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5. Does Alpha-lipoic acid improve effects on polycystic ovary syndrome?

Author

LAGANÀ, A. S., MONTI, N., FEDELI, V., GULLO, G., and BIZZARRI, M.

Abstract

Alpha-lipoic acid (ALA) plays a key role in many physiological processes, exerting anti-inflammatory, immunomodulatory, antioxidant, detoxifying, and insulin sensitizing activities. Since ALA improves insulin resistance (IR), it has been suggested that ALA could be beneficial it in the treatment of PCOS. The natural polyol myo-Inositol (myo-Ins) and its isomers (D-Chiro-Inositol, D-Chiro-Ins) has proven to improve PCOS features and clinical outcome, according to a compelling body of available studies. Few studies have proposed to strengthen the inositol effect by associating ALA. ALA does not seem to influence significantly reproductive hormones, while its beneficial effects are presumably restricted to the metabolic features of insulin resistant PCOS women. Therefore, ALA usefulness in improving inositol activity still awaits convincingly confirmation. Experimental studies as well as proper randomized, clinical trials should be specifically tailored to assess this hypothesis. In absence of reliable evidence, ALA should not be recommended in the routinary clinical management of PCOS, even if associated to myo-Ins. [ABSTRACT FROM AUTHOR]

Published
2022

7. Luminescent protein staining with Re(i) tetrazolato complexes

Author

Fiorini, V., Bergamini, L., Monti, N., Zacchini, S., Plush, S., Massi, Massimiliano, Hochkoeppler, A., Stefan, A., Stagni, S., Fiorini, V., Bergamini, L., Monti, N., Zacchini, S., Plush, S., Massi, Massimiliano, Hochkoeppler, A., Stefan, A., and Stagni, S.

Abstract

Within the general framework of our past and current studies dealing with the investigation of the photophysical properties and the biological behavior of the family of tetrazolato and tetrazole Re(i) complexes, we have endeavored to investigate their potential in the luminescent staining of proteins purified by acrylamide gel electrophoresis. With the aim to provide the first examples of luminescent Re(i) complexes to be exploited for this specific purpose, we have designed and prepared four new Re(i)-based species with the general formula fac-[Re(CO)3(N^N)(Tph)]2-/0, where Tph is the 5-(phenyl)tetrazolato anion and N^N is in turn represented by bathophenanthroline disulfonate (BPS), bathocuproine disulfonate (BCS) or by the SO3-free bathocuproine (BC). In this latter case, the neutral complex fac-[Re(CO)3(BC)(Tph)] served as a model species for the characterization of the former disulfonate complexes. Its cationic analogue fac-[Re(CO)3(BC)(Tph-Me)]+was also prepared by a straightforward methylation reaction. All complexes displayed bright phosphorescence in organic media and, relative to their water solubility, the dianionic species fac-[Re(CO)3(BPS)(Tph)]2-and fac-[Re(CO)3(BCS)(Tph)]2-were also highly emissive in aqueous solution. The sulfonate groups played a key role in promoting and significantly enhancing the luminescent staining performances of both the Re(i) complexes fac-[Re(CO)3(BPS)(Tph)]2-and fac-[Re(CO)3(BCS)(Tph)]2-for proteins. Highlighting a response superior to that of Coomassie Blue and comparable to the one obtained by the well-known silver staining method, these dianionic Re(i)-complexes could efficiently detect up to 50 ng of pure Bovine Serum Albumin (BSA), as well as all proteins found in a Standard Protein Marker mix and from a total protein extract. A lower but still good response for luminescent protein staining was surprisingly obtained by employing the-SO3-free neutral and cationic complexes fac-[Re(CO)3(BC)(Tph)] and fac-[Re(CO)3(BC)(Tp

Published
2018

9. Slavery as Social Institution

Author

Kevin Bales and Monti N. Datta

Subjects
Sex trafficking, Gender studies, Human trafficking, Sociology, Social institution
Abstract

This article is a replacement of the previous edition article by O. Patterson, volume 21, pp. 14146–14152, © 2001, Elsevier Ltd.

Published
2015
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19. �ber Alkaloide und verwandte K�rper

Author

Reichard, C., Rupp, E., Zinnius, E., Merck, E., Bertrand, G., Javillier, M., Weigel, G., Arnold, Behrens, Greshoff, M., Candussio, G., Barral, Et, Heyl, G., and Monti, N.

Subjects
Biochemistry, Analytical Chemistry
Abstract

n/a

Published
1912
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27. Colourless luminescent solar concentrators based on Iridium(III)-Phosphors

Author

Loris Giorgini, Greta Santi, Nicola Monti, Massimiliano Massi, Valentina Fiorini, Stefano Stagni, Giulia Vigarani, Michele Pavone, Francesca Fasulo, Ana B. Muñoz-García, Andrea Pucci, Fiorini, V., Monti, N., Vigarani, G., Santi, G., Fasulo, F., Massi, M., Giorgini, L., Munoz-Garcia, A. B., Pavone, M., Pucci, A., Stagni, S., Fiorini V., Monti N., Vigarani G., Santi G., Fasulo F., Massi M., Giorgini L., Munoz-Garcia A.B., Pavone M., Pucci A., and Stagni S.

Subjects
Materials science, Colourless LSCs, Ir(III) cyclometalated complexes, Luminescent solar concentrators, Phosphorescent metal complexes, Stokes-shifts, Tetrazole ligands, Transparent polymers, Colourless LSC, General Chemical Engineering, chemistry.chemical_element, Phosphor, 02 engineering and technology, 010402 general chemistry, Methacrylate, 01 natural sciences, chemistry.chemical_compound, Tetrazole ligand, Stokes-shift, Iridium, Methyl methacrylate, Acrylate, Luminescent solar concentrator, Process Chemistry and Technology, 021001 nanoscience & nanotechnology, Phosphorescent metal complexe, 0104 chemical sciences, chemistry, Ir(III) cyclometalated complexe, 2-Phenylpyridine, 0210 nano-technology, Luminescence, Phosphorescence, Nuclear chemistry
Abstract

