Your search keyword '"Massimo Maccagno"' showing total 48 results

1. 2‐Aryl‐3‐Vinyl Substituted Imidazo[1,2‐ a ]pyridines and Fluorescent Electrocyclization Derivatives therefrom

Author

Gianluca Giorgi, Giovanni Petrillo, Lara Bianchi, Massimo Maccagno, Alice Benzi, and Cinzia Tavani

Subjects

Chemistry, Aryl, General Chemistry, Fluorescence, imidazopyridines, chemistry.chemical_compound, electrocyclic reactions, fluorescence, Michael addition, polyheterocycles, Polymer chemistry, Michael reaction, electrocyclic reactions, fluorescence, imidazopyridines, Michael addition, polyheterocycles

Published

2020

2. A Nitrocarbazole as a New Microtubule-Targeting Agent in Breast Cancer Treatment

Author

Marco Ponassi, Jessica Ceramella, Lara Bianchi, Domenico Spinelli, Alexia Barbarossa, Giovanni Petrillo, Maria Stefania Sinicropi, Domenico Iacopetta, Alice Benzi, Cinzia Tavani, Camillo Rosano, and Massimo Maccagno

Subjects

Programmed cell death, Technology, Cell cycle checkpoint, QH301-705.5, QC1-999, Context (language use), breast cancer, Microtubule, medicine, General Materials Science, Biology (General), carbazoles, ellipticine, tubulin, breast cancer, apoptosis, docking simulations, Instrumentation, QD1-999, Fluid Flow and Transfer Processes, docking simulations, biology, Chemistry, Process Chemistry and Technology, Physics, General Engineering, apoptosis, Engineering (General). Civil engineering (General), In vitro, Computer Science Applications, Vinblastine, carbazoles, Tubulin, tubulin, Apoptosis, Cancer research, biology.protein, TA1-2040, ellipticine, medicine.drug

Abstract

Breast cancer is still considered a high-incidence disease, and numerous are the research efforts for the development of new useful and effective therapies. Among anticancer drugs, carbazole compounds are largely studied for their anticancer properties and their ability to interfere with specific targets, such as microtubule components. The latter are involved in vital cellular functions, and the perturbation of their dynamics leads to cell cycle arrest and subsequent apoptosis. In this context, we report the anticancer activity of a series of carbazole analogues 1–8. Among them, 2-nitrocarbazole 1 exhibited the best cytotoxic profile, showing good anticancer activity against two breast cancer cell lines, namely MCF-7 and MDA-MB-231, with IC50 values of 7 ± 1.0 and 11.6 ± 0.8 μM, respectively. Furthermore, compound 1 did not interfere with the growth of the normal cell line MCF-10A, contrarily to Ellipticine, a well-known carbazole derivative used as a reference molecule. Finally, in vitro immunofluorescence analysis and in silico studies allowed us to demonstrate the ability of compound 1 to interfere with tubulin organization, similarly to vinblastine: a feature that results in triggering MCF-7 cell death by apoptosis, as demonstrated using a TUNEL assay.

Published

2021

3. An Easy Access to Furan-Fused Polyheterocyclic Systems

Author

Alice Benzi, Lara Bianchi, Gianluca Giorgi, Massimo Maccagno, Giovanni Petrillo, Domenico Spinelli, and Cinzia Tavani

Subjects

nitrostilbenes, naphthofurans, cyclization, electrocyclization, Chemistry (miscellaneous), Alcohols, Organic Chemistry, Drug Discovery, Molecular Medicine, Pharmaceutical Science, Thiophenes, Amines, Physical and Theoretical Chemistry, Furans, Carbon, Analytical Chemistry

Abstract

Nitrostilbenes characterized by two different or differently substituted aryl moieties can be obtained from the initial ring-opening of 3-nitrobenzo[b]thiophene with amines. Such versatile building blocks couple the well-recognized double electrophilic reactivity of the nitrovinyl moiety (addition to the double bond, followed by, e.g., intramolecular replacement of the nitro group) with the possibility to exploit a conjugated system of double bonds within an electrocyclization process. Herein, nitrostilbenes are reacted with different aromatic enols provided by a double (carbon and oxygen) nucleophilicity, leading to novel, interesting naphthodihydrofurans. From these, as a viable application, aromatization and electrocyclization lead in turn to valuable polycondensed, fully aromatic O-heterocycles.

Published

2022

4. 3-Aryl-4-nitrobenzothiochromans S,S-dioxide: From Calcium-Channel Modulators Properties to Multidrug-Resistance Reverting Activity

Author

Massimo Maccagno, Domenico Spinelli, Maurizio Viale, Cinzia Tavani, Maria Frosini, Alberto Chiarini, Matteo Micucci, Rosaria Gangemi, Roberta Budriesi, Lara Bianchi, Micucci, Matteo, Viale, Maurizio, Chiarini, Alberto, Spinelli, Domenico, Frosini, Maria, Tavani, Cinzia, Maccagno, Massimo, Bianchi, Lara, Gangemi, Rosaria, and Budriesi, Roberta

Subjects

cardiovascular activity, Drug Resistance, Pharmaceutical Science, Drug resistance, Pharmacology, 01 natural sciences, Analytical Chemistry, l-Type Calcium Channels (LTCC), chemistry.chemical_compound, Biological profile, Drug Discovery, Thiamine, 0303 health sciences, Tumor, Drug Synergism, Drug Resistance, Multiple, Subfamily B, Chemistry (miscellaