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2. CNN-Based Cell Analysis: From Image to Quantitative Representation

Author

Allier C, Herve L, Paviolo C, mandula O, Cioni O, Pierre W, Andriani F, Padmanabhan K, and Morales S

Abstract

We present a novel deep learning-based quantification pipeline for the analysis of cell culture images acquired by lens-free microscopy. The image reconstruction part of the pipeline features a convolutional neural network performing phase unwrapping and accelerating the inverse problem optimization. It allows phase retrieval at the 4K level (3,840 × 2,748 pixels) in 3s. The analysis part of the pipeline features a suite of convolutional neural networks estimating different cell metrics from the reconstructed image, that is, cell surface area, cell dry mass, cell length, and cell thickness. The networks have been trained to predict quantitative representation of the cell measurements that can be next translated into measurement lists with a local maxima algorithm. In this article, we discuss the performance and limitations of this novel deep learning-based quantification pipeline in comparison with a standard image processing solution. The main advantage brought by this method is the fast processing time, that is, the analysis rate of ∼25.000 cells measurements per second. Although our proof of principle has been established with lens-free microscopy, the approach of using quantitative cell representation in a deep learning framework can be similarly applied to other microscopy techniques. &nbsp

Published
2022

3. L’assedio e l’incendio di Rocavecchia (LE) nel Bronzo Medio: uno scheletro umano dal crollo della porta monumentale

Author

Maggio E., Vincenti G., Andriani F., Fabbri P. F., Maggio, E., Vincenti, G., Andriani, F., and Fabbri, P. F.

Subjects
Età del Bronzo, Rocavecchia, Incendio, Assedio, Guerra
Abstract

Durante gli scavi del 2017 nel sito di Rocavecchia (Lecce) è stato rinvenuto lo scheletro denominato RA7. L’individuo si trovava all’interno del crollo delle fortificazioni dell’Età del Bronzo (US 14202) nell’area della Porta Monumentale e si aggiunge a quelli già rinvenuti nel vano sud della porta stessa e nelle postierle B e C. Insieme costituiscono il più cospicuo campione di vittime di guerra insepolte rinvenuto in Italia in tale periodo. RA7 era un adulto di sesso probabilmente maschile che presenta tracce di combustione sulle ossa e gli esiti di un trauma cranico antemortem. E’ stato realizzato un rilievo fotogrammetrico 3D dello scheletro e dell’area circostante.

Published
2020

7. Development and Validity of Fluid Intelligence Test Based on Cattle-Horn-Carrol Theory: a Pilot Project

Author

Andriani, F. (Fitri), Andriani, F. (Fitri), Hadi, C. (Cholichul), Paramita, P. P. (Pramesti), Andriani, F. (Fitri), Andriani, F. (Fitri), Hadi, C. (Cholichul), and Paramita, P. P. (Pramesti)

Abstract

This study aimed to examine the validity of the Fluid Intelligence Test, constructed based on the Cattel-Horn-Carroll theory. There were two sources of validity used in this study, which were evidence based on the internal structure and evidence based on relation with other variables. Sixty-four items have been composed and tested to 242 people. The data was analyzed using confirmatory factor analysis technique and correlations technique to examine test validity. The result of this study showed that the prepared model worked quite well in describing the narrow abilities of fluid intelligence, as showed by the receipt of fit indexes accuracy of the model, such as Chi-Square value .42 (p = .518), Goodness Fit Index (GFI) = 1, and Rooted Mean Square Error (RMSEA) = .00. Similar result was also showed by its correlation with other variables, which are .717 (TIKI) and .606 (CFIT). This suggested that Fluid Intelligence Test has good validity.

Published
2016

9. Differential glycosylation of extracellular matrix specifically modulates lung cancer initiating cells subsets

Author

Bertolini, G, Gardelli, C, Andriani, F, Moro, M, Russo, L, Cipolla, L, Sozzi, G, Roz, L, Bertolini, G, Gardelli, C, Andriani, F, Moro, M, Russo, L, Cipolla, L, Sozzi, G, and Roz, L

Subjects
collagen, glycosylation, ECM, lung cancer
Abstract

In lung cancer CD133+ cells have properties of cancer initiating cells (CICs) as stemness features, high tumorigenic potential and chemoresistance. Within the CD133+ CICs, we have recently identified a specific subset, defined as CD133+CXCR4+EpCAM-, endowed with high dissemination and metastatic potential (metastasis initiating cells, MICs). In normal tissues stem cells reside in specialized niches composed of both stromal cells and extracellular matrix proteins (ECM) while factors responsible for CICs maintenance and modulation are relatively unknown. Collagen, the most abundant protein of ECM, plays a pivotal role in mediating regulation of adhesion, survival and proliferation of tumor cells. The relevance of collagen glycosylation, a fundamental post-translational modification controlling several biological processes, remains however largely unexplored. To investigate the effects of interactions between tumor cells and differentially glycosylated ECM epitopes, we cultured primary (LT73) and established lung cancer cell lines (A549, H460) on type I collagen films neo-glycosylated with glucose, galactose or sialic acid residues. Our results showed a general increase of CICs subsets, evaluated by flow cytometry, in tumor cells cultured on glycosylated collagen compared to pristine collagen or tissue culture plates with a concomitant increased expression of stemness-related genes. Particularly, we observed that collagen functionalized with glucose had the highest efficiency in enriching for MICs (3-fold change). Analysis of proliferation and viability of tumor cells cultured on collagen films showed that glucose residues were particularly proficient in causing G1 phase growth arrest and cell death compared to pristine collagen resulting in an overall decrease in the bulk population and CICs enrichment. In PKH label-retention assays, glucose-glycosylated collagen also selected and increased the fraction of PHK-labeled quiescent tumor cells, enriched for MICs component, confirming the preferential selection/survival of MICs subset. Using LT73 cell line depleted for CD133+ cells, we then proved that CICs increase was also due to a de novo generation of CD133+ cells and in particular of CD133+CXCR4+EpCAM- metastatic subset through non-CICs to CICs conversion. The immunophenotypic increase of CD133+ cells was functionally validated in vivo by a limiting dilution tumorigenic assay that estimated a 4.6 higher frequency of CICs in LT73 cells cultured on glucose-glycosylated collagen compared to control group. Moreover tumors derived from cells exposed to glucose residues retained a higher contents of MICs associated with an increased dissemination potential compared to controls. Our results suggest that differential collagen glycosylation could play an essential role in the creation of a niche favorable for the generation and selection/survival of lung metastasis initiating cells

Published
2016

10. Widespread activation of microglial cells in the hippocampus of chronic epileptic rats correlates only partially with neurodegeneration

Author

Uwe Heinemann, Ismini Papageorgiou, Andrea Lewen, Andriani F. Fetani, and Oliver Kann

