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171 results on '"De Candia, A"'

1. Novel 6-alkyl-bridged 4-arylalkylpiperazin-1-yl derivatives of azepino[4,3-b]indol-1(2H)-one as potent BChE-selective inhibitors showing protective effects against neurodegenerative insults

Author

Samarelli, Francesco, primary, Purgatorio, Rosa, additional, Lopopolo, Gianfranco, additional, Deruvo, Caterina, additional, Catto, Marco, additional, Andresini, Michael, additional, Carrieri, Antonio, additional, Nicolotti, Orazio, additional, De Palma, Annalisa, additional, Miniero, Daniela Valeria, additional, de Candia, Modesto, additional, and Altomare, Cosimo D., additional

Published
2024
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3. Association of laboratory test results with the bleeding history in patients with inherited platelet function disorders (the BAT-LAB substudy): communication from the Platelet Physiology ISTH-SSC

Author

Gresele, Paolo, primary, Falcinelli, Emanuela, additional, Bury, Loredana, additional, Alessi, Marie-Christine, additional, Guglielmini, Giuseppe, additional, Falaise, Céline, additional, Podda, Gianmarco, additional, Fiore, Mathieu, additional, Mazziotta, Francesco, additional, Sevivas, Teresa, additional, Bermejo, Nuria, additional, De Candia, Erica, additional, Chitlur, Meera, additional, Lambert, Michele P., additional, Barcella, Luca, additional, Glembotsky, Ana C., additional, and Lordkipanidzé, Marie, additional

Published
2023
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4. Regulatory T cells as metabolic sensors

Author

Paola de Candia, Claudio Procaccini, Claudia Russo, Maria Teresa Lepore, Giuseppe Matarese, de Candia, Paola, Procaccini, Claudio, Russo, Claudia, Lepore, Maria Teresa, and Matarese, Giuseppe

Subjects
Infectious Diseases, autoimmunity, immunometabolism, Homeostasi, Immunology, Interleukin-2 Receptor alpha Subunit, Homeostasis, Immunology and Allergy, Forkhead Transcription Factors, Immunotherapy, metabolic disease, T-Lymphocytes, Regulatory, Treg cell
Abstract

Compelling experimental evidence links immunity and metabolism. In this perspective, we propose forkhead-box-P3 (FoxP3)+CD4+CD25+ regulatory T (Treg) cells as key metabolic sensors controlling the immunological state in response to their intrinsic capacity to perceive nutritional changes. Treg cell high anabolic state in vivo, residency in metabolically crucial districts, and recirculation between lymphoid and non-lymphoid sites enable them to recognize the metabolic cues and adapt their intracellular metabolism and anti-inflammatory function at the paracrine and systemic levels. As privileged regulators at the interface between neuroendocrine and immune systems, the role of Treg cells in maintaining metabolic homeostasis makes these cells promising targets of therapeutic strategies aimed at restoring organismal homeostasis not only in autoimmune but also metabolic disorders.

Published
2022
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5. Synthesis, computational and experimental pharmacological studies for (thio)ether-triazine 5-HT6R ligands with noticeable action on AChE/BChE and chalcogen-dependent intrinsic activity in search for new class of drugs against Alzheimer's disease

Author

Czarnota-Łydka, Kinga, primary, Sudoł-Tałaj, Sylwia, additional, Kucwaj-Brysz, Katarzyna, additional, Kurczab, Rafał, additional, Satała, Grzegorz, additional, de Candia, Modesto, additional, Samarelli, Francesco, additional, Altomare, Cosimo Damiano, additional, Carocci, Alessia, additional, Barbarossa, Alexia, additional, Żesławska, Ewa, additional, Głuch-Lutwin, Monika, additional, Mordyl, Barbara, additional, Kubacka, Monika, additional, Wilczyńska-Zawal, Natalia, additional, Jastrzębska-Więsek, Magdalena, additional, Partyka, Anna, additional, Khan, Nadia, additional, Więcek, Małgorzata, additional, Nitek, Wojciech, additional, Honkisz-Orzechowska, Ewelina, additional, Latacz, Gniewomir, additional, Wesołowska, Anna, additional, Carrieri, Antonio, additional, and Handzlik, Jadwiga, additional

Published
2023
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6. In-vitro and in-silico studies of annelated 1,4,7,8-tetrahydroazocine ester derivatives as nanomolar selective inhibitors of human butyrylcholinesterase

Author

de Candia, Modesto, primary, Titov, Alexander A., additional, Viayna, Antonio, additional, Kulikova, Larisa N., additional, Purgatorio, Rosa, additional, Piergiovanni, Brigida, additional, Niso, Mauro, additional, Catto, Marco, additional, Voskressensky, Leonid G., additional, Luque, F. Javier, additional, and Altomare, Cosimo D., additional

Published
2023
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8. A study of events with photoelectric emission in the DarkSide-50 liquid argon Time Projection Chamber

Author

Agnes, P, Albuquerque, I, Alexander, T, Alton, A, Ave, M, Back, H, Batignani, G, Biery, K, Bocci, V, Bonivento, W, Bottino, B, Bussino, S, Cadeddu, M, Cadoni, M, Calaprice, F, Caminata, A, Canci, N, Caravati, M, Cargioli, N, Cariello, M, Carlini, M, Carpinelli, M, Catalanotti, S, Cataudella, V, Cavalcante, P, Cavuoti, S, Chepurnov, A, Cicalo, C, Cocco, A, Covone, G, D'Angelo, D, Davini, S, De Candia, A, De Cecco, S, De Filippis, G, De Rosa, G, Derbin, A, Devoto, A, D'Incecco, M, Dionisi, C, Dordei, F, Downing, M, D'Urso, D, Fiorillo, G, Franco, D, Gabriele, F, Galbiati, C, Ghiano, C, Giganti, C, Giovanetti, G, Gorchakov, O, Goretti, A, Grobov, A, Gromov, M, Guan, M, Guardincerri, Y, Gulino, M, Hackett, B, Herner, K, Hosseini, B, Hubaut, F, Hungerford, E, Ianni, A, Ippolito, V, Keeter, K, Kendziora, C, Kochanek, I, Korablev, D, Korga, G, Kubankin, A, Kuss, M, La Commara, M, Lai, M, Li, X, Lissia, M, Longo, G, Machulin, I, Mapelli, L, Mari, S, Maricic, J, Martoff, C, Messina, A, Meyers, P, Milincic, R, Morrocchi, M, Muratova, V, Musico, P, Agasson, A, Nozdrina, A, Oleinik, A, Ortica, F, Pagani, L, Pallavicini, M, Pandola, L, Pantic, E, Paoloni, E, Pelczar, K, Pelliccia, N, Picciau, E, Pocar, A, Pordes, S, Poudel, S, Pralavorio, P, Ragusa, F, Razeti, M, Razeto, A, Renshaw, A, Rescigno, M, Rode, J, Romani, A, Sablone, D, Samoylov, O, Sands, W, Sanfilippo, S, Savarese, C, Schlitzer, B, Semenov, D, Shchagin, A, Sheshukov, A, Skorokhvatov, M, Smirnov, O, Sotnikov, A, Stracka, S, Suvorov, Y, Tartaglia, R, Testera, G, Tonazzo, A, Unzhakov, E, Vishneva, A, Vogelaar, R, Wada, M, Wang, H, Wang, Y, Westerdale, S, Wojcik, M, Xiao, X, Yang, C, Zuzel, G, Agnes P., Albuquerque I. F. M., Alexander T., Alton A. K., Ave M., Back H. O., Batignani G., Biery K., Bocci V., Bonivento W. M., Bottino B., Bussino S., Cadeddu M., Cadoni M., Calaprice F., Caminata A., Canci N., Caravati M., Cargioli N., Cariello M., Carlini M., Carpinelli M., Catalanotti S., Cataudella V., Cavalcante P., Cavuoti S., Chepurnov A., Cicalo C., Cocco A. G., Covone G., D'Angelo D., Davini S., De Candia A., De Cecco S., De Filippis G., De Rosa G., Derbin A. V., Devoto A., D'Incecco M., Dionisi C., Dordei F., Downing M., D'Urso D., Fiorillo G., Franco D., Gabriele F., Galbiati C., Ghiano C., Giganti C., Giovanetti G. K., Gorchakov O., Goretti A. M., Grobov A., Gromov M., Guan M., Guardincerri Y., Gulino M., Hackett B. R., Herner K., Hosseini B., Hubaut F., Hungerford E. V., Ianni A., Ippolito V., Keeter K., Kendziora C. L., Kochanek I., Korablev D., Korga G., Kubankin A., Kuss M., La Commara M., Lai M., Li X., Lissia M., Longo G., Machulin I. N., Mapelli L. P., Mari S. M., Maricic J., Martoff C. J., Messina A., Meyers P. D., Milincic R., Morrocchi M., Muratova V. N., Musico P., Agasson A. N., Nozdrina A. O., Oleinik A., Ortica F., Pagani L., Pallavicini M., Pandola L., Pantic E., Paoloni E., Pelczar K., Pelliccia N., Picciau E., Pocar A., Pordes S., Poudel S. S., Pralavorio P., Ragusa F., Razeti M., Razeto A., Renshaw A. L., Rescigno M., Rode J., Romani A., Sablone D., Samoylov O., Sands W., Sanfilippo S., Savarese C., Schlitzer B., Semenov D. A., Shchagin A., Sheshukov A., Skorokhvatov M. D., Smirnov O., Sotnikov A., Stracka S., Suvorov Y., Tartaglia R., Testera G., Tonazzo A., Unzhakov E. V., Vishneva A., Vogelaar R. B., Wada M., Wang H., Wang Y., Westerdale S., Wojcik M. M., Xiao X., Yang C., Zuzel G., Agnes, P, Albuquerque, I, Alexander, T, Alton, A, Ave, M, Back, H, Batignani, G, Biery, K, Bocci, V, Bonivento, W, Bottino, B, Bussino, S, Cadeddu, M, Cadoni, M, Calaprice, F, Caminata, A, Canci, N, Caravati, M, Cargioli, N, Cariello, M, Carlini, M, Carpinelli, M, Catalanotti, S, Cataudella, V, Cavalcante, P, Cavuoti, S, Chepurnov, A, Cicalo, C, Cocco, A, Covone, G, D'Angelo, D, Davini, S, De Candia, A, De Cecco, S, De Filippis, G, De Rosa, G, Derbin, A, Devoto, A, D'Incecco, M, Dionisi, C, Dordei, F, Downing, M, D'Urso, D, Fiorillo, G, Franco, D, Gabriele, F, Galbiati, C, Ghiano, C, Giganti, C, Giovanetti, G, Gorchakov, O, Goretti, A, Grobov, A, Gromov, M, Guan, M, Guardincerri, Y, Gulino, M, Hackett, B, Herner, K, Hosseini, B, Hubaut, F, Hungerford, E, Ianni, A, Ippolito, V, Keeter, K, Kendziora, C, Kochanek, I, Korablev, D, Korga, G, Kubankin, A, Kuss, M, La Commara, M, Lai, M, Li, X, Lissia, M, Longo, G, Machulin, I, Mapelli, L, Mari, S, Maricic, J, Martoff, C, Messina, A, Meyers, P, Milincic, R, Morrocchi, M, Muratova, V, Musico, P, Agasson, A, Nozdrina, A, Oleinik, A, Ortica, F, Pagani, L, Pallavicini, M, Pandola, L, Pantic, E, Paoloni, E, Pelczar, K, Pelliccia, N, Picciau, E, Pocar, A, Pordes, S, Poudel, S, Pralavorio, P, Ragusa, F, Razeti, M, Razeto, A, Renshaw, A, Rescigno, M, Rode, J, Romani, A, Sablone, D, Samoylov, O, Sands, W, Sanfilippo, S, Savarese, C, Schlitzer, B, Semenov, D, Shchagin, A, Sheshukov, A, Skorokhvatov, M, Smirnov, O, Sotnikov, A, Stracka, S, Suvorov, Y, Tartaglia, R, Testera, G, Tonazzo, A, Unzhakov, E, Vishneva, A, Vogelaar, R, Wada, M, Wang, H, Wang, Y, Westerdale, S, Wojcik, M, Xiao, X, Yang, C, Zuzel, G, Agnes P., Albuquerque I. F. M., Alexander T., Alton A. K., Ave M., Back H. O., Batignani G., Biery K., Bocci V., Bonivento W. M., Bottino B., Bussino S., Cadeddu M., Cadoni M., Calaprice F., Caminata A., Canci N., Caravati M., Cargioli N., Cariello M., Carlini M., Carpinelli M., Catalanotti S., Cataudella V., Cavalcante P., Cavuoti S., Chepurnov A., Cicalo C., Cocco A. G., Covone G., D'Angelo D., Davini S., De Candia A., De Cecco S., De Filippis G., De Rosa G., Derbin A. V., Devoto A., D'Incecco M., Dionisi C., Dordei F., Downing M., D'Urso D., Fiorillo G., Franco D., Gabriele F., Galbiati C., Ghiano C., Giganti C., Giovanetti G. K., Gorchakov O., Goretti A. M., Grobov A., Gromov M., Guan M., Guardincerri Y., Gulino M., Hackett B. R., Herner K., Hosseini B., Hubaut F., Hungerford E. V., Ianni A., Ippolito V., Keeter K., Kendziora C. L., Kochanek I., Korablev D., Korga G., Kubankin A., Kuss M., La Commara M., Lai M., Li X., Lissia M., Longo G., Machulin I. N., Mapelli L. P., Mari S. M., Maricic J., Martoff C. J., Messina A., Meyers P. D., Milincic R., Morrocchi M., Muratova V. N., Musico P., Agasson A. N., Nozdrina A. O., Oleinik A., Ortica F., Pagani L., Pallavicini M., Pandola L., Pantic E., Paoloni E., Pelczar K., Pelliccia N., Picciau E., Pocar A., Pordes S., Poudel S. S., Pralavorio P., Ragusa F., Razeti M., Razeto A., Renshaw A. L., Rescigno M., Rode J., Romani A., Sablone D., Samoylov O., Sands W., Sanfilippo S., Savarese C., Schlitzer B., Semenov D. A., Shchagin A., Sheshukov A., Skorokhvatov M. D., Smirnov O., Sotnikov A., Stracka S., Suvorov Y., Tartaglia R., Testera G., Tonazzo A., Unzhakov E. V., Vishneva A., Vogelaar R. B., Wada M., Wang H., Wang Y., Westerdale S., Wojcik M. M., Xiao X., Yang C., and Zuzel G.

