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: UMLS:C0917816 (
mental retardation
)
15,867
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
We report on the molecular characterization of a translocation t(1;19)(q21.3;q13.2) in a female with
mental retardation
, ataxia and atrophy of the brain. Sequence analysis of the breakpoints revealed an ALU:-repeat-mediated mechanism of recombination that led to truncation of two genes: the kinase CLK2 and
PAFAH1B3
, the gene product of which interacts with LIS1 as part of a heterotrimeric G protein complex PAF-AH1B. In addition, two reciprocal fusion genes are present. One expressed fusion gene encodes the first 136 amino acids of
PAFAH1B3
followed by the complete CLK2 protein. Truncated PAFAH1B3 protein lost its potential to interact with LIS1 whereas CLK2 activity was conserved within the fusion protein. These data emphasize the importance of PAF-AH1B in brain development and functioning and demonstrate the first fusion gene apparently not associated with cancer.
...
PMID:Functional hemizygosity of PAFAH1B3 due to a PAFAH1B3-CLK2 fusion gene in a female with mental retardation, ataxia and atrophy of the brain. 1128 45
The engrailed homeobox protein (EN) plays an important role in the regionalization of the neural tube. EN distribution regulates the cerebellum and midbrain morphogenesis, as well as retinotectal synaptogenesis. In humans, the
EN1
and
EN2
genes code for the EN family of transcription factors. Genetic alterations in the expression of
EN2
have been related to different neurologic conditions and more particularly to autism spectrum disorders (ASD). We aimed to study and compare the phenotypes of three series of patients: (1) patients with encephalic structural anomalies (ESA) and abnormalities in the genomic (DNA) and/or transcriptomic (RNAm) of
EN2
(EN2-g), (2) ESA patients having other gene mutations (OG-g), and (3) ESA patients free of these mutations (NM-g).
Subjects and Methods:
We have performed a descriptive study on 109 patients who suffer from
mental retardation
(MR), cerebral palsy (CP), epilepsy (EP), and behavioral disorders (BD), showing also ESA in their encephalic MRI. We studied genomic DNA and transcriptional analysis (cDNA) on
EN2
gene (EN2), and in other genes (OG):
LIS1, PTAFR, PAFAH1B2,
PAFAH1B3
, FGF8, PAX2, D17S379, D17S1866
, and
SMG6 (D17S5)
, as a routine genetic diagnosis in ESA patients.
Results:
From 109 patients, fifteen meet the exclusion criteria. From the remaining 94 patients, 12 (12.8%) showed mutations in
EN2
(EN2-g), 20 showed mutations in other studied genes (OG-g), and 62 did not showed any mutation (NM-g). All EN2-g patients, suffered from MR, nine EP, seven BD and four CP. The proportions of these phenotypes in EN2-g did not differ from those in the OG-g, but it was significantly higher when comparing EN2-g with NM-g (MR:
p
= 0.013; EP:
p
= 0.001; BD:
p
= 0.0001; CP:
p
= 0.07, ns). Groups EN2-g and OG-g showed a 100 and a 70% of comorbidity, respectively, being significantly (
p
= 0.04) greater than NM-group (62.9%).
Conclusion:
Our series reflects a significant effect of
EN2
gene alterations in neurodevelopmental abnormalities associated to ESA. Conversely, although these
EN2
related anomalies might represent a predisposition to develop brain diseases, our results did not support direct relationship between
EN2
mutations and specific clinical phenotypes.
...
PMID:Clinical Phenotypes Associated to Engrailed 2 Gene Alterations in a Series of Neuropediatric Patients. 3014 46
