Hypoxia induces adhesion molecules on cancer cells: A missing link between Warburg effect and induction of selectin-ligand carbohydrates

Koike, Tetsufumi; Kimura, Naoko; Miyazaki, Kohji; Yabuta, Tetsuro; Kumamoto, Kensuke; Takenoshita, Seiichi; Chen, Jian; Kobayashi, Masanobu; Hosokawa, Masuo; Taniguchi, Akiyoshi; Kojima, Tetsuhito; Ishida, Nobuhiro; Kawakita, Masao; Yamamoto, Harumi; Takematsu, Hiromu; Suzuki, Akemi; Kozutsumi, Yasunori; Kanangi, Reiji

doi:10.1073/pnas.0402088101

Cited by 209 publications

(162 citation statements)

References 45 publications

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“…A similar phenomenon was found by labelling with HPA and anti-sLe a and no difference in the binding pattern or intensity was detected between both strains of mice. This observation leads to the idea that the expression of selectin ligands of the tumour cells can vary and that their selectin-binding pattern is probably influenced by the different environment of the tumour cells, as already shown by Koike et al (2004), who showed that oxygenation influences selectin-binding site expression. This difference in expression pattern is explained by the observation that transformational effects, such as growth to high cell densities, 2D vs 3D growth or hypoxia, lead to an alteration of carbohydrate patterns between tumour cells grown in vivo and in vitro (Warren et al, 1978).…”

Section: Discussionmentioning

confidence: 93%

E-/P-selectins and colon carcinoma metastasis: first in vivo evidence for their crucial role in a clinically relevant model of spontaneous metastasis formation in the lung

et al. 2009

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BACKGROUND: Interactions of endothelial selectins with tumour cell glycoconjugates have been shown to have a major role in tumour cell dissemination in previous experiments. However, experiments validating this observation were limited in value, as 'metastases' in these experiments were artificially induced by i.v. injection rather than developed spontaneously as in true metastases. METHODS: Endothelial (E) and platelet (P)-selectin-deficient severe combined immunodeficient (scid) mice were generated and human HT 29 colon cancer cells were subcutaneously inoculated in these mice and in wild-type scid mice. Tumour growth, spontaneous metastasis formation in the lung and adherence of HT29 cells to E-and P-selectin under flow were determined. RESULTS: The number of metastases decreased by 84% in E-and P-selectin-deficient scid mice, compared with wild-type scid mice. The remaining 16% metastases in the E-and P-selectin-deficient scid mice grew within the pulmonary artery and not in the alveolar septae as they did in wild-type scid mice. Flow experiments indicate that tumour cells roll and tether on an E-and P-selectin matrix similar to leukocytes; however, firm adhesion is mainly mediated in E-selectin. CONCLUSION: Our results indicate that E-and P-selectins have a crucial role in spontaneous metastasis formation. As the human HT 29 colon cancer cells are positive for the lectin Helix pomatia agglutinin (HPA), which identified the metastatic phenotype in earlier clinical studies, these results are of particular clinical relevance.

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Section: Discussionmentioning

confidence: 93%

E-/P-selectins and colon carcinoma metastasis: first in vivo evidence for their crucial role in a clinically relevant model of spontaneous metastasis formation in the lung

et al. 2009

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“…The increment in the expression of these genes occurs in the advanced stage of cancers and partially explains the enhancement of sialyl Lewis a/x in advanced cancers. 39) The enhanced expression of sialyl Lewis a/x , however, is already obvious in the early stages of cancers.…”

Section: Induction Of Sialyl Lewis A/x Expression In Epithelial Cancementioning

confidence: 99%

Carbohydrate‐mediated cell adhesion in cancer metastasis and angiogenesis

et al. 2004

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“…[6][7][8][9] To assess vascularization, frozen sections of the tumors were stained for the mouse CD31, an endothelial cell determinant and examined by fluorescence microscopy. As shown in Figure 5a, there is a striking difference between the tumors with respect to the vascular architecture and microvessel density.…”

