AI Article Synopsis
- Shb is an adapter protein linked to VEGFR-2, playing a crucial role in endothelial cell function and vascular health.
- Shb knockout mice showed reduced tumor growth and angiogenesis, along with notable structural changes in endothelial cells.
- The study suggests that targeting Shb signaling could offer new strategies for controlling tumor-related blood vessel formation.
Article Abstract
Shb (Src homology 2 protein B) is an adapter protein downstream of the vascular endothelial growth factor receptor receptor-2 (VEGFR-2). Previous experiments have suggested a role for Shb in endothelial cell function. Recently, the Shb gene was inactivated and Shb null mice were obtained on a mixed genetic background, but not on C57Bl6 mice. The present study was performed to address endothelial function in the Shb knockout mouse and its relevance for tumor angiogenesis. Tumor growth was retarded in Shb mutant mice, and this correlated with decreased angiogenesis both in tumors and in Matrigel plugs. Shb null mice display an abnormal endothelial ultrastructure in liver sinusoids and heart capillaries with cytoplasmic extensions projecting toward the lumen. Shb null heart VE-cadherin staining was less distinct than that of control heart, exhibiting in the former case a wavy and punctuate pattern. Experiments on isolated endothelial cells suggest that these changes could partly reflect cytoskeletal abnormalities. Vascular permeability was increased in Shb null mice in heart, kidney, and skin, whereas VEGF-stimulated vascular permeability was reduced in Shb null mice. It is concluded that Shb plays an important role in maintaining a functional vasculature in adult mice, and that interference with Shb signaling may provide novel means to regulate tumor angiogenesis.
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| http://dx.doi.org/10.1158/0008-5472.CAN-08-3797 | DOI Listing |
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Article Synopsis
- Shb is an adapter protein linked to VEGFR-2, playing a crucial role in endothelial cell function and vascular health.
- Shb knockout mice showed reduced tumor growth and angiogenesis, along with notable structural changes in endothelial cells.
- The study suggests that targeting Shb signaling could offer new strategies for controlling tumor-related blood vessel formation.
Shb null allele is inherited with a transmission ratio distortion and causes reduced viability in utero.
Dev Dyn
September 2007
Department of Medical Cell Biology, Uppsala University, Uppsala, Sweden.
SHB is an Src homology 2 domain-containing adapter protein that has been found to be involved in numerous cellular responses. We have generated an Shb knockout mouse. No Shb-/- pups or embryos were obtained on the C57Bl6 background, indicating an early defect as a consequence of Shb- gene inactivation on this genetic background.
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