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51. The prognostic value of the immunohistochemical expression of phosphorylated RB and p16 proteins in association with cyclin D1 and the p53 pathway in a large cohort of patients with breast cancer treated with taxane-based adjuvant chemotherapy

Author

Gavressea, T. Kalogeras, K.T. Koliou, G.-A. Zagouri, F. Lazaridis, G. Gogas, H. Tsigaridas, K. Koutras, A. Petraki, K. Markopoulos, C. Pazarli, E. Aravantinos, G. Papadimitriou, C. Papakostas, P. Koufopoulos, N. Karanikiotis, C. Chrisafi, S. Kalofonos, H.P. Pectasides, D. Fountzilas, G. Pavlakis, K.

Abstract

Background: The retinoblastoma (RB) gene is a tumor-suppressor gene that plays a central role in regulating the cell cycle. Inactivation of this gene is involved in breast cancer. Patients and Methods: A total of 827 patients with breast cancer treated with taxane-based adjuvant chemotherapy were included in the study. Protein expression of RB, phosphorylated RB (pRB), p16, cyclin D1 and p53 was evaluated by immunohistochemistry. Results: Neither of the retinoblastoma markers (RB and pRB) reached statistical significance in terms of their association with disease-free or overall survival. Nevertheless, when clustering analysis was performed, patients with tumors featuring low levels of p16, cyclin D1 and p53 with concomitantly high levels of pRB had reduced risk for relapse (Wald's p=0.015). Conclusion: The p53-mediated sensitivity of breast cancer cells to chemotherapeutic agents appears to be driven mostly by pRB. Using agents that enhance RB phosphorylation might possibly increase the chemosensitivity of breast cancer cells.

Published
2017

52. Clinical evidence supporting genomic tests in early breast cancer: Do all genomic tests provide the same information?

Author

Markopoulos, C. van de Velde, C. Zarca, D. Ozmen, V. and Masetti, R.

Abstract

Breast cancer (BC) has historically been treated as a single disease entity; however, in the last decade, insights into its molecular heterogeneity have underpinned the development/commercialisation of several genomic tools whose goal is to guide patient management in early BC. These include the Oncotype DX Breast Recurrence ScoreTM assay, MammaPrint, Prosigna, and EndoPredict. Although these assays are similar in that they are all multigene assays reflecting risk of recurrence, they differ substantially in the technological platform used to measure gene expression; the number and identity of genes assessed; the patient populations used for development and validation; and the level of evidence supporting clinical utility. They also differ in the amount of evidence demonstrating their impact on treatment decisions and cost effectiveness in different countries. This review discusses these 4 assays, highlighting the clinical evidence that supports each of them, while focussing on the Recurrence Score assay. This assay has the greatest body of evidence supporting its clinical utility and decision impact/effectiveness, and currently is the only one validated as a predictor of response to adjuvant chemotherapy in hormone -receptor positive early BC patients treated with endocrine therapy and to be included as such in international/national BC treatment guidelines. The review also discusses ongoing prospective trials investigating the 4 assays, recent outcome studies, as well as analyses comparing different assays on the same tumour blocks. (C) 2016 Elsevier Ltd, BASO - The Association for Cancer Surgery, and the European Society of Surgical Oncology. All rights reserved.

Published
2017

54. Effect of radiotherapy after mastectomy and axillary surgery on 10-year recurrence and 20-year breast cancer mortality: meta-analysis of individual patient data for 8135 women in 22 randomised trials

