Inflammatory signals, changes in levels of
reactive oxygen species, ultraviolet radiation, protein synthesis inhibitors, and a variety of stress stimuli can activate JNK. One way this activation may occur is through disruption of the conformation of sensitive
protein phosphatase enzymes; specific phosphatases normally inhibit the activity of JNK itself and the activity of proteins linked to JNK activation. JNKs can associate with
scaffold proteins
JNK interacting proteins (JIP) as well as their upstream kinases
JNKK1 and
JNKK2 following their activation. JNK, by phosphorylation, modifies the activity of numerous proteins that reside at the mitochondria or act in the nucleus. Downstream molecules that are activated by JNK include
c-Jun,
ATF2,
ELK1,
SMAD4,
p53 and
HSF1. The downstream molecules that are inhibited by JNK activation include
NFAT4,
NFATC1 and
STAT3. By activating and inhibiting other small molecules in this way, JNK activity regulates several important cellular functions including cell growth, differentiation, survival and apoptosis. JNK1 is involved in
apoptosis,
neurodegeneration, cell differentiation and proliferation, inflammatory conditions and
cytokine production mediated by AP-1 (
activation protein 1) such as
RANTES,
IL-8 and
GM-CSF. Recently, JNK1 has been found to regulate
Jun protein turnover by
phosphorylation and activation of the
ubiquitin ligase Itch.
Neurotrophin binding to
p75NTR activates a JNK signaling pathway causing apoptosis of developing neurons. JNK, through a series of intermediates, activates
p53 and p53 activates
Bax which initiates apoptosis.
TrkA can prevent p75NTR-mediated JNK pathway apoptosis. JNK can directly phosphorylate Bim-EL, a splicing
isoform of
Bcl-2 interacting mediator of cell death (Bim), which activates Bim-EL apoptotic activity. JNK activation is required for apoptosis but
c-jun, a protein involved in the JNK pathway, is not always required. ==Roles in DNA repair==