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51. Real World Use of Antidiabetic Drugs in the Years 2011–2017: A Population-Based Study from Southern Italy

Author

Ingrasciotta, Ylenia, primary, Bertuccio, Maria Paola, additional, Crisafulli, Salvatore, additional, Ientile, Valentina, additional, Muscianisi, Marco, additional, L’Abbate, Luca, additional, Pastorello, Maurizio, additional, Provenzano, Vincenzo, additional, Scorsone, Alessandro, additional, Scondotto, Salvatore, additional, and Trifirò, Gianluca, additional

Published
2020
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53. Additional file 2 of In search of potential predictors of erythropoiesis-stimulating agents (ESAs) hyporesponsiveness: a population-based study

Author

Ingrasciotta, Ylenia, Lacava, Viviana, Marcianò, Ilaria, Giorgianni, Francesco, Tripepi, Giovanni, Arrigo, Graziella D’, Chinellato, Alessandro, Tari, Daniele Ugo, Santoro, Domenico, and Trifirò, Gianluca

Subjects
hemic and lymphatic diseases
Abstract

Additional file 2. Multivariate binary logistic regression to evaluate non responsiveness to ESAs between the 2nd and the 6th month after ID in CKD patients.

Published
2020
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54. Additional file 1 of In search of potential predictors of erythropoiesis-stimulating agents (ESAs) hyporesponsiveness: a population-based study

Author

Ingrasciotta, Ylenia, Lacava, Viviana, Marcianò, Ilaria, Giorgianni, Francesco, Tripepi, Giovanni, Arrigo, Graziella D’, Chinellato, Alessandro, Tari, Daniele Ugo, Santoro, Domenico, and Trifirò, Gianluca

Subjects
hemic and lymphatic diseases
Abstract

Additional file 1. Distribution of Hb values during the follow-up among incident ESA users, stratified by indication for use: a) CKD; b) Cancer.

Published
2020
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55. Additional file 5 of In search of potential predictors of erythropoiesis-stimulating agents (ESAs) hyporesponsiveness: a population-based study

Author

Ingrasciotta, Ylenia, Lacava, Viviana, Marcianò, Ilaria, Giorgianni, Francesco, Tripepi, Giovanni, Arrigo, Graziella D’, Chinellato, Alessandro, Tari, Daniele Ugo, Santoro, Domenico, and Trifirò, Gianluca

Abstract

Additional file 5. ROC curve to predict the discriminant power of non-responsiveness in Cancer.

Published
2020
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56. Additional file 4 of In search of potential predictors of erythropoiesis-stimulating agents (ESAs) hyporesponsiveness: a population-based study

Author

Ingrasciotta, Ylenia, Lacava, Viviana, Marcianò, Ilaria, Giorgianni, Francesco, Tripepi, Giovanni, Arrigo, Graziella D’, Chinellato, Alessandro, Tari, Daniele Ugo, Santoro, Domenico, and Trifirò, Gianluca

Subjects
hemic and lymphatic diseases
Abstract

Additional file 4. Multivariate binary logistic regression to evaluate non responsiveness to ESAs between the 2nd and the 6th month after ID in cancer patients.

Published
2020
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57. Additional file 3 of In search of potential predictors of erythropoiesis-stimulating agents (ESAs) hyporesponsiveness: a population-based study

Author

Ingrasciotta, Ylenia, Lacava, Viviana, Marcianò, Ilaria, Giorgianni, Francesco, Tripepi, Giovanni, Arrigo, Graziella D’, Chinellato, Alessandro, Tari, Daniele Ugo, Santoro, Domenico, and Trifirò, Gianluca

Subjects
urologic and male genital diseases, female genital diseases and pregnancy complications
Abstract

Additional file 3. ROC curve to predict the discriminant power of non-responsiveness in CKD.

Published
2020
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58. Large-Scale Postmarketing Surveillance of Biological Drugs for Immune-Mediated Inflammatory Diseases Through an Italian Distributed Multi-Database Healthcare Network: The VALORE Project.

Author

Trifirò, Gianluca, Isgrò, Valentina, Ingrasciotta, Ylenia, Ientile, Valentina, L'Abbate, Luca, Foti, Saveria S., Belleudi, Valeria, Poggi, Francesca, Fontana, Andrea, Moretti, Ugo, Lora, Riccardo, Sabaini, Alberto, Senesi, Ilenia, Sorrentino, Carla, Puzo, Maria R., Padula, Angela, Fusco, Mariano, Giordana, Roberta, Solfrini, Valentina, and Puccini, Aurora

Subjects
DRUG utilization, TUMOR necrosis factors, DRUG approval, NETWORK analysis (Planning), OPTIC neuritis
Abstract

Background: Biological drugs have improved the management of immune-mediated inflammatory diseases (IMIDs) despite being associated with important safety issues such as immunogenicity, infections, and malignancies in real-world settings. Objective: The aim of this study was to explore the potential of a large Italian multi-database distributed network for use in the postmarketing surveillance of biological drugs, including biosimilars, in patients with IMID. Methods: A retrospective cohort study was conducted using 13 Italian regional claims databases during 2010–2019. A tailor-made R-based tool developed for distributed analysis of claims data using a study-specific common data model was customized for this study. We measured the yearly prevalence of biological drug users and the frequency of switches between originator and biosimilars for infliximab, etanercept, and adalimumab separately and stratified them by calendar year and region. We then calculated the cumulative number of users and person-years (PYs) of exposure to individual biological drugs approved for IMIDs. For a number of safety outcomes (e.g., severe acute respiratory syndrome coronavirus 2 [SARS-COV-2] infection), we conducted a sample power calculation to estimate the PYs of exposure required to investigate their association with individual biological drugs approved for IMIDs, considering different strengths of association. Results: From a total underlying population of almost 50 million inhabitants from 13 Italian regions, we identified 143,602 (0.3%) biological drug users, with a cumulative exposure of 507,745 PYs during the entire follow-up. The mean age ± standard deviation of biological drug users was 49.3 ± 16.3, with a female-to-male ratio of 1.2. The age-adjusted yearly prevalence of biological drug users increased threefold from 0.7 per 1000 in 2010 to 2.1 per 1000 in 2019. Overall, we identified 40,996 users of biosimilars of tumor necrosis factor (TNF)-α inhibitors (i.e., etanercept, adalimumab, and infliximab) in the years 2015–2019. Of these, 46% (N = 18,845) switched at any time between originator and biosimilars or vice versa. To investigate a moderate association (incidence rate ratio 2) between biological drugs approved for IMIDs and safety events of interest, such as optic neuritis (lowest background incidence rate 10.4/100,000 PYs) or severe infection (highest background incidence rate 4312/100,000 PYs), a total of 43,311 PYs and 104 PYs of exposure to individual biological drugs, respectively, would be required. As such, using this network, of 15 individual biological drugs approved for IMIDs, the association with those adverse events could be investigated for four (27%) and 14 (93%), respectively. Conclusion: The VALORE project multi-database network has access to data on more than 140,000 biological drug users (and > 0.5 million PYs) from 13 Italian regions during the years 2010–2019, which will be further expanded with the inclusion of data from other regions and more recent calendar years. Overall, the cumulated amount of person-time of exposure to biological drugs approved for IMIDs provides enough statistical power to investigate weak/moderate associations of almost all individual compounds and the most relevant safety outcomes. Moreover, this network may offer the opportunity to investigate the interchangeability of originator and biosimilars of several TNFα inhibitors in different therapeutic areas in real-world settings. [ABSTRACT FROM AUTHOR]

