Reduction in drug-induced DNA double-strand breaks associated with β1 integrin–mediated adhesion correlates with drug resistance in U937 cells

Hazlehurst, Lori A.; Valkov, Nikola; Wisner, Lee; Storey, Jonathan A.; Boulware, David; Sullivan, Daniel M.; Dalton, William S.

doi:10.1182/blood.v98.6.1897

Cited by 119 publications

(81 citation statements)

References 29 publications

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“…30 Furthermore, integrin-mediated adhesion in hemapoeitic cancer cells reduced DNA double-strand breaks and apoptosis caused by chemotherapeutic agents such as mitoxantrone and etoposide. 31 This primarily a5b1-mediated reduction in DNA damage correlated with decreased topoisomerase-II enzymatic activity. However, the a5b1 integrin is not found in SCLC cells and is reduced in other carcinomas.…”

Section: Discussionmentioning

confidence: 95%

ECM overrides DNA damage-induced cell cycle arrest and apoptosis in small-cell lung cancer cells through β1 integrin-dependent activation of PI3-kinase

et al. 2006

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The emergence of resistance to chemotherapy remains a principle problem in the treatment of small-cell lung cancer (SCLC). We demonstrate that extracellular matrix (ECM) activates phosphatidyl inositol 3-kinase (PI3-kinase) signaling in SCLC cells and prevents etoposide-induced caspase-3 activation and subsequent apoptosis in a b1 integrin/PI3-kinase-dependent manner. Crucially we show that etoposide and radiation induce G2/M cell cycle arrest in SCLC cells prior to apoptosis and that ECM prevents this by overriding the upregulation of p21 Cip1/WAF1 and p27 Kip1 and the downregulation of cyclins E, A and B. These effects are abrogated by pharmacological and genetic inhibition of PI3-kinase signaling. Importantly we show that chemoprotection is not mediated by altered SCLC cell proliferation or DNA repair. Thus, ECM via b1 integrin-mediated PI3-kinase activation overrides treatment-induced cell cycle arrest and apoptosis, allowing SCLC cells to survive with persistent DNA damage, providing a model to account for the emergence of acquired drug resistance.

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Section: Discussionmentioning

confidence: 95%

ECM overrides DNA damage-induced cell cycle arrest and apoptosis in small-cell lung cancer cells through β1 integrin-dependent activation of PI3-kinase

et al. 2006

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“…The examination of various transformed cell lines and primary cell strains has raised evidence for chemo-and radioprotective effects of specific ECM proteins (Vlodavsky et al, 1980;Fuks et al, 1992;Rose et al, 1999;Hazlehurst et al, 2001;Cordes et al, 2002Cordes et al, in press (a), 2003Cordes and Meineke, 2003;. As reported (Bouterfa et al, 1999;Oz et al, 2000;Mahesparan et al, 2003), FN, laminin, collagen-IV and -I, decorin, tenascin and vitronectin are ECM proteins produced and secreted by cells of malignant tumours of glial origin in vitro and in vivo.…”

Section: Discussionmentioning

confidence: 99%

“…Each heterodimer consists of one a-and one b-chain. Integrins are involved in the regulation of several cell functions such as differentiation, cell cycle progression, apoptotic pathways and DNA repair mechanisms (Adams and Watt, 1990;Assoian, 1997;Hazlehurst et al, 2001). To date avb3 (Brooks et al, 1996;Rooprai et al, 1999), a5b1 (Ohnishi et al, 1998) and other b1-integrin combinations (Paulus et al, 1993;Chintala et al, 1996;Friedlander et al, 1996) have been identified to participate in cell migration and invasion.…”

mentioning

confidence: 99%

Irradiation differentially affects substratum-dependent survival, adhesion, and invasion of glioblastoma cell lines

