Your search keyword '"G., Giaccone"' showing total 1,170 results

1. KEYNOTE-867: Phase 3, Randomized, Placebo-Controlled Study of Stereotactic Body Radiotherapy (SBRT) with or without Pembrolizumab in Patients with Unresected Stage I or II Non–Small-Cell Lung Cancer (NSCLC)

Author

S.K. Jabbour, B. Houghton, A.G. Robinson, X. Quantin, T. Wehler, D. Kowalski, M.J. Ahn, M. Erman, G. Giaccone, H. Borghaei, J. McLean, Y. Xu, F. Souza, and G. Pall

Subjects

Cancer Research, Radiation, Oncology, Radiology, Nuclear Medicine and imaging

Published

2022

2. 1024P Net treatment benefit of OSE2101 in HLA-A2+ non-small cell lung cancer (NSCLC) patients after failure to immune checkpoint inhibitors (IO) in phase III Atalante-1 randomized trial

Author

M.E. Buyse, F. Montestruc, J-C. Chiem, V. Deltuvaite-Thomas, S. Salvaggio, M.R. Garcia Campelo, M. Cobo Dols, E. Quoix, A-C. Madroszyk Flandin, F. Cappuzzo, G. Romano, S. Viteri Ramirez, W. Schuette, A. Zer, S. Comis, B. Vasseur, R. Dziadziuszko, G. Giaccone, B. Besse, and E. Felip

Subjects

Oncology, Hematology

Published

2022

3. 492TiP A phase I study of synthetic lethal, IDE397 (MAT2A inhibitor) as a monotherapy and in combination with chemotherapy in advanced solid tumors harboring MTAP deletion

Author

M.L. Johnson, J. Rodon, R. Aljumaily, M. Villalona-Calero, E. Borazanci, M. Pishvaian, A. Turk, R.D. Carvajal, C. Mantia, G. Giaccone, Z. Mounir, A. Patel, M. Maurer, C. Neilan, D. Rajendran, U. Ganesan, J. Hinkle, and A.W. Tolcher

Subjects

Oncology, Hematology

Published

2022

4. 172P Phase I study of JTX-8064, a LILRB2 (ILT4) inhibitor, as monotherapy and combination with pimivalimab (pimi), a PD-1 inhibitor (PD-1i), in patients (pts) with advanced solid tumors

Author

K. Papadopoulos, T. Li, N. Lakhani, J. Powderly, T. George, D.G.K. Teoh, D. Kilari, G. Giaccone, R.E. Sanborn, S. Ghamande, P. LoRusso, G. Gibney, V.T-L. Ma, K. Yalamanchili, J. Brown, N. Mota, C. Tasillo Kadra, B. Umiker, X. Xiao, and E. Trehu

Subjects

Oncology, Immunology and Allergy

Published

2022

5. IGNYTE: A Phase 1/2 Multi-Cohort Clinical Trial of RP1 ± Nivolumab in Patients with Non-Small Cell Lung Cancer and Other Solid Tumors

Author

H. Emamekhoo, S. Patel, E. Rodriguez, M.K. Riaz, G. Giaccone, M. Furqan, J.J. Sacco, P. Bommareddy, S. Raza, S. He, K. Harrington, and M.R. Middleton

Subjects

Cancer Research, Radiation, Oncology, Radiology, Nuclear Medicine and imaging

Published

2022

6. 1019P Pattern of clinical activity of anticancer vaccine OSE2101 in HLA-A2+ non-small cell lung cancer (NSCLC) patients after failure to immune checkpoint inhibitors (IO) in phase III Atalante-1 randomized trial

Author

M.R. Garcia Campelo, E. Felip, B. Besse, M. Cobo Dols, E. Quoix, A-C. Madroszyk Flandin, F. Cappuzzo, F. Denis, W. Hilgers, G. Romano, D. Debieuvre, D. Galetta, E. Baldini, S. Viteri Ramirez, M. Duc Phan, W. Schuette, A. Zer, B. Vasseur, R. Dziadziuszko, and G. Giaccone

Subjects

Oncology, Hematology

Published

2022

7. 61P IMpower110: Exploratory analyses of the impact of first-line (1L) atezolizumab on the efficacy of next-line of therapy in PD-L1–selected NSCLC

Author

S.P. Patel, J.E. Reuss, K. Scilla, G. Giaccone, D.R. Spigel, C. Ngiam, Q. Zhu, I. Bara, B. Ding, and R.S. Herbst

Subjects

Oncology, Hematology

Published

2021

8. A Neurotoxic and Gliotrophic Fragment of the Prion Protein Increases Plasma Membrane Microviscosity

Author

M. Salmona, G. Forloni, L. Diomede, M. Algeri, L. De Gioia, N. Angeretti, G. Giaccone, F. Tagliavini, and O. Bugiani

Subjects

Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

Prion-related encephalopathies are characterized by astrogliosis and nerve cell degeneration and loss. These lesions might be the consequence of an interaction between the abnormal isoform of the cellular prion protein that accumulates in nervous tissue and the plasma membranes. Previously we found that a synthetic peptide, homologous to residues 106–126 of the human prion protein, is fibrillogenic and toxic to neurons and trophic to astrocytesin vitro.This study dealt with the ability of the peptide to interact with membranes. Accordingly, we compared PrP 106–126 with different synthetic PrP peptides (PrP 89–106, PrP 127–147, a peptide with a scrambled sequence of 106–126, and PrP 106–126 amidated at the C-terminus) as to the ability to increase the microviscosity of artificial and natural membranes. The first three had no effect on nerve and glial cellsin vitro,whereas the amidated peptide caused neuronal death. Using a fluorescent probe that becomes incorporated into the hydrocarbon core of the lipid bilayer and records the lipid fluidity, we found PrP 106–126 able to increase significantly the membrane microviscosity of liposomes and of all cell lines investigated. This phenomenon was associated with the distribution of the peptide over the cell surface, but not with changes in the membrane lipid or protein content, or with membrane lipid phase transitions. Accordingly, we deduced that increased membrane microviscosity was unrelated to changes in the membrane native components and was the result of increased lipid density following PrP 106–126 embedding into the lipid bilayer. No control peptides had comparable effects on the membrane microviscosity, except PrP 106–126 amidated at the C-terminus. Since the latter was as neurotoxic, but not as fibrillogenic, as PrP 106–126, we argued that the ability of PrP 106–126 to increase membrane microviscosity was unrelated to the propensity of the peptide to raise fibrils. Rather, it could be connected with the primary structure of PrP 106–126, characterized by two opposing regions, one hydrophilic and the other hydrophobic, that enabled the peptide to interact with the lipid bilayer. Based on these findings, we speculated that the glial and nerve cell involvement occurring in prion-related encephalopathies might be caused by the interaction with the plasma membrane of a PrP 106–126-like fragment or of the sequence spanning residues 106–126 of the abnormal isoform of the prion protein.

Published

1997

9. Common variants in Alzheimer’s disease and risk stratification by polygenic risk scores

Author

de Rojas, I. Moreno-Grau, S. Tesi, N. Grenier-Boley, B. Andrade, V. Jansen, I.E. Pedersen, N.L. Stringa, N. Zettergren, A. Hernández, I. Montrreal, L. Antúnez, C. Antonell, A. Tankard, R.M. Bis, J.C. Sims, R. Bellenguez, C. Quintela, I. González-Perez, A. Calero, M. Franco-Macías, E. Macías, J. Blesa, R. Cervera-Carles, L. Menéndez-González, M. Frank-García, A. Royo, J.L. Moreno, F. Huerto Vilas, R. Baquero, M. Diez-Fairen, M. Lage, C. García-Madrona, S. García-González, P. Alarcón-Martín, E. Valero, S. Sotolongo-Grau, O. Ullgren, A. Naj, A.C. Lemstra, A.W. Benaque, A. Pérez-Cordón, A. Benussi, A. Rábano, A. Padovani, A. Squassina, A. de Mendonça, A. Arias Pastor, A. Kok, A.A.L. Meggy, A. Pastor, A.B. Espinosa, A. Corma-Gómez, A. Martín Montes, A. Sanabria, Á. DeStefano, A.L. Schneider, A. Haapasalo, A. Kinhult Ståhlbom, A. Tybjærg-Hansen, A. Hartmann, A.M. Spottke, A. Corbatón-Anchuelo, A. Rongve, A. Borroni, B. Arosio, B. Nacmias, B. Nordestgaard, B.G. Kunkle, B.W. Charbonnier, C. Abdelnour, C. Masullo, C. Martínez Rodríguez, C. Muñoz-Fernandez, C. Dufouil, C. Graff, C. Ferreira, C.B. Chillotti, C. Reynolds, C.A. Fenoglio, C. Van Broeckhoven, C. Clark, C. Pisanu, C. Satizabal, C.L. Holmes, C. Buiza-Rueda, D. Aarsland, D. Rujescu, D. Alcolea, D. Galimberti, D. Wallon, D. Seripa, D. Grünblatt, E. Dardiotis, E. Düzel, E. Scarpini, E. Conti, E. Rubino, E. Gelpi, E. Rodriguez-Rodriguez, E. Duron, E. Boerwinkle, E. Ferri, E. Tagliavini, F. Küçükali, F. Pasquier, F. Sanchez-Garcia, F. Mangialasche, F. Jessen, F. Nicolas, G. Selbæk, G. Ortega, G. Chêne, G. Hadjigeorgiou, G. Rossi, G. Spalletta, G. Giaccone, G. Grande, G. Binetti, G. Papenberg, G. Hampel, H. Bailly, H. Zetterberg, H. Soininen, H. Karlsson, I.K. Alvarez, I. Appollonio, I. Giegling, I. Skoog, I. Saltvedt, I. Rainero, I. Rosas Allende, I. Hort, J. Diehl-Schmid, J. Van Dongen, J. Vidal, J.-S. Lehtisalo, J. Wiltfang, J. Thomassen, J.Q. Kornhuber, J. Haines, J.L. Vogelgsang, J. Pineda, J.A. Fortea, J. Popp, J. Deckert, J. Buerger, K. Morgan, K. Fließbach, K. Sleegers, K. Molina-Porcel, L. Kilander, L. Weinhold, L. Farrer, L.A. Wang, L.-S. Kleineidam, L. Farotti, L. Parnetti, L. Tremolizzo, L. Hausner, L. Benussi, L. Froelich, L. Ikram, M.A. Deniz-Naranjo, M.C. Tsolaki, M. Rosende-Roca, M. Löwenmark, M. Hulsman, M. Spallazzi, M. Pericak-Vance, M.A. Esiri, M. Bernal Sánchez-Arjona, M. Dalmasso, M.C. Martínez-Larrad, M.T. Arcaro, M. Nöthen, M.M. Fernández-Fuertes, M. Dichgans, M. Ingelsson, M. Herrmann, M.J. Scherer, M. Vyhnalek, M. Kosmidis, M.H. Yannakoulia, M. Schmid, M. Ewers, M. Heneka, M.T. Wagner, M. Scamosci, M. Kivipelto, M. Hiltunen, M. Zulaica, M. Alegret, M. Fornage, M. Roberto, N. van Schoor, N.M. Seidu, N.M. Banaj, N. Armstrong, N.J. Scarmeas, N. Scherbaum, N. Goldhardt, O. Hanon, O. Peters, O. Skrobot, O.A. Quenez, O. Lerch, O. Bossù, P. Caffarra, P. Dionigi Rossi, P. Sakka, P. Hoffmann, P. Holmans, P.A. Fischer, P. Riederer, P. Yang, Q. Marshall, R. Kalaria, R.N. Mayeux, R. Vandenberghe, R. Cecchetti, R. Ghidoni, R. Frikke-Schmidt, R. Sorbi, S. Hägg, S. Engelborghs, S. Helisalmi, S. Botne Sando, S. Kern, S. Archetti, S. Boschi, S. Fostinelli, S. Gil, S. Mendoza, S. Mead, S. Ciccone, S. Djurovic, S. Heilmann-Heimbach, S. Riedel-Heller, S. Kuulasmaa, T. del Ser, T. Lebouvier, T. Polak, T. Ngandu, T. Grimmer, T. Bessi, V. Escott-Price, V. Giedraitis, V. Deramecourt, V. Maier, W. Jian, X. Pijnenburg, Y.A.L. Smith, A.D. Saenz, A. Bizzarro, A. Lauria, A. Vacca, A. Solomon, A. Anastasiou, A. Richardson, A. Boland, A. Koivisto, A. Daniele, A. Greco, A. Marianthi, A. McGuinness, B. Fin, B. Ferrari, C. Custodero, C. Ferrarese, C. Ingino, C. Mangone, C. Reyes Toso, C. Martínez, C. Cuesta, C. Muchnik, C. Joachim, C. Ortiz, C. Besse, C. Johansson, C. Zoia, C.P. Laske, C. Anastasiou, C. Palacio, D.L. Politis, D.G. Janowitz, D. Craig, D. Mann, D.M. Neary, D. Jürgen, D. Daian, D. Belezhanska, D. Kohler, E. Castaño, E.M. Koutsouraki, E. Chipi, E. De Roeck, E. Costantini, E. Vardy, E.R.L.C. Piras, F. Roveta, F. Piras, F. Prestia, F.A. Assogna, F. Salani, F. Sala, G. Lacidogna, G. Novack, G. Wilcock, G. Thonberg, H. Kölsch, H. Weber, H. Boecker, H. Etchepareborda, I. Piaceri, I. Tuomilehto, J. Lindström, J. Laczo, J. Johnston, J. Deleuze, J.-F. Harris, J. Schott, J.M. Priller, J. Bacha, J.I. Snowden, J. Lisso, J. Mihova, K.Y. Traykov, L. Morelli, L. Brusco, L.I. Rainer, M. Takalo, M. Bjerke, M. Del Zompo, M. Serpente, M. Sanchez Abalos, M. Rios, M. Peltonen, M. Herrman, M.J. Kosmidis, M.H. Kohler, M. Rojo, M. Jones, M. Orsini, M. Medel, N. Olivar, N. Fox, N.C. Salvadori, N. Hooper, N.M. Galeano, P. Solis, P. Bastiani, P. Mecocci, P. Passmore, P. Heun, R. Antikainen, R. Olaso, R. Perneczky, R. Germani, S. López-García, S. Love, S. Mehrabian, S. Bagnoli, S. Kochen, S. Andreoni, S. Teipel, S. Todd, S. Pickering-Brown, S. Natunen, T. Tegos, T. Laatikainen, T. Strandberg, T. Polvikoski, T.M. Matoska, V. Ciullo, V. Cores, V. Solfrizzi, V. Lisetti, V. Sevillano, Z. Abdelnour, C. Aguilera, N. Alarcon, E. Alegret, M. Benaque, A. Boada, M. Buendia, M. Cañabate, P. Carracedo, A. Corbatón-Anchuelo, A. Diego, S. Espinosa, A. Gailhajenet, A. Gil, S. Guitart, M. Hernández, I. Ibarria, M. Lafuente, A. Macias, J. Maroñas, O. Martín, E. Martínez, M.T. Marquié, M. Mauleón, A. Montrreal, L. Moreno-Grau, S. Moreno, M. Orellana, A. Ortega, G. Pancho, A. Pelejá, E. Pérez-Cordon, A. Pineda, J.A. Preckler, S. Quintela, I. Real, L.M. Rosende-Roca, M. Ruiz, A. Sáez, M.E. Sanabria, A. Serrano-Rios, M. Sotolongo-Grau, O. Tárraga, L. Valero, S. Vargas, L. Adarmes-Gómez, A.D. Alarcón-Martín, E. Alonso, M.D. Álvarez, I. Álvarez, V. Amer-Ferrer, G. Antequera, M. Antúnez, C. Baquero, M. Bernal, M. Blesa, R. Boada, M. Buiza-Rueda, D. Bullido, M.J. Burguera, J.A. Calero, M. Carrillo, F. Carrión-Claro, M. Casajeros, M.J. Clarimón, J. Cruz-Gamero, J.M. de Pancorbo, M.M. del Ser, T. Diez-Fairen, M. Escuela, R. Garrote-Espina, L. Fortea, J. Franco-Macías, E. Frank-García, A. García-Alberca, J.M. Garcia Madrona, S. Garcia-Ribas, G. Gómez-Garre, P. Hernández, I. Hevilla, S. Jesús, S. Labrador Espinosa, M.A. Lage, C. Legaz, A. Lleó, A. Lopez de Munain, A. López-García, S. Macias-García, D. Manzanares, S. Marín, M. Marín-Muñoz, J. Marín, T. Marquié, M. Martín Montes, A. Martínez, B. Martínez, C. Martínez, V. Martínez-Lage Álvarez, P. Medina, M. Mendioroz Iriarte, M. Mir, P. Molinuevo, J.L. Pastor, P. Pérez Tur, J. Periñán-Tocino, T. Pineda-Sanchez, R. Piñol-Ripoll, G. Rábano, A. Real de Asúa, D. Rodrigo, S. Rodríguez-Rodríguez, E. Royo, J.L. Ruiz, A. Sanchez del Valle Díaz, R. Sánchez-Juan, P. Sastre, I. Valero, S. Vicente, M.P. Vigo-Ortega, R. Vivancos, L. Macleod, C. McCracken, C. Brayne, C. Bresner, C. Grozeva, D. Bellou, E. Sommerville, E.W. Matthews, F. Leonenko, G. Menzies, G. Windle, G. Harwood, J. Phillips, J. Bennett, K. Luckuck, L. Clare, L. Woods, R. Saad, S. Burholt, V. Jansen, I.E. Rongve, A. Kehoe, P.G. Garcia-Ribas, G. Sánchez-Juan, P. Pastor, P. Pérez-Tur, J. Piñol-Ripoll, G. Lopez de Munain, A. García-Alberca, J.M. Bullido, M.J. Álvarez, V. Lleó, A. Real, L.M. Scheltens, P. Holstege, H. Marquié, M. Sáez, M.E. Carracedo, Á. Amouyel, P. Schellenberg, G.D. Williams, J. Seshadri, S. van Duijn, C.M. Mather, K.A. Sánchez-Valle, R. Serrano-Ríos, M. Orellana, A. Tárraga, L. Blennow, K. Huisman, M. Andreassen, O.A. Posthuma, D. Clarimón, J. Boada, M. van der Flier, W.M. Ramirez, A. Lambert, J.-C. van der Lee, S.J. Ruiz, A. EADB contributors The GR@ACE study group DEGESCO consortium IGAP (ADGC, CHARGE, EADI, GERAD) PGC-ALZ consortia