Published
2022

9. The folate way to T cell fate

Author

Paola De Candia, Giuseppe Matarese, de Candia, P., and Matarese, G.

Subjects
Infectious Diseases, Immunology, Immunology and Allergy
Abstract

The role of folate-dependent one carbon (1C) metabolism in CD4+ T cell polarization is incompletely understood. In this issue of Immunity, Sugiura et al. (2021) provide evidence that blocking the 1C metabolic enzyme MTHFD2 may curb pro-inflammatory CD4+ T cells, while redirecting them toward a regulatory T cell phenotype.

Published
2022
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10. Protective effect of oral anticoagulant drugs in atrial fibrillation patients admitted for COVID-19: Results from the CORIST study

Author

Erica De Candia, Walter Ageno, Licia Iacoviello, and Augusto Di Castelnuovo

Subjects
Male, 2019-20 coronavirus outbreak, medicine.medical_specialty, Coronavirus disease 2019 (COVID-19), Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), Letter to the Editors-in-Chief, Administration, Oral, Risk Factors, Cause of Death, Thromboembolism, Internal medicine, Atrial Fibrillation, medicine, Humans, Anticoagulants, Propensity Score, SARS-CoV-2, COVID-19, Stroke, Aged, Retrospective Studies, Aged, 80 and over, business.industry, Settore MED/09 - MEDICINA INTERNA, Atrial fibrillation, Hematology, medicine.disease, Survival Rate, Italy, Population Surveillance, Propensity score matching, Oral anticoagulant, Female, business
Abstract

Coronavirus disease 2019 (COVID-19) global pandemic has strikingly high mortality rate with hypercoagulability state being part of the imputed mechanisms. We aimed to compare the rates of in hospital mortality in propensity score matched cohorts of COVID-19 patients in chronic anticoagulation versus those that were not.In this population-based study in the Veneto Region, we retrospectively reviewed all patients aged 65 years or older, with a laboratory-confirmed COVID-19 diagnosis. We compared, after propensity score matching, those who received chronic anticoagulation for atrial fibrillation with those who did not.Overall, 4697 COVID-19 patients fulfilled inclusion criteria, and the propensity score matching yielded 559 patients per arm. All-cause mortality rate ratio was significantly higher among non-anticoagulated patients (32.2% vs 26.5%, p = 0.036). On time to event analysis, all-cause mortality was found lower among anticoagulated patients, although the estimate was not statistically significant. (HR 0.81, 95%CI 0.65-1.01, p = 0.054).Among elderly patients with COVID-19, those on chronic oral anticoagulant treatment for atrial fibrillation seem to be at lower risk of all-cause mortality compared to their propensity score matched non-anticoagulated counterpart. This finding needs to be confirmed in further studies.

Published
2021
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13. A study of events with photoelectric emission in the DarkSide-50 liquid argon Time Projection Chamber

Author

Agnes, P., primary, Albuquerque, I.F.M., additional, Alexander, T., additional, Alton, A.K., additional, Ave, M., additional, Back, H.O., additional, Batignani, G., additional, Biery, K., additional, Bocci, V., additional, Bonivento, W.M., additional, Bottino, B., additional, Bussino, S., additional, Cadeddu, M., additional, Cadoni, M., additional, Calaprice, F., additional, Caminata, A., additional, Canci, N., additional, Caravati, M., additional, Cargioli, N., additional, Cariello, M., additional, Carlini, M., additional, Carpinelli, M., additional, Catalanotti, S., additional, Cataudella, V., additional, Cavalcante, P., additional, Cavuoti, S., additional, Chepurnov, A., additional, Cicalò, C., additional, Cocco, A.G., additional, Covone, G., additional, D’Angelo, D., additional, Davini, S., additional, De Candia, A., additional, De Cecco, S., additional, De Filippis, G., additional, De Rosa, G., additional, Derbin, A.V., additional, Devoto, A., additional, D’Incecco, M., additional, Dionisi, C., additional, Dordei, F., additional, Downing, M., additional, D’Urso, D., additional, Fiorillo, G., additional, Franco, D., additional, Gabriele, F., additional, Galbiati, C., additional, Ghiano, C., additional, Giganti, C., additional, Giovanetti, G.K., additional, Gorchakov, O., additional, Goretti, A.M., additional, Grobov, A., additional, Gromov, M., additional, Guan, M., additional, Guardincerri, Y., additional, Gulino, M., additional, Hackett, B.R., additional, Herner, K., additional, Hosseini, B., additional, Hubaut, F., additional, Hungerford, E.V., additional, Ianni, An., additional, Ippolito, V., additional, Keeter, K., additional, Kendziora, C.L., additional, Kochanek, I., additional, Korablev, D., additional, Korga, G., additional, Kubankin, A., additional, Kuss, M., additional, La Commara, M., additional, Lai, M., additional, Li, X., additional, Lissia, M., additional, Longo, G., additional, Machulin, I.N., additional, Mapelli, L.P., additional, Mari, S.M., additional, Maricic, J., additional, Martoff, C.J., additional, Messina, A., additional, Meyers, P.D., additional, Milincic, R., additional, Morrocchi, M., additional, Muratova, V.N., additional, Musico, P., additional, Agasson, A. Navrer, additional, Nozdrina, A.O., additional, Oleinik, A., additional, Ortica, F., additional, Pagani, L., additional, Pallavicini, M., additional, Pandola, L., additional, Pantic, E., additional, Paoloni, E., additional, Pelczar, K., additional, Pelliccia, N., additional, Picciau, E., additional, Pocar, A., additional, Pordes, S., additional, Poudel, S.S., additional, Pralavorio, P., additional, Ragusa, F., additional, Razeti, M., additional, Razeto, A., additional, Renshaw, A.L., additional, Rescigno, M., additional, Rode, J., additional, Romani, A., additional, Sablone, D., additional, Samoylov, O., additional, Sands, W., additional, Sanfilippo, S., additional, Savarese, C., additional, Schlitzer, B., additional, Semenov, D.A., additional, Shchagin, A., additional, Sheshukov, A., additional, Skorokhvatov, M.D., additional, Smirnov, O., additional, Sotnikov, A., additional, Stracka, S., additional, Suvorov, Y., additional, Tartaglia, R., additional, Testera, G., additional, Tonazzo, A., additional, Unzhakov, E.V., additional, Vishneva, A., additional, Vogelaar, R.B., additional, Wada, M., additional, Wang, H., additional, Wang, Y., additional, Westerdale, S., additional, Wojcik, Ma.M., additional, Xiao, X., additional, Yang, C., additional, and Zuzel, G., additional

