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Query: UMLS:C0013421 (
dystonia
)
8,418
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Although manganese is an essential trace metal, little is known about its transport and homeostatic regulation. Here we have identified a cohort of patients with a novel autosomal recessive manganese transporter defect caused by mutations in
SLC39A14
. Excessive accumulation of manganese in these patients results in rapidly progressive childhood-onset parkinsonism-
dystonia
with distinctive brain magnetic resonance imaging appearances and neurodegenerative features on post-mortem examination. We show that mutations in
SLC39A14
impair manganese transport in vitro and lead to manganese dyshomeostasis and altered locomotor activity in zebrafish with CRISPR-induced slc39a14 null mutations. Chelation with disodium calcium edetate lowers blood manganese levels in patients and can lead to striking clinical improvement. Our results demonstrate that
SLC39A14
functions as a pivotal manganese transporter in vertebrates.
...
PMID:Mutations in SLC39A14 disrupt manganese homeostasis and cause childhood-onset parkinsonism-dystonia. 2773 5
Mutations in human
ZIP14
have been linked to symptoms of the early onset of Parkinsonism and
Dystonia
. This phenotype is likely related to excess manganese accumulation in the CNS. The metal transporter ZIP14 (
SLC39A14
) is viewed primarily as a zinc transporter that is inducible via proinflammatory stimuli.
In vitro
evidence shows that ZIP14 can also transport manganese. To examine a role for ZIP14 in manganese homeostasis, we used
Zip14
knock-out (KO) male and female mice to conduct comparative metabolic, imaging, and functional studies. Manganese accumulation was fourfold to fivefold higher in brains of
Zip14
KO mice compared with young adult wild-type mice. There was less accumulation of subcutaneously administered
54
Mn in the liver, gallbladder, and gastrointestinal tract of the KO mice, suggesting that manganese elimination is impaired with
Zip14
ablation. Impaired elimination creates the opportunity for atypical manganese accumulation in tissues, including the brain. The intensity of MR images from brains of the
Zip14
KO mice is indicative of major manganese accumulation. In agreement with excessive manganese accumulation was the impaired motor function observed in the
Zip14
KO mice. These results also demonstrate that ZIP14 is not essential for manganese uptake by the brain. Nevertheless, the upregulation of signatures of brain injury observed in the
Zip14
KO mice demonstrates that normal ZIP14 function is an essential factor required to prevent manganese-linked neurodegeneration.
SIGNIFICANCE STATEMENT
Manganese is an essential micronutrient. When acquired in excess, manganese accumulates in tissues of the CNS and is associated with neurodegenerative disease, particularly Parkinson-like syndrome and
dystonia
. Some members of the ZIP metal transporter family transport manganese. Using mutant mice deficient in the ZIP14 metal transporter, we have discovered that ZIP14 is essential for manganese elimination via the gastrointestinal tract, and a lack of ZIP14 results in manganese accumulation in critical tissues such as the brain, as measured by MRI, and produces signatures of brain injury and impaired motor function. Humans with altered ZIP14 function would lack this gatekeeper function of ZIP14 and therefore would be prone to manganese-related neurological diseases.
...
PMID:Metal Transporter
Zip14
(
Slc39a14
) Deletion in Mice Increases Manganese Deposition and Produces Neurotoxic Signatures and Diminished Motor Activity. 2853 73
SLC39A14
(also known as ZIP14), a member of the SLC39A transmembrane metal transporter family, has been reported to mediate the cellular uptake of iron and zinc. Recently, however, mutations in the
SLC39A14
gene have been linked to manganese (Mn) accumulation in the brain and childhood-onset parkinsonism
dystonia
. It has therefore been suggested that
SLC39A14
deficiency impairs hepatic Mn uptake and biliary excretion, resulting in the accumulation of Mn in the circulation and brain. To test this hypothesis, we generated and characterized global
Slc39a14
-knockout (
Slc39a14
-/-
) mice and hepatocyte-specific
Slc39a14
-knockout (
Slc39a14
fl/fl
;Alb-Cre
+
) mice.
