Pilot Study on “Pericytic Mimicry” and Potential Embryonic/Stem Cell Properties of Angiotropic Melanoma Cells Interacting with the Abluminal Vascular Surface

Lugassy, Claire; Wadehra, Madhuri; Li, Xinmin; Corselli, Mirko; Akhavan, David; Binder, Scott W.; Péault, Bruno; Cochran, Alistair J.; Mischel, Paul S.; Kleinman, Hynda K.; Barnhill, Raymond L.

doi:10.1007/s12307-012-0128-5

Cited by 51 publications

(59 citation statements)

References 59 publications

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“…Building on these findings, human melanoma cells were shown to localize to both endothelial tubules formed in vitro as well as invade in a perivascular fashion when injected ex vivo into the brains of mice [6,36] . Pericyte mimicry in melanoma has been confirmed at the immunophenotypic level, where angiotropic melanoma cells express pericyte antigens PDGFR-β, NG2, and CD146 [30] . Further, microarray analysis showed increased expression of PDGF-β after migration of melanoma cells along the abluminal surface of endothelial tubules during the co-culture of endothelial cells and melanoma cells [30] , indicating increased expression of a receptor key in the endothelium's recruitment of pericytes.…”

Section: Pericyte Mimicry / Extravascular Migratory Metastasismentioning

confidence: 95%

“…Pericyte mimicry in melanoma has been confirmed at the immunophenotypic level, where angiotropic melanoma cells express pericyte antigens PDGFR-β, NG2, and CD146 [30] . Further, microarray analysis showed increased expression of PDGF-β after migration of melanoma cells along the abluminal surface of endothelial tubules during the co-culture of endothelial cells and melanoma cells [30] , indicating increased expression of a receptor key in the endothelium's recruitment of pericytes. Additionally, the interaction between the abluminal endothelial tubules and angiotropic melanoma cells induced differential expression of malignancy associated genes, linked to metastasis (CCL2, ICAM1 and IL6) and disease progression (CCL2, ICAM1, SELE, TRAF1, IL6, SERPINB2 and CXCL6) [30] .…”

Section: Pericyte Mimicry / Extravascular Migratory Metastasismentioning

confidence: 95%

“…Further, microarray analysis showed increased expression of PDGF-β after migration of melanoma cells along the abluminal surface of endothelial tubules during the co-culture of endothelial cells and melanoma cells [30] , indicating increased expression of a receptor key in the endothelium's recruitment of pericytes. Additionally, the interaction between the abluminal endothelial tubules and angiotropic melanoma cells induced differential expression of malignancy associated genes, linked to metastasis (CCL2, ICAM1 and IL6) and disease progression (CCL2, ICAM1, SELE, TRAF1, IL6, SERPINB2 and CXCL6) [30] . Angiotropism has been shown to be clinically quite relevant, as angiotropism is a poor prognostic indicator in malignant melanoma [37] .…”

Section: Pericyte Mimicry / Extravascular Migratory Metastasismentioning

confidence: 98%

“…Pericyte mimicry, or angiotropism, has been most thoroughly studied in melanoma [5,6,14,[29][30][31] . Lugassy et al first described the pericyte-like position of invading melanoma cells along the blood vessel basal lamina [32][33][34] .…”

Section: Pericyte Mimicry / Extravascular Migratory Metastasismentioning

confidence: 99%

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Review of Pericytes in Tumor Biology

Scott¹,

Jia²,

Lam³

et al. 2015

International Journal of Orthopaedics

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Pericytes are contractile cells that surround the endothelium of capillaries and venules throughout the body. Pericytes were once thought to have a limited role in blood pressure control and angiogenesis. Today, knowledge about pericytes and other perivascular stem cells has vastly expanded. The understanding of the biologic significance of pericytes was most changed by the recognition of the perivascular identity of mesenchymal stem cells. The following review article will summarize the known functions and importance of pericytes in particular relevance to tumor biology. These roles include: (1) pericytes as the potential cell of origin for multiple soft tissue tumors; (2) the role of pericyte in regulating tumor cell vascular invasion; and 3) angiotropism or 'pericytic mimicry' as a mechanism of malignant tumor spread. Although not discussed, the role of pericytes in pathophysiology far exceeds the realms of tumor biology, including cardiovascular atherosclerotic disease, chronic kidney disease, fibrotic repair processes, and fibroproliferative diseases. In summary, the known roles of pericytes in tumor formation, growth, and invasion have greatly expanded. These include pericytic differentiation in soft tissue tumors, regulation of vascular invasion in solid tumors, and extravascular migratory migration of common malignancies.