Published
2022
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14. PO-1845 Surface guided adjuvant radiotherapy tattoo-free for breast cancer

Author

Cuscito, R., primary, Fragnoli, F., additional, Indelicati, C., additional, Sanfrancesco, G., additional, De Pascali, C., additional, De Masi, M., additional, Parabita, R., additional, Aga, A., additional, Berloco, F., additional, Brana', L., additional, Ciocia, A., additional, Curci, D., additional, Ladisa, G., additional, Nardiello, M., additional, Nardelli, D., additional, De Candia, V., additional, Gregucci, F., additional, Surgo, A., additional, Carbonara, R., additional, Cliliberti, M.P., additional, Caliandro, M., additional, Bonaparte, I., additional, and Fiorentino, A., additional

Published
2022
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15. T Cells: Warriors of SARS-CoV-2 Infection

Author

Giuseppe Matarese, Silvia Garavelli, Paola de Candia, Francesco Prattichizzo, de Candia, P., Prattichizzo, F., Garavelli, S., and Matarese, G.

Subjects
Opinion, T-Lymphocytes, viruses, T cell, Immunology, Adaptive Immunity, Immune system, T-Lymphocyte Subsets, Immunity, Immunopathology, Humans, Medicine, Immunology and Allergy, Innate immune system, SARS-CoV-2, business.industry, Models, Immunological, COVID-19, Immunosenescence, biochemical phenomena, metabolism, and nutrition, Acquired immune system, medicine.disease, Immunity, Innate, medicine.anatomical_structure, Cytokines, business, Cytokine storm, Immunologic Memory
Abstract

Severe infection with severe acute respiratory syndrome coronavirus (SARS-CoV)-2 is characterized by massive cytokine release and T cell loss. The exaggerated host immune response, incapable of viral clearance, instead aggravates respiratory distress, as well as cardiac, and/or damage to other organs. The mortality pattern of SARS-CoV-2 infection, higher in older versus younger adults and almost absent in children, is possibly caused by the effects of age and pre-existing comorbidities on innate and adaptive immunity. Here, we speculate that the abnormal and excessive immune response to SARS-CoV-2 infection partly depends on T cell immunological memory, which is more pronounced in adults compared with children, and may significantly contribute to immunopathology and massive collateral damage in coronavirus disease 2019 (COVID-19) patients., Highlights T cell-mediated immunity is crucial for the effective clearance of severe acute respiratory syndrome coronavirus (SARS-CoV)-2 infection. In severe and critical coronavirus disease 2019 (COVID-19) patients, peripheral blood T cells are significantly decreased and show a phenotype of hyperactivation/exhaustion relative to controls. Older age, characterized by high basal proinflammatory status coupled with a progressive inability to mount proper immune responses, is a major risk factor for severe and critical SARS-CoV-2 infection. Children are nearly always asymptomatic in SARS-CoV2 infection; this clinical observation may be linked to a higher proportion of naïve T cells in circulation than adults and, consequently, a presumed reduced susceptibility to hyperinflammatory collateral damage.

Published
2021
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17. ImpaCt of an Optimal Implantation Strategy on Absorb Long-Term Outcomes: The CIAO Registry

Author

Rapetto, Claudio, primary, Leoncini, Massimo, additional, Cerrato, Enrico, additional, Regazzoli, Damiano, additional, Cortese, Bernardo, additional, Rossi, Angelica, additional, Fetiveau, Raffaela, additional, Geraci, Salvatore, additional, De Angelis, Maria Carmen, additional, Tespili, Maurizio, additional, Iannaccone, Mario, additional, Centola, Antonio, additional, Durante, Alessandro, additional, De Carlo, Marco, additional, De Caterina, Alberto, additional, Ribichini, Flavio, additional, Favaretto, Enrico, additional, Testa, Luca, additional, Pirisi, Raimondo, additional, Varbella, Ferdinando, additional, Nicolini, Elisa, additional, di Palma, Gaetano, additional, Loi, Bruno, additional, Poli, Arnaldo, additional, Caramanno, Giuseppe, additional, Varricchio, Attilio, additional, Garbo, Roberto, additional, Cuculo, Andrea, additional, Petronio, Anna Sonia, additional, Berti, Sergio, additional, Bollati, Mario, additional, Spedicato, Leonardo, additional, De Candia, Gianfranco, additional, Piva, Tommaso, additional, Quadri, Giorgio, additional, Colombo, Antonio, additional, and Ielasi, Alfonso, additional

Published
2021
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18. Extracellular RNAs: A Secret Arm of Immune System Regulation

Author

Veronica De Rosa, Giuseppe Matarese, Paola de Candia, Maurizio Casiraghi, de Candia, Paola, DE ROSA, Veronica, Casiraghi, Maurizio, Matarese, Giuseppe, De Candia, P, De Rosa, V, Casiraghi, M, and Matarese, G

Subjects
0301 basic medicine, Cell signaling, Cell type, Cell-free RNA, Cell Communication, lymphocyte, Adaptive Immunity, Biology, Biochemistry, 03 medical and health sciences, Immune system, microRNA, Animals, Humans, cellular immune response, Molecular Biology, Cell-free RNAs, RNA, T cells, Treg cells, extracellular vesicles, immune system, nucleic acid, Genetics, Animal, T cell, MicroRNA, Minireviews, Cell Biology, Acquired immune system, BIO/10 - BIOCHIMICA, Treg cell, Cell biology, MicroRNAs, Multicellular organism, 030104 developmental biology, extracellular vesicle, Human, Extracellular RNA
Abstract

The immune system has evolved to protect multicellular organisms from the attack of a variety of pathogens. To exert this function efficiently, the system has developed the capacity to coordinate the function of different cell types and the ability to down-modulate the response when the foreign attack is over. For decades, immunologists believed that these two characteristics were primarily related to cytokine/chemokine-based communication and cell-to-cell direct contact. More recently, it has been shown that immune cells also communicate by transferring regulatory RNAs, microRNAs in particular, from one cell to the other. Several studies have suggested a functional role of extracellular regulatory RNAs in cell-to-cell communication in different cellular contexts. This minireview focuses on the potential role of extracellular RNA transfer in the regulation of adaptive immune response, also contextualizing it in a broader field of what is known of cell-free RNAs in communication among different organisms in the evolutionary scale.

Published
2016
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22. Signals of pseudo-starvation unveil the amino acid transporter SLC7A11 as key determinant in the control of Treg cell proliferative potential

Author

Procaccini, Claudio, primary, Garavelli, Silvia, additional, Carbone, Fortunata, additional, Di Silvestre, Dario, additional, La Rocca, Claudia, additional, Greco, Dario, additional, Colamatteo, Alessandra, additional, Lepore, Maria Teresa, additional, Russo, Claudia, additional, De Rosa, Giusy, additional, Faicchia, Deriggio, additional, Prattichizzo, Francesco, additional, Grossi, Sarah, additional, Campomenosi, Paola, additional, Buttari, Fabio, additional, Mauri, Pierluigi, additional, Uccelli, Antonio, additional, Salvetti, Marco, additional, Brescia Morra, Vincenzo, additional, Vella, Danila, additional, Galgani, Mario, additional, Mottola, Maria, additional, Zuccarelli, Bruno, additional, Lanzillo, Roberta, additional, Maniscalco, Giorgia Teresa, additional, Centonze, Diego, additional, de Candia, Paola, additional, and Matarese, Giuseppe, additional

Published
2021
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23. Modulatory effect of simultaneously released magnesium, strontium, and silicon ions on injectable silk hydrogels for bone regeneration

Author

Hala Zreiqat, Jeffrey Shi, David L. Kaplan, Xinquan Jiang, Young Jung No, Wang Jie, Iman Roohani-Esfahani, Christian de Candia, Xinchao Miao, and Zufu Lu

Subjects
Male, Silicon, Bone Regeneration, Materials science, Compressive Strength, Biocompatibility, Sonication, Silk, chemistry.chemical_element, Fibroin, Bioengineering, macromolecular substances, 02 engineering and technology, 010402 general chemistry, 01 natural sciences, Injections, Biomaterials, Elastic Modulus, Animals, Humans, Magnesium, Bone regeneration, Cell Proliferation, Inflammation, Ions, Osteoblasts, fungi, technology, industry, and agriculture, Hydrogels, Hydrogen-Ion Concentration, Alkaline Phosphatase, Bombyx, 021001 nanoscience & nanotechnology, 0104 chemical sciences, Mice, Inbred C57BL, Platelet Endothelial Cell Adhesion Molecule-1, SILK, Chemical engineering, chemistry, Strontium, Mechanics of Materials, Self-healing hydrogels, Alkaline phosphatase, Collagen, 0210 nano-technology
Abstract

