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2. Italian Guidelines in patch testing - Adapted from the European Society of Contact Dermatitis (ESCD)

Author

Stingeni, L, Bianchi, L, Hansel, K, Corazza, M, Gallo, R, Guarneri, F, Patruno, C, Rigano, L, Romita, P, Pigattoatt, P, Calzavara-Pintoton, P, Agostinelli, S, Albertazzi, D, Angelini, G, Angerosa, F, Arigliano, P, Assalve, D, Ayala, F, Bellonifortina, A, Berta, M, Biale, C, Biasini, I, Boccaletti, V, Bonamonte, D, Borghi, A, Brambilla, L, Bressan, M, Bruno, A, Caccavale, S, Calogiuri, G, Cannavò, S, Carugno, A, Cataldi, I, Chiarelli, G, Chiesa, A, Cirla, A, Cossutta, M, Cova, L, Cristaudo, A, Dalcan-Ton, M, Damiani, G, Danese, P, Desalvo, V, Fantini, C, Ferrucci, S, Flori, M, Fontana, E, Foti, C, Francalanci, S, Frasin, L, Gola, M, Gravante, M, Guastaferro, D, Ingordo, V, Lauriola, M, Leghissa, P, Lisi, P, Lombardi, P, Lorenzini, M, Magrini, L, Marone, G, Martina, E, Mascagni, P, Matteinichiari, M, Meligeni, L, Melino, M, Milanesi, N, Molinu, A, Monfrecola, G, Morelli, P, Motolese, A, Musumeci, M, Napolitano, M, Nasca, M, Paganini, P, Papini, M, Pasolini, G, Peroni, A, Peserico, A, Piras, V, Pugliese, A, Raponi, F, Raviolo, P, Rebora, A, Recchia, G, Riva, F, Rossi, M, Ruggieri, M, Saggiorato, F, Sartorelli, P, Schena, D, Schettino, A, Spano, G, Stinchi, C, Taddei, L, Tasin, L, Tramontana, M, Valsecchi, R, Vascellaro, A, Venturini, M, Stingeni, L., Bianchi, L., Hansel, K., Corazza, M., Gallo, R., Guarneri, F., Patruno, C., Rigano, L., Romita, P., Pigattoatt, P. D., Calzavara-Pintoton, P., Agostinelli, S., Albertazzi, D., Angelini, G., Angerosa, F., Arigliano, P. L., Assalve, D., Ayala, F., Bellonifortina, A., Berta, M., Biale, C., Biasini, I., Boccaletti, V., Bonamonte, D., Borghi, A., Brambilla, L., Bressan, M., Bruno, A., Caccavale, S., Calogiuri, G., Cannavò, S. P., Carugno, A., Cataldi, I., Chiarelli, G., Chiesa, A., Cirla, A. M., Cossutta, M., Cova, L. M., Cristaudo, A., Dalcan-Ton, M., Damiani, G., Danese, P., Desalvo, V., Fantini, C., Ferrucci, S. M., Flori, M. L., Fontana, E., Foti, C., Francalanci, S., Frasin, L. A., Gola, M., Gravante, M., Guastaferro, D., Ingordo, V., Lauriola, M. M., Leghissa, P., Lisi, P., Lombardi, P., Lorenzini, M., Magrini, L., Marone, G., Martina, E., Mascagni, P., Matteinichiari, M., Meligeni, L., Melino, M., Milanesi, N., Molinu, A. A., Monfrecola, G., Morelli, P., Motolese, A., Musumeci, M. L., Napolitano, M., Nasca, M. R., Paganini, P., Papini, M., Pasolini, G., Peroni, A., Peserico, A., Piras, V., Pugliese, A., Raponi, F., Raviolo, P. D., Rebora, A., Recchia, G. P., Riva, F., Rossi, M., Ruggieri, M., Saggiorato, F., Sartorelli, P., Schena, D., Schettino, A., Spano, G., Stinchi, C., Taddei, L., Tasin, L., Tramontana, M., Valsecchi, R. H., Vascellaro, A., Venturini, M., Stingeni, L, Bianchi, L, Hansel, K, Corazza, M, Gallo, R, Guarneri, F, Patruno, C, Rigano, L, Romita, P, Pigattoatt, P, Calzavara-Pintoton, P, Agostinelli, S, Albertazzi, D, Angelini, G, Angerosa, F, Arigliano, P, Assalve, D, Ayala, F, Bellonifortina, A, Berta, M, Biale, C, Biasini, I, Boccaletti, V, Bonamonte, D, Borghi, A, Brambilla, L, Bressan, M, Bruno, A, Caccavale, S, Calogiuri, G, Cannavò, S, Carugno, A, Cataldi, I, Chiarelli, G, Chiesa, A, Cirla, A, Cossutta, M, Cova, L, Cristaudo, A, Dalcan-Ton, M, Damiani, G, Danese, P, Desalvo, V, Fantini, C, Ferrucci, S, Flori, M, Fontana, E, Foti, C, Francalanci, S, Frasin, L, Gola, M, Gravante, M, Guastaferro, D, Ingordo, V, Lauriola, M, Leghissa, P, Lisi, P, Lombardi, P, Lorenzini, M, Magrini, L, Marone, G, Martina, E, Mascagni, P, Matteinichiari, M, Meligeni, L, Melino, M, Milanesi, N, Molinu, A, Monfrecola, G, Morelli, P, Motolese, A, Musumeci, M, Napolitano, M, Nasca, M, Paganini, P, Papini, M, Pasolini, G, Peroni, A, Peserico, A, Piras, V, Pugliese, A, Raponi, F, Raviolo, P, Rebora, A, Recchia, G, Riva, F, Rossi, M, Ruggieri, M, Saggiorato, F, Sartorelli, P, Schena, D, Schettino, A, Spano, G, Stinchi, C, Taddei, L, Tasin, L, Tramontana, M, Valsecchi, R, Vascellaro, A, Venturini, M, Stingeni, L., Bianchi, L., Hansel, K., Corazza, M., Gallo, R., Guarneri, F., Patruno, C., Rigano, L., Romita, P., Pigattoatt, P. D., Calzavara-Pintoton, P., Agostinelli, S., Albertazzi, D., Angelini, G., Angerosa, F., Arigliano, P. L., Assalve, D., Ayala, F., Bellonifortina, A., Berta, M., Biale, C., Biasini, I., Boccaletti, V., Bonamonte, D., Borghi, A., Brambilla, L., Bressan, M., Bruno, A., Caccavale, S., Calogiuri, G., Cannavò, S. P., Carugno, A., Cataldi, I., Chiarelli, G., Chiesa, A., Cirla, A. M., Cossutta, M., Cova, L. M., Cristaudo, A., Dalcan-Ton, M., Damiani, G., Danese, P., Desalvo, V., Fantini, C., Ferrucci, S. M., Flori, M. L., Fontana, E., Foti, C., Francalanci, S., Frasin, L. A., Gola, M., Gravante, M., Guastaferro, D., Ingordo, V., Lauriola, M. M., Leghissa, P., Lisi, P., Lombardi, P., Lorenzini, M., Magrini, L., Marone, G., Martina, E., Mascagni, P., Matteinichiari, M., Meligeni, L., Melino, M., Milanesi, N., Molinu, A. A., Monfrecola, G., Morelli, P., Motolese, A., Musumeci, M. L., Napolitano, M., Nasca, M. R., Paganini, P., Papini, M., Pasolini, G., Peroni, A., Peserico, A., Piras, V., Pugliese, A., Raponi, F., Raviolo, P. D., Rebora, A., Recchia, G. P., Riva, F., Rossi, M., Ruggieri, M., Saggiorato, F., Sartorelli, P., Schena, D., Schettino, A., Spano, G., Stinchi, C., Taddei, L., Tasin, L., Tramontana, M., Valsecchi, R. H., Vascellaro, A., and Venturini, M.

