Evaluation of Direct and Cell-Mediated Lactoferrin Gene Therapy for the Maxillofacial Area Abscesses in Rats

Agatieva, Elima; Ksembaev, Said; Sokolov, Mikhail; Markosyan, Vage; Газизов, И. М.; Цыплаков, Д. Э.; Шмаров, М. М.; Тутыхина, И. Л.; Naroditsky, Boris S.; Logunov, Denis Y.; Поздеев, О. К.; Morozova, L. G.; Yapparova, Kamilya; Islamov, R. R.

doi:10.3390/pharmaceutics13010058

Cited by 5 publications

(1 citation statement)

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“…In addition, this approach can be useful to obtain UCB-MCs with the therapeutic effects required for the treatment of human diseases based on the temporal synthesis and secretion of specific bioactive therapeutic molecules responsible for the correction of a particular pathological disorder. We have recently demonstrated the positive effect of UCB-MCs transduced with Ad5-LTF carrying the human lactoferrin gene on the recovery of maxillofacial phlegmon in rats [52] and the induction of angiogenesis by UCB-MCs transduced with Ad5-VEGF165 applied in an in vivo Matrigel plug assay [53]. However, the biosafety of UCB-MC transduction using an adenoviral vector and transgene overexpression on the native functional characteristics of UCB-MCs remains unclear.…”

Section: Introductionmentioning

confidence: 99%

A Biosafety Study of Human Umbilical Cord Blood Mononuclear Cells Transduced with Adenoviral Vector Carrying Human Vascular Endothelial Growth Factor cDNA In Vitro

et al. 2023

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The biosafety of gene therapy remains a crucial issue for both the direct and cell-mediated delivery of recombinant cDNA encoding biologically active molecules for the pathogenetic correction of congenital or acquired disorders. The diversity of vector systems and cell carriers for the delivery of therapeutic genes revealed the difficulty of developing and implementing a safe and effective drug containing artificial genetic material for the treatment of human diseases in practical medicine. Therefore, in this study we assessed changes in the transcriptome and secretome of umbilical cord blood mononuclear cells (UCB-MCs) genetically modified using adenoviral vector (Ad5) carrying cDNA encoding human vascular endothelial growth factor (VEGF165) or reporter green fluorescent protein (GFP). A preliminary analysis of UCB-MCs transduced with Ad5-VEGF165 and Ad5-GFP with MOI of 10 showed efficient transgene expression in gene-modified UCB-MCs at mRNA and protein levels. The whole transcriptome sequencing of native UCB-MCs, UCB-MC+Ad5-VEGF165, and UCB-MC+Ad5-GFP demonstrated individual sample variability rather than the effect of Ad5 or the expression of recombinant vegf165 on UCB-MC transcriptomes. A multiplex secretome analysis indicated that neither the transduction of UCB-MCs with Ad5-GFP nor with Ad5-VEGF165 affects the secretion of the studied cytokines, chemokines, and growth factors by gene-modified cells. Here, we show that UCB-MCs transduced with Ad5 carrying cDNA encoding human VEGF165 efficiently express transgenes and preserve transcriptome and secretome patterns. This data demonstrates the biosafety of using UCB-MCs as cell carriers of therapeutic genes.

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Section: Introductionmentioning

confidence: 99%