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103. ALK determination: Liquid and tissue biopsy. Comparing techniques and effectiveness of alectinib in a controversial clinical case [Determinazione di ALK: Tra biopsia liquida e tissutale. Tecniche a confronto ed efficacia di alectinib in un caso clinico controverso]

Author

Cortinovis D., Migliorati F., Pagni F., Cortinovis, D, Migliorati, F, and Pagni, F

Subjects
ALK, Crizotinib, FISH, Liquid biopsy, Tyrosin kinase inhibitor, NGS, Driver mutation, Tyrosin kinase inhibitors, Alectinib, NSCLC, Target therapy, TKI
Abstract

The next generation sequencing (NGS) applied to liquid biopsy is useful to determine the biomolecular identity of the prevalent neoplastic cell population. The sensitivity of ALK detection in liquid biopsy is comparable to that showed by the gold standard tissue biopsy and its usefulness is demonstrated in clinical practice by the similar efficacy of ALK TKIs to obtain prolonged disease control. ALK ve+ lung cancer today presents a large number of therapeutic opportunities leading to a long/term survival. Correct evaluation of ALK translocation is a paramount in order to guide the correct therapeutic strategy as illustrated in the present clinical case.

Published
2020

104. ‘Indeterminate for malignancy’ (Tir3/Thy3 in the Italian and British systems for classification) thyroid fine needle aspiration (FNA) cytology reporting: morphological criteria and clinical impact

Author

Pagni, F., Prada, M., Goffredo, P., Isimbaldi, G., Crippa, S., Di Bella, C., Leone, B. E., Capra, Maurizio, Colombo, Manuela, Perego, Rita, Pincelli, Angela Ida, Perotti, Mario, Grassi, Guido, Colombo, Giovanni, Giannobi, Paolo, Scardilli, Marcella, and Giardini, Vittorio

Published
2014
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105. A Compound L1196M/G1202R ALK Mutation in a Patient with ALK-Positive Lung Cancer with Acquired Resistance to Brigatinib Also Confers Primary Resistance to Lorlatinib

Author

Sharma, G, Cortinovis, D, Agustoni, F, Arosio, G, Villa, M, Cordani, N, Bidoli, P, Bisson, W, Pagni, F, Piazza, R, Gambacorti-Passerini, C, Mologni, L, Sharma G. G., Cortinovis D., Agustoni F., Arosio G., Villa M., Cordani N., Bidoli P., Bisson W. H., Pagni F., Piazza R., Gambacorti-Passerini C., Mologni L., Sharma, G, Cortinovis, D, Agustoni, F, Arosio, G, Villa, M, Cordani, N, Bidoli, P, Bisson, W, Pagni, F, Piazza, R, Gambacorti-Passerini, C, Mologni, L, Sharma G. G., Cortinovis D., Agustoni F., Arosio G., Villa M., Cordani N., Bidoli P., Bisson W. H., Pagni F., Piazza R., Gambacorti-Passerini C., and Mologni L.

Published
2019

106. ActivinA: a new leukemia-promoting factor conferring migratory advantage to B-cell precursor-acute lymphoblastic leukemic cells

Author

Portale, F, Cricrì, G, Bresolin, S, Lupi, M, Gaspari, S, Silvestri, D, Russo, B, Marino, N, Ubezio, P, Pagni, F, Vergani, P, Te Kronnie, G, Valsecchi, M, Locatelli, F, Rizzari, C, Biondi, A, Dander, E, D'Amico, G, Portale F, Cricrì G, Bresolin S, Lupi M, Gaspari S, Silvestri D, Russo B, Marino N, Ubezio P, Pagni F, Vergani P, Te Kronnie G, Valsecchi MG, Locatelli F, Rizzari C, Biondi A, Dander E, D'Amico G., Portale, F, Cricrì, G, Bresolin, S, Lupi, M, Gaspari, S, Silvestri, D, Russo, B, Marino, N, Ubezio, P, Pagni, F, Vergani, P, Te Kronnie, G, Valsecchi, M, Locatelli, F, Rizzari, C, Biondi, A, Dander, E, D'Amico, G, Portale F, Cricrì G, Bresolin S, Lupi M, Gaspari S, Silvestri D, Russo B, Marino N, Ubezio P, Pagni F, Vergani P, Te Kronnie G, Valsecchi MG, Locatelli F, Rizzari C, Biondi A, Dander E, and D'Amico G.

Abstract

B-cell precursor-acute lymphoblastic leukemia modulates the bone marrow (BM) niche to become leukemia-supporting and chemo-protective by reprogramming the stromal microenvironment. New therapies targeting the interplay between leukemia and stroma can help improve disease outcome. We identified ActivinA, a TGF-b family member with a well-described role in promoting several solid malignancies, as a factor favoring leukemia that could represent a new potential target for therapy. ActivinA resulted over-expressed in the leukemic BM and its production was strongly induced in mesenchymal stromal cells after culture with leukemic cells. Moreover, MSCs isolated from BM of leukemic patients showed an intrinsic ability to secrete higher amounts of ActivinA compared to their normal counterparts. The pro-inflammatory leukemic BM microenvironment synergized with leukemic cells to induce stromal-derived ActivinA. Gene expression analysis of ActivinA-treated leukemic cells showed that this protein was able to significantly influence motility-associated pathways. Interestingly, ActivinA promoted random motility and CXCL12-driven migration of leukemic cells, even at suboptimal chemokine concentrations, characterizing the leukemic niche. Conversely, ActivinA severely impaired CXCL12-induced migration of healthy CD34 + cells. This opposite effect can be explained by the ability of ActivinA to increase intracellular calcium only in leukemic cells, boosting cytoskeleton dynamics through a higher rate of actin polymerization. Moreover, by stimulating the invasiveness of the leukemic cells, ActivinA was found to be a leukemia-promoting factor. Importantly, the ability of ActivinA to enhance BM engraftment and the metastatic potential of leukemic cells was confirmed in a xenograft mouse model of the disease. Overall, ActivinA was seen to be a key factor in conferring a migratory advantage to leukemic cells over healthy hematopoiesis within the leukemic niche.

Published
2019

107. MALDI-MSI Pilot Study Highlights Glomerular Deposits of Macrophage Migration Inhibitory Factor (MIF) as a Possible Indicator of Response to Therapy in Membranous Nephropathy

Author

L'Imperio, V, Smith, A, Ajello, E, Piga, I, Stella, M, Denti, V, Tettamanti, S, Sinico, R, Pieruzzi, F, Garozzo, M, Vischini, G, Nebuloni, M, Pagni, F, Magni, F, L'Imperio V, Smith A, Ajello E, Piga I, Stella M, Denti V, Tettamanti S, Sinico RA, Pieruzzi F, Garozzo M, Vischini G, Nebuloni M, Pagni F, Magni F., L'Imperio, V, Smith, A, Ajello, E, Piga, I, Stella, M, Denti, V, Tettamanti, S, Sinico, R, Pieruzzi, F, Garozzo, M, Vischini, G, Nebuloni, M, Pagni, F, Magni, F, L'Imperio V, Smith A, Ajello E, Piga I, Stella M, Denti V, Tettamanti S, Sinico RA, Pieruzzi F, Garozzo M, Vischini G, Nebuloni M, Pagni F, and Magni F.

Abstract

Membranous Nephropathy (MN) is the most frequent cause of nephrotic syndrome in adults and the disease course is characterised by the "rule of third", with one third of patients experiencing complete remission and the remaining experiencing relapses or progression of the disease. Additionally, the therapeutic approach is not standardised, leading to further heterogeneity in terms of response and outcome. In this pilot study, MALDI-MSI analysis was performed on renal biopsies (n = 13) obtained from two homogeneous groups of patients which differentially responded to the immunosuppressive treatments (Ponticelli regimen). A signal at m/z 1303 displayed the greatest discriminatory power when comparing the two groups and was observed to be of higher intensity in the glomeruli of the non-responding patients. The corresponding tryptic peptide was identified as macrophage migration inhibitory factor (MIF). Despite much effort being made in recent years to understand the pathogenesis of MN, a biomarker able to predict the outcome of these patients following therapeutic treatment is still lacking. Here, we highlight a protein (MIF), verified by immunohistochemistry, which can differentiate between these MN patients and could be a valuable starting point for a further study focused on verifying its predictive role in therapy response. This article is protected by copyright. All rights reserved