Abstract

Patch testing is the standard procedure used to diagnose allergic contact dermatitis. It is an in-vivo test, which reproduces the reaction to a contact allergen. This in-vivo test aims to reproduce the elicitation phase of allergic contact dermatitis and is performed applying allergens under occlusion on the skin under standardized conditions. These guidelines for the best practice in performing patch test have been developed by an Italian group of experts taking in account the Italian legislation and local pharmacological governance. Guidelines are adapted from the original article under the guidance of the European Society of Contact Dermatitis (ESCD) and on the basis of the SIDAPA guidelines.

Published
2019

3. Italian guidelines for therapy of atopic dermatitis-Adapted from consensus-based European guidelines for treatment of atopic eczema (atopic dermatitis)

Author

Damiani, G, Calzavara-Pinton, P, Stingeni, L, Hansel, K, Cusano, F, 'Skin Allergy' Group of SIDeMaST, 'ADOI' (Associazione Dermatologi Ospedalieri Italiani), 'SIDAPA' (Società Italiana di Dermatologia Allergologica Professionale, e Ambientale), Agostinelli, D., Albertazzi, D., Angelini, G, Angerosa, F, Arigliano, Pl, Assalve, D, Ayala, F, Barbagallo, T, Belloni-Fortina, A, Berta, M, Biale, C, Bianchi, L, Biasini, I, Boccaletti, V, Bonamonte, D, Borghi, A, Bragazzi, Nl, Brambilla, L, Bressan, M, Brunasso, Amg, Bruni, F, Bruni, P, Caccavale, S, Calogiuri, G, Cannavò, Sp, Carugno, A, Cataldi, I, Chiarelli, G, Cirla, Am, Corazza, M, Cossutta, M, Cova, L, Cristaudo, A, Danese, P, Dal Canton, M, De Pità, O, De Salvo, P, Donini, M, Fantini, F, Ferrucci, Sm, Flori, Ml, Fontana, E, Foti, C, Francalci, S, Frasin, La, Gallo, R, Gasparini, G, Gola, M, Gravante, M, Guarnieri, F, Guastaferro, D, Ingordo, V, Lauriola, Mm, Leghissa, P, Lisi, P, Lombardi, P, Lorenzini, M, Malara, G, Magrini, L, Marone, G, Martina, E, Mascagni, P, Matteini Chiari, M, Meligeni, L, Melino, M, Miccio, L, Milanesi, N, Molinu, A, Monfrecola, G, Morelli, P, Motolese, A, Musumeci, Ml, Naldi, L, Napolitano, M, Nasca, Mr, Pacifico, A, Paganini, P, Papini, M, Pasolini, G, Patruno, C, Pellegrino, M, Peroni, A, Peserico, A, Piras, V, Pugliese, A, Raponi, F, Raviolo, Pd, Rebora, A, Recchia, Gp, Riva, F, Romita, P, Rossi, M, Ruggieri, M, Saggiorato, F, Sartorelli, P, Schena, D, Schettino, A, Spanò, G, Stinchi, C, Tasin, L, Tramontana, M, Taddei, L, Valsecchi, Re, Russo, F, Vascellaro, A, Venturini, M, Vincenzi, C, Virgili, A, Pigatto PDM, Zucca M)., Damiani, G, Calzavara-Pinton, P, Stingeni, L, Hansel, K, Cusano, F, Pigatto, P, Agostinelli, D, Albertazzi, D, Angelini, G, Angerosa, F, Arigliano, P, Assalve, D, Ayala, F, Barbagallo, T, Belloni-Fortina, A, Berta, M, Biale, C, Bianchi, L, Biasini, I, Boccaletti, V, Bonamonte, D, Borghi, A, Bragazzi, N, Brambilla, L, Bressan, M, Brunasso, A, Bruni, F, Bruni, P, Caccavalle, S, Calogiuri, G, Cannavo, S, Carugno, A, Cataldi, I, Chiarelli, G, Cirla, A, Corazza, M, Cossutta, M, Cova, L, Cristaudo, A, Danese, P, Dal Canton, M, Depita, O, De Salvo, P, Donini, M, Fantini, F, Ferrucci, S, Flori, M, Fontana, E, Foti, C, Francalci, S, Frasin, L, Gallo, R, Gasparini, G, Gola, M, Gravante, M, Guarnieri, F, Guastaferro, D, Ingordo, V, Lauriola, M, Leghissa, P, Lisi, P, Lombardi, P, Lorenzini, M, Malara, G, Magrini, L, Marone, G, Martina, E, Mascagni, P, Chiari, M, Meligeni, L, Melino, M, Miccio, L, Milanesi, N, Molinu, A, Monfrecola, G, Morelli, P, Motolese, A, Musumeci, M, Naldi, L, Napolitano, M, Nasca, M, Pacifico, A, Paganini, P, Papini, M, Pasolini, G, Patruno, C, Pellegrino, M, Peroni, A, Peserico, A, Piras, V, Pugliese, A, Raponi, F, Raviolo, P, Rebora, A, Recchia, G, Riva, F, Romita, P, Rossi, M, Ruggieri, M, Saggiorato, F, Sartorelli, P, Schena, D, Schettino, A, Spano, G, Stinchi, C, Tasin, L, Tramontana, M, Taddei, L, Valsecchi, R, Russo, F, Vascellaro, A, Venturini, M, Vincenzi, C, Virgili, A, Zucca, M, G., Damiani, P., Calzavara-Pinton, L., Stingeni, K., Hansel, F., Cusano, L Arigliano, P, L Bragazzi, N, G Brunasso, A M, Caccavale, S, P Cannavò, S, M Cirla, A, De Pità, O, M Ferrucci, S, L Flori, M, A Frasin, L, M Lauriola, M, Matteini Chiari, M, L Musumeci, M, R Nasca, M, D Raviolo, P, P Recchia, G, Spanò, G, E Valsecchi, R, and P. D. M., Pigatto

