Your search keyword '"Alex Amaya"' showing total 14 results

1. El acelerón sindicalista y sus contradicciones internas: imagen y realidad en la propaganda de la OSE, 1957-1969

Author

Quer, Àlex Amaya

Published

2009

2. Factores prenatales e intraparto relacionados con puntaje de APGAR bajo en Hospital Nacional Zacamil

Author

Enrique López, José Raúl Arevalo, Alex Amaya Claros, and Universidad Evangélica de El Salvador

Subjects

Recien naciidos, Polymers and Plastics, Business and International Management, Neonato, Estado general del menor, Salud del recién nacido, Industrial and Manufacturing Engineering

Abstract

En el Hospital Nacional Zacamil se realizó un estudio Descriptivo, retrospectivo de 44 casos de madres que tuvieron hijos con puntaje de APGAR bajo al primer o al quinto minuto de vida durante el año 2004, con el objetivo de conocer la frecuencia, factores obstétricos relacionados, vía del parto y métodos de reanimación utilizados en el neonato con APGAR bajo en el servicio de Partos de dicha institución. Se encontr6 que durante el año 2004 se asistieron un total de 3,027 partos de los cuales 44 casos tuvieron APGAR de 6 6 menos representando una frecuencia de 1.4%. De los neonatos con APGAR bajo al minuto se encontró una Casa de recuperación satisfactoria mayor al 80% a los 5min. La mayor incidencia se obsero6 en neonatos de termino con peso entre rangos normales. Se concluy6 que la edad materna, prirniparidad, control prenatal incompleto o ausente, distocias de parto y cesáreas son factores de riesgo para que el recién nacido presente APGAR bajo.

Published

2020

3. Phase Ib study of a novel bivalent IAP antagonist APG-1387 in combination of pembrolizumab for patients with advanced solid tumors

Author

Yifan Zhai, Drew W. Rasco, Yuefen Tang, Alex Amaya, Zhiyan Liang, Nehal Lakhani, Hengbang Wang, Jiao Ji, Dajun Yang, and Jason Chen

Subjects

Antitumor activity, Immune modulator, Cancer Research, Oncology, business.industry, Cancer research, Antagonist, Medicine, Iap antagonist, Pembrolizumab, business, Inhibitor of apoptosis, Bivalent (genetics)

Abstract

3508 Background: APG-1387 is an IAP (inhibitor of apoptosis proteins) antagonist that has strong antitumor activity in multiple xenograft cancer models and acts as a host immune modulator, supporting its exploration for use in combination with checkpoint inhibitors for cancer therapy. Methods: This “3+3” dose escalation and dose expansion study evaluated APG-1387 combined with pembrolizumab in patients with refractory or intolerant advanced solid tumors (NCT03386526). APG-1387 was administered IV once weekly with pembrolizumab 200 mg on day 1 of a 21-day cycle. Study aims were to assess safety/tolerability, recommended phase 2 dose (RP2D), pharmacokinetics (PK), pharmacodynamics (PD), and efficacy. Results: As of December 25, 2019, total 28 patients had been treated in 3 dose cohorts of APG-1387: 20 mg (n = 4), 30 mg (n = 3), and 45 mg (n = 21, 18 in dose expansion). The median line of prior systemic cancer therapies was 3.0 (1-12). No dose-limiting toxicity was observed. The most common treatment-related adverse events (TRAEs; ≥10%) were fatigue (28.6%), arthralgia (14.3%), headache (14.3%), and tumor pain (10.7%). One patient in the 45-mg cohort had grade 2 Bell’s Palsy. G3+ TRAEs were autoimmune colitis, hypoxia, increased lipase, mucosal inflammation, pneumonitis, and tumor pain in 1 patient each (3.6%). Treatment-related SAEs were 1 G3 autoimmune colitis, 1 G2 myocarditis, and 1 G3 pneumonitis. The maximum tolerated dose (MTD)/RP2D for APG-1387 was 45 mg. Among 25 efficacy-evaluable patients, 1 with ER+, HER2‒ breast cancer receiving APG-1387 30 mg after failing 5 lines of therapy (PD-1 treatment-naïve, microsatellite stable) achieved confirmed PR (-79.2%) for 6 cycles but discontinued due to pneumonitis; another patient with PD-L1‒ non‒small-cell lung cancer treated at 45 mg had confirmed PR (-65.0%) for 6 cycles (ongoing). Other 11 patients had SD for 2-11 cycles. The disease control rate was 52%. Preliminary PK data showed a dose-proportional increase in APG-1387 exposure from 20 mg to 45 mg. Preliminary PD data showed that APG-1387 induced rapid degradation of cellular IAP1 and X-linked IAP in peripheral blood mononuclear cell samples; Increased serum release of interleukins (IL-12, IL-10) and monocyte chemotactic protein 4 was dose and time dependent. Conclusions: APG-1387 combined with pembrolizumab is well tolerated. Encouraging antitumor effects were observed in patients with several tumor types. The ongoing study will further evaluate the efficacy of this combination. Clinical trial information: NCT03386526 .