Published
2019

109. RAS as a positive predictive biomarker: focus on lung and colorectal cancer patients

Author

Malapelle, U, Passiglia, F, Cremolini, C, Reale, M, Pepe, F, Pisapia, P, Avallone, A, Cortinovis, D, De Stefano, A, Fassan, M, Fontanini, G, Galetta, D, Lauricella, C, Listì, A, Loupakis, F, Pagni, F, Pietrantonio, F, Pilotto, S, Righi, L, Bianchi, A, Parra, H, Tiseo, M, Verzè, M, Troncone, G, Novello, S, Malapelle, Umberto, Passiglia, Francesco, Cremolini, Chiara, Reale, Maria Lucia, Pepe, Francesco, Pisapia, Pasquale, Avallone, Antonio, Cortinovis, Diego, De Stefano, Alfonso, Fassan, Matteo, Fontanini, Gabriella, Galetta, Domenico, Lauricella, Calogero, Listì, Angela, Loupakis, Fotios, Pagni, Fabio, Pietrantonio, Filippo, Pilotto, Sara, Righi, Luisella, Bianchi, Andrea Sartore, Parra, Hector Soto, Tiseo, Marcello, Verzè, Michela, Troncone, Giancarlo, Novello, Silvia, Malapelle, U, Passiglia, F, Cremolini, C, Reale, M, Pepe, F, Pisapia, P, Avallone, A, Cortinovis, D, De Stefano, A, Fassan, M, Fontanini, G, Galetta, D, Lauricella, C, Listì, A, Loupakis, F, Pagni, F, Pietrantonio, F, Pilotto, S, Righi, L, Bianchi, A, Parra, H, Tiseo, M, Verzè, M, Troncone, G, Novello, S, Malapelle, Umberto, Passiglia, Francesco, Cremolini, Chiara, Reale, Maria Lucia, Pepe, Francesco, Pisapia, Pasquale, Avallone, Antonio, Cortinovis, Diego, De Stefano, Alfonso, Fassan, Matteo, Fontanini, Gabriella, Galetta, Domenico, Lauricella, Calogero, Listì, Angela, Loupakis, Fotios, Pagni, Fabio, Pietrantonio, Filippo, Pilotto, Sara, Righi, Luisella, Bianchi, Andrea Sartore, Parra, Hector Soto, Tiseo, Marcello, Verzè, Michela, Troncone, Giancarlo, and Novello, Silvia

Abstract

Rat sarcoma (RAS) oncogenes have intensively been investigated during the last decades. Taking into account all human tumours, Kirsten Rat Sarcoma Viral Oncogene Homolog (KRAS) gene is the most frequently mutated (about 22%) among the three isoforms, followed by Neuroblastoma RAS Viral Oncogene Homolog (NRAS) (8%) and Harvey Rat Sarcoma Viral Oncogene Homolog (HRAS) (3%). In the last years, careful attention has been paid on KRAS and NRAS gene mutations in non-small-cell lung cancer (NSCLC) and colorectal cancer (CRC) patients because of their prognostic and predictive roles. In particular, a large body of literature data has been generated investigating clinical outcomes of targeted treatments in NSCLC and CRC KRAS- and NRAS-mutated patients. The latest evidences are here reviewed, providing also an overview of the real-world RAS mutation testing practice across different Italian laboratories. On this basis, we propose a knowledge-based system, www.rasatlas.com, to support the healthcare personnel in the management of patients featuring RAS gene mutations in the landscape of precision oncology.

Published
2021

110. The Role of the Pathologist in the Next-Generation Era of Tumor Molecular Characterization

Author

Angerilli, V, Galuppini, F, Pagni, F, Fusco, N, Malapelle, U, Fassan, M, Angerilli, Valentina, Galuppini, Francesca, Pagni, Fabio, Fusco, Nicola, Malapelle, Umberto, Fassan, Matteo, Angerilli, V, Galuppini, F, Pagni, F, Fusco, N, Malapelle, U, Fassan, M, Angerilli, Valentina, Galuppini, Francesca, Pagni, Fabio, Fusco, Nicola, Malapelle, Umberto, and Fassan, Matteo

Abstract

Current pathology practice is being shaped by the increasing complexity of modern medicine, in particular of precision oncology, and major technological advances. In the "next-generation technologies era", the pathologist has become the person responsible for the integration and interpretation of morphologic and molecular information and for the delivery of critical answers to diagnostic, prognostic and predictive queries, acquiring a prominent position in the molecular tumor boards.

Published
2021

111. RNA-Based Assay for Next-Generation Sequencing of Clinically Relevant Gene Fusions in Non-Small Cell Lung Cancer

Author

De Luca, C, Pepe, F, Iaccarino, A, Pisapia, P, Righi, L, Listì, A, Greco, L, Gragnano, G, Campione, S, De Dominicis, G, Pagni, F, Sgariglia, R, Nacchio, M, Tufano, R, Conticelli, F, Vigliar, E, Bellevicine, C, Cortinovis, D, Novello, S, Molina-Vila, M, Rosell, R, Troncone, G, Malapelle, U, De Luca, Caterina, Pepe, Francesco, Iaccarino, Antonino, Pisapia, Pasquale, Righi, Luisella, Listì, Angela, Greco, Lorenza, Gragnano, Gianluca, Campione, Severo, De Dominicis, Gianfranco, Pagni, Fabio, Sgariglia, Roberta, Nacchio, Mariantonia, Tufano, Rossella, Conticelli, Floriana, Vigliar, Elena, Bellevicine, Claudio, Cortinovis, Diego Luigi, Novello, Silvia, Molina-Vila, Miguel Angel, Rosell, Rafael, Troncone, Giancarlo, Malapelle, Umberto, De Luca, C, Pepe, F, Iaccarino, A, Pisapia, P, Righi, L, Listì, A, Greco, L, Gragnano, G, Campione, S, De Dominicis, G, Pagni, F, Sgariglia, R, Nacchio, M, Tufano, R, Conticelli, F, Vigliar, E, Bellevicine, C, Cortinovis, D, Novello, S, Molina-Vila, M, Rosell, R, Troncone, G, Malapelle, U, De Luca, Caterina, Pepe, Francesco, Iaccarino, Antonino, Pisapia, Pasquale, Righi, Luisella, Listì, Angela, Greco, Lorenza, Gragnano, Gianluca, Campione, Severo, De Dominicis, Gianfranco, Pagni, Fabio, Sgariglia, Roberta, Nacchio, Mariantonia, Tufano, Rossella, Conticelli, Floriana, Vigliar, Elena, Bellevicine, Claudio, Cortinovis, Diego Luigi, Novello, Silvia, Molina-Vila, Miguel Angel, Rosell, Rafael, Troncone, Giancarlo, and Malapelle, Umberto

Abstract

Gene fusions represent novel predictive biomarkers for advanced non-small cell lung cancer (NSCLC). In this study, we validated a narrow NGS gene panel able to cover therapeutically-relevant gene fusions and splicing events in advanced-stage NSCLC patients. To this aim, we first assessed minimal complementary DNA (cDNA) input and the limit of detection (LoD) in different cell lines. Then, to evaluate the feasibility of applying our panel to routine clinical samples, we retrospectively selected archived lung adenocarcinoma histological and cytological (cell blocks) samples. Overall, our SiRe RNA fusion panel was able to detect all fusions and a splicing event harbored in a RNA pool diluted up to 2 ng/µL. It also successfully analyzed 46 (95.8%) out of 48 samples. Among these, 43 (93.5%) out of 46 samples reproduced the same results as those obtained with conventional techniques. Intriguingly, the three discordant results were confirmed by a CE-IVD automated real-time polymerase chain reaction (RT-PCR) analysis (Easy PGX platform, Diatech Pharmacogenetics, Jesi, Italy). Based on these findings, we conclude that our new SiRe RNA fusion panel is a valid and robust tool for the detection of clinically relevant gene fusions and splicing events in advanced NSCLC.

