Abstract

The sequence of events that leads to tumor vessel regression and the functional characteristics of these vessels during hormone–ablation therapy are not known. This is because of the lack of an appropriate animal model and monitoring technology. By using in vivo microscopy and in situ molecular analysis of the androgen-dependent Shionogi carcinoma grown in severe combined immunodeficient mice, we show that castration of these mice leads to tumor regression and a concomitant decrease in vascular endothelial growth factor (VEGF) expression. Androgen withdrawal is known to induce apoptosis in Shionogi tumor cells. Surprisingly, tumor endothelial cells begin to undergo apoptosis before neoplastic cells, and rarefaction of tumor vessels precedes the decrease in tumor size. The regressing vessels begin to exhibit normal phenotype, i.e., lower diameter, tortuosity, vascular permeability, and leukocyte adhesion. Two weeks after castration, a second wave of angiogenesis and tumor growth begins with a concomitant increase in VEGF expression. Because human tumors often relapse following hormone–ablation therapy, our data suggest that these patients may benefit from combined anti-VEGF therapy.

Keywords

AngiogenesisAndrogenVascular permeabilityVascular endothelial growth factorEndocrinologyInternal medicineGrowth factorBiologyEndothelial stem cellVascular endothelial growth factor ANeovascularizationCancer researchMedicineHormoneReceptorIn vitro

MeSH Terms

AndrogensAnimalsBlottingNorthernCastrationCell DeathEndothelial Growth FactorsEndotheliumVascularHumansLymphokinesMaleMiceMiceSCIDNeoplasmsHormone-DependentNeovascularizationPathologicRNAMessengerVascular Endothelial Growth Factor AVascular Endothelial Growth Factors

Affiliated Institutions

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Publication Info

Year
1998
Type
article
Volume
95
Issue
18
Pages
10820-10825
Citations
376
Access
Closed

Citation Metrics

376
OpenAlex
5
Influential

Cite This

Rakesh K. Jain, Nina Safabakhsh, Axel Sckell et al. (1998). Endothelial cell death, angiogenesis, and microvascular function after castration in an androgen-dependent tumor: Role of vascular endothelial growth factor. Proceedings of the National Academy of Sciences , 95 (18) , 10820-10825. https://doi.org/10.1073/pnas.95.18.10820

Identifiers

DOI
10.1073/pnas.95.18.10820
PMID
9724788
PMCID
PMC27979

Data Quality

Data completeness: 86%