Author

Mcgale, P., Taylor, C., Correa, C., Cutter, D., Duane, F., Ewertz, M., Gray, R., Mannu, G., Peto, R., Whelan, T., Wang, Y., Wang, Z., Darby, S., Albain, K., Anderson, S., Arriagada, R., Barlow, W., Bergh, J., Bergsten Nordström, E., Bliss, J., Burrett, J. A., Buyse, M., Cameron, D., Carrasco, E., Clarke, M., Coleman, R., Coates, A., Collins, R., Costantino, J., Cuzick, J., Davidson, N., Davies, C., Davies, K., Delmestri, A., Di Leo, A., Dowsett, M., Elphinstone, P., Evans, V., Forbes, J., Gelber, R., Gettins, L., Geyer, C., Gianni, L., Gnant, M., Goldhirsch, A., Godwin, J., Gregory, C., Hayes, D., Hill, C., Ingle, J., Jakesz, R., James, S., Janni, W., Kaufmann, M., Kerr, A., Liu, H., Mackinnon, E., Martín, M., Mchugh, T., Morris, P., Norton, L., Ohashi, Y., Paik, S., Pan, H. C., Perez, E., Piccart, M., Pierce, L., Pritchard, K., Pruneri, G., Raina, V., Ravdin, P., Robertson, J., Rutgers, E., Shao, Y. F., Sparano, J., Swain, S., Valagussa, P., Viale, G., Von Minckwitz, G., Winer, E., Wiang, X., Wood, Abe O, W., Abe, R, Enomoto, K, Kikuchi, K, Koyama, H, Masuda, H, Nomura, Y, Ohashi, Y, Sakai, K, Sugimachi, K, Toi, M, Tominaga, T, Uchino, J, Yoshida, M, Haybittle, Jl, Leonard, Cf, Calais, G, Geraud, P, Collett, V, Davies, C, Delmestri, A, Sayer, J, Harvey, Vj, Holdaway, Im, Kay, Rg, Mason, Bh, Forbes, Jf, Wilcken, N, Bartsch, R, Dubsky, P, Fesl, C, Fohler, H, Gnant, M, Greil, R, Jakesz, R, Lang, A, Luschin-Ebengreuth, G, Marth, C, Mlineritsch, B, Samonigg, H, Singer, Cf, Steger, Gg, Stöger, H, Canney, P, Yosef, Hm, Focan, C, Peek, U, Oates, Gd, Powell, J, Durand, M, Mauriac, L, Di Leo, A, Dolci, S, Larsimont, D, Nogaret, Jm, Philippson, C, Piccart, Mj, Masood, Mb, Parker, D, Price, Jj, Lindsay, Ma, Mackey, J, Martin, M, Hupperets, Ps, Bates, T, Blamey, Rw, Chetty, U, Ellis, Io, Mallon, E, Morgan, Da, Patnick, J, Pinder, S, Olivotto, I, Ragaz, J, Berry, D, Broadwater, G, Cirrincione, C, Muss, H, Norton, L, Weiss, Rb, Abu-Zahra, Ht, Portnoj, Sm, Bowden, S, Brookes, C, Dunn, J, Fernando, I, Lee, M, Poole, C, Rea, D, Spooner, D, Barrett-Lee, Pj, Mansel, Re, Monypenny, Ij, Gordon, Nh, Davis, Hl, Cuzick, J, Lehingue, Y, Romestaing, P, Dubois, Jb, Delozier, T, Griffon, B, Mace Lesech, J, Brain, E, de La Lande, B, Mouret-Fourme, E, Mustacchi, G, Petruzelka, L, Pribylova, O, Owen, Jr, Harbeck, N, Jänicke, F, Meisner, C, Schmitt, M, Thomssen, C, Meier, P, Shan, Y, Shao, Yf, Wang, X, Zhao, Db, Chen, Zm, Pan, Hc, Howell, A, Swindell, R, Burrett, Ja, Clarke, M, Collins, R, Correa, C, Cutter, D, Darby, S, Davies, K, Elphinstone, P, Evans, V, Gettins, L, Godwin, J, Gray, R, Gregory, C, Hermans, D, Hicks, C, James, S, Kerr, A, Liu, H, Mackinnon, E, Lay, M, Mcgale, P, Mchugh, T, Morris, P, Peto, R, Taylor, C, Wang, Y, Albano, J, de Oliveira CF, Gervásio, H, Gordilho, J, Ejlertsen, B, Jensen, Mb, Johansen, H, Mouridsen, H, Palshof, T, Gelman, Rs, Harris, Jr, Hayes, D, Henderson, C, Shapiro, Cl, Winer, E, Christiansen, P, Ewertz, M, Møller, S, Mouridsen, Ht, Trampisch, Hj, Dalesio, O, de Vries EG, Rodenhuis, S, van Tinteren, H, Comis, Rl, Davidson, Ne, Robert, N, Sledge, G, Solin, Lj, Sparano, Ja, Tormey, Dc, Wood, W, Cameron, D, Dixon, Jm, Forrest, P, Jack, W, Kunkler, I, Rossbach, J, Klijn, Jg, Treurniet-Donker, Ad, van Putten WL, Rotmensz, N, Veronesi, U, Viale, G, Bartelink, H, Bijker, N, Bogaerts, J, Cardoso, F, Cufer, T, Julien, Jp, Rutgers, E, van de Velde CJ, Cunningham, Mp, Huovinen, R, Joensuu, H, Costa, A, Bonadonna, G, Gianni, L, Valagussa, P, Goldstein, Lj, Bonneterre, J, Fargeot, P, Fumoleau, P, Kerbrat, P, Luporsi, E, Namer, M, Eiermann, W, Hilfrich, J, Jonat, W, Kaufmann, M, Kreienberg, R, Schumacher, M, Bastert, G, Rauschecker, H, Sauer, R, Sauerbrei, W, Schauer, A, Blohmer, Ju, Costa, Sd, Eidtmann, H, Gerber, B, Jackisch, C, Loibl, S, von Minckwitz, G, de Schryver, A, Vakaet, L, Belfiglio, M, Nicolucci, A, Pellegrini, F, Pirozzoli, Mc, Sacco, M, Valentini, M, Mcardle, Cs, Smith, Dc, Stallard, S, Dent, Dm, Gudgeon, Ca, Hacking, A, Murray, E, Panieri, E, Werner, Id, Carrasco, E, Segui, Ma, Galligioni, E, Lopez, M, Erazo, A, Medina, Jy, Horiguchi, J, Takei, H, Fentiman, Is, Hayward, Jl, Rubens, Rd, Skilton, D, Scheurlen, H, Sohn, Hc, Untch, M, Dafni, U, Markopoulos, C, Fountzilas, G, Mavroudis, D, Klefstrom, P, Blomqvist, C, Saarto, T, Gallen, M, Tinterri, C, Margreiter, R, de Lafontan, B, Mihura, J, Roché, H, Asselain, B, Salmon, Rj, Vilcoq, Jr, André, F, Arriagada, R, Delaloge, S, Hill, C, Koscielny, S, Michiels, S, Rubino, C, A'Hern, R, Bliss, J, Ellis, P, Kilburn, L, Yarnold, Jr, Benraadt, J, Kooi, M, van de Velde AO, van Dongen JA, Vermorken, Jb, Castiglione, M, Coates, A, Colleoni, M, Collins, J, Forbes, J, Gelber, Rd, Goldhirsch, A, Lindtner, J, Price, Kn, Regan, Mm, Rudenstam, Cm, Senn, Hj, Thuerlimann, B, Bliss, Jm, Chilvers, Ce, Coombes, Rc, Hall, E, Marty, M, Buyse, M, Possinger, K, Schmid, P, Wallwiener, D, Foster, L, George, Wd, Stewart, Hj, Stroner, P, Borovik, R, Hayat, H, Inbar, Mj, Peretz, T, Robinson, E, Bruzzi, P, Del Mastro, L, Pronzato, P, Sertoli, Mr, Venturini, M, Camerini, T, De Palo, G, Di Mauro MG, Formelli, F, Amadori, D, Martoni, A, Pannuti, F, Camisa, R, Cocconi, G, Colozza, A, Passalacqua, R, Aogi, K, Takashima, S, Abe, O, Ikeda, T, Inokuchi, K, Sawa, K, Sonoo, H, Korzeniowski, S, Skolyszewski, J, Ogawa, M, Yamashita, J, Bastiaannet, E, van de Water, W, van Nes JG, Christiaens, R, Neven, P, Paridaens, R, Van den Bogaert, W, Braun, S, Martin, P, Romain, S, Janauer, M, Seifert, M, Sevelda, P, Zielinski, Cc, Hakes, T, Hudis, Ca, Wittes, R, Giokas, G, Kondylis, D, Lissaios, B, de la Huerta, R, Sainz, Mg, Altemus, R, Camphausen, K, Cowan, K, Danforth, D, Lichter, A, Lippman, M, O'Shaughnessy, J, Pierce, Lj, Steinberg, S, Venzon, D, Zujewski, Ja, D'Amico, C, Lioce, M, Paradiso, A, Chapman, Ja, Gelmon, K, Goss, Pe, Levine, Mn, Meyer, R, Parulekar, W, Pater, Jl, Pritchard, Ki, Shepherd, Le, Tu, D, Whelan, T, Ohno, S, Anderson, S, Bass, G, Brown, A, Bryant, J, Costantino, J, Dignam, J, Fisher, B, Geyer, C, Mamounas, Ep, Paik, S, Redmond, C, Swain, S, Wickerham, L, Wolmark, N, Baum, M, Jackson, Im, Palmer, Mk, Perez, E, Ingle, Jn, Suman, Vj, Bengtsson, No, Emdin, S, Jonsson, H, Lythgoe, Jp, Kissin, M, Erikstein, B, Hannisdal, E, Jacobsen, Ab, Varhaug, Je, Gundersen, S, Hauer-Jensen, M, Høst, H, Nissen-Meyer, R, Reinertsen, K, Mitchell, Ak, Robertson, Jf, Ueo, H, Di Palma, M, Mathé, G, Misset, Jl, Levine, M, Morimoto, K, Takatsuka, Y, Crossley, E, Harris, A, Talbot, D, Taylor, M, di Blasio, B, Ivanov, V, Paltuev, R, Semiglazov, V, Brockschmidt, J, Cooper, Mr, Falkson, Ci, Dowsett, M, Makris, A, Parton, M, Pennert, K, Powles, Tj, Smith, Ie, Gazet, Jc, Browne, L, Graham, P, Corcoran, N, Businico, A, Deshpande, N, di Martino, L, Douglas, P, Lindtner, A, Notter, G, Bryant, Aj, Ewing, Gh, Firth, La, Krushen-Kosloski, Jl, Anderson, H, Killander, F, Malmström, P, Rydén, L, Arnesson, Lg, Carstensen, J, Dufmats, M, Fohlin, H, Nordenskjöld, B, Söderberg, M, Carpenter, Jt, Murray, N, Royle, Gt, Simmonds, Pd, Albain, K, Barlow, W, Crowley, J, Gralow, J, Hortobagyi, G, Livingston, R, Martino, S, Osborne, Ck, Ravdin, Pm, Adolfsson, J, Bergh, J, Bondesson, T, Celebioglu, F, Dahlberg, K, Fornander, T, Fredriksson, I, Frisell, J, Göransson, E, Iiristo, M, Johansson, U, Lenner, E, Löfgren, L, Nikolaidis, P, Perbeck, L, Rotstein, S, Sandelin, K, Skoog, L, Svane, G, af Trampe, E, Wadström, C, Janni, W, Maibach, R, Thürlimann, B, Hakama, M, Holli, K, Isola, J, Rouhento, K, Saaristo, R, Brenner, H, Hercbergs, A, Yoshimoto, M, Paterson, Ah, Fyles, A, Meakin, Jw, Panzarella, T, Bahi, J, Reid, M, Spittle, M, Bishop, H, Bundred, Nj, Forsyth, S, Pinder, Se, Sestak, I, Deutsch, Gp, Kwong, Dl, Pai, Vr, Senanayake, F, Martin, Al, Boccardo, F, Rubagotti, A, Hackshaw, A, Houghton, J, Ledermann, J, Monson, K, Tobias, Js, Carlomagno, C, De Laurentiis, M, De Placido, S, Williams, L, Broglio, K, Buzdar, Au, Hsu, L, Love, Rr, Ahlgren, J, Garmo, H, Holmberg, L, Liljegren, G, Lindman, H, Wärnberg, F, Asmar, L, Jones, Se, Gluz, O, Liedtke, C, Nitz, U, Litton, A, Wallgren, A, Karlsson, P, Linderholm, Bk, Chlebowski, Rt, Caffier, H., McGale, P, Taylor, C, Correa, C, Cutter, D, Duane, F, Ewertz, M, Gray, R, Mannu, G, Peto, R, Whelan, T, Wang, Y, Wang, Z, Darby, S, Biomedische Technologie, RS: GROW - Oncology, RS: GROW - R3 - Innovative Cancer Diagnostics & Therapy, Mcgale, P, DE LAURENTIIS, Michelino, Other departments, CCA -Cancer Center Amsterdam, and Radiotherapy

Subjects
medicine.medical_specialty, medicine.medical_treatment, Breast Neoplasms, Rate ratio, Lower risk, Systemic therapy, Statistical significance, Medicine, Humans, Mastectomy, Randomized Controlled Trials as Topic, business.industry, Articles, General Medicine, Surgery, Radiation therapy, Axilla, Neoplasm Recurrence, medicine.anatomical_structure, Local, Meta-analysis, Lymphatic Metastasis, Lymph Node Excision, Female, Neoplasm Recurrence, Local, business, Breast Neoplasm, Human
Abstract

BACKGROUND: Postmastectomy radiotherapy was shown in previous meta-analyses to reduce the risks of both recurrence and breast cancer mortality in all women with node-positive disease considered together. However, the benefit in women with only one to three positive lymph nodes is uncertain. We aimed to assess the effect of radiotherapy in these women after mastectomy and axillary dissection.METHODS: We did a meta-analysis of individual data for 8135 women randomly assigned to treatment groups during 1964-86 in 22 trials of radiotherapy to the chest wall and regional lymph nodes after mastectomy and axillary surgery versus the same surgery but no radiotherapy. Follow-up lasted 10 years for recurrence and to Jan 1, 2009, for mortality. Analyses were stratified by trial, individual follow-up year, age at entry, and pathological nodal status.FINDINGS: 3786 women had axillary dissection to at least level II and had zero, one to three, or four or more positive nodes. All were in trials in which radiotherapy included the chest wall, supraclavicular or axillary fossa (or both), and internal mammary chain. For 700 women with axillary dissection and no positive nodes, radiotherapy had no significant effect on locoregional recurrence (two-sided significance level [2p]>0·1), overall recurrence (rate ratio [RR], irradiated vs not, 1·06, 95% CI 0·76-1·48, 2p>0·1), or breast cancer mortality (RR 1·18, 95% CI 0·89-1·55, 2p>0·1). For 1314 women with axillary dissection and one to three positive nodes, radiotherapy reduced locoregional recurrence (2pINTERPRETATION: After mastectomy and axillary dissection, radiotherapy reduced both recurrence and breast cancer mortality in the women with one to three positive lymph nodes in these trials even when systemic therapy was given. For today's women, who in many countries are at lower risk of recurrence, absolute gains might be smaller but proportional gains might be larger because of more effective radiotherapy.FUNDING: Cancer Research UK, British Heart Foundation, UK Medical Research Council.

Published
2016
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55. Abstract P1-06-04: Simplified histological grading of breast carcinoma – potential for improved concordance and consistency in breast cancer grading?

Author

Bartlett, JMS, primary, Thomas, J, additional, Mallon, E, additional, Piper, T, additional, Bayani, J, additional, Hasenburg, A, additional, Kieback, DG, additional, Markopoulos, C, additional, Dirix, L, additional, Seynaeve, C, additional, van de Velde, CJH, additional, and Rea, DW, additional

Published
2018
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56. Abstract P1-06-02: Comparative survival analysis of multiparametric tests in the TEAM pathology study: What to do when molecular tests disagree?