Subjects
Male, Pathology, medicine.medical_specialty, Histology, Stereology, Cell Count, Status epilepticus, Biology, Hippocampal formation, Muscarinic Agonists, Hippocampus, medicine, Animals, Rats, Wistar, Analysis of Variance, CD11b Antigen, Epilepsy, Microglia, General Neuroscience, Dentate gyrus, Neurodegeneration, Calcium-Binding Proteins, Microfilament Proteins, Pilocarpine, medicine.disease, Rats, Disease Models, Animal, medicine.anatomical_structure, nervous system, Integrin alpha M, Chronic Disease, Nerve Degeneration, biology.protein, Anatomy, medicine.symptom, Neuroscience, medicine.drug
Abstract

Activation of microglial cells (brain macrophages) soon after status epilepticus has been suggested to be critical for the pathogenesis of mesial temporal lobe epilepsy (MTLE). However, microglial activation in the chronic phase of experimental MTLE has been scarcely addressed. In this study, we questioned whether microglial activation persists in the hippocampus of pilocarpine-treated, epileptic Wistar rats and to which extent it is associated with segmental neurodegeneration. Microglial cells were immunostained for the universal microglial marker, ionized calcium-binding adapter molecule-1 and the activation marker, CD11b (also known as OX42, Mac-1). Using quantitative morphology, i.e., stereology and Neurolucida-based reconstructions, we investigated morphological correlates of microglial activation such as cell number, ramification, somatic size and shape. We find that microglial cells in epileptic rats feature widespread, activation-related morphological changes such as increase in cell number density, massive up-regulation of CD11b and de-ramification. The parameters show heterogeneity in different hippocampal subregions. For instance, de-ramification is most prominent in the outer molecular layer of the dentate gyrus, whereas CD11b expression dominates in hilus. Interestingly, microglial activation only partially correlates with segmental neurodegeneration. Major neuronal death in the hilus, CA3 and CA1 coincides with strong up-regulation of CD11b. However, microglial activation is also observed in subregions that do not feature neurodegeneration, such as the molecular and granular layer of the dentate gyrus. This in vivo study provides solid experimental evidence that microglial cells feature widespread heterogeneous activation that only partially correlates with hippocampal segmental neuronal loss in experimental MTLE.

Published
2014

11. An in-vitro comparison of apical filling quality using of the root canals filled with the Element Obturation Unit and the EndoTwinn using the continuous condensation wave technique

Author

Andriani F., Sauro S., BARONI, CHIARA, GANDOLFI, MARIA GIOVANNA, Andriani F., Baroni C., Sauro S., and Gandolfi M.G.

Subjects
APICAL SEAL BY FLUID FILTRATION, ELEMENT OBTURATION UNIT, ENDOTWINN
Abstract

To evaluate by fluid filtration method the quality of endodontic apical seal obtained byEndoTwinn system as compared with Element Obturation Unit

Published
2006

13. Redistribution of astrocytic glutamine synthetase in the hippocampus of chronic epileptic rats

Author

Oliver Kann, Andriani F. Fetani, Siegrun Gabriel, Uwe Heinemann, and Ismini Papageorgiou

Subjects
Male, medicine.medical_specialty, Tissue Fixation, Excitotoxicity, Cell Count, Hippocampal formation, Muscarinic Agonists, medicine.disease_cause, Epileptogenesis, Hippocampus, Cellular and Molecular Neuroscience, Glutamate-Ammonia Ligase, Glutamine synthetase, Internal medicine, Glial Fibrillary Acidic Protein, medicine, Animals, Rats, Wistar, CA1 Region, Hippocampal, Microscopy, Confocal, Glial fibrillary acidic protein, biology, Glutamate receptor, Pilocarpine, CA3 Region, Hippocampal, Immunohistochemistry, Rats, Glutamine, Perfusion, Endocrinology, nervous system, Neurology, Epilepsy, Temporal Lobe, Astrocytes, biology.protein, Blood Vessels, medicine.drug
Abstract

Glutamine synthetase (GS) is an astrocytic enzyme, which catalyzes the synthesis of glutamine from glutamate and ammonia. In the central nervous system, GS prevents glutamate-dependent excitotoxicity and detoxifies nitrogen. Reduction in both expression and activity of GS was reported in the hippocampus of patients with temporal lobe epilepsy (TLE), and this reduction has been suggested to contribute to epileptogenesis. In this study, we characterized hippocampal GS expression in the pilocarpine model of TLE in Wistar rats by means of stereology and morphometric analysis. Neither the GS positive cell number nor the GS containing cell volume was found to be altered in different hippocampal subregions of chronic epileptic rats when compared with controls. Instead, redistribution of the enzyme at both intracellular and tissue levels was observed in the epileptic hippocampus; GS was expressed more in proximal astrocytic branches, and GS expressing astrocytic somata was located in closer proximity to vascular walls. These effects were not due to shrinkage of astrocytic processes, as revealed by glial fibrillary acidic protein staining. Our results argue for GS redistribution rather than downregulation in the rat pilocarpine model of TLE. The potential contribution of increased GS perivascular affinity to the pathogenesis of epilepsy is discussed as well.

Published
2011

16. FHIT and p53 status and response to platinum-based treatment in advanced non-small cell lung cancer

Author

Cortinovis, D, Andriani, F, Livio, A, Fabbri, A, Perrone, F, Marcomini, B, Pilotti, S, Mariani, L, Bidoli, P, Bajetta, E, Roz, L, Sozzi, G, Cortinovis, DL, Cortinovis, D, Andriani, F, Livio, A, Fabbri, A, Perrone, F, Marcomini, B, Pilotti, S, Mariani, L, Bidoli, P, Bajetta, E, Roz, L, Sozzi, G, and Cortinovis, DL

Abstract

Inactivation of the FHIT and TP53 genes is frequently observed in primary non-small cell lung cancers (NSCLC) and cell lines and may contribute to resistance to apoptotic stimuli elicited by various anti-tumor drugs. To evaluate a possible relationship between FHIT and TP53 status and response to platinum-analogue regimens, we retrospectively selected 55 NSCLC patients treated with carboplatin/gemcitabine. Pre-treatment formalin fixed biopsies were analyzed for FHIT and p53 protein expression by immunohistochemistry and representative micro dissected tissue for TP53 mutations by DG-DGGE/sequencing. The FHIT-negative immunophenotype (FHIT-, pathologic) was found in 33 patients (60%) and p53 over expression/mutation (p53+, pathologic) in 25 patients (45%). The FHIT-/p53+ combination was present in 12 patients (22%). Overall, there was partial response in 21 patients (38%), with subgroup response rates of 33% in FHIT+/p53-, 46% in FHIT+/p53+, 38% in FHIT-/p53- and 33% in FHIT-/p53+ patients. Median progression-free survival (PFS) was 9.6, 7.9, 6.8 and 5.9 months and median overall survival (OS) was 12.8, 11.9, 10.5 and 8.7 months in the four groups, respectively. The Group comparison showed significantly worse PFS (p=0.04) in FHIT-/p53+ than the other groups. There was no significant difference in OS between the groups. A trend (p=0.07) for shorter OS was found in FHIT- cases suggesting that NSCLC tumors carrying this feature are less responsive to treatment. This retrospective study indicates that FHIT-/p53+ status might be a biological variable influencing the efficacy of carboplatin/gemcitabine treatment in NSCLC.

