Your search keyword '"Torretta E"' showing total 106 results

1. Endoparasites of the European hare (Lepus europaeus) (Pallas, 1778) in central Italy

Author

Sergi V., Romeo G., Serafini M., Torretta E., and Macchioni F.

Subjects

brown hare, necroscopical analysis, coprological analysis, host-parasite, Microbiology, QR1-502

Abstract

Brown hare (Lepus europaeus) populations in Europe have declined through decades due to several, but not clear yet, factors. Parasite infections and diseases are some of the causes that directly affected the survival and breeding rates of animal population.

Published

2018

2. Same landscape, different connectivity: contrasting patterns of gene flow in two sympatric ungulates in a mountain area

Author

Lecis, R, Chirichella, R, Dondina, O, Orioli, V, Azzu, S, Canu, A, Torretta, E, Bani, L, Apollonio, M, Scandura, M, Lecis, Roberta, Chirichella, Roberta, Dondina, Olivia, Orioli, Valerio, Azzu, Silvia, Canu, Antonio, Torretta, Elisa, Bani, Luciano, Apollonio, Marco, Scandura, Massimo, Lecis, R, Chirichella, R, Dondina, O, Orioli, V, Azzu, S, Canu, A, Torretta, E, Bani, L, Apollonio, M, Scandura, M, Lecis, Roberta, Chirichella, Roberta, Dondina, Olivia, Orioli, Valerio, Azzu, Silvia, Canu, Antonio, Torretta, Elisa, Bani, Luciano, Apollonio, Marco, and Scandura, Massimo

Abstract

Comparative landscape genetics studies provide insights on the impact of landscape elements on gene flow patterns of different species inhabiting the same geographic area. We investigated the population genetic structure of two sympatric ungulates, roe deer Capreolus capreolus and Northern chamois Rupicapra rupicapra, in a mountain area of the central Italian Alps (Trentino, northern Italy). A total of 122 chamois and 72 roe deer samples were genotyped by two species-specific panels of 11 polymorphic microsatellite loci and analyzed by aspatial and spatially explicit analyses. While the roe deer population resulted unstructured, a clear population structure was detected in chamois, with two main groups, one inhabiting the eastern and the other spread in the western part of the study area. Landscape genetics analysis confirmed these scenarios and revealed a different effect of landscape on gene flow. An IBD (Isolation-By-Distance) model best explained genetic variation in roe deer, while IBR (Isolation-By-Resistance) was found as the process underlying genetic variation patterns in chamois, suggesting arable lands, coniferous forests, watercourses, and main roads as potential barriers. Species distribution and landscape use might explain these results: roe deer mostly occupy valley floors relatively connected to each other, and their spatial behavior may promote gene flow across areas. On the other hand, chamois prefer higher elevations and their movements may be hindered by valleys, rivers, and road networks. This study highlights the different impacts of natural and anthropic landscape elements on gene flow in two sympatric species, resulting from their different ecological requirements.

Published

2024

3. Hide-and-Seek in a Highly Human-Dominated Landscape: Insights into Movement Patterns and Selection of Resting Sites of Rehabilitated Wolves (Canis lupus) in Northern Italy

Author

Torretta, E, Corradini, A, Pedrotti, L, Bani, L, Bisi, F, Dondina, O, Torretta E., Corradini A., Pedrotti L., Bani L., Bisi F., Dondina O., Torretta, E, Corradini, A, Pedrotti, L, Bani, L, Bisi, F, Dondina, O, Torretta E., Corradini A., Pedrotti L., Bani L., Bisi F., and Dondina O.

Abstract

Assessing the behavioural responses of floating wolves to human presence is crucial for investigating the chance of wolf populations expanding into urbanised landscapes. We studied the movement ecology of three rehabilitated wolves in a highly human-dominated landscape (Po Plain, Italy) to explore wolf’s plasticity amid widespread human pressure. To reach this aim, we estimated individual 95% utilisation distributions (UD) after the release and inspected both 95% UDs and net squared displacements to identify individual movement patterns; tested for differences in movement patterns during day and night; and analysed the selection of resting sites during dispersal movement in a highly human-altered environment. Both the 95% UDs and step lengths were smaller for wolves settling in suitable areas than for those settling in more urbanised areas. All wolves exhibited strong temporal segregation with humans during all movement phases, particularly while dispersing across highly urbanised areas. Main roads and proximity to built-up areas were shown to limit wolves’ dispersal, whereas small-wooded patches that provide shelter during rest facilitated long-distance movements. This study provides important insights into wolf movement and settling in urban and peri-urban areas, providing critical knowledge to promote human–carnivore coexistence.

Published

2023

4. Skeletal muscle proteomic profile revealed gender-related metabolic responses in a diet-induced obesity animal model

Author

Moriggi, M, Belloli, S, Barbacini, P, Murtaj, V, Torretta, E, Chaabane, L, Canu, T, Penati, S, Malosio, M, Esposito, A, Gelfi, C, Moresco, R, Capitanio, D, Moriggi M., Belloli S., Barbacini P., Murtaj V., Torretta E., Chaabane L., Canu T., Penati S., Malosio M. L., Esposito A., Gelfi C., Moresco R. M., Capitanio D., Moriggi, M, Belloli, S, Barbacini, P, Murtaj, V, Torretta, E, Chaabane, L, Canu, T, Penati, S, Malosio, M, Esposito, A, Gelfi, C, Moresco, R, Capitanio, D, Moriggi M., Belloli S., Barbacini P., Murtaj V., Torretta E., Chaabane L., Canu T., Penati S., Malosio M. L., Esposito A., Gelfi C., Moresco R. M., and Capitanio D.

Abstract

Obesity is a chronic, complex pathology associated with a risk of developing secondary pathologies, including cardiovascular diseases, cancer, type 2 diabetes (T2DM) and musculoskeletal disorders. Since skeletal muscle accounts for more than 70% of total glucose disposal, metabolic alterations are strictly associated with the onset of insulin resistance and T2DM. The present study relies on the proteomic analysis of gastrocnemius muscle from 15 male and 15 female C56BL/J mice fed for 14 weeks with standard, 45% or 60% high-fat diets (HFD) adopting a label-free LC–MS/MS approach followed by bioinformatic pathway analysis. Results indicate changes in males due to HFD, with increased muscular stiffness (Col1a1, Col1a2, Actb), fiber-type switch from slow/oxida-tive to fast/glycolytic (decreased Myh7, Myl2, Myl3 and increased Myh2, Mylpf, Mybpc2, Myl1), increased oxidative stress and mitochondrial dysfunction (decreased respiratory chain complex I and V and increased complex III subunits). At variance, females show few alterations and activation of compensatory mechanisms to counteract the increase of fatty acids. Bioinformatics analysis allows identifying upstream molecules involved in regulating pathways identified at variance in our analysis (Ppargc1a, Pparg, Cpt1b, Clpp, Tp53, Kdm5a, Hif1a). These findings underline the presence of a gender-specific response to be considered when approaching obesity and related comor-bidities.

Published

2021

5. Muscle proteomic profile before and after enzyme replacement therapy in late-onset pompe disease

Author

Moriggi, M, Capitanio, D, Torretta, E, Barbacini, P, Bragato, C, Sartori, P, Moggio, M, Maggi, L, Mora, M, Gelfi, C, Moriggi M., Capitanio D., Torretta E., Barbacini P., Bragato C., Sartori P., Moggio M., Maggi L., Mora M., Gelfi C., Moriggi, M, Capitanio, D, Torretta, E, Barbacini, P, Bragato, C, Sartori, P, Moggio, M, Maggi, L, Mora, M, Gelfi, C, Moriggi M., Capitanio D., Torretta E., Barbacini P., Bragato C., Sartori P., Moggio M., Maggi L., Mora M., and Gelfi C.

Abstract

Mutations in the acidic alpha-glucosidase (GAA) coding gene cause Pompe disease. Late-onset Pompe disease (LOPD) is characterized by progressive proximal and axial muscle weakness and atrophy, causing respiratory failure. Enzyme replacement therapy (ERT), based on recombinant human GAA infusions, is the only available treatment; however, the efficacy of ERT is variable. Here we address the question whether proteins at variance in LOPD muscle of patients before and after 1 year of ERT, compared withhealthy age-matched subjects (CTR), reveal a specific signature. Proteins extracted from skeletal muscle of LOPD patients and CTR were analyzed by combining gel based (two-dimensional difference gel electrophoresis) and label-free (liquid chromatography-mass spectrometry) proteomic approaches, and ingenuity pathway analysis. Upstream regulators targeting autophagy and lysosomal tethering were assessed by immunoblotting. 178 proteins were changed in abundance in LOPD patients, 47 of them recovered normal level after ERT. Defects in oxidative metabolism, muscle contractile protein regulation, cytoskeletal rearrangement, and membrane reorganization persisted. Metabolic changes, ER stress and UPR (unfolded protein response) contribute to muscle proteostasis dysregulation with active membrane remodeling (high levels of LC3BII/LC3BI) and accumulation of p62, suggesting imbalance in the autophagic process. Active lysosome biogenesis characterizes both LOPD PRE and POST, unparalleled by molecules involved in lysosome tethering (VAMP8, SNAP29, STX17, and GORASP2) and BNIP3. In conclusion this study reveals a specific signature that suggests ERT prolongation and molecular targets to ameliorate patient’s outcome.

Published

2021

6. Spatial and temporal adjustments allowing the coexistence among carnivores in Liguria (N-W Italy)

Author

Torretta, E., Serafini, M., Puopolo, F., and Schenone, L.

Published

2016

7. Nitrosative Redox Homeostasis and Antioxidant Response Defense in Disused Vastus lateralis Muscle in Long-Term Bedrest (Toulouse Cocktail Study)

Author

Blottner, D., Capitanio, D., Trautmann, G., Furlan, S., Gambara, G., Moriggi, M., Block, K., Barbacini, P., Torretta, E., Py, G., Chopard, A., Vida, I., Volpe, P., Gelfi, C., Salanova, M., Charité - UniversitätsMedizin = Charité - University Hospital [Berlin], University of Milan, Institute of Neuroscience [Milan, Italy] (CNR), Center for Space Medicine Berlin, Università degli Studi di Milano, IRCCS Policlinico San Donato, Centro San Giovanni di Dio, Fatebenefratelli, Brescia (IRCCS), Università degli Studi di Brescia [Brescia], Dynamique Musculaire et Métabolisme (DMEM), Université de Montpellier (UM)-Institut National de Recherche pour l’Agriculture, l’Alimentation et l’Environnement (INRAE), University Hospital of Padua, Federal Department of Economy and Energy (BMWi) through Deutsches Zentrum fuer Luft-und Raumfahrt (DLR e.V., Bonn-Oberkassel, Germany) 50WB1421/1718, 50WB1826, Agenzia Spaziale Italiana (ASI) 2018-9-U.O STOPBROS, and Charite-Universitatsmedizin Berlin

Subjects

sarcopenia, Antioxidant systems, Bedrest muscle disuse, Oxidative stress, RNS in cell signaling, Sarcopenia, Skeletal muscle redox homeostasis, lcsh:Therapeutics. Pharmacology, skeletal muscle redox homeostasis, lcsh:RM1-950, [SDV.SP.PHARMA]Life Sciences [q-bio]/Pharmaceutical sciences/Pharmacology, oxidative stress, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, antioxidant systems, bedrest muscle disuse, Article

Abstract

Increased oxidative stress by reactive oxygen species (ROS) and reactive nitrogen species (RNS) is a major determinant of disuse-induced muscle atrophy. Muscle biopsies (thigh vastus lateralis,VL) obtained from healthy male subjects enrolled in the Toulouse Cocktail bedrest (BR) study were used to assess efficacy of an antioxidant cocktail (polyphenols, omega-3, vitamin E, and selenium) to counteract the increased redox homeostasis and enhance the antioxidant defense response by using label-free LC-MS/MS and NITRO-DIGE (nitrosated proteins), qPCR, and laser confocal microscopy. Label-free LC-MS/MS indicated that treatment prevented the redox homeostasis dysregulation and promoted structural remodeling (TPM3, MYH7, MYBPC, MYH1, MYL1, HRC, and LUM), increment of RyR1, myogenesis (CSRP3), and skeletal muscle development (MUSTN1, LMNA, AHNAK). These changes were absent in the Placebo group. Glycolysis, tricarboxylic acid cycle (TCA), oxidative phosphorylation, fatty acid beta-oxidation, and mitochondrial transmembrane transport were normalized in treated subjects. Proteins involved in protein folding were also normalized, whereas protein entailed in ion homeostasis decreased. NITRO-DIGE analysis showed significant protein nitrosylation changes for CAT, CA3, SDHA, and VDAC2 in Treatment vs. Placebo. Similarly, the nuclear factor erythroid 2-related factor 2 (Nrf-2) antioxidant response element (Nrf-2 ARE) signaling pathway showed an enhanced response in the Treatment group. Increased nitrosative redox homeostasis and decreased antioxidant defense response were found in post-BR control (Placebo,n= 10) vs. the antioxidant cocktail treated group (Treatment,n= 10). Taken together, increased nitrosative redox homeostasis and muscle deterioration during BR-driven physical inactivity were prevented, whereas decreased antioxidant nitrosative stress defense response was attenuated by Treatment suggesting positive effects of the nutritional intervention protocol in bedrest.

