Your search keyword '"Clizia Chinello"' showing total 123 results

1. Automated radiosynthesis and preclinical evaluation of two new PSMA-617 derivatives radiolabelled via [18F]AlF2+ method

Author

Marco Nicola Iannone, Silvia Valtorta, Stefano Stucchi, Stefano Altomonte, Elia Anna Turolla, Elisa Vino, Paolo Rainone, Valentina Zecca, Alessia Lo Dico, Marco Maspero, Mariangela Figini, Matteo Bellone, Samuele Ciceri, Diego Colombo, Clizia Chinello, Lisa Pagani, Rosa Maria Moresco, Sergio Todde, and Patrizia Ferraboschi

Subjects

PSMA-617, NODA, RESCA, [18F]AlF2+, Fluorine-18, Automation, Medical physics. Medical radiology. Nuclear medicine, R895-920, Therapeutics. Pharmacology, RM1-950

Abstract

Abstract Background In the last decade the development of new PSMA-ligand based radiopharmaceuticals for the imaging and therapy of prostate cancer has been a highly active and important area of research. The most promising derivative in terms of interaction with the antigen and clinical properties has been found to be “PSMA-617”, and its lutetium-177 radiolabelled version has recently been approved by EU and USA regulatory agencies for therapeutic purposes. For the above reasons, the development of new derivatives of PSMA-617 radiolabelled with fluorine-18 may still be of great interest. This paper proposes the comparison of two different PSMA-617 derivatives functionalized with NODA and RESCA chelators, respectively, radiolabelled via [18F]AlF2+ complexation. Results The organic synthesis of two PSMA-617 derivatives and their radiolabelling via [18F]AlF2+ complexation resulted to proceed efficiently and successfully. Moreover, stability in solution and in plasma has been evaluated. The whole radiosynthesis procedure has been fully automated, and the final products have been obtained with radiochemical yield and purity potentially suitable for clinical studies. The biodistribution of the two derivatives was performed both in prostate cancer and glioma tumour models. Compared with the reference [18F]F-PSMA-1007 and [18F]F-PSMA-617-RESCA, [18F]F-PSMA-617-NODA derivative showed a higher uptake in both tumors, faster clearance in non-target organs, and lower uptake in salivary glands. Conclusion PSMA-617 NODA and RESCA derivatives were radiolabelled successfully via [18F]AlF2+ chelation, the former being more stable in solution and human plasma. Moreover, preclinical biodistribution studies showed that [18F]F-PSMA-617-NODA might be of potential interest for clinical applications.

Published

2024

2. Reproducing extracellular matrix adverse remodelling of non-ST myocardial infarction in a large animal model

Author

Paolo Contessotto, Renza Spelat, Federico Ferro, Vaidas Vysockas, Aušra Krivickienė, Chunsheng Jin, Sandrine Chantepie, Clizia Chinello, Audrys G. Pauza, Camilla Valente, Mindaugas Rackauskas, Alvise Casara, Vilma Zigmantaitė, Fulvio Magni, Dulce Papy-Garcia, Niclas G. Karlsson, Eglė Ereminienė, Abhay Pandit, and Mark Da Costa

Subjects

Science

Abstract

The study of the pathophysiology and possible interventions for non-ST-segment elevation myocardial infarction is hindered by the lack of a reproducible pre-clinical model. Here, authors develop an ovine model to reproduce post-ischemic remodeling in non-ST myocardial infarction and reveal distinct complex sugar moieties in cellular membranes and extracellular matrix patterns in infarcted tissue.

Published

2023

3. Metabolic reprogramming and membrane glycan remodeling as potential drivers of zebrafish heart regeneration

Author

Renza Spelat, Federico Ferro, Paolo Contessotto, Amal Aljaabary, Sergio Martin-Saldaña, Chunsheng Jin, Niclas G. Karlsson, Maura Grealy, Markus M. Hilscher, Fulvio Magni, Clizia Chinello, Michelle Kilcoyne, and Abhay Pandit

Subjects

Biology (General), QH301-705.5

Abstract

Transcriptomic and proteomic analyses reveal that glycosylation and carbohydrate metabolism are central processes in heart regeneration in zebrafish, including a shift from OXPHOS to glycolysis seven days after injury.

Published

2022

4. Untargeted Mass Spectrometry Approach to Study SARS-CoV-2 Proteins in Human Plasma and Saliva Proteome

Author

Lisa Pagani, Clizia Chinello, Allia Mahajneh, Francesca Clerici, Lucrezia Criscuolo, Andrea Favalli, Paola Gruarin, Renata Grifantini, Alessandra Bandera, Andrea Lombardi, Riccardo Ungaro, Antonio Muscatello, Francesco Blasi, Andrea Gori, and Fulvio Magni

Subjects

COVID-19, saliva, plasma, proteomics, biomarker, Therapeutics. Pharmacology, RM1-950, Biochemistry, QD415-436

Abstract

Since the start of the COVID-19 outbreak, more than four million people have died of this disease. Given its ability to provide a precise response, mass spectrometry-based proteomics could represent a useful tool to study this pathology. To this end, an untargeted nLC-ESI-MS/MS-based method to characterise SARS-CoV-2 proteins, including possible variants, and investigate human saliva and plasma proteome in a single analysis was developed for further application in patients. Four SARS-CoV-2 recombinant proteins, three (S1–S2–RBD) belonging to the spike glycoprotein (S) and one corresponding to the nucleoprotein (N), were prepared and analysed with nLC-UHRTOF by injecting decreasing amounts to establish the limit of detection (LOD) of the method. This was determined as 10 pg for all the components of the S protein and for N (71 amol and 213 amol, respectively). Various viral inactivation strategies plus deglycosylation and digestion approaches were then tested in saliva and plasma spiked with different quantities of SARS-CoV-2 recombinant proteins. The limit of characterisation (LOC) in saliva for the N and S proteins was observed at 100 pg (coverage of 20% and 3%, respectively); instead, in plasma, it was 33 pg for N and 330 pg for the S protein, with a coverage of 4% for both. About 300 and 800 human proteins were identified in plasma and saliva, respectively, including several key effectors and pathways that are known to be altered in COVID-19 patients. In conclusion, this approach allows SARS-CoV-2 proteins and the human proteome to be simultaneously explored, both for plasma and saliva, showing a high relevant potential for retrospective studies aimed at investigating possible virus variants and for patient stratification.

Published

2022

5. Towards the Definition of the Molecular Hallmarks of Idiopathic Membranous Nephropathy in Serum Proteome: A DIA-PASEF Approach

Author

Paolo Previtali, Lisa Pagani, Giulia Risca, Giulia Capitoli, Eleonora Bossi, Glenda Oliveira, Isabella Piga, Antonella Radice, Barbara Trezzi, Renato Alberto Sinico, Fulvio Magni, and Clizia Chinello

Subjects

membranous nephropathies, proteomics, mass spectrometry, DIA-PASEF, serum, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Idiopathic membranous nephropathy (IMN) is a pathologically defined disorder of the glomerulus, primarily responsible for nephrotic syndromes (NS) in nondiabetic adults. The underlying molecular mechanisms are still not completely clarified. To explore possible molecular and functional signatures, an optimised mass spectrometry (MS) method based on next-generation data-independent acquisition combined with ion-mobility was applied to serum of patients affected by IMN (n = 15) or by other glomerulopathies (PN) (n = 15). The statistical comparison highlighted a panel of 57 de-regulated proteins with a significant increase in lipoprotein-related proteins (APOC1, APOB, APOA1, APOL1 and LCAT) and a substantial quantitative alteration of key serpins (including A4, D1, A7, A6, F2, F1 and 1) possibly associated with IMN or NS and podocyte stress. A critical dysregulation in metabolisms of lipids (e.g., VLDL assembly and clearance) likely to be related to known hyperlipidemia in IMN, along with involvement of non-classical complement pathways and a putative enrolment of ficolin-2 in sustaining the activation of the lectin-mediated complement system have been pinpointed. Moreover, mannose receptor CD206 (MRC1-down in IMN) and biotinidase (BTD-up in IMN) are able alone to accurately distinguish IMN vs. PN. To conclude, our work provides key proteomic insights into the IMN complexity, opening the way to an efficient stratification of MN patients.

Published

2023

6. ETNK1 mutations induce a mutator phenotype that can be reverted with phosphoethanolamine

Author

Diletta Fontana, Mario Mauri, Rossella Renso, Mattia Docci, Ilaria Crespiatico, Lisa M. Røst, Mi Jang, Antonio Niro, Deborah D’Aliberti, Luca Massimino, Mayla Bertagna, Giovanni Zambrotta, Mario Bossi, Stefania Citterio, Barbara Crescenzi, Francesca Fanelli, Valeria Cassina, Roberta Corti, Domenico Salerno, Luca Nardo, Clizia Chinello, Francesco Mantegazza, Cristina Mecucci, Fulvio Magni, Guido Cavaletti, Per Bruheim, Delphine Rea, Steen Larsen, Carlo Gambacorti-Passerini, and Rocco Piazza

Subjects

Science

Abstract

ETNK1 mutations are recurrent in leukemia but how they contribute to oncogenesis is still unclear. Here, the authors show that ETNK1 mutations increase mitochondrial activity, ROS and H2AX levels and that these effects can be rescued upon phosphoethanolamine supplementation.

