Literature DB >> 18071063

Time courses of growth and remodeling of porcine aortic media during hypertension: a quantitative immunohistochemical examination.

Jin-Jia Hu1, Andy Ambrus, Theresa W Fossum, Matthew W Miller, Jay D Humphrey, Emily Wilson.   

Abstract

Arteries undergo marked structural and functional changes in human and experimental hypertension that generally involve smooth muscle cell (SMC) hypertrophy/hyperplasia as well as abnormal extracellular matrix turnover. In this study we examined time courses of changes in SMC activity and matrix protein content in a novel mini-pig aortic coarctation model. Cell proliferation was evaluated by immunostaining of Ki-67, apoptosis was assessed by TUNEL, and phenotypic changes were monitored by immunostaining three SMC contractile markers (caldesmon, calponin, and smoothelin). Changes in medial collagen and elastin were examined by picrosirius red and Verhoeff-van Gieson staining, respectively. LabVIEW-based image analysis routines were developed to objectively and efficiently quantify the (immuno)histochemical results. We found that significant cell proliferation and matrix production occurred in the early stages of this coarctation model and then declined gradually; the SMCs also tended to exhibit a less contractile phenotype following these cellular and extracellular changes. Specifically, different aspects of the phenotypic changes associated with hypertension occurred at different rates: cell proliferation and collagen production occurred early and peaked by 2 weeks, whereas changes in contractile protein expression continued to decrease over the entire 8-week study period. Temporal changes found in this study emphasize the importance of simultaneously tracing time courses of SMC growth and differentiation as well as matrix protein production and content. SMCs are multifunctional, and caution must be used to not overdefine phenotype. This manuscript contains online supplemental material at http://www.jhc.org. Please visit this article online to view these materials.

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Year:  2007        PMID: 18071063      PMCID: PMC2326104          DOI: 10.1369/jhc.7A7324.2007

Source DB:  PubMed          Journal:  J Histochem Cytochem        ISSN: 0022-1554            Impact factor:   2.479


  49 in total

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5.  Automated selection of DAB-labeled tissue for immunohistochemical quantification.

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6.  Differential transmural distribution of gene expression for collagen types I and III proximal to aortic coarctation in the rabbit.

Authors:  C Xu; C K Zarins; H S Bassiouny; W H Briggs; C Reardon; S Glagov
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Review 8.  Molecular regulation of vascular smooth muscle cell differentiation in development and disease.

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9.  A novel aortic coarctation model for studying hypertension in the pig.

Authors:  Theresa W Fossum; Wendy I Baltzer; Matthew W Miller; Maria Aguirre; Debbi Whitlock; Phil Solter; Lori A Makarski; Michelle M McDonald; Mi-Young An; Jay D Humphrey
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10.  Quantitative structural changes of the rat thoracic aorta in early spontaneous hypertension. Tissue composition, and hypertrophy and hyperplasia of smooth muscle cells.

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Review 8.  Elastin and collagen fibre microstructure of the human aorta in ageing and disease: a review.

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9.  Alterations in Pulse Pressure Affect Artery Function.

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