Published

2020

4. A phase I study of a novel MDM2 antagonist APG-115 in patients with advanced solid tumors

Author

Drew W. Rasco, Alex Amaya, Joan Sun, Yingjie Huang, Nehal Lakhani, Dajun Yang, Yuefen Tang, Yifan Zhai, Jiao Ji, Kathy Estkowski, Zhiyan Liang, Yufeng Li, Hengbang Wang, and Lichuang Men

Subjects

Cancer Research, biology, business.industry, Antagonist, Pharmacology, Phase i study, 03 medical and health sciences, 0302 clinical medicine, Orally active, Mdm2 Protein, Oncology, Apoptosis, 030220 oncology & carcinogenesis, biology.protein, Mdm2, Medicine, In patient, business, Function (biology), 030215 immunology

Abstract

3126 Background: APG-115 is a potent and orally active small-molecule MDM2 protein inhibitor. Binding to MDM2 protein, APG-115 restores p53 tumor suppressive function via induction of apoptosis in tumor cells retaining wild-type p53. In addition, enhanced antitumor activity was demonstrated in the syngeneic tumor models after APG-115 combined with PD-1 blockade. Methods: This Phase I study (APG-115-US-001) was designed to enroll the patients with advanced solid tumors in US (NCT02935907). Study objectives included to assess safety, dose limited toxicity (DLT), pharmacokinetics (PK), pharmacodynamics (PD), and antitumor activity (assessed every 8 weeks per RECIST v1.1). The patients received APG-115 orally every other day (QOD) at the designated dose (ranging from 10 to 300 mg) for first 21 days of a 28-day cycle, until disease progression. Results: Up until Jan 4 2019, total 28 patients were treated with APG-115 at various doses (one patient at 10mg, 20mg and 50mg, respectively; 14 patients at 100mg, 6 patients at 200mg, and 5 patients at 300mg). The median number of prior systemic anticancer therapies was 4 (range 0-15). The DLTs were observed during cycle 1, including one grade 2 thrombocytopenia at 200mg, one grade 3 thrombocytopenia at 300mg, and one grade 3 fatigue at 100mg and 300mg respectively. The most common AEs (reported in ≥10% of pts) included: fatigue, nausea, vomiting, diarrhea, decreased appetite, dehydration, neutrophil count decreased, white blood cell count decreased, pain in extremity, thrombocytopenia. The most common Grade 3 or 4 treatment related AEs were fatigue (10.7%), and thrombocytopenia (10.7%). Six patients had stable disease (SD) after two cycle treatments, two of them are continuing in this study. PK analyses indicated that exposure (Cmax and AUC) generally increases with the increase of dose level from 20 mg to 300 mg. Conclusions: APG-115 was well tolerated and had manageable adverse events. The MTD/RP2D of APG-115 monotherapy with oral administration, QOD for 21 days of a 28-day cycle for treatment of patients with advanced solid tumors was determined as 100 mg. Further evaluation of APG-115 in combination with pembrolizumab in patients with advanced solid tumors is ongoing. Clinical trial information: NCT02935907.