Published
2008

28. Fragile histidine triad gene inactivation in lung cancer: the European Early Lung Cancer project.

Author

Verri C, Roz L, Conte D, Liloglou T, Livio A, Vesin A, Fabbri A, Andriani F, Brambilla C, Tavecchio L, Calarco G, Calabrò E, Mancini A, Tosi D, Bossi P, Field JK, Brambilla E, Sozzi G, EUELC Consortium, and Verri, Carla

Abstract

Rationale: Fragile histidine triad (FHIT) is a tumor suppressor gene involved in the pathogenesis of lung cancer.Objectives: The purpose of this study was to investigate the different molecular alterations leading to the inactivation of FHIT gene function and to validate their use as biomarkers of risk for progression of the disease in patients belonging to the multicentric European study for the Early detection of Lung Cancer (EUELC) who were resected for early-stage lung tumors.Methods: FHIT immunostaining was performed on 305 tumor samples. The methylation status of FHIT promoter was assessed by nested methylation-specific polymerase chain reaction (MSP-PCR) in 232 tumor and 225 normal lung samples of which a subset of 187 patients had available normal/tumor DNA pairs. Loss of heterozygosity (LOH) at the FHIT locus was analyzed in 202 informative cases by D3S1300 and D3S1234 microsatellite markers.Measurements and Main Results: Lost or reduced FHIT expression was found in 36.7 and 75.7% of the tumor samples, respectively. Methylation of the FHIT promoter was found in 36.7% of tumor and 32.7% of normal lung samples, whereas LOH was detected in 61.9% of the tumors. A strong association with complete loss of FHIT expression was present when methylation and LOH were analyzed together (P = 0.0064). Loss of FHIT protein expression was significantly more frequent in squamous cell carcinoma histotype (P < 0.0001) and in smokers (P = 0.008). FHIT methylation in normal lung was associated with an increased risk of progressive disease (OR, 2.27; P = 0.0415).Conclusions: Our results indicate that different molecular mechanisms interplay to inactivate FHIT expression and support the proposition that FHIT methylation in normal lung tissue could represent a prognostic marker for progressive disease. [ABSTRACT FROM AUTHOR]

Published
2009
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29. Plasma DNA quantification in lung cancer computed tomography screening: five-year results of a prospective study.

Author

Sozzi G, Roz L, Conte D, Mariani L, Andriani F, Lo Vullo S, Verri C, Pastorino U, Sozzi, Gabriella, Roz, Luca, Conte, Davide, Mariani, Luigi, Andriani, Francesca, Lo Vullo, Salvatore, Verri, Carla, and Pastorino, Ugo

Abstract

Rationale: Free circulating plasma DNA has emerged as a potential biomarker for early lung cancer detection. In a previous case-control study we have shown that high levels of plasma DNA are a strong risk factor for lung cancer. Objectives: To assess the diagnostic performance and prognostic value of plasma DNA levels in a cohort of 1,035 heavy smokers monitored by annual spiral computed tomography (CT) for 5 years. Methods: Plasma DNA levels were determined through real-time quantitative PCR at baseline and at time of lung cancer diagnosis. Screening performance of the assay was calculated through the area under the receiver-operating characteristic curve (AUC-ROC). Kaplan-Meier analyses were computed for association with prognosis. Measurements and Main Results: Median baseline concentration of plasma DNA was not different in individuals who developed CT-detected lung cancers in the 5-year period (n = 38) versus cancer-free control subjects (AUC-ROC, 0.496; P = 0.9330), and only slightly higher at the time of cancer diagnosis (AUC-ROC, 0.607; P = 0.0369). At surgery, plasma DNA was higher in tumors detected at baseline (AUC-ROC, 0.80; P < 0.0001) and in Stage II to IV tumors detected during the first 2 years of screening (AUC-ROC, 0.87; P < 0.0001). A longitudinal study of plasma DNA levels showed increased values approaching to lung cancer diagnosis (P = 0.0010). Higher plasma DNA was significantly associated with poorer 5-year survival (P = 0.0066). Conclusions: Baseline assessment of plasma DNA level does not improve the accuracy of lung cancer screening by spiral CT in heavy smokers. Higher levels of plasma DNA at surgery might represent a risk factor for aggressive disease. [ABSTRACT FROM AUTHOR]

Published
2009
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35. Differential glycosylation of collagen modulates lung cancer stem cell subsets through β1 integrin-mediated interactions

Author

Ornella Rondinone, Laura Cipolla, Laura Russo, Luca Roz, Cecilia Gardelli, Francesco Nicotra, Gabriella Sozzi, Massimo Moro, Francesca Andriani, Giulia Bertolini, Gardelli, C, Russo, L, Cipolla, L, Moro, M, Andriani, F, Rondinone, O, Nicotra, F, Sozzi, G, Bertolini, G, and Roz, L

Subjects
0301 basic medicine, cancer stem cells, collagen, Cancer Research, cancer stem cell, Glycosylation, Stromal cell, Lung Neoplasms, Mice, SCID, tumor–extracellular matrix interaction, Extracellular matrix, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Cell, Molecular, and Stem Cell Biology, Cancer stem cell, Cell Line, Tumor, medicine, Animals, Humans, AC133 Antigen, Lung cancer, Lung, Extracellular Matrix Proteins, glycan, Chemistry, Integrin beta1, General Medicine, medicine.disease, Phenotype, Cell biology, Extracellular Matrix, Crosstalk (biology), lung cancer, 030104 developmental biology, Oncology, A549 Cells, 030220 oncology & carcinogenesis, Neoplastic Stem Cells, glycans, tumor–extracellular matrix interactions, Original Article, Stem cell, Signal Transduction
Abstract