Injectable silk hydrogels are ideal carriers of therapeutic agents due to their biocompatibility and low immunogenicity. Injectable silk hydrogels for bone regeneration have been previously developed but often utilize expensive biologics. In this study, we have developed an injectable silk composite incorporated with a triphasic ceramic called MSM-10 (54 Mg2SiO4, 36 Si3Sr5 and 10 MgO (wt%)) capable of simultaneously releasing magnesium, silicon, and strontium ions into its environment. These ions have been previously reported to possess therapeutic effects for bone regeneration. MSM-10 particles were incorporated into the silk hydrogels at various weight percentages [0.1 (SMH-0.1), 0.6 (SMH-0.6), 1 (SMH-1) and 2 (SMH-2)]. The effects of the released ions on the physicochemical and biological properties of the silk hydrogel were comprehensively evaluated. Increased MSM-10 loading was found to hinder the gelation kinetics of the silk hydrogel through the reduction of beta-sheet phase formation, which in turn affected the required sonication time for gelation, compressive strength, force of injection, microstructure and in vitro degradation rate. Primary human osteoblasts seeded on SMH-0.6 demonstrated increased proliferation and early alkaline phosphatase activity, as well as enhanced osteogenic gene expression compared to pure silk hydrogel and SMH-0.1. In vivo results in subcutaneous mouse models showed both decreased fibrous capsule formation and increased number of new blood vessels around the injected SMH-0.1 and SMH-0.6 implants compared to pure silk hydrogels. The results in this study indicate that the ions released from MSM-10 is able to influence the physicochemical and biological properties of silk hydrogels, and SMH-0.6 in particular shows promising properties for bone regeneration.

Published
2019
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24. PO-1845 Surface guided adjuvant radiotherapy tattoo-free for breast cancer

Author

R. Cuscito, F. Fragnoli, C. Indelicati, G. Sanfrancesco, C. De Pascali, M. De Masi, R. Parabita, A. Aga, F. Berloco, L. Brana', A. Ciocia, D. Curci, G. Ladisa, M. Nardiello, D. Nardelli, V. De Candia, F. Gregucci, A. Surgo, R. Carbonara, M.P. Cliliberti, M. Caliandro, I. Bonaparte, and A. Fiorentino

Subjects
Oncology, Radiology, Nuclear Medicine and imaging, Hematology
Published
2022
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25. Diabetes and kidney disease: emphasis on treatment with SGLT-2 inhibitors and GLP-1 receptor agonists

Author

Antonio Ceriello, Francesco Prattichizzo, Paola de Candia, Prattichizzo, F., de Candia, P., and Ceriello, A.

Subjects
Blood Glucose, 0301 basic medicine, Endocrinology, Diabetes and Metabolism, Blood Pressure, Type 2 diabetes, Pharmacology, Kidney, medicine.disease_cause, Cardiovascular System, SGLT-2, Diabetic nephropathy, 0302 clinical medicine, Endocrinology, Risk Factors, Diabetic Nephropathies, Sodium-Glucose Transporter 2 Inhibitor, Epigenetic, Diabetes treatment algorithm, Human, Diabetes mellitu, medicine.medical_specialty, 030209 endocrinology & metabolism, Low-grade inflammation, Diabetes complication, Glucagon-Like Peptide-1 Receptor, Nephropathy, 03 medical and health sciences, Internal medicine, Diabetes mellitus, Glucose control, Diabetes Mellitus, medicine, Animals, Humans, Hypoglycemic Agents, Sodium-Glucose Transporter 2 Inhibitors, Glucagon-like peptide 1 receptor, miRNA, Hypoglycemic Agent, Animal, business.industry, Risk Factor, medicine.disease, 030104 developmental biology, Blood pressure, Oxidative stre, GLP-1, business, Oxidative stress, Kidney disease
Abstract

Kidney disease is a frequent microvascular complication of both type 1 and type 2 diabetes. Historic trials have demonstrated that a tight glycaemic control is the most powerful approach to decrease the chances of developing diabetic nephropathy. However, having an HbA1c < 7% does not completely suppress the risk of kidney disease. The observed residual risk is likely ascribable to two phenomena: 1- the presence of risk factors and alterations additive to and independent of glycaemia, and 2- the activation of long-lasting imbalances by periods of exposure to uncontrolled glycemia, a phenomenon referred to as metabolic memory or legacy effect. Long-lasting oxidative stress, epigenetic alterations, cellular senescence, and the resulting chronic low-grade inflammation are all candidate mechanisms explaining the development of nephropathy despite proper control of risk factors. Recently, two classes of drugs, i.e. glucagon-like peptide (GLP) 1 receptor agonists (RA) and sodium-glucose transporter 2 inhibitors (SGLT-i) have changed this scenario. Indeed, cardiovascular outcome and other trials have clearly shown a renoprotective effect for these drugs, well-beyond their glucose-lowering properties. In this review, we summarize: 1- selected key trials and mechanisms underlying the development of diabetic kidney disease and 2- the results relative to renal endpoints in clinical trials of GLP-1 RA and SGLT-2i. Then, we briefly discuss some of the hypotheses posited to explain the marked renoprotective properties of these two classes, evidencing the still existing gaps in knowledge and proposing future directions to further implement the use of these powerful, disease-modifying drugs.

Published
2021
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26. Targeting a Mirabegron precursor by BH3-mediated continuous flow reduction process

Author

Leonardo Degennaro, Paolo Celestini, Gabriele Rebuzzini, Sonia De Angelis, Claudia Carlucci, Modesto de Candia, Renzo Luisi, and Massimiliano Riscazzi

Subjects
010405 organic chemistry, Continuous flow, General Chemistry, Flow chemistry, 010402 general chemistry, 01 natural sciences, Catalysis, 0104 chemical sciences, Reduction (complexity), chemistry.chemical_compound, chemistry, Scientific method, Diamine, medicine, Organic chemistry, Mirabegron, medicine.drug
Abstract

A continuous-flow reduction of (R)-2-hydroxy-N-[2-(4-nitrophenyl)ethyl]-2-phenylacetamide, involved in the synthetic pathway of Mirabegron, has been developed. This study demonstrated the possibility to safely handling BH3 complexes within microfluidic reactors using 2-MeTHF as greener alternative to traditional solvents, and without requiring any additive such as DMI. In addition, NMR and HPLC purity analysis revealed that the sole by-product of this process is the diamine 3, which wouldn’t affect the following synthetic steps towards Mirabegron.

Published
2018
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27. Nonalcoholic fatty liver disease (NAFLD) severity is associated to a nonhemostatic contribution and proinflammatory phenotype of platelets

Author

Miele, Luca, primary, Alberelli, Maria Adele, additional, Martini, Maurizio, additional, Liguori, Antonio, additional, Marrone, Giuseppe, additional, Cocomazzi, Alessandra, additional, Vecchio, Fabio Maria, additional, Landolfi, Raffaele, additional, Gasbarrini, Antonio, additional, Grieco, Antonio, additional, and De Candia, Erica, additional

Published
2021
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28. The ISTH bleeding assessment tool as predictor of bleeding events in inherited platelet disorders: Communication from the ISTH SSC Subcommittee on Platelet Physiology

Author

Gresele, Paolo, primary, Falcinelli, Emanuela, additional, Bury, Loredana, additional, Pecci, Alessandro, additional, Alessi, Marie‐Christine, additional, Borhany, Munira, additional, Heller, Paula G., additional, Santoro, Cristina, additional, Cid, Ana Rosa, additional, Orsini, Sara, additional, Fontana, Pierre, additional, De Candia, Erica, additional, Podda, Gianmarco, additional, Kannan, Meganathan, additional, Jurk, Kerstin, additional, Castaman, Giancarlo, additional, Falaise, Céline, additional, Guglielmini, Giuseppe, additional, Noris, Patrizia, additional, Zaninetti, Carlo, additional, Fiore, Mathieu, additional, Tosetto, Alberto, additional, Zuniga, Pamela, additional, Miyazaki, Koji, additional, Dupuis, Arnaud, additional, Hayward, Catherine, additional, Casonato, Alessandra, additional, Grandone, Elvira, additional, Mazzucconi, Maria Gabriella, additional, James, Paula, additional, Fabris, Fabrizio, additional, Henskens, Yvonne, additional, Napolitano, Mariasanta, additional, Curnow, Jennifer, additional, Gkalea, Vasiliki, additional, Fedor, Marian, additional, Lambert, Michele P., additional, Zieger, Barbara, additional, Barcella, Luca, additional, Cosmi, Benilde, additional, Giordano, Paola, additional, Porri, Claudia, additional, Melazzini, Federica, additional, Abid, Madiha, additional, Glembotsky, Ana C., additional, Ferrara, Grazia, additional, Russo, Alexandra, additional, Deckmyn, Hans, additional, Frelinger, Andrew L., additional, Harrison, Paul, additional, Mezzano, Diego, additional, Mumford, Andrew D, additional, and Lordkipanidzé, Marie, additional

Published
2021
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30. Tackling the pillars of ageing to fight COVID-19

Author

Antonio Ceriello, Jacopo Sabbatinelli, Fabiola Olivieri, Paola de Candia, Francesco Prattichizzo, Prattichizzo, F., Sabbatinelli, J., de Candia, P., Olivieri, F., and Ceriello, A.