Published

2020

7. Detecting Proteomic Indicators to Distinguish Diabetic Nephropathy from Hypertensive Nephrosclerosis by Integrating Matrix-Assisted Laser Desorption/Ionization Mass Spectrometry Imaging with High-Mass Accuracy Mass Spectrometry

Author

Andrew Smith, Vadim Iablokov, Mariafrancesca Mazza, Sonia Guarnerio, Vanna Denti, Mariia Ivanova, Martina Stella, Isabella Piga, Clizia Chinello, Bram Heijs, Peter A. van Veelen, Hallgrimur Benediktsson, Daniel A. Muruve, and Fulvio Magni

Subjects

diabetic nephropathy, hypertensive nephrosclerosis, chronic kidney disease, matrix-assisted laser desorption/ionization mass spectrometry imaging, mass spectrometry, proteomics, Dermatology, RL1-803, Diseases of the circulatory (Cardiovascular) system, RC666-701, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Introduction: Diabetic nephropathy (DN) and hypertensive nephrosclerosis (HN) represent the most common causes of chronic kidney disease (CKD) and many patients progress to ­end-stage renal disease. Patients are treated primarily through the management of cardiovas­cular risk factors and hypertension; however patients with HN have a more favorable outcome. A noninvasive clinical approach to separate these two entities, especially in hypertensive patients who also have diabetes, would allow for targeted treatment and more appropriate resource allocation to those patients at the highest risk of CKD progression. Meth­ods: In this preliminary study, high-spatial-resolution matrix-assisted laser desorption/ion­ization (MALDI) mass spectrometry imaging (MSI) was integrated with high-mass accuracy MALDI-FTICR-MS and nLC-ESI-MS/MS analysis in order to detect tissue proteins within kidney biopsies to discriminate cases of DN (n = 9) from cases of HN (n = 9). Results: Differences in the tryptic peptide profiles of the 2 groups could clearly be detected, with these becoming even more evident in the more severe histological classes, even if this was not evident with routine histology. In particular, 4 putative proteins were detected and had a higher signal intensity within regions of DN tissue with extensive sclerosis or fibrosis. Among these, 2 proteins (PGRMC1 and CO3) had a signal intensity that increased at the latter stages of the disease and may be associated with progression. Discussion/Conclusion: This preliminary study represents a valuable starting point for a future study employing a larger cohort of patients to develop sensitive and specific protein biomarkers that could reliably differentiate between diabetic and hypertensive causes of CKD to allow for improved diagnosis, fewer biopsy procedures, and refined treatment approaches for clinicians.

Published

2020

8. Proteomic Fingerprint of Lung Fibrosis Progression and Response to Therapy in Bleomycin-Induced Mouse Model

Author

Lucrezia Principi, Erica Ferrini, Roberta Ciccimarra, Lisa Pagani, Clizia Chinello, Paolo Previtali, Andrew Smith, Gino Villetti, Matteo Zoboli, Francesca Ravanetti, Franco Fabio Stellari, Fulvio Magni, and Isabella Piga

Subjects

lung fibrosis, bleomycin mouse model, proteomics, bottom-up mass spectrometry, nintedanib, Coronin-1A, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Idiopathic pulmonary fibrosis (IPF) is a chronic lung disease characterized by the aberrant accumulation of extracellular matrix in the lungs. nintedanib is one of the two FDA-approved drugs for IPF treatment; however, the exact pathophysiological mechanisms of fibrosis progression and response to therapy are still poorly understood. In this work, the molecular fingerprint of fibrosis progression and response to nintedanib treatment have been investigated by mass spectrometry-based bottom-up proteomics in paraffin-embedded lung tissues from bleomycin-induced (BLM) pulmonary fibrosis mice. Our proteomics results unveiled that (i) samples clustered depending on the tissue fibrotic grade (mild, moderate, and severe) and not on the time course after BLM treatment; (ii) the dysregulation of different pathways involved in fibrosis progression such as the complement coagulation cascades, advanced glycation end products (AGEs) and their receptors (RAGEs) signaling, the extracellular matrix-receptor interaction, the regulation of actin cytoskeleton, and ribosomes; (iii) Coronin 1A (Coro1a) as the protein with the highest correlation when evaluating the progression of fibrosis, with an increased expression from mild to severe fibrosis; and (iv) a total of 10 differentially expressed proteins (padj-value ≤ 0.05 and Fold change ≤−1.5 or ≥1.5), whose abundance varied in the base of the severity of fibrosis (mild and moderate), were modulated by the antifibrotic treatment with nintedanib, reverting their trend. Notably, nintedanib significantly restored lactate dehydrogenase B (Ldhb) expression but not lactate dehydrogenase A (Ldha). Notwithstanding the need for further investigations to validate the roles of both Coro1a and Ldhb, our findings provide an extensive proteomic characterization with a strong relationship with histomorphometric measurements. These results unveil some biological processes in pulmonary fibrosis and drug-mediated fibrosis therapy.

Published

2023

9. Plasma Proteomic Variables Related to COVID-19 Severity: An Untargeted nLC-MS/MS Investigation

Author

Lisa Pagani, Clizia Chinello, Giulia Risca, Giulia Capitoli, Lucrezia Criscuolo, Andrea Lombardi, Riccardo Ungaro, Davide Mangioni, Isabella Piga, Antonio Muscatello, Francesco Blasi, Andrea Favalli, Martina Martinovic, Andrea Gori, Alessandra Bandera, Renata Grifantini, and Fulvio Magni

Subjects

COVID-19, proteomics, mass spectrometry, SARS-CoV-2, plasma, blood, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

Severe Acute Respiratory Syndrome Coronavirus-2 (SARS-CoV-2) infection leads to a wide range of clinical manifestations and determines the need for personalized and precision medicine. To better understand the biological determinants of this heterogeneity, we explored the plasma proteome of 43 COVID-19 patients with different outcomes by an untargeted liquid chromatography-mass spectrometry approach. The comparison between asymptomatic or pauci-symptomatic subjects (MILDs), and hospitalised patients in need of oxygen support therapy (SEVEREs) highlighted 29 proteins emerged as differentially expressed: 12 overexpressed in MILDs and 17 in SEVEREs. Moreover, a supervised analysis based on a decision-tree recognised three proteins (Fetuin-A, Ig lambda-2chain-C-region, Vitronectin) that are able to robustly discriminate between the two classes independently from the infection stage. In silico functional annotation of the 29 deregulated proteins pinpointed several functions possibly related to the severity; no pathway was associated exclusively to MILDs, while several only to SEVEREs, and some associated to both MILDs and SEVEREs; SARS-CoV-2 signalling pathway was significantly enriched by proteins up-expressed in SEVEREs (SAA1/2, CRP, HP, LRG1) and in MILDs (GSN, HRG). In conclusion, our analysis could provide key information for ‘proteomically’ defining possible upstream mechanisms and mediators triggering or limiting the domino effect of the immune-related response and characterizing severe exacerbations.

Published

2023

10. A Blood Bank Standardized Production of Human Platelet Lysate for Mesenchymal Stromal Cell Expansion: Proteomic Characterization and Biological Effects

Author

Andrea Bianchetti, Clizia Chinello, Michele Guindani, Simona Braga, Arabella Neva, Rosanna Verardi, Giovanna Piovani, Lisa Pagani, Gina Lisignoli, Fulvio Magni, Domenico Russo, and Camillo Almici

Subjects

mesenchymal stromal cells, human platelet lysate, growth factors, mass spectrometry, blood banks standards, Biology (General), QH301-705.5

Abstract

Human platelet lysate (hPL) is considered a valid substitute to fetal bovine serum (FBS) in the expansion of mesenchymal stromal cells (MSC), and it is commonly produced starting from intermediate side products of whole blood donations. Through freeze–thaw cycles, hPL is highly enriched in chemokines, growth factors, and adhesion and immunologic molecules. Cell therapy protocols, using hPL instead of FBS for the expansion of cells, are approved by regulatory authorities without concerns, and its administration in patients is considered safe. However, published data are fairly difficult to compare, since the production of hPL is highly variable. This study proposes to optimize and standardize the hPL productive process by using instruments, technologies, and quality/safety standards required for blood bank activities and products. The quality and improved selection of the starting material (i.e., the whole blood), together with the improvement of the production process, guarantee a product characterized by higher content and quality of growth factors as well as a reduction in batch-to-batch variability. By increasing the number of freeze/thaw cycles from one (hPL1c) to four (hPL4c), we obtained a favorable effect on the release of growth factors from platelet α granules. Those changes have directly translated into biological effects leading to a decreasing doubling time (DT) of MSC expansion at 7 days (49.41 ± 2.62 vs. 40.61 ± 1.11 h, p < 0.001). Furthermore, mass spectrometry (MS)-based evaluation has shown that the proliferative effects of hPL4c are also combined with a lower batch-to-batch variability (10–15 vs. 21–31%) at the proteomic level. In conclusion, we have considered lot-to-lot hPL variability, and by the strict application of blood bank standards, we have obtained a standardized, reproducible, safe, cheap, and ready-to-use product.

Published

2021

11. Definition of IgG Subclass-Specific Glycopatterns in Idiopathic Membranous Nephropathy: Aberrant IgG Glycoforms in Blood

Author

Clizia Chinello, Noortje de Haan, Giulia Capitoli, Barbara Trezzi, Antonella Radice, Lisa Pagani, Lucrezia Criscuolo, Stefano Signorini, Stefania Galimberti, Renato Alberto Sinico, Manfred Wuhrer, and Fulvio Magni

Subjects

IMN, IgG, LC-MS, N-glycans, glycosylation, galactosylation, Biology (General), QH301-705.5, Chemistry, QD1-999

Abstract

The podocyte injury, and consequent proteinuria, that characterize the pathology of idiopathic membranous nephropathy (IMN) is mediated by an autoimmune reaction against podocyte antigens. In particular, the activation of pathways leading to abundant renal deposits of complement is likely to involve the binding of mannose-binding lectin (MBL) to aberrant glycans on immunoglobulins. To obtain a landscape of circulatory IgG Fc glycosylation characterizing this disease, we conducted a systematic N-glycan profiling study of IgG1, 2, and 4 by mass spectrometry. The cohort included 57 IMN patients, a pathological control group with nephrotic syndrome (PN) (n = 20), and 88 healthy control subjects. The effect of sex and age was assessed in all groups and controlled by rigorous matching. Several IgG Fc glycan traits were found to be associated with IMN. Interestingly, among them, only IgG4-related results were specific for IMN and not for PN. Hypo-galactosylation of IgG4, already shown for IMN, was observed to occur in the absence of core fucose, in line with a probable increase of pro-inflammatory IgG. In addition, elevated levels of fucosylated IgG4, along with low levels of hybrid-type glycans, were detected. Some of these IgG4 alterations are likely to be more pronounced in high PLA2R (phospholipase A2 receptor) patients. IgG Fc glycosylation patterns associated with IMN warrant further studies of their role in disease mechanisms and may eventually enrich the diagnostic spectrum regarding patient stratification.