Published

2021

8. En route to the North: modelling crested porcupine habitat suitability and dispersal flows across a highly anthropized area in northern Italy

Author

Torretta, E, Orioli, V, Bani, L, Mantovani, S, Dondina, O, Torretta, Elisa, Orioli, Valerio, Bani, Luciano, Mantovani, Sergio, Dondina, Olivia, Torretta, E, Orioli, V, Bani, L, Mantovani, S, Dondina, O, Torretta, Elisa, Orioli, Valerio, Bani, Luciano, Mantovani, Sergio, and Dondina, Olivia

Abstract

The crested porcupine (Hystrix cristata) underwent a rapid and widespread range expansion in Italy. Nowadays the species is moving towards the northernmost regions of the country and its occurrence is increasing in the highly anthropized Po Plain. Our objectives were to evaluate the suitability of the Po Plain for the species, as well as to identify dispersal corridors connecting the northern Apennines occurrence areas and the Prealps. We modelled the species home-range scale habitat suitability based on an ensemble modelling approach. Additionally, a habitat suitability prediction carried out at a finer scale was used to parametrize the landscape resistance, based on which we modelled the potential dispersal corridors for the species using a factorial least-cost path approach. The ensemble prediction estimated a potential occurrence of the crested porcupine in 27.4% of the study area. The species occurrence probability was mainly driven by the distribution of extensive cultivations, woodlands and shrublands, and water courses and by the annual mean temperature. Conversely, the movements of the species resulted mainly sustained by woodlands and shrublands and highly hindered by simple arable lands and rice paddies. The connectivity prediction showed that three main dispersal routes are likely to connect crested porcupine occurrence areas in the northern Apennines to currently unoccupied but highly suitable areas in the Prealps. The study allowed us to identify the areas in the Prealps with the highest probability to be colonized by the crested porcupine in the near future and provided important insights for the conservation of a strictly protected species in a human-dominated landscape.

Published

2021

9. Combining ensemble models and connectivity analyses to predict wolf expected dispersal routes through a lowland corridor

Author

Dondina, O, Orioli, V, Torretta, E, Merli, F, Bani, L, Meriggi, A, Dondina, O, Orioli, V, Torretta, E, Merli, F, Bani, L, and Meriggi, A

Abstract

The Italian wolf (Canis lupus italicus) population has remained isolated South of the Alps for the last few thousand years. After a strong decline, the species has recolonized the Apennines and the Western Alps, while it is currently struggling to colonize the Eastern Alps. Recently, the species was detected in a lowland park connecting the Northern Apennines to the Central Alps. If the park was able to sustain a net wolf dispersal flow, this could significantly boost the connection with the Eastern Alps and the Dinaric-Balkan population. We investigated the suitability of the park as a functional ecological corridor for the wolf through the unhospitable lowland of Northern Italy. We collected wolf occurrence data in two study areas. We modeled species distribution running a separate ensemble model for each study area and then merging the output of the models to obtain an integrated suitability map. We used this map to identify corridors for the wolf adopting a factorial least-cost path and a cumulative resistant kernel approach. The connectivity models showed that only two corridors exist in the lowland areas between the Northern Apennines and the Central Alps. The Western corridor is a blind route, while the eastern corridor passes through the park and has a continuous course. However, the models also revealed a scarce resilience of corridor connectivity in the passageways between the park and the Apennines and the Prealps, which suggests that urgent management actions are necessary to ensure the future functionality of this important corridor.

Published

2020

10. First assessment of habitat suitability and connectivity for the golden jackal in north-eastern Italy

Author

Torretta, E, Dondina, O, Delfoco, C, Riboldi, L, Orioli, V, Lapini, L, Meriggi, A, Riboldi L., Torretta, E, Dondina, O, Delfoco, C, Riboldi, L, Orioli, V, Lapini, L, Meriggi, A, and Riboldi L.

Abstract

Compared with the rapid expansion across Europe, the golden jackal colonization of Italy is still limited and slow. No study focused on the habitat selection or landscape connectivity for this species was performed in Italy; thus, the potential distribution and dispersal patterns in the country remain unknown. Our objectives were to evaluate the suitability of the Friuli-Venezia Giulia region (north-eastern Italy) for the golden jackal, as well as to identify the ecological corridors connecting the areas currently occupied by the species. Corridors modelling allowed us both to hypothesize the dispersal dynamics occurring in the study region and to identify possible obstacles to future range expansion. We surveyed golden jackal presence in two study areas, covering an area of 500 km2, from March 2017 to February 2018. Using collected data, we modelled the species home-range scale habitat suitability based on an ensemble modelling approach. Subsequently, a habitat suitability prediction at a finer scale was used to estimate landscape resistance, starting from which, we modelled dispersal corridors among areas currently occupied by the species using a factorial least cost path and a cumulative resistant kernel approach. Our results indicated a moderate potential for large parts of the study region to support the occurrence of golden jackal family groups, whose presence seems to be mainly driven by the presence of wide areas covered by broadleaved forests and shrublands and by the absence of wide intensive agricultural areas. The predicted connectivity networks showed that three main permeable corridors are likely to connect golden jackal occurrence areas within the study region, while all the other corridors are characterized by a very low path density. Both the habitat selection and connectivity analyses showed a strong negative impact of the intensive cultivated plain on species stable presence and movement providing critical information for the conservation of

Published

2020

11. Recent Changes in Wolf Habitat Occupancy and Feeding Habits in Italy: Implications for Conservation and Reducing Conflict with Humans

Author

Angelici, FM, Rossi, L, Meriggi, A, Torretta, E, Dondina, O, Angelici, FM, Rossi, L, Meriggi, A, Torretta, E, and Dondina, O

Abstract

Despite the generally positive trend of European populations, the wolf (Canis lupus) is still today a challenging species to conserve, particularly in the most anthropogenic southern European countries, because of its conflict with humans. In this chapter we summarize the dynamics of wolf distribution in Italy, one of the most densely populated European countries, over the last 50 years. We track changes in the wolf’s diet by comparing its change in Italy with other countries, with the aim of understanding how these changes may have affected the evolution of the human-predator conflict in Italy. In particular, we summarize the results of studies both in Italy and in other European countries to clarify the true impact of wolf predation on both livestock and wild ungulates, which represent the two main causes of predator-human conflict. In order to provide specific insight about the past and the current distribution and feeding habits of the wolf in Italy, and to take stock of the conflict between wolves and humans, we present three case studies. All were carried out over recent decades in northern Italy, i.e. in the area where wolf packs, and particularly their ability to produce dispersing individuals, could affect the future of the entire Italian population. Finally, we consider how to mitigate wolf-human conflict and suggest effective management of wolf populations.

Published

2020

12. Time partitioning in mesocarnivore communities from different habitats of NW Italy: Insights into martens' competitive abilities

Author

Torretta, E, Mosini, A, Piana, M, Tirozzi, P, Serafini, M, Puopolo, F, Saino, N, Balestrieri, A, Torretta E., Mosini A., Piana M., Tirozzi P., Serafini M., Puopolo F., Saino N., Balestrieri A., Torretta, E, Mosini, A, Piana, M, Tirozzi, P, Serafini, M, Puopolo, F, Saino, N, Balestrieri, A, Torretta E., Mosini A., Piana M., Tirozzi P., Serafini M., Puopolo F., Saino N., and Balestrieri A.

Abstract

Most studies focused on species coexistence have been directed at the differential use of habitat and food resources; nonetheless, the differential use of the diel cycle may enhance the coexistence of same-sized species. We investigated the activity patterns of mesocarnivores (red fox (Vulpes vulpes), European badger (Meles meles), pine marten (Martes martes), stone marten (M. foina)) in NW Italy via camera-trapping. We hypothesized that the smallest species would tend to avoid competition by selecting time periods when larger species were less active. Foxes, badgers, and stone martens were mainly nocturnal. In lowland areas overlap between coexisting species was generally low, while in Mediterranean habitats all activity patterns tended to be unimodal and overlap was generally high. The pine marten showed a cathemeral pattern. We suggest that the lower ability of the stone marten to avoid interference competition at community-level may play a major role in determining its widespread exclusion from forested areas by the pine marten.

Published

2017

13. TCA cycle rewiring fosters metabolic adaptation to oxygen restriction in skeletal muscle from rodents and humans

Author

Capitanio D. 1, Fania C. 2, Torretta E. 1, Vigano A 1, Moriggi M. 3, Bravatà V. 3, Caretti A. 4, Levett D.Z.H. 5, 6, 7, Grocott M.P.W. 5, Samaja M. 4, Cerretelli P. 3, Gelfi C. 8, 9, Capitanio, D, Fania, C, Torretta, E, Viganò, A, Moriggi, M, Bravatà, V, Caretti, A, Levett, D, Grocott, M, Samaja, M, Cerretelli, P, and Gelfi, C

Subjects

Proteomics, 0301 basic medicine, Time Factors, BIO/12 - BIOCHIMICA CLINICA E BIOLOGIA MOLECOLARE CLINICA, Proteome, Citric Acid Cycle, Gene Expression, lcsh:Medicine, Rodentia, Biology, TCA cycle, skeletal muscle, proteomics, 2D-DIGE, hypoxia, Models, Biological, Article, 03 medical and health sciences, Autophagy, Basic Helix-Loop-Helix Transcription Factors, medicine, Animals, Humans, Muscle, Skeletal, lcsh:Science, chemistry.chemical_classification, Multidisciplinary, 030102 biochemistry & molecular biology, lcsh:R, Skeletal muscle, Hexosamines, Metabolism, Hypoxia (medical), Hypoxia-Inducible Factor 1, alpha Subunit, Adaptation, Physiological, BIO/10 - BIOCHIMICA, Oxygen, Glutamine, Citric acid cycle, Cytosol, 030104 developmental biology, Enzyme, medicine.anatomical_structure, chemistry, Hypoxia-inducible factors, Biochemistry, lcsh:Q, medicine.symptom, Energy Metabolism, Metabolic Networks and Pathways, Signal Transduction

Abstract

In mammals, hypoxic stress management is under the control of the Hypoxia Inducible Factors, whose activity depends on the stabilization of their labile α subunit. In particular, the skeletal muscle appears to be able to react to changes in substrates and O2 delivery by tuning its metabolism. The present study provides a comprehensive overview of skeletal muscle metabolic adaptation to hypoxia in mice and in human subjects exposed for 7/9 and 19 days to high altitude levels. The investigation was carried out combining proteomics, qRT-PCR mRNA transcripts analysis, and enzyme activities assessment in rodents, and protein detection by antigen antibody reactions in humans and rodents. Results indicate that the skeletal muscle react to a decreased O2 delivery by rewiring the TCA cycle. The first TCA rewiring occurs in mice in 2-day hypoxia and is mediated by cytosolic malate whereas in 10-day hypoxia the rewiring is mediated by Idh1 and Fasn, supported by glutamine and HIF-2α increments. The combination of these specific anaplerotic steps can support energy demand despite HIFs degradation. These results were confirmed in human subjects, demonstrating that the TCA double rewiring represents an essential factor for the maintenance of muscle homeostasis during adaptation to hypoxia.

