Your search keyword '"Ceruti A"' showing total 141 results

1. An unusual neurological manifestation of granulomatosis with polyangiitis: A case report and literature review

Author

Nikhil N. Tarte, Ronald Ceruti, and Vasudev Tati

Subjects

aspirin, central nervous system, dysphagia, granulomatosis with polyangiitis, hypercoagulable state, stroke, Medicine, Medicine (General), R5-920

Abstract

Abstract Ischemic stroke is an incredibly rare manifestation of granulomatosis with polyangiitis. It is important for the clinician to be aware of this unusual complication so that efforts can be made to reduce the risk of this event.

Published

2020

2. The Concise Guide to PHARMACOLOGY 2023/24: G protein-coupled receptors

Author

Alexander, SPH, Christopoulos, A, Davenport, AP, Kelly, E, Mathie, AA, Peters, JA, Veale, EL, Armstrong, JF, Faccenda, E, Harding, SD, Davies, JA, Abbracchio, MP, Abraham, G, Agoulnik, A, Alexander, W, Al-hosaini, K, Back, M, Baker, JG, Barnes, NM, Bathgate, R, Beaulieu, J-M, Beck-Sickinger, AG, Behrens, M, Bernstein, KE, Bettler, B, Birdsall, NJM, Blaho, V, Boulay, F, Bousquet, C, Brauner-Osborne, H, Burnstock, G, Calo, G, Castano, JP, Catt, KJ, Ceruti, S, Chazot, P, Chiang, N, Chini, B, Chun, J, Cianciulli, A, Civelli, O, Clapp, LH, Couture, R, Cox, HM, Csaba, Z, Dahlgren, C, Dent, G, Douglas, SD, Dournaud, P, Eguchi, S, Escher, E, Filardo, EJ, Fong, T, Fumagalli, M, Gainetdinov, RR, Garelja, ML, de Gasparo, M, Gerard, C, Gershengorn, M, Gobeil, F, Goodfriend, TL, Goudet, C, Gratz, L, Gregory, KJ, Gundlach, AL, Hamann, J, Hanson, J, Hauger, RL, Hay, DL, Heinemann, A, Herr, D, Hollenberg, MD, Holliday, ND, Horiuchi, M, Hoyer, D, Hunyady, L, Husain, A, Ijzerman, AP, Inagami, T, Jacobson, KA, Jensen, RT, Jockers, R, Jonnalagadda, D, Karnik, S, Kaupmann, K, Kemp, J, Kennedy, C, Kihara, Y, Kitazawa, T, Kozielewicz, P, Kreienkamp, H-J, Kukkonen, JP, Langenhan, T, Larhammar, D, Leach, K, Lecca, D, Lee, JD, Leeman, SE, Leprince, J, Li, XX, Lolait, SJ, Lupp, A, Macrae, R, Maguire, J, Malfacini, D, Mazella, J, McArdle, CA, Melmed, S, Michel, MC, Miller, LJ, Mitolo, V, Mouillac, B, Mueller, CE, Murphy, PM, Nahon, J-L, Ngo, T, Norel, X, Nyimanu, D, O'Carroll, A-M, Offermanns, S, Panaro, MA, Parmentier, M, Pertwee, RG, Pin, J-P, Prossnitz, ER, Quinn, M, Ramachandran, R, Ray, M, Reinscheid, RK, Rondard, P, Rovati, GE, Ruzza, C, Sanger, GJ, Schoeneberg, T, Schulte, G, Schulz, S, Segaloff, DL, Serhan, CN, Singh, KD, Smith, CM, Stoddart, LA, Sugimoto, Y, Summers, R, Tan, VP, Thal, D, Thomas, WW, Timmermans, PBMWM, Tirupula, K, Toll, L, Tulipano, G, Unal, H, Unger, T, Valant, C, Vanderheyden, P, Vaudry, D, Vaudry, H, Vilardaga, J-P, Walker, CS, Wang, JM, Ward, DT, Wester, H-J, Willars, GB, Williams, TL, Woodruff, TM, Yao, C, Ye, RD, Alexander, SPH, Christopoulos, A, Davenport, AP, Kelly, E, Mathie, AA, Peters, JA, Veale, EL, Armstrong, JF, Faccenda, E, Harding, SD, Davies, JA, Abbracchio, MP, Abraham, G, Agoulnik, A, Alexander, W, Al-hosaini, K, Back, M, Baker, JG, Barnes, NM, Bathgate, R, Beaulieu, J-M, Beck-Sickinger, AG, Behrens, M, Bernstein, KE, Bettler, B, Birdsall, NJM, Blaho, V, Boulay, F, Bousquet, C, Brauner-Osborne, H, Burnstock, G, Calo, G, Castano, JP, Catt, KJ, Ceruti, S, Chazot, P, Chiang, N, Chini, B, Chun, J, Cianciulli, A, Civelli, O, Clapp, LH, Couture, R, Cox, HM, Csaba, Z, Dahlgren, C, Dent, G, Douglas, SD, Dournaud, P, Eguchi, S, Escher, E, Filardo, EJ, Fong, T, Fumagalli, M, Gainetdinov, RR, Garelja, ML, de Gasparo, M, Gerard, C, Gershengorn, M, Gobeil, F, Goodfriend, TL, Goudet, C, Gratz, L, Gregory, KJ, Gundlach, AL, Hamann, J, Hanson, J, Hauger, RL, Hay, DL, Heinemann, A, Herr, D, Hollenberg, MD, Holliday, ND, Horiuchi, M, Hoyer, D, Hunyady, L, Husain, A, Ijzerman, AP, Inagami, T, Jacobson, KA, Jensen, RT, Jockers, R, Jonnalagadda, D, Karnik, S, Kaupmann, K, Kemp, J, Kennedy, C, Kihara, Y, Kitazawa, T, Kozielewicz, P, Kreienkamp, H-J, Kukkonen, JP, Langenhan, T, Larhammar, D, Leach, K, Lecca, D, Lee, JD, Leeman, SE, Leprince, J, Li, XX, Lolait, SJ, Lupp, A, Macrae, R, Maguire, J, Malfacini, D, Mazella, J, McArdle, CA, Melmed, S, Michel, MC, Miller, LJ, Mitolo, V, Mouillac, B, Mueller, CE, Murphy, PM, Nahon, J-L, Ngo, T, Norel, X, Nyimanu, D, O'Carroll, A-M, Offermanns, S, Panaro, MA, Parmentier, M, Pertwee, RG, Pin, J-P, Prossnitz, ER, Quinn, M, Ramachandran, R, Ray, M, Reinscheid, RK, Rondard, P, Rovati, GE, Ruzza, C, Sanger, GJ, Schoeneberg, T, Schulte, G, Schulz, S, Segaloff, DL, Serhan, CN, Singh, KD, Smith, CM, Stoddart, LA, Sugimoto, Y, Summers, R, Tan, VP, Thal, D, Thomas, WW, Timmermans, PBMWM, Tirupula, K, Toll, L, Tulipano, G, Unal, H, Unger, T, Valant, C, Vanderheyden, P, Vaudry, D, Vaudry, H, Vilardaga, J-P, Walker, CS, Wang, JM, Ward, DT, Wester, H-J, Willars, GB, Williams, TL, Woodruff, TM, Yao, C, and Ye, RD

Abstract

The Concise Guide to PHARMACOLOGY 2023/24 is the sixth in this series of biennial publications. The Concise Guide provides concise overviews, mostly in tabular format, of the key properties of approximately 1800 drug targets, and about 6000 interactions with about 3900 ligands. There is an emphasis on selective pharmacology (where available), plus links to the open access knowledgebase source of drug targets and their ligands (https://www.guidetopharmacology.org), which provides more detailed views of target and ligand properties. Although the Concise Guide constitutes almost 500 pages, the material presented is substantially reduced compared to information and links presented on the website. It provides a permanent, citable, point-in-time record that will survive database updates. The full contents of this section can be found at http://onlinelibrary.wiley.com/doi/bph.16177. G protein-coupled receptors are one of the six major pharmacological targets into which the Guide is divided, with the others being: ion channels, nuclear hormone receptors, catalytic receptors, enzymes and transporters. These are presented with nomenclature guidance and summary information on the best available pharmacological tools, alongside key references and suggestions for further reading. The landscape format of the Concise Guide is designed to facilitate comparison of related targets from material contemporary to mid-2023, and supersedes data presented in the 2021/22, 2019/20, 2017/18, 2015/16 and 2013/14 Concise Guides and previous Guides to Receptors and Channels. It is produced in close conjunction with the Nomenclature and Standards Committee of the International Union of Basic and Clinical Pharmacology (NC-IUPHAR), therefore, providing official IUPHAR classification and nomenclature for human drug targets, where appropriate.

Published

2023

3. Which patient may benefit the most from penile prosthesis implantation?

Author

La Croce, Giovanni, primary, Schifano, Nicolò, additional, Pescatori, Edoardo, additional, Caraceni, Enrico, additional, Colombo, Fulvio, additional, Bettocchi, Carlo, additional, Carrino, Maurizio, additional, Vitarelli, Antonio, additional, Pozza, Diego, additional, Fiordelise, Stefano, additional, Varvello, Francesco, additional, Paradiso, Matteo, additional, Silvani, Mauro, additional, Mondaini, Nicola, additional, Natali, Alessandro, additional, Falcone, Marco, additional, Ceruti, Carlo, additional, Salonia, Andrea, additional, Antonini, Gabriele, additional, Cai, Tommaso, additional, Palmieri, Alessandro, additional, Dehò, Federico, additional, and Capogrosso, Paolo, additional

Published

2022

4. Pharmacological and clinical monitoring in children with acute lymphoblastic leukemia treated with a biogeneric PEG‐l‐asparaginase product

Author

Matteo, Cristina, primary, Colombini, Antonella, additional, Bettini, Laura Rachele, additional, Porcu, Luca, additional, Barzaghi, Silvia, additional, Ceruti, Tommaso, additional, Silvestri, Daniela, additional, Amoroso, Angela, additional, Dell'Acqua, Fabiola, additional, Gotti, Giacomo, additional, Nastasi, Claudia, additional, Zucchetti, Massimo, additional, and Rizzari, Carmelo, additional

Published

2022

5. Effects of direct‐acting antiviral agents on lipid and glucose profile in HCV patients with type 2 diabetes: A real‐life Italian experience

Author

Dalbeni, Andrea, primary, Villani, Rosanna, additional, Bevilacqua, Michele, additional, Sacco, Federica, additional, Faccincani, Diego, additional, Cattazzo, Filippo, additional, Cavallone, Francesco, additional, Mantovani, Anna, additional, Ceruti, Vittoria, additional, Ieluzzi, Donatella, additional, Paon, Veronica, additional, Mantovani, Alessandro, additional, Serviddio, Gaetano, additional, and Sacerdoti, David, additional

Published

2022

6. Cutaneous sensitivity modulation by Aquaphilus dolomiae extract‐G3 on in vitro models of neuro‐inflammation

Author

F. Lestienne, Hélène Duplan, S. Carrere, N. Castex-Rizzi, C. Viode, I. Ceruti, and Sandrine Bessou-Touya

Subjects

Keratinocytes, 0301 basic medicine, Substance P, Dermatology, Pharmacology, Dermatitis, Atopic, Sensitive skin, 030207 dermatology & venereal diseases, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Humans, Medicine, Skin, Inflammation, Neurogenic inflammation, Innate immune system, Corneocyte, integumentary system, business.industry, Atopic dermatitis, medicine.disease, Neisseriaceae, 030104 developmental biology, Infectious Diseases, chemistry, business, Histamine, Ex vivo

Abstract

Background Inflammatory skin disorders, including atopic dermatitis (AD), associated pruritus and sensitive skin, have a complex multifactorial pathogenesis including neurogenic inflammation involving the release in blood and skin of neurotransmitters such as substance P (SP). Aims and methods In vitro models evaluated the effect of the original biological extract of Aquaphilus dolomiae extract-G3 (ADE-G3) on cutaneous neurogenic inflammation. Results ADE-G3 significantly inhibited SP-stimulated release of IL-1β and TNF-α from normal human epidermal keratinocytes; significantly and dose-dependently inhibited SP-stimulated activation of human mast cells; significantly inhibited veratridine-stimulated release of SP from human sensory neurons; modulated expression of genes involved in lipid synthesis, innate immunity, corneocyte scaffolding and epidermal differentiation in a histamine-sensitized reconstructed human epidermis model; and, when applied topically to ex vivo human explants, inhibited IL-8 and histamine release. Conclusions Topically applied ADE-G3, once formulated, may improve neuro-inflammation in patients with inflammatory skin disorders.

Published

2020

7. An unusual neurological manifestation of granulomatosis with polyangiitis: A case report and literature review

Author

Ronald Ceruti, Nikhil N. Tarte, and Vasudev H. Tati

Subjects

medicine.medical_specialty, aspirin, dysphagia, hypercoagulable state, lcsh:Medicine, Case Report, Case Reports, 030204 cardiovascular system & hematology, vasculitis, 03 medical and health sciences, 0302 clinical medicine, medicine, Neurological manifestation, Stroke, lcsh:R5-920, granulomatosis with polyangiitis, business.industry, fungi, lcsh:R, food and beverages, General Medicine, medicine.disease, central nervous system, Dermatology, Wegener's granulomatosis, stroke, 030220 oncology & carcinogenesis, Ischemic stroke, Granulomatosis with polyangiitis, business, Complication, Vasculitis, lcsh:Medicine (General)

Abstract

Ischemic stroke is an incredibly rare manifestation of granulomatosis with polyangiitis. It is important for the clinician to be aware of this unusual complication so that efforts can be made to reduce the risk of this event.