Abstract

Genetic discoveries of Alzheimer’s disease are the drivers of our understanding, and together with polygenetic risk stratification can contribute towards planning of feasible and efficient preventive and curative clinical trials. We first perform a large genetic association study by merging all available case-control datasets and by-proxy study results (discovery n = 409,435 and validation size n = 58,190). Here, we add six variants associated with Alzheimer’s disease risk (near APP, CHRNE, PRKD3/NDUFAF7, PLCG2 and two exonic variants in the SHARPIN gene). Assessment of the polygenic risk score and stratifying by APOE reveal a 4 to 5.5 years difference in median age at onset of Alzheimer’s disease patients in APOE ɛ4 carriers. Because of this study, the underlying mechanisms of APP can be studied to refine the amyloid cascade and the polygenic risk score provides a tool to select individuals at high risk of Alzheimer’s disease. © 2021, The Author(s).

Published

2021

10. Early and long-term cognitive features in sporadic Creutzfeldt-Jakob disease

Author

M, Meattini, G, Giaccone, L, D'Incerti, and A R, Giovagnoli

Subjects

Cerebral Cortex, Cognition, Humans, Creutzfeldt-Jakob Syndrome

Published

2020

11. An atypical presentation of diffuse midline pontine glioma in a middle age patient: Case report

Author

S. Floro, D. Belvedere, C. Rosci, M. Secchi, C. Casellato, G. Oggioni, C. Gambini, L. Campiglio, M. Zardoni, R. Altavilla, F. Bianchi, A. D'Arrigo, F. Bartesaghi, M. Egidi, C. Uggetti, G. Giaccone, G. Marucci, A. Mastronuzzi, M. Vinci, and A. Priori

Subjects

medicine.medical_specialty, medicine.diagnostic_test, business.industry, Cranial nerves, Magnetic resonance imaging, General Medicine, Fluid-attenuated inversion recovery, medicine.disease, Middle age, 03 medical and health sciences, 0302 clinical medicine, Neurology, 030220 oncology & carcinogenesis, Physiology (medical), Glioma, Biopsy, medicine, Surgery, Neurology (clinical), Radiology, Young adult, business, 030217 neurology & neurosurgery, Ethambutol, medicine.drug

Abstract

Introduction Diffuse midline glioma is a newly WHO defined entity (grade IV) (Louis et al., 2016) which includes diffuse intrinsic pontine glioma (DIPG) reported in pediatric population and, occasionally, in young adults. Here, we present a detailed description of an atypical case of diffuse midline glioma in a 53 years old woman. Case report A caucasian woman aged 53 from Ukraine, was referred to another neurological department complaining of 3 months history of progressive postural instability and gait impairment with frequent falling. Magnetic resonance demonstrated two brainstem lesions, hyperintense in FLAIR with “patchy” peripheral enhancement, leptomeningeal and cranial nerves enhancement. CSF was normal. Due to positive antinuclear antibodies test (ANA 1:360), intravenous steroid treatment was administered and reported to initially improve the patient condition. However, the following weeks the lady worsened. Imaging features were unchanged. Because quantiferon test resulted positive, MRI-Spectroscopy showed an inflammatory pattern and MRI perfusion study and brain FDG-PET, were normal, tubercolar granulomatous hypothesis was initially favored. Antitubercular therapy with isoniazid, pyrazinamide, ethambutol and rifampicin was started without any clinical improvement. Hence, the biopsy was proposed. The procedure revealed a diffuse midline pontine glioma. Considering the advanced stage of the disease, radiotherapy was not indicated. Patient died after eight months from the onset of neurological disturbances. Conclusion Our case shows that diffuse midline glioma is a CNS tumor not limited to young population but occurring also in middle aged patients with an insidious pattern. We therefore recommend to perform biopsy at very early stages in patients with atypical brainstem lesions.

Published

2020

12. Design and conduct of early clinical studies of immunotherapy agent combinations: recommendations from the task force on Methodology for the Development of Innovative Cancer Therapies

Author

M. Smoragiewicz, J. Bogaerts, E. Calvo, A. Marabelle, A. Perrone, L. Seymour, A. Shalabi, L.L. Siu, J. Tabernero, G. Giaccone, M. Atkins, U. Banerji, S. Bates, F. De Braud, J.Y. Douillard, P. Keegan, R. Kumar, P. LoRusso, F. Pignatti, R. Plummer, G. Schwartz, G. Shapiro, P. Therasse, and A. Yang

Subjects

medicine.medical_specialty, Biomedical Research, medicine.medical_treatment, Computed tomography, 03 medical and health sciences, 0302 clinical medicine, Neoplasms, Tumor Microenvironment, medicine, Humans, Medical physics, 030212 general & internal medicine, Practice Patterns, Physicians', Combination immunotherapy, Clinical Trials as Topic, medicine.diagnostic_test, Task force, business.industry, Surrogate endpoint, Patient Selection, Cancer, Hematology, Immunotherapy, medicine.disease, Clinical trial, Oncology, Research Design, 030220 oncology & carcinogenesis, Practice Guidelines as Topic, business, Early phase

Abstract

The Methodology for the Development of Innovative Cancer Therapies task force considered aspects of the design and conduct of early studies of combinations of immunotherapy agents during their 2018 meeting. The task force defined the relevant data to justify combination clinical trials, which includes a robust hypothesis for the combination, pre-clinical data with evidence of efficacy and an understanding of the pharmacodynamics effects of each agent, and ideally evidence of single agent activity. Evaluation of pharmacodynamic biomarkers is critical in early phase combination trials, and should be incorporated into trial objectives and go/no-go decisions. The task force also identified the need to develop assessment tools and end points that capture the unique patterns of tumour responses to immunotherapy, including pseudoprogression and hyperprogression. At least one additional tumour measurement before baseline and an early CT scan (at 4 weeks for example) would help define the incidence of hyperprogression, although a common definition is needed. Finally, the task force highlighted substantial redundancy and inefficiency in the combination immunotherapy space, and recommended the adoption of innovative trial designs.

Published

2018

13. Defective Differentiation of Myeloid and Plasmacytoid Dendritic Cells in Advanced Cancer Patients is not Normalized by Tyrosine Kinase Inhibition of the Vascular Endothelial Growth Factor Receptor

Author

T. D. de Gruijl, G. Giaccone, R. J. Scheper, H. van Cruijsen, K. Hoekman, B. C. Kuenen, A. J. M. van den Eertwegh, and A. G. M. Stam

Subjects

Immunologic diseases. Allergy, RC581-607

Published

2007

14. Phase 3, Randomized, Placebo-Controlled Study of Stereotactic Body Radiotherapy (SBRT) with or Without Pembrolizumab in Patients with Inoperable Stage I/IIA Non–Small-Cell Lung Cancer (NSCLC): KEYNOTE-867

Author

D. Kowalski, T. Wehler, Xavier Quantin, Andrew G. Robinson, Jin Zhang, G. Giaccone, Hossein Borghaei, M. Erman, F. Souza, Salma K. Jabbour, Roy H. Decker, B. Houghton, Myung-Ju Ahn, and J. McLean

Subjects

Cancer Research, medicine.medical_specialty, Radiation, business.industry, Placebo-controlled study, non-small cell lung cancer (NSCLC), Pembrolizumab, medicine.disease, Oncology, Medicine, Radiology, Nuclear Medicine and imaging, In patient, Radiology, business, Stereotactic body radiotherapy

Published

2020

15. 1260MO Activity of OSE-2101 in HLA-A2+ non-small cell lung cancer (NSCLC) patients after failure to immune checkpoint inhibitors (ICI): Step 1 results of phase III ATALANTE-1 randomised trial

Author

G. Giaccone, E. Felip, M. Cobo, R. Garcia Campelo, F. DENIS, E. Quoix, A. Madroszyk, D. Debieuvre, W. Hilgers, T. Moran, D. Galetta, G.D. Romano, F. Cappuzzo, G. Robinet, P. Masson, S. Viteri, N. Peled, D. Costantini, R. Dziadziuszko, and B. Besse

Subjects

Oncology, Hematology, Article

Published

2020

16. A phase III study of belagenpumatucel-L, an allogeneic tumour cell vaccine, as maintenance therapy for non-small cell lung cancer

Author

G. Giaccone, L.A. Bazhenova, J. Nemunaitis, M. Tan, E. Juhász, R. Ramlau, M.M. van den Heuvel, R. Lal, G.H Kloecker, K.D. Eaton, Q. Chu, D.J. Dunlop, M. Jain, E.B. Garon, C.S. Davis, E. Carrier, S.C. Moses, D.L. Shawler, and H. Fakhrai

Subjects

Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Lung Neoplasms, Time Factors, medicine.medical_treatment, Kaplan-Meier Estimate, Placebo, Cancer Vaccines, Disease-Free Survival, Maintenance Chemotherapy, Double-Blind Method, Maintenance therapy, Carcinoma, Non-Small-Cell Lung, Internal medicine, medicine, Clinical endpoint, Humans, Lung cancer, Aged, Proportional Hazards Models, Chemotherapy, Proportional hazards model, business.industry, Hazard ratio, Middle Aged, medicine.disease, Intention to Treat Analysis, Surgery, Belagenpumatucel-L, Treatment Outcome, Disease Progression, Female, business

Abstract

Background Treatment options after first-line chemotherapy are limited in non-small cell lung cancer (NSCLC). Belagenpumatucel-L is a therapeutic vaccine comprised of 4 transforming growth factor (TGF)-β2-antisense gene-modified, irradiated, allogeneic NSCLC cell lines that may be useful for maintenance after initial treatment. Methods Stage III/IV NSCLC patients who did not progress after platinum-based chemotherapy were randomised 1:1 to receive maintenance belagenpumatucel-L or placebo. Patients were eligible for randomisation between one and four months from the end of induction chemotherapy. The primary endpoint was overall survival. Results This phase III trial enrolled 270 patients in the belagenpumatucel-L arm and 262 in the control arm. Belagenpumatucel-L was well tolerated with no serious safety concerns. There was no difference in survival between the arms (median survival 20.3 versus 17.8months with belagenpumatucel-L versus placebo, respectively; hazard ratio (HR) 0.94, p =0.594). There were also no differences in progression-free survival (4.3months versus 4.0 for belagenpumatucel-L vs placebo, respectively; HR 0.99, p =0.947). A prespecified Cox regression analysis demonstrated that the time elapsed between randomisation and the end of induction chemotherapy had a significant impact on survival ( p =0.002) and that prior radiation was a positive prognostic factor (median survival 28.4months with belagenpumatucel-L versus 16.0months with placebo; HR 0.61, p =0.032). Conclusions Although the overall trial did not meet its survival endpoint, improved survival for belagenpumatucel-L is suggested in patients who were randomised within 12weeks of completion of chemotherapy and in those who had received prior radiation. Further studies of belagenpumatucel-L in NSCLC are warranted.

