A Cytoplasmic Inhibitor of the JNK Signal Transduction Pathway

Dickens, Martin; Rogers, Jeffrey S.; Cavanagh, Julie; Raitano, Art; Xia, Zhengui; Halpern, Jocelyn R.; Greenberg, Michael E.; Sawyers, Charles L.; Davis, Roger J.

doi:10.1126/science.277.5326.693

Cited by 645 publications

(638 citation statements)

References 31 publications

Supporting

Mentioning

603

Contrasting

Unclassified

Order By: Relevance

“…Such transfer is obviously impaired in our tumor cell lines, because we detect inhibitor-containing cyclin E-cdk2 complexes in the cytoplasm. Cyclin E-cdk2(-inhibitor) complexes in transformed cells could be associated with a protein that causes cytoplasmic retention was recently shown for JIP-1 associated JNK (Dickens et al, 1997). A cytoplasmic retention signal can be dominant over the NLS as is the case with cyclin B-cdc2 complexes (Pines and Hunter, 1994).…”

Section: Discussionmentioning

confidence: 93%

Cytoplasmic displacement of cyclin E-cdk2 inhibitors p21Cip1 and p27Kip1 in anchorage-independent cells

1998

View full text Add to dashboard Cite

Loss of attachment to an extracellular matrix substrate arrests the growth of untransformed cells in the G1 phase. This anchorage-dependent cell cycle arrest is linked to increased expression of the p21 Cip1 (p21) and p27 Kip1 (p27) cyclin-dependent kinase inhibitors. The result is a loss of cdk2-associated kinase activity, especially that of cyclin E-cdk2. The levels of p21 and p27 are also upregulated in unattached transformed cells, but cyclin E-cdk2 activity remains high, and the cells are able to grow in an anchorage-independent manner. Increased expression of cyclin E and cdk2 appears to be partially responsible for the maintenance of cyclin E-cdk2 activity in transformed cells. To explore further the regulation of cyclin E-cdk2 in transformed cells, we have analysed the subcellular distribution of cyclin-cdk complexes and their inhibitors in normal human ®broblasts, their transformed counterparts, and in various human tumor cell lines. In substrateattached normal ®broblasts, cyclin E and cdk2 were exclusively in the nuclear fraction, associated with one another. When normal ®broblasts were detached and held in suspension, cyclin E-cdk2 complexes remained nuclear, but were now found associated with the p21 and p27 cdk inhibitors and lacked histone H1 phosphorylating activity. In contrast, the transformed ®broblasts and tumor cells, which are anchorage-independent, had more than half of their cyclin E, cdk2, p21 and p27 in the cytoplasmic fraction, both in attached and suspended cultures. The cytoplasmic p21 and p27 were bound to cyclin E-cdk2, as well as to complexes containing cyclin A and cyclin D. The nuclear cyclin E-cdk2 complexes from the transformed cells grown in suspension contained only low levels of p21 and p27 and had histone H1 kinase activity. Thus, at least three mechanisms contribute to keeping cyclin Ecdk2 complexes active in suspended anchorage-independent cells: cyclin E and cdk2 are upregulated, as reported previously, cdk inhibitors are sequestered away from the nucleus by cytoplasmic cyclin-cdk complexes, and the binding of the inhibitors to nuclear cyclin E-cdk2 complexes is impaired.

show abstract

Section: Discussionmentioning

confidence: 93%

Cytoplasmic displacement of cyclin E-cdk2 inhibitors p21Cip1 and p27Kip1 in anchorage-independent cells

1998

View full text Add to dashboard Cite

show abstract

“…Bcr-Abl also activates SAPK (Raitano et al, 1995). Significantly, both the JIP-1 inhibitor of SAPK and a dominant negative mutant of c-Jun block transforming activity of Bcr-Abl (Dickens et al, 1997;Raitano et al, 1995).These ®ndings have suggested that Bcr-Abl induces Jun-responsive promoters through a Ras-and SAPK-dependent pathway.…”

Section: Introductionmentioning

confidence: 94%

Regulation of Bcr-Abl-induced SAP kinase activity and transformation by the SHPTP1 protein tyrosine phosphatase

et al. 1998

View full text Add to dashboard Cite

The oncogenic Bcr-Abl variant of the c-Abl tyrosine kinase transforms cells by a mechanism dependent on activation of the stress-activated protein kinase (SAPK). Other work has shown that c-Abl interacts with the SHPTP1 protein tyrosine phosphatase in induction of SAPK activity by genotoxic stress. The present studies demonstrate that Bcr-Abl binds constitutively to SHPTP1. We show that Bcr-Abl phosphorylates SHPTP1 on C-terminal Y536 and Y564 sites. The functional signi®cance of the Bcr-Abl/SHPTP1 interaction is supported by the ®nding that SHPTP1 regulates Bcr-Abl-induced SAPK activity. Importantly, SHPTP1 also decreases Bcr-Abl-dependent transformation of ®broblasts. These ®ndings indicate that SHPTP1 functions as a tumor suppressor in cells transformed by Bcr-Abl.