Published

2022

12. Functional heterogeneity of lymphocytic patterns in primary melanoma dissected through single-cell multiplexing

Author

Francesca Maria Bosisio, Asier Antoranz, Yannick van Herck, Maddalena Maria Bolognesi, Lukas Marcelis, Clizia Chinello, Jasper Wouters, Fulvio Magni, Leonidas Alexopoulos, Marguerite Stas, Veerle Boecxstaens, Oliver Bechter, Giorgio Cattoretti, and Joost van den Oord

Subjects

melanoma, multiplex, tumor-infiltrating lymphocytes, TILs, microenvironment, brisk, Medicine, Science, Biology (General), QH301-705.5

Abstract

In melanoma, the lymphocytic infiltrate is a prognostic parameter classified morphologically into ‘brisk’, ‘non-brisk’ and ‘absent’ entailing a functional association that has never been proved. Recently, it has been shown that lymphocytic populations can be very heterogeneous, and that anti-PD-1 immunotherapy supports activated T cells. Here, we characterize the immune landscape in primary melanoma by high-dimensional single-cell multiplex analysis in tissue sections (MILAN technique) followed by image analysis, RT-PCR and shotgun proteomics. We observed that the brisk and non-brisk patterns are heterogeneous functional categories that can be further sub-classified into active, transitional or exhausted. The classification of primary melanomas based on the functional paradigm also shows correlation with spontaneous regression, and an improved prognostic value when compared to that of the brisk classification. Finally, the main inflammatory cell subpopulations that are present in the microenvironment associated with activation and exhaustion and their spatial relationships are described using neighbourhood analysis.

Published

2020

13. Does the Urinary Proteome Reflect ccRCC Stage and Grade Progression?

Author

Lucia Santorelli, Martina Stella, Clizia Chinello, Giulia Capitoli, Isabella Piga, Andrew Smith, Angelica Grasso, Marco Grasso, Giorgio Bovo, and Fulvio Magni

Subjects

clear cell renal cell carcinoma, proteomics, urine, tumor grade, tumor stage, Medicine (General), R5-920

Abstract

Due its ability to provide a global snapshot of kidney physiology, urine has emerged as a highly promising, non-invasive source in the search for new molecular indicators of disease diagnosis, prognosis, and surveillance. In particular, proteomics represents an ideal strategy for the identification of urinary protein markers; thus, a urinomic approach could also represent a powerful tool in the investigation of the most common kidney cancer, which is clear cell Renal Cell Carcinoma (ccRCC). Currently, these tumors are classified after surgical removal using the TNM and nuclear grading systems and prognosis is usually predicted based upon staging. However, the aggressiveness and clinical outcomes of ccRCC remain heterogeneous within each stratified group, highlighting the need for novel molecular indicators that can predict the progression of these tumors. In our study, we explored the association between the urinary proteome and the ccRCC staging and grading classification. The urine proteome of 44 ccRCC patients with lesions of varying severity was analyzed via label-free proteomics. MS data revealed several proteins with altered abundance according to clinicopathological stratification. Specifically, we determined a panel of dysregulated proteins strictly related to stage and grade, suggesting the potential utility of MS-based urinomics as a complementary tool in the staging process of ccRCC.

Published

2021

14. Lipidomic Typing of Colorectal Cancer Tissue Containing Tumour-Infiltrating Lymphocytes by MALDI Mass Spectrometry Imaging

Author

Vanna Denti, Allia Mahajneh, Giulia Capitoli, Francesca Clerici, Isabella Piga, Lisa Pagani, Clizia Chinello, Maddalena Maria Bolognesi, Giuseppe Paglia, Stefania Galimberti, Fulvio Magni, and Andrew Smith

Subjects

MALDI-MSI, lipidomics, colorectal cancer, lymphocytes, immunity, Microbiology, QR1-502

Abstract

Predicting the prognosis of colorectal cancer (CRC) patients remains challenging and a characterisation of the tumour immune environment represents one of the most crucial avenues when attempting to do so. For this reason, molecular approaches which are capable of classifying the immune environments associated with tumour infiltrating lymphocytes (TILs) are being readily investigated. In this proof of concept study, we aim to explore the feasibility of using spatial lipidomics by MALDI-MSI to distinguish CRC tissue based upon their TIL content. Formalin-fixed paraffin-embedded tissue from human thymus and tonsil was first analysed by MALDI-MSI to obtain a curated mass list from a pool of single positive T lymphocytes, whose putative identities were annotated using an LC-MS-based lipidomic approach. A CRC tissue microarray (TMA, n = 30) was then investigated to determine whether these cases could be distinguished based upon their TIL content in the tumour and its microenvironment. MALDI-MSI from the pool of mature T lymphocytes resulted in the generation of a curated mass list containing 18 annotated m/z features. Initially, subsets of T lymphocytes were then distinguished based on their state of maturation and differentiation in the human thymus and tonsil tissue. Then, when applied to a CRC TMA containing differing amounts of T lymphocyte infiltration, those cases with a high TIL content were distinguishable from those with a lower TIL content, especially within the tumour microenvironment, with three lipid signals being shown to have the greatest impact on this separation (p < 0.05). On the whole, this preliminary study represents a promising starting point and suggests that a lipidomics MALDI-MSI approach could be a promising tool for subtyping the diverse immune environments in CRC.

Published

2021

15. Proteomics and Matrix-Assisted Laser Desorption/Ionization Mass Spectrometry Imaging as a Modern Diagnostic Tool in Kidney Diseases

Author

Mariia Ivanova, Olena Dyadyk, Andrew Smith, Lucia Santorelli, Martina Stella, Manuel Galli, Clizia Chinello, and Fulvio Magni

Subjects

сhronic kidney disease, proteomics, matrix-assisted laser desorption/ionization mass spectrometry imaging, сhronic kidney disease outcome prognosis, predict treatment response, Diseases of the genitourinary system. Urology, RC870-923

Abstract

As a result of the rapid evolution of modern science, we are continually improving our knowledge of disease pathogenesis and morphology on a daily basis. Due to the era of omics sciences, such as genomics, transcriptomics, and proteomics, there is a strong desire to comprehend the molecular mechanisms of diseases and organisms. The final aims would be to perform more successful diagnosis/prognosis, identify potential therapeutic targets, and predict treatment response. Chronic kidney disease (CKD) is a worldwide health problem with a rapidly increasing incidence, with CKD itself encompassing a large subset of diseases. Recently, modern proteomic technologies, such as matrix-assisted laser desorption/ionization mass spectrometry imaging, have been employed in order to study CKD. Notwithstanding the general infancy of these methodologies, there are already an impressive number of studies and publications related to this subject.

Published

2017

16. 3D gelatin-chitosan hybrid hydrogels combined with human platelet lysate highly support human mesenchymal stem cell proliferation and osteogenic differentiation

Author

Federica Re, Luciana Sartore, Vladimira Moulisova, Marco Cantini, Camillo Almici, Andrea Bianchetti, Clizia Chinello, Kamol Dey, Silvia Agnelli, Cristina Manferdini, Simona Bernardi, Nicola F. Lopomo, Emilio Sardini, Elisa Borsani, Luigi F. Rodella, Fabio Savoldi, Corrado Paganelli, Pierangelo Guizzi, Gina Lisignoli, Fulvio Magni, Manuel Salmeron-Sanchez, and Domenico Russo

Subjects

Biochemistry, QD415-436

Abstract

Bone marrow and adipose tissue human mesenchymal stem cells were seeded in highly performing 3D gelatin–chitosan hybrid hydrogels of varying chitosan content in the presence of human platelet lysate and evaluated for their proliferation and osteogenic differentiation. Both bone marrow and adipose tissue human mesenchymal stem cells in gelatin–chitosan hybrid hydrogel 1 (chitosan content 8.1%) or gelatin–chitosan hybrid hydrogel 2 (chitosan 14.9%) showed high levels of viability (80%–90%), and their proliferation and osteogenic differentiation was significantly higher with human platelet lysate compared to fetal bovine serum, particularly in gelatin–chitosan hybrid hydrogel 1. Mineralization was detected early, after 21 days of culture, when human platelet lysate was used in the presence of osteogenic stimuli. Proteomic characterization of human platelet lysate highlighted 59 proteins mainly involved in functions related to cell adhesion, cellular repairing mechanisms, and regulation of cell differentiation. In conclusion, the combination of our gelatin–chitosan hybrid hydrogels with hPL represents a promising strategy for bone regenerative medicine using human mesenchymal stem cells.

Published

2019

17. Urinary Extracellular Vesicles and Salt-Losing Tubulopathies: A Proteomic Approach

Author

Francesca Raimondo, Clizia Chinello, Luigi Porcaro, Fulvio Magni, and Marina Pitto

Subjects

exosomes, extracellular vesicles, Gitelman syndrome, Bartter syndrome, diagonal electrophoresis, Microbiology, QR1-502

Abstract

Renal tubular cells release urinary extracellular vesicles (uEV) that are considered a promising source of molecular markers for renal dysfunction and injury. We investigated uEV proteomes of patients with hereditary salt-losing tubulopathies (SLTs), focusing on those caused by Gitelman and Bartter (BS) syndromes, to provide potential markers for differential diagnosis. Second morning urine was collected from patients with genetically proven SLTs and uEV were isolated by the ultracentrifugation-based protocol. The uEV proteome was run through a diagonal bidimensional electrophoresis (16BAC/SDS-PAGE), to improve hydrophobic protein resolution. Sixteen differential spots from the proteome of two variants (BS2 and BS3) were analysed by nLC-ESI-MS/MS after in-gel tryptic digestion. A total of 167 protein species were identified from 7 BS2 spots and 9 BS3 spot. Most of these proteins were membrane-associated proteins, in particular transmembrane proteins, and were related to typical renal functions. The differential content of some uEV was then validated by immunoblotting. Our work suggests that uEV proteomics represents a promising strategy for the identification of differential SLT proteins. This could play a role in understanding the pathophysiological disease mechanisms and may support the recognition of different syndromes.