Published

2015

17. MS08.03 Optimal Management of Metastatic Thymic Carcinoma

Author

G. Giaccone

Subjects

Pulmonary and Respiratory Medicine, Oncology, business.industry, Metastatic thymic carcinoma, Cancer research, Medicine, business, Optimal management

Published

2019

18. Talactoferrin alfa versus placebo in patients with refractory advanced non-small-cell lung cancer (FORTIS-M trial)

Author

S. Ramalingam, J. Crawford, A. Chang, C. Manegold, R. Perez-Soler, J.-Y. Douillard, N. Thatcher, F. Barlesi, T. Owonikoko, Y. Wang, P. Pultar, J. Zhu, R. Malik, G. Giaccone, S. Della-Fiorentina, S. Begbie, R. Jennens, J. Dass, K. Pittman, N. Ivanova, T. Koynova, P. Petrov, A. Tomova, V. Tzekova, F. Couture, V. Hirsh, R. Burkes, R. Sangha, M. Ambrus, T. Janaskova, J. Musil, J. Novotny, P. Zatloukal, J. Jakesova, K. Klenha, J. Roubec, J. Vanasek, J. Fayette, J. Bennouna-Louridi, C. Chouaid, J. Mazières, H. Vallerand, G. Robinet, P.-J. Souquet, D. Spaeth, R. Schott, H. Lena, Y. Martinet, C. El Kouri, N. Baize, A. Scherpereel, O. Molinier, F. Fuchs, K.M. Josten, N. Marschner, F. Schneller, T. Overbeck, M. Thomas, J. von Pawel, M. Reck, W. Schuette, V. Hagen, C.-P. Schneider, V. Georgoulias, I. Varthalitis, K. Zarogoulidis, K. Syrigos, C. Papandreou, C. Bocskei, E. Csanky, E. Juhasz, G. Losonczy, Z. Mark, I. Molnar, Z. Papai-Szekely, S. Tehenes, I. Vinkler, S. Almel, A. Bakshi, S. Bondarde, A. Maru, A. Pathak, R.M. Pedapenki, K. Prasad, S.V.S.S. Prasad, N. Kilara, D. Gorijavolu, C.D. Deshmukh, S. John, L.M. Sharma, D. Amoroso, E. Bajetta, P. Bidoli, A. Bonetti, F. De Marinis, M. Maio, R. Passalacqua, S. Cascinu, A. Bearz, M. Bitina, A. Brize, G. Purkalne, M. Skrodele, A.A. Baba, K. Ratnavelu, M.H. Saw, M.C. Samson-Fernando, G.E. Ladrera, J. Jassem, P. Koralewski, P. Serwatowski, M. Krzakowski, C. Cebotaru, D. Filip, D.E. Ganea-Motan, C.H. Ianuli, I.G. Manolescu, A. Udrea, O. Burdaeva, M. Byakhov, A. Filippov, S. Lazarev, I. Mosin, S. Orlov, D. Udovitsa, A. Khorinko, S. Protsenko, H.L. Lim, Y.O. Tan, E.H. Tan, R. Bastus Piulats, J. Garcia-Foncillas, J. Valdivia, J. de Castro, M. Domine Gomez, S.W. Kim, J.-S. Lee, H.K. Kim, J.S. Lee, S.W. Shin, D.-W. Kim, Y.-C. Kim, K.C. Park, C.-S. Chang, G.-C. Chang, Y.-G. Goan, W.-C. Su, C.-M. Tsai, H.-P. Kuo, M. Benekli, G. Demir, E. Gokmen, A. Sevinc, M. Haigentz, M. Agarwal, S. Pandit, R. Araujo, N. Vrindavanam, P. Bonomi, A. Berg, J. Wade, R. Bloom, B. Amin, R. Camidge, D. Hill, M. Rarick, P. Flynn, L. Klein, K. Lo Russo, M. Neubauer, P. Richards, R. Ruxer, M. Savin, D. Weckstein, R. Rosenberg, T. Whittaker, D. Richards, W. Berry, C. Ottensmeier, A. Dangoor, N. Steele, Y. Summers, E. Rankin, K. Rowley, S. Giridharan, H. Kristeleit, C. Humber, P. Taylor, Ramalingam, S, Crawford, J, Chang, A, Manegold, C, Perez-Soler, R, Douillard, J, Thatcher, N, Barlesi, F, Owonikoko, T, Wang, Y, Pultar, P, Zhu, J, Malik, R, Giaccone, G, and Bidoli, P

Subjects

Male, medicine.medical_specialty, Population, Kaplan-Meier Estimate, Placebo, Gastroenterology, Disease-Free Survival, Drug Administration Schedule, Placebos, Double-Blind Method, Talactoferrin Alfa, Carcinoma, Non-Small-Cell Lung, Internal medicine, Talactoferrin, Humans, Medicine, Phase III study, Progression-free survival, education, Lung cancer, Survival rate, Aged, Neoplasm Staging, education.field_of_study, business.industry, Surrogate endpoint, Hazard ratio, Hematology, Middle Aged, medicine.disease, Surgery, oral dendritic cell (DC)-mediated immunotherapy, Lactoferrin, Treatment Outcome, Oncology, Female, Immunotherapy, Immunotherapy, Non-small-cell lung cancer, Phase III study, Talactoferrin, business, Non-small-cell lung cancer

Abstract

Background Talactoferrin alfa is an oral dendritic cell (DC)-mediated immunotherapy (DCMI). We tested whether talactoferrin was superior to placebo in advanced non-small-cell lung cancer (NSCLC). Patients and methods An FORTIS-M trial was an international, multicenter, randomized, double-blind comparison of talactoferrin (1.5g p.o. BID) versus placebo BID, in patients with stage IIIB/IV NSCLC whose disease had failed two or more prior regimens. Treatment was administered for a maximum of five 14-week cycles. The primary efficacy end point was overall survival (OS); secondary end points included 6- and 12-month survival, progression-free survival (PFS), and disease control rate (DCR). Results Seven hundred and forty-two patients were randomly assigned (2:1) to talactoferrin (497) or placebo (245). The median OS in the intent-to-treat (ITT) population was 7.66 months in the placebo arm and 7.49 months in the talactoferrin arm [hazard ratio (HR), 1.04; 95% CI, 0.873–1.24; P = 0.6602]. The 6-month survival rates were 59.9% (95% CI, 53.4% to 65.8%) and 55.7% (95% CI, 51.1% to 59.9%), respectively. The 12-month survival rates were 32.2% (95% CI, 26.3% to 38.2%) and 30.9% (95% CI, 26.8% to 35%), respectively. The median PFS rates were 1.64 months and 1.68 months, respectively (HR, 0.99; 95% CI, 0.835–1.16; P = 0.8073). The DCRs were 38.4 and 37.6%, respectively [stratified odds ratio (OR), 0.96; 95% CI, 0.698–1.33; P = 0.8336]. The safety profiles were comparable between arms. Conclusions There was no improvement in efficacy with talactoferrin alfa in patients with advanced NSCLC whose disease had failed two or more previous regimens.

Published

2013

19. Reproducibility of the WHO classification of thymomas: Practical implications

Author

Massimo Roncalli, Emanuele Voulaz, Iacopo Petrini, G. Giaccone, L. Di Tommaso, Armando Santoro, Paolo Andrea Zucali, Marco Alloisio, Serena Battista, Laura Giordano, Matteo Simonelli, Maria J. Merino, F. De Vincenzo, Elena Lorenzi, and Hye Seung Lee

Subjects

Adult, Male, Pulmonary and Respiratory Medicine, Cancer Research, medicine.medical_specialty, Pathology, Disease free survival, Consensus, Thymoma, Consensus Development Conferences as Topic, Thymomas, World Health Organization, Article, Disease-Free Survival, Young Adult, 80 and over, medicine, Humans, Practical implications, Aged, Neoplasm Staging, Aged, 80 and over, WHO classification, Reproducibility, business.industry, Reproducibility of Results, Large series, Middle Aged, Prognosis, medicine.disease, Oncology, Female, Practice Guidelines as Topic, Neoplasm staging, Radiology, Who classification, business

Abstract

The WHO-classification was shown to be an independent prognostic marker in some but not all retrospective studies possibly due to lack of reproducibility. We investigated the reproducibility of the WHO-classification and its prognostic implication using a large series of resected thymomas.Four independent pathologists histologically classified a surgical series of 129 thymic tumors in a blinded fashion. Fleiss' kappa-coefficient was used to assess the pathologists' overall agreement, and Cohen-Kappa to assess the agreement between two observers. Disease-related-survival (DRS) and progression-free-survival (PFS) curves were generated by Kaplan-Meier method and compared by log-rank test.In 63/129 (48.8%) cases there was a complete agreement; in 43/129 (33.3%) cases 3/4 pathological diagnoses were identical; in 15/129 (11.6%) cases the diagnoses were identical by pair; in 8/129 (6.2%) cases three different pathological diagnoses were on record. The Kappa-correlation coefficient was only moderate (0.53). A following web review carried out on the 23 cases with at least two different diagnoses reached a complete consensus. The histotype showed a statistically significant impact on PFS and DRS in the classification provided by only two pathologists.In this study, the agreement on WHO classification of thymomas was only moderate and this impacted on patients management. Web consensus conference on the diagnosis, more stringent diagnostic criteria or the adoption of referral diagnostic centres may substantially reduce discrepancies.

Published

2013

20. Lectures

Author

D. S. Chen, D. M. Feltquate, F. Smothers, A. Hoos, S. Langermann, S. Marshall, R. May, M. Fleming, F. S. Hodi, A. Senderowicz, K. G. Wiman, S. de Dosso, W. Fiedler, L. Gianni, S. Cresta, H. B. Schulze-Bergkamen, L. Gurrieri, M. Salzberg, B. Dietrich, A. Danielczyk, H. Baumeister, S. Goletz, C. Sessa, D. Strumberg, B. Schultheis, A. Santel, F. Gebhardt, W. Meyer-Sabellek, O. Keil, K. Giese, J. Kaufmann, M. Maio, G. Choy, A. Covre, G. Parisi, H. Nicolay, E. Fratta, E. Fonsatti, L. Sigalotti, S. Coral, P. Taverna, M. Azab, E. Deutsch, C. Lepechoux, J. P. Pignon, Y. T. Tao, S. Rivera, B. C. Bourgier, M. Angokai, R. Bahleda, K. Slimane, E. Angevin, B. B. Besse, J. C. Soria, K. Dragnev, J. H. Beumer, B. Anyang, T. Ma, F. Galimberti, C. P. Erkmen, W. Nugent, J. Rigas, K. Abraham, D. Johnstone, V. Memoli, E. Dmitrovsky, E. E. Voest, L. Siu, F. Janku, A. Tsimberidou, R. Kurzrock, J. Tabernero, J. Rodon, R. Berger, A. Onn, G. Batist, C. Bresson, V. Lazar, J. J. Molenaar, J. Koster, M. Ebus, D. A. Zwijnenburg, P. van Sluis, F. Lamers, L. Schild, I. van der Ploeg, H. N. Caron, R. Versteeg, J. Pouyssegur, I. Marchiq, J. Chiche, D. Roux, R. Le Floch, S. E. Critchlow, R. F. Wooster, S. Agresta, K. E. Yen, P. A. Janne, E. R. Plummer, G. Trinchieri, L. Ellis, S. L. Chan, W. Yeo, A. T. Chan, F. Mouliere, S. El Messaoudi, C. Gongora, P. J. Lamy, M. del Rio, E. Lopez-Crapez, B. Gillet, M. Mathonnet, D. Pezet, M. Ychou, A. R. Thierry, V. Ribrag, W. Vainchenker, S. Constantinescu, H. Keilhack, I. A. Umelo, A. Noeparast, G. Chen, M. Renard, C. Geers, J. Vansteenkiste, E. Teugels, J. de Greve, O. Rixe, X. Qi, Z. Chu, J. Celerier, L. Leconte, N. Minet, J. Pakradouni, B. Kaur, F. Cuttitta, A. J. Wagner, Y. X. Zhang, E. Sicinska, J. T. Czaplinski, S. P. Remillard, G. D. Demetri, S. Weng, L. Debussche, L. Agoni, E. P. Reddy, C. Guha, K. Silence, A. Thibault, H. de Haard, T. Dreier, P. Ulrichts, M. Moshir, S. Gabriels, J. Luo, C. Carter, A. Rajan, S. Khozin, A. Thomas, A. Lopez-Chavez, C. Brzezniak, L. Doyle, C. Keen, M. Manu, M. Raffeld, G. Giaccone, S. Lutzker, J. M. Melief, S. G. Eckhardt, L. Trusolino, G. Migliardi, E. R. Zanella, F. Cottino, F. Galimi, F. Sassi, S. Marsoni, P. M. Comoglio, A. Bertotti, M. Hidalgo, S. J. Weroha, P. Haluska, M. A. Becker, S. C. Harrington, K. M. Goodman, S. E. Gonzalez, M. al Hilli, K. A. Butler, K. R. Kalli, A. L. Oberg, I. J. Huijbers, R. Bin Ali, C. Pritchard, M. Cozijnsen, N. Proost, J. Y. Song, P. Krimpenfort, E. Michalak, J. Jonkers, A. Berns, U. Banerji, A. Stewart, P. Thavasu, S. Banerjee, and S. B. Kaye

