Tamoxifen Resistance in Breast Cancer

Dorssers, Lambert C. J.; Flier, S. van der; Brinkman, Arend; Agthoven, Ton van; Veldscholte, Jos; Berns, Els M.J.J.; Klijn, Jan G.M.; Beex, L.V.A.M.; Foekens, John A.

doi:10.2165/00003495-200161120-00004

Cited by 105 publications

(63 citation statements)

References 128 publications

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“…BCAR1, which encodes p130CAS, is upregulated in breast tumours resistant to tamoxifen 121,122 . Consistently, the over-expression of p130CAS in breast cancer cells induces proliferative signals that are not sensitive to treatment with either tamoxifen or oestrogen receptor antagonist fulvestrant 121,123 . Although it has been reported that a possible mechanism through which p130CAS induces tamoxifen resistance is its binding to BCAR3/AND34, a putative GEF for RALA, RAP, and RRAS GTPases 124 , the exact mechanism by which p130CAS and BCAR3 induce anti-oestrogen resistance remains unclear.…”

Section: Clinical Implications Of Integrin Adaptorsmentioning

confidence: 67%

Integrin signalling adaptors: not only figurants in the cancer story

et al. 2010

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Current evidence highlights the ability of adaptor (or scaffold) proteins to create signalling platforms that drive cellular transformation upon integrin-dependent adhesion and growth factor receptor activation. The understanding of the biological effects regulated by these adaptors in tumours might be crucial for the identification of novel targets and the development of innovative therapeutic strategies for human cancer. In this review we will discuss the relevance of adaptor proteins in signalling originating from integrin-mediated cell-extracellular matrix (ECM) adhesion and growth factor stimulation within the context of cell transformation and tumour progression.Herein, we will specifically underline the contribution of p130CAS, NEDD9, CRK, and the IPP complex (ILK, PINCH and PARVIN) to cancer, along with the more recently identified p140CAP.

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Section: Clinical Implications Of Integrin Adaptorsmentioning

confidence: 67%

Integrin signalling adaptors: not only figurants in the cancer story

et al. 2010

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“…In addition, in the absence of oxygen, P450 reductase interacts with anthracyclines, leading to cleavage of the anthracycline glycosidic bond and producing a molecule with no antitumour activity (Pan et al, 1981). In the CMF-treated group, most patients also received TAM concomitantly, which could have counterbalanced the cytotoxic resistance induced by hypoxia at least in part since the drug induces apoptosis that is ER mediated (Dorssers et al, 2001) and may not be influenced by tumour oxygenation. It has been demonstrated that the oxygenation status of human tumours is independent of clinical tumour size stage and grade (Wouters et al, 2002).…”

Section: Discussionmentioning

confidence: 99%

Pretreatment haemoglobin levels significantly predict the tumour response to primary chemotherapy in human breast cancer

et al. 2003

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The purpose of this study was to evaluate whether tumour response to primary chemotherapy in human breast cancer is influenced by baseline haemoglobin (Hb) status. A total of 157 patients with T2-4, N0-1 M0 breast cancer were treated with chemotherapy consisting of either the CMF regimen þ tamoxifen (the first 76 cases) or the single-agent epirubicin (the subsequent 81) before definitive surgery. In total, 144 patients were fully assessable. Ki67, p53, bcl-2, c-erbB2, steroid hormone receptor, and microvessel density were evaluated immunohistochemically in tumour specimens obtained before chemotherapy and at surgery. Tumour shrinkage 450% occurred in 72.1% of patients. Responding patients had higher baseline Hb levels and red blood cell counts than nonresponders (Po0.01 and o0.003, respectively). The distribution of disease response according to increasing cutoffs of baseline Hb status showed that from 12.5 mg l À1 onwards, patients with Hb levels above the cutoff obtained a greater response rate than those with lower Hb values. The difference attained the statistical significance at 12.5 (76.1 vs 59.5%, Po0.05) and 13.0 g/dl À1 (81.0 vs 57.6%, Po0.002) cutoffs, respectively. The predictive role of Hb levels was maintained in multivariate analysis after adjustment for clinical and biological characteristics and treatment regimen. Patients with baseline Hb levels p13 g dl À1 showed a lower treatmentinduced reduction in Ki67 expression (Po0.04) and a higher Ki67 expression at postoperative evaluation (Po0.02) than their counterparts. In conclusion, low Hb levels may negatively influence the response rate of chemotherapy in breast cancer patients. Inhibition of antiproliferative activity could be a possible mechanism.

