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6. C9orf72 intermediate repeats confer genetic risk for severe covid-19 pneumonia independently of age

Author

Zanella, I, Zacchi, E, Piva, S, Filosto, M, Beligni, G, Alaverdian, D, Amitrano, S, Fava, F, Baldassarri, M, Frullanti, E, Meloni, I, Renieri, A, Castelli, F, Quiros-Roldan, E, Mari, F, Daga, S, Benetti, E, Furini, S, Fallerini, C, Valentino, F, Doddato, G, Giliberti, A, Tita, R, Bruttini, M, Croci, S, Pinto, A, Mencarelli, M, Rizzo, C, Montagnani, F, Tumbarello, M, Rancan, I, Sarno, L, Palmieri, M, Carriero, M, Fabbiani, M, Rossetti, B, Bargagli, E, Bergantini, L, D'Alessandro, M, Cameli, P, Bennett, D, Anedda, F, Marcantonio, S, Scolletta, S, Franchi, F, Mazzei, M, Guerrini, S, Conticini, E, Cantarini, L, Frediani, B, Tacconi, D, Raffaelli, C, Feri, M, Donati, A, Scala, R, Guidelli, L, Spargi, G, Corridi, M, Nencioni, C, Croci, L, Caldarelli, G, Spagnesi, M, Piacentini, P, Bandini, M, Desanctis, E, Cappelli, S, Canac-Cini, A, Verzuri, A, Anemoli, V, Ognibene, A, Pancrazi, A, Lorubbio, M, Vaghi, M, Monforte, A, Miraglia, F, Mondelli, M, Bruno, R, Marco, V, Mantovani, S, Ludovisi, S, Girardis, M, Venturelli, S, Busani, S, Cossarizza, A, Antinori, A, Vergori, A, Emiliozzi, A, Rusconi, S, Siano, M, Gabrieli, A, Riva, A, Francisci, D, Schiaroli, E, Tommasi, A, Paciosi, F, Scotton, P, Andretta, F, Panese, S, Scaggiante, R, Gatti, F, Parisi, S, Antoni, M, Monica, M, Piscopo, C, Capasso, M, Russo, R, Andolfo, I, Iolascon, A, Fiorentino, G, Carella, M, Castori, M, Merla, G, Squeo, G, Aucella, F, Raggi, P, Marciano, C, Perna, R, Bassetti, M, Biagio, A, Sanguinetti, M, Masucci, L, Valente, S, Mandala, M, Giorli, A, Salerni, L, Zucchi, P, Parravicini, P, Menatti, E, Baratti, S, Trotta, T, Giannattasio, F, Coiro, G, Lena, F, Coviello, D, Mussini, C, Bosio, G, Martinelli, E, Mancarella, S, Tavecchia, L, Belli, M, Crotti, L, Parati, G, Picchiotti, N, Gori, M, Gabbi, C, Sanarico, M, Ceri, S, Pinoli, P, Raimondi, F, Bis-Carini, F, Stella, A, Rizzi, M, Maggiolo, F, Ripamonti, D, Suardi, C, Bachetti, T, Rovere, M, Sarzi-Braga, S, Bussotti, M, Capitani, K, Zguro, K, Dei, S, Ravaglia, S, Artuso, R, Perrella, A, Bianchi, F, Bergomi, P, Catena, E, Colombo, R, Perticaroli, V, Gennarelli, M, Magri, C, Basiotto, G, Zizioli, D, Giliani, S, Monti, E, Foca, E, Carriero, C, Latronico, N, Padovani, A, Brugnoni, D, Zanella I., Zacchi E., Piva S., Filosto M., Beligni G., Alaverdian D., Amitrano S., Fava F., Baldassarri M., Frullanti E., Meloni I., Renieri A., Castelli F., Quiros-Roldan E., Mari F., Daga S., Benetti E., Furini S., Fallerini C., Valentino F., Doddato G., Giliberti A., Tita R., Bruttini M., Croci S., Pinto A. M., Mencarelli M. A., Rizzo C. L., Montagnani F., Tumbarello M., Rancan I., Sarno L. D., Palmieri M., Carriero M. L., Fabbiani M., Rossetti B., Bargagli E., Bergantini L., D'alessandro M., Cameli P., Bennett D., Anedda F., Marcantonio S., Scolletta S., Franchi F., Mazzei M. A., Guerrini S., Conticini E., Cantarini L., Frediani B., Tacconi D., Raffaelli C. S., Feri M., Donati A., Scala R., Guidelli L., Spargi G., Corridi M., Nencioni C., Croci L., Caldarelli G. P., Spagnesi M., Piacentini P., Bandini M., Desanctis E., Cappelli S., Canac-Cini A., Verzuri A., Anemoli V., Ognibene A., Pancrazi A., Lorubbio M., Vaghi M., Monforte A. D., Miraglia F. G., Mondelli M. U., Bruno R., Marco V., Mantovani S., Ludovisi S., Girardis M., Venturelli S., Busani S., Cossarizza A., Antinori A., Vergori A., Emiliozzi A., Rusconi S., Siano M., Gabrieli A., Riva A., Francisci D., Schiaroli E., Tommasi A., Paciosi F., Scotton P. G., Andretta F., Panese S., Scaggiante R., Gatti F., Parisi S. G., Antoni M. D., Monica M. D., Piscopo C., Capasso M., Russo R., Andolfo I., Iolascon A., Fiorentino G., Carella M., Castori M., Merla G., Squeo G. M., Aucella F., Raggi P., Marciano C., Perna R., Bassetti M., Biagio A. D., Sanguinetti M., Masucci L., Valente S., Mandala M., Giorli A., Salerni L., Zucchi P., Parravicini P., Menatti E., Baratti S., Trotta T., Giannattasio F., Coiro G., Lena F., Coviello D. A., Mussini C., Bosio G., Martinelli E., Mancarella S., Tavecchia L., Belli M. A., Crotti L., Parati G., Picchiotti N., Gori M., Gabbi C., Sanarico M., Ceri S., Pinoli P., Raimondi F., Bis-Carini F., Stella A., Rizzi M., Maggiolo F., Ripamonti D., Suardi C., Bachetti T., Rovere M. T. L., Sarzi-Braga S., Bussotti M., Capitani K., Zguro K., Dei S., Ravaglia S., Artuso R., Perrella A., Bianchi F., Bergomi P., Catena E., Colombo R., Perticaroli V., Gennarelli M., Magri C., Basiotto G., Zizioli D., Giliani S., Monti E., Foca E., Carriero C., Latronico N., Padovani A., Brugnoni D., Zanella, I, Zacchi, E, Piva, S, Filosto, M, Beligni, G, Alaverdian, D, Amitrano, S, Fava, F, Baldassarri, M, Frullanti, E, Meloni, I, Renieri, A, Castelli, F, Quiros-Roldan, E, Mari, F, Daga, S, Benetti, E, Furini, S, Fallerini, C, Valentino, F, Doddato, G, Giliberti, A, Tita, R, Bruttini, M, Croci, S, Pinto, A, Mencarelli, M, Rizzo, C, Montagnani, F, Tumbarello, M, Rancan, I, Sarno, L, Palmieri, M, Carriero, M, Fabbiani, M, Rossetti, B, Bargagli, E, Bergantini, L, D'Alessandro, M, Cameli, P, Bennett, D, Anedda, F, Marcantonio, S, Scolletta, S, Franchi, F, Mazzei, M, Guerrini, S, Conticini, E, Cantarini, L, Frediani, B, Tacconi, D, Raffaelli, C, Feri, M, Donati, A, Scala, R, Guidelli, L, Spargi, G, Corridi, M, Nencioni, C, Croci, L, Caldarelli, G, Spagnesi, M, Piacentini, P, Bandini, M, Desanctis, E, Cappelli, S, Canac-Cini, A, Verzuri, A, Anemoli, V, Ognibene, A, Pancrazi, A, Lorubbio, M, Vaghi, M, Monforte, A, Miraglia, F, Mondelli, M, Bruno, R, Marco, V, Mantovani, S, Ludovisi, S, Girardis, M, Venturelli, S, Busani, S, Cossarizza, A, Antinori, A, Vergori, A, Emiliozzi, A, Rusconi, S, Siano, M, Gabrieli, A, Riva, A, Francisci, D, Schiaroli, E, Tommasi, A, Paciosi, F, Scotton, P, Andretta, F, Panese, S, Scaggiante, R, Gatti, F, Parisi, S, Antoni, M, Monica, M, Piscopo, C, Capasso, M, Russo, R, Andolfo, I, Iolascon, A, Fiorentino, G, Carella, M, Castori, M, Merla, G, Squeo, G, Aucella, F, Raggi, P, Marciano, C, Perna, R, Bassetti, M, Biagio, A, Sanguinetti, M, Masucci, L, Valente, S, Mandala, M, Giorli, A, Salerni, L, Zucchi, P, Parravicini, P, Menatti, E, Baratti, S, Trotta, T, Giannattasio, F, Coiro, G, Lena, F, Coviello, D, Mussini, C, Bosio, G, Martinelli, E, Mancarella, S, Tavecchia, L, Belli, M, Crotti, L, Parati, G, Picchiotti, N, Gori, M, Gabbi, C, Sanarico, M, Ceri, S, Pinoli, P, Raimondi, F, Bis-Carini, F, Stella, A, Rizzi, M, Maggiolo, F, Ripamonti, D, Suardi, C, Bachetti, T, Rovere, M, Sarzi-Braga, S, Bussotti, M, Capitani, K, Zguro, K, Dei, S, Ravaglia, S, Artuso, R, Perrella, A, Bianchi, F, Bergomi, P, Catena, E, Colombo, R, Perticaroli, V, Gennarelli, M, Magri, C, Basiotto, G, Zizioli, D, Giliani, S, Monti, E, Foca, E, Carriero, C, Latronico, N, Padovani, A, Brugnoni, D, Zanella I., Zacchi E., Piva S., Filosto M., Beligni G., Alaverdian D., Amitrano S., Fava F., Baldassarri M., Frullanti E., Meloni I., Renieri A., Castelli F., Quiros-Roldan E., Mari F., Daga S., Benetti E., Furini S., Fallerini C., Valentino F., Doddato G., Giliberti A., Tita R., Bruttini M., Croci S., Pinto A. M., Mencarelli M. A., Rizzo C. L., Montagnani F., Tumbarello M., Rancan I., Sarno L. D., Palmieri M., Carriero M. L., Fabbiani M., Rossetti B., Bargagli E., Bergantini L., D'alessandro M., Cameli P., Bennett D., Anedda F., Marcantonio S., Scolletta S., Franchi F., Mazzei M. A., Guerrini S., Conticini E., Cantarini L., Frediani B., Tacconi D., Raffaelli C. S., Feri M., Donati A., Scala R., Guidelli L., Spargi G., Corridi M., Nencioni C., Croci L., Caldarelli G. P., Spagnesi M., Piacentini P., Bandini M., Desanctis E., Cappelli S., Canac-Cini A., Verzuri A., Anemoli V., Ognibene A., Pancrazi A., Lorubbio M., Vaghi M., Monforte A. D., Miraglia F. G., Mondelli M. U., Bruno R., Marco V., Mantovani S., Ludovisi S., Girardis M., Venturelli S., Busani S., Cossarizza A., Antinori A., Vergori A., Emiliozzi A., Rusconi S., Siano M., Gabrieli A., Riva A., Francisci D., Schiaroli E., Tommasi A., Paciosi F., Scotton P. G., Andretta F., Panese S., Scaggiante R., Gatti F., Parisi S. G., Antoni M. D., Monica M. D., Piscopo C., Capasso M., Russo R., Andolfo I., Iolascon A., Fiorentino G., Carella M., Castori M., Merla G., Squeo G. M., Aucella F., Raggi P., Marciano C., Perna R., Bassetti M., Biagio A. D., Sanguinetti M., Masucci L., Valente S., Mandala M., Giorli A., Salerni L., Zucchi P., Parravicini P., Menatti E., Baratti S., Trotta T., Giannattasio F., Coiro G., Lena F., Coviello D. A., Mussini C., Bosio G., Martinelli E., Mancarella S., Tavecchia L., Belli M. A., Crotti L., Parati G., Picchiotti N., Gori M., Gabbi C., Sanarico M., Ceri S., Pinoli P., Raimondi F., Bis-Carini F., Stella A., Rizzi M., Maggiolo F., Ripamonti D., Suardi C., Bachetti T., Rovere M. T. L., Sarzi-Braga S., Bussotti M., Capitani K., Zguro K., Dei S., Ravaglia S., Artuso R., Perrella A., Bianchi F., Bergomi P., Catena E., Colombo R., Perticaroli V., Gennarelli M., Magri C., Basiotto G., Zizioli D., Giliani S., Monti E., Foca E., Carriero C., Latronico N., Padovani A., and Brugnoni D.

Abstract

A cytokine storm, autoimmune features and dysfunctions of myeloid cells significantly contribute to severe coronavirus disease 2019 (COVID-19), caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection. Genetic background of the host seems to be partly responsible for severe phenotype and genes related to innate immune response seem critical host determinants. The C9orf72 gene has a role in vesicular trafficking, autophagy regulation and lyso-some functions, is highly expressed in myeloid cells and is involved in immune functions, regulating the lysosomal degradation of mediators of innate immunity. A large non-coding hexanucleotide repeat expansion (HRE) in this gene is the main genetic cause of frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS), both characterized by neuroinflammation and high systemic levels of proinflammatory cytokines, while HREs of intermediate length, although rare, are more frequent in autoimmune disorders. C9orf72 full mutation results in haploinsufficiency and intermediate HREs seem to modulate gene expression as well and impair autophagy. Herein, we sought to explore whether intermediate HREs in C9orf72 may be a risk factor for severe COVID-19. Although we found intermediate HREs in only a small portion of 240 patients with severe COVID-19 pneumonia, the magnitude of risk for requiring non-invasive or mechanical ventilation conferred by harboring intermediate repeats >10 units in at least one C9orf72 allele was more than twice respect to having shorter expansions, when adjusted for age (odds ratio (OR) 2.36; 95% confidence interval (CI) 1.04–5.37, p = 0.040). The association between intermediate repeats >10 units and more severe clinical outcome (p = 0.025) was also validated in an independent cohort of 201 SARS-CoV-2 infected patients. These data suggest that C9orf72 HREs >10 units may influence the pathogenic process driving more severe COVID-19 phenotypes.

Published
2021

7. C9orf72 intermediate repeats confer genetic risk for severe covid-19 pneumonia independently of age

Author

Zanella, I., Zacchi, E., Piva, S., Filosto, M., Beligni, G., Alaverdian, D., Amitrano, S., Fava, F., Baldassarri, M., Frullanti, E., Meloni, I., Renieri, A., Castelli, F., Quiros-Roldan, E., Mari, F., Daga, S., Benetti, E., Furini, S., Fallerini, C., Valentino, Francesca, Doddato, G., Giliberti, A., Tita, R., Bruttini, M., Croci, S., Pinto, A. M., Mencarelli, Marta, Rizzo, C. L., Montagnani, F., Tumbarello, Mario, Rancan, I., Sarno, L. D., Palmieri, Marco, Carriero, M. L., Fabbiani, M., Rossetti, Barbara, Bargagli, E., Bergantini, L., D'Alessandro, Michele, Cameli, P., Bennett, D., Anedda, F., Marcantonio, S., Scolletta, S., Franchi, Francesca, Mazzei, M. A., Guerrini, S., Conticini, E., Cantarini, L., Frediani, B., Tacconi, D., Raffaelli, C. S., Feri, M., Donati, Andrea, Scala, R., Guidelli, L., Spargi, G., Corridi, M., Nencioni, C., Croci, L., Caldarelli, G. P., Spagnesi, M., Piacentini, P., Bandini, M., Desanctis, E., Cappelli, S., Canac-Cini, A., Verzuri, A., Anemoli, V., Ognibene, A., Pancrazi, A., Lorubbio, M., Vaghi, M., Monforte, A. D., Miraglia, F. G., Mondelli, M. U., Bruno, R., Marco, V., Mantovani, Susanna, Ludovisi, S., Girardis, M., Venturelli, S., Busani, S., Cossarizza, A., Antinori, Armando, Vergori, A., Emiliozzi, A., Rusconi, S., Siano, M., Gabrieli, A., Riva, A., Francisci, D., Schiaroli, E., Tommasi, A., Paciosi, F., Scotton, P. G., Andretta, F., Panese, S., Scaggiante, R., Gatti, F., Parisi, S. G., Antoni, M. D., Monica, M. D., Piscopo, C., Capasso, Monica, Russo, R., Andolfo, I., Iolascon, A., Fiorentino, Giuseppe, Carella, M., Castori, M., Merla, G., Squeo, G. M., Aucella, F., Raggi, P., Marciano, C., Perna, Raffaella, Bassetti, M., Biagio, A. D., Sanguinetti, Maurizio, Masucci, Luca, Valente, S., Mandala, M., Giorli, A., Salerni, L., Zucchi, P., Parravicini, P., Menatti, E., Baratti, S., Trotta, T., Giannattasio, F., Coiro, G., Lena, Francesco, Coviello, D. A., Mussini, C., Bosio, Giacomo, Martinelli, E., Mancarella, S., Tavecchia, L., Belli, M. A., Crotti, L., Parati, G., Picchiotti, N., Gori, Mario, Gabbi, Chiara, Sanarico, M., Ceri, S., Pinoli, P., Raimondi, F., Bis-Carini, F., Stella, A., Rizzi, M., Maggiolo, F., Ripamonti, D., Suardi, C., Bachetti, T., Rovere, M. T. L., Sarzi-Braga, S., Bussotti, M., Capitani, K., Zguro, K., Dei, S., Ravaglia, S., Artuso, R., Perrella, A., Bianchi, F., Bergomi, P., Catena, E., Colombo, R., Perticaroli, V., Gennarelli, Massimo, Magri, Carlotta, Basiotto, G., Zizioli, D., Giliani, S., Monti, E., Foca, E., Carriero, C., Latronico, N., Padovani, A., Brugnoni, D., Zanella, I., Zacchi, E., Piva, S., Filosto, M., Beligni, G., Alaverdian, D., Amitrano, S., Fava, F., Baldassarri, M., Frullanti, E., Meloni, I., Renieri, A., Castelli, F., Quiros-Roldan, E., Mari, F., Daga, S., Benetti, E., Furini, S., Fallerini, C., Valentino, F., Doddato, G., Giliberti, A., Tita, R., Bruttini, M., Croci, S., Pinto, A. M., Mencarelli, M. A., Rizzo, C. L., Montagnani, F., Tumbarello, M., Rancan, I., Sarno, L. D., Palmieri, M., Carriero, M. L., Fabbiani, M., Rossetti, B., Bargagli, E., Bergantini, L., D'Alessandro, M., Cameli, P., Bennett, D., Anedda, F., Marcantonio, S., Scolletta, S., Franchi, F., Mazzei, M. A., Guerrini, S., Conticini, E., Cantarini, L., Frediani, B., Tacconi, D., Raffaelli, C. S., Feri, M., Donati, A., Scala, R., Guidelli, L., Spargi, G., Corridi, M., Nencioni, C., Croci, L., Caldarelli, G. P., Spagnesi, M., Piacentini, P., Bandini, M., Desanctis, E., Cappelli, S., Canac-Cini, A., Verzuri, A., Anemoli, V., Ognibene, A., Pancrazi, A., Lorubbio, M., Vaghi, M., Monforte, A. D., Miraglia, F. G., Mondelli, M. U., Bruno, R., Marco, V., Mantovani, S., Ludovisi, S., Girardis, M., Venturelli, S., Busani, S., Cossarizza, A., Antinori, A., Vergori, A., Emiliozzi, A., Rusconi, S., Siano, M., Gabrieli, A., Riva, A., Francisci, D., Schiaroli, E., Tommasi, A., Paciosi, F., Scotton, P. G., Andretta, F., Panese, S., Scaggiante, R., Gatti, F., Parisi, S. G., Antoni, M. D., Monica, M. D., Piscopo, C., Capasso, M., Russo, R., Andolfo, I., Iolascon, A., Fiorentino, G., Carella, M., Castori, M., Merla, G., Squeo, G. M., Aucella, F., Raggi, P., Marciano, C., Perna, R., Bassetti, M., Biagio, A. D., Sanguinetti, M., Masucci, L., Valente, S., Mandala, M., Giorli, A., Salerni, L., Zucchi, P., Parravicini, P., Menatti, E., Baratti, S., Trotta, T., Giannattasio, F., Coiro, G., Lena, F., Coviello, D. A., Mussini, C., Bosio, G., Martinelli, E., Mancarella, S., Tavecchia, L., Belli, M. A., Crotti, L., Parati, G., Picchiotti, N., Gori, M., Gabbi, C., Sanarico, M., Ceri, S., Pinoli, P., Raimondi, F., Bis-Carini, F., Stella, A., Rizzi, M., Maggiolo, F., Ripamonti, D., Suardi, C., Bachetti, T., Rovere, M. T. L., Sarzi-Braga, S., Bussotti, M., Capitani, K., Zguro, K., Dei, S., Ravaglia, S., Artuso, R., Perrella, A., Bianchi, F., Bergomi, P., Catena, E., Colombo, R., Perticaroli, V., Gennarelli, M., Magri, C., Basiotto, G., Zizioli, D., Giliani, S., Monti, E., Foca, E., Carriero, C., Latronico, N., Padovani, A., Brugnoni, D., Zanella, I, Zacchi, E, Piva, S, Filosto, M, Beligni, G, Alaverdian, D, Amitrano, S, Fava, F, Baldassarri, M, Frullanti, E, Meloni, I, Renieri, A, Castelli, F, Quiros-Roldan, E, Mari, F, Daga, S, Benetti, E, Furini, S, Fallerini, C, Valentino, F, Doddato, G, Giliberti, A, Tita, R, Bruttini, M, Croci, S, Pinto, A, Mencarelli, M, Rizzo, C, Montagnani, F, Tumbarello, M, Rancan, I, Sarno, L, Palmieri, M, Carriero, M, Fabbiani, M, Rossetti, B, Bargagli, E, Bergantini, L, D'Alessandro, M, Cameli, P, Bennett, D, Anedda, F, Marcantonio, S, Scolletta, S, Franchi, F, Mazzei, M, Guerrini, S, Conticini, E, Cantarini, L, Frediani, B, Tacconi, D, Raffaelli, C, Feri, M, Donati, A, Scala, R, Guidelli, L, Spargi, G, Corridi, M, Nencioni, C, Croci, L, Caldarelli, G, Spagnesi, M, Piacentini, P, Bandini, M, Desanctis, E, Cappelli, S, Canac-Cini, A, Verzuri, A, Anemoli, V, Ognibene, A, Pancrazi, A, Lorubbio, M, Vaghi, M, Monforte, A, Miraglia, F, Mondelli, M, Bruno, R, Marco, V, Mantovani, S, Ludovisi, S, Girardis, M, Venturelli, S, Busani, S, Cossarizza, A, Antinori, A, Vergori, A, Emiliozzi, A, Rusconi, S, Siano, M, Gabrieli, A, Riva, A, Francisci, D, Schiaroli, E, Tommasi, A, Paciosi, F, Scotton, P, Andretta, F, Panese, S, Scaggiante, R, Gatti, F, Parisi, S, Antoni, M, Monica, M, Piscopo, C, Capasso, M, Russo, R, Andolfo, I, Iolascon, A, Fiorentino, G, Carella, M, Castori, M, Merla, G, Squeo, G, Aucella, F, Raggi, P, Marciano, C, Perna, R, Bassetti, M, Biagio, A, Sanguinetti, M, Masucci, L, Valente, S, Mandala, M, Giorli, A, Salerni, L, Zucchi, P, Parravicini, P, Menatti, E, Baratti, S, Trotta, T, Giannattasio, F, Coiro, G, Lena, F, Coviello, D, Mussini, C, Bosio, G, Martinelli, E, Mancarella, S, Tavecchia, L, Belli, M, Crotti, L, Parati, G, Picchiotti, N, Gori, M, Gabbi, C, Sanarico, M, Ceri, S, Pinoli, P, Raimondi, F, Bis-Carini, F, Stella, A, Rizzi, M, Maggiolo, F, Ripamonti, D, Suardi, C, Bachetti, T, Rovere, M, Sarzi-Braga, S, Bussotti, M, Capitani, K, Zguro, K, Dei, S, Ravaglia, S, Artuso, R, Perrella, A, Bianchi, F, Bergomi, P, Catena, E, Colombo, R, Perticaroli, V, Gennarelli, M, Magri, C, Basiotto, G, Zizioli, D, Giliani, S, Monti, E, Foca, E, Carriero, C, Latronico, N, Padovani, A, and Brugnoni, D

