Differential expression and responsiveness of chemokine receptors (CXCR1–3) by human microvascular endothelial cells and umbilical vein endothelial cells

Salcedo, Rosalba; Resau, James H.; Halverson, David; Hudson, Eric A.; Dambach, Michael; Powell, Douglas; Wasserman, Ken; Oppenheim, Joost J.

doi:10.1096/fj.99-0963com

Cited by 236 publications

(182 citation statements)

References 29 publications

(38 reference statements)

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“…This possibility is raised by the recently reported capacity of human IP -10 for inhibiting endothelial cell growth, although the expression of the IP-10 receptor CXCR3 by normal and transformed endothelial cells is still a matter of controversy. 27,51,52 H5V cell cultures failed to express CXCR3 and were not sensitive to the MVMpmediated production of IP-10 (present work and Ref. [27 ]).…”

Section: Discussionsupporting

confidence: 50%

Suppression of metastatic hemangiosarcoma by a parvovirus MVMp vector transducing the IP-10 chemokine into immunocompetent mice

et al. 2002

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We have previously shown that the growth of human tumor xenografts in immunodeficient mice can be efficiently suppressed upon infection with the autonomous parvovirus H -1 or with cytokine -transducing derivatives thereof. To further evaluate the benefits of implementing parvoviruses in cancer gene therapy, we have created a new recombinant vector, MVMp / IP -10, transducing the immunoactive, antiangiogenic chemokine IP -10, and used this virus to treat syngeneic tumors grown in immunocompetent mice. Intratumoral / intraperitoneal administration of only 3Â10 7 replication units of MVMp / IP -10 per animal strongly inhibited the progression of established H5V cell -induced vascular tumors, a highly malignant mouse model for human cavernous hemangioma and Kaposi's sarcoma. Retardation of recurrent tumor growth and suppression of life -threatening metastatic dissemination to internal organs were accompanied by a striking delay in hemangioma -associated mortality. Parental MVMp did not have a significant effect under these conditions up to the dose of 10 10 infectious units / animal, but had strong antihemangiosarcoma activity when used to infect H5V cells ex vivo prior to implantation. In all cases, virus therapy was very well tolerated. Virus -induced suppression of hemangiosarcoma was dependent on host T cells and associated with intratumoral persistence of IFN -expressing cytotoxic lymphocytes, and led to the reduced expression of hepatic plasminogen activator inhibitor -1 ( PAI -1 ), a metastasis -linked marker. This proof of principle study demonstrates that MVMp / IP -10 can aid the treatment of vascular tumors and that autonomous parvovirus -based vectors can be considered potent tools for cancer gene therapy purposes.

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Section: Discussionsupporting

confidence: 50%

Suppression of metastatic hemangiosarcoma by a parvovirus MVMp vector transducing the IP-10 chemokine into immunocompetent mice

et al. 2002

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“…The role of each of these receptors in IL-8-mediated activity remains controversial. Previous studies have shown that the angiogenic effects of IL-8 in human microvascular endothelial cells and NSCLC were mediated by CXCR2 (Addison et al, 2000;Salcedo et al, 2000;Heidemann et al, 2003). The chemotactic response of melanoma cells to IL-8 was mediated by CXCR1 (Ramjeesingh et al, 2003), and the mitogenic activity of IL-8 was mediated by both CXCR1 and CXCR2 in colon cancer (Li et al, 2001), but only by CXCR1 in monocytes (Browning et al, 2000).…”

Section: Discussionmentioning

confidence: 95%

Interleukin-8/CXCL8 is a growth factor for human lung cancer cells

et al. 2004

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Interleukin-8/CXCL8 (IL-8) is a chemokine and angiogenic factor. Recently, IL-8 was identified as an autocrine growth factor in several human cancers. Here, we investigated the expression and function of IL-8 in lung cancer cells. The expressions of IL-8 and its receptors, CXCR1 and CXCR2, were examined in a panel of non-small cell lung cancer (NSCLC) and small cell lung cancer (SCLC) cell lines. Using reverse transcription -polymerase chain reaction (RT -PCR) and enzyme-linked immunosorbent assay, we found that all NSCLC cell lines tested produced modest or high levels of IL-8 (up to 51 ng ml À1 10 6 cells À1 ). Expression of CXCR1 and CXCR2 was found by RT -PCR and flow cytometry in two out of three cell lines. In contrast, SCLC cell lines produced very low or undetectable levels of IL-8, but expressed CXCR1 and CXCR2. We next investigated whether IL-8 could act as an autocrine growth factor in two NSCLC cell lines (H460 and MOR/P) expressing both IL-8 and its receptors. We found that cell proliferation was attenuated by anti-IL-8 neutralising antibody to 71 and 76% in H460 and MOR/P, respectively (Po0.05). Exogenous IL-8 significantly stimulated cell proliferation in four SCLC cell lines tested in a dose-dependent fashion. Cell proliferation was increased by between 18% (Po0.05) and 37% (Po0.05). Stimulation of cell proliferation by IL-8 was also demonstrated by analysis of proliferating cell nuclear antigen expression and cell cycle in H69 cells. Furthermore, we investigated which receptor(s) mediated the mitogenic function of IL-8 in lung cancer cells. We found that cell proliferation was significantly reduced by anti-CXCR1 antibody but not by anti-CXCR2 antibody. In conclusion, IL-8 can act as an autocrine and/or paracrine growth factor for lung cancer cells, and the mitogenic function of IL-8 in lung cancer is mediated mainly by CXCR1 receptor.