The first real examples of luminescent solar concentrators (LSCs) based on Ir(III) cyclometalates, are described herein. Two new Ir(III) tetrazole complexes, namely [Ir(ppy)2(iQTZ-PPG)]+ and [Ir(npy)2(iQTZ-PPG)]+, where (C^N) = ppy, 2 phenylpyridine or npy = 2-(naphthalen-2-yl)pyridine and iQTZ-PPG = 1-(2-(prop-2-yn-1-yl)-2H-tetrazol-5-yl)isoquinoline, were synthesized, fully characterized and tested as phosphors for colourless LSCs. Notably, increasing quantities (0.2–1.8 wt %) of the new Ir(III) based phosphors were dispersed in different acrylate polymers like poly(methyl methacrylate), PMMA, poly(benzyl methacrylate), PBzMA and poly(cyclohexyl methacrylate), PCHMA, leading to visible transparent polymeric films exhibiting excellent photostability and bright yellow to orange phosphorescent emissions. The performances as solar collectors of all the Ir(III)-doped polymers were investigated, providing results comparable, or superior, to those obtained from colourless LSC based on organic fluorophores. In fact, the best optical efficiency (ηopt up to 7%, combined to transmittance close to 80% at 390 nm) was displayed by the polymer film obtained from physical dispersion of [Ir(ppy)2(iQTZ-PPG)]+ (1.4 wt %) in PCHMA.

Published
2021

29. Antibacterial activity of a new class of tris homoleptic Ru (II)-complexes with alkyl-tetrazoles as diimine-type ligands

Author

Nicola Monti, Massimiliano Massi, Stefano Zacchini, Alejandro Hochkoeppler, Alessandra Stefan, Loris Giorgini, Stefano Stagni, Valentina Fiorini, Monti N., Zacchini S., Massi M., Hochkoeppler A., Giorgini L., Fiorini V., Stefan A., and Stagni S.

Subjects
Tris, chemistry.chemical_classification, Deinococcus radioduran, biology, Gram-positive bacteria, Tetrazoles, Deinococcus radiodurans, General Chemistry, biology.organism_classification, Medicinal chemistry, Inorganic Chemistry, Antibacterial, chemistry.chemical_compound, chemistry, gram-positive bacteria, ruthenium (II) complexe, Homoleptic, Antibacterial activity, Diimine, Alkyl
Abstract

Herein, we describe a new family of tris chelate homoleptic Ru (II) complexes, [Ru(N^N)3]2+, where the role of the diimine-type ligands (N^N) was fulfilled by 2-pyridyl (PTZ) or 2-quinolyl tetrazole (QTZ) derivatives decorated with various alkyl substituents at the N-2 position of the tetrazole ring. The new Ru (II) complexes with general formula [Ru (PTZ-R)3]2+ and [Ru (QTZ-R)3]2+, were obtained as mixtures of facial (fac) and meridional (mer) isomers, as suggested by NMR (1H, 13C) experiments, and confirmed in the case of mer-[Ru (QTZ-Me)3]2+, by X-ray crystallography. The photophysical behavior of the tetrazole-based [Ru(N^N)3]2+ type species was investigated by UV–vis absorption spectroscopy, providing trends typical of polypyridyl Ru (II) complexes. The new homoleptic complexes fac/mer-[Ru (PTZ-R)3]2+ and fac/mer-[Ru (QTZ-R)3]2+ have been assessed for any eventual antimicrobial activity towards two different bacteria such as Gram-negative Escherichia coli and Gram-positive Deinococcus radiodurans. Whereas being inactive toward E. coli, the response of agar disks diffusion tests suggested that some of the new fac/mer Ru (II) complexes could inhibit the growth of D. radiodurans. This effect was further investigated by determining the growth kinetics in liquid medium of D. radiodurans exposed to the fac/mer-[Ru (PTZ-R)3]2+ and fac/mer-[Ru (QTZ-R)3]2+ complexes at different concentrations. The outcome of these experiments highlighted that the turn-on of the growth inhibitory effect took place as the linear hexyl chain was appended to the PTZ or QTZ scaffold, suggesting also how the inhibitory activity appeared more pronouncedly exerted by the facial isomers fac-[Ru (PTZ-Hex)3]2+ and fac-[Ru (QTZ-Hex)3]2+ (MIC = ca. 3.0 μg/ml) with respect to the corresponding meridional isomers (MIC = ca. 6.0 μg/ml).

Published
2020

30. Microgravity Modifies the Phenotype of Fibroblast and Promotes Remodeling of the Fibroblast–Keratinocyte Interaction in a 3D Co-Culture Model

Author

Valeria Fedeli, Alessandra Cucina, Simona Dinicola, Gianmarco Fabrizi, Angela Catizone, Luisa Gesualdi, Simona Ceccarelli, Abdel Halim Harrath, Saleh H. Alwasel, Giulia Ricci, Paola Pedata, Mariano Bizzarri, Noemi Monti, Fedeli, V., Cucina, A., Dinicola, S., Fabrizi, G., Catizone, A., Gesualdi, L., Ceccarelli, S., Harrath, A. H., Alwasel, S. H., Ricci, G., Pedata, P., Bizzarri, M., and Monti, N.

Subjects
Keratinocytes, Myofibroblast, Weightlessness, Organic Chemistry, α-SMA, General Medicine, Fibroblasts, Coculture Techniques, Catalysis, Computer Science Applications, Inorganic Chemistry, Phenotype, Fibroblast, Microgravity, Co-culture, Physical and Theoretical Chemistry, microgravity, fibroblasts, myofibroblasts, cytoskeleton, keratinocytes, co-culture, Molecular Biology, Weightlessness Simulation, Cytoskeleton, Keratinocyte, Spectroscopy
Abstract

Microgravity impairs tissue organization and critical pathways involved in the cell–microenvironment interplay, where fibroblasts have a critical role. We exposed dermal fibroblasts to simulated microgravity by means of a Random Positioning Machine (RPM), a device that reproduces conditions of weightlessness. Molecular and structural changes were analyzed and compared to control samples growing in a normal gravity field. Simulated microgravity impairs fibroblast conversion into myofibroblast and inhibits their migratory properties. Consequently, the normal interplay between fibroblasts and keratinocytes were remarkably altered in 3D co-culture experiments, giving rise to several ultra-structural abnormalities. Such phenotypic changes are associated with down-regulation of α-SMA that translocate in the nucleoplasm, altogether with the concomitant modification of the actin-vinculin apparatus. Noticeably, the stress associated with weightlessness induced oxidative damage, which seemed to concur with such modifications. These findings disclose new opportunities to establish antioxidant strategies that counteract the microgravity-induced disruptive effects on fibroblasts and tissue organization.

