Your search keyword '"SERAFINI, MARTA"' showing total 15 results

1. Establishment of bone marrow and hematopoietic niches in vivo by reversion of chondrocyte differentiation of human bone marrow stromal cells

Author

Serafini, Marta, Sacchetti, Benedetto, Pievani, Alice, Redaelli, Daniela, Remoli, Cristina, Biondi, Andrea, Riminucci, Mara, and Bianco, Paolo

Published

2014

2. The multicomponent Passerini reaction as a means of accessing diversity in structure, activity and properties: Soft and hard vanilloid/cannabinoid modulators.

Author

Lamberti, Angela, Serafini, Marta, Aprile, Silvio, Bhela, Irene Preet, Goutsiou, Georgia, Pessolano, Emanuela, Fernandez-Ballester, Gregorio, Ferrer-Montiel, Antonio, Di Martino, Rita Maria Concetta, Fernandez-Carvajal, Asia, and Pirali, Tracey

Subjects

*G protein coupled receptors, *ENZYME inactivation, *LIGANDS (Biochemistry), *TRPV cation channels, *THERAPEUTICS

Abstract

A growing body of evidence points to the existence of a crosstalk between the endovanilloid (EV)- and the endocannabinoid (EC) systems, leading to the concept of a single system based on a shared set of endogenous ligands and regulation mechanisms. The EV/EC system encompasses the ion channel TRPV1, the G protein coupled receptors CB1 and CB2, their endogenous ligands and the enzymes for biosynthesis and inactivation. Disorders in which the EV/EC interaction is involved are inflammation, pain, neurodegenerative diseases and disorders of bones and skin. In the present paper, with the aim of targeting the EV/EC system, the Passerini reaction is used in a diversity-oriented approach to generate a series of α-acyloxycarboxamides bearing different substructures that resemble endogenous ligands. Compounds have been screened for activity on TRPV1, CB1 and CB2 and metabolic stability in skin cells, liver subcellular fractions and plasma. This protocol allowed to generate agents characterized by a diverse activity on TRPV1, CB1 and CB2, as well as heterogeneous metabolic stability that could allow different routes of administration, from soft drugs for topical treatment of skin diseases to hard drugs for systemic use in inflammation and pain. Compared to natural mediators, these compounds have a better drug-likeness. Among them, 41 stands out as an agonist endowed with a well-balanced activity on both TRPV1 and CB2, high selectivity over TRPM8, TRPA1 and CB1, metabolic stability and synthetic accessibility. [Display omitted] • The crosstalk between the vanilloid and the endocannabinoid systems plays a key role in pain and skin diseases. • Only a few drug-like modulators that target both the systems are known. • Using the Passerini multicomponent reaction compounds able to target the two systems have been discovered. • A dual modulator targeting TRPV1/CB2 is reported. [ABSTRACT FROM AUTHOR]

Published

2024

3. Soft drugs for dermatological applications: recent trends.

Author

Aprile, Silvio, Serafini, Marta, and Pirali, Tracey

Subjects

*TRPV cation channels, *HISTONE deacetylase, *TREATMENT effectiveness, *ATOPIC dermatitis

Abstract

• A dermatological SD is stable in skin and is rapidly inactivated once entering systemic circulation. • The SD design allows the development of safer drugs. • The design and development of a successful SD should fulfil a set of softness criteria. • Soft targeting has recently involved PDE4, S1PR1, TRPV1, JAK, caspase 1 and HDAC. A soft drug (SD) displays a metabolically labile spot and, after having exerted its activity in the site of action, undergoes a fast metabolism, leading to inactive metabolites. The SD approach has recently found widespread application in the dermatological field because it provides a means of localising the therapeutic effect in skin, while minimising systemic exposure. The literature is rapidly growing of successful examples of compounds targeting sphingosine-1-phosphate receptor 1 (S1PR1), transient receptor potential vanilloid 1 (TRPV1), Janus kinase (JAK), caspase 1, and histone deacetylase (HDAC), for the treatment of skin inflammatory, autoimmune, and oncological diseases. As a demonstration of the potential of this strategy, the SD approach recently led to the approval of crisaborole, a soft phosphodiesterase 4 (PDE4) inhibitor, for atopic dermatitis, while other agents are in clinical development. The soft drug approach is an effective strategy to define the action of topical dermatological drugs in the skin and obtain safer drugs. [ABSTRACT FROM AUTHOR]