Author

Bartlett, JMS, primary, Bayani, J, additional, Kornaga, E, additional, Piper, T, additional, Mallon, E, additional, Yao, CQ, additional, Boutros, PC, additional, Hasenburg, A, additional, Kieback, DG, additional, Markopoulos, C, additional, Dirix, L, additional, Seynaeve, C, additional, Can de Velde, CJH, additional, and Rea, DW, additional

Published
2018
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57. Abstract P2-09-17: Evaluation of the oncomine comprehensive assay for the identification of actionable mutations for therapeutic stratification from the TEAM pathology cohort

Author

Bayani, J, primary, Crozier, C, additional, Quintayo, MA, additional, Amemiya, Y, additional, Zhang, X, additional, Larivière, M, additional, Sadis, S, additional, Smith, JM, additional, Hasenburg, A, additional, Kieback, D, additional, Markopoulos, C, additional, Dirix, L, additional, Yaffe, M, additional, Seth, A, additional, Feilotter, H, additional, Rea, D, additional, and Bartlett, JMS, additional

Published
2018
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58. Abstract PD4-11: Copy-number and targeted sequencing analyses to identify distinct prognostic groups: Implications for patient selection to targeted therapies amongst anti-endocrine therapy resistant early breast cancers

Author

Bayani, J, primary, Kornaga, EN, additional, Crozier, C, additional, Jang, GH, additional, Kalatskaya, I, additional, Trinh, QM, additional, Yao, CQ, additional, Livingstone, J, additional, Hasenburg, A, additional, Kieback, DG, additional, Markopoulos, C, additional, Dirix, L, additional, Boutros, PC, additional, Spears, M, additional, Stein, LD, additional, Rea, D, additional, and Bartlett, JMS, additional

Published
2018
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60. Adjuvant bisphosphonates in early breast cancer: Consensus guidance for clinical practice from a European Panel

Author

Hadji, P. Coleman, R.E. Wilson, C. Powles, T.J. Clézardin, P. Aapro, M. Costa, L. Body, J.-J. Markopoulos, C. Santini, D. Diel, I. Di Leo, A. Cameron, D. Dodwell, D. Smith, I. Gnant, M. Gray, R. Harbeck, N. Thurlimann, B. Untch, M. Cortes, J. Martin, M. Albert, U.-S. Conte, P.-F. Ejlertsen, B. Bergh, J. Kaufmann, M. Holen, I.

Abstract

Bisphosphonates have been studied in randomised trials in early breast cancer to investigate their ability to prevent cancer treatment-induced bone loss (CTIBL) and reduce the risk of disease recurrence and metastasis. Treatment benefits have been reported but bisphosphonates do not currently have regulatory approval for either of these potential indications. This consensus paper provides a review of the evidence and offers guidance to breast cancer clinicians on the use of bisphosphonates in early breast cancer. Using the nominal group methodology for consensus, a systematic review of the literature was augmented by a workshop held in October 2014 for breast cancer and bone specialists to present and debate the available pre-clinical and clinical evidence for the use of adjuvant bisphosphonates. This was followed by a questionnaire to all members of the writing committee to identify areas of consensus. The panel recommended that bisphosphonates should be considered as part of routine clinical practice for the prevention of CTIBL in all patients with a T score of 18 000 patients supports clinically significant benefits of bisphosphonates on the development of bone metastases and breast cancer mortality in post-menopausal women or those receiving ovarian suppression therapy. Therefore, the panel recommends that bisphosphonates (either intravenous zoledronic acid or oral clodronate) are considered as part of the adjuvant breast cancer treatment in this population and the potential benefits and risks discussed with relevant patients. © The Author 2015. Published by Oxford University Press on behalf of the European Society for Medical Oncology. All rights reserved.

Published
2016

61. White blood cell and platelet indices as prognostic markers in patients with invasive ductal breast carcinoma

Author

Mantas, D. Kostakis, I.D. Machairas, N. Markopoulos, C.

Abstract

A growing body of evidence suggests that oncogenesis is associated with systemic inflammation. The present study investigated white blood cell and platelet indices, whose values change during the inflammatory response, in women with invasive ductal breast carcinoma. Preoperatively obtained white blood cell and platelet counts from 53 patients with early breast cancer, who developed systemic metastases over a mean follow-up period of 65 months, were analyzed and compared with those of a matching control group formed of 37 patients with the same characteristics, who remained recurrence-free during the same time period. Patients who developed distant metastasis had a significantly higher mean platelet volume and lower neutrophil count than patients who did not present with distant metastasis. Furthermore, time to distant metastasis development was longer in patients with a lower mean platelet volume, whilst patients with a lower neutrophil count had a shorter systemic disease-free time interval. However, receiver operating characteristic curve analysis demonstrated that these parameters provided moderate accuracy in predicting which patients may develop distant metastasis. No differences were detected between patient groups regarding additional parameters. Patients who developed systemic disease during a mean follow-up period of 65 months were observed to have an increased mean platelet volume and decreased neutrophil count preoperatively. These results indicate that such parameters may be of prognostic value in patients with breast cancer. Studies with a larger number of patients are required to further investigate this hypothesis. © 2016, Spandidos Publications. All rights reserved.

Published
2016

63. Incidence of inactive allele CYP2D6∗4 among Greek women suffering from hormone-sensitive breast cancer

Author

Kykalos, S. Mantas, D. Charalampoudis, P. Kouraklis, G. and Markopoulos, C.

Subjects
skin and connective tissue diseases
Abstract

Background: The incidence of CYP2D6*4 among Caucasians is estimated up to 27%, while it is present in up to 90% of all poor metabolizers within the Caucasian population. The hypothesis under question is whether the presence of one or two non-functioning (null) alleles predicts an inferior outcome in postmenopausal women with breast cancer receiving adjuvant treatment with tamoxifen. The aim of the present study is to estimate the incidence of CYP2D6*4, in the Greek population and more precisely among females suffering from breast cancer. Materials and Methods: Eighty unrelated mainland Greek female volunteers suffering from hormone-sensitive breast cancer were recruited during their primary handling or follow-up examination in order to provide samples for purification and polymerase chain reaction/restriction fragment length polymorphism (PCR-RFLP) of genomic DNA derived from buccal swabs. Results: The incidence of individuals with at least one present allele*4 within the Hellenic population was estimated to be as high as 30% (n = 24/80), with a 95% confidence interval of 20% to 40%. From the statistical point of view, it can be securely stated that incidence of *4 among Greek women is over 20%. The incidence of homozygous carriers of *4 in the present sample occurred in 8.75%, while the incidence of allele*4 haplotype occurred in 19.4% (n=160). Conclusion: Although the outcoming results for Greek women are actually in line with existing data for other European nations, it should be noted, that a routine CYP2D6 testing of women suffering from breast cancer is formally not recommended, as the clinical significance of CYP2D6 phenotype in treatment and outcome of breast cancer remains unclear.

Published
2016

64. Cornus mas L. (cornelian cherry), an important European and Asian traditional food and medicine: Ethnomedicine, phytochemistry and pharmacology for its commercial utilization in drug industry

Author

Dinda, B. Kyriakopoulos, A.M. Dinda, S. Zoumpourlis, V. Thomaidis, N.S. Velegraki, A. Markopoulos, C. Dinda, M.

Subjects
food and beverages
Abstract

Ethnopharmacological relevance Cornus mas L. (cornelian cherry) fruits have been used for centuries as traditional cuisine and folk medicine in various countries of Europe and Asia. In folk medicines, the fruits and other parts of the plant have been used for prevention and treatment of a wide range of diseases such as diabetes, diarrhea, gastrointestinal disorders, fevers, rheumatic pain, skin and urinary tract infections, kidney and liver diseases, sunstroke, among others. This review provides a systematic and constructive overview of ethnomedicinal uses, chemical constituents and pharmacological activities of this plant as well as future research need for its commercial utilization as nutraceutical food supplement and medicine. Materials and methods This review is based on available literature on ethnomedicinal uses, phytochemical, pharmacological, toxicity and clinical studies on Cornus mas L. (cornelian cherry) fruits and other organs that was collected from electronic (SciFinder, PubMed, Science Direct and ACS among others) and library searches of books and journals. Results Versatile ethnomedicinal uses of the plant in different European and Asian countries have been reported. Phytochemical investigations on different parts of this plant have resulted in the identification of 101 compounds, among which anthocyanins, flavonoids and iridoids are the predominant groups. The crude extracts of fruits and other parts of the plant and their pure isolates exhibit a broad spectrum of pharmacological activities such as anti-microbial, anti-diabetic, anti-atherosclerotic, cyto-, hepato-, neuro- and renalprotective, antiplatelet and antiglaucomic activities. Anthocyanins, flavonoids, iridoids and vitamin C are the major bioactive constituents of the fruits. Fruits are non-toxic and safe food on acute toxicity studies in rat and human models. Clinical trials in diabetic type2 and hyperlipidemic patients showed significant trends of amelioration in sugar level, insulin secretion in diabetic patients and amelioration of lipid profile, apolipoprotein status and vascular inflammation in hyperlipidemic patients. Conclusion Based on our review, Cornus mas L. (cornelian cherry) fruits and leaves can be used mainly in the treatment of diabetes, obesity, atherosclerosis, skin diseases, gastrointestinal and rheumatic problems. Some indications from ethnomedicines have been validated by pharmacological activities of the fruits and its extracts/pure isolates. The reported data reveal that the fruits are a potential source for treatment of diabetes, obesity, hyperlipidemia and gastrointestinal disorders. Unfortunately, the pharmacological studies in these areas are still insufficient to substantiate these preventive effects in confirmatory trials on the mass-scale clinical settings. Future studies on mechanisms of action, bioavailability, pharmacokinetics and adverse effects of the extracts and their bioactive constituents as well as their effective doses and long term toxic effects in humans are needed for commercial applications of these extracts/isolates in modern medicines. The available literature showed that most of the activities of the extracts are due to their constituents, anthocyanins, flavonoids and other phenolics, iridoids and vitamins for their antioxidant and other properties. © 2016 Elsevier Ireland Ltd

Published
2016

65. Effects of TP53 and PIK3CA mutations in early breast cancer: a matter of co-mutation and tumor-infiltrating lymphocytes

Author

Kotoula, V. Karavasilis, V. Zagouri, F. Kouvatseas, G. Giannoulatou, E. Gogas, H. Lakis, S. Pentheroudakis, G. Bobos, M. Papadopoulou, K. Tsolaki, E. Pectasides, D. Lazaridis, G. Koutras, A. Aravantinos, G. Christodoulou, C. Papakostas, P. Markopoulos, C. Zografos, G. Papandreou, C. Fountzilas, G.