Published

2020

18. Proteomic and Bioinformatic Studies for the Characterization of Response to Pemetrexed in Platinum Drug Resistant Ovarian Cancer

Author

Leda Severi, Lorena Losi, Sergio Fonda, Laura Taddia, Gaia Gozzi, Gaetano Marverti, Fulvio Magni, Clizia Chinello, Martina Stella, Jalid Sheouli, Elena I. Braicu, Filippo Genovese, Angela Lauriola, Chiara Marraccini, Alessandra Gualandi, Domenico D'Arca, Stefania Ferrari, and Maria P. Costi

Subjects

pemetrexed, folate pathway, drug resistance, ovarian cancer, proteomics, mass spectrometry, Therapeutics. Pharmacology, RM1-950

Abstract

Proteomics and bioinformatics are a useful combined technology for the characterization of protein expression level and modulation associated with the response to a drug and with its mechanism of action. The folate pathway represents an important target in the anticancer drugs therapy. In the present study, a discovery proteomics approach was applied to tissue samples collected from ovarian cancer patients who relapsed after the first-line carboplatin-based chemotherapy and were treated with pemetrexed (PMX), a known folate pathway targeting drug. The aim of the work is to identify the proteomic profile that can be associated to the response to the PMX treatment in pre-treatement tissue. Statistical metrics of the experimental Mass Spectrometry (MS) data were combined with a knowledge-based approach that included bioinformatics and a literature review through ProteinQuest™ tool, to design a protein set of reference (PSR). The PSR provides feedback for the consistency of MS proteomic data because it includes known validated proteins. A panel of 24 proteins with levels that were significantly different in pre-treatment samples of patients who responded to the therapy vs. the non-responder ones, was identified. The differences of the identified proteins were explained for the patients with different outcomes and the known PMX targets were further validated. The protein panel herein identified is ready for further validation in retrospective clinical trials using a targeted proteomic approach. This study may have a general relevant impact on biomarker application for cancer patients therapy selection.

Published

2018

19. [Untitled]

Author

Paulo Ornellas, Antonio Augusto Ornellas, Clizia Chinello, Erica Gianazza, Veronica Mainini, Marta Cazzaniga, Denise Abreu Pereira, Vanessa Sandim, Ana Sheila Cypriano, Leandro Koifman, Paulo Cesar Barbosa da Silva, Gilda Alves, and Fulvio Magni

Subjects

Penis, Penis Cancer, Carcinoma, Squamous Cell, Plasma, Proteomics, Complement C3b Inactivator Proteins, Diseases of the genitourinary system. Urology, RC870-923

Abstract

PurposeTo investigate the use of ClinProt technique to identify cancer markers in plasma of patients suffering from squamous cell carcinoma of the penis (SCCP).Materials and MethodsPlasma of 36 healthy subjects and 25 patients with penile carcinoma who underwent surgical treatment between June 2010 and June 2011 was collected and analyzed by the ClinProt/MALDI/ToF technique. Then the peptides were identified from the C8 MB eluted fraction of patients' and control subjects' plasma by LIFT MS/MS.ResultsA cluster of 2 peptides (A=m/z 1897.22 ± 9 Da and B=m/z 2021.99 ± 9 Da) was able to discriminate patients from control subjects. Cross validation analysis using the whole casuistic showed 62.5% and 86.76% sensitivity and specificity, respectively. The cluster also showed very high sensitivity (100%) and specificity (97%) for SCCP patients that died due to the disease. Furthermore, patients with lymph node involvement presented sensitivity and specificity of 80% and 97%, respectively. These two peptides were identified by the proteomic approach based on a MALDI-TOF/TOF as fragments of C3 (m/z 1896.17) and C4a/b (m/z 2021.26) complement proteins.ConclusionsThe results showed that as the disease progresses, the fragments C3 and C4 A/B are less expressed in comparison with healthy subjects. These results may be useful as prognostic tools.

Published

2012

20. Downregulation of C3 and C4A/B complement factor fragments in plasma from patients with squamous cell carcinoma of the penis

Author

Paulo Ornellas, Antonio Augusto Ornellas, Clizia Chinello, Erica Gianazza, Veronica Mainini, Marta Cazzaniga, Denise Abreu Pereira, Vanessa Sandim, Ana Sheila Cypriano, Leandro Koifman, Paulo Cesar Barbosa da Silva, Gilda Alves, and Fulvio Magni

Subjects

Penis, Penis Cancer, Carcinoma, Squamous Cell, Plasma, Proteomics, Complement C3b Inactivator Proteins, Diseases of the genitourinary system. Urology, RC870-923

Abstract

Purpose To investigate the use of ClinProt technique to identify cancer markers in plasma of patients suffering from squamous cell carcinoma of the penis (SCCP). Materials and Methods Plasma of 36 healthy subjects and 25 patients with penile carcinoma who underwent surgical treatment between June 2010 and June 2011 was collected and analyzed by the ClinProt/MALDI/ToF technique. Then the peptides were identified from the C8 MB eluted fraction of patients' and control subjects' plasma by LIFT MS/MS. Results A cluster of 2 peptides (A=m/z 1897.22 ± 9 Da and B=m/z 2021.99 ± 9 Da) was able to discriminate patients from control subjects. Cross validation analysis using the whole casuistic showed 62.5% and 86.76% sensitivity and specificity, respectively. The cluster also showed very high sensitivity (100%) and specificity (97%) for SCCP patients that died due to the disease. Furthermore, patients with lymph node involvement presented sensitivity and specificity of 80% and 97%, respectively. These two peptides were identified by the proteomic approach based on a MALDI-TOF/TOF as fragments of C3 (m/z 1896.17) and C4a/b (m/z 2021.26) complement proteins. Conclusions The results showed that as the disease progresses, the fragments C3 and C4 A/B are less expressed in comparison with healthy subjects. These results may be useful as prognostic tools.

Published

2012

21. Urinary signatures of Renal Cell Carcinoma investigated by peptidomic approaches.

Author

Clizia Chinello, Marta Cazzaniga, Gabriele De Sio, Andrew James Smith, Erica Gianazza, Angelica Grasso, Francesco Rocco, Stefano Signorini, Marco Grasso, Silvano Bosari, Italo Zoppis, Mohammed Dakna, Yuri E M van der Burgt, Giancarlo Mauri, and Fulvio Magni

Subjects

Medicine, Science

Abstract

Renal Cell Carcinoma (RCC) is typically asymptomatic and surgery usually increases patient's lifespan only for early stage tumours. Moreover, solid renal masses cannot be confidently differentiated from RCC. Therefore, markers to distinguish malignant kidney tumours and for their detection are needed. Two different peptide signatures were obtained by a MALDI-TOF profiling approach based on urine pre-purification by C8 magnetic beads. One cluster of 12 signals could differentiate malignant tumours (n = 137) from benign renal masses and controls (n = 153) with sensitivity of 76% and specificity of 87% in the validation set. A second cluster of 12 signals distinguished clear cell RCC (n = 118) from controls (n = 137) with sensitivity and specificity values of 84% and 91%, respectively. Most of the peptide signals used in the two models were observed at higher abundance in patient urines and could be identified as fragments of proteins involved in tumour pathogenesis and progression. Among them: the Meprin 1α with a pro-angiogenic activity, the Probable G-protein coupled receptor 162, belonging to the GPCRs family and known to be associated with several key functions in cancer, the Osteopontin that strongly correlates to tumour stages and invasiveness, the Phosphorylase b kinase regulatory subunit alpha and the SeCreted and TransMembrane protein 1.

Published

2014

22. Proteomic investigation of therapy induced senescence in cancer cells by a DIA-PASEF mass spectrometry approach

Author

Pagani, L, Crescenzi, E, Porto, N, Chinello, C, Magni, F, Lisa Pagani, Elvira Crescenzi, Natalia Shelly Porto, Clizia Chinello, Fulvio Magni, Pagani, L, Crescenzi, E, Porto, N, Chinello, C, Magni, F, Lisa Pagani, Elvira Crescenzi, Natalia Shelly Porto, Clizia Chinello, and Fulvio Magni

Published

2024

23. Robust Conclusions in Mass Spectrometry Analysis.

Author

Italo Zoppis, Riccardo Dondi, Massimiliano Borsani, Erica Gianazza, Clizia Chinello, Fulvio Magni, and Giancarlo Mauri

Published

2015

24. Customization of LC-MS-based proteomic workflows for biological studies in the clinical field

Author

Pagani, L, Previtali, P, Chinello, C, Capitoli, G, Risca, G, Radice, A, Sinico, R, Trezzi, B, Lombardi, A, Gori, A, Bandera, A, Grifantini, R, Meregalli, C, Cavaletti, G, Magni, F, Lisa Pagani, Paolo Previtali, Clizia Chinello, Giulia Capitoli, Giulia Risca, Antonella Radice, Renato Alberto Sinico, Barbara Trezzi, Andrea Lombardi, Andrea Gori, Alessandra Bandera, Renata Grifantini, Cristina Meregalli, Guido Cavaletti, Fulvio Magni, Pagani, L, Previtali, P, Chinello, C, Capitoli, G, Risca, G, Radice, A, Sinico, R, Trezzi, B, Lombardi, A, Gori, A, Bandera, A, Grifantini, R, Meregalli, C, Cavaletti, G, Magni, F, Lisa Pagani, Paolo Previtali, Clizia Chinello, Giulia Capitoli, Giulia Risca, Antonella Radice, Renato Alberto Sinico, Barbara Trezzi, Andrea Lombardi, Andrea Gori, Alessandra Bandera, Renata Grifantini, Cristina Meregalli, Guido Cavaletti, and Fulvio Magni