Published

2019

4. Arynes and isocyanides: Two close-knit partners in multicomponent reactions.

Author

Serafini, Marta and Pirali, Tracey

Subjects

ARYNE, ISOCYANIDES, BENZYNES, RING formation (Chemistry), REACTIVITY (Chemistry)

Abstract

Despite benzyne has been known since 1940, this fascinating species has received much attention only over the last decades. The renaissance of interest in aryne chemistry is ascribable to the seminal discovery that arynes can be generated in situ from stable and commercially available precursors under mild and neutral conditions. Thanks to their high reactivity, arynes are key intermediates in countless chemical transformations ranging from cycloadditions to insertions and, among all these approaches, multicomponent reactions (MCRs) are currently standing out in this field. In particular, this short article is focused on MCRs involving the concomitant use of benzyne and isocyanides. Furthermore, the first overview on aryne MCRs triggered by α-isocyanoacetamides is presented. [ABSTRACT FROM AUTHOR]

Published

2018

5. The use of 2-hydroxymethyl benzoic acid as an effective water surrogate in the Passerini reaction: A straightforward access to α-hydroxyamides.

Author

Serafini, Marta, Griglio, Alessia, Oberto, Elena, Pirali, Tracey, and Tron, Gian Cesare

Subjects

*BENZOIC acid, *WATER chemistry, *AMIDE synthesis, *CHEMICAL reactions, *MULTIPHASE flow, *ISOCYANIDES

Abstract

Dozens of strategies have been described for the synthesis of α-hydroxyamides over the years, but they share common drawbacks in terms of generality and tolerability, especially to acid labile functionalities. Here we report a truncated Passerini reaction suitable for the easy and mild preparation of functionalized α-hydroxyamides. In particular, this procedure is tolerant to acid sensitive protecting groups, which remain intact during the multicomponent reaction. [ABSTRACT FROM AUTHOR]

Published

2017

6. STIM1 and ORAI1 mutations leading to tubular aggregate myopathies are sensitive to the Store-operated Ca2+-entry modulators CIC-37 and CIC-39.

Author

Riva, Beatrice, Pessolano, Emanuela, Quaglia, Edoardo, Cordero-Sanchez, Celia, Bhela, Irene P., Topf, Ana, Serafini, Marta, Cox, Daniel, Harris, Elizabeth, Garibaldi, Matteo, Barresi, Rita, Pirali, Tracey, and Genazzani, Armando A.

Abstract

• STIM1 and ORAI1 gain-of-function mutations trigger tubular aggregate myopathies. • These mutations lead to an increased basal Ca2+ and store-operated Ca2+-entry. • These mutations are sensitive to store-operated Ca2+-entry modulators. Gain-of-function mutations on STIM1 and ORAI1 genes are responsible for an increased store-operated calcium entry, and underlie the characteristic symptoms of three overlapping ultra-rare genetic disorders (i.e tubular aggregate myopathy, Stormorken syndrome, York platelet syndrome) that can be grouped as tubular aggregate myopathies. These mutations lead to a wide spectrum of defects, which usually include muscle weakness and cramps. Negative modulators of store-operated Ca2+-entry targeting wild-type STIM1 and ORAI1 have entered clinical trials for a different array of disorders, including pancreatitis, COVID-19, cancer, and autoimmune disorders and, while efficacy data is awaited, safety data indicates tolerability of this STIM1/ORAI1 mutations are amenable to pharmacological intervention. If this were so, given that there are no approved treatments or clinical trials ongoing for these rare disorders, it could be envisaged that these agents could also rehabilitate tubular aggregate myopathy patients. In the present contribution we characterized the Ca2+-entry patterns induced by eleven STIM1 and three ORAI1 mutations in heterologous systems or in patient-derived cells, i.e. fibroblasts and myotubes, and evaluated the effect of CIC-37 and CIC-39, two novel store-operated calcium entry modulators. Our data show that all STIM1 and ORAI1 gain-of-function mutations tested, with the possible exception of the R304Q STIM1 mutation, are amenable to inhibition, albeit with slightly different sensitivities, paving the way to the development of SOCE modulators in tubular aggregate myopathies. [Display omitted] [ABSTRACT FROM AUTHOR]