Published
2021

112. Monocyte–macrophage polarization and recruitment pathways in the tumour microenvironment of B-cell acute lymphoblastic leukaemia

Author

Dander, E., Fallati, A., Gulic, T., Pagni, F., Gaspari, S., Silvestri, D., Cricri, G., Bedini, G., Portale, F., Buracchi, C., Starace, R., Pasqualini, F., D'Angio, M., Brizzolara, L., Maglia, O., Mantovani, A., Garlanda, C., Valsecchi, M. G., Locatelli, Franco, Biondi, A., Bottazzi, B., Allavena, P., D'Amico, G., Locatelli F. (ORCID:0000-0002-7976-3654), Dander, E., Fallati, A., Gulic, T., Pagni, F., Gaspari, S., Silvestri, D., Cricri, G., Bedini, G., Portale, F., Buracchi, C., Starace, R., Pasqualini, F., D'Angio, M., Brizzolara, L., Maglia, O., Mantovani, A., Garlanda, C., Valsecchi, M. G., Locatelli, Franco, Biondi, A., Bottazzi, B., Allavena, P., D'Amico, G., and Locatelli F. (ORCID:0000-0002-7976-3654)

Abstract

B-cell acute lymphoblastic leukaemia (B-ALL) reprograms the surrounding bone marrow (BM) stroma to create a leukaemia-supportive niche. To elucidate the contribution of immune cells to the leukaemic microenvironment, we investigated the involvement of monocyte/macrophage compartments, as well as several recruitment pathways in B-ALL development. Immunohistochemistry analyses showed that CD68-expressing macrophages were increased in leukaemic BM biopsies, compared to controls and predominantly expressed the M2-like markers CD163 and CD206. Furthermore, the "non-classical" CD14+CD16++ monocyte subset, expressing high CX3CR1 levels, was significantly increased in B-ALL patients' peripheral blood. CX3CL1 was shown to be significantly upregulated in leukaemic BM plasma, thus providing an altered migratory pathway possibly guiding NC monocyte recruitment into the BM. Additionally, the monocyte/macrophage chemoattractant chemokine ligand 2 (CCL2) strongly increased in leukaemic BM plasma, possibly because of the interaction of leukaemic cells with mesenchymal stromal cells and vascular cells and due to a stimulatory effect of leukaemia-related inflammatory mediators. C5a, a macrophage chemoattractant and M2-polarizing factor, further appeared to be upregulated in the leukaemic BM, possibly as an effect of PTX3 decrease, that could unleash complement cascade activation. Overall, deregulated monocyte/macrophage compartments are part of the extensive BM microenvironment remodelling at B-ALL diagnosis and could represent valuable targets for novel treatments to be coupled with classical chemotherapy.

Published
2021

113. ctDNA analysis in the personalized clinical management of gastroesophageal adenocarcinoma: turning hope into reality

Author

Salati, M, Venetis, K, Fassan, M, Malapelle, U, Pagni, F, Sajjadi, E, Fusco, N, Ghidini, M, Salati, Massimiliano, Venetis, Konstantinos, Fassan, Matteo, Malapelle, Umberto, Pagni, Fabio, Sajjadi, Elham, Fusco, Nicola, Ghidini, Michele, Salati, M, Venetis, K, Fassan, M, Malapelle, U, Pagni, F, Sajjadi, E, Fusco, N, Ghidini, M, Salati, Massimiliano, Venetis, Konstantinos, Fassan, Matteo, Malapelle, Umberto, Pagni, Fabio, Sajjadi, Elham, Fusco, Nicola, and Ghidini, Michele

Abstract

Gastroesophageal adenocarcinoma (GEA) is a global health issue with a high fatality-to-case ratio and a 5-year overall survival that has only slightly improved. High-throughput molecular profiling has uncovered a profound complexity and heterogeneity in GEA biology, which limits considerably the treatment advances. Liquid biopsy with circulating tumor (ct)DNA analysis could elucidate GEA molecular heterogeneity and provide diagnostic, prognostic and predictive information to guide clinical decision-making. However, only a handful of studies have shown positive results for the application of ctDNA analysis in GEA clinical management. As a result, no comprehensive information is available to date on this continuously evolving topic. Here, we discuss the current state of knowledge, along with promises and challenges related to ctDNA analysis in GEA.

Published
2021

115. Cytopathology of Bronchoalveolar Lavages in COVID-19 Pneumonia: A Pilot Study

Author

Canini, V, Bono, F, Calzavacca, P, Capitoli, G, Foti, G, Fraggetta, F, Galimberti, S, Gianatti, A, Giani, M, Nasr, A, Paciocco, G, Pagni, F, Rona, R, L'Imperio, V, Canini, Valentina, Bono, Francesca, Calzavacca, Paolo, Capitoli, Giulia, Foti, Giuseppe, Fraggetta, Filippo, Galimberti, Stefania, Gianatti, Andrea, Giani, Marco, Nasr, Ahmed, Paciocco, Giuseppe, Pagni, Fabio, Rona, Roberto, L'Imperio, Vincenzo, Canini, V, Bono, F, Calzavacca, P, Capitoli, G, Foti, G, Fraggetta, F, Galimberti, S, Gianatti, A, Giani, M, Nasr, A, Paciocco, G, Pagni, F, Rona, R, L'Imperio, V, Canini, Valentina, Bono, Francesca, Calzavacca, Paolo, Capitoli, Giulia, Foti, Giuseppe, Fraggetta, Filippo, Galimberti, Stefania, Gianatti, Andrea, Giani, Marco, Nasr, Ahmed, Paciocco, Giuseppe, Pagni, Fabio, Rona, Roberto, and L'Imperio, Vincenzo

Abstract

BACKGROUND: Bronchoalveolar lavage (BAL) in patients with severe coronavirus disease 2019 (COVID-19) may provide additional and complementary findings for the management of these patients admitted to intensive care units (ICUs). This study addresses the cytological features of the infection and highlights the more influential inflammatory components. The correlation between pathological variables and clinical data is also analyzed. METHODS: The authors performed a retrospective analysis of the cytopathological features of BAL in 20 COVID-19 patients and 20 members of a matched cohort from a critical ICU who had acute respiratory distress syndrome caused by other pulmonary conditions. RESULTS: A comparison of the controls (n = 20) and the COVID-19 patients (n = 20) revealed that the latter had a higher neutrophil count (median, 63.8% of the cell count) with lower percentages of macrophages and lymphocytes. An increase in the expression of CD68-positive, monocytic multinucleated giant cells (MGCs) was reported; megakaryocytes were not detected on CD61 staining. Perls staining showed isolated elements. In situ RNA analysis demonstrated scattered chromogenic signals in type II pneumocytes. An ultrastructural analysis confirmed the presence of intracytoplasmic vacuoles containing rounded structures measuring 140 nm in diameter (putative viral particles). In COVID-19 patients, the clinicopathological correlation revealed a positive correlation between lactate dehydrogenase values and MGCs (r = 0.54). CONCLUSIONS: The analysis of BAL samples might be implemented as a routine practice for the evaluation of COVID-19 patients in ICUs in the appropriate clinical scenario. Additional studies using a larger sample size of patients who developed COVID-19 during the second wave of the epidemic in the autumn of 2020 are needed to further support our findings.

Published
2021

116. PD-L1 Testing and Squamous Cell Carcinoma of the Head and Neck: A Multicenter Study on the Diagnostic Reproducibility of Different Protocols

Author

Crosta, S, Boldorini, R, Bono, F, Brambilla, V, Dainese, E, Fusco, N, Gianatti, A, L'Imperio, V, Morbini, P, Pagni, F, Crosta, Simona, Boldorini, Renzo, Bono, Francesca, Brambilla, Virginia, Dainese, Emanuele, Fusco, Nicola, Gianatti, Andrea, L'Imperio, Vincenzo, Morbini, Patrizia, Pagni, Fabio, Crosta, S, Boldorini, R, Bono, F, Brambilla, V, Dainese, E, Fusco, N, Gianatti, A, L'Imperio, V, Morbini, P, Pagni, F, Crosta, Simona, Boldorini, Renzo, Bono, Francesca, Brambilla, Virginia, Dainese, Emanuele, Fusco, Nicola, Gianatti, Andrea, L'Imperio, Vincenzo, Morbini, Patrizia, and Pagni, Fabio

Abstract

Immune checkpoint inhibitors for blocking the programmed cell death protein 1 (PD-1)/programmed death-ligand 1 (PD-L1) axis are now available for squamous cell carcinoma of the head and neck (HNSCC) in relapsing and/or metastatic settings. In this work, we compared the resulting combined positive score (CPS) of PD-L1 using alternative methods adopted in routine clinical practice and determined the level of diagnostic agreement and inter-observer reliability in this setting. The study applied 5 different protocols on 40 tissue microarrays from HNSCC. The error rate of the individual protocols ranged from a minimum of 7% to a maximum of 21%, the sensitivity from 79% to 96%, and the specificity from 50% to 100%. In the intermediate group (1 ≤ CPS < 20), the majority of errors consisted of an underestimation of PD-L1 expression. In strong expressors, 5 out of 14 samples (36%) were correctly evaluated by all the protocols, but no protocol was able to correctly identify all the "strong expressors". The overall inter-observer agreement in PD-L1 CPS reached 87%. The inter-observer reliability was moderate, with an ICC of 0.774 (95% CI (0.651; 0.871)). In conclusion, our study showed moderate interobserver reliability among different protocols. In order to improve the performances, adequate specific training to evaluate PD-L1 by CPS in the HNSCC setting should be coordinated.