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“…These observations highlight the fact that different mechanisms for TR are likely and may involve adaptive changes as well as 'antiestrogen resistance genes'. Perhaps breast tumors in carriers of so called 'antiestrogen resistance genes' (Dorssers et al 2001) 274 www.endocrinology.org have a lesser ability to modulate MAPK and aromatase as adaptive processes than those with 'adaptive TR'.…”

Section: Discussionmentioning

confidence: 99%

New approaches to the understanding of tamoxifen action and resistance.

Lm¹,

Zheng²,

W³

et al. 2003

Endocrine-Related Cancer

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Tamoxifen (TAM) provides an effective agent for treatment of hormone-dependent breast cancer but resistance uniformly ensues upon continued use. Additional studies are required to define more precisely the mechanisms involved in development of resistance. We conducted systematic experimental and clinical studies based on the hypothesis that tumors exposed to TAM long-term may develop resistance by becoming hypersensitive to its estrogenic effects. These investigations uncovered new features of the TAM resistance (TR) phenomenon and identified possible means for its prevention and/or elimination. Initially we confirmed that TR may be divided into two subtypes, primary and acquired resistance, and that these differ by certain important characteristics including the level of the possible involvement of adaptive and genetic components. Then we distinguished at least three consequent stages of this phenomenon: stage I when TAM behaves as an antiestrogen, stage II with development of increased sensitivity to the agonistic (pro-estrogenic) properties of TAM and stage III with an adaptive increase in sensitivity to estradiol (E 2 ). During this evolutionary process, as shown in vitro, MAP kinase (MAPK) and aromatase activities increase. The time frame of the increase in MAPK activity as a rule outpaces the increase in aromatase activity during the course of the development of TR. This may occur as a response to estrogen deprivation or interruption of the process of estrogen signaling and can be one of the promoting factors of increased aromatase activation. On the other hand, the chronology of these events indicates that changes in the MAPK cascade can be more important for the early steps of the development and maintenance of the TR state. Changes in local estrogen production/sensitivity to E 2 are perhaps essential for the later steps of this phenomenon.We have explored the use of a growth factor-blocking agent to abrogate the adaptive changes in sensitivity. Farnesylthiosalicylic acid (FTS), an inhibitor of GTP-Ras binding to its membrane acceptor site, reduces the increase in the number of MCF-7 cells induced by long-term TAM treatment. It also decreases MAPK activity in TAM-treated MCF-7 cells and in established TR cell lines. Alone or in combination with letrozole (presumably, through the influence on MAPK pathway) FTS exerts moderate inhibitory effects on aromatase activity in estrogen-deprived or estrogen-exposed MCF-7 cells. Taken together, our observations suggest that FTS is a 'candidate drug' for the treatment of TR. Both the adaptive and genetic types of resistance may be amenable to this approach. Our studies underline the possible importance of starting the treatment/prevention of TR early on. From our clinical studies using immunohistochemistry, there is a rather strong rationale to include as a predisposing factor in the development of TR the increase in MAPK and aromatase activities in human primary breast tumors.In summary, data obtained during the course of this project may be considered as e...

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Tamoxifen Resistance in Breast Cancer

Cited by 105 publications

References 128 publications

Integrin signalling adaptors: not only figurants in the cancer story

Integrin signalling adaptors: not only figurants in the cancer story

Pretreatment haemoglobin levels significantly predict the tumour response to primary chemotherapy in human breast cancer

New approaches to the understanding of tamoxifen action and resistance.

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