Published

2019

5. A phase I study of a novel IAP inhibitor APG-1387 as a monotherapy or in combination with pembrolizumab in treatments of patients with advanced solid tumors

Author

Dajun Yang, Jiao Ji, Alex Amaya, Joan Sun, Drew W. Rasco, Lichuang Men, Yifan Zhai, Yuefen Tang, Yingjie Huang, Zhiyan Liang, Yufeng Li, and Hengbang Wang

Subjects

Cancer Research, business.industry, Pembrolizumab, Inhibitor of apoptosis, Small molecule, Bivalent (genetics), Phase i study, 03 medical and health sciences, 0302 clinical medicine, Oncology, 030220 oncology & carcinogenesis, Cancer research, Medicine, business, 030215 immunology

Abstract

3125 Background: APG-1387 is a novel, bivalent small molecule IAP (inhibitor of apoptosis proteins) inhibitor. It has shown strong antitumor activities in multiple human xenograft cancer models. APG-1387 also acts as host immune modulator, supporting the notion that APG-1387 in combination with anti-PD1 antibody for cancer therapy. Methods: This study consists of two parts (NCT03386526). Part 1 is the dose escalation study of APG-1387 including a mPC (metastatic pancreatic cancer) cohort expansion. Part 2 is the dose escalation and cohort expansion study of APG-1387 in combination with pembrolizumab. APG-1387 is administrated IV for 30 minutes once weekly in a 21-day-cycle. Pembrolizumab is administrated at 200mg IV on day1 of a 21-day-cycle. The study objectives are to assess the safety, pharmacokinetics (PK), pharmacodynamics (PD), and efficacy (assessed per RECIST v1.1 every 6 weeks). Results: Through Jan 4, 2019, total 23 patients had been treated in 4 cohorts of APG-1387 (20mg, 30mg, 45mg, 60mg). Two DLTs were observed at 60mg including lipase increase and Bell’s palsy, MTD was determined as 45mg. Nineteen of 23 patients experienced at least 1 TEAE. The most common TEAEs were nausea (21.7%), fatigue (17.4%), decreased appetite (13.0%), and abdominal pain (13.0%). Three grade 3 TEAEs including elevated bilirubin, lipase increase, and shortness of breath were documented at 45mg and 60mg. Three out of six mPC patients (one at 60mg, two at 45mg) achieved SD, one of them at 45mg has been treated > 5 cycles with confirmed SD (-18%). Two patients, who were treated with APG-1387 at 20mg in combination with pembrolizumab, had no DLT observed during the first cycle. Preliminary PK data of APG-1387 showed a dose proportionality in exposure (Cmax and AUC) over the dose range of 20-60 mg. Conclusions: APG-1387 was well tolerated and had manageable adverse events. The potential effects of APG-1387 alone or in combination with pembrolizumab deserve further exploration in patients with advanced solid tumors, especially in the mPC patients. Clinical trial information: NCT03386526.

Published

2019

6. A phase 1 study of anti-TGFβ receptor type-II monoclonal antibody LY3022859 in patients with advanced solid tumors

Author

Ivelina Gueorguieva, S. R. Prasad Kambhampati, Shande Tang, John S. Kauh, Jan Cosaert, Kyla Driscoll, Sarina Anne Piha-Paul, Richard Kimbung, Jordan Berlin, Emily Chan, Anthony W. Tolcher, Alex Amaya, and David S. Hong

Subjects

0301 basic medicine, Adult, Male, Cancer Research, medicine.medical_specialty, Maximum Tolerated Dose, medicine.drug_class, medicine.medical_treatment, Antineoplastic Agents, Pharmacology, Receptor type, Toxicology, Monoclonal antibody, Gastroenterology, Article, Cohort Studies, 03 medical and health sciences, Young Adult, Pharmacokinetics, Internal medicine, Neoplasms, Dose escalation, Medicine, Humans, Pharmacology (medical), In patient, Infusions, Intravenous, Aged, Dose-Response Relationship, Drug, business.industry, Antibodies, Monoclonal, Middle Aged, medicine.disease, Cytokine release syndrome, 030104 developmental biology, Cytokine, Treatment Outcome, Oncology, Cohort, Cytokines, Female, business, Receptors, Transforming Growth Factor beta, Half-Life

Abstract

LY3022859 is an anti-TGFβRII IgG1 monoclonal antibody that inhibits receptor-mediated signaling activation. The primary objective of this phase I study was to determine a phase II dose in patients with advanced solid tumors. Secondary objectives were to assess safety and pharmacokinetics (PK). LY3022859 was infused intravenously (IV) at 1.25 mg/kg over 1 h every 2 weeks (Q2W) (cohort 1A) and at flat doses of 12.5 mg (cohort 1B) and 25 mg (cohort 2) over 3 h Q2W. Fourteen patients were enrolled in cohorts 1A (n = 2), 1B (n = 5), and 2 (n = 7). DLTs were experienced by both patients in cohort 1A (infusion-related reaction) and 2 patients in cohort 2 (cytokine release syndrome and infusion-related reaction). No MTD was determined. At the 25 mg dose level (cohort 2), after fifth infusion, LY3022859 had a short t1/2 (4.37-7.80 h) and rapid clearance (CLss, 0.412 L/h). Exposure increased twofold (from 28.5 to 60.2 μg·h/mL) with increase in dose from 12.5 to 25 mg. No accumulation was observed after repeat administration. The MTD for LY3022859 was not determined. Dose escalation beyond 25 mg was considered unsafe due to worsening symptoms (uncontrolled cytokine release) despite prophylaxis (corticosteroids and antihistamines). clinicaltrials.gov Identifier: NCT01646203.

