Neovascularization and Angiogenic Gene Expression Following Chronic Arsenic Exposure in Mice

Soucy, Nicole V.; Mayka, Debra; Klei, Linda R.; Nemec, Antonia A.; Bauer, John; Barchowsky, Aaron

doi:10.1385/ct:5:1:029

Cited by 68 publications

(64 citation statements)

References 45 publications

Supporting

Mentioning

Contrasting

Order By: Relevance

“…The purpose of the current studies was to demonstrate that exposing mice to drinking water containing environmentally relevant levels of arsenic promoted endothelial cell dysfunction and pathologic vascular remodeling. Increased angiogenesis, neovascularization, and inflammatory cell infiltration was observed in Matrigel plugs implanted in C57BL/6 mice following 5 week exposures to 5-500 ppb arsenic (Soucy et al, 2005). Therefore, functional in vivo effects of arsenic on endothelial cell function and vessel remodeling in an endogenous vascular bed were investigated in the liver.…”

Section: Introductionmentioning

confidence: 99%

“…This limitation is confounded by the current bias that intact rodent models are insensitive to the health effects of arsenic. The vascular effects of arsenic are an exception since vascular activation and dysfunction occur in mice exposed to low ppb levels of arsenic (Kamat et al, 2005;Liu et al, 2006;Soucy et al, 2003;Soucy et al, 2005). The importance of identifying in vivo endpoints that can be used to test for the vascular effects of low to moderate arsenic exposures is underscored by the multiple dose-dependent mechanisms elicited by arsenic exposures.…”

Section: Introductionmentioning

confidence: 99%

“…Thus endothelial cells generate the angiogenic response, but they cannot complete vessel maturation without recruitment of pericytes and smooth muscle cells in a process called vascular myogenesis (Ricousse-Roussanne et al, 2004;Carmeliet, 2000). Pathogenic endothelial cell activation and angiogenesis in rodent models are sensitive to low, environmentally relevant arsenic exposures (Soucy et al, 2003;Soucy et al, 2005;Kamat et al, 2005). Arsenic stimulates the angiogenic process in cultured cells and neovascularization in vivo (Barchowsky et al, 1996;Kao et al, 2003;Kamat et al, 2005;Liu et al, 2006;Soucy et al, 2003;Soucy et al, 2005).…”

Section: Introductionmentioning

confidence: 99%

“…Pathogenic endothelial cell activation and angiogenesis in rodent models are sensitive to low, environmentally relevant arsenic exposures (Soucy et al, 2003;Soucy et al, 2005;Kamat et al, 2005). Arsenic stimulates the angiogenic process in cultured cells and neovascularization in vivo (Barchowsky et al, 1996;Kao et al, 2003;Kamat et al, 2005;Liu et al, 2006;Soucy et al, 2003;Soucy et al, 2005). However, this stimulation occurs only at low to moderate concentrations of arsenic (5-500 ppb in vivo, 0.1-5.0 μM in cell culture; (Barchowsky et al, 1996;Kao et al, 2003;Soucy et al, 2003;Soucy et al, 2005)).…”

Section: Introductionmentioning

confidence: 99%

“…Arsenic stimulates the angiogenic process in cultured cells and neovascularization in vivo (Barchowsky et al, 1996;Kao et al, 2003;Kamat et al, 2005;Liu et al, 2006;Soucy et al, 2003;Soucy et al, 2005). However, this stimulation occurs only at low to moderate concentrations of arsenic (5-500 ppb in vivo, 0.1-5.0 μM in cell culture; (Barchowsky et al, 1996;Kao et al, 2003;Soucy et al, 2003;Soucy et al, 2005)). Concentrations of arsenic above 5 μM are toxic to confluent endothelial cells and limit tube formation in culture (Barchowsky et al, 1996;Roboz et al, 2000).…”

Section: Introductionmentioning

confidence: 99%

See 4 more Smart Citations

Low level arsenic promotes progressive inflammatory angiogenesis and liver blood vessel remodeling in mice

Straub

Stolz

Vin

et al. 2007

Toxicology and Applied Pharmacology

Self Cite

View full text Add to dashboard Cite

The vascular effects of arsenic in drinking water are global health concerns contributing to human disease worldwide. Arsenic targets the endothelial cells lining blood vessels and endothelial cell activation or dysfunction may underlie the pathogenesis of both arsenic-induced vascular diseases and arsenic-enhanced tumorigenesis. The purpose of the current studies was to demonstrate that exposing mice to drinking water containing environmentally relevant levels of arsenic promoted endothelial cell dysfunction and pathologic vascular remodeling. Increased angiogenesis, neovascularization, and inflammatory cell infiltration was observed in Matrigel plugs implanted in C57BL/6 mice following 5 week exposures to 5-500 ppb arsenic (Soucy et al., 2005). Therefore, functional in vivo effects of arsenic on endothelial cell function and vessel remodeling in an endogenous vascular bed were investigated in the liver. Liver sinusoidal endothelial cells (LSEC) became progressively defenestrated and underwent capillarization to decrease vessel porosity following exposure to 250 ppb arsenic for 2 weeks. Sinusoidal expression of PECAM-1 and laminin-1 proteins, a hallmark of capillarization, was also increased by 2 weeks of exposure. LSEC caveolin-1 protein and caveolae expression were induced after 2 weeks of exposure indicating a compensatory change. Likewise, CD45/CD68 positive inflammatory cells did not accumulate in the livers until after LSEC porosity was decreased; indicating that inflammation is a consequence and not a cause of the arsenic-induced LSEC phenotype. The data demonstrate that the liver vasculature is an early target of pathogenic arsenic effects and that the mouse liver vasculature is a sensitive model for investigating vascular health effects of arsenic.

show abstract

Section: Introductionmentioning

confidence: 99%