Published

2020

8. Influence of the degree of hydrolysis on the bioactive properties of whey protein hydrolysates using Alcalase®

Author

Enrique José Mammarella, Agustina Eberhardt, Fernanda Marino, Guillermo Adrian Sihufe, Roberto Julio Ceruti, Emilse Camila López, and Ricardo Martín Manzo

Subjects

ANGIOTENSIN-CONVERTING ENZYME, Whey protein, Otras Ingenierías y Tecnologías, Chemistry, Process Chemistry and Technology, 0402 animal and dairy science, DAIRY TECHNOLOGY, Bioengineering, WHEY PROTEIN CONCENTRATE, INGENIERÍAS Y TECNOLOGÍAS, 04 agricultural and veterinary sciences, 040401 food science, 040201 dairy & animal science, Hydrolysate, Degree (temperature), Alimentos y Bebidas, Hydrolysis, 0404 agricultural biotechnology, Food science, FUNCTIONAL PROPERTIES, Food Science

Abstract

Whey protein concentrate was enzymatically hydrolysed at several time courses using the commercial preparation Alcalase® 2.4 L, different hydrolysates were achieved, and the effect of degree of hydrolysis (DH) on both technological and biological properties was studied. Results have shown that solubility, antioxidant and ACE inhibition activities were increased as DH was also augmented from about 8 to 17%. RP-HPLC studies also revealed a decrease in hydrophobicity when samples were hydrolysed in comparison with controls. When the enzyme hydrolytic action was augmented, it stimulated both the bioactivity of whey protein and relevant technological properties, allowing these hydrolysates to be employed as additives in the development of food formulations. Fil: Eberhardt, Agustina. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Santa Fe. Instituto de Desarrollo Tecnológico para la Industria Química. Universidad Nacional del Litoral. Instituto de Desarrollo Tecnológico para la Industria Química; Argentina Fil: López, Emilse Camila. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Santa Fe. Instituto de Desarrollo Tecnológico para la Industria Química. Universidad Nacional del Litoral. Instituto de Desarrollo Tecnológico para la Industria Química; Argentina Fil: Ceruti, Roberto Julio. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Santa Fe. Instituto de Desarrollo Tecnológico para la Industria Química. Universidad Nacional del Litoral. Instituto de Desarrollo Tecnológico para la Industria Química; Argentina Fil: Marino, Fernanda. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Santa Fe. Instituto de Desarrollo Tecnológico para la Industria Química. Universidad Nacional del Litoral. Instituto de Desarrollo Tecnológico para la Industria Química; Argentina Fil: Mammarella, Enrique José. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Santa Fe. Instituto de Desarrollo Tecnológico para la Industria Química. Universidad Nacional del Litoral. Instituto de Desarrollo Tecnológico para la Industria Química; Argentina Fil: Manzo, Ricardo Martín. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Santa Fe. Instituto de Desarrollo Tecnológico para la Industria Química. Universidad Nacional del Litoral. Instituto de Desarrollo Tecnológico para la Industria Química; Argentina Fil: Sihufe, Guillermo Adrian. Consejo Nacional de Investigaciones Científicas y Técnicas. Centro Científico Tecnológico Conicet - Santa Fe. Instituto de Desarrollo Tecnológico para la Industria Química. Universidad Nacional del Litoral. Instituto de Desarrollo Tecnológico para la Industria Química; Argentina

Published

2019

9. THE CONCISE GUIDE TO PHARMACOLOGY 2021/22: G protein‐coupled receptors

Author

Alexander, Stephen P H, primary, Christopoulos, Arthur, additional, Davenport, Anthony P, additional, Kelly, Eamonn, additional, Mathie, Alistair, additional, Peters, John A, additional, Veale, Emma L, additional, Armstrong, Jane F, additional, Faccenda, Elena, additional, Harding, Simon D, additional, Pawson, Adam J, additional, Southan, Christopher, additional, Davies, Jamie A, additional, Abbracchio, Maria Pia, additional, Alexander, Wayne, additional, Al‐hosaini, Khaled, additional, Bäck, Magnus, additional, Barnes, Nicholas M., additional, Bathgate, Ross, additional, Beaulieu, Jean‐Martin, additional, Bernstein, Kenneth E., additional, Bettler, Bernhard, additional, Birdsall, Nigel J.M., additional, Blaho, Victoria, additional, Boulay, Francois, additional, Bousquet, Corinne, additional, Bräuner‐Osborne, Hans, additional, Burnstock, Geoffrey, additional, Caló, Girolamo, additional, Castaño, Justo P., additional, Catt, Kevin J., additional, Ceruti, Stefania, additional, Chazot, Paul, additional, Chiang, Nan, additional, Chini, Bice, additional, Chun, Jerold, additional, Cianciulli, Antonia, additional, Civelli, Olivier, additional, Clapp, Lucie H., additional, Couture, Réjean, additional, Csaba, Zsolt, additional, Dahlgren, Claes, additional, Dent, Gordon, additional, Singh, Khuraijam Dhanachandra, additional, Douglas, Steven D., additional, Dournaud, Pascal, additional, Eguchi, Satoru, additional, Escher, Emanuel, additional, Filardo, Edward J., additional, Fong, Tung, additional, Fumagalli, Marta, additional, Gainetdinov, Raul R, additional, Gasparo, Marc de, additional, Gerard, Craig, additional, Gershengorn, Marvin, additional, Gobeil, Fernand, additional, Goodfriend, Theodore L., additional, Goudet, Cyril, additional, Gregory, Karen J., additional, Gundlach, Andrew L., additional, Hamann, Jörg, additional, Hanson, Julien, additional, Hauger, Richard L., additional, Hay, Debbie L., additional, Heinemann, Akos, additional, Hollenberg, Morley D., additional, Holliday, Nicholas D., additional, Horiuchi, Mastgugu, additional, Hoyer, Daniel, additional, Hunyady, László, additional, Husain, Ahsan, additional, IJzerman, Adriaan P., additional, Inagami, Tadashi, additional, Jacobson, Kenneth A., additional, Jensen, Robert T., additional, Jockers, Ralf, additional, Jonnalagadda, Deepa, additional, Karnik, Sadashiva, additional, Kaupmann, Klemens, additional, Kemp, Jacqueline, additional, Kennedy, Charles, additional, Kihara, Yasuyuki, additional, Kitazawa, Takio, additional, Kozielewicz, Pawel, additional, Kreienkamp, Hans‐Jürgen, additional, Kukkonen, Jyrki P., additional, Langenhan, Tobias, additional, Leach, Katie, additional, Lecca, Davide, additional, Lee, John D., additional, Leeman, Susan E., additional, Leprince, Jérôme, additional, Li, Xaria X., additional, Williams, Tom Lloyd, additional, Lolait, Stephen J., additional, Lupp, Amelie, additional, Macrae, Robyn, additional, Maguire, Janet, additional, Mazella, Jean, additional, McArdle, Craig A., additional, Melmed, Shlomo, additional, Michel, Martin C., additional, Miller, Laurence J., additional, Mitolo, Vincenzo, additional, Mouillac, Bernard, additional, Müller, Christa E., additional, Murphy, Philip, additional, Nahon, Jean‐Louis, additional, Ngo, Tony, additional, Norel, Xavier, additional, Nyimanu, Duuamene, additional, O’Carroll, Anne‐Marie, additional, Offermanns, Stefan, additional, Panaro, Maria Antonietta, additional, Parmentier, Marc, additional, Pertwee, Roger G., additional, Pin, Jean‐Philippe, additional, Prossnitz, Eric R., additional, Quinn, Mark, additional, Ramachandran, Rithwik, additional, Ray, Manisha, additional, Reinscheid, Rainer K., additional, Rondard, Philippe, additional, Rovati, G. Enrico, additional, Ruzza, Chiara, additional, Sanger, Gareth J., additional, Schöneberg, Torsten, additional, Schulte, Gunnar, additional, Schulz, Stefan, additional, Segaloff, Deborah L., additional, Serhan, Charles N., additional, Stoddart, Leigh A., additional, Sugimoto, Yukihiko, additional, Summers, Roger, additional, Tan, Valerie P., additional, Thal, David, additional, Thomas, Walter (Wally), additional, Timmermans, Pieter B. M. W. M., additional, Tirupula, Kalyan, additional, Tulipano, Giovanni, additional, Unal, Hamiyet, additional, Unger, Thomas, additional, Valant, Celine, additional, Vanderheyden, Patrick, additional, Vaudry, David, additional, Vaudry, Hubert, additional, Vilardaga, Jean‐Pierre, additional, Walker, Christopher S., additional, Wang, Ji Ming, additional, Ward, Donald T., additional, Wester, Hans‐Jürgen, additional, Willars, Gary B, additional, Woodruff, Trent M., additional, Yao, Chengcan, additional, and Ye, Richard D., additional

Published

2021

10. THE CONCISE GUIDE TO PHARMACOLOGY 2021/22: G protein-coupled receptors

Author

Alexander, SPH, Christopoulos, A, Davenport, AP, Kelly, E, Mathie, A, Peters, JA, Veale, EL, Armstrong, JF, Faccenda, E, Harding, SD, Pawson, AJ, Southan, C, Davies, JA, Abbracchio, MP, Alexander, W, Al-hosaini, K, Baeck, M, Barnes, NM, Bathgate, R, Beaulieu, J-M, Bernstein, KE, Bettler, B, Birdsall, NJM, Blaho, V, Boulay, F, Bousquet, C, Braeuner-Osborne, H, Burnstock, G, Calo, G, Castano, JP, Catt, K, Ceruti, S, Chazot, P, Chiang, N, Chini, B, Chun, J, Cianciulli, A, Civelli, O, Clapp, LH, Couture, R, Csaba, Z, Dahlgren, C, Dent, G, Singh, KD, Douglas, SD, Dournaud, P, Eguchi, S, Escher, E, Filardo, EJ, Fong, T, Fumagalli, M, Gainetdinov, RR, de Gasparo, M, Gerard, C, Gershengorn, M, Gobeil, F, Goodfriend, TL, Goudet, C, Gregory, KJ, Gundlach, AL, Hamann, J, Hanson, J, Hauger, RL, Hay, DL, Heinemann, A, Hollenberg, MD, Holliday, ND, Horiuchi, M, Hoyer, D, Hunyady, L, Husain, A, IJzerman, AP, Inagami, T, Jacobson, KA, Jensen, RT, Jockers, R, Jonnalagadda, D, Karnik, S, Kaupmann, K, Kemp, J, Kennedy, C, Kihara, Y, Kitazawa, T, Kozielewicz, P, Kreienkamp, H-J, Kukkonen, JP, Langenhan, T, Leach, K, Lecca, D, Lee, JD, Leeman, SE, Leprince, J, Li, XX, Williams, TL, Lolait, SJ, Lupp, A, Macrae, R, Maguire, J, Mazella, J, McArdle, CA, Melmed, S, Michel, MC, Miller, LJ, Mitolo, V, Mouillac, B, Mueller, CE, Murphy, P, Nahon, J-L, Ngo, T, Norel, X, Nyimanu, D, Ocarroll, A-M, Offermanns, S, Panaro, MA, Parmentier, M, Pertwee, RG, Pin, J-P, Prossnitz, ER, Quinn, M, Ramachandran, R, Ray, M, Reinscheid, RK, Rondard, P, Rovati, GE, Ruzza, C, Sanger, GJ, Schoeneberg, T, Schulte, G, Schulz, S, Segaloff, DL, Serhan, CN, Stoddart, LA, Sugimoto, Y, Summers, R, Tan, VP, Thal, D, Thomas, WW, Timmermans, PMWM, Tirupula, K, Tulipano, G, Unal, H, Unger, T, Valant, C, Vanderheyden, P, Vaudry, D, Vaudry, H, Vilardaga, J-P, Walker, CS, Wang, JM, Ward, DT, Wester, H-J, Willars, GB, Woodruff, TM, Yao, C, Ye, RD, Alexander, SPH, Christopoulos, A, Davenport, AP, Kelly, E, Mathie, A, Peters, JA, Veale, EL, Armstrong, JF, Faccenda, E, Harding, SD, Pawson, AJ, Southan, C, Davies, JA, Abbracchio, MP, Alexander, W, Al-hosaini, K, Baeck, M, Barnes, NM, Bathgate, R, Beaulieu, J-M, Bernstein, KE, Bettler, B, Birdsall, NJM, Blaho, V, Boulay, F, Bousquet, C, Braeuner-Osborne, H, Burnstock, G, Calo, G, Castano, JP, Catt, K, Ceruti, S, Chazot, P, Chiang, N, Chini, B, Chun, J, Cianciulli, A, Civelli, O, Clapp, LH, Couture, R, Csaba, Z, Dahlgren, C, Dent, G, Singh, KD, Douglas, SD, Dournaud, P, Eguchi, S, Escher, E, Filardo, EJ, Fong, T, Fumagalli, M, Gainetdinov, RR, de Gasparo, M, Gerard, C, Gershengorn, M, Gobeil, F, Goodfriend, TL, Goudet, C, Gregory, KJ, Gundlach, AL, Hamann, J, Hanson, J, Hauger, RL, Hay, DL, Heinemann, A, Hollenberg, MD, Holliday, ND, Horiuchi, M, Hoyer, D, Hunyady, L, Husain, A, IJzerman, AP, Inagami, T, Jacobson, KA, Jensen, RT, Jockers, R, Jonnalagadda, D, Karnik, S, Kaupmann, K, Kemp, J, Kennedy, C, Kihara, Y, Kitazawa, T, Kozielewicz, P, Kreienkamp, H-J, Kukkonen, JP, Langenhan, T, Leach, K, Lecca, D, Lee, JD, Leeman, SE, Leprince, J, Li, XX, Williams, TL, Lolait, SJ, Lupp, A, Macrae, R, Maguire, J, Mazella, J, McArdle, CA, Melmed, S, Michel, MC, Miller, LJ, Mitolo, V, Mouillac, B, Mueller, CE, Murphy, P, Nahon, J-L, Ngo, T, Norel, X, Nyimanu, D, Ocarroll, A-M, Offermanns, S, Panaro, MA, Parmentier, M, Pertwee, RG, Pin, J-P, Prossnitz, ER, Quinn, M, Ramachandran, R, Ray, M, Reinscheid, RK, Rondard, P, Rovati, GE, Ruzza, C, Sanger, GJ, Schoeneberg, T, Schulte, G, Schulz, S, Segaloff, DL, Serhan, CN, Stoddart, LA, Sugimoto, Y, Summers, R, Tan, VP, Thal, D, Thomas, WW, Timmermans, PMWM, Tirupula, K, Tulipano, G, Unal, H, Unger, T, Valant, C, Vanderheyden, P, Vaudry, D, Vaudry, H, Vilardaga, J-P, Walker, CS, Wang, JM, Ward, DT, Wester, H-J, Willars, GB, Woodruff, TM, Yao, C, and Ye, RD