Subjects
neoplasms
Abstract

The purpose of this study is to investigate whether the outcome of breast cancer (BC) patients treated with adjuvant chemotherapy is affected by co-mutated TP53 and PIK3CA according to stromal tumor-infiltrating lymphocytes (TILs). Paraffin tumors of all clinical subtypes from 1661 patients with operable breast cancer who were treated within 4 adjuvant trials with anthracycline–taxanes chemotherapy were informative for TP53 and PIK3CA mutation status (semiconductor sequencing genotyping) and for stromal TILs density. Disease-free survival (DFS) was examined. TP53 mutations were associated with higher (p

Published
2016

67. Adjuvant bisphosphonate treatment in early breast cancer: meta-analyses of individual patient data from randomised trials

Author

Early Breast Cancer Trialists' Collaborative Group (EBCTCG), Coleman, R, Powles, T, Paterson, A, Gnant, M, Anderson, S, Diel, I, Gralow, J, von Minckwitz, G, Moebus, V, Bergh, J, Pritchard, KI, Bliss, J, Cameron, D, Evans, V, Pan, H, Peto, R, Bradley, R, Gray, R, Bartsch, R, Dubsky, P, Fesl, C, Fohler, H, Greil, R, Jakesz, R, Lang, A, Luschin-Ebengreuth, G, Marth, C, Mlineritsch, B, Samonigg, H, Singer, CF, Steger, GG, Stoger, H, Olivotto, I, Ragaz, J, Christiansen, P, Ejlertsen, B, Ewertz, M, Jensen, M-B, Moller, S, Mouridsen, HT, Eiermann, W, Hilfrich, J, Jonat, W, Kaufmann, M, Kreienberg, R, Schumacher, M, Blohmer, JU, Costa, SD, Eidtmann, H, Gerber, B, Jackisch, C, Loibl, S, Dafni, U, Markopoulos, C, Blomqvist, C, Saarto, T, Ahn, J-H, Jung, KH, Perrone, F, Bass, G, Brown, A, Bryant, J, Costantino, J, Dignam, J, Fisher, B, Geyer, C, Mamounas, EP, Paik, S, Redmond, C, Swain, S, Wickerham, L, Wolmark, N, Perez, E, Ingle, JN, Suman, VJ, Hadji, P, A'Hern, R, Dowsett, M, Makris, A, Parton, M, Pennert, K, Powles, TJ, Smith, IE, Yarnold, JR, Clack, G, Van Poznak, C, Safra, T, Bell, R, Coleman, RE, Dodwell, D, Hinsley, S, Marshall, HC, Solomayer, E, Fehm, T, Lester, J, Winter, MC, Horsman, JM, Aft, R, Brufsky, AM, and Llombart, HA

Abstract

Background Bisphosphonates have profound effects on bone physiology, and could modify the process of metastasis. We undertook collaborative meta-analyses to clarify the risks and benefits of adjuvant bisphosphonate treatment in breast cancer. Methods We sought individual patient data from all unconfounded trials in early breast cancer that randomised between bisphosphonate and control. Primary outcomes were recurrence, distant recurrence, and breast cancer mortality. Primary subgroup investigations were site of first distant recurrence (bone or other), menopausal status (postmenopausal [combining natural and artificial] or not), and bisphosphonate class (aminobisphosphonate [eg, zoledronic acid, ibandronate, pamidronate] or other [ie, clodronate]). Intention-to-treat log-rank methods yielded bisphosphonate versus control first-event rate ratios (RRs). Findings We received data on 18 766 women (18 206 [97%] in trials of 2–5 years of bisphosphonate) with median follow-up 5·6 woman-years, 3453 first recurrences, and 2106 subsequent deaths. Overall, the reductions in recurrence (RR 0·94, 95% CI 0·87–1·01; 2p=0·08), distant recurrence (0·92, 0·85–0·99; 2p=0·03), and breast cancer mortality (0·91, 0·83–0·99; 2p=0·04) were of only borderline significance, but the reduction in bone recurrence was more definite (0·83, 0·73–0·94; 2p=0·004). Among premenopausal women, treatment had no apparent effect on any outcome, but among 11 767 postmenopausal women it produced highly significant reductions in recurrence (RR 0·86, 95% CI 0·78–0·94; 2p=0·002), distant recurrence (0·82, 0·74–0·92; 2p=0·0003), bone recurrence (0·72, 0·60–0·86; 2p=0·0002), and breast cancer mortality (0·82, 0·73–0·93; 2p=0·002). Even for bone recurrence, however, the heterogeneity of benefit was barely significant by menopausal status (2p=0·06 for trend with menopausal status) or age (2p=0·03), and it was non-significant by bisphosphonate class, treatment schedule, oestrogen receptor status, nodes, tumour grade, or concomitant chemotherapy. No differences were seen in non-breast cancer mortality. Bone fractures were reduced (RR 0·85, 95% CI 0·75–0·97; 2p=0·02). Interpretation Adjuvant bisphosphonates reduce the rate of breast cancer recurrence in the bone and improve breast cancer survival, but there is definite benefit only in women who were postmenopausal when treatment began. Funding Cancer Research UK, Medical Research Council.

Published
2015

71. Clinical evidence supporting genomic tests in early breast cancer: Do all genomic tests provide the same information?

Author

Markopoulos, C., van de Velde, C., Zarca, D., Ozmen, V., Masetti, Riccardo, Masetti R. (ORCID:0000-0002-7520-9111), Markopoulos, C., van de Velde, C., Zarca, D., Ozmen, V., Masetti, Riccardo, and Masetti R. (ORCID:0000-0002-7520-9111)

Abstract

Breast cancer (BC) has historically been treated as a single disease entity; however, in the last decade, insights into its molecular heterogeneity have underpinned the development/commercialisation of several genomic tools whose goal is to guide patient management in early BC. These include the Oncotype DX® Breast Recurrence ScoreTM assay, MammaPrint®, Prosigna®, and EndoPredict®. Although these assays are similar in that they are all multigene assays reflecting risk of recurrence, they differ substantially in the technological platform used to measure gene expression; the number and identity of genes assessed; the patient populations used for development and validation; and the level of evidence supporting clinical utility. They also differ in the amount of evidence demonstrating their impact on treatment decisions and cost effectiveness in different countries. This review discusses these 4 assays, highlighting the clinical evidence that supports each of them, while focussing on the Recurrence Score assay. This assay has the greatest body of evidence supporting its clinical utility and decision impact/effectiveness, and currently is the only one validated as a predictor of response to adjuvant chemotherapy in hormone-receptor positive early BC patients treated with endocrine therapy and to be included as such in international/national BC treatment guidelines. The review also discusses ongoing prospective trials investigating the 4 assays, recent outcome studies, as well as analyses comparing different assays on the same tumour blocks.

Published
2017

72. 117P - Multigene panel testing results for hereditary breast cancer in 1325 individuals: Implications for gene selection and considerations for guidelines

Author

Tsaousis, G.N., Tsoulos, N., Papadopoulou, E., Agiannitopoulos, K., Pepe, G., Diamantopoulos, N., Floros, T.I., Iosifidou, R., Markopoulos, C., Papazisis, K., Venizelos, V., Xepapadakis, G., Banu, E., Eniu, D.T., Stanculeanu, D.L., Ungureanu, A., Tansan, S., Tekinel, M., Yalcin, S., and Nasioulas, G.

Published
2019
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73. In-vitro simulation of luminal conditions for evaluation of performance of oral drug products: Choosing the appropriate test media

Author

Markopoulos, C. Andreas, C.J. Vertzoni, M. Dressman, J. Reppas, C.

Abstract

Background Biorelevant media for evaluation of dosage form performance in the gastrointestinal lumen were first introduced in the late 1990s. Since then, a variety of additional media have been proposed, making it now possible to simulate most regions in the gastrointestinal tract in both prandial states. However, recent work suggests that the complexity and degree of biorelevance required to predict in-vivo release varies with the drug, dosage form and dosing conditions. Objective The aim of this commentary was to establish which levels of biorelevant media are appropriate to various combinations of active pharmaceutical ingredient(s), dosage form and dosing conditions. With regard to their application, a decision tree for the selection of the appropriate biorelevant medium/media is proposed and illustrative case scenarios are provided. Additionally, media to represent the distal small intestine in both prandial states are presented. Conclusion The newly proposed levels of biorelevance and accompanying decision tree may serve as a useful tool during formulation development in order to ensure high quality, predictive performance results without unnecessary complexity of media. In future work, further specific case examples will be evolved, which will additionally address the need to take gastrointestinal passage times and type and intensity of agitation into consideration. © 2015 Elsevier B.V. All rights reserved.

Published
2015

75. Characterization of Contents of Distal Ileum and Cecum to Which Drugs/Drug Products are Exposed during Bioavailability/Bioequivalence Studies in Healthy Adults

Author

Reppas, C. Karatza, E. Goumas, C. Markopoulos, C. Vertzoni, M.