Published
2022
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31. Inositol Restores Appropriate Steroidogenesis in PCOS Ovaries Both In Vitro and In Vivo Experimental Mouse Models.

Author

Fedeli V, Unfer V, Dinicola S, Laganà AS, Canipari R, Monti N, Querqui A, Galante E, Laurenzi G, and Bizzarri M

Subjects
Female, Animals, Mice, Granulosa Cells metabolism, Granulosa Cells drug effects, Theca Cells metabolism, Theca Cells drug effects, Steroids biosynthesis, Polycystic Ovary Syndrome metabolism, Polycystic Ovary Syndrome pathology, Polycystic Ovary Syndrome drug therapy, Inositol pharmacology, Disease Models, Animal, Aromatase metabolism, Aromatase genetics, Receptors, FSH metabolism, Receptors, FSH genetics, Ovary metabolism, Ovary drug effects, Ovary pathology
Abstract

Androgen excess is a key feature of several clinical phenotypes of polycystic ovary syndrome (PCOS). However, the presence of FSH receptor (FSHR) and aromatase (CYP19A1) activity responses to physiological endocrine stimuli play a critical role in the pathogenesis of PCOS. Preliminary data suggest that myo-Inositol (myo-Ins) and D-Chiro-Inositol (D-Chiro-Ins) may reactivate CYP19A1 activity. We investigated the steroidogenic pathway of Theca (TCs) and Granulosa cells (GCs) in an experimental model of murine PCOS induced in CD1 mice exposed for 10 weeks to a continuous light regimen. The effect of treatment with different combinations of myo-Ins and D-Chiro-Ins on the expression of Fshr , androgenic, and estrogenic enzymes was analyzed by real-time PCR in isolated TCs and GCs and in ovaries isolated from healthy and PCOS mice. Myo-Ins and D-Chiro-Ins, at a ratio of 40:1 at pharmacological and physiological concentrations, positively modulate the steroidogenic activity of TCs and the expression of Cyp19a1 and Fshr in GCs. Moreover, in vivo, inositols (40:1 ratio) significantly increase Cyp19a1 and Fshr . These changes in gene expression are mirrored by modifications in hormone levels in the serum of treated animals. Myo-Ins and D-Chiro-Ins in the 40:1 formula efficiently rescued PCOS features by up-regulating aromatase and FSHR levels while down-regulating androgen excesses produced by TCs.

Published
2024
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33. System Biology Approach in Investigating Epithelial-Mesenchymal Transition (EMT).

Author

Monti N, Querqui A, Lentini G, Tafani M, and Bizzarri M

Subjects
Humans, Epithelial-Mesenchymal Transition genetics, Epithelial Cells, Biology, Biomarkers, Tumor Microenvironment, Transforming Growth Factor beta1, Neoplasms
Abstract

Epithelial-mesenchymal transition (EMT) is a trans-differentiating and reversible process that leads to dramatic cell phenotypic changes, enabling epithelial cells in acquiring mesenchymal phenotypes and behaviors. EMT plays a crucial role during embryogenesis, and occurs in several para-physiologic and pathological conditions, as during fibrosis or cancer development. EMT displays some hallmarks of critical transitions, as a sudden change in the overall configuration of a system in correspondence of specific tipping point around which a "catastrophic bifurcation" happens. The transition occurs when external conditions breach specific thresholds. This definition helps in highlighting two main aspects: (1) the change involves the overall system, rather than single, discrete components; (2) cues from the microenvironment play an irreplaceable role in triggering the transition. This evidence implies that critical transition should be ascertained focusing the investigation at the system level (rather than investigating only molecular parameters) in a well-defined context, as the transition is strictly dependent on the microenvironment in which it occurs. Therefore, we need a systems biology approach to investigate EMT across the Waddington-like epigenetic landscape wherein the participation of both internal and external cues can be studied to follow the extent and the main characteristics of the phenotypic transition. Herein, we suggest a set of systems parameters (motility, invasiveness) altogether with specific molecular/histological markers to identify those critical observables, which can be integrated into a comprehensive mechanistic model., (© 2024. The Author(s), under exclusive license to Springer Science+Business Media, LLC, part of Springer Nature.)

Published
2024
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34. Carboxyhemoglobin as biomarker of late-onset sepsis in preterm infants.

Author

Dani C, Remaschi G, Monti N, and Pratesi S

Subjects
Infant, Female, Infant, Newborn, Humans, Carboxyhemoglobin, Retrospective Studies, Biomarkers, Infant, Premature, Sepsis diagnosis
Abstract

Carboxyhemoglobin (COHb) is considered a biomarker of oxidative stress and previous studies reported an increase in COHb levels in preterm infants who develop late-onset sepsis (LOS). Our aim was to assess the correlation between COHb levels and the risk for LOS development. We retrospectively studied 100 preterm infants, 50 in the LOS and 50 in the no LOS group. COHb levels were measured on the day of diagnosis of the first episode of LOS, 3, 2, and 1 days before and 1 and 4 days after the onset of LOS. Logistic regression analysis showed that a higher level of COHb 2 days before the diagnosis of LOS increases the risk for LOS development (OR 12.150, 95% Cl 1.311-12.605; P = 0.028). A COHb level of 1.55% measured 2 days before the diagnosis of LOS is the best predictive threshold for LOS with a sensitivity of 70% and a specificity of 70%.    Conclusion: Increased levels of COHb may predict the diagnosis of LOS in very preterm infants with a good accuracy. If further studies confirm our findings, this easy-to-measure biomarker could provide neonatologists with another tool for monitoring and early diagnosis of sepsis in high-risk patients. What is Known: • Carboxyhemoglobin (COHb) is a biomarker of oxidative stress. • Previous studies reported an increase in COHb levels in preterm infants who develop late-onset sepsis (LOS). What is New: • COHb levels increased two days before the diagnosis of LOS and this increase was associated with the risk for developing LOS. • ROC curve analysis for COHb measured two days before the diagnosis of LOS showed that 1.55% is the best predictive threshold for LOS with a sensitivity of 70% and a specificity of 70%., (© 2023. The Author(s).)

