共 46 条
Neuropilin-1 Identifies a Subset of Bone Marrow Gr1-Monocytes That Can Induce Tumor Vessel Normalization and Inhibit Tumor Growth
被引:44
作者:

Carrer, Alessandro
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ICGEB, Mol Med Lab, I-34149 Trieste, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

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Zacchigna, Serena
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ICGEB, Mol Med Lab, I-34149 Trieste, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Pattarini, Lucia
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机构:
ICGEB, Mol Med Lab, I-34149 Trieste, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Zentilin, Lorena
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ICGEB, Mol Med Lab, I-34149 Trieste, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Ruozi, Giulia
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ICGEB, Mol Med Lab, I-34149 Trieste, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Mano, Miguel
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ICGEB, Mol Med Lab, I-34149 Trieste, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Sinigaglia, Milena
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ICGEB, Mol Med Lab, I-34149 Trieste, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Maione, Federica
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机构:
Univ Turin, Dept Oncol Sci, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy
Univ Turin, Div Vasc Biol, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Serini, Guido
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Univ Turin, Dept Oncol Sci, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy
Univ Turin, Div Vasc Biol, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Giraudo, Enrico
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机构:
Univ Turin, Dept Oncol Sci, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy
Univ Turin, Div Vasc Biol, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Bussolino, Federico
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h-index: 0
机构:
Univ Turin, Dept Oncol Sci, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy
Univ Turin, Div Vasc Biol, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy

Giacca, Mauro
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机构:
ICGEB, Mol Med Lab, I-34149 Trieste, Italy
Univ Trieste, Dept Med Sci, Fac Med, Trieste, Italy ICGEB, Mol Med Lab, I-34149 Trieste, Italy
机构:
[1] ICGEB, Mol Med Lab, I-34149 Trieste, Italy
[2] Univ Trieste, Dept Med Sci, Fac Med, Trieste, Italy
[3] Univ Turin, Dept Oncol Sci, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy
[4] Univ Turin, Div Vasc Biol, Inst Canc Res & Treatment IRCC, Sch Med, Candiolo, Italy
基金:
欧洲研究理事会;
关键词:
SEMAPHORIN;
3A;
MYELOID CELLS;
MACROPHAGE POLARIZATION;
ANGIOGENESIS;
CANCER;
MONOCYTES;
EXPRESSION;
NEOVASCULARIZATION;
RECEPTORS;
HYPOXIA;
D O I:
10.1158/0008-5472.CAN-12-0762
中图分类号:
R73 [肿瘤学];
学科分类号:
100214 ;
摘要:
Improving tumor perfusion, thus tempering tumor-associated hypoxia, is known to impair cancer progression. Previous work from our laboratory has shown that VEGF-A165 and semaphorin 3A (Sema3A) promote vessel maturation through the recruitment of a population of circulating monocytes expressing the neuropilin-1 (Nrp1) receptor (Nrp1-expressing monocytes; NEM). Here, we define the characteristics of bone marrow NEMs and assess whether these cells might represent an exploitable tool to induce tumor vessel maturation. Gene expression signature and surface marker analysis have indicated that NEMs represent a specific subset of CD11b+ Nrp1+ Gr1- resident monocytes, distinctively recruited by Sema3A. NEMs were found to produce several factors involved in vessel maturation, including PDGFb, TGF-beta, thrombospondin-1, and CXCL10; consistently, they were chemoattractive for vascular smooth muscle cells in vitro. When directly injected into growing tumors, NEMs, isolated either from the bone marrow or from Sema3A-expressing muscles, exerted antitumor activity despite having no direct effects on the proliferation of tumor cells. NEM inoculation specifically promoted mural cell coverage of tumor vessels and decreased vascular leakiness. Tumors treated with NEMs were smaller, better perfused and less hypoxic, and had a reduced level of activation of HIF-1 alpha. We conclude that NEMs represent a novel, unique population of myeloid cells that, once inoculated into a tumor, induce tumor vessel normalization and inhibit tumor growth. Cancer Res; 72( 24); 6371-81. (c) 2012 AACR.
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页码:6371 / 6381
页数:11
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Univ Penn, Thorac Oncol Res Lab, Philadelphia, PA 19104 USA Biogen Idec, Oncol Cell Signaling, Cambridge, MA 02142 USA

Sun, Jing
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Univ Penn, Thorac Oncol Res Lab, Philadelphia, PA 19104 USA Biogen Idec, Oncol Cell Signaling, Cambridge, MA 02142 USA

Kim, Samuel
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Univ Penn, Thorac Oncol Res Lab, Philadelphia, PA 19104 USA Biogen Idec, Oncol Cell Signaling, Cambridge, MA 02142 USA

Kapoor, Veena
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Univ Penn, Thorac Oncol Res Lab, Philadelphia, PA 19104 USA Biogen Idec, Oncol Cell Signaling, Cambridge, MA 02142 USA

Cheng, Guanjun
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Univ Penn, Thorac Oncol Res Lab, Philadelphia, PA 19104 USA Biogen Idec, Oncol Cell Signaling, Cambridge, MA 02142 USA

Ling, Leona
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Biogen Idec, Oncol Cell Signaling, Cambridge, MA 02142 USA Biogen Idec, Oncol Cell Signaling, Cambridge, MA 02142 USA

Worthen, G. Scott
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Univ Penn, Div Neonatol, Childrens Hosp Philadelphia, ARC, Philadelphia, PA 19104 USA Biogen Idec, Oncol Cell Signaling, Cambridge, MA 02142 USA

Albelda, Steven M.
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Univ Penn, Thorac Oncol Res Lab, Philadelphia, PA 19104 USA Biogen Idec, Oncol Cell Signaling, Cambridge, MA 02142 USA