Published

2022

7. The impact of immunogenetics and clinical factors on the outcome of unrelated cord blood transplantation: The Milano Cord Blood Bank data

Author

Serafini, Marta, Poli, Francesca, Torelli, Rosanna, Fleischhauer, Katharina, Zino, Elisabetta, Arias, Alejandro Espadas de, Longhi, Elena, Frison, Sara, Karpasitou, Katherina, Pezzali, Ilaria, Lecchi, Lucilla, and Scalamogna, Mario

Subjects

*IMMUNOGENETICS, *HEALTH outcome assessment, *CORD blood, *CELL transplantation, *HLA histocompatibility antigens, *GRAFT rejection, *BLOOD banks

Abstract

Abstract: In this article we examined the role of HLA incompatibility, of KIR C1 and C2 ligands and of other clinical factors on 99 cord blood transplants performed using single units from Milano Cord Blood Bank (MICB). We analyzed the occurrence of rejection, overall patient survival (OS) and occurrence of acute GvHD ⩾2 grade (severe aGvHD). No correlation was found between the end points and the number of HLA-A,-B, -DRB1 and -DQB1 mismatches. Only HLA-C disparities are associated with the occurrence of rejection (P =0.03). Our results showed that the presence of the C1 ligand in the donor decreased the occurrence of aGvHD (grade ⩾2) in the recipient while recipients of donors expressing the C2 KIR ligand experienced more frequently aGvHD (P =0.03). The HLA-C1 ligand, therefore, proved to have a protective effect towards severe aGvHD. The probability of rejection increased in KIR epitope-mismatched recipient/donor pairs (P =0.01). Finally the stage of disease at transplantation and cell dose were important for patient survival (P =0.003, P =0.048 respectively). [Copyright &y& Elsevier]

Published

2010

8. A multicomponent approach in the discovery of indoleamine 2,3-dioxygenase 1 inhibitors: Synthesis, biological investigation and docking studies.

Author

Griglio, Alessia, Torre, Enza, Serafini, Marta, Bianchi, Alice, Schmid, Roberta, Coda Zabetta, Giulia, Massarotti, Alberto, Sorba, Giovanni, Pirali, Tracey, and Fallarini, Silvia

Subjects

*INDOLEAMINE 2,3-dioxygenase, *MOLECULAR docking, *IMMUNOLOGICAL tolerance, *CANCER immunotherapy, *TARGETED drug delivery

Abstract

Indoleamine 2,3-dioxygenase plays a crucial role in immune tolerance and has emerged as an attractive target for cancer immunotherapy. In this study, the Passerini and Ugi multicomponent reactions have been employed to assemble a small library of imidazothiazoles that target IDO1. While the p -bromophenyl and the imidazothiazole moieties have been kept fixed, a full SAR study has been performed on the side-chain, leading to the discovery of nine compounds with sub-micromolar IC 50 values in the enzyme-based assay. Compound 7d , displaying a α-acyloxyamide substructure, is the most potent compound, with an IC 50 value of 0.20 µM, but a low activity in a cell-based assay. Compound 6o , containing a α-acylaminoamide moiety, shows an IC 50 value of 0.81 µM in the IDO1-based assay, a full biocompatibility at 10 µM, together with a modest inhibitory activity in A375 cells. Molecular docking studies show that both 7d and 6o display a unique binding mode in the IDO1 active site, with the side-chain protruding in an additional pocket C, where a crucial hydrogen bond is formed with Lys238. Overall, this work describes an isocyanide based-multicomponent approach as a straightforward and versatile tool to rapidly access IDO1 inhibitors, providing a new direction for their future design and development. [ABSTRACT FROM AUTHOR]

Published

2018

9. 406: Detailed investigation of obstetric factors influencing isolation efficiency of fetal mesenchymal stem cells (FMSCS) from amniotic fluid and cord blood samples.

Author

Russo, Francesca Maria, Vergani, Patrizia, Gatto, Francesca, Marzorati, Simona, Follesa, Ilaria, Ornaghi, Sara, and Serafini, Marta

Published

2009

10. 407: Characterization of fetal mesenchymal stem cells isolated from umbilical cord blood and amniotic fluid of the same donor.

