Your search keyword '"Perla, F"' showing total 122 results

1. Study about American Trypanosomiasis and Chagas Disease: An Approach towards Sexual Transmission

Author

Gomes, Clever, primary, Almeida, Adriana B., additional, Rosa, Ana C., additional, Araujo, Perla F., additional, and Teixeira, Antonio R. L., additional

Published

2022

2. Histoire du sport et de la médecine au sein de la Fédération française d'athlétisme

Author

Depiesse, F., primary, Edouard, P., additional, Bruneau, A., additional, Agbojan, M.-M., additional, Colle, F., additional, Perla, F., additional, and Pruvost, J., additional

Published

2022

3. Organisation médicale et métiers médicaux et paramédicaux au sein de la Fédération française d’athlétisme

Author

Depiesse, F., primary, Edouard, P., additional, Bruneau, A., additional, Agbojan, M.-M., additional, Perla, F., additional, and Pruvost, J., additional

Published

2022

4. American trypanosomiasis and Chagas disease: Sexual transmission

Author

Gomes, Clever, Almeida, Adriana B., Rosa, Ana C., Araujo, Perla F., and Teixeira, Antonio R.L.

Published

2019

5. American trypanosomiasis and Chagas disease: Sexual transmission

Author

Clever Gomes, Adriana B. Almeida, Ana C. Rosa, Perla F. Araujo, and Antonio R.L. Teixeira

Subjects

Infectious and parasitic diseases, RC109-216

Abstract

Objective: To contribute to the discussion on the research findings indicating the sexual transmission of American trypanosomiasis and Chagas disease in humans. Methods: A review of the literature was performed to investigate the routes of transmission of Trypanosoma cruzi parasites and to evaluate the distribution of Chagas disease, which is now found across five continents. Results: The epidemiological profile of American trypanosomiasis, which is still considered a neglected disease of the poor people of Latin America, has changed over time. A family-based study demonstrated that the blood protozoan T. cruzi can be transmitted sexually from infected males and females to naïve mates. Conclusions: Evidence that Chagas disease can be transmitted sexually, coupled with the migration of individuals with Chagas disease to previously non-endemic countries and increased travel to endemic countries, has implications for public health. Improved screening of blood supplies and prenatal care are required to prevent congenital spread. Keywords: Trypanosoma cruzi, Chagas disease, Sexual transmission, Humans, Mouse model system, Vertical transmission, Diagnosis, Prevention

Published

2019

6. The Role of Registers in Increasing Knowledge and Improving Management of Children and Adolescents Affected by Familial Hypercholesterolemia: the LIPIGEN Pediatric Group

Author

Gazzotti, M, Casula, M, Bertolini, S, Capra, M, Olmastroni, E, Catapano, A, Pederiva, C, Allevi, M, Arca, M, Auricchio, R, Averna, M, Baldera, D, Banderali, G, Bartuli, A, Biasucci, G, Borghi, C, Bruzzi, P, Buganza, R, Buonuomo, P, Calabro, P, Calandra, S, Carubbi, F, Cesaro, A, Cipollone, F, Citroni, N, Covetti, G, Cremonini, A, D'Addato, S, Ben, M, Di Taranto, M, Fortunato, G, Franceschi, R, Galimberti, F, Genovesi, S, Giammanco, A, Grigore, L, Guardamagna, O, Iannuzzi, A, Iannuzzo, G, Lascala, L, Locatelli, F, Iughetti, L, Madaghiele, S, Mandraffino, G, Mannarino, M, Marco, B, Maroni, L, Minicocci, I, Mombelli, G, Muntoni, S, Nascimbeni, F, Parati, G, Passaro, A, Pavanello, C, Pellegatta, F, Perla, F, Generale, M, Pirro, M, Pisciotta, L, Pujia, A, Purrello, F, Rinaldi, E, Sarzani, R, Scicali, R, Suppressa, P, Tarugi, P, Verachtert, S, Vigna, G, Werba, J, Zambon, A, Zambon, S, Zenti, M, Gazzotti M., Casula M., Bertolini S., Capra M. E., Olmastroni E., Catapano A. L., Pederiva C., Allevi M., Arca M., Auricchio R., Averna M., Baldera D., Banderali G., Bartuli A., Biasucci G., Borghi C., Bruzzi P., Buganza R., Buonuomo P. S., Calabro P., Calandra S., Carubbi F., Cesaro A., Cipollone F., Citroni N., Covetti G., Cremonini A., D'Addato S., Ben M. D., Di Taranto M. D., Fortunato G., Franceschi R., Galimberti F., Genovesi S., Giammanco A., Grigore L., Guardamagna O., Iannuzzi A., Iannuzzo G., Lascala L., Locatelli F., Iughetti L., Madaghiele S., Mandraffino G., Mannarino M. R., Marco B., Maroni L., Minicocci I., Mombelli G., Muntoni S., Nascimbeni F., Parati G., Passaro A., Pavanello C., Pellegatta F., Perla F. M., Generale M., Pirro M., Pisciotta L., Pujia A., Purrello F., Rinaldi E., Sarzani R., Scicali R., Suppressa P., Tarugi P., Verachtert S., Vigna G. B., Werba J. P., Zambon A., Zambon S., Zenti M. G., Gazzotti, M, Casula, M, Bertolini, S, Capra, M, Olmastroni, E, Catapano, A, Pederiva, C, Allevi, M, Arca, M, Auricchio, R, Averna, M, Baldera, D, Banderali, G, Bartuli, A, Biasucci, G, Borghi, C, Bruzzi, P, Buganza, R, Buonuomo, P, Calabro, P, Calandra, S, Carubbi, F, Cesaro, A, Cipollone, F, Citroni, N, Covetti, G, Cremonini, A, D'Addato, S, Ben, M, Di Taranto, M, Fortunato, G, Franceschi, R, Galimberti, F, Genovesi, S, Giammanco, A, Grigore, L, Guardamagna, O, Iannuzzi, A, Iannuzzo, G, Lascala, L, Locatelli, F, Iughetti, L, Madaghiele, S, Mandraffino, G, Mannarino, M, Marco, B, Maroni, L, Minicocci, I, Mombelli, G, Muntoni, S, Nascimbeni, F, Parati, G, Passaro, A, Pavanello, C, Pellegatta, F, Perla, F, Generale, M, Pirro, M, Pisciotta, L, Pujia, A, Purrello, F, Rinaldi, E, Sarzani, R, Scicali, R, Suppressa, P, Tarugi, P, Verachtert, S, Vigna, G, Werba, J, Zambon, A, Zambon, S, Zenti, M, Gazzotti M., Casula M., Bertolini S., Capra M. E., Olmastroni E., Catapano A. L., Pederiva C., Allevi M., Arca M., Auricchio R., Averna M., Baldera D., Banderali G., Bartuli A., Biasucci G., Borghi C., Bruzzi P., Buganza R., Buonuomo P. S., Calabro P., Calandra S., Carubbi F., Cesaro A., Cipollone F., Citroni N., Covetti G., Cremonini A., D'Addato S., Ben M. D., Di Taranto M. D., Fortunato G., Franceschi R., Galimberti F., Genovesi S., Giammanco A., Grigore L., Guardamagna O., Iannuzzi A., Iannuzzo G., Lascala L., Locatelli F., Iughetti L., Madaghiele S., Mandraffino G., Mannarino M. R., Marco B., Maroni L., Minicocci I., Mombelli G., Muntoni S., Nascimbeni F., Parati G., Passaro A., Pavanello C., Pellegatta F., Perla F. M., Generale M., Pirro M., Pisciotta L., Pujia A., Purrello F., Rinaldi E., Sarzani R., Scicali R., Suppressa P., Tarugi P., Verachtert S., Vigna G. B., Werba J. P., Zambon A., Zambon S., and Zenti M. G.

Abstract

Pathology registers can be a useful tool to overcome obstacles in the identification and management of familial hypercholesterolemia since childhood. In 2018, the LIPIGEN pediatric group was constituted within the Italian LIPIGEN study to focus on FH subjects under 18 years. This work aimed at discussing its recent progress and early outcomes. Demographic, biochemical, and genetic baseline characteristics were collected, with an in-depth analysis of the genetic defects. The analysis was carried out on 1,602 children and adolescents (mean age at baseline 9.9 ± 4.0 years), and almost the whole cohort underwent the genetic test (93.3%). Overall, the untreated mean value of LDL-C was 220.0 ± 97.2 mg/dl, with an increasing gradient from subjects with a negative (N = 317; mean untreated LDL-C = 159.9 ± 47.7 mg/dl), inconclusive (N = 125; mean untreated LDL-C = 166.4 ± 56.5 mg/dl), or positive (N = 1,053; mean untreated LDL-C = 246.5 ± 102.1 mg/dl) genetic diagnosis of FH. In the latter group, the LDL-C values presented a great variability based on the number and the biological impact of involved causative variants. The LIPIGEN pediatric group represents one of the largest cohorts of children with FH, allowing the deepening of the characterization of their baseline and genetic features, providing the basis for further longitudinal investigations for complete details.

Published

2022

7. Photocatalytic activity of ZnO nanoparticles synthesized from zinc nitrate and botanical extracts of neem, chrysanthemum, Mexican marigold and shiitake mushroom

Author

López‐López, Juan R., primary, Tejeda‐Ochoa, Armando, additional, Cervantes‐Gaxiola, Maritza E., additional, Herrera‐Ramirez, José M., additional, and Méndez‐Herrera, Perla F., additional

Published

2023

8. Photocatalytic activity of <scp>ZnO</scp> nanoparticles synthesized from zinc nitrate and botanical extracts of neem, chrysanthemum, Mexican marigold and shiitake mushroom

Author

Juan R. López‐López, Armando Tejeda‐Ochoa, Maritza E. Cervantes‐Gaxiola, José M. Herrera‐Ramirez, and Perla F. Méndez‐Herrera

Subjects

Inorganic Chemistry, Fuel Technology, Renewable Energy, Sustainability and the Environment, General Chemical Engineering, Organic Chemistry, Pollution, Waste Management and Disposal, Biotechnology

Published

2023

9. Study about American Trypanosomiasis and Chagas Disease: An Approach towards Sexual Transmission

Author

Clever Gomes, Adriana B. Almeida, Ana C. Rosa, Perla F. Araujo, and Antonio R. L. Teixeira

Published

2022

10. CHAPITRE 1 - Histoire du sport et de la médecine au sein de la Fédération française d'athlétisme

Author

Depiesse, F., Edouard, P., Bruneau, A., Agbojan, M.-M., Colle, F., Perla, F., and Pruvost, J.

Published

2022

11. CHAPITRE2 - Organisation médicale et métiers médicaux et paramédicaux au sein de la Fédération française d’athlétisme

Author

Depiesse, F., Edouard, P., Bruneau, A., Agbojan, M.-M., Perla, F., and Pruvost, J.