Subjects
Male, 2019-20 coronavirus outbreak, Health (social science), Coronavirus disease 2019 (COVID-19), business.industry, Severe acute respiratory syndrome coronavirus 2 (SARS-CoV-2), lcsh:R, lcsh:Medicine, COVID-19, lcsh:Geriatrics, Virology, Metformin, Cohort Studies, lcsh:RC952-954.6, Psychiatry and Mental health, Diabetes Mellitus, Type 2, Correspondence, Humans, Medicine, Female, Obesity, Geriatrics and Gerontology, Family Practice, business, Retrospective Studies
Abstract

Type 2 diabetes and obesity, as states of chronic inflammation, are risk factors for severe COVID-19. Metformin has cytokine-reducing and sex-specific immunomodulatory effects. Our aim was to identify whether metformin reduced COVID-19-related mortality and whether sex-specific interactions exist.In this retrospective cohort analysis, we assessed de-identified claims data from UnitedHealth Group (UHG)'s Clinical Discovery Claims Database. Patient data were eligible for inclusion if they were aged 18 years or older; had type 2 diabetes or obesity (defined based on claims); at least 6 months of continuous enrolment in 2019; and admission to hospital for COVID-19 confirmed by PCR, manual chart review by UHG, or reported from the hospital to UHG. The primary outcome was in-hospital mortality from COVID-19. The independent variable of interest was home metformin use, defined as more than 90 days of claims during the year before admission to hospital. Covariates were comorbidities, medications, demographics, and state. Heterogeneity of effect was assessed by sex. For the Cox proportional hazards, censoring was done on the basis of claims made after admission to hospital up to June 7, 2020, with a best outcome approach. Propensity-matched mixed-effects logistic regression was done, stratified by metformin use.6256 of the 15 380 individuals with pharmacy claims data from Jan 1 to June 7, 2020 were eligible for inclusion. 3302 (52·8%) of 6256 were women. Metformin use was not associated with significantly decreased mortality in the overall sample of men and women by either Cox proportional hazards stratified model (hazard ratio [HR] 0·887 [95% CI 0·782-1·008]) or propensity matching (odds ratio [OR] 0·912 [95% CI 0·777-1·071], p=0·15). Metformin was associated with decreased mortality in women by Cox proportional hazards (HR 0·785, 95% CI 0·650-0·951) and propensity matching (OR 0·759, 95% CI 0·601-0·960, p=0·021). There was no significant reduction in mortality among men (HR 0·957, 95% CI 0·82-1·14; p=0·689 by Cox proportional hazards).Metformin was significantly associated with reduced mortality in women with obesity or type 2 diabetes who were admitted to hospital for COVID-19. Prospective studies are needed to understand mechanism and causality. If findings are reproducible, metformin could be widely distributed for prevention of COVID-19 mortality, because it is safe and inexpensive.National Heart, Lung, and Blood Institute; Agency for Healthcare Research and Quality; Patient-Centered Outcomes Research Institute; Minnesota Learning Health System Mentored Training Program, M Health Fairview Institutional Funds; National Center for Advancing Translational Sciences; and National Cancer Institute.

Published
2021
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31. Role of metabolism in neurodegenerative disorders

Author

Giuseppe Matarese, Mario Galgani, Luigi Formisano, Paola de Candia, Alessandra Colamatteo, Claudio Procaccini, Marianna Santopaolo, Deriggio Faicchia, Veronica De Rosa, Procaccini, C, Santopaolo, M, Faicchia, D, Colamatteo, A, Formisano, L, De Candia, P, Galgani M., De Rosa, V, and Matarese, G.

Subjects
0301 basic medicine, medicine.medical_specialty, Huntingtin, Parkinson's disease, Endocrinology, Diabetes and Metabolism, Context (language use), Biology, Multiple sclerosis, 03 medical and health sciences, Endocrinology, Internal medicine, medicine, Humans, Brain-derived neurotrophic factor, Leptin, Huntington's diseases, Neurodegeneration, Neurodegenerative Diseases, Huntington's disease, Receptor Cross-Talk, Alzheimer's disease, medicine.disease, Hormones, Metabolism, 030104 developmental biology, Ghrelin, Energy Metabolism
Abstract

Along with the increase in life expectancy over the last century, the prevalence of age-related disorders, such as neurodegenerative diseases continues to rise. This is the case of Alzheimer's, Parkinson's, Huntington's diseases and Multiple sclerosis, which are chronic disorders characterized by neuronal loss in motor, sensory or cognitive systems. Accumulating evidence has suggested the presence of a strong correlation between metabolic changes and neurodegeneration. Indeed epidemiologic studies have shown strong associations between obesity, metabolic dysfunction, and neurodegeneration, while animal models have provided insights into the complex relationships between these conditions. In this context, hormones such as leptin, ghrelin, insulin and IGF-1 seem to play a key role in the regulation of neuronal damage, toxic insults and several other neurodegenerative processes. This review aims to presenting the most recent evidence supporting the crosstalk linking energy metabolism and neurodegeneration, and will focus on metabolic manipulation as a possible therapeutic tool in the prevention and treatment of neurodegenerative diseases.

Published
2016
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34. Caloric Restriction Promotes Immunometabolic Reprogramming Leading to Protection from Tuberculosis

Author

Palma, Carla, primary, La Rocca, Claudia, additional, Gigantino, Vincenzo, additional, Aquino, Gabriella, additional, Piccaro, Giovanni, additional, Di Silvestre, Dario, additional, Brambilla, Francesca, additional, Rossi, Rossana, additional, Bonacina, Fabrizia, additional, Lepore, Maria Teresa, additional, Audano, Matteo, additional, Mitro, Nico, additional, Botti, Gerardo, additional, Bruzzaniti, Sara, additional, Fusco, Clorinda, additional, Procaccini, Claudio, additional, De Rosa, Veronica, additional, Galgani, Mario, additional, Alviggi, Carlo, additional, Puca, Annibale, additional, Grassi, Fabio, additional, Rezzonico-Jost, Tanja, additional, Norata, Giuseppe Danilo, additional, Mauri, Pierluigi, additional, Netea, Mihai G., additional, de Candia, Paola, additional, and Matarese, Giuseppe, additional

Published
2021
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38. Validation of the ISTH/SSC bleeding assessment tool for inherited platelet disorders: A communication from the Platelet Physiology SSC

Author

Gresele, Paolo, primary, Orsini, Sara, additional, Noris, Patrizia, additional, Falcinelli, Emanuela, additional, Alessi, Marie Christine, additional, Bury, Loredana, additional, Borhany, Munira, additional, Santoro, Cristina, additional, Glembotsky, Ana C., additional, Cid, Ana Rosa, additional, Tosetto, Alberto, additional, De Candia, Erica, additional, Fontana, Pierre, additional, Guglielmini, Giuseppe, additional, Pecci, Alessandro, additional, Heller, Paula G., additional, Rodorigo, Giuseppina, additional, Lammle, Bernhard, additional, Trinchero, Alice, additional, Paolo, Radossi, additional, Ferrari, Silvia, additional, Rancitelli, Davide, additional, Stolinski, Amy, additional, Arulselvan, Abinaya, additional, Lassandro, Giuseppe, additional, Luceros, Analia Sanchez, additional, Jandrot‐Perrus, Martine, additional, Kunishima, Shinji, additional, Rivera Pozo, José, additional, Lordkipanidzé, Marie, additional, Melazzini, Federica, additional, Falaise, Céline, additional, Casonato, Alessandra, additional, Podda, Gianmarco, additional, Kannan, Meganathan, additional, Jurk, Kerstin, additional, Sevivas, Teresa, additional, Castaman, Giancarlo, additional, Grandone, Elvira, additional, Fiore, Mathieu, additional, Zuniga, Pamela, additional, Henskens, Yvonne, additional, Miyazaki, Koji, additional, Dupuis, Arnaud, additional, Hayward, Catherine, additional, Zaninetti, Carlo, additional, Abid, Madiha, additional, Ferrara, Grazia, additional, Mazzucconi, Maria Gabriella, additional, Tagariello, Giuseppe, additional, James, Paula, additional, Fabris, Fabrizio, additional, Russo, Alexandra, additional, Bermejo, Nuria, additional, Napolitano, Mariasanta, additional, Curnow, Jennifer, additional, Vasiliki, Gkalea, additional, Zieger, Barbara, additional, Fedor, Marian, additional, Chitlur, Meera, additional, Lambert, Michele, additional, Barcella, Luca, additional, Cosmi, Benilde, additional, Giordano, Paola, additional, Porri, Claudia, additional, Eker, Ibrahim, additional, Morel‐Kopp, Marie‐Christine, additional, Deckmyn, Hans, additional, Frelinger, Andrew L., additional, Harrison, Paul, additional, Mezzano, Diego, additional, and Mumford, Andrew D., additional

Published
2020
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39. Electroluminescence pulse shape and electron diffusion in liquid argon measured in a dual-phase TPC