Author

Russo, Francesca Maria, Vergani, Patrizia, Gatto, Francesca, Marzorati, Simona, Follesa, Ilaria, Ornaghi, Sara, and Serafini, Marta

Published

2009

11. Hematopoietic Stem Cell Transplantation for Mucopolysaccharidoses: Past, Present, and Future.

Author

Taylor, Madeleine, Khan, Shaukat, Stapleton, Molly, Wang, Jianmin, Chen, Jing, Wynn, Robert, Yabe, Hiromasa, Chinen, Yasutsugu, Boelens, Jaap Jan, Mason, Robert W., Kubaski, Francyne, Horovitz, Dafne D.G., Barth, Anneliese L., Serafini, Marta, Bernardo, Maria Ester, Kobayashi, Hironori, Orii, Kenji E., Suzuki, Yasuyuki, Orii, Tadao, and Tomatsu, Shunji

Subjects

*HEMATOPOIETIC stem cell transplantation, *ISCHEMIC preconditioning, *DRUG side effects, *CENTRAL nervous system, *THERAPEUTICS

Abstract

• Several factors, including donor type, particular mucopolysaccharidoses (MPS) disorder, disease stage, clinical severity, preconditioning regimen, and potential complications, affect the overall efficacy and outcome of hematopoietic stem cell transplantation (HSCT). • HSCT can eliminate the immune response against infused enzymes by enzyme replacement therapy. • The cost-effectiveness of generally a one-time treatment makes HSCT an attractive option for patients with MPS. • HSCT is currently the preferred treatment for those patients with MPS with central nervous system manifestations. • Advancements in medicine have made HSCT a safer, more effective, and widely used treatment option for patients with MPS. Allogenic hematopoietic stem cell transplantation (HSCT) has proven to be a viable treatment option for a selected group of patients with mucopolysaccharidoses (MPS), including those with MPS types I, II, IVA, VI, and VII. Early diagnosis and timely referral to an expert in MPS are critical, followed by a complete examination and evaluation by a multidisciplinary team, including a transplantation physician. Treatment recommendations for MPS are based on multiple biological, sociological, and financial factors, including type of MPS, clinical severity, prognosis, present clinical signs and symptoms (disease stage), age at onset, rate of progression, family factors and expectations, financial burden, feasibility, availability, risks and benefits of available therapies such as HSCT, enzyme replacement therapy (ERT), surgical interventions, and other supportive care. International collaboration and data review are critical to evaluating the therapeutic efficacy and adverse effects of HSCT for MPS. Collaborative efforts to assess HSCT for MPS have been ongoing since the first attempt at HSCT in a patient with MPS reported in 1981. The accumulation of data since then has made it possible to identify early outcomes (ie, transplantation outcomes) and long-term disease-specific outcomes resulting from HSCT. The recent identification of predictive factors and the development of innovative regimens have significantly improved the outcomes of both engraftment failure and transplantation-related mortality. Assessment of long-term outcomes has considered a variety of factors, including type of MPS, type of graft, age at transplantation, and stage of disease progression, among others. Studies on long-term outcomes are considered a key factor in the use of HSCT in patients with MPS. These studies have shown the effects and limitations of HSCT on improving disease manifestations and quality of life. In this review, we summarize the efficacy, side effects, risks, and cost of HSCT for each type of MPS. [ABSTRACT FROM AUTHOR]

Published

2019

12. Comparative analysis of multilineage properties of mesenchymal stromal cells derived from fetal sources shows an advantage of mesenchymal stromal cells isolated from cord blood in chondrogenic differentiation potential.

Author

PIEVANI, ALICE, SCAGLIOTTI, VALERIA, RUSSO, FRANCESCA MARIA, AZARIO, ISABELLA, RAMBALDI, BENEDETTA, SACCHETTI, BENEDETTO, MARZORATI, SIMONA, ERBA, EUGENIO, GIUDICI, GIOVANNI, RIMINUCCI, MARA, BIONDI, ANDREA, VERGANI, PATRIZIA, and SERAFINI, MARTA

Subjects

*MESENCHYMAL stem cells, *CORD blood, *AMNIOTIC liquid, *CELL differentiation, *IN situ hybridization

Abstract

The article discusses the chondrogenic differentiation of mesenchymal stromal cell (MSC) sources from cord blood (CB) and amniotic fluid (AF). It notes that there is a lack of standardized protocols for isolation and differentiation of CB and AF for their use in treatment of various diseases. The fetal origin of isolated MSC strains was indicated in fluoresence in situ hybridization. Differences in biological and differentiation properties of CB-MSCs and AF-MSCs were identified.

