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:C0085584 (
encephalopathy
)
18,178
document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)
Contamination of parenteral nutrition solutions with aluminum may result in accumulation of this element in bones and, in premature infants, may inhibit bone calcium uptake and induce cholestasis. We measured the aluminum concentration of small-volume parenterals, amino acid solutions, lipid emulsions, and special solutions containing glucose, amino acids, electrolytes, and trace elements (standard I for children with a body weight of 3-5 kg, standard II for children with a body weight of 5-10 kg). The method used was graphite furnace atomic absorption spectrometry
GTA
-AAS (SpectrAA-400 Plus, Varian, PtY Ltd., Mulgrave, Australia). Quality control was run with the use of control serum (Seronorm, Nycomed, Oslo, Norway). The aluminum contents of parenterally administered solutions were: pediatric trace elements, 130 micrograms/L, and pediatric trace elements, 3000 micrograms/L; phosphorus salts: K-phosphates, 9800 micrograms/L, and Na/K phosphates, 13,000 micrograms/L; 10% calcium gluconate, 4400 micrograms/L; 6.5% amino acids, 30 micrograms/L; 10% amino acids, 120 micrograms/L; 12.5% amino acids, 121 micrograms/L; 20% lipid emulsion, 30 micrograms/L; 20% lipid emulsion, 180 micrograms/L; water-soluble vitamins, 12 micrograms/L; lipid soluble vitamins, 360 micrograms/L; standard I, 55 micrograms/L; standard II, 90 micrograms/L; The aluminum intake from parenteral nutrition was 6.6-10.8 micrograms.kg-1.d-1--a dose exceeding the safety limit of 2 micrograms.kg-1.d-1. The possible association of aluminum not only with metabolic bone disease, but also with
encephalopathy
, dictates caution when dealing with the pediatric population on long-term parenteral nutrition. In the absence of reliable label information, it seems proper to monitor the aluminum concentration in parenteral nutrition products and to report it in professional journals.
...
PMID:Aluminum contamination of parenteral nutrition additives, amino acid solutions, and lipid emulsions. 1046 17
Mutations within
STXBP1
have been associated with a range of neurodevelopmental disorders implicating the pleotropic impact of this gene. Although the frequency of
de novo
mutations within
STXBP1
for selective cohorts with early onset epileptic
encephalopathy
is more than 1%, there is no evidence for a hotspot within the gene. In this study, we analyzed the genomic context of
de novo STXBP1
mutations to examine whether certain motifs indicated a greater risk of mutation. Through a comprehensive context analysis of 136
de novo
/rare mutation (SNV/Indels) sites in this gene, strikingly 26.92% of all SNV mutations occurred within 5bp upstream or downstream of a '
GTA
' motif (
P
< 0.0005). This implies a genomic context modulated mutagenesis. Moreover, 51.85% (14 out of 27) of the '
GTA
' mutations are splicing compared to 14.70% (20 out of 136) of all reported mutations within
STXBP1
We also noted that 11 of these 14 '
GTA
' associated mutations are
de novo
in origin. Our analysis provides strong evidence of DNA motif modulated mutagenesis for
STXBP1 de novo
splicing mutations.
...
PMID:Genomic Context Analysis of
de Novo STXBP1
Mutations Identifies Evidence of Splice Site DNA-Motif Associated Hotspots. 2943 95
