Circulating tumour cells demonstrate an altered response to hypoxia and an aggressive phenotype

被引：100

作者：

Ameri, K. ^{[1
]}

Luong, R. ^{[2
]}

Zhang, H. ^{[1
]}

Powell, A. A. ^{[1
]}

Montgomery, K. D. ^{[3
]}

Espinosa, I. ^{[3
]}

Bouley, D. M. ^{[2
]}

Harris, A. L. ^{[4
,5
]}

Jeffrey, S. S. ^{[1
]}

机构：

[1] Stanford Univ, Sch Med, Dept Surg, Stanford, CA 94305 USA

[2] Stanford Univ, Sch Med, Dept Comparat Med, Stanford, CA 94305 USA

[3] Stanford Univ, Sch Med, Dept Pathol, Stanford, CA 94305 USA

[4] Univ Oxford, Dept Med Oncol, Oxford, England

[5] Univ Oxford, Mol Oncol Lab, Weatherall Inst Mol Med, Oxford, England

来源：

BRITISH JOURNAL OF CANCER | 2010年 / 102卷 / 03期

基金：

美国国家卫生研究院;

关键词：

hypoxia; anoxia; circulating tumour cells; metastasis; xenograft; ACTIVATING TRANSCRIPTION FACTOR-4; UNFOLDED PROTEIN RESPONSE; BREAST-CANCER CELLS; ASPARAGINE SYNTHETASE; DRUG-RESISTANCE; LYSYL OXIDASE; SOLID TUMORS; EXPRESSION; GENE; STRESS;

D O I：

10.1038/sj.bjc.6605491

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

BACKGROUND: Tumours contain hypoxic regions that select for an aggressive cell phenotype; tumour hypoxia induces metastasis- associated genes. Treatment refractory patients with metastatic cancer show increased numbers of circulating tumour cells (CTCs), which are also associated with disease progression. The aim of this study was to examine the as yet unknown relationship between hypoxia and CTCs. METHODS: We generated human MDA-MB-231 orthotopic xenografts and, using a new technology, isolated viable human CTCs from murine blood. The CTCs and parental MDA-MB-231 cells were incubated at 21 and 0.2% (hypoxia) oxygen, respectively. Colony formation was assayed and levels of hypoxia-and anoxia-inducible factors were measured. Xenografts generated from CTCs and parental cells were compared. RESULTS: MDA-MB-231 xenografts used to generate CTCs were hypoxic, expressing hypoxia factors: hypoxia-inducible factor1 alpha (HIF1 alpha) and glucose transporter protein type 1 (GLUT1), and anoxia-induced factors: activating transcription factor 3 and 4 (ATF3 and ATF4). Parental MDA-MB-231 cells induced ATF3 in hypoxia, whereas CTCs expressed it constitutively. Asparagine synthetase (ASNS) expression was also higher in CTCs. Hypoxia induced ATF4 and the HIF1 alpha target gene apelin in CTCs, but not in parental cells. Hypoxia induced lower levels of carbonic anhydrase IX (CAIX), GLUT1 and BCL2/adenovirus E1B 19-KD protein-interacting protein 3 (BNIP3) proteins in CTCs than in parental cells, supporting an altered hypoxia response. In chronic hypoxia, CTCs demonstrated greater colony formation than parental cells. Xenografts generated from CTCs were larger and heavier, and metastasised faster than MDA-MB-231 xenografts. CONCLUSION: CTCs show an altered hypoxia response and an enhanced aggressive phenotype in vitro and in vivo. British Journal of Cancer (2010) 102, 561-569. doi:10.1038/sj.bjc.6605491 www.bjcancer.com Published online 5 January 2010 (C) 2010 Cancer Research UK

引用

页码：561 / 569

页数：9

共 41 条

[1] GLUT-1 and CAIX as intrinsic markers of hypoxia in carcinoma of the cervix: Relationship to pimonidazole binding [J].