In lung cancer, CD133+ cells represent the subset of cancer stem cells (CSC) able to sustain tumor growth and metastatic dissemination. CSC function is tightly regulated by specialized niches composed of both stromal cells and extracellular matrix (ECM) proteins, mainly represented by collagen. The relevance of collagen glycosylation, a fundamental post‐translational modification controlling several biological processes, in regulating tumor cell phenotype remains, however, largely unexplored. To investigate the bioactive effects of differential ECM glycosylation on lung cancer cells, we prepared collagen films functionalized with glucose (Glc‐collagen) and galactose (Gal‐collagen) exploiting a neoglycosylation approach based on a reductive amination of maltose and lactose with the amino residues of collagen lysines. We demonstrate that culturing of tumor cells on collagen determines a glycosylation‐dependent positive selection of CSC and triggers their expansion/generation. The functional relevance of CD133+ CSC increase was validated in vivo, proving an augmented tumorigenic and metastatic potential. High expression of integrin β1 in its active form is associated with an increased proficiency of tumor cells to sense signaling from glycosylated matrices (glyco‐collagen) and to acquire stemness features. Accordingly, inhibition of integrin β1 in tumor cells prevents CSC enrichment, suggesting that binding of integrin β1 to Glc‐collagen subtends CSC expansion/generation. We provide evidence suggesting that collagen glycosylation could play an essential role in modulating the creation of a niche favorable for the generation and selection/survival of lung CSC. Interfering with this crosstalk may represent an innovative therapeutic strategy for lung cancer treatment., Glycans are well known for their involvement in recognition phenomena between cells; however, the role of small glycan epitopes in cell–extracellular matrix (ECM) interactions needs to be further elucidated. Here we exploit bioactive ECM mimetics, functionalizing type I collagen films with different glycans, to investigate the relevance of specific ECM glycosignatures in tumor‐ECM interactions. We show that in vitro culturing of lung cancer cells on glycosylated collagen films results in differential modulation of cancer stem cells (CSC), associated in vivo with an enhanced tumor initiation ability and increased metastatic potential. Interactions of CSC with glycosylated collagen are regulated through the active form of integrin β1. Interfering with integrin β1 signaling results in abrogation of CSC enrichment induced by glycosylated collagen.

Published
2021

36. nEU-Med project. Two cases of disability in an equestrian context from a 10th century royal court in Tuscany (Italy)

Author

Alexander Agostini, Serena Viva, Serena Siena, Giovanna Bianchi, Fabio Andriani, Pier Francesco Fabbri, Viva, S., Andriani, F., Siena, S., Agostini, A., Bianchi, G., and Fabbri, P. F.

Subjects
010506 paleontology, Archeology, medicine.medical_specialty, History, medicine.medical_treatment, Archaeological record, Context (language use), Archeologia altomedievale, Interpersonal violence, 01 natural sciences, Antropologia funeraria, Middle Age, Rare case, medicine, 0601 history and archaeology, Amputation, Polytraumatism, 0105 earth and related environmental sciences, 060102 archaeology, General surgery, Asymmetry, Excavation, 06 humanities and the arts, Antropologia funeraria, Archeologia altomedievale, Femoral diaphysis, Horse-riding
Abstract

Excavation carried out at the cemetery of Vetricella and dated between the 10th-11th centuries CE, has returned a high percentage of traumatized individuals, including two polytraumatized male skeletons, one featuring a well-healed amputation of the right leg, the other a mended femoral diaphysis fracture. Evidence of a healed amputation, the result of surgical work or interpersonal violence, is a rare case in the archaeological record. The focus of this study is the nature of the recorded trauma, leading to observations on the effects of equestrian practice in an early medieval community, as well as survival and physical adaptation to new conditions, all of which have ultimately contributed towards the general interpretation of the archaeological context. Images from CT scanning, external diameters and the degree of osteoarthrosis were used to quantify asymmetry between the left and right skeletal elements, providing further evidence of post-traumatic conditions. The recording of an iron spike-ferrule from the same burial area, identified as the lower end of a staff, would provide material indications as to the use of walking aids associated with individuals marked by clear issues of mobility.

Published
2021

37. Circulating mir-320a promotes immunosuppressive macrophages M2 phenotype associated with lung cancer risk

Author

Federica Facchinetti, Massimo Milione, Chiara Camisaschi, Francesca Andriani, Agata Cova, Gabriella Sozzi, Orazio Fortunato, Laura Caleca, Davide Conte, Veronica Huber, Ugo Pastorino, Massimo Moro, Valeria Cancila, Giovanni Centonze, Carla Verri, Luca Roz, Cristina Borzi, Claudio Tripodo, Chiara Castelli, Mattia Boeri, Fortunato O., Borzi C., Milione M., Centonze G., Conte D., Boeri M., Verri C., Moro M., Facchinetti F., Andriani F., Roz L., Caleca L., Huber V., Cova A., Camisaschi C., Castelli C., Cancila V., Tripodo C., Pastorino U., and Sozzi G.

Subjects
Male, Cancer Research, Cell type, Lung Neoplasms, Carcinogenesis, Neutrophils, Macrophage, Mice, SCID, Biology, medicine.disease_cause, Molecular Cancer Biology, 03 medical and health sciences, Paracrine signalling, Mice, 0302 clinical medicine, Immune system, Cell Line, Tumor, microRNA, medicine, Tobacco Smoking, Animals, Humans, Circulating MicroRNA, Lung cancer, Lung, Carcinogenesi, Tumor microenvironment, Animal, Macrophages, Gene Expression Profiling, Neutrophil, STAT4 Transcription Factor, medicine.disease, microenvironment, Xenograft Model Antitumor Assays, 3. Good health, Gene Expression Regulation, Neoplastic, Lung Neoplasm, MicroRNAs, lung cancer, Oncology, 030220 oncology & carcinogenesis, Cancer cell, Cancer research, Female, Tumor Escape, Human
Abstract

miRNAs play a central role in the complex signaling network of cancer cells with the tumor microenvironment. Little is known on the origin of circulating miRNAs and their relationship with the tumor microenvironment in lung cancer. Here, we focused on the cellular source and relative contribution of different cell types to circulating miRNAs composing our risk classifier of lung cancer using in vitro/in vivo models and clinical samples. A cell‐type specific expression pattern and topography of several miRNAs such as mir‐145 in fibroblasts, mir‐126 in endothelial cells, mir‐133a in skeletal muscle cells was observed in normal and lung cancer tissues. Granulocytes and platelets are the major contributors of miRNAs release in blood. miRNAs modulation observed in plasma of lung cancer subjects was consistent with de‐regulation of the same miRNAs observed during immunosuppressive conversion of immune cells. In particular, activated neutrophils showed a miRNA profile mirroring that observed in plasma of lung cancer subjects. Interestingly mir‐320a secreted by neutrophils of high‐risk heavy‐smokers promoted an M2‐like protumorigenic phenotype through downregulation of STAT4 when shuttled into macrophages. These findings suggest a multifactorial and nonepithelial cell‐autonomous origin of circulating miRNAs associated with risk of lung cancer and that circulating miRNAs may act in paracrine signaling with causative role in lung carcinogenesis and immunosuppression., What's new? microRNAs play a central role in the complex signaling network of cancer cells with the tumor microenvironment. However, little is known on the origin of circulating miRNAs and their mechanisms of action. This study found a multifactorial and non‐epithelial cell‐autonomous origin of circulating miRNAs associated with lung cancer risk. The findings also suggest a link between an immunosuppressive and pro‐tumorigenic microenvironment and modulation of circulating miRNAs associated with lung cancer risk. The authors propose a novel mechanism whereby miRNA released by neutrophils induce macrophage polarization to support lung cancer growth, highlighting the potential for reprogramming macrophages toward an anti‐tumor polarization.

