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Publication
Featured researches published by J. Marín.
European Journal of Haematology | 2007
Jose Rodriguez; Eulogio Conde; Antonio Gutiérrez; Reyes Arranz; Angel Leon; J. Marín; Maurizio Bendandi; Carmen Albo; Maria Dolores Caballero
Objective: Retrospective data shows that peripheral T‐cell lymphoma (PTCL) patients sensitive to conventional chemotherapy for aggressive lymphomas may respond better if this treatment is consolidated with frontline autologous stem cell transplantation (ASCT). Here, we present data from a prospective phase II trial of high‐dose chemotherapy and ASCT as a frontline consolidation therapy for aggressive nodal PTCL.
British Journal of Haematology | 2000
Juan José Lahuerta; Joaquin Martinez-Lopez; Carlos Grande; Joan Bladé; Javier de la Serna; Adrian Alegre; José García-Laraña; Dolores Caballero; Ana Sureda; Javier de la Rubia; Ana M. Alvarez; J. Marín; Antonio Escudero; Eulogio Conde; Katy Perez‐Equiza; Juan Ruiz; José M. Moraleda; Angel Leon; J. Bargay; Rafael Cabrera; Miguel T. Hernández-García; Joaquín Díaz-Mediavilla; Jesús F. San Miguel
High‐dose chemoradiotherapy conditioning regimens for autologous stem cell transplantation (ASCT) are generally held to give similar results in multiple myeloma (MM), but no specific comparative study has been published. We addressed this issue by comparing the main high‐dose chemoradiotherapy regimens used in the Spanish Registry. Patient cohorts included 315 cases treated with 200 mg/m2 melphalan (MEL200), 127 patients with 140 mg/m2 melphalan plus total body irradiation (MEL140 + TBI) and 121 cases with 12 mg/kg busulphan plus 140 mg/m2 melphalan (BUMEL). After ASCT, granulocyte and platelet recovery time was similar in all conditioning groups. There were no differences in transplant‐related mortality. All regimens yielded a similar response in reference to pre‐ASCT MM status, although BUMEL produced a slightly better overall response when compared with the other regimens (97% vs. 89% and 92%, P = 0·003). The 5‐year overall survival (OS) with BUMEL was 47% [95% confidence interval (CI) 26–68] compared with 43% (CI 31–54) for MEL140 + TBI and 37% (CI: 18–56) for MEL200. The median survival for the BUMEL group was 64 months compared with 45 and 37 months for the MEL200 and MEL140 + TBI groups respectively. These differences were non‐significant (P = 0·2). The median event‐free survival (EFS) was better for BUMEL (32 months) than for MEL200 (22 months) or for MEL140 + TBI (20 months). The differences in EFS between BUMEL and the other conditioning regimens reached statistical significance (P = 0·01). Nevertheless, the adjusted multivariate analysis for OS and EFS revealed that the conditioning regimens had no independent prognostic value. We concluded that three different conditioning regimens, commonly used for ASCT in MM, have a similar antimyeloma effect. However, the trend for better results observed in our series with BUMEL requires a prospective trial.
British Journal of Haematology | 2001
David Gallardo; Juan I. Aróstegui; A. Balas; Antonio Torres; Dolores Caballero; Enric Carreras; Salut Brunet; Antonio M. Jimenez; Rodolfo Mataix; David Serrano; Carlos Vallejo; Guillermo Sanz; Carlos Solano; Marta Rodríguez‐Luaces; J. Marín; Julio Baro; César Sanz; Jose Roman; Marcos González; Jaume Martorell; Jorge Sierra; Carmen Martín; Rafael de la Cámara; Albert Grañena
Disparity for the minor histocompatibility antigen HA‐1 between patient and donor has been associated with an increased risk of acute graft‐versus‐host disease (GvHD) after allogeneic human leucocyte antigen (HLA)‐identical sibling donor stem cell transplantation (SCT). However, no data concerning the impact of such disparity on chronic GvHD, relapse or overall survival are available. A retrospective multicentre study was performed on 215 HLA‐A2‐positive patients who received an HLA‐identical sibling SCT, in order to determine the differences in acute and chronic GvHD incidence on the basis of the presence or absence of the HA‐1 antigen mismatch. Disease‐free survival and overall survival were also analysed. We detected 34 patient–donor pairs mismatched for HA‐1 antigen (15·8%). Grades II–IV acute GvHD occurred in 51·6% of the HA‐1‐mismatched pairs compared with 37·1% of the non‐mismatched. The multivariate logistic regression model showed statistical significance (P: 0·035, OR: 2·96, 95% CI: 1·07–8·14). No differences were observed between the two groups for grades III–IV acute GvHD, chronic GvHD, disease‐free survival or overall survival. These results confirmed the association between HA‐1 mismatch and risk of mild acute GvHD, but HA‐1 mismatch was not associated with an increased incidence of chronic GvHD and did not affect relapse or overall survival.