Published
2021

117. Ex vivo thyroid fine needle aspirations as an alternative for MALDI-MSI proteomic investigation: intra-patient comparison

Author

Piga, I, Capitoli, G, Clerici, F, Mahajneh, A, Brambilla, V, Smith, A, Leni, D, L'Imperio, V, Galimberti, S, Pagni, F, Magni, F, Piga, Isabella, Capitoli, Giulia, Clerici, Francesca, Mahajneh, Allia, Brambilla, Virginia, Smith, Andrew, Leni, Davide, L'Imperio, Vincenzo, Galimberti, Stefania, Pagni, Fabio, Magni, Fulvio, Piga, I, Capitoli, G, Clerici, F, Mahajneh, A, Brambilla, V, Smith, A, Leni, D, L'Imperio, V, Galimberti, S, Pagni, F, Magni, F, Piga, Isabella, Capitoli, Giulia, Clerici, Francesca, Mahajneh, Allia, Brambilla, Virginia, Smith, Andrew, Leni, Davide, L'Imperio, Vincenzo, Galimberti, Stefania, Pagni, Fabio, and Magni, Fulvio

Abstract

Fine needle aspiration (FNA) is the reference standard for the diagnosis of thyroid nodules. Matrix-assisted laser desorption/ionization mass spectrometry imaging (MALDI-MSI) has been successfully used to discriminate the proteomic profiles of benign and malignant thyroid FNAs within the scope of providing support to pathologists for the classification of morphologically borderline cases. However, real FNAs provide a limited amount of material due to sample collection restrictions. Ex vivo FNAs could represent a valuable alternative, increasing sample size and the power of statistical conclusions. In this study, we compared the real and ex vivo MALDI-MSI proteomic profiles, extracted from thyrocyte containing regions of interest, of 13 patients in order to verify their similarity. Statistical analysis demonstrated the mass spectra similarity of the proteomic profiles by performing intra-patient comparison, using statistical similarity systems. In conclusion, these results show that post-surgical FNAs represent a possible alternative source of material for MALDI-MSI proteomic investigations in instances where pre-surgical samples are unavailable or the number of cells is scarce.

Published
2021

118. Liquid-based shaking of core needle biopsy samples for the molecular characterization of tumors: A fallback in cytopathology

Author

L'Imperio, V, Corral, L, Pagni, F, L'Imperio, Vincenzo, Corral, Lilia, Pagni, Fabio, L'Imperio, V, Corral, L, Pagni, F, L'Imperio, Vincenzo, Corral, Lilia, and Pagni, Fabio

Abstract

Cytological specimens may be the ideal source of nucleic acids for the molecular characterization of tumors in the next generation sequencing (NGS) era. Liquid‐based shaking of core needle biopsy samples could enhance the diagnostic yield, allowing additional material to be examined in parallel with histopathology.

Published
2021

121. MALDI-MS imaging in glomerular kidney diseases: from diagnostics to precision medicine?

Author

Smith, A, L'Imperio, Vincenzo, Piga, I, Denti, V, Chinello, C, Pagni, F, Magni, F, Smith, A, L'Imperio, V, Piga, I, Denti, V, Chinello, C, Pagni, F, and Magni, F

Subjects
kidney, precision medicine, MALDI-MSI, imaging, proteomic
Abstract

Introduction/Rationale: Glomerular kidney diseases represent the third leading cause of end-stage renal disease in Western countries and the need for both diagnostic and predictive markers is becoming ever more pressing. In particular, there still remains a fair degree of heterogeneity in terms of patient response and outcome and such markers could lead to more targeted therapy and focused monitoring guidelines for clinicians. Given the high degree of tissue heterogeneity associated with these diseases, MALDI-MSI therefore represents an ideal tool in this branch of renal histopathology, offering a complementary molecular dimension. Here we present our recent contributions to this area of research and highlight how this approach can be employed to detect groups of patients which may require more precise therapeutic treatment. Methods: MALDI-MSI was applied to FFPE tissue samples from patients with membranous nephropathy (MN, n=13), diabetic nephropathy (DN, n=9) and hypertensive nephrosclerosis (HN, n=9). For the cases of MN, images were acquired with an ultrafleXtreme™ MALDI-TOF/TOF MS using a single spot laser setting of 40 µm and and raster sampling of 50 μm. For the cases of DN and HN, images were acquired using a rapifleX MALDI Tissuetyper™, employing a single spot laser setting of 18 µm and raster sampling of 20 μm. Finally, in order perform high spatial resolution MALDI-MS imaging, additional cases of MN (n=10) were acquired using a rapifleX MALDI Tissuetyper™, employing a single spot laser setting of 10 µm and a raster sampling of 10 μm. Results: In this preliminary work, we highlight the potential role of MALDI-MS imaging in the precision medicine of two frequently occurring glomerular kidney diseases, membranous nephropathy and diabetic nephropathy. In MN we were able to distinguish groups of patients who responded differentially to standard immunosuppressive therapy and, in particular, observed an increased expression of macrophage migration inhibitory factor (MIF) in patients who did not respond to the treatment. This increased expression of MIF was then validated using immunohistochemistry, with the protein depositing on podocyte and parietal epithelial cells within the glomeruli. When focusing on DN and HN, alterations in the tissue proteome of the two disease groups could clearly be detected. These proteomic alterations were particularly notable at the latter disease stages, even if no discernible differences were evident using routine histology. In particular, four putatively identified proteins were observed to have a higher signal intensity within regions of DN tissue with extensive sclerosis or fibrosis. Among these, two of them (progesterone receptor membrane component 1 and complement component 3) had a signal intensity that increased at the latter stages of the disease and may be associated with progression. Finally, we underline how high spatial resolution MALDI-MSI could further assist in the study of these complex renal diseases by going beyond what was previously possible and visualising the spatial localisation of proteins within the sub-compartments of glomeruli and tubulointerstitium. Conclusions/Novelty: This body of work exemplifies the potential role of MALDI-MSI in renal pathology. Our final goal is to obtain complementary proteomic information that can be used to assist nephrologists in the clinical management of these patients, leading to more targeted therapy and more focused monitoring guidelines. Funding: The research leading to these results has received funding from MIUR: FIRB 2007 (RBRN07BMCT_11), FAR 2014–2016 and in part by Fondazione Gigi & Pupa Ferrari Onlus.

Published
2019

125. Kidney Function, CKD Causes, and Histological Classification

Author

Ferrario, F, Pagni, F, Bolognesi, M, Ajello, E, L'Imperio, V, Masella, C, Capasso, G, Ferrario F., Pagni F., Bolognesi M., Ajello E., L'Imperio V., Masella C., Capasso G., Ferrario, F, Pagni, F, Bolognesi, M, Ajello, E, L'Imperio, V, Masella, C, Capasso, G, Ferrario F., Pagni F., Bolognesi M., Ajello E., L'Imperio V., Masella C., and Capasso G.

Abstract

Kidneys accomplish many important physiological tasks, ranging from the continuous blood filtration and consequent formation of urine, detoxification from endogenous and exogenous substances, production of active and inactive hormones (e.g., Vitamin D, Erythropoietin, and renin), and maintenance of the electrolytes balance. However, its function can be readily impaired by many pathogen noxae, leading to the so-called chronic kidney disease (CKD). This condition can be clinically assessed by the estimation of the glomerular filtration rate (eGFR), an indirect index of the renal function, that do not give any further information of which kind of injury affects the kidney. For this reason, the gold standard to determine the CKD cause is represented by the renal biopsy and the histomorphological criteria are essential for the interpretation of the tissue sample. In this chapter, the clinical and histopathological aspects of CKD will be discussed, with a final section on the future challenges represented by the molecular analysis and digital pathology in renal disease.

Published
2018

126. Update on: proteome analysis in thyroid pathology - part II: overview of technical and clinical enhancement of proteomic investigation of the thyroid lesions

Author

Piga, I, Casano, S, Smith, A, Tettamanti, S, Leni, D, Capitoli, G, Pincelli, A, Scardilli, M, Galimberti, S, Magni, F, Pagni, F, Piga I, Casano S, Smith A, Tettamanti S, Leni D, Capitoli G, Pincelli AI, Scardilli M, Galimberti S, Magni F, Pagni F., Piga, I, Casano, S, Smith, A, Tettamanti, S, Leni, D, Capitoli, G, Pincelli, A, Scardilli, M, Galimberti, S, Magni, F, Pagni, F, Piga I, Casano S, Smith A, Tettamanti S, Leni D, Capitoli G, Pincelli AI, Scardilli M, Galimberti S, Magni F, and Pagni F.