Published

2016

7. A phase I study of novel dual Bcl-2/Bcl-xL inhibitor APG-1252 in patients with advanced small cell lung cancer (SCLC) or other solid tumor

Author

Lichuang Men, Sreenivasa R Chandana, Yvette Cole, Yingjie Huang, Hengbang Wang, Nehal Lakhani, Kyriakos P. Papadopoulos, Timothy J. O'Rourke, Anthony W. Tolcher, Amita Patnaik, Qi Dong, Jiao Ji, Alex Amaya, Dajun Yang, Theresa Mays, Drew W. Rasco, Yifan Zhai, and Brianne Kaiser

Subjects

0301 basic medicine, Cancer Research, business.industry, Phase i study, Bcl 2 bcl xl, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Oncology, In vivo, 030220 oncology & carcinogenesis, Toxicity, Cancer research, Medicine, Platelet, In patient, Non small cell, business, Solid tumor

Abstract

2594Background: We have developed a unique strategy to tactically reduce on-target platelet toxicity with APG-1252, a novel dual Bcl-2/Bcl-xL inhibitor, while maintaining strong in vivo antitumor a...

Published

2018

8. A phase 1b study of combined angiogenesis blockade with nesvacumab, a selective monoclonal antibody (MAb) to angiopoietin-2 (Ang2) and ziv-aflibercept in patients with advanced solid malignancies

Author

Albiruni Ryan Abdul Razak, Jason A. Konner, Lieve Adriaens, Carrie Brownstein, Ana Kostic, Bo Gao, Drew W. Rasco, Amita Patnaik, Daniela Matei, Pamela Trail, A. Thomas DiCioccio, Philippe L. Bedard, Alex Amaya, Kyriakos P. Papadopoulos, Anthony W. Tolcher, Lainie P. Martin, Israel Lowy, Lillian L. Siu, Kathleen N. Moore, and Donna M. Graham

Subjects

Nesvacumab, Cancer Research, medicine.drug_class, Angiogenesis, business.industry, Ziv-Aflibercept, Pharmacology, Monoclonal antibody, Fusion protein, Blockade, law.invention, Oncology, law, cardiovascular system, medicine, Recombinant DNA, Decoy, business

Abstract

2522 Background: Nesvacumab (N) is a selective, human Ang-2 MAb, that potently blocks Ang2 signaling through the Tie2 receptor. Ziv-aflibercept (Z) is a recombinant human fusion protein and a decoy...

Published

2014

9. Design of a phase I clinical trial with PNT2258, a novel DNA interference oligonucleotide (DNAi), in patients with advanced solid tumors

Author

Drew W. Rasco, Neal Goodwin, Wendi V. Rodrigueza, Shari Kay Gaylor, Amita Patnaik, Alex Amaya, Timothy David Moore, Robert Forgey, Anthony W. Tolcher, Kyriakos P. Papadopoulos, and Charles L. Bisgaier

Subjects

Cancer Research, Oligonucleotide, business.industry, dnaI, Phases of clinical research, Drug resistance, Molecular biology, chemistry.chemical_compound, Oncology, chemistry, Cancer cell, Cancer research, Medicine, In patient, business, DNA, Cell survival