Published
2019

38. Prefazione

Author

Michele Carducci, G. Andriani, F. Saponaro, and Carducci, Michele

Published
2017

39. FHIT and p53 status and response to platinum-based treatment in advanced non-small cell lung cancer

Author

B. Marcomini, Federica Perrone, Luca Roz, S. Pilotti, Francesca Andriani, A. Fabbri, Luigi Mariani, D. Cortinovis, E. Bajetta, Anna Livio, Gabriella Sozzi, P. Bidoli, Cortinovis, D, Andriani, F, Livio, A, Fabbri, A, Perrone, F, Marcomini, B, Pilotti, S, Mariani, L, Bidoli, P, Bajetta, E, Roz, L, and Sozzi, G

Subjects
Oncology, Male, p53, Cancer Research, Lung Neoplasms, medicine.medical_treatment, Deoxycytidine, Polymerase Chain Reaction, Carboplatin, Immunoenzyme Techniques, chemistry.chemical_compound, FHIT, Carcinoma, Non-Small-Cell Lung, Drug Discovery, Antineoplastic Combined Chemotherapy Protocols, Middle Aged, Prognosis, Acid Anhydride Hydrolases, Neoplasm Proteins, Survival Rate, Treatment Outcome, Immunohistochemistry, Female, Lung cancer, medicine.drug, Adult, medicine.medical_specialty, Biology, Internal medicine, Carcinoma, medicine, Biomarkers, Tumor, Humans, Chemotherapy, neoplasms, Survival rate, Aged, Neoplasm Staging, Retrospective Studies, Pharmacology, medicine.disease, Gemcitabine, chemistry, Mutation, Tumor Suppressor Protein p53
Abstract

Inactivation of the FHIT and TP53 genes is frequently observed in primary non-small cell lung cancers (NSCLC) and cell lines and may contribute to resistance to apoptotic stimuli elicited by various anti-tumor drugs. To evaluate a possible relationship between FHIT and TP53 status and response to platinum-analogue regimens, we retrospectively selected 55 NSCLC patients treated with carboplatin/gemcitabine. Pre-treatment formalin fixed biopsies were analyzed for FHIT and p53 protein expression by immunohistochemistry and representative micro dissected tissue for TP53 mutations by DG-DGGE/sequencing. The FHIT-negative immunophenotype (FHIT-, pathologic) was found in 33 patients (60%) and p53 over expression/mutation (p53+, pathologic) in 25 patients (45%). The FHIT-/p53+ combination was present in 12 patients (22%). Overall, there was partial response in 21 patients (38%), with subgroup response rates of 33% in FHIT+/p53-, 46% in FHIT+/p53+, 38% in FHIT-/p53- and 33% in FHIT-/p53+ patients. Median progression-free survival (PFS) was 9.6, 7.9, 6.8 and 5.9 months and median overall survival (OS) was 12.8, 11.9, 10.5 and 8.7 months in the four groups, respectively. The Group comparison showed significantly worse PFS (p=0.04) in FHIT-/p53+ than the other groups. There was no significant difference in OS between the groups. A trend (p=0.07) for shorter OS was found in FHIT- cases suggesting that NSCLC tumors carrying this feature are less responsive to treatment. This retrospective study indicates that FHIT-/p53+ status might be a biological variable influencing the efficacy of carboplatin/gemcitabine treatment in NSCLC.

Published
2008

40. The Perceptions and Experiences of Older People Living in the Aftermath of Lombok Earthquakes, Indonesia: A Qualitative Study.

Author

Aurizki GE, Efendi F, Indarwati R, Andriani F, Sari DW, and Noguchi-Watanabe M

Subjects
Humans, Indonesia, Aged, Male, Female, Aged, 80 and over, Interviews as Topic, Adaptation, Psychological, Middle Aged, Disasters, Earthquakes, Qualitative Research
Abstract

Introduction: Despite the growing knowledge of people's vulnerability following natural disasters, the perspective of older people has received limited attention. This study aimed to explore the perceptions and experiences of older people encountering the 2018 Lombok earthquakes., Methods: This exploratory qualitative study involved 16 older people living in one of the villages most affected by the 2018 earthquakes in Lombok Island, Nusa Tenggara Barat, Indonesia. The data were collected in June 2019 using semi-structured interviews. Participants' responses were digitally recorded and transcribed verbatim for analysis. The data were analysed using qualitative content analysis managed in NVivo., Results: From older people's perspectives, three themes were generated: surviving the disaster, dealing with life changes and navigating through challenges and hope. Each theme comprised two categories, which reflected the journey of older people from the early to the later phase of the disaster., Conclusions: Older people experienced critical conditions and difficulties both physically and mentally. They also experienced various emotional responses before accepting living situations following a disaster. Nurses should play a role in fulfilling the physical and mental health needs of older people in post-disaster conditions., Implications for Practice: This study can inform nurses and other key stakeholders about the needs of older people during and after natural disasters. Nurses need to be equipped with the skills and abilities to identify and meet the needs of older people in difficult situations and with limited resources., (© 2024 The Author(s). International Journal of Older People Nursing published by John Wiley & Sons Ltd.)

Published
2024
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41. Oxidative Carboxylation of Lignin: Exploring Reactivity of Different Lignin Types.

Author

Andriani F and Lawoko M

Subjects
Hydrogen Peroxide chemistry, Carboxylic Acids chemistry, Acetic Acid chemistry, Hydrolysis, Lignin chemistry, Oxidation-Reduction
Abstract

The increased interest in the utilization of lignin in biobased applications is evident from the rise in lignin valorization studies. The present study explores the responsiveness of lignin toward oxidative valorization using acetic acid and hydrogen peroxide. The pristine lignins and their oxidized equivalents were analyzed comprehensively using NMR and SEC. The study revealed ring opening of phenolic rings yielding muconic acid- and ester-end groups and side-chain oxidations of the benzylic hydroxyls. Syringyl units were more responsive to these reactions than guaiacyl units. The high selectivity of the reaction yielded oligomeric oxidation products with a narrower dispersity than pristine lignins. Mild alkaline hydrolysis of methyl esters enhanced the carboxylic acid content of oxidized lignin, presenting the potential to adjust the carboxylic acid content of lignin. While oxidation reactions in lignin valorization are well documented, this study showed the feasibility of employing optimized oxidation conditions to engineer tailored lignin-based material precursors.

Published
2024
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42. Whole-Genome Sequencing and Mutation Analyses of SARS-CoV-2 Isolates from Indonesia.