Subjects
digestive system
Abstract

Purpose: Characterize the contents of distal ileum and cecum in healthy adults under conditions simulating the bioavailability/bioequivelance studies of drug products in fasted and fed state. Methods: Twelve males participated in a two-phase crossover study. Phase I: subjects remained fasted overnight plus 4.5 h in the morning prior to colonoscopy. Phase II: subjects remained fasted overnight, consumed breakfast in the morning, and abstain from food until colonoscopy, 4.5 h after breakfast. Upon sampling, volume, pH and buffer capacity were measured; after ultracentrifugation, supernatant was physicochemically characterized and non-liquid particles diameter was measured. Results: In distal ileum, pH is ~8.1 and size of non-liquid particles is ~200 μm, regardless of dosing conditions; in fed state, liquid fraction was lower whereas osmolality and carbohydrate content were higher. In cecum, the environment was similar with previously characterized environment in the ascending colon; in fasted state, size of non-liquid particles is smaller than in distal ileum (~70 μm). Fluid composition in distal ileum is different from cecum, especially in fasted state. Conclusion: Differences in luminal environment between distal ileum and cecum may impact the performance of orally administered products which deliver drug during residence in lower intestine. Dosing conditions affect cecal environment more than in distal ileum. © 2015 Springer Science+Business Media New York.

Published
2015

77. Two-Stage Single-Compartment Models to Evaluate Dissolution in the Lower Intestine

Author

Markopoulos, C. Vertzoni, M. Symillides, M. Kesisoglou, F. Reppas, C.

Abstract

The purpose was to propose two-stage single-compartment models for evaluating dissolution characteristics in distal ileum and ascending colon, under conditions simulating the bioavailability and bioequivalence studies in fasted and fed state by using the mini-paddle and the compendial flow-through apparatus (closed-loop mode). Immediate release products of two highly dosed active pharmaceutical ingredients (APIs), sulfasalazine and L-870,810, and one mesalamine colon targeting product were used for evaluating their usefulness. Change of medium composition simulating the conditions in distal ileum (SIFileum) to a medium simulating the conditions in ascending colon in fasted state and in fed state was achieved by adding an appropriate solution in SIFileum. Data with immediate release products suggest that dissolution in lower intestine is substantially different than in upper intestine and is affected by regional pH differences > type/intensity of fluid convection > differences in concentration of other luminal components. Asacol® (400 mg/tab) was more sensitive to type/intensity of fluid convection. In all the cases, data were in line with available human data. Two-stage single-compartment models may be useful for the evaluation of dissolution in lower intestine. The impact of type/intensity of fluid convection and viscosity of media on luminal performance of other APIs and drug products requires further exploration. © 2015 Wiley Periodicals, Inc. and the American Pharmacists Association.

Published
2015

78. In vitro biorelevant models for evaluating modified release mesalamine products to forecast the effect of formulation and meal intake on drug release

Author

Andreas, C.J. Chen, Y.-C. Markopoulos, C. Reppas, C. Dressman, J.

Abstract

Aims Postprandial administration of solid oral dosage forms greatly changes the dissolution environment compared to fasted state administration. The aims of this study were to investigate and forecast the effect of co-administration of a meal on drug release for delayed and/or extended release mesalamine formulations as well as design of in vitro tests to distinguish among formulations in a biorelevant way. Methods Five different mesalamine formulations (Asacol® 400 mg, Mezavant® 1200 mg, Pentasa® 500 mg and Salofalk® in the 250 mg and 500 mg strengths) were investigated with biorelevant dissolution methods using the USP apparatus III and USP apparatus IV (open loop mode) under both fasted and fed state conditions, as well as with the dissolution methods described in pharmacopeia for delayed and extended release mesalamine products. Results Using the biorelevant experimental conditions proposed in this study, changes in release in the proximal gut due to meal intake are forecast to be minimal for Asacol®, Mezavant®, Pentasa® and Salofalk® 500 mg, while for Salofalk® 250 mg release was predicted to occur much earlier under fed state conditions. The USP apparatus III generally tended to result in faster dissolution rates and forecast more pronounced food effects for Salofalk® 250 mg than the USP apparatus IV. The biorelevant dissolution gradients were also able to reflect the in vivo behavior of the formulations. Conclusions In vitro biorelevant models can be useful in the comparison of the release behavior from different delayed and extended release mesalamine formulations as well as forecasting effects of concomitant meal intake on drug release. © 2015 Elsevier B.V. All rights reserved.

Published
2015

79. Time dependence of biomarkers: non-proportional effects of immunohistochemical panels predicting relapse risk in early breast cancer

Author

Stephen, J., Murray, G., Cameron, D.A., Thomas, J., Kunkler, I.H., Jack, W., Kerr, G.R., Piper, T., Brookes, C.L., Rea, D.W., Velde, C.J.H. van de, Hasenburg, A., Markopoulos, C., Dirix, L., Seynaeve, C., Bartlett, J.M.S., and Medical Oncology

Subjects
Risk, biomarkers, Breast Neoplasms, relapse risk, time dependency, Immunohistochemistry, Cohort Studies, breast cancer, SDG 3 - Good Health and Well-being, Clinical Study, Biomarkers, Tumor, Humans, Female, Neoplasm Recurrence, Local
Abstract

Background:We investigated the impact of follow-up duration to determine whether two immunohistochemical prognostic panels, IHC4 and Mammostrat, provide information on the risk of early or late distant recurrence using the Edinburgh Breast Conservation Series and the Tamoxifen vs Exemestane Adjuvant Multinational (TEAM) trial.Methods:The multivariable fractional polynomial time (MFPT) algorithm was used to determine which variables had possible non-proportional effects. The performance of the scores was assessed at various lengths of follow-up and Cox regression modelling was performed over the intervals of 0-5 years and >5 years.Results:We observed a strong time dependence of both the IHC4 and Mammostrat scores, with their effects decreasing over time. In the first 5 years of follow-up only, the addition of both scores to clinical factors provided statistically significant information (P

Published
2014
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80. Measurement of the semileptonic branching ratio of charm hadrons produced in ${\rm Z}^0\to{\rm c\bar c}$ decays

Author

Abbiendi, G., Ackerstaff, K., Alexander, G., Allison, John, Altekamp, N., Anderson, K.J., Anderson, S., Arcelli, S., Asai, S., Ashby, S.F., Axen, D., Azuelos, G., Ball, A.H., Barberio, E., Barlow, Roger J., Bartoldus, R., Batley, J.R., Baumann, S., Bechtluft, J., Behnke, T., Bell, Kenneth Watson, Bella, G., Bellerive, A., Bentvelsen, S., Bethke, S., Betts, S., Biebel, O., Biguzzi, A., Bird, S.D., Blobel, V., Bloodworth, I.J., Bobinski, M., Bock, P., Bohme, J., Bonacorsi, D., Boutemeur, M., Braibant, S., Bright-Thomas, P., Brigliadori, L., Brown, Robert M., Burckhart, H.J., Burgard, C., Burgin, R., Capiluppi, P., Carnegie, R.K., Carter, A.A., Carter, J.R., Chang, C.Y., Charlton, David G., Chrisman, D., Ciocca, C., Clarke, P.E.L., Clay, E., Cohen, I., Conboy, J.E., Cooke, O.C., Couyoumtzelis, C., Coxe, R.L., Cuffiani, M., Dado, S., Dallavalle, G.Marco, Davis, R., De Jong, S., del Pozo, L.A., de Roeck, A., Desch, K., Dienes, B., Dixit, M.S., Dubbert, J., Duchovni, E., Duckeck, G., Duerdoth, I.P., Eatough, D., Estabrooks, P.G., Etzion, E., Evans, H.G., Fabbri, F., Fanti, M., Faust, A.A., Fiedler, F., Fierro, M., Fleck, I., Folman, R., Furtjes, A., Futyan, D.I., Gagnon, P., Gary, J.W., Gascon, J., Gascon-Shotkin, S.M., Gaycken, G., Geich-Gimbel, C., Giacomelli, G., Giacomelli, P., Gibson, V., Gibson, W.R., Gingrich, D.M., Glenzinski, D., Goldberg, J., Gorn, W., Grandi, C., Gross, E., Grunhaus, J., Gruwe, M., Hanson, G.G., Hansroul, M., Hapke, M., Harder, K., Hargrove, C.K., Hartmann, C., Hauschild, M., Hawkes, C.M., Hawkings, R., Hemingway, R.J., Herndon, M., Herten, G., Heuer, R.D., Hildreth, M.D., Hill, J.C., Hillier, S.J., Hobson, P.R., Hocker, James Andrew, Homer, R.J., Honma, A.K., Horvath, D., Hossain, K.R., Howard, R., Huntemeyer, P., Igo-Kemenes, P., Imrie, D.C., Ishii, K., Jacob, F.R., Jawahery, A., Jeremie, H., Jimack, M., Jones, C.R., Jovanovic, P., Junk, T.R., Karlen, D., Kartvelishvili, V., Kawagoe, K., Kawamoto, T., Kayal, P.I., Keeler, R.K., Kellogg, R.G., Kennedy, B.W., Klier, A., Kluth, S., Kobayashi, T., Kobel, M., Koetke, D.S., Kokott, T.P., Kolrep, M., Komamiya, S., Kowalewski, Robert V., Kress, T., Krieger, P., von Krogh, J., Kuhl, T., Kyberd, P., Lafferty, G.D., Lanske, D., Lauber, J., Lautenschlager, S.R., Lawson, I., Layter, J.G., Lazic, D., Lee, A.M., Lellouch, D., Letts, J., Levinson, L., Liebisch, R., List, B., Littlewood, C., Lloyd, A.W., Lloyd, S.L., Loebinger, F.K., Long, G.D., Losty, M.J., Ludwig, J., Lui, D., Macchiolo, A., Macpherson, A., Mader, W., Mannelli, M., Marcellini, S., Markopoulos, C., Martin, A.J., Martin, J.P., Martinez, G., Mashimo, T., Mattig, Peter, McDonald, W.John, McKenna, J., Mckigney, E.A., McMahon, T.J., McPherson, R.A., Meijers, F., Menke, S., Merritt, F.S., Mes, H., Meyer, J., Michelini, A., Mihara, S., Mikenberg, G., Miller, D.J., Mir, R., Mohr, W., Montanari, A., Mori, T., Nagai, K., Nakamura, I., Neal, H.A., Nellen, B., Nisius, R., O'Neale, S.W., Oakham, F.G., Odorici, F., Ogren, H.O., Oreglia, M.J., Orito, S., Palinkas, J., Pasztor, G., Pater, J.R., Patrick, G.N., Patt, J., Perez-Ochoa, R., Petzold, S., Pfeifenschneider, P., Pilcher, J.E., Pinfold, J., Plane, David E., Poffenberger, P., Polok, J., Przybycien, M., Rembser, C., Rick, H., Robertson, S., Robins, S.A., Rodning, N., Roney, J.M., Roscoe, K., Rossi, A.M., Rozen, Y., Runge, K., Runolfsson, O., Rust, D.R., Sachs, K., Saeki, T., Sahr, O., Sang, W.M., Sarkisian, E.K.G., Sbarra, C., Schaile, A.D., Schaile, O., Scharf, F., Scharff-Hansen, P., Schieck, J., Schmitt, B., Schmitt, S., Schoning, A., Schroder, Matthias, Schumacher, M., Schwick, C., Scott, W.G., Seuster, R., Shears, T.G., Shen, B.C., Shepherd-Themistocleous, C.H., Sherwood, P., Siroli, G.P., Sittler, A., Skuja, A., Smith, A.M., Snow, G.A., Sobie, R., Soldner-Rembold, S., Sproston, M., Stahl, A., Stephens, K., Steuerer, J., Stoll, K., Strom, David M., Strohmer, R., Surrow, B., Talbot, S.D., Tanaka, S., Taras, P., Tarem, S., Teuscher, R., Thiergen, M., Thomson, M.A., von Torne, E., Torrence, E., Towers, S., Trigger, I., Trocsanyi, Z., Tsur, E., Turcot, A.S., Turner-Watson, M.F., Van Kooten, Rick J., Vannerem, P., Verzocchi, M., Voss, H., Wackerle, F., Wagner, A., Ward, C.P., Ward, D.R., Watkins, P.M., Watson, A.T., Watson, N.K., Wells, P.S., Wermes, N., White, J.S., Wilson, G.W., Wilson, J.A., Wyatt, T.R., Yamashita, S., Yekutieli, G., Zacek, V., and Zer-Zion, D.