Published
2023
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35. Myo-Inositol Reverses TGF-β1-Induced EMT in MCF-10A Non-Tumorigenic Breast Cells.

Author

Monti N, Dinicola S, Querqui A, Fabrizi G, Fedeli V, Gesualdi L, Catizone A, Unfer V, and Bizzarri M

Abstract

Epithelial-Mesenchymal Transition (EMT), triggered by external and internal cues in several physiological and pathological conditions, elicits the transformation of epithelial cells into a mesenchymal-like phenotype. During EMT, epithelial cells lose cell-to-cell contact and acquire unusual motility/invasive capabilities. The associated architectural and functional changes destabilize the epithelial layer consistency, allowing cells to migrate and invade the surrounding tissues. EMT is a critical step in the progression of inflammation and cancer, often sustained by a main driving factor as the transforming growth factor-β1 (TGF-β1). Antagonizing EMT has recently gained momentum as an attractive issue in cancer treatment and metastasis prevention. Herein, we demonstrate the capability of myo-inositol (myo-Ins) to revert the EMT process induced by TGF-β1 on MCF-10A breast cells. Upon TGF-β1 addition, cells underwent a dramatic phenotypic transformation, as witnessed by structural (disappearance of the E-cadherin-β-catenin complexes and the emergence of a mesenchymal shape) and molecular modifications (increase in N-cadherin, Snai1, and vimentin), including the release of increased collagen and fibronectin. However, following myo-Ins, those changes were almost completely reverted. Inositol promotes the reconstitution of E-cadherin-β-catenin complexes, decreasing the expression of genes involved in EMT, while promoting the re-expression of epithelial genes (keratin-18 and E-cadherin). Noticeably, myo-Ins efficiently inhibits the invasiveness and migrating capability of TGF-β1 treated cells, also reducing the release of metalloproteinase (MMP-9) altogether with collagen synthesis, allowing for the re-establishment of appropriate cell-to-cell junctions, ultimately leading the cell layer back towards a more compact state. Inositol effects were nullified by previous treatment with an siRNA construct to inhibit CDH1 transcripts and, hence, E-cadherin synthesis. This finding suggests that the reconstitution of E-cadherin complexes is an irreplaceable step in the inositol-induced reversion of EMT. Overall, such a result advocates for the useful role of myo-Ins in cancer treatment.

Published
2023
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36. Myo-Inositol and D-Chiro-Inositol as Modulators of Ovary Steroidogenesis: A Narrative Review.

Author

Bizzarri M, Monti N, Piombarolo A, Angeloni A, and Verna R

Subjects
Humans, Female, Aromatase, Inositol Phosphates, Glucose, Inositol pharmacology, Inositol chemistry, Polycystic Ovary Syndrome
Abstract

Myo-inositol is a natural polyol, the most abundant among the nine possible structural isomers available in living organisms. Inositol confers some distinctive traits that allow for a striking distinction between prokaryotes and eukaryotes, the basic clusters into which organisms are partitioned. Inositol cooperates in numerous biological functions where the polyol participates or by furnishing the fundamental backbone of several related derived metabolites, mostly obtained through the sequential addition of phosphate groups (inositol phosphates, phosphoinositides, and pyrophosphates). Overall myo-inositol and its phosphate metabolites display an entangled network, which is involved in the core of the biochemical processes governing critical transitions inside cells. Noticeably, experimental data have shown that myo-inositol and its most relevant epimer D-chiro-inositol are both necessary to permit a faithful transduction of insulin and of other molecular factors. This improves the complete breakdown of glucose through the citric acid cycle, especially in glucose-greedy tissues, such as the ovary. In particular, while D-chiro-inositol promotes androgen synthesis in the theca layer and down-regulates aromatase and estrogen expression in granulosa cells, myo-inositol strengthens aromatase and FSH receptor expression. Inositol effects on glucose metabolism and steroid hormone synthesis represent an intriguing area of investigation, as recent results have demonstrated that inositol-related metabolites dramatically modulate the expression of several genes. Conversely, treatments including myo-inositol and its isomers have proven to be effective in the management and symptomatic relief of a number of diseases associated with the endocrine function of the ovary, namely polycystic ovarian syndrome.

Published
2023
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37. Carboxyhemoglobin as biomarker of prematurity complications.

Author

Dani C, Remaschi G, Monti N, Pizzetti C, and Pratesi S

Subjects
Infant, Female, Infant, Newborn, Humans, Infant, Premature, Carboxyhemoglobin, Retrospective Studies, Gestational Age, Cerebral Hemorrhage complications, Biomarkers, Infant, Newborn, Diseases, Bronchopulmonary Dysplasia, Retinopathy of Prematurity complications
Abstract

Background: Carboxyhemoglobin (COHb) is considered a biomarker of oxidative stress and previous studies suggest a correlation between its blood level and prematurity complications. Our aim in this study was to assess the correlation between COHb levels and the risk for bronchopulmonary dysplasia (BPD), intraventricular hemorrhage (IVH), and retinopathy of prematurity (ROP)., Methods: We retrospectively studied 178 preterm infants with gestational age of 27.0 ± 1.5 weeks, among which 121 (68 %) had BPD, 43 (24 %) IVH, and 33 (19 %) ROP. COHb levels measured during the first seven days of life were recorded., Results: Logistic regression analysis showed that higher levels of COHb on the seventh day of life increases the risk for moderate-to-severe BPD (OR 4.552, 95 % Cl 1.220-16.997; P = 0.024), while higher levels of COHb on the fourth day of life increases the risk for grade 2-4 IVH (OR 5.537, 95 % Cl 1.602-19.134; P = 0.007)., Conclusions: COHb measured in the first week of life can contribute to predicting the risk for BPD and IVH, but not for ROP, in very preterm infants. Since COHb can be readily measured, its assessment can be useful in clinical practice for early identification of preterm infants at high risk for oxidative stress related complications., Competing Interests: Declaration of Competing Interest The authors declare that they have no known competing financial interests or personal relationships that could have appeared to influence the work reported in this paper., (Copyright © 2023. Published by Elsevier B.V.)