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Section: Pericyte Mimicry / Extravascular Migratory Metastasismentioning

confidence: 95%

Section: Pericyte Mimicry / Extravascular Migratory Metastasismentioning

confidence: 95%

Section: Pericyte Mimicry / Extravascular Migratory Metastasismentioning

confidence: 98%

Section: Pericyte Mimicry / Extravascular Migratory Metastasismentioning

confidence: 99%

See 2 more Smart Citations

Review of Pericytes in Tumor Biology

Scott¹,

Jia²,

Lam³

et al. 2015

International Journal of Orthopaedics

Self Cite

View full text Add to dashboard Cite

show abstract

“…In cancer research there is an emerging idea of "pericyte mimicry", prompted by the finding that a subset of melanoma cells can express the classical pericyte markers PDGFRβ and NG2 and display stem cell properties (Lugassy et al 2013). This implies that these markers are not specific to pericytes, but can be expressed by various populations of stem cells in response to environmental cues.…”

mentioning

confidence: 99%

Mesenchymal cells emerge as primary contributors to fibrosis in multiple tissues

Tsang

2013

Journal of Cell Communication and Signaling

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A longstanding controversy exists regarding the cellular origin of myofibroblasts in tissue fibrosis. A recent study by Hung and colleagues (Am J Respir Crit Care Med 188 (7):820-830, 2013) used genetic fate mapping of FoxD1 embryonic progenitor cells to show a major and direct contribution of mesenchymal cells to fibrogenesis in the lung. Future studies using FoxD1-specific inducible knockout models of pro-fibrotic genes such as CCN2 will be valuable for determining anti-fibrotic drug targets. The emergence of pericyte-like myofibroblast precursors also raises the question of whether mesenchymal stem cells in various niches contribute to fibrotic responses throughout the body.

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Skin Progenitor Cells Contribute to Bleomycin‐Induced Skin Fibrosis

Liu

Hérault

Leask

2014

Arthritis & Rheumatology

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Objective. The origin of the cells that contribute to skin fibrosis is unclear. We undertook the present study to assess the contribution of Sox2-expressing skin progenitor cells to bleomycin-induced scleroderma.Methods. Scleroderma was induced, by bleomycin administration, in wild-type mice and in mice in which CCN2 was deleted from Sox2-expressing cells. Lineage tracing analysis was performed to assess whether cells expressing Sox2 are recruited to fibrotic lesions in response to bleomycin-induced scleroderma.Results. In response to bleomycin, Sox2-positive/ ␣-smooth muscle actin-positive cells were recruited to fibrotic tissue. CCN2-conditional knockout mice in which CCN2 was deleted from Sox2-expressing cells exhibited resistance to bleomycin-induced skin fibrosis. Collectively, these results indicate that CCN2 is required for the recruitment of progenitor cells and that CCN2-expressing progenitor cells are essential for bleomycin-induced skin fibrosis. Lineage tracing analysis using mice in which a tamoxifen-dependent Cre recombinase was expressed under the control of the Sox2 promoter confirmed that progenitor cells were recruited to the fibrotic lesion in response to bleomycin, and that this did not occur in CCN2-knockout mice. The ability of serum to induce ␣-smooth muscle actin expression in skin progenitor cells required the presence of CCN2.Conclusion. Sox2-positive skin progenitor cells are required in order for bleomycin-induced skin fibrosis to occur, and CCN2 is required for the recruitment of these cells to the fibrotic lesion. Targeting stem cell recruitment or CCN2 may therefore represent a useful therapeutic approach in combating fibrotic skin disease.

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Pilot Study on “Pericytic Mimicry” and Potential Embryonic/Stem Cell Properties of Angiotropic Melanoma Cells Interacting with the Abluminal Vascular Surface

Cited by 51 publications

References 59 publications

Review of Pericytes in Tumor Biology

Review of Pericytes in Tumor Biology

Mesenchymal cells emerge as primary contributors to fibrosis in multiple tissues

Skin Progenitor Cells Contribute to Bleomycin‐Induced Skin Fibrosis

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