Subjects
dermatological agents, Cultural context, atopic eczema, Dermatitis, azatioprin, 030207 dermatology & venereal diseases, 0302 clinical medicine, cclosporin, topical, atopic dermatitis, cyclosporin, dupilumab, methotrexate, phototherapy, topicals, Adult, Biological Products, Child, Dermatitis, Atopic, Dermatologic Agents, Dermatology, Humans, Italy, Practice Guidelines as Topic, General Medicine, Atopic dermatitis, Dupilumab, 030220 oncology & carcinogenesis, Revolutionary change, Biological Product, Human, atopic dermatiti, medicine.medical_specialty, atopic dermatitis, atopic eczema, azatioprin, cclosporin, dupilumab, methotrexate, phototherapy, topicals, adult, biological products, child, dermatological agents, Dermatologic Agent, Socio-culturale, Context (language use), Atopic, 03 medical and health sciences, Therapeutic approach, Settore MED/35, Eczema atopic dermatitis, medicine, business.industry, medicine.disease, Family medicine, Good clinical practice, business
Abstract

Atopic dermatitis (AD) therapeutic approach calls for a long-term treatment. Treatment options for AD have recently undergone a revolutionary change by the introduction of the first biologic drug. Availability in daily practice of the last version of international AD guidelines, taking peculiarities of the country into account, can contribute to good clinical practice in Italy. To adapt European Dermatology Forum (EDF) guidelines for AD to the Italian medical–legal context, the EDF guidelines were assessed independently by two independent Italian renowned experts in the field and further integrated with articles published and systematically reviewed before May 2019. The first draft was collegially corrected and updated by the members of the SIDEMAST, ADOI, and SIDAPA. Recommendation levels (A; B; C; D) were graded based on the evidence levels (1–4). The adapted guidelines presented here focus on topical and systemic therapies in AD patients, both children and adults. As opposed to previous Italian guidelines, they include indications about biologics. New relevant evidence available from very recent literature and peculiarities of the Italian medical and legal context have been integrated in the revision process. If compared to general guidelines for AD not adapted to a specific national and cultural context, a revision for specific Italian needs is now available: It comprises the option of implementing the new biologic treatments and is likely to provide an important contribution to the improvement of clinical practice in Italy. Cooperation between patients, dermatologists, allergologists, and pediatricians remains mandatory in AD management. The authors of the present revision recommend an update of the Italian guidelines to be performed at least every second year.

Published
2019

4. Italian Guidelines in Patch Testing - adapted from the European Society of Contact Dermatitis (ESCD)

Author

Stingeni, Luca, Bianchi, Leonardo, Hansel, Katharina, Corazza, Monica, Gallo, Rosella, Guarneri, Fabrizio, Patruno, Cataldo, Rigano, Luigi, Romita, Paolo, Pigatto, Paolo D, Calzavara-Pinton, Piergiacomo, Agostinelli, D, Albertazzi, D, Angelini, G, Angerosa, F, Arigliano, Pl, Assalve, D, Ayala, F, Belloni, Fortina, A, Berta, M, Biale, C, Biasini, I, Boccaletti, V, Bonamonte, D, Borghi, A, Brambilla, L, Bressan, M, Bruno, A, Caccavale, S, Calogiuri, G, Cannavò, Sp, Carugno, A, Cataldi, I, Chiarelli, G, Chiesa, A, Cirla, Am, Cossutta, M, Cova, Lm, Cristaudo, A, Dal Canton, M, Damiani, G, Danese, P, De Salvo, V, Fantini, C, Ferrucci, Sm, Flori, Ml, Fontana, E, Foti, C, Francalanci, S, Frasin, La, Gola, M, Gravante, M, Guastaferro, D, Ingordo, V, Lauriola, Mm, Leghissa, P, Lisi, P, Lombardi, P, Lorenzini, M, Magrini, L, Marone, G, Martina, E, Mascagni, P, Matteini, Chiari, M, Meligeni, L, Melino, M, Milanesi, N, Molinu, Aa, Monfrecola, G, Morelli, P, Motolese, A, Musumeci, Ml, Napolitano, M, Nasca, Mr, Paganini, P, Papini, M, Pasolini, G, Peroni, A, Peserico, A, Piras, V, Pugliese, A, Raponi, F, Raviolo, Pd, Rebora, A, Recchia, Gp, Riva, F, Rossi, M, Ruggieri, M, Saggiorato, F, Sartorelli, P, Schena, D, Schettino, A, Spano, G, Stinchi, C, Taddei, L, Tasin, L, Tramontana, M, Valsecchi, Rh, Vascellaro, A, Venturini, M, Vincenzi, C, Virgili, A, Zucca, M, Stingeni, L, Bianchi, L, Hansel, K, Corazza, M, Gallo, R, Guarneri, F, Patruno, C, Rigano, L, Romita, P, Pigattoatt, P, Calzavara-Pintoton, P, Agostinelli, S, Albertazzi, D, Angelini, G, Angerosa, F, Arigliano, P, Assalve, D, Ayala, F, Bellonifortina, A, Berta, M, Biale, C, Biasini, I, Boccaletti, V, Bonamonte, D, Borghi, A, Brambilla, L, Bressan, M, Bruno, A, Caccavale, S, Calogiuri, G, Cannavò, S, Carugno, A, Cataldi, I, Chiarelli, G, Chiesa, A, Cirla, A, Cossutta, M, Cova, L, Cristaudo, A, Dalcan-Ton, M, Damiani, G, Danese, P, Desalvo, V, Fantini, C, Ferrucci, S, Flori, M, Fontana, E, Foti, C, Francalanci, S, Frasin, L, Gola, M, Gravante, M, Guastaferro, D, Ingordo, V, Lauriola, M, Leghissa, P, Lisi, P, Lombardi, P, Lorenzini, M, Magrini, L, Marone, G, Martina, E, Mascagni, P, Matteinichiari, M, Meligeni, L, Melino, M, Milanesi, N, Molinu, A, Monfrecola, G, Morelli, P, Motolese, A, Musumeci, M, Napolitano, M, Nasca, M, Paganini, P, Papini, M, Pasolini, G, Peroni, A, Peserico, A, Piras, V, Pugliese, A, Raponi, F, Raviolo, P, Rebora, A, Recchia, G, Riva, F, Rossi, M, Ruggieri, M, Saggiorato, F, Sartorelli, P, Schena, D, Schettino, A, Spano, G, Stinchi, C, Taddei, L, Tasin, L, Tramontana, M, Valsecchi, R, Vascellaro, A, Venturini, M, Pigatto, Pd, Calzavara-Pinton, P, 'Skin Allergy' group of SIDeMaST and 'SIDAPA' (Agostinelli, D, Arigliano, Pl, Belloni Fortina, A, Cannavò, Sp, Cirla, Am, Cova, Lm, Dal Canton, M, De Salvo, V, Ferrucci, Sm, Flori, Ml, Frasin, La, Lauriola, Mm, Matteini Chiari, M, Molinu, Aa, Musumeci, Ml, Nasca, Mr, Raviolo, Pd, Recchia, Gp, Valsecchi, Rh, Vincenzi, C, Virgili, A, and Zucca, M).