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“…4 IL-8 is expressed in tumor cells and the IL-8 receptors CXCR1 and CXCR2, which are also receptors for the chemokines MIP-2 and GRO␣, are largely expressed in neutrophils. 47 Although expression of CXCR2 has also been reported in endothelial cells, 48,49 evidence has clearly shown that neutrophils are necessary mediators of the angiogenic response induced by CXCR2 agonists in vivo. 50 In wound-healing studies, angiogenesis begins immediately after injury and peaks after 7 days.…”

Section: Discussionmentioning

confidence: 99%

Transient inflammatory response induced by apoptotic cells is an important mediator of melanoma cell engraftment and growth

Correa

Machado

Carneiro

et al. 2004

Intl Journal of Cancer

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The current model for cancer development outlines a multistep process during which a cell acquires multiple genetic mutations. 1 However, several lines of investigation suggest that concomitant changes also occur in the surrounding tissue, with important consequences in the induction, selection and expansion of neoplastic cells. 2-4 Specific host factors available both locally, such as the stroma and surrounding normal cells, and distally, via humoral or diffusible factors, can provide the necessary information to create a permissive environment for malignant cell growth. 5,6 In particular, ECM composition and growth factor activity in the stroma can enhance the tumorigenicity of subsequently injected tumor cell lines. 7 Additionally, many malignancies can be initiated by infection, 8 -10 suggesting that cancer may arise in areas of inflammation as part of the normal host response. For instance, solid human tumors are often infiltrated by host immune and inflammatory cells. 11 Whereas increased levels of leukocyte infiltration into primary tumors are usually a good prognostic sign, 12 the presence of inflammatory cell infiltrates has been correlated with cytokine and growth factor production, which may provide a favorable microenvironment for neoplastic proliferation. [13][14][15][16] Clearance of apoptotic cells by phagocytes plays a significant role in the resolution of inflammation, 17 and although the lack of an inflammatory infiltrate is by definition a hallmark of death by apoptosis, several lines of investigation have challenged this concept. Indeed, apoptotic cells can evoke an inflammatory response depending on how apoptosis is initiated, in what cell type it occurs and whether or not particular cofactors are present. 18 -21 Considering that the nature of the microenvironment is one of several factors involved in the failure of tumor cells to proliferate, we tested whether apoptotic cells present in the host tissue environment could promote the growth of tumor cells in vivo. Results showed that (i) the presence of apoptotic cells in the tumor microenvironment positively modulates tumor take when the number of tumor cells alone is insufficient to produce tumors, (ii) injection of apoptotic cells induces an inflammatory response with an intense recruitment of neutrophils and macrophages and (iii) inflammatory cells recruited by apoptotic cells may be an important factor in promoting tumor engraftment when suboptimal concentrations of tumor cells are used. Taken together, our results provide new insights for the mechanisms underlying the microenvironment helper effect, with potential clinical implications for cancer therapy. Material and methods Cell culture, proliferation assay and reagentsThe murine melanocyte cell line melan-a (50th passage), 22 a kind gift of Dr. M. Rabinovitch (Discipline of Parasitology, Universidade Federal de São Paulo), was cultured in RPMI (pH 6.9) supplemented with 5% FCS and 200 nM 12-o-tetradecanoyl PMA (Sigma, St. Louis, MO). Tumor cell lines derived from melan-a (Tm1 and...

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Differential expression and responsiveness of chemokine receptors (CXCR1–3) by human microvascular endothelial cells and umbilical vein endothelial cells

Cited by 236 publications

References 29 publications

Suppression of metastatic hemangiosarcoma by a parvovirus MVMp vector transducing the IP-10 chemokine into immunocompetent mice

Suppression of metastatic hemangiosarcoma by a parvovirus MVMp vector transducing the IP-10 chemokine into immunocompetent mice

Interleukin-8/CXCL8 is a growth factor for human lung cancer cells

Transient inflammatory response induced by apoptotic cells is an important mediator of melanoma cell engraftment and growth

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