Published
2023
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38. Paradoxical Behavior of Oncogenes Undermines the Somatic Mutation Theory.

Author

Monti N, Verna R, Piombarolo A, Querqui A, Bizzarri M, and Fedeli V

Subjects
Carcinogenesis genetics, DNA, Humans, Mutation, Oncogenes genetics, Tumor Microenvironment genetics, Neoplasms genetics, Neoplasms pathology
Abstract

The currently accepted theory on the influence of DNA mutations on carcinogenesis (the Somatic Mutation Theory, SMT) is facing an increasing number of controversial results that undermine the explanatory power of mutated genes considered as "causative" factors. Intriguing results have demonstrated that several critical genes may act differently, as oncogenes or tumor suppressors, while phenotypic reversion of cancerous cells/tissues can be achieved by modifying the microenvironment, the mutations they are carrying notwithstanding. Furthermore, a high burden of mutations has been identified in many non-cancerous tissues without any apparent pathological consequence. All things considered, a relevant body of unexplained inconsistencies calls for an in depth rewiring of our theoretical models. Ignoring these paradoxes is no longer sustainable. By avoiding these conundrums, the scientific community will deprive itself of the opportunity to achieve real progress in this important biomedical field. To remedy this situation, we need to embrace new theoretical perspectives, taking the cell-microenvironment interplay as the privileged pathogenetic level of observation, and by assuming new explanatory models based on truly different premises. New theoretical frameworks dawned in the last two decades principally focus on the complex interaction between cells and their microenvironment, which is thought to be the critical level from which carcinogenesis arises. Indeed, both molecular and biophysical components of the stroma can dramatically drive cell fate commitment and cell outcome in opposite directions, even in the presence of the same stimulus. Therefore, such a novel approach can help in solving apparently inextricable paradoxes that are increasingly observed in cancer biology.

Published
2022
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39. Microgravity Modifies the Phenotype of Fibroblast and Promotes Remodeling of the Fibroblast-Keratinocyte Interaction in a 3D Co-Culture Model.

Author

Fedeli V, Cucina A, Dinicola S, Fabrizi G, Catizone A, Gesualdi L, Ceccarelli S, Harrath AH, Alwasel SH, Ricci G, Pedata P, Bizzarri M, and Monti N

Subjects
Coculture Techniques, Fibroblasts metabolism, Keratinocytes, Phenotype, Weightlessness Simulation, Weightlessness
Abstract

Microgravity impairs tissue organization and critical pathways involved in the cell-microenvironment interplay, where fibroblasts have a critical role. We exposed dermal fibroblasts to simulated microgravity by means of a Random Positioning Machine (RPM), a device that reproduces conditions of weightlessness. Molecular and structural changes were analyzed and compared to control samples growing in a normal gravity field. Simulated microgravity impairs fibroblast conversion into myofibroblast and inhibits their migratory properties. Consequently, the normal interplay between fibroblasts and keratinocytes were remarkably altered in 3D co-culture experiments, giving rise to several ultra-structural abnormalities. Such phenotypic changes are associated with down-regulation of α-SMA that translocate in the nucleoplasm, altogether with the concomitant modification of the actin-vinculin apparatus. Noticeably, the stress associated with weightlessness induced oxidative damage, which seemed to concur with such modifications. These findings disclose new opportunities to establish antioxidant strategies that counteract the microgravity-induced disruptive effects on fibroblasts and tissue organization.

Published
2022
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40. Personalization of medical treatments in oncology: time for rethinking the disease concept to improve individual outcomes.

Author

Bizzarri M, Fedeli V, Monti N, Cucina A, Jalouli M, Alwasel SH, and Harrath AH

Abstract

The agenda of pharmacology discovery in the field of personalized oncology was dictated by the search of molecular targets assumed to deterministically drive tumor development. In this perspective, genes play a fundamental "causal" role while cells simply act as causal proxies, i.e., an intermediate between the molecular input and the organismal output. However, the ceaseless genomic change occurring across time within the same primary and metastatic tumor has broken the hope of a personalized treatment based only upon genomic fingerprint. Indeed, current models are unable in capturing the unfathomable complexity behind the outbreak of a disease, as they discard the contribution of non-genetic factors, environment constraints, and the interplay among different tiers of organization. Herein, we posit that a comprehensive personalized model should view at the disease as a "historical" process, in which different spatially and timely distributed factors interact with each other across multiple levels of organization, which collectively interact with a dynamic gene-expression pattern. Given that a disease is a dynamic, non-linear process - and not a static-stable condition - treatments should be tailored according to the "timing-frame" of each condition. This approach can help in detecting those critical transitions through which the system can access different attractors leading ultimately to diverse outcomes - from a pre-disease state to an overt illness or, alternatively, to recovery. Identification of such tipping points can substantiate the predictive and the preventive ambition of the Predictive, Preventive and Personalized Medicine (PPPM/3PM). However, an unusual effort is required to conjugate multi-omics approaches, data collection, and network analysis reconstruction (eventually involving innovative Artificial Intelligent tools) to recognize the critical phases and the relevant targets, which could help in patient stratification and therapy personalization., Competing Interests: Conflict of interestThe authors declare no competing interests., (© The Author(s) 2021.)

Published
2021
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41. PCOS and Inositols: Controversial Results and Necessary Clarifications. Basic Differences Between D-Chiro and Myo-Inositol.

Author

Monastra G, Vucenik I, Harrath AH, Alwasel SH, Kamenov ZA, Laganà AS, Monti N, Fedeli V, and Bizzarri M

Subjects
Female, Humans, Inositol chemistry, Inositol therapeutic use, Polycystic Ovary Syndrome drug therapy
Abstract

Competing Interests: In the past, GM was employed as advisor by the company Lo.Li Pharma Co., Italy. The authors declare that this study did not receive any funding from private companies. Supporting funds were only received from King Saud University. The funder was not involved in the study design, collection, analysis, interpretation of data, the writing of this article or the decision to submit it for publication. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest.

