Real-Time Imaging Reveals Local, Transient Vascular Permeability, and Tumor Cell Intravasation Stimulated by TIE2hi Macrophage–Derived VEGFA

Harney, Allison S.; Arwert, Esther N.; Entenberg, David; Wang, Yarong; Guo, Peng; Qi, Bin; Oktay, Maja H.; Pollard, Jeffrey W.; Jones, Joan G.; Condeelis, John S.

doi:10.1158/2159-8290.cd-15-0012

Cited by 489 publications

(697 citation statements)

References 36 publications

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“…Similar to macrophage-specifi c Vegfa inactivation, the physical elimination of the tumor macrophages decreased the number of circulating cancer cells in the mice ( 5 ). This fi nding is in line with previous observations and supports the notion that macrophages facilitate the initial steps of tumor metastasis, at least in mouse models of breast cancer ( 1 ( 1 ).…”

supporting

confidence: 89%

“…For example, perivascular macrophages that express the angiopoietin receptor TIE2 are proangiogenic ( 2,3 ) and molecularly distinct from other tumor macrophage subpopulations ( 4 ). In this issue of Cancer Discovery , Harney and colleagues ( 5 ) use intravital microscopy to analyze vascular permeability at sites where TIE2-expressing macrophages (TEM) make contacts with the endothelial cells (EC) that line the tumor blood vessels. They found higher vascular permeability at these sites, compared with vessel segments lacking macrophages.…”

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confidence: 99%

“…An important result of the study ( 5 ) was that the peak of vascular permeability at the TMEM site was both spatially and temporally associated with the attraction of neighboring cancer cells, some of which could enter the bloodstream and leave the tumor. Diffusion of plasma proteins from leaky vessels is known to attract cancer cells and enhance their motility ( 1 ).…”

mentioning

confidence: 99%

“…Diffusion of plasma proteins from leaky vessels is known to attract cancer cells and enhance their motility ( 1 ). Furthermore, the authors noted that the molecular junctions that normally seal adjacent ECs to limit vascular leakiness were more frequently disrupted at the hyperpermeable TMEM sites ( 5 ). Therefore, the cancer cells could more easily fi nd their way to the systemic circulation through these temporarily opened gates.…”

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Cancer Metastasis: Perivascular Macrophages Under Watch

Kadioglu

Palma

2015

Cancer Discovery

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Summary: TIE2-expressing macrophages cluster around blood vessels and sustain tumor angiogenesis. Harney and colleagues now use live imaging of mouse mammary tumors to show that these perivascular macrophages also promote the transient opening of tumor blood vessels to facilitate hematogenous cancer cell dissemination and metastasis. Cancer Discov; 5(9); ©2015 AACR. See related article by Harney et al., p. 932 (5).Tumors often contain abundant macrophage infi ltrates, which are largely derived from circulating monocytes. After tumor colonization, the macrophages acquire specialized phenotypes that appear to be instructed by the distinct signals they are exposed to in different tumor microenvironments, such as perivascular, stromal, or necrotic tumor areas ( 1 ). For example, perivascular macrophages that express the angiopoietin receptor TIE2 are proangiogenic ( 2, 3 ) and molecularly distinct from other tumor macrophage subpopulations ( 4 ). In this issue of Cancer Discovery , Harney and colleagues ( 5 ) use intravital microscopy to analyze vascular permeability at sites where TIE2-expressing macrophages (TEM) make contacts with the endothelial cells (EC) that line the tumor blood vessels. They found higher vascular permeability at these sites, compared with vessel segments lacking macrophages. Furthermore, cancer cell invasion of the blood vessels (intravasation)-the fi rst step in the metastatic cascade-occurred selectively at the macrophage-EC contacts. These new fi ndings provide insight into the regulation of cancer cell dissemination by perivascular macrophages.Previous work by these authors identifi ed perivascular microanatomical structures, called "tumor microenvironment of metastasis" (TMEM), in which a macrophage, a specialized cancer cell, and a blood vessel establish tripartite contacts (ref. 6 ; Fig. 1 ). To study the properties of the TMEM ensemble in live tumors, Harney and colleagues ( 5 ) performed intravital imaging of mouse mammary tumors after the intravenous delivery of a high-molecular weight marker, which would not diffuse across the EC layer of the tumor blood vessels. Video imaging of the tumor blood vessels indeed showed that most of the injected marker had remained entrapped in the vessels. However, the authors also identifi ed discrete sites, in fact, the TMEM structures, where the marker could leak from the vessels. Computer-assisted analysis of the recorded videos revealed that leakage of the marker, which is indicative of high vascular permeability, occurred at different time points after its injection, depending on which TMEM structure was imaged. Also, vascular permeability at each TMEM site was only transient; indeed, it peaked and demised rapidly, showing a pulsating nature. Together, these observations indicate that although permeability appears erratic and ephemeral throughout the tumor vasculature, it occurs specifi cally at vascular sites harboring TMEM structures.An important result of the study ( 5 ) was that the peak of vascular permeability at the TMEM site was bot...

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confidence: 89%

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confidence: 99%

mentioning

confidence: 99%

mentioning

confidence: 99%

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Cancer Metastasis: Perivascular Macrophages Under Watch

Kadioglu

Palma

2015

Cancer Discovery

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“…Using this method, Harney et al (2015) showed that intravasation can occur simultaneously when a macrophage, tumour cell and an endothelial cell are in direct contact, because the VEGFA signalling from macrophages induces local, transient vascular permeability and subsequent tumour cell intravasation [63].…”

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The Role of EphB4 and Ephrin-B2 Interactions in Prostate Cancer Models of Intravasation and Extravasation

Protsenko¹

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Understanding the In Vivo Fate of Advanced Materials by Imaging

Garlin

et al. 2020

Adv Funct Materials

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Engineered materials are ubiquitous in biomedical applications ranging from systemic drug delivery systems to orthopedic implants, and their actions unfold across multiple time‐ and length‐scales. The efficacy and safety of biologics, nanomaterials, and macroscopic implants are all dictated by the same general principles of pharmacology as applied to small molecule drugs, comprising how the body affects materials (pharmacokinetics, PK) and conversely how materials affect the body (pharmacodynamics, PD). Imaging technologies play an increasingly insightful role in monitoring both of these processes, often simultaneously: translational macroscopic imaging modalities such as magnetic resonance imaging and positron emission tomography/computed tomography offer whole‐body quantitation of biodistribution and structural or molecular response, while ex vivo approaches and optical imaging via in vivo (intravital) microscopy reveal behaviors at subcellular resolution. In this review, the authors survey developments in imaging the in situ behavior of systemically and locally administered materials, with a particular focus on using microscopy to understand transport, target engagement, and downstream host responses at a single‐cell level. The themes of microenvironmental influence, controlled drug release, on‐target molecular action, and immune response, especially as mediated by macrophages and other myeloid cells, are examined. Finally, the future directions of how new imaging technologies may propel efficient clinical translation of next‐generation therapeutics and medical devices are proposed.

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Real-Time Imaging Reveals Local, Transient Vascular Permeability, and Tumor Cell Intravasation Stimulated by TIE2hi Macrophage–Derived VEGFA

Cited by 489 publications

References 36 publications

Cancer Metastasis: Perivascular Macrophages Under Watch

Cancer Metastasis: Perivascular Macrophages Under Watch

The Role of EphB4 and Ephrin-B2 Interactions in Prostate Cancer Models of Intravasation and Extravasation

Understanding the In Vivo Fate of Advanced Materials by Imaging

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