Abstract

An accurate diagnostic classification of thyroid lesions remains an important clinical aspect that needs to be addressed in order to avoid "diagnostic" thyroidectomies. Among the several "omics" techniques, proteomics is playing a pivotal role in the search for diagnostic markers. In recent years, different approaches have been used, taking advantage of the technical improvements related to mass spectrometry that have occurred. Areas covered: The review provides an update of the recent findings in diagnostic classification, in genetic definition and in the investigation of thyroid lesions based on different proteomics approaches and on different type of specimens: cytological, surgical and biofluid samples. A brief section will discuss how these findings can be integrated with those obtained by metabolomics investigations. Expert commentary: Among the several proteomics approaches able to deepen our knowledge of the molecular alterations of the different thyroid lesions, MALDI-MSI is strongly emerging above all. In fact, MS-imaging has also been demonstrated to be capable of distinguishing thyroid lesions, based on their different molecular signatures, using cytological specimens. The possibility to use the material obtained by the fine needle aspiration makes MALDI-MSI a highly promising technology that could be implemented into the clinical and pathological units

Published
2018

128. Kidney Involvement

Author

Sinico, R, Pagni, F, L’Imperio, V, Binda, V, Fabbrini, P, Pieruzzi, F, Moroni, G, Sinico, Renato Alberto, Pagni, Fabio, L’Imperio, Vincenzo, Binda, Valentina, Fabbrini, Paolo, Pieruzzi, Federico, Moroni, Gabriella, Sinico, R, Pagni, F, L’Imperio, V, Binda, V, Fabbrini, P, Pieruzzi, F, Moroni, G, Sinico, Renato Alberto, Pagni, Fabio, L’Imperio, Vincenzo, Binda, Valentina, Fabbrini, Paolo, Pieruzzi, Federico, and Moroni, Gabriella

Abstract

Renal involvement is a frequent and severe complication of antineutrophil cytoplasmic autoantibody (ANCA)-associated vasculitides (AAV). It is generally characterized by a pauci-immune necrotizing and crescentic glomerulonephritis with a very rapid decline of renal function (rapidly progressive glomerulonephritis). Even though there are no qualitative differences in glomerular lesions in patients with granulomatosis with polyangiitis (GPA) or microscopic polyangiitis (MPA), chronic damage is usually higher in MPA (and/or P-ANCA-positive patients) than in GPA (and/or CANCA-positive patients). If untreated, necrotizing and crescentic glomerulonephritis has an unfavorable course leading in a few weeks or months to end-stage renal disease (ESRD). Serum creatinine at diagnosis, sclerotic lesions, and the number of normal glomeruli at kidney biopsy are the best predictors of renal outcome. Corticosteroids and cyclophosphamide or rituximab (with the addition of plasma exchange in the most severe cases) are the cornerstone of induction treatment of ANCA-associated renal vasculitis, followed by azathioprine (or methotrexate, mycophenolate, rituximab) for maintenance. Despite significant improvement in patient outcomes over the past decades, AAV still results in ESRD in a quarter of patients over 5 years. Relapse rates are significantly lower in patients on chronic dialysis. Patient survival on regular replacement treatment (RRT) does not differ between AAV and matched nondiabetic patients, while it is lower than that of glomerulonephritis. Patients with AAV who undergo kidney transplantation have a mortality not different from the matched control group of primary glomerulonephritides, and favorable transplant survival is similar to that of the matched control groups.

Published
2020

129. Integrated Genomic, Functional, and Prognostic Characterization of Atypical Chronic Myeloid Leukemia

Author

Fontana, D, Ramazzotti, D, Aroldi, A, Redaelli, S, Magistroni, V, Pirola, A, Niro, A, Massimino, L, Mastini, C, Brambilla, V, Bombelli, S, Bungaro, S, Morotti, A, Rea, D, Stagno, F, Martino, B, Campiotti, L, Caocci, G, Usala, E, Merli, M, Onida, F, Bregni, M, Elli, E, Fumagalli, M, Ciceri, F, Perego, R, Pagni, F, Mologni, L, Piazza, R, Gambacorti-Passerini, C, Fontana, Diletta, Ramazzotti, Daniele, Aroldi, Andrea, Redaelli, Sara, Magistroni, Vera, Pirola, Alessandra, Niro, Antonio, Massimino, Luca, Mastini, Cristina, Brambilla, Virginia, Bombelli, Silvia, Bungaro, Silvia, Morotti, Alessandro, Rea, Delphine, Stagno, Fabio, Martino, Bruno, Campiotti, Leonardo, Caocci, Giovanni, Usala, Emilio, Merli, Michele, Onida, Francesco, Bregni, Marco, Elli, Elena Maria, Fumagalli, Monica, Ciceri, Fabio, Perego, Roberto A, Pagni, Fabio, Mologni, Luca, Piazza, Rocco, Gambacorti-Passerini, Carlo, Fontana, D, Ramazzotti, D, Aroldi, A, Redaelli, S, Magistroni, V, Pirola, A, Niro, A, Massimino, L, Mastini, C, Brambilla, V, Bombelli, S, Bungaro, S, Morotti, A, Rea, D, Stagno, F, Martino, B, Campiotti, L, Caocci, G, Usala, E, Merli, M, Onida, F, Bregni, M, Elli, E, Fumagalli, M, Ciceri, F, Perego, R, Pagni, F, Mologni, L, Piazza, R, Gambacorti-Passerini, C, Fontana, Diletta, Ramazzotti, Daniele, Aroldi, Andrea, Redaelli, Sara, Magistroni, Vera, Pirola, Alessandra, Niro, Antonio, Massimino, Luca, Mastini, Cristina, Brambilla, Virginia, Bombelli, Silvia, Bungaro, Silvia, Morotti, Alessandro, Rea, Delphine, Stagno, Fabio, Martino, Bruno, Campiotti, Leonardo, Caocci, Giovanni, Usala, Emilio, Merli, Michele, Onida, Francesco, Bregni, Marco, Elli, Elena Maria, Fumagalli, Monica, Ciceri, Fabio, Perego, Roberto A, Pagni, Fabio, Mologni, Luca, Piazza, Rocco, and Gambacorti-Passerini, Carlo

Abstract

Atypical chronic myeloid leukemia (aCML) is a BCR-ABL1-negative clonal disorder, which belongs to the myelodysplastic/myeloproliferative group. This disease is characterized by recurrent somatic mutations in SETBP1, ASXL1 and ETNK1 genes, as well as high genetic heterogeneity, thus posing a great therapeutic challenge. To provide a comprehensive genomic characterization of aCML we applied a high-throughput sequencing strategy to 43 aCML samples, including both whole-exome and RNA-sequencing data. Our dataset identifies ASXL1, SETBP1, and ETNK1 as the most frequently mutated genes with a total of 43.2%, 29.7 and 16.2%, respectively. We characterized the clonal architecture of 7 aCML patients by means of colony assays and targeted resequencing. The results indicate that ETNK1 variants occur early in the clonal evolution history of aCML, while SETBP1 mutations often represent a late event. The presence of actionable mutations conferred both ex vivo and in vivo sensitivity to specific inhibitors with evidence of strong in vitro synergism in case of multiple targeting. In one patient, a clinical response was obtained. Stratification based on RNA-sequencing identified two different populations in terms of overall survival, and differential gene expression analysis identified 38 significantly overexpressed genes in the worse outcome group. Three genes correctly classified patients for overall survival.

