Molecular Background of Toxic-Substances-Induced Morphological Alterations in the Umbilical Cord Vessels and Fetal Red Blood Cells.
Szabolcs ZahoránÁgnes MártonKrisztina DugmonitsPayal ChakrabortyAli KhamitPéter HegyiHajnalka OrvosEdit HermeszPublished in: International journal of molecular sciences (2022)
The relationship between smoking and human health has been investigated mostly in adults, despite the fact that the chemicals originating from sustained maternal smoking disrupt the carefully orchestrated regulatory cascades in the developing fetus. In this study, we followed molecular alterations in the umbilical cord (UC) vessels and fetal red blood cells (RBCs), which faithfully reflect the in vivo status of the fetus. We showed evidence for the decreased level of DNA-PKcs-positive nuclei in samples with smoking origin, which is associated with the impaired DNA repair system. Furthermore, we pointed out the altered ratio of MMP-9 metalloproteinase and its endogenous inhibitor TIMP-1, which might be a possible explanation for the morphological abnormalities in the UC vessels. The presented in vivo dataset emphasizes the higher vulnerability of the veins, as the primary target for the toxic materials unfiltered by the placenta. All these events become amplified by the functionally impaired fetal RBC population via a crosstalk mechanism between the vessel endothelium and the circulating RBCs. In our ex vivo approach, we looked for the molecular explanation of metal-exposure-induced alterations, where expressions of the selected genes were upregulated in the control group, while samples with smoking origin showed a lack of response, indicative of prior long-term in utero exposure.
Keyphrases
- red blood cell
- umbilical cord
- mesenchymal stem cells
- dna repair
- smoking cessation
- human health
- risk assessment
- high glucose
- climate change
- diabetic rats
- dna damage
- nitric oxide
- drug induced
- bone marrow
- dna damage response
- circulating tumor
- dna methylation
- gene expression
- pregnancy outcomes
- transcription factor
- pulmonary embolism
- high resolution
- physical activity
- cell migration
- nucleic acid
- bioinformatics analysis
- stress induced
- gestational age