Subjects

Oncology, Hematology

Published

2013

21. P2.12-03 Phase I/II Trial Of 177Lu-DOTA0-Tyr3-Octreotate (Lutathera) And Nivolumab for Patients with Extensive-Stage Small Cell Lung Cancer (ES-SCLC)

Author

G. Giaccone, Chul Kim, D. Subramaniam, and Stephen V. Liu

Subjects

0301 basic medicine, Pulmonary and Respiratory Medicine, Oncology, medicine.medical_specialty, business.industry, 177Lu-DOTA0-Tyr3-Octreotate, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Phase i ii, 030220 oncology & carcinogenesis, Internal medicine, medicine, Nivolumab, business, Extensive-stage small cell lung cancer

Published

2018

22. P1.01-47 Phase I/II Trial of Dasatinib and Osimertinib in Patients with Advanced EGFR-Mutant Non-Small Cell Lung Cancer (NSCLC)

Author

Chul Kim, D. Subramaniam, G. Giaccone, and Stephen V. Liu

Subjects

Pulmonary and Respiratory Medicine, business.industry, Mutant, non-small cell lung cancer (NSCLC), medicine.disease, Dasatinib, 03 medical and health sciences, 0302 clinical medicine, Phase i ii, 030228 respiratory system, Oncology, 030220 oncology & carcinogenesis, Cancer research, Medicine, Osimertinib, In patient, business, medicine.drug

Published

2018

23. A phase I and pharmacokinetic study of gemcitabine given by 24-h hepatic arterial infusion

Author

A.C. Laan, C. J. van Groeningen, R. Ruyter, J. M. G. H. Van Riel, Richard J. Honeywell, Lemonitsa H. Mammatas, F.G. van den Berg, G.J. Peters, G. Giaccone, Medical oncology, Medical oncology laboratory, Radiology and nuclear medicine, and CCA - Innovative therapy

Subjects

Adult, Male, Antimetabolites, Antineoplastic, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, medicine.drug_class, medicine.medical_treatment, Cmax, Deoxycytidine, Gastroenterology, Antimetabolite, chemistry.chemical_compound, Hepatic Artery, Hepatic arterial infusion, Pharmacokinetics, Internal medicine, medicine, Humans, Infusions, Intra-Arterial, Infusions, Intravenous, Aged, Chemotherapy, business.industry, Liver Neoplasms, Middle Aged, Thrombocytopenia, Gemcitabine, Treatment Outcome, Endocrinology, Oncology, chemistry, Toxicity, Female, business, medicine.drug

Abstract

This study was performed to assess the toxicities, the maximum-tolerated dose (MTD), the pharmacokinetics and the anti-tumour activity of gemcitabine given by 24-h hepatic arterial infusion (HAI).Patients with liver malignancies received gemcitabine by 24-h HAI, weekly x 3, every 4 weeks. On day 1 or day 8 of the first cycle, patients received one administration by 24-h intravenous infusion for pharmacokinetic comparison and to determine hepatic extraction.Thirteen patients received gemcitabine at the dose levels of 75, 135 and 180 mg/m(2). The MTD was 180 mg/m(2) with thrombocytopaenia as the dose-limiting toxicity. Pharmacokinetic analysis showed a significantly lower maximum gemcitabine plasma concentration (C(max): HAI, 26, 80 and 128 nM, respectively; IV, 229, 264 and 293 nM, respectively) and area under the plasma-concentration-versus-time curve (AUC(0-24h): HAI, 386, 1247 and 2033 nmol x h/L, respectively; IV, 3526, 4818 and 5363 nmol x h/L, respectively) during HAI, compared with intravenous infusion (both P0.001). Additionally, the mean hepatic extraction ratios of gemcitabine at the 75, 135 and 180 mg/m(2) dose level were 0.89, 0.75 and 0.55, respectively. Hepatic extraction decreased linearly with increasing dose. The C(max) and AUC(0-24h) of 2',2'-difluoro-2'-deoxyuridine, the deaminated product of gemcitabine, were similar for HAI and intravenous infusion. Seven patients had stable disease for a median duration of 9 months (range: 2-11 months).Gemcitabine given by 24-h HAI was well tolerated and resulted in significantly lower systemic gemcitabine plasma concentrations than intravenous infusion due to a relatively high hepatic extraction.

Published

2009

24. Src as a potential therapeutic target in non-small-cell lung cancer

Author

G. Giaccone and P.A. Zucali

Subjects

Oncology, medicine.medical_specialty, Lung Neoplasms, business.industry, Angiogenesis, medicine.medical_treatment, Cancer, Hematology, Disease, medicine.disease_cause, medicine.disease, Models, Biological, Targeted therapy, src-Family Kinases, Carcinoma, Non-Small-Cell Lung, Internal medicine, Immunology, medicine, Humans, Carcinogenesis, business, Lung cancer, Tyrosine kinase, Proto-oncogene tyrosine-protein kinase Src

Abstract

Lung cancer is the most common cause of cancer-related death, with non-small-cell lung cancer (NSCLC) accounting for 80%-85% of all cases. Although survival rates are reasonably good for patients diagnosed with very early disease, the majority of patients present with advanced disease. For these patients, palliation and improvements in quality of life are the primary goals of therapy. Although chemotherapeutic agents remain the cornerstone of first-line therapy, these agents have limited use in patients who have relapsed and have metastatic disease. Therefore, new strategies are required to improve survival and quality of life in this setting. With the substantial advances in our understanding of tumour biology, it has been possible to identify signalling pathways involved in mediating tumour growth and progression. These pathways offer targets for new biological agents such as small molecule inhibitors and monoclonal antibodies. One such target is Src, a tyrosine kinase that is involved in multiple aspects of tumorigenesis including proliferation, migration and angiogenesis. Increased levels of Src expression have been found in a range of cancers, especially breast, colorectal, prostate and lung. Preliminary preclinical data and pharmacodynamic data suggest that Src inhibition is a viable therapeutic option in the treatment of advanced NSCLC.

Published

2008

25. Review of taxonomy situation of marine vegetables in Mediterranean Countries within the Mediterranean Initiative on Taxonomy (MIT)

Author

G. Giaccone

Subjects

Mediterranean climate, Convention on Biological Diversity, Ecology, business.industry, Environmental resource management, Marine botany, Geography, Environmental protection, Aquatic environment, General Earth and Planetary Sciences, Mediterranean area, Taxonomy (biology), business, Ecology, Evolution, Behavior and Systematics, General Environmental Science

Abstract

The Project of the Mediterranean Initiative on Taxonomy (MIT) aims at carrying out in the Mediterranean area the objectives of the Global Taxonomy Initiative (GTI), within the outline of the Convention on Biological Diversity (CBD). As an exemplification the present work reports, through the knowledge on vegetable taxonomy, an evaluation of the state of taxonomy of marine vegetable organisms in the Mediterranean Countries and in particular in Italy. An accurate evaluation on the state of taxonomy of the marine vegetable organisms in the Mediterranean Countries needs data collection from scientists and scientific organisations operating within every single Nation. Available statistical data on the distribution of Phycologists in the Mediterranean area, shows a significant but not always sufficient number of specialists according to the development of the coastal area in Spain, France, Italy, Greece, Turkey, Russia, Romania, and Israel. Qualified presences can also be found in Egypt and Tunisia. All Countri...

Published

2008

26. Early Intervention with Epoetin Alfa During Platinum-Based Chemotherapy: An Analysis of Quality-of-Life Results of a Multicenter, Randomized, Controlled Trial Compared with Population Normative Data

Author

Cees J. van Groeningen, G. Giaccone, L.W. Wormhoudt, and Jorine H. Savonije

Subjects

Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Anemia, medicine.medical_treatment, education, Population, Antineoplastic Agents, Platinum Compounds, law.invention, Hemoglobins, Randomized controlled trial, Quality of life, Reference Values, law, Neoplasms, Sickness Impact Profile, Internal medicine, medicine, Humans, Erythropoietin, Fatigue, Aged, Chemotherapy, education.field_of_study, business.industry, Epoetin alfa, Cancer, Middle Aged, medicine.disease, Recombinant Proteins, Epoetin Alfa, Treatment Outcome, Hematinics, Quality of Life, Physical therapy, Normative, Female, business, medicine.drug

Abstract

To evaluate the effect of epoetin alfa on quality of life (QOL) in patients with solid tumors and mild-to-moderate anemia receiving platinum-based chemotherapy relative to population norms.In the original study, patients (n = 316) with hemoglobin (Hb) levelsor =12.1 g/dl were randomized 2:1 to receive either epoetin alfa at a dose of 10,000 U thrice weekly s.c. or best supportive care (BSC) to compare the effects on transfusion use, hematologic response, and QOL (measured by the Functional Assessment of Cancer Therapy-Anemia [FACT-An]and Cancer Linear Analogue Scale [CLAS]). The QOL data from this previously reported trial were reanalyzed here relative to population norms.Mean baseline QOL scores were similar between groups. At study completion, mean CLAS, FACT-An, FACT-An Anemia subscale, and FACT-An Fatigue subscale scores were significantly higher for patients given epoetin alfa than for those treated with BSC. Compared with population norms, both groups had impaired QOL at baseline. Differences in mean QOL change scores from baseline to study end for epoetin alfa versus BSC were 3.17 points for the FACT-General Total, 9.90 for the FACT-An Fatigue subscale, and 7.30 for the FACT-An Anemia subscale. This was equivalent to corrections in QOL deficits attributable to epoetin alfa of 97.3%, 40.7%, and 38.0% for the FACT-General Total, FACT-An Fatigue, and FACT-An Anemia subscale scores, respectively, versus BSC. A somewhat greater QOL benefit was observed for the FACT-An Fatigue and FACT-An Anemia subscales in the subset of patients with baseline Hb levels10.5 g/dl.Patients in this study had impaired QOL compared with population norms. Early treatment with epoetin alfa to correct anemia improved QOL in a statistically significant and clinically meaningful way, and improvements were greater in patients with baseline Hb levels10.5 g/dl.

Published

2006

27. Early Intervention with Epoetin Alfa During Platinum-Based Chemotherapy: An Analysis of the Results of a Multicenter, Randomized, Controlled Trial Based on Initial Hemoglobin Level

Author

G. Giaccone, L.W. Wormhoudt, Cees J. van Groeningen, and Jorine H. Savonije

Subjects

Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Blood transfusion, Anemia, medicine.medical_treatment, education, Antineoplastic Agents, Platinum Compounds, law.invention, Hemoglobins, Quality of life, Randomized controlled trial, law, Neoplasms, Sickness Impact Profile, Internal medicine, medicine, Humans, Blood Transfusion, Erythropoietin, Fatigue, Aged, Chemotherapy, business.industry, Epoetin alfa, Cancer, Middle Aged, medicine.disease, Recombinant Proteins, Surgery, Epoetin Alfa, Treatment Outcome, Hematinics, Quality of Life, Female, business, medicine.drug

Abstract

This analysis of the results of a randomized, controlled trial evaluating the effects of epoetin alfa (EPO) therapy on transfusion requirements, hemoglobin (Hb), and quality of life (QOL) in patients with cancer receiving platinum-based chemotherapy was conducted to evaluate the effect of initial Hb level on study outcomes.Patients with Hb levelsor =12.1 g/dl were randomized 2:1 to receive EPO, 10,000 U three times weekly s.c. or best supportive care (BSC) until 4 weeks after their last chemotherapy cycle. For this analysis, patients were stratified by baseline Hb level (or =9.7 g/dl,9.7 g/dl toor =10.5 g/dl,10.5 g/dl toor =11.3 g/dl, and11.3 g/dl toor =12.1 g/dl), and study results were reanalyzed.Significantly fewer EPO patients than BSC patients with initial Hb levels9.7 g/dl toor =12.1 g/dl required transfusions. EPO maintained Hb levels throughout the study for patients with Hb levels11.3 g/dl toor =12.1 g/dl, compared with a decrease with BSC. For patients with baseline Hb levels10.5 g/dl, for whom the mean changes from baseline to last assessment were measured by the Cancer Linear Analogue Scale assessments of energy and overall QOL as well as by the Functional Assessment of Cancer Therapy (FACT)-Fatigue and FACT-An Anemia subscale, QOL scores were significantly greater with EPO than with BSC. QOL declined in patients receiving BSC, and the mean decreases in QOL scores were greater for BSC patients with baseline Hb levels10.5 g/dl, compared with the overall BSC group.In patients with cancer receiving platinum-based chemotherapy and with baseline Hb levels10.5 g/dl, early intervention with EPO reduces transfusions, maintains Hb level, and maintains or improves QOL. This study supports the positive effects of early intervention when analyzed according to initial Hb value.