Subjects
Physics, Particle physics, Physics and Astronomy (miscellaneous), Meson, 010308 nuclear & particles physics, Branching fraction, Hadron, 01 natural sciences, 0103 physical sciences, Charm (quantum number), 010306 general physics, Engineering (miscellaneous), Particle Physics - Experiment, Lepton
Abstract

The inclusive charm hadron semileptonic branching fractions B(c to e) and B(c to mu) in Z to ccbar events have been determined using 4.4 million hadronic Z decays collected with the OPAL detector at LEP. A charm-enriched sample is obtained by selecting events with reconstructed D*+- mesons. Using leptons found in the hemisphere opposite that of the D*+- mesons, the semileptonic branching fractions of charm hadrons are measured to be B(c to e) = 0.103 +-0.009 +0.009 -0.008 and B(c to mu) = 0.090 +-0.007 +0.007 -0.006 where the first errors are in each case statistical and the others systematic. Combining these measurements, an inclusive semileptonic branching fraction of charm hadrons of B(c to l) = 0.095 +-0.006 +0.007 -0.006 is obtained. The inclusive charm hadron semileptonic branching fractions B(c to e) and B(c to mu) in Z to ccbar events have been determined using 4.4 million hadronic Z decays collected with the OPAL detector at LEP. A charm-enriched sample is obtained by selecting events with reconstructed D*+- mesons. Using leptons found in the hemisphere opposite that of the D*+- mesons, the semileptonic branching fractions of charm hadrons are measured to be B(c to e) = 0.103 +-0.009 +0.009 -0.008 and B(c to mu) = 0.090 +-0.007 +0.007 -0.006 where the first errors are in each case statistical and the others systematic. Combining these measurements, an inclusive semileptonic branching fraction of charm hadrons of B(c to l) = 0.095 +-0.006 +0.007 -0.006 is obtained.

Published
1999
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81. Dose-dense sequential adjuvant chemotherapy followed, as indicated, by trastuzumab for one year in patients with early breast cancer: First report at 5-year median follow-up of a Hellenic Cooperative Oncology Group randomized phase III trial

Author

Fountzilas, G. Dafni, U. Papadimitriou, C. Timotheadou, E. Gogas, H. Eleftheraki, A.G. Xanthakis, I. Christodoulou, C. Koutras, A. Papandreou, C.N. Papakostas, P. Miliaras, S. Markopoulos, C. Dimitrakakis, C. Korantzopoulos, P. Karanikiotis, C. Bafaloukos, D. Kosmidis, P. Samantas, E. Varthalitis, I. Pavlidis, N. Pectasides, D. Dimopoulos, M.-A.

Abstract

Background: Dose-dense sequential chemotherapy including anthracyclines and taxanes has been established in the adjuvant setting of high-risk operable breast cancer. However, the preferable taxane and optimal schedule of administration in a dose-dense regimen have not been defined yet.Methods: From July 2005 to November 2008, 1001 patients (990 eligible) were randomized to receive, every 2 weeks, 3 cycles of epirubicin 110 mg/m2 followed by 3 cycles of paclitaxel 200 mg/m2 followed by 3 cycles of intensified CMF (Arm A; 333 patients), or 3 cycles of epirubicin followed by 3 cycles of CMF, as in Arm A, followed 3 weeks later by 9 weekly cycles of docetaxel 35 mg/m2 (Arm B; 331), or 9 weekly cycles of paclitaxel 80 mg/m2 (Arm C; 326). Trastuzumab was administered for one year to HER2-positive patients post-radiation.Results: At a median follow-up of 60.5 months, the 3-year disease-free survival (DFS) rate was 86%, 90% and 88%, for Arms A, B and C, respectively, while the 3-year overall survival (OS) rate was 96% in all arms. No differences were found in DFS or OS between the combined B and C Arms versus Arm A (DFS: HR = 0.81, 95% CI: 0.59-1.11, P = 0.20; OS: HR = 0.84, 95% CI: 0.55-1.30, P = 0.43). Among the 255 patients who received trastuzumab, 189 patients (74%) completed 1 year of treatment uneventfully. In all arms, the most frequently reported severe adverse events were neutropenia (30% vs. 27% vs. 26%) and leucopenia (12% vs. 13% vs. 12%), while febrile neutropenia occurred in fifty-one patients (6% vs. 4% vs. 5%). Patients in Arm A experienced more often severe pain (P = 0.002), neurological complications (P = 0.004) and allergic reactions (P = 0.004), while patients in Arm B suffered more often from severe skin reactions (P = 0.020).Conclusions: No significant differences in survival between the regimens were found in the present phase III trial. Taxane scheduling influenced the type of severe toxicities. HER2-positive patients demonstrated comparable 3-year DFS and OS rates with those reported in other similar studies.Trial registration: Australian New Zealand Clinical Trials Registry ACTRN12610000151033. © 2014 Fountzilas et al.; licensee BioMed Central Ltd.

Published
2014

82. A new mathematical model for the interpretation of translational research evaluating six CTLA-4 polymorphisms in high-risk melanoma patients receiving adjuvant interferon

Author

Pancoska, P. Kirkwood, J.M. Bouros, S. Spyropoulou-Vlachou, M. Pectasides, E. Tsoutsos, D. Polyzos, A. Markopoulos, C. Panagiotou, P. Castana, O. Bafaloukos, D. Fountzilas, G. Gogas, H.

Abstract

Adjuvant therapy of stage IIB/III melanoma with interferon reduces relapse and mortality by up to 33% but is accompanied by toxicity-related complications. Polymorphisms of the CTLA-4 gene associated with autoimmune diseases could help in identifying interferon treatment benefits. We previously genotyped 286 melanoma patients and 288 healthy (unrelated) individuals for six CTLA-4 polymorphisms (SNP). Previous analyses found no significant differences between the distributions of CTLA-4 polymorphisms in the melanoma population vs. controls, no significant difference in relapse free and overall survivals among patients and no correlation between autoimmunity and specific alleles. We report new analysis of these CTLA-4 genetic profiles, using Network Phenotyping Strategy (NPS). It is graph-theory based method, analyzing the SNP patterns. Application of NPS on CTLA-4 polymorphism captures allele relationship pattern for every patient into 6-partite mathematical graph P. Graphs P are combined into weighted 6-partite graph S, which subsequently decomposed into reference relationship profiles (RRP). Finally, every individual CTLA-4 genotype pattern is characterized by the graph distances of P from eight identified RRP's. RRP's are subgraphs of S, collecting equally frequent binary allele co-occurrences in all studied loci. If S topology represents the genetic "dominant model", the RRP's and their characteristic frequencies are identical to expectation-maximization derived haplotypes and maximal likelihood estimates of their frequencies. The graphrepresentation allows showing that patient CTLA-4 haplotypes are uniquely different from the controls by absence of specific SNP combinations. New function-related insight is derived when the 6-partite graph reflects allelic state of CTLA-4. We found that we can use differences between individual P and specific RRPs to identify patient subpopulations with clearly different polymorphic patterns relatively to controls as well as to identify patients with significantly different survival. © 2014 Pancoska et al.

Published
2014

83. Impact of CYP2D∗6 in the adjuvant treatment of breast cancer patients with tamoxifen

Author

Markopoulos, C. Kykalos, S. Mantas, D.