Published

2023

25. DIA-PASEF mass spectrometry as a tailored proteomic approach to explore Idiopathic Membranous Nephropathy

Author

Pagani, L, Previtali, P, Risca, G, Capitoli, G, Bossi, E, Oliveira, G, Piga, I, Radice, A, Trezzi, B, Sinico, R, Magni, F, Chinello, C, Lisa Pagani, Paolo Previtali, Giulia Risca, Giulia Capitoli, Eleonora Bossi, Glenda Oliveira, Isabella Piga, Antonella Radice, Barbara Trezzi, Renato A. Sinico, Fulvio Magni, Clizia Chinello, Pagani, L, Previtali, P, Risca, G, Capitoli, G, Bossi, E, Oliveira, G, Piga, I, Radice, A, Trezzi, B, Sinico, R, Magni, F, Chinello, C, Lisa Pagani, Paolo Previtali, Giulia Risca, Giulia Capitoli, Eleonora Bossi, Glenda Oliveira, Isabella Piga, Antonella Radice, Barbara Trezzi, Renato A. Sinico, Fulvio Magni, and Clizia Chinello

Published

2023

26. Towards the Definition of the Molecular Hallmarks of Idiopathic Membranous Nephropathy in Serum Proteome: A DIA-PASEF Approach

Author

Previtali, P, Pagani, L, Risca, G, Capitoli, G, Bossi, E, Oliveira, G, Piga, I, Radice, A, Trezzi, B, Sinico, R, Magni, F, Chinello, C, Paolo Previtali, Lisa Pagani, Giulia Risca, Giulia Capitoli, Eleonora Bossi, Glenda Oliveira, Isabella Piga, Antonella Radice, Barbara Trezzi, Renato Alberto Sinico, Fulvio Magni, Clizia Chinello, Previtali, P, Pagani, L, Risca, G, Capitoli, G, Bossi, E, Oliveira, G, Piga, I, Radice, A, Trezzi, B, Sinico, R, Magni, F, Chinello, C, Paolo Previtali, Lisa Pagani, Giulia Risca, Giulia Capitoli, Eleonora Bossi, Glenda Oliveira, Isabella Piga, Antonella Radice, Barbara Trezzi, Renato Alberto Sinico, Fulvio Magni, and Clizia Chinello

Abstract

Idiopathic membranous nephropathy (IMN) is a pathologically defined disorder of the glomerulus, primarily responsible for nephrotic syndromes (NS) in nondiabetic adults. The underlying molecular mechanisms are still not completely clarified. To explore possible molecular and functional signatures, an optimised mass spectrometry (MS) method based on next-generation data-independent acquisition combined with ion-mobility was applied to serum of patients affected by IMN (n = 15) or by other glomerulopathies (PN) (n = 15). The statistical comparison highlighted a panel of 57 de-regulated proteins with a significant increase in lipoprotein-related proteins (APOC1, APOB, APOA1, APOL1 and LCAT) and a substantial quantitative alteration of key serpins (including A4, D1, A7, A6, F2, F1 and 1) possibly associated with IMN or NS and podocyte stress. A critical dysregulation in metabolisms of lipids (e.g., VLDL assembly and clearance) likely to be related to known hyperlipidemia in IMN, along with involvement of non-classical complement pathways and a putative enrolment of ficolin-2 in sustaining the activation of the lectin-mediated complement system have been pinpointed. Moreover, mannose receptor CD206 (MRC1-down in IMN) and biotinidase (BTD-up in IMN) are able alone to accurately distinguish IMN vs. PN. To conclude, our work provides key proteomic insights into the IMN complexity, opening the way to an efficient stratification of MN patients.

Published

2023

27. Correction to Spatial Multiomics of Lipids, N-Glycans, and Tryptic Peptides on a Single FFPE Tissue Section

Author

Vanna Denti, Giulia Capitoli, Isabella Piga, Francesca Clerici, Lisa Pagani, Lucrezia Criscuolo, Greta Bindi, Lucrezia Principi, Clizia Chinello, Giuseppe Paglia, Fulvio Magni, and Andrew Smith

Subjects

General Chemistry, Biochemistry

Published

2023

28. Analysis of Correlation Structures in Renal Cell Carcinoma Patient Data.

Author

Italo Zoppis, Massimiliano Borsani, Erica Gianazza, Clizia Chinello, Francesco Rocco, Giancarlo Albo, André M. Deelder, Yuri E. M. van der Burgt, Fulvio Magni, Marco Antoniotti, and Giancarlo Mauri

Published

2012

29. Протеоміка та мас-спектрометрія з матрично-активованою лазерною десорбцією/іонізацією як сучасний діагностичний інструмент при захворюваннях нирок

Author

Lucia Santorelli, Andrew J. Smith, Clizia Chinello, Fulvio Magni, Mariia Ivanova, Martina Stella, Manuel Galli, and Olena O Dyadyk

Subjects

Matrix-assisted laser desorption/ionization, Chromatography, Chemistry, Mass spectrometry imaging

Abstract

Внаслідок швидкого розвитку сучасної науки ми постійно, день у день, удосконалюємо наші знання про патогенез і морфологію захворювань. У зв’язку з настанням ери наукомік, таких як геноміка, транскріптоміка та протеоміка, є велика необхідність у розумінні молекулярних механізмів хвороб і організмів. Кінцевими цілями повинні бути такі: більш успішні діагностика та прогноз, виявлення потенційних терапевтичних мішеней і прогнозування відповіді на лікування. Хронічна хвороба нирок (ХХН) є всесвітньою проблемою охорони здоров’я, що характеризується швидкозростаючою захворюваністю, a сам термін «ХХН» охоплює велику підмножину захворювань. Останнім часом для вивчення ХХН використовуються сучасні технології протеоміки, такі як мас-спектрометрія з матрично-активованою лазерною десорбцією/іонізацією. Незважаючи на ранній етап розвитку подібних методик, уже існує значна кількість досліджень і публікацій, присвячених цій темі.

Published

2021

30. Spatial Multiomics of Lipids, N-Glycans, and Tryptic Peptides on a Single FFPE Tissue Section

Author

Vanna Denti, Giulia Capitoli, Isabella Piga, Francesca Clerici, Lisa Pagani, Lucrezia Criscuolo, Greta Bindi, Lucrezia Principi, Clizia Chinello, Giuseppe Paglia, Fulvio Magni, Andrew Smith, Denti, V, Capitoli, G, Piga, I, Clerici, F, Pagani, L, Criscuolo, L, Bindi, G, Principi, L, Chinello, C, Paglia, G, Magni, F, and Smith, A

Subjects

tumor, Paraffin Embedding, Tissue Fixation, renal cancer, multiomic, General Chemistry, Biochemistry, Lipids, Kidney Neoplasms, N-glycomic, Mice, lipidomic, Polysaccharides, Formaldehyde, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, MALDI-MS imaging, Animals, Humans, spatial proteomic, Peptides, Carcinoma, Renal Cell, proteomic

Abstract

Mass spectrometry imaging (MSI) is an emerging technology that is capable of mapping various biomolecules within their native spatial context, and performing spatial multiomics on formalin-fixed paraffin-embedded (FFPE) tissues may further increase the molecular characterization of pathological states. Here we present a novel workflow which enables the sequential MSI of lipids, N-glycans, and tryptic peptides on a single FFPE tissue section and highlight the enhanced molecular characterization that is offered by combining the multiple spatial omics data sets. In murine brain and clear cell renal cell carcinoma (ccRCC) tissue, the three molecular levels provided complementary information and characterized different histological regions. Moreover, when the spatial omics data was integrated, the different histopathological regions of the ccRCC tissue could be better discriminated with respect to the imaging data set of any single omics class. Taken together, these promising findings demonstrate the capability to more comprehensively map the molecular complexity within pathological tissue.

Published

2022

31. A Mutual Information Approach to Data Integration for Alzheimer's Disease Patients.

Author

Italo Zoppis, Erica Gianazza, Clizia Chinello, Veronica Mainini, Carmen Galbusera, Carlo Ferrarese, Gloria Galimberti, Alessandro Sorbi, Barbara Borroni, Fulvio Magni, and Giancarlo Mauri

Published

2009

32. Reproducing extracellular matrix adverse remodelling of non-ST myocardial infarction in a large animal model

Author

Paolo Contessotto, Renza Spelat, Vaidas Vysockas, Aušra Krivickienė, Chunsheng Jin, Sandrine Chantepie, Clizia Chinello, Audrys G. Pauza, Mindaugas Rackauskas, Vilma Zigmantaitė, Fulvio Magni, Dulce Papy-Garcia, Niclas G. Karlsson, Eglė Ereminienė, Abhay Pandit, and Mark Da Costa

Abstract

The rising incidence of non-ST-segment elevation myocardial infarction (NSTEMI) and associated long-term high mortality constitutes an urgent clinical issue. Unfortunately, the study of possible interventions to treat this pathology lacks a reproducible pre-clinical model. Indeed, currently adopted small and large animal models of MI mimic only full-thickness, ST-segment-elevation (STEMI) infarcts, and hence cater only for investigation into therapeutics and interventions directed at this subset of MI. Thus, we developed an ovine model of NSTEMI by ligating the myocardial muscle at precise intervals parallel to the left anterior descending coronary artery. After validating the presented model both by histology and functional analysis with clinical data, further omics analyses highlighted the distinctive features of post-NSTEMI tissue remodelling. Here, by looking at the transcriptome and proteome-derived pathways emerging at acute (7 days) and late (28 days) post-surgery timepoints, we discovered specific alterations in cardiac post-ischaemic extracellular matrix (ECM). Together with the rise of well-known markers of inflammation and fibrosis, NSTEMI ischaemic regions showed distinctive patterns in the expression of complex N-glycans and glycosaminoglycans in cellular membranes and ECM. Identifying such changes in molecular moieties accessible to infusible and intra-myocardial injectable drugs sheds light on the development of targeted pharmacological solutions to contrast adverse fibrotic remodelling.

