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Hypoxic regulation of ADAMTS-2 and -3 (a disintegrin and matrix metalloproteinase with thrombospondin motifs 2 and 3) procollagen N proteinases by HIF-1α in endothelial cells. | LitMetric

AI Article Synopsis

  • ADAMTS-2 and ADAMTS-3 are enzymes that process collagen precursors, with ADAMTS-2 found in type I collagen-rich tissues and ADAMTS-3 mainly in cartilage and the nervous system.
  • Recent research shows that hypoxia (low oxygen conditions) significantly boosts the expression of both ADAMTS-2 and ADAMTS-3 at the mRNA and protein levels in HUVECs (human umbilical vein endothelial cells).
  • The study found that the hypoxia-inducible factor HIF-1α binds to specific regions in the promoters of these genes, indicating that low oxygen levels enhance their transcriptional activity.

Article Abstract

ADAMTS-2 and ADAMTS-3, known as procollagen amino proteases (PNP), are primarily responsible for processing the amino ends of the fibrillar collagen precursors. ADAMTS-2 is a highly expressed gene in type I collagen-rich tissues, such as skin, bones, tendons, and aorta. ADAMTS-3 is mainly expressed in cartilage, where it colocalizes with type II procollagen and in the nervous system. Studies about ADAMTS-2 and ADAMTS-3 enzymes primarily focused on their collagen processing activity. Knowledge about the transcriptional regulations of these genes is rather limited. Here we analyzed the transcriptional regulations of ADAMTS-2 and ADAMTS-3 genes under chemically induced hypoxic conditions in endothelial cell model, HUVECs. We elucidated that hypoxia is the potent positive regulator of ADAMTS-2 and ADAMTS-3 genes. qRT-PCR and western blotting studies revealed that ADAMTS-2 and ADAMTS-3 expressions were increased at mRNA and protein levels under chemically induced hypoxic conditions in HUVECs. In addition, Transient transfection experiments of ADAMTS-2 and ADAMTS-3 promoter-reporter constructs indicated that low oxygen conditions increased ADAMTS-2 and ADAMTS-3 promoter activities. Furthermore, the DNA-protein interaction assay provided evidence of the functional binding of HIF-1α on bioinformatically determined HRE regions on the ADAMTS-2 and ADAMTS-3 promoters.

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Source
http://dx.doi.org/10.1007/s11010-022-04549-3DOI Listing

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