Subjects
skin and connective tissue diseases, digestive system
Abstract

Biotransformation of tamoxifen to the potent antiestrogen endoxifen is performed by cytochrome P450 (CYP) enzymes, in particular the CYP2D6 isoform. CYP2D6∗4 is one of the most frequent alleles associated with loss of enzymatic activity. The incidence of CYP2D6∗4 among Caucasians is estimated up to 27%, while it is present in up to 90% of all poor metabolizers within the Caucasian population. The hypothesis under question is whether the presence of one or two non-functioning (null) alleles predicts an inferior outcome in postmenopausal women with breast cancer receiving adjuvant treatment with tamoxifen. The numerous existing studies investigating the association of CYP2D6 with treatment failure in breast cancer are inconsistent and give rather conflicting results. Currently, routine CYP2D6 testing among women with breast cancer is not recommended and the significance of CYP2D6 phenotype in decision making regarding the administration of tamoxifen is unclear. The present study summarizes current literature regarding clinical studies on CYP2D6∗4, particularly in terms of response to tamoxifen therapy and breast cancer outcome. © 2014 Baishideng Publishing Group Inc. All rights reserved.

Published
2014

84. Time dependence of biomarkers: non-proportional effects of immunohistochemical panels predicting relapse risk in early breast cancer

Author

Stephen, J. Murray, G. Cameron, D. A. Thomas, J. and Kunkler, I. H. Jack, W. Kerr, G. R. Piper, T. Brookes, C. L. Rea, D. W. van de Velde, C. J. H. Hasenburg, A. and Markopoulos, C. Dirix, L. Seynaeve, C. Bartlett, J. M. S.

Abstract

Background: We investigated the impact of follow-up duration to determine whether two immunohistochemical prognostic panels, IHC4 and Mammostrat, provide information on the risk of early or late distant recurrence using the Edinburgh Breast Conservation Series and the Tamoxifen vs Exemestane Adjuvant Multinational (TEAM) trial. Methods: The multivariable fractional polynomial time (MFPT) algorithm was used to determine which variables had possible nonproportional effects. The performance of the scores was assessed at various lengths of follow-up and Cox regression modelling was performed over the intervals of 0- 5 years and 45 years. Results: We observed a strong time dependence of both the IHC4 and Mammostrat scores, with their effects decreasing over time. In the first 5 years of follow- up only, the addition of both scores to clinical factors provided statistically significant information (Po0.05), with increases in R-2 between 5 and 6% and increases in D-statistic between 0.16 and 0.21. Conclusions: Our analyses confirm that the IHC4 and Mammostrat scores are strong prognostic factors for time to distant recurrence but this is restricted to the first 5 years after diagnosis. This provides evidence for their combined use to predict early recurrence events in order to select those patients who may/will benefit from adjuvant chemotherapy.

Published
2014

85. Dose-dense sequential adjuvant chemotherapy followed, as indicated, by trastuzumab for one year in patients with early breast cancer: first report at 5-year median follow-up of a Hellenic Cooperative Oncology Group randomized phase III trial

Author

Fountzilas, George, Dafni, U., Papadimitriou, C., Timotheadou, E., Gogas, H., Eleftheraki, A. G., Xanthakis, I., Christodoulou, C., Koutras, A. K., Papandreou, C. N., Papakostas, P., Miliaras, S., Markopoulos, C., Dimitrakakis, C., Korantzopoulos, Panagiotis, Karanikiotis, C., Bafaloukos, Dimitrios, Kosmidis, Paraskevas A., Samantas, E., Varthalitis, I., Pavlidis, Nicholas, Pectasides, Dimitrios, Dimopoulos, M. A., and Pavlidis, Nicholas [0000-0002-2195-9961]

Subjects
Oncology, Survival rate, Neurologic disease, Docetaxel, Skin disease, Multiple cycle treatment, Eye disease, Breast cancer, Phase 3 clinical trial, Antineoplastic agents, Antineoplastic Combined Chemotherapy Protocols, Pathology, Drug fatality, Anthracyclines, Disease free survival, Open study, Fulvestrant, Mastectomy, Dose-dense sequential chemotherapy, Multicenter study, Clinical trial, Antineoplastic agent, Randomized controlled trial, Granulocyte colony stimulating factor, Goserelin, Thrombocyte, Infection, Human, Diarrhea, medicine.medical_specialty, Paclitaxel, Vomiting, Febrile neutropenia, Heart failure, Antineoplastic Agents, Major clinical study, Side effect, Heart disease, Anastrozole, Vascular disease, Article, Disease-Free Survival, Drug Administration Schedule, Epidermal growth factor receptor 2, Taxanes, Median follow-up, Genetics, Humans, Hemoglobin, Phase 3 clinical trial (topic), Cyclophosphamide, Aged, Follow up, Leukopenia, Myalgia, medicine.disease, Metabolic disorder, Cancer combination chemotherapy, Regimen, Tamoxifen, Methotrexate, Cancer adjuvant therapy, Asymptomatic disease, Comparative study, Breast neoplasms, Cancer Research, Partial mastectomy, Heart ejection fraction, Gonadorelin, Skin manifestation, Monoclonal, Edema, Overall survival, Middle aged, Humanized, Fatigue, Adjuvant, Drug withdrawal, Neutrophil, Nausea, Middle Aged, Gastrointestinal disease, Arthralgia, Anorexia, Chemotherapy, Adjuvant, Cancer radiotherapy, Female, Fluorouracil, Epirubicin, medicine.drug, Research Article, Monoclonal antibody, Adult, Neutropenia, Disease-free survival, Pain, Breast Neoplasms, Follow-up studies, Antibodies, Monoclonal, Humanized, Antibodies, Young Adult, Mucosa inflammation, Internal medicine, Antineoplastic combined chemotherapy protocols, medicine, Chemotherapy, Early cancer, Taxane, business.industry, Drug administration, Loading drug dose, Lymphocytopenia, Drug administration schedule, Allergic reaction, Patient compliance, Aromatase inhibitor, Leukocyte, Trastuzumab, Adjuvant chemotherapy, Drug efficacy, Young adult, Lung disease, business, Controlled study, Follow-Up Studies
Abstract

Background: Dose-dense sequential chemotherapy including anthracyclines and taxanes has been established in the adjuvant setting of high-risk operable breast cancer. However, the preferable taxane and optimal schedule of administration in a dose-dense regimen have not been defined yet.Methods: From July 2005 to November 2008, 1001 patients (990 eligible) were randomized to receive, every 2 weeks, 3 cycles of epirubicin 110 mg/m2 followed by 3 cycles of paclitaxel 200 mg/m2 followed by 3 cycles of intensified CMF (Arm A; 333 patients), or 3 cycles of epirubicin followed by 3 cycles of CMF, as in Arm A, followed 3 weeks later by 9 weekly cycles of docetaxel 35 mg/m2 (Arm B; 331), or 9 weekly cycles of paclitaxel 80 mg/m2 (Arm C; 326). Trastuzumab was administered for one year to HER2-positive patients post-radiation.Results: At a median follow-up of 60.5 months, the 3-year disease-free survival (DFS) rate was 86%, 90% and 88%, for Arms A, B and C, respectively, while the 3-year overall survival (OS) rate was 96% in all arms. No differences were found in DFS or OS between the combined B and C Arms versus Arm A (DFS: HR = 0.81, 95% CI: 0.59-1.11, P = 0.20; OS: HR = 0.84, 95% CI: 0.55-1.30, P = 0.43). Among the 255 patients who received trastuzumab, 189 patients (74%) completed 1 year of treatment uneventfully. In all arms, the most frequently reported severe adverse events were neutropenia (30% vs. 27% vs. 26%) and leucopenia (12% vs. 13% vs. 12%), while febrile neutropenia occurred in fifty-one patients (6% vs. 4% vs. 5%). Patients in Arm A experienced more often severe pain (P = 0.002), neurological complications (P = 0.004) and allergic reactions (P = 0.004), while patients in Arm B suffered more often from severe skin reactions (P = 0.020).Conclusions: No significant differences in survival between the regimens were found in the present phase III trial. Taxane scheduling influenced the type of severe toxicities. HER2-positive patients demonstrated comparable 3-year DFS and OS rates with those reported in other similar studies.Trial registration: Australian New Zealand Clinical Trials Registry ACTRN12610000151033. © 2014 Fountzilas et al.; licensee BioMed Central Ltd. 14 1

Published
2013

86. Should all postmenopausal patients with hormone receptor-positive breast cancer receive initial therapy with aromatase inhibitors?

Author

Aapro, M. van de Velde, C.J.H. Markopoulos, C. Bartlett, J.M.S. Putter, H. Coleman, R.E.

Abstract

Background: In the past few years aromatase inhibitors (AIs) have shown superior efficacy to the previous standard adjuvant endocrine therapy, tamoxifen, and are now recommended as part of current adjuvant endocrine therapy. A range of treatment strategies have been explored. Materials and methods: We assess the role of initial AI therapy for postmenopausal women with hormone receptor-positive breast cancer and consider the relative value of initial therapy with an AI compared with switch or extended (>5-yr) adjuvant therapy. Results: Both initial AI therapy and switching/sequential tamoxifen followed by an AI are associated with longer disease- and relapse-free survival versus 5 years of tamoxifen alone. Trials comparing initial therapy with the sequence of tamoxifen followed by an AI have not demonstrated any major efficacy differences between the treatment strategies. Several analyses have been conducted to identify prognostic or predictive markers of treatment benefit to enable selection of the most appropriate adjuvant therapy. Conclusions: Initial and switching/sequential regimens are equally appropriate adjuvant treatment options for postmenopausal patients with hormone receptor-positive breast cancer. The exact tumour biology which allows for initial AI therapy has not yet been determined with certainty. © 2013 .

Published
2013

87. Do type 1 receptor tyrosine kinases inform treatment choice? A prospectively planned analysis of the TEAM trial

Author

Bartlett, J. M. S. Brookes, C. L. Piper, T. van de Velde, C. J. H. Stocken, D. Lyttle, N. Hasenburg, A. Quintayo, M. A. Kieback, D. G. Putter, H. Markopoulos, C. Kranenbarg, E. M-K Mallon, E. A. Dirix, L. Y. Seynaeve, C. Rea, D. W.