Abstract

The Concise Guide to PHARMACOLOGY 2021/22 is the fifth in this series of biennial publications. The Concise Guide provides concise overviews, mostly in tabular format, of the key properties of nearly 1900 human drug targets with an emphasis on selective pharmacology (where available), plus links to the open access knowledgebase source of drug targets and their ligands (www.guidetopharmacology.org), which provides more detailed views of target and ligand properties. Although the Concise Guide constitutes over 500 pages, the material presented is substantially reduced compared to information and links presented on the website. It provides a permanent, citable, point-in-time record that will survive database updates. The full contents of this section can be found at http://onlinelibrary.wiley.com/doi/bph.15538. G protein-coupled receptors are one of the six major pharmacological targets into which the Guide is divided, with the others being: ion channels, nuclear hormone receptors, catalytic receptors, enzymes and transporters. These are presented with nomenclature guidance and summary information on the best available pharmacological tools, alongside key references and suggestions for further reading. The landscape format of the Concise Guide is designed to facilitate comparison of related targets from material contemporary to mid-2021, and supersedes data presented in the 2019/20, 2017/18, 2015/16 and 2013/14 Concise Guides and previous Guides to Receptors and Channels. It is produced in close conjunction with the Nomenclature and Standards Committee of the International Union of Basic and Clinical Pharmacology (NC-IUPHAR), therefore, providing official IUPHAR classification and nomenclature for human drug targets, where appropriate.

Published

2021

11. The dramatic COVID 19 outbreak in Italy is responsible of a huge drop of urological surgical activity: a multicenter observational study

Author

Rocco, Bernardo, primary, Sighinolfi, Maria Chiara, additional, Sandri, Marco, additional, Altieri, Vincenzo, additional, Amenta, Michele, additional, Annino, Filippo, additional, Antonelli, Alessandro, additional, Baio, Raffaele, additional, Bertolo, Riccardo, additional, Bocciardi, AldoMassimo, additional, Borghesi, Marco, additional, Bove, Pierluigi, additional, Bozzini, Giorgio, additional, Brunocilla, Eugenio, additional, Cacciamani, Giovanni, additional, Calori, Alberto, additional, Cafarelli, Angelo, additional, Celia, Antonio, additional, Carbone, Antonio, additional, Cocci, Andrea, additional, Corsaro, Alfio, additional, Costa, Giovanni, additional, Ceruti, Carlo, additional, Cindolo, Luca, additional, Crivellaro, Simone, additional, Dalpiaz, Orietta, additional, D’Agostino, Daniele, additional, Dall’Oglio, Bruno, additional, Dente, Donato, additional, Falabella, Roberto, additional, Falsaperla, Mario, additional, Ferrari, Giovanni, additional, Finocchiaro, Marinella, additional, Flammia, Simone, additional, Gaboardi, Franco, additional, Galfano, Antonio, additional, Gallo, Fabrizio, additional, Gatti, Lorenzo, additional, Greco, Francesco, additional, Khorrami, Sada, additional, Leonardo, Costantino, additional, Marenghi, Carlo, additional, Nucciotti, Roberto, additional, Oderda, Marco, additional, Pagliarulo, Vincenzo, additional, Parma, Paolo, additional, Pastore, Antonio L., additional, Pini, Giovannalberto, additional, Porreca, Angelo, additional, Pucci, Luigi, additional, Schenone, Maurizio, additional, Schiavina, Riccardo, additional, Sciorio, Carmine, additional, Spirito, Lorenzo, additional, Tafuri, Alessandro, additional, Terrone, Carlo, additional, Umari, Paolo, additional, Varca, Virginia, additional, Veneziano, Domenico, additional, Verze, Paolo, additional, Volpe, Alessandro, additional, Micali, Salvatore, additional, Berti, Lorenzo, additional, Zaramella, Stefano, additional, Zegna, Luisa, additional, Bertellini, Elisabetta, additional, and Minervini, Andrea, additional

Published

2020

12. Cutaneous sensitivity modulation by Aquaphilus dolomiae extract‐G3 on in vitro models of neuro‐inflammation

Author

Lestienne, F., primary, Viodé, C., additional, Ceruti, I., additional, Carrere, S., additional, Bessou‐Touya, S., additional, Duplan, H., additional, and Castex‐Rizzi, N., additional

Published

2020

13. Rates of hypogonadism forms in Klinefelter patients undergoing testicular sperm extraction: A multicenter cross‐sectional study

Author

Pozzi, Edoardo, primary, Boeri, Luca, additional, Capogrosso, Paolo, additional, Palmisano, Franco, additional, Preto, Mirko, additional, Sibona, Mattia, additional, Franceschelli, Alessandro, additional, Ruiz‐Castañé, Eduard, additional, Sarquella‐Geli, Joaquim, additional, Bassas‐Arnau, Lluís, additional, Scroppo, Fabrizio I., additional, Gentile, Giorgio, additional, Falcone, Marco, additional, Timpano, Massimiliano, additional, Ceruti, Carlo, additional, Gadda, Franco, additional, Colombo, Fulvio, additional, Rolle, Luigi, additional, Gontero, Paolo, additional, Montorsi, Francesco, additional, Sánchez‐Curbelo, Josvany, additional, Montanari, Emanuele, additional, and Salonia, Andrea, additional

Published

2020

14. An unusual neurological manifestation of granulomatosis with polyangiitis: A case report and literature review

Author

Tarte, Nikhil N., primary, Ceruti, Ronald, additional, and Tati, Vasudev, additional

Published

2020

15. Sperm retrieval rates in non‐mosaic Klinefelter patients undergoing testicular sperm extraction: What expectations do we have in the real‐life setting?

Author

Boeri, Luca, primary, Palmisano, Franco, additional, Preto, Mirko, additional, Sibona, Mattia, additional, Capogrosso, Paolo, additional, Franceschelli, Alessandro, additional, Ruiz‐Castañé, Eduard, additional, Sarquella‐Geli, Joaquim, additional, Bassas‐Arnau, Lluís, additional, Scroppo, Fabrizio Ildefonso, additional, Saccà, Antonino, additional, Gentile, Giorgio, additional, Falcone, Marco, additional, Timpano, Massimiliano, additional, Ceruti, Carlo, additional, Gadda, Franco, additional, Trost, Landon, additional, Colombo, Fulvio, additional, Rolle, Luigi, additional, Gontero, Paolo, additional, Montorsi, Francesco, additional, Sánchez‐Curbelo, Josvany, additional, Salonia, Andrea, additional, and Montanari, Emanuele, additional

Published

2020

16. THE CONCISE GUIDE TO PHARMACOLOGY 2017/18: Overview

Author

Leigh Stoddart, Henry Sackin, Stephen Tucker, Katherine Leach, Daniel Hoyer, Eric Prossnitz, Julien Hanson, Michael Spedding, Jérôme Leprince, Thiruma Arumugam, Lucie Clapp, Marta Fumagalli, Raul R Gainetdinov, David Clapham, Craig McArdle, Peter Monk, Detlev Boison, Stefan Offermanns, Susan Pyne, Gareth Sanger, Joanna Sharman, David MacEwan, Ken-ichi Inui, Cyril Goudet, Victoria Blaho, Elena Faccenda, Bernhard Bettler, Roger Summers, Nan Chiang, Gregory David Stewart, Anthony Futerman, Davide Lecca, Jörg Hamann, Simon Douglas Harding, Anthony Peter Davenport, Trent Woodruff, Mark Connor, Israel Hanukoglu, Adam Pawson, Bernard MOUILLAC, Stefania Ceruti, Nicholas Holliday, Arthur Christopoulos, Stefan Broer, Jamie Davies, Paul Chazot, Ian Kerr, Christopher Southan, William Catterall, Jyrki Kukkonen, and Elvir Becirovic

Subjects

0301 basic medicine, Pharmacology, Clinical pharmacology, Nomenclature Committee, business.industry, 3. Good health, law.invention, 03 medical and health sciences, 030104 developmental biology, 0302 clinical medicine, Summary information, law, Medicine, Catalytic receptors, business, 030217 neurology & neurosurgery

Abstract

The Concise Guide to PHARMACOLOGY 2017/18 is the third in this series of biennial publications. This version provides concise overviews of the key properties of nearly 1800 human drug targets with an emphasis on selective pharmacology (where available), plus links to an open access knowledgebase of drug targets and their ligands (www.guidetopharmacology.org), which provides more detailed views of target and ligand properties. Although the Concise Guide represents approximately 400 pages, the material presented is substantially reduced compared to information and links presented on the website. It provides a permanent, citable, point-in-time record that will survive database updates. The full contents of this section can be found at http://onlinelibrary.wiley.com/doi/10.1111/bph.13882/full. In addition to this overview, in which are identified 'Other protein targets' which fall outside of the subsequent categorisation, there are eight areas of focus: G protein-coupled receptors, ligand-gated ion channels, voltage-gated ion channels, other ion channels, nuclear hormone receptors, catalytic receptors, enzymes and transporters. These are presented with nomenclature guidance and summary information on the best available pharmacological tools, alongside key references and suggestions for further reading. The landscape format of the Concise Guide is designed to facilitate comparison of related targets from material contemporary to mid-2017, and supersedes data presented in the 2015/16 and 2013/14 Concise Guides and previous Guides to Receptors and Channels. It is produced in close conjunction with the Nomenclature Committee of the Union of Basic and Clinical Pharmacology (NC-IUPHAR), therefore, providing official IUPHAR classification and nomenclature for human drug targets, where appropriate.

