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3. Anti-Glycation Properties of Zinc-Enriched Arthrospira platensis (Spirulina) Contribute to Prevention of Metaflammation in a Diet-Induced Obese Mouse Model

Author

Aimaretti, Eleonora, primary, Porchietto, Elisa, additional, Mantegazza, Giacomo, additional, Gargari, Giorgio, additional, Collotta, Debora, additional, Einaudi, Giacomo, additional, Ferreira Alves, Gustavo, additional, Marzani, Enrica, additional, Algeri, Alessandro, additional, Dal Bello, Federica, additional, Aragno, Manuela, additional, Cifani, Carlo, additional, Guglielmetti, Simone, additional, Mastrocola, Raffaella, additional, and Collino, Massimo, additional

Published
2024
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5. Dietary Intake of Fructooligosaccharides Protects against Metabolic Derangements Evoked by Chronic Exposure to Fructose or Galactose in Rats

Author

Almasri, Fidèle, primary, Collotta, Debora, additional, Aimaretti, Eleonora, additional, Sus, Nadine, additional, Aragno, Manuela, additional, Dal Bello, Federica, additional, Eva, Carola, additional, Mastrocola, Raffaella, additional, Landberg, Rikard, additional, Frank, Jan, additional, and Collino, Massimo, additional

Published
2023
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11. Anti-inflammatory and anti-glycative properties of zinc-enriched spirulina in diet-induced obese/diabetic mice

Author

Aimaretti, Eleonora, primary, Murzio, Carlo, additional, Alves, Gustavo Ferreira, additional, Einaudi, Giacomo, additional, Collotta, Debora, additional, Porchietto, Elisa, additional, Cifani, Carlo, additional, Algeri, Alessandro, additional, Aragno, Manuela, additional, Collino, Massimo, additional, and Mastrocola, Raffaella, additional

Published
2022
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12. ICOS-Fc as innovative immunomodulatory approach to counteract inflammation and organ injury in sepsis

Author

Alves, Gustavo Ferreira, primary, Stoppa, Ian, additional, Aimaretti, Eleonora, additional, Monge, Chiara, additional, Mastrocola, Raffaella, additional, Porchietto, Elisa, additional, Einaudi, Giacomo, additional, Collotta, Debora, additional, Bertocchi, Ilaria, additional, Boggio, Elena, additional, Gigliotti, Casimiro Luca, additional, Clemente, Nausicaa, additional, Aragno, Manuela, additional, Fernandes, Daniel, additional, Cifani, Carlo, additional, Thiemermann, Christoph, additional, Dianzani, Chiara, additional, Dianzani, Umberto, additional, and Collino, Massimo, additional

Published
2022
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15. Inhibition of Macrophage Migration Inhibitory Factor Activity Attenuates Haemorrhagic Shock-Induced Multiple Organ Dysfunction in Rats

Author

Patel, Nikita M., primary, Yamada, Noriaki, additional, Oliveira, Filipe R. M. B., additional, Stiehler, Lara, additional, Zechendorf, Elisabeth, additional, Hinkelmann, Daniel, additional, Kraemer, Sandra, additional, Stoppe, Christian, additional, Collino, Massimo, additional, Collotta, Debora, additional, Alves, Gustavo Ferreira, additional, Ramos, Hanna Pillmann, additional, Sordi, Regina, additional, Marzi, Ingo, additional, Relja, Borna, additional, Marx, Gernot, additional, Martin, Lukas, additional, and Thiemermann, Christoph, additional

Published
2022
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16. Pharmacological Inhibition of FAK-Pyk2 Pathway Protects Against Organ Damage and Prolongs the Survival of Septic Mice

Author

Alves, Gustavo Ferreira, primary, Aimaretti, Eleonora, additional, Einaudi, Giacomo, additional, Mastrocola, Raffaella, additional, de Oliveira, Junior Garcia, additional, Collotta, Debora, additional, Porchietto, Elisa, additional, Aragno, Manuela, additional, Cifani, Carlo, additional, Sordi, Regina, additional, Thiemermann, Christoph, additional, Fernandes, Daniel, additional, and Collino, Massimo, additional

Published
2022
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18. In Vitro Evaluation of the Toxicological Profile and Oxidative Stress of Relevant Diet-Related Advanced Glycation End Products and Related 1,2-Dicarbonyls

Author

Cepas, Vanesa, primary, Manig, Friederike, additional, Mayo, Juan C., additional, Hellwig, Michael, additional, Collotta, Debora, additional, Sanmartino, Valentina, additional, Carrocera-Pumarino, Rebeca, additional, Collino, Massimo, additional, Henle, Thomas, additional, and Sainz, Rosa M., additional