Published

2022

33. Definition of IgG subclass-specific glycopatterns in idiopathic membranous nephropathy

Author

Clizia Chinello, Noortje de Haan, Giulia Capitoli, Barbara Trezzi, Antonella Radice, Lisa Pagani, Lucrezia Criscuolo, Stefano Signorini, Stefania Galimberti, Renato Alberto Sinico, Manfred Wuhrer, Fulvio Magni, Chinello, C, de Haan, N, Capitoli, G, Trezzi, B, Radice, A, Pagani, L, Criscuolo, L, Signorini, S, Galimberti, S, Sinico, R, Wuhrer, M, and Magni, F

Subjects

Male, Nephrotic Syndrome, glycosylation, IgG, N-glycans, Kidney, Glomerulonephritis, Membranous, Catalysis, Inorganic Chemistry, Humans, glycoproteomics, Physical and Theoretical Chemistry, Molecular Biology, Spectroscopy, Autoantibodies, Podocytes, IMN, Organic Chemistry, glycoproteomic, General Medicine, Computer Science Applications, LC-MS, Immunoglobulin G, N-glycan, Female, galactosylation

Abstract

The podocyte injury, and consequent proteinuria, that characterize the pathology of idiopathic membranous nephropathy (IMN) is mediated by an autoimmune reaction against podocyte antigens. In particular, the activation of pathways leading to abundant renal deposits of complement is likely to involve the binding of mannose-binding lectin (MBL) to aberrant glycans on immunoglobulins. To obtain a landscape of circulatory IgG Fc glycosylation characterizing this disease, we conducted a systematic N-glycan profiling study of IgG1, 2, and 4 by mass spectrometry. The cohort included 57 IMN patients, a pathological control group with nephrotic syndrome (PN) (n = 20), and 88 healthy control subjects. The effect of sex and age was assessed in all groups and controlled by rigorous matching. Several IgG Fc glycan traits were found to be associated with IMN. Interestingly, among them, only IgG4-related results were specific for IMN and not for PN. Hypo-galactosylation of IgG4, already shown for IMN, was observed to occur in the absence of core fucose, in line with a probable increase of pro-inflammatory IgG. In addition, elevated levels of fucosylated IgG4, along with low levels of hybrid-type glycans, were detected. Some of these IgG4 alterations are likely to be more pronounced in high PLA2R (phospholipase A2 receptor) patients. IgG Fc glycosylation patterns associated with IMN warrant further studies of their role in disease mechanisms and may eventually enrich the diagnostic spectrum regarding patient stratification.

Published

2022

34. Plasma proteome investigation of COVID-19 patients with different outcomes through an untargeted label-free LC-MS/MS approach.

Author

Pagani, L, Chinello, C, Mahajneh, A, Clerici, F, Criscuolo, L, Favalli, A, Gruarin, P, Grifantini, R, Bandera, A, Lombardi, A, Ungaro, R, Muscatello, A, Blasi, F, Gori and Fulvio Magni, A, Lisa Pagani, Clizia Chinello, Allia Mahajneh, Francesca Clerici, Lucrezia Criscuolo, Andrea Favalli, Paola Gruarin, Renata Grifantini, Alessandra Bandera, Andrea Lombardi, Riccardo Ungaro, Antonio Muscatello, Francesco Blasi, Andrea Gori and Fulvio Magni, Pagani, L, Chinello, C, Mahajneh, A, Clerici, F, Criscuolo, L, Favalli, A, Gruarin, P, Grifantini, R, Bandera, A, Lombardi, A, Ungaro, R, Muscatello, A, Blasi, F, Gori and Fulvio Magni, A, Lisa Pagani, Clizia Chinello, Allia Mahajneh, Francesca Clerici, Lucrezia Criscuolo, Andrea Favalli, Paola Gruarin, Renata Grifantini, Alessandra Bandera, Andrea Lombardi, Riccardo Ungaro, Antonio Muscatello, Francesco Blasi, and Andrea Gori and Fulvio Magni

Published

2022

35. Generation of a spectral library for DIA proteomics analysis and application to serum samples using TIMS-TOF MS/MS

Author

Pagani, L, Chinello, C, Piga, I, Previtali, P, Principi, L, Bindi, G, Piazza and Fulvio Magni, M, Lisa Pagani, Clizia Chinello, Isabella Piga, Paolo Previtali, Lucrezia Principi, Greta Bindi, Martin Piazza and Fulvio Magni, Pagani, L, Chinello, C, Piga, I, Previtali, P, Principi, L, Bindi, G, Piazza and Fulvio Magni, M, Lisa Pagani, Clizia Chinello, Isabella Piga, Paolo Previtali, Lucrezia Principi, Greta Bindi, and Martin Piazza and Fulvio Magni

Published

2022

36. Plasma proteome investigation of COVID-19 patients with different outcomes through an untargeted label-free LC-MS/MS approach

Author

Lisa Pagani, Clizia Chinello, Allia Mahajneh, Francesca Clerici, Lucrezia Criscuolo, Andrea Favalli, Paola Gruarin, Renata Grifantini, Alessandra Bandera, Andrea Lombardi, Riccardo Ungaro, Antonio Muscatello, Francesco Blasi, Andrea Gori and Fulvio Magni, Pagani, L, Chinello, C, Mahajneh, A, Clerici, F, Criscuolo, L, Favalli, A, Gruarin, P, Grifantini, R, Bandera, A, Lombardi, A, Ungaro, R, Muscatello, A, Blasi, F, and Gori and Fulvio Magni, A

Subjects

COVID-19, Mass spectrometry, Proteomics

Published

2022

37. Generation of a spectral library for DIA proteomics analysis and application to serum samples using TIMS-TOF MS/MS

Author

Lisa Pagani, Clizia Chinello, Isabella Piga, Paolo Previtali, Lucrezia Principi, Greta Bindi, Martin Piazza and Fulvio Magni, Pagani, L, Chinello, C, Piga, I, Previtali, P, Principi, L, Bindi, G, and Piazza and Fulvio Magni, M

Subjects

Mass spectrometry, DIA, proteomics, biofluids

Published

2022

38. Serum Mass Spectrometry Proteomics and Protein Set Identification in Response to FOLFOX-4 in Drug-Resistant Ovarian Carcinoma

Author

Domenico D’Arca, Leda Severi, Stefania Ferrari, Luca Dozza, Gaetano Marverti, Fulvio Magni, Clizia Chinello, Lisa Pagani, Lorenzo Tagliazucchi, Marco Villani, Gianluca d’Addese, Isabella Piga, Vincenza Conteduca, Lorena Rossi, Giorgia Gurioli, Ugo De Giorgi, Lorena Losi, Maria Paola Costi, D'Arca, D, Severi, L, Ferrari, S, Dozza, L, Marverti, G, Magni, F, Chinello, C, Pagani, L, Tagliazucchi, L, Villani, M, D'Addese, G, Piga, I, Conteduca, V, Rossi, L, Gurioli, G, De Giorgi, U, Losi, L, and Costi, M

Subjects

Cancer Research, ovarian cancer, FOLFOX-4, time lapse detection, Oncology, protein panel, mass spectrometry proteomic, network enrichment analysi, mass spectrometry proteomics, serum samples, network enrichment analysis, cancer molecular pathways, cancer molecular pathway, serum sample

Abstract

Ovarian cancer is a highly lethal gynecological malignancy. Drug resistance rapidly occurs, and different therapeutic approaches are needed. So far, no biomarkers have been discovered to predict early response to therapies in the case of multi-treated ovarian cancer patients. The aim of our investigation was to identify a protein panel and the molecular pathways involved in chemotherapy response through a combination of studying proteomics and network enrichment analysis by considering a subset of samples from a clinical setting. Differential mass spectrometry studies were performed on 14 serum samples from patients with heavily pretreated platinum-resistant ovarian cancer who received the FOLFOX-4 regimen as a salvage therapy. The serum was analyzed at baseline time (T0) before FOLFOX-4 treatment, and before the second cycle of treatment (T1), with the aim of understanding if it was possible, after a first treatment cycle, to detect significant proteome changes that could be associated with patients responses to therapy. A total of 291 shared expressed proteins was identified and 12 proteins were finally selected between patients who attained partial response or no-response to chemotherapy when both response to therapy and time dependence (T0, T1) were considered in the statistical analysis. The protein panel included APOL1, GSN, GFI1, LCATL, MNA, LYVE1, ROR1, SHBG, SOD3, TEC, VPS18, and ZNF573. Using a bioinformatics network enrichment approach and metanalysis study, relationships between serum and cellular proteins were identified. An analysis of protein networks was conducted and identified at least three biological processes with functional and therapeutic significance in ovarian cancer, including lipoproteins metabolic process, structural component modulation in relation to cellular apoptosis and autophagy, and cellular oxidative stress response. Five proteins were almost independent from the network (LYVE1, ROR1, TEC, GFI1, and ZNF573). All proteins were associated with response to drug-resistant ovarian cancer resistant and were mechanistically connected to the pathways associated with cancer arrest. These results can be the basis for extending a biomarker discovery process to a clinical trial, as an early predictive tool of chemo-response to FOLFOX-4 of heavily treated ovarian cancer patients and for supporting the oncologist to continue or to interrupt the therapy.