Subjects
Dermatitis, contact, Guideline, Patch tests, medicine.medical_specialty, Allergic Contact, Socio-culturale, Dermatitis, Dermatology, Patch tests, Guideline, contact, Patch test, Patch testing, Standard procedure, 030207 dermatology & venereal diseases, 03 medical and health sciences, 0302 clinical medicine, Dermatitis, contact, Allergens, Dermatitis, Allergic Contact, Humans, Italy, Patch Tests, medicine, Allergic contact dermatitis, business.industry, Contact dermatitis, medicine.disease, Test (assessment), Family medicine, business
Abstract

Patch testing is the standard procedure used to diagnose allergic contact dermatitis. It is an in-vivo test, which reproduces the reaction to a contact allergen. This in-vivo test aims to reproduce the elicitation phase of allergic contact dermatitis and is performed applying allergens under occlusion on the skin under standardized conditions. These guidelines for the best practice in performing patch test have been developed by an Italian group of experts taking in account the Italian legislation and local pharmacological governance. Guidelines are adapted from the original article under the guidance of the European Society of Contact Dermatitis (ESCD) and on the basis of the SIDAPA guidelines.

Published
2019

6. Gender health and policies: the state of the art from exposure to solutions

Author

Siliquini, Roberta, Piat, SC, Versino, Elisabetta, Gianino, Maria Michela, Mutu, D, Cossutta, M, Manzoli, Lamberto, Siliquini, Roberta, Piat, SC, Versino, Elisabetta, Gianino, Maria Michela, Mutu, D, Cossutta, M, and Manzoli, Lamberto

Abstract

Objective. To synthesize the determinants of gender inequalities through a narrative review that: (i) describes gender related var- iables that can create different levels of health; (ii) describes key points that may assist in policy development and its reorientation towards gender differences; (iii) debates potential approaches in understanding gender issues. Methods. Review of the international literature through online databases (Pubmed), search engines, publications and documents from ?grey literature?. Inclusion criteria: publications from 1997, English language; keywords used: gender based analysis; gender and public policy; women?s health; gender differences; health policy; gender impact assessment. Among the 300 papers retrieved, 55 were selected for relevance. Results. We performed a narrative synthesis of the included literature, regarding: (i) gender differences and their determi-nants; (ii) elements for the changing; (iii) possible approaches; (iv) gender influences the pursuit of health and health care access through specific variables; (v) health policies can modify these variables only by a minimal percentage. These interventions should guarantee equity and allow efficient resources allocation. The gap between political announce- ments and real policy implementation remains unchanged. (vi) Standard approaches to the topic are not feasible due to the scarcity of a specific literature and the numerous cultural differences. Conclusions. Gender analysis of policies suggests they can dif- ferently affect women in comparison to men. However, reforms, strategies and interventions introduced in the last two decades, have achieved a limited success towards better gender equality in health. The main aim is to attack the structural sources of gender inequity in the society.

Published
2009

7. Gender health and policies: The state of the art from exposure to solutions

Author

Siliquini, R., Chiadò Piat, S., Versino, E., Maria Michela Gianino, Mutu, D., Cossutta, M., and Manzoli, L.

Subjects
Male, Health Policy, Health Status, Gender, Equity, Health Promotion, Health Status Disparities, Policies, Sex Factors, Italy, Humans, Women's Health, Female, Healthcare Disparities, Men's Health, Prejudice
Abstract

Objective. To synthesize the determinants of gender inequalities through a narrative review that: (i) describes gender related var- iables that can create different levels of health; (ii) describes key points that may assist in policy development and its reorientation towards gender differences; (iii) debates potential approaches in understanding gender issues. Methods. Review of the international literature through online databases (Pubmed), search engines, publications and documents from ?grey literature?. Inclusion criteria: publications from 1997, English language; keywords used: gender based analysis; gender and public policy; women?s health; gender differences; health policy; gender impact assessment. Among the 300 papers retrieved, 55 were selected for relevance. Results. We performed a narrative synthesis of the included literature, regarding: (i) gender differences and their determi-nants; (ii) elements for the changing; (iii) possible approaches; (iv) gender influences the pursuit of health and health care access through specific variables; (v) health policies can modify these variables only by a minimal percentage. These interventions should guarantee equity and allow efficient resources allocation. The gap between political announce- ments and real policy implementation remains unchanged. (vi) Standard approaches to the topic are not feasible due to the scarcity of a specific literature and the numerous cultural differences. Conclusions. Gender analysis of policies suggests they can dif- ferently affect women in comparison to men. However, reforms, strategies and interventions introduced in the last two decades, have achieved a limited success towards better gender equality in health. The main aim is to attack the structural sources of gender inequity in the society., Journal of Preventive Medicine and Hygiene, Vol 50, No 1 (2009)

9. The blood count as a compass to navigate in the ever-changing landscape of the carrier state of hemoglobinopathies: a single-center Italian experience.

Author

Marchesani S, Di Mauro M, Ceglie G, Grassia G, Carletti M, Cristofaro RC, Cossutta M, Curcio C, and Palumbo G

Abstract

Introduction: Approximately 7% of the worldwide population exhibits variations in the globin genes. The recent migration of populations from countries where hemoglobin disorders are endemic has resulted in important epidemiological changes with the diffusion of newly discovered or poorly characterized genetic variants and new combinations and very heterogeneous clinical phenotypes. The aim of our study is to assess the parameters that are more significant in predicting a positive genetic testing outcome for hemoglobinopathies in a pediatric population of patients presenting with anemia or microcythemia, without a definite diagnosis., Methods and Materials: This study included patients evaluated in our hematological outpatient clinic for anemia and/or microcythemia despite normal ferritin levels. A screening of pathological hemoglobins using high-performance liquid chromatography (HPLC) was performed for the entire population of the study. Subsequently, patients with hemoglobin (Hb) S trait and patients with an HPLC profile compatible with beta thalassemia trait were excluded from the study. Genetic screening tests for hemoglobinopathies were performed on the remaining patients, which involved measuring the red blood cell (RBC) counts, red blood cells distribution width (RDW), reticulocyte count, and mean corpuscular volume of reticulocytes (MCVr)., Results: This study evaluated a total of 65 patients, consisting of nine patients with negative genetic analysis results and 56 patients with positive genetic analysis results. The Hb and RDW values in these two groups did not demonstrate statistical significance. On the other hand, there were statistically significant differences observed in the mean corpuscular volume (MCV), RBC count, reticulocyte count, and MCVr between the two groups. Furthermore, in the group of patients with positive genetic test results, specific genetic findings associated with different HPLC results were observed. In particular, 13 patients with positive genetic test results had normal HPLC findings., Discussion: This study has demonstrated that HPLC, while serving as a valuable first-level test, has some limitations. Specifically, it has been observed that some patients may exhibit a negative HPLC result despite a positive genetic analysis. In addition to the presence of low levels of Hb and HPLC alterations, other parameters could potentially indicate the underlying mutations in the globin genes. Therefore, we propose that the complete blood cell count be utilized as a widely available parameter for conducting targeted genetic analyses to avoid the risk of overlooking rare hemoglobinopathies., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (© 2023 Marchesani, Di Mauro, Ceglie, Grassia, Carletti, Cristofaro, Cossutta, Curcio and Palumbo.)

