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Ning Wei, Ph.D.
Research Scientist
Yale University, OML 127
PO Box 208103, 266 Whitney Ave
New Haven, CT 06520
Email: ning.wei@yale.edu
Phone: (203) 432-3897 |
We work on an evolutionarily conserved protein
complex known as the COP9 signalosome (CSN) and
its related molecules in mammalian cell culture
as well as mouse and Arabidopsis genetic systems.
CSN subunits have been identified as signaling
regulators influencing a wide range of cellular
processes including stress and mitogen-activated
protein kinase pathways, cell-cycle progression,
cancer, nuclear hormone receptor mediated gene
expression, plant light responses and flower development.
Structurally, CSN is composed of 8 subunits homologous
to the lid subcomplex of the 26S proteasome. The
CSN signature domains are also found in components
of translation initiation factor 3 (eIF3) complex.
The biochemical activities of CSN are directly
related to the ubiquitin-proteasome pathway.
Ubiquitin (Ub) is a polypeptide that can be
attached by an isopeptide bond to the lysine side
chain of specific protein substrates through an
enzymatic cascade involving Ub-activating enzymes
(E1), Ub conjugating enzymes (E2) and Ub ligases
(E3). The poly-ubiquitin "tagged" proteins are
normally targeted for degradation by the 26S proteasome
so that they can be rapidly removed from the cell.
Covalent modifications by Ub or Ub-like polypeptides
are also used in cells as signals regulating events
such as transcription, nuclear translocation,
and DNA repair. CSN is involved in the conjugation
cycles of the Ub-like protein Nedd8/Rub1, whose
modification on cullin family proteins modulates
the activity and assembly of cullin-based Ub ligase
complexes. CSN acts to remove Nedd8/Rub1 from
cullins through a metalloprotease activity.
With the de-neddylation activity together with
the associated de-ubiquitin activity, CSN regulates
the efficiencies of multiple cullin-based ubiquitin
ligases targeting numerous protein substrates,
many of which cell cycle regulators. This has
been demonstrated in our recent mouse Csn2 knock-out
study, in which de-regulated accumulation of cyclin
E and tumor suppressor p53 have been found in
mutant embryos. Disruption of the CSN complex
in mice leads to early embryonic lethality, which
echoes the lethal phenotype of csn mutants in
Arabidopsis and Drosophila and highlights the
fundamental nature of CSN functions in metazoans.
Conditional knock-out of CSN in mouse is underway
in an effort to investigate the cellular and physiological
function of CSN in vertebrate animal development.
Components of CSN (CSN2 and CSN5/Jab1) have
also been found to bind transcription factors
and nuclear hormone receptors and are believed
to have a role in gene expression. In addition,
we have shown that CSN1 inhibits stress-activated
MAP kinase pathway, suppresses c-Jun phosphorylation,
and it can repress activation of c-fos expression
in response to serum and UV-irradiation. In parallel,
our Arabidopsis genetic study showed that the
N-terminal domain (NTD) of CSN1 carries an unidentified
function essential for plant development and is
distinct from the cullin de-neddylation activity
of the CSN complex. We are actively pursuing this
new aspect of CSN functions.
We are also interested in a group of functionally
related and highly conserved molecules such as
cullins (Ub E3 ligases), DDB1(damaged DNA binding
protein 1), COP1, and DET1. Cullins and DDB1 interact
with CSN biochemically and functionally. COP1
is a component of Ub E3 ligase containing a RING
and WD domain, which ubiquitinates c-Jun and p53
in humans, and photomorphogenic-activating transcription
factors in Arabidopsis. DET1 binds histones in
an acetylation-dependent manner and it forms a
stable complex with DDB1. It is tempting to hypothesis
that DET1 and DDB1 may represent a link between
chromatin activity and the Ub regulatory mechanism.
This will be another focus of our research.
Selected Publications
Lykke-Andersen K, Schaefer L, Menon S, Deng XW,
Miller JB, Wei N. (2003) Disruption of the COP9
Signalosome Csn2 Subunit in Mice Causes Deficient
Cell Proliferation, Accumulation of p53 and Cyclin
E, and Early Embryonic Death. Mol Cell Biol.
23(19):6790-7.
Yang, X, Menon, S, Lykke-Andersen, K. Tsuge,
T., Xiao, D. Wang, X., Rodriguez-Suarez, R. J.,
Zhang,H., and Wei, N (2002) The COP9 signalosome
inhibits p27kip1 degradation and impedes G1-S
phase progression via de-neddylation of SCF Cul1.
Curr. Biol. 12, 667-672.
Tsuge T., Matsui M., and Wei N. (2001) The subunit
1 of the COP9 signalosome suppresses gene expression
through its N-terminal domain and incorporates
into the complex through the PCI domain. J.
Mol. Biol. 305, 1-9.
Wei N., and Deng X.W. (1999). Making sense of
the COP9 signalosome, a regulatory protein complex
conserved from Arabidopsis to human. Trends
Genetics. 15, 98-103.
Wang, H. Kang, D., Deng, X.-W., and Wei, N. (1999)
Evidence for functional conservation of a mammalian
homologue of the light-responsive plant protein
COP1. Curr. Biol. 9, 711-714.
Wei, N., Tsuge, T., Serino., G., Dohmae, N.,
Takio, K., Matsui., M., and Deng, X.-W. (1998).
The COP9 complex is conserved between plants and
mammals and is related to the 26S proteasome regulatory
complex. Curr. Biol. 8, 919-922.
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