Author

Oktavianthi S, Lages AC, Kusuma R, Kurniasih TS, Trimarsanto H, Andriani F, Rustandi D, Meriyanti T, Yusuf I, Malik SG, Jo J, and Suriapranata I

Abstract

The SARS-CoV-2 infection that caused the COVID-19 pandemic has become a significant public health concern. New variants with distinct mutations have emerged, potentially impacting its infectivity, immune evasion capacity, and vaccine response. A whole-genome sequencing study of 292 SARS-CoV-2 isolates collected from selected regions of Indonesia between January and October 2021 was performed to identify the distribution of SARS-CoV-2 variants and common mutations in Indonesia. During January-April 2021, Indonesian lineages B.1.466.2 and B.1.470 dominated, but from May 2021, Delta's AY.23 lineage outcompeted them. An analysis of 7515 published sequences from January 2021 to June 2022 revealed a decline in Delta in November 2021, followed by the emergence of Omicron variants in December 2021. We identified C241T (5'UTR), P314L (NSP12b), F106F (NSP3), and D614G (Spike) mutations in all sequences. The other common substitutions included P681R (76.4%) and T478K (60%) in Spike, D377Y in Nucleocapsid (61%), and I82T in Membrane (60%) proteins. Breakthrough infection and prolonged viral shedding cases were associated with Delta variants carrying the Spike T19R, G142D, L452R, T478K, D614G, P681R, D950N, and V1264L mutations. The dynamic of SARS-CoV-2 variants in Indonesia highlights the importance of continuous genomic surveillance in monitoring and identifying potential strains leading to disease outbreaks.

Published
2024
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43. Hybrid epithelial-mesenchymal status of lung cancer dictates metastatic success through differential interaction with NK cells.

Author

Parodi M, Centonze G, Murianni F, Orecchia P, Andriani F, Roato I, Gardelli C, Balsamo M, Moro M, Taiè G, Pastorino U, Petretto A, Lavarello C, Milione M, Sozzi G, Roz L, Vitale M, and Bertolini G

Subjects
Humans, Epithelial-Mesenchymal Transition, Killer Cells, Natural, Transcription Factors, Lung Neoplasms pathology, Carcinoma, Non-Small-Cell Lung pathology
Abstract

Background: Epithelial to mesenchymal transition (EMT) endows cancer cells with pro-metastatic properties, which appear most effective when cells enter an intermediate hybrid (H) state, characterized by integrated mesenchymal (M) and epithelial (E) traits. The reasons for this advantage are poorly known and, especially, it is totally unexplored whether the interplay between H-cells and NK cells could have a role. Here we characterize the pro-metastatic mechanics of non-small cell lung cancer (NSCLC) H-cells and their subset of cancer-initiating cells (CICs), dissecting crucial interactions with NK cells., Methods: Human lung cancer cell lines and sublines representative of E, M, or H states, assessed by proteomics, were analyzed in vivo for their tumor-forming and disseminating capabilities. Interactions with NK cells were investigated in vitro using migration assays, cytotoxic degranulation assays, and evaluation of CD133+ CICs modulation after coculture, and validated in vivo through NK cell neutralization assays. Correlation between EMT status, NK cell infiltration, and survival data, was evaluated in a cohort of surgically resected NSCLC cases (n=79)., Results: We demonstrated that H-cells, have limited dissemination capability but show the highest potential to initiate metastases in vivo. This property was related to their ability to escape NK cell surveillance. Mechanistically, H-cells expressed low levels of NK-attracting chemokines (CXCL1 and CXCL8), generating poorly infiltrated metastases. Accordingly, proteomics and GO enrichment analysis of E, H, M cell lines showed that the related secretory processes could change during EMT.Furthermore, H-CICs uniquely expressed high levels of the inhibitory ligand B7-H3, which protected H-CIC from NK cell-mediated clearance. In vivo neutralization assays confirmed that, indeed, the pro-metastatic properties of H-cells are poorly controlled by NK cells.Finally, the analysis of patients revealed that detection of hybrid phenotypes associated with low NK infiltration in NSCLC clinical specimens could identify a subset of patients with poor prognosis., Conclusions: Our study demonstrates that H-cells play a central role in the metastatic spread in NSCLC. Such pro-metastatic advantage of H-cells is supported by their altered interaction with NK cells and by the critical role of B7-H3 in preserving their H-CIC component, indicating B7-H3 as a potential target in combined NK-based therapies., Competing Interests: Competing interests: None declared., (© Author(s) (or their employer(s)) 2024. Re-use permitted under CC BY-NC. No commercial re-use. See rights and permissions. Published by BMJ.)

Published
2024
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44. Evaluation of IL-4, MIP-1α, and MMP-9 gene expression levels in peri-implant tissues in peri-implantitis.

Author

Giro G, Taira J, Andriani F, Watinaga S, Bastos MF, and Shibli JA

Subjects
Humans, Chemokine CCL3 genetics, Interleukin-4 genetics, Case-Control Studies, Matrix Metalloproteinase 9 genetics, Gene Expression, Peri-Implantitis genetics, Peri-Implantitis metabolism, Peri-Implantitis pathology, Dental Implants
Abstract

This case-control study evaluated the gene expression levels of interleukin (IL)-4, macrophage inflammatory protein type 1 alpha (MIP-1α), and metalloproteinase (MMP)-9, factors involved in the formation of giant cells in healthy peri-implant tissue and peri-implantitis. Thirty-five subjects (15 healthy and 20 with peri-implantitis), who met the inclusion and exclusion criteria, were included in this study. The peri-implant tissue biopsies were subjected to total RNA extraction, DNAse treatment, and cDNA synthesis. Subsequently, the reaction of real-time PCR was performed to evaluate the gene expression levels of IL-4, MIP-1α, and MMP-9 concerning the reference gene. IL-4 gene expression showed higher (18-fold) values in the Peri-Implantitis Group of Patients when compared with the Healthy (Control) Group (p<0.0001). Although MIP- 1α and MMP-9 gene expression levels were higher in diseased implants, they showed no significant differences (p=0.06 and p=0.2337), respectively. Within the limitations of this study, the results showed that in tissues affected by peri-implantitis, only levels of Il-4 were increased when compared with tissues in the control group.

Published
2023
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45. Mammalian PERIOD2 regulates H2A.Z incorporation in chromatin to orchestrate circadian negative feedback.