Abstract

TPS3110 Background: With the knowledge that Bcl-2 facilitates drug resistance and cell survival, a DNA interference (DNAi) strategy was applied to silence Bcl-2 in cancer cells and promote apoptosis. DNAi differs from cytoplasmic mRNA targeting (antisense, RNAi, and miRNA targets) as it targets genomic DNA, blocking transcription. PNT100, a first in class DNAi, is a novel single-stranded 24-base unmodified DNA designed to bind to an upstream region of the Bcl-2 promoter. The drug product (PNT2258) is PNT100 encapsulated in a specialized pH tunable liposome and is being assessed for safety and tolerability in a phase I trial. PNT2258 avoids the toxicities associated with modified oligonucleotides and double-stranded RNAs; since the liposome formulation is anionic and contains no surface spacers, vehicle toxicities are minimal. Xenograft experiments demonstrated marked single agent activity in a diffuse large cell lymphoma, and therapy potentiation when combined with either rituximab in Daudi-Burkitt’s Lymphoma or docetaxel in A375 melanoma. Methods: An open-label, single-arm, first-in-man phase I dose-escalation study of PNT2258 in patients with advanced solid tumors was designed to evaluate safety, tolerability, dose-limiting toxicities, pharmacokinetics, and pharmacodynamics of PNT2258 to recommend a dose for phase II studies. In this phase I study, pharmacodynamic effects of PNT2258 will be evaluated through analyses of soluble serum and plasma markers and peripheral blood mononuclear cells. Patients will receive PNT2258 as an intravenous infusion over 2 hours once daily for 5 consecutive days (days 1-5) of each 21-day treatment cycle (3 weeks). The starting dose of 1 mg/m2 with PNT2258 administered to one patient per cohort and dose-escalation will proceed by dose-doubling in each successive cohort until a dose level of 64 mg/m2 is attained, provided no dose-limiting toxicities are observed in cycle 1. Thereafter, dose escalations shall proceed at 33% increments of the previous cohort dose-level to 85, 113, and 150 mg/m2 with expansions of up to six patients per cohort as needed. The ten planned dose cohorts have been completed with all patients enrolled.

Published

2012

10. Phase I development of a weekly dosing schedule for the oral taxane tesetaxel

Author

Muralidhar Beeram, Ronald Drengler, Kelly Barnhurst, Amita Patnaik, Lon Smith, Loretta M. Itri, Kyriakos P. Papadopoulos, Anthony W. Tolcher, Amy Lang, and Alex Amaya

Subjects

Cancer Research, Taxane, business.industry, Neurotoxicity, Cancer, Neutropenia, Pharmacology, medicine.disease, Metastatic breast cancer, chemistry.chemical_compound, Regimen, Oncology, chemistry, Medicine, Dosing, business, Tesetaxel

Abstract

2555 Background: Tesetaxel (TST) has anticancer activity in patients (pts) with metastatic breast cancer (MBC) and gastric cancer when administered orally once every 3 weeks (Q3W). This drug is not a Pgp substrate, does not cause hypersensitivity reactions, and may be associated with less neurotoxicity. The maximally tolerated dose (MTD) on the Q3W schedule is 27 mg/m2, and neutropenia is dose-limiting. Since taxane activity may be schedule-dependent, we conducted a weekly, dose-ranging, and PK evaluation of TST. Methods: Eligibility: advanced solid tumors; ECOG PS 0-2; adequate organ function. TST was given once weekly for 3 weeks in a 28-day cycle, beginning at a total flat dose of 25 mg/cycle with progressive increases in total dose up to 75 mg/cycle. Subsequently, dosing was converted to a weight-based regimen at weekly doses of 12.5, 15, and 17.5 mg/m2 (i.e., total per cycle dose up to 52.5 mg/m2). Serial plasma samples were assayed by HPLC. Results: 26 pts were treated in 8 dose cohorts. The MTD was 15 mg/m2/wk (total cycle dose, 45 mg/m2). With repeated cycles, constitutional symptoms (fatigue and anorexia) rather than neutropenia proved dose-limiting at 17.5 mg/m2/wk. Only 1 pt (at 12.5 mg/m2/wk) developed grade 3 neutropenia; no other episodes of Grade 3-4 myelotoxicity were observed. One pt with MBC (who had progressed after 2 prior taxane regimens) achieved a PR; 1 pt with prostate cancer has maintained prolonged reduction of PSA (> 57%). PK analyses showed low but progressive increases in trough TST concentrations (0.4–4.6 nmol/mL) 7 days after each succeeding dose, which was consistent with the prolonged T½ of this drug (~180 hrs). There was no substantial drug accumulation over multiple cycles. Conclusions: Weekly oral TST is safe, provides long-term low-level drug exposure, and increases the total delivered dose over 12 wks by 25%. Interestingly, this regimen is not associated with significant myelosuppression. Thus, weekly TST dosing provides a highly convenient, “dose-dense”, taxane regimen that is not associated with neutropenia, which should facilitate its integration into multiple chemotherapy regimens. An ongoing study is evaluating efficacy of weekly TST dosing in MBC.