Published

2014

13. Description and molecular modeling of two novel HLA alleles: HLA-A*0343 and A*0345

Author

Frison, Sara, Crivello, Pietro, Longhi, Elena, Andreini, Emanuela, Tivelli, Mara, Serafini, Marta, Tagliaferri, Cinzia, Scalamogna, Mario, and Poli, Francesca

Subjects

*MOLECULAR models, *HLA histocompatibility antigens, *GLOBULINS, *NUCLEOTIDES, *GENETIC mutation, *BONE marrow transplantation, *AMINO acids, *SMALL intestine, *TRANSPLANTATION of organs, tissues, etc.

Abstract

Abstract: We report the identification of two novel human leucocyte antigen (HLA) in two Caucasian individuals. HLA-A*0343 differs from A*03010101 by four changes at nucleotides 411–414 (CCGG→TGAA) and by a point mutation at position 418 (G→C). These differences lead to two amino acid substitutions at codon 114, where arginine has changed into negatively charged glutamic acid, and at codon 116, where aspartic acid has changed into positively charged histidine. Molecular modeling showed that these changes have a profound influence on the overall charge of the F pocket of the groove, resulting in potentially important changes in the peptide repertoire. HLA-A*0345 was found in a hematological female patient candidate to bone marrow transplantation. This new variant differs from HLA-A*03010101 at position 845 (C→A) encoding an amino acid change of threonine to asparagine at codon 258 located in the α3 domain. Molecular modeling does not suggest a substantial role of this substitutions on the interaction with β2-microglobulin or CD8. [Copyright &y& Elsevier]

Published

2010

14. Solitary juvenile xanthogranuloma of the hypopharynx. Clinico-pathologic study in a child with β-Thalassemia Major and Cutaneous Mastocytosis.

Author

de Soccio, Giulia, Savastano, Vincenzo, Minasi, Simone, Bertin, Serena, Serafini, Marta, Vittori, Tommaso, Riminucci, Mara, and Corsi, Alessandro

Subjects

*MAST cell disease, *ERDHEIM-Chester disease, *NON-langerhans-cell histiocytosis, *BETA-Thalassemia

Abstract

Juvenile Xanthogranuloma (JXG), the most common pediatric non-Langerhans cell histiocytosis, may rarely occur in association with Neurofibromatosis (types 1 and 2), Juvenile Myelomonocytic Leukemia and Cutaneous Mastocytosis (CM) and, morphologically, mimics Erdheim-Chester Disease tissue lesions and ALK-positive histiocytosis. We describe a 4-year-old girl with Beta-Thalassemia Major who developed an hypopharyngeal BRAFV600E- and ALK-negative JXG and CM. JXG has been rarely reported in the aerodigestive tract and in association with CM. In this molecular era, knowledge of genetic heterogeneity of JXG and clinical scenarios in which it may develop is essential for the appropriate diagnosis and treatment of each individual patient. [ABSTRACT FROM AUTHOR]

Published

2020

15. Description of HLA-A*0127N, a novel nonexpressed allele identified by SBT

Author

Longhi, Elena, Frison, Sara, Andreini, Emanuela, Karpasitou, Katerina, Serafini, Marta, and Poli, Francesca

Subjects

*NUCLEOTIDE sequence, *GENETIC code, *NUCLEIC acid analysis, *NUCLEOTIDES

Abstract

Summary: We describe the isolation and characterization of a novel HLA-A null allele, officially named A*0127N. The A*0127N exon 2, 3, and 4 nucleotide sequence is identical to that of A*010101 except at position 553, where a G is substituted by a T, resulting in a coding change in exon 3 (GAG>TAG) from Glu to the stop codon AMB. The mutation described is responsible for the premature ending of the translation. [Copyright &y& Elsevier]

Published

2007