Airley, RE ;

Loncaster, J ;

Raleigh, JA ;

Harris, AL ;

Davidson, SE ;

Hunter, RD ;

West, CML ;

Stratford, IJ .

INTERNATIONAL JOURNAL OF CANCER, 2003, 104 (01) :85-91

[2] Induction of activating transcription factor 3 by anoxia is independent of p53 and the hypoxic HIF signalling pathway [J].

Ameri, K. ;

Hammond, E. M. ;

Culmsee, C. ;

Raida, M. ;

Katschinski, D. M. ;

Wenger, R. H. ;

Wagner, E. ;

Davis, R. J. ;

Hai, T. ;

Denko, N. ;

Harris, A. L. .

ONCOGENE, 2007, 26 (02) :284-289

[3] Anoxic induction of ATF-4 through HIF-1-independent pathways of protein stabilization in human cancer cells [J].

Ameri, K ;

Lewis, CE ;

Raida, M ;

Sowter, H ;

Hai, TW ;

Harris, AL .

BLOOD, 2004, 103 (05) :1876-1882

[4] Activating transcription factor 4 [J].

Ameri, Kurosh ;

Harris, Adrian L. .

INTERNATIONAL JOURNAL OF BIOCHEMISTRY & CELL BIOLOGY, 2008, 40 (01) :14-21

[5] Activating transcription factor 4 is translationally regulated by hypoxic stress [J].

Blais, JD ;

Filipenko, V ;

Bi, MX ;

Harding, HP ;

Ron, D ;

Koumenis, C ;

Wouters, BG ;

Bell, JC .

MOLECULAR AND CELLULAR BIOLOGY, 2004, 24 (17) :7469-7482

[6] The Lysyl Oxidase Inhibitor, β-Aminopropionitrile, Diminishes the Metastatic Colonization Potential of Circulating Breast Cancer Cells [J].

Bondareva, Alla ;

Downey, Charlene M. ;

Ayres, Fabio ;

Liu, Wei ;

Boyd, Steven K. ;

Hallgrimsson, Benedikt ;

Jirik, Frank R. .

PLOS ONE, 2009, 4 (05)

[7]

Brizel DM, 1996, CANCER RES, V56, P941

[8] Enhanced expression of asparagine synthetase under glucose-deprived conditions protects pancreatic cancer cells from apoptosis induced by glucose deprivation and cisplatin [J].

Cui, Hongyan ;

Darmanin, Stephanie ;

Natsuisaka, Mitsuteru ;

Kondo, Takeshi ;

Asaka, Masahiro ;

Shindoh, Masanobu ;

Higashino, Fumihiro ;

Hamuro, Junji ;

Okada, Futoshi ;

Kobayashi, Masataka ;

Nakagawa, Koji ;

Koide, Hideyuki ;

Kobayashi, Masanobu .

CANCER RESEARCH, 2007, 67 (07) :3345-3355

[9] Circulating Tumor Cells in Metastatic Breast Cancer From Prognostic Stratification to Modification of the Staging System? [J].

Dawood, Shaheenah ;

Broglio, Kristine ;

Valero, Vicente ;

Reuben, James ;

Handy, Beverly ;

Islam, Rabiul ;

Jackson, Summer ;

Hortobagyi, Gabriel N. ;

Fritsche, Herbert ;

Cristofanilli, Massimo .

CANCER, 2008, 113 (09) :2422-2430

[10] Monitoring serial changes in circulating human breast cancer cells in murine xenograft models [J].

Eliane, Jean-Pierre ;

Repollet, Madeline ;

Luker, Kathryn E. ;

Brown, Martha ;

Rae, James M. ;

Dontu, Gabriela ;

Schott, Anne F. ;

Wicha, Max ;

Doyle, Gerald V. ;

Hayes, Daniel F. ;

Luker, Gary D. .

CANCER RESEARCH, 2008, 68 (14) :5529-5532

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