Published
2021
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42. Survival Pathways Are Differently Affected by Microgravity in Normal and Cancerous Breast Cells.

Author

Monti N, Masiello MG, Proietti S, Catizone A, Ricci G, Harrath AH, Alwasel SH, Cucina A, and Bizzarri M

Subjects
Cell Adhesion, Cell Line, Cell Survival, Cytoskeleton metabolism, Extracellular Matrix Proteins metabolism, Extracellular Signal-Regulated MAP Kinases metabolism, Female, Humans, MCF-7 Cells, Proto-Oncogene Proteins c-akt metabolism, Signal Transduction, Apoptosis, Breast Neoplasms metabolism, Weightlessness
Abstract

Metazoan living cells exposed to microgravity undergo dramatic changes in morphological and biological properties, which ultimately lead to apoptosis and phenotype reprogramming. However, apoptosis can occur at very different rates depending on the experimental model, and in some cases, cells seem to be paradoxically protected from programmed cell death during weightlessness. These controversial results can be explained by considering the notion that the behavior of adherent cells dramatically diverges in respect to that of detached cells, organized into organoids-like, floating structures. We investigated both normal (MCF10A) and cancerous (MCF-7) breast cells and found that appreciable apoptosis occurs only after 72 h in MCF-7 cells growing in organoid-like structures, in which major modifications of cytoskeleton components were observed. Indeed, preserving cell attachment to the substrate allows cells to upregulate distinct Akt- and ERK-dependent pathways in MCF-7 and MCF-10A cells, respectively. These findings show that survival strategies may differ between cell types but cannot provide sufficient protection against weightlessness-induced apoptosis alone if adhesion to the substrate is perturbed.

Published
2021
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43. CpG and non-CpG Presenilin1 methylation pattern in course of neurodevelopment and neurodegeneration is associated with gene expression in human and murine brain.

Author

Monti N, Cavallaro RA, Stoccoro A, Nicolia V, Scarpa S, Kovacs GG, Fiorenza MT, Lucarelli M, Aronica E, Ferrer I, Coppedè F, Troen AM, and Fuso A

Subjects
Aged, Aged, 80 and over, Alzheimer Disease metabolism, Animals, Brain growth & development, Brain pathology, CpG Islands, Female, Humans, Male, Mice, Presenilin-1 metabolism, Alzheimer Disease genetics, Brain metabolism, DNA Methylation, Presenilin-1 genetics
Abstract

The Presenilin1 ( PSEN1 ) gene encodes the catalytic peptide of the γ-secretase complex, a key enzyme that cleaves the amyloid-β protein precursor (AβPP), to generate the amyloid-β (Aβ) peptides, involved in Alzheimer's Disease (AD). Other substrates of the γ-secretase, such as E-cadherin and Notch1, are involved in neurodevelopment and haematopoiesis. Gene-specific DNA methylation influences PSEN1 expression in AD animal models. Here we evaluated canonical and non-canonical cytosine methylation patterns of the PSEN1 5'-flanking during brain development and AD progression, in DNA extracted from the frontal cortex of AD transgenic mice (TgCRND8) and post-mortem human brain. Mapping CpG and non-CpG methylation revealed different methylation profiles in mice and humans. PSEN1 expression only correlated with DNA methylation in adult female mice. However, in post-mortem human brain, lower methylation, both at CpG and non-CpG sites, correlated closely with higher PSEN1 expression during brain development and in disease progression. PSEN1 methylation in blood DNA was significantly lower in AD patients than in controls. The present study is the first to demonstrate a temporal correlation between dynamic changes in PSEN1 CpG and non-CpG methylation patterns and mRNA expression during neurodevelopment and AD neurodegeneration. These observations were made possible by the use of an improved bisulphite methylation assay employing primers that are not biased towards non-CpG methylation. Our findings deepen the understanding of γ-secretase regulation and support the hypothesis that epigenetic changes can promote the pathophysiology of AD. Moreover, they suggest that PSEN1 DNA methylation in peripheral blood may provide a biomarker for AD.

Published
2020
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44. Rediscovery of natural compounds acting via multitarget recognition and noncanonical pharmacodynamical actions.

Author

Bizzarri M, Giuliani A, Monti N, Verna R, Pensotti A, and Cucina A

Subjects
Animals, Drug Discovery methods, Humans, Biological Products chemistry, Biological Products pharmacology
Abstract

Most drugs have a natural compound 'ancestor' acting as the lead molecule. Classic pharmacology does not explicitly take into consideration the peculiarities of natural origin compounds, the mechanism of action of which is interpreted by the same target-specific mode of action used for synthetic molecules. Over the past few decades, this approach has entered a crisis of efficacy, requiring general reconsideration of the nature of chemobiological interactions. Taking both the unique properties of natural compounds and their original presence in complex mixtures into account pushes researchers to enlarge the range of mechanisms of action well beyond the drug-receptor interaction and has the potential to overcome the current drug discovery crisis., (Copyright © 2020 Elsevier Ltd. All rights reserved.)

Published
2020
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45. Constraints Shape Cell Function and Morphology by Canalizing the Developmental Path along the Waddington's Landscape.

Author

Bizzarri M, Giuliani A, Minini M, Monti N, and Cucina A

Subjects
Cell Engineering, Environment, Gravitation, Humans, Kinetics, Models, Theoretical, Cellular Reprogramming genetics, Epigenesis, Genetic, Genotype, Phenotype
Abstract

Studies performed in absence of gravitational constraint show that a living system is unable to choose between two different phenotypes, thus leading cells to segregate into different, alternative stable states. This finding demonstrates that the genotype does not determine by itself the phenotype but requires additional, physical constraints to finalize cell differentiation. Constraints belong to two classes: holonomic (independent of the system's dynamical states, as being established by the space-time geometry of the field) and non-holonomic (modified during those biological processes to which they contribute in shaping). This latter kind of "constraints", in which dynamics works on the constraint to recreate them, have emerged as critical determinants of self-organizing systems, by manifesting a "closure of constraints." Overall, the constraints act by harnessing the "randomness" represented by the simultaneous presence of equiprobable events restraining the system within one attractor. These results cast doubt on the mainstream scientific concept and call for a better understanding of causation in cell biology., (© 2020 WILEY Periodicals, Inc.)