Subjects
Male, Severity of Illness Index, Risk Factors, C9orf72, Odds Ratio, Age Factor, Biology (General), Spectroscopy, Innate immunity, Age Factors, General Medicine, Middle Aged, Computer Science Applications, Chemistry, Intermediate alleles, Female, Haploinsufficiency, Human, Adult, Genotype, Logistic Model, QH301-705.5, Intermediate allele, Article, Settore MED/07 - MICROBIOLOGIA E MICROBIOLOGIA CLINICA, Catalysis, Inorganic Chemistry, Immune system, medicine, Autophagy, Humans, Genetic Predisposition to Disease, Physical and Theoretical Chemistry, Allele, QD1-999, Molecular Biology, COVID-19, Genetic risk, SARS-CoV-2, Aged, Amyotrophic Lateral Sclerosis, C9orf72 Protein, Logistic Models, Microsatellite Repeats, Innate immune system, business.industry, Risk Factor, Organic Chemistry, medicine.disease, Immunology, Cytokine storm, business, Trinucleotide repeat expansion, Amyotrophic Lateral Sclerosi
Abstract

A cytokine storm, autoimmune features and dysfunctions of myeloid cells significantly contribute to severe coronavirus disease 2019 (COVID-19), caused by the severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection. Genetic background of the host seems to be partly responsible for severe phenotype and genes related to innate immune response seem critical host determinants. The C9orf72 gene has a role in vesicular trafficking, autophagy regulation and lysosome functions, is highly expressed in myeloid cells and is involved in immune functions, regulating the lysosomal degradation of mediators of innate immunity. A large non-coding hexanucleotide repeat expansion (HRE) in this gene is the main genetic cause of frontotemporal dementia (FTD) and amyotrophic lateral sclerosis (ALS), both characterized by neuroinflammation and high systemic levels of proinflammatory cytokines, while HREs of intermediate length, although rare, are more frequent in autoimmune disorders. C9orf72 full mutation results in haploinsufficiency and intermediate HREs seem to modulate gene expression as well and impair autophagy. Herein, we sought to explore whether intermediate HREs in C9orf72 may be a risk factor for severe COVID-19. Although we found intermediate HREs in only a small portion of 240 patients with severe COVID-19 pneumonia, the magnitude of risk for requiring non-invasive or mechanical ventilation conferred by harboring intermediate repeats &gt, 10 units in at least one C9orf72 allele was more than twice respect to having shorter expansions, when adjusted for age (odds ratio (OR) 2.36, 95% confidence interval (CI) 1.04–5.37, p = 0.040). The association between intermediate repeats &gt, 10 units and more severe clinical outcome (p = 0.025) was also validated in an independent cohort of 201 SARS-CoV-2 infected patients. These data suggest that C9orf72 HREs &gt, 10 units may influence the pathogenic process driving more severe COVID-19 phenotypes.

Published
2021

13. A Report on the 2012 Seismic Sequence in Emilia (Northern Italy)

Author

Lo Presti, D., Sassu, M., Luzi, L., Pacor, F., Castaldini, Doriano, Tosatti, Giovanni, Meisina, C., Zizioli, D., Zucca, F., Rossi, G., Saccarotti, G., and Piccinini, D.

Subjects
Geotechnical Engineering, Seismology, Surface Effects, Soil Liquefaction
Published
2013

17. Molecular cloning and knockdown of galactocerebrosidase in zebrafish: New insights into the pathogenesis of Krabbe's disease

Author

Zizioli, D., Guarienti, M., Tobia, C., Gariano, G., Borsani, G., Bresciani, R., Ronca, R., Giacopuzzi, E., Preti, A., Gaudenzi, G., Belleri, M., Di Salle, E., Fabriàs, Gemma, Casas, Josefina, Ribatti, Domenico, Monti, Eugenio, Presta, M., Zizioli, D., Guarienti, M., Tobia, C., Gariano, G., Borsani, G., Bresciani, R., Ronca, R., Giacopuzzi, E., Preti, A., Gaudenzi, G., Belleri, M., Di Salle, E., Fabriàs, Gemma, Casas, Josefina, Ribatti, Domenico, Monti, Eugenio, and Presta, M.

Abstract

The lysosomal hydrolase galactocerebrosidase (GALC) catalyzes the removal of galactose from galactosylceramide and from other sphingolipids. GALC deficiency is responsible for globoid cell leukodystrophy (GLD), or Krabbe's disease, an early lethal inherited neurodegenerative disorder characterized by the accumulation of the neurotoxic metabolite psychosine in the central nervous system (CNS). The poor outcome of current clinical treatments calls for novel model systems to investigate the biological impact of GALC down-regulation and for the search of novel therapeutic strategies in GLD. Zebrafish (Danio rerio) represents an attractive vertebrate model for human diseases. Here, lysosomal GALC activity was demonstrated in the brain of zebrafish adults and embryos. Accordingly, we identified two GALC co-orthologs (named galca and galcb) dynamically co-expressed in CNS during zebrafish development. Both genes encode for lysosomal enzymes endowed with GALC activity. Single down-regulation of galca or galcb by specific antisense morpholino oligonucleotides results in a partial decrease of GALC activity in zebrafish embryos that was abrogated in double galca/. galcb morphants. However, no psychosine accumulation was observed in galca/. galcb double morphants. Nevertheless, double galca/. galcb knockdown caused reduction and partial disorganization of the expression of the early neuronal marker neuroD and an increase of apoptotic events during CNS development. These observations provide new insights into the pathogenesis of GLD, indicating that GALC loss-of-function may have pathological consequences in developing CNS independent of psychosine accumulation. Also, they underscore the potentiality of the zebrafish system in studying the pathogenesis of lysosomal neurodegenerative diseases, including GLD. © 2014 Elsevier B.V.

Published
2014

18. The survey and mapping of sand-boil landforms related to the Emilia 2012 earthquakes: Preliminary results

Author

Ninfo, A, Zizioli, D, Meisina, C, Castaldini, D, Zucca, F, Luzi, L, DE AMICIS, M, Ninfo, a, DE AMICIS, MATTIA GIOVANNI MARIA, Ninfo, A, Zizioli, D, Meisina, C, Castaldini, D, Zucca, F, Luzi, L, DE AMICIS, M, Ninfo, a, and DE AMICIS, MATTIA GIOVANNI MARIA

Abstract

After a large earthquake, a lot of coseismic phenomena can occur in the field, and the spatial distribution is very important to understand the fault geometry. In this framework, the application of terrestrial photogrammetry is a less expensive and more rapid method to map the micro-morphology of sand volcanoes, compared to (terrestrial/aerial) laser scanning. The centimetric DEMs obtained can be processed and correlated with other datasets later, to create a complete geodatabase of coseismic features. The 3D reconstruction of sand boils and cracks can be of great interest for geomorphological research, as well as for the documentation of coseismic features. A detailed 3D database of landforms that are so ephemeral can also provide a more useful comparison with paleo-forms that are now buried by sediments.

Published
2012

21. Early embryonic death of mice deficient in gamma-adaptin.

Author

Zizioli, D, Meyer, C, Guhde, G, Saftig, P, von Figura, K, and Schu, P

Abstract

Intracellular protein transport and sorting by vesicles in the secretory and endocytic pathways requires the formation of a protein coat on the membrane. The heterotetrameric adaptor protein complex 1 (AP-1) promotes the formation of clathrin-coated vesicles at the trans-Golgi network. AP-1 interacts with various sorting signals in the cytoplasmic tails of cargo molecules, thus indicating a function in protein sorting. We generated mutants of the gamma-adaptin subunit of AP-1 in mice to investigate its role in post-Golgi vesicle transport and sorting processes. gamma-Adaptin-deficient embryos develop until day 3.5 post coitus and die during the prenidation period, revealing that AP-1 is essential for viability. In heterozygous mice the amount of AP-1 complexes is reduced to half of controls. Free beta1- or micro1 chains were not detectable, indicating that they are unstable unless they are part of AP-1 complexes. Heterozygous mice weigh less then their wild-type littermates and show impaired T cell development.