Published

2012

11. SUTURELESS VESICO-URETHRAL ANASTOMOSIS AFTER RADICAL PROSTATECTOMY: INITIAL CLINICAL FEASIBILITY DATA FROM THE CONTINUUM STUDY

Author

Jaime Landman, Gregory W. Hruby, Alireza Moinzadeh, John A. Libertino, Naveen Kella, Linda Topjian, Ingolf A. Tuerk, Mitchell C. Benson, Bruce Roser, and Alex Amaya

Subjects

medicine.medical_specialty, Continuum (topology), Vesico urethral, Prostatectomy, business.industry, Urology, medicine.medical_treatment, medicine, Anastomosis, business

Published

2008

12. FACTORES PRENATALES E INTRAPARTO RELACIONADOS CON PUNTAJE DE APGAR BAJO EN HOSPITAL NACIONAL ZACAMIL.

Author

Claros, Alex Amaya, Arévalo, José Raúl, and López, Enrique

Abstract

En el Hospital Nacional Zacamil se realizó un estudio Descriptivo, retrospectivo de 44 casos de madres que tuvieron hijos con pun taje de APGAR bajo al primer o al quinto minuto de vida durante el año 2004, con el objetivo de conocer la frecuencia, factores obstétricos relacionados, vía del parto y métodos de reanimación utilizados en el neonato con APGAR bajo en el servicio de Partos de dicha institución. Se encontró que durante el año 2004 se asistieron un total de 3,027 partos de los cuales 44 casos tuvieron APGAR de 6 ó menos representando una frecuencia de 1.4%. De los neonatos con APGAR bajo al minuto se encontró una tasa de recuperacion satisfactoria mayor al 80% a los 5min. La mayor incidencia se observó en neonatos de término con peso entre rangos normales. Se concluyó que Ia edad materna, primiparidad, control prenatal incompleto o ausente, distocias de parto y cesáreas son factores de riesgo para que el recién nacido presente APGAR bajo. [ABSTRACT FROM AUTHOR]

Published

2005

13. La figura de Franco en el discurso de la Organización Sindical Española durante los años del desarrollismo a través del Diario Pueblo (1957-1969)

Author

Àlex Amaya Quer

Subjects

franco, organización sindical, propaganda, desarrollo económico, Social Sciences

Abstract

Este artículo plantea un análisis de la figura de Francisco Franco en el marco del discurso emitido por el aparato de propaganda de la Organización Sindical Española, a través de su órgano principal, el Diario Pueblo, y de otras publicaciones sindicales durante el periodo conocido por Desarrollismo y sus antecedentes. El trabajo quiere establecer las características y evolución de una construcción propagandística de la figura mitificada de Franco ajustada a los intereses políticos del nacionalsindicalismo. Asimismo intenta situarse tanto en el contexto interno de la Organización Sindical, inmersa en un proceso de impulso, reorganización y adaptación, como en la cambiante realidad socio-económica española de los años 60.

Published

2008

14. Com escriure una tesi d’història: consells, tècniques i recursos

Author

Àlex Amaya

Subjects

Doctorat, tesi, tècniques d'escriptura, recursos de discurs, recerca, Modern history, 1453-, D204-475

Abstract

El propòsit d’aquest article és donar consells útils, comprensibles i fàcilment aplicables sobre el procés de redacció d’una tesi doctoral d’història. Certament, no sempre un candidat a doctor té el temps necessari o les eines suficients per abordar amb confiança i possibilitats d’èxit la complexa tasca de posar sobre paper el coneixement acumulat fruit d’anys de recerca. En moltes ocasions el doctorand no té a mà els recursos per realitzar una planificació eficient de la redacció o per anticipar la possibilitat de bloquejos que poden suposar la pèrdua d’un temps preciós. És amb la intenció de cobrir una part d’aquestes necessitats que aquest article, basat en la intervenció que va fer l’autor a les Jornades Doctorials del Departament d’Història Moderna i Contemporània de la UAB el maig de 2012, vol servir d’eina o recurs per a aquells doctorands que assumeixin la importància i beneficis d’escriure bé el seu treball de recerca.

Published

2012