Published
2021
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59. MOESM1 of In search of potential predictors of erythropoiesis-stimulating agents (ESAs) hyporesponsiveness: a population-based study

Author

Ingrasciotta Ylenia, Lacava Viviana, Marcianò Ilaria, Giorgianni Francesco, Tripepi Giovanni, D’ Graziella, Chinellato Alessandro, Tari Ugo, Santoro Domenico, and Trifirò Gianluca

Subjects
hemic and lymphatic diseases
Abstract

Additional file 1. Distribution of Hb values during the follow-up among incident ESA users, stratified by indication for use: a) CKD; b) Cancer.

Published
2019
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62. How Have Intravitreal Anti-VEGF and Dexamethasone Implant Been Used in Italy? A Multiregional, Population-Based Study in the Years 2010–2016

Author

Scondotto, Giulia, primary, Sultana, Janet, additional, Ientile, Valentina, additional, Ingrasciotta, Ylenia, additional, Fontana, Andrea, additional, Copetti, Massimiliano, additional, Mirabelli, Eliana, additional, Trombetta, Costantino J., additional, Rapisarda, Carlo, additional, Reibaldi, Michele, additional, Avitabile, Teresio, additional, Longo, Antonio, additional, Toro, Patricia Ibanez, additional, Vadalà, Maria, additional, Cillino, Salvatore, additional, Virgili, Gianni, additional, Gini, Rosa, additional, Leoni, Olivia, additional, Pollina Addario, Sebastiano Walter, additional, Cananzi, Pasquale, additional, La Cavera, Claudia, additional, Puzo, Maria Rosalia, additional, De Sarro, Giovambattista, additional, De Francesco, Adele, additional, and Trifirò, Gianluca, additional

Published
2020
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64. Role of healthcare databases and registries for surveillance of orphan drugs in the real-world setting: the Italian case study

Author

Crisafulli, Salvatore, primary, Sultana, Janet, additional, Ingrasciotta, Ylenia, additional, Addis, Antonio, additional, Cananzi, Pasquale, additional, Cavagna, Lorenzo, additional, Conter, Valentino, additional, D’Angelo, Gabriella, additional, Ferrajolo, Carmen, additional, Mantovani, Lorenzo, additional, Pastorello, Maurizio, additional, Scondotto, Salvatore, additional, and Trifirò, Gianluca, additional

Published
2019
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65. The Role of European Healthcare Databases for Post-Marketing Drug Effectiveness, Safety and Value Evaluation: Where Does Italy Stand?

Author

Trifirò, G, Gini, R, Barone-Adesi, F, Beghi, E, Cantarutti, A, Capuano, A, Carnovale, C, Clavenna, A, Dellagiovanna, M, Ferrajolo, C, Franchi, M, Ingrasciotta, Y, Kirchmayer, U, Lapi, F, Leone, R, Leoni, O, Lucenteforte, E, Moretti, U, Mugelli, A, Naldi, L, Poluzzi, E, Rafaniello, C, Rea, F, Sultana, J, Tettamanti, M, Traversa, G, Vannacci, A, Mantovani, L, Corrao, G, Trifirò, Gianluca, Gini, Rosa, Barone-Adesi, Francesco, Beghi, Ettore, Cantarutti, Anna, Capuano, Annalisa, Carnovale, Carla, Clavenna, Antonio, Dellagiovanna, Mirosa, Ferrajolo, Carmen, Franchi, Matteo, Ingrasciotta, Ylenia, Kirchmayer, Ursula, Lapi, Francesco, Leone, Roberto, Leoni, Olivia, Lucenteforte, Ersilia, Moretti, Ugo, Mugelli, Alessandro, Naldi, Luigi, Poluzzi, Elisabetta, Rafaniello, Concita, Rea, Federico, Sultana, Janet, Tettamanti, Mauro, Traversa, Giuseppe, Vannacci, Alfredo, Mantovani, Lorenzo, Corrao, Giovanni, Trifirò, G, Gini, R, Barone-Adesi, F, Beghi, E, Cantarutti, A, Capuano, A, Carnovale, C, Clavenna, A, Dellagiovanna, M, Ferrajolo, C, Franchi, M, Ingrasciotta, Y, Kirchmayer, U, Lapi, F, Leone, R, Leoni, O, Lucenteforte, E, Moretti, U, Mugelli, A, Naldi, L, Poluzzi, E, Rafaniello, C, Rea, F, Sultana, J, Tettamanti, M, Traversa, G, Vannacci, A, Mantovani, L, Corrao, G, Trifirò, Gianluca, Gini, Rosa, Barone-Adesi, Francesco, Beghi, Ettore, Cantarutti, Anna, Capuano, Annalisa, Carnovale, Carla, Clavenna, Antonio, Dellagiovanna, Mirosa, Ferrajolo, Carmen, Franchi, Matteo, Ingrasciotta, Ylenia, Kirchmayer, Ursula, Lapi, Francesco, Leone, Roberto, Leoni, Olivia, Lucenteforte, Ersilia, Moretti, Ugo, Mugelli, Alessandro, Naldi, Luigi, Poluzzi, Elisabetta, Rafaniello, Concita, Rea, Federico, Sultana, Janet, Tettamanti, Mauro, Traversa, Giuseppe, Vannacci, Alfredo, Mantovani, Lorenzo, and Corrao, Giovanni