Published
1999

22. The survey and mapping of sand-boil landforms related to the Emilia 2012 earthquakes: Preliminary results

Author

Lucia Luzi, Mattia De Amicis, Doriano Castaldini, Davide Zizioli, Caludia Meisina, Francesco Zucca, Andrea Ninfo, Ninfo, A, Zizioli, D, Meisina, C, Castaldini, D, Zucca, F, Luzi, L, and DE AMICIS, M

Subjects
Earthquake, Water table, Population, GEO/04 - GEOGRAFIA FISICA E GEOMORFOLOGIA, lcsh:QC851-999, Emilia, Geomorphology, Sand boils, Digital elevation model, Liquefaction, Earthquake, Italy, Sand boils, LIQUEFACTION-INDUCED FEATURES, Digital elevation model, education, Geomorphology, Soil liquefaction, geography, education.field_of_study, geography.geographical_feature_category, northern Italy, Landform, lcsh:QC801-809, EVOLUTION, Liquefaction, Alluvial plain, lcsh:Geophysics. Cosmic physics, Geophysics, Italy, Volcano, lcsh:Meteorology. Climatology, Sand boil, Geology, Seismology
Abstract

Sand boils, which are also known as sand blows or sand volcanoes, are among the most common superficial effects induced by high-magnitude earthquakes. These generally occur in or close to alluvial plains when a strong earthquake (M >5) strikes on a lens of saturated and unconsolidated sand deposits that are constrained between silt-clay layers [Ambraseys 1988, Carter and Seed 1988, Galli 2000, Tuttle 2001, Obermeier et al. 2005], where the sediments are converted into a fluid suspension. The liquefaction phenomena requires the presence of saturated and uncompacted sand, and a groundwater table near the ground surface. This geological–geomorphological setting is common and widespread for the Po Plain (Italy) [Castiglioni et al. 1997]. The Po Plain (ca. 46,000 km2) represents 15% of the Italian territory. It hosts a population of about 20 million people (mean density of 450 people/km2) and many infrastructures. Thus, the Po Plain is an area of high vulnerability when considering the liquefaction potential in the case of a strong earthquake. Despite the potential, such phenomena are rarely observed in northern Italy [Cavallin et al. 1977, Galli 2000], because strong earthquakes are not frequent in this region; e.g., historical data report soil liquefaction near Ferrara in 1570 (M 5.3) and in Argenta 1624 (M 5.5) [Prestininzi and Romeo 2000, Galli 2000]. In the Emilia quakes of May 20 and 29, 2012, the most widespread coseismic effects were soil liquefaction and ground cracks, which occurred over wide areas in the Provinces of Modena, Ferrara, Bologna, Reggio Emilia and Mantova (Figure 1). […]

Published
2012

23. Ancient landscape changes in the North Marche region : an archaeological and geomorphological appraisal in the Cesano valley

Author

P. L. Dall’Aglio, E. Giorgi, M. Silani, M. Aldrovandi, C. Franceschelli, O. Nesci, D. Savelli, F. Troiani, L. Pellegrini, D. Zizioli, F. Bertoncello et F. Braemer, Dall'Aglio Pier Luigi, Enrico Giorgi, Michele Silani, Martina Aldrovandi, Carlotta Franceschelli, Olivia Nesci, Daniele Savelli, Francesco Troiani, Luisa Pellegrini, Davide Zizioli, Frédérique Bertoncello et Frank Braemer, P. L. Dall’Aglio, E. Giorgi, M. Silani, M. Aldrovandi, C. Franceschelli, O. Nesci, D. Savelli, F. Troiani, L. Pellegrini, D. Zizioli, Dall’Aglio, P. L., Giorgi, E., Silani, M., Aldrovandi, M., Franceschelli, C., Nesci, O., Savelli, D., Troiani, F., Pellegrini, L., and Zizioli, D.

Subjects
SUASA, ARCHEOLOGIA DEL PAESAGGIO, VALLE DEL CESANO, GEOMORFOLOGIA, MARCHE, TOPOGRAFIA ANTICA
Abstract

il contributo prende in analisi il rapporto tra il popolamento antio della valle del cesano e l'evoluzione della geografia fisica, allo scopo di ricostruire le variazioni del paesaggio legate in particolare alle vicende della città romana di suasa

Published
2012

24. The expression level of VEGFR2 regulates mechanotransduction, tumor growth and metastasis of high grade serous ovarian cancer cells.

Author

Grillo E, Ravelli C, Corsini M, Domenichini M, Scamozzi M, Zizioli D, Capoferri D, Bresciani R, Romani C, and Mitola S

Subjects
Female, Humans, Cell Line, Tumor, Animals, Neoplasm Metastasis, Cell Movement, Cystadenocarcinoma, Serous metabolism, Cystadenocarcinoma, Serous pathology, Cystadenocarcinoma, Serous genetics, Mice, Adaptor Proteins, Signal Transducing metabolism, Adaptor Proteins, Signal Transducing genetics, Transcription Factors metabolism, Transcription Factors genetics, Neoplasm Invasiveness, YAP-Signaling Proteins metabolism, Gene Expression Regulation, Neoplastic, Mice, Nude, Vascular Endothelial Growth Factor Receptor-2 metabolism, Vascular Endothelial Growth Factor Receptor-2 genetics, Ovarian Neoplasms pathology, Ovarian Neoplasms metabolism, Ovarian Neoplasms genetics, Mechanotransduction, Cellular, Cell Proliferation
Abstract

Recent data shows that alterations in the expression and/or activation of the vascular endothelial growth factor receptor 2 (VEGFR2) in high grade serous ovarian cancer (HGSOC) modulate tumor progression. However, controversial results have been obtained, showing that in some cases VEGFR2 inhibition can promote tumorigenesis and metastasis. Thus, it is urgent to better define the role of the VEGF/VEGFR2 system to understand/predict the effects of its inhibitors administered as anti-angiogenic in HGSOC. Here, we modulated the expression levels of VEGFR2 and analyzed the effects in two cellular models of HGSOC. VEGFR2 silencing (or its pharmacological inhibition) promote the growth and invasive potential of OVCAR3 cells in vitro and in vivo. Consistent with this, the low levels of VEGFR2 in OV7 cells are associated with more pronounced proliferative and motile phenotypes when compared to OVCAR3 cells, and VEGFR2 overexpression in OV7 cells inhibits cell growth. In vitro data confirmed that VEGFR2 silencing in OVCAR3 cells favors the acquisition of an invasive phenotype by loosening cell-ECM contacts, reducing the size and the signaling of focal adhesion contacts (FAs). This is translated into a reduced FAK activity at FAs, ECM-dependent alterations of mechanical forces through FAs and YAP nuclear translocation. Together, the data show that low expression, silencing or inhibition of VEGFR2 in HGSOC cells alter mechanotransduction and lead to the acquisition of a pro-proliferative/invasive phenotype which explains the need for a more cautious use of anti-VEGFR2 drugs in ovarian cancer., 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 © 2024. Published by Elsevier GmbH.)

Published
2024
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26. miR-23b-3p, miR-126-3p and GAS5 delivered by extracellular vesicles inhibit breast cancer xenografts in zebrafish.

Author

Pelisenco IA, Zizioli D, Guerra F, Grossi I, Bucci C, Mignani L, Girolimetti G, Di Corato R, D'Agostino VG, Marchina E, De Petro G, and Salvi A

Subjects
Animals, Humans, Female, Cell Line, Tumor, RNA, Long Noncoding genetics, RNA, Long Noncoding metabolism, Cell Proliferation drug effects, Xenograft Model Antitumor Assays, Zebrafish genetics, Extracellular Vesicles metabolism, Extracellular Vesicles genetics, MicroRNAs genetics, MicroRNAs metabolism, Breast Neoplasms pathology, Breast Neoplasms genetics, Breast Neoplasms drug therapy, Breast Neoplasms metabolism
Abstract

Background: Extracellular vesicles (EVs) are a group of nanoscale cell-derived membranous structures secreted by all cell types, containing molecular cargoes involved in intercellular communication. EVs can be used to mimic "nature's delivery system" to transport nucleic acids, peptides, lipids, and metabolites to target recipient cells. EVs offer a range of advantages over traditional synthetic carriers, thus paving the way for innovative drug delivery approaches that can be used in different diseases, including cancer. Here, by using breast cancer (BC) cells treated with the multi-kinase inhibitor sorafenib, we generated EVs enriched in specific non-coding RNAs (miR-23b-3p, miR-126-3p, and the long ncRNA GAS5) and investigated their potential impact on the aggressive properties of the BC in vitro and in vivo using zebrafish., Methods: EVs were collected from 4 different BC cell lines (HCC1937, MDA-MB-231, MCF-7, and MDA-MB-453) and characterized by western blotting, transmission electron microscopy and nanoparticle tracking analysis. Levels of encapsulated miR-23b-3p, miR-126-3p, and GAS5 were quantified by ddPCR. The role of the EVs as carriers of ncRNAs in vivo was established by injecting MDA-MB-231 and MDA-MB-453 cells into zebrafish embryos followed by EV-based treatment of the xenografts with EVs rich in miR-23b-3p, miR-126-3p and GAS5., Results: ddPCR analysis revealed elevated levels of miR-23b-3p, miR-126-3p, and GAS5, encapsulated in the EVs released by the aforementioned cell lines, following sorafenib treatment. The use of EVs as carriers of these specific ncRNAs in the treatment of BC cells resulted in a significant increase in the expression levels of the three ncRNAs along with the inhibition of cellular proliferation in vitro. In vivo experiments demonstrated a remarkable reduction of xenograft tumor area, suppression of angiogenesis, and decreased number of micrometastasis in the tails after administration of EVs enriched with these ncRNAs., Conclusions: Our study demonstrated that sorafenib-induced EVs, enriched with specific tumor-suppressor ncRNAs, can effectively inhibit the aggressive BC characteristics in vitro and in vivo. Our findings indicate an alternative way to enrich EVs with specific tumor-suppressor ncRNAs by treating the cells with an anticancer drug and support the development of new potential experimental molecular approaches to target the aggressive properties of cancer cells., Competing Interests: Declarations Ethics approval and consent to participate Not applicable. Consent for publication Not applicable. Competing interests The authors declare no competing interests., (© 2024. The Author(s).)

Published
2024
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27. Ecotoxicological evaluation of an aqueous phytoextract of Melia azedarach L.

Author

Popescu VS, Zhang L, Papa G, Giuliani C, Ribaudo G, Abate G, Bulgari D, Mac Sweeney E, Pucci M, Bottoni M, Milani F, Zizioli D, Negri I, Gianoncelli A, Gobbi E, Uberti D, Lucini L, Memo M, Fico G, Peron G, and Mastinu A

Subjects
Animals, Plant Extracts toxicity, Ecotoxicology, Humans, Bees drug effects, Insecticides toxicity, Germination drug effects, Zebrafish, Melia azedarach
Abstract

Melia azedarach L. is a Meliaceae that has shown important insecticidal activities. However, few researchers have extensively studied the toxicology of aqueous extracts of M. azedarach (MAE). Therefore, the main objective of this study was to characterize the phyto-eco-toxicological profile of MAE. First, a botanical and phytochemical characterization of MAE was performed using a histological, and metabolomic multi-analytical approach. Second, the toxicological effects on pollinating insects (Apis mellifera ligustica) and soil collembola (Folsomia candida) were evaluated. In addition, acute toxicity was evaluated in zebrafish (Danio rerio) to assess effects on aquatic fauna, and toxicity was determined in human neuroblastoma (SH-SY5Y) and fibroblast (FB-21) cell models. Finally, phytotoxic effects on germination of Cucumis sativus L., Brassica rapa L. and Sorghum vulgare L. were considered. Metabolomic analyses revealed the presence of not only limonoids but also numerous alkaloids, flavonoids and terpenoids in MAE. Histological analyses allowed us to better localize the areas of leaf deposition of the identified secondary metabolites. Regarding the ecotoxicological data, no significant toxicity was observed in bees and collembola at all doses tested. In contrast, severe cardiac abnormalities were observed in zebrafish embryos at concentrations as low as 25 μg/mL. In addition, MAE showed toxicity at 1.6 μg/mL and 6.25 μg/mL in FB-21 and SH-SY5Y cells, respectively. Finally, MAE inhibited seed germination with inhibitory concentrations starting from 5.50 μg/mL in B. rapa, 20 μg/mL in S. vulgare, and 31 μg/mL in C. sativus. Although M. azedarach extracts are considered valuable natural insecticides, their ecological impact cannot be underestimated. Even the use of an environmentally friendly solvent (an aqueous solution), for the first time, is not without side effects. Therefore, the data collected in this study show the importance of evaluating the dosages, modes of administration and production methods of M. azedarach phytoextracts in agricultural settings., Competing Interests: Declaration of competing interest The authors declare no conflict of interest., (Copyright © 2024 The Author(s). Published by Elsevier B.V. All rights reserved.)