Author

Agnes, P, Albuquerque, I, Alexander, T, Alton, A, Asner, D, Ave, M, Back, H, Baldin, B, Batignani, G, Biery, K, Bocci, V, Bonfini, G, Bonivento, W, Bossa, M, Bottino, B, Budano, F, Bussino, S, Cadeddu, M, Cadoni, M, Calaprice, F, Caminata, A, Canci, N, Candela, A, Caravati, M, Cariello, M, Carlini, M, Carpinelli, M, Catalanotti, S, Cataudella, V, Cavalcante, P, Cavuoti, S, Chepurnov, A, Cicalò, C, Cocco, A, Covone, G, D'Angelo, D, D'Incecco, M, D'Urso, D, Davini, S, De Candia, A, De Cecco, S, De Deo, M, De Filippis, G, De Rosa, G, De Vincenzi, M, Demontis, P, Derbin, A, Devoto, A, Di Eusanio, F, Di Pietro, G, Dionisi, C, Edkins, E, Fan, A, Fiorillo, G, Fomenko, K, Franco, D, Gabriele, F, Gabrieli, A, Galbiati, C, Ghiano, C, Giagu, S, Giganti, C, Giovanetti, G, Goretti, A, Granato, F, Gromov, M, Guan, M, Guardincerri, Y, Gulino, M, Hackett, B, Herner, K, Hughes, D, Humble, P, Hungerford, E, Ianni, A, James, I, Johnson, T, Keeter, K, Kendziora, C, Kochanek, I, Koh, G, Korablev, D, Korga, G, Kubankin, A, Kuss, M, Li, X, Lissia, M, Loer, B, Longo, G, Ma, Y, Machado, A, Machulin, I, Mandarano, A, Mari, S, Maricic, J, Martoff, C, Messina, A, Meyers, P, Milincic, R, Monte, A, Morrocchi, M, Mount, B, Muratova, V, Musico, P, Navrer Agasson, A, Nozdrina, A, Oleinik, A, Orsini, M, Ortica, F, Pagani, L, Pallavicini, M, Pandola, L, Pantic, E, Paoloni, E, Pazzona, F, Pelczar, K, Pelliccia, N, Pocar, A, Pordes, S, Qian, H, Razeti, M, Razeto, A, Reinhold, B, Renshaw, A, Rescigno, M, Riffard, Q, Romani, A, Rossi, B, Rossi, N, Sablone, D, Samoylov, O, Sands, W, Sanfilippo, S, Sant, M, Savarese, C, Schlitzer, B, Segreto, E, Semenov, D, Sheshukov, A, Singh, P, Skorokhvatov, M, Smirnov, O, Sotnikov, A, Stanford, C, Suffritti, G, Suvorov, Y, Tartaglia, R, Testera, G, Tonazzo, A, Trinchese, P, Unzhakov, E, Verducci, M, Vishneva, A, Vogelaar, B, Wada, M, Waldrop, T, Walker, S, Wang, H, Wang, Y, Watson, A, Westerdale, S, Wojcik, M, Xiang, X, Xiao, X, Yang, C, Ye, Z, Zhu, C, Zuzel, G, Agnes, P., Albuquerque, I. F. M., Alexander, T., Alton, A. K., Asner, D. M., Ave, M. P., Back, H. O., Baldin, B., Batignani, G., Biery, K., Bocci, V., Bonfini, G., Bonivento, W., Bossa, M., Bottino, B., Budano, F., Bussino, S., Cadeddu, M., Cadoni, M., Calaprice, F., Caminata, A., Canci, N., Candela, A., Caravati, M., Cariello, M., Carlini, M., Carpinelli, M., Catalanotti, S., Cataudella, V., Cavalcante, P., Cavuoti, S., Chepurnov, A., Cicalò, C., Cocco, A. G., Covone, G., D'Angelo, D., D'Incecco, M., D'Urso, D., Davini, S., De Candia, A., De Cecco, S., De Deo, M., De Filippis, G., De Rosa, G., De Vincenzi, M., Demontis, P., Derbin, A. V., Devoto, A., Di Eusanio, F., Di Pietro, G., Dionisi, C., Edkins, E., Fan, A., Fiorillo, G., Fomenko, K., Franco, D., Gabriele, F., Gabrieli, A., Galbiati, C., Ghiano, C., Giagu, S., Giganti, C., Giovanetti, G. K., Goretti, A. M., Granato, F., Gromov, M., Guan, M., Guardincerri, Y., Gulino, M., Hackett, B. R., Herner, K., Hughes, D., Humble, P., Hungerford, E. V., Ianni, An., James, I., Johnson, T. N., Keeter, K., Kendziora, C. L., Kochanek, I., Koh, G., Korablev, D., Korga, G., Kubankin, A., Kuss, M., Li, X., Lissia, M., Loer, B., Longo, G., Ma, Y., Machado, A. A., Machulin, I. N., Mandarano, A., Mari, S. M., Maricic, J., Martoff, C. J., Messina, A., Meyers, P. D., Milincic, R., Monte, A., Morrocchi, M., Mount, B. J., Muratova, V. N., Musico, P., Navrer Agasson, A., Nozdrina, A., Oleinik, A., Orsini, M., Ortica, F., Pagani, L., Pallavicini, M., Pandola, L., Pantic, E., Paoloni, E., Pazzona, F., Pelczar, K., Pelliccia, N., Pocar, A., Pordes, S., Qian, H., Razeti, M., Razeto, A., Reinhold, B., Renshaw, A. L., Rescigno, M., Riffard, Q., Romani, A., Rossi, B., Rossi, N., Sablone, D., Samoylov, O., Sands, W., Sanfilippo, S., Sant, M., Savarese, C., Schlitzer, B., Segreto, E., Semenov, D. A., Sheshukov, A., Singh, P. N., Skorokhvatov, M. D., Smirnov, O., Sotnikov, A., Stanford, C., Suffritti, G. B., Suvorov, Y., Tartaglia, R., Testera, G., Tonazzo, A., Trinchese, P., Unzhakov, E. V., Verducci, M., Vishneva, A., Vogelaar, B., Wada, M., Waldrop, T. J., Walker, S., Wang, H., Wang, Y., Watson, A. W., Westerdale, S., Wojcik, M. M., Xiang, X., Xiao, X., Yang, C., Ye, Z., Zhu, C., Zuzel, G., Agnes, P, Albuquerque, I, Alexander, T, Alton, A, Asner, D, Ave, M, Back, H, Baldin, B, Batignani, G, Biery, K, Bocci, V, Bonfini, G, Bonivento, W, Bossa, M, Bottino, B, Budano, F, Bussino, S, Cadeddu, M, Cadoni, M, Calaprice, F, Caminata, A, Canci, N, Candela, A, Caravati, M, Cariello, M, Carlini, M, Carpinelli, M, Catalanotti, S, Cataudella, V, Cavalcante, P, Cavuoti, S, Chepurnov, A, Cicalò, C, Cocco, A, Covone, G, D'Angelo, D, D'Incecco, M, D'Urso, D, Davini, S, De Candia, A, De Cecco, S, De Deo, M, De Filippis, G, De Rosa, G, De Vincenzi, M, Demontis, P, Derbin, A, Devoto, A, Di Eusanio, F, Di Pietro, G, Dionisi, C, Edkins, E, Fan, A, Fiorillo, G, Fomenko, K, Franco, D, Gabriele, F, Gabrieli, A, Galbiati, C, Ghiano, C, Giagu, S, Giganti, C, Giovanetti, G, Goretti, A, Granato, F, Gromov, M, Guan, M, Guardincerri, Y, Gulino, M, Hackett, B, Herner, K, Hughes, D, Humble, P, Hungerford, E, Ianni, A, James, I, Johnson, T, Keeter, K, Kendziora, C, Kochanek, I, Koh, G, Korablev, D, Korga, G, Kubankin, A, Kuss, M, Li, X, Lissia, M, Loer, B, Longo, G, Ma, Y, Machado, A, Machulin, I, Mandarano, A, Mari, S, Maricic, J, Martoff, C, Messina, A, Meyers, P, Milincic, R, Monte, A, Morrocchi, M, Mount, B, Muratova, V, Musico, P, Navrer Agasson, A, Nozdrina, A, Oleinik, A, Orsini, M, Ortica, F, Pagani, L, Pallavicini, M, Pandola, L, Pantic, E, Paoloni, E, Pazzona, F, Pelczar, K, Pelliccia, N, Pocar, A, Pordes, S, Qian, H, Razeti, M, Razeto, A, Reinhold, B, Renshaw, A, Rescigno, M, Riffard, Q, Romani, A, Rossi, B, Rossi, N, Sablone, D, Samoylov, O, Sands, W, Sanfilippo, S, Sant, M, Savarese, C, Schlitzer, B, Segreto, E, Semenov, D, Sheshukov, A, Singh, P, Skorokhvatov, M, Smirnov, O, Sotnikov, A, Stanford, C, Suffritti, G, Suvorov, Y, Tartaglia, R, Testera, G, Tonazzo, A, Trinchese, P, Unzhakov, E, Verducci, M, Vishneva, A, Vogelaar, B, Wada, M, Waldrop, T, Walker, S, Wang, H, Wang, Y, Watson, A, Westerdale, S, Wojcik, M, Xiang, X, Xiao, X, Yang, C, Ye, Z, Zhu, C, Zuzel, G, Agnes, P., Albuquerque, I. F. M., Alexander, T., Alton, A. K., Asner, D. M., Ave, M. P., Back, H. O., Baldin, B., Batignani, G., Biery, K., Bocci, V., Bonfini, G., Bonivento, W., Bossa, M., Bottino, B., Budano, F., Bussino, S., Cadeddu, M., Cadoni, M., Calaprice, F., Caminata, A., Canci, N., Candela, A., Caravati, M., Cariello, M., Carlini, M., Carpinelli, M., Catalanotti, S., Cataudella, V., Cavalcante, P., Cavuoti, S., Chepurnov, A., Cicalò, C., Cocco, A. G., Covone, G., D'Angelo, D., D'Incecco, M., D'Urso, D., Davini, S., De Candia, A., De Cecco, S., De Deo, M., De Filippis, G., De Rosa, G., De Vincenzi, M., Demontis, P., Derbin, A. V., Devoto, A., Di Eusanio, F., Di Pietro, G., Dionisi, C., Edkins, E., Fan, A., Fiorillo, G., Fomenko, K., Franco, D., Gabriele, F., Gabrieli, A., Galbiati, C., Ghiano, C., Giagu, S., Giganti, C., Giovanetti, G. K., Goretti, A. M., Granato, F., Gromov, M., Guan, M., Guardincerri, Y., Gulino, M., Hackett, B. R., Herner, K., Hughes, D., Humble, P., Hungerford, E. V., Ianni, An., James, I., Johnson, T. N., Keeter, K., Kendziora, C. L., Kochanek, I., Koh, G., Korablev, D., Korga, G., Kubankin, A., Kuss, M., Li, X., Lissia, M., Loer, B., Longo, G., Ma, Y., Machado, A. A., Machulin, I. N., Mandarano, A., Mari, S. M., Maricic, J., Martoff, C. J., Messina, A., Meyers, P. D., Milincic, R., Monte, A., Morrocchi, M., Mount, B. J., Muratova, V. N., Musico, P., Navrer Agasson, A., Nozdrina, A., Oleinik, A., Orsini, M., Ortica, F., Pagani, L., Pallavicini, M., Pandola, L., Pantic, E., Paoloni, E., Pazzona, F., Pelczar, K., Pelliccia, N., Pocar, A., Pordes, S., Qian, H., Razeti, M., Razeto, A., Reinhold, B., Renshaw, A. L., Rescigno, M., Riffard, Q., Romani, A., Rossi, B., Rossi, N., Sablone, D., Samoylov, O., Sands, W., Sanfilippo, S., Sant, M., Savarese, C., Schlitzer, B., Segreto, E., Semenov, D. A., Sheshukov, A., Singh, P. N., Skorokhvatov, M. D., Smirnov, O., Sotnikov, A., Stanford, C., Suffritti, G. B., Suvorov, Y., Tartaglia, R., Testera, G., Tonazzo, A., Trinchese, P., Unzhakov, E. V., Verducci, M., Vishneva, A., Vogelaar, B., Wada, M., Waldrop, T. J., Walker, S., Wang, H., Wang, Y., Watson, A. W., Westerdale, S., Wojcik, M. M., Xiang, X., Xiao, X., Yang, C., Ye, Z., Zhu, C., and Zuzel, G.