Abstract

Enormous progress has been made globally in the use of evidence derived from patients’ clinical information as they access their routine medical care. The value of real-world data lies in their complementary nature compared with data from randomised controlled trials: less detailed information on drug efficacy but longer observational periods and larger, more heterogeneous study populations reflecting clinical practice because individuals are included who would not usually be recruited in trials. Real-world data can be collected in various types of electronic sources, such as electronic health records, claims databases and drug or disease registries. These data sources vary in nature from country to country, according to national healthcare system structures and national policies. In Italy, a growing number of healthcare databases have been used to evaluate post-marketing drug utilisation and safety in the last two decades. The aim of this narrative review is to describe the available Italian sources of real-world data and their contribution to generating post-marketing evidence on drug use and safety. We also discuss the strengths and limitations of the most commonly used Italian healthcare databases in addressing various research questions concerning drug utilisation, comparative effectiveness and safety studies, as well as health technology assessment and other areas

Published
2019

66. Direct healthcare costs of chronic kidney disease management in Italy: What cost‐savings can be achieved with higher biosimilar uptake and more appropriate use of erythropoiesis‐stimulating agents?

Author

Ingrasciotta, Ylenia, Sultana, Janet, Formica, Dario, Ientile, Valentina, Aiello, Andrea, Chinellato, Alessandro, Tari, Daniele Ugo, Gini, Rosa, Pastorello, Maurizio, Scondotto, Salvatore, Cananzi, Pasquale, Traversa, Giuseppe, Rossi, Mariangela, Santoro, Domenico, and Trifirò, Gianluca

Abstract

Purpose Erythropoiesis‐stimulating agents (ESAs), are used for treating chronic kidney disease (CKD)‐related anemia, contributing to CKD costs. The study was aimed at investigating direct healthcare costs of CKD patients treated with ESAs and the potential savings achievable by increasing the use of biosimilars and preventing inappropriate ESA use. Methods: A multi‐center, cohort study was conducted using claims databases of five large Italian geographic areas. Yearly mean direct healthcare costs per patient were estimated, stratifying by CKD stage. The total yearly cost and potential savings related to ESA use were estimated: (a) considering 25/50/75% of originator ESA substitution with biosimilars; (b) eliminating inappropriate ESA dispensing. Results: During the study period, the ESA‐related yearly mean cost represented 17% of total yearly costs in stage I‐III, decreasing to 13% in stage IV‐V and 6% in dialysis. Among originator users, assuming a 25% of biosimilar uptake, the annual cost‐savings of ESA treatment would represent 10.5% of total ESA costs in CKD stage I‐V and 7.7% in dialysis. Among incident ESA users for which hemoglobin levels were available, 9% started inappropriately ESA treatment, increasing to 62.0% during the first year of maintenance therapy. Hypothesizing prevention of the first inappropriate ESA dispensing, the total yearly cost‐savings would amount to €35 772, increasing to €167 641 eliminating the inappropriate dispensing during maintenance therapy. Conclusions: Higher use of lowest cost ESA, prevention of inappropriate ESA use as well as other strategies aimed at slowing down the progressive renal impairment are essential for minimizing clinical and economic burden of CKD. [ABSTRACT FROM AUTHOR]

Published
2021
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68. The Role of European Healthcare Databases for Post-Marketing Drug Effectiveness, Safety and Value Evaluation: Where Does Italy Stand?

Author

Trifirò, Gianluca, primary, Gini, Rosa, additional, Barone-Adesi, Francesco, additional, Beghi, Ettore, additional, Cantarutti, Anna, additional, Capuano, Annalisa, additional, Carnovale, Carla, additional, Clavenna, Antonio, additional, Dellagiovanna, Mirosa, additional, Ferrajolo, Carmen, additional, Franchi, Matteo, additional, Ingrasciotta, Ylenia, additional, Kirchmayer, Ursula, additional, Lapi, Francesco, additional, Leone, Roberto, additional, Leoni, Olivia, additional, Lucenteforte, Ersilia, additional, Moretti, Ugo, additional, Mugelli, Alessandro, additional, Naldi, Luigi, additional, Poluzzi, Elisabetta, additional, Rafaniello, Concita, additional, Rea, Federico, additional, Sultana, Janet, additional, Tettamanti, Mauro, additional, Traversa, Giuseppe, additional, Vannacci, Alfredo, additional, Mantovani, Lorenzo, additional, and Corrao, Giovanni, additional

Published
2018
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70. Pattern of Use of Biosimilar and Originator Somatropin in Italy: A Population-Based Multiple Databases Study During the Years 2009–2014

Author

Marcianò, Ilaria, primary, Ingrasciotta, Ylenia, additional, Giorgianni, Francesco, additional, Ientile, Valentina, additional, Chinellato, Alessandro, additional, Tari, Daniele Ugo, additional, Gini, Rosa, additional, Cannavò, Salvatore, additional, Pastorello, Maurizio, additional, Scondotto, Salvatore, additional, Cananzi, Pasquale, additional, Traversa, Giuseppe, additional, Trotta, Francesco, additional, Belleudi, Valeria, additional, Addis, Antonio, additional, and Trifirò, Gianluca, additional

Published
2018
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73. In Search of Predictors of Switching Between Erythropoiesis-Stimulating Agents in Clinical Practice: A Multi-Regional Cohort Study.