Published
2021
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19. A Synthetic Peptide Designed to Neutralize Lipopolysaccharides Attenuates Metaflammation and Diet-Induced Metabolic Derangements in Mice

Author

Mohammad, Shireen, primary, Al Zoubi, Sura, additional, Collotta, Debora, additional, Krieg, Nadine, additional, Wissuwa, Bianka, additional, Ferreira Alves, Gustavo, additional, Purvis, Gareth S. D., additional, Norata, Giuseppe Danilo, additional, Baragetti, Andrea, additional, Catapano, Alberico Luigi, additional, Solito, Egle, additional, Zechendorf, Elisabeth, additional, Schürholz, Tobias, additional, Correa-Vargas, Wilmar, additional, Brandenburg, Klaus, additional, Coldewey, Sina M., additional, Collino, Massimo, additional, Yaqoob, Muhammad M., additional, Martin, Lukas, additional, and Thiemermann, Christoph, additional

Published
2021
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20. Altered hepatic sphingolipid metabolism in insulin resistant mice: Role of advanced glycation endproducts

Author

Mastrocola, Raffaella, Mastrocola, Raffaella, Dal Bello, Federica, Cento, Alessia S., Gaens, Katrien, Collotta, Debora, Aragno, Manuela, Medana, Claudio, Collino, Massimo, Wouters, Kristiaan, Schalkwijk, Casper G., Mastrocola, Raffaella, Mastrocola, Raffaella, Dal Bello, Federica, Cento, Alessia S., Gaens, Katrien, Collotta, Debora, Aragno, Manuela, Medana, Claudio, Collino, Massimo, Wouters, Kristiaan, and Schalkwijk, Casper G.

Abstract

High plasma levels of the sphingolipid intermediates ceramide (Cer) and sphingosine-1-phosphate (S1P) are suggested to be involved in the development of insulin resistance (IR). Recent evidence indicates that advanced glycation endproducts (AGEs) can alter the sphingolipids metabolism equilibrium. Since enzymes responsible for sphingolipid rheostat maintenance are highly expressed in liver, we thus investigated whether AGEs accumulation can affect hepatic sphingolipids metabolism in insulin resistant mice. Two different models of IR were examined: genetically diabetic LeptrDb-/- (DbDb) and diet-induced insulin resistant C57Bl/6J mice fed a 60% trans-fat diet (HFD). In addition, a group of HFD mice was supplemented with the anti-AGEs compound pyridoxamine. AGEs were evaluated in the liver by western blotting. Cer and S1P were measured by UHPLC-MS/MS. The expression of RAGE and of enzymes involved in sphingolipid metabolism were assessed by RT-PCR and western blotting. HepG2 cells were used to study the effect of the major AGE N epsilon(carboxymethyl)lysine (CML)-albumin on sphingolipid metabolism and the role of the receptor of AGEs (RAGE). High levels of AGEs and RAGE were detected in the liver of both DbDb and HFD mice in comparison to controls. The expression of enzymes of sphingolipid metabolism was altered in both models, accompanied by increased levels of Cer and S1P. Specifically, ceramide synthase 5 and sphingosine kinase 1 were increased, while neutral ceramidase was reduced. Pyridoxamine supplementation to HFD mice diminished hepatic AGEs and prevented alterations of sphingolipid metabolism and the development of IR. CML administration to HepG2 cells evoked alterations similar to those observed in vivo, that were in part mediated by the binding to RAGE. The present study shows a direct involvement of AGEs in alterations of sphingolipid metabolism associated to the development of IR. The modulation of sphingolipids metabolism through the prevention of AGE

Published
2021

23. The inhibition of Macrophage Migration Inhibitory Factor by ISO-1 attenuates trauma-induced multi organ dysfunction in rats

Author

Martin, Lukas, primary, Patel, Nikita Mayur, additional, Yamada, Noriaki, additional, Borges Oliveira, Filipe Rodolfo Moreira, additional, Stiehler, Lara, additional, Zechendorf, Elisabeth, additional, Hinkelmann, Daniel, additional, Kraemer, Sandra, additional, Stoppe, Christian, additional, Collino, Massimo, additional, Collotta, Debora, additional, Alves, Gustavo Ferreira, additional, Ramos, Hanna Pillmann, additional, Sordi, Regina, additional, Marzi, Ingo, additional, Relja, Borna, additional, Marx, Gernot, additional, and Thiemermann, Christoph, additional

Published
2021
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26. X-Linked Immunodeficient Mice With No Functional Bruton's Tyrosine Kinase Are Protected From Sepsis-Induced Multiple Organ Failure