Published

2022

12. The Italian multiple sclerosis register

Author

Trojano, M, Bergamaschi, R, Amato, M, Comi, G, Ghezzi, A, Lepore, V, Marrosu, M, Mosconi, P, Patti, F, Ponzio, M, Zaratin, P, Battaglia, M, Acquistapace, D, Aguglia, U, Annunziata, P, Ardito, B, Avolio, C, Balgera, R, Bandini, F, Banfi, P, Barone, P, Bellantonio, P, Bertolotto, A, Bertora, P, Bombardi, R, Bosco Zimatore, G, Bossio, R, Bramanti, P, Brescia Morra, V, Brioschi, A, Bruzzone, M, Buccafusca, M, Busillo, V, Caneve, G, Caniatti, L, Capone, L, Capone, F, Cappellani, A, Cargnelutti, D, Cavaletti, G, Cavalla, P, Celani, M, Centonze, D, Chiveri, L, Clerici, R, Clerico, M, Cocco, E, Comi, C, Coniglio, M, Cordera, S, Corea, F, Cortese, A, Costantino, G, Cottone, S, Crociani, P, D’Andrea, F, Danni, M, De Luca, G, de Pascalis, D, De Robertis, F, De Stefano, N, Di Battista, G, Di Napoli, M, Falcini, M, Fausto, F, Ferrò, M, Florio, C, Fortunato, M, Frittelli, C, Galgani, S, Gallo, P, Gatto, M, Gazzola, P, Geda, C, Giordano, A, Granella, F, Grasso, M, Grimaldi, L, Imperiale, D, Lo Russo, L, Logullo, F, Lugaresi, A, Lus, G, Maccarrone, G, Maimone, D, Malagù, S, Marconi, R, Maritato, P, Massacesi, L, Mazzoni, M, Meucci, G, Mirabella, M, Montepietra, S, Nasuelli, D, Neri, W, Orefice, G, Parodi, S, Pasquali, L, Passarella, B, Peresson, M, Perla, F, Pesci, I, Piantadosi, C, Piras, M, Pizio, N, Pozzilli, C, Protti, A, Pugliatti, M, Quatrale, R, Ragno, M, Rezzonico, M, Ribizzi, G, Riva, M, Ronzoni, M, Rosso, M, Rottoli, M, Rovaris, M, Salemi, G, Salvetti, M, Santangelo, M, Santangelo, G, Santuccio, G, Sarchielli, P, Scarpini, E, Sechi, G, Severi, S, Sinisi, L, Sola, P, Spitaleri, D, Tassinari, T, Tedeschi, G, Tonietti, S, Torri Clerici, V, Totaro, R, Traccis, S, Turla, M, Uccelli, A, Ulivelli, M, Valentino, P, Valeriani, M, Venturi, S, Vianello, M, Zaffaroni, M, Trojano, Maria, Bergamaschi, Roberto, Amato, Maria Pia, Comi, Giancarlo, Ghezzi, Angelo, Lepore, Vito, Marrosu, Maria Giovanna, Mosconi, Paola, Patti, Francesco, Ponzio, Michela, Zaratin, Paola, Battaglia, Mario Alberto, Acquistapace, D., Aguglia, U., Amato, M. P., Annunziata, P., Ardito, B., Avolio, C., Balgera, R., Bandini, F., Banfi, P., Barone, P., Bellantonio, P., Bergamaschi, R., Bertolotto, A., Bertora, P., Bombardi, R., Bosco Zimatore, G., Bossio, R. B., Bramanti, P., Brescia Morra, V., Brioschi, A. M., Bruzzone, M., Buccafusca, M., Busillo, V., Caneve, G., Caniatti, L. M., Capone, L., Capone, F., Cappellani, A., Cargnelutti, D., Cavaletti, G., Cavalla, P., Celani, M. G., Centonze, D., Chiveri, L., Clerici, R., Clerico, M., Cocco, E., Comi, G., Comi, C., Coniglio, M. G., Cordera, S., Corea, F., Cortese, A., Costantino, G., Cottone, S., Crociani, P., D’Andrea, F., Danni, M. C., De Luca, G., de Pascalis, D., De Robertis, F., De Stefano, N., Di Battista, G., Di Napoli, M., Falcini, M., Fausto, F., Ferrò, M. T., Florio, C., Fortunato, M., Frittelli, C., Galgani, S., Gallo, P., Gatto, M., Gazzola, P., Geda, C., Giordano, A., Granella, F., Grasso, M. G., Grimaldi, L. M. E., Imperiale, D., Lo Russo, L., Logullo, F. O., Lugaresi, A., Lus, G., Maccarrone, G., Maimone, D., Malagù, S., Marconi, R., Maritato, P., Massacesi, L., Mazzoni, M., Meucci, G., Mirabella, M., Montepietra, S., Nasuelli, D., Neri, W., Orefice, G., Parodi, S., Pasquali, L., Passarella, B., Patti, F., Peresson, M., Perla, F., Pesci, I., Piantadosi, C., Piras, M. L., Pizio, N. R., Pozzilli, C., Protti, A., Pugliatti, M., Quatrale, R., Ragno, M., Rezzonico, M., Ribizzi, G., Riva, M., Ronzoni, M., Rosso, M. G., Rottoli, M., Rovaris, M., Salemi, G., Salvetti, M., Santangelo, M., Santangelo, G., Santuccio, G., Sarchielli, P., Scarpini, E., Sechi, G. P., Severi, S., Sinisi, L., Sola, P., Spitaleri, D., Tassinari, T., Tedeschi, G., Tonietti, S., Torri Clerici, V., Totaro, R., Traccis, S., Trojano, M., Turla, M., Uccelli, A., Ulivelli, M., Valentino, P., Valeriani, M., Venturi, S., Vianello, M., Zaffaroni, M., Trojano, M, Bergamaschi, R, Amato, M, Comi, G, Ghezzi, A, Lepore, V, Marrosu, M, Mosconi, P, Patti, F, Ponzio, M, Zaratin, P, Battaglia, M, Acquistapace, D, Aguglia, U, Annunziata, P, Ardito, B, Avolio, C, Balgera, R, Bandini, F, Banfi, P, Barone, P, Bellantonio, P, Bertolotto, A, Bertora, P, Bombardi, R, Bosco Zimatore, G, Bossio, R, Bramanti, P, Brescia Morra, V, Brioschi, A, Bruzzone, M, Buccafusca, M, Busillo, V, Caneve, G, Caniatti, L, Capone, L, Capone, F, Cappellani, A, Cargnelutti, D, Cavaletti, G, Cavalla, P, Celani, M, Centonze, D, Chiveri, L, Clerici, R, Clerico, M, Cocco, E, Comi, C, Coniglio, M, Cordera, S, Corea, F, Cortese, A, Costantino, G, Cottone, S, Crociani, P, D’Andrea, F, Danni, M, De Luca, G, de Pascalis, D, De Robertis, F, De Stefano, N, Di Battista, G, Di Napoli, M, Falcini, M, Fausto, F, Ferrò, M, Florio, C, Fortunato, M, Frittelli, C, Galgani, S, Gallo, P, Gatto, M, Gazzola, P, Geda, C, Giordano, A, Granella, F, Grasso, M, Grimaldi, L, Imperiale, D, Lo Russo, L, Logullo, F, Lugaresi, A, Lus, G, Maccarrone, G, Maimone, D, Malagù, S, Marconi, R, Maritato, P, Massacesi, L, Mazzoni, M, Meucci, G, Mirabella, M, Montepietra, S, Nasuelli, D, Neri, W, Orefice, G, Parodi, S, Pasquali, L, Passarella, B, Peresson, M, Perla, F, Pesci, I, Piantadosi, C, Piras, M, Pizio, N, Pozzilli, C, Protti, A, Pugliatti, M, Quatrale, R, Ragno, M, Rezzonico, M, Ribizzi, G, Riva, M, Ronzoni, M, Rosso, M, Rottoli, M, Rovaris, M, Salemi, G, Salvetti, M, Santangelo, M, Santangelo, G, Santuccio, G, Sarchielli, P, Scarpini, E, Sechi, G, Severi, S, Sinisi, L, Sola, P, Spitaleri, D, Tassinari, T, Tedeschi, G, Tonietti, S, Torri Clerici, V, Totaro, R, Traccis, S, Turla, M, Uccelli, A, Ulivelli, M, Valentino, P, Valeriani, M, Venturi, S, Vianello, M, Zaffaroni, M, Trojano, Maria, Bergamaschi, Roberto, Amato, Maria Pia, Comi, Giancarlo, Ghezzi, Angelo, Lepore, Vito, Marrosu, Maria Giovanna, Mosconi, Paola, Patti, Francesco, Ponzio, Michela, Zaratin, Paola, Battaglia, Mario Alberto, Acquistapace, D., Aguglia, U., Amato, M. P., Annunziata, P., Ardito, B., Avolio, C., Balgera, R., Bandini, F., Banfi, P., Barone, P., Bellantonio, P., Bergamaschi, R., Bertolotto, A., Bertora, P., Bombardi, R., Bosco Zimatore, G., Bossio, R. B., Bramanti, P., Brescia Morra, V., Brioschi, A. M., Bruzzone, M., Buccafusca, M., Busillo, V., Caneve, G., Caniatti, L. M., Capone, L., Capone, F., Cappellani, A., Cargnelutti, D., Cavaletti, G., Cavalla, P., Celani, M. G., Centonze, D., Chiveri, L., Clerici, R., Clerico, M., Cocco, E., Comi, G., Comi, C., Coniglio, M. G., Cordera, S., Corea, F., Cortese, A., Costantino, G., Cottone, S., Crociani, P., D’Andrea, F., Danni, M. C., De Luca, G., de Pascalis, D., De Robertis, F., De Stefano, N., Di Battista, G., Di Napoli, M., Falcini, M., Fausto, F., Ferrò, M. T., Florio, C., Fortunato, M., Frittelli, C., Galgani, S., Gallo, P., Gatto, M., Gazzola, P., Geda, C., Giordano, A., Granella, F., Grasso, M. G., Grimaldi, L. M. E., Imperiale, D., Lo Russo, L., Logullo, F. O., Lugaresi, A., Lus, G., Maccarrone, G., Maimone, D., Malagù, S., Marconi, R., Maritato, P., Massacesi, L., Mazzoni, M., Meucci, G., Mirabella, M., Montepietra, S., Nasuelli, D., Neri, W., Orefice, G., Parodi, S., Pasquali, L., Passarella, B., Patti, F., Peresson, M., Perla, F., Pesci, I., Piantadosi, C., Piras, M. L., Pizio, N. R., Pozzilli, C., Protti, A., Pugliatti, M., Quatrale, R., Ragno, M., Rezzonico, M., Ribizzi, G., Riva, M., Ronzoni, M., Rosso, M. G., Rottoli, M., Rovaris, M., Salemi, G., Salvetti, M., Santangelo, M., Santangelo, G., Santuccio, G., Sarchielli, P., Scarpini, E., Sechi, G. P., Severi, S., Sinisi, L., Sola, P., Spitaleri, D., Tassinari, T., Tedeschi, G., Tonietti, S., Torri Clerici, V., Totaro, R., Traccis, S., Trojano, M., Turla, M., Uccelli, A., Ulivelli, M., Valentino, P., Valeriani, M., Venturi, S., Vianello, M., and Zaffaroni, M.

Abstract

The past decade has seen extraordinary increase in worldwide availability of and access to several large multiple sclerosis (MS) databases and registries. MS registries represent powerful tools to provide meaningful information on the burden, natural history, and long-term safety and effectiveness of treatments. Moreover, patients, physicians, industry, and policy makers have an active interest in real-world observational studies based on register data, as they have the potential to answer the questions that are most relevant to daily treatment decision-making. In 2014, the Italian MS Foundation, in collaboration with the Italian MS clinical centers, promoted and funded the creation of the Italian MS Register, a project in continuity with the existing Italian MS Database Network set up from 2001. Main objective of the Italian MS Register is to create an organized multicenter structure to collect data of all MS patients for better defining the disease epidemiology, improving quality of care, and promoting research projects in high-priority areas. The aim of this article is to present the current framework and network of the Italian MS register, including the methodology used to improve the quality of data collection and to facilitate the exchange of data and the collaboration among national and international groups.

Published

2019

13. On parallel asset-liability management in life insurance: a forward risk-neutral approach

Author

Corsaro, S., De Angelis, P.L., Marino, Z., Perla, F., and Zanetti, P.

Published

2010

14. Upregulated monocyte expression of PLIN2 is associated with early arterial injury in children with overweight/obesity

Author

Pisano, Eugenia, Pacifico, L., Perla, F. M., Liuzzo, Giovanna, Chiesa, C., Lavorato, M., Mingrone, Geltrude, Fabrizi, M., Fintini, D., Severino, Anna, Manco, M., Pisano E., Liuzzo G. (ORCID:0000-0002-5714-0907), Mingrone G. (ORCID:0000-0003-2021-528X), Severino A., Pisano, Eugenia, Pacifico, L., Perla, F. M., Liuzzo, Giovanna, Chiesa, C., Lavorato, M., Mingrone, Geltrude, Fabrizi, M., Fintini, D., Severino, Anna, Manco, M., Pisano E., Liuzzo G. (ORCID:0000-0002-5714-0907), Mingrone G. (ORCID:0000-0003-2021-528X), and Severino A.

Abstract

Background and aims: Perilipin 2 (PLIN2) regulates intracellular lipid metabolism in macrophages, and thus, plays a role in atherosclerosis. Aim of the study was to evaluate whether PLIN2 dysregulation is involved in the onset of preclinical atherosclerosis in children with overweight/obesity and to explore dysregulation mechanisms. Methods: Sixty-three children with overweight/obesity and 21 normal weight children (controls) of the same age and sex were enrolled. Carotid intima media thickness (cIMT) was evaluated; mRNA expression of PLIN2 and proteasome subunits (PSMD3, PSMC4) was determined by Real Time PCR, and protein expression of PLIN2, LAMP2A and Hsc70 by Western blot analysis; fluorimetric assay was used to measure proteasome chymotrypsin like activity. We performed transient LAMP2A downregulation by siRNA and quantified intracellular lipids in monocytes by Nile Red staining and flow cytometry analysis. Results: PLIN2 protein levels were significantly higher in children with overweight/obesity and correlated with cIMT after adjusting for confounders. Accordingly, monocytes of children with overweight/obesity showed a higher intracellular amount of lipids compared with controls. mRNA expression of the regulatory subunits PSMC4 and PSMD3 and proteasome activity were lower in children with overweight/obesity, while expression of LAMP2A and Hsc70 proteins, which belong to the chaperone-mediated autophagy (CMA) pathway, was not different, suggesting that PLIN2 dysregulation in monocytes was due to an impairment of proteasome efficiency and was not CMA related. Conclusion: PLIN2 was overexpressed in monocytes of children with overweight/obesity and could contribute to the onset of arteropathy. Our data suggest that proteasome impairment could contribute to PLIN2 overexpression.