Published
2023
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11. Inflammatory status in pediatric sickle cell disease: Unravelling the role of immune cell subsets.

Author

Marchesani S, Bertaina V, Marini O, Cossutta M, Di Mauro M, Rotulo GA, Palma P, Sabatini L, Petrone MI, Frati G, Monteleone G, Palumbo G, and Ceglie G

Abstract

Introduction: The mutation of the beta-globin gene that causes sickle cell disease (SCD) results in pleiotropic effects, such as hemolysis and vaso-occlusive crisis that can induce inflammatory mechanisms with deleterious consequences on the organism. Moreover, SCD patients display an increased susceptibility to infections. Few studies are currently available that evaluate a wide immunological profile in a pediatric population. This study proposes an evaluation of the immune profile in subjects with SCD in a pediatric population through a detailed analysis by flow cytometry. Methods and Materials: Peripheral blood samples from 53 pediatric patients with SCD (mean age 9.8 years, interquartile range 9 years) were obtained and then analyzed by flow cytometry, in order to evaluate changes in the immune populations compared to 40 healthy donors (mean age 7.3 years, interquartile range 9.5 years). Results: Our data showed an increase in neutrophils (with a reduction in the CD62L + subpopulation) and monocytes (with a decrease in HLA-DRlow monocytes) with normal values of lymphocytes in SCD patients. In the lymphocyte subpopulations analysis we observed lower values of CD4 + T cells (with higher number of memory and central memory T lymphocytes) with increased frequency of CD8 + T cells (with a predominant naive pattern). Moreover, we observed higher values of CD39 + Tregs and lower HLA-DR+ and CD39 - T cells with an increased Th17, Th1-17 and Th2 response. Conclusion: We observed immunological alterations typical of an inflammatory status (increase in activated neutrophils and monocytes) associated with a peculiar Treg pattern (probably linked to a body attempt to minimize inflammation intrinsic to SCD). Furthermore, we highlighted a T helper pathway associated with inflammation in line with other studies. Our data showed that immunological markers may have an important role in the understanding the pathophysiology of SCD and in optimizing targeted therapeutic strategies for each patient., Competing Interests: The authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2023 Marchesani, Bertaina, Marini, Cossutta, Di Mauro, Rotulo, Palma, Sabatini, Petrone, Frati, Monteleone, Palumbo and Ceglie.)

Published
2023
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12. Immunological profile in a pediatric population of patients with spherocytosis. A single-center experience.

Author

Marchesani S, Sabatini L, Bertaina V, Marini O, Ambrosi M, Di Mauro M, Cossutta M, Schettini L, Lodi M, Rotulo GA, Palma P, Palumbo G, and Ceglie G

Subjects
Child, Humans, Splenectomy, Spleen, Erythrocyte Count, Erythrocytes, Spherocytosis, Hereditary surgery
Abstract

Spherocytosis is a hereditary disease caused by the deficiencies of different membrane proteins of red blood cells. Currently, splenectomy is the main therapeutic strategy available, although it is accompanied by an increased risk of sepsis. Several evidences have supported the hypothesis of spleen dysfunction in patients with spherocytosis that haven't yet undergone splenectomy. The aim of this study is to furtherly characterize this aspect, by describing the immune subpopulations in peripheral blood samples obtained from 41 pediatric patients with hereditary spherocytosis by flow cytometry, in order to evaluate changes in the composition of the immune populations compared to 16 healthy donors. Patients were divided in two groups: splenectomized and non-splenectomized. In the splenectomized population, data showed neutrophilic leukocytosis, thrombocytosis, increase in NK and reduction in CD4+ lymphocytes. However, we observed that most of the results obtained in the splenectomized group were found in the non-splenectomized patients as well (increase in neutrophils, in NK, reduction of CD19+, CD4+ lymphocytes and CD4+ and CD8+ naïve cells). The alterations of the immune system may be mainly due to the disease itself, regardless of splenectomy. Therefore, immunological criteria could be included in clinical phenotype assessment in order to better optimize the timing for splenectomy., Competing Interests: Declaration of competing interest None., (Copyright © 2022. Published by Elsevier Inc.)

Published
2023
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14. Nucleolin Therapeutic Targeting Decreases Pancreatic Cancer Immunosuppression.

Author

Ponzo M, Debesset A, Cossutta M, Chalabi-Dchar M, Houppe C, Pilon C, Nicolas-Boluda A, Meunier S, Raineri F, Thiolat A, Nicolle R, Maione F, Brundu S, Cojocaru CF, Bouvet P, Bousquet C, Gazeau F, Tournigand C, Courty J, Giraudo E, Cohen JL, and Cascone I

Abstract

Background: The pancreatic ductal adenocarcinoma (PDAC) microenvironment is highly fibrotic and hypoxic, with poor immune cell infiltration. Recently, we showed that nucleolin (NCL) inhibition normalizes tumour vessels and impairs PDAC growth. Methods: Immunocompetent mouse models of PDAC were treated by the pseudopeptide N6L, which selectively inhibits NCL. Tumour-infiltrating immune cells and changes in the tumour microenvironment were analysed. Results: N6L reduced the proportion of regulatory T cells (Tregs) and myeloid-derived suppressor cells (MDSCs) and increased tumour-infiltrated T lymphocytes (TILs) with an activated phenotype. Low-dose anti-VEGFR2 treatment normalized PDAC vessels but did not modulate the immune suppressive microenvironment. RNAseq analysis of N6L-treated PDAC tumours revealed a reduction of cancer-associated fibroblast (CAF) expansion in vivo and in vitro. Notably, N6L treatment decreased IL-6 levels both in tumour tissues and in serum. Treating mPDAC by an antibody blocking IL-6 reduced the proportion of Tregs and MDSCs and increased the amount of TILs, thus mimicking the effects of N6L. Conclusions: These results demonstrate that NCL inhibition blocks the amplification of lymphoid and myeloid immunosuppressive cells and promotes T cell activation in PDAC through a new mechanism of action dependent on the direct inhibition of the tumoral stroma.

Published
2022
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15. Polymerization-Induced Self-Assembly (PISA) for in situ drug encapsulation or drug conjugation in cancer application.