Published

2023

39. Lipidomic Typing of Colorectal Cancer Tissue Containing Tumour-Infiltrating Lymphocytes by MALDI Mass Spectrometry Imaging

Author

Maddalena Maria Bolognesi, Francesca Clerici, Giulia Capitoli, Allia Mahajneh, Lisa Pagani, Clizia Chinello, Giuseppe Paglia, Isabella Piga, Andrew Smith, Fulvio Magni, Vanna Denti, Stefania Galimberti, Denti, V, Mahajneh, A, Capitoli, G, Clerici, F, Piga, I, Pagani, L, Chinello, C, Bolognesi, M, Paglia, G, Galimberti, S, Magni, F, and Smith, A

Subjects

lymphocytes, Colorectal cancer, Endocrinology, Diabetes and Metabolism, colorectal cancer, Biology, Biochemistry, Microbiology, Mass spectrometry imaging, Immune system, Lipidomics, medicine, MALDI-MSI, Molecular Biology, Tissue microarray, Communication, Lipidomic, T lymphocyte, medicine.disease, immunity, Subtyping, QR1-502, digestive system diseases, medicine.anatomical_structure, Tonsil, Cancer research, lipidomics, Lymphocyte

Abstract

Predicting the prognosis of colorectal cancer (CRC) patients remains challenging and a characterisation of the tumour immune environment represents one of the most crucial avenues when attempting to do so. For this reason, molecular approaches which are capable of classifying the immune environments associated with tumour infiltrating lymphocytes (TILs) are being readily investigated. In this proof of concept study, we aim to explore the feasibility of using spatial lipidomics by MALDI-MSI to distinguish CRC tissue based upon their TIL content. Formalin-fixed paraffin-embedded tissue from human thymus and tonsil was first analysed by MALDI-MSI to obtain a curated mass list from a pool of single positive T lymphocytes, whose putative identities were annotated using an LC-MS-based lipidomic approach. A CRC tissue microarray (TMA, n = 30) was then investigated to determine whether these cases could be distinguished based upon their TIL content in the tumour and its microenvironment. MALDI-MSI from the pool of mature T lymphocytes resulted in the generation of a curated mass list containing 18 annotated m/z features. Initially, subsets of T lymphocytes were then distinguished based on their state of maturation and differentiation in the human thymus and tonsil tissue. Then, when applied to a CRC TMA containing differing amounts of T lymphocyte infiltration, those cases with a high TIL content were distinguishable from those with a lower TIL content, especially within the tumour microenvironment, with three lipid signals being shown to have the greatest impact on this separation (p < 0.05). On the whole, this preliminary study represents a promising starting point and suggests that a lipidomics MALDI-MSI approach could be a promising tool for subtyping the diverse immune environments in CRC.

Published

2021

40. Elaboration Pipeline for the Management of MALDI-MS Imaging Datasets

Author

Andrew, Smith, Isabella, Piga, Vanna, Denti, Clizia, Chinello, and Fulvio, Magni

Subjects

Diagnostic Imaging, Proteomics, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Data Mining

Abstract

Matrix-assisted laser desorption/ionization (MALDI)-time of flight (TOF)-mass spectrometry imaging (MSI) enables the spatial localization of proteins to be mapped directly on tissue sections, simultaneously detecting hundreds in a single analysis. However, the large data size, as well as the complexity of MALDI-MSI proteomics datasets, requires the appropriate tools and statistical approaches in order to reduce the complexity and mine the dataset in a successful manner. Here, a pipeline for the management of MALDI-MSI data is described, starting with preprocessing of the raw data, followed by statistical analysis using both supervised and unsupervised statistical approaches and, finally, annotation of those discriminatory protein signals highlighted by the data mining procedure.

Published

2021

41. Proteomics of liquid biopsies: Depicting RCC infiltration into the renal vein by MS analysis of urine and plasma

Author

Clizia Chinello, Vanna Denti, Marta Varallo, Andrew Smith, Marco Grasso, Isabella Piga, Martina Stella, Fulvio Magni, Marina Del Puppo, Mariia Ivanova, Angelica Grasso, Giorgio Bovo, Apostolos Zaravinos, Chinello, C, Stella, M, Piga, I, Smith, A, Bovo, G, Varallo, M, Ivanova, M, Denti, V, Grasso, M, Grasso, A, Del Puppo, M, Zaravinos, A, and Magni, F

Subjects

Proteomics, 0301 basic medicine, Pathology, medicine.medical_specialty, Proteome, Urinary system, Biophysics, Renal vein invasion, Urine, Biochemistry, Renal Veins, Plasma, 03 medical and health sciences, Tandem Mass Spectrometry, Renal cell carcinoma, Biomarkers, Tumor, medicine, Humans, Neoplasm Invasiveness, Carcinoma, Renal Cell, Kidney, Mass spectrometry, 030102 biochemistry & molecular biology, business.industry, Liquid Biopsy, Proteomic, medicine.disease, Kidney Neoplasms, 030104 developmental biology, medicine.anatomical_structure, Biophysic, Renal vein, business, Infiltration (medical), Chromatography, Liquid

Abstract

Liquid biopsies, as blood and urine, could offer an invaluable, easily accessible source of biomarkers, and evidences for elucidating the pathological processes. Only few studies integrated the proteomes driven by more than one biofluid. Furthermore, it is not clear which biofluid better mirrors the alterations triggered by disease. Venous infiltrating RCC(Renal Cell Carcinoma) could represent an advantageous model for exploring this aspect. Herein, we investigate how blood and urine “proteomically” reflect the changes occurring during RCC infiltration into renal vein(RV) by label-free nLC-ESI-MS/MS. We found 574 and 58 differentially expressed proteins(DEPs) in response to vascular involvement. To the augment of vascular involvement, the abundance of only three proteins in urine(UROM,RALA,CNDP1) and two in plasma(APOA1,K2C1) diminished while increased for twenty-six urinary proteins. 80 proteins were found both in urine and plasma, among which twenty-eight were DEPs. A huge overlap between the two biofluids was highlighted, as expected, being urine the filtrate of blood. However, this consistency decreases when RV-occlusion occurs suggesting alternative protein releases, and a loss of kidney architecture. Moreover, several proteomic and functional signatures were biofluid-specific. In conclusion, the complementarity between the specimens allowed to achieve a deeper level of molecular complexity of the RCC venous infiltration. Significance: Although plasma and urine are strongly interconnected, only few proteomic studies investigated the complementarity of these fluids as bio-sources of information. Moreover, none of them was focused to their analysis and comparison in the context of vascular infiltration of renal cancer. Herein, new insights were gained regarding the impact into urinary and plasma proteome of the changes triggered by the ccRCC invasion into vascular system and renal vein. Furthermore, the integration of the information driven by the two liquid biopsies permits to unravel biological processes otherwise lost.

Published

2019

42. A Blood Bank Standardized Production of Human Platelet Lysate for Mesenchymal Stromal Cell Expansion: Proteomic Characterization and Biological Effects

Author

Michele Guindani, Camillo Almici, Rosanna Verardi, Andrea Bianchetti, Simona Braga, Giovanna Piovani, Fulvio Magni, Gina Lisignoli, Arabella Neva, Clizia Chinello, Domenico Russo, Lisa Pagani, Bianchetti, A, Chinello, C, Guindani, M, Braga, S, Neva, A, Verardi, R, Piovani, G, Pagani, L, Lisignoli, G, Magni, F, Russo, D, and Almici, C

Subjects

0301 basic medicine, Chemokine, Stromal cell, QH301-705.5, human platelet lysate, blood banks standards, 030204 cardiovascular system & hematology, growth factors, mass spectrometry, mesenchymal stromal cells, Cell therapy, Andrology, Cell and Developmental Biology, 03 medical and health sciences, 0302 clinical medicine, Methods, Doubling time, Platelet, Biology (General), Whole blood, biology, Chemistry, Mesenchymal stem cell, growth factor, Cell Biology, 030104 developmental biology, mesenchymal stromal cell, blood banks standard, biology.protein, Fetal bovine serum, Developmental Biology

Abstract

Human platelet lysate (hPL) is considered a valid substitute to fetal bovine serum (FBS) in the expansion of mesenchymal stromal cells (MSC), and it is commonly produced starting from intermediate side products of whole blood donations. Through freeze–thaw cycles, hPL is highly enriched in chemokines, growth factors, and adhesion and immunologic molecules. Cell therapy protocols, using hPL instead of FBS for the expansion of cells, are approved by regulatory authorities without concerns, and its administration in patients is considered safe. However, published data are fairly difficult to compare, since the production of hPL is highly variable. This study proposes to optimize and standardize the hPL productive process by using instruments, technologies, and quality/safety standards required for blood bank activities and products. The quality and improved selection of the starting material (i.e., the whole blood), together with the improvement of the production process, guarantee a product characterized by higher content and quality of growth factors as well as a reduction in batch-to-batch variability. By increasing the number of freeze/thaw cycles from one (hPL1c) to four (hPL4c), we obtained a favorable effect on the release of growth factors from platelet α granules. Those changes have directly translated into biological effects leading to a decreasing doubling time (DT) of MSC expansion at 7 days (49.41 ± 2.62 vs. 40.61 ± 1.11 h, p < 0.001). Furthermore, mass spectrometry (MS)-based evaluation has shown that the proliferative effects of hPL4c are also combined with a lower batch-to-batch variability (10–15 vs. 21–31%) at the proteomic level. In conclusion, we have considered lot-to-lot hPL variability, and by the strict application of blood bank standards, we have obtained a standardized, reproducible, safe, cheap, and ready-to-use product.

Published

2021

43. Elastin-like recombinamers-based hydrogel modulates post-ischemic remodeling in a non-transmural myocardial infarction in sheep

Author

Michelle Kilcoyne, Sandrine Chantepie, José Carlos Rodríguez-Cabello, Peter Dockery, Clizia Chinello, John Newell, Doriana Orbanic, Mark Da Costa, Niclas G. Karlsson, Paolo Contessotto, Abhay Pandit, Fulvio Magni, Chunsheng Jin, Dulce Papy-Garcia, and Peter Owens

Subjects

Proteomics, 0301 basic medicine, Pathology, medicine.medical_specialty, Stromal cell, Angiogenesis, Myocardial Infarction, 030204 cardiovascular system & hematology, Extracellular matrix, 03 medical and health sciences, 0302 clinical medicine, Fibrosis, Animals, Medicine, Myocardial infarction, Sheep, Ventricular Remodeling, biology, business.industry, Myocardium, Cardiac muscle, Hydrogels, General Medicine, medicine.disease, Elastin, Endothelial stem cell, 030104 developmental biology, medicine.anatomical_structure, biology.protein, business

Abstract

Ischemic heart disease is a leading cause of mortality due to irreversible damage to cardiac muscle. Inspired by the post-ischemic microenvironment, we devised an extracellular matrix (ECM)-mimicking hydrogel using catalyst-free click chemistry covalent bonding between two elastin-like recombinamers (ELRs). The resulting customized hydrogel included functional domains for cell adhesion and protease cleavage sites, sensitive to cleavage by matrix metalloproteases overexpressed after myocardial infarction (MI). The scaffold permitted stromal cell invasion and endothelial cell sprouting in vitro. The incidence of non-transmural infarcts has increased clinically over the past decade, and there is currently no treatment preventing further functional deterioration in the infarcted areas. Here, we have developed a clinically relevant ovine model of non-transmural infarcts induced by multiple suture ligations. Intramyocardial injections of the degradable ELRs-hydrogel led to complete functional recovery of ejection fraction 21 days after the intervention. We observed less fibrosis and more angiogenesis in the ELRs-hydrogel-treated ischemic core region compared to the untreated animals, as validated by the expression, proteomic, glycomic, and histological analyses. These findings were accompanied by enhanced preservation of GATA4+ cardiomyocytes in the border zone of the infarct. We propose that our customized ECM favors cardiomyocyte preservation in the border zone by modulating the ischemic core and a marked functional recovery. The functional benefits obtained by the timely injection of the ELRs-hydrogel in a clinically relevant MI model support the potential utility of this treatment for further clinical translation.