Published

2021

15. Déchirure isolée de la jonction myotendineuse du muscle infra-épineux traité par injections de plasma riche en plaquettes. À propos d’un cas

Author

Perla, F., Gueret, P., Rotari, V., Aihonnou, T., and Mencière, M.L.

Published

2020

16. Variations of the perforin gene in patients with multiple sclerosis

Author

Cappellano, G, Orilieri, E, Comi, C, Chiocchetti, A, Bocca, S, Boggio, E, Bernardone, I S, Cometa, A, Clementi, R, Barizzone, N, D'Alfonso, S, Corrado, L, Galimberti, D, Scarpini, E, Guerini, F R, Caputo, D, Paolicelli, D, Trojano, M, Figà-Talamanca, L, Salvetti, M, Perla, F, Leone, M, Monaco, F, and Dianzani, U

Published

2008

17. Inheritance of DNA transferred from American trypanosomes to human hosts.

Author

Mariana M Hecht, Nadjar Nitz, Perla F Araujo, Alessandro O Sousa, Ana de Cássia Rosa, Dawidson A Gomes, Eduardo Leonardecz, and Antonio R L Teixeira

Subjects

Medicine, Science

Abstract

Interspecies DNA transfer is a major biological process leading to the accumulation of mutations inherited by sexual reproduction among eukaryotes. Lateral DNA transfer events and their inheritance has been challenging to document. In this study we modified a thermal asymmetric interlaced PCR by using additional targeted primers, along with Southern blots, fluorescence techniques, and bioinformatics, to identify lateral DNA transfer events from parasite to host. Instances of naturally occurring human infections by Trypanosoma cruzi are documented, where mitochondrial minicircles integrated mainly into retrotransposable LINE-1 of various chromosomes. The founders of five families show minicircle integrations that were transferred vertically to their progeny. Microhomology end-joining of 6 to 22 AC-rich nucleotide repeats in the minicircles and host DNA mediates foreign DNA integration. Heterogeneous minicircle sequences were distributed randomly among families, with diversity increasing due to subsequent rearrangement of inserted fragments. Mosaic recombination and hitchhiking on retrotransposition events to different loci were more prevalent in germ line as compared to somatic cells. Potential new genes, pseudogenes, and knockouts were identified. A pathway of minicircle integration and maintenance in the host genome is suggested. Thus, infection by T. cruzi has the unexpected consequence of increasing human genetic diversity, and Chagas disease may be a fortuitous share of negative selection. This demonstration of contemporary transfer of eukaryotic DNA to the human genome and its subsequent inheritance by descendants introduces a significant change in the scientific concept of evolutionary biology and medicine.

Published

2010

18. On High-Performance Software Development for the Numerical Simulation of Life Insurance Policies

Author

Marino, Z, primary, Perla, F, additional, Corsaro, S, additional, and De Angelis, P, additional

Published

2007

19. Potassium Ferrate and/or Sodium Ferrate Generation Using a Prototype of Electrochemical Reactor without Membrane

Author

López, Juan R., primary, Peñuelas Fong, Dora C., additional, Méndez Herrera, Perla F., additional, Pérez Sicairos, Sergio, additional, Calderón Ayala, Ignacio, additional, and Ortíz del Castillo, Jesús R., additional

Published

2019

20. Sexual transmission of American trypanosomiasis in humans: a new potential pandemic route for Chagas parasites

Author

Manuela M Britto, Carlos Fernando Pimentel, Rozeneide M. Alves, Ana C. Rosa, Perla F. Araujo, Antonio R. L. Teixeira, Sebastião Aldo da Silva Valente, Adriano R. Silva, Adriana B. Almeida, Alessandro O. Sousa, Luciana Hagström, and Vera da Costa Valente

Subjects

0301 basic medicine, Male, Chagas disease, Enzyme-Linked Immunospot Assay, lcsh:QR1-502, Polymerase Chain Reaction, Brasil / epidemiologia, lcsh:Microbiology, law.invention, Serology, 0302 clinical medicine, ELISPOT / m?todos, law, Doen?as Sexualmente Transmiss?veis / parasitologia, Doen?a de Chagas / epidemiologia, Longitudinal Studies, humans, Child, Fluorescent Antibody Technique, Indirect, Polymerase chain reaction, Doen?a de Chagas / transmiss?o, ELISPOT, Articles, Middle Aged, Humanos, Amazônia, Child, Preschool, Acute Disease, Population study, Trypanosoma cruzi / imunologia, epidemiology, Female, Antibody, Doen?as Sexualmente Transmiss?veis / patologia, Brazil, Microbiology (medical), Adult, Sexual transmission, lcsh:Arctic medicine. Tropical medicine, Adolescent, lcsh:RC955-962, Trypanosoma cruzi, 030231 tropical medicine, Sexually Transmitted Diseases, Estudos Longitudinais, Biology, Trypanosoma cruzi / gen?tica, 03 medical and health sciences, Young Adult, parasitic diseases, medicine, Rea??o em Cadeia da Polimerase / m?todos, Humans, family study, Doen?as Sexualmente Transmiss?veis / epidemiologia, Epidemiologia, Amazon, Pandemics, Aged, Chagas, Doença de, medicine.disease, biology.organism_classification, Virology, 030104 developmental biology, Immunology, biology.protein, T?cnica Indireta de Fluoresc?ncia para Anticorpo / m?todos

Abstract

Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. Minist?rio da Sa?de. Secretaria de Vigil?ncia em Sa?de. Instituto Evandro Chagas. Ananindeua, PA, Brasil. Minist?rio da Sa?de. Secretaria de Vigil?ncia em Sa?de. Instituto Evandro Chagas. Ananindeua, PA, Brasil. Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. Universidade de Bras?lia. Faculdade de Medicina. Laborat?rio Multidisciplinar de Pesquisa em Doen?a de Chagas. Bras?lia, DF, Brasil. BACKGROUND: The Trypanosoma cruzi infection endemic in Latin America has now spread to several countries across four continents; this endemic involves triatomine vector-free protists. We hypothesised that the sexual transmission of T. cruzi contributes to the ongoing spread of Chagas disease. OBJECTIVES: A short-term longitudinal study was conducted to evaluate this hypothesis. METHODS: The study population comprised 109 subjects from four families, among whom 21 had been diagnosed with acute Chagas disease by direct parasitological analysis. Blood mononuclear cells and serum samples were obtained from each study subject once per year for three consecutive years. Enzyme-linked immunosorbent assay (ELISA) and indirect immunofluorescence serological examinations were used to detect specific T. cruzi antibodies. Polymerase chain reaction of T. cruzi DNA revealed 188-nucleotide bands, which hybridised to a specific radiolabelled probe and were confirmed by cloning and sequencing. RESULTS: Three independent assessments at different time points revealed T. cruzi nuclear DNA footprints in 76% (83/109) of the study population with active infection. In contrast, the ELISA and indirect immunofluorescence assays detected the T. cruzi antibody in 28.4% (31/109) of the study samples. Moreover, the semen from 82.6% (19/23) of subjects people revealed harboured the 188- bp base pair T. cruzi footprint. Interestingly, the ejaculates of nuclear DNA-positive Chagas patient transmitted the T. cruzi upon peritoneal injection or infusion in the vagina of mice, and amastigotes were detected in the skeletal muscle, myocardium, vas deferens, and uterine tube. MAIN CONCLUSIONS: T. cruzi infections can be transmitted from females or males to na?ve mates through intercourse, and progeny showed discrepancies between the ratios of nuclear DNA footprints and specific antibody that can be explained by the tolerance attained during early embryo growth. Additional studies are needed to develop drugs to eradicate the infections. Additionally, the importance of a vigorous education, information, and communication program to prevent sexually transmitted Chagas disease in humans cannot be underemphasised.

Published

2017

21. Sexual transmission of american trypanosomes from males and females to naive mates

Author

Francisco Ernesto Moreno Bernal, Ana de Cássia Rosa, Antonio R. L. Teixeira, Sebastião Aldo da Silva Valente, Perla F. Araujo, and Adriana B. Almeida

Subjects

Male, 0301 basic medicine, Chagas disease, Sexual transmission, Offspring, Transmiss?o Vertical de Doen?a Infecciosa, Trypanosoma cruzi, General Chemical Engineering, Doen?a de Chagas / parasitologia, Doen?a de Chagas / imunologia, Population, Sexually Transmitted Diseases, Physiology, Semen, Chick Embryo, General Biochemistry, Genetics and Molecular Biology, Mice, 03 medical and health sciences, 0302 clinical medicine, parasitic diseases, medicine, Animals, Humans, Chagas Disease, education, education.field_of_study, Doen?a de Chagas / transmiss?o, General Immunology and Microbiology, biology, General Neuroscience, Chagas, Doença de, biology.organism_classification, Epididymis, medicine.disease, 030104 developmental biology, Seminiferous tubule, medicine.anatomical_structure, 030220 oncology & carcinogenesis, Tripanossoma cruzi, Female

Abstract

Foundation for the Advancement of Science (FAPDF) ; National Research Council, Ministry of Science and Technology (CNPq/MCT) ; Agency for Training Human Resources, Ministry of Education (CAPES/ME), Brazil . Universidade de Brasilia. Faculdade de Medicina. Multidisciplinar de Pesquisa em Doen?as de Chagas. Brasilia, DF, Brazil. Universidade de Brasilia. Faculdade de Medicina. Multidisciplinar de Pesquisa em Doen?as de Chagas. Brasilia, DF, Brazil. Universidade de Brasilia. Faculdade de Medicina. Multidisciplinar de Pesquisa em Doen?as de Chagas. Brasilia, DF, Brazil. Universidade de Brasilia. Faculdade de Medicina. Multidisciplinar de Pesquisa em Doen?as de Chagas. Brasilia, DF, Brazil. Minist?rio da Sa?de. Secretaria de Vigil?ncia em Sa?de. Instituto Evandro Chagas. Ananindeua, PA, Brasil. Universidade de Brasilia. Faculdade de Medicina. Multidisciplinar de Pesquisa em Doen?as de Chagas. Brasilia, DF, Brazil. American trypanosomiasis is transmitted to humans by triatomine bugs through the ingestion of contaminated food, by blood transfusions or accidently in hospitals and research laboratories. In addition, the Trypanosoma cruzi infection is transmitted congenitally from a chagasic mother to her offspring, but the male partner's contribution to in utero contamination is unknown. The findings of nests and clumps of amastigotes and of trypomastigotes in the theca cells of the ovary, in the goniablasts and in the lumen of seminiferous tubules suggest that T. cruzi infections are sexually transmitted. The research protocol herein presents the results of a family study population showing parasite nuclear DNA in the diploid blood mononuclear cells and in the haploid gametes of human subjects. Thus, three independent biological samples collected one year apart confirmed that T. cruzi infections were sexually transmitted to progeny. Interestingly, the specific T. cruzi antibody was absent in the majority of family progeny that bore immune tolerance to the parasite antigen. Immune tolerance was demonstrated in chicken refractory to T. cruzi after the first week of embryonic growth, and chicks hatched from the flagellate-inoculated eggs were unable to produce the specific antibody. Moreover, the instillation of the human semen ejaculates intraperitoneally or into the vagina of naive mice yielded T. cruzi amastigotes in the epididymis, seminiferous tubule, vas deferens and uterine tube with an absence of inflammatory reactions in the immune privileged organs of reproduction. The breeding of T. cruzi-infected male and female mice with naive mates resulted in acquisition of the infections, which were later transmitted to the progeny. Therefore, a robust education, information and communication program that involves the population and social organizations is deemed necessary to prevent Chagas disease.