Published

2017

17. THE CONCISE GUIDE TO PHARMACOLOGY 2019/20: G protein-coupled receptors

Author

Alexander, SPH, Christopoulos, A, Davenport, AP, Kelly, E, Mathie, A, Peters, JA, Veale, EL, Armstrong, JF, Faccenda, E, Harding, SD, Pawson, AJ, Sharman, JL, Southan, C, Davies, JA, Arumugam, TV, Bennett, A, Sjogren, B, Sobey, C, Wong, SS, Abbracchio, MP, Alexander, W, Al-hosaini, K, Back, M, Beaulieu, J-M, Bernstein, KE, Bettler, B, Birdsall, NJM, Blaho, V, Bousquet, C, Brauner-Osborne, H, Burnstock, G, Calo, G, Castano, JP, Catt, KJ, Ceruti, S, Chazot, P, Chiang, N, Chun, J, Cianciulli, A, Clapp, LH, Couture, R, Csaba, Z, Dent, G, Singh, KD, Douglas, SD, Dournaud, P, Eguchi, S, Escher, E, Filardo, E, Fong, TM, Fumagalli, M, Gainetdinov, RR, de Gasparo, M, Gershengorn, M, Gobeil, F, Goodfriend, TL, Goudet, C, Gregory, KJ, Gundlach, AL, Hamann, J, Hanson, J, Hauger, RL, Hay, D, Heinemann, A, Hollenberg, MD, Holliday, ND, Horiuchi, M, Hoyer, D, Hunyady, L, Husain, A, Ijzerman, AP, Inagami, T, Jacobson, KA, Jensen, RT, Jockers, R, Jonnalagadda, D, Karnik, S, Kaupmann, K, Kemp, J, Kennedy, C, Kihara, Y, Kozielewicz, P, Kreienkamp, H-J, Kukkonen, JP, Langenhan, T, Leach, K, Lecca, D, Lee, JD, Leeman, SE, Leprince, J, Lolait, SJ, Lupp, A, Macrae, R, Maguire, J, Mazella, J, McArdle, CA, Melmed, S, Michel, MC, Miller, L, Mitolo, V, Mouillac, B, Murphy, PM, Nahon, J-L, Norel, X, Nyimanu, D, O'Carroll, A-M, Offermanns, S, Panaro, MA, Pertwee, RG, Pin, J-P, Prossnitz, E, Ramachandran, R, Reinscheid, RK, Rondard, P, Rovati, GE, Ruzza, C, Sanger, G, Schoeneberg, T, Schulte, G, Schulz, S, Segaloff, DL, Serhan, CN, Stoddart, LA, Sugimoto, Y, Summers, R, Tan, V, Thomas, W, Timmermans, PBMWM, Tirupula, K, Tulipano, G, Unal, H, Unger, T, Vanderheyden, P, Vaudry, D, Vaudry, H, Vilardaga, J-P, Walker, CS, Ward, DT, Wester, H-J, Willars, GB, Williams, TL, Woodruff, TM, Yao, C, Aldrich, RW, Becirovic, E, Biel, M, Catterall, WA, Conner, AC, Davies, P, Delling, M, Di Virgilio, F, Falzoni, S, George, C, Goldstein, SAN, Grissmer, S, Ha, K, Hammelmann, V, Hanukoglu, I, Jarvis, M, Jensen, AA, Kaczmarek, LK, Kellenberger, S, King, B, Lynch, JW, Perez-Reyes, E, Plant, LD, Rash, LD, Ren, D, Sivilotti, LG, Smart, TG, Snutch, TP, Tian, J, Van den Eynde, C, Vriens, J, Wei, AD, Winn, BT, Wulff, H, Xu, H, Yue, L, Zhang, X, Zhu, M, Coons, L, Fuller, P, Korach, KS, Young, M, Bryant, C, Farndale, RW, Hobbs, A, Jarvis, GE, MacEwan, D, Monie, TP, Waldman, S, Beuve, A, Boison, D, Brouckaert, P, Burnett, JC, Burns, K, Dessauer, C, Friebe, A, Garthwaite, J, Gertsch, J, Helsby, N, Izzo, AA, Koesling, D, Kuhn, M, Ostrom, R, Papapetropoulos, A, Potter, LR, Pyne, NJ, Pyne, S, Russwurm, M, Schmidt, HHHW, Seifert, R, Stasch, J-P, Szabo, C, van der Stelt, M, van der Vliet, A, Watts, V, Anderson, CMH, Broer, S, Dawson, P, Hagenbuch, B, Hammond, JR, Hancox, J, Inui, K-I, Kanai, Y, Kemp, S, Thwaites, DT, Verri, T, Alexander, SPH, Christopoulos, A, Davenport, AP, Kelly, E, Mathie, A, Peters, JA, Veale, EL, Armstrong, JF, Faccenda, E, Harding, SD, Pawson, AJ, Sharman, JL, Southan, C, Davies, JA, Arumugam, TV, Bennett, A, Sjogren, B, Sobey, C, Wong, SS, Abbracchio, MP, Alexander, W, Al-hosaini, K, Back, M, Beaulieu, J-M, Bernstein, KE, Bettler, B, Birdsall, NJM, Blaho, V, Bousquet, C, Brauner-Osborne, H, Burnstock, G, Calo, G, Castano, JP, Catt, KJ, Ceruti, S, Chazot, P, Chiang, N, Chun, J, Cianciulli, A, Clapp, LH, Couture, R, Csaba, Z, Dent, G, Singh, KD, Douglas, SD, Dournaud, P, Eguchi, S, Escher, E, Filardo, E, Fong, TM, Fumagalli, M, Gainetdinov, RR, de Gasparo, M, Gershengorn, M, Gobeil, F, Goodfriend, TL, Goudet, C, Gregory, KJ, Gundlach, AL, Hamann, J, Hanson, J, Hauger, RL, Hay, D, Heinemann, A, Hollenberg, MD, Holliday, ND, Horiuchi, M, Hoyer, D, Hunyady, L, Husain, A, Ijzerman, AP, Inagami, T, Jacobson, KA, Jensen, RT, Jockers, R, Jonnalagadda, D, Karnik, S, Kaupmann, K, Kemp, J, Kennedy, C, Kihara, Y, Kozielewicz, P, Kreienkamp, H-J, Kukkonen, JP, Langenhan, T, Leach, K, Lecca, D, Lee, JD, Leeman, SE, Leprince, J, Lolait, SJ, Lupp, A, Macrae, R, Maguire, J, Mazella, J, McArdle, CA, Melmed, S, Michel, MC, Miller, L, Mitolo, V, Mouillac, B, Murphy, PM, Nahon, J-L, Norel, X, Nyimanu, D, O'Carroll, A-M, Offermanns, S, Panaro, MA, Pertwee, RG, Pin, J-P, Prossnitz, E, Ramachandran, R, Reinscheid, RK, Rondard, P, Rovati, GE, Ruzza, C, Sanger, G, Schoeneberg, T, Schulte, G, Schulz, S, Segaloff, DL, Serhan, CN, Stoddart, LA, Sugimoto, Y, Summers, R, Tan, V, Thomas, W, Timmermans, PBMWM, Tirupula, K, Tulipano, G, Unal, H, Unger, T, Vanderheyden, P, Vaudry, D, Vaudry, H, Vilardaga, J-P, Walker, CS, Ward, DT, Wester, H-J, Willars, GB, Williams, TL, Woodruff, TM, Yao, C, Aldrich, RW, Becirovic, E, Biel, M, Catterall, WA, Conner, AC, Davies, P, Delling, M, Di Virgilio, F, Falzoni, S, George, C, Goldstein, SAN, Grissmer, S, Ha, K, Hammelmann, V, Hanukoglu, I, Jarvis, M, Jensen, AA, Kaczmarek, LK, Kellenberger, S, King, B, Lynch, JW, Perez-Reyes, E, Plant, LD, Rash, LD, Ren, D, Sivilotti, LG, Smart, TG, Snutch, TP, Tian, J, Van den Eynde, C, Vriens, J, Wei, AD, Winn, BT, Wulff, H, Xu, H, Yue, L, Zhang, X, Zhu, M, Coons, L, Fuller, P, Korach, KS, Young, M, Bryant, C, Farndale, RW, Hobbs, A, Jarvis, GE, MacEwan, D, Monie, TP, Waldman, S, Beuve, A, Boison, D, Brouckaert, P, Burnett, JC, Burns, K, Dessauer, C, Friebe, A, Garthwaite, J, Gertsch, J, Helsby, N, Izzo, AA, Koesling, D, Kuhn, M, Ostrom, R, Papapetropoulos, A, Potter, LR, Pyne, NJ, Pyne, S, Russwurm, M, Schmidt, HHHW, Seifert, R, Stasch, J-P, Szabo, C, van der Stelt, M, van der Vliet, A, Watts, V, Anderson, CMH, Broer, S, Dawson, P, Hagenbuch, B, Hammond, JR, Hancox, J, Inui, K-I, Kanai, Y, Kemp, S, Thwaites, DT, and Verri, T

Abstract

The Concise Guide to PHARMACOLOGY 2019/20 is the fourth in this series of biennial publications. The Concise Guide provides concise overviews of the key properties of nearly 1800 human drug targets with an emphasis on selective pharmacology (where available), plus links to the open access knowledgebase source of drug targets and their ligands (www.guidetopharmacology.org), which provides more detailed views of target and ligand properties. Although the Concise Guide represents approximately 400 pages, the material presented is substantially reduced compared to information and links presented on the website. It provides a permanent, citable, point-in-time record that will survive database updates. The full contents of this section can be found at http://onlinelibrary.wiley.com/doi/10.1111/bph.14748. G protein-coupled receptors are one of the six major pharmacological targets into which the Guide is divided, with the others being: ion channels, nuclear hormone receptors, catalytic receptors, enzymes and transporters. These are presented with nomenclature guidance and summary information on the best available pharmacological tools, alongside key references and suggestions for further reading. The landscape format of the Concise Guide is designed to facilitate comparison of related targets from material contemporary to mid-2019, and supersedes data presented in the 2017/18, 2015/16 and 2013/14 Concise Guides and previous Guides to Receptors and Channels. It is produced in close conjunction with the International Union of Basic and Clinical Pharmacology Committee on Receptor Nomenclature and Drug Classification (NC-IUPHAR), therefore, providing official IUPHAR classification and nomenclature for human drug targets, where appropriate.

Published

2019

18. SNX27, a protein involved in down syndrome, regulates GPR17 trafficking and oligodendrocyte differentiation

Author

Fiorenza Stagni, Maria P. Abbracchio, Stefania Ceruti, Renata Bartesaghi, Marta Boccazzi, Fabiola Valenza, Davide Lecca, A. Fratangeli, Veronica Meraviglia, Alessandro Francesco Ulivi, Maria Passafaro, Andrea Giacomini, and Patrizia Rosa

Subjects

0301 basic medicine, SNX27, Endocytic cycle, PDZ domain, Oligodendrocyte differentiation, Biology, Endocytosis, Cell biology, Retromer complex, 03 medical and health sciences, Cellular and Molecular Neuroscience, 030104 developmental biology, 0302 clinical medicine, Neurology, Gene silencing, Receptor, 030217 neurology & neurosurgery

Abstract

The G protein-coupled receptor 17 (GPR17) plays crucial roles in myelination. It is highly expressed during transition of oligodendrocyte progenitor cells to immature oligodendrocytes, but, after this stage, it must be down-regulated to allow generation of mature myelinating cells. After endocytosis, GPR17 is sorted into lysosomes for degradation or recycled to the plasma membrane. Balance between degradation and recycling is important for modulation of receptor levels at the cell surface and thus for the silencing/activation of GPR17-signaling pathways that, in turn, affect oligodendrocyte differentiation. The molecular mechanisms at the basis of these processes are still partially unknown and their characterization will allow a better understanding of myelination and provide cues to interpret the consequences of GPR17 dysfunction in diseases. Here, we demonstrate that the endocytic trafficking of GPR17 is mediated by the interaction of a type I PDZ-binding motif located at the C-terminus of the receptor and SNX27, a recently identified protein of the endosome-associated retromer complex and whose functions in oligodendrocytes have never been studied. SNX27 knock-down significantly reduces GPR17 plasma membrane recycling in differentiating oligodendrocytes while accelerating cells' terminal maturation. Interestingly, trisomy-linked down-regulation of SNX27 expression in the brain of Ts65Dn mice, a model of Down syndrome, correlates with a decrease in GPR17(+) cells and an increase in mature oligodendrocytes, which, however, fail in reaching full maturation, eventually leading to hypomyelination. Our data demonstrate that SNX27 modulates GPR17 plasma membrane recycling and stability, and that disruption of the SNX27/GPR17 interaction might contribute to pathological oligodendrocyte differentiation defects. GLIA 2016. GLIA 2016;64:1437-1460.

Published

2016

19. Influence of the degree of hydrolysis on the bioactive properties of whey protein hydrolysates using Alcalase®

Author

Eberhardt, Agustina, primary, López, Emilse C, additional, Ceruti, Roberto J, additional, Marino, Fernanda, additional, Mammarella, Enrique J, additional, Manzo, Ricardo M, additional, and Sihufe, Guillermo A, additional

Published

2019

20. A prospective multicentric international study on the surgical outcomes and patients’ satisfaction rates of the ‘sliding’ technique for end-stage Peyronie's disease with severe shortening of the penis and erectile dysfunction

Author

Marco Oderda, Franklin E. Kuehhas, Giulio Garaffa, Paolo Gontero, Mirko Preto, Luigi Rolle, M. Sibona, Marco Falcone, Massimiliano Timpano, David Ralph, Bruno Frea, Omid Sedigh, Carlo Ceruti, and Arianna Gillo

Subjects

Male, medicine.medical_specialty, Prosthesis-Related Infections, Blood transfusion, Peyronie's disease, Urology, medicine.medical_treatment, Penile Induration, 030232 urology & nephrology, Penile Implantation, Postoperative Hemorrhage, 03 medical and health sciences, 0302 clinical medicine, Erectile Dysfunction, Penile lengthening, medicine, Humans, Prospective Studies, Stage (cooking), Aged, 030219 obstetrics & reproductive medicine, business.industry, erectile dysfunction, patch graft surgery for Peyronie's disease, penile lengthening, penile prosthesis, Penile prosthesis, Middle Aged, medicine.disease, Surgery, Treatment Outcome, medicine.anatomical_structure, Erectile dysfunction, Patient Satisfaction, Operative time, business, Penis, Follow-Up Studies

Abstract

Objectives To report the results from a prospective multicentric study of patients with Peyronie's disease (PD) treated with the ‘sliding’ technique (ST). Patients and Methods From June 2010 to January 2014, 28 consecutive patients affected by stable PD with severe penile shortening and end-stage erectile dysfunction (ED) were enrolled in three European PD tertiary referral centres. The validated International Index of Erectile Function (IIEF) questionnaire, the Sexual Encounter Profile (SEP) Questions 2 and 3, and the Peyronie's disease questionnaire (PDQ) were completed preoperatively by all patients. At the follow-up visits (at 3, 6 and 12 months), the IIEF, the SEP Questions 2 and 3, the PDQ, and the Erectile Dysfunction Inventory of Treatment Satisfaction (EDITS) were completed. The outcome analysis was focused on penile length restoration, and intra- and postoperative complications classified according the Clavien–Dindo Classification. Results The mean (range) follow-up was 37 (9–60) months. A malleable penile prosthesis (PP) was implanted in seven patients, while an inflatable three-pieces PP was placed in the remainder. In the case of inflatable PP implantation, porcine small intestinal submucosa and acellular porcine dermal matrix were used to cover the tunical defects. While in patients undergoing malleable PP implantation, collagen-fibrin sponge was used. The mean operative time was 145 min in the inflatable PP group and 115 min in the malleable PP group. There were no intraoperative complications. Postoperative complications included profuse bleeding requiring a blood transfusion in one patient (3.5%) on anticoagulation therapy for a mechanical heart valve (Grade II) and PP infection requiring the removal of the device (7%) (Grade III). There were no late recurrences of the shaft deformation. The postoperative functional data showed a progressive improvement in the score of all questionnaires, peaking at 12 months postoperatively. The mean (range) penile lengthening was 3.2 (2.5–4) cm and no patient reported recurrence of the curvature. Conclusions The present series suggests that, in the hands of experienced high-volume surgeons, penile length restoration with the use of the ST represents an effective option for end-stage PD associated with ED and severe shortening of the shaft. Larger series and longer follow-up will be required to fully establish the efficacy of this procedure.

