MAPK15
MAPK15
MAPK15
inright uterine tubeolfactory zone of nasal mucosaleft testisright testisleft lobe of thyroid glandleft
function
transferase activity
nucleotide binding
protein binding
ATP binding
kinase activity
chromatin binding
Cellular component
extracellular region
nucleus
cytoplasm
autophagosome
centriole
cell-cell junction
axoneme
Golgi apparatus
meiotic spindle
spindle
cytoskeleton
cell junction
cytoplasmic vesicle
cell projection
Biological process
phosphorylation
protein phosphorylation
MAPK cascade
protein autophosphorylation
regulation of gene expression
regulation of autophagy
dopamine uptake
Sources:Amigo /
QuickGOOrthologsSpeciesHumanMouseEntrez225689332110EnsemblENSG00000181085ENSG0
0000274205ENSMUSG00000063704UniProtQ8TD08Q80Y86RefSeq
HumanView/Edit Mouse
Mitogen-activated protein kinase 15, also known as MAPK15, ERK7, or ERK8, is an enzyme that in
Function[edit]
The protein encoded by this gene is a member of the MAP (mitogen-activated protein) kinase family.
MAP kinases are also known as extracellular signal-regulated kinases (ERKs), and are involved in
differentiation, and transcriptional regulation. MAPK15 is often referred to as ERK7 or ERK8, and
the latter two share 69% amino acid sequence similarity; at least one study has suggested that the
In vertebrate models, ERK8 is not constitutively active, and exhibits relatively low basal kinase
activity.[7] It contains two SH3 (SRC homology 3) binding motifs in its C-terminal region, and is likely
proto-oncogene) that has been implicated in cancer growth and progression in humans when it is
overexpressed. The exact function of MAPK15 is unknown, though a number of studies have
Specifically, MAPK15 expression is significantly reduced in human lung and breast carcinomas, and
MAPK15 down-regulation is correlated with increased cell motility.[7] MAPK15 has also been found
which a sugar molecule is covalently attached to an oxygen atom on an amino acid residue.[7]
Mammalian MAPK15 is a putative regulator of the cellular localization and transcriptional activity of
estrogen-related receptor alpha (ERRa), as well as an inhibitor of proliferating cell nuclear antigen
(PCNA) degradation.[8][9] PCNA is critical for DNA replication, and is an essential factor in
protecting genome stability. MAPK15 has also been shown to regulate ciliogenesis in X. laevis
Interactions[edit]
protein (GABARAP) and microtubule-associated proteins 1A/1B light chain 3A (MAP1LC3A, or LC3)
in a process that stimulates autophagy.[11] A number of additional proteins also interact with
Due to its role in protecting genomic integrity and cell motility, MAPK15 has been identified as a
potential target for cancer therapeutics.[12] Additionally, given the putative role that MAPK15 plays
in the regulation of ciliogenesis, it may be an ideal target for diseases related to human ciliary
References[edit]
^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National
Library of Medicine.
^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library
of Medicine.
^ a b Abe MK, Saelzler MP, Espinosa R, Kahle KT, Hershenson MB, Le Beau MM, Rosner MR (May
2002). "ERK8, a new member of the mitogen-activated protein kinase family". The Journal of
cellular localization and inhibits its transcriptional activity". The Journal of Biological Chemistry. 286
^ Groehler AL, Lannigan DA (Aug 2010). "A chromatin-bound kinase, ERK8, protects genomic
integrity by inhibiting HDM2-mediated degradation of the DNA clamp PCNA". The Journal of Cell
PMID 25823377.
Pianella A, Chiariello M (Dec 2012). "MAPK15/ERK8 stimulates autophagy by interacting with LC3
PMID 22948227.
"Structure prediction and validation of the ERK8 kinase domain". PLOS ONE. 8 (1): e52011.
PMID 23326322.
Further reading[edit]
Saelzler MP, Spackman CC, Liu Y, Martinez LC, Harris JP, Abe MK (Jun 2006). "ERK8
Chiariello M (Apr 2006). "Activation of the Erk8 mitogen-activated protein (MAP) kinase by
RET/PTC3, a constitutively active form of the RET proto-oncogene" (PDF). The Journal of Biological
Klevernic IV, Stafford MJ, Morrice N, Peggie M, Morton S, Cohen P (Feb 2006). "Characterization of
the reversible phosphorylation and activation of ERK8". The Biochemical Journal. 394 (Pt 1):
(Sep 2004). "Sequence comparison of human and mouse genes reveals a homologous block
Kinet S, Bernard F, Mongellaz C, Perreau M, Goldman FD, Taylor N (Oct 2002). "gp120-mediated
induction of the MAPK cascade is dependent on the activation state of CD4(+) lymphocytes". Blood.
Qian Z, Okuhara D, Abe MK, Rosner MR (Jan 1999). "Molecular cloning and characterization of a
External links[edit]
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