Published

2019

22. American trypanosomiasis and Chagas disease: Sexual transmission

Author

Adriana B. Almeida, Antonio R. L. Teixeira, Clever C. Gomes, Perla F. Araujo, and Ana C. Rosa

Subjects

0301 basic medicine, Microbiology (medical), Chagas disease, Male, medicine.medical_specialty, Sexual transmission, 030106 microbiology, Sexually Transmitted Diseases, Prenatal care, lcsh:Infectious and parasitic diseases, 03 medical and health sciences, 0302 clinical medicine, Environmental health, Epidemiology, parasitic diseases, medicine, Humans, lcsh:RC109-216, Chagas Disease, 030212 general & internal medicine, Trypanosoma cruzi, Travel, biology, business.industry, Transmission (medicine), Public health, Research, Neglected Disease, Neglected Diseases, Prenatal Care, General Medicine, medicine.disease, biology.organism_classification, Infectious Diseases, Latin America, Female, business

Abstract

Objective: To contribute to the discussion on the research findings indicating the sexual transmission of American trypanosomiasis and Chagas disease in humans. Methods: A review of the literature was performed to investigate the routes of transmission of Trypanosoma cruzi parasites and to evaluate the distribution of Chagas disease, which is now found across five continents. Results: The epidemiological profile of American trypanosomiasis, which is still considered a neglected disease of the poor people of Latin America, has changed over time. A family-based study demonstrated that the blood protozoan T. cruzi can be transmitted sexually from infected males and females to naïve mates. Conclusions: Evidence that Chagas disease can be transmitted sexually, coupled with the migration of individuals with Chagas disease to previously non-endemic countries and increased travel to endemic countries, has implications for public health. Improved screening of blood supplies and prenatal care are required to prevent congenital spread. Keywords: Trypanosoma cruzi, Chagas disease, Sexual transmission, Humans, Mouse model system, Vertical transmission, Diagnosis, Prevention

Published

2018

23. Chemi-Structural Stabilization of Formamidinium Lead Iodide Perovskite by Using Embedded Quantum Dots for High-Performance Solar Cells

Author

Masi, Sofia, primary, Echeverría-Arrondo, Carlos, primary, Muhammed, Salim K.P., primary, Ngo, Thi Tuyen, primary, Méndez, Perla F., primary, López-Fraguas, Eduardo, primary, Macias-Pinilla, David F., primary, Planelles, Josep, primary, Climente, Juan I., primary, and Mora-Seró, Iván, primary

Published

2019

24. Sexual Transmission of American Trypanosomes from Males and Females to Naive Mates

Author

Almeida, Adriana B., primary, Araújo, Perla F., additional, Bernal, Francisco M., additional, Rosa, Ana de Cassia, additional, Valente, Sebastião A., additional, and Teixeira, Antonio R.L., additional

Published

2019

25. PbS quantum dots as additives in methylammonium halide perovskite solar cells: the effect of quantum dot capping

Author

Ngo, Thi Tuyen, primary, Masi, Sofia, additional, Mendez, Perla F., additional, Kazes, Miri, additional, Oron, Dan, additional, and Seró, Iván Mora, additional

Published

2019

26. Controlling the interfacial concentrations of I 3 − and Li + ions in illuminated ruthenium (II) complex-sensitized nanoparticulate TiO 2 photoanodes chemically coated by poly(amidoamide) dendrimers generation 4.0 for enhancing the performance of dye-sensitized solar cells

Author

N.J. Pérez-Viramontes, Selene Sepúlveda, C.M. Díaz-Acosta, Erika Bustos, A. Rodríguez, Luis A. Godínez, Perla F. Mendez, Francisco Javier Yate Rodríguez, S. Murcio-Hernández, and Juan Manríquez

Subjects

Materials science, General Chemical Engineering, Photoresistor, Inorganic chemistry, Energy conversion efficiency, chemistry.chemical_element, Photovoltaic conversion efficiency, Ion, law.invention, Ruthenium, Dye-sensitized solar cell, Chemical engineering, chemistry, law, Dendrimer, Electrode, Electrochemistry

Abstract

Ruthenium (II) complex-sensitized TiO 2 electrodes were chemically coated with NH 2 -terminated poly(amidoamide) dendrimers generation 4.0 in order to improve the performance of dye-sensitized solar cells using these photoanodes. The presence of dendrimers in these photodevices produced a global photovoltaic conversion efficiency of 6.78%, which was higher than that obtained for photocells without them (5.43%). The experimental results indicated that this treatment of the dye-sensitized TiO 2 electrodes allowed for controlling the concentrations of I 3 − anions and Li + cations into the dendrimers-modified dyed-TiO 2 pores during operation of the photocells. Consequently, the charge interception reaction and the charge accumulation process at the conduction band of the TiO 2 electrodes were simultaneously balanced by the establishment of I 2 ···NH 2 , NH···I − and C = O···Li + bonds at the branches of the confined dendrimers for increasing their global conversion efficiency.

Published

2014

27. A Multicentric Prospective Incidence Study of Guillain-Barré Syndrome in Italy. The ITANG Study

Author

Benedetti, M, Pugliatti, M, Dalessandro, R, BEGHI, ETTORE, Chiò, A, Logroscino, G, Filippini, G, Galeotti, F, Massari, M, Santuccio, C, Raschetti, R, Abruzzi, L, Agazzi, E, Agostoni, E, Ambrogio, L, Amidei, S, Arbasino, C, Argentiero, V, Arnaboldi, M, Baldini, D, Barki, R, Bassi, P, Basso, F, Belcastro, V, Bellotti, M, Bersano, E, Besana, R, Bettoni, L, Bezzi, G, Bianconi, C, Bondavalli, M, Bonometti, A, Borghi, AM, Borsato, C, Bortolotto, S, Bottacchi, EF, Bresolin, N, Bruno, S, Burlina, A, Cafasso, G, Callegarini, C, Calvo, A, Candeloro, E, Casano, A, Cattaneo, SI, Cavallo, R, Cheldi, A, Ciardo, G, Cirignotta, F, Clerici, AM, Clerici, R, Comi, G, Conti, R, Coppo, F, Covelli, V, Crespi, V, Currò Dossi, M, Curtò, NA, D'Adda, E, Dallocchio, C, D'Anna, S, De Massis, P, De Toni Franceschini, L, Di Vito, N, Didonè, G, Dileone, M, Donati, E, Dotta, M, Fazio, R, Federico, F, FERRARESE, CARLO, Ferrazzini, F, Ferrero, B, Filosto, M, Frasson, E, Fusina, S, Galbussera, A, Gastaldo, E, Geda, C, Ghiglione, P, Giometto, B, Gionco, M, Giorgetti, A, Giussani, G, Gobbin, F, Grampa, G, Granieri, E, Greco, G, Guidetti, D, Guidi, C, Guidotti, M, Gusmaroli, G, Imperiale, D, Internò, S, Jann, S, La Spina, I, Leo, A, Leone, M, Leoni, S, Leotta, D, Lerario, R, Liotta, G, Livrea, P, Luda di Cortemiglio, E, Maggio, B, Magni, E, Magnoni, A, Maistrelli, J, Manca, D, Mandrioli, J, Manera, U, Marcello, N, Marchi, P, Marchini, C, Marconi, S, Mattioli, M, Mauro, A, Mazzaglia, G, Medici, D, Meineri, P, Meola, G, Micaglio, G, Michelucci, R, Michieli, G, Micieli, G, Minardi, C, Moglia, C, Monaco, S, Montanari, E, Moretto, G, Munerati, V, Mura, G, Mussutto, V, Nascimbene, C, Neri, W, Nichelli, P, Nobile Orazio, E, Oddenino, E, Onorato, S, Padovani, A, Palermo, M, Papurello, DM, Passarella, B, Pavesi, G, Penza, MT, Perini, M, Perini, F, Perla, F, Perlotto, N, Perrone, P, Pignatta, P, Pisano, F, Poglio, F, Polo, A, Poloni, M, Porazzi, D, Pradotto, L, Previdi, P, Quatrale, R, Rasi, F, Ravasio, A, Ravetti, C, Repaci, M, Riccardi, T, Riguzzi, P, Rinaldi, R, Riva, M, Romeo, V, Romorini, A, Rosso, T, Rotondo, G, Sacquegna, T, Sanson, F, Santamato, V, Santoro, D, Sartori, V, Sasanelli, F, Savio, K, Serena, M, Silani, V, Silvestri, L, Simioni, V, Squintani, GM, Suardelli, M, Tartagla, L, Terenghi, F, Terlizzi, E, Terzano, M, Tesser, F, Testa, L, Ticca, A, Ticozzi, N, Tiriticco, M, Tola, MR, Tonietti, S, Trianni, G, Trojano, M, Trotta, F, Turatti, M, Ursino, E, Vanotti, A, Vercellino, M, Villani, A, Vitelli, E, Zambito Marsala, S, Zanette, G, Zarcone, D, Zimatore, G, Zoccolella, S., Benedetti, Md, Pugliatti, M, D'Alessandro, R, Beghi, E, Chiò, A, Logroscino, G, Filippini, G, Galeotti, F, Massari, M, Santuccio, C, Comi, Giancarlo, Raschetti, R, ITANG Study, Group, Giometto, B, Benedetti, M, Dalessandro, R, Abruzzi, L, Agazzi, E, Agostoni, E, Ambrogio, L, Amidei, S, Arbasino, C, Argentiero, V, Arnaboldi, M, Baldini, D, Barki, R, Bassi, P, Basso, F, Belcastro, V, Bellotti, M, Bersano, E, Besana, R, Bettoni, L, Bezzi, G, Bianconi, C, Bondavalli, M, Bonometti, A, Borghi, A, Borsato, C, Bortolotto, S, Bottacchi, E, Bresolin, N, Bruno, S, Burlina, A, Cafasso, G, Callegarini, C, Calvo, A, Candeloro, E, Casano, A, Cattaneo, S, Cavallo, R, Cheldi, A, Ciardo, G, Cirignotta, F, Clerici, A, Clerici, R, Comi, G, Conti, R, Coppo, F, Covelli, V, Crespi, V, Currò Dossi, M, Curtò, N, D'Adda, E, Dallocchio, C, D'Anna, S, De Massis, P, De Toni Franceschini, L, Di Vito, N, Didonè, G, Dileone, M, Donati, E, Dotta, M, Fazio, R, Federico, F, Ferrarese, C, Ferrazzini, F, Ferrero, B, Filosto, M, Frasson, E, Fusina, S, Galbussera, A, Gastaldo, E, Geda, C, Ghiglione, P, Gionco, M, Giorgetti, A, Giussani, G, Gobbin, F, Grampa, G, Granieri, E, Greco, G, Guidetti, D, Guidi, C, Guidotti, M, Gusmaroli, G, Imperiale, D, Internò, S, Jann, S, La Spina, I, Leo, A, Leone, M, Leoni, S, Leotta, D, Lerario, R, Liotta, G, Livrea, P, Luda di Cortemiglio, E, Maggio, B, Magni, E, Magnoni, A, Maistrelli, J, Manca, D, Mandrioli, J, Manera, U, Marcello, N, Marchi, P, Marchini, C, Marconi, S, Mattioli, M, Mauro, A, Mazzaglia, G, Medici, D, Meineri, P, Meola, G, Micaglio, G, Michelucci, R, Michieli, G, Micieli, G, Minardi, C, Moglia, C, Monaco, S, Montanari, E, Moretto, G, Munerati, V, Mura, G, Mussutto, V, Nascimbene, C, Neri, W, Nichelli, P, Nobile Orazio, E, Oddenino, E, Onorato, S, Padovani, A, Palermo, M, Papurello, D, Passarella, B, Pavesi, G, Penza, M, Perini, M, Perini, F, Perla, F, Perlotto, N, Perrone, P, Pignatta, P, Pisano, F, Poglio, F, Polo, A, Poloni, M, Porazzi, D, Pradotto, L, Previdi, P, Quatrale, R, Rasi, F, Ravasio, A, Ravetti, C, Repaci, M, Riccardi, T, Riguzzi, P, Rinaldi, R, Riva, M, Romeo, V, Romorini, A, Rosso, T, Rotondo, G, Sacquegna, T, Sanson, F, Santamato, V, Santoro, D, Sartori, V, Sasanelli, F, Savio, K, Serena, M, Silani, V, Silvestri, L, Simioni, V, Squintani, G, Suardelli, M, Tartagla, L, Terenghi, F, Terlizzi, E, Terzano, M, Tesser, F, Testa, L, Ticca, A, Ticozzi, N, Tiriticco, M, Tola, M, Tonietti, S, Trianni, G, Trojano, M, Trotta, F, Turatti, M, Ursino, E, Vanotti, A, Vercellino, M, Villani, A, Vitelli, E, Zambito Marsala, S, Zanette, G, Zarcone, D, Zimatore, G, and Zoccolella, S

Subjects

Adult, Male, Pediatrics, medicine.medical_specialty, Epidemiology, Population, Guillain-Barre Syndrome, Rate ratio, NO, Young Adult, Axonal and demyelinating GBS, Guillain-Barré syndrome, Incidence, Prospective study, Trend, Neurology (clinical), Aged, Aged, 80 and over, Female, Humans, Italy, Middle Aged, 80 and over, medicine, Young adult, education, Prospective cohort study, education.field_of_study, Guillain-Barre syndrome, business.industry, Medicine (all), Incidence (epidemiology), medicine.disease, Vaccination, Settore MED/26 - NEUROLOGIA, business, Human

Abstract

Background: To assess Guillain-Barré syndrome (GBS) incidence we relied on the Italian Network for the study of GBS (ITANG) established in 2010 in 7 Italian regions to analyse the association between influenza vaccination and GBS. Methods: All individuals aged ≥18 years, presenting with clinical manifestations that suggested GBS according to the universally accepted Asbury's diagnostic criteria (1990) were prospectively notified to a centralised database by ITANG neurologists over the period October 1, 2010-September 30, 2011. Through a telephone survey, 9 trained interviewers followed up the cases to diagnosis and then for 1 year since hospital discharge. Validation of case reporting was performed with the support of administrative data in 5 regions. Results: We found 365 cases fulfilling the definition for GBS or one of its variants over 19,846,068 population ≥18 years of age, yielding an annual incidence rate of 1.84 per 100,000 (95% CI 1.65-2.03), 2.30 (95% CI 1.99-2.60) in men and 1.41 (95% CI 1.18-1.64) in women. A highly significant peak of incidence was observed in February 2011 as compared to reference month (September 2011, rate ratio 3.3:1, p < 0.01). Conclusions: In Italy, GBS incidence was among the highest reported in Europe and higher than previously observed in Italian studies.

