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Disease
Symptom
Drug
Enzyme
Compound
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Target Concepts:
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Query: UMLS:C0013421 (
dystonia
)
8,418
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Phenylketonuria (PKU, phenylalanine hydroxylase deficiency), an inborn error of metabolism, can be detected through newborn screening for hyperphenylalaninemia (HPA). Most individuals with HPA harbor mutations in the gene encoding phenylalanine hydroxylase (PAH), and a small proportion (2%) exhibit tetrahydrobiopterin (BH
4
) deficiency with additional neurotransmitter (dopamine and serotonin) deficiency. Here we report six individuals from four unrelated families with HPA who exhibited progressive neurodevelopmental delay,
dystonia
, and a unique profile of neurotransmitter deficiencies without mutations in PAH or BH
4
metabolism disorder-related genes. In these six affected individuals, whole-exome sequencing (WES) identified biallelic mutations in
DNAJC12
, which encodes a heat shock co-chaperone family member that interacts with phenylalanine, tyrosine, and tryptophan hydroxylases catalyzing the BH
4
-activated conversion of phenylalanine into tyrosine, tyrosine into L-dopa (the precursor of dopamine), and tryptophan into 5-hydroxytryptophan (the precursor of serotonin), respectively.
DNAJC12
was undetectable in fibroblasts from the individuals with null mutations. PAH enzyme activity was reduced in the presence of
DNAJC12
mutations. Early treatment with BH
4
and/or neurotransmitter precursors had dramatic beneficial effects and resulted in the prevention of neurodevelopmental delay in the one individual treated before symptom onset. Thus,
DNAJC12
deficiency is a preventable and treatable cause of intellectual disability that should be considered in the early differential diagnosis when screening results are positive for HPA. Sequencing of
DNAJC12
may resolve any uncertainty and should be considered in all children with unresolved HPA.
...
PMID:Biallelic Mutations in DNAJC12 Cause Hyperphenylalaninemia, Dystonia, and Intellectual Disability. 2813 89
Biallelic
DNAJC12
mutations were described in children with hyperphenylalaninemia, neurodevelopmental delay, and
dystonia
. We identified
DNAJC12
homozygous null variants (c.187A>T;p.K63* and c.79-2A>G;p.V27Wfs*14) in two kindreds with early-onset parkinsonism. Both probands had mild intellectual disability, mild nonprogressive, motor symptoms, sustained benefit from small dose of levodopa, and substantial worsening of symptoms after levodopa discontinuation. Neuropathology (Proband-A) revealed no alpha-synuclein pathology, and substantia nigra depigmentation with moderate cell loss.
DNAJC12
transcripts were reduced in both patients. Our results suggest that
DNAJC12
mutations (absent in 500 early-onset patients with Parkinson's disease) rarely cause dopa-responsive nonprogressive parkinsonism in adulthood, but broaden the clinical spectrum of
DNAJC12
deficiency. Ann Neurol 2017;82:640-646.
...
PMID:DNAJC12 and dopa-responsive nonprogressive parkinsonism. 2889 70
Patients with hyperphenylalaninemia (HPA) are detected through newborn screening for phenylketonuria (PKU). HPA is known to be caused by deficiencies of the enzyme phenylalanine hydroxylase (PAH) or its cofactor tetrahydrobiopterin (BH
4
). Current guidelines for the differential diagnosis of HPA would, however, miss a recently described
DNAJC12
deficiency. The co-chaperone
DNAJC12
is, together with the 70kDa heat shock protein (HSP70), responsible for the proper folding of PAH. All
DNAJC12
-deficient patients investigated to date responded to a challenge with BH
4
by lowering their blood phenylalanine levels. In addition, the patients presented with low levels of biogenic amine in CSF and responded to supplementation with BH
4
, L-dopa/carbidopa and 5-hydroxytryptophan. The phenotypic spectrum ranged from mild autistic features or hyperactivity to severe intellectual disability,
dystonia
and parkinsonism. Late diagnosis result in permanent neurological disability, while early diagnosed and treated patients develop normally. Molecular diagnostics for
DNAJC12
variants are thus mandatory in all patients in which deficiencies of PAH and BH
4
are genetically excluded.
...
PMID:DNAJC12 deficiency: A new strategy in the diagnosis of hyperphenylalaninemias. 2917 66
Recently, mutations of
DNAJC12
gene were reported to be associated with early-onset parkinsonism, progressive neurodevelopmental delay, and
dystonia
in several unrelated pedigrees. This study aimed to evaluate
DNAJC12
coding mutations in sporadic Chinese Han patients with Parkinson's disease (PD) and test whether an age-of-onset effect exists. Seven hundred two Chinese Han sporadic PD patients, including 181 early-onset PD and 521 late-onset PD, and 728 healthy controls were recruited. No documented disease-causing mutation of
DNAJC12
was identified, but we found 7 single-nucleotide polymorphisms. Allele frequencies did not differ between all the PD patients and controls or between any 2 subgroups for all these single-nucleotide polymorphisms. Our study suggests that
DNAJC12
mutation is not a risk factor of PD in Chinese Han population, and no age-of-onset effect was verified.
...
PMID:DNAJC12 mutation is rare in Chinese Han population with Parkinson's disease. 2980 56
Hyperphenylalaninemia, movement disorder, and intellectual disability due to variants in
DNAJC12
is a recently reported inherited neurotransmitter disorder. We report two new patients with this new genetic disorder. Patient 1 is a 6-year-11-month-old boy with mild hyperphenylalaninemia and global developmental delay (GDD). Seventeen-year-old male sibling of patient 1 had GDD from the first year of life. He had mild hyperphenylalaninemia at 11.5 years of age following his younger brother's diagnosis. He had low levels of homovanillic acid and 5-hydroxyindolacetic acid in the cerebrospinal fluid. Whole-exome sequencing (WES) was normal in 2016. After the first description of
DNAJC12
-associated hyperphenylalaninemia,
dystonia
, and intellectual disability in 2017, WES re-analysis identified a homozygous c.58_59delGG (p.(Gly20Metfs*2)) variant in
DNAJC12
. His younger brother was homozygous for the same variant, confirming the diagnosis of
DNAJC12
-associated hyperphenylalaninemia, movement disorder, and intellectual disability. Mild hyperphenylalaninemia and GDD should warrant targeted
DNAJC12
genetic testing for the early diagnosis of
DNAJC12
-associated hyperphenylalaninemia, movement disorder, and intellectual disability.
...
PMID:DNAJC12-associated developmental delay, movement disorder, and mild hyperphenylalaninemia identified by whole-exome sequencing re-analysis. 3013 87
