Abstract

Leakiness of blood vessels in tumors may contribute to disease progression and is key to certain forms of cancer therapy, but the structural basis of the leakiness is unclear. We sought to determine whether endothelial gaps or transcellular holes, similar to those found in leaky vessels in inflammation, could explain the leakiness of tumor vessels. Blood vessels in MCa-IV mouse mammary carcinomas, which are known to be unusually leaky (functional pore size 1.2-2 microm), were compared to vessels in three less leaky tumors and normal mammary glands. Vessels were identified by their binding of intravascularly injected fluorescent cationic liposomes and Lycopersicon esculentum lectin and by CD31 (PECAM) immunoreactivity. The luminal surface of vessels in all four tumors had a defective endothelial monolayer as revealed by scanning electron microscopy. In MCa-IV tumors, 14% of the vessel surface was lined by poorly connected, overlapping cells. The most superficial lining cells, like endothelial cells, had CD31 immunoreactivity and fenestrae with diaphragms, but they had a branched phenotype with cytoplasmic projections as long as 50 microm. Some branched cells were separated by intercellular openings (mean diameter 1.7 microm; range, 0.3-4.7 microm). Transcellular holes (mean diameter 0.6 microm) were also present but were only 8% as numerous as intercellular openings. Some CD31-positive cells protruded into the vessel lumen; others sprouted into perivascular tumor tissue. Tumors in RIP-Tag2 mice had, in addition, tumor cell-lined lakes of extravasated erythrocytes. We conclude that some tumor vessels have a defective cellular lining composed of disorganized, loosely connected, branched, overlapping or sprouting endothelial cells. Openings between these cells contribute to tumor vessel leakiness and may permit access of macromolecular therapeutic agents to tumor cells.

Keywords

CD31TranscellularPathologyEndotheliumBiologyBlood vesselMicrovesselIntravasationEndothelial stem cellAngiogenesisSpheroidAnatomyCell biologyCancer cellCancerCell cultureIn vitroMedicineCancer research

MeSH Terms

AnimalsBlood VesselsCapillary PermeabilityEndotheliumVascularExtracellular SpaceFemaleMaleMammary NeoplasmsAnimalMiceMicroscopyElectronMicroscopyElectronScanningMicroscopyFluorescenceNeoplasm Transplantation

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Publication Info

Year
2000
Type
article
Volume
156
Issue
4
Pages
1363-1380
Citations
1650
Access
Closed

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Cite This

Hiroya Hashizume, Peter Bałuk, Shunichi Morikawa et al. (2000). Openings between Defective Endothelial Cells Explain Tumor Vessel Leakiness. American Journal Of Pathology , 156 (4) , 1363-1380. https://doi.org/10.1016/s0002-9440(10)65006-7

Identifiers

DOI
10.1016/s0002-9440(10)65006-7
PMID
10751361
PMCID
PMC1876882

Data Quality

Data completeness: 86%