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Query: UMLS:C0004134 (
ataxia
)
15,886
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Chance discovery of spontaneous mutants with atrophy of the cerebellar cortex has unearthed genes involved in optimizing motor coordination. Rotorod, stationary beam, and suspended wire tests are useful in delineating behavioral phenotypes of spontaneous mutants with cerebellar atrophy such as Grid2
Lc
, Grid2
ho
, Rora
sg
, Agtpbp1
pcd
, Reln
rl
, and Dab1
scm
. Likewise, transgenic or null mutants serving as experimental models of spinocerebellar
ataxia
(SCA) are phenotyped with the same tests. Among experimental models of autosomal dominant SCA, rotorod deficits were reported in SCA1 to 3, SCA5 to 8, SCA14, SCA17, and
SCA27
and stationary beam deficits in SCA1 to 3, SCA5, SCA6, SCA13, SCA17, and
SCA27
. Beam tests are sensitive to experimental therapies of various kinds including molecules affecting glutamate signaling, mesenchymal stem cells, anti-oligomer antibodies, lentiviral vectors carrying genes, interfering RNAs, or neurotrophic factors, and interbreeding with other mutants.
...
PMID:Motor Performances of Spontaneous and Genetically Modified Mutants with Cerebellar Atrophy. 3082 Aug 66
Multiple voltage-gated Na
+
(Nav) channelopathies can be ascribed to subtle changes in the Nav macromolecular complex.
Fibroblast growth factor 14
(
FGF14
) is a functionally relevant component of the Nav1.6 channel complex, a causative link to spinocerebellar
ataxia
27 (SCA27) and an emerging risk factor for neuropsychiatric disorders. Yet, how this protein:channel complex is regulated in the cell is still poorly understood. To search for key cellular pathways upstream of the
FGF14
:Nav1.6 complex, we have developed, miniaturized and optimized an in-cell assay in 384-well plates by stably reconstituting the
FGF14
:Nav1.6 complex using the split-luciferase complementation assay. We then conducted a high-throughput screening (HTS) of 267 FDA-approved compounds targeting known mediators of cellular signaling. Of the 65 hits initially detected, 24 were excluded based on counter-screening and cellular toxicity. Based on target analysis, potency and dose-response relationships, 5 compounds were subsequently repurchased for validation and confirmed as hits. Among those, the tyrosine kinase inhibitor lestaurtinib was highest ranked, exhibiting submicromolar inhibition of
FGF14
:Nav1.6 assembly. While providing evidence for a robust in-cell HTS platform that can be adapted to search for any channelopathy-associated regulatory proteins, these results lay the potential groundwork for repurposing cancer drugs for neuropsychopharmacology.
...
PMID:High-throughput screening against protein:protein interaction interfaces reveals anti-cancer therapeutics as potent modulators of the voltage-gated Na
+
channel complex. 3172 29
We report four patients from two families who presented attacks of childhood-onset episodic
ataxia
associated with pathogenic mutations in the
FGF14
gene. Attacks were triggered by fever, lasted several days, and had variable frequencies. Nystagmus and/or postural tremor and/or learning disabilities were noticed in individuals harboring
FGF14
mutation with or without episodic
ataxia
. These cases and literature data delineate the
FGF14
-mutation-related episodic
ataxia
phenotype: wide range of age at onset (from childhood to adulthood), variable durations and frequencies, triggering factors including fever, and association to chronic symptoms. We propose to add
FGF14
-related episodic
ataxia
to the list of primary episodic
ataxia
as Episodic
Ataxia
type 9.
...
PMID:FGF14-related episodic ataxia: delineating the phenotype of Episodic Ataxia type 9. 3216 47
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