Abstract

We report the measurement of the longitudinal diffusion constant in liquid argon with the DarkSide-50 dual-phase time projection chamber. The measurement is performed at drift electric fields of 100 V/cm, 150 V/cm, and 200 V/cm using high statistics 39Ar decays from atmospheric argon. We derive an expression to describe the pulse shape of the electroluminescence signal (S2) in dual-phase TPCs. The derived S2 pulse shape is fit to events from the uppermost portion of the TPC in order to characterize the radial dependence of the signal. The results are provided as inputs to the measurement of the longitudinal diffusion constant DL, which we find to be (4.12 ± 0.09) cm2/s for a selection of 140 keV electron recoil events in 200 V/cm drift field and 2.8 kV/cm extraction field. To study the systematics of our measurement we examine data sets of varying event energy, field strength, and detector volume yielding a weighted average value for the diffusion constant of (4.09 ± 0.12) cm2/s. The measured longitudinal diffusion constant is observed to have an energy dependence, and within the studied energy range the result is systematically lower than other results in the literature.

Published
2018

40. The position of fluorine in CP-118,954 affects AChE inhibition potency and PET imaging quantification for AChE expression in the rat brain

Author

Byung Chul Lee, Byung Seok Moon, Jae Ho Jung, Do Dam Park, Modesto de Candia, Hyun Soo Park, Hyun Sik Park, Nunzio Denora, Sang Eun Kim, and Cosimo Altomare

Subjects
Fluorine Radioisotopes, medicine.drug_class, Stereochemistry, Microdialysis, Pharmaceutical Science, 010402 general chemistry, 01 natural sciences, Rats, Sprague-Dawley, chemistry.chemical_compound, Piperidines, In vivo, Nucleophilic aromatic substitution, medicine, Animals, Moiety, Potency, IC50, 010405 organic chemistry, Brain, Fluorine, Isoxazoles, Ligand (biochemistry), Acetylcholinesterase, 0104 chemical sciences, chemistry, Acetylcholinesterase inhibitor, Positron-Emission Tomography, Cholinesterase Inhibitors
Abstract

The in vitro inhibition potency against acetylcholinesterase (AChE) of fluorinated derivatives of CP-118,954 (1) has been shown to depend upon the position of aromatic fluorine (F) substitution on the N-benzyl moiety. Indeed, the meta-F-substituted compound 3 (IC50=1.4nM) shows similar potency with the parent compound 1 (IC50=1.2nM), whereas the ortho-F derivative 2 (IC50=3.2nM) and para-F derivative 4 (IC50=10.8nM) were found to be less potent AChE inhibitors. A comparative in vivo microdialysis study in rats showed that 3 has the strongest effect on the neuropharmacological properties as AChE inhibitor. For PET imaging studies, a radiolabeled ligand ([18F]3) was synthesized through nucleophilic aromatic substitution reaction of diaryliodonium salt-based aldehyde precursor followed by reductive alkylation in a two-step radiolabeling procedure with 11.5 ± 1.2% (n=24, non-decay corrected) radiochemical yield and over 99% radiochemical purity. In a comparative PET imaging study of the three 18F-containing derivatives of CP-118,954 ([18F]2-4), [18F]3 showed the highest radioactivity in the AChE-rich region of normal rat brain which visually reflected the in vitro AChE-binding affinity of 3. These findings support [18F]3 as a promising AChE-targeted PET imaging ligand for the assessment of cholinergic activity into the brain, providing also insights into the AChE ligand disposition, which depends upon the position of the aromatic fluorine in the benzyl moiety.

Published
2017
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41. Pharmaceutical development of novel lactate-based 6-fluoro-l-DOPA formulations

Author

Cosimo Altomare, Anna Tolomeo, Vincenzo Dimiccoli, Angela Lopedota, Leonardo Degennaro, Nunzio Denora, Antonio Scilimati, Massimo Franco, Domenico Tricarico, Saverio Cellamare, Antonietta Mele, Valentino Laquintana, Renzo Luisi, Annalisa Cutrignelli, and Modesto de Candia

Subjects
Male, 0301 basic medicine, Chemistry, Pharmaceutical, Pharmaceutical Science, Mice, 03 medical and health sciences, chemistry.chemical_compound, Acetic acid, 0302 clinical medicine, In vivo, Animals, Humans, media_common.cataloged_instance, Chelation, Lactic Acid, Viability assay, European union, media_common, Sodium bicarbonate, Chromatography, Aqueous solution, Hydrogen-Ion Concentration, Dihydroxyphenylalanine, Rats, Mice, Inbred C57BL, Oxygen, 030104 developmental biology, chemistry, Biochemistry, Positron-Emission Tomography, 030220 oncology & carcinogenesis, Radiopharmaceuticals
Abstract

6-[ 18 F]fluoro- l -dihydroxyphenylalanine ( 18 F–DOPA) is a diagnostic positron emission tomography (PET) agent, which has been used for decades in imaging the loss of dopaminergic neurons in Parkinson's disease, and more recently to detect, stage and restage neuroendocrine tumors (NETs) and to search for recurrence of viable glioma tissue. The commercially available 18 F–DOPA PET radiopharmaceutical for diagnostic use in European Union countries, is formulated in an aqueous solution of acetic acid (1.05 mg/mL) and has the disadvantages that, immediately before injection, the pH must be adjusted to 4.0–5.0 by the addition of a sterile solution of sodium bicarbonate (84 mg/mL) causing a light and transient burning sensation at the injection site. To overcome these drawbacks, preformulation studies were accomplished to confirm that F-DOPA degradation was affected by pH. Hence, two formulations of F-DOPA, namely ND1 and ND2 , were prepared maintaining the pH = 5.0 using 1 mM l -(+)-lactate buffer, excluding oxygen, and incorporating in the formula the chelating agent Na 2 EDTA (1 mM). F-DOPA oxygen exposure, the presence of free metal cations in formulation and high pH values seem to promote F-DOPA degradation. The resulting formulations proved to guarantee the chemical stability of F-DOPA in solution at pH 5.0, value also compatible with the direct infusion. In vitro cell viability tests on mouse skeletal muscle fibers, renal tsa201 and neuronal SH-SY5Y cell lines, and in vivo studies in rats reported elsewhere, showed cell tolerability to the new F-DOPA formulations providing the basis for their further in vivo evaluation.

Published
2017
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42. New azepino[4,3-b]indole derivatives as nanomolar selective inhibitors of human butyrylcholinesterase showing protective effects against NMDA-induced neurotoxicity

Author

Modesto de Candia, Domenico Tricarico, Giorgia Zaetta, Saverio Cellamare, Cosimo Altomare, María Majellaro, and Nunzio Denora

Subjects
0301 basic medicine, Indoles, N-Methylaspartate, 01 natural sciences, Neuroprotection, 03 medical and health sciences, Alzheimer Disease, Cell Line, Tumor, Drug Discovery, medicine, Humans, Viability assay, Butyrylcholinesterase, Cholinesterase, Neurons, Pharmacology, Indole test, biology, 010405 organic chemistry, Chemistry, Organic Chemistry, Neurotoxicity, Azepines, General Medicine, medicine.disease, 0104 chemical sciences, Neuroprotective Agents, 030104 developmental biology, Biochemistry, Lipophilicity, biology.protein, NMDA receptor, Cholinesterase Inhibitors
Abstract

Several 6-substituted 3,4,5,6-tetrahydroazepino[4,3-b]indol-1(2H)-one (THAI) derivatives were synthesized and evaluated for their activity as cholinesterase (ChE) inhibitors. The most potent inhibitors were identified among 6-(2-phenylethyl)-THAI derivatives, and in particular compounds 12b and 12d proved to be very active against human BChE (IC50 = 13 and 1.8 nM, respectively), with 1000-fold selectivity over AChE. Structure-activity relationships highlighted critical features (e.g., ring fusion [4,3-b], integrity of the lactam CONH function) and favorable physicochemical properties of the 6-(2-phenylethyl) group (i.e., optimal position, size and lipophilicity of phenyl substituents). The effects of a number of compounds against NMDA-induced SH-SY5Y neuronal cell injury were also evaluated. Treatment with 12b increased cell viability in SH-SY5Y cells pretreated with 250 μM NMDA, with significant effects (P

Published
2017
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44. Data on the application of early coagulation support protocol in the management of major trauma patients

Author

Bocci, Maria Grazia, primary, Nardi, Giuseppe, additional, Veronesi, Giovanni, additional, Rondinelli, Maria Beatrice, additional, Palma, Antonella, additional, Fiore, Valentina, additional, De Candia, Erica, additional, Bianchi, Maria, additional, Maresca, Maddalena, additional, Barelli, Roberta, additional, Tersali, Alessandra, additional, Dell’Anna, Antonio Maria, additional, De Pascale, Gennaro, additional, Cutuli, Salvatore Lucio, additional, Mercurio, Giovanna, additional, Caricato, Anselmo, additional, Grieco, Domenico Luca, additional, Antonelli, Massimo, additional, and Cingolani, Emiliano, additional