Published

2015

28. Growth dynamics of polyamidoamine dendrimer encapsulated CdS nanoparticles

Author

Francisco Javier Yate Rodríguez, Selene Sepúlveda, Luis A. Godínez, A. Rodríguez, Perla F. Mendez, Erika Bustos, and Juan Manríquez

Subjects

Inorganic Chemistry, Template, Chemical engineering, Average diameter, Chemistry, Diffusion, Dendrimer, Materials Chemistry, Nanoparticle, Organic chemistry, Growth model, Condensed Matter Physics, Nanomaterials

Abstract

A2. Growth models from solutions B1. Nanomaterials B1. Polyamidoamine dendrimers B2. Semiconducting cadmium compounds abstract CdS nanoparticles (CdS-nps) were synthesized employing charged and neutral polyamidoamide (PAMAM) dendrimers (generation G3.5, G4.0 and G4.0-OH with 64 -COO � ,- NH 3 and -OH peripheral groups, respectively) as templates. The morphological characterization of CdS-nps was carried out using TEM measurements that showed spherical nanoparticles characterized by average diameter values between 3.6 and 4.7 nm. Using UV-vis experiments, CdS-nps formation was evaluated using a diffusion controlled growth model where the S 2� diffusion coefficient throughout the external and internal functional groups of dendrimers was found to be an important parameter. In this way, the results indicate that nanoparticle formation is primarily affected by the charged nature of the external functional groups of the dendrimer template.

Published

2012

29. Genetic burden of common variants in progressive and bout-onset multiple sclerosis

Author

SOROSINA M, BRAMBILLA P, CLARELLI F, BARIZZONE N, LUPOLI S, GUASCHINO C, OSICEANU AM, MOIOLA L, GHEZZI A, CONIGLIO G, PATTI F, MANCARDI G, MANUNTA P, GLORIOSO N, GUERINI FR, BERGAMASCHI R, PERLA F, PROGRESSO, PROGEMUS, MARTINELLI V, CUSI D, LEONE M, COMI G, D'ALFONSO S, MARTINELLI BONESCHI F, Among the collaborators, TEDESCHI, Gioacchino, Sorosina, M, Brambilla, P, Clarelli, F, Barizzone, N, Lupoli, S, Guaschino, C, Osiceanu, Am, Moiola, L, Ghezzi, An, Coniglio, G, Patti, F, Mancardi, G, Manunta, P, Glorioso, N, Guerini, Fr, Bergamaschi, R, Perla, F, Martinelli, V, Cusi, D, Leone, M, Comi, G, D’Alfonso, S, MARTINELLI-BONESCHI, F, PROGRESSO STUDY, Group, PROGEMUS STUDY, Group, Ghezzi, A, Progresso, Progemu, D'Alfonso, S, MARTINELLI BONESCHI, F, D'Ambrosio, Alessandro, and Tedeschi, Gioacchino

Subjects

Oncology, Male, Genome-wide association study, Sex Factor, Disease, Heritability, Multiple sclerosis, Primary progressive, Relapsing-remitting, Adolescent, Adult, Aged, Aged, 80 and over, Female, Genetic Markers, Genetic Predisposition to Disease, Genome-Wide Association Study, Humans, Italy, Magnetic Resonance Imaging, Middle Aged, Multiple Sclerosis, Chronic Progressive, Phenotype, Risk Factors, Sex Factors, Young Adult, Polymorphism, Single Nucleotide, Neurology, Neurology (clinical), Genetic Marker, 80 and over, Genetic risk, Genetics, Multiple Sclerosis, Chronic Progressive, Explained variation, Human, medicine.medical_specialty, Single-nucleotide polymorphism, Polymorphism, Single Nucleotide, Internal medicine, medicine, Multiple sclerosi, business.industry, Risk Factor, medicine.disease, business

Abstract

Background: The contribution of genetic variants underlying the susceptibility to different clinical courses of multiple sclerosis (MS) is still unclear. Objective: The aim of the study is to evaluate and compare the proportion of liability explained by common SNPs and the genetic burden of MS-associated SNPs in progressive onset (PrMS) and bout-onset (BOMS) cases. Methods: We estimated the proportion of variance in disease liability explained by 296,391 autosomal SNPs in cohorts of Italian PrMS and BOMS patients using the genome-wide complex trait analysis (GCTA) tool, and we calculated a weighted genetic risk score (wGRS) based on the known MS-associated loci. Results: Our results identified that common SNPs explain a greater proportion of phenotypic variance in BOMS (36.5%±10.1%) than PrMS (20.8%±6.0%) cases, and a trend of decrease was observed when testing primary progressive (PPMS) without brain MRI inflammatory activity ( p = 7.9 × 10−3). Similarly, the wGRS and the variance explained by MS-associated SNPs were higher in BOMS than PPMS in males (wGRS: 6.63 vs 6.51, p = 0.04; explained variance: 4.8%±1.5% vs 1.7%±0.6%; p = 0.05). Conclusions: Our results suggest that the liability of disease is better captured by common genetic variants in BOMS than PrMS cases. The absence of inflammatory activity and male gender further raise the difference between clinical courses.

Published

2014

30. A 12-month prospective, observational study evaluating the impact of disease-modifying treatment on emotional burden in recently-diagnosed multiple sclerosis patients: The POSIDONIA study

Author

Montanari, E., Rottoli, M., Maimone, D., Confalonieri, P., Plewnia, K., Frigo, M., Francia, A., Pala, A., Losignore, N. A., Ragonese, P., Veneziano, A., Traccis, S., Bosco, G., Dotta, M., Severi, S., Ragno, M., Candeago, R. M., Feleppa, M., Stecchi, S., Bosco, D., Tola, M. R., Massacesi, Luca, Costantino, G., Solaro, C. M., Serrati, C., Totaro, R., Coniglio, M. G., Scarpini, E., Zuliani, C., Perla, F., Ticca, A., Cottone, S., Iudice, A., Koudriavteva, T., Di Battista, G., Gasperini, C., Perin, C., Meola, G., Pugliatti, M., Bandini, F., Cavalla, P., Posteraro, F., Consoli, D., Montanari E, Rottoli M, Maimone D, Confalonieri P, Plewnia K, Frigo M, Francia A, Pala A, Losignore NA, Ragonese P, Veneziano A, and POSIDONIA study group

Subjects

Male, Psychometrics, Anxiety, Hospital Anxiety and Depression Scale, 0302 clinical medicine, Immunologic Factor, Multiple sclerosis, Disease-modifying treatment, Emotional burden, Anxiety, Depression, Multiple Sclerosi, Disease-modifying treatment, 030212 general & internal medicine, Prospective Studies, Prospective cohort study, Depression (differential diagnoses), Depression, Middle Aged, Psychiatric Status Rating Scale, Treatment Outcome, Italy, Neurology, Female, Settore MED/26 - Neurologia, medicine.symptom, Psychology, Psychometric, Human, Adult, medicine.medical_specialty, Multiple Sclerosis, Mood Disorder, Adolescent, Logistic Model, 03 medical and health sciences, Young Adult, Rating scale, medicine, Humans, Immunologic Factors, Aged, Psychiatric Status Rating Scales, Mood Disorders, medicine.disease, Prospective Studie, Logistic Models, Mood disorders, Physical therapy, Emotional burden, Observational study, Neurology (clinical), 030217 neurology & neurosurgery

Abstract

Introduction Depression and anxiety are common among patients with multiple sclerosis (MS) and are frequently present at the time of MS diagnosis. Methods POSIDONIA was a 12-month, observational, prospective study conducted in Italy to evaluate the impact of disease-modifying treatment (DMT) on emotional burden in patients with recently-diagnosed MS. The Hospital Anxiety and Depression Scale (HADS), specifically HADS anxiety (HADS-A) and depression (HADS-D) subscale scores, the Short-Form 36 Health Survey (SF-36) and the Impact of Event Scale – Revised (IES-R) were used to measure patient-reported outcomes. The Hamilton Depression Rating Scale (HDRS), HDRS-17, was used as a measure of healthcare provider-reported outcomes. The primary study outcome was change from baseline in feelings of anxiety and depression over 12 months (via HADS). Results Of 250 enrolled patients, 222 (88.8%) completed the study. At baseline, mean HADS total, HADS-A and HADS-D subscale scores were within the normal range. There were no significant changes over time in mean HADS total and HADS-A and HADS-D subscale scores, although the subgroup of patients with baseline scores indicative of anxiety or depression tended to improve over time. Both the HDRS and IES-R total scores improved over time, but there were no statistically significant changes in SF-36. Conclusion In the patient population of the POSIDONIA study depression and anxiety were present in a minority of patients thus not allowing to detect the impact of starting DMT. However DMT appears to have a positive effect in patients with measurable anxiety or depression at baseline.

Published

2016

31. Is it possible a new definition of metabolic syndrome in childhood?

Author

Martino, F., Pannarale, G., Puddu, P. E., Colantoni, C., Zanoni, C., Martino, E., Torromeo, C., Paravati, V., Perla, F. M., and Francesco BARILLA'

Subjects

Male, Metabolic Syndrome, Adolescent, Cholesterol, HDL, Alanine Transaminase, Blood Pressure, tg/hdl ratio, age 6-14 years, Settore MED/11, Cross-Sectional Studies, Italy, metabolic syndrome, quantile distributions, risk factors, Non-alcoholic Fatty Liver Disease, Risk Factors, Humans, Female, Insulin Resistance, Child, Triglycerides

Abstract

To investigate whether a group of Italian children and adolescents who were diagnosed to have metabolic syndrome (MS) according to a new ethnic age and gender specific definition had, in comparison with a control group, other signs and metabolic risk factors which are commonly associated with MS.The cross-sectional study population included 300 subjects (51% boys, age range 6-14 years), who were divided into 2 groups according to the presence of MS, diagnosed on the basis of 3/5 factors derived from the age and gender specific quantile distribution of MS components in a large regional Italian population survey (Calabrian Sierras Community Study, CSCS). In all subjects the following data were collected: anthropometric measures, blood pressure, liver function, C-reactive protein (hsCRP), uric acid blood levels, lipid and glucose profile. Triglycerides/HDL-cholesterol (TG/HDL-C) ratio was calculated.There were 38 subjects (13%) with MS, who had higher indices of growth and fat distribution and higher blood levels of uric acid, alanine aminotransferase and gamma-glutamyltransferase. TG/HDL ratio was higher (median 3.11 vs. 1.14, p = 0.00001) in MS subjects who had lower apolipoprotein A and higher apolipoprotein B and non-HDL-C levels. hsCRP was not different between groups.Our ethnic age and gender specific definition of MS in Italian children and adolescents was able to identify in a youth group different cardiometabolic risk factors related to insulin resistance, endothelial damage and nonalcoholic fatty liver disease, which are commonly associated with MS diagnosis.