Published
2024
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28. The Bioactive Gamma-Oryzanol from Oryza sativa L. Promotes Neuronal Differentiation in Different In Vitro and In Vivo Models.

Author

Abate G, Pezzotta A, Pucci M, Bortolotto V, Ribaudo G, Bonini SA, Mastinu A, Maccarinelli G, Ongaro A, Tirelli E, Zizioli D, Gianoncelli A, Memo M, Grilli M, and Uberti D

Abstract

Gamma-oryzanol (ORY), found in rice ( Oryza sativa L.), is a mixture of ferulic acid esters with triterpene alcohols, well-known for its antioxidant and anti-inflammatory properties. Our past research demonstrated its positive impact on cognitive function in adult mice, influencing synaptic plasticity and neuroprotection. In this study, we explored whether ORY can exert neuro-differentiating effects by using different experimental models. For this purpose, chemical characterization identified four components that are most abundant in ORY. In human neuroblastoma cells, we showed ORY's ability to stimulate neurite outgrowth, upregulating the expression of GAP43, BDNF, and TrkB genes. In addition, ORY was found to guide adult mouse hippocampal neural progenitor cells (NPCs) toward a neuronal commitment. Microinjection of ORY in zebrafish Tg ( -3.1 neurog1 :GFP) amplified neurog1 -GFP signal, islet1 , and bdnf mRNA levels. Zebrafish nrf2a and nrf2b morphants (MOs) were utilized to assess ORY effects in the presence or absence of Nrf2. Notably, ORY's ability to activate bdnf was nullified in nrf2a-MO and nrf2b-MO . Furthermore, computational analysis suggested ORY's single components have different affinities for the Keap1-Kelch domain. In conclusion, although more in-depth studies are needed, our findings position ORY as a potential source of bioactive molecules with neuro-differentiating potential involving the Nrf2 pathway.

Published
2024
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29. Ecotoxicity Assessment of α-Amino Acid-Derived Polyamidoamines Using Zebrafish as a Vertebrate Model.

Author

Treccani S, Ferruti P, Alongi J, Monti E, Zizioli D, and Ranucci E

Abstract

The aquatic ecotoxicity of three α-amino acid-derived polyamidoamines (PAAs) was studied using zebrafish embryos as a viable vertebrate model organism. The PAAs examined were water-soluble amphoteric polyelectrolytes with a primarily negative charge, which were efficient flame retardants for cotton. The fish embryo acute toxicity test performed with PAA water solutions using 1.5-500 mg L -1 concentrations showed that toxicity did not statistically differ from the control. The survival rates were indeed >90%, even at the highest concentration; the hatching rates were >80%; and the numbers of morphological defects were comparable to those of the control. Tests using transgenic zebrafish lines indicated that the numbers of microscopic vascular and musculoskeletal defects were comparable to the control, with one random concentration showing doubled alterations. Sensory-motor tests in response to visual and tactile stimuli were also performed. In the presence of PAAs, embryos exposed to alternating light/dark cycles showed an insignificant mobility reduction during the dark phase. Touch-evoked response tests revealed a mild effect of PAAs on the neuromotor system at concentrations > 10 mg L -1 . The cystine/glycine copolymer at 100 mg L -1 exhibited the greatest effect. Overall, the studied PAAs showed a minimal impact on aquatic systems and should be further considered as promising ecofriendly materials.

Published
2024
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30. Dolutegravir and Folic Acid Interaction during Neural System Development in Zebrafish Embryos.

Author

Zizioli D, Quiros-Roldan E, Ferretti S, Mignani L, Tiecco G, Monti E, Castelli F, and Zanella I

Subjects
Animals, Embryo, Nonmammalian drug effects, Embryo, Nonmammalian metabolism, Neural Tube Defects chemically induced, Neurogenesis drug effects, Female, Zebrafish, Heterocyclic Compounds, 3-Ring pharmacology, Folic Acid metabolism, Oxazines pharmacology, Pyridones pharmacology, Piperazines pharmacology
Abstract

Dolutegravir (DTG) is one of the most prescribed antiretroviral drugs for treating people with HIV infection, including women of child-bearing potential or pregnant. Nonetheless, neuropsychiatric symptoms are frequently reported. Early reports suggested that, probably in relation to folic acid (FA) shortage, DTG may induce neural tube defects in infants born to women taking the drug during pregnancy. Subsequent reports did not definitively confirm these findings. Recent studies in animal models have highlighted the association between DTG exposure in utero and congenital anomalies, and an increased risk of neurologic abnormalities in children exposed during in utero life has been reported. Underlying mechanisms for DTG-related neurologic symptoms and congenital anomalies are not fully understood. We aimed to deepen our knowledge on the neurodevelopmental effects of DTG exposure and further explore the protective role of FA by the use of zebrafish embryos. We treated embryos at 4 and up to 144 h post fertilization (hpf) with a subtherapeutic DTG concentration (1 μM) and observed the disruption of the anterior-posterior axis and several morphological malformations in the developing brain that were both prevented by pre-exposure (2 hpf) and rescued by post-exposure (10 hpf) with FA. By whole-mount in situ hybridization with riboprobes for genes that are crucial during the early phases of neurodevelopment ( ntl , pax2a , ngn1 , neurod1 ) and by in vivo visualization of the transgenic Tg( ngn1 :EGFP) zebrafish line, we found that DTG induced severe neurodevelopmental defects over time in most regions of the nervous system (notochord, midbrain-hindbrain boundary, eye, forebrain, midbrain, hindbrain, spinal cord) that were mostly but not completely rescued by FA supplementation. Of note, we observed the disruption of ngn1 expression in the dopaminergic regions of the developing forebrain, spinal cord neurons and spinal motor neuron projections, with the depletion of the tyrosine hydroxylase (TH) + dopaminergic neurons of the dorsal diencephalon and the strong reduction in larvae locomotion. Our study further supports previous evidence that DTG can interfere with FA pathways in the developing brain but also provides new insights regarding the mechanisms involved in the increased risk of DTG-associated fetal neurodevelopmental defects and adverse neurologic outcomes in in utero exposed children, suggesting the impairment of dopaminergic pathways., Competing Interests: G.T., F.C. and E.Q.-R. received travel grants from Bristol-Myers Squibb, Gilead Sciences, ViiV Healthcare, Janssen-Cilag, and Merck, Sharp, and Dohme, and E.Q.-R. also received consultancy fees from Janssen-Cilag, ViiV Healthcare, and Merck, Sharp, and Dohme. All other authors declare that the research was conducted in the absence of any commercial or financial relationships that could be considered as a potential conflict of interest.

Published
2024
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31. The D647N mutation of FGFR1 induces ligand-independent receptor activation.

Author

Domenichini M, Ravelli C, Corsini M, Codenotti S, Moreschi E, Gogna A, Capoferri D, Zizioli D, Bresciani R, Grillo E, and Mitola S

Subjects
Humans, Ligands, Cell Line, Tumor, Phosphorylation, Mutation, Receptor, Fibroblast Growth Factor, Type 1 genetics, Receptor, Fibroblast Growth Factor, Type 1 metabolism, Signal Transduction
Abstract

The activation loop (A-loop) of kinases, a key regulatory region, is recurrently mutated in several kinase proteins in cancer resulting in dysregulated kinase activity and response to kinase inhibitors. FGFR1 receptor tyrosine kinase represents an important oncogene and therapeutic target for solid and hematological tumors. Here we investigate the biochemical and molecular effects of D647N mutation lying in the A-loop of FGFR1. When expressed in normal and tumoral in vitro cell models, FGFR1 D647N is phosphorylated also in the absence of ligands, and this is accompanied by the activation of intracellular signaling. The expression of FGFR1 D647N significantly increases single and collective migration of cancer cells in vitro and in vivo, when compared to FGFR1 WT . FGFR1 D647N expression exacerbates the aggressiveness of cancer cells, increasing their invasiveness in vitro and augmenting their pro-angiogenic capacity in vivo. Remarkably, the D647N mutation significantly increases the sensitivity of FGFR1 to the ATP-competitive inhibitor Erdafitinib suggesting the possibility that this mutation could become a specific target for the development of new inhibitors. Although further efforts are warranted for an exhaustive description of the activation mechanisms, for the identification of more specific inhibitors and for confirming the clinical significance of mutated FGFR1 D647N , overall our data demonstrate that the D647N substitution of FGFR1 is a novel pro-oncogenic activating mutation of the receptor that, when found in cancer patients, may anticipate good response to erdafitinib treatment., Competing Interests: Declaration of Competing Interest The authors declare the following financial interests/personal relationships which may be considered as potential competing interests: Mitola Stefania and Michela Corsini reports financial support was provided by Italian Association for Cancer Research. Silvia Codenotti and Elisabetta Grillo reports financial support was provided by Umberto Veronesi Foundation., (Copyright © 2023 The Authors. Published by Elsevier B.V. All rights reserved.)

Published
2023
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32. Downregulation of Zebrafish Cytosolic Sialidase Neu3.2 Affects Skeletal Muscle Development.

Author

Zizioli D, Codenotti S, Benaglia G, Manzoni M, Massardi E, Fanzani A, Borsani G, and Monti E

Subjects
Animals, Down-Regulation, Muscle, Skeletal, Muscle Development genetics, Neuraminidase genetics, Zebrafish, Zebrafish Proteins genetics
Abstract

Sialidases remove terminal sialic acids residues from the non-reducing ends of glycoconjugates. They have been recognized as catabolic enzymes that work within different subcellular compartments and can ensure the proper turn-over of glycoconjugates. Four mammalian sialidases (NEU1-4) exist, with different subcellular localization, pH optimum and substrate specificity. In zebrafish, seven different sialidases, with high homology to mammalian counterparts, have been identified. Zebrafish Neu3.2 is similar to the human cytosolic sialidase NEU2, which is involved in skeletal muscle differentiation and exhibits a broad substrate specificity toward gangliosides and glycoproteins. In zebrafish neu3.2 , mRNA is expressed during somite development, and its enzymatic activity has been detected in the skeletal muscle and heart of adult animals. In this paper, 1-4-cell-stage embryos injected with neu3.2 splice-blocking morpholino showed severe embryonic defects, mainly in somites, heart and anterior-posterior axis formation. Myog and myod1 expressions were altered in morphants, and impaired musculature formation was associated with a defective locomotor behavior. Finally, the co-injection of Neu2 mouse mRNA in morphants rescued the phenotype. These data are consistent with the involvement of cytosolic sialidase in pathologies related to muscle formation and support the validity of the model to investigate the pathogenesis of the diseases.