Published

2017

14. ECM Remodeling in Breast Cancer with Different Grade: Contribution of 2D-DIGE Proteomics

Author

Moriggi M 1, Giussani M 2, Torretta E 1, Capitanio D 1, 3, Sandri M 2, Leone R 1, De Palma S 4, Vasso M4, Vozzi G 5, 6, Tagliabue E 2, and Gelfi C 1

Subjects

TN tumors, 0301 basic medicine, Proteome, Integrin, Breast Neoplasms, Biology, Proteomics, Biochemistry, Two-Dimensional Difference Gel Electrophoresis, Focal adhesion, Extracellular matrix, 03 medical and health sciences, breast cancer, 0302 clinical medicine, Gene cluster, Gene expression, Humans, Epithelial–mesenchymal transition, 2D-DIGE, ECM, mass spectrometry, Molecular Biology, Mechanotransduction, Extracellular Matrix Proteins, Mass Spectrometry, Extracellular Matrix, Cell biology, 030104 developmental biology, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, 030220 oncology & carcinogenesis, biology.protein, Female, Neoplasm Grading

Abstract

Tumor extracellular matrix (ECM) plays a pivotal role in outcome of breast cancer (BC) patients. Overespression of 58 genes, encoding 43 structural ECM proteins, has been identified to determine a specific cluster of BC with accelerated metastatic potential only in the undifferentiated (grade III) phenotype. The scope of this study was to characterize protein repertoire able to predict patient outcome in BC according to ECM gene expression pattern and histological grade. The differential proteomic analysis has been based on 2D-DIGE, MALDI-MS, bioinformatics and immunoblotting. Results suggested a relationship among ECM remodeling, signal mechanotransduction and metabolic rewiring in BCs characterized by a specific mRNA ECM signature and identified a set of dysregulated proteins characteristic of hormone receptors expression as fibrinogen beta chain (FGB), collagen alpha-1 (VI) chain (COL6A1) and alpha-1B-glycoprotein (A1BG). Furthermore, in triple negative tumors (TN) with ECM signature, the FGG and ?5?1/?v?3 integrins increased whereas detyrosinated alpha-tubulin, and mimecan (OGN) decreased leading to unorganized integrin presentation involving focal adhesion kinase (FAK), activation of Rho GTPases associated to epithelial mesenchymal transition. In hormone receptors negative BCs characterized by a specific ECM gene cluster, the differentially regulated proteins, identified in the present study,can be potentially relevant to predict patient's outcome.

Published

2018

15. Collagen VI null mice as a model for early onset muscle decline in aging

Author

Capitanio, D, Moriggi, M, De Palma, S, Bizzotto, D, Molon, S, Torretta, E, Fania, C, Bonaldo, P, Gelfi, C, Braghetta, P, Capitanio, Daniele, Moriggi, Manuela, De Palma, Sara, Bizzotto, Dario, Molon, Sibilla, Torretta, Enrica, Fania, Chiara, Bonaldo, Paolo, Gelfi, Cecilia, Braghetta, Paola, Capitanio, D, Moriggi, M, De Palma, S, Bizzotto, D, Molon, S, Torretta, E, Fania, C, Bonaldo, P, Gelfi, C, Braghetta, P, Capitanio, Daniele, Moriggi, Manuela, De Palma, Sara, Bizzotto, Dario, Molon, Sibilla, Torretta, Enrica, Fania, Chiara, Bonaldo, Paolo, Gelfi, Cecilia, and Braghetta, Paola

Abstract

Collagen VI is an extracellular matrix (ECM) protein playing a key role in skeletal muscles and whose deficiency leads to connective tissue diseases in humans and in animal models. However, most studies have been focused on skeletal muscle features. We performed an extensive proteomic profiling in two skeletal muscles (diaphragm and gastrocnemius) of wild-type and collagen VI null (Col6a1−/−) mice at different ages, from 6- (adult) to 12- (aged) month-old to 24 (old) month-old. While in wild-type animals the number of proteins and the level of modification occurring during aging were comparable in the two analyzed muscles, Col6a1−/− mice displayed a number of muscle-type specific variations. In particular, gastrocnemius displayed a limited number of dysregulated proteins in adult mice, while in aged muscles the modifications were more pronounced in terms of number and level. In diaphragm, the differences displayed by 6-month-old Col6a1−/− mice were more pronounced compared to wild-type mice and persisted at 12 months of age. In adult Col6a1−/− mice, the major variations were found in the enzymes belonging to the glycolytic pathway and the tricarboxylic acid (TCA) cycle, as well as in autophagy-related proteins. When compared to wild-type animals Col6a1−/− mice displayed a general metabolic rewiring which was particularly prominent the diaphragm at 6 months of age. Comparison of the proteomic features and the molecular analysis of metabolic and autophagic pathways in adult and aged Col6a1−/− diaphragm indicated that the effects of aging, culminating in lipotoxicity and autophagic impairment, were already present at 6 months of age. Conversely, the effects of aging in Col6a1−/−gastrocnemius were similar but delayed becoming apparent at 12 months of age. A similar metabolic rewiring and autophagic impairment was found in the diaphragm of 24-month-old wild-type mice, confirming that fatty acid synthase (FASN) increment and decreased microtubule-associated proteins 1A/1B

Published

2017

16. Intermediate and low abundant protein analysis of Vitamin D deficient obese and non-obese subjects by MALDI-profiling

Author

Al-Daghri, N, Torretta, E, Capitanio, D, Fania, C, Guerini, F, Sabico, S, Clerici, M, Gelfi, C, Al-Daghri, Nasser M, Torretta, Enrica, Capitanio, Daniele, Fania, Chiara, Guerini, Franca Rosa, Sabico, Shaun B, Clerici, Mario, Gelfi, Cecilia, Al-Daghri, N, Torretta, E, Capitanio, D, Fania, C, Guerini, F, Sabico, S, Clerici, M, Gelfi, C, Al-Daghri, Nasser M, Torretta, Enrica, Capitanio, Daniele, Fania, Chiara, Guerini, Franca Rosa, Sabico, Shaun B, Clerici, Mario, and Gelfi, Cecilia

Abstract

Obesity is a pathological condition caused by genetic and environmental factors, including vitamin D deficiency, which increases the risk of developing cardiovascular disorders and diabetes. This case-control study was designed to verify whether serum profiles could be identified differentiating obese and non-obese Saudis characterized by vitamin D deficiency and pathological levels of triglycerides, high-density lipoprotein cholesterol and high total cholesterol levels. The serum protein profiles of 64 vitamin D deficient (serum 25(OH)D < 50nmol/L) individuals with metabolic syndrome and with (n = 31; BMI ≥ 30) or without (n = 33; BMI < 30) obesity were analyzed by a quantitative label-free mass spectrometry approach (MALDI-profiling), combined with different serum immunodepletion strategies (Human7 and Human14 immuno-chromatographies), to analyze the intermediate- and low-abundant protein components. The analysis of intermediate-abundant proteins (Human7) in obese vs. non-obese subjects identified 14 changed peaks (p < 0.05) in the m/z range 1500-35000. Furthermore, the Human14 depletion provided new profiles related to obesity (121 changed peaks). Among changed peaks, 11 were identified in the m/z range 1500-4000 Da by high-resolution tandem mass spectrometry, belonging to apolipoprotein CIII, apolipoprotein B100, alpha-1-antichymotrypsin and complement C3. Data herein show that distinct protein profiles identify specific peptides belonging to lipid metabolism and inflammation processes that are associated with obesity and vitamin D deficiency.

Published

2017

17. Time partitioning in mesocarnivore communities from different habitats of NW Italy: insights into martens’ competitive abilities

Author

Torretta, E., primary, Mosini, A., additional, Piana, M., additional, Tirozzi, P., additional, Serafini, M., additional, Puopolo, F., additional, Saino, N., additional, and Balestrieri, A., additional

Published

2017

18. NEU3 sialidase protein interactors in the plasma membrane and in the endosomes

Author

Cirillo, F, Ghiroldi, A, Fania, C, Piccoli, M, Torretta, E, Tettamanti, G, Gelfi, C, Anastasia, L, Cirillo, Federica, Ghiroldi, Andrea, Fania, Chiara, Piccoli, Marco, Torretta, Enrica, Tettamanti, Guido, Gelfi, Cecilia, Anastasia, Luigi, Cirillo, F, Ghiroldi, A, Fania, C, Piccoli, M, Torretta, E, Tettamanti, G, Gelfi, C, Anastasia, L, Cirillo, Federica, Ghiroldi, Andrea, Fania, Chiara, Piccoli, Marco, Torretta, Enrica, Tettamanti, Guido, Gelfi, Cecilia, and Anastasia, Luigi

Abstract

NEU3 sialidase has been shown to be a key player in many physio- and pathological processes, including cell differentiation, cellular response to hypoxic stress, and carcinogenesis. The enzyme, peculiarly localized on the outer leaflet of the plasma membrane, has been shown to be able to remove sialic acid residues from the gangliosides present on adjacent cells, thus creating cell to cell interactions. Nonetheless, herein we report that the enzyme localization is dynamically regulated between the plasma membrane and the endosomes, where a substantial amount of NEU3 is stored with low enzymatic activity. However, under opportune stimuli,NEU3is shifted from the endosomes to the plasma membrane, where it greatly increases the sialidase activity. Finally, we found that NEU3 possesses also the ability to interact with specific proteins, many of which are different in each cell compartment. They were identified by mass spectrometry, and some selected ones were also confirmed by cross-immunoprecipitation with the enzyme, supporting NEU3 involvement in the cell stress response, protein folding, and intracellular trafficking.

Published

2016

19. Specific protein changes contribute to the differential muscle mass loss during ageing

Author

Capitanio, D, Vasso, M, De Palma, S, Fania, C, Torretta, E, Cammarata, F, Magnaghi, V, Procacci, P, Gelfi, C, Capitanio, Daniele, Vasso, Michele, De Palma, Sara, Fania, Chiara, Torretta, Enrica, Cammarata, Francesco P, Magnaghi, Valerio, Procacci, Patrizia, Gelfi, Cecilia, Capitanio, D, Vasso, M, De Palma, S, Fania, C, Torretta, E, Cammarata, F, Magnaghi, V, Procacci, P, Gelfi, C, Capitanio, Daniele, Vasso, Michele, De Palma, Sara, Fania, Chiara, Torretta, Enrica, Cammarata, Francesco P, Magnaghi, Valerio, Procacci, Patrizia, and Gelfi, Cecilia

Abstract

In the skeletal muscle, the ageing process is characterized by a loss of muscle mass and strength, coupled with a decline of mitochondrial function and a decrease of satellite cells. This profile is more pronounced in hindlimb than in forelimb muscles, both in humans and in rodents. Utilizing light and electron microscopy, myosin heavy chain isoform distribution, proteomic analysis by 2D-DIGE, MALDI-TOF MS and quantitative immunoblotting, this study analyzes the protein levels and the nuclear localization of specific molecules, which can contribute to a preferential muscle loss. Our results identify the molecular changes in the hindlimb (gastrocnemius) and forelimb (triceps) muscles during ageing in rats (3- and 22-month-old). Specifically, the oxidative metabolism contributes to tissue homeostasis in triceps, whereas respiratory chain disruption and oxidative-stress-induced damage imbalance the homeostasis in gastrocnemius muscle. High levels of dihydrolipoyllysine-residue acetyltransferase (Dlat) and ATP synthase subunit alpha (Atp5a1) are detected in triceps and gastrocnemius, respectively. Interestingly, in triceps, both molecules are increased in the nucleus in aged rats and are associated to an increased protein acetylation and myoglobin availability. Furthermore, autophagy is retained in triceps whereas an enhanced fusion, decrement of mitophagy and of regenerative potential is observed in aged gastrocnemius muscle.