Published
2020
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46. Active Fraction from Embryo Fish Extracts Induces Reversion of the Malignant Invasive Phenotype in Breast Cancer through Down-regulation of TCTP and Modulation of E-cadherin/β-catenin Pathway.

Author

Proietti S, Cucina A, Pensotti A, Biava PM, Minini M, Monti N, Catizone A, Ricci G, Leonetti E, Harrath AH, Alwasel SH, and Bizzarri M

Subjects
Animals, Apoptosis drug effects, Biomarkers, Tumor metabolism, Cadherins metabolism, Cell Line, Tumor, Cell Movement drug effects, Down-Regulation, Humans, Phenotype, Tumor Protein, Translationally-Controlled 1, Zebrafish, beta Catenin metabolism, Antineoplastic Agents pharmacology, Breast Neoplasms metabolism, Embryo, Nonmammalian chemistry, Tissue Extracts pharmacology
Abstract

Some yet unidentified factors released by both oocyte and embryonic microenvironments demonstrated to be non-permissive for tumor development and display the remarkable ability to foster cell/tissue reprogramming, thus ultimately reversing the malignant phenotype. In the present study we observed how molecular factors extracted from Zebrafish embryos during specific developmental phases (20 somites) significantly antagonize proliferation of breast cancer cells, while reversing a number of prominent aspects of malignancy. Embryo extracts reduce cell proliferation, enhance apoptosis, and dramatically inhibit both invasiveness and migrating capabilities of cancer cells. Counteracting the invasive phenotype is a relevant issue in controlling tumor spreading and metastasis. Moreover, such effect is not limited to cancerous cells as embryo extracts were also effective in inhibiting migration and invasiveness displayed by normal breast cells undergoing epithelial-mesenchymal transition upon TGF-β1 stimulation. The reversion program involves the modulation of E-cadherin/β-catenin pathway, cytoskeleton remodeling with dramatic reduction in vinculin, as well as downregulation of TCTP and the concomitant increase in p53 levels. Our findings highlight that-contrary to the prevailing current "dogma", which posits that neoplastic cells are irreversibly "committed"-the malignant phenotype can ultimately be "reversed", at least partially, in response to environmental morphogenetic influences., Competing Interests: The authors declare they have not conflict of interest. The authors confirm that the funders had no influence over the study design, content of the article, or selection of this journal.

Published
2019
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47. Luminescent protein staining with Re(i) tetrazolato complexes.

Author

Fiorini V, Bergamini L, Monti N, Zacchini S, Plush SE, Massi M, Hochkoeppler A, Stefan A, and Stagni S

Subjects
Escherichia coli Proteins chemistry, L-Lactate Dehydrogenase chemistry, Lactoglobulins chemistry, Luminescence, Muramidase chemistry, Ovalbumin chemistry, Serum Albumin, Bovine chemistry, beta-Galactosidase chemistry, Coordination Complexes chemistry, Phenanthrolines chemistry, Rhenium chemistry
Abstract

Within the general framework of our past and current studies dealing with the investigation of the photophysical properties and the biological behavior of the family of tetrazolato and tetrazole Re(i) complexes, we have endeavored to investigate their potential in the luminescent staining of proteins purified by acrylamide gel electrophoresis. With the aim to provide the first examples of luminescent Re(i) complexes to be exploited for this specific purpose, we have designed and prepared four new Re(i)-based species with the general formula fac-[Re(CO)3(N^N)(Tph)]2-/0, where Tph is the 5-(phenyl)tetrazolato anion and N^N is in turn represented by bathophenanthroline disulfonate (BPS), bathocuproine disulfonate (BCS) or by the SO3- free bathocuproine (BC). In this latter case, the neutral complex fac-[Re(CO)3(BC)(Tph)] served as a model species for the characterization of the former disulfonate complexes. Its cationic analogue fac-[Re(CO)3(BC)(Tph-Me)]+ was also prepared by a straightforward methylation reaction. All complexes displayed bright phosphorescence in organic media and, relative to their water solubility, the dianionic species fac-[Re(CO)3(BPS)(Tph)]2- and fac-[Re(CO)3(BCS)(Tph)]2- were also highly emissive in aqueous solution. The sulfonate groups played a key role in promoting and significantly enhancing the luminescent staining performances of both the Re(i) complexes fac-[Re(CO)3(BPS)(Tph)]2- and fac-[Re(CO)3(BCS)(Tph)]2- for proteins. Highlighting a response superior to that of Coomassie Blue and comparable to the one obtained by the well-known silver staining method, these dianionic Re(i)-complexes could efficiently detect up to 50 ng of pure Bovine Serum Albumin (BSA), as well as all proteins found in a Standard Protein Marker mix and from a total protein extract. A lower but still good response for luminescent protein staining was surprisingly obtained by employing the -SO3- free neutral and cationic complexes fac-[Re(CO)3(BC)(Tph)] and fac-[Re(CO)3(BC)(Tph-Me)]+, respectively. These preliminary results open up new possibilities for the further widening of the use of Re(i)-based complexes as luminescent protein staining agents.

Published
2018
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48. Kinetic analysis of thapsigargin-induced thymocyte apoptosis.

