Semaphorin 3A is an endogenous angiogenesis inhibitor that blocks tumor growth and normalizes tumor vasculature in transgenic mouse models
Federica Maione, … , Federico Bussolino, Enrico Giraudo
Federica Maione, … , Federico Bussolino, Enrico Giraudo
Published October 5, 2009
Citation Information: J Clin Invest. 2009;119(11):3356-3372. https://doi.org/10.1172/JCI36308.
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Semaphorin 3A is an endogenous angiogenesis inhibitor that blocks tumor growth and normalizes tumor vasculature in transgenic mouse models

Abstract

Tumor growth and progression rely upon angiogenesis, which is regulated by pro- and antiangiogenic factors, including members of the semaphorin family. By analyzing 3 different mouse models of multistep carcinogenesis, we show here that during angiogenesis, semaphorin 3A (Sema3A) is expressed in ECs, where it serves as an endogenous inhibitor of angiogenesis that is present in premalignant lesions and lost during tumor progression. Pharmacologic inhibition of endogenous Sema3A during the angiogenic switch, the point when pretumoral lesions initiate an angiogenic phase that persists throughout tumor growth, enhanced angiogenesis and accelerated tumor progression. By contrast, when, during the later stages of carcinogenesis following endogenous Sema3A downmodulation, Sema3A was ectopically reintroduced into islet cell tumors by somatic gene transfer, successive waves of apoptosis ensued, first in ECs and then in tumor cells, resulting in reduced vascular density and branching and inhibition of tumor growth and substantially extended survival. Further, long-term reexpression of Sema3A markedly improved pericyte coverage of tumor blood vessels, something that is thought to be a key property of tumor vessel normalization, and restored tissue normoxia. We conclude, therefore, that Sema3A is an endogenous and effective antiangiogenic agent that stably normalizes the tumor vasculature.

Authors

Federica Maione, Fabiola Molla, Claudia Meda, Roberto Latini, Lorena Zentilin, Mauro Giacca, Giorgio Seano, Guido Serini, Federico Bussolino, Enrico Giraudo

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Figure 5

Sema3A induces apoptosis first in vascular ECs and then in tumor cells.

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Sema3A induces apoptosis first in vascular ECs and then in tumor cells. ...
(A) Compared with 14-week-old AAV8-LacZ controls, AAV8-Sema3A treatment of 12-week-old RipTag2 mice promoted apoptosis in ECs (arrows) and tumor cells (arrowheads) 2 (short trial) and 4 (long trial) weeks after AAV gene delivery, respectively. EC apoptotic rate was detected by colocalization of Meca-32 (green) with activated caspase-3 (red). Images are representative of 5 fields per mouse from a total of 10 mice per 2- and 4-week-long treatment. (B and C) Percentage of cleaved caspase-3+ cells on total cells in the short (B) and long (C) trial, compared with controls (**P < 0.001). (D) Upon Sema3A treatment, no apoptotic ECs were detected in blood vessels of normal pancreatic tissue in either short or long trial. (E) In long trials, anti-Ki67 immunostaining revealed no difference in proliferation rate in AAV8-Sema3A–treated compared with control animals. (F) Islet tumor hypoxia as detected by the formation of pimonidazole adducts (green). In short trials, Sema3A transiently enhanced tumor hypoxia compared with control, while in long trials, Sema3A-treated insulinomas were normoxic. Values are mean ± SD (n = 10 mice per 2- and 4 week-long treatment). Scale bars: 50 μm.