show abstract

“…IB1/ JIP-1 can influence JNK signalling both positively and negatively, depending on the amounts of IB1/JIP-1 and its interacting kinases. [19][20][21] Our aim is to identify the critical features of the powerful protective action of the D-JNKI1 peptide and to examine JNK targets in excitotoxic neuronal death pathways. This can offer important clues to produce new inhibitors of excitotoxicity.…”

mentioning

confidence: 99%

Role of the JNK pathway in NMDA-mediated excitotoxicity of cortical neurons

et al. 2006

View full text Add to dashboard Cite

Excitotoxic insults induce c-Jun N-terminal kinase (JNK) activation, which leads to neuronal death and contributes to many neurological conditions such as cerebral ischemia and neurodegenerative disorders. The action of JNK can be inhibited by the Dretro-inverso form of JNK inhibitor peptide (D-JNKI1), which totally prevents death induced by N-methyl-D-aspartate (NMDA) in vitro and strongly protects against different in vivo paradigms of excitotoxicity. To obtain optimal neuroprotection, it is imperative to elucidate the prosurvival action of D-JNKI1 and the death pathways that it inhibits. In cortical neuronal cultures, we first investigate the pathways by which NMDA induces JNK activation and show a rapid and selective phosphorylation of mitogen-activated protein kinase kinase 7 (MKK7), whereas the only other known JNK activator, mitogen-activated protein kinase kinase 4 (MKK4) In many nervous system disorders, including cerebral ischemia, traumatic brain injury and neurodegenerative diseases, overactivation of N-methyl-d-aspartate (NMDA) receptors leads to neuronal damage, resulting in neuronal loss and consequent severe neurological impairment. This cascade of neuronal injury, referred to as 'excitotoxicity', is still only partly understood. Dying neurons activate complex signal transduction events to trigger their death program, and the c-Jun N-terminal kinase (JNK) pathway plays an important role in this process. 1 D-retro-inverso form of JNK inhibitor (D-JNKI1) is an extremely potent neuroprotectant against excitotoxicity of cortical neurons and against different in vivo paradigms of neurodegeneration. [2][3][4] The active part of this peptide contains a retro-inverso form of a 20-amino-acid sequence (JBD 20 ) from the JNK-binding domain (JBD) of the scaffold protein JNK-interacting protein-1 (IB1/JIP-1), and it blocks the access of JNK to many of its targets. [5][6][7] Recently, Negri et al. 8,9 performed a detailed re-examination of the JBD-containing proteins and identified 19 different substrates of JNK. They then proved in a cell-free assay that the JBD 20 sequence prevented interactions and phosphorylations by JNK of nine of these targets. Among these nine substrates, we have studied the following four that might participate in regulating the death of cortical neurons: (1) MADD/DENN (MAPK-activating death domain-containing protein/differentially expressed in normal and neoplastic cells); (2-3) mitogen-activated protein kinase kinase 4 (MKK4) and mitogen-activated protein kinase kinase 7 (MKK7), the two direct upstream activators of JNK and (4) the scaffold protein IB1/JIP-1.,In particularly, MADD/DENN was identified as a substrate for JNK3, 10 the isoform most clearly involved in excitotoxicity 11,12 and mostly expressed in the brain. [10][11][12] Increasing evidence supports a strong correlation between low MADD/ DENN expression and neuronal loss. 13,14 MKK4 and MKK7 are the only known JNK activators. In some cell types, MKK4 activates JNK primarily by stress stimuli and MKK7 by inflammatory cytoki...

show abstract

A Cytoplasmic Inhibitor of the JNK Signal Transduction Pathway

Cited by 645 publications

References 31 publications

Cytoplasmic displacement of cyclin E-cdk2 inhibitors p21Cip1 and p27Kip1 in anchorage-independent cells

Cytoplasmic displacement of cyclin E-cdk2 inhibitors p21Cip1 and p27Kip1 in anchorage-independent cells

Regulation of Bcr-Abl-induced SAP kinase activity and transformation by the SHPTP1 protein tyrosine phosphatase

Role of the JNK pathway in NMDA-mediated excitotoxicity of cortical neurons

Contact Info

Product

Resources

About