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Microenvironmental VEGF concentration, not total dose, determines a threshold between normal and aberrant angiogenesis
Clare R. Ozawa, … , Donald M. McDonald, Helen M. Blau
Clare R. Ozawa, … , Donald M. McDonald, Helen M. Blau
Published February 15, 2004
Citation Information: J Clin Invest. 2004;113(4):516-527. https://doi.org/10.1172/JCI18420.
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Article Cardiology

Microenvironmental VEGF concentration, not total dose, determines a threshold between normal and aberrant angiogenesis

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Abstract

Use of long-term constitutive expression of VEGF for therapeutic angiogenesis may be limited by the growth of abnormal blood vessels and hemangiomas. We investigated the relationship between VEGF dosage and the morphology and function of newly formed blood vessels by implanting retrovirally transduced myoblasts that constitutively express VEGF164 into muscles of adult mice. Reducing VEGF dosage by decreasing the total number of VEGF myoblasts implanted did not prevent vascular abnormalities. However, when clonal populations of myoblasts homogeneously expressing different levels of VEGF were implanted, a threshold between normal and aberrant angiogenesis was found. Clonal myoblasts that expressed low to medium levels of VEGF induced growth of stable, pericyte-coated capillaries of uniform size that were not leaky and became VEGF independent, as shown by treatment with the potent VEGF blocker VEGF-TrapR1R2. In contrast, clones that expressed high levels of VEGF induced hemangiomas. Remarkably, when different clonal populations were mixed, even a small proportion of cells with high production of VEGF was sufficient to cause hemangioma growth. These results show for the first time to our knowledge that the key determinant of whether VEGF-induced angiogenesis is normal or aberrant is the microenvironmental amount of growth factor secreted, rather than the overall dose. Long-term continuous delivery of VEGF, when maintained below a threshold microenvironmental level, can lead to normal angiogenesis without other exogenous growth factors.

Authors

Clare R. Ozawa, Andrea Banfi, Nicole L. Glazer, Gavin Thurston, Matthew L. Springer, Peggy E. Kraft, Donald M. McDonald, Helen M. Blau

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Figure 5

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Plasma leakage correlates with the total amount of VEGF produced and is ...
Plasma leakage correlates with the total amount of VEGF produced and is transient. (a) Evans blue extravasation at sites of implanted LacZ control, polyclonal VEGF (Poly. VEGF), and 10%, 100%, or 325% clone myoblasts at 4 days after implantation. ND, not detected. (b) Evans blue extravasation in ears implanted with LacZ control and 10% clone at 28 days after implantation. Leakage at this time point had returned to the baseline level. Values are mean ± SEM (n = 3–6 per group).

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