Published
2023
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33. Comparison of Efavirenz and Doravirine Developmental Toxicity in an Embryo Animal Model.

Author

Zizioli D, Ferretti S, Tiecco G, Mignani L, Monti E, Castelli F, Quiros-Roldan E, and Zanella I

Subjects
Humans, Child, Animals, Rats, Zebrafish, Reverse Transcriptase Inhibitors toxicity, Lipids pharmacology, Embryo, Nonmammalian, HIV Infections drug therapy, Anti-HIV Agents pharmacology
Abstract

In the past, one of the most widely used non-nucleoside reverse transcriptase inhibitors (NNRTI) in first-line antiretroviral therapy (ART) of HIV infection was efavirenz (EFV), which is already used as a cost-effective treatment in developing countries due to its efficacy, tolerability, and availability. However, EFV also demonstrates several adverse effects, like hepatotoxicity, altered lipid profile, neuropsychological symptoms, and behavioral effects in children after in utero exposure. In 2018, another NNRTI, doravirine (DOR), was approved due to its similar efficacy but better safety profile. Preclinical safety studies demonstrated that DOR is not genotoxic and exhibits no developmental toxicity or effects on fertility in rats. Zebrafish ( Danio rerio ) embryos have been widely accepted as a vertebrate model for pharmacological and developmental studies. We used zebrafish embryos as an in vivo model to investigate the developmental toxicity of DOR compared to EFV. After exposure of the embryos to the drugs from the gastrula stage up to different developmental stages (30 embryos for each arm, in three independent experiments), we assessed their survival, morphology, hatching rate, apoptosis in the developing head, locomotion behavior, vasculature development, and neutral lipid distribution. Overall, DOR showed a better safety profile than EFV in our model. Therapeutic and supra-therapeutic doses of DOR induced very low mortality [survival rates: 92, 90, 88, 88, and 81% at 1, 5, 10, 25, and 50 μM, respectively, at 24 h post fecundation (hpf), and 88, 85, 88, 89, and 75% at the same doses, respectively, at 48 hpf] and mild morphological alterations compared to EFV exposure also in the sub-therapeutic ranges (survival rates: 80, 77, 69, 63, and 44% at 1, 5, 10, 25, and 50 μM, respectively, at 24 hpf and 72, 70, 63, 52, and 0% at the same doses, respectively, at 48 hpf). Further, DOR only slightly affected the hatching rate at supra-therapeutic doses (97, 98, 96, 87, and 83% at 1, 5, 10, 25, and 50 μM, respectively, at 72 hpf), while EFV already strongly reduced hatching at sub-therapeutic doses (83, 49, 11, 0, and 0% at 1, 5, 10, 25, and 50 μM, respectively, at the same time endpoint). Both DOR at therapeutic doses and most severely EFV at sub-therapeutic doses enhanced apoptosis in the developing head during crucial phases of embryo neurodevelopment and perturbed the locomotor behavior. Furthermore, EFV strongly affected angiogenesis and disturbed neutral lipid homeostasis even at sub-therapeutic doses compared to DOR at therapeutic concentrations. Our findings in zebrafish embryos add further data confirming the higher safety of DOR with respect to EFV regarding embryo development, neurogenesis, angiogenesis, and lipid metabolism. Further studies are needed to explore the molecular mechanisms underlying the better pharmacological safety profile of DOR, and further human studies are required to confirm these results in the zebrafish animal model.

Published
2023
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34. FSCN1 as a new druggable target in adrenocortical carcinoma.

Author

Ruggiero C, Tamburello M, Rossini E, Zini S, Durand N, Cantini G, Cioppi F, Hantel C, Kiseljak-Vassiliades K, Wierman ME, Landwehr LS, Weigand I, Kurlbaum M, Zizioli D, Turtoi A, Yang S, Berruti A, Luconi M, Sigala S, and Lalli E

Subjects
Animals, Cell Line, Tumor, Cell Proliferation, Gene Expression Regulation, Neoplastic, Neoplasm Recurrence, Local drug therapy, Neoplasm Recurrence, Local genetics, Zebrafish, Adrenal Cortex Neoplasms drug therapy, Adrenal Cortex Neoplasms genetics, Adrenal Cortex Neoplasms metabolism, Adrenocortical Carcinoma drug therapy, Adrenocortical Carcinoma genetics, Adrenocortical Carcinoma metabolism
Abstract

Adrenocortical carcinoma (ACC) is a rare endocrine malignancy with a high risk of relapse and metastatic spread. The actin-bundling protein fascin (FSCN1) is overexpressed in aggressive ACC and represents a reliable prognostic indicator. FSCN1 has been shown to synergize with VAV2, a guanine nucleotide exchange factor for the Rho/Rac GTPase family, to enhance the invasion properties of ACC cancer cells. Based on those results, we investigated the effects of FSCN1 inactivation by CRISPR/Cas9 or pharmacological blockade on the invasive properties of ACC cells, both in vitro and in an in vivo metastatic ACC zebrafish model. Here, we showed that FSCN1 is a transcriptional target for β-catenin in H295R ACC cells and that its inactivation resulted in defects in cell attachment and proliferation. FSCN1 knock-out modulated the expression of genes involved in cytoskeleton dynamics and cell adhesion. When Steroidogenic Factor-1 (SF-1) dosage was upregulated in H295R cells, activating their invasive capacities, FSCN1 knock-out reduced the number of filopodia, lamellipodia/ruffles and focal adhesions, while decreasing cell invasion in Matrigel. Similar effects were produced by the FSCN1 inhibitor G2-044, which also diminished the invasion of other ACC cell lines expressing lower levels of FSCN1 than H295R. In the zebrafish model, metastases formation was significantly reduced in FSCN1 knock-out cells and G2-044 significantly reduced the number of metastases formed by ACC cells. Our results indicate that FSCN1 is a new druggable target for ACC and provide the rationale for future clinical trials with FSCN1 inhibitors in patients with ACC., (© 2023 The Authors. International Journal of Cancer published by John Wiley & Sons Ltd on behalf of UICC.)

Published
2023
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35. Deficiency of AP1 Complex Ap1g1 in Zebrafish Model Led to Perturbation of Neurodevelopment, Female and Male Fertility; New Insight to Understand Adaptinopathies.

Author

Mignani L, Facchinello N, Varinelli M, Massardi E, Tiso N, Ravelli C, Mitola S, Schu P, Monti E, Finazzi D, Borsani G, and Zizioli D

Subjects
Animals, Female, Humans, Male, Mice, Endosomes metabolism, Epithelial Cells metabolism, Protein Isoforms metabolism, trans-Golgi Network metabolism, Zebrafish genetics, Zebrafish metabolism, Neurodevelopmental Disorders genetics, Transcription Factor AP-1 metabolism, Zebrafish Proteins metabolism
Abstract

In vertebrates, two homologous heterotetrameric AP1 complexes regulate the intracellular protein sorting via vesicles. AP-1 complexes are ubiquitously expressed and are composed of four different subunits: γ, β1, μ1 and σ1. Two different complexes are present in eukaryotic cells, AP1G1 (contains γ1 subunit) and AP1G2 (contains γ2 subunit); both are indispensable for development. One additional tissue-specific isoform exists for μ1A, the polarized epithelial cells specific to μ1B; two additional tissue-specific isoforms exist for σ1A: σ1B and σ1C. Both AP1 complexes fulfil specific functions at the trans -Golgi network and endosomes. The use of different animal models demonstrated their crucial role in the development of multicellular organisms and the specification of neuronal and epithelial cells. Ap1g1 (γ1) knockout mice cease development at the blastocyst stage, while Ap1m1 (μ1A) knockouts cease during mid-organogenesis. A growing number of human diseases have been associated with mutations in genes encoding for the subunits of adaptor protein complexes. Recently, a new class of neurocutaneous and neurometabolic disorders affecting intracellular vesicular traffic have been referred to as adaptinopathies. To better understand the functional role of AP1G1 in adaptinopathies, we generated a zebrafish ap1g1 knockout using CRISPR/Cas9 genome editing. Zebrafish ap1g1 knockout embryos cease their development at the blastula stage. Interestingly, heterozygous females and males have reduced fertility and showed morphological alterations in the brain, gonads and intestinal epithelium. An analysis of mRNA profiles of different marker proteins and altered tissue morphologies revealed dysregulated cadherin-mediated cell adhesion. These data demonstrate that the zebrafish model organism enables us to study the molecular details of adaptinopathies and thus also develop treatment strategies.

Published
2023
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36. Preclinical Evidence of Progesterone as a New Pharmacological Strategy in Human Adrenocortical Carcinoma Cell Lines.

Author

Tamburello M, Abate A, Rossini E, Basnet RM, Zizioli D, Cosentini D, Hantel C, Laganà M, Tiberio GAM, Grisanti S, Memo M, Berruti A, and Sigala S

Subjects
Animals, Humans, Progesterone pharmacology, Progesterone therapeutic use, Matrix Metalloproteinase 2, Zebrafish, Cell Line, Tumor, Adrenocortical Carcinoma pathology, Adrenal Cortex Neoplasms metabolism
Abstract

Background: Adrenocortical cancer (ACC) is a rare malignancy with a dismal prognosis. The treatment includes mitotane and EDP chemotherapy (etoposide, doxorubicin, and cisplatin). However, new therapeutic approaches for advanced ACC are needed, particularly targeting the metastatic process. Here, we deepen the role of progesterone as a new potential drug for ACC, in line with its antitumoral effect in other cancers., Methods: NCI-H295R, MUC-1, and TVBF-7 cell lines were used and xenografted in zebrafish embryos. Migration and invasion were studied using transwell assays, and MMP2 activity was studied using zymography. Apoptosis and cell cycle were analyzed by flow cytometry., Results: Progesterone significantly reduced xenograft tumor area and metastases formation in embryos injected with metastatic lines, MUC-1 and TVBF-7. These results were confirmed in vitro, where the reduction of invasion was mediated, at least in part, by the decrease in MMP2 levels. Progesterone exerted a long-lasting effect in metastatic cells. Progesterone caused apoptosis in NCI-H295R and MUC-1, inducing changes in the cell-cycle distribution, while autophagy was predominantly activated in TVBF-7 cells., Conclusion: Our results give support to the role of progesterone in ACC. The involvement of its analog (megestrol acetate) in reducing ACC progression in ACC patients undergoing EDP-M therapy is now under investigation in the PESETA phase II clinical study.

Published
2023
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38. Developmental safety of nirmatrelvir in zebrafish (Danio rerio) embryos.

