论文信息 - Physical nanoscale conduit-mediated communication between tumour cells and the endothelium modulates endothelial phenotype - 字舞流文

Physical nanoscale conduit-mediated communication between tumour cells and the endothelium modulates endothelial phenotype

Metastasis is a major cause of mortality and remains a hurdle in the search for a cure for cancer. Not much is known about metastatic cancer cells and endothelial cross-talk, which occurs at multiple stages during metastasis. Here we report a dynamic regulation of the endothelium by cancer cells through the formation of nanoscale intercellular membrane bridges, which act as physical conduits for transfer of microRNAs. The communication between the tumour cell and the endothelium upregulates markers associated with pathological endothelium, which is reversed by pharmacological inhibition of these nanoscale conduits. These results lead us to define the notion of ‘metastatic hijack': cancer cell-induced transformation of healthy endothelium into pathological endothelium via horizontal communication through the nanoscale conduits. Pharmacological perturbation of these nanoscale membrane bridges decreases metastatic foci in vivo. Targeting these nanoscale membrane bridges may potentially emerge as a new therapeutic opportunity in the management of metastatic cancer.

Shiladitya Sengupta | Yonatan Tekleab | Amjad Husain | Seema Sehrawat | Or Gadish | Seema Sehrawat | H. Dvorak | Shiladitya Sengupta | B. Zetter | V. Sabbisetti | A. Kulkarni | Ashish Kulkarni | Venkata Sabbisetti | Shelly Kaushik | Bruce Zetter | Yamicia Connor | Sarah Tekleab | Shyama Nandakumar | Cherelle Walls | Harold Dvorak | Elazer R Edelman | Y. Connor | O. Gadish | Amjad Husain | Shelly Kaushik | S. Nandakumar | Sarah Tekleab | C. Walls | Y. Tekleab | Elazer R. Edelman

[1] L Orci,et al. In vitro rapid organization of endothelial cells into capillary-like networks is promoted by collagen matrices , 1983, The Journal of cell biology.

[2] Simon C Watkins,et al. Functional connectivity between immune cells mediated by tunneling nanotubules. , 2005, Immunity.

[3] G. Condorelli,et al. TGFβ Triggers miR-143/145 Transfer From Smooth Muscle Cells to Endothelial Cells, Thereby Modulating Vessel Stabilization. , 2015, Circulation research.

[4] Yibin Kang,et al. Unravelling the complexity of metastasis — molecular understanding and targeted therapies , 2011, Nature Reviews Cancer.

[5] G. Sledge,et al. Rethinking the metastatic cascade as a therapeutic target , 2011, Nature Reviews Clinical Oncology.

[6] D. Hanahan,et al. Hallmarks of Cancer: The Next Generation , 2011, Cell.

[7] P. Steeg,et al. Metastasis: a therapeutic target for cancer , 2008, Nature Clinical Practice Oncology.

[8] S. Tavazoie,et al. A microRNA regulon that mediates endothelial recruitment and metastasis by cancer cells , 2011, Nature.

[9] F. Hofstaedter,et al. CD137 Expression in Tumor Vessel Walls , 2001 .

[10] D. Ingber,et al. Forty-Year Journey of Angiogenesis Translational Research , 2011, Science Translational Medicine.

[11] E. Edelman,et al. Stromal Endothelial Cells Directly Influence Cancer Progression , 2011, Science Translational Medicine.

[12] George A Calin,et al. MicroRNAs miR-221 and miR-222: a new level of regulation in aggressive breast cancer , 2011, Genome Medicine.

[13] Fang Liu,et al. miR-92a family and their target genes in tumorigenesis and metastasis. , 2014, Experimental cell research.

[14] J. Li,et al. MicroRNA-885-3p inhibits the growth of HT-29 colon cancer cell xenografts by disrupting angiogenesis via targeting BMPR1A and blocking BMP/Smad/Id1 signaling , 2014, Oncogene.

[15] M. Hou,et al. Up-regulation of miR-182 by β-catenin in breast cancer increases tumorigenicity and invasiveness by targeting the matrix metalloproteinase inhibitor RECK. , 2013, Biochimica et biophysica acta.

[16] Zhaoshi Jiang,et al. Tumour‐secreted miR‐9 promotes endothelial cell migration and angiogenesis by activating the JAK‐STAT pathway , 2012, The EMBO journal.