Author

Ingrasciotta, Ylenia, Belleudi, Valeria, Trotta, Francesco, Addis, Antonio, Fontana, Andrea, Chinellato, Alessandro, Ientile, Valentina, Tari, Daniele Ugo, Roberto, Giuseppe, Pastorello, Maurizio, Scondotto, Salvatore, Cananzi, Pasquale, Traversa, Giuseppe, Davoli, Marina, Rossi, Mariangela, Trifirò, Gianluca, On behalf of the Italian Biosimilars Network (I-BioNetwork), Caputi, Achille P., Bolcato, Jenny, and Pirolo, Roberta

Subjects
*COHORT analysis, *CHRONIC kidney failure, *CHRONICALLY ill
Abstract

Background and objectives: Switching between different erythropoiesis-stimulating agents (ESAs) during the first year of therapy is frequent (15–20%), much more so toward reference products than biosimilars. The objectives of this study were to investigate the frequency and identify the potential predictors of switching between biosimilar and originator ESAs during the first year of treatment in patients with chronic kidney disease (CKD), or chemotherapy-related anemia from six large Italian geographic areas in the years 2009–2015. Methods: A retrospective cohort study was conducted using six Italian regional claims databases (≥ 13 million inhabitants) during 2009–2015. Among incident epoetin users, the frequency of single, multiple, and backward switch during the first year of treatment was evaluated. Using frailty Cox models, potential predictors of first switch were identified. All analyses were stratified by the main indications for use. Results: Among 102,240 incident epoetin users, 15,853 (15.5%) switched to another epoetin during the first year of therapy; only 18% of these switched to biosimilars. Single switch was more common (62.2% of the switchers) than multiple (23.5%) or backward switch (14.3%). In cancer, the cumulative number of transfusions and iron preparations dispensed, as well as hyperparathyroidism, were predictors of switching. In CKD, the cumulative number of transfusions, number of vitamin A/D preparations dispensed, and CKD severity increased the probability of switching. Conclusions: Switching between ESAs was frequent in both CKD and cancer patients. The number of cumulative transfusions and severity of disease seemed to affect the switch. [ABSTRACT FROM AUTHOR]

Published
2020
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74. Effectiveness and Safety of Switching Originator and Biosimilar Epoetins in Patients with Chronic Kidney Disease in a Large-Scale Italian Cohort Study.

Author

Belleudi, Valeria, Trotta, Francesco, Addis, Antonio, Ingrasciotta, Ylenia, Ientile, Valentina, Tari, Michele, Gini, Rosa, Pastorello, Maurizio, Scondotto, Salvatore, Cananzi, Pasquale, Traversa, Giuseppe, Davoli, Marina, Trifirò, Gianluca, the Italian Biosimilar Network (ItaBioNet), Caputi, Achille P., Giorgianni, Francesco, Marcianò, Ilaria, Chinellato, Alessandro, Bolcato, Jenny, and Pirolo, Roberta

Subjects
KIDNEY diseases, MEDICAL decision making, EPOETIN alfa (Drug), CONFIDENCE intervals, COHORT analysis, BIOTHERAPY, CHRONIC kidney failure complications, ANEMIA, BIOLOGICAL products, CHRONIC kidney failure, COMMERCIAL product evaluation, ERYTHROPOIETIN, LONGITUDINAL method, MEDICAL record linkage, PROBABILITY theory, TREATMENT effectiveness, RETROSPECTIVE studies, DISEASE complications
Abstract

Introduction: Real-world data on the comparative effectiveness and safety of switching among different epoetins (including originators and biosimilars) are limited. In light of current debate about interchangeability, prescribers, some patient groups and decision makers are calling for additional post-marketing evidence on the clinical effects of switching between originator and biosimilar epoetins in chronic kidney disease (CKD) patients.Objective: The objective of this study was to evaluate the effectiveness and safety of switching versus non-switching and of switching from originator/biosimilar epoetin alpha (ESA α) to any other epoetin in CKD patients.Methods: An observational, record-linkage, multi-database, retrospective cohort study was carried out in four Italian geographical areas. All subjects with at least one ESA α dispensing between 1 January 2009 and 31 December 2015 were retrieved. Switching was defined as any transition between originator/biosimilar ESA α to any other epoetin in a series of two consecutive prescriptions up to 2 years. Switchers were matched 1:1 with non-switchers by baseline propensity score and by duration of ESA α treatment. Switchers and non-switchers were followed up from switching date to a maximum of 1 year. Lack of effectiveness and safety of switching versus non-switching were evaluated through Cox regression models (hazard ratio [HR], 95% confidence interval [CI]). A direct comparison between the two switcher categories (switchers from originator/biosimilar ESA α to any other epoetin) was also performed.Results: Overall, 14,400 incident users of ESA α for anaemia due to CKD (61.4% originator, 38.6% biosimilar) were available for analysis. During the follow-up, we found no differences on effectiveness (HR 1.02, 95% CI 0.79-1.31 originators; HR 1.16, 95% CI 0.75-1.79 biosimilars) and safety outcomes (HR 1.08, 95% CI 0.77-1.50 originators; HR 1.20, 95% CI 0.66-2.21 biosimilars) between switchers and non-switchers of ESA α. Cumulative probabilities of recording an adverse event, either in terms of lack of effectiveness or safety issue, were the same for two switching categories CONCLUSIONS: In this large-scale Italian observational multi-database study, switching versus non-switching as well as switching from biosimilar/originator ESA α to any other epoetin in CKD patients is not associated with any effectiveness and safety outcomes. [ABSTRACT FROM AUTHOR]

Published
2019
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75. Quanto sono utilizzati in Italia i farmaci biosimilari? Uno studio retrospettivo sull'uso degli agenti stimolanti l'eritropoiesi negli anni 2009-2013

Author

Ingrasciotta, Ylenia, Giorgianni, Francesco, Bolcato, Jenny, Chinellato, Alessandro, Pirolo, Roberta, Tari, Daniele Ugo, Troncone, Chiara, Fontana, Andrea, Ien6le, Valen6na, Gini, Rosa, Santoro, Domenico, Santarpia, Mariacarmela, Genazzani, Armando, Uomo, Ilaria, Pastorello, Maurizio, Addario, Walter Sebas6ano Pollina, Scondo_o, Salvatore, Cananzi, Pasquale, Caputi Achille Patrizio, and Trifiro', Gianluca

Published
2015

76. Comparative Effectiveness of Biosimilar, Reference Product and Other Erythropoiesis-Stimulating Agents (ESAs) Still Covered by Patent in Chronic Kidney Disease and Cancer Patients: An Italian Population-Based Study