Published

2015

21. P2Y2receptor antagonists as anti-allodynic agents in acute and sub-chronic trigeminal sensitization: Role of satellite glial cells

Author

Claudia Verderio, D. Merli, Maria P. Abbracchio, Stefania Ceruti, and G. Magni

Subjects

P2Y receptor, business.industry, Antagonist, Pharmacology, Cellular and Molecular Neuroscience, Trigeminal ganglion, chemistry.chemical_compound, Allodynia, Neurology, chemistry, Freund's adjuvant, Hyperalgesia, medicine, PPADS, Purinergic P2Y Receptor Antagonists, medicine.symptom, business, Neuroscience

Abstract

Trigeminal (TG) pain often lacks a satisfactory pharmacological control. A better understanding of the molecular cross-talk between TG neurons and surrounding satellite glial cells (SGCs) could help identifying innovative targets for the development of more effective analgesics. We have previously demonstrated that neuronal pro-algogenic mediators upregulate G protein-coupled nucleotide P2Y receptors (P2YRs) expressed by TG SGCs in vitro. Here, we have identified the specific P2YR subtypes involved (i.e., the ADP-sensitive P2Y1 R and the UTP-responsive P2Y2 R subtypes), and demonstrated the contribution of neuron-derived prostaglandins to their upregulation. Next, we have translated these data to an in vivo model of TG pain (namely, rats injected with Complete Freund's adjuvant in the temporomandibular joint), by demonstrating activation of SGCs and upregulation of P2Y1 R and P2Y2 R in the ipsi-lateral TG. To unequivocally link P2YRs to the development of facial allodynia, we treated animals with various purinergic antagonists. The selective P2Y2 R antagonist AR-C118925 completely inhibited SGCs activation, exerted a potent anti-allodynic effect that lasted over time, and was still effective when administration was started 6-days post induction of allodynia, i.e. under subchronic pain conditions. Conversely, the selective P2Y1 R antagonist MRS2179 was completely ineffective. Moreover, similarly to the anti-inflammatory drug acetylsalicylic acid and the known anti-migraine agent sumatriptan, the P2X/P2Y nonselective antagonist PPADS was only partially effective, and completely lost its activity under sub-chronic conditions. Taken together, our results highlight glial P2Y2 Rs as potential "druggable" targets for the successful management of TG-related pain.

Published

2015

22. Characterization of a human epidermis model reconstructed from hair follicle keratinocytes and comparison with two commercially models and native skin

Author

C. Saint-Martory, Y. Palvadeau, I. Ceruti, S. Mas, N. Castex-Rizzi, Hélène Duplan, H. Hernandez-Pigeon, Sandrine Bessou-Touya, and B. Guiraud

Subjects

Keratinocytes, Aging, Stratum granulosum, Gene Expression, Pharmaceutical Science, Dermatology, Filaggrin Proteins, Biology, Outer root sheath, Cell morphology, Models, Biological, Colloid and Surface Chemistry, Drug Discovery, medicine, Humans, Stratum spinosum, Involucrin, integumentary system, Epidermis (botany), Cell Cycle, Cell Differentiation, Anatomy, Molecular biology, medicine.anatomical_structure, Chemistry (miscellaneous), Epidermis, Keratinocyte, Biomarkers, Hair, Filaggrin

Abstract

Synopsis Objective Outer root sheath (ORS) cells of human hair follicles are a readily available, non-invasive source of keratinocytes for epidermis reconstruction. The aim of this study was to characterize a model of epidermis reconstructed from ORS cells (ORS-derived model) and to evaluate its reproducibility, in comparison with native human skin and two marketed reconstructed skin models (model A, Episkin® and model B, Skinethic®). Methods Cell morphology and tissue architecture of the three models were analysed histologically and proliferation and differentiation marker expression by immunohistochemistry and mRNA quantification. Results All models displayed the same general epidermal architecture as native epidermis, but with a thicker stratum corneum in models A and B. Compared with native epidermis, Ki67 was correctly localized in epidermal basal cells in all models, as K10 in suprabasal layers. In all skin models, transglutaminase 1 (TGM1) was prematurely expressed in suprabasal layers. However, this expression was only observed from the upper stratum spinosum in the ORS-derived model. In this model, filaggrin and loricrin were correctly located in the stratum granulosum. Filaggrin, involucrin, loricrin and TGM1 mRNAs (markers of keratinocyte terminal differentiation) were transcriptionally expressed in all models. In the ORS-derived model, transcriptional expression level was similar to that of native skin. Conclusion ORS cell-based reconstructed epidermis is a valid and reproducible model for human epidermis and it may be used to evaluate the effects of active substances and cosmetic formulations. Resume Objectif Les cellules ORS de la gaine epitheliale externe des follicules pileux humains sont une source facilement disponible, non invasive de keratinocytes pour la reconstruction des epidermes. L'objectif de la presente etude est de caracteriser un modele d'epiderme reconstitue realise a partir des cellules ORS (modele derive d'ORS), et d'evaluer sa reproductibilite, par rapport a la peau humaine native et a deux modeles commercialises d'epidermes reconstruits (modele A, Episkin ® et le modele B, Skinethic ®). Methodes La morphologie cellulaire et l'architecture des tissus des 3 modeles ont ete analyses sur le plan histologique et l'expression des marqueurs de proliferation et de differenciation ont ete analyses par immunohistochimie et quantification d'ARNm. Resultats Tous les modeles ont une architecture epidermique generale similaire a celle de l'epiderme natif, mais avec un stratum corneum plus epais pour les modeles A et B. Par comparaison avec l'epiderme natif, Ki67 est correctement localise dans les cellules basales epidermiques dans tous les modeles, de meme que K10 dans les couches suprabasales. Dans tous les modeles, la transglutaminase 1 (TGM1) est prematurement exprimee dans les couches suprabasales. Toutefois, cette expression a ete observee uniquement a partir de la couche epineuse superieure dans le modele derive d'ORS. Dans ce modele, la filaggrine et la loricrine sont correctement situees au niveau de la couche granuleuse. Les ARNm de la filaggrine, l'involucrine, la loricrine et la TGM1 (marqueurs de la differenciation terminale des keratinocytes) sont exprimes dans tous les modeles. Dans le modele derive d'ORS, le niveau d'expression transcriptionnel est semblable a celui de la peau native. Conclusion Ce modele reconstruit est un modele d'epiderme humain reproductible et interessant pour l'evaluation de principes actifs et des produits cosmetiques.

Published

2014

23. Thoraco-abdominal asymmetry and asynchrony in congenital diaphragmatic hernia

Author

Ernesto Leva, Francesco Macchini, Clara Ceruti, M. Torricelli, Andrea Aliverti, Marianna Laviola, Rita Priori, and Andrea Zanini

Subjects

Pulmonary and Respiratory Medicine, medicine.medical_specialty, Rib cage, Supine position, business.industry, Diaphragmatic breathing, Congenital diaphragmatic hernia, medicine.disease, Surgery, Pulmonary function testing, Diaphragm (structural system), Pediatrics, Perinatology and Child Health, Breathing, Medicine, business, Tidal volume

Abstract

Objective:Congenitaldiaphragmatichernia(CDH)consistsofanincompleteformation of the diaphragm and the subsequent herniation of abdominal bowels. Diaphragmatic defect can be repaired by primary closure or placing a patch. Respiratory follow up usually focuses on spirometric and clinical evaluation. The aim of the study was to assess thoraco-abdominal volumes in CDH patients and to verify whether the action of the diaphragm on the chest wall is altered leading to an asymmetric and asynchronous expansion of the different thoracoabdominal compartments. Patients and Methods: Total and compartmental chest wall volumes and asynchronies were measured by Opto-Electronic Plethysmography in 14 CDH patients (7M/7F, age 5 � 2 years, 12 left side operated) and in 9 age matched healthy subjects during quiet spontaneous breathing in supine position. Patients were divided in two groups: five patients with suture (group S) and nine patients with diaphragmatic patch (group P). Pulmonary function was assessedbyspirometryandspirometricparameterswereexpressedasZ-score.Results:Ingroup P abdominal contribution to tidal volume was lower than healthy controls and group S. Unlike controls, in both CDH groups the right side of pulmonary rib cage moved inward with a correspondentleft side expansionduringinspiration. IngroupS,thoraco-abdominal asynchronies were higher than in group P and controls, especially in the right side. Five patients belonging to group P had a spirometric obstructive pattern. Conclusions: In overall CDH patients a reduced action of the treated (left) hemi-diaphragm is evident. In patients treated by primary suture, a compensatory action of the right side allows to reach a normal total diaphragmatic displacement and a proper contribution of the whole diaphragm to tidal volume. In patients treated by diaphragmatic patch, instead, thoraco-abdominal asynchronies are prevented. Pediatr

Published

2014

24. New insights in the use of pleural ultrasonography for diagnosis and treatment of pleural disease

Author

Marchetti, Giampietro, primary, Arondi, Sabrina, additional, Baglivo, Francesca, additional, Lonni, Sara, additional, Quadri, Federico, additional, Valsecchi, Alberto, additional, Venturoli, Nicola, additional, and Ceruti, Paolo, additional

Published

2018

25. Engineering optimization based on dynamic technique for order preference by similarity to ideal solution fitness: Application to unmanned aerial vehicle wing airfoil geometry definition

Author

Ceruti, Alessandro, primary, Fiorini, Tommaso, additional, Boggi, Stefano, additional, and Mischi, Lorenzo, additional

Published

2018

26. Purines regulate adult brain subventricular zone cell functions: Contribution of reactive astrocytes

Author

Stefania Ceruti, Maria P. Abbracchio, Annalisa Buffo, Marta Boccazzi, and Chiara Rolando

Subjects

Neurogenesis, Purinergic receptor, Glutamate receptor, Subventricular zone, Biology, medicine.disease, Neural stem cell, Astrogliosis, Cell biology, Cellular and Molecular Neuroscience, medicine.anatomical_structure, nervous system, Neurology, Neuroblast, medicine, Progenitor cell, Neuroscience

Abstract

Brain injuries modulate activation of neural stem cells (NSCs) in the adult brain. In pathological conditions, the concentrations of extracellular nucleotides (eNTs) raise several folds, contribute to reactive gliosis, and possibly directly affect subventricular zone (SVZ) cell functioning. Among eNTs and derived metabolites, the P2Y1 receptor agonist ADP strongly promotes astrogliosis and might also influence SVZ progenitor activity. Here, we tested the ability of the stable P2Y1 agonist adenosine 5'-O-(2-thiodiphosphate) (ADPβS) to control adult NSC functions both in vitro and in vivo, with a focus on the possible effects exerted by reactive astrocytes. In the absence of growth factors, ADPβS promoted proliferation and differentiation of SVZ progenitors. Moreover, ADPβS-activated astrocytes markedly changed the pattern of released cytokines and chemokines, and strongly modulated neurosphere-forming capacity of SVZ progenitors. Notably, a significant enhancement in proliferation was observed when SVZ cells, initially grown in the supernatant of astrocytes exposed to ADPβS, were shifted to normal medium. In vivo, ADPβS administration in the lateral ventricle of adult mice by osmotic minipumps caused diffused reactive astrogliosis, and a strong response of SVZ progenitors. Indeed, proliferation of glial fibrillary acidic protein-positive NSCs increased and led to a significant expansion of SVZ transit-amplifying progenitors and neuroblasts. Lineage tracing experiments performed in the GLAST::CreERT2;Rosa-YFP transgenic mice further demonstrated that ADPβS promoted proliferation of glutamate/aspartate transporter-positive progenitors and sustained their progression toward the generation of rapidly dividing progenitors. Altogether, our results show that the purinergic system crucially affects SVZ progenitor activities both directly and through the involvement of reactive astrocytes.