Published

2006

28. Phase II study of tailored chemotherapy for advanced colorectal cancer with either 5-fluouracil and leucovorin or oxaliplatin and irinotecan based on the expression of thymidylate synthase and dihydropyrimidine dehydrogenase

Author

G. Giaccone, G.J. Peters, C. H. Smorenburg, W. W. Dercksen, P. Noordhuis, A. M. G. H. van Riel, Herbert M. Pinedo, Kees Smid, and C. J. van Groeningen

Subjects

Adult, Male, medicine.medical_specialty, Organoplatinum Compounds, Population, Leucovorin, Irinotecan, Thymidylate synthase, Gastroenterology, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Dihydropyrimidine dehydrogenase, Humans, Prospective Studies, RNA, Messenger, education, Dihydrouracil Dehydrogenase (NADP), Aged, education.field_of_study, Predictive marker, biology, Reverse Transcriptase Polymerase Chain Reaction, business.industry, Thymidylate Synthase, Hematology, Middle Aged, Prognosis, Chemotherapy regimen, Surgery, Oxaliplatin, Survival Rate, Oncology, Fluorouracil, biology.protein, Camptothecin, Female, Colorectal Neoplasms, business, medicine.drug

Abstract

Background: Thymidylate synthase (TS) and dihydropyrimidine dehydrogenase (DPD) are essential enzymes for 5-fluorouracil (5-FU) metabolism. In patients with advanced colorectal cancer (ACRC), retrospective studies have shown that low expression levels of TS and DPD correlated with response to 5-FU. We performed a prospective study in which the choice of first-line chemotherapy with either 5-FU or a non-5-FU containing regimen was based on TS and DPD expression. Patients and methods: Fresh-frozen samples of metastases were obtained from 58 previously untreated patients with ACRC. mRNA expression of TS and DPD was quantified using an RT–PCR assay. Patients with low tumor expression of both TS and DPD received weekly bolus 5-FU/leucovorin (LV) 500 mg/m2 (group A); patients with high TS and/or DPD received 3-weekly oxaliplatin 85 mg/m2 and irinotecan 200 mg/m2 (group B). After progression, cross-over to the alternative regimen was attempted. Results: Of 53 eligible patients, 31 had tumors with both low TS and low DPD, and were treated in group A. A response was observed in 11 patients [35%; 95% confidence interval (CI) 19% to 54%]. Cross-over to second-line oxaliplatin/irinotecan resulted in a partial response in two out of 16 patients (13%; 95% CI 1% to 38%). In group B, four out of 22 patients responded (18%; 95% CI 5% to 40%), while no responses were observed in 12 patients after cross-over to 5-FU/LV (0%; 95% CI 0% to 28%). Conclusions: Prospective selection of 5-FU/LV chemotherapy based on low TS and DPD expression in patients with ACRC did not confirm the high response rates reported in retrospective studies. The procedure of obtaining metastatic tissue and quantitation of enzymes appeared feasible but cumbersome. Before assessing the clinical utility of a predictive marker in a randomized trial, future studies should focus on prospective validation of the assay in a large and well defined population.

Published

2006

29. Recombinant human endostatin administered as a 28-day continuous intravenous infusion, followed by daily subcutaneous injections: a phase I and pharmacokinetic study in patients with advanced cancer

Author

Epie Boven, G. Giaccone, H.M. Pinedo, I. van der Horst, Klaas Hoekman, A. H. G. Hansma, Yuana Yuana, H. J. Broxterman, and VU University medical center

Subjects

Adult, Male, Angiogenesis, Injections, Subcutaneous, Pharmacology, Drug Administration Schedule, Pharmacokinetics, Neoplasms, Humans, Medicine, In patient, Dosing, Infusions, Intravenous, Aged, business.industry, Hematology, Middle Aged, Advanced cancer, Recombinant Proteins, Endostatins, Treatment Outcome, Oncology, Area Under Curve, Toxicity, Female, Endostatin, business, Perfusion

Abstract

Background: Endostatin is an endogenous collagen XVIII-fragment with anti-angiogenic properties and remarkable antitumor activity in mice. Preclinical data suggest that continuous low dose administration of endostatin is much more potent than intermittent dosing. The feasibility of this approach is tested in a phase I study. Patients and methods: We determined the safety and pharmacokinetic profile of 4-week continuous intravenous infusion of recombinant human (rh)-endostatin, followed after an interval of 1 week by twice daily subcutaneous injections in patients with advanced cancer. Thirty-two patients received rh-endostatin in six dosing cohorts, ranging from 3.75 mg/m2/day to 120 mg/m2/day. Serum endostatin pharmacokinetics, toxicity and antitumor response were determined. Results: A total of 160 cycles were delivered without significant toxicities. Pharmacokinetic analysis showed a linear increase of steady-state serum endostatin concentrations with dose (i.v. r2 = 0.96; s.c. r2 = 0.99) reaching 300–1000 ng/ml for the two highest doses, with considerable interpatient variation. The main pharmacokinetic values for both routes of administration were similar. The apparent steady-state concentration and AUC reached at 60–120 mg/m2/day were within the range expected to induce anti-angiogenic and antitumor effects based on preclinical tumor models. Although no objective responses were observed, two patients had long-lasting stable disease (defined as a tumor increase Conclusion: rh-endostatin was safely administered both by continuous infusion and by twice daily subcutaneous injections up to 120 mg/m2/day. Predictable pK was seen in this dose range and the target endostatin levels were reached from 60 mg/m2/day and above.

Published

2005

30. Medical treatment of non-small-cell lung cancer

Author

Jan Buter and G. Giaccone

Subjects

Oncology, medicine.medical_specialty, Lung Neoplasms, Cetuximab, Antineoplastic Agents, Antibodies, Monoclonal, Humanized, Erlotinib Hydrochloride, Carcinoma, Non-Small-Cell Lung, Internal medicine, Epidemiology of cancer, Humans, Medicine, Lung cancer, Protein Kinase Inhibitors, Medical treatment, business.industry, Respiratory disease, Antibodies, Monoclonal, Cancer, Gefitinib, Hematology, medicine.disease, ErbB Receptors, Chemotherapy, Adjuvant, Quinazolines, Non small cell, business, medicine.drug

Published

2005

31. Phase I and pharmacokinetic study of the novel chemoprotector BNP7787 in combination with cisplatin and attempt to eliminate the hydration schedule

Author

Epie Boven, I Zegers, C. J. van Groeningen, M Westerman, W.J.F. van der Vijgh, Miranda Verschraagen, G. Giaccone, and R. Ruijter

Subjects

Adult, Male, Cancer Research, medicine.medical_specialty, Nausea, medicine.medical_treatment, Urology, cisplatin, Pharmacology, Nephrotoxicity, Pharmacokinetics, Neoplasms, Antineoplastic Combined Chemotherapy Protocols, Clinical Studies, medicine, Humans, Saline, Mesna, Cisplatin, Dehydration, business.industry, Middle Aged, phase I, saline hydration, BNP7787, Oncology, Toxicity, Vomiting, mesna, Female, Kidney Diseases, medicine.symptom, business, pharmacokinetics, medicine.drug

Abstract

BNP7787 (disodium 2,2'-dithio-bis-ethane sulphonate; Tavocept) is a novel agent developed to protect against cisplatin (cis-diammine-dichloroplatinum(II))-associated chronic toxicities. In this study, we determined the recommended dose of BNP7787 when preceding a fixed dose of cisplatin, the pharmacokinetics (PKs) and the possible reduction of saline hydration. Patients with advanced solid tumours received BNP7787 in escalating doses of 4.1-41 g m(-2) as a 15-min intravenous (i.v.) infusion followed by cisplatin 75 mg m(-2) as a 60-min i.v. infusion together with pre- and postcisplatin saline hydration in a volume of 2200 ml; cycles were repeated every 3 weeks. PK was carried out using BNP7787, cisplatin and the combination. Twenty-five patients were enrolled in stage I of the study to determine the recommended dose of BNP7787. No dose-limiting toxicity was reached. The highest dose level of 41 g m(-2) resulted in a low incidence of grade 2 toxicities, being nausea and vomiting, dry mouth or bad taste and i.v. injection site discomfort. Doses of BNP7787or = 18.4 g m(-2) did not show a drug interaction between BNP7787 and cisplatin. In stage II of the study, patients received a fixed dose of BNP7787 of 18.4 g m(-2) preceding cisplatin and were entered in prespecified reduced saline hydration steps. A total of 21 patients in cohorts of six to nine patients received reduced saline hydration of 1600 ml (step A), 1000 ml (step B) and 500 ml (step C). In step C, two out of six evaluable patients experienced grade 1 nephrotoxicity. Cisplatin acute toxicities in all 46 patients were as expected. Only five patients complained of paresthesias grade 1 and six developed slight audiometric changes. Partial tumour response was observed in four patients and stable disease in 15 patients. In conclusion, BNP7787 was tolerated well up to doses of 41 g m(-2). The recommended dose of 18.4 g m(-2) enabled safe reduction of the saline hydration schedule for cisplatin to 1000 ml. Further studies will assess whether BNP7787 offers protection against platinum-related late side effects.

Published

2005

32. Cryptobenthic fishes of the 'Ciclopi Islands' marine reserve (central Mediterranean Sea): assemblage composition, structure and relations with habitat features

Author

G. Giaccone, M. Micalizzi, Marino Vacchi, and G. La Mesa

Subjects

geography, geography.geographical_feature_category, Ecology, biology, Scorpaenidae, Marine reserve, Species diversity, Aquatic Science, biology.organism_classification, Rocky shore, Mediterranean sea, Oceanography, Archipelago, Gobiesocidae, Species richness, Ecology, Evolution, Behavior and Systematics

Abstract

The fish assemblage of the “Ciclopi Islands” marine reserve, which is located along the eastern coast of Sicily (Central Mediterranean), was unknown until our study provided insight into the cryptobenthic fish assemblage inhabiting this integral reserve zone. Visual census surveys were periodically conducted along the littoral rocky shores of Lachea, the largest island of the Ciclopi archipelago. The fish assemblage, which comprised 20 species belonging to Blenniidae, Gobiidae, Tripterygiidae, Scorpaenidae and Gobiesocidae, was dominated by Scorpaena maderensis and Trypterigion delaisi. Species richness (S) did not show significant differences between the northern, eastern, southern and western island coasts, whereas both species diversity (H′) and evenness (J) were significantly higher on the western coast than on the northern coast. The effect of the island coast on fish density was not significant with regard to the whole assemblage or to single species, except for S. maderensis and T. delaisi. The pattern of variation of assemblage parameters was mainly positively correlated with microhabitat variables, especially substratum composition and type of cover. The best predictors of fish total density were bottom slope, rugosity and substratum composition. Variations in relative species density were specified by a different combination of macro- and microhabitat variables. The density pattern of S. maderensis showed a positive relationship with depth. In T. delaisi, the influence of slope was interrelated to that of exposure to waves. This species preferentially inhabited flat habitat, sheltered from the open sea and covered by small boulders, but also more-exposed rockwalls. The population densities of Tripterygion melanurus and Lipophrys trigloides were negatively affected by depth, thus reflecting their preference for the upper infralittoral. T. melanurus was associated with a more complex habitat (stones and boulders), whereas L. trigloides was mainly censused on a narrow strip of solid rock between the waterline and 1 m depth.

Published

2004

33. Phase II trial of cisplatin and gemcitabine in patients with advanced gastric cancer

Author

Godefridus J. Peters, Judith R. Kroep, A. van Bochove, G. Giaccone, H.M. Pinedo, C.J. van Groeningen, J. F. Snijders, S.M. de Lange, and VU University medical center

Subjects

Adult, Male, medicine.medical_specialty, Maximum Tolerated Dose, Nausea, medicine.drug_class, Phases of clinical research, Adenocarcinoma, Gastroenterology, Antimetabolite, Deoxycytidine, Stomach Neoplasms, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Aged, Neoplasm Staging, Salvage Therapy, Leukopenia, business.industry, Hematology, Middle Aged, Gemcitabine, Surgery, Survival Rate, Regimen, Treatment Outcome, Oncology, Toxicity, Vomiting, Female, medicine.symptom, Cisplatin, business, medicine.drug

Abstract

Background This phase II study was performed to determine the efficacy and toxicity of cisplatin and gemcitabine in patients with advanced gastric cancer. Patients and methods Forty chemo-naive patients with measurable locoregionally advanced or metastatic gastric cancer were included; the median patient age was 53 years (range 35–71). Cisplatin was administered at a dose of 50 mg/m2, given in 1 h intravenously (i.v.) on days 1 and 8, followed after 24 h by gemcitabine at a dose of 800 mg/m2 given in 30 min i.v. on days 2, 9 and 16, every 28 days. Results A median number of four therapy cycles were given (range 2–8). Myelosuppresion was the most important toxicity. Grade 3–4 thrombopenia was observed in 19 patients (48%) and grade 3–4 leukopenia was observed in 23 (58%). Myelotoxicity was cumulative and caused omission of gemcitabine on day 16 in 55% of cycles. Non-haematological toxicity consisted mainly of grade 1–2 nausea and vomiting. Objective responses were observed in 30% of patients including two complete remissions and 10 partial remissions. Median survival was 11 months (range 3–27+). Conclusions This cisplatin–gemcitabine regimen had moderate efficacy in patients with advanced gastric cancer, with manageable toxicity. Further studies with this combination may be warranted.