Published

2015

32. Sexual transmission of American trypanosomiasis in humans: a new potential pandemic route for Chagas parasites

Author

Araujo, Perla F, primary, Almeida, Adriana B, additional, Pimentel, Carlos F, additional, Silva, Adriano R, additional, Sousa, Alessandro, additional, Valente, Sebastião A, additional, Valente, Vera C, additional, Britto, Manuela M, additional, Rosa, Ana C, additional, Alves, Rozeneide M, additional, Hagström, Luciana, additional, and Teixeira, Antonio RL, additional

Published

2017

33. Stock price forecasting with an hybrid model

Author

Corsaro, S., primary, De Angelis, P.L., additional, Marino, Z., additional, Perla, F., additional, Zanetti, P., additional, and Fiore, U., additional

Published

2017

34. First on-line survey of an international multidisciplinary working group (MightyMedic) on current practice in diagnosis, therapy and follow-up of dyslipidemias

Author

Stefanutti, C, D'Alessandri, G, Petta, A, Harada-Shiba, M, Julius, U, Soran, H, Moriarty, P. M, Romeo, S, Drogari, E, Jaeger, B. R, Bianciardi, G, Bosco, G, Cossu, M, De Fusco, G, Di Giacomo, S, Ewald, N, Gualdi, G, Lanti, A, Marson, P, Martino, F, Migliori, G, Parasassi, T, Pavan, A, Perla, F. M, Perrone, G, Pisciotta, L, Renga, S, Ries, W, and Romano, N

Subjects

medicine.medical_specialty, Time Factors, International Cooperation, Practice Patterns, Coronary artery disease, Dyslipidemia, Lipoprotein apheresis, Multicenter study, Survey, Biomarkers, Blood Component Removal, Cardiovascular Diseases, Cooperative Behavior, Dyslipidemias, Guideline Adherence, Health Care Surveys, Humans, Hypolipidemic Agents, Lipids, Molecular Diagnostic Techniques, Practice Guidelines as Topic, Practice Patterns, Physicians', Predictive Value of Tests, Risk Factors, Surveys and Questionnaires, Treatment Outcome, Internet, Internal Medicine, Cardiology and Cardiovascular Medicine, Multidisciplinary approach, medicine, Parallel field, Therapeutic apheresis, Physicians', business.industry, General Medicine, medicine.disease, Clinical trial, Current practice, Family medicine, Physical therapy, business

Abstract

The MightyMedic (Multidisciplinary International Group for Hemapheresis TherapY and MEtabolic DIsturbances Contrast) Working Group has been founded in 2013. The leading idea was to establish an international network of interdisciplinary nature aimed at working to cross national borders research projects, clinical trials, educational initiatives (meetings, workshops, summer schools) in the field of metabolic diseases, namely hyperlipidemias, and diabetes, preventive cardiology, and atherosclerosis. Therapeutic apheresis, its indications and techniques, is a parallel field of investigation. The first on-line survey of the Group has been completed in the first half of 2014. The survey included # 24 Centers in Italy, Germany, Greece, UK, Sweden, Japan and USA. Relevant data have been collected on current practice in diagnosis, therapy and follow-up of dyslipidemias. 240 subjects with hyperlipidemia and treated with lipoprotein apheresis have been reported in the survey, but a large percentage of patients (35%) who could benefit from this therapeutic option are still treated by conventional drug approach. Genetic molecular diagnosis is performed in only 33% of patients while Lipoprotein(a) (Lp(a)) is included in cardiovascular disease risk assessment in 71% of participating Centers. New detailed investigations and prospective multicenter studies are needed to evaluate changes induced by the impact of updated indications and strategies, as well as new treatment options, targeting standardization of therapeutic and diagnostic approaches. (C) 2015 Elsevier Ireland Ltd. All rights reserved.

Published

2015

35. PbS quantum dots as additives in methylammonium halide perovskite solar cells: the effect of quantum dot capping.

Author

Thi Tuyen Ngo, Masi, Sofia, Mendez, Perla F., Kazes, Miri, Oron, Dan, and Seró, Iván Mora

Published

2019

36. Euro-Par 2010 Parallel Processing Workshops

Author

Alexander M, Cannataro M, Danelutto M, Hast A, Guarracino M, Knupfer A, Perla F, Trae J. L, Vivien F., DI MARTINO, Beniamino, Alexander, M, Cannataro, M, Danelutto, M, DI MARTINO, Beniamino, Hast, A, Guarracino, M, Knupfer, A, Perla, F, Trae J., L, and Vivien, F.

Published

2011

37. Neutralizing antibodies in multiple sclerosis patients treated with 375 microg interferon-beta-1b

Author

Durelli, L, Ricci, A, Barbero, P, Cucci, A, Ferrero, B, Festa, E, Contessa, G, De Mercanti, S, Ripellino, P, Lapuma, D, Viglietta, E, Ferrero, C, Bergui, M, Versino, E, Clerico, M, Rottoli, M, Moroni, S, Teatini, F, Schoenhuber, R, Spissu, A, Reggio, A, Lo Fermo S, Liberto, A, Perla, F, Grasso, E, Montanari, E, Pesci, I, Manneschi, L, Grezzi, A, Zaffaroni, M, Carolei, A, Totaro, R, Giuliani, G, Pucci, E, Cartechini, E, Scarpini, E, Clerici, R, Protti, A, Erminio, C, Cotrufo, R, Lus, G, Bergamaschi, R, Romani, A, Iudice, A, Frittelli, C, Motti, L, Marcello, N, Meola, G, Robotti, M, Cavallo, R, Ravetti, C, Deotto, L., SAVETTIERI, Giovanni, SALEMI, Giuseppe, Durelli, L, Ricci, A, Barbero, P, Cucci, A, Ferrero, B, Festa, E, Contessa, G, De Mercanti, S, Ripellino, P, Lapuma, D, Viglietta, E, Ferrero, C, Bergui, M, Versino, E, Clerico, M, Rottoli, M, Moroni, S, Teatini, F, Schoenhuber, R, Spissu, A, Reggio, A, Lo Fermo S, Liberto, A, Perla, F, Grasso, E, Montanari, E, Pesci, I, Manneschi, L, Grezzi, A, Zaffaroni, M, Carolei, A, Totaro, R, Giuliani, G, Pucci, E, Cartechini, E, Scarpini, E, Clerici, R, Protti, A, Erminio, C, Cotrufo, R, Lus, G, Savettieri, G, Salemi, G, Bergamaschi, R, Romani, A, Iudice, A, Frittelli, C, Motti, L, Marcello, N, Meola, G, Robotti, M, Cavallo, R, Ravetti, C, and Deotto, L

Subjects

Multiple sclerosis, interferon-beta-1b, Settore MED/26 - Neurologia

Published

2009

38. THE OPTIMIZATION OF INTERFERON FOR MS STUDY: 375 MICROG INTERFERON BETA-1B IN SUBOPTIMAL RESPONDERS

Author

Durelli L, Barbero P, Verdun E, Ferrero B, Clerico M, Ricci A, Cucci A, Contessa G, Rivoiro C, Ferrero C, Picco E, Ripellino P, Viglietti D, Bergui M, Zhong JJ, Versino E, Rottoli M, Moroni S, Teatini F, Schoenhuber R, Spissu A, Reggio A, Lo Fermo S, Liberto A, Perla F, Grasso E, Montanari E, Pesci I, Manneschi L, Ghezzi A, Zaffaroni M, Carolei A, Totaro R, Giuliani G, Pucci E, Cartechini E, Scarpini E, Clerici R, Protti A, Erminio C, Cotrufo R, Lus G, Bergamaschi R, Romani A, Bassano MA, Policreti A, Iudice A, Frittelli C, Motti L, Marcello N, Meola G, Robotti M, Cavallo R, Ravetti C, Deotto K., SAVETTIERI, Giovanni, SALEMI, Giuseppe, Durelli L, Barbero P, Verdun E, Ferrero B, Clerico M, Ricci A, Cucci A, Contessa G, Rivoiro C, Ferrero C, Picco E, Ripellino P, Viglietti D, Bergui M, Zhong JJ, Versino E, Rottoli M, Moroni S, Teatini F, Schoenhuber R, Spissu A, Reggio A, Lo Fermo S, Liberto A, Perla F, Grasso E, Montanari E, Pesci I, Manneschi L, Ghezzi A, Zaffaroni M, Carolei A, Totaro R, Giuliani G, Pucci E, Cartechini E, Scarpini E, Clerici R, Protti A, Erminio C, Cotrufo R, Lus G, Savettieri G, Salemi G, Bergamaschi R, Romani A, Bassano MA, Policreti A, Iudice A, Frittelli C, Motti L, Marcello N, Meola G, Robotti M, Cavallo R, Ravetti C, and Deotto K

Subjects

Adult, medicine.medical_specialty, Time Factors, Adolescent, Injections, Subcutaneous, suboptimal treatment response, Gastroenterology, Drug Administration Schedule, law.invention, Young Adult, Multiple Sclerosis, Relapsing-Remitting, Adjuvants, Immunologic, Randomized controlled trial, law, Internal medicine, medicine, Humans, Single-Blind Method, Prospective Studies, Adverse effect, Prospective cohort study, interferon beta (IFNβ), immunomodulatory drug, Subclinical infection, Dose-Response Relationship, Drug, business.industry, Interferon beta-1b, Interferon-beta, Middle Aged, Magnetic Resonance Imaging, Confidence interval, Surgery, Clinical trial, Treatment Outcome, Neurology, Relative risk, multiple sclerosi, MRI activity, Settore MED/26 - Neurologia, Neurology (clinical), business, Follow-Up Studies

Abstract

We aimed to evaluate the safety and MRI efficacy of interferon beta-1b (IFNbeta-1b) 375 microg (subcutaneously [sc] every other day [eod]) in relapsing-remitting multiple sclerosis (RRMS) patients with a suboptimal response to IFNbeta-1b 250 microg, i.e., with MRI activity or relapses. The OPTimization of Interferon for MS (OPTIMS) study was a prospective multicenter randomized phase 2 trial comprising a 6-month run-in phase (to identify suboptimal responders) and a 6-month randomized phase of open-label clinical and blinded MRI follow-up. During run-in all patients were treated with IFNbeta-1b 250 microg sc eod; during the study phase suboptimal treatment responders were randomized either to IFNbeta-1b 250 or 375 microg sc eod. Primary outcome was the proportion of patients without MRI activity during study Months 9-12 according to the intention-to-treat principle. 216 RRMS patients entered the study: 83 suboptimal responders were identified and randomized, 7 refused to continue treatment, 76 were included in the analysis. More patients treated with 375 microg had no MRI activity at Months 9-12 (30/36 vs.16/40; relative risk, 0.28; 95 % confidence interval, 0.08-0.47; p = 0.0001). Sensitivity analysis ("worst case scenario") confirmed the results. No new or unexpected adverse events were observed, but there was a trend towards more withdrawals in the 375 microg group. Increasing the dose of IFNbeta-1b from 250 microg to 375 microg is a successful strategy for reducing subclinical signs of disease activity in RRMS patients. Further studies are needed to show whether this dose may also improve clinical efficacy.

Published

2008

39. MRI activity and neutralising antibody as predictors of response to interferon beta treatment in multiple sclerosis

Author

DURELLI L, BARBERO P, BERGUI M, VERSINO E, BASSANO MA, VERDUN E, RIVOIRO C, FERRERO C, PICCO E, RIPELLINO P, GIULIANI G, MONTANARI E, CLERICO M, ITALIAN MULTIPLE SCLEROSIS STUDY GROUP DURELLI L, FERRERO B, PIPIERI A, RICCI A, CUCCI A, FESTA E, ROVERA A, TAVELLA A, CONTESSA G, DELFICO L, ZHONG JJ, ROTTOLI M, MORONI S, TEATINI F, SCHOENHUBER R, SPISSU A, REGGIO A, LO FERMO S, LIBERTO A, PERLA F, GRASSO E, PESCI I, MANNESCHI L, GHEZZI A, ZAFFARONI M, CAROLEI A, TOTARO R, PUCCI, Enzo, CARTECHINI E, SCARPINI E, CLERICI R, PROTTI A, ERMINIO C, COTRUFO R, LUS G, SAVETTIERI, Giovanni, SALEMI, Giuseppe, BERGAMASCHI R, ROMANI A, POLICRETI A, IUDICE A, FRITTELLI C, MOTTI L, MARCELLO N, MEOLA G, ROBOTTI M, CAVALLO R, RAVETTI C, DEOTTO L., DURELLI L, BARBERO P, BERGUI M, VERSINO E, BASSANO MA, VERDUN E, RIVOIRO C, FERRERO C, PICCO E, RIPELLINO P, GIULIANI G, MONTANARI E, CLERICO M, ITALIAN MULTIPLE SCLEROSIS STUDY GROUP DURELLI L, FERRERO B, PIPIERI A, RICCI A, CUCCI A, FESTA E, ROVERA A, TAVELLA A, CONTESSA G, DELFICO L, ZHONG JJ, ROTTOLI M, MORONI S, TEATINI F, SCHOENHUBER R, SPISSU A, REGGIO A, LO FERMO S, LIBERTO A, PERLA F, GRASSO E, PESCI I, MANNESCHI L, GHEZZI A, ZAFFARONI M, CAROLEI A, TOTARO R, PUCCI E, CARTECHINI E, SCARPINI E, CLERICI R, PROTTI A, ERMINIO C, COTRUFO R, LUS G, SAVETTIERI G, SALEMI G, BERGAMASCHI R, ROMANI A, POLICRETI A, IUDICE A, FRITTELLI C, MOTTI L, MARCELLO N, MEOLA G, ROBOTTI M, CAVALLO R, RAVETTI C, and DEOTTO L

