Gorham-stout syndrome: A monocyte-mediated cytokine propelled disease

Silvia Colucci; Giulia Taraboletti; Luca Primo; Andrea Viale; Cristina Roca; Donatella Valdembri; Massimo Geuna; Marco Pagano; Maria Grano; Anthony M. Pogrel; Adrian L. Harris; Nicholas N. Athanasou; Alberto Mantovani; Alberta Zallone; Federico Bussolino

doi:10.1359/JBMR.051019

Gorham-stout syndrome: A monocyte-mediated cytokine propelled disease

Silvia Colucci, Giulia Taraboletti, Luca Primo, Andrea Viale, Cristina Roca, Donatella Valdembri, Massimo Geuna, Marco Pagano, Maria Grano, Anthony M. Pogrel, Adrian L. Harris, Nicholas N. Athanasou, Alberto Mantovani, Alberta Zallone, Federico Bussolino

Research output: Contribution to journal › Article › peer-review

58 Scopus citations

Abstract

We studied the biological features and the immunophenotype of a cell culture established from the lesion of soft tissues of a woman affected by Gorham-Stout syndrome. We found that these cells belonged to a monocytic lineage with some characteristics of immature osteoclasts and were able to release large amounts of osteoclastogenic and angiogenic molecules that may contribute to disease progression. Introduction: Gorham-Stout syndrome is a rare disease characterized by osteolysis and proliferation of vascular or lymphatic vessels, with a severe outcome. Its etiology and the identification of the cell types involved are completely unknown. Materials and Methods: A cell culture from a lesion of soft tissues was established, and its behavior in vitro and in immunodeficient mice was studied. We analyzed (1) the cell phenotype by flow cytometry; (2) the adhesive and migratory properties on different substrates; (3) the ability to differentiate into mature osteoclasts; (4) the production of osteclastogenic and angiogenic molecules; (5) the in vivo angiogenic activity of the cells subcutaneously implanted in mouse in a Matrigel plug; and (6) the ability to recapitulate the disease when transplanted in nude mice. Results and Conclusions: The established culture consisted of a morphologically homogeneous cell population belonging to a monocytic lineage having some features of an osteoclast-like cell type. Cells had an invasive phenotype, were angiogenic, and produced osteoclastogenic (IL-6, TGF-β1, IL-1β) and angiogenic (vascular endothelial growth factor-A [VEGF-A], CXCL-8) molecules when challenged with inflammatory cytokines. Immunodeficient mice injected with these cells did not show any bone lesions or vascular alteration, but had high amounts of circulating human IL-6 and VEGF-A. Cells isolated from a cutaneous lymphangiomatosis did not show any of these findings. These data suggest that cells of monocyte-macrophage lineage play an essential role in the pathogenesis of Gorham-Stout disease, whose progression is propelled by cytokine circuits that accelerate angiogenesis and osteoclastogenesis.

Original language	English (US)
Pages (from-to)	207-218
Number of pages	12
Journal	Journal of Bone and Mineral Research
Volume	21
Issue number	2
DOIs	https://doi.org/10.1359/JBMR.051019
State	Published - Feb 2006
Externally published	Yes

Keywords

Angiogenesis
Cytokine
Gorham-Stout disease
Monocyte
Osteoclast

ASJC Scopus subject areas

Endocrinology, Diabetes and Metabolism
Orthopedics and Sports Medicine

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10.1359/JBMR.051019

Cite this

Colucci, S., Taraboletti, G., Primo, L., Viale, A., Roca, C., Valdembri, D., Geuna, M., Pagano, M., Grano, M., Pogrel, A. M., Harris, A. L., Athanasou, N. N., Mantovani, A., Zallone, A., & Bussolino, F. (2006). Gorham-stout syndrome: A monocyte-mediated cytokine propelled disease. Journal of Bone and Mineral Research, 21(2), 207-218. https://doi.org/10.1359/JBMR.051019