Published

2016

20. HPTLC-MALDI MS for (glyco)sphingolipid multiplexing in tissues and blood: A promising strategy for biomarker discovery and clinical applications

Author

Torretta, E, Fania, C, Vasso, M, Gelfi, C, Torretta, Enrica, Fania, Chiara, Vasso, Michele, Gelfi, Cecilia, Torretta, E, Fania, C, Vasso, M, Gelfi, C, Torretta, Enrica, Fania, Chiara, Vasso, Michele, and Gelfi, Cecilia

Abstract

Sphingolipids have hydrophilic and hydrophobic properties, different saturation and combination of the oligosaccharide chains and mass homology of species located in a narrow m/z region hampering their recognition. To target sphingolipids for diagnostic purposes, standardized methods for lipid extraction, quali- and quantitative assessments are required. In this study, HPTLC-MALDI MS was adopted to establish sphingolipid and glycosphingolipid profiles in muscle, brain and serum to create a database of molecules to be searched in the preclinical and clinical investigations. Specific protocols for lipid extraction were set up based on the characteristics of the tissue or/and fluids; this approach maximizes the HPTLC-MALDI MS analytical throughput both for lipids extracted in organic and aqueous phase. This study indicates that alkaline hydrolysis is necessary for the detection of low abundant species such as Gb3Cer and ceramides in serum and Gb4Cer, CerP and HexCer in muscle tissue. The high hydrophobicity of ceramides has been overcome by the development of HPTLC plate in chloroform:methanol/50:3.5, which increases the number and the intensity of low abundant Cer species. MS/MS analysis has been conducted directly on HPTLC plate allowing the molecular recognition; furthermore a dataset of spectra was acquired to create a database for future profiling of these molecules.

Published

2016

21. Sprague Dawley rats: A model of successful heart aging

Author

Capitanio, D, Leone, R, Fania, C, Torretta, E, Gelfi, C, Capitanio, Daniele, Leone, Roberta, Fania, Chiara, Torretta, Enrica, Gelfi, Cecilia, Capitanio, D, Leone, R, Fania, C, Torretta, E, Gelfi, C, Capitanio, Daniele, Leone, Roberta, Fania, Chiara, Torretta, Enrica, and Gelfi, Cecilia

Abstract

Aging is a universal phenomenon involving the whole body and is characterized by metabolic and physiological decline, leading to cardiovascular defects and heart failure. To characterize the molecular basis of physiological cardiac aging, the proteomic profiles of Sprague Dawley rat hearts of 6, 22 and 30 months were analysed by DIGE and immunoblotting. Results indicate changes in myosin binding protein C, aldehyde dehydrogenase, serpins and sirtuin-3 which protects from the opening of the mitochondrial permeability transition pore induced by cyclophilin D increment. Conversely, an increase of fusion, a decrease of mitochondrial fission and the activation of the non-canonical autophagy pathway were observed. These results support the hypothesis of successful aging in this rat model.

Published

2016

22. A PSA-guided approach for a better diagnosis of prostatic adenocarcinoma based on MALDI profiling and peptide identification

Author

Fania, C, Sogno, I, Vasso, M, Torretta, E, Leone, R, Bruno, A, Consonni, P, Albini, A, Gelfi, C, Chiara Fania, Ilaria Sogno, Michele Vasso, Enrica Torretta, Roberta Leone, Antonino Bruno, Paolo Consonni, Adriana Albini, Cecilia Gelfi, Fania, C, Sogno, I, Vasso, M, Torretta, E, Leone, R, Bruno, A, Consonni, P, Albini, A, Gelfi, C, Chiara Fania, Ilaria Sogno, Michele Vasso, Enrica Torretta, Roberta Leone, Antonino Bruno, Paolo Consonni, Adriana Albini, and Cecilia Gelfi

Abstract

Background: Prostate cancer (PCa) is the second cause of mortality in men worldwide. The prostate-specific antigen (PSA) test is routinely adopted in diagnosis; nevertheless more reliable biomarkers are continuously under investigation by monitoring the release of molecules into the bloodstream. The serum protein profiles appear to provide cancer-specific fingerprints that help to discriminate patients (especially with low PSA level) from controls, improving the performance of existing clinical tests. Methods: Samples from healthy controls and PCa patients with low (≤. 4. ng/mL) and high PSA (>. 4. ng/mL) levels were analyzed by MALDI profiling, and by a multi fractionation approach coupled to ESI-MS for peaks identification. Results: MALDI profiling achieved to detect 10 and 14 changed peaks (p-value <. 0.05), respectively, in PCa patients with low and high PSA versus controls. In particular, a peak identified as C3f fragment, resulted overexpressed in low PSA PCa patients. Conclusions: PSA test, coupled to MALDI profiling, is able to detect changes, specifically related to PCa, in low molecular weight protein range. Furthermore, for the first time in prostate cancer research, the identification and quantification of the small peptide C3f appears to be relevant for the detection of false negatives, providing an additive diagnostic power to PSA (p<. 0.01) and suggesting its use in clinical tests.

Published

2015

23. Spatial and temporal adjustments allowing the coexistence among carnivores in Liguria (N-W Italy)

Author

Torretta, E., primary, Serafini, M., additional, Puopolo, F., additional, and Schenone, L., additional

Published

2015

24. Setup for human sera MALDI profiling: The case of rhEPO treatment

Author

Fania C. 1, Vasso M. 1, 2, Torretta E. 1, Robach P. 3, Cairo G. 4, Lundby C. 5, and Gelfi C. 1

Subjects

Serum, 2-D differential gel electrophoresis, Immunodepletion, MALDI profiling, EPO

Abstract

The implementation of high-throughput technologies based on qualitative and quantitative methodologies for the characterization of complex protein mixtures is increasingly required in clinical laboratories. MALDI profiling is a robust and sensitive technology although the serum high dynamic range imposes a major limitation hampering the identification of less abundant species decreasing the quality of MALDI profiling. A setup to improve these parameters has been performed for recombinant human erythropoietin (rhEPO) monitoring in serum, analyzing the effects of two commercially available columns (MARS Hu7 and Hu14) for immunodepletion, and two matrices (±-cyano-4-hydroxycinnamic acid and 2',4'-dihydroxyacetophenone) for peak quality improvement. The immunodepletion capability of both columns was determined by 2-D DIGE, which precisely revealed the efficacy of Hu14 in protein removal and the serum dynamic range decrement. In addition, the type of matrix, the sample dilution, and the efficacy of optimized parameters were used for serum profiling of ten healthy subjects before and after rhEPO treatment. The principal component analysis indicates that a combination of Hu14 column and 2',4'-dihydroxyacetophenone matrix increases data quality allowing the discrimination between treated and untreated samples, making serum MALDI profiling suitable for clinical monitoring of rhEPO.

Published

2011

25. Gangliosides as a potential new class of stem cell markers: the case of GD1a in human bone marrow mesenchymal stem cells

Author

Bergante, S, Torretta, E, Creo, P, Sessarego, N, Papini, N, Piccoli, M, Fania, C, Cirillo, F, Conforti, E, Ghiroldi, A, Tringali, C, Venerando, B, Ibatici, A, Gelfi, C, Tettamanti, G, Anastasia, L, Bergante, Sonia, Torretta, Enrica, Creo, Pasquale, Sessarego, Nadia, Papini, Nadia, Piccoli, Marco, Fania, Chiara, Cirillo, Federica, Conforti, Erika, Ghiroldi, Andrea, Tringali, Cristina, Venerando, Bruno, Ibatici, Adalberto, Gelfi, Cecilia, Tettamanti, Guido, Anastasia, Luigi, Bergante, S, Torretta, E, Creo, P, Sessarego, N, Papini, N, Piccoli, M, Fania, C, Cirillo, F, Conforti, E, Ghiroldi, A, Tringali, C, Venerando, B, Ibatici, A, Gelfi, C, Tettamanti, G, Anastasia, L, Bergante, Sonia, Torretta, Enrica, Creo, Pasquale, Sessarego, Nadia, Papini, Nadia, Piccoli, Marco, Fania, Chiara, Cirillo, Federica, Conforti, Erika, Ghiroldi, Andrea, Tringali, Cristina, Venerando, Bruno, Ibatici, Adalberto, Gelfi, Cecilia, Tettamanti, Guido, and Anastasia, Luigi

Abstract

Owing to their exposure on the cell surface and the possibility of being directly recognized with specific antibodies, glycosphingolipids have aroused great interest in the field of stem cell biology. In the search for specific markers of the differentiation of human bone marrow mesenchymal stem cells (hBMSCs ) toward osteoblasts, we studied their glycosphingolipid pattern, with particular attention to gangliosides. After lipid extraction and fractionation, gangliosides, metabolically 3H-labeled in the sphingosine moiety, were separated by high-performance TLC and chemically characterized by MALDI MS. Upon induction of osteogenic differentiation, a 3-fold increase of ganglioside GD1a was observed. Therefore, the hypothesis of GD1a involvement in hBMSCs commitment toward the osteogenic phenotype was tested by comparison of the osteogenic propensity of GD1a-highly expressing versus GD1a-low expressing hBMSCs and direct addition of GD1a in the differentiation medium. It was found that either the high expression of GD1a in hBMSCs or the addition of GD1a in the differentiation medium favored osteogenesis, providing a remarkable increase of alkaline phosphatase. It was also observed that ganglioside GD2, although detectable in hBMSCs by immunohistochemistry with an anti-GD2 antibody, could not be recognized by chemical analysis, likely reflecting a case, not uncommon, of molecular mimicry

Published

2014

26. Application of direct HPTLC-MALDI for the qualitative and quantitative profiling of neutral and acidic glycosphingolipids: the case of NEU3 overexpressing C2C12 murine myoblasts

Author

Torretta, E, Vasso, M, Fania, C, Capitanio, D, Bergante, S, Piccoli, M, Tettamanti, G, Anastasia, L, Gelfi, C, Torretta, Enrica, Vasso, Michele, Fania, Chiara, Capitanio, Daniele, Bergante, Sonia, Piccoli, Marco, Tettamanti, Guido, Anastasia, Luigi, Gelfi, Cecilia, Torretta, E, Vasso, M, Fania, C, Capitanio, D, Bergante, S, Piccoli, M, Tettamanti, G, Anastasia, L, Gelfi, C, Torretta, Enrica, Vasso, Michele, Fania, Chiara, Capitanio, Daniele, Bergante, Sonia, Piccoli, Marco, Tettamanti, Guido, Anastasia, Luigi, and Gelfi, Cecilia

Abstract

Glycosphingolipids (GSLs) are a class of ubiquitous lipids characterized by a wide structural repertoire and a variety of functional implications. Importantly, altered levels have been correlated with different diseases, suggesting their crucial role in health. Conventional methods for the characterization and quantification are based on high-performance TLC (HPTLC) separation and comparison with the migration distance of standard samples or on MS. We set up and herein report the application of an ImagePrep method for glycosphingolipids qualitative and quantitative profiling through direct HPTLC-MALDI with particular application to wild-type and NEU3 sialidase-overexpressing C2C12 myoblasts. Lipids were analyzed by HPTLC, coupled with MALDI-TOF, and the resulting GSLs profiles were compared to the [3H]sphingolipids HPTLC patterns obtained after metabolic radiolabeling. GSLs detection by HPTLC-MALDI was optimized by testing different methods for matrix delivery and by performing quantitative analyses using serial dilutions of GSLs standards. Through this approach an accurate analysis of each variant of neutral and acidic GSLs, including the detection of different fatty-acid chain variants for each GSL, was provided and these results demonstrated that HPTLC-MALDI is an easy and high-throughput analytical method for GSLs profiling, suggesting its use for an early detection of markers in different diseases, including cancer and heart ischemia

Published

2014

27. Detection of bovine herpes virus I (BHV-I) semen infections by a dot-blot hybridization assay

Author

Pacciarini, M., primary, Agresti, A., additional, Desimone, F., additional, Poli, G., additional, Torretta, E., additional, Siccardi, A.G., additional, Meneveri, R., additional, and Ginelli, E., additional

Published

1988

28. NEU3 sialidase protein interactors in the plasma membrane and in the endosomes

Author

Marco Piccoli, Cecilia Gelfi, Chiara Fania, Luigi Anastasia, Enrica Torretta, Andrea Ghiroldi, Guido Tettamanti, Federica Cirillo, Cirillo, F, Ghiroldi, A, Fania, C, Piccoli, M, Torretta, E, Tettamanti, G, Gelfi, C, Anastasia, L, Cirillo, F., Ghiroldi, A., Fania, C., Piccoli, M., Torretta, E., Tettamanti, G., Gelfi, C., and Anastasia, L.