Published

2021

44. Elaboration Pipeline for the Management of MALDI-MS Imaging Datasets

Author

Vanna Denti, Clizia Chinello, Fulvio Magni, Andrew Smith, and Isabella Piga

Subjects

Data processing, Maldi ms, Computer science, business.industry, Pipeline (computing), Pattern recognition, Proteomics, Annotation, ComputingMethodologies_PATTERNRECOGNITION, Preprocessor, Statistical analysis, Artificial intelligence, Raw data, business

Abstract

Matrix-assisted laser desorption/ionization (MALDI)-time of flight (TOF)-mass spectrometry imaging (MSI) enables the spatial localization of proteins to be mapped directly on tissue sections, simultaneously detecting hundreds in a single analysis. However, the large data size, as well as the complexity of MALDI-MSI proteomics datasets, requires the appropriate tools and statistical approaches in order to reduce the complexity and mine the dataset in a successful manner. Here, a pipeline for the management of MALDI-MSI data is described, starting with preprocessing of the raw data, followed by statistical analysis using both supervised and unsupervised statistical approaches and, finally, annotation of those discriminatory protein signals highlighted by the data mining procedure.

Published

2021

45. Synthesis and automated fluorine-18 radiolabeling of new PSMA-617 derivatives with a CuAAC radiosynthetic approach

Author

Marco N. Iannone, Stefano Stucchi, Elia A. Turolla, Chiara Beretta, Samuele Ciceri, Clizia Chinello, Lisa Pagani, Sergio Todde, Patrizia Ferraboschi, Iannone, M, Stucchi, S, Turolla, E, Beretta, C, Ciceri, S, Chinello, C, Pagani, L, Todde, S, and Ferraboschi, P

Subjects

Male, Fluorine Radioisotopes, PSMA ligand, urologic and male genital diseases, Biochemistry, Analytical Chemistry, Heterocyclic Compounds, 1-Ring, Cell Line, Tumor, Drug Discovery, Humans, Radiology, Nuclear Medicine and imaging, PETPSM, Spectroscopy, automation, Organic Chemistry, click-chemistry, 3-triazole, CuAAC, PSMA ligands, PSMA-617, prostate cancer, Prostatic Neoplasms, Dipeptides, Prostate-Specific Antigen, Radiopharmaceuticals, 1,2,3-triazole

Abstract

In the last decade, the development of new radiopharmaceuticals for the imaging and therapy of prostate cancer has been a highly active and important area of research, especially focusing on the prostate-specific membrane antigen (PSMA), an antigen which is upregulated in prostate, as well as in other tumor cells. A large variety of PSMA ligands have been radiolabeled, to date. Among the various derivatives, PSMA-617 resulted to be one of the most interesting in terms of interaction with the antigen and clinical properties, and its lutetium-177 labeled version has recently been approved by regulatory agencies for therapeutic purposes. For this reasons, the radiolabeling with fluorine-18 of a PSMA-617 derivative might be of interest. Beside other methodologies to radiolabel macromolecules with fluorine-18, the "click-chemistry" approach resulted to be very useful, and the copper-catalyzed azide-alkyne cycloaddition (CuAAC) is considered one of most efficient and reliable. This paper proposes the synthesis of a suitable precursor for the radiolabeling with fluorine-18 of a new PSMA-617 derivative. The whole radiosynthetic procedure has been fully automated, and the final product, which proved to be stable in plasma, has been obtained with radiochemical yield and purity suitable for subsequent preclinical studies.

Published

2021

46. Spatial lipidomics of tumour-infiltrating lymphocytes for the typing of colorectal cancer by MALDI mass spectrometry imaging

Author

Vanna Denti, Allia Mahajneh, Giulia Capitoli, Francesca Clerici, Isabella Piga, Lisa Pagani, Clizia Chinello, Maddalena Maria Bolognesi, Giuseppe Paglia, Stefania Galimberti, Fulvio Magni, Andrew Smith, Denti, V, Mahajneh, A, Capitoli, G, Clerici, F, Piga, I, Pagani, L, Chinello, C, Bolognesi, M, Paglia, G, Galimberti, S, Magni, F, and Smith, A

Subjects

Lipidomics, tumour-infiltrating lymphocytes, MALDI-MSI

Published

2021

47. Untargeted mass spectrometry approach to study SARS-CoV-2 proteins and characterize human plasma and saliva proteome in COVID-19 patients

Author

Lisa Pagani, Clizia Chinello, Allia Mahajneh, Francesca Clerici, Gaia Panarello, Andrea Favalli, Paola Gruarin, Renata Grifantini, Alessandra Bandera, Riccardo Ungaro, Antonio Muscatello, Francesco Blasi, Andrea Gori, Fulvio Magni, Pagani, L, Chinello, C, Mahajneh, A, Clerici, F, Panarello, G, Favalli, A, Gruarin, P, Grifantini, R, Bandera, A, Ungaro, R, Muscatello, A, Blasi, F, Gori, A, and Magni, F

Subjects

mass spectrometry, proteomics, COVID-19, plasma, saliva

Published

2021

48. Untargeted mass spectrometry approach to study SARS-CoV-2 proteins and characterize human plasma and saliva proteome in COVID-19 patients.

Author

Pagani, L, Chinello, C, Mahajneh, A, Clerici, F, Panarello, G, Favalli, A, Gruarin, P, Grifantini, R, Bandera, A, Ungaro, R, Muscatello, A, Blasi, F, Gori, A, Magni, F, Lisa Pagani, Clizia Chinello, Allia Mahajneh, Francesca Clerici, Gaia Panarello, Andrea Favalli, Paola Gruarin, Renata Grifantini, Alessandra Bandera, Riccardo Ungaro, Antonio Muscatello, Francesco Blasi, Andrea Gori, Fulvio Magni, Pagani, L, Chinello, C, Mahajneh, A, Clerici, F, Panarello, G, Favalli, A, Gruarin, P, Grifantini, R, Bandera, A, Ungaro, R, Muscatello, A, Blasi, F, Gori, A, Magni, F, Lisa Pagani, Clizia Chinello, Allia Mahajneh, Francesca Clerici, Gaia Panarello, Andrea Favalli, Paola Gruarin, Renata Grifantini, Alessandra Bandera, Riccardo Ungaro, Antonio Muscatello, Francesco Blasi, Andrea Gori, and Fulvio Magni

Published

2021

49. Spatial lipidomics of tumour-infiltrating lymphocytes for the typing of colorectal cancer by MALDI mass spectrometry imaging

Author

Denti, V, Mahajneh, A, Capitoli, G, Clerici, F, Piga, I, Pagani, L, Chinello, C, Bolognesi, M, Paglia, G, Galimberti, S, Magni, F, Smith, A, Vanna Denti, Allia Mahajneh, Giulia Capitoli, Francesca Clerici, Isabella Piga, Lisa Pagani, Clizia Chinello, Maddalena Maria Bolognesi, Giuseppe Paglia, Stefania Galimberti, Fulvio Magni, Andrew Smith, Denti, V, Mahajneh, A, Capitoli, G, Clerici, F, Piga, I, Pagani, L, Chinello, C, Bolognesi, M, Paglia, G, Galimberti, S, Magni, F, Smith, A, Vanna Denti, Allia Mahajneh, Giulia Capitoli, Francesca Clerici, Isabella Piga, Lisa Pagani, Clizia Chinello, Maddalena Maria Bolognesi, Giuseppe Paglia, Stefania Galimberti, Fulvio Magni, and Andrew Smith

Published

2021

50. Metabolic reprogramming and membrane glycan remodeling as potential drivers of zebrafish heart regeneration

Author

Renza Spelat, Federico Ferro, Paolo Contessotto, Amal Aljaabary, Sergio Martin-Saldaña, Chunsheng Jin, Niclas G. Karlsson, Maura Grealy, Markus M. Hilscher, Fulvio Magni, Clizia Chinello, Michelle Kilcoyne, and Abhay Pandit

Subjects

Mammals, Proteomics, Myocytes, Animals, Glycolysis, Myocytes, Cardiac, Zebrafish, Medicine (miscellaneous), General Agricultural and Biological Sciences, Cardiac, General Biochemistry, Genetics and Molecular Biology

Abstract

The ability of the zebrafish heart to regenerate following injury makes it a valuable model to deduce why this capability in mammals is limited to early neonatal stages. Although metabolic reprogramming and glycosylation remodeling have emerged as key aspects in many biological processes, how they may trigger a cardiac regenerative response in zebrafish is still a crucial question. Here, by using an up-to-date panel of transcriptomic, proteomic and glycomic approaches, we identify a metabolic switch from mitochondrial oxidative phosphorylation to glycolysis associated with membrane glycosylation remodeling during heart regeneration. Importantly, we establish the N- and O-linked glycan structural repertoire of the regenerating zebrafish heart, and link alterations in both sialylation and high mannose structures across the phases of regeneration. Our results show that metabolic reprogramming and glycan structural remodeling are potential drivers of tissue regeneration after cardiac injury, providing the biological rationale to develop novel therapeutics to elicit heart regeneration in mammals.

Published

2020