Published

2004

34. Pharmacokinetics of S-1, an oral formulation of ftorafur, oxonic acid and 5-chloro-2,4-dihydroxypyridine (molar ratio 1:0.4:1) in patients with solid tumors

Author

S. L. Turner, M. Swart, Jantien Wanders, G.J. Peters, Kees Smid, C. J. van Groeningen, A. H. van Gennip, Helen Gall, P. Noordhuis, A. B. P. Van Kuilenburg, Pierre Fumoleau, Jan H. Schornagel, G. Giaccone, U. Holwerda, D. Voorn, AGEM - Amsterdam Gastroenterology Endocrinology Metabolism, CCA -Cancer Center Amsterdam, and Laboratory Genetic Metabolic Diseases

Subjects

Adult, Male, Antimetabolites, Antineoplastic, Cancer Research, Metabolic Clearance Rate, Pyridines, Cmax, Biological Availability, Pharmacology, Toxicology, Tegafur, chemistry.chemical_compound, Pharmacokinetics, Oral administration, Neoplasms, medicine, Dihydropyrimidine dehydrogenase, Humans, Tissue Distribution, Pharmacology (medical), Uracil, Aged, Dose-Response Relationship, Drug, Middle Aged, Prodrug, Drug Combinations, Oxonic Acid, Oncology, chemistry, Biochemistry, Fluorouracil, Area Under Curve, Female, Half-Life, medicine.drug

Abstract

S-1 is an oral formulation of ftorafur (FT), oxonic acid and 5-chloro-2,4-dihydroxypyridine (CDHP) at a molar ratio of 1:0.4:1. FT is a 5-fluorouracil (5-FU) prodrug, CDHP is a dihydropyrimidine dehydrogenase (DPD) inhibitor and oxonic acid is an inhibitor of 5-FU phosphoribosylation in the gastrointestinal mucosa and was included to prevent gastrointestinal toxicity. We determined the pharmacokinetics of S-1 in 28 patients at doses of 25, 35, 40 and 45 mg/m(2). The plasma C(max) values of FT, 5-FU, oxonic acid and CDHP increased dose-dependently and after 1-2 h were in the ranges 5.8-13 microM, 0.4-2.4 microM, 0.026-1.337 microM, and 1.1-3.6 microM, respectively. Uracil levels, indicative of DPD inhibition, also increased dose-dependently from basal levels of 0.03-0.25 microM to 3.6-9.4 microM after 2-4 h, and 0.09-0.9 microM was still present after 24 h. The pharmacokinetics of CDHP and uracil were linear over the dose range. The areas under the plasma concentration curves (AUC) for CDHP and uracil were in the ranges 418-1735 and 2281-8627 micromol x min/l, respectively. The t(1/2) values were in the ranges 213-692 and 216-354 min, respectively. Cumulative urinary excretion of FT was predominantly as 5-FU and was 2.2-11.9%; the urinary excretion of both fluoro-beta-alanine and uracil was generally maximal between 6 and 18 h. During 28-day courses with twice-daily S-1 administration, 5-FU and uracil generally increased. Before each intake of S-1, 5-FU varied between 0.5 and 1 microM and uracil was in the micromolar range (up to 7 microM), indicating that effective DPD inhibition was maintained during the course. In a biopsy of an esophageal adenocarcinoma metastasis that had regressed, thymidylate synthase, the target of 5-FU, was inhibited 50%, but increased four- to tenfold after relapse in subsequent biopsies. In conclusion, oral S-1 administration resulted in prolonged exposure to micromolar 5-FU concentrations due to DPD inhibition, and the decrease in uracil levels after 6 h followed the pattern of CDHP and indicates reversible DPD inhibition.

Published

2003

35. Economic evaluation of antibiotic prophylaxis in small-cell lung cancer patients receiving chemotherapy: an EORTC double-blind placebo-controlled phase III study (08923)

Author

Thierry Gorlia, R. Crott, G. Giaccone, E. Buccholz, Andrea Ardizzoni, J.T.M. Burghouts, Pieter E. Postmus, C. Debruyne, Bonne Biesma, Christian Manegold, Vcg Tjan-Heijnen, S. Caleo, and VU University medical center

Subjects

Adult, Male, medicine.medical_specialty, Lung Neoplasms, Fever, Survival, medicine.drug_class, medicine.medical_treatment, Cost-Benefit Analysis, Antibiotics, Administration, Oral, Placebo, Small-cell carcinoma, law.invention, Placebos, Randomized controlled trial, Double-Blind Method, law, Cost Savings, Risk Factors, Interventional oncology [UMCN 1.5], Internal medicine, Antineoplastic Combined Chemotherapy Protocols, Granulocyte Colony-Stimulating Factor, medicine, Humans, Antibiotic prophylaxis, Carcinoma, Small Cell, Cyclophosphamide, health care economics and organizations, Antibacterial agent, Aged, Etoposide, Chemotherapy, business.industry, Incidence, Hematology, Health Care Costs, Leukopenia, Antibiotic Prophylaxis, Middle Aged, medicine.disease, Surgery, Clinical trial, Hospitalization, Oncology, Doxorubicin, Female, business

Abstract

Item does not contain fulltext BACKGROUND: To determine whether the cost of prophylactic antibiotics during chemotherapy is offset by cost savings due to a decreased incidence of febrile leukopenia (FL). PATIENTS AND METHODS: Small-cell lung cancer (SCLC) patients were randomised to standard or intensified chemotherapy with granulocyte colony-stimulating factor to assess the impact on survival (n = 244). In addition, patients were randomised to prophylactic ciprofloxacin and roxithromycin or placebo to assess the impact on FL (n = 161). The economic evaluation examined the costs and effects of patients taking antibiotics versus placebo. Medical resource utilisation was documented prospectively, including 33 patients from one centre in The Netherlands (NL) and 49 patients from one centre in Germany (GE). The evaluation takes the perspective of the health insurance systems and of the hospitals. Sensitivity analyses were performed. RESULTS: In the main trial, prophylactic antibiotics reduced the incidence of FL, hospitalisation due to FL and use of therapeutic antibiotics by 50%. In GE, the incidence of FL was not reduced by prophylaxis. This resulted in an average cost difference of only 35 Euros [95% confidence interval (CI) (-)1.713-2.263] in favour of prophylaxis (not significant). In NL, prophylaxis reduced the incidence of FL by nearly 50%, comparable with the results of the main trial, resulting in a cost difference of 2706 Euros [95% CI 810-5948], demonstrating savings in favour of prophylactic antibiotics of nearly 45%. Sensitivity analyses indicate that with an efficacy of prophylaxis of 50%, and with expected costs of antibiotic prophylaxis of 500 Euros or less, cost savings will incur over a broad range of baseline risks for FL; that is, a risk >10-20% for FL per cycle. CONCLUSIONS: Giving oral prophylactic antibiotics to SCLC patients undergoing chemotherapy is the dominant strategy in both GE and NL, demonstrating both cost-savings and superior efficacy. The sensitivity analyses demonstrate that, due to the efficacy of prophylactic antibiotics and their low unit cost, cost savings will incur over a broad range of baseline risks for FL. We recommend the use of prophylactic antibiotics in patients at risk for FL during chemotherapy.

Published

2003

36. Hereditary cerebral hemorrhage with amyloidosis associated with E693K mutation of APP

Author

O. BUGIANI, G. GIACCONE, G. ROSSI, M. MANGIERI, R. CAPOBIANCO, M. MORBIN, G. MAZZOLENI, C. CUPIDI, G. MARCON, A. GIOVAGNOLI, A. BIZZI, G. DI FEDE, F. CARELLA, A. SALMAGGI, A. ROMORINI, G. M. PATRUNO, M. MAGONI, A. PADOVANI, F. TAGLIAVINI, PUOTI, Gianfranco, O., Bugiani, G., Giaccone, G., Rossi, M., Mangieri, R., Capobianco, M., Morbin, G., Mazzoleni, C., Cupidi, G., Marcon, A., Giovagnoli, A., Bizzi, G., DI FEDE, Puoti, Gianfranco, F., Carella, A., Salmaggi, A., Romorini, G. M., Patruno, M., Magoni, A., Padovani, and F., Tagliavini

Published

2010

37. An update of the epidemiology of sporadic Creutzfeldt-Jakob disease in Italy based on neuropathologic and molecular typing of a large cohort of patients

Author

G. Giaccone, L. Ingrosso, S. Ferrari, D. Imperiale, S. Taraglio, S. Monaco, M. Pocchiari, F. Tagliavini, CAPELLARI, SABINA, PARCHI, PIERO, AINP BOARD AND AIRIC BOARD, G. Giaccone, S. Capellari, L. Ingrosso, S. Ferrari, D. Imperiale, S. Taraglio, S. Monaco, M. Pocchiari, F. Tagliavini, and P. Parchi

Subjects

CJD, PRION, PRNP

Abstract

Despite its proven heterogeneity, sporadic CJD (sCJD) to date has been only analyzed epidemiologically as a single entity. Taking advantage of the current high autopsy rate for clinically suspected CJD cases, we evaluated the frequency of sCJD subtypes in Italy in a large cohort of consecutive cases. Inclusion criteria were onset of symptoms within the period 2000 – 2005 and neuropathologic disease confirmation. Patients carrying pathogenic mutations in the coding region of PRNP and/or having a positive family history were excluded. PRNP genotyping was performed in 402 (87.9%) cases and showed 283 (70.4%) MM, 62 (15.4%) MVand 57 (14.2%) VV subjects. Most cases belonged to MM/MV1 (51%), mixed MM/MV1+2C (22%), VV2 (15%) and MV2 (8%) subtypes, while the remaining 4% comprised rare variants or atypical cases. Our study provides the first estimate of the incidence of the sCJD variants in a large cohort of consecutive patients and the basis for the study of spatial and temporal sCJD clustering in Italy.

Published

2009

38. A phase I study of sequential intravenous topotecan and etoposide in lung cancer patients

Author

E.F. Smit, G. Giaccone, Cynthia Huisman, and Pe Postmus

Subjects

Adult, Male, medicine.medical_specialty, Lung Neoplasms, Neutropenia, medicine.medical_treatment, Gastroenterology, Drug Administration Schedule, Carcinoma, Non-Small-Cell Lung, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Topoisomerase II Inhibitors, Carcinoma, Small Cell, Enzyme Inhibitors, Lung cancer, Etoposide, Aged, Chemotherapy, Cross-Over Studies, Dose-Response Relationship, Drug, business.industry, Hematology, Middle Aged, medicine.disease, Crossover study, Treatment Outcome, Oncology, Toxicity, Immunology, Female, Topotecan, Topoisomerase I Inhibitors, business, Febrile neutropenia, medicine.drug

Abstract

Summary Purpose The topoisomerase I inhibitor topotecan (T) and the topoisomerase II inhibitor etoposide (E) are active drugs in lung cancer The complementary functions of their targets may suggest benefit from the combined use of these agents but drug scheduling has been shown to play a critical role in preclinical models To establish the optimal schedule and assess the impact of sequential administration of the combination of T and E, we conducted a dose finding study of sequential intravenous T and E in a four-weekly-schedule in relapsed lung cancer patients Patients and methods The importance of drug sequence was assessed in consecutive patients throughout all dose levels, patients received in the first course either T followed by E (the TE group Ton days 1–3 and E on days 4–6) or E before T (the ET group E on days 1–3 and T on days 4–6) The sequence of T and E was alternated in the successive courses In this crossover design, each patient served as his own control for analysis of hematological toxicity in which TE sequence was compared to that of the ET sequence Moreover, hematological toxicity after the first course was compared between the TE and the ET groups The starting dose was T/E 0 75/75 mg/m2 at dose level 1 and dose escalation was planned to T/E 1 00/75 mg/m2 at dose level 2, T/E 1 00/100 mg/m2 at dose level 3, T/E 1 25/100 mg/m2 at dose level 4 and T/E 1 50/100 mg/m2 at dose level 5 Nineteen patients (small-cell lung cancer 7, non-small-cell lung cancer 11, mesothelioma 1 patient) were included Results The principal toxicity was myelosuppression, primarily neutropenia and thrombocytopenia At dose level 3 several grade 4 toxicities were observed DLT (febrile neutropenia) occurred in two patients, one in the TE and one in the ET group and precluded further dose escalation There was no significant difference in WBC and platelet nadirs during the first course between the TE and the ET group The influence of the sequence of administration of topotecan and etoposide was calculated by comparing the nadir values of cycles I and II for each patient For none of the dose levels, a significant sequence-dependent effect could be detected The MTD was reached at the doses of 100 mg/m2 topotecan and 75 mg/m2 etoposide No objective responses were seen Conclusion Although the combined use of topoisomerase I and II inhibitors is attractive on theoretical grounds, excessive myelosuppression prevents substantial dose escalation

Published

2001

39. Hepatic arterial 5-fluorouracil in patients with liver metastases of colorectal cancer: Single-centre experience in 145 patients

Author

H.M. Pinedo, Sybren L. Meijer, G. Giaccone, S. H. M. Albers, J.M.G.H. van Riel, C.J. van Groeningen, F. G. van den Berg, R. Bleichrodt, and M. Cazemier

Subjects

Adult, Male, Antimetabolites, Antineoplastic, medicine.medical_specialty, Colorectal cancer, medicine.medical_treatment, Rectum, mogelijke oorzaken en gevolgen (sepsis en ontsteking) [Sepsis en niet-bacteriële gegeneraliseerde ontsteking], causes and effects (sepsis and inflammation) [Sepsis and non-bacterial generalized inflammation], Gastroenterology, Metastasis, Hepatic Artery, Internal medicine, medicine, Humans, Infusions, Intra-Arterial, Aged, Aged, 80 and over, Chemotherapy, business.industry, Liver Neoplasms, Thrombosis, Hematology, Middle Aged, Prognosis, medicine.disease, Survival Analysis, Chemotherapy regimen, Surgery, Catheter, Treatment Outcome, medicine.anatomical_structure, Oncology, Fluorouracil, Female, Colorectal Neoplasms, business, Complication, medicine.drug

Abstract

Background Hepatic arterial chemotherapy for liver metastases of colorectal cancer is still under discussion. Mainly because of the technical complications of this mode of treatment and the lack of a survival benefit in randomized studies. We performed an analysis of hepatic arterial 5-fluorouracil (5-FU) chemotherapy in 145 consecutive patients treated at a single institution. Patients and methods One hundred forty-five patients with inoperable liver metastases from colorectal cancer were included. 5-FU, 1000 mg/m2/day continuous infusion for five days every three weeks, was delivered in the hepatic artery by percutaneous catheter or arterial access device. Results The response rate was 34% for all patients, 40% in patients with extrahepatic disease, and 15% in patients with i.v. 5-FU-based pretreatment. TTP and OS for all patients were 7.5 and 14.3 months, respectively. In patients with extrahepatic disease or i.v. 5-FU-based pretreatment, OS was significantly shorter compared to patients without extrahepatic disease or 5-FU-based pretreatment (9.7 vs. 19.3 months and 10.1 vs. 17.4 months, respectively). forty-seven percent of patients stopped treatment because of a complication. Complications most often seen in patients with arterial ports were hepatic artery thrombosis (48%) and dislocation of the catheter (22%). Conclusions The results of our analysis are in line with previous phase III studies. Extrahepatic disease and i.v. 5-FU-based pretreatment were prognostic for reduced OS. The complication rate of hepatic arterial delivery was worrisome, although, no negative impact on survival could be established. There is a strong need for improvement of hepatic arterial delivery methods before further evaluation of hepatic arterial 5-FU will be worthwhile.