Slc39a14
-/-
mice develop markedly increased Mn concentrations in the brain and several extrahepatic tissues, as well as motor deficits that can be rescued by treatment with the metal chelator Na
2
CaEDTA. In contrast,
Slc39a14
fl/fl
;Alb-Cre
+
mice do not accumulate Mn in the brain or other extrahepatic tissues and do not develop motor deficits, indicating that the loss of
Slc39a14
expression selectively in hepatocytes is not sufficient to cause Mn accumulation. Interestingly,
Slc39a14
fl/fl
;Alb-Cre
+
mice fed a high Mn diet have increased Mn levels in the serum, brain and pancreas, but not in the liver. Taken together, our results indicate that
Slc39a14
-/-
mice develop brain Mn accumulation and motor deficits that cannot be explained by a loss of
Slc39a14
expression in hepatocytes. These findings provide insight into the physiological role that
SLC39A14
has in maintaining Mn homeostasis. Our tissue-specific
Slc39a14
-knockout mouse model can serve as a valuable tool for further dissecting the organ-specific role of
SLC39A14
in regulating the body's susceptibility to Mn toxicity.
...
PMID:Manganese transporter Slc39a14 deficiency revealed its key role in maintaining manganese homeostasis in mice. 2875 76
Congenital disorders of manganese metabolism are rare occurrences in children, and medical management of these disorders is complex and challenging. Homozygous exonic mutations in the manganese transporter
SLC39A14
have recently been associated with a pediatric-onset neurodegenerative disorder characterized by brain manganese accumulation and clinical signs of manganese neurotoxicity, including parkinsonism-
dystonia
. We performed whole exome sequencing on DNA samples from two unrelated female children from the United Arab Emirates with progressive movement disorder and brain mineralization, identified a novel homozygous intronic mutation in
SLC39A14
in both children, and demonstrated that the mutation leads to aberrant splicing. Both children had consistently elevated serum manganese levels and were diagnosed with
SLC39A14
-associated manganism. Over a four-year period, we utilized a multidisciplinary management approach for Patient 1 combining decreased manganese dietary intake and chelation with symptomatic management of
dystonia
. Our treatment strategy appeared to slow disease progression, but did not lead to a cure or reversal of already established deficits. Clinicians should consider testing for noncoding mutations in the diagnosis of congenital disorders of manganese metabolism and utilizing multidisciplinary approaches in the management of these disorders.
...
PMID:Novel founder intronic variant in SLC39A14 in two families causing Manganism and potential treatment strategies. 2968 58
Mouse models that replicate facets of human neurological diseases are often used at the pre-clinical stage to better understand the underlying mechanisms of a disease and test the target engagement of potential therapeutic interventions. We recently characterized a mouse model of childhood-onset parkinsonism-
dystonia
, a disease caused by a homozygous loss-of-function mutation in the
SLC39A14
gene. The disease manifests itself phenotypically by impairments in locomotor behaviour and postural abnormalities. Our initial characterization of the model revealed that the Slc39a14
-/-
mice showed altered Mn homeostasis and compromised locomotor performance in vertical pole-descending, horizontal beam-traversing, and rotarod tests (Jenkitkasemwong et al., 2018). However, some of the mice also displayed torticollis and Straub tail. In this study, we investigated whether these postural abnormalities affected the performance in the above motility tests and consequently, biased and compromised the external validity of reported abnormal locomotor profiles. Our analyses showed that the Slc39a14
-/-
mice displaying torticollis and/or Straub tail had tests scores comparable to scores of their counterparts that never displayed these postural abnormalities. The z-score general index of performance revealed that the Slc39a14
-/-
model presents a complex pathological motor phenotype relevant to the complexity of phenotypes identified in childhood-onset parkinsonism-
dystonia
.
...
PMID:Phenotypic evaluation of a childhood-onset parkinsonism-dystonia mouse model with inherent postural abnormalities. 3314 20