Subjects

0301 basic medicine, Protein Folding, Endosome, Cellular differentiation, Cell, Glycobiology and Extracellular Matrices, NEU3, Neuraminidase, Endosomes, Biology, Sialidase, HeLa Cell, Biochemistry, Cell membrane, protein-protein interaction, 03 medical and health sciences, chemistry.chemical_compound, HEK293 Cell, Stress, Physiological, medicine, Humans, Endoplasmic Reticulum Chaperone BiP, endosome, Molecular Biology, Heat-Shock Proteins, ganglioside, sialidase, Cell Membrane, Heat-Shock Protein, Cell Biology, Recombinant Protein, Recombinant Proteins, Transport protein, Cell biology, Sialic acid, Up-Regulation, Protein Transport, HEK293 Cells, 030104 developmental biology, medicine.anatomical_structure, chemistry, sphingolipid, Intracellular, HeLa Cells, Human

Abstract

NEU3 sialidase has been shown to be a key player in many physio- and pathological processes, including cell differentiation, cellular response to hypoxic stress, and carcinogenesis. The enzyme, peculiarly localized on the outer leaflet of the plasma membrane, has been shown to be able to remove sialic acid residues from the gangliosides present on adjacent cells, thus creating cell to cell interactions. Nonetheless, herein we report that the enzyme localization is dynamically regulated between the plasma membrane and the endosomes, where a substantial amount of NEU3 is stored with low enzymatic activity. However, under opportune stimuli, NEU3 is shifted from the endosomes to the plasma membrane, where it greatly increases the sialidase activity. Finally, we found that NEU3 possesses also the ability to interact with specific proteins, many of which are different in each cell compartment. They were identified by mass spectrometry, and some selected ones were also confirmed by cross-immunoprecipitation with the enzyme, supporting NEU3 involvement in the cell stress response, protein folding, and intracellular trafficking.

Published

2016

29. Gangliosides as a potential new class of stem cell markers : the case of GD1a in human bone marrow mesenchymal stem cells

Author

Adalberto Ibatici, Pasquale Creo, Luigi Anastasia, Nadia Papini, Guido Tettamanti, Nadia Sessarego, Federica Cirillo, Erika Conforti, Cristina Tringali, Chiara Fania, Bruno Venerando, Marco Piccoli, Cecilia Gelfi, Andrea Ghiroldi, Enrica Torretta, Sonia Bergante, Bergante, S., Torretta, E., Creo, P., Sessarego, N., Papini, N., Piccoli, M., Fania, C., Cirillo, F., Conforti, E., Ghiroldi, A., Tringali, C., Venerando, B., Ibatici, A., Gelfi, C., Tettamanti, G., Anastasia, L., Bergante, S, Torretta, E, Creo, P, Sessarego, N, Papini, N, Piccoli, M, Fania, C, Cirillo, F, Conforti, E, Ghiroldi, A, Tringali, C, Venerando, B, Ibatici, A, Gelfi, C, Tettamanti, G, and Anastasia, L

Subjects

endocrine system, Cellular differentiation, osteogenic differentiation, Gene Expression, Stem cells characterization, Bone Marrow Cells, Core Binding Factor Alpha 1 Subunit, stem cells characterization, QD415-436, Stem cell marker, Biochemistry, Sphingolipid, chemistry.chemical_compound, Endocrinology, Osteogenesis, Gangliosides, Osteogenic differentiation, Humans, Osteopontin, gangliosides, mesenchymal stem cells, Research Articles, Cells, Cultured, Sphingolipids, Ganglioside, Osteoblasts, biology, Dose-Response Relationship, Drug, Reverse Transcriptase Polymerase Chain Reaction, Stem Cells, Mesenchymal stem cell, Cell Differentiation, Mesenchymal Stem Cells, Cell Biology, Glycosphingolipid, Dermis, Fibroblasts, Alkaline Phosphatase, Flow Cytometry, Molecular biology, carbohydrates (lipids), chemistry, biology.protein, Alkaline phosphatase, lipids (amino acids, peptides, and proteins), Stem cell, Biomarkers

Abstract

Owing to their exposure on the cell surface and the possibility of being directly recognized with specific antibodies, glycosphingolipids have aroused great interest in the field of stem cell biology. In the search for specific markers of the differentiation of human bone marrow mesenchymal stem cells (hBMSCs) toward osteoblasts, we studied their glycosphingolipid pattern, with particular attention to gangliosides. After lipid extraction and fractionation, gangliosides, metabolically (3)H-labeled in the sphingosine moiety, were separated by high-performance TLC and chemically characterized by MALDI MS. Upon induction of osteogenic differentiation, a 3-fold increase of ganglioside GD1a was observed. Therefore, the hypothesis of GD1a involvement in hBMSCs commitment toward the osteogenic phenotype was tested by comparison of the osteogenic propensity of GD1a-highly expressing versus GD1a-low expressing hBMSCs and direct addition of GD1a in the differentiation medium. It was found that either the high expression of GD1a in hBMSCs or the addition of GD1a in the differentiation medium favored osteogenesis, providing a remarkable increase of alkaline phosphatase. It was also observed that ganglioside GD2, although detectable in hBMSCs by immunohistochemistry with an anti-GD2 antibody, could not be recognized by chemical analysis, likely reflecting a case, not uncommon, of molecular mimicry.

Published

2014

30. Skeletal Muscle Proteomic Profile Revealed Gender-Related Metabolic Responses in a Diet-Induced Obesity Animal Model

Author

Manuela Moriggi, Sara Belloli, Pietro Barbacini, Valentina Murtaj, Enrica Torretta, Linda Chaabane, Tamara Canu, Silvia Penati, Maria Luisa Malosio, Antonio Esposito, Cecilia Gelfi, Rosa Maria Moresco, Daniele Capitanio, Moriggi, M, Belloli, S, Barbacini, P, Murtaj, V, Torretta, E, Chaabane, L, Canu, T, Penati, S, Malosio, M, Esposito, A, Gelfi, C, Moresco, R, and Capitanio, D

Subjects

Male, Proteomics, obesity, Sarcopenia, QH301-705.5, Diet, High-Fat, Article, MED/50 - SCIENZE TECNICHE MEDICHE APPLICATE, Mice, Sex Factors, Tandem Mass Spectrometry, insulin resistance, Animals, Insulin, Biology (General), skeletal muscle, Muscle, Skeletal, QD1-999, Proteomic, proteomics, sarcopenia, Mice, Inbred C57BL, Chemistry, Disease Models, Animal, Oxidative Stress, Glucose, Diabetes Mellitus, Type 2, Female, Chromatography, Liquid

Abstract

Obesity is a chronic, complex pathology associated with a risk of developing secondary pathologies, including cardiovascular diseases, cancer, type 2 diabetes (T2DM) and musculoskeletal disorders. Since skeletal muscle accounts for more than 70% of total glucose disposal, metabolic alterations are strictly associated with the onset of insulin resistance and T2DM. The present study relies on the proteomic analysis of gastrocnemius muscle from 15 male and 15 female C56BL/J mice fed for 14 weeks with standard, 45% or 60% high-fat diets (HFD) adopting a label-free LC-MS/MS approach followed by bioinformatic pathway analysis. Results indicate changes in males due to HFD, with increased muscular stiffness (Col1a1, Col1a2, Actb), fiber-type switch from slow/oxidative to fast/glycolytic (decreased Myh7, Myl2, Myl3 and increased Myh2, Mylpf, Mybpc2, Myl1), increased oxidative stress and mitochondrial dysfunction (decreased respiratory chain complex I and V and increased complex III subunits). At variance, females show few alterations and activation of compensatory mechanisms to counteract the increase of fatty acids. Bioinformatics analysis allows identifying upstream molecules involved in regulating pathways identified at variance in our analysis (Ppargc1a, Pparg, Cpt1b, Clpp, Tp53, Kdm5a, Hif1a). These findings underline the presence of a gender-specific response to be considered when approaching obesity and related comorbidities.

Published

2021

31. Muscle Proteomic Profile before and after Enzyme Replacement Therapy in Late-Onset Pompe Disease

Author

Cinzia Bragato, Enrica Torretta, Cecilia Gelfi, Maurizio Moggio, Lorenzo Maggi, Marina Mora, Patrizia Sartori, Daniele Capitanio, Pietro Barbacini, Manuela Moriggi, Moriggi, M, Capitanio, D, Torretta, E, Barbacini, P, Bragato, C, Sartori, P, Moggio, M, Maggi, L, Mora, M, and Gelfi, C

Subjects

Male, Proteome, Muscle Proteins, lcsh:Chemistry, Tandem Mass Spectrometry, Electrophoresis, Gel, Two-Dimensional, lcsh:QH301-705.5, Spectroscopy, mass spectrometry, Glycogen Storage Disease Type II, pompe disease, General Medicine, Enzyme replacement therapy, Recombinant Proteins, Computer Science Applications, medicine.anatomical_structure, Female, Adult, medicine.medical_specialty, congenital, hereditary, and neonatal diseases and abnormalities, autophagy, Difference gel electrophoresis, rare disease, Catalysis, Article, Inorganic Chemistry, sarcopenia, Atrophy, proteomics, Microscopy, Electron, Transmission, Internal medicine, Lysosome, medicine, Humans, Enzyme Replacement Therapy, Physical and Theoretical Chemistry, Muscle, Skeletal, Molecular Biology, business.industry, Organic Chemistry, Autophagy, Skeletal muscle, Proteomic, nutritional and metabolic diseases, medicine.disease, Endocrinology, Proteostasis, lcsh:Biology (General), lcsh:QD1-999, Unfolded protein response, Glucan 1,4-alpha-Glucosidase, business, Lysosomes, Chromatography, Liquid

Abstract

Mutations in the acidic alpha-glucosidase (GAA) coding gene cause Pompe disease. Late-onset Pompe disease (LOPD) is characterized by progressive proximal and axial muscle weakness and atrophy, causing respiratory failure. Enzyme replacement therapy (ERT), based on recombinant human GAA infusions, is the only available treatment, however, the efficacy of ERT is variable. Here we address the question whether proteins at variance in LOPD muscle of patients before and after 1 year of ERT, compared withhealthy age-matched subjects (CTR), reveal a specific signature. Proteins extracted from skeletal muscle of LOPD patients and CTR were analyzed by combining gel based (two-dimensional difference gel electrophoresis) and label-free (liquid chromatography-mass spectrometry) proteomic approaches, and ingenuity pathway analysis. Upstream regulators targeting autophagy and lysosomal tethering were assessed by immunoblotting. 178 proteins were changed in abundance in LOPD patients, 47 of them recovered normal level after ERT. Defects in oxidative metabolism, muscle contractile protein regulation, cytoskeletal rearrangement, and membrane reorganization persisted. Metabolic changes, ER stress and UPR (unfolded protein response) contribute to muscle proteostasis dysregulation with active membrane remodeling (high levels of LC3BII/LC3BI) and accumulation of p62, suggesting imbalance in the autophagic process. Active lysosome biogenesis characterizes both LOPD PRE and POST, unparalleled by molecules involved in lysosome tethering (VAMP8, SNAP29, STX17, and GORASP2) and BNIP3. In conclusion this study reveals a specific signature that suggests ERT prolongation and molecular targets to ameliorate patient’s outcome.

Published

2021

32. Dal pater familias al «buon padre di famiglia» e oltre: un percorso giuridico e di genere tra Italia e Francia

Author

Maestri, Gabriele, Somma, Anna Lisa, Paola Torretta e Veronica Valenti, Maestri, Gabriele, and Somma, Anna Lisa

Published

2021

33. En route to the North: modelling crested porcupine habitat suitability and dispersal flows across a highly anthropized area in northern Italy

Author

Elisa Torretta, Sergio Mantovani, Olivia Dondina, Luciano Bani, Valerio Orioli, Torretta, E, Orioli, V, Bani, L, Mantovani, S, and Dondina, O

Subjects

0106 biological sciences, Range (biology), Woodland, 010603 evolutionary biology, 01 natural sciences, Shrubland, Hystrix cristata, Range expansion, biology.animal, Po River Plain, Ecology, Evolution, Behavior and Systematics, geography, Connectivity, geography.geographical_feature_category, biology, Resistance (ecology), Ecology, 010604 marine biology & hydrobiology, biology.organism_classification, Ensemble model, Animal ecology, Habitat suitability, Biological dispersal, Animal Science and Zoology, Porcupine

Abstract

The crested porcupine (Hystrix cristata) underwent a rapid and widespread range expansion in Italy. Nowadays the species is moving towards the northernmost regions of the country and its occurrence is increasing in the highly anthropized Po Plain. Our objectives were to evaluate the suitability of the Po Plain for the species, as well as to identify dispersal corridors connecting the northern Apennines occurrence areas and the Prealps. We modelled the species home-range scale habitat suitability based on an ensemble modelling approach. Additionally, a habitat suitability prediction carried out at a finer scale was used to parametrize the landscape resistance, based on which we modelled the potential dispersal corridors for the species using a factorial least-cost path approach. The ensemble prediction estimated a potential occurrence of the crested porcupine in 27.4% of the study area. The species occurrence probability was mainly driven by the distribution of extensive cultivations, woodlands and shrublands, and water courses and by the annual mean temperature. Conversely, the movements of the species resulted mainly sustained by woodlands and shrublands and highly hindered by simple arable lands and rice paddies. The connectivity prediction showed that three main dispersal routes are likely to connect crested porcupine occurrence areas in the northern Apennines to currently unoccupied but highly suitable areas in the Prealps. The study allowed us to identify the areas in the Prealps with the highest probability to be colonized by the crested porcupine in the near future and provided important insights for the conservation of a strictly protected species in a human-dominated landscape.