Author

Zizioli D, Ferretti S, Mignani L, Castelli F, Tiecco G, Zanella I, and Quiros-Roldan E

Subjects
Humans, Pregnancy, Female, Animals, Rabbits, Rats, Zebrafish, Embryo, Nonmammalian abnormalities, COVID-19, Water Pollutants, Chemical toxicity
Abstract

Background: Nirmatrelvir, in combination with ritonavir, is one of the first orally available antiviral treatment for coronavirus disease 2019 (COVID-19). Symptomatic pregnant women are at increased risk for severe illness and complications that can affect the developing baby. No malformations or lower embryo-fetal survival have been observed when nirmatrelvir were administered to pregnant rats and rabbits. Safety evaluation of drugs used for treating COVID-19 also in pregnancy is urgent for public health, then in this study we further investigated nirmatrelvir developmental toxicity using zebrafish as in vivo model., Material and Methods: Using the standardized Fish Embryo Toxicity (FET) test, we first determined the lethal concentration 50 (LC50), exposing embryos from gastrula stage up to 120 hr post fertilization (hpf) and daily recording lethality. Then, we exposed embryos to five doses comprising the human therapeutic one and up to the LC50 (25 μM). Morphology was evaluated at 72 and 120 hpf., Results: Nirmatrelvir did not affect survival rate and did not induce morphological defects up to the human therapeutic dose. Exposure at higher doses (2.4× and 3× the human C max ) however resulted in decreased hatching rate, reduced growth, slower heartbeat with pericardial edema, reduction of eye dimension, absence of the swim bladder and disruption of the anterior-posterior axis, with lack of tail detachment, spinal curvature and straight and smaller head., Conclusions: Our findings in zebrafish embryos add further information about developmental nirmatrelvir safety. Further studies are needed for pharmacological safety assessment of nirmatrelvir exposure during pregnancy., (© 2022 Wiley Periodicals LLC.)

Published
2023
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39. Cabotegravir Exposure of Zebrafish ( Danio rerio ) Embryos Impacts on Neurodevelopment and Behavior.

Author

Zizioli D, Zanella I, Mignani L, Degli Antoni M, Castelli F, and Quiros-Roldan E

Subjects
Humans, Animals, Rabbits, Rats, Zebrafish, Embryo, Nonmammalian, Heart Rate, Larva, HIV Infections, Water Pollutants, Chemical toxicity
Abstract

As most new medications, Cabotegravir (CAB) was recently approved as an antiretroviral treatment of HIV infection without in-depth safety information on in utero exposure. Although no developmental toxicity in rats and rabbits was reported, recent studies demonstrated that CAB decreases pluripotency of human embryonic stem cells. CAB exposure effects during development were assessed in zebrafish embryos by the Fish Embryo Toxicity test after exposure at subtherapeutic concentrations up to 25× the human C max . Larvae behavior was assessed by the light-dark locomotion test. The expression of factors involved in neurogenesis was evaluated by whole-mount in situ hybridization. CAB did not cause gross morphological defects at low doses, although pericardial edema, uninflated swim bladder, decreased heartbeats, growth delay, and decreased hatching rate were observed at the highest concentrations. Decreased locomotion was observed even at the subtherapeutic dose, suggesting alterations of nervous system integrity. This hypothesis was supported by the observation of decreased expression of crucial factors involved in early neuronal differentiation in diencephalic and telencephalic dopaminergic areas, midbrain/hindbrain boundary, and craniofacial ganglia. These findings support CAB effects on neurogenesis in zebrafish embryos and suggest long-term follow-up of exposed infants to provide data on drug safety during pregnancy.

Published
2023
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40. Synapsin III Regulates Dopaminergic Neuron Development in Vertebrates.

Author

Faustini G, Longhena F, Muscò A, Bono F, Parrella E, La Via L, Barbon A, Pizzi M, Onofri F, Benfenati F, Missale C, Memo M, Zizioli D, and Bellucci A

Subjects
Animals, Humans, Mice, Brain-Derived Neurotrophic Factor genetics, Dopamine, Induced Pluripotent Stem Cells metabolism, Methylphenidate therapeutic use, Mice, Knockout, Zebrafish metabolism, Dopaminergic Neurons metabolism, Synapsins genetics, Synapsins metabolism
Abstract

Attention deficit and hyperactivity disorder (ADHD) is a neurodevelopmental disorder characterized by alterations in the mesocorticolimbic and nigrostriatal dopaminergic pathways. Polymorphisms in the Synapsin III (Syn III) gene can associate with ADHD onset and even affect the therapeutic response to the gold standard ADHD medication, methylphenidate (MPH), a monoamine transporter inhibitor whose efficacy appears related with the stimulation of brain-derived neurotrophic factor (BDNF). Interestingly, we previously showed that MPH can bind Syn III, which can regulate neuronal development. These observations suggest that Syn III polymorphism may impinge on ADHD onset and response to therapy by affecting BDNF-dependent dopaminergic neuron development. Here, by studying zebrafish embryos exposed to Syn III gene knock-down (KD), Syn III knock-out (ko) mice and human induced pluripotent stem cells (iPSCs)-derived neurons subjected to Syn III RNA interference, we found that Syn III governs the earliest stages of dopaminergic neurons development and that this function is conserved in vertebrates. We also observed that in mammals Syn III exerts this function acting upstream of brain-derived neurotrophic factor (BDNF)- and cAMP-dependent protein kinase 5 (Cdk5)-stimulated dendrite development. Collectively, these findings own significant implications for deciphering the biological basis of ADHD.

Published
2022
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41. Bi-Allelic Mutations in Zebrafish pank2 Gene Lead to Testicular Atrophy and Perturbed Behavior without Signs of Neurodegeneration.

Author

Mignani L, Zizioli D, Khatri D, Facchinello N, Schiavone M, De Palma G, and Finazzi D

Subjects
Animals, Phosphotransferases (Alcohol Group Acceptor) metabolism, Mutation, Coenzyme A genetics, Atrophy, Zebrafish genetics, Zebrafish metabolism, Pantothenate Kinase-Associated Neurodegeneration genetics, Pantothenate Kinase-Associated Neurodegeneration pathology
Abstract

Coenzyme A (CoA) is an essential cofactor in all living organisms, being involved in a large number of chemical reactions. Sequence variations in pantothenate kinase 2 (PANK2), the first enzyme of CoA biosynthesis, are found in patients affected by Pantothenate Kinase Associated Neurodegeneration (PKAN), one of the most common forms of neurodegeneration, with brain iron accumulation. Knowledge about the biochemical and molecular features of this disorder has increased a lot in recent years. Nonetheless, the main culprit of the pathology is not well defined, and no treatment option is available yet. In order to contribute to the understanding of this disease and facilitate the search for therapies, we explored the potential of the zebrafish animal model and generated lines carrying biallelic mutations in the pank2 gene. The phenotypic characterization of pank2 -mutant embryos revealed anomalies in the development of venous vascular structures and germ cells. Adult fish showed testicular atrophy and altered behavioral response in an anxiety test but no evident signs of neurodegeneration. The study suggests that selected cell and tissue types show a higher vulnerability to pank2 deficiency in zebrafish. Deciphering the biological basis of this phenomenon could provide relevant clues for better understanding and treating PKAN.

Published
2022
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42. Hyperactive Akt1 Signaling Increases Tumor Progression and DNA Repair in Embryonal Rhabdomyosarcoma RD Line and Confers Susceptibility to Glycolysis and Mevalonate Pathway Inhibitors.

Author

Codenotti S, Zizioli D, Mignani L, Rezzola S, Tabellini G, Parolini S, Giacomini A, Asperti M, Poli M, Mandracchia D, Vezzoli M, Bernardi S, Russo D, Mitola S, Monti E, Triggiani L, Tomasini D, Gastaldello S, Cassandri M, Rota R, Marampon F, and Fanzani A

Subjects
Animals, Child, DNA Repair, DNA-Activated Protein Kinase genetics, Deoxyglucose, Doxorubicin pharmacology, Glucose, Glycolysis, Hexokinase metabolism, Histones metabolism, Humans, Ki-67 Antigen metabolism, Lovastatin, MTOR Inhibitors, Mevalonic Acid, Oxidoreductases metabolism, Phosphatidylinositol 3-Kinases metabolism, Phosphatidylinositols, Ribosomal Protein S6 Kinases, 70-kDa metabolism, Sirolimus pharmacology, TOR Serine-Threonine Kinases metabolism, Zebrafish genetics, Proto-Oncogene Proteins c-akt metabolism, Rhabdomyosarcoma, Embryonal drug therapy
Abstract

In pediatric rhabdomyosarcoma (RMS), elevated Akt signaling is associated with increased malignancy. Here, we report that expression of a constitutively active, myristoylated form of Akt1 (myrAkt1) in human RMS RD cells led to hyperactivation of the mammalian target of rapamycin (mTOR)/70-kDa ribosomal protein S6 kinase (p70S6K) pathway, resulting in the loss of both MyoD and myogenic capacity, and an increase of Ki67 expression due to high cell mitosis. MyrAkt1 signaling increased migratory and invasive cell traits, as detected by wound healing, zymography, and xenograft zebrafish assays, and promoted repair of DNA damage after radiotherapy and doxorubicin treatments, as revealed by nuclear detection of phosphorylated H2A histone family member X (γH2AX) through activation of DNA-dependent protein kinase (DNA-PK). Treatment with synthetic inhibitors of phosphatidylinositol-3-kinase (PI3K) and Akt was sufficient to completely revert the aggressive cell phenotype, while the mTOR inhibitor rapamycin failed to block cell dissemination. Furthermore, we found that pronounced Akt1 signaling increased the susceptibility to cell apoptosis after treatments with 2-deoxy-D-glucose (2-DG) and lovastatin, enzymatic inhibitors of hexokinase, and 3-hydroxy-3-methyl-glutaryl-coenzyme A reductase (HMGCR), especially in combination with radiotherapy and doxorubicin. In conclusion, these data suggest that restriction of glucose metabolism and the mevalonate pathway, in combination with standard therapy, may increase therapy success in RMS tumors characterized by a dysregulated Akt signaling.

Published
2022
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43. Pro-Angiogenetic Effects of Purified Extracts from Helix aspersa during Zebrafish Development.

Author

Zizioli D, Mastinu A, Muscò A, Bonini SA, Finazzi D, Avisani R, Kron Morelli GB, Pecorelli S, and Memo M

Abstract

Helix aspersa is a species of land snail belonging to the Helicidae family, widespread in the Mediterranean and continental area up to Northern Europe. In some areas it is appreciated as a food, but is mostly considered a parasite of gardens and cultivated fields. The mucus of Helix aspersa has found multiple applications in the cosmetic and health fields. In the present study, we investigated for the first time the angiogenetic properties of purified extracts from Helix aspersa using a transgenic zebrafish line Tg ( kdrl :EGFP). The angiogenesis induced by purified snail extracts was demonstrated by their capability to increase the three well-established parameters of angiogenesis: generation of intersegmental vessels, modeling of caudal venous plexus, and formation of sub-intestinal venous plexus. The effects appeared to be mediated by the vascular endothelial growth factor (VEGF) pathway, being prevented by pretreatment of embryos with the selective VEGF receptor antagonist SU5416, and supported by the increased VEGF mRNA levels found in snail-extract-treated embryos. Insufficient vascular supply is underlined by low VEGF signaling, primarily because of its indispensable role in preventing capillary loss. Our findings might have a pharmacological impact by counteracting VEGF hypofunction and promoting angiogenesis to maintain adequate microvascular and vascular density in normal and suffering tissues and organs.

Published
2022
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44. Cytotoxic effects of targeted agent alone or with chemotherapy in the treatment of adenoid cystic carcinoma: a preclinical study.