Published
2020

130. BRAF as a positive predictive biomarker: Focus on lung cancer and melanoma patients

Author

Malapelle, U, Rossi, G, Pisapia, P, Barberis, M, Buttitta, F, Castiglione, F, Cecere, F, Grimaldi, A, Iaccarino, A, Marchetti, A, Massi, D, Medicina, D, Mele, F, Minari, R, Orlando, E, Pagni, F, Palmieri, G, Righi, L, Russo, A, Tommasi, S, Vermi, W, Troncone, G, Malapelle, Umberto, Rossi, Giulio, Pisapia, Pasquale, Barberis, Massimo, Buttitta, Fiamma, Castiglione, Francesca, Cecere, Fabiana Letizia, Grimaldi, Antonio Maria, Iaccarino, Antonino, Marchetti, Antonio, Massi, Daniela, Medicina, Daniela, Mele, Fabio, Minari, Roberta, Orlando, Elisabetta, Pagni, Fabio, Palmieri, Giuseppe, Righi, Luisella, Russo, Alessandro, Tommasi, Stefania, Vermi, William, Troncone, Giancarlo, Malapelle, U, Rossi, G, Pisapia, P, Barberis, M, Buttitta, F, Castiglione, F, Cecere, F, Grimaldi, A, Iaccarino, A, Marchetti, A, Massi, D, Medicina, D, Mele, F, Minari, R, Orlando, E, Pagni, F, Palmieri, G, Righi, L, Russo, A, Tommasi, S, Vermi, W, Troncone, G, Malapelle, Umberto, Rossi, Giulio, Pisapia, Pasquale, Barberis, Massimo, Buttitta, Fiamma, Castiglione, Francesca, Cecere, Fabiana Letizia, Grimaldi, Antonio Maria, Iaccarino, Antonino, Marchetti, Antonio, Massi, Daniela, Medicina, Daniela, Mele, Fabio, Minari, Roberta, Orlando, Elisabetta, Pagni, Fabio, Palmieri, Giuseppe, Righi, Luisella, Russo, Alessandro, Tommasi, Stefania, Vermi, William, and Troncone, Giancarlo

Abstract

In the era of personalized medicine, BRAF mutational assessment is mandatory in advanced-stage melanoma and non-small cell lung cancer (NSCLC) patients. The identification of actionable mutations is crucial for the adequate management of these patients. To date various drugs have been implemented in clinical practice. Similarly, various methods may be adopted for the identification of BRAF mutations. Here, we briefly review the current literature on BRAF in melanoma and NSCLC, focusing attention in particular on the different methods and drugs adopted in these patients. In addition, an overview of the real-world practice in different Italian laboratories with high expertise in molecular predictive pathology testing is provided.

Published
2020

131. KRAS inhibition in non-small cell lung cancer: Past failures, new findings and upcoming challenges

Author

Passiglia, F, Malapelle, U, Del Re, M, Righi, L, Pagni, F, Furlan, D, Danesi, R, Troncone, G, Novello, S, Passiglia, Francesco, Malapelle, Umberto, Del Re, Marzia, Righi, Luisella, Pagni, Fabio, Furlan, Daniela, Danesi, Romano, Troncone, Giancarlo, Novello, Silvia, Passiglia, F, Malapelle, U, Del Re, M, Righi, L, Pagni, F, Furlan, D, Danesi, R, Troncone, G, Novello, S, Passiglia, Francesco, Malapelle, Umberto, Del Re, Marzia, Righi, Luisella, Pagni, Fabio, Furlan, Daniela, Danesi, Romano, Troncone, Giancarlo, and Novello, Silvia

Abstract

Despite the high prevalence of Kirsten rat sarcoma (KRAS) mutations in non-small cell lung cancer (NSCLC), for a long time it has been defined as an 'undruggable target', with precision medicine not considered as an adequate approach to treat this subgroup of patients. After several years of efforts, preliminary data from early clinical trials have recently demonstrated that direct pharmacological inhibition of KRAS p.G12C mutation is possible, emerging as an effective targeted treatment for about 10-12% of patients with advanced NSCLC, with potential relevant impact on their long-term survival and quality of life. This review reports the current status of KRAS mutations detection in the Italian real-word scenario, summarises the biological basis of KRAS inhibition in NSCLC and provides an updated overview of therapeutic strategies, discussing the potential reasons for past failures and analysing the upcoming challenges related to the advent of new targeted agents in clinical practice.

Published
2020

132. Molecular trait of follicular-patterned thyroid neoplasms defined by MALDI-imaging

Author

Piga, I, Capitoli, G, Clerici, F, Brambilla, V, Leni, D, Scardilli, M, Canini, V, Cipriani, N, Bono, F, Valsecchi, M, Galimberti, S, Magni, F, Pagni, F, Piga, Isabella, Capitoli, Giulia, Clerici, Francesca, Brambilla, Virginia, Leni, Davide, Scardilli, Marcella, Canini, Valentina, Cipriani, Nicole, Bono, Francesca, Valsecchi, Maria Grazia, Galimberti, Stefania, Magni, Fulvio, Pagni, Fabio, Piga, I, Capitoli, G, Clerici, F, Brambilla, V, Leni, D, Scardilli, M, Canini, V, Cipriani, N, Bono, F, Valsecchi, M, Galimberti, S, Magni, F, Pagni, F, Piga, Isabella, Capitoli, Giulia, Clerici, Francesca, Brambilla, Virginia, Leni, Davide, Scardilli, Marcella, Canini, Valentina, Cipriani, Nicole, Bono, Francesca, Valsecchi, Maria Grazia, Galimberti, Stefania, Magni, Fulvio, and Pagni, Fabio

Abstract

In the field of thyroid neoplasms, the most interesting recent change regards the introduction of a new terminology for follicular-patterned thyroid tumors, named Noninvasive Thyroid Neoplasm with Papillary-like Nuclear Features (NIFTP). This pre-malignant tumor is considered to be the putative precursor of invasive carcinomas. However, given that several issues are still unresolved, the application of ancillary tools, based on omics-techniques, may improve the clinical management of these challenging cases. The present paper highlights the proteomic profiles of a series of NIFTPs submitted to Fine Needle Aspirations (FNAs) and analysed by MALDI-imaging in order to confirm the heterogeneous phenotype of nodules included in the present NIFTP terminology and to underline the necessity of more accurate biomarkers that can be used for their characterization. Ethical and economic implications in terms of healthcare costs, operative risks, morbidity, as well as the potential need for lifelong hormone replacement therapy, seem to be significant reasons to approach the characterization of NIFTPs using alternative tools such as MALDI-MSI.

Published
2020

133. Digital Pathology and PD-L1 Testing in Non Small Cell Lung Cancer: A Workshop Record

Author

Pagni, F, Malapelle, U, Doglioni, C, Fontanini, G, Fraggetta, F, Graziano, P, Marchetti, A, Guerini Rocco, E, Pisapia, P, Vigliar, E, Buttitta, F, Jaconi, M, Fusco, N, Barberis, M, Troncone, G, Pagni, Fabio, Malapelle, Umberto, Doglioni, Claudio, Fontanini, Gabriella, Fraggetta, Filippo, Graziano, Paolo, Marchetti, Antonio, Guerini Rocco, Elena, Pisapia, Pasquale, Vigliar, Elena V, Buttitta, Fiamma, Jaconi, Marta, Fusco, Nicola, Barberis, Massimo, Troncone, Giancarlo, Pagni, F, Malapelle, U, Doglioni, C, Fontanini, G, Fraggetta, F, Graziano, P, Marchetti, A, Guerini Rocco, E, Pisapia, P, Vigliar, E, Buttitta, F, Jaconi, M, Fusco, N, Barberis, M, Troncone, G, Pagni, Fabio, Malapelle, Umberto, Doglioni, Claudio, Fontanini, Gabriella, Fraggetta, Filippo, Graziano, Paolo, Marchetti, Antonio, Guerini Rocco, Elena, Pisapia, Pasquale, Vigliar, Elena V, Buttitta, Fiamma, Jaconi, Marta, Fusco, Nicola, Barberis, Massimo, and Troncone, Giancarlo

Abstract

A meeting among expert pathologists was held in 2019 in Rome to verify the results of the previous harmonization efforts on the PD-L1 immunohistochemical testing by scoring a representative series of non-small cell lung cancer (NSCLC) digital slides. The current paper shows the results of this digital experimental meeting and the expertise achieved by the community of Italian pathologists. PD-L1 protein expression was determined using tumor proportion score (TPS), i.e., the percentage of viable tumor cells showing partial or complete membrane staining at any intensity. The gold standard was defined as the final PD-L1 score formulated by a panel of seven lung committed pathologists. PD-L1 status was clustered in three categories, namely negative (TPS < 1), low (TPS 1-49%), and high (TPS ≥ 50%). In 23 cases (71.9%) PD-L1 staining was performed using the companion diagnostic 22C3 pharmDx kit on Dako Autostainer, while in nine (28.1%) cases it was performed using the SP263 Ventana kit on BenchMark platform. A complete PD-L1 scoring agreement between the panel of experts and the participants was reached in 57.1% of cases, whereas a minor disagreement in 16.1% of cases was recorded. Italian pathologists performed best in strong positive cases (i.e., tumor proportion score TPS > 50%), whereas only 10.8% of disagreement with the gold standard was observed, and 55.6% regarded a single challenging case. The worst performance was achieved in the negative cases, with 32.0% disagreement. A significant difference resulted from the analysis of the data separated by the different clones used: 22.3% and 38.1% disagreement (p = 0.01) was found in the group of cases analyzed by 22C3 and SP263 antibody clones, respectively. In conclusion, this workshop record proposed the application of a digital pathology platform to share controversial cases in educational meetings as an alternative possibility for improving the interpretation and reporting of specific histological tools. Due t