Author

Phan H, Cossutta M, Houppe C, Le Cœur C, Prevost S, Cascone I, Courty J, Penelle J, and Couturaud B

Subjects
Doxorubicin metabolism, Doxorubicin pharmacology, Drug Carriers, Humans, Methacrylates, Micelles, Polymerization, Polymers, Nanoparticles, Neoplasms
Abstract

Hypothesis: We describe the possibility of using the same block copolymer carriers prepared by PISA for in situ drug encapsulation or drug conjugation., Experiments: Block copolymers containing poly((ethylene glycol) methacrylate)-co-poly(pentafluorophenyl methacrylate)-b-poly(hydroxypropyl methacrylate) (P((PEGMA-co-PFBMA)-b-PHPMA)) were synthesized at 10 wt% using PISA. The first approach involved in situ Doxorubicin (DOX) loading during PISA, while the second exhibited surface functionalization of PISA-made vesicles with dual drug therapies, N-acetyl cysteine (NAC) and DOX using para-fluoro-thiol reaction (PFTR) and carbodiimide chemistry, respectively. Cytotoxicity, cell uptake, and cell apoptosis were assessed on MDA-MB-231 cell lines., Findings: P((PEGMA-co-PFBMA)-b-PHPMA) nanocarriers were prepared, showing size and shape transformations from spheres, cylinders to raspberry-forming vesicles. DOX was readily loaded into NPs during PISA with relatively high encapsulation efficiency of 70 %, whereas the plain PISA-made vesicles could be functionalized with NAC and DOX at high yields. DOX-free NPs showed biocompatibility, whilst DOX-conjugated NPs imparted a concentration-dependent cytotoxicity, as well as an enhanced cell uptake compared to free DOX. The results demonstrated that the same PISA-derived self-assemblies enabled either in situ drug encapsulation, or post-polymerization surface engineering with useful functionalities upon tuning the macro-CTA block, thus holding promises for future drug delivery and biomedical applications., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2022 Elsevier Inc. All rights reserved.)

Published
2022
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17. The Extracellular Matrix in Pancreatic Cancer: Description of a Complex Network and Promising Therapeutic Options.

Author

Ferrara B, Pignatelli C, Cossutta M, Citro A, Courty J, and Piemonti L

Abstract

The stroma is a relevant player in driving and supporting the progression of pancreatic ductal adenocarcinoma (PDAC), and a large body of evidence highlights its role in hindering the efficacy of current therapies. In fact, the dense extracellular matrix (ECM) characterizing this tumor acts as a natural physical barrier, impairing drug penetration. Consequently, all of the approaches combining stroma-targeting and anticancer therapy constitute an appealing option for improving drug penetration. Several strategies have been adopted in order to target the PDAC stroma, such as the depletion of ECM components and the targeting of cancer-associated fibroblasts (CAFs), which are responsible for the increased matrix deposition in cancer. Additionally, the leaky and collapsing blood vessels characterizing the tumor might be normalized, thus restoring blood perfusion and allowing drug penetration. Even though many stroma-targeting strategies have reported disappointing results in clinical trials, the ECM offers a wide range of potential therapeutic targets that are now being investigated. The dense ECM might be bypassed by implementing nanoparticle-based systems or by using mesenchymal stem cells as drug carriers. The present review aims to provide an overview of the principal mechanisms involved in the ECM remodeling and of new promising therapeutic strategies for PDAC.

Published
2021
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18. Nucleolin Targeting by N6L Inhibits Wnt/β-Catenin Pathway Activation in Pancreatic Ductal Adenocarcinoma.

Author

Raineri F, Bourgoin-Voillard S, Cossutta M, Habert D, Ponzo M, Houppe C, Vallée B, Boniotto M, Chalabi-Dchar M, Bouvet P, Couvelard A, Cros J, Debesset A, Cohen JL, Courty J, and Cascone I

Abstract

Pancreatic ductal adenocarcinoma (PDAC) is a highly aggressive and resistant cancer with no available effective therapy. We have previously demonstrated that nucleolin targeting by N6L impairs tumor growth and normalizes tumor vessels in PDAC mouse models. Here, we investigated new pathways that are regulated by nucleolin in PDAC. We found that N6L and nucleolin interact with β-catenin. We found that the Wnt/β-catenin pathway is activated in PDAC and is necessary for tumor-derived 3D growth. N6L and nucleolin loss of function induced by siRNA inhibited Wnt pathway activation by preventing β-catenin stabilization in PDAC cells. N6L also inhibited the growth and the activation of the Wnt/β-catenin pathway in vivo in mice and in 3D cultures derived from MIA PaCa2 tumors. On the other hand, nucleolin overexpression increased β-catenin stabilization. In conclusion, in this study, we identified β-catenin as a new nucleolin interactor and suggest that the Wnt/β-catenin pathway could be a new target of the nucleolin antagonist N6L in PDAC.

Published
2021
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19. Antagonist of nucleolin, N6L, inhibits neovascularization in mouse models of retinopathies.

Author

Darche M, Cossutta M, Caruana L, Houppe C, Gilles ME, Habert D, Guilloneau X, Vignaud L, Paques M, Courty J, and Cascone I

Subjects
Animals, Cell Proliferation, Choroidal Neovascularization etiology, Choroidal Neovascularization metabolism, Choroidal Neovascularization pathology, Disease Models, Animal, Intravitreal Injections, Mice, Mice, Inbred C57BL, Oxygen adverse effects, Phosphorylation, Retinal Diseases etiology, Retinal Diseases metabolism, Retinal Diseases pathology, Nucleolin, Angiogenesis Inhibitors pharmacology, Choroidal Neovascularization prevention & control, Peptides pharmacology, Phosphoproteins antagonists & inhibitors, RNA-Binding Proteins antagonists & inhibitors, Retinal Diseases prevention & control
Abstract

Retinal vascular diseases (RVD) have been identified as a major cause of blindness worldwide. These pathologies, including the wet form of age-related macular degeneration, retinopathy of prematurity, and diabetic retinopathy are currently treated by intravitreal delivery of anti-vascular endothelial growth factor (VEGF) agents. However, repeated intravitreal injections can lead to ocular complications and resistance to these treatments. Thus, there is a need to find new targeted therapies. Nucleolin regulates the endothelial cell (EC) activation and angiogenesis. In previous studies, we designed a pseudopeptide, N6L, that binds the nucleolin and blocks the tumor angiogenesis. In this study, the effect of N6L was investigated in two experimental models of retinopathies including oxygen-induced retinopathy (OIR) and choroidal neovascularization (CNV). We found that in mouse OIR, intraperitoneal injection of N6L is delivered to activated ECs and induced a 50% reduction of pathological neovascularization. The anti-angiogenic effect of N6L has been tested in CNV model in which the systemic injection of N6L induced a 33% reduction of angiogenesis. This effect is comparable to those obtained with VEGF-trap, a standard of care drug for RVD. Interestingly, with preventive and curative treatments, neoangiogenesis is inhibited by 59%. Our results have potential interest in the development of new therapies targeting other molecules than VEGF for RVD., (© 2020 Federation of American Societies for Experimental Biology.)

