Activated
PERK
PERK
Extracellular physiological, developmental, and stress signals
PERK
sensor
Protein
synthesis
Intracellular signals
ER signals
ER
Translation
of specific
genes
Reduction of
co-translational
import
nucleus
Modulation of secretory capacity:
maintenance of differentiated state, cell
mass, secretory machinery
PERK regulates a continuum of normal developmental and
ER stress related processes
Normal developmental and physiological modulation of
ER activity regulates PERK activity which in turn
activates/represses genes that modulate normal
growth and development.
ER stress hyperactivates PERK leading to the activation of
stress response genes.
Thus, the degree to which PERK is activated determines
which particular subset of regulatory circuits are activated or
repressed.
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