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NO mediates mural cell recruitment and vessel morphogenesis in murine melanomas and tissue-engineered blood vessels
Satoshi Kashiwagi, Yotaro Izumi, Takeshi Gohongi, Zoe N. Demou, Lei Xu, Paul L. Huang, Donald G. Buerk, Lance L. Munn, Rakesh K. Jain, Dai Fukumura
Satoshi Kashiwagi, Yotaro Izumi, Takeshi Gohongi, Zoe N. Demou, Lei Xu, Paul L. Huang, Donald G. Buerk, Lance L. Munn, Rakesh K. Jain, Dai Fukumura
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Research Article Angiogenesis

NO mediates mural cell recruitment and vessel morphogenesis in murine melanomas and tissue-engineered blood vessels

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Abstract

NO has been shown to mediate angiogenesis; however, its role in vessel morphogenesis and maturation is not known. Using intravital microscopy, histological analysis, α–smooth muscle actin and chondroitin sulfate proteoglycan 4 staining, microsensor NO measurements, and an NO synthase (NOS) inhibitor, we found that NO mediates mural cell coverage as well as vessel branching and longitudinal extension but not the circumferential growth of blood vessels in B16 murine melanomas. NO-sensitive fluorescent probe 4,5-diaminofluorescein imaging, NOS immunostaining, and the use of NOS-deficient mice revealed that eNOS in vascular endothelial cells is the predominant source of NO and induces these effects. To further dissect the role of NO in mural cell recruitment and vascular morphogenesis, we performed a series of independent analyses. Transwell and under-agarose migration assays demonstrated that endothelial cell–derived NO induces directional migration of mural cell precursors toward endothelial cells. An in vivo tissue-engineered blood vessel model revealed that NO mediates endothelial–mural cell interaction prior to vessel perfusion and also induces recruitment of mural cells to angiogenic vessels, vessel branching, and longitudinal extension and subsequent stabilization of the vessels. These data indicate that endothelial cell–derived NO induces mural cell recruitment as well as subsequent morphogenesis and stabilization of angiogenic vessels.

Authors

Satoshi Kashiwagi, Yotaro Izumi, Takeshi Gohongi, Zoe N. Demou, Lei Xu, Paul L. Huang, Donald G. Buerk, Lance L. Munn, Rakesh K. Jain, Dai Fukumura

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Figure 10

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Endothelial–mural cell interaction and vessel density in the tissue-engi...
Endothelial–mural cell interaction and vessel density in the tissue-engineered blood vessels. (A) Temporal changes in the mural cell coverage of endothelial cells. All vessels including both perfused (right) and nonperfused (left) were analyzed. (B) Temporal changes in total (left) and perfused (right) tissue-engineered vessel density. *P < 0.05, compared with corresponding controls; Mann–Whitney U test. Four locations of each tissue-engineered vessel model were observed. Six animals each for the HUVECs-10T1/2 cells co-implantation models, and 3 animals each for implantation with HUVEC alone were examined.

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ISSN: 0021-9738 (print), 1558-8238 (online)

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