UMLS:C0029713 - FACTA Search

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Query: UMLS:C0029713 (immaturity)
4,335 document(s) hit in 31,850,051 MEDLINE articles (0.00 seconds)

Because of a lack in drug evaluation in children, they receive many off license drugs prescription, which means drugs prescribed in an indication, dosage, formulation or age different from the license terms. However, drug evaluation is crucial in paediatrics population because of pharmacokinetics and pharmacodynamics modifications throughout organism development, which make usually wrong any extrapolation to children of data obtained in adults. Drug safety is generally better in infants except in newborns who are at a particularly high drug-related risk because of high frequency of off license drug use, many drugs association and drugs metabolism immaturity. The lack of evaluation in children, the fact that children are the unique target population of some drugs or the maturation phenomena explain some adverse effects more specific in children. The more the children are young, the more they are exposed to medication or drug utilization errors. Physician must take what the SPC, as found in the Vidal dictionary, mentions about children into account while prescribing. Drugs with a paediatric license must be preferred overall, however it should be kept in mind that a paediatric license means only that the drug is active in the indication of the license but it doesn't position it regarding other therapeutic alternatives. Off labeling prescription should be based on a supposed benefit, which had to be justified if a severe side effect occurred.
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PMID:[Prescriptions and children]. 1634 69

Mature retinal ganglion cells (RGCs) have distinct morphologies that often reflect specialized functional properties such as On and Off responses. But the structural correlates of many complex receptive field (RF) properties (e.g. responses to motion) remain to be deciphered. In this study, we have investigated whether motion anisotropies (non-homogeneities) characteristic of embryonic turtle RGCs arise from immature dendritic arborization in these cells. To test this hypothesis, we have looked at structure-function correlates of developing turtle RGCs from Stage 23 (S23) when light responses emerge, until 15 weeks post-hatching (PH). Using whole cell patch clamp recordings, RGCs were labelled with Lucifer Yellow (LY) while recording their responses to moving edges of light. Comparison of RF and dendritic arbor layouts revealed a weak correlation. To obtain a larger structural sample of developing RGCs, we have looked at dendritic morphology in RGCs retrogradely filled with the tracer horseradish peroxidase (HRP) from S22 (when RGCs become spontaneously active, shortly before they become sensitive to light) until two weeks PH. We found that there was intense dendritic growth from S22 onwards, reaching peak proliferation at S25 (a week before hatching), while RGCs are still exhibiting significant motion anisotropies. Based on these observations, we suggest that immature anisotropic RGC RFs must originate from sparse synaptic inputs onto RGCs rather than from the immaturity of their growing dendritic trees.
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PMID:Receptive field structure-function correlates in developing turtle retinal ganglion cells. 1693 Apr 8