Published

2013

27. a-SiOxCoatings Grown on Dental Materials by PECVD: Compositional Analysis and Preliminary Investigation of Biocompatibility Improvements

Author

Carlo Ricciardi, Federico Mussano, Paola Ceruti, Pietro Mandracci, and Stefano Carossa

Subjects

Materials science, Biocompatibility, Process Chemistry and Technology, PECVD, Nanotechnology, Surfaces and Interfaces, General Chemistry, silicon oxide, EDX, Plasma-enhanced chemical vapor deposition, cytotoxicity, dental materials, biomaterials, Silicon oxide

Published

2010

28. Antifungal activity of bis-azasqualenes, inhibitors of oxidosqualene cyclase

Author

Maria Grazia Sarpietro, Samuele Voyron, Valeria Filipello Marchisio, Alessandra Fiorio Pla, Giovanna Cristina Varese, Flavio Rocco, Paolo E. Forni, and Maurizio Ceruti

Subjects

biology, Broth microdilution, Dermatology, General Medicine, biology.organism_classification, In vitro, Microbiology, Squalene, chemistry.chemical_compound, Minimum inhibitory concentration, Infectious Diseases, chemistry, Cell culture, Toxicity, Trichophyton, Microsporum canis

Abstract

The antifungal activity and in vitro toxicity toward animal cells of two inhibitors of oxidosqualene cyclase, squalene bis-diethylamine (SBD) and squalene bis-diethylmethylammonium iodide (SBDI) were studied. Minimum inhibitory concentration (MIC) against dermatophytes and other fungi involved in cutaneous and systemic infections (12 isolates from seven species) were determined by the broth microdilution method based on the reference documents M38-A and M27-A2 of Clinical and Laboratory Standards Institute (CLSI). Both compounds exerted fungistatic activities, although with different action. SBDI was the more active compound and displayed low MIC values (in the 3.12-12.5 μg ml(-1) range) against Microsporum canis, Trichophyton mentagrophytes and one isolate of Scopulariopsis brevicaulis, while SBD showed MIC values against these species in the 3.12-25 μg ml(-1) range. Toxicity was tested on Madin-Darby canine kidney (MDCK) epithelial cells and human microvascular endothelial cells (HMEC). SBDI proved the less toxic compound: it inhibited M. canis, T. mentagrophytes and S. brevicaulis at concentrations below those found toxic for MDCK cells. HMEC were the more sensitive cells.

Published

2009

29. Opposite effects of uracil and adenine nucleotides on the survival of murine cardiomyocytes

Author

Silvia Ferrario, Simona Cosentino, Emanuela Amoruso, Stefania Ceruti, Elena Beltrami, Maria P. Abbracchio, Davide Lecca, Alessia Mazzola, and Elena Tremoli

Subjects

P2Y receptor, Programmed cell death, P2Y receptors, Cell Survival, Uracil Nucleotides, heart failure, Biology, chemistry.chemical_compound, Adenosine Triphosphate, Adenine nucleotide, Purinergic P2 Receptor Antagonists, Animals, Drug Interactions, Myocytes, Cardiac, heterocyclic compounds, Receptor, Cells, Cultured, Cell Nucleus, Cell Death, Dose-Response Relationship, Drug, Adenine Nucleotides, Receptors, Purinergic P2, Tumor Necrosis Factor-alpha, apoptosis, Uracil, Articles, Cell Biology, Fibrosis, Molecular biology, cytokines, Rats, Cell biology, chemistry, Bisbenzimidazole, Molecular Medicine, Signal transduction, Adenosine triphosphate, Uracil nucleotide, signal transduction

Abstract

We previously showed that the human heart expresses all known P2X and P2Y receptors activated by extra-cellular adenine or uracil nucleotides. Despite evidence that, both in humans and rodents, plasma levels of ATP and UTP markedly increase during myocardial infarction, the differential effects mediated by the various adenine- and uracil-preferring myocardial P2 receptors are still largely unknown. Here, we studied the effects of adenine and uracil nucleotides on murine HL-1 cardiomyocytes. RT-PCR analysis showed that HL-1 cardiomyocytes express all known P2X receptors (except for P2X(2)), as well as the P2Y(2,4,6,14) subtypes. Exposure of cardiomyocytes to adenine nucleotides (ATP, ADP or BzATP) induced apoptosis and necrosis, as determined by flow-cytometry. Cell death was exacerbated by tumour necrosis factor (TNF)-alpha, a cytokine implicated in chronic heart failure progression. Conversely, uracil nucleotides (UTP, UDP and UDPglucose) had no effect 'per se', but fully counteracted the deleterious effects induced by adenine nucleotides and TNF-alpha, even if added to cardiomyocytes after beginning exposure to these cell death-inducing agents. Thus, exposure of cardiomyocytes to elevated concentrations of ATP or ADP in the presence of TNF-alpha contributes to cell death, an effect which is counteracted by uracil-preferring P2 receptors. Cardiomyocytes do not need to be 'primed' by uracil nucleotides to become insensitive to adenine nucleotides-induced death, suggesting the existence of a possible 'therapeutic' window for uracil nucleotides-mediated protection. Thus, release of UTP during cardiac ischaemia and in chronic heart failure may protect against myocardial damage, setting the basis for developing novel cardioprotective agents that specifically target uracil-preferring P2Y receptors.

Published

2008

30. Lactoferrin, a major defense protein of innate immunity, is a novel maturation factor for human dendritic cells

Author

Guido Forni, Federica Pericle, Mirella Giovarelli, Atul Varadhachary, Michela Spadaro, Cristiana Caorsi, and Patrizia Ceruti

Subjects

T-Lymphocytes, Antigen presentation, chemical and pharmacologic phenomena, In Vitro Techniques, Biology, Lymphocyte Activation, Models, Biological, Biochemistry, Monocytes, Chemokine receptor, Antigen, T-cell activation, Genetics, Humans, CXCL10, adaptive immunity, antigen presentation, innate immunity, Molecular Biology, CD86, Innate immune system, Cell Differentiation, hemic and immune systems, Dendritic Cells, Acquired immune system, Immunity, Innate, Recombinant Proteins, Lactoferrin, Immunology, Cytokines, CD80, Biotechnology

Abstract

Lactoferrin (LF) is an important protein component of the innate immune system that is broadly distributed within the body fluids. LF is endowed with multiple biological activities. Talactoferrin (TLF), a recombinant human LF, is in clinical development as an anticancer agent and is entering Phase III clinical trials. Here, we show that TLF induces the maturation of human dendritic cells (DCs) derived from monocytes. TLF, at physiologically relevant concentrations (100 microg/ml) up-regulates the expression of human leukocyte antigen (HLA) class II, CD83, CD80, and CD86 costimulatory molecule and CXCR4 and CCR7 chemokine receptors, acting primarily through the p38 MAPK signaling pathway. DCs matured by TLF displayed an enhanced release of IL-8 and CXCL10, as well as a significantly reduced production of IL-6, IL-10, and CCL20. They also display a reduced ability to take up antigen and increased capacity to trigger proliferation and release IFN-gamma in the presence of allogeneic human T cells. TLF-matured DCs are able to prime naive T cells to respond to KLH antigen and display a significantly increased capacity to present Flu-MA(58-66) peptide to HLA-A2-matched T cells. These data suggest that a key immunomodulatory function that may be mediated by TLF is to link the innate with adaptive immunity through DC maturation.

Published

2008

31. INK4 proteins, a family of mammalian CDK inhibitors with novel biological functions

Author

Mariela C. Marazita, Maria Florencia Ogara, Eduardo T. Cánepa, Pablo Federico Sirkin, María Elida Scassa, Abel L. Carcagno, and Julieta M. Ceruti

Subjects

DNA Repair, DNA repair, Clinical Biochemistry, Cyclin A, Apoptosis, Biochemistry, Cyclin-dependent kinase, Genetics, Animals, Humans, E2F, Molecular Biology, Cellular Senescence, Cyclin-Dependent Kinase Inhibitor Proteins, Cyclin, biology, Cyclin-Dependent Kinase 4, Cell Biology, Cell cycle, Cell biology, Cell Transformation, Neoplastic, Multigene Family, biology.protein, Ankyrin repeat, Cyclin-dependent kinase 6

Abstract

The cyclin D-Cdk4-6/INK4/Rb/E2F pathway plays a key role in controlling cell growth by integrating multiple mitogenic and antimitogenic stimuli. The members of INK4 family, comprising p16(INK4a), p15(INK4b), p18(INK4c), and p19(INK4d), block the progression of the cell cycle by binding to either Cdk4 or Cdk6 and inhibiting the action of cyclin D. These INK4 proteins share a similar structure dominated by several ankyrin repeats. Although they appear to be structurally redundant and equally potent as inhibitors, the INK4 family members are differentially expressed during mouse development. The striking diversity in the pattern of expression of INK4 genes suggested that this family of cell cycle inhibitors might have cell lineage-specific or tissue-specific functions. The INK4 proteins are commonly lost or inactivated by mutations in diverse types of cancer, and they represent established or candidate tumor suppressors. Apart from their capacity to arrest cells in the G1-phase of the cell cycle they have been shown to participate in an increasing number of cellular processes. Given their emerging roles in fundamental physiological as well as pathological processes, it is interesting to explore the diverse roles for the individual INK4 family members in different functions other than cell cycle regulation. Extensive studies, over the past few years, uncover the involvement of INK4 proteins in senescence, apoptosis, DNA repair, and multistep oncogenesis. We will focus the discussion here on these unexpected issues.

Published

2007

32. A role for P2X7in microglial proliferation

Author

Claudia Verderio, Maria P. Abbracchio, Davide Ferrari, Michela Matteoli, Cinzia Pizzirani, Marta Fumagalli, Alessio Colombo, Fabio Bianco, Francesco Di Virgilio, and Stefania Ceruti

Subjects

Lipopolysaccharides, medicine.medical_specialty, Blotting, Western, Biology, Biochemistry, Cell Line, Mice, Cellular and Molecular Neuroscience, Internal medicine, medicine, Animals, RNA, Small Interfering, Receptor, Egtazic Acid, Cell Proliferation, Benzoxazoles, Microglia, Receptors, Purinergic P2, Reverse Transcriptase Polymerase Chain Reaction, Effector, Apyrase, Cell growth, Quinolinium Compounds, Flow Cytometry, Cell biology, medicine.anatomical_structure, Endocrinology, Apoptosis, Cell culture, Neuroglia, Calcium, RNA Interference, Receptors, Purinergic P2X7, Oxidation-Reduction

Abstract

Microglia, glial cells with an immunocompetent role in the CNS, react to stimuli from the surrounding environment with alterations of their phenotypic response. Amongst other activating signals, the endotoxin lipopolysaccharide (LPS) is widely used as a tool to mimic bacterial infection in the CNS. LPS-activated microglia undergo dramatic changes in cell morphology/activity; in particular, they stop proliferating and differentiate from resting to effector cells. Activated microglia also show modifications of purinoreceptor signalling with a significant decrease in P2X(7) expression. In this study, we demonstrate that the down-regulation of the P2X(7) receptor in activated microglia may play an important role in the antiproliferative effect of LPS. Indeed, chronic blockade of the P2X(7) receptor by antagonists (oxidized ATP, KN62 and Brilliant Blue G), or treatment with the ATP-hydrolase apyrase, severely decreases microglial proliferation, down-regulation of P2X(7) receptor expression by small RNA interference (siRNA) decreases cell proliferation, and the proliferation of P2X(7)-deficient N9 clones and primary microglia, in which P2X(7) expression is down-regulated by siRNA, is unaffected by either LPS or P2X(7) antagonists. Furthermore, flow cytometric analysis indicates that exposure to oxidized ATP or treatment with LPS reversibly decreases cell cycle progression, without increasing the percentage of apoptotic cells. Overall, our data show that the P2X(7) receptor plays an important role in controlling microglial proliferation by supporting cell cycle progression.