Author

Tartour K, Andriani F, Folco EG, Letkova D, Schneider R, Saidi I, Sato T, Welz PS, Benitah SA, Allier C, and Padmanabhan K

Subjects
ARNTL Transcription Factors genetics, ARNTL Transcription Factors metabolism, Animals, Circadian Rhythm physiology, Feedback, Mammals genetics, Mice, Nucleosomes, Chromatin, Histones metabolism, Period Circadian Proteins metabolism
Abstract

Mammalian circadian oscillators are built on a feedback loop in which the activity of the transcription factor CLOCK-BMAL1 is repressed by the PER-CRY complex. Here, we show that murine Per -/- fibroblasts display aberrant nucleosome occupancy around transcription start sites (TSSs) and at promoter-proximal and distal CTCF sites due to impaired histone H2A.Z deposition. Knocking out H2A.Z mimicked the Per null chromatin state and disrupted cellular rhythms. We found that endogenous mPER2 complexes retained CTCF as well as the specific H2A.Z-deposition chaperone YL1-a component of the ATP-dependent remodeler SRCAP and p400-TIP60 complex. While depleting YL1 or mutating chaperone-binding sites on H2A.Z lengthened the circadian period, H2A.Z deletion abrogated BMAL1 chromatin recruitment and promoted its proteasomal degradation. We propose that a PER2-mediated H2A.Z deposition pathway (1) compacts CLOCK-BMAL1 binding sites to establish negative feedback, (2) organizes circadian chromatin landscapes using CTCF and (3) bookmarks genomic loci for BMAL1 binding to impinge on the positive arm of the subsequent cycle., (© 2022. The Author(s), under exclusive licence to Springer Nature America, Inc.)

Published
2022
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46. MiR-486-5p Targets CD133+ Lung Cancer Stem Cells through the p85/AKT Pathway.

Author

Moro M, Fortunato O, Bertolini G, Mensah M, Borzi C, Centonze G, Andriani F, Di Paolo D, Perri P, Ponzoni M, Pastorino U, Sozzi G, and Boeri M

Abstract

Despite improvements in therapies and screening strategies, lung cancer prognosis still remains dismal, especially for metastatic tumors. Cancer stem cells (CSCs) are endowed with properties such as chemoresistance, dissemination, and stem-like features, that make them one of the main causes of the poor survival rate of lung cancer patients. MicroRNAs (miRNAs), small molecules regulating gene expression, have a role in lung cancer development and progression. In particular, miR-486-5p is an onco-suppressor miRNA found to be down-modulated in the tumor tissue of lung cancer patients. In this study, we investigate the role of this miRNA in CD133+ lung CSCs and evaluate the therapeutic efficacy of coated cationic lipid-nanoparticles entrapping the miR-486-5p miRNA mimic (CCL-486) using lung cancer patient-derived xenograft (PDX) models. In vitro, miR-486-5p overexpression impaired the PI3K/Akt pathway and decreased lung cancer cell viability. Moreover, miR-486-5p overexpression induced apoptosis also in CD133+ CSCs, thus affecting the in vivo tumor-initiating properties of these cells. Finally, we demonstrated that in vivo CCL-486 treatment decreased CD133+ percentage and inhibited tumor growth in PDX models. In conclusion, we provided insights on the efficacy of a novel miRNA-based compound to hit CD133+ lung CSCs, setting the basis for new combined therapeutic strategies.

Published
2022
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47. Differential glycosylation of collagen modulates lung cancer stem cell subsets through β1 integrin-mediated interactions.

Author

Gardelli C, Russo L, Cipolla L, Moro M, Andriani F, Rondinone O, Nicotra F, Sozzi G, Bertolini G, and Roz L

Subjects
A549 Cells, AC133 Antigen metabolism, Animals, Cell Line, Tumor, Extracellular Matrix metabolism, Extracellular Matrix Proteins metabolism, Glycosylation, Humans, Lung metabolism, Mice, Mice, SCID, Signal Transduction physiology, Collagen metabolism, Integrin beta1 metabolism, Lung Neoplasms metabolism, Neoplastic Stem Cells metabolism
Abstract

In lung cancer, CD133+ cells represent the subset of cancer stem cells (CSC) able to sustain tumor growth and metastatic dissemination. CSC function is tightly regulated by specialized niches composed of both stromal cells and extracellular matrix (ECM) proteins, mainly represented by collagen. The relevance of collagen glycosylation, a fundamental post-translational modification controlling several biological processes, in regulating tumor cell phenotype remains, however, largely unexplored. To investigate the bioactive effects of differential ECM glycosylation on lung cancer cells, we prepared collagen films functionalized with glucose (Glc-collagen) and galactose (Gal-collagen) exploiting a neoglycosylation approach based on a reductive amination of maltose and lactose with the amino residues of collagen lysines. We demonstrate that culturing of tumor cells on collagen determines a glycosylation-dependent positive selection of CSC and triggers their expansion/generation. The functional relevance of CD133+ CSC increase was validated in vivo, proving an augmented tumorigenic and metastatic potential. High expression of integrin β1 in its active form is associated with an increased proficiency of tumor cells to sense signaling from glycosylated matrices (glyco-collagen) and to acquire stemness features. Accordingly, inhibition of integrin β1 in tumor cells prevents CSC enrichment, suggesting that binding of integrin β1 to Glc-collagen subtends CSC expansion/generation. We provide evidence suggesting that collagen glycosylation could play an essential role in modulating the creation of a niche favorable for the generation and selection/survival of lung CSC. Interfering with this crosstalk may represent an innovative therapeutic strategy for lung cancer treatment., (© 2020 The Authors. Cancer Science published by John Wiley & Sons Australia, Ltd on behalf of Japanese Cancer Association.)

Published
2021
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48. Circulating mir-320a promotes immunosuppressive macrophages M2 phenotype associated with lung cancer risk.

Author

Fortunato O, Borzi C, Milione M, Centonze G, Conte D, Boeri M, Verri C, Moro M, Facchinetti F, Andriani F, Roz L, Caleca L, Huber V, Cova A, Camisaschi C, Castelli C, Cancila V, Tripodo C, Pastorino U, and Sozzi G

Subjects
Animals, Carcinogenesis immunology, Cell Line, Tumor, Circulating MicroRNA blood, Female, Gene Expression Profiling, Gene Expression Regulation, Neoplastic immunology, Humans, Lung pathology, Lung Neoplasms blood, Lung Neoplasms genetics, Lung Neoplasms pathology, Macrophages metabolism, Male, Mice, Mice, SCID, MicroRNAs blood, Neutrophils immunology, Neutrophils metabolism, STAT4 Transcription Factor genetics, STAT4 Transcription Factor metabolism, Tobacco Smoking blood, Tobacco Smoking immunology, Xenograft Model Antitumor Assays, Circulating MicroRNA metabolism, Lung Neoplasms immunology, Macrophages immunology, MicroRNAs metabolism, Tumor Escape genetics
Abstract