Published
2019
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45. Early coagulation support protocol: A valid approach in real-life management of major trauma patients. Results from two Italian centres

Author

Bocci, Maria Grazia, primary, Nardi, Giuseppe, additional, Veronesi, Giovanni, additional, Rondinelli, Maria Beatrice, additional, Palma, Antonella, additional, Fiore, Valentina, additional, De Candia, Erica, additional, Bianchi, Maria, additional, Maresca, Maddalena, additional, Barelli, Roberta, additional, Tersali, Alessandra, additional, Dell'Anna, Antonio Maria, additional, De Pascale, Gennaro, additional, Cutuli, Salvatore Lucio, additional, Mercurio, Giovanna, additional, Caricato, Anselmo, additional, Grieco, Domenico Luca, additional, Antonelli, Massimo, additional, and Cingolani, Emiliano, additional

Published
2019
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46. Investigating 1,2,3,4,5,6-hexahydroazepino[4,3-b]indole as scaffold of butyrylcholinesterase-selective inhibitors with additional neuroprotective activities for Alzheimer's disease

Author

Purgatorio, Rosa, primary, de Candia, Modesto, additional, Catto, Marco, additional, Carrieri, Antonio, additional, Pisani, Leonardo, additional, De Palma, Annalisa, additional, Toma, Maddalena, additional, Ivanova, Olga A., additional, Voskressensky, Leonid G., additional, and Altomare, Cosimo D., additional

Published
2019
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47. New organic nitrate-containing benzyloxy isonipecotanilide derivatives with vasodilatory and anti-platelet activity

Author

Giorgia Zaetta, Modesto de Candia, Antonella Di Stilo, Cosimo Altomare, Saverio Cellamare, and Elisabetta Marini

Subjects
Adult, Male, Serum, Carbamate, Platelet Aggregation, Stereochemistry, Vasodilator Agents, medicine.medical_treatment, Pharmaceutical Science, Aorta, Thoracic, In Vitro Techniques, Nitric oxide, chemistry.chemical_compound, Antiplatelet activity, Nitrate, Amide, Nitric oxide-donors, medicine, Animals, Humans, Moiety, Nitrooxy alkyl carbamate derivatives, Rats, Wistar, chemistry.chemical_classification, Isonipecotamides, Vasodilation, 3003, Nitrates, Hydrolysis, Middle Aged, Methyl carbamate, Enzyme, chemistry, Piperidine, Platelet Aggregation Inhibitors
Abstract

A number of new nitric oxide (NO)-precursors were synthesized by grafting nitrate-containing moieties on the structures of the benzyloxy isonipecotanilide derivatives 1 and 2 already reported as moderately potent antiplatelet agents. Various nitrooxy (ONO2)-alkyl side chains were covalently linked to the piperidine nitrogen of the parent compounds through carbamate and amide linkage, and the synthesis of a benzyl nitrate analog (15) of compound 1 was also achieved. The in vitro vasodilatory activities, as well as platelet anti-aggregatory effects, of the newly synthesized organic nitrates were assessed. The (ONO2)methyl carbamate-based derivative 5a and the benzyl nitrate analog 15, which on the other hand retain activity as inhibitors of ADP-induced platelet aggregation, exhibited strong NO-mediated vasodilatory effects on pre-contracted rat aorta strips, with EC50 values in the low nanomolar range (13 and 29 nM, respectively). Experiments carried out with the selectively inhibited soluble guanylate cyclase (sGC), which is the key enzyme of the NO-mediated pathway leading to vascular smooth muscle relaxation, confirmed the involvement of NO in the observed vasodilation. The nitrate derivatives proved to be stable in acidic aqueous solution and at pH 7.4. In human serum, unlike 5a, which showed not to undergo enzyme-catalyzed decomposition, the other tested (ONO2)-alkyl carbamate-based compounds (5b and 5e) and benzyl nitrate 15 underwent a faster degradation. However, their decomposition rates in serum were quite slow (t½ > 2.6 h), which suggests that nitrate moiety is poorly metabolized in blood plasma and that much of the in vitro anti-platelet activity has to be attributed to the intact (ONO2)-containing molecules.

Published
2015
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48. Evolutionary behavioral genetics

Author

Matthew C. Keller, Teresa R de Candia, and Brendan P. Zietsch

Subjects
Scientific enterprise, Cognitive science, Cognitive Neuroscience, Evolutionary neuroscience, Data science, Evolutionary psychology, Article, Genetic architecture, Behavioral Neuroscience, Psychiatry and Mental health, Mutation–selection balance, ComputingMethodologies_GENERAL, Human behavioral ecology, Human behaviour genetics, Psychology, Behavioural genetics
Abstract

We describe the scientific enterprise at the intersection of evolutionary psychology and behavioral genetics — a field that could be termed Evolutionary Behavioral Genetics — and how modern genetic data is revolutionizing our ability to test questions in this field. We first explain how genetically informative data and designs can be used to investigate questions about the evolution of human behavior, and describe some of the findings arising from these approaches. Second, we explain how evolutionary theory can be applied to the investigation of behavioral genetic variation. We give examples of how new data and methods provide insight into the genetic architecture of behavioral variation and what this tells us about the evolutionary processes that acted on the underlying causal genetic variants.

Published
2015
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49. EFFECTS OF ASSORTATIVE MATING ON ESTIMATES OF SNP HERITABILITY

Author

Matthew C. Keller, Jian Yang, Teresa R de Candia, Matt Jones, Lindon J. Eaves, Michael E. Goddard, Rasool Tahmasbi, David M. Evans, Luke M. Evans, and Peter M. Visscher

Subjects
Pharmacology, Natural selection, Assortative mating, Biology, Heritability, Covariance, Twin study, Regression, Psychiatry and Mental health, Neurology, Similarity (network science), Sample size determination, Statistics, Pharmacology (medical), Neurology (clinical), Biological Psychiatry
Abstract

Background Mates are similar to one another across a large number of traits, including liabilities underlying psychiatric disorders. It has long been known that when such phenotypic similarity implies genetic similarity (hereafter, assortative mating), heritability estimates from family and twin studies can be biased. However, the effects of assortative mating, if any, on estimates of heritability from all SNPs in unrelated individuals (SNP-based heritability, h2SNP) have not been investigated to date. Methods We derived mathematically the expected behavior of estimates from Haseman-Elston regression and GREML, and assessed these predictions via simulation. We then assessed in the UK Biobank whether the predicted signatures of assortative mating on h2SNP were observed. Results We show analytically and via simulation that estimates of h2SNP from both GREML and Haseman-Elston regression are typically biased upwards in the presence of assortative mating. However, estimates from Haseman-Elston regression are roughly constant as a function of sample size and number of markers, whereas the ratio of sample size to number of markers strongly affects those from GREML. This difference in estimate behavior allows one to assess in real data whether assortative mating is affecting estimates of h2SNP. When we did this in the UK Biobank for height and IQ, we observed that h2SNP estimates for height that behaved as predicted, but not for h2SNP estimates for IQ. Discussion For many traits, the degree of bias in estimates of h2SNP is expected to be small, but it can be non-trivial for other traits, depending on the degree of assortative mating and the heritability of the traits. For example, based on spousal similarity, we predict that h2SNP estimates of height and IQ are ~25% greater than their true equilibrium values. That we did not observe the predicted pattern of h2SNP estimates for IQ may either suggest that spousal similarity for IQ occurs via mechanisms that do not lead to genetic similarity (e.g., social homogamy) or that the effects of assortative mating on the covariance between causal variants is counter-acted by the forces of natural selection.

Published
2019
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50. Functional role of protease activated receptors in vascular biology

Author

Erica De Candia and Maria Adele Alberelli

Subjects
Blood Platelets, Protease activated receptors, medicine.medical_specialty, Proteases, Vascular smooth muscle, Physiology, Myocytes, Smooth Muscle, Receptors, Proteinase-Activated, Vascular permeability, Biology, Lung injury, Cardiovascular System, Vascular biology, Muscle, Smooth, Vascular, Proinflammatory cytokine, Thrombin, Internal medicine, medicine, Animals, Humans, Endothelium, Receptor, Pharmacology, Settore MED/09 - MEDICINA INTERNA, Cell biology, Endocrinology, Smooth muscle cells, Molecular Medicine, Endothelium, Vascular, Protein C, medicine.drug
Abstract

Protease activated receptors (PARs) are a small family of G protein-coupled receptors (GPCR) mediating the cellular effects of some proteases of the coagulation system, such as thrombin, or other proteases, such as trypsin or metalloproteinase 1. As the prototype of PARs, PAR1 is a seven transmembrane GPCR that, upon cleavage by thrombin, unmasks a new amino-terminus able to bind intramolecularly to PAR1 itself thus inducing signaling. In the vascular system, thrombin and other proteases of the coagulation-fibrinolysis system, such as plasmin, factor VIIa and factor Xa, activated protein C, are considered physiologically relevant agonists, and PARs appear to largely account for the cellular effects of these enzymes. In the vasculature, PARs are expressed on platelets, endothelial cells (ECs) and vascular smooth muscle cells (VSMCs). In the vessel wall, under physiological conditions, PARs are mainly expressed in ECs and participate in the regulation of vascular tone, by inducing endothelium-dependent relaxation. PAR activation on ECs promotes conversion of these cells into a proinflammatory phenotype, causes increase of vascular permeability, and the exposure/secretion of proteins and cytokines mediating the local accumulation of platelets and leukocytes. These effects contribute to the vascular consequences of sepsis and of diseases such as acute lung injury and acute respiratory distress syndrome. In normal arteries PARs are to a much lesser amount expressed on VSMCs. However, in conditions associated with endothelial dysfunction, PARs mediate contraction, proliferation, migration, hypertrophy of VSMCs and their production of extracellular matrix, thereby contributing to the pathophysiology of atherosclerosis and hypertension. Inhibition of protease-PAR interaction might thus become a potential therapeutic target in various vascular diseases.

Published
2014
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