[17] Zhaoli Chen,et al. microRNA-92a Promotes Lymph Node Metastasis of Human Esophageal Squamous Cell Carcinoma via E-Cadherin* , 2010, The Journal of Biological Chemistry.

[18] C. Mierke. Role of the Endothelium during Tumor Cell Metastasis: Is the Endothelium a Barrier or a Promoter for Cell Invasion and Metastasis? , 2009, Journal of biophysics.

[19] M. Kuroda,et al. Leukemia cell to endothelial cell communication via exosomal miRNAs , 2013, Oncogene.

[20] A. Mogilner,et al. The physics of filopodial protrusion. , 2005, Biophysical journal.

[21] Daya Luo,et al. A systematic evaluation of miRNA:mRNA interactions involved in the migration and invasion of breast cancer cells , 2013, Journal of Translational Medicine.

[22] I. Melero,et al. Agonist anti-CD137 mAb act on tumor endothelial cells to enhance recruitment of activated T lymphocytes. , 2011, Cancer research.

[23] R. Weinberg,et al. Tumour invasion and metastasis initiated by microRNA-10b in breast cancer , 2007, Nature.

[24] Q. Sattentau,et al. Membrane nanotubes physically connect T cells over long distances presenting a novel route for HIV-1 transmission , 2008, Nature Cell Biology.

[25] E. Edelman,et al. Dysfunctional endothelial cells directly stimulate cancer inflammation and metastasis , 2013, International journal of cancer.

[26] D. Hanahan,et al. Patterns and Emerging Mechanisms of the Angiogenic Switch during Tumorigenesis , 1996, Cell.

[27] N. Tsubota,et al. A role for heterologous gap junctions between melanoma and endothelial cells in metastasis. , 2000, The Journal of clinical investigation.

[28] S. Milstien,et al. Is tail vein injection a relevant breast cancer lung metastasis model? , 2013, Journal of thoracic disease.

[29] P. Steeg. Tumor metastasis: mechanistic insights and clinical challenges , 2006, Nature Medicine.

[30] K. Manova-Todorova,et al. Intercellular communication in malignant pleural mesothelioma: properties of tunneling nanotubes , 2014, Front. Physiol..

[31] P. Majumder,et al. Temporally sequenced anticancer drugs overcome adaptive resistance by targeting a vulnerable chemotherapy-induced phenotypic transition , 2015, Nature Communications.

[32] T. Kornberg,et al. Cytoneme-Mediated Contact-Dependent Transport of the Drosophila Decapentaplegic Signaling Protein , 2014, Science.

[33] J. Wood,et al. Hepatocyte Growth Factor/Scatter Factor Can Induce Angiogenesis Independently of Vascular Endothelial Growth Factor , 2003, Arteriosclerosis, thrombosis, and vascular biology.

[34] J. Folkman,et al. Blood Vessel Formation: What Is Its Molecular Basis? , 1996, Cell.

[35] E. Hodneland,et al. Selective block of tunneling nanotube (TNT) formation inhibits intercellular organelle transfer between PC12 cells , 2009, FEBS letters.

[36] R. Deng,et al. Suppression of MIM by microRNA-182 activates RhoA and promotes breast cancer metastasis , 2014, Oncogene.

[37] V. Thayanithy,et al. Tumor-stromal cross talk: direct cell-to-cell transfer of oncogenic microRNAs via tunneling nanotubes. , 2014, Translational research : the journal of laboratory and clinical medicine.

[38] A. Børresen-Dale,et al. Identifying microRNAs regulating B7-H3 in breast cancer: the clinical impact of microRNA-29c , 2014, British Journal of Cancer.

[39] P. Moore,et al. Identification and Characterization of Angiogenesis Targets through Proteomic Profiling of Endothelial Cells in Human Cancer Tissues , 2013, PloS one.

[40] S. Rafii,et al. Preferential transfer of mitochondria from endothelial to cancer cells through tunneling nanotubes modulates chemoresistance , 2013, Journal of Translational Medicine.

[41] Yunshan Wang,et al. B7-H3 expression in ductal and lobular breast cancer and its association with IL-10. , 2013, Molecular medicine reports.

[42] A. Griffioen,et al. MicroRNAs in the tumor endothelium: novel controls on the angioregulatory switchboard. , 2010, Biochimica et biophysica acta.

[43] Nathan M Sherer,et al. Cytonemes and tunneling nanotubules in cell-cell communication and viral pathogenesis. , 2008, Trends in cell biology.