Antimicrobial Agents and Chemotherapy | 1983
Josep M. Gatell; J G San Miguel; L Zamora; V Araujo; M Bonet; M Bohé; M. T. Jiménez de Anta; M Farré; M. Elena; A. Ballesta; J. Marín
A total of 157 patients were treated with tobramycin or amikacin in a controlled prospective randomized trial. Dosages were adjusted to renal function according to a nomogram. Trough and peak aminoglycoside levels were available at the end of the trial. Of the above total, 113 recipients of nine or more doses of tobramycin or six or more doses of amikacin, without other apparent cause of renal failure, were evaluated for nephrotoxicity. Thirty-six patients were evaluated for auditory toxicity. The patients in groups evaluated for either nephrotoxicity or auditory toxicity were similar with respect to intensity and etiology of bacterial disease, concurrent exposure to other antimicrobial drugs, age and sex distribution, initial serum creatinine level, and total dose and duration of antimicrobial therapy. Nephrotoxicity of similar severity developed in 4 of 59 (6.8%) recipients of tobramycin and in 7 of 54 (13.1%) recipients of amikacin (P greater than 0.05). Mild auditory toxicity developed in 3 of 19 (15.7%) recipients of tobramycin and in 2 of 17 (11.7%) recipients of amikacin (P greater than 0.05). When patients with abnormally high mean trough or peak aminoglycoside levels were excluded from comparison, nephrotoxicity was 6.12 and 5.12% (P greater than 0.05) and auditory toxicity was 17.6 and 7.69% (P greater than 0.05) in the groups given tobramycin and amikacin, respectively. We conclude that the nephrotoxicity and auditory toxicity of amikacin and tobramycin are not significantly different and that such toxicities are indeed infrequent events when the dosages of these drugs are adjusted to hold blood levels within the safe boundaries suggested by the studies of others.
Nephron | 1985
Josep M. Gatell; J G SanMiguel; L Zamora; V Araujo; C. Castells; Asunción Moreno; M.T. Jimenez de Anta; J. Marín; M. Elena; A. Ballesta
108 patients who received tobramycin or amikacin could be evaluated for nephrotoxicity in a prospective randomized trial. Both groups had similar illnesses, and causative agents, concurrent drug admin
Annals of Oncology | 2005
Anna Sureda; M. Constans; A. Iriondo; Reyes Arranz; M. D. Caballero; M. J. Vidal; J. Petit; A. López; Juan-José Lahuerta; Enric Carreras; Javier García-Conde; José García-Laraña; Rufino Cabrera; Isidro Jarque; D. Carrera; J. C. García-Ruiz; M. J. Pascual; J. Rifón; J.M. Moraleda; K. Pérez-Equiza; Carmen Albo; J. Díaz-Mediavilla; A. Torres; P. Torres; J. Besalduch; J. Marín; M. V. Mateos; J. M. Fernández-Rañada; Josep M. Sierra; Eulogio Conde
Annals of Oncology | 2006
J. Rodriguez; Eulogio Conde; Antonio Gutiérrez; Reyes Arranz; Arturo Vera-Ponce de León; J. Marín; M Bendandi; Carmen Albo; Caballero
Annals of Oncology | 2003
M. D. Caballero; José A. Pérez-Simón; A. Iriondo; Juan-José Lahuerta; Josep M. Sierra; J. Marín; M. Gandarillas; Reyes Arranz; Javier Zuazu; Viñas Rubio; A. Fernández de Sevilla; Enric Carreras; Javier García-Conde; José García-Laraña; Carlos Grande; Anna Sureda; M. J. Vidal; J. Rifón; C. Pérez-Equiza; R. Varela; J.M. Moraleda; J. C. García Ruíz; Carmen Albo; Rufino Cabrera; J. F. San Miguel; Eulogio Conde
Haematologica | 2003
J. Rodriguez; Caballero; Antonio Gutiérrez; M. Gandarillas; Josep M. Sierra; Armando López-Guillermo; Anna Sureda; Javier Zuazu; J. Marín; Reyes Arranz; Enric Carreras; Arturo Vera-Ponce de León; Af De Sevilla; J. F. San Miguel; Eulogio Conde
Annals of Oncology | 2004
J. Rodriguez; M. D. Caballero; Antonio Gutiérrez; Carlos Solano; Reyes Arranz; Juan-José Lahuerta; Josep M. Sierra; M. Gandarillas; José A. Pérez-Simón; Javier Zuazu; Armando López-Guillermo; Anna Sureda; Enric Carreras; José García-Laraña; J. Marín; J. C. Garcia; A. Fernández de Sevilla; J. Rifón; R. Varela; I. Jarque; Carmen Albo; Arturo Vera-Ponce de León; J. SanMiguel; Eulogio Conde
