Publication:
Morphogenetic Variability as Potential Biomarker of Neurogenic Lesion Degree in Children with Spina Bifida.

dc.contributor.authorPetronic, Ivana
dc.contributor.authorMarinkovic, Dragoslav
dc.contributor.authorNikolic, Dejan
dc.contributor.authorCirovic, Dragana
dc.contributor.authorGolubovic, Zoran
dc.contributor.authorMilanovic, Filip
dc.contributor.authorCvjeticanin, Suzana
dc.date.accessioned2025-04-15T10:06:24Z
dc.date.available2025-04-15T10:06:24Z
dc.date.issued2020-03-24
dc.description.abstractIn this study we analyzed the degree of genetic homozygosity among spina bifida patients with different degrees of neurogenic lesion ( = 82), as well as their clinical and neurological characteristics, compared to healthy control individuals ( = 100).
dc.description.abstractAccording to clinical and electromyographic findings, we separately assessed the type of neurogenic lesion (paresis or paralysis). Regarding the degree of neurogenic lesion, patients were classified into three groups: mild, moderate and severe. We analyzed six muscles. For assessing the degree of individual genetic homozygosity, we tested the presence and distribution of 15 homozygous recessive characteristics (HRC).
dc.description.abstractThe predominant type of neurogenic lesion was paresis. Every third evaluated muscle was affected in the group with mild neurogenic lesion, while more than half were affected in the group with severe neurogenic lesion. The average values of HRCs among different groups of patients and the control showed the population-genetic differences that exist among them (control =3.0±0.2; mild =3.6±0.2; moderate =4.8±0.3; severe neurogenic lesion =5.0±0.3).
dc.description.abstractSpina bifida patients have a significant increase of recessive homozygosity and a decreased variability compared to the control group. As neurogenic lesions are more severe, more affected muscles are present, as well as the increase of individual recessive homozygosity.
dc.identifier.doi10.3390/healthcare8010068
dc.identifier.pmid32214024
dc.identifier.urihttps://remedy.med.bg.ac.rs/handle/123456789/79
dc.language.isoen
dc.relation.ispartofHealthcare (Basel, Switzerland)
dc.relation.issn2227-9032
dc.subjectgenetic homozygosity
dc.subjectgenetic variability
dc.subjectneurogenic lesion
dc.subjectspina bifida
dc.titleMorphogenetic Variability as Potential Biomarker of Neurogenic Lesion Degree in Children with Spina Bifida.
dc.typetext::journal::journal article
dspace.entity.typePublication
oaire.citation.issue1
oaire.citation.volume8

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