Published

2021

34. Le donne e la rappresentanza politica, tra norme elettorali e regolazione dei partiti

Author

Maestri, Gabriele, Paola Torretta e Veronica Valenti, and Maestri, Gabriele

Published

2021

35. Combining ensemble models and connectivity analyses to predict wolf expected dispersal routes through a lowland corridor

Author

Luciano Bani, Federico Merli, Olivia Dondina, Valerio Orioli, Elisa Torretta, Alberto Meriggi, Dondina, O, Orioli, V, Torretta, E, Merli, F, Bani, L, and Meriggi, A

Subjects

0106 biological sciences, European People, Corridors, Species distribution, Population Dynamics, Endangered species, Marine and Aquatic Sciences, 01 natural sciences, Geographical Locations, Ethnicities, Mammals, education.field_of_study, Connectivity, Multidisciplinary, biology, Eukaryota, Ruminants, Plants, Italian wolf, Italian People, Habitats, Europe, Canis, Geography, Habitat, Italy, Experimental Organism Systems, Vertebrates, Medicine, Research Article, Freshwater Environments, BIO/05 - ZOOLOGIA, Science, Population, Animals, Wild, Research and Analysis Methods, 010603 evolutionary biology, Models, Biological, Rivers, Plant and Algal Models, Genetics, Animals, Ecosystem, Grasses, education, Evolutionary Biology, Wolves, Population Biology, 010604 marine biology & hydrobiology, Deer, Endangered Species, Ecology and Environmental Sciences, Canis lupus italicu, Organisms, Biology and Life Sciences, Aquatic Environments, Bodies of Water, biology.organism_classification, Amniotes, People and Places, Earth Sciences, Animal Studies, Biological dispersal, Population Groupings, Physical geography, Rice, Population Genetics

Abstract

The Italian wolf (Canis lupus italicus) population has remained isolated South of the Alps for the last few thousand years. After a strong decline, the species has recolonized the Apennines and the Western Alps, while it is currently struggling to colonize the Eastern Alps. Recently, the species was detected in a lowland park connecting the Northern Apennines to the Central Alps. If the park was able to sustain a net wolf dispersal flow, this could significantly boost the connection with the Eastern Alps and the Dinaric-Balkan population. We investigated the suitability of the park as a functional ecological corridor for the wolf through the unhospitable lowland of Northern Italy. We collected wolf occurrence data in two study areas. We modeled species distribution running a separate ensemble model for each study area and then merging the output of the models to obtain an integrated suitability map. We used this map to identify corridors for the wolf adopting a factorial least-cost path and a cumulative resistant kernel approach. The connectivity models showed that only two corridors exist in the lowland areas between the Northern Apennines and the Central Alps. The Western corridor is a blind route, while the eastern corridor passes through the park and has a continuous course. However, the models also revealed a scarce resilience of corridor connectivity in the passageways between the park and the Apennines and the Prealps, which suggests that urgent management actions are necessary to ensure the future functionality of this important corridor.

Published

2020

36. Sprague Dawley rats: A model of successful heart aging

Author

Enrica Torretta, Cecilia Gelfi, Roberta Leone, Daniele Capitanio, Chiara Fania, Capitanio, D, Leone, R, Fania, C, Torretta, E, and Gelfi, C

Subjects

0301 basic medicine, medicine.medical_specialty, Successful aging, Special Section: Proceedings of the 9th Annual EuPA Congress “Proteomics - Back to the Future” (June 23 - 28, 2015, Milano, Italy), Aldehyde dehydrogenase, Heart proteome, 030204 cardiovascular system & hematology, Biology, Biochemistry, 03 medical and health sciences, 0302 clinical medicine, 2-D DIGE, Internal medicine, medicine, Sprague dawley rats, Animal model, ComputingMethodologies_COMPUTERGRAPHICS, Mass spectrometry, Autophagy, medicine.disease, Molecular biology, Sprague dawley, 030104 developmental biology, Endocrinology, Mitochondrial permeability transition pore, Heart failure, biology.protein, Mitochondrial fission

Abstract

Graphical abstract, Highlights • Sprague Dawley rat hearts of 6, 22 and 30 months were analysed by DIGE and blotting. • Results indicate that this animal model experiences the so-called successful aging. • Mybpc3, Aldh2 and serpins could be used as early biomarkers. • Sirtuin-3 increment suggests the activation of protective non-canonical autophagy., Aging is a universal phenomenon involving the whole body and is characterized by metabolic and physiological decline, leading to cardiovascular defects and heart failure. To characterize the molecular basis of physiological cardiac aging, the proteomic profiles of Sprague Dawley rat hearts of 6, 22 and 30 months were analysed by DIGE and immunoblotting. Results indicate changes in myosin binding protein C, aldehyde dehydrogenase, serpins and sirtuin-3 which protects from the opening of the mitochondrial permeability transition pore induced by cyclophilin D increment. Conversely, an increase of fusion, a decrease of mitochondrial fission and the activation of the non-canonical autophagy pathway were observed. These results support the hypothesis of successful aging in this rat model.

Published

2016

37. Specific protein changes contribute to the differential muscle mass loss during ageing

Author

Cecilia Gelfi, Michele Vasso, Patrizia Procacci, Sara De Palma, Daniele Capitanio, Enrica Torretta, Francesco Paolo Cammarata, Chiara Fania, Valerio Magnaghi, Capitanio, D, Vasso, M, De Palma, S, Fania, C, Torretta, E, Cammarata, F, Magnaghi, V, Procacci, P, and Gelfi, C

Subjects

Male, Proteomics, 0301 basic medicine, Aging, Respiratory chain, Muscle Proteins, Hindlimb, Muscle Protein, Muscle proteome, Biology, Biochemistry, Rats, Sprague-Dawley, Two-Dimensional Difference Gel Electrophoresis, Muscle ageing, 03 medical and health sciences, Gastrocnemius muscle, chemistry.chemical_compound, Muscular Diseases, Myosin, Autophagy, medicine, Animals, Muscle, Skeletal, Molecular Biology, Tissue homeostasis, Myosin Heavy Chains, Mass spectrometry, Animal, Muscular Disease, Myosin Heavy Chain, Two-Dimensional Difference Gel Electrophoresi, Proteomic, Skeletal muscle, Animal proteomics, Intermediate metabolism, Mitochondria, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Myoglobin, chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, 2D-DIGE, Animal proteomic, Forelimb

Abstract

In the skeletal muscle, the ageing process is characterized by a loss of muscle mass and strength, coupled with a decline of mitochondrial function and a decrease of satellite cells. This profile is more pronounced in hindlimb than in forelimb muscles, both in humans and in rodents. Utilizing light and electron microscopy, myosin heavy chain isoform distribution, proteomic analysis by 2D-DIGE, MALDI-TOF MS and quantitative immunoblotting, this study analyzes the protein levels and the nuclear localization of specific molecules, which can contribute to a preferential muscle loss. Our results identify the molecular changes in the hindlimb (gastrocnemius) and forelimb (triceps) muscles during ageing in rats (3- and 22-month-old). Specifically, the oxidative metabolism contributes to tissue homeostasis in triceps, whereas respiratory chain disruption and oxidative-stress-induced damage imbalance the homeostasis in gastrocnemius muscle. High levels of dihydrolipoyllysine-residue acetyltransferase (Dlat) and ATP synthase subunit alpha (Atp5a1) are detected in triceps and gastrocnemius, respectively. Interestingly, in triceps, both molecules are increased in the nucleus in aged rats and are associated to an increased protein acetylation and myoglobin availability. Furthermore, autophagy is retained in triceps whereas an enhanced fusion, decrement of mitophagy and of regenerative potential is observed in aged gastrocnemius muscle.

Published

2016

38. Intermediate and low abundant protein analysis of vitamin D deficient obese and non-obese subjects by MALDI-profiling

Author

Daniele Capitanio, Enrica Torretta, Cecilia Gelfi, Franca Rosa Guerini, Shaun Sabico, Nasser M. Al-Daghri, Mario Clerici, Chiara Fania, Al-Daghri, N, Torretta, E, Capitanio, D, Fania, C, Guerini, F, Sabico, S, Clerici, M, and Gelfi, C

Subjects

0301 basic medicine, Adult, Blood Glucose, Male, medicine.medical_specialty, BIO/12 - BIOCHIMICA CLINICA E BIOLOGIA MOLECOLARE CLINICA, Apolipoprotein B, lcsh:Medicine, 030204 cardiovascular system & hematology, Biology, vitamin D deficiency, Article, Body Mass Index, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, Diabetes mellitus, medicine, Vitamin D and neurology, Humans, Obesity, Vitamin D, lcsh:Science, Triglycerides, Aged, 2. Zero hunger, Multidisciplinary, vitamin D, obesity, MALDI-profiling, lcsh:R, Lipid metabolism, Blood Proteins, Middle Aged, medicine.disease, Lipid Metabolism, Vitamin D Deficiency, 3. Good health, 030104 developmental biology, Endocrinology, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, biology.protein, lcsh:Q, Female, Metabolic syndrome, Body mass index

Abstract

Obesity is a pathological condition caused by genetic and environmental factors, including vitamin D deficiency, which increases the risk of developing cardiovascular disorders and diabetes. This case-control study was designed to verify whether serum profiles could be identified differentiating obese and non-obese Saudis characterized by vitamin D deficiency and pathological levels of triglycerides, high-density lipoprotein cholesterol and high total cholesterol levels. The serum protein profiles of 64 vitamin D deficient (serum 25(OH)D vs. non-obese subjects identified 14 changed peaks (p

Published

2017

39. Time partitioning in mesocarnivore communities from different habitats of NW Italy: Insights into martens' competitive abilities

Author

M. Serafini, F. Puopolo, Pietro Tirozzi, A. Mosini, E. Torretta, Alessandro Balestrieri, Nicola Saino, M. Piana, Torretta, E, Mosini, A, Piana, M, Tirozzi, P, Serafini, M, Puopolo, F, Saino, N, and Balestrieri, A

Subjects

0106 biological sciences, biology, Badger, Vulpes, Ecology, camera-trapping, media_common.quotation_subject, community-level interaction, coexistence, interference, activity pattern, Meles, biology.organism_classification, 010603 evolutionary biology, 01 natural sciences, Competition (biology), 010601 ecology, Behavioral Neuroscience, Habitat, biology.animal, Cathemerality, Animal Science and Zoology, Mesocarnivore, Marten, media_common

Abstract

Most studies focused on species coexistence have been directed at the differential use of habitat and food resources; nonetheless, the differential use of the diel cycle may enhance the coexistence of same-sized species. We investigated the activity patterns of mesocarnivores (red fox (Vulpes vulpes), European badger (Meles meles), pine marten (Martes martes), stone marten (M. foina)) in NW Italy via camera-trapping. We hypothesized that the smallest species would tend to avoid competition by selecting time periods when larger species were less active. Foxes, badgers, and stone martens were mainly nocturnal. In lowland areas overlap between coexisting species was generally low, while in Mediterranean habitats all activity patterns tended to be unimodal and overlap was generally high. The pine marten showed a cathemeral pattern. We suggest that the lower ability of the stone marten to avoid interference competition at community-level may play a major role in determining its widespread exclusion from forested areas by the pine marten.