Author

Ingrasciotta, Ylenia, primary, Giorgianni, Francesco, additional, Marcianò, Ilaria, additional, Bolcato, Jenny, additional, Pirolo, Roberta, additional, Chinellato, Alessandro, additional, Ientile, Valentina, additional, Santoro, Domenico, additional, Genazzani, Armando A., additional, Alibrandi, Angela, additional, Fontana, Andrea, additional, Caputi, Achille P., additional, and Trifirò, Gianluca, additional

Published
2016
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77. Association of Individual Non-Steroidal Anti-Inflammatory Drugs and Chronic Kidney Disease: A Population-Based Case Control Study

Author

Ingrasciotta, Ylenia, primary, Sultana, Janet, additional, Giorgianni, Francesco, additional, Fontana, Andrea, additional, Santangelo, Antonio, additional, Tari, Daniele Ugo, additional, Santoro, Domenico, additional, Arcoraci, Vincenzo, additional, Perrotta, Margherita, additional, Ibanez, Luisa, additional, and Trifirò, Gianluca, additional

Published
2015
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78. Interchangeability of biosimilar and biological reference product: updated regulatory positions and pre- and post-marketing evidence

Author

Trifirò, Gianluca, Marcianò, Ilaria, and Ingrasciotta, Ylenia

Abstract

ABSTRACTIntroduction: Since 2006, biosimilars have been available in several countries worldwide, thus allowing for potential savings in pharmaceutical expenditure. However, there have been numerous debates about the interchangeability of biosimilars and reference products based on concerns of immunogenicity by switching between biological products, which may cause lack of effect and toxicity.Areas covered: The authors provide the reader with an overview of the different positions of regulatory authorities on the interchangeability and automatic substitution of biosimilars and reference products. Presently, the FDA allows automatic substitution without prescriber intervention if the biosimilar is interchangeable with reference products, while the European Medicines Agency delegate to each single EU member state.Expert opinion: Different approaches in defining interchangeability and automatic substitution call for harmonization to increase confidence of healthcare professionals and patients about the clinical impact of switching. Networks of electronic healthcare records and administrative databases, potentially linkable to clinical charts and registries may rapidly assess frequency and benefit-risk profile of different switching patterns in routine care at different levels, thus integrating and strengthening pre-marketing evidence.

Published
2018
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79. The Burden of Nephrotoxic Drug Prescriptions in Patients with Chronic Kidney Disease: A Retrospective Population-Based Study in Southern Italy

Author

Ingrasciotta, Ylenia, primary, Sultana, Janet, additional, Giorgianni, Francesco, additional, Caputi, Achille Patrizio, additional, Arcoraci, Vincenzo, additional, Tari, Daniele Ugo, additional, Linguiti, Claudio, additional, Perrotta, Margherita, additional, Nucita, Andrea, additional, Pellegrini, Fabio, additional, Fontana, Andrea, additional, Cavagna, Lorenzo, additional, Santoro, Domenico, additional, and Trifirò, Gianluca, additional

Published
2014
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80. Chronic Kidney Disease Requiring Healthcare Services: A New Approach to Evaluate Epidemiology of Renal Disease

Author

Trifirò, Gianluca, primary, Sultana, Janet, additional, Giorgianni, Francesco, additional, Ingrasciotta, Ylenia, additional, Buemi, Michele, additional, Muscianisi, Marco, additional, Tari, Daniele Ugo, additional, Perrotta, Margherita, additional, Canale, Valeria, additional, Arcoraci, Vincenzo, additional, and Santoro, Domenico, additional

Published
2014
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81. In search of potential predictors of erythropoiesis-stimulating agents (ESAs) hyporesponsiveness: a population-based study.

Author

Ylenia, Ingrasciotta, Viviana, Lacava, Ilaria, Marcianò, Francesco, Giorgianni, Giovanni, Tripepi, Graziella, D' Arrigo, Alessandro, Chinellato, Ugo, Tari Daniele, Domenico, Santoro, Gianluca, Trifirò, Ingrasciotta, Ylenia, Lacava, Viviana, Marcianò, Ilaria, Giorgianni, Francesco, Tripepi, Giovanni, D' Arrigo, Graziella, Chinellato, Alessandro, Ugo Tari, Daniele, Santoro, Domenico, and Trifirò, Gianluca

Subjects
CHRONICALLY ill, ERYTHROPOIESIS, CHRONIC kidney failure, CANCER patients, DRUG efficacy, ANEMIA treatment, BIOSIMILARS, PUBLIC health surveillance, RESEARCH, HEMATOPOIETIC agents, RESEARCH methodology, RETROSPECTIVE studies, EVALUATION research, MEDICAL cooperation, COMPARATIVE studies, ANEMIA, FORECASTING, RESEARCH funding, TUMORS, ERYTHROPOIETIN, LONGITUDINAL method, PHARMACODYNAMICS
Abstract

Background: Evidences show that around 20% of biosimilar or originator erythropoiesis-stimulating agents (ESAs) users are hyporesponsive. Controversial post-marketing data exist on the predictors of ESA hyporesponsiveness. The aim of this study was to identify predictors of ESA hyporesponsiveness in patients with chronic kidney disease (CKD) or cancer in clinical practice.Methods: During the years 2009-2015, a multi-center, population-based, cohort study was conducted using claims databases of Treviso and Caserta Local Health Units (LHUs). All incident ESA users were characterized at baseline and the differences between the baseline hemoglobin (Hb) value, that is the Hb registered within 30 days prior to the first ESA dispensing (index date, ID) and each outcome Hb value (registered between 30 and 180 days after ID) were calculated and defined as delta Hb (ΔHb). Incident ESA users were defined as hyporesponsive if, during follow-up, they registered at least one ΔHb < 0 g/dL. Including all potential predictors of ESA hyporesponsiveness and stratifying by indication for use, univariate and multivariate binary logistic regression models and Receiver Operating Characteristic (ROC) curves were carried out.Results: In general, 1080 incident ESA users (CKD: 57.0%; cancer: 43.0%) were identified. In CKD, predictors of ESA hyporesponsiveness were C-reactive protein (OR = 1.2, 95% CI: 1.0-1.5; P-value = 0.060) and high levels of baseline Hb (OR = 1.7, 95% CI: 1.2-2.2; P-value< 0,001), the latter being also predictor of ESA hyporesponsiveness in cancer (OR = 1.7, 95% CI: 1.1-2.4; P-value = 0.007). Both in CKD and in cancer, the type of ESA, biosimilar or originator, was not a predictor of ESA hyporesponsiveness. In CKD, concomitant use of iron preparations (OR = 0.3, 95% CI: 0.2-0.7; P-value = 0.002) and of high dosage of angiotensin-converting enzyme inhibitors/angiotensin II-receptor blockers (OR = 0.5, 95% CI: 0.3-0.9; P-value = 0.022) were protective factors against ESA hyporesponsiveness.Conclusions: The study confirmed traditional potential predictors of hyporesponsiveness to ESA. The use of biosimilar or originator ESA was not a predictor of hyporesponsiveness in an outpatient setting from two large Italian areas. A better knowledge of the predictors of ESA response would allow a better anemia management to improve patients' quality of life. [ABSTRACT FROM AUTHOR]

