369 research outputs found

    Advanced head and neck cancer treatment: A basic step forward

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    Multidrug resistance in solid tumours

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    Introduction: Most cancers show heterogeneity of response to chemotherapy. This may be due in part to the differential expression of drug resistance proteins and the molecular targets of the drugs concerned. Methods: An ex vivo ATP-based Tumour Chemosensitivity Assay (ATP-TCA), immunohistochemistry and quantitative RT-PCR have been used to assess the chemosensitivity and resistance of a variety of solid tumours and cell lines. Results: (a) Melanoma cell lines showed higher chemosensitivity than tumour-derived cells, partially reversible by lowering the serum concentration, and hence the proliferation rate of the cells. (b) Studies of retinoblastoma samples confirmed that this malignancy is susceptible to cytotoxic drugs of all types, though multidrug resistance may occur in some cases. (c) The ATP-TCA was used to study the activity of high-dose doxorubicin in combination with other cytotoxic agents in ovarian adenocarcinoma samples. The combination of liposomal doxorubicin + vinorelbine was selected for further development. (d) A number of experimental drugs with varying sensitivity to resistance mechanisms were also assessed. One drug, XR5944, has entered phase I/II clinical trials during the course of this project, and the data have provided clinical indications. (e) An inhibitor of multi-drug resistance, tariquidar, has been tested in combination with doxorubicin, vinorelbine or paclitaxel, and has been shown to reverse this resistance. (f) Molecular studies have determined the expression of topoisomerases and drug transporters in tumour cells before and after exposure to chemotherapeutic agents. P-gp expression has been found to be a determinant of sensitivity to a certain number of drugs. Conclusion: The results suggest that drug resistance contributes to heterogeneity of chemosensitivity in many solid tumour types, as well as other mechanisms. Reversal of such resistance may benefit a subset of patients undergoing chemotherapy

    Cancer of unknown primary: challenges and progress in clinical management

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    Distant metastases are the main cause of cancer-related deaths in patients with advanced tumors. A standard diagnostic workup usually contains the identification of the tissue-of-origin of metastatic tumors, although under certain circumstances, it remains elusive. This disease setting is defined as cancer of unknown primary (CUP). Accounting for approximately 3–5% of all cancer diagnoses, CUPs are characterized by an aggressive clinical behavior and represent a real therapeutic challenge. The lack of determination of a tissue of origin precludes CUP patients from specific evidence-based therapeutic options or access to clinical trial, which significantly impacts their life expectancy. In the era of precision medicine, it is essential to characterize CUP molecular features, including the expression profile of non-coding RNAs, to improve our understanding of CUP biology and identify novel therapeutic strategies. This review article sheds light on this enigmatic disease by summarizing the current knowledge on CUPs focusing on recent discoveries and emerging diagnostic strategies
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