Published

2000

40. Schedule-dependent pharmacodynamic effects of gemcitabine and cisplatin in mice bearing Lewis lung murine non-small cell lung tumours

Author

E. M. Comijn, G. Giaccone, G. Veerman, W.J.F. van der Vijgh, Godefridus J. Peters, D.A. Voorn, Pieter E. Postmus, C.J.A. van Moorsel, H.M. Pinedo, Kees Smid, and B Lakerveld

Subjects

inorganic chemicals, Cancer Research, medicine.drug_class, Bone Marrow Cells, Pharmacology, Kidney, Deoxycytidine, Antimetabolite, Carcinoma, Lewis Lung, Mice, Pharmacokinetics, In vivo, Antineoplastic Combined Chemotherapy Protocols, medicine, Animals, Doubling time, neoplasms, Cisplatin, Chemistry, Kidney metabolism, Gemcitabine, Mice, Inbred C57BL, Oncology, Immunology, Toxicity, Female, medicine.drug

Abstract

The combination of 2',2'-difluorodeoxycytidine (gemcitabine, dFdC) and cis-diammine-dichloroplatinum(II) (cisplatin, CDDP) is increasingly applied in clinical oncology. We studied the underlying mechanisms of the in vivo schedule dependency and supraadditive interaction between dFdC and CDDP in C57/B16 mice bearing Lewis lung (LL) tumours. Mice were treated with CDDP (6 mg/kg) and dFdC (60 mg/kg) either simultaneously or in a 4 or 24 h interval with dFdC preceding CDDP or vice versa. Four, 8 (in some cases 12) and 24 h after treatment mice were sacrificed and tumours, kidneys, blood and bone marrow (BM) were collected. Since CDDP acts by formation of Platinum (Pt)-DNA adducts and dFdC by incorporation of its triphosphate (dFdCTP) into DNA, we measured total Pt levels, dFdCTP accumulation and Pt-DNA adducts by atomic absorption spectrometry (AAS), high performance liquid chromatography (HPLC) and 2P-postlabelling, respectively. These levels were related to the previously determined antitumour efficacy and toxicity of the dFdC/CDDP combination. Peak dFdCTP accumulation in tumours (11 pmol/mg) was found 4 h after dFdC treatment, while CDDP tended to reduce this in a time-dependent way. Peak levels of total Pt in tumours were found 4 h after CDDP treatment (581 fmol/mg) and dropped 1.8-fold after simultaneous treatment with dFdC (P = 0.04). Treatment with dFdC 4 h after or simultaneously with CDDP increased Pt retention (level 24 h after CDDP treatment) 1.4- and 1.6-fold (P = 0.04 and P = 0.03, respectively). Peak Pt-DNA adduct levels in tumours were also found 4 h after CDDP treatment (7 fmol/microg DNA) and were decreased 3-fold by dFdC treatment 24 h prior to CDDP (P = 0.04). Pt-DNA adduct retention was only decreased when dFdC was given 4 h before CDDP (8-fold (P < 0.01)). The retention and the area-under the concentration time curve of Pt-DNA adducts were related to decreased tumour doubling time (linear regression coefficient (R) = 0.95; P < 0.05, 0.96 P = 0.04 and 0.90; P = 0.04. Pt-DNA adduct levels in the BM cells reached a plateau level 4-24 h after CDDP treatment (approximately 10 fmol/microg DNA), which was increased by dFdC when given either simultaneously with, 4 h before or 4 h after CDDP (6-, 3- and 5-fold at 28 h, 8 h and 28 h, respectively (P < or = 0.04)). Peak Pt-DNA adduct formation (24 h: 8 fmol/microg DNA) in kidneys was enhanced by dFdC when given simultaneously with or 4 h before CDDP (4 h timepoint) (P < 0.01). However, retention was 4- and 6-fold decreased when dFdC was given 4 or 24 h after CDDP, respectively (P < or = 0.01). dFdC given 24 h before CDDP decreased all Pt-DNA adduct levels in kidneys 3-fold or more (P < or = 0.03). Pt-DNA adduct levels were inversely related to kidney toxicity when the most toxic schedule was excluded from the analysis. Peak levels of total Pt in kidneys were reached 24 h after CDDP treatment (4.3 fmol/mg) and the 8 h levels were increased 2-fold by dFdC when given 4 h after CDDP (P = 0.07).

Published

2000

41. Gemcitabine and Cisplatin as Induction Regimen for Patients With Biopsy-Proven Stage IIIA N2 Non–Small-Cell Lung Cancer: A Phase II Study of the European Organization for Research and Treatment of Cancer Lung Cancer Cooperative Group (EORTC 08955)

Author

A. Termeer, C. Debruyne, Franz M.N.H. Schramel, N. van Zandwijk, E.F. Smit, J. Festen, Desmond Curran, Steven Gans, Gijsbert W.P.M. Kramer, G. Giaccone, and N.J. J. Schlosser

Subjects

Adult, Male, Oncology, Cancer Research, medicine.medical_specialty, Lung Neoplasms, medicine.medical_treatment, Deoxycytidine, Pneumonectomy, Carcinoma, Non-Small-Cell Lung, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Lung cancer, Aged, Neoplasm Staging, Chemotherapy, Performance status, business.industry, Induction chemotherapy, Cancer, Middle Aged, medicine.disease, Combined Modality Therapy, Survival Analysis, Gemcitabine, Surgery, Regimen, Female, Cisplatin, business, medicine.drug

Abstract

PURPOSE: Our objective was to better define the activity/feasibility of gemcitabine/cisplatin (GC) as induction chemotherapy in patients with stage IIIA N2 non–small-cell lung cancer (NSCLC) followed by surgery or radiotherapy within a large, ongoing comparative study (EORTC 08941). PATIENTS AND METHODS: Forty-seven chemotherapy-naive patients with NSCLC, median age of 58 years, stage IIIA N2 disease, World Health Organization performance status of 0 or 1, and the ability to tolerate a pneumonectomy received gemcitabine 1,000 mg/m2 on days 1, 8, and 15 and cisplatin 100 mg/m2 on day 2, every 4 weeks. Patients received induction chemotherapy (three cycles) before re-evaluation and randomization to surgery or radiotherapy. RESULTS: Grade 3/4 thrombocytopenia, the main hematologic toxicity, occurred in 60% of patients but was not associated with bleeding. Full-dose gemcitabine was given in 48% of the courses. Severe nonhematologic toxicity was uncommon. Two patients with preexisting, autoimmune pulmonary fibrosis had deterioration of pulmonary function after radiotherapy. Thirty-three (70.2%; 95% confidence interval, 55.1% to 82.7%) of the 47 eligible patients had objective responses (three complete responses and 30 partial responses). Mediastinal nodes were tumor-free after induction therapy in 53% of cases. Resections were considered complete in 71% of the patients who underwent thoracotomy after induction therapy. Median survival for all recruited patients (N = 53) was 18.9 months, with an estimated 1-year survival rate of 69%. CONCLUSION: In patients with N2 stage IIIA NSCLC, GC is a highly active and well-tolerated induction regimen. GC should be explored in combination with surgery or radiotherapy in stage I and II patients.

Published

2000

42. Caelyx™ in malignant mesothelioma: A phase II EORTC study

Author

H. Groen, J. Van Meerbeeck, P. Baas, G. Giaccone, S. Daamen, Sjaak Burgers, and Hugo Schouwink

Subjects

Adult, Male, Mesothelioma, medicine.medical_specialty, Adolescent, Anemia, Pleural Neoplasms, medicine.medical_treatment, Phases of clinical research, Antineoplastic Agents, Gastroenterology, Internal medicine, medicine, Humans, Doxorubicin, Aged, Chemotherapy, Cardiotoxicity, business.industry, Hematology, Middle Aged, medicine.disease, Survival Analysis, Chemotherapy regimen, Surgery, Oncology, Liposomes, Toxicity, Pleura, Female, business, medicine.drug

Abstract

Summary Background The use of doxorubicin has shown some activity in malignant mesothelioma but prolonged administration is hampered by cardiotoxicity. Caelyx™, a new liposomal and pegylated form of doxorubicin has shown a better pharmaco-kinetic and toxic profile then doxorubicin. In a phase II study, the efficacy and toxicity of Caelyx™ was tested in previously untreated patients with malignant pleural mesothelioma. Patients and methods Thirty-three patients who had measurable or evaluable histologically confirmed malignant pleural mesothelioma were included in the study. Caelyx™ (45 mg/m2) was given i.v. on outpatient base every four weeks for nine cycles or till progression or unacceptable toxicity occurred. Results Of the 33 patients, 32 were evaluable for toxicity, and 31 for response. Two patients had a partial response (6%, 95% confidence interval: 0.2%–20.2%). The median survival was 13 months. Forty percent of the patients received >6 cycles. Toxicity was mild with palmar plantar erythrodyses-thesia being most pronounced (62% grade 1–2, 6% grade 3) and of limited duration. Ten percent of patients had grade 3 anemia and 3% grade 3 thrombocytopenia. Two patients (6%) had grade 3 or 4 cardiac toxicity, which was not drug related. Conclusion At the prescribed dose, single agent Caelyx™ is well tolerated but its activity in chemotherapy-naive mesothelioma patients does not warrant further investigation as a single agent.

Published

2000

43. Downstream molecular determinants of response to 5-fluorouracil and antifolate thymidylate synthase inhibitors

Author

B. Van Triest, H.M. Pinedo, Godefridus J. Peters, and G. Giaccone

Subjects

Antimetabolites, Antineoplastic, Methyltransferase, DNA Repair, DNA repair, DNA damage, Thymidylate synthase, chemistry.chemical_compound, Neoplasms, medicine, Humans, biology, DNA synthesis, Thymidylate Synthase, Hematology, Genes, p53, Prognosis, Molecular biology, Gene Expression Regulation, Neoplastic, Oncology, chemistry, Drug Design, Antifolate, biology.protein, Folic Acid Antagonists, Nolatrexed, Fluorouracil, Raltitrexed, medicine.drug

Abstract

Thymidylate synthase (TS) is an essential enzyme for the de novo synthesis of thymidylate and subsequently DNA synthesis. TS has been used as a target for cancer chemotherapy in the development of fluoropyrimidines such as 5-fluorouracil (5-FU) and 5-fluorodeoxyuridine and of novel folate-based TS inhibitors such as ZD1694 (Tomudex, Raltitrexed), ZD9331, LY231514 (ALIMTA, Pemetrexed), AG337 (Thymitaq, Nolatrexed) and AG331. Although TS has been considered as a target for chemotherapy, the precise mechanism by which TS inhibition leads to cell death is still not completely resolved. TS inhibition results in depletion of dTTP, an essential precursor for DNA, and an increase in dUTP. This results in the so-called thymine-less death due to misincorporation of dUTP into DNA; its excision, catalysed by uracil-DNA glycosylase, results in DNA damage. Both this imbalance in dTTP/dUTP and DNA damage can result in induction of downstream events, leading to apoptosis. On the other hand a specific interaction exists between oncogenes and TS, by binding of TS protein to the p53 and c-myc RNA, while wt p53 can also inhibit TS promotor activity. TS inhibition by either 5-FU or antifolates can also result in a depression of TS protein mediated inhibition of TS mRNA translation leading to induction of more TS protein synthesis, and p53 protein may further deregulate this process. These complex indirect and direct interactions between oncogenes and TS may have as yet unclear clinical implications, since most data are based on in vitro or in vivo studies and some results are contradictive. In some preliminary clinical studies evidence was postulated for a combined prognostic role for TS and p53. This knowledge should be used to design clinical studies with the aim to deliver effective treatment to potentially sensitive patients both in the adjuvant setting and in advanced stage disease.

Published

2000

44. A phase I–II study of gemcitabine and paclitaxel in advanced non-small-cell lung cancer patients

Author

H.M. Pinedo, Egbert F. Smit, H. van Tinteren, D. Laan, Richard P. Golding, G. Giaccone, Ted A.W. Splinter, Pieter E. Postmus, J.P. van Meerbeeck, Pulmonary Medicine, and Medical Oncology

Subjects

Oncology, Antimetabolites, Antineoplastic, medicine.medical_specialty, Lung Neoplasms, Paclitaxel, Side effect, medicine.medical_treatment, Phases of clinical research, Deoxycytidine, Drug Administration Schedule, chemistry.chemical_compound, SDG 3 - Good Health and Well-being, Carcinoma, Non-Small-Cell Lung, Internal medicine, Antineoplastic Combined Chemotherapy Protocols, medicine, Humans, Lung cancer, Neoplasm Staging, Chemotherapy, Dose-Response Relationship, Drug, business.industry, Hematology, medicine.disease, Gemcitabine, Surgery, Regimen, chemistry, business, medicine.drug

Abstract

Thirty patients with chemotherapy-naïve advanced non-small-cell lung cancer (NSCLC) were given escalating doses of paclitaxel (150, 175, 200 mg/m2) on day 1 in three consecutive cycles, together with a fixed dose of gemcitabine 1000 mg/m2 on days 1 and 8; cycles were repeated every three weeks. The dose escalation of paclitaxel was feasible in the majority of patients. Subsequently, 30 other NSCLC patients received a dose of 200 mg/m2 paclitaxel with gemcitabine 1000 mg/m2 in a phase II study. The major side effect was mild myelosuppression. A response rate of 24% was achieved in 49 fully evaluable patients. This regimen proved to be safe and easy to administer on an out-patient setting, and constitutes now one of the arms of the current EORTC randomized study for advanced NSCLC.