Published
2020
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20. Weibel-Palade Bodies Orchestrate Pericytes During Angiogenesis.

Author

Cossutta M, Darche M, Carpentier G, Houppe C, Ponzo M, Raineri F, Vallée B, Gilles ME, Villain D, Picard E, Casari C, Denis C, Paques M, Courty J, and Cascone I

Subjects
Angiopoietin-2 physiology, Animals, Cells, Cultured, Endothelial Cells physiology, Exocytosis, Humans, Mice, Mice, Inbred C57BL, Neoplasms blood supply, Retina physiology, Vascular Endothelial Growth Factor A antagonists & inhibitors, Vascular Endothelial Growth Factor A physiology, Neovascularization, Pathologic physiopathology, Neovascularization, Physiologic physiology, Pericytes physiology, Weibel-Palade Bodies physiology
Abstract

Objective Weibel-Palade bodies (WPBs) are endothelial cell (EC)-specific organelles formed by vWF (von Willebrand factor) polymerization and that contain the proangiogenic factor Ang-2 (angiopoietin-2). WPB exocytosis has been shown to be implicated for vascular repair and inflammatory responses. Here, we investigate the role of WPBs during angiogenesis and vessel stabilization. Approach and Results WPB density in ECs decreased at the angiogenic front of retinal vascular network during development and neovascularization compared with stable vessels. In vitro, VEGF (vascular endothelial growth factor) induced a VEGFR-2 (vascular endothelial growth factor receptor-2)-dependent exocytosis of WPBs that contain Ang-2 and consequently the secretion of vWF and Ang-2. Blocking VEGF-dependant WPB exocytosis and Ang-2 secretion promoted pericyte migration toward ECs. Pericyte migration was inhibited by adding recombinant Ang-2 or by silencing Ang-1 (angiopoietin-1) or Tie2 (angiopoietin-1 receptor) in pericytes. Consistently, in vivo anti-VEGF treatment induced accumulation of WPBs in retinal vessels because of the inhibition of WPB exocytosis and promoted the increase of pericyte coverage of retinal vessels during angiogenesis. In tumor angiogenesis, depletion of WPBs in vWF knockout tumor-bearing mice promoted an increase of tumor angiogenesis and a decrease of pericyte coverage of tumor vessels. By another approach, normalized tumor vessels had higher WPB density. Conclusions We demonstrate that WPB exocytosis and Ang-2 secretion are regulated during angiogenesis to limit pericyte coverage of remodeling vessels by disrupting Ang-1/Tie2 autocrine signaling in pericytes.

Published
2019
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21. Dissecting Effects of Anti-cancer Drugs and Cancer-Associated Fibroblasts by On-Chip Reconstitution of Immunocompetent Tumor Microenvironments.

Author

Nguyen M, De Ninno A, Mencattini A, Mermet-Meillon F, Fornabaio G, Evans SS, Cossutta M, Khira Y, Han W, Sirven P, Pelon F, Di Giuseppe D, Bertani FR, Gerardino A, Yamada A, Descroix S, Soumelis V, Mechta-Grigoriou F, Zalcman G, Camonis J, Martinelli E, Businaro L, and Parrini MC

Subjects
Animals, Cancer-Associated Fibroblasts drug effects, Cattle, Cell Communication drug effects, Cell Line, Tumor, Human Umbilical Vein Endothelial Cells drug effects, Human Umbilical Vein Endothelial Cells metabolism, Humans, Neoplasm Invasiveness, Receptor, ErbB-2 metabolism, Stromal Cells drug effects, Stromal Cells metabolism, Trastuzumab pharmacology, Antineoplastic Agents pharmacology, Cancer-Associated Fibroblasts pathology, Immunocompetence drug effects, Tumor Microenvironment drug effects
Abstract

A major challenge in cancer research is the complexity of the tumor microenvironment, which includes the host immunological setting. Inspired by the emerging technology of organ-on-chip, we achieved 3D co-cultures in microfluidic devices (integrating four cell populations: cancer, immune, endothelial, and fibroblasts) to reconstitute ex vivo a human tumor ecosystem (HER2 + breast cancer). We visualized and quantified the complex dynamics of this tumor-on-chip, in the absence or in the presence of the drug trastuzumab (Herceptin), a targeted antibody therapy directed against the HER2 receptor. We uncovered the capacity of the drug trastuzumab to specifically promote long cancer-immune interactions (>50 min), recapitulating an anti-tumoral ADCC (antibody-dependent cell-mediated cytotoxicity) immune response. Cancer-associated fibroblasts (CAFs) antagonized the effects of trastuzumab. These observations constitute a proof of concept that tumors-on-chip are powerful platforms to study ex vivo immunocompetent tumor microenvironments, to characterize ecosystem-level drug responses, and to dissect the roles of stromal components., (Copyright © 2018 The Authors. Published by Elsevier Inc. All rights reserved.)

Published
2018
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22. Multivalent cationic pseudopeptide polyplexes as a tool for cancer therapy.

Author

Diamantopoulou Z, Gilles ME, Sader M, Cossutta M, Vallée B, Houppe C, Habert D, Brissault B, Leroy E, Maione F, Giraudo E, Destouches D, Penelle J, Courty J, and Cascone I

Abstract

In this study, a novel anticancer reagent based on polyplexes nanoparticles was developed. These nanoparticles are obtained by mixing negatively charged polyelectrolytes with the antitumour cationically-charged pseudopeptide N6L. Using two in vivo experimental tumor pancreatic models based upon PANC-1 and mPDAC cells, we found that the antitumour activity of N6L is significantly raised via its incorporation in polyplexed nanoparticles. Study of the mechanism of action using affinity isolation and si-RNA experiments indicated that N6L-polyplexes are internalized through their interaction with nucleolin. In addition, using a very aggressive model of pancreatic cancer in which gemcitabine, a standard of care for this type of cancer, has a weak effect on tumour growth, we observed that N6L-polyplexes administration has a stronger efficacy than gemcitabine. Biodistribution studies carried out in tumour-bearing mice indicated that N6L-polyplexes localises in tumour tissue, in agreement with its antitumour effect. These results support the idea that N6L nanoparticles could develop into a promising strategy for the treatment of cancer, especially hard-to-treat pancreatic cancers., Competing Interests: CONFLICTS OF INTEREST A potential conflicts of interests could exist related to this study, since José Courty is a co-author of a existing patent on the used of N6L in the treatment of cancer.

Published
2017
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23. Nucleolin Targeting Impairs the Progression of Pancreatic Cancer and Promotes the Normalization of Tumor Vasculature.