Published
2020

134. Analysis of Hashimoto's thyroiditis on fine needle aspiration samples by MALDI-Imaging

Author

Capitoli, G, Piga, I, Clerici, F, Brambilla, V, Mahajneh, A, Leni, D, Garancini, M, Pincelli, A, L'Imperio, V, Galimberti, S, Magni, F, Pagni, F, Capitoli, Giulia, Piga, Isabella, Clerici, Francesca, Brambilla, Virginia, Mahajneh, Allia, Leni, Davide, Garancini, Mattia, Pincelli, Angela Ida, L'Imperio, Vincenzo, Galimberti, Stefania, Magni, Fulvio, Pagni, Fabio, Capitoli, G, Piga, I, Clerici, F, Brambilla, V, Mahajneh, A, Leni, D, Garancini, M, Pincelli, A, L'Imperio, V, Galimberti, S, Magni, F, Pagni, F, Capitoli, Giulia, Piga, Isabella, Clerici, Francesca, Brambilla, Virginia, Mahajneh, Allia, Leni, Davide, Garancini, Mattia, Pincelli, Angela Ida, L'Imperio, Vincenzo, Galimberti, Stefania, Magni, Fulvio, and Pagni, Fabio

Abstract

Matrix-Assisted Laser Desorption/Ionization (MALDI)-Mass Spectrometry imaging (MSI) has been applied in various diseases aimed to biomarkers discovery. In this study diagnosis and prognosis of Hashimoto Thyroiditis (HT) in cytopathology by MALDI-MSI has been investigated. Specimens from a routine series of subjects who underwent UltraSound-guided thyroid Fine Needle Aspirations (FNAs) were used. The molecular classifier trained in a previous study was modified to include HT as a separate entity in the group of benign lesions, in the diagnostic proteomic triage of thyroid nodules. The statistical analysis confirmed the existence of signals that HT shares with hyperplastic lesions and others that are specific and characterize this subgroup. Statistically relevant HT-related peaks were included in the model. Then, the discriminatory capability of the classifier was tested in a second validation phase, showing a good agreement with cytological diagnoses. The possibility to overlap the molecular signatures of both the lymphocytes and epithelial cells components (ROIs or pixel-by-pixel analysis) confirmed the composite proteomic background of HT. These results open the way to their possible translation as alternative serum biomarkers of this autoimmune condition.

Published
2020

137. The spectrum of the cytopathological features of primary effusion lymphoma and human herpes virus 8-related lymphoproliferative disorders

Author

Verga, L, Leni, D, Cazzaniga, G, Crosta, S, Seminati, D, Rossi, M, L'Imperio, V, Pagni, F, Verga, Luisa, Leni, Davide, Cazzaniga, Giorgio, Crosta, Simona, Seminati, Davide, Rossi, Marianna, L'Imperio, Vincenzo, Pagni, Fabio, Verga, L, Leni, D, Cazzaniga, G, Crosta, S, Seminati, D, Rossi, M, L'Imperio, V, Pagni, F, Verga, Luisa, Leni, Davide, Cazzaniga, Giorgio, Crosta, Simona, Seminati, Davide, Rossi, Marianna, L'Imperio, Vincenzo, and Pagni, Fabio

Abstract

Introduction: Human herpes virus 8-related lymphoproliferative disorders are a complex and heterogeneous group of entities and some of them are eminently diagnosed by cytopathology. In a routine laboratory, these lesions account for less than 1% of the effusion fluids samples. However, they represent up to 30% of all the lymphoma diagnosis from effusion cytological samples and their consideration in the diagnostic flow chart is mandatory, especially in human immunodeficiency virus-positive patients. Methods: A retrospective series of cytological specimens from cavity effusions (n = 605) were analysed. Five human herpes virus 8-related lymphoproliferative processes were recruited. A combination of morphological criteria (enhanced with May-Grünwald Giemsa staining), cell block-based immunocytochemistry and flow cytometry were undertaken for final characterisation. Results: The identification of malignant cells may be difficult. Some specimens are particularly rich, easily leading to suspect a lymphoproliferative process, whereas in other cases, the presence of abundant reactive mesothelial cells, histiocytes, neutrophils, small reactive T and B lymphocytes may obscure the neoplastic process. The biological behaviour may be very heterogeneous and a standardised therapy for these cases is still lacking, although some patients may benefit from antiretroviral therapy in a human immunodeficiency virus setting. Conclusions: The present case series highlights some characteristic findings of these entities to reaffirm useful cytopathological diagnostic criteria, stressing the crucial role of the appropriate technical processing of effusion fluids to obtain the best performances.

Published
2020

138. #EBUSTwitter: Novel use of social media for conception, coordination, and completion of an international, multicenter pathology study

Author

Lepe, M, Oltulu, P, Canepa, M, Wu, R, Deeken, A, Alex, D, Dinares, C, Doxtader, E, Fitzhugh, V, Gibier, J, Jain, D, Janaki, N, Jelinek, A, Labiano, T, L'Imperio, V, Michael, C, Mukhopadhyay, S, Pagni, F, Panizo, A, Pijuan, L, Quintana, L, Roy-Chowdhuri, S, Sanchez-Font, A, Sansano, I, Sauter, J, Skipper, D, Spruill, L, Torous, V, Gardner, J, Jiang, X, Lepe, Marcos, Oltulu, Pembe, Canepa, Mariana, Wu, Roseann I, Deeken, Amy, Alex, Deepu, Dinares, Carme, Doxtader, Erika E, Fitzhugh, Valerie A, Gibier, Jean-Baptiste, Jain, Deepali, Janaki, Nafiseh, Jelinek, Alexis, Labiano, Tania, L'Imperio, Vincenzo, Michael, Claire, Mukhopadhyay, Sanjay, Pagni, Fabio, Panizo, Angel, Pijuan, Lara, Quintana, Liza M, Roy-Chowdhuri, Sinchita, Sanchez-Font, Albert, Sansano, Irene, Sauter, Jennifer, Skipper, Daniel, Spruill, Laura S, Torous, Vanda, Gardner, Jerad Michael, Jiang, Xiaoyin Sara, Lepe, M, Oltulu, P, Canepa, M, Wu, R, Deeken, A, Alex, D, Dinares, C, Doxtader, E, Fitzhugh, V, Gibier, J, Jain, D, Janaki, N, Jelinek, A, Labiano, T, L'Imperio, V, Michael, C, Mukhopadhyay, S, Pagni, F, Panizo, A, Pijuan, L, Quintana, L, Roy-Chowdhuri, S, Sanchez-Font, A, Sansano, I, Sauter, J, Skipper, D, Spruill, L, Torous, V, Gardner, J, Jiang, X, Lepe, Marcos, Oltulu, Pembe, Canepa, Mariana, Wu, Roseann I, Deeken, Amy, Alex, Deepu, Dinares, Carme, Doxtader, Erika E, Fitzhugh, Valerie A, Gibier, Jean-Baptiste, Jain, Deepali, Janaki, Nafiseh, Jelinek, Alexis, Labiano, Tania, L'Imperio, Vincenzo, Michael, Claire, Mukhopadhyay, Sanjay, Pagni, Fabio, Panizo, Angel, Pijuan, Lara, Quintana, Liza M, Roy-Chowdhuri, Sinchita, Sanchez-Font, Albert, Sansano, Irene, Sauter, Jennifer, Skipper, Daniel, Spruill, Laura S, Torous, Vanda, Gardner, Jerad Michael, and Jiang, Xiaoyin Sara

Abstract

Context.-Social media sites are increasingly used for education, networking, and rapid dissemination of medical information, but their utility for facilitating research has remained largely untapped. Objective.-To describe in detail our experience using a social media platform (Twitter) for the successful initiation, coordination, and completion of an international, multi-institution pathology research study. Design.-Following a tweet describing a hitherto-unreported biopsy-related histologic finding in a mediastinal lymph node following endobronchial ultrasound-guided transbronchial needle aspiration, a tweet was posted to invite pathologists to participate in a validation study. Twitter's direct messaging feature was used to create a group to facilitate communication among participating pathologists. Contributing pathologists reviewed consecutive cases of mediastinal lymph node resection following endobronchial ultrasound-guided transbronchial needle aspiration and examined them specifically for biopsy site changes. Data spreadsheets containing deidentified data and digital photomicrographs of suspected biopsy site changes were submitted via an online file hosting service for central review by 5 pathologists from different institutions. Results.-A total of 24 pathologists from 14 institutions in 5 countries participated in the study within 143 days of study conception, and a total of 297 cases were collected and analyzed. The time interval between study conception and acceptance of the manuscript for publication was 346 days. Conclusions.-To our knowledge, this is the first time that a social media platform has been used to generate a research idea based on a tweet, recruit coinvestigators publicly, communicate with collaborating pathologists, and successfully complete a pathology study.