Author

Bustamante J, Di Libero E, Fernandez-Cobo M, Monti N, Cadenas E, and Boveris A

Subjects
Animals, Calcium metabolism, Carcinogens toxicity, Cell Culture Techniques, Kinetics, Male, Microsomes drug effects, Microsomes metabolism, Mitochondria drug effects, Mitochondria metabolism, Nitric Oxide metabolism, Rats, Rats, Sprague-Dawley, Thymus Gland cytology, Thymus Gland physiology, Apoptosis drug effects, Thapsigargin toxicity, Thymus Gland drug effects
Abstract

Thapsigargin addition to thymocytes increased cytosolic Ca2+ by a factor of 8.5 with a time for half maximal effect (t1/2) of 2.5 min. Calcium signaling increased mitocondrial and endoplasmic reticulum nitric oxide synthase (NOS) activities by five and six times, with t1/2 of 16 and 48 min, respectively, followed by increases of 140% in intracellular [H2O2], 73% in hydroperoxide content, and 250% in thiobarbituric reactive substance content, with t1/2 of 13, 27, and 30 min, respectively. Mitochondrial dysfunction followed, and was characterized by decreased respiratory control, membrane depolarization, and decrease cytochrome c content release, processes with t1/2 of 101, 129, and 133 min, respectively. Increased UDP-GT gene expression, observed by mRNA synthesis, and the enzymatic activity of this protein had t1/2 of 52 and 187 min, respectively. These events were followed by caspase-3 activation (t1/2 = 210 min) and DNA laddering (t1/2 = 260 min) at the completion of the cell death program. Preincubation of thymocytes with NOS inhibitors (NG-methyl-L-arginine and L-Nomega-nitro-L-arginine methylester) halted the whole process through inhibition of mitochondrial and endoplasmic reticulum NOS activities and of DNA laddering.

Published
2004
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49. Pharmacokinetic behaviour of antithrombin III following intravenous infusion in healthy volunteers.

Author

Marzo A, Ceppi-Monti N, Giusti A, Abbiati G, and Parenti M

Subjects
Adult, Antithrombin III administration & dosage, Antithrombin III pharmacology, Area Under Curve, Blood Coagulation drug effects, Female, Half-Life, Humans, Infusions, Intravenous, Male, Middle Aged, Serine Proteinase Inhibitors administration & dosage, Serine Proteinase Inhibitors pharmacology, Sterilization, Ultrafiltration, Antithrombin III pharmacokinetics, Serine Proteinase Inhibitors pharmacokinetics
Abstract

Antithrombin III (CAS 52014-67-2) is produced from plasma of healthy donors and is purified from any detectable agent of transmissible infection. This drug is used in therapy by i.v. route to manage acute thrombotic episodes and to treat patients suffering from its deficiency. The present trial was conducted with the aim to evaluate the pharmacokinetics and the safety of a new preparation of antithrombin III, which in the purification procedure has included a nanofiltration step to increase the safety against the transmission of any agent of infection. The trial was conducted in twelve healthy volunteers of either sex. All the ethics procedures were fully respected, namely the approval from Ethics Committee, the notification to the central regulatory authority, the approval of consent form in writing. Volunteers were hospitalized about 36 h before drug treatment. The baseline situation was investigated throughout the day before the treatment (day-1). On day 1, the drug was infused i.v. for 20 min. Twenty blood samples were drawn from each volunteer, in baseline situation, during and after the infusion. Functional antithrombin III, antithrombin III antigen, prothrombin time, partial thromboplastin time were evaluated in all plasma samples. Both functional antithrombin III and antithrombin III antigen produced well defined plasma concentration-time profiles after the infusion, which allowed net values of these two analytes to be obtained subtracting baseline from post-infusion concentrations. Net pharmacokinetic parameters of functional antithrombin III and antithrombin III antigen proved to be almost superimposable. A comparison of data obtained in this trial on healthy volunteers with those previously obtained by other authors on target population demonstrates similar and fully comparable results. The authors conclude that the nanofiltration step neither affects at all the pharmacokinetics/pharmacodynamics nor the safety of the formulation investigated.

Published
2002
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50. Comparative bioavailability of two formulations containing atenolol and chlortalidone associated in a 4:1 fixed combination.

Author

Marzo A, Monti NC, Dal Bo L, Mazzucchelli P, Crivelli F, Tettamanti RA, Ismaili S, Uhr MR, Ronchi C, and Porziotta E

Subjects
Adrenergic beta-Antagonists administration & dosage, Adult, Antihypertensive Agents administration & dosage, Area Under Curve, Atenolol administration & dosage, Biological Availability, Chlorthalidone administration & dosage, Diuretics, Drug Combinations, Female, Half-Life, Humans, Male, Sodium Chloride Symporter Inhibitors administration & dosage, Therapeutic Equivalency, Adrenergic beta-Antagonists pharmacokinetics, Antihypertensive Agents pharmacokinetics, Atenolol pharmacokinetics, Benzothiadiazines, Chlorthalidone pharmacokinetics, Sodium Chloride Symporter Inhibitors pharmacokinetics
Abstract

Atenolol (CAS 29122-68-7) and chlortalidone (CAS 77-36-1) are marketed associated in a 4:1 strength ratio (100/25 and 50/12.5 mg) for the treatment of hypertension. According to EU guidelines, the bioequivalence of one dosage strength can also cover additional strengths when the pharmacokinetics of a given drug is linearly related with the dose. The kinetics of atenolol is linearly correlated with the dose and chlortalidone has linear kinetics with doses < or = 100 mg. Thus this trial carried out on the 100/25 mg strength also covers the 50/12.5 mg strength. The trial was carried out on 18 healthy volunteers (9 males and 9 females) according to a single dose, two-period, two-treatment, two-sequence study design with washout. Timed atenolol plasma concentrations and chlortalidone blood concentrations were used to assess primary pharmacokinetic parameters Cmax, tmax and AUC extrapolated to infinity by a non-compartmental model. The bioavailability of the two formulations was compared through the 90% confidence intervals (C.I.) of Cmax and AUC in accordance with operating guidelines. C.I. of chlortalidone were fully comprised in the 0.80-1.25 range. In the case of atenolol, which displayed a higher data dispersion, C.I. were comprised in the enlarged 0.70-1.43 range. Time to peak, tmax, did not show any statistically significant difference between the test and reference product with respect to both analytes. Pharmacodynamic measurements of the decrease in systolic blood pressure led to fully overlapping results with test and reference. The authors conclude that the test formulation should be considered bioequivalent with the reference with chlortalidone and in the borderline of bioequivalence with atenolol. As no safety problems were involved and pharmacodynamics led to overlapping results as between test and reference, the bioequivalence conclusion could be extended also to atenolol.

Published
2000
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