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title = "Gorham-stout syndrome: A monocyte-mediated cytokine propelled disease",

abstract = "We studied the biological features and the immunophenotype of a cell culture established from the lesion of soft tissues of a woman affected by Gorham-Stout syndrome. We found that these cells belonged to a monocytic lineage with some characteristics of immature osteoclasts and were able to release large amounts of osteoclastogenic and angiogenic molecules that may contribute to disease progression. Introduction: Gorham-Stout syndrome is a rare disease characterized by osteolysis and proliferation of vascular or lymphatic vessels, with a severe outcome. Its etiology and the identification of the cell types involved are completely unknown. Materials and Methods: A cell culture from a lesion of soft tissues was established, and its behavior in vitro and in immunodeficient mice was studied. We analyzed (1) the cell phenotype by flow cytometry; (2) the adhesive and migratory properties on different substrates; (3) the ability to differentiate into mature osteoclasts; (4) the production of osteclastogenic and angiogenic molecules; (5) the in vivo angiogenic activity of the cells subcutaneously implanted in mouse in a Matrigel plug; and (6) the ability to recapitulate the disease when transplanted in nude mice. Results and Conclusions: The established culture consisted of a morphologically homogeneous cell population belonging to a monocytic lineage having some features of an osteoclast-like cell type. Cells had an invasive phenotype, were angiogenic, and produced osteoclastogenic (IL-6, TGF-β1, IL-1β) and angiogenic (vascular endothelial growth factor-A [VEGF-A], CXCL-8) molecules when challenged with inflammatory cytokines. Immunodeficient mice injected with these cells did not show any bone lesions or vascular alteration, but had high amounts of circulating human IL-6 and VEGF-A. Cells isolated from a cutaneous lymphangiomatosis did not show any of these findings. These data suggest that cells of monocyte-macrophage lineage play an essential role in the pathogenesis of Gorham-Stout disease, whose progression is propelled by cytokine circuits that accelerate angiogenesis and osteoclastogenesis.",

keywords = "Angiogenesis, Cytokine, Gorham-Stout disease, Monocyte, Osteoclast",

author = "Silvia Colucci and Giulia Taraboletti and Luca Primo and Andrea Viale and Cristina Roca and Donatella Valdembri and Massimo Geuna and Marco Pagano and Maria Grano and Pogrel, {Anthony M.} and Harris, {Adrian L.} and Athanasou, {Nicholas N.} and Alberto Mantovani and Alberta Zallone and Federico Bussolino",

note = "Funding Information: The authors would like to acknowledge the financial support from the National Science Foundation of China (NSFC 41473105, U1133005 and 41303077) and National Water Pollution Control Program of China (2014ZX07206-005). Thanks to Agilent Technologies China for assistance in identification of photodegradation by-products. This is a Contribution No. IS-2262 from GIGCAS.",

year = "2006",

month = feb,

doi = "10.1359/JBMR.051019",

language = "English (US)",

volume = "21",

pages = "207--218",

journal = "Journal of Bone and Mineral Research",

issn = "0884-0431",

publisher = "Wiley-Blackwell",

number = "2",

}

TY - JOUR

T1 - Gorham-stout syndrome

T2 - A monocyte-mediated cytokine propelled disease

AU - Colucci, Silvia

AU - Taraboletti, Giulia

AU - Primo, Luca

AU - Viale, Andrea

AU - Roca, Cristina

AU - Valdembri, Donatella

AU - Geuna, Massimo

AU - Pagano, Marco

AU - Grano, Maria

AU - Pogrel, Anthony M.

AU - Harris, Adrian L.

AU - Athanasou, Nicholas N.

AU - Mantovani, Alberto

AU - Zallone, Alberta

AU - Bussolino, Federico

N1 - Funding Information: The authors would like to acknowledge the financial support from the National Science Foundation of China (NSFC 41473105, U1133005 and 41303077) and National Water Pollution Control Program of China (2014ZX07206-005). Thanks to Agilent Technologies China for assistance in identification of photodegradation by-products. This is a Contribution No. IS-2262 from GIGCAS.