Published
2019
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82. Covid Vaccines Effectiveness (CoVE) Effectiveness of heterologous and booster COVID-19 vaccination in 5 European countries, using a cohort approach in children and adults with a full primary COVID-19 vaccination regimen

Author

Martín-Merino, Elisa, Riefolo, Fabio, Vaz, Tiago, Grimaldi, Lamiae, Gini, Rosa, Castillo Cano, Belén, Messina, Davide, Elbers, Roel, Martín Pérez, Mar, Brink-Kwakkel, Dorieke, Villalobos, Felipe, Ientile, Valentina, Swart-Polinder, Karin, Souverein, Patrick, Barbieri, Elisa, García Poza, Patricia, Ingrasciotta, Ylenia, Siiskonen, Satu, Riefolo, Fabio, Garcia de Albeniz, Xavier, Saiz, Luis Carlos, Stona, Luca, Bissacco, Carlo Alberto, and Klungel, Olaf

Subjects
real-word data, vaccines effectiveness, booster, COVID-19, heterologous and homologous vaccine schedule
Abstract

2.3.Rationale and background Real-world effectiveness data demonstrated that COVID-19 vaccines' protection against severe SARS-CoV-2 infection is high in the short term but wanes over time, also depending on the virus variants. The vaccine effectiveness (VE) can vary depending on the vaccine brand or type (e.g., among mRNA or adenoviral platforms). Mixing brands for the primary vaccination and/or boosters (heterologous vaccination schedules) has been applied in different countries or regions although the effectiveness of heterologous schedules was not fully understood beyond immunogenic clinical data. With its increased ability to elude immunity and cause reinfections, the SARS-CoV-2 Omicron variant became dominant worldwide and led to the highest ever COVID-19 incidence, also in countries with high vaccination coverage, increasing as well hospitalization and severe outcomes cases in paediatrics populations, particularly in the presence of comorbidities. Moreover, only limited real-life data information on VE for children and adolescents in the EU is available. Further evidence about the VE of homologous (use of the same COVID-19 vaccine for the primary vaccination and booster dose) and heterologous (use of different COVID-19 vaccines for the primary vaccination or booster dose) vaccination schedules are needed both in adult ad paediatrics populations to keep fueling regulatory authorities' preparedness in case of urgent decision-making situations. 2.4.Research questions and objectives To investigate the VE and waning of immunity of diverse COVID-19 primary vaccination (1st and 2nd doses) and booster (3rd dose) schedules with Comirnaty (PF), Spikevax (MD), and Vaxzevria (AZ) vaccines in preventing different COVID-19-related disease outcomes. Primary objectives To estimate the VE, and its waning, in adults (>17 years old) and adolescents (12-17 years old), separately, between heterologous and homologous primary vaccinations. To estimate the VE, and its waning, in children (5-14 years old) between homologous primary vaccinations and non-vaccination. To estimate the VE, and its waning, in adults and adolescents with full homologous primary regimen between those with a homologous booster and heterologous booster, separately, compared to those without any booster. To estimate the VE, and its waning, in adults and adolescents with full heterologous primary regimen between those with any booster and those without any booster. For patients free of prior COVID-19 infection (all analysis), that VE was estimated: By vaccine brand of the primary homologous scheme, the combinations in the heterologous scheme, and booster dose (3rd dose) By age categories. By time since a complete primary vaccination regimen (2nd dose receipt) or booster among the compared groups. Among clinical subgroups associated with a high risk of severe COVID-19 (immunocompromised patients and patients with cancer, transplants, severe renal disease, and Down syndrome). For patients with prior COVID-19, the overall VE of different vaccination schemes against severe COVID-19 and COVID-19-related death was estimated. Secondary objective To estimate the VE against all-cause mortality in ≥60 years old adults with a full primary regimen (homologous or heterologous) between those with any booster and those without any booster. This estimation complements the results of COVID-19-related death of the primary objective. 2.5. Study design Herein, we present a retrospective cohort study to estimate the VE of different COVID-19 vaccines schemes, and their waning, using different SARS-CoV-2 infection-related outcomes: (i) non-severe COVID-19, (ii) severe COVID-19, and (ii) COVID-19 with death. The study used data from 6 European different data sources and focused on the period ranging from the beginning of the vaccination campaign (December 2020) to the last data available from the participating data sources (ranging from December 2021 to February 2022). Thus, it mainly covered the Delta-Omicron predominant SARS-CoV-2 virus variant periods within the full vaccination regimen (first vaccination scheme and booster doses). 2.6.Setting We retrospectively used data from 6 electronic health care databases in Southern, Northern, and Western Europe: the Italian Caserta local health database (IT-INSPIRE srl), the Italian Societa Servizi Informatici (IT-PEDIANET) database, the Spanish Pharmacoepidemiological Research Database for Public Health System (ES-BIFAP), the Spanish Sistema d’Informació per el Desenvolupament de la Investigació en Atenció Primària (ES-SIDIAP) database, the Dutch PHARMO Database Network (NL-PHARMO), and the British Clinical Practice Research Datalink (UK-CPRD) Aurum. Participants were matched 1:1 on the calendar date of the vaccination of interest (2nd vaccination-time0, for the primary vaccination scheme analysis; 3rd vaccination-booster-time0, for the booster vaccination analysis), the calendar date of the 1st vaccine dose, the vaccine brand of the 1st dose (Comirnaty, Spikevax, Vaxzervria), vaccinees age, sex, geographical region, clinical subgroup, and SARS-CoV-2 infection prior 1st vaccination dose. For primary vaccination schedules, the date of cohort entry (time0) was the date when the participant received the 2nd dose. For the booster vaccinations, the date of cohort entry (booster-time0) was the date when the participant received the 3rd dose. For the non-boosted comparators, the same calendar date as the corresponding boosted-matched individual (booster-time0) was used for comparison. Children and pre-adolescents were defined as “not vaccinated” until the date of the receipt of the 