Published

2000

45. Skin tests predict survival after autologous tumor cell vaccination in metastatic melanoma

Author

Anita G.M. Stam, Arnold Baars, H.M. Pinedo, A.J.M. van den Eertwegh, Sybren L. Meijer, H.E. Gall, Jan B. Vermorken, John Wagstaff, C. J. L. M. Meijer, A. M. E. Claessen, R.J. Scheper, G. Giaccone, Medical oncology, Pathology, AII - Cancer immunology, CCA - Cancer biology and immunology, CCA - Imaging and biomarkers, and Internal medicine

Subjects

Oncology, Adult, Male, medicine.medical_specialty, Skin Neoplasms, medicine.medical_treatment, Injections, Subcutaneous, Cancer Vaccines, Disease-Free Survival, Adjuvants, Immunologic, Predictive Value of Tests, Internal medicine, Skin Ulcer, medicine, Humans, Hypersensitivity, Delayed, Radical surgery, Melanoma, Aged, Skin Tests, business.industry, Hematology, Immunotherapy, Middle Aged, medicine.disease, Autologous tumor cell, Surgery, Vaccination, Delayed hypersensitivity, BCG Vaccine, Female, Metastasectomy, business, Adjuvant

Abstract

Background: Currently there is no standard adjuvant treatment following surgical resection of metastatic melanoma. We investigated whether surgery followed by autologous tumor cell-BCG vaccination was beneficial for malignant melanoma patients. In this study we focus on the prognostic value of DTH response following vaccination therapy. Patients and methods: Eighty-one patients with AJCC stage III and IV melanoma were selected. Whenever feasible, radical metastasectomy was performed. ASI was initiated by the administration of three weekly intra-cutaneous vaccinations with l07 irradiated autologous tumor cells, starting four weeks after surgery. Depending on the size of DTH response to the first three injections, subsequent vaccinations were planned. The first two vaccines also contained l07 BCG organisms as an immune stimulatory adjuvant. Results: Induration as well as erythema correlated strongly with survival (P < 0.0001 and P = 0.0004). After radical metastasectomy in stage III melanoma patients a five-year survival of 48% was observed. In stage IV disease, a five-year survival of 34% was seen, after radical surgery had been performed. When macroscopic disease was present at start of vaccination treatment, no clinical responses occurred. Apart from transient skin ulceration at the site of BCG-containing vaccinations, no serious side effects were observed. Conclusions: This study shows that large-scale preparation of autologous melanoma cell vaccines is feasible, while vaccination results in DTH responses that correlate significantly with survival. ASI seemed to be beneficial in stage III and stage IV melanoma when given in the adjuvant setting, while causing only very mild side effects.

Published

2000

46. Effects of α-galactosylceramide (KRN7000), interleukin-12 and interleukin-7 on phenotype and cytokine profile of human Vα24+ Vβ11+T cells

Author

H.M. Pinedo, B.M.E. von Blomberg, H. J. J. Van Der Vliet, A.J.M. van den Eertwegh, R.J. Scheper, M. A. Peyrat, G. Giaccone, Nobusuke Nishi, and Yasuhiko Koezuka

Subjects

CD40, biology, ZAP70, Immunology, Natural killer T cell, Molecular biology, Interleukin 21, CD1D, biology.protein, Interleukin 12, Immunology and Allergy, Cytotoxic T cell, IL-2 receptor

Abstract

The alpha-galactosylceramide KRN7000 was reported to be presented by CD1d to natural killer (NK) T cells, cells that are thought to play an important role in the rejection of malignant tumours and in the regulation of several autoimmune diseases. Here we analysed human peripheral blood (PB) NK T cells (Valpha24+ Vbeta11+ T cells) before and after a short-term culture in the presence of KRN7000. KRN7000 strongly activated PB Valpha24+ Vbeta11+ T cells and, when stimulated, the vast majority of these cells expressed interferon-gamma (IFN-gamma). Exposure of these KRN7000-cultured Valpha24+ Vbeta11+ T cells to interleukin-12 (IL-12), but not to IL-7, resulted in a relative increase in IFN-gamma-expressing Valpha24+ Vbeta11+ T cells, compared with IL-4-expressing Valpha24+ Vbeta11+ T cells, indicating a shift towards a T-helper type 1 (Th1) phenotype. KRN7000 strongly up-regulated the expression of the cytotoxic molecule granzyme B (GrB) in Valpha24+ Vbeta11+ T cells. Although IL-7 resulted in a decrease in GrB levels in KRN7000-cultured Valpha24+ Vbeta11+ T cells, IL-12 increased GrB levels in both Valpha24+ Vbeta11+ T cells and in Valpha24+ Vbeta11+ T-cell clones and increased cytotoxicity against hCD1d-transfected HeLa cells. Our data provide further insight into the characteristics of human Valpha24+ Vbeta11+ T cells and indicate that KRN7000 is a potent activator of Valpha24+ Vbeta11+ T cells. Combined with the established anti-tumour effects of KRN7000 in mouse models, these results may support the use of KRN7000 as an anti-tumour agent in man.

Published

1999

47. Current chemotherapeutic possibilities in pancreaticobiliary cancer

Author

G. Giaccone, H.M. Pinedo, C.J. van Groeningen, and J.M.G.H. van Riel

Subjects

Oncology, medicine.medical_specialty, business.industry, medicine.medical_treatment, Cancer, Hematology, medicine.disease, Chemotherapy regimen, Gemcitabine, Surgery, Radiation therapy, Internal medicine, Pancreatic cancer, Adjuvant therapy, Medicine, Combined Modality Therapy, business, Neoadjuvant therapy, medicine.drug

Abstract

Summary At time of presentation the majority of patients with pancreaticobiliary cancer have locally advanced or metastatic disease which makes them unamenable for curative surgery. In these patients chemotherapy is an option which has gained more support over the past few years. Special problems faced in chemotherapeutic treatment are the patient's poor condition and the difficulties faced in evaluating response. 5-FU has been the only drug with some efficacy for a long time, but more recently gemcitabine appeared to be more efficient. In locally advanced pancreatic cancer the combination of chemotherapy with radiotherapy has not gained much support. However, studies are implicating better local control with combined treatment and recurrences appear more often at distant sides. In some cases irresectable tumors became resectable. Because of the poor survival after surgery with curative intent, adjuvant and neoadjuvant therapy are becoming important issues. Although studies of adjuvant therapy suggest benefit, research is seriously hampered by poor patient accrual due to the morbidity of pancreaticodu odenectomy. Neoadjuvant treatment may overcome this problem. Until now there has been only modest improvement in the treatment of pancreatic cancer. Hopefully, new treatment modalities such as immunotherapy, gene therapy and antiangiogenic therapy will alter this dismal picture. In biliary cancer the role of chemotherapy is less well defined, since only few studies with low patients numbers have been performed.

Published

1999

48. P53 and chemosensitivity

Author

Carlos Gil Ferreira, G. Giaccone, C. Tolis, and VU University medical center

Subjects

Programmed cell death, Lung Neoplasms, Cell cycle checkpoint, Tumor suppressor gene, DNA repair, Cell, Apoptosis, Breast Neoplasms, medicine, Humans, Gastrointestinal Neoplasms, Ovarian Neoplasms, business.industry, Cell Cycle, Hematology, Cell cycle, medicine.disease, Gene Expression Regulation, Neoplastic, medicine.anatomical_structure, Oncology, Drug Resistance, Neoplasm, Immunology, Cancer research, Female, Germ cell tumors, Tumor Suppressor Protein p53, business

Abstract

Summary Background Although hematologic malignancies and some solid tumors such as germ cell tumors and pediatric malignancies can be cured by cytotoxic treatment, the most prevalent solid tumors are relatively resistant to these interventions. Apoptosis is involved in the cell kill of anticancer drugs and p53 is believed to be of principal importance in this process. However p53 also plays a role in cell cycle arrest and DNA repair, cellular processes that can decrease the sensitivity to chemotherapy. Therefore, p53 may play a dual role after exposure to cytotoxic treatment, activating either mechanisms that lead to apoptosis or launching processes directing to DNA repair and survival of the cell. Design In this article, we review in details the p53 functions involved in the mediation of chemosensitivity. The preclinical and clinical data published in the recent years about the relation between p53 and chemosensitivity are discussed and the potential pitfalls associated to most of these studies, and that may account for the contradictory results produced so far are also mentioned.

Published

1999

49. Characterization of human soft-tissue sarcoma xenografts for use in secondary drug screening

Author

Peter G. Scheffer, Wilbert H.M. Peters, Hennie M.M. Schlüper, C. A. M. Erkelens, A. H. Van Hattum, Epie Boven, C. M. Kuiper, G. Giaccone, H.M. Pinedo, and J. van Ark-Otte

Subjects

Cancer Research, medicine.medical_treatment, Transplantation, Heterologous, Glutathione reductase, Mice, Nude, Antineoplastic Agents, Soft Tissue Neoplasms, Gene Expression Regulation, Enzymologic, Mice, chemistry.chemical_compound, Nude mouse, Antigens, Neoplasm, medicine, Animals, Doxorubicin, Etoposide, chemistry.chemical_classification, Chemotherapy, biology, Topoisomerase, Glutathione peroxidase, biology.organism_classification, Nitrogen mustard, DNA-Binding Proteins, Gene Expression Regulation, Neoplastic, Isoenzymes, DNA Topoisomerases, Type II, Oncology, chemistry, Immunology, Linear Models, Cancer research, biology.protein, Female, Sarcoma, Experimental, Drug Screening Assays, Antitumor, Genes, MDR, Neoplasm Transplantation, Research Article, medicine.drug

Abstract

We have established ten transplantable human soft-tissue sarcoma (STS) xenografts grown as subcutaneous tumours in the nude mouse. Nine xenografts originated from patients that needed chemotherapy in the course of their disease. The xenografts were tested for their sensitivity to maximum tolerated doses of five anti-cancer agents. Growth of treated tumours was expressed as a percentage of control tumour growth and a growth inhibition > 75% was measured for doxorubicin in 20% of the STS xenografts, for cyclophosphamide in 30%, for ifosfamide in 20%, for vincristine in 20%, whereas etoposide was not effective in the STS xenografts. In three out of ten STS xenografts MDR1 mRNA was detectable, but this was not related to the resistance against doxorubicin, vincristine or etoposide. Topoisomerase IIalpha mRNA expression levels did not reflect sensitivity to doxorubicin or etoposide. In all STS tissues, however, these levels were lower than topoisomerase IIalpha mRNA in a drug-sensitive human ovarian cancer xenograft. Glutathione concentrations and the activities of glutathione S-transferase, glutathione peroxidase and glutathione reductase were not related to resistance against the alkylating agents or doxorubicin. Of interest, in all STS tissues, glutathione S-transferase pi was the predominant isoenzyme present. In conclusion, chemosensitivity of the STS xenografts reflects clinical response rates in phase II trials on the same compounds in adult STS patients. Relatively low levels of topoisomerase IIalpha mRNA may partly account for intrinsic resistance against, for example, doxorubicin. Additional factors must contribute to moderate responsiveness to alkylating agents. Images Figure 1 Figure 2

Published

1998

50. Randomized study of paclitaxel-cisplatin versus cisplatin-teniposide in patients with advanced non-small-cell lung cancer. The European Organization for Research and Treatment of Cancer Lung Cancer Cooperative Group

Author

Q.G.C.M. van Hoesel, Pilar Lianes, C. Debruyne, Desmond Curran, G. Giaccone, G.V. Scagliotti, Tarek Sahmoud, M.C. Pennucci, N. van Zandwijk, Ted A.W. Splinter, Pe Postmus, J. Van Meerbeeck, and G. S. Kho

Subjects

Cisplatin, Cancer Research, medicine.medical_specialty, Chemotherapy, Performance status, business.industry, medicine.medical_treatment, Cancer, Neutropenia, medicine.disease, Gastroenterology, Surgery, Oncology, Internal medicine, medicine, business, Lung cancer, Febrile neutropenia, medicine.drug, Teniposide

Abstract

PURPOSE To compare two cisplatin based chemotherapy schedules in patients with advanced non-small-cell lung cancer (NSCLC). PATIENTS AND METHODS A total of 332 patients with advanced NSCLC were randomized to receive cisplatin 80 mg/m2 on day 1 either in combination with teniposide 100 mg/m2 on days 1, 3, and 5 (arm A) or paclitaxel 175 mg/m2 by 3-hour infusion on day 1 (arm B); cycles were repeated every 3 weeks. RESULTS Fifteen patients were ineligible; patient characteristics were well balanced between the two arms: 71% were male, 71% had less than 5% weight loss, 89% had a World Health Organization (WHO) performance status of 0 to 1, 51% had adenocarcinoma, and 61% had stage IV disease. Hematologic toxicity was significantly more severe in arm A (leukopenia, neutropenia, and thrombocytopenia grade 3 or 4: 66% v 19%, 83% v 55%, 36% v 2% in arms A and B, respectively), which resulted in more febrile neutropenia (27% v 3% in arms A and B, respectively), dose reductions, and treatment delays. There were a total of nine toxic deaths, six due to neutropenic sepsis: five in arm A and one in arm B. In contrast, arthralgia/myalgia (grade 2 or 3, 4% v 17%), peripheral neurotoxicity (grade 2 or 3, 6% v 29%), and hypersensitivity reactions (1% v 7%, all grades) were significantly more frequent in arm B. The frequency and severity of other toxicities were comparable between the two arms. Responses were one complete and 44 partial on arm A (28%) and two complete and 61 partial (41%) on arm B (P = .018). There was no significant difference in survival, with median and 1-year survivals 9.9 versus 9.7 months and 41% versus 43%, respectively in arm A and B. Progression-free survival was 4.9 and 5.4 months in arm A and B, respectively. Selected centers participated in a quality-of-life (QoL) assessment, which was performed by the European Organization for Research and Treatment of Cancer (EORTC) QLQ-C30 and LC-13 administered at baseline and every 6 weeks thereafter. Arm B achieved a better score at week 6 for emotional, cognitive and social functioning, global health status, fatigue, and appetite loss, which was lost at 12 weeks. In conclusion, arm B appears superior to arm A with regard to response rate, side effects, and QoL. CONCLUSION Although survival was not improved, arm B offers a better palliation for advanced NSCLC patients than arm A.

Published

1998