Author

Savarese T, Abate A, Basnet RM, Lorini L, Gurizzan C, Tomasoni M, Lombardi D, Tomasini D, Zizioli D, Memo M, Berruti A, Bonini SA, Sigala S, and Bossi P

Subjects
Animals, Cisplatin pharmacology, Cisplatin therapeutic use, Doxorubicin pharmacology, Doxorubicin therapeutic use, Humans, Neoplasm Recurrence, Local drug therapy, Zebrafish, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Carcinoma, Adenoid Cystic drug therapy, Carcinoma, Adenoid Cystic pathology
Abstract

Adenoid cystic carcinoma (ACC) is a rare malignancy characterized by high incidence of relapse. When relapsing, ACC has an indolent but relentless behaviour, thus leading to a poor long-term prognosis. The treatment of choice of relapsing ACC remains surgery followed by radiotherapy, whenever feasible. Therapeutic weapons are limited to systemic drugs. The most widely used chemotherapy regimen is the combination of cisplatin and doxorubicin, however with low response rate and not long lasting; there is also a lack of alternatives for second line therapies in case of disease progression. Therefore, a more comprehensive strategy aimed at identifying at preclinical level the most promising drugs or combination is clearly needed. In this study, the cytotoxic effects of two standard chemotherapy drugs, cisplatin and doxorubicin, and of five targeted therapy-drugs was tested in vitro, on an h-TERT immortalized ACC cell line, and in vivo, on zebrafish embryos with ACC tumoral cell xenograft. Then, combinations of one standard chemotherapy drug plus one targeted therapy drug were also evaluated, in order to find the best treatment strategy for ACC. Data obtained demonstrated that both vorinostat and olaparib significantly increased the standard chemotherapy cytotoxic effects, suggesting new interesting therapeutic options for ACC., (© 2022. The Author(s).)

Published
2022
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45. An exploratory pilot study on the involvement of APOE, HFE, C9ORF72 variants and comorbidities in neurocognitive and physical performance in a group of HIV-infected people.

Author

Zanella I, Zacchi E, Fornari C, Fumarola B, Antoni MD, Zizioli D, and Quiros-Roldan E

Subjects
C9orf72 Protein genetics, Genotype, Hemochromatosis Protein genetics, Humans, Inflammation, Middle Aged, Neuropsychological Tests, Pilot Projects, Apolipoproteins E genetics, HIV Infections complications, HIV Infections epidemiology, HIV Infections genetics, Physical Functional Performance
Abstract

Cognitive decline of aging is modulated by chronic inflammation and comorbidities. In people with HIV-infection (PWH) it may also be affected by HIV-induced inflammation, lifestyle and long-term effects of antiretroviral therapies (ART). The role of genetics in the susceptibility to HIV-associated neurocognitive disorders (HAND) is not fully understood. Here we explored the possible relations among variants in 3 genes involved in inflammation and neurodegenerative disorders (APOE: ε2/ε3/ε4; HFE: H63D; C9ORF72: hexanucleotide expansions ≥ 9 repeats), cognitive/functional impairment (MiniMental State Examination MMSE, Clock Drawing Test CDT, Short Physical Performance Battery SPPB), comorbidities and HIV-related variables in a cohort of > 50 years old PWH (n = 60) with at least 10 years efficient ART. Patients with diabetes or hypertension showed significantly lower MMSE (p = .031) or SPPB (p = .010) scores, respectively, while no relations between HIV-related variables and cognitive/functional scores were observed. Patients with at least one APOEε3 allele had higher CDT scores (p = .019), APOEε2/ε4 patients showing the lowest scores in all tests. Patients with HFE-H63D variant showed more frequently hypertriglyceridemia (p = .023) and those harboring C9ORF72 expansions > 9 repeats had higher CD4 + -cell counts (p = .032) and CD4% (p = .041). Multiple linear regression analysis computed to verify possible associations among cognitive/functional scores and all variables further suggested positive association between higher CDT scores and the presence of at least one APOEε3 allele (2,2; 95% CI [0,03 0,8]; p = .037), independent of other variables, although the model did not reach the statistical significance (p = .14). These data suggest that in PWH on efficient ART cognitive abilities and physical performances may be partly associated with comorbidities and genetic background. However, further analyses are needed to establish whether they could be also dependent and influenced by comorbidities and genetic background., (© 2022. The Author(s).)

Published
2022
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47. Coenzyme a Biochemistry: From Neurodevelopment to Neurodegeneration.

Author

Mignani L, Gnutti B, Zizioli D, and Finazzi D

Abstract

Coenzyme A (CoA) is an essential cofactor in all living organisms. It is involved in a large number of biochemical processes functioning either as an activator of molecules with carbonyl groups or as a carrier of acyl moieties. Together with its thioester derivatives, it plays a central role in cell metabolism, post-translational modification, and gene expression. Furthermore, recent studies revealed a role for CoA in the redox regulation by the S-thiolation of cysteine residues in cellular proteins. The intracellular concentration and distribution in different cellular compartments of CoA and its derivatives are controlled by several extracellular stimuli such as nutrients, hormones, metabolites, and cellular stresses. Perturbations of the biosynthesis and homeostasis of CoA and/or acyl-CoA are connected with several pathological conditions, including cancer, myopathies, and cardiomyopathies. In the most recent years, defects in genes involved in CoA production and distribution have been found in patients affected by rare forms of neurodegenerative and neurodevelopmental disorders. In this review, we will summarize the most relevant aspects of CoA cellular metabolism, their role in the pathogenesis of selected neurodevelopmental and neurodegenerative disorders, and recent advancements in the search for therapeutic approaches for such diseases.

Published
2021
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48. Cisplatin Cytotoxicity in Human Testicular Germ Cell Tumor Cell Lines Is Enhanced by the CDK4/6 Inhibitor Palbociclib.

Author

Rossini E, Bosatta V, Abate A, Fragni M, Salvi V, Basnet RM, Zizioli D, Bosisio D, Piovani G, Valcamonico F, Mirabella G, Berruti A, Memo M, and Sigala S

Subjects
Animals, Cell Line, Tumor, Cisplatin pharmacology, Cisplatin therapeutic use, Cyclin-Dependent Kinase 4, Humans, Male, Neoplasms, Germ Cell and Embryonal, Piperazines, Pyridines, Zebrafish, Antineoplastic Agents pharmacology, Antineoplastic Agents therapeutic use, Testicular Neoplasms drug therapy
Abstract

Background: Cisplatin-based chemotherapy is the mainstay of pharmacological treatment of testicular germ cell tumors (TGCTs) that, together with early diagnosis, surgery, and/or radiotherapy, has dramatically improved the prognosis. However, under the pressure of such pharmacological therapy (both classical cytotoxic drugs and targeted therapy), cancer cells may develop resistance. Thus, combination therapy that may include cytotoxic drugs and targeted therapy could offer an advantage to curing cancers. Here, we investigated the in vitro and in vivo antitumor activity of cisplatin, as a single-agent or in combination with palbociclib., Patients and Methods: The cell viability of Ntera-2/cl.D1 (NT2/D1) and 833K after exposure to palbociclib and/or cisplatin was evaluated by MTT dye reduction assay and by ATPLite Luminescence Assay. Gene and protein expression was evaluated by quantitative reverse transcription polymerase chain reaction and by western blot. Flow cytometric cell-cycle analysis was performed, as well. The in vivo experiments were conducted on NT2/D1 xenografts in AB zebrafish embryos exposed to the drugs., Results: Palbociclib and cisplatin decreased TGCT cell viability both in vitro and in vivo. This effect was additive when cells were exposed to the drug combination. In the NT2/D1 cell lines, the drug combination also exerted a positive effect with regard to delaying cell recovery after the toxic insult. In the combination experiments, cisplatin-induced cell accumulation in G2/M was predominant compared with the palbociclib effect., Conclusions: These results could provide the rationale for developing further studies to improve the pharmacological treatment of TGCTs, but they must be demonstrated in a dedicated clinical trial., (Copyright © 2021. Published by Elsevier Inc.)

Published
2021
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49. Tenofovir, Another Inexpensive, Well-Known and Widely Available Old Drug Repurposed for SARS-COV-2 Infection.

Author

Zanella I, Zizioli D, Castelli F, and Quiros-Roldan E

Abstract

Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2) infection is spreading worldwide with different clinical manifestations. Age and comorbidities may explain severity in critical cases and people living with human immunodeficiency virus (HIV) might be at particularly high risk for severe progression. Nonetheless, current data, although sometimes contradictory, do not confirm higher morbidity, risk of more severe COVID-19 or higher mortality in HIV-infected people with complete access to antiretroviral therapy (ART). A possible protective role of ART has been hypothesized to explain these observations. Anti-viral drugs used to treat HIV infection have been repurposed for COVID-19 treatment; this is also based on previous studies on severe acute respiratory syndrome virus (SARS-CoV) and Middle East respiratory syndrome virus (MERS-CoV). Among them, lopinavir/ritonavir, an inhibitor of viral protease, was extensively used early in the pandemic but it was soon abandoned due to lack of effectiveness in clinical trials. However, remdesivir, a nucleotide analog that acts as reverse-transcriptase inhibitor, which was tested early during the pandemic because of its wide range of antiviral activity against several RNA viruses and its safety profile, is currently the only antiviral medication approved for COVID-19. Tenofovir, another nucleotide analog used extensively for HIV treatment and pre-exposure prophylaxis (PrEP), has also been hypothesized as effective in COVID-19. No data on tenofovir's efficacy in coronavirus infections other than COVID-19 are currently available, although information relating to SARS-CoV-2 infection is starting to come out. Here, we review the currently available evidence on tenofovir's efficacy against SARS-CoV-2.

Published
2021
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50. Caffeine Inhibits Direct and Indirect Angiogenesis in Zebrafish Embryos.

Author

Basnet RM, Zizioli D, Muscò A, Finazzi D, Sigala S, Rossini E, Tobia C, Guerra J, Presta M, and Memo M

Subjects
Animals, Cell Line, Tumor, Embryo, Nonmammalian, Embryonic Development drug effects, Gene Expression Regulation, Developmental drug effects, Heterografts, Humans, In Situ Hybridization, Neovascularization, Pathologic genetics, Neovascularization, Pathologic pathology, Neovascularization, Physiologic genetics, Zebrafish genetics, Zebrafish growth & development, Caffeine pharmacology, Fibroblast Growth Factor 2 genetics, Neovascularization, Pathologic drug therapy, Neovascularization, Physiologic drug effects
Abstract

In this study, we report the effects of caffeine on angiogenesis in zebrafish embryos both during normal development and after exposure to Fibroblast Growth Factor 2 (FGF2). As markers of angiogenesis, we measured the length and width of intersegmental vessels (ISVs), performed whole-mount in situ hybridization with fli1 and cadh5 vascular markers, and counted the number of interconnecting vessels (ICVs) in sub-intestinal venous plexus (SIVP). In addition, we measured angiogenesis after performing zebrafish yolk membrane (ZFYM) assay with microinjection of fibroblast growth factor 2 (FGF2) and perivitelline tumor xenograft assay with microinjection of tumorigenic FGF2-overexpressing endothelial (FGF2-T-MAE) cells. The results showed that caffeine treatment causes a shortening and thinning of ISVs along with a decreased expression of the vascular marker genes and a decrease in the number of ICVs in the SIVP. Caffeine was also able to block angiogenesis induced by exogenous FGF2 or FGF2-producing cells. Overall, our results are suggestive of the inhibitory effect of caffeine in both direct and indirect angiogenesis.

Published
2021
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