Published

2006

33. Ambulatory Blood Pressure Monitoring in Secondary Arterial Hypertension Due to Adrenal Diseases

Author

Michele Ceruti, S. Cerci, Domenico Vitolo, C. Caliumi, Dario Cotesta, Antonio Ciardi, Claudio Letizia, Valentina Serra, Luigi Petramala, Giorgio De Toma, and Monica Iorio

Subjects

Male, medicine.medical_specialty, Ambulatory blood pressure, Endocrinology, Diabetes and Metabolism, Adrenal Gland Diseases, Essential hypertension, Adrenocortical adenoma, Primary aldosteronism, Internal medicine, Heart rate, Internal Medicine, medicine, Humans, Risk factor, business.industry, Blood Pressure Monitoring, Ambulatory, Middle Aged, medicine.disease, Original Papers, Circadian Rhythm, Blood pressure, Hypertension, Cardiology, Female, Cardiology and Cardiovascular Medicine, Adrenal hypertension, business

Abstract

The aim of this study was to evaluate ambulatory blood pressure monitoring in patients with essential hypertension and hypertension caused by adrenal pathology. Sixty‐six patients with primary aldosteronism, 37 with pheochromocytomas, and 45 with adrenal incidentalomas were included. These patients were compared with 152 essential hypertensive patients and 64 normotensive subjects. Ambulatory blood pressure monitoring evaluated daytime and nighttime systolic and diastolic blood pressure and heart rate. The authors found that the “nondipper” phenomenon was present in 51.5% of patients with primary aldosteronism, 43.2% with pheochromocytomas, 42.2% with incidentalomas, 34.2% with hypertension, and 15% of subjects who were normotensive. In 58% of primary aldosteronism patients with idiopathic adrenal hyperplasia, there was an absence of the physiologic blood pressure nocturnal fall (nondipper), which was statistically significant (P

Published

2006

34. Synthesis and biological activity of new lodoacetamide derivatives on mutants of squalene-hopene cyclase

Author

Gianni Balliano, Flavio Rocco, A. Lenhart, Francesco Castelli, Paola Milla, Maurizio Ceruti, and Georg E. Schulz

Subjects

Spectrometry, Mass, Electrospray Ionization, Magnetic Resonance Spectroscopy, biology, Stereochemistry, Organic Chemistry, Mutant, Active site, Bacillus, Biological activity, Cell Biology, Squalene-hopene cyclase, Biochemistry, Cyclase, Iodoacetamide, Serine, chemistry.chemical_compound, chemistry, Mutation, biology.protein, Intramolecular Transferases, Cysteine

Abstract

New iodoacetamide derivatives, containing a dodecyl or a squalenyl moiety, were synthesized. The effect of these new thiol-reacting molecules was studied on two mutants of Alicyclobacillus acidocaldarius squalene-hopene cyclase constructed especially for this purpose. In the quintuple mutant, all five cysteine residues of the enzyme are substituted with serine; in the sextuple mutant, this quintuple substitution is accompanied by the substitution of aspartate D376, located at the enzyme's active site, with a cysteine. N-Dodecyliodoacetamide had little activity toward either mutant, whereas N-squalenyliodoacetamide showed a stronger effect on the sextuple than on the quintuple mutant, as expected.

Published

2005

35. Regulation of A2B adenosine receptor functioning by tumour necrosis factor a in human astroglial cells

Author

Alessia Mazzola, Nico Mitro, Maria Letizia Trincavelli, M Marroni, D. Tuscano, Claudia Martini, Stefania Ceruti, and Maria P. Abbracchio

Subjects

medicine.medical_specialty, MRS-1706, Biology, Adenosine A3 receptor, Biochemistry, Adenosine receptor, Adenosine, Cell biology, Adenylyl cyclase, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Endocrinology, chemistry, Internal medicine, medicine, Enzyme-linked receptor, Receptor, Adenosine A2B receptor, medicine.drug

Abstract

Low-affinity A2B adenosine receptors (A2B ARs), which are expressed in astrocytes, are mainly activated during brain hypoxia and ischaemia, when large amounts of adenosine are released. Cytokines, which are also produced at high levels under these conditions, may regulate receptor responsiveness. In the present study, we detected A2B AR in human astrocytoma cells (ADF) by both immunoblotting and real-time PCR. Functional studies showed that the receptor stimulated adenylyl cyclase through Gs proteins. Moreover, A2B ARs were phosphorylated and desensitized following stimulation of the receptors with high agonist concentration. Tumour necrosis factor alpha (TNF-α) treatment (24- h) increased A2B AR functional response and receptor G protein coupling, without any changes in receptor protein and mRNA levels. TNF-α markedly reduced agonist-dependent receptor phosphorylation on threonine residues and attenuated agonist-mediated A2B ARs desensitization. In the presence of TNF-α, A2B AR stimulation in vitro induced the elongation of astrocytic processes, a typical morphological hallmark of in vivo reactive astrogliosis. This event was completely prevented by the selective A2B AR antagonist MRS 1706 and required the presence of TNF-α. These results suggest that, in ADF cells, TNF-α selectively modulates A2B AR coupling to G proteins and receptor functional response, providing new insights to clarify the pathophysiological role of A2B AR in response to brain damage.

Published

2004

36. Blockade of A2A adenosine receptors prevents basic fibroblast growth factor-induced reactive astrogliosis in rat striatal primary astrocytes

Author

Maria P. Abbracchio, Roberta Brambilla, Stefania Ceruti, Lorenzo Cottini, and Marta Fumagalli

Subjects

medicine.medical_specialty, Adenosine, Adenosine A2 Receptor Agonists, Receptor, Adenosine A2A, Vasodilator Agents, Basic fibroblast growth factor, Fluorescent Antibody Technique, Adenosine-5'-(N-ethylcarboxamide), Biology, Neuroprotection, Cellular and Molecular Neuroscience, chemistry.chemical_compound, Internal medicine, Glial Fibrillary Acidic Protein, Phenethylamines, medicine, Animals, Drug Interactions, Gliosis, RNA, Messenger, Receptor, Cells, Cultured, Cerebral Cortex, Dose-Response Relationship, Drug, Reverse Transcriptase Polymerase Chain Reaction, Triazoles, medicine.disease, Adenosine A3 receptor, Adenosine receptor, Corpus Striatum, Adenosine A2 Receptor Antagonists, Rats, Cell biology, Astrogliosis, Neuroprotective Agents, Pyrimidines, Endocrinology, medicine.anatomical_structure, Animals, Newborn, Neurology, chemistry, Purines, Astrocytes, Neuroglia, Fibroblast Growth Factor 2, Cell Division, Astrocyte

Abstract

Previous literature data show that blockade of A(2A) adenosine receptors via selective antagonists induces protection in various models of neurodegenerative diseases. The mechanisms underlying this effect are still largely unknown. Since it is known that excessive reactive astrogliosis is a factor contributing to cell death in diseases characterized by neurodegenerative events, the present study has been aimed at determining whether selective A(2A) receptor antagonists can counteract the formation of reactive astrocytes induced in vitro by basic fibroblast growth factor (bFGF), a typical trigger of this reaction. Exposure of primary rat striatal astrocytes to the selective A(2A) antagonist SCH58261 resulted in concentration-dependent abolition of bFGF induction of astrogliosis in vitro. This effect could also be reproduced with the chemically unrelated A(2A) antagonist KW-6002. The direct activation of A(2A) adenosine receptors by selective receptor agonists was not sufficient per se to induce astrogliosis, suggesting that the A(2A) receptor needs to act in concert with other bFGF-induced genes to trigger the formation of reactive astrocytes. These results provide a mechanism at the basis of the neuroprotection induced by A(2A) receptor antagonists in models of brain damage and highlight this adenosine receptor subtype as a novel target for the pharmacological modulation of the gliotic reaction.

Published

2003

37. Intracellular phosphorylation of chloro-adenosine analogs is a prerequisite for activation of caspase-3 and induction of apoptosis in human astrocytoma cells

Author

Flaminio Cattabeni, Maria P. Abbracchio, Elena Beltrami, Davide Passera, Elena Piantoni, Stefania Ceruti, and Alessia Mazzola

Subjects

Programmed cell death, biology, Kinase, Caspase 3, Adenosine, Cell biology, Enzyme activator, Biochemistry, Apoptosis, Drug Discovery, medicine, biology.protein, Intracellular, Caspase, medicine.drug

Abstract

We previously demonstrated that both Cladribine (2-chloro-deoxyadenosine) and the related compound 2-chloroadenosine induce apoptosis of human astrocytoma cells (Ceruti et al. [2000] J Neurosci Res 60:388-400). In the present study we have characterized the role of the most important effector caspase (caspase-3) in the same experimental model and the relationship between the intracellular phosphorylation of the two adenosine analogs and activation of this enzyme. Data show that: 1) both adenosine analogs can activate caspase-3 in a time-dependent fashion; 2) significant activation of the enzyme (i.e., 6-7-fold over control level) can be detected before any appearance of nuclear signs of apoptosis; 3) the degree of caspase-3 activation is proportional to the percentage of apoptosis at the end of the incubation period, suggesting a causal relationship between enzyme activation and induction of cell death; and 4) both activation of caspase-3 and induction of cell death can be completely prevented by preexposure of cultures to inhibitors of the intracellular phosphorylation of 2-chloroadenosine and 2-chloro-2'-deoxyadenosine (namely, 5-iodotubercidin and 2'-deoxycytidine, respectively). Adenosine analogs act, therefore, as prodrugs and the toxic species are represented by the corresponding chloronucleotides. The pathways upstream of caspase-3 activation in human astrocytoma cells still remain to be elucidated. Taken together, these data strongly suggest a possible use of adenosine analogs in the pharmacological treatment of central nervous system tumors and of all tumors characterized by a high activity of nucleoside kinases leading to selective intracellular accumulation of toxic chloro-nucleotides.

Published

2003

38. Capillaria hepatica Infection in Wild Brown Rats (Rattus norvegicus) from the Urban Area of Milan, Italy

Author

Eugenio Scanziani, F. Vezzoli, S. Cammarata, A. M. Giusti, Roberta Ceruti, O. Sonzogni, and F. Origgi

Subjects

Pathology, medicine.medical_specialty, Liver infection, biology, Urban Health, Animals, Wild, Enoplida Infections, SINGLE LOBE, General Medicine, Capillaria hepatica, biology.organism_classification, Rats, Rodent Diseases, Italy, Liver, Hepatica, Capillaria, parasitic diseases, Prevalence, medicine, Animals, Humans, Disease Reservoirs

Abstract

Summary Forty-seven wild brown rats (Rattus norvegicus) collected from the urban area of Milan (Italy) were screened for Capillaria hepatica liver infection. The liver of each rat was grossly and histologically examined for the presence of C. hepatica adults, eggs and typical C. hepatica-induced lesions. In 17 rats (36%) liver lesions consistent with C. hepatica infection were detected. Grossly, white‐yellow nodules of 1‐5 mm in diameter were present, either scattered on the liver surface or localized in a single lobe. Histologically, granulomatous liver lesions associated with eggs and/or worms were observed. The degree of gross liver involvement was moderate in most of the positive cases (71%). About 30 cases of C. hepatica infection in humans have been documented world-wide, most of which are reported in children from 1 to 5 years of age. Our results suggest that the potential transmission of C. hepatica to children in the study area should be considered an important health issue.

Published

2001

39. Acute methylprednisolone administration induces a transient alteration of glucose tolerance and pyruvate dehydrogenase in humans

Author

Gianfranco Pagano, Paolo Cavallo-Perin, Silvia Mioletti, Pellacani A, M.T. Rinaudo, A. Bruno, C. Ceruti, M. Curto, and Paolo Fornengo

Subjects

medicine.medical_specialty, Glucose tolerance test, medicine.diagnostic_test, Insulin, medicine.medical_treatment, Clinical Biochemistry, General Medicine, Carbohydrate metabolism, Biology, Pyruvate dehydrogenase complex, Biochemistry, Endocrinology, Methylprednisolone, Internal medicine, medicine, Lipolysis, Glucocorticoid, Ex vivo, medicine.drug

Abstract

Background Glucocorticoid administration induces alteration of glucose tolerance, and impairment of glucose oxidation may contribute to glucocorticoid-induced derangement of glucose metabolism. We investigated glucose tolerance following methylprednisolone administration in humans. In the same model, we evaluated pyruvate dehydrogenase (PDH), the rate limiting enzyme of glucose oxidation, in peripheral blood mononuclear cells. Materials and methods Methylprednisolone (2 × 40 mg, iv, one dose every 12 h) was administered to six healthy volunteers. Glucose tolerance was evaluated through an oral glucose tolerance test (oGTT, 75 g glucose) at least a week before and after drug administration (2 and 24 h post-drug). To assess modifications of lipid metabolism circulating free fatty acids (FFA) and glycerol were measured, during fasting and oGTT. The active form of PDH (PDHa) was evaluated in peripheral blood mononuclear cells, both as ex vivo activity and as in vitro response to insulin (30pmol l−1). Results Methylprednisolone induced an alteration of glucose tolerance 2 h after its administration. Such alteration was completely reversed at 24 h. Alteration of glucose tolerance was accompanied by decreased ex vivo PDHa activity. PDH responsiveness to insulin in vitro was also impaired. Circulating FFA were unmodified, but decreased glycerol levels suggested a slight inhibition of lipolysis. Conclusions Acute methylprednisolone administration in humans induced a transient decrease of glucose tolerance 2 h after drug administration, accompanied by hyperinsulinaemia, inhibition of ex vivo PDH activity and its response to insulin in vitro. These alterations were completely abolished at 24 h, suggesting that methylprednisolone can be safely administered acutely. Furthermore, methylprednisolone induced only minor modifications of circulating FFA and glycerol, indicating minimal impact on lipid metabolism.