1st COVID-19 vaccine dose, thus, potentially selected as unvaccinated control. Participants were considered to have a complete primary vaccination regimen when the record of a 2nd COVID-19 vaccine dose existed after more than 19 days from the 1st dose. Individuals were defined as “boosted” (homologous or heterologous) from the date of the 3rd COVID-19 vaccine dose receipt if at least 28 days after the 2nd one. Participants were defined as “non-boosted” until the date of 3rd vaccine dose administration, thus, potentially selected as non-boosted control. Among individuals with complete vaccination schemes, both homologous/heterologous primary vaccinations and booster/non-boosted cohorts were identified separately. Statistical data analyses Inverse probability weighted (IPW) Cox models (CI, 95%) have been used to derive the average hazard ratio (HR) of COVID-19-related outcomes. The adjusted VE (%) values were estimated as 1 minus the adjusted HR multiplied by 100. Various covariates have been considered potential confounders for the IPW. The VE for each matched cohort was estimated by (i) vaccine brands, (ii) time after vaccination, (iii) age categories, (iv) high-risk of severe COVID-19 clinical subpopulations (for the participant databases able to identify them through diagnosis or medications prescriptions, (v) and SARS-CoV-2 infection before vaccination, and (vi) dominant SARS-CoV-2 variants (defined as the variant reaching 50% of the total sequenced specimens at (booster-)time 0). Three main SARS-CoV-2 variants’ periods have been identified (pre-Delta, Delta, and Omicrons) specifically for each participating country. Random-effects meta-analyses, using the main estimates against severe COVID-19 outcomes from each data source, were performed for clinical subgroups for both adult and children populations. Sensitivity analysis restricting to patients with prior SARS-CoV-2 negative tests was performed to control for surveillance bias. 2.7.Subjects and study size Study Population The source population comprises all children, adolescents, and adults registered in any of the data sources during the study period (December 2020 -February 2022 for ES-BIFAP and IT-INSPIRE and -December 2021 for the other data sources). Eligible study participants had at least 2 years of available healthcare data. The vaccinated study population includes all individuals with at least two recorded vaccinations since the start of the study period. Study size The study cohorts contained more than 20 million adolescents and adults with a complete primary vaccination scheme (1st and 2nd dose receipt) and 3 to 6 months of follow-up across all the participating data sources. We could match ≈24-51% of the population for the heterologous vaccination scheme (comparator) and ≈0.5-1.5% for the homologous scheme. The majority of adults and adolescents were free of SARS-CoV-2 infection prior to vaccination (58-95% across the total matched population for all the data sources). During the study period, approximately 308,000 children with around 3 months of follow-up were vaccinated with two doses and included in the study across all the participating data sources. Based on the matching criteria, a total of 295,573 children were matched for the primary vaccination schedule (95% of the total children). Of the matched children, the main population (97%, 287,050 children) did not have encountered prior SARS-CoV-2 infection. 2.8.Variables and data sources Data sources captured vaccination and outcomes from hospitalization and/or general practice and/or test registries. This study considered different outcomes related to COVID-19: non-severe SARS-CoV-2 infection, hospitalized COVID-19 (severe), COVID-19 with death, and all-cause mortality (secondary objective). The main exposure of interest was the receipt of a different primary regimen or booster COVID-19 vaccine (receiving the same 1st dose brand), the dose, and its brand. Selection of covariates, primary care physician’ visits, clinical conditions, and medication use (including influenza vaccination among others), were collected up to 2 years before (booster-)time 0 (or 7 days before, for visits to control by healthy vaccinees effect) and considered as potential confounders for the IPW. 2.9.Results The shown VE percentages are statistically significant and reported in ranges of values across the data sources, otherwise, the mention of non-statistically significance is specified. Primary Objectives Adults, Primary Vaccination Among 89,528 adults’ matched pairs, overall, homologous primary vaccinations showed a slightly decreased VE (-27% to –36% by data source) compared to heterologous regimens against non-severe COVID-19, mostly receiving AZ as the first dose (VE ranged from -43% to –27% across data sources). By time since vaccination, or, by age categories, no clear patterns were found. In ES-BIFAP, the lower VE with homologous was more marked during the Delta (-39%) than the Omicron (–24%) periods. No differences between homologous and heterologous regimens were observed for severe COVID-19 (estimated in Spanish data sources) and no sufficient cases of death with COVID-19 were found to analyse. Adolescents, Primary Vaccination We matched 1,329 pairs among adolescents. Considering non-severe COVID-19, no differences were found in the VE estimates comparing homologous versus heterologous primary vaccinations. The small sample size hampered the VE estimation related to the other severe outcomes. Children, Primary Vaccination 287,000 children without prior COVID-19 were matched. Considering non-severe COVID-19, homologous primary two doses of both the mRNA vaccines (PF or MD) showed VE, varying from 29% to 77% across data sources, during the Delta predominant variant period, when compared to unvaccinated individuals. VE remained 4-5 months. During the Omicron predominance, VE decreased from 77% to 42% in IT-INSPIRE and reverted to an increased risk of non-severe SARS-CoV-2 infection, from 29 to -44%, in ES-BIFAP. Estimates did not show protection among children with prior SARS-CoV-2 infection. The protection against severe COVID-19 was >90% in ES-SIDIAP (during the Delta period) and ≈50% in ES-BIFAP for PF vaccine versus unvaccinated individuals. In ES-BIFAP, VE during the Delta period was 61%, but non-statistically significant, and 50% during the Omicron period. No data for waning of immunity, from other data sources, vaccine brands and COVID-19 with death were available. Adults, Booster Vaccination 5.6 million adults without prior SARS-CoV-2 infection were matched. 