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H19, a developmentally regulated gene, is reexpressed in rat vascular smooth muscle cells after injury.
D K Kim, … , V J Dzau, R E Pratt
D K Kim, … , V J Dzau, R E Pratt
Published January 1, 1994
Citation Information: J Clin Invest. 1994;93(1):355-360. https://doi.org/10.1172/JCI116967.
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Research Article

H19, a developmentally regulated gene, is reexpressed in rat vascular smooth muscle cells after injury.

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Abstract

Vascular smooth muscle cell migration, proliferation, and differentiation are central to blood vessel development. Since neointimal formation after vascular injury may require the reexpression of a smooth muscle developmental sequence, we examined the expression of H19, a developmentally regulated gene, in rat blood vessels. Expression of the H19 gene is associated with the differentiation process that takes place during development of many tissues. Consistent with this, H19 was highly expressed in the 1-d-old rat aorta but was undetectable in the adult. H19 transcripts were only minimally detected in uninjured carotid artery but were abundant at 7 and 14 d after injury and were localized by in situ hybridization, primarily to the neointima. H19 transcript were undetectable in proliferating neointimal cells in culture but became highly abundant in postconfluent, differentiated neointimal cells. H19 transcripts were only minimally expressed in adult medial smooth muscle cells grown under the identical conditions. Thus, H19 may play an important role in the normal development and differentiation of the blood vessel and in the phenotypic changes of the smooth muscle cells, which are associated with neointimal lesion formation. The vascular injury model may be a useful system to use in examining the function of H19.

Authors

D K Kim, L Zhang, V J Dzau, R E Pratt

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