[44] Sonja Loges,et al. Recent molecular discoveries in angiogenesis and antiangiogenic therapies in cancer. , 2013, The Journal of clinical investigation.

[45] G. Collins. The next generation. , 2006, Scientific American.

[46] Hua Yu,et al. B7-H3 Associated with Tumor Progression and Epigenetic Regulatory Activity in Cutaneous Melanoma , 2013, The Journal of investigative dermatology.

[47] M. Neil,et al. Structurally Distinct Membrane Nanotubes between Human Macrophages Support Long-Distance Vesicular Traffic or Surfing of Bacteria1 , 2006, The Journal of Immunology.

[48] B. Fabry,et al. Breakdown of the Endothelial Barrier Function in Tumor Cell Transmigration , 2007, Biophysical journal.

[49] S. Anand,et al. MicroRNA-132–mediated loss of p120RasGAP activates the endothelium to facilitate pathological angiogenesis , 2010, Nature Medicine.

[50] H. Gerdes,et al. Intercellular transfer mediated by tunneling nanotubes. , 2008, Current opinion in cell biology.

[51] Qing Zhou,et al. MicroRNA-29b promotes high-fat diet-stimulated endothelial permeability and apoptosis in apoE knock-out mice by down-regulating MT1 expression. , 2014, International journal of cardiology.

[52] H. Gerdes,et al. The art of cellular communication: tunneling nanotubes bridge the divide , 2008, Histochemistry and Cell Biology.

[53] S. Seaman,et al. Genes that distinguish physiological and pathological angiogenesis. , 2007, Cancer cell.

[54] T. Kuwana,et al. Nanotubular Highways for Intercellular Organelle Transport , 2004 .

[55] Guanqing Ou,et al. Tissue mechanics modulate microRNA-dependent PTEN expression to regulate malignant progression , 2014, Nature Medicine.

[56] B. Zetter,et al. Angiogenesis and tumor metastasis. , 1998, Annual review of medicine.

[57] Weiying Zhou,et al. Cancer-secreted miR-105 destroys vascular endothelial barriers to promote metastasis. , 2014, Cancer cell.

[58] Qiong Shao,et al. MicroRNA miR-21 overexpression in human breast cancer is associated with advanced clinical stage, lymph node metastasis and patient poor prognosis. , 2008, RNA.

[59] J. Lötvall,et al. Exosome-mediated transfer of mRNAs and microRNAs is a novel mechanism of genetic exchange between cells , 2007, Nature Cell Biology.

[60] Pengyuan Yang,et al. Microenvironmental regulation of cancer metastasis by miRNAs. , 2014, Trends in cell biology.

[61] Hong Wu,et al. Expression of microRNA-150 targeting vascular endothelial growth factor-A is downregulated under hypoxia during liver regeneration. , 2013, Molecular medicine reports.

[62] J. Howard,et al. Flexural rigidity of microtubules and actin filaments measured from thermal fluctuations in shape , 1993, The Journal of cell biology.

[63] P. Francis,et al. Strategies for the discovery and development of therapies for metastatic breast cancer , 2012, Nature Reviews Drug Discovery.

[64] Gema Moreno-Bueno,et al. Melanoma exosomes educate bone marrow progenitor cells toward a pro-metastatic phenotype through MET , 2012, Nature Medicine.

[65] Scott A Gerber,et al. Dicer-dependent endothelial microRNAs are necessary for postnatal angiogenesis , 2008, Proceedings of the National Academy of Sciences.

[66] Z. Werb,et al. GATA3 suppresses metastasis and modulates the tumour microenvironment by regulating microRNA-29b expression , 2013, Nature Cell Biology.

[67] Giuseppe Rainaldi,et al. miRNAs Regulate miRNAs: Coordinated Transcriptional and Post-Transcriptional Regulation , 2006, Cell cycle.

[68] Jayanta Debnath,et al. Modelling glandular epithelial cancers in three-dimensional cultures , 2005, Nature Reviews Cancer.

[69] R M Hochmuth,et al. Micropipette suction for measuring piconewton forces of adhesion and tether formation from neutrophil membranes. , 1996, Biophysical journal.

[70] Jun Ma,et al. miR‐34c Regulates the Permeability of Blood–Tumor Barrier via MAZ‐Mediated Expression Changes of ZO‐1, Occludin, and Claudin‐5 , 2015, Journal of cellular physiology.