PY - 2006/2

Y1 - 2006/2

N2 - We studied the biological features and the immunophenotype of a cell culture established from the lesion of soft tissues of a woman affected by Gorham-Stout syndrome. We found that these cells belonged to a monocytic lineage with some characteristics of immature osteoclasts and were able to release large amounts of osteoclastogenic and angiogenic molecules that may contribute to disease progression. Introduction: Gorham-Stout syndrome is a rare disease characterized by osteolysis and proliferation of vascular or lymphatic vessels, with a severe outcome. Its etiology and the identification of the cell types involved are completely unknown. Materials and Methods: A cell culture from a lesion of soft tissues was established, and its behavior in vitro and in immunodeficient mice was studied. We analyzed (1) the cell phenotype by flow cytometry; (2) the adhesive and migratory properties on different substrates; (3) the ability to differentiate into mature osteoclasts; (4) the production of osteclastogenic and angiogenic molecules; (5) the in vivo angiogenic activity of the cells subcutaneously implanted in mouse in a Matrigel plug; and (6) the ability to recapitulate the disease when transplanted in nude mice. Results and Conclusions: The established culture consisted of a morphologically homogeneous cell population belonging to a monocytic lineage having some features of an osteoclast-like cell type. Cells had an invasive phenotype, were angiogenic, and produced osteoclastogenic (IL-6, TGF-β1, IL-1β) and angiogenic (vascular endothelial growth factor-A [VEGF-A], CXCL-8) molecules when challenged with inflammatory cytokines. Immunodeficient mice injected with these cells did not show any bone lesions or vascular alteration, but had high amounts of circulating human IL-6 and VEGF-A. Cells isolated from a cutaneous lymphangiomatosis did not show any of these findings. These data suggest that cells of monocyte-macrophage lineage play an essential role in the pathogenesis of Gorham-Stout disease, whose progression is propelled by cytokine circuits that accelerate angiogenesis and osteoclastogenesis.

AB - We studied the biological features and the immunophenotype of a cell culture established from the lesion of soft tissues of a woman affected by Gorham-Stout syndrome. We found that these cells belonged to a monocytic lineage with some characteristics of immature osteoclasts and were able to release large amounts of osteoclastogenic and angiogenic molecules that may contribute to disease progression. Introduction: Gorham-Stout syndrome is a rare disease characterized by osteolysis and proliferation of vascular or lymphatic vessels, with a severe outcome. Its etiology and the identification of the cell types involved are completely unknown. Materials and Methods: A cell culture from a lesion of soft tissues was established, and its behavior in vitro and in immunodeficient mice was studied. We analyzed (1) the cell phenotype by flow cytometry; (2) the adhesive and migratory properties on different substrates; (3) the ability to differentiate into mature osteoclasts; (4) the production of osteclastogenic and angiogenic molecules; (5) the in vivo angiogenic activity of the cells subcutaneously implanted in mouse in a Matrigel plug; and (6) the ability to recapitulate the disease when transplanted in nude mice. Results and Conclusions: The established culture consisted of a morphologically homogeneous cell population belonging to a monocytic lineage having some features of an osteoclast-like cell type. Cells had an invasive phenotype, were angiogenic, and produced osteoclastogenic (IL-6, TGF-β1, IL-1β) and angiogenic (vascular endothelial growth factor-A [VEGF-A], CXCL-8) molecules when challenged with inflammatory cytokines. Immunodeficient mice injected with these cells did not show any bone lesions or vascular alteration, but had high amounts of circulating human IL-6 and VEGF-A. Cells isolated from a cutaneous lymphangiomatosis did not show any of these findings. These data suggest that cells of monocyte-macrophage lineage play an essential role in the pathogenesis of Gorham-Stout disease, whose progression is propelled by cytokine circuits that accelerate angiogenesis and osteoclastogenesis.

KW - Angiogenesis

KW - Cytokine

KW - Gorham-Stout disease

KW - Monocyte

KW - Osteoclast

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Gorham-stout syndrome: A monocyte-mediated cytokine propelled disease

Abstract

Keywords

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