Cordes¹,

Hansmeier²,

Beinke³

et al. 2003

Br J Cancer

100

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Effects of ionising radiation on extracellular matrix (ECM)-modulated cell survival and on adhesion and invasion are not well understood. In particular, the aggressiveness of glioblastoma multiforme has been associated with tumour cell invasion into adjacent normal brain tissue. To examine these effects in more depth, four human glioblastoma cell lines (A-172, U-138, were irradiated on fibronectin (FN), Matrigel, BSA or polystyrene. Major findings of this study include a significantly increased survival of irradiated A-172 but not of irradiated U-138, LN-229, and LN-18 cells on FN or Matrigel compared to cells irradiated on polystyrene or BSA. Irradiation induced a dose-dependent increase in functional b1-and b3-integrins in all four glioma cell lines. This integrin induction caused improved cell adhesion to FN or Matrigel. In contrast to U-138, LN-229 and LN-18 cells, irradiation strongly impaired A-172 cell invasion. Invasion of all cell lines was inhibited by anti-integrin antibodies, the disintegrin echistatin and the MMP-2/-9 inhibitor III. Additionally, b1-and b3-integrins modulated basal and radiation-altered gelatinolytic activity of MMP-2. Tested glioblastoma cell lines showed a differential cellular susceptibility to FN or Matrigel which affected the cellular radiosensitivity. Three out of four glioma cell lines demonstrated a combination of a substratum-independent survival after irradiation and an invasive potential which was not affected by irradiation. b1-and b3-integrins were identified to play a substantial, regulatory role in survival, adhesion, invasion and MMP-2 activity. Detailed insights into radioresistance and invasion processes might offer new therapeutic strategies to enhance cell killing of lethal high-grade astrocytoma.

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“…18,19,24,[32][33][34] MM is a latent disease of the BM, where the tumor cell phenotype likely reflects a combination of multiple interactions including cell-cell, cell-ECM, and cellgrowth factor. In this study, we demonstrate that the presence of BMSCs during treatment of H929 or RPMI 8226 cells with mitoxantrone significantly reduces apoptosis in myeloma cell lines.…”

Section: Discussionmentioning

confidence: 99%

Bone marrow stromal-derived soluble factors and direct cell contact contribute to de novo drug resistance of myeloma cells by distinct mechanisms

2003

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The tumor microenvironment plays a critical role in determining the fate of tumor cells. We have previously reported that adhesion of human myeloma and leukemia cell lines to the extracellular matrix protein, fibronectin, confers a multidrugresistant phenotype. Mechanisms associated with this cell adhesion-mediated drug resistance are drug-type specific. In the present study, we examined the influence of bone marrow stromal cells (BMSCs) on myeloma cell response to the topoisomerase II inhibitor, mitoxantrone. Apoptosis was inhibited by more than 50% when cells were adhered to BMSCs as compared to myeloma cells maintained in suspension. To investigate the mechanisms contributing to the resistance of myeloma cells in contact with BMSCs, we examined the protective effects of BMSCs under four separate conditions:(1) direct cell contact; (2) BMSCs conditioned medium; (3) medium conditioned by coculturing myeloma cells in direct contact with BMSCs; and (4) medium conditioned by coculturing myeloma cells and BMSCs without direct physical contact. Conditioned medium from BMSCs alone was not sufficient to protect myeloma cells from drug-induced apoptosis; however, soluble factors produced during the myeloma-BMSCs interaction decreased the sensitivity of myeloma cells to mitoxantrone, suggesting a dynamic interaction between myeloma cells and BMSCs. We also found that myeloma cells in direct contact with BMSCs underwent growth arrest, whereas soluble factors produced by myeloma cells-BMSCs coincubation stimulated the proliferation of myeloma cells. These data show that both cell-cell adhesion of BMSCs with myeloma cells and soluble factors induced by this cell-cell interaction are involved in the protection of myeloma cells from mitoxantrone-induced apoptosis; however, the mechanisms contributing to the drug resistance are different.

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Reduction in drug-induced DNA double-strand breaks associated with β1 integrin–mediated adhesion correlates with drug resistance in U937 cells

Cited by 119 publications

References 29 publications

ECM overrides DNA damage-induced cell cycle arrest and apoptosis in small-cell lung cancer cells through β1 integrin-dependent activation of PI3-kinase

ECM overrides DNA damage-induced cell cycle arrest and apoptosis in small-cell lung cancer cells through β1 integrin-dependent activation of PI3-kinase

Irradiation differentially affects substratum-dependent survival, adhesion, and invasion of glioblastoma cell lines

Bone marrow stromal-derived soluble factors and direct cell contact contribute to de novo drug resistance of myeloma cells by distinct mechanisms

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