Published

2017

40. Collagen VI null mice as a model for early onset muscle decline in aging

Author

Daniele Capitanio, Manuela Moriggi, Sara De Palma, Dario Bizzotto, Sibilla Molon, Enrica Torretta, Chiara Fania, Paolo Bonaldo, Cecilia Gelfi, Paola Braghetta, Capitanio, D, Moriggi, M, De Palma, S, Bizzotto, D, Molon, S, Torretta, E, Fania, C, Bonaldo, P, Gelfi, C, and Braghetta, P

Subjects

0301 basic medicine, medicine.medical_specialty, Connective tissue, Aging muscle proteome, Autophagy, Collagen VI, Lipotoxicity, Skeletal muscle, Molecular Biology, Cellular and Molecular Neuroscience, Biology, lcsh:RC321-571, 03 medical and health sciences, 0302 clinical medicine, Internal medicine, medicine, Glycolysis, lcsh:Neurosciences. Biological psychiatry. Neuropsychiatry, Original Research, Diaphragm (structural system), Fatty acid synthase, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, biology.protein, 030217 neurology & neurosurgery, Neuroscience

Abstract

Collagen VI is an extracellular matrix (ECM) protein playing a key role in skeletal muscles and whose deficiency leads to connective tissue diseases in humans and in animal models. However, most studies have been focused on skeletal muscle features. We performed an extensive proteomic profiling in two skeletal muscles (diaphragm and gastrocnemius) of wild-type and collagen VI null (Col6a1−/−) mice at different ages, from 6- (adult) to 12- (aged) month-old to 24 (old) month-old. While in wild-type animals the number of proteins and the level of modification occurring during aging were comparable in the two analyzed muscles, Col6a1−/− mice displayed a number of muscle-type specific variations. In particular, gastrocnemius displayed a limited number of dysregulated proteins in adult mice, while in aged muscles the modifications were more pronounced in terms of number and level. In diaphragm, the differences displayed by 6-month-old Col6a1−/− mice were more pronounced compared to wild-type mice and persisted at 12 months of age. In adult Col6a1−/− mice, the major variations were found in the enzymes belonging to the glycolytic pathway and the tricarboxylic acid (TCA) cycle, as well as in autophagy-related proteins. When compared to wild-type animals Col6a1−/− mice displayed a general metabolic rewiring which was particularly prominent the diaphragm at 6 months of age. Comparison of the proteomic features and the molecular analysis of metabolic and autophagic pathways in adult and aged Col6a1−/− diaphragm indicated that the effects of aging, culminating in lipotoxicity and autophagic impairment, were already present at 6 months of age. Conversely, the effects of aging in Col6a1−/− gastrocnemius were similar but delayed becoming apparent at 12 months of age. A similar metabolic rewiring and autophagic impairment was found in the diaphragm of 24-month-old wild-type mice, confirming that fatty acid synthase (FASN) increment and decreased microtubule-associated proteins 1A/1B light chain 3B (LC3B) lipidation are hallmarks of the aging process. Altogether these data indicate that the diaphragm of Col6a1−/− animal model can be considered as a model of early skeletal muscle aging.

Published

2017

41. HPTLC-MALDI MS for (glyco)sphingolipid multiplexing in tissues and blood: A promising strategy for biomarker discovery and clinical applications

Author

Enrica, Torretta, Chiara, Fania, Michele, Vasso, Cecilia, Gelfi, Torretta, E, Fania, C, Vasso, M, and Gelfi, C

Subjects

Animal, Hydrolysis, HPTLC-MALDI MS, Brain, Biomarker, Hydrolysi, Glycosphingolipids, Multiplexing, Sphingolipid, Mice, Inbred C57BL, Mice, Ganglioside, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Animals, Chromatography, Thin Layer, Muscle, Skeletal, Biomarkers, Glycosphingolipid

Abstract

Sphingolipids have hydrophilic and hydrophobic properties, different saturation and combination of the oligosaccharide chains and mass homology of species located in a narrow m/z region hampering their recognition. To target sphingolipids for diagnostic purposes, standardized methods for lipid extraction, quali- and quantitative assessments are required. In this study, HPTLC-MALDI MS was adopted to establish sphingolipid and glycosphingolipid profiles in muscle, brain and serum to create a database of molecules to be searched in the preclinical and clinical investigations. Specific protocols for lipid extraction were set up based on the characteristics of the tissue or/and fluids; this approach maximizes the HPTLC-MALDI MS analytical throughput both for lipids extracted in organic and aqueous phase. This study indicates that alkaline hydrolysis is necessary for the detection of low abundant species such as Gb3Cer and ceramides in serum and Gb4Cer, CerP and HexCer in muscle tissue. The high hydrophobicity of ceramides has been overcome by the development of HPTLC plate in chloroform:methanol/50:3.5, which increases the number and the intensity of low abundant Cer species. MS/MS analysis has been conducted directly on HPTLC plate allowing the molecular recognition; furthermore a dataset of spectra was acquired to create a database for future profiling of these molecules.

Published

2016

42. Setup for human sera MALDI profiling: The case of rhEPO treatment

Author

Gaetano Cairo, Michele Vasso, Enrica Torretta, Carsten Lundby, Cecilia Gelfi, Paul Robach, Chiara Fania, Fania, C, Vasso, M, Torretta, E, Robach, P, Cairo, G, Lundby, C, and Gelfi, C

Subjects

Male, Clinical Biochemistry, Biology, Biochemistry, Serum profiling, Analytical Chemistry, 03 medical and health sciences, 0302 clinical medicine, Blood Protein, Principal Component Analysi, Humans, Electrophoresis, Gel, Two-Dimensional, Sample dilution, Erythropoietin, Immunosorbent Techniques, 030304 developmental biology, Principal Component Analysis, 0303 health sciences, Chromatography, Healthy subjects, Blood Proteins, Recombinant Protein, Immunosorbent Technique, Recombinant Proteins, Complex protein, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, 030220 oncology & carcinogenesis, Electrophoresis, Polyacrylamide Gel, Drug Monitoring, Human

Abstract

The implementation of high-throughput technologies based on qualitative and quantitative methodologies for the characterization of complex protein mixtures is increasingly required in clinical laboratories. MALDI profiling is a robust and sensitive technology although the serum high dynamic range imposes a major limitation hampering the identification of less abundant species decreasing the quality of MALDI profiling. A setup to improve these parameters has been performed for recombinant human erythropoietin (rhEPO) monitoring in serum, analyzing the effects of two commercially available columns (MARS Hu7 and Hu14) for immunodepletion, and two matrices (α-cyano-4-hydroxycinnamic acid and 2',4'-dihydroxyacetophenone) for peak quality improvement. The immunodepletion capability of both columns was determined by 2-D DIGE, which precisely revealed the efficacy of Hu14 in protein removal and the serum dynamic range decrement. In addition, the type of matrix, the sample dilution, and the efficacy of optimized parameters were used for serum profiling of ten healthy subjects before and after rhEPO treatment. The principal component analysis indicates that a combination of Hu14 column and 2',4'-dihydroxyacetophenone matrix increases data quality allowing the discrimination between treated and untreated samples, making serum MALDI profiling suitable for clinical monitoring of rhEPO.

Published

2011

43. Protein signature in cerebrospinal fluid and serum of Alzheimer’s disease patients: The case of apolipoprotein A-1 proteoforms

Author

Beatrice Arosio, Cecilia Gelfi, Daniele Capitanio, Enrica Torretta, Chiara Fania, Daniela Mari, Evelyn Ferri, Cristina Gussago, Fania, C, Arosio, B, Capitanio, D, Torretta, E, Gussago, C, Ferri, E, Mari, D, and Gelfi, C

Subjects

Male, 0301 basic medicine, Serum Proteins, BIO/12 - BIOCHIMICA CLINICA E BIOLOGIA MOLECOLARE CLINICA, Apolipoprotein B, Physiology, lcsh:Medicine, Nervous System, Biochemistry, 0302 clinical medicine, Cerebrospinal fluid, Medicine and Health Sciences, Electrophoresis, Gel, Two-Dimensional, Phosphorylation, lcsh:Science, Cerebrospinal Fluid, Aged, 80 and over, Principal Component Analysis, Multidisciplinary, biology, Neurodegenerative Diseases, Blood proteins, Body Fluids, Neurology, Area Under Curve, Proteome, Female, Anatomy, CSF, Apolipoprotein AI, MALDI-profiling, proteomics, Alzheimer's disease, iNPH, Alzheimer's disease, Hydrocephalus, Research Article, Gene isoform, Lipoproteins, Enzyme-Linked Immunosorbent Assay, tau Proteins, Statistics, Nonparametric, 03 medical and health sciences, Alzheimer Disease, Diagnostic Medicine, Mental Health and Psychiatry, medicine, Humans, Dementia, Aged, Amyloid beta-Peptides, Apolipoprotein A-I, lcsh:R, Case-control study, Biology and Life Sciences, Proteins, medicine.disease, Peptide Fragments, Apolipoproteins, 030104 developmental biology, ROC Curve, Case-Control Studies, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, Immunology, biology.protein, lcsh:Q, Peptides, Biomarkers, 030217 neurology & neurosurgery

Abstract

In the diagnosis of Alzheimer’s disease (AD) total tau (T-tau), tau phosphorylated at threonine 181 (P-tau181), and the 42 amino acid isoform of alpha β-amyloid (Aβ) are well established surrogate CSF markers. However, there is a constant need for new diagnostic markers to identify the disease at a very early stage. The identification of new molecules for AD diagnosis and monitoring in CSF is hampered by several “confounding” factors including intra- and inter-individual, pre-analytical and analytical variabilities. In an attempt to partially overcome patient’s variability and to determine new molecules significantly dysregulated in CSF, we assessed the proteome profile of low molecular weight protein species in CSF and serum of the same patients. CSFs and sera from 36 ADs, 32 iNPHs (idiopathic normal pressure hydrocephalus) and 12 controls were compared by MALDI profiling (non-parametric statistics, CV0.750). After protein identification by mass spectrometry, the proteoform composition was assessed by 2-D DIGE/MS. Results indicated that CSF of iNPH can be used as control. Serum and CSF of AD patients shows a specific protein profile compared to iNPH samples. A variation (p

Published

2017

44. A PSA-guided approach for a better diagnosis of prostatic adenocarcinoma based on MALDI profiling and peptide identification

Author

Roberta Leone, Cecilia Gelfi, Adriana Albini, Antonino Bruno, Michele Vasso, Enrica Torretta, Chiara Fania, Paolo Consonni, Ilaria Sogno, Fania, C, Sogno, I, Vasso, M, Torretta, E, Leone, R, Bruno, A, Consonni, P, Albini, A, and Gelfi, C

Subjects

PCA3, Oncology, Male, medicine.medical_specialty, Clinical tests, Immunodepletion, Clinical Biochemistry, Peptide, Adenocarcinoma, urologic and male genital diseases, Bioinformatics, Biochemistry, Prostate cancer, Antigen, Internal medicine, Small peptide, medicine, MALDI profiling, Humans, fImmunodepletion, False Negative Reactions, Aged, chemistry.chemical_classification, Aged, 80 and over, Prostatic adenocarcinoma, business.industry, Biochemistry (medical), Complement C3, fImmunodepletion, MALDI profiling, Prostate cancer, Prostate-specific antigen, Prostatic Neoplasms, General Medicine, Complement C3, Middle Aged, Prostate-Specific Antigen, medicine.disease, Prostate-specific antigen, Complement C3f, chemistry, Spectrometry, Mass, Matrix-Assisted Laser Desorption-Ionization, business

Abstract

Background: Prostate cancer (PCa) is the second cause of mortality in men worldwide. The prostate-specific antigen (PSA) test is routinely adopted in diagnosis; nevertheless more reliable biomarkers are continuously under investigation by monitoring the release of molecules into the bloodstream. The serum protein profiles appear to provide cancer-specific fingerprints that help to discriminate patients (especially with low PSA level) from controls, improving the performance of existing clinical tests. Methods: Samples from healthy controls and PCa patients with low (≤. 4. ng/mL) and high PSA (>. 4. ng/mL) levels were analyzed by MALDI profiling, and by a multi fractionation approach coupled to ESI-MS for peaks identification. Results: MALDI profiling achieved to detect 10 and 14 changed peaks (p-value

Published

2014

45. Effects of Pulsed Electromagnetic Field Treatment on Skeletal Muscle Tissue Recovery in a Rat Model of Collagenase-Induced Tendinopathy: Results from a Proteome Analysis.

