Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Pivot Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Target Concepts:
Gene/Protein
Disease
Symptom
Drug
Enzyme
Compound
Query: EC:3.1.3.16 (
calcineurin
)
17,112
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Medulloblastoma is the most common malignant childhood brain tumor. The
protein phosphatase
and oncogene
WIP1
is over-expressed or amplified in a significant number of primary human medulloblastomas and cell lines. In the present study, we examine an important mechanism by which
WIP1
promotes medulloblastoma growth using in vitro and in vivo models. Human cell lines and intracerebellar xenografted animal models were used to study the role of
WIP1
and the major TP53 regulator, HDM2, in medulloblastoma growth. Stable expression of
WIP1
enhances growth of TP53 wild-type medulloblastoma cells, compared with cells with stable expression of an empty-vector or mutant
WIP1
. In an animal model,
WIP1
enhances proliferation and reduces the survival of immunodeficient mice bearing intracerebellar xenografted human medulloblastoma cells. Cells with increased
WIP1
expression also exhibit increased expression of HDM2. HDM2 knockdown or treatment with the HDM2 inhibitor Nutlin-3a, the active enantomer of Nutlin-3, specifically inhibits the growth of medulloblastoma cells with increased
WIP1
expression. Nutlin-3a does not affect growth of medulloblastoma cells with stable expression of an empty vector or of mutant
WIP1
. Knockdown of
WIP1
or treatment with the
WIP1
inhibitor CCT007093 results in increased phosphorylation of known
WIP1
targets, reduced HDM2 expression, and reduced growth specifically in
WIP1
wild-type and high-expressing medulloblastoma cells. Combined
WIP1
and HDM2 inhibition is more effective than
WIP1
inhibition alone in blocking growth of
WIP1
high-expressing medulloblastoma cells. Our preclinical study supports a role for therapies that target
WIP1
and HDM2 in the treatment of medulloblastoma.
...
PMID:HDM2 promotes WIP1-mediated medulloblastoma growth. 2237 89
High-level amplification of the
protein phosphatase
PPM1D (
WIP1
) is present in a subset of medulloblastomas (MBs) that have an expression profile consistent with active Sonic Hedgehog (SHH) signaling. We found that
WIP1
overexpression increased expression of Shh target genes and cell proliferation in response to Shh stimulation in NIH3T3 and cerebellar granule neuron precursor cells in a p53-independent manner. Thus, we developed a mouse in which
WIP1
is expressed in the developing brain under control of the Neurod2 promoter (ND2:
WIP1
). The external granule layer (EGL) in early postnatal ND2:
WIP1
mice exhibited increased proliferation and expression of Shh downstream targets. MB incidence increased and survival decreased when ND2:
WIP1
mice were crossed with an Shh-activated MB mouse model. Conversely, Wip1 knockout significantly suppressed MB formation in two independent mouse models of Shh-activated MB. Furthermore, Wip1 knockdown or treatment with a
WIP1
inhibitor suppressed the effects of Shh stimulation and potentiated the growth inhibitory effects of SHH pathway-inhibiting drugs in Shh-activated MB cells in vitro. This suggests an important cross-talk between SHH and
WIP1
pathways that accelerates tumorigenesis and supports
WIP1
inhibition as a potential treatment strategy for MB.
...
PMID:WIP1 modulates responsiveness to Sonic Hedgehog signaling in neuronal precursor cells and medulloblastoma. 2708 29
