EGFR-mediated stimulation of sodium/glucose cotransport promotes survival of irradiated human A549 lung adenocarcinoma cells

被引：39

作者：

Huber, Stephan M. ^{[1
]}

Misovic, Milan ^{[1
]}

Mayer, Claus ^{[2
]}

Rodemann, Hans-Peter ^{[2
]}

Dittmann, Klaus ^{[2
]}

机构：

[1] Univ Tubingen, Dept Radiat Oncol, D-72076 Tubingen, Germany

[2] Univ Tubingen, Div Radiobiol & Mol Environm Res, D-72076 Tubingen, Germany

来源：

RADIOTHERAPY AND ONCOLOGY | 2012年 / 103卷 / 03期

关键词：

Patch-clamp; Current-clamp; H-3 glucose uptake; Colony formation; A549 cell line; FaDu cell line; Phlorizin; Erlotinib; SGLT; GROWTH-FACTOR RECEPTOR; INTESTINAL EPITHELIAL-CELLS; IONIZING-RADIATION; TUMOR-CELLS; GLUCOSE TRANSPORTERS; INDUCED APOPTOSIS; CANCER-CELLS; EXPRESSION; ACTIVATION; CARCINOMA;

D O I：

10.1016/j.radonc.2012.03.008

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Background and purpose: Solid tumor cells may adapt to an ischemic microenvironment by upregulation of sodium/glucose cotransport (SGLT) in the plasma membrane which supplies the tumor cell with glucose even at very low extracellular glucose concentration. Since SGLT activity has been shown to depend on the epithelial growth factor receptor (EGFR) and EGFR reportedly is activated by ionizing radiation, we tested for irradiation-induced SGLT activity. Materials and methods: A549 lung adenocarcinoma and FaDu head and neck squamous cancer cells were irradiated with 0 and 4 Gy X-ray and electrogenic SGLT transport activity was recorded by patch clamp current clamp in the presence and absence of extracellular glucose (5 mM), the SGLT inhibitor phlorizin (500 mu M), and the inhibitor of the EGFR tyrosine kinase activity erlotinib (1 mu M). In addition, the effect of phlorizin and erlotinib on glucose uptake and clonogenic survival was tested in irradiated and control cells by tracer flux and colony formation assays, respectively. Results: Irradiated A549 cells exhibited a significantly lower membrane potential 3 h after irradiation than the control cells. Phlorizin, erlotinib or removal of extracellular glucose, hyperpolarized the irradiated A549 cells to a significantly higher extent than the control cells. Similarly, but less pronounced, glucose removal hyperpolarized irradiated FaDu cells. In addition, irradiated A549 cells exhibited a highly increased H-3-glucose uptake which was sensitive to phlorizin. Finally, phlorizin radiosensitized the A549 and FaDu cells as evident from the colony formation assays. Conclusions: Taken together, these data suggest an irradiation-stimulated and EGFR-mediated increase in SGLT-generated glucose uptake which is required for the survival of the genotoxically stressed tumor cells. (C) 2012 Elsevier Ireland Ltd. All rights reserved. Radiotherapy and Oncology 103 (2012) 373-379

引用

页码：373 / 379

页数：7

共 38 条

[21] Glucose handling by the kidney [J].

Mather, Amanda ;

Pollock, Carol .

KIDNEY INTERNATIONAL, 2011, 79 :S1-S6

[22] Selection of radioresistant tumor cells and presence of ALDH1 activity in vitro [J].

Mihatsch, Julia ;

Toulany, Mahmoud ;

Bareiss, Petra M. ;

Grimm, Sabrina ;

Lengerke, Claudia ;

Kehlbach, Rainer ;

Rodemann, H. Peter .

RADIOTHERAPY AND ONCOLOGY, 2011, 99 (03) :300-306

[23] In tumor cells regulation of DNA double strand break repair through EGF receptor involves both NHEJ and HR and is independent of p53 and K-Ras status [J].

Myllynen, Laura ;

Rieckmann, Thorsten ;

Dahm-Daphi, Jochen ;

Kasten-Pisula, Ulla ;

Petersen, Cordula ;

Dikomey, Ekkehard ;

Kriegs, Matte .

RADIOTHERAPY AND ONCOLOGY, 2011, 101 (01) :147-151

[24]

NELSON JAS, 1993, ANTICANCER RES, V13, P2287

[25] Enhanced response to C225 of A431 tumor xenografts growing in irradiated tumor bed [J].

Riesterer, Oliver ;

Mason, Kathryn A. ;

Raju, Uma ;

Yang, Qiuan ;

Wang, Li ;

Hittelman, Walter N. ;

Ang, K. Kian ;

Milas, Luka .

RADIOTHERAPY AND ONCOLOGY, 2009, 92 (03) :383-387

[26] The Na+/glucose cotransporters: from genes to therapy [J].

Sabino-Silva, R. ;

Mori, R. C. ;

David-Silva, A. ;

Okamoto, M. M. ;

Freitas, H. S. ;

Machado, U. F. .

BRAZILIAN JOURNAL OF MEDICAL AND BIOLOGICAL RESEARCH, 2010, 43 (11) :1019-1026

[27] Mechanism of lapatinib-mediated radiosensitization of breast cancer cells is primarily by inhibition of the Raf > MEK > ERK mitogen-activated protein kinase cascade and radiosensitization of lapatinib-resistant cells restored by direct inhibition of MEK [J].

Sambade, Maria J. ;

Camp, J. Terese ;

Kimple, Randall J. ;

Sartor, Carolyn I. ;

Shields, Janiel M. .

RADIOTHERAPY AND ONCOLOGY, 2009, 93 (03) :639-644

[28] Epithelial-to-mesenchymal transition and c-myc expression are the determinants of cetuximab-induced enhancement of squamous cell carcinoma radioresponse [J].

Skvortsova, Ira ;

Skyortsov, Sergej ;

Raju, Uma ;

Stasyk, Taras ;

Riesterer, Oliver ;

Schottdorf, Eva-Maria ;

Popper, Bela-Andre ;

Schiestl, Bernhard ;

Eichberger, Paul ;

Debbage, Paul ;

Neher, Andreas ;

Bonn, Guenther K. ;

Huber, Lukas A. ;

Milas, Luka ;

Lukas, Peter .

RADIOTHERAPY AND ONCOLOGY, 2010, 96 (01) :108-115

[29] Ionizing radiation induces migration of glioblastoma cells by activating BK K+ channels [J].

Steinle, Marc ;

Palme, Daniela ;

Misovic, Milan ;

Rudner, Justine ;

Dittmann, Klaus ;

Lukowski, Robert ;

Ruth, Peter ;

Huber, Stephan M. .

RADIOTHERAPY AND ONCOLOGY, 2011, 101 (01) :122-126

[30] The deletion mutant EGFRvIII significantly contributes to stress resistance typical for the tumour microenvironment [J].

Theys, Jan ;

Jutten, Barry ;

Dubois, Ludwig ;

Rouschop, Kasper M. A. ;

Chiu, Roland K. ;

Li, Younan ;

Paesmans, Kim ;

Lambin, Philippe ;

Lammering, Guido ;

Wouters, Bradly G. .

RADIOTHERAPY AND ONCOLOGY, 2009, 92 (03) :399-404

← 1 2 3 4 →