Author

Torretta E, Moriggi M, Capitanio D, Orfei CP, Raffo V, Setti S, Cadossi R, de Girolamo L, and Gelfi C

Subjects

Animals, Rats, Male, YAP-Signaling Proteins metabolism, Proteomics methods, Glycolysis, Electromagnetic Fields, Tendinopathy therapy, Tendinopathy metabolism, Tendinopathy chemically induced, Muscle, Skeletal metabolism, Muscle, Skeletal radiation effects, Rats, Sprague-Dawley, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha metabolism, Proteome metabolism, Collagenases metabolism, Disease Models, Animal, Magnetic Field Therapy methods

Abstract

Tendon disorders often result in decreased muscle function and atrophy. Pulsed Electromagnetic Fields (PEMFs) have shown potential in improving tendon fiber structure and muscle recovery. However, the molecular effects of PEMF therapy on skeletal muscle, beyond conventional metrics like MRI or markers of muscle decline, remain largely unexplored. This study investigates the metabolic and structural changes in PEMF-treated muscle tissue using proteomics in a rat model of Achilles tendinopathy induced by collagenase. Sprague Dawley rats were unilaterally induced for tendinopathy with type I collagenase injection and exposed to PEMFs for 8 h/day. Gastrocnemius extracts from untreated or PEMF-treated rats were analyzed with LC-MS/MS, and proteomics differential analysis was conducted through label-free quantitation. PEMF-treated animals exhibited decreased glycolysis and increased LDHB expression, enhancing NAD signaling and ATP production, which boosted respiratory chain activity and fatty acid beta-oxidation. Antioxidant protein levels increased, controlling ROS production. PEMF therapy restored PGC1alpha and YAP levels, decreased by tendinopathy. Additionally, myosins regulating slow-twitch fibers and proteins involved in fiber alignment and force transmission increased, supporting muscle recovery and contractile function. Our findings show that PEMF treatment modulates NAD signaling and oxidative phosphorylation, aiding muscle recovery through the upregulation of YAP and PGC1alpha and increasing slow myosin isoforms, thus speeding up physiological recovery.

Published

2024

46. Characterization of Proteome Changes in Aged and Collagen VI-Deficient Human Pericyte Cultures.

Author

Moriggi M, Torretta E, Cescon M, Russo L, Gregorio I, Braghetta P, Sabatelli P, Faldini C, Merlini L, Gargioli C, Bonaldo P, Gelfi C, and Capitanio D

Subjects

Humans, Cells, Cultured, Adult, Middle Aged, Aged, Aging metabolism, Proteomics methods, Male, Female, Oxidative Stress, Cell Differentiation, Pericytes metabolism, Collagen Type VI metabolism, Collagen Type VI genetics, Proteome metabolism

Abstract

Pericytes are a distinct type of cells interacting with endothelial cells in blood vessels and contributing to endothelial barrier integrity. Furthermore, pericytes show mesenchymal stem cell properties. Muscle-derived pericytes can demonstrate both angiogenic and myogenic capabilities. It is well known that regenerative abilities and muscle stem cell potential decline during aging, leading to sarcopenia. Therefore, this study aimed to investigate the potential of pericytes in supporting muscle differentiation and angiogenesis in elderly individuals and in patients affected by Ullrich congenital muscular dystrophy or by Bethlem myopathy, two inherited conditions caused by mutations in collagen VI genes and sharing similarities with the progressive skeletal muscle changes observed during aging. The study characterized pericytes from different age groups and from individuals with collagen VI deficiency by mass spectrometry-based proteomic and bioinformatic analyses. The findings revealed that aged pericytes display metabolic changes comparable to those seen in aging skeletal muscle, as well as a decline in their stem potential, reduced protein synthesis, and alterations in focal adhesion and contractility, pointing to a decrease in their ability to form blood vessels. Strikingly, pericytes from young patients with collagen VI deficiency showed similar characteristics to aged pericytes, but were found to still handle oxidative stress effectively together with an enhanced angiogenic capacity.

Published

2024

47. Nitrosative Stress in Astronaut Skeletal Muscle in Spaceflight.

Author

Blottner D, Moriggi M, Trautmann G, Furlan S, Block K, Gutsmann M, Torretta E, Barbacini P, Capitanio D, Rittweger J, Limper U, Volpe P, Gelfi C, and Salanova M

Abstract

Long-duration mission (LDM) astronauts from the International Space Station (ISS) (>180 ISS days) revealed a close-to-normal sarcolemmal nitric oxide synthase type-1 (NOS1) immunoexpression in myofibers together with biochemical and quantitative qPCR changes in deep calf soleus muscle. Nitro-DIGE analyses identified functional proteins (structural, metabolic, mitochondrial) that were over-nitrosylated post- vs. preflight. In a short-duration mission (SDM) astronaut (9 ISS days), s-nitrosylation of a nodal protein of the glycolytic flux, specific proteins in tricarboxylic acid (TCA) cycle, respiratory chain, and over-nitrosylation of creatine kinase M-types as signs of impaired ATP production and muscle contraction proteins were seen. S-nitrosylation of serotransferrin (TF) or carbonic anhydrase 3 (CA3b and 3c) represented signs of acute response microgravity muscle maladaptation. LDM nitrosoprofiles reflected recovery of mitochondrial activity, contraction proteins, and iron transporter TF as signs of muscle adaptation to microgravity. Nitrosated antioxidant proteins, alcohol dehydrogenase 5/S-nitrosoglutathione reductase (ADH5/GSNOR), and selenoprotein thioredoxin reductase 1 (TXNRD1) levels indicated signs of altered redox homeostasis and reduced protection from nitrosative stress in spaceflight. This work presents a novel spaceflight-generated dataset on s-nitrosylated muscle protein signatures from astronauts that helps both to better understand the structural and molecular networks associated to muscular nitrosative stress and to design countermeasures to dysfunction and impaired performance control in human spaceflight missions.

Published

2024

48. GBA1 inactivation in oligodendrocytes affects myelination and induces neurodegenerative hallmarks and lipid dyshomeostasis in mice.

Author

Gregorio I, Russo L, Torretta E, Barbacini P, Contarini G, Pacinelli G, Bizzotto D, Moriggi M, Braghetta P, Papaleo F, Gelfi C, Moro E, and Cescon M

Subjects

Animals, Mice, alpha-Synuclein metabolism, Animals, Genetically Modified metabolism, Glucosylceramidase genetics, Glucosylceramidase metabolism, Lipids, Mutation, Gaucher Disease genetics, Gaucher Disease metabolism, Parkinson Disease metabolism

Abstract

Background: Mutations in the β-glucocerebrosidase (GBA1) gene do cause the lysosomal storage Gaucher disease (GD) and are among the most frequent genetic risk factors for Parkinson's disease (PD). So far, studies on both neuronopathic GD and PD primarily focused on neuronal manifestations, besides the evaluation of microglial and astrocyte implication. White matter alterations were described in the central nervous system of paediatric type 1 GD patients and were suggested to sustain or even play a role in the PD process, although the contribution of oligodendrocytes has been so far scarcely investigated., Methods: We exploited a system to study the induction of central myelination in vitro, consisting of Oli-neu cells treated with dibutyryl-cAMP, in order to evaluate the expression levels and function of β-glucocerebrosidase during oligodendrocyte differentiation. Conduritol-B-epoxide, a β-glucocerebrosidase irreversible inhibitor was used to dissect the impact of β-glucocerebrosidase inactivation in the process of myelination, lysosomal degradation and α-synuclein accumulation in vitro. Moreover, to study the role of β-glucocerebrosidase in the white matter in vivo, we developed a novel mouse transgenic line in which β-glucocerebrosidase function is abolished in myelinating glia, by crossing the Cnp1-cre mouse line with a line bearing loxP sequences flanking Gba1 exons 9-11, encoding for β-glucocerebrosidase catalytic domain. Immunofluorescence, western blot and lipidomic analyses were performed in brain samples from wild-type and knockout animals in order to assess the impact of genetic inactivation of β-glucocerebrosidase on myelination and on the onset of early neurodegenerative hallmarks, together with differentiation analysis in primary oligodendrocyte cultures., Results: Here we show that β-glucocerebrosidase inactivation in oligodendrocytes induces lysosomal dysfunction and inhibits myelination in vitro. Moreover, oligodendrocyte-specific β-glucocerebrosidase loss-of-function was sufficient to induce in vivo demyelination and early neurodegenerative hallmarks, including axonal degeneration, α-synuclein accumulation and astrogliosis, together with brain lipid dyshomeostasis and functional impairment., Conclusions: Our study sheds light on the contribution of oligodendrocytes in GBA1-related diseases and supports the need for better characterizing oligodendrocytes as actors playing a role in neurodegenerative diseases, also pointing at them as potential novel targets to set a brake to disease progression., (© 2024. The Author(s).)

Published

2024

49. Changes in Wolf Occupancy and Feeding Habits in the Northern Apennines: Results of Long-Term Predator-Prey Monitoring.

Author

Torretta E, Brangi A, and Meriggi A

Abstract

The comprehension of the factors that have influenced the recent changes in wolf ( Canis lupus ) range and diet that have occurred in our study area, characterized by a highly heterogeneous landscape, can shed light on their current process of expansion toward the plain. Wolf presence was monitored using a standardized protocol from 2007 to 2022 by carrying out eight monitoring sessions organized in seasonal surveys, during which, we collected wolf presence data. To model wolf range dynamics, we used dynamic occupancy models considering land cover types and wild ungulate abundances as covariates. Moreover, we studied the wolf diet through scat analysis, identifying the consumed items from undigested remains. Wolf occupancy in the study area progressed from mountains to lower hills gradually; the observed range dynamics were driven by prey abundance and human presence: in particular, the probability of colonization increased with roe deer ( Capreolus capreolus ) abundance, whereas the probability of extinction increased with urban areas. The wolf diet showed a gradual shift from the prevalent consumption of wild boar (2007-2008 and 2011-2012) to the prevalent consumption of roe deer (continuously increasing from 2015 onward). Our results might be related to a specific adaptation of the predator to the local ecology of the most consumed species: the roe deer.

Published

2024

50. Safety of blood reinfusion drains after local infiltration analgesia in total joint replacement.

Author

Legnani C, Torretta E, Attanasio M, Gelfi C, Parente F, Ventura A, and Oriani G

Subjects

Humans, Analgesia methods, Anesthetics, Local, Levobupivacaine, Arthroplasty, Replacement, Hip, Arthroplasty, Replacement, Knee, Drainage adverse effects

Abstract

Background: Local infiltration analgesia (LIA) is frequently administered to patient undergoing joint replacement surgical procedures. The aim of the present research was to verify the safety of collected shed blood to be reinfused postoperatively, by measuring levobupivacaine levels in drainage blood in patients undergoing LIA during knee replacement surgery., Patients and Methods: 24 patients who underwent total knee arthroplasty (TKA) and 12 scheduled for total hip arthroplasty (THA) who received intraoperative LIA were considered. Blood samples were collected from shed blood which was present in drainage 2 and 5 hours after surgery and serum was analysed by liquid chromatography-tandem mass spectrometry., Results: At 2 hours postoperatively, the median levobupivacaine serum concentration in the collected shed blood was 1.2 mg/L (SD: 4.2) for TKA and 17.13 mg/L (SD: 24.4) for THA. At 5 hours, levobupivacaine concentration was 1.84 mg/L (SD: 2.2) for TKA and 17.5 mg/L (SD: 25.2) for THA. Higher values of average serum levobupivacaine concentration were reported in drains collected from patients who had undergone THA compared to TKA (p<0.001). BMI significantly influenced levels of serum drug, that resulted to be higher in patients with BMI<25 (p= 0.01)., Conclusion: Levobupivacaine from collected shed blood that would have been returned to the patient, was below toxicity level at 2 and 5 hours after LIA during total joint replacement. The average serum levobupivacaine concentration was found to be higher in drains taken from THA patients than TKA patients. Patients with lower BMI demonstrated the highest levels of levobupivacaine in shed blood and a lower blood volume needed for central nervous system toxicity. Therefore, in patients with a lower BMI undergoing THA, anaesthetic dosage should be reduced or autotransfusion should be avoided to prevent potential risks of toxicity., (© 2024. The Author(s).)

Published

2024