Subjects
body regions
Abstract

Background: Epidermal growth factor receptors contribute to breast cancer relapse during endocrine therapy. Substitution of aromatase inhibitors (AIs) may improve outcomes in HER-positive cancers. Methods: Tissue microarrays were constructed. Quantitative analysis of HER1, HER2, and HER3 was performed. Data were analysed relative to disease-free survival and treatment using outcomes at 2.75 and 6.5 years. Results: Among 4541 eligible samples, 4225 (93%) had complete HER1-3 data. Overall, 5% were HER1-positive, 13% HER2positive, and 21% HER3-positive; 32% (n = 1351) overexpressed at least one HER receptor. In the HER1-3-negative subgroup, the hazard ratio (HR) for upfront exemestane vs tamoxifen at 2.75 years was 0.67 (95% confidence interval (CI), 0.52-0.87), in the HER1-3-positive subgroup, the HR was 1.15 (95% CI, 0.85-1.56). A prospectively planned treatment-by-marker analysis demonstrated a significant interaction between HER1-3 and treatment at 2.75 years (HR 0.58; 95% CI, 0.39-0.87; P 0.008), as confirmed by multivariate regression analysis adjusting for prognostic factors (HR 0.55; 95% CI, 0.36-0.85; P 0.005). This effect was time dependent. Conclusion: In the 2.75 years prior to switching patients initially treated with tamoxifen to exemestane, a significant treatmentby- marker effect exists between AI/tamoxifen treatment and HER1-3 expression, suggesting HER expression could be used to select appropriate endocrine treatment at diagnosis to prevent or delay early relapses.

Published
2013

88. In vitro and Ex vivo investigation of the impact of luminal lipid phases on passive permeability of lipophilic small molecules using PAMPA

Author

Markopoulos, C. Imanidis, G. Vertzoni, M. Symillides, M. Parrott, N. Reppas, C.

Abstract

Purpose: Evaluate the impact of luminal micellar phase on passive permeability of five lipophilic (1.9 ≤ clogP ≤ 9.0) small molecules using biorelevant media and evaluate the impact of luminal coarse lipid particles on danazol permeability after oral administration of a triglyceride solution to fed adults using PAMPA. Methods: Permeability of carbamazepine, furosemide, danazol, and Compound A was evaluated using Prisma™ HT, FaSSIF-V2, and FeSSIF-V2 in the donor compartment. Compound B could not be tested using Prisma™ HT, due to negligible solubility. Individual intestinal aspirates collected after administration of danazol solution in the olive oil portion of a meal and corresponding micellar phases were subjected to PAMPA. Commercially available Acceptor Sink Buffer was used in all cases. Results: Unlike with furosemide (under constant pH) and Compound B, permeability of carbamazepine, danazol, and Compound A steadily decreased in the presence of increasing micelle concentration of media. Danazol permeability from aspirates was reduced compared to that from micellar phases; fluxes were similar. Conclusions: Using PAMPA, the impact of luminal micellar phase on passive permeability of lipophilic molecules varies with the molecule. After administration of a triglyceride solution of danazol, high danazol concentrations in coarse lipid particles balance in terms of drug flux the reduced permeability. [Figure not available: see fulltext.] © 2013 Springer Science+Business Media New York.

Published
2013

93. Postoperative dose-dense sequential versus concomitant administration of epirubicin and paclitaxel in patients with node-positive breast cancer: 5-Year results of the Hellenic Cooperative Oncology Group HE 10/00 phase III Trial

Author

Gogas, H. Dafni, U. Karina, M. Papadimitriou, C. Batistatou, A. Bobos, M. Kalofonos, H.P. Eleftheraki, A.G. Timotheadou, E. Bafaloukos, D. Christodoulou, C. Markopoulos, C. Briasoulis, E. Papakostas, P. Samantas, E. Kosmidis, P. Stathopoulos, G.P. Karanikiotis, C. Pectasides, D. Dimopoulos, M.A. Fountzilas, G.

Abstract

To explore the impact of dose intensity (DI) in the adjuvant setting of breast cancer, a randomized phase III trial was conducted comparing postoperative dose-dense sequential chemotherapy with epirubicin, paclitaxel, and cyclophosphamide, methotrexate and fluorouracil (CMF)in high-risk breast cancer patients. From Oct 2000 to June 2005, 1,121 node-positive patients were randomized to dose-dense sequential epirubicin 110 mg/m 2 and paclitaxel (Taxol®, Bristol Myers-Squibb, Princeton, NJ) 250 mg/m 2 (group A), or concurrent epirubicin 83 mg/m 2 and paclitaxel 187 mg/m 2 (group B), both followed by three cycles of "intensified" combination chemotherapy with CMF. By protocol design total cumulative dose and duration of treatment were identical in both groups. Dose intensity of epirubicin and paclitaxel was double in the dose-dense arm. Prophylactic treatment with granulocyte colony-stimulating factor was given with the dose-dense treatments. Disease-free survival (DFS) was the primary endpoint. At a median follow-up of 76 months, 253 patients (23%) had documented disease relapse (123 vs. 130 in groups A and B, respectively) and 208 deaths (101, group A and 107, group B) had been observed. The 5-year DFS rate of 74 and 74% and OS rate of 86 and 85% were observed for group A and group B, respectively. No differences were found in DFS or OS between the two treatment groups (P = 0.78 and P = 0.45 for DFS and OS, respectively). Safety analysis results showing that both regimens were well tolerated and safe have been previously published (Fountzilas et al. Ann Oncol 2008). No DFS or OS benefit from the dose-dense sequential epirubicin and paclitaxel was detected when compared to the concurrent administration of the same drugs. No additional safety issues were raised with long-term follow-up. © 2011 Springer Science+Business Media, LLC.

Published
2012

95. Luminal lipid phases after administration of a triglyceride solution of danazol in the fed state and their contribution to the flux of danazol across Caco-2 cell monolayers

Author

Vertzoni, M. Markopoulos, C. Symillides, M. Goumas, C. Imanidis, G. Reppas, C.

Abstract

The first aim of this study was to characterize the luminal contents and their micellar phase after the administration of a heterogeneous liquid meal to healthy adults. The second aim was to evaluate the impact of micellar lipids and coarse lipid particles on danazol flux through intestinal monolayers. A third aim was to compare the micellar composition in the upper small intestine with the composition of fed state simulating intestinal fluid (FeSSIF-V2), a medium that has been proposed for investigating dissolution of poorly soluble drugs in the fed state. Danazol (150 mg), predissolved in the olive oil portion of the meal, was administered via the gastric port of a two-lumen tube to the antrum of eight adults. Aspirates from the ligament of Treitz [collected up to 4 h postdosing (∼15 mL every 30 min)] were characterized physicochemically. Comparison of these characteristics with FeSSIF-V2 indicates that FeSSIF-V2 is an appropriate medium for evaluating drug solubilization in the luminal micellar phase in the fed state. Individual aspirates and their corresponding micellar phases were also diluted with aqueous transport medium and subjected to Caco-2 cell permeation experiments. Permeability coefficients for danazol in the diluted aspirates were smaller than those for the diluted micellar phases, which in turn were similar to those for aqueous transport medium. The high danazol concentrations overcompensated the reduced permeability coefficient values in the diluted aspirates in terms of total drug flux. We conclude that drug dissolved in the coarse lipid particles formed after administration of a triglyceride solution can directly contribute to the flux of lipophilic drugs across the intestinal mucosa. © 2012 American Chemical Society.

Published
2012

98. Estrogen receptor and progesterone receptor as predictive biomarkers of response to endocrine therapy: A prospectively powered pathology study in the tamoxifen and exemestane adjuvant multinational trial

Author

Bartlett, J.M.S. Brookes, C.L. Robson, T. Van De Velde, C.J.H. Billingham, L.J. Campbell, F.M. Grant, M. Hasenburg, A. Hille, E.T.M. Kay, C. Kieback, D.G. Putter, H. Markopoulos, C. Kranenbarg, E.M.-K. Mallon, E.A. Dirix, L. Seynaeve, C. Rea, D.

Subjects
skin and connective tissue diseases, hormones, hormone substitutes, and hormone antagonists
Abstract

Purpose The Tamoxifen and Exemestane Adjuvant Multinational (TEAM) trial included a prospectively planned pathology substudy testing the predictive value of progesterone receptor (PgR) expression for outcome of estrogen receptor-positive (ER-positive) early breast cancer treated with exemestane versus tamoxifen. Patients and Methods Pathology blocks from 4,781 TEAM patients randomly assigned to exemestane versus tamoxifen followed by exemestane for 5 years of total therapy were collected centrally, and tissue microarrays were constructed from samples from 4,598 patients. Quantitative analysis of hormone receptors (ER and PgR) was performed by using image analysis and immunohistochemistry, and the results were linked to outcome data from the main TEAM trial and analyzed relative to disease-free survival and treatment. Results Of 4,325 eligible ER-positive patients, 23% were PgR-poor (Allred < 4) and 77% were PgRrich (Allred ≥ 5). No treatment-by-marker effect for PgR was observed for exemestane versus tamoxifen (PgR-rich hazard ratio [HR], 0.83; 95% CI, 0.65 to 1.05; PgR-poor HR, 0.85; 95% CI, 0.61 to 1.19; P=.88 for interaction). Both PgR and ER expression were associated with patient prognosis in univariate (PgR HR, 0.53; 95% CI, 0.43 to 0.65; P < 01; ER HR, 0.66; 95% CI, 0.51 to 0.86; P=.002), and multivariate analyses (P < .001 and P=.001, respectively). A trend toward a treatment-by-marker effect for ER-rich patients was observed. Conclusion Preferential exemestane versus tamoxifen treatment benefit was not predicted by PgR expression; conversely, patients with ER-rich tumors may derive additional benefit from exemestane. Quantitative analysis of ER and PgR expression provides highly significant information on risk of early relapse (within 1 to 3 years) during treatment. © 2011 by American Society of Clinical Oncology.

Published
2011

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