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Altering macrophage polarization in the tumor environment: the role of response gene to complement 32 被引量:2

Altering macrophage polarization in the tumor environment: the role of response gene to complement 32
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摘要 macrophages in tumors are a major problem. They are dynamic and heterogeneous cells, and their differenti- ation, tissue distribution and responsiveness to stimuli are governed by distinct mechanisms. In response to certain signals, macrophages can undergo either M1- or M2-type activation, which result in two distinct functional phenotypes. macrophages in tumors are a major problem. They are dynamic and heterogeneous cells, and their differenti- ation, tissue distribution and responsiveness to stimuli are governed by distinct mechanisms. In response to certain signals, macrophages can undergo either M1- or M2-type activation, which result in two distinct functional phenotypes.
作者 Matteo Santoni Stefano Cascinu Charles D Mills
机构地区 Clinica di Oncologia Medica BioMedical Consultants
出处 《Cellular & Molecular Immunology》 SCIE CAS CSCD 2015年第6期783-784,共2页 中国免疫学杂志(英文版)
分类号 Q26 [生物学—细胞生物学] Q51 [生物学—生物化学]
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参考文献10

  • 1Mills CD, Shearer J, Evans R, Caldwell MD. Macrophage arginine metabolism and theinhibition or stimulation of cancer. J Immunol 1992, 149: 2709-2714.
  • 2Hibbs JB Jr, Vavrin Z, Taintor RR. L-arginine is required for expression of the activated macrophage effector mechanism causing selective metabolic inhibition in target cells. J Immuno11987, 138: 550-565.
  • 3Mills CD. M 1 and M2 macrophages: oracles of health and disease. Crit Rev Irnmunol 2012, 32: 463-488.
  • 4Noy R, Pollard JW. Tumor-associated macrophages: from mechanisms to therapy. Immunity2014, 41: 49-61.
  • 5Santoni M, Massari F, Amantini C, Nabissi M, Maines F, Burattini Let al. Emerging role of tumor-associated macrophages as therapeutic targets in patients with metastatic renal cell carcinoma. Cancer Immunol Immunother 2013: 62: 1757-1768.
  • 6Zhao P, Gao D, Wang Q, Song B, Shao Q, Sun Jet al. Response Gene to Complement 32 expression on M2-polarized macrophage and tumor associated macrophages is M-CSF dependent and enhanced by tumor-derived I L-4. Ceil Mol Immuno/2014, 12: 692-699.
  • 7Albina JE, Mills CD, Henry WL Jr, Caldwell MD. Temporal expression of different pathways of 1-arginine metabolism in healing wounds. J Immuno/1990, 144: 3877-3880.
  • 8Mills CD, Ley K. M1 and M2 macrophages: the chicken and the egg of immunity. J Innate Immun 2014, 6: 716-726.
  • 9Pyonteck SM, Akkari L, Schuhmacher A J, Bowman RL, Sevenich L, Quail DF et al. CSF-1R inhibition alters macrophage polarization and blocks tumor progression. NatMed2014, 19: 1262-1274.
  • 10Daley JM, Brancato SK, Thomay AA, Reichner JS, Aibina JE. The phenotype of murine wound macrophages. J Leukoc Biol 2010: 87: 59-67.

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Cellular & Molecular Immunology
2015年 第6期

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