Subjects

Male, Neutralising antibody, MULTICENTER, PLACEBO-CONTROLLED TRIAL, GUIDELINES, Gastroenterology, DOUBLE-BLIND, Interferon β, MAGNETIC-RESONANCE, Prospective Studies, Neurologic Examination, biology, Brain, IMPAIRMENT, Middle Aged, Predictive value, Magnetic Resonance Imaging, Recombinant Proteins, Psychiatry and Mental health, Treatment Outcome, Settore MED/26 - Neurologia, Female, Antibody, Interferon beta-1b, Adult, medicine.medical_specialty, DIAGNOSTIC-CRITERIA, Injections, Subcutaneous, Antibodies, Drug Administration Schedule, Disease activity, Multiple Sclerosis, Relapsing-Remitting, Adjuvants, Immunologic, Neutralization Tests, Internal medicine, medicine, Humans, Interferon beta, business.industry, Multiple sclerosis, DISABILITY, MS, Interferon-beta, medicine.disease, Confidence interval, Surgery, biology.protein, Neurology (clinical), business, Follow-Up Studies

Abstract

Objective: To prospectively validate MRI activity and neutralising anti-interferon antibody (NAb) during the first 6 months of interferon β treatment as response indicators in multiple sclerosis (MS). Methods: Patients with relapsing–remitting MS were followed during the first 2 years of treatment. Neurological assessments were performed every 3 months or when a relapse was suspected. MRI scans performed at baseline and at 3, 4, 5 and 6 months after the start of treatment were assessed centrally for disease activity: new T2 or gadolinium enhancing T1 lesions. NAb were assessed using the MxA protein assay; positivity was defined as two consecutive titres ⩾20 NU/ml. We evaluated the predictivity of an active scan, NAb positivity, or both, during the first 6 months of treatment, on the occurrence of clinical disease activity in the following 18 months. Results: 147 patients were assessed at 16 centres. Predictivity parameters (with confidence intervals) were as follows: active scan, sensitivity (SN) 52% (34–69%), specificity (SP) 80% (65–91%), negative predictive value (NPV) 73% (58–77%), positive predictive value (PPV) 62% (42–79%), p = 0.002; NAb positivity, SN 71% (45–88%), SP 66% (55–76%), NPV 92% (82–97%), PPV 29% (16–45%), p = 0.01; active scan and NAb positivity, SN 71% (38–91%), SP 86% (73–94%), NPV 94% (86–98%), PPV 50% (29–70%), p = 0.0003. Conclusions: MRI activity and NAb occurrence during the first 6 months of interferon β treatment were reliable predictors of long term clinical response, particularly when combined. Patients with negative predictors showed a less than 10% risk of developing clinical activity. Patients with positive predictors showed a 50% risk of further clinical activity. These patients need to be followed carefully with further MRI and NAb tests.

Published

2008

40. Epidemiology and control of schistosomiasis in the Philippines: progress report as of 1987

Author

Bayani L. Blas, Perla F. Velasco, Ofélia B. Aliaiy, Edgardo S. Erce, José C. Basas, and Edgardo S. Bautista

Subjects

Microbiology, QR1-502, Infectious and parasitic diseases, RC109-216

Published

1989

41. A Multicentric Prospective Incidence Study of Guillain-Barre Syndrome in Italy. the ITANG Study

Author

Benedetti, M. D., Pugliatti, M., Dalessandro, R., Beghi, E., Chio, A., Logroscino, G., Filippini, G., Galeotti, F., Massari, M., Santuccio, C., Raschetti R., Abruzzi L, Agazzi, E, Agostoni, E, Ambrogio, L, Amidei, S, Arbasino, C, Argentiero, V, Arnaboldi, M, Baldini, D, Barki, R, Bassi, P, Basso, F, Belcastro, V, Bellotti, M, Bersano, E, Besana, R, Bettoni, L, Bezzi, G, Bianconi, C, Bondavalli, M, Bonometti, A, Borghi, Am, Borsato, C, Bortolotto, S, Bottacchi, Ef, Bresolin, N, Bruno, S, Burlina, A, Cafasso, G, Callegarini, C, Calvo, A, Candeloro, E, Casano, A, Cattaneo, Si, Cavallo, R, Cheldi, A, Ciardo, G, Cirignotta, F, Clerici, Am, Clerici, R, Comi, G, Conti, R, Coppo, F, Covelli, V, Crespi, V, Currò Dossi, M, Curtò, Na, D'Adda, E, Dallocchio, C, D'Anna, S, De Massis, P, De Toni Franceschini, L, Di Vito, N, Didonè, G, Dileone, M, Donati, E, Dotta, M, Fazio, R, Federico, F, Ferrarese, C, Ferrazzini, F, Ferrero, B, Filosto, M, Frasson, E, Fusina, S, Galbussera, A, Gastaldo, E, Geda, C, Ghiglione, P, Giometto, B, Gionco, M, Giorgetti, A, Giussani, G, Gobbin, F, Grampa, G, Granieri, E, Greco, G, Guidetti, D, Guidi, C, Guidotti, M, Gusmaroli, G, Imperiale, D, Internò, S, Jann, S, La Spina, I, Leo, A, Leone, M, Leoni, S, Leotta, D, Lerario, R, Liotta, G, Livrea, P, Luda di Cortemiglio, E, Maggio, B, Magni, Eugenio, Magnoni, A, Maistrelli, J, Manca, D, Mandrioli, J, Manera, U, Marcello, N, Marchi, P, Marchini, C, Marconi, S, Mattioli, M, Mauro, A, Mazzaglia, G, Medici, D, Meineri, P, Meola, G, Micaglio, G, Michelucci, R, Michieli, G, Micieli, G, Minardi, C, Moglia, C, Monaco, S, Montanari, E, Moretto, G, Munerati, V, Mura, G, Mussutto, V, Nascimbene, C, Neri, W, Nichelli, P, Nobile-Orazio, E, Oddenino, E, Onorato, S, Padovani, A, Palermo, M, Papurello, Dm, Passarella, B, Pavesi, G, Penza, Mt, Perini, M, Perini, F, Perla, F, Perlotto, N, Perrone, P, Pignatta, P, Pisano, F, Poglio, F, Polo, A, Poloni, M, Porazzi, D, Pradotto, L, Previdi, P, Quatrale, R, Rasi, F, Ravasio, A, Ravetti, C, Repaci, M, Riccardi, T, Riguzzi, P, Rinaldi, R, Riva, M, Romeo, V, Romorini, A, Rosso, T, Rotondo, G, Sacquegna, T, Sanson, F, Santamato, V, Santoro, D, Sartori, V, Sasanelli, F, Savio, K, Serena, M, Silani, V, Silvestri, L, Simioni, V, Squintani, Gm, Suardelli, M, Tartagla, L, Terenghi, F, Terlizzi, E, Terzano, Mg, Tesser, F, Testa, L, Ticca, A, Ticozzi, N, Tiriticco, M, Tola, Mr, Tonietti, S, Trianni, G, Trojano, M, Trotta, F, Turatti, M, Ursino, E, Vanotti, A, Vercellino, M, Villani, A, Vitelli, E, Zambito Marsala, S, Zanette, G, Zarcone, D, Zimatore, G, Zoccolella, S., Magni E (ORCID:0000-0002-2235-2280), Benedetti, M. D., Pugliatti, M., Dalessandro, R., Beghi, E., Chio, A., Logroscino, G., Filippini, G., Galeotti, F., Massari, M., Santuccio, C., Raschetti R., Abruzzi L, Agazzi, E, Agostoni, E, Ambrogio, L, Amidei, S, Arbasino, C, Argentiero, V, Arnaboldi, M, Baldini, D, Barki, R, Bassi, P, Basso, F, Belcastro, V, Bellotti, M, Bersano, E, Besana, R, Bettoni, L, Bezzi, G, Bianconi, C, Bondavalli, M, Bonometti, A, Borghi, Am, Borsato, C, Bortolotto, S, Bottacchi, Ef, Bresolin, N, Bruno, S, Burlina, A, Cafasso, G, Callegarini, C, Calvo, A, Candeloro, E, Casano, A, Cattaneo, Si, Cavallo, R, Cheldi, A, Ciardo, G, Cirignotta, F, Clerici, Am, Clerici, R, Comi, G, Conti, R, Coppo, F, Covelli, V, Crespi, V, Currò Dossi, M, Curtò, Na, D'Adda, E, Dallocchio, C, D'Anna, S, De Massis, P, De Toni Franceschini, L, Di Vito, N, Didonè, G, Dileone, M, Donati, E, Dotta, M, Fazio, R, Federico, F, Ferrarese, C, Ferrazzini, F, Ferrero, B, Filosto, M, Frasson, E, Fusina, S, Galbussera, A, Gastaldo, E, Geda, C, Ghiglione, P, Giometto, B, Gionco, M, Giorgetti, A, Giussani, G, Gobbin, F, Grampa, G, Granieri, E, Greco, G, Guidetti, D, Guidi, C, Guidotti, M, Gusmaroli, G, Imperiale, D, Internò, S, Jann, S, La Spina, I, Leo, A, Leone, M, Leoni, S, Leotta, D, Lerario, R, Liotta, G, Livrea, P, Luda di Cortemiglio, E, Maggio, B, Magni, Eugenio, Magnoni, A, Maistrelli, J, Manca, D, Mandrioli, J, Manera, U, Marcello, N, Marchi, P, Marchini, C, Marconi, S, Mattioli, M, Mauro, A, Mazzaglia, G, Medici, D, Meineri, P, Meola, G, Micaglio, G, Michelucci, R, Michieli, G, Micieli, G, Minardi, C, Moglia, C, Monaco, S, Montanari, E, Moretto, G, Munerati, V, Mura, G, Mussutto, V, Nascimbene, C, Neri, W, Nichelli, P, Nobile-Orazio, E, Oddenino, E, Onorato, S, Padovani, A, Palermo, M, Papurello, Dm, Passarella, B, Pavesi, G, Penza, Mt, Perini, M, Perini, F, Perla, F, Perlotto, N, Perrone, P, Pignatta, P, Pisano, F, Poglio, F, Polo, A, Poloni, M, Porazzi, D, Pradotto, L, Previdi, P, Quatrale, R, Rasi, F, Ravasio, A, Ravetti, C, Repaci, M, Riccardi, T, Riguzzi, P, Rinaldi, R, Riva, M, Romeo, V, Romorini, A, Rosso, T, Rotondo, G, Sacquegna, T, Sanson, F, Santamato, V, Santoro, D, Sartori, V, Sasanelli, F, Savio, K, Serena, M, Silani, V, Silvestri, L, Simioni, V, Squintani, Gm, Suardelli, M, Tartagla, L, Terenghi, F, Terlizzi, E, Terzano, Mg, Tesser, F, Testa, L, Ticca, A, Ticozzi, N, Tiriticco, M, Tola, Mr, Tonietti, S, Trianni, G, Trojano, M, Trotta, F, Turatti, M, Ursino, E, Vanotti, A, Vercellino, M, Villani, A, Vitelli, E, Zambito Marsala, S, Zanette, G, Zarcone, D, Zimatore, G, Zoccolella, S., and Magni E (ORCID:0000-0002-2235-2280)

Abstract

To assess Guillain-Barre syndrome (GBS) incidence we relied on the Italian Network for the study of GBS (ITANG) established in 2010 in 7 Italian regions to analyse the association between influenza vaccination and GBS. Methods: All individuals aged ≥18 years, presenting with clinical manifestations that suggested GBS according to the universally accepted Asbury's diagnostic criteria (1990) were prospectively notified to a centralised database by ITANG neurologists over the period October 1, 2010-September 30, 2011. Through a telephone survey, 9 trained interviewers followed up the cases to diagnosis and then for 1 year since hospital discharge. Validation of case reporting was performed with the support of administrative data in 5 regions. Results: We found 365 cases fulfilling the definition for GBS or one of its variants over 19,846,068 population ≥18 years of age, yielding an annual incidence rate of 1.84 per 100,000 (95% CI 1.65-2.03), 2.30 (95% CI 1.99-2.60) in men and 1.41 (95% CI 1.18-1.64) in women. A highly significant peak of incidence was observed in February 2011 as compared to reference month (September 2011, rate ratio 3.3:1, p < 0.01). Conclusions: In Italy, GBS incidence was among the highest reported in Europe and higher than previously observed in Italian studies.