Section: Vasculogenesis Is Inhibited In Fut1-derived Tumorsmentioning

confidence: 99%

“…3 Besides, several lines of evidence from selectin-deficient mice studies pointed out the contribution of selectins in facilitating tumor growth and progression. 4,5 In particular, E-selectin and its sLex-containing glycoconjugate ligands have been shown to be involved in the essential events of tumor angiogenesis, [6][7][8][9] including the fact that coinjection of tumor cells expressing high level of sLe x together with endothelial cells constitutively expressing E-selectin, has been found to promote tumor angiogenesis and growth. 10 We have recently succeeded in strongly blocking the expression of sLex on digestive cancer cells by a virally-delivered a(1,2)-fucosyltransferase-I (FUT1).…”

mentioning

confidence: 99%

Introducing α(1,2)‐linked fucose into hepatocarcinoma cells inhibits vasculogenesis and tumor growth

Mathieu¹,

Gerolami²,

Luis³

et al. 2007

Intl Journal of Cancer

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The glycoantigen sialyl-Lewis x (sLex) and its isomer sialy-Lewis a (sLea) are frequently associated with advanced states of cancer and metastasis. In a previous work, we have shown that hepatocarcinoma cells (HCC) HepG2 interact with the endothelial Eselectin exclusively through sLe x oligosaccharides, the synthesis of which could be completely prevented by the a(1,2)-fucosyltransferase-I (FUT1), thus resulting in a strong inhibition of adhesion and rolling on activated endothelial cells. The purpose of the present study was to evaluate the impact of inhibiting sLex synthesis and the subsequent E-selectin adhesion, on HCC tumor growth in nude mice. Four weeks after subcutaneous transplantation of cells, no FUT1-derived tumor could be detected, whereas 75% of control animals developed large size tumor nodules. Between the 4th and the 8th week postinoculation, 33% tumors arose from FUT1-transduced cells but showed a slow growth (nodule volumes less than 500 mm 3 ), while more than 50% of control tumors reached volumes between 1,500 and 3,000 mm 3 . Several parameters were examined, including cell division and proliferation, apoptosis, adhesion to extracellular matrix components and angiogenesis/vasculogenesis. We provide evidence that among all, vasculogenesis was the most clearly affected by FUT1 expression, suggesting that tumor angiomorphogenesis may, at least partly, depend on Eselectin-mediated interaction between HCC and endothelial cells, the inhibition of which remarkably retards tumor growth. ' 2007 Wiley-Liss, Inc.Key words: a(1,2)-fucosyltransferase-I; E-selectin; sialyl-Lewis; antitumor; vasculogenesisThe sialyl-Lewis antigens (sLex and sLea) are blood grouprelated antigens naturally expressed on leukocytes to initiate leukocyte-endothelium interaction mediated by the cytokine-inducible endothelial adhesion molecule E-selectin. 1,2 In addition to this physiological role in inflammation, sialyl-Lewis antigens are also considered as tumor markers expressed on many cancer cells and therefore, they are thought to be involved in metastasis by initiating tumor cell-endothelium adhesion. 3 Indeed, the expression of sialyl-Lewis antigens on carcinoma cells is frequently associated with advanced states of cancer and a statistically relevant relationship has been established between the postoperative prognosis of patients and the degree of expression of sialyl-Lewis antigens on cancer tissues. 3 Besides, several lines of evidence from selectin-deficient mice studies pointed out the contribution of selectins in facilitating tumor growth and progression. 4,5 In particular, E-selectin and its sLex-containing glycoconjugate ligands have been shown to be involved in the essential events of tumor angiogenesis, 6-9 including the fact that coinjection of tumor cells expressing high level of sLe x together with endothelial cells constitutively expressing E-selectin, has been found to promote tumor angiogenesis and growth. 10 We have recently succeeded in strongly blocking the expression of sLex on digestive cancer cells...

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Hypoxia induces adhesion molecules on cancer cells: A missing link between Warburg effect and induction of selectin-ligand carbohydrates

Cited by 209 publications

References 45 publications

E-/P-selectins and colon carcinoma metastasis: first in vivo evidence for their crucial role in a clinically relevant model of spontaneous metastasis formation in the lung

E-/P-selectins and colon carcinoma metastasis: first in vivo evidence for their crucial role in a clinically relevant model of spontaneous metastasis formation in the lung

Carbohydrate‐mediated cell adhesion in cancer metastasis and angiogenesis

Introducing α(1,2)‐linked fucose into hepatocarcinoma cells inhibits vasculogenesis and tumor growth

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