miRNAs play a central role in the complex signaling network of cancer cells with the tumor microenvironment. Little is known on the origin of circulating miRNAs and their relationship with the tumor microenvironment in lung cancer. Here, we focused on the cellular source and relative contribution of different cell types to circulating miRNAs composing our risk classifier of lung cancer using in vitro/in vivo models and clinical samples. A cell-type specific expression pattern and topography of several miRNAs such as mir-145 in fibroblasts, mir-126 in endothelial cells, mir-133a in skeletal muscle cells was observed in normal and lung cancer tissues. Granulocytes and platelets are the major contributors of miRNAs release in blood. miRNAs modulation observed in plasma of lung cancer subjects was consistent with de-regulation of the same miRNAs observed during immunosuppressive conversion of immune cells. In particular, activated neutrophils showed a miRNA profile mirroring that observed in plasma of lung cancer subjects. Interestingly mir-320a secreted by neutrophils of high-risk heavy-smokers promoted an M2-like protumorigenic phenotype through downregulation of STAT4 when shuttled into macrophages. These findings suggest a multifactorial and nonepithelial cell-autonomous origin of circulating miRNAs associated with risk of lung cancer and that circulating miRNAs may act in paracrine signaling with causative role in lung carcinogenesis and immunosuppression., (© 2018 The Authors. International Journal of Cancer published by John Wiley & Sons Ltd on behalf of UICC.)

Published
2019
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49. Diagnostic role of circulating extracellular matrix-related proteins in non-small cell lung cancer.

Author

Andriani F, Landoni E, Mensah M, Facchinetti F, Miceli R, Tagliabue E, Giussani M, Callari M, De Cecco L, Colombo MP, Roz L, Pastorino U, and Sozzi G

Subjects
Aged, Carcinoma, Non-Small-Cell Lung genetics, Carcinoma, Non-Small-Cell Lung pathology, Circulating Tumor DNA blood, Disease-Free Survival, Extracellular Matrix, Extracellular Matrix Proteins blood, Extracellular Matrix Proteins genetics, Female, Gene Expression Regulation, Neoplastic, Humans, Male, Middle Aged, Prognosis, Sex Characteristics, Smokers, Carcinoma, Non-Small-Cell Lung blood, Collagen Type X blood, Collagen Type XI blood, Osteonectin blood
Abstract

Background: Interactions between cancer cells and the surrounding microenvironment are crucial determinants of cancer progression. During this process, bi-directional communication among tumor cells and cancer associated fibroblasts (CAF) regulate extracellular matrix (ECM) deposition and remodeling. As a result of this dynamic process, soluble ECM proteins can be released into the bloodstream and may represent novel circulating biomarkers useful for cancer diagnosis. The aim of the present study was to measure the levels of three circulating ECM related proteins (COL11A1, COL10A1 and SPARC) in plasma samples of lung cancer patients and in healthy heavy-smokers controls and test whether such measurements have diagnostic or prognostic value., Methods: Gene expression profiling of lung fibroblasts isolated from paired normal and cancer tissue of NSCLC patients was performed by gene expression microarrays. The prioritization of the candidates for the study of circulating proteins in plasma was based on the most differentially expressed genes in cancer associated fibroblasts. Soluble ECM proteins were assessed by western blot in the conditioned medium of lung fibroblasts and by ELISA assays in plasma samples., Results: Plasma samples from lung cancer patients and healthy heavy-smokers controls were tested for levels of COL11A1 and COL10A1 (n = 57 each) and SPARC (n = 90 each). Higher plasma levels of COL10A1 were detected in patients (p ≤ 0.001), a difference that was driven specifically by females (p < 0.001). No difference in COL11A1 levels between patients and controls was found. SPARC levels were also higher in plasma patients than controls (p < 0.001) with good performance in discriminating the two groups (AUC = 0.744). No significant association was observed between plasma proteins levels and clinicopathological features or survival., Conclusion: Soluble factors related to proficient tumor-stroma cross-talk are detectable in plasma of primary lung cancer patients and may represent a valuable complementary diagnostic tool to discriminate lung cancer patients from healthy heavy-smokers individuals as shown for the SPARC protein.

Published
2018
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50. MiR-16 regulates the pro-tumorigenic potential of lung fibroblasts through the inhibition of HGF production in an FGFR-1- and MEK1-dependent manner.

Author

Andriani F, Majorini MT, Mano M, Landoni E, Miceli R, Facchinetti F, Mensah M, Fontanella E, Dugo M, Giacca M, Pastorino U, Sozzi G, Delia D, Roz L, and Lecis D

Subjects
Animals, Female, Lung pathology, Mice, Fibroblasts metabolism, Hepatocyte Growth Factor antagonists & inhibitors, Lung metabolism, MicroRNAs metabolism, Receptor, Fibroblast Growth Factor, Type 1 metabolism
Abstract

Background: Fibroblasts are crucial mediators of tumor-stroma cross-talk through synthesis and remodeling of the extracellular matrix and production of multiple soluble factors. Nonetheless, little is still known about specific determinants of fibroblast pro-tumorigenic activity in lung cancer. Here, we aimed at understanding the role of miRNAs, which are often altered in stromal cells, in reprogramming fibroblasts towards a tumor-supporting phenotype., Methods: We employed a co-culture-based high-throughput screening to identify specific miRNAs modulating the pro-tumorigenic potential of lung fibroblasts. Multiplex assays and ELISA were instrumental to study the effect of miRNAs on the secretome of both primary and immortalized lung fibroblasts from lung cancer patients and to evaluate plasmatic levels of HGF in heavy smokers. Direct mRNA targeting by miRNAs was investigated through dual-luciferase reporter assay and western blot. Finally, the pro-tumorigenic activity of fibroblasts and their conditioned media was tested by employing in vitro migration experiments and mouse xenografts., Results: We identified miR-16 as a master regulator of fibroblast secretome and showed that its upregulation reduces HGF secretion by fibroblasts, impairing their capacity to promote cancer cell migration. This effect is due to a pleiotropic activity of miR-16 which prevents HGF expression through direct inhibition of FGFR-1 signaling and targeting of HGF mRNA. Mechanistically, miR-16 targets FGFR-1 downstream mediator MEK1, thus reducing ERK1/2 activation. Consistently, chemical or genetic inhibition of FGFR-1 mimics miR-16 activity and prevents HGF production. Of note, we report that primary fibroblast cell lines derived from lungs of heavy smokers express reduced miR-16 levels compared to those from lungs not exposed to smoke and that HGF concentration in heavy smokers' plasma correlates with levels of tobacco exposure. Finally, in vivo experiments confirmed that restoration of miR-16 expression in fibroblasts reduced their ability to promote tumor growth and that HGF plays a central role in the pro-tumorigenic activity of fibroblasts., Conclusions: Overall, these results uncover a central role for miR-16 in regulating HGF production by lung fibroblasts, thus affecting their pro-tumorigenic potential. Correlation between smoking exposure and miR-16 levels could provide novel clues regarding the formation of a tumor-proficient milieu during the early phases of lung cancer development.

Published
2018
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