79,076 cases of non-severe COVID-19 among boosted versus 138,638 among unboosted adults were captured in 5 data sources. VE against non-severe COVID-19 ranged 31-69% for homologous boosters and 42-70% for heterologous boosters across data sources, independently from the vaccine brand. Considering severe COVID-19, 1,015 cases among boosted versus 3,362 among comparators were captured in 3 data sources with hospitalization information (mostly in ES-BIFAP and ES-SIDIAP and a few in IT-INSPIRE). Against severe COVID-19, heterologous boosters (homologous doses 1 and 2), independently from the vaccine brand, showed a VE of 73-81% across data sources whereas homologous boosters have a VE of 42-67%, compared to their respective unboosted controls. Considering death with COVID-19, 313 cases of death with COVID-19 among adults who received any booster versus 1,367 among comparators were captured (mostly in ES-BIFAP and ES-SIDIAP and a few in UK-CPRD). Protection against death with COVID-19 was similar among homologous and heterologous schemes (70-88% across schemes and data sources). Duration of immunization varied from 1 to 6 months across data sources and events, independently of the booster schedule. Considering both, severe COVID-19 and death outcomes, no clear VE differences were identified during both the Delta and Omicron periods across data sources. In patients with cancer, effectiveness against severe COVID-19 ranged from 54% to 77% with heterologous and from 49% to 61% with homologous boosters across data sources, whereas in patients with immunodeficiency VE was between 60-78% with any scheme. Among patients with prior SARS-Cov-2 infection, VE against severe COVID-19 was 69% (ES-BIFAP) and 71% (ES-SIDIAP) for heterologous and 43% (ES-SIDIAP) for homologous 3 doses schemes. VE against death with COVID-19 was 92% (ES-BIFAP) for heterologous and 68% (ES-SIDIAP) for homologous boosters in these patients. Adolescents, Booster Vaccination We matched 17,652 adolescent pairs of which 408 cases of non-severe COVID-19 among boosted versus 936 cases among unboosted individuals were captured in 5 data sources (ES-BIFAP, ES-SIDIAP, IT-INSPIRE, UK-CPRD and NL-PHARMO). Among adolescents with a homologous primary vaccination, the VE of homologous booster doses against non-severe COVID-19 varied from 35-67% across vaccine brands and data sources, whereas VE of heterologous boosters was 48% in ES-BIFAP (the only data source in which heterologous boosters were found) for PF as 1st and 2nd dose, and MD as 3rd dose, when compared to the respective unboosted controls. During the Delta predominance period, VE was only observed in Italy (69%) for homologous boosters. During the Omicron predominance, VE varied from 67% (IT-INSPIRE) to 44% (ES-BIFAP) for homologous boosters whereas, for the heterologous ones, was 51% (ES-BIFAP). VE for the homologous boosters lasted up to one month in Italy (75%; later on, severe COVID-19 and death with COVID-19 outcomes due to the low number of cases (Sensitivity Analysis Balancing by any prior testing, the VE against non-severe infection remained 57-59% for primary vaccination among children and 30-55% for boosters in adults. Against severe COVID-19, VE remained moderate (55-59%) for homologous boosters and high (70-81%) for heterologous boosters. Against death with COVID-19, VE was 67-79% for homologous and 77-81% for heterologous boosters among adults. Meta Analysis In adults, the pooled VE of homologous boosters against severe COVID-19 was 62% (95% CI: 57 to 67%; I2=0%) among subjects with immunodeficiency, 54% (95% CI: 41 to 64%; I2=18%) among patients with cancer, 24% (95% CI: -54 to 63%; I2=0%) among patients with a transplant and 57% (95% CI: -20 to 84%; I2=65%) among those with severe renal disease. Additionally, the pooled VE of homologous booster against death with COVID-19 was 73% (95% CI: 63 to 80%; I2=15%) among immunocompromised patients, 75% (95% CI: 65 to 82%; I2=0%) among patients with cancer, and 75% (95% CI: -38 to 96%; I2=63%) for those with severe renal disease. The pooled VE of heterologous boosters against severe COVID-19 (homologous primary vaccination) was 72% (95% CI: 66 to 77%; I2 =0%) among adults with immunodeficiency and 68% (95% CI: 36 to 84%; I2 =77%) for adults with cancer. In addition, the pooled VE of heterologous boosters against death with COVID-19 was 80% (95% CI: 70 to 86%; I2 =0%) among immunocompromised patients and 81% (CI=95% CI: 70 to 89%; I2 =0%) among those with cancer. Among children, the pooled VE of primary vaccination against severe COVID-19 in the Delta predominance period, was 82% (95% CI: -10 to 97%; I2=62%) in Spain. Secondary Objective (any cause of death) In patients aged ≥60 years old, the VE against any cause of death for any booster dose (whether homologous or heterologous), following a homologous primary vaccination schedule, ranged between 72% and 96% across 10-by-10 age categories and data sources (ES, UK and NL). VE was higher during the Delta (75% for homologous and 83% for heterologous boosters) than the Omicron variant period (67% for both booster types). A few heterologous primary vaccinations were used, showing effectiveness (74%) only in 80+ years old in UK. 2.10.Discussion Using real-world data from 6 different databases in Europe, various schemes of COVID-19 vaccination (primary vaccination and booster doses) were identified among adults, adolescents, and children (only in 3 countries) in Spain, Italy, the Netherlands, and the UK from the beginning of the vaccination campaign to December 2021 or February 2022 (in Italy and Spain). Most of the adults participating in our study were fully vaccinated from mid of 202, The research leading to these results was conducted as part of the activities of the EU PE&PV (Pharmacoepidemiology and Pharmacovigilance) Research Network (led by Utrecht University) with collaboration from the Vaccine Monitoring Collaboration for Europe network (VAC4EU). This study was funded by the European Medicines Agency. The views expressed in this article are the personal views of the author(s) and may not be understood or quoted as being made on behalf of or reflecting the position of the European Medicines Agency or one of its committees or working parties. The project has received support from the European Medicines Agency under the Framework service contract nr EMA/2020/46/TDA/L5.06.

Published
2023
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