Author

O'Riordan, Caroline E., primary, Purvis, Gareth S. D., additional, Collotta, Debora, additional, Krieg, Nadine, additional, Wissuwa, Bianka, additional, Sheikh, Madeeha H., additional, Ferreira Alves, Gustavo, additional, Mohammad, Shireen, additional, Callender, Lauren A., additional, Coldewey, Sina M., additional, Collino, Massimo, additional, Greaves, David R., additional, and Thiemermann, Christoph, additional

Published
2020
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28. Inhibition of Bruton's TK regulates macrophage NF‐κB and NLRP3 inflammasome activation in metabolic inflammation

Author

Purvis, Gareth S.D., primary, Collino, Massimo, additional, Aranda‐Tavio, Haidee, additional, Chiazza, Fausto, additional, O'Riordan, Caroline E., additional, Zeboudj, Lynda, additional, Mohammad, Shireen, additional, Collotta, Debora, additional, Verta, Roberta, additional, Guisot, Nicolas E.S., additional, Bunyard, Peter, additional, Yaqoob, Magdi M., additional, Greaves, David R., additional, and Thiemermann, Christoph, additional

Published
2020
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30. Effects of Exogenous Dietary Advanced Glycation End Products on the Cross-Talk Mechanisms Linking Microbiota to Metabolic Inflammation

Author

Mastrocola, Raffaella, primary, Collotta, Debora, additional, Gaudioso, Giulia, additional, Le Berre, Marie, additional, Cento, Alessia Sofia, additional, Ferreira Alves, Gustavo, additional, Chiazza, Fausto, additional, Verta, Roberta, additional, Bertocchi, Ilaria, additional, Manig, Friederike, additional, Hellwig, Michael, additional, Fava, Francesca, additional, Cifani, Carlo, additional, Aragno, Manuela, additional, Henle, Thomas, additional, Joshi, Lokesh, additional, Tuohy, Kieran, additional, and Collino, Massimo, additional

Published
2020
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31. Ticagrelor Conditioning Effects Are Not Additive to Cardioprotection Induced by Direct NLRP3 Inflammasome Inhibition: Role of RISK, NLRP3, and Redox Cascades

Author

Penna, Claudia, primary, Aragno, Manuela, additional, Cento, Alessia Sofia, additional, Femminò, Saveria, additional, Russo, Isabella, additional, Bello, Federica Dal, additional, Chiazza, Fausto, additional, Collotta, Debora, additional, Alves, Gustavo Ferreira, additional, Bertinaria, Massimo, additional, Zicola, Elisa, additional, Mercurio, Valentina, additional, Medana, Claudio, additional, Collino, Massimo, additional, and Pagliaro, Pasquale, additional

Published
2020
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34. Ribonuclease 1 attenuates septic cardiomyopathy and cardiac apoptosis in a murine model of polymicrobial sepsis

Author

Zechendorf, Elisabeth, primary, O’Riordan, Caroline E., additional, Stiehler, Lara, additional, Wischmeyer, Natalie, additional, Chiazza, Fausto, additional, Collotta, Debora, additional, Denecke, Bernd, additional, Ernst, Sabrina, additional, Müller-Newen, Gerhard, additional, Coldewey, Sina M., additional, Wissuwa, Bianka, additional, Collino, Massimo, additional, Simon, Tim-Philipp, additional, Schuerholz, Tobias, additional, Stoppe, Christian, additional, Marx, Gernot, additional, Thiemermann, Christoph, additional, and Martin, Lukas, additional

Published
2020
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36. Bruton's Tyrosine Kinase Inhibition Attenuates the Cardiac Dysfunction Caused by Cecal Ligation and Puncture in Mice

Author

O'Riordan, Caroline E., primary, Purvis, Gareth S. D., additional, Collotta, Debora, additional, Chiazza, Fausto, additional, Wissuwa, Bianka, additional, Al Zoubi, Sura, additional, Stiehler, Lara, additional, Martin, Lukas, additional, Coldewey, Sina M., additional, Collino, Massimo, additional, and Thiemermann, Christoph, additional

Published
2019
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38. Identification of AnnexinA1 as an Endogenous Regulator of RhoA, and Its Role in the Pathophysiology and Experimental Therapy of Type-2 Diabetes

Author

Purvis, Gareth S. D., primary, Collino, Massimo, additional, Loiola, Rodrigo A., additional, Baragetti, Andrea, additional, Chiazza, Fausto, additional, Brovelli, Martina, additional, Sheikh, Madeeha H., additional, Collotta, Debora, additional, Cento, Alessia, additional, Mastrocola, Raffaella, additional, Aragno, Manuela, additional, Cutrin, Juan C., additional, Reutelingsperger, Chris, additional, Grigore, Liliana, additional, Catapano, Alberico L., additional, Yaqoob, Magdi M., additional, Norata, Giuseppe Danilo, additional, Solito, Egle, additional, and Thiemermann, Christoph, additional