Published

2015

42. Sexual transmission of American trypanosomiasis in humans: a new potential pandemic route for Chagas parasites

Author

Perla F Araujo, Adriana B Almeida, Carlos F Pimentel, Adriano R Silva, Alessandro Sousa, Sebastião A Valente, Vera C Valente, Manuela M Britto, Ana C Rosa, Rozeneide M Alves, Luciana Hagström, and Antonio RL Teixeira

Subjects

Amazon, Trypanosoma cruzi, Chagas disease, family study, humans, epidemiology, Microbiology, QR1-502, Infectious and parasitic diseases, RC109-216

Abstract

BACKGROUND The Trypanosoma cruzi infection endemic in Latin America has now spread to several countries across four continents; this endemic involves triatomine vector-free protists. We hypothesised that the sexual transmission of T. cruzi contributes to the ongoing spread of Chagas disease. OBJECTIVES A short-term longitudinal study was conducted to evaluate this hypothesis. METHODS The study population comprised 109 subjects from four families, among whom 21 had been diagnosed with acute Chagas disease by direct parasitological analysis. Blood mononuclear cells and serum samples were obtained from each study subject once per year for three consecutive years. Enzyme-linked immunosorbent assay (ELISA) and indirect immunofluorescence serological examinations were used to detect specific T. cruzi antibodies. Polymerase chain reaction of T. cruzi DNA revealed 188-nucleotide bands, which hybridised to a specific radiolabelled probe and were confirmed by cloning and sequencing. RESULTS Three independent assessments at different time points revealed T. cruzi nuclear DNA footprints in 76% (83/109) of the study population with active infection. In contrast, the ELISA and indirect immunofluorescence assays detected the T. cruzi antibody in 28.4% (31/109) of the study samples. Moreover, the semen from 82.6% (19/23) of subjects people revealed harboured the 188- bp base pair T. cruzi footprint. Interestingly, the ejaculates of nuclear DNA-positive Chagas patient transmitted the T. cruzi upon peritoneal injection or infusion in the vagina of mice, and amastigotes were detected in the skeletal muscle, myocardium, vas deferens, and uterine tube. MAIN CONCLUSIONS T. cruzi infections can be transmitted from females or males to naïve mates through intercourse, and progeny showed discrepancies between the ratios of nuclear DNA footprints and specific antibody that can be explained by the tolerance attained during early embryo growth. Additional studies are needed to develop drugs to eradicate the infections. Additionally, the importance of a vigorous education, information, and communication program to prevent sexually transmitted Chagas disease in humans cannot be underemphasised.

43. Genetic burden of common variants in progressive and bout-onset multiple sclerosis

Author

Sorosina, M, Brambilla, P, Clarelli, F, Barizzone, N, Lupoli, S, Guaschino, C, Osiceanu, Am, Moiola, L, Ghezzi, A, Coniglio, G, Patti, F, Mancardi, G, Manunta, P, Glorioso, N, Guerini, Fr, Bergamaschi, R, Perla, F, Martinelli, V, Cusi, D, Leone, M, Comi, G, D'Alfonso, S, Martinelli Boneschi, F. F., Liberatore, G, Rodegher, M, Rossi, P, Radaelli, M, Colombo, B, Annovazzi, P, Capra, R, Amato, Mp, Nacmias, B, D'Ambrosio, A, Tedeschi, G, Cavalla, P, D'Amico, E, Galimberti, D, Scarpini, E, Atzori, M, Gallo, Paolo, Bucello, S, Grimaldi, L, Capello, E, Naldi, P, Di Sapio, A, Caputo, D, Rosso, G, Cordera, S, Cavallo, R, Benedetti, D, and Salvetti, M.

Published

2013

44. Actor-driven workflow execution in distributed environments

Author

Berretz, F., Skorupa, S., Sander, V., Belloum, A., Bubak, M., Guarracino, M.R., Vivien, F., Larsson Träff, J., Cannataro, M., Danelutto, M., Hast, A., Perla, F., Knüpfer, A., Di Martino, B., Alexander, M., Computational Science Lab (IVI, FNWI), and System and Network Engineering (IVI, FNWI)

Subjects

Service (systems architecture), Computer science, business.industry, media_common.quotation_subject, Distributed computing, Perspective (graphical), Grid, Task (project management), Workflow, Resource (project management), Software engineering, business, Autonomy, Workflow management system, media_common

Abstract

Currently, most workflow management systems (WfMS) in Grid environments provide push-oriented task distribution strategies, where tasks are directly bound to suitable resources. In those scenarios the dedicated resources execute the submitted tasks according to the request of a WfMS or sometimes by support of a Meta-Scheduling service. This approach has specific problems, especially because of various conditions and constrains that have to be taken into account like local policies or the sites’ autonomy. To deal with such issues, this paper takes a closer look to the task distribution strategies. The established Grid WfMSs essentially support control-flow and data perspectives. However, they neglect the resource perspective. This paper exposes the advantages to deal with this perspective and demonstrates its feasability by a prototype implementation that integrates the missing resource patterns into UNICORE.

Published

2011

45. Inheritance of DNA transferred from American trypanosomes to human hosts

Author

Ana de Cássia Rosa, Dawidson Assis Gomes, Antonio R. L. Teixeira, Nadjar Nitz, Perla F. Araujo, Mariana Hecht, Alessandro O. Sousa, and Eduardo Leonardecz

Subjects

Male, Genoma humano, Public Health and Epidemiology/Infectious Diseases, Eukaryotic DNA replication, Genome, Microbiology/Parasitology, Child, Evolutionary Biology/Genomics, In Situ Hybridization, Fluorescence, Recombination, Genetic, Genetics and Genomics/Medical Genetics, Genetics, Multidisciplinary, Geography, U937 Cells, Middle Aged, Pedigree, Medicine, Female, Brazil, Research Article, Infectious Diseases/Tropical and Travel-Associated Diseases, Adult, Mitochondrial DNA, Adolescent, Gene Transfer, Horizontal, Trypanosoma cruzi, Pseudogene, Science, Molecular Sequence Data, Immunology/Autoimmunity, Molecular Biology/Molecular Evolution, Biology, Minicircle, Host-Parasite Interactions, Young Adult, Animals, Humans, Chagas Disease, DNA Integration, Gene, Aged, Genome, Human, Infectious Diseases/Protozoal Infections, DNA, Chagas, Doença de, Sequence Analysis, DNA, DNA, Protozoan, Long Interspersed Nucleotide Elements, Infectious Diseases/Neglected Tropical Diseases, Tripanossoma cruzi, Human genome

Abstract

Interspecies DNA transfer is a major biological process leading to the accumulation of mutations inherited by sexual reproduction among eukaryotes. Lateral DNA transfer events and their inheritance has been challenging to document. In this study we modified a thermal asymmetric interlaced PCR by using additional targeted primers, along with Southern blots, fluorescence techniques, and bioinformatics, to identify lateral DNA transfer events from parasite to host. Instances of naturally occurring human infections by Trypanosoma cruzi are documented, where mitochondrial minicircles integrated mainly into retrotransposable LINE-1 of various chromosomes. The founders of five families show minicircle integrations that were transferred vertically to their progeny. Microhomology end-joining of 6 to 22 AC-rich nucleotide repeats in the minicircles and host DNA mediates foreign DNA integration. Heterogeneous minicircle sequences were distributed randomly among families, with diversity increasing due to subsequent rearrangement of inserted fragments. Mosaic recombination and hitchhiking on retrotransposition events to different loci were more prevalent in germ line as compared to somatic cells. Potential new genes, pseudogenes, and knockouts were identified. A pathway of minicircle integration and maintenance in the host genome is suggested. Thus, infection by T. cruzi has the unexpected consequence of increasing human genetic diversity, and Chagas disease may be a fortuitous share of negative selection. This demonstration of contemporary transfer of eukaryotic DNA to the human genome and its subsequent inheritance by descendants introduces a significant change in the scientific concept of evolutionary biology and medicine.

Published

2010

46. The Pathogenesis of Chagas Disease in Mammals and Birds

Author

Antonio RL Teixeira, Nadjar Nitz, Perla F Araujo, and Mariana M Hecht

Abstract

After the horizontal transference of kDNA minicircle sequences into the genome of chagasic mammals it was possible to show the heritage of the kDNA mutation into those rabbits breed. However, mammals are permissive to infection by T. cruzi, which may persist through the animal life. To ensure that the kDNA mutation was not only a noise produced by the cryptic infection it was necessary to dismiss this possibility. This was possible through experiments using birds that are refractory to T. cruzi infection but are permissive to infection only in the first 10 days of embryonic life. When the fertile eggs were inoculated with T. cruzi the breed was born without infection but presenting the kDNA mutation. In this regard, rabbits and birds with kDNA mutation presented typical Chagas disease lesions: minimal rejection unit which is characteristic of the pathology of this disease where the non-parasitized target cell was destroyed by the cells from the vertebrate host´s immune system. These experiments showed that the minimal rejection unit is the common denominator of the pathogenesis of Chagas disease in vertebrate animals. In the chicken model refractory to T. cruzi the cardiomegaly was linked to the minimal rejection unit’s inflammatory infiltration. Therefore the parasite-free chicken heart pathology seen in kDNA-mutated chickens could be linked to the genotype and phenotype alterations. The mechanism whereby these alterations induce the immune rejection of the chicken’s heart requires further investigation.

Published

2009

47. Stroke in età pediatrica: nuova emergenza neurologica

Author

Spalice, A, DEL BALZO, F, Papetti, L, Nicita, F, Perla, F, Iacobini, M, Properzi, Enrico, Ursitti, F, and Iannetti, P.

Published

2009

48. Variations of the perforin gene in patiens with multiple sclerosis

Author

Cappellano, G., Orilieri, E., Comi, C., Chiocchetti, A., Bocca, S., Boggio, E., Bernardone, I.S., Cometa, A., Clementi, R., Barizzone, N., D'Alfonso, S., Corrado, L., Galimberti, D., Scarpini, E., Guerini, F.R., Caputo, D., Paolicelli, D., Trojano, M., Figà Talamasca, L., Salvetti, M., Perla, F., Leone, M., Monaco, F., and Dianziani, U.

Subjects

Settore MED/26 - Neurologia

Published

2008

49. Duloxetine for treating multiple sclerosis related-symptoms: a multicenter study

Author

Solaro, C, Cavalla, P, Merola, A, Mattioda, A, Bergamaschi, R, Biargigga, V, Patti, Francesco, Cimino, V, Perla, F, Restivo, D, Tanganelli, P, and Bohmker, M.

Published

2008

50. Up-regulation of EphB and ephrin-B expression in rhabdomyosarcoma

Author

Anna C. Berardi, Marsilio, S., Rofani, C., Salvucci, O., Altavista, P., Perla, F. M., Diomedi-Camassei, F., Uccini, S., Kokai, G., Landuzzi, L., Mcdowell, H. P., Dominici, C., A.C. Berardi, S. Marsilio, C. Rofani, O. Salvucci, P. Altavista, F.M. Perla, F. Diomedi-Camassei, S. Uccini, G. Kokai, L. Landuzzi, H.P. McDowell, and C. Dominici.

Subjects

Cell Line, Tumor, Eph-B, Humans, Ephrin-B2, Ephrin-B1, RNA, Messenger, Ligands, Ephrins, RHABDOMYOSARCOMA, EPHRIN, Receptors, Eph Family, Up-Regulation

Abstract

BACKGROUND: Increased expression of Eph receptors and their ephrin ligands has been implicated in promoting angiogenesis and tumour progression in several malignancies. Here the expression of mRNA for ephrin-B and EphB receptors in rhabdomyosarcoma (RMS) cell lines and primary tumours was investigated. MATERIALS AND METHODS: Expression of mRNA for ephrin-B and EphB receptors in RMS cell lines and primary tumours was measured by real-time RT-PCR and compared with the expression in normal striated muscle. RESULTS: A dysregulation of both ligands and receptors was found in all cell lines. In embryonal tumours, overexpression of ephrin-B1 correlated with overexpression of EphB1 (r = 0.97, p < 0.01) and EphB3 (r = 0.94, p < 0.05); overexpression of ephrin-B2 correlated with overexpression of EphB1 (r = 0.94, p < 0.05), EphB2 (r = 0.88, p < 0.01) and EphB4 (r = 0.76, p < 0.01). In alveolar tumours, no similar correlations were found. A correlation between EphB2 and EphB4 receptors was demonstrated in both tumour types, being positive in embryonal cases (r = 0.81, p < 0.01) and negative in alveolar (r = -1.00, p < 0.01). CONCLUSION: A global up-regulation of ephrin-B and EphB receptors in RMS tumours was found. The correlation between EphB2 and EphB4 receptors suggests a possible role for ephrin-B and EphB receptors in RMS development

Published

2008