Published

1999

40. Best second trimester sonographic markers for the detection of trisomy 21

Author

Patrizia Ceruti, Eloisa Mariani, Patrizia Vergani, Alessandro Ghidini, John C. Pezzullo, Anna Locatelli, and Maria Giovanna Piccoli

Subjects

Adult, medicine.medical_specialty, Aneuploidy, Gestational Age, Ultrasonography, Prenatal, Pyelectasis, Pregnancy, medicine, Humans, Radiology, Nuclear Medicine and imaging, Univariate analysis, Radiological and Ultrasound Technology, business.industry, Echogenicity, Odds ratio, Middle Aged, medicine.disease, Confidence interval, Fetal Diseases, Logistic Models, Pregnancy Trimester, Second, Female, Choroid plexus, Radiology, Down Syndrome, business, Trisomy, Maternal Age

Abstract

We analyzed all genetic sonograms obtained during a 6 year period to establish the independent ability of the following sonographic markers of aneuploidy in the diagnosis of trisomy 21: structural anomalies, cardiac abnormalities, nuchal fold thickness of 6 mm or greater, bowel echogenicity, choroid plexus cysts, and renal pyelectasis. With the exception of bowel echogenicity and choroid plexus cysts, the sonographic markers were more common in trisomy 21 than euploid fetuses (all P < 0.001). Logistic regression analysis demonstrated that cardiac anomalies (odds ratio = 255; 95% confidence interval, 25, 2592), other structural anomalies (odds ratio = 25; 95% confidence interval, 6, 97), and nuchal fold thickness of 6 mm or greater (odds ratio = 13; 95% confidence interval, 3, 50) were the only independent predictors of trisomy 21. The false-positive rate and sensitivity were 5.3% (48 of 898) and 59.2% (13 of 22), respectively, when any of the sonographic markers significant at univariate analysis was considered, and 3.1% (28 of 898) and 54.5% (12 of 22), respectively, when any of the predictors at multivariate analysis was present. Because a considerable overlap of sonographic markers exists among trisomy 21 fetuses, use of those that are not independent predictors leads to an increase in false-positive rate without a gain in sensitivity.

Published

1999

41. Complexity and the Unfinished Nature of Human Evolution

Author

Gianluca Bocchi and Mauro Ceruti

Subjects

History and Philosophy of Science, Human evolution, Evolutionary biology, General Neuroscience, Sociology, General Biochemistry, Genetics and Molecular Biology

Published

1999

42. Cyclo-oxygenase-2 mediates P2Y receptor-induced reactive astrogliosis

Author

Albino Bonazzi, Geoffrey Burnstock, Maria P. Abbracchio, Flaminio Cattabeni, Roberta Brambilla, and Stefania Ceruti

Subjects

Pharmacology, medicine.medical_specialty, P2Y receptor, Alpha (ethology), Biology, medicine.disease, Astrogliosis, medicine.anatomical_structure, Endocrinology, Gliosis, Downregulation and upregulation, Internal medicine, medicine, Neuroglia, medicine.symptom, Receptor, Astrocyte

Abstract

Excessive cyclo-oxygenase-2 (COX-2) induction may play a role in chronic neurological diseases characterized by inflammation and astrogliosis. We have previously identified an astroglial receptor for extracellular nucleotides, a P2Y receptor, whose stimulation leads to arachidonic acid (AA) release, followed, 3 days later, by morphological changes resembling reactive astrogliosis. Since COX-2 may be upregulated by AA metabolites, we assessed a possible role for COX-2 in P2Y receptor-mediated astrogliosis. A brief challenge of rat astrocytes with the ATP analogue alpha,beta-methylene ATP (alpha,beta(me)ATP) resulted, 24 h later, in significantly increased COX-2 expression. The selective COX-2 inhibitor NS-398 completely abolished alpha,beta(me)ATP-induced astrocytic activation. Constitutive astroglial COX-1 or COX-2 did not play any role in purine-induced reactive astrogliosis. PGE2, a main metabolite of COX-2, also induced astrocytic activation. These data suggest that a P2Y receptor mediates reactive astrogliosis via induction of COX-2. Antagonists selective for this receptor may counteract excessive COX-2 activation in both acute and chronic neurological diseases.

Published

1999

43. SNX27, a protein involved in down syndrome, regulates GPR17 trafficking and oligodendrocyte differentiation

Author

Meraviglia, Veronica, primary, Ulivi, Alessandro Francesco, additional, Boccazzi, Marta, additional, Valenza, Fabiola, additional, Fratangeli, Alessandra, additional, Passafaro, Maria, additional, Lecca, Davide, additional, Stagni, Fiorenza, additional, Giacomini, Andrea, additional, Bartesaghi, Renata, additional, Abbracchio, Maria P., additional, Ceruti, Stefania, additional, and Rosa, Patrizia, additional

Published

2016

44. Characterization of the signalling pathways involved in ATP and basic fibroblast growth factor-induced astrogliosis

Author

Stefania Ceruti, Lina Puglisi, Geoffrey Burnstock, Roberta Brambilla, Flaminio Cattabeni, Chiara Bolego, and Maria P. Abbracchio

Subjects

Pharmacology, Phospholipase C, Basic fibroblast growth factor, P2 receptor, Biology, medicine.disease, Pertussis toxin, Receptor tyrosine kinase, Astrogliosis, Cell biology, Adenylyl cyclase, chemistry.chemical_compound, chemistry, Biochemistry, medicine, biology.protein, Protein kinase C

Abstract

1. A brief challenge of rat astrocytes with either alpha, beta-methyleneATP (alpha, beta-meATP) or basic fibroblast growth factor (bFGF) resulted, three days later, in morphological differentiation of cells, as shown by marked elongation of astrocytic processes. The P2 receptor antagonist suramin prevented alpha, beta-meATP- but not bFGF-induced astrocytic elongation. Similar effects on astrocytic elongation were also observed with ATP and other P2 receptor agonists (beta, gamma meATP, ADP beta S, 2meSATP and, to a lesser extent, UTP). 2. Pertussis toxin completely abolished alpha, beta-meATP- but not bFGF-induced effects. No effects were exerted by alpha, beta-meATP on cyclic AMP production; similarly, neomycin had no effects on elogation of processes induced by the purine analogue, suggesting that adenylyl cyclase and phospholipase C are probably not involved in alpha, beta-meATP-induced effects (see also the accompanying paper by Centemeri et al., 1997). The tyrosine-kinase inhibitor genistein greatly reduced bFGF- but not alpha, beta-meATP-induced astrocytic elongation. 3. Challenge of cultures with alpha, beta-meATP rapidly and concentration-dependently increased [3H]-arachidonic acid (AA) release from cells, suggesting that activation of phospholipase A2 (PLA2) may be involved in the long-term functional effects evoked by purine analogues. Consistently, exogenously added AA markedly elongated astrocytic processes. Moreover, various PLA2 inhibitors (e.g. mepacrine and dexamethasone) prevented both the early alpha, beta-meATP-induced [3H]-AA release and/or the associated long-term morphological changes, without affecting the astrocytic elongation induced by bFGF. Finally, the protein kinase C (PKC) inhibitor H7 fully abolished alpha, beta-meATP- but not bFGF-induced effects. 4. Both alpha, beta-meATP and bFGF rapidly and transiently induced the nuclear accumulation of Fos and Jun. Both c-fos and c-jun induction by the purine analogue could be fully prevented by pretreatment with suramin. In contrast, the effects of bFGF were unaffected by this P2 receptor antagonist. 5. It was concluded that alpha, beta-meATP- and bFGF-morphological differentiation of astrocytes occurs via independent transductional pathways. For the purine analogue, signalling involves a Gi/G(o) protein-coupled P2Y-receptor which may be linked to activation of PLA2 (involvement of an arachidonate-sensitive PKC is speculated); for bFGF, a tyrosine kinase receptor is involved. Both pathways merge on some common intracellular target, as suggested by induction of primary response genes, which in turn may regulate late response genes mediating long-term phenotypic changes of astroglial cells. 6. These findings implicate P2 receptors as novel targets for the pharmacological regulation of reactive astrogliosis, which has intriguing implications in nervous system diseases characterized by degenerative events.

Published

1997

45. Mass spectrometric behaviour of some 19-aza and 2-aza squalene derivatives

Author

Marizio Ceruti and Roberta Seraglia

Subjects

Squalene, chemistry.chemical_compound, chemistry, Organic Chemistry, Organic chemistry, Mass spectrometric, Spectroscopy, Analytical Chemistry

Published

1997

46. Effects of ATP analogues and basic fibroblast growth factor on astroglial cell differentiation in primary cultures of rat striatum

Author

R. Langfelder, Stefania Ceruti, Maria P. Abbracchio, F. Cattabeni, M. J. Saffrey, and Geoffrey Burnstock

Subjects

Cellular differentiation, medicine.medical_treatment, Suramin, Basic fibroblast growth factor, Alpha (ethology), Rats, Sprague-Dawley, chemistry.chemical_compound, Adenosine Triphosphate, Developmental Neuroscience, Glial Fibrillary Acidic Protein, medicine, Animals, Cells, Cultured, Glial fibrillary acidic protein, biology, Growth factor, Cell Differentiation, Rats, Cell biology, Neostriatum, chemistry, Fluorescent Antibody Technique, Direct, Purines, Astrocytes, biology.protein, Fibroblast Growth Factor 2, Adenosine triphosphate, Intracellular, Developmental Biology, medicine.drug

Abstract

We have used primary cultures of rat striatum to study the effects of ATP analogues on the elongation of astrocytic processes, a parameter of astroglial cell differentiation. Parallel studies were performed with basic fibroblast growth factor, a known regulator of astroglial cell function. After three days in culture, both the growth factor and alpha beta-methylene-ATP induced dramatic increases in the mean length of astrocytic processes/cell. For both agents, effects were dose-dependent. The effect of alpha beta-methylene-ATP was antagonized by the trypanoside suramin and mimicked by 2-methyl-thio-ATP, suggesting the involvement of a suramin-sensitive P2-purinoceptor. Neither an additive nor a synergistic effect between alpha beta-methylene-ATP and basic fibroblast growth factor on the elongation of processes was detected in cultures exposed to both agents. Indeed, an inhibition with respect to the effects induced by either agent alone was recorded, suggesting that the growth factor and the purine analogue can modulate astrocytic differentiation by activation of common intracellular pathways. It is concluded that, like basic fibroblast growth factor, ATP can promote the maturation of astrocytes towards a more differentiated phenotype characterized by the presence of longer astrocytic processes. These findings might have interesting implications for astroglial cell differentiation during brain development and for ischemia- and trauma-associated hypergliosis.

Published

1995

47. Preliminary screening of some squalenoid derivatives for toxicity towards dermatophytes

Author

D. Airaudi, V. Filipello Marchisio, Maurizio Ceruti, and A. Giannetta

Subjects

Squalene, biology, Serial dilution, Squalene monooxygenase, Chemistry, Arthrodermataceae, Drug Evaluation, Preclinical, Biological activity, Microbial Sensitivity Tests, Dermatology, General Medicine, biology.organism_classification, medicine.disease_cause, Cyclase, Microbiology, Minimum inhibitory concentration, Infectious Diseases, Dermatophyte, medicine, Trichophyton, Microsporum canis

Abstract

We report a preliminary study of the in vitro anti-dermatophyte activity of six squalenoid derivatives that inhibit 2,3-oxidosqualene cyclase and squalene epoxidase: 2-aza-2,3-dihydrosqualene, 22,23-epoxy-2-aza-2,3-dihydrosqualene, azasqualene alcohol, 19-aza-18,19,22,23-tetrahydrosqualene, 2,3-epoxy-19-aza-18,19,22,23-tetrahydrosqualene and hexafluorosqualene epoxide. The tests were done by inoculating 10 microliters of Trichophyton mentagrophytes (Robin) Blanchard or Microsporum canis Bodin homogenate into 1 ml of Sabouraud glucose liquid medium containing serial dilutions from 100 to 0.25 micrograms ml-1 of the substance. For each compound the minimum inhibitory concentration (MIC) and the minimum fungicidal concentration (MFC) were determined. The most effective compounds were 22,23-epoxy-2-aza-2,3-dihydrosqualene and azasqualene alcohol, with MICs respectively of 3 and 6.25 micrograms ml-1 for each of the two species of dermatophyte. The first of these compounds was the only one to show fungicidal activity over the range of concentrations tested.

Published

1995

48. A prospective multicentric international study on the surgical outcomes and patients’ satisfaction rates of the ‘sliding’ technique for end-stage Peyronie's disease with severe shortening of the penis and erectile dysfunction

Author

Rolle, Luigi, primary, Falcone, Marco, additional, Ceruti, Carlo, additional, Timpano, Massimiliano, additional, Sedigh, Omid, additional, Ralph, David J., additional, Kuehhas, Franklin, additional, Oderda, Marco, additional, Preto, Mirko, additional, Sibona, Mattia, additional, Gillo, Arianna, additional, Garaffa, Giulio, additional, Gontero, Paolo, additional, and Frea, Bruno, additional

Published

2015

49. ChemInform Abstract: Study of (1-Alkoxyethyl) Diphenylphosphine Oxides. Part 4. Conclusive Conformational Study by NMR and Molecular Mechanics Calculations

Author

Davide Viterbo, M. Giannini, Lionello Pogliani, Piero Ugliengo, and Maurizio Ceruti

Subjects

chemistry.chemical_compound, Diphenylphosphine, chemistry, Organic chemistry, General Medicine, Molecular mechanics

Published

2010

50. ChemInform Abstract: 2,3-Oxidosqualene Cyclase and Squalene Epoxidase as Target Enzymes for the Development of New Sterol Biosynthesis Inhibitors

Author

Franca Viola, Maurizio Ceruti, Gianni Balliano, and Luigi Cattel

Subjects

chemistry.chemical_classification, 2,3-Oxidosqualene, chemistry.chemical_compound, Enzyme, chemistry, Biochemistry, Squalene monooxygenase, Stereochemistry, General Medicine, Sterol biosynthesis, Cyclase

Published

2010