Published
2019
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40. Reduced Susceptibility to Sugar-Induced Metabolic Derangements and Impairments of Myocardial Redox Signaling in Mice Chronically Fed with D-Tagatose when Compared to Fructose

Author

Collotta, Debora, primary, Lucarini, Laura, additional, Chiazza, Fausto, additional, Cento, Alessia Sofia, additional, Durante, Mariaconcetta, additional, Sgambellone, Silvia, additional, Chini, Jacopo, additional, Baratta, Francesca, additional, Aragno, Manuela, additional, Mastrocola, Raffaella, additional, Masini, Emanuela, additional, and Collino, Massimo, additional

Published
2018
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41. Inhibition of NF-κB Pathway with IKK-16 or Linagliptin Attenuates the Cardiac Dysfunction Associated with Polymicrobial Sepsis in Mice with Preexisting Type 2 Diabetes Mellitus (T2DM)

Author

ZOUBI, SURA AL, primary, CHEN, JIANMIN, additional, MARTIN, LUKAS, additional, MURPHY, CATHERINE, additional, PURVIS, GARETH S., additional, CHIAZZA, FAUSTO, additional, COLLOTTA, DEBORA, additional, COLLINO, MASSIMO, additional, and THIEMERMANN, CHRISTOPH, additional

Published
2018
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43. Fructose liquid and solid formulations differently affect gut integrity, microbiota composition and related liver toxicity: a comparative in vivo study

Author

Mastrocola, Raffaella, primary, Ferrocino, Ilario, additional, Liberto, Erica, additional, Chiazza, Fausto, additional, Cento, Alessia Sofia, additional, Collotta, Debora, additional, Querio, Giulia, additional, Nigro, Debora, additional, Bitonto, Valeria, additional, Cutrin, Juan Carlos, additional, Rantsiou, Kalliopi, additional, Durante, Mariaconcetta, additional, Masini, Emanuela, additional, Aragno, Manuela, additional, Cordero, Chiara, additional, Cocolin, Luca, additional, and Collino, Massimo, additional

Published
2018
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44. Genetic deletion of RAGE in Dbdb mice interferes with AGEs receptors and detoxifying systems in liver

Author

Cento, Alessia S., primary, Chiazza, Fausto, additional, Collotta, Debora, additional, Barutta, Federica, additional, Robertus, Margee, additional, Aragno, Manuela, additional, Scheijen, Jean, additional, Collino, Massimo, additional, Gaens, Katrien H., additional, Schalkwijk, Casper G., additional, Wouters, Kristiaan, additional, and Mastrocola, Raffaella, additional

Published
2018
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45. Pharmacological Inhibition of NLRP3 Inflammasome Attenuates Myocardial Ischemia/Reperfusion Injury by Activation of RISK and Mitochondrial Pathways

Author

Mastrocola, Raffaella, primary, Penna, Claudia, additional, Tullio, Francesca, additional, Femminò, Saveria, additional, Nigro, Debora, additional, Chiazza, Fausto, additional, Serpe, Loredana, additional, Collotta, Debora, additional, Alloatti, Giuseppe, additional, Cocco, Mattia, additional, Bertinaria, Massimo, additional, Pagliaro, Pasquale, additional, Aragno, Manuela, additional, and Collino, Massimo, additional

Published
2016
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48. [Exploring Tyrosine Kinase Inhibitor (TKI)-Induced Nephrotoxicity: An Emerging Issue from Bench to Bedside].

Author

Collotta D, Aimaretti E, and Collino M

Subjects
Humans, Tyrosine Kinase Inhibitors, Protein Kinase Inhibitors adverse effects
Abstract

Tyrosine Kinase Inhibitors (TKIs) have significantly contributed to revolutionizing cancer treatment, as they are orally administered small molecules able to target key pathways involved in tumor growth and angiogenesis. However, the clinical utility of TKIs may be compromised by adverse effects, which can affect tissues and organs, including kidneys. This comprehensive review offers a general overview of studies reporting the incidence and clinical characteristics of TKI-related nephrotoxicity and it explores the mechanisms underlying the intricate relationship between TKIs and renal toxicity. The biological rationale for the kidney manifestations of toxicity associated with TKI agents is here discussed, underlying potential off-target effects and emphasizing the importance of accurate risk assessment and tailored patient management strategies. Deep insight into the molecular mechanisms of TKI nephrotoxicity will help to improve the global understanding of the pathophysiology of this peculiar toxicity and to develop more effective and safer therapies., (Copyright by Società Italiana di Nefrologia SIN, Rome, Italy.)

Published
2023

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