Published
2020

139. MALDI imaging in Fabry nephropathy: a multicenter study

Author

L'Imperio, V, Smith, A, Pisani, A, D'Armiento, M, Scollo, V, Casano, S, Sinico, R, Nebuloni, M, Tosoni, A, Pieruzzi, F, Magni, F, Pagni, F, Sinico, RA, L'Imperio, V, Smith, A, Pisani, A, D'Armiento, M, Scollo, V, Casano, S, Sinico, R, Nebuloni, M, Tosoni, A, Pieruzzi, F, Magni, F, Pagni, F, and Sinico, RA

Abstract

Background The current study evaluates the application of histology and in situ proteomics (MALDI-MSI) in Fabry nephropathy (FN), showing investigative and classification role for this coupled approach. Methods A retrospective series of 14 formalin fixed paraffin embedded (FFPE) renal biopsies with diagnosis of FN and 1 biopsy from a patient bearing a galactosidase-alpha (GLA) genetic variant of unknown significance (GVUS, c.376A>G) have been classified for clinical characteristics. Groups were compared for histological differences (following the ISGFN scoring system). Moreover, renal biopsies from these cases have been analyzed with MALDI-MSI as previously described to find proteomic signatures among different mutations and phenotypes. Results Comparison of clinical features revealed lower mean 24 h proteinuria in females (225 mg/24 h) than in males (1477.5 mg/24 h, p = 0.006). As for clinical characteristics, females significantly differed from males only for lower arterial sclerosis, with a mean value of 0.82 vs. 1.05 (p = 0.001). Proteomic analysis demonstrated specific signatures in different subgroups of FN patients. Moreover, MALDI correctly classified cases with undetermined mutation or GVUS. Conclusions The present study demonstrated the feasible application of MALDI-MSI in the analysis of FN FFPE renal biopsies, allowing the detection of putative signatures for phenotypic distinction and demonstrating genetic classification capabilities.

Published
2020

140. Combined Plasmatic and Tissue Approach to Membranous Nephropathy-Proposal of a Diagnostic Algorithm Including Immunogold Labelling: Changing the Paradigm of a Serum-based Approach

Author

L'Imperio, V, Pieruzzi, F, Sinico, R, Nebuloni, M, Tosoni, A, Granata, A, Santoro, D, Capelli, I, Garozzo, M, Casano, S, Smith, A, Radice, A, Pagni, F, Sinico, RA, L'Imperio, V, Pieruzzi, F, Sinico, R, Nebuloni, M, Tosoni, A, Granata, A, Santoro, D, Capelli, I, Garozzo, M, Casano, S, Smith, A, Radice, A, Pagni, F, and Sinico, RA

Abstract

Membranous nephropathy represents the most frequent cause of nephrotic syndrome in the adult, leading to end-stage renal disease in one third of all the patients. In the last years, the discovery of circulating autoantibodies against phospholipase A2 receptor 1 (PLA2R) and thrombospondin type-1 containing 7A domain (THSD7A), shed light on the pathogenesis of idiopathic forms, being responsible for 70% and 3% of all the cases, respectively. These identifications allowed the development of serological and histologic tests to detect autoantibodies and relative targets for diagnostic and prognostic purposes. Rising evidences suggest that serum titer correlates with disease activity and response to therapy. For these reasons, for patients with nephrotic syndrome, a serum-based approach has been proposed, reserving renal biopsy only in cases with doubtful/negative serology. However, the recent introduction of useful criteria for the interpretation of PLA2R/THSD7A immunohistochemistry could lead to high values of sensitivity and specificity for the in situ detection of target antigens. The present multicentric study on a series of membranous nephropathy cases with available serum/histologic correlation will show the importance of the crosstalk among the different techniques, recovering the possible role of electron microscopy in challenging situations.

Published
2020

143. MALDI-MS imaging in the search for proteomic indicators of response to therapy in membranous nephropathy

Author

Smith, A, L'Imperio, V, Pagni, F, Magni, F, Smith, A, L'Imperio, V, Pagni, F, and Magni, F

Subjects
kidney, MALDI-MSI, proteomics: membranous nephropathy
Abstract

Membranous Nephropathy (MN) is the most frequent cause of nephrotic syndrome in adults and the disease course is characterised by the “rule of third”, with one third of patients experiencing complete remission and the remaining experiencing relapses or progression of the disease. Additionally, the therapeutic approach is not standardised, leading to further heterogeneity in terms of response and outcome. In this pilot study, MALDI-MSI analysis was performed on renal biopsies obtained from two groups of patients, selected from 120 subjects with MN, which differentially responded to the range of immunosuppressive treatments administered. All the mass spectra were acquired in reflectron positive mode in the mass range of m/z 750 to 3500 using a rapifleX MALDI Tissuetyper™ with a pixel width and raster setting of 10µm, respectively. Three signals were determined to have a statistical significance when comparing the two patient groups (m/z 1111, 1198 and 1303) and had an altered signal intensity within glomeruli and tubular regions. Furthermore, the results highlighted the benefit of performing high spatial resolution MALD-MSI in the search prognostic markers of this frequent glomerulopathy. In particular, the signals that correlated with the response of the patient to the therapy could be spatially resolved within the different glomerular sub-structures and this localisation had a significant impact on the prognostic outlook of the patient. Despite much effort being made in recent years to understand the pathogenesis of MN, a panel of biomarkers able to predict the outcome of these patients following therapeutic treatment is still lacking. Here, we highlight a prospective panel of markers that can differentiate between these MN patients and could be a valuable starting point for a further study focused on verifying their predictive role in the treatment of Membranous Nephropathy

Published
2018

144. Progress in clinical applications for the proteomics MALDI Imaging analysis of thyroid fine needle aspiration biopsies

Author

Piga, I, Capitoli, G, Tettamanti, S, Denti, V, Smith, AJ, Chinello, C, Stella, M, Leni, D, Garancini, M, Galimberti, S, Magni, F, Pagni, F, Piga, I, Capitoli, G, Tettamanti, S, Denti, V, Smith, A, Chinello, C, Stella, M, Leni, D, Garancini, M, Galimberti, S, Magni, F, and Pagni, F

Subjects
Fine needle aspiration, MALDI-MSI proteomics, PreservCyt and CytoLyt stability, similarity score, thyroid, cancer
Published
2018

146. Progress in clinical applications for the MALDI-imaging analysis of thyroid fine needle aspiration biopsies: evaluation of proteomic stability in preservative solutions

Author

Piga, I, Capitoli, G, Tettamanti, S, Denti, V, Smith, AJ, Chinello, C, Stella, M, leni, D, Garancini, M, Galimberti, S, Magni, F, Pagni, F, Piga, I, Capitoli, G, Tettamanti, S, Denti, V, Smith, A, Chinello, C, Stella, M, Leni, D, Garancini, M, Galimberti, S, Magni, F, and Pagni, F

Subjects
Fine needle aspiration, MALDI-MSI proteomics, PreservCyt and CytoLyt stability, similarity score, thyroid, cancer
Published
2018

148. Advances in clinical proteomics for analysis of fine needle aspiration biopsies: evaluating proteomics stability in preservative solutions

Author

Piga, I, Capitoli, G, Tettamanti, S, Denti, V, Smith, AJ, Chinello, C, Stella, M, Leni, D, Garancini, M, Galimberti, S, Magni, F, Pagni, F, Piga, I, Capitoli, G, Tettamanti, S, Denti, V, Smith, A, Chinello, C, Stella, M, Leni, D, Garancini, M, Galimberti, S, Magni, F, and Pagni, F

Subjects
similarity score, cancer, thyroid, Fine needle aspiration, MALDI-MSI proteomics, PreservCyt and CytoLyt stability
Published
2018

149. Tissue MALDI Imaging

Author

Pagni, F, Antonia Vlahou, Harald Mischak, Jerome Zoidakis, Fulvio Magni, and Pagni, F

Subjects
MALDI Imaging
Published
2018

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