Author

Gilles ME, Maione F, Cossutta M, Carpentier G, Caruana L, Di Maria S, Houppe C, Destouches D, Shchors K, Prochasson C, Mongelard F, Lamba S, Bardelli A, Bouvet P, Couvelard A, Courty J, Giraudo E, and Cascone I

Subjects
Animals, Cell Proliferation drug effects, Disease Models, Animal, Disease Progression, Humans, Mice, Tissue Array Analysis, Nucleolin, Carcinoma, Pancreatic Ductal pathology, Neovascularization, Pathologic pathology, Pancreatic Neoplasms pathology, Peptides pharmacology, Phosphoproteins antagonists & inhibitors, RNA-Binding Proteins antagonists & inhibitors
Abstract

Pancreatic cancer is a highly aggressive tumor, mostly resistant to the standard treatments. Nucleolin is overexpressed in cancers and its inhibition impairs tumor growth. Herein, we showed that nucleolin was overexpressed in human specimens of pancreatic ductal adenocarcinoma (PDAC) and that the overall survival significantly increased in patients with low levels of nucleolin. The nucleolin antagonist N6L strongly impaired the growth of primary tumors and liver metastasis in an orthotopic mouse model of PDAC (mPDAC). Similar antitumor effect of N6L has been observed in a highly angiogenic mouse model of pancreatic neuroendocrine tumor RIP-Tag2. N6L significantly inhibited both human and mouse pancreatic cell proliferation and invasion. Notably, the analysis of tumor vasculature revealed a strong increase of pericyte coverage and vessel perfusion both in mPDAC and RIP-Tag2 tumors, in parallel to an inhibition of tumor hypoxia. Nucleolin inhibition directly affected endothelial cell (EC) activation and changed a proangiogenic signature. Among the vascular activators, nucleolin inhibition significantly decreased angiopoietin-2 (Ang-2) secretion and expression in ECs, in the tumor and in the plasma of mPDAC mice. As a consequence of the observed N6L-induced tumor vessel normalization, pre-treatment with N6L efficiently improved chemotherapeutic drug delivery and increased the antitumor properties of gemcitabine in PDAC mice. In conclusion, nucleolin inhibition is a new anti-pancreatic cancer therapeutic strategy that dually blocks tumor progression and normalizes tumor vasculature, improving the delivery and efficacy of chemotherapeutic drugs. Moreover, we unveiled Ang-2 as a potential target and suitable response biomarker for N6L treatment in pancreatic cancer. Cancer Res; 76(24); 7181-93. ©2016 AACR., (©2016 American Association for Cancer Research.)

Published
2016
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24. Gender health and policies: the state of the art from exposure to solutions.

Author

Siliquini R, Piat SC, Versino E, Gianino MM, Mutu D, Cossutta M, and Manzoli L

Subjects
Female, Health Promotion, Health Status, Humans, Italy, Male, Prejudice, Sex Factors, Health Policy, Health Status Disparities, Healthcare Disparities, Men's Health, Women's Health
Abstract

Objective: To synthesize the determinants of gender inequalities through a narrative review that: (i) describes gender related variables that can create different levels of health; (ii) describes key points that may assist in policy development and its reorientation towards gender differences; (iii) debates potential approaches in understanding gender issues., Methods: Review of the international literature through online databases (Pubmed), search engines, publications and documents from "grey literature"., Inclusion Criteria: publications from 1997, English language; keywords used: gender based analysis; gender and public policy; women's health; gender differences; health policy; gender impact assessment. Among the 300 papers retrieved, 55 were selected for relevance., Results: We performed a narrative synthesis of the included literature, regarding: (i) gender differences and their determinants; (ii) elements for the changing; (iii) possible approaches; (iv) gender influences the pursuit of health and health care access through specific variables; (v) health policies can modify these variables only by a minimal percentage. These interventions should guarantee equity and allow efficient resources allocation. The gap between political announcements and real policy implementation remains unchanged. (vi) Standard approaches to the topic are not feasible due to the scarcity of a specific literature and the numerous cultural differences., Conclusions: . Gender analysis of policies suggests they can differently affect women in comparison to men. However, reforms, strategies and interventions introduced in the last two decades, have achieved a limited success towards better gender equality in health. The main aim is to attack the structural sources of gender inequity in the society.

Published
2009

25. Blood stem cells autografts in patients with high risk multiple myeloma.

Author

Montuoro A, De Rosa L, Zoli V, Pandolfi A, Cossutta M, Lanti T, and De Laurenzi A

Subjects
Adult, Female, Humans, Male, Middle Aged, Retrospective Studies, Risk Factors, Blood Transfusion, Autologous methods, Hematopoietic Stem Cell Transplantation, Multiple Myeloma therapy
Abstract

Five patients with high risk multiple myeloma not responsive to standard chemotherapy were treated by high-dose chemotherapy (Melphalan, Cyclophosphamide) (HDC) and total body irradiation (TBI) followed by autografting with blood stem cells. These cells were previously collected by leukaphereses from eight to twelve occasions during hematopoietic recovery following profound aplasia induced by each course of intensive chemotherapy (Vincristine, Adriamycin, Cyclosphosphamide, Prednisone) when the patient reached a neutrophil count of 1,000/microliters and a platelet count of 100,000/microliters. No patients had evidence of tumor plasmacells in leukaphereses products using cytology, immunocytochemistry and immunofluorescence. At this time the patient 5 is not evaluable because of the short follow-up. One died at day 30 from heart failure. All living patients achieved a complete remission which persisted at a follow-up of 300, 261 and 136 days. Autologous blood derived hematopoietic stem cells induced successful and sustained engraftment in all living patients. Our results indicate the feasibility of this therapeutic approach over allogenic or autologous bone marrow transplantation in selected patients with high tumour mass multiple myeloma.

Published
1990

26. Collection of peripheral blood stem cells by apheresis with continuous flow blood cell separator Dideco Vivacell.

Author

Del Monte C, Basso P, Consoli P, Cossutta M, Morara R, Pescarollo A, and Lanti T

Subjects
Adult, Female, Humans, Male, Middle Aged, Specimen Handling methods, Blood Component Removal methods, Cell Separation instrumentation, Hematopoietic Stem Cells
Abstract

In S. Camillo Hospital, Rome, the Apheresis Center (CNTS-CRI) and the Haematological Division, Authors treated 17 patients affected by haematologic malignances and solid tumours with leukoapheresis procedures for PBSC collection. Nine patients were treated with continuous-flow cell separator Dideco Vivacell, performing a total of 50 collection procedures. Mean values of total collected NC and MNC were 6.5 x 10(9) and 5.5 x 10(9), with a mean recovery 24% and 52%. Authors took patient's blood samples during the procedure, in order to analyze the MNC collection and to optimize the separation efficiency. Haemopoietic reconstitution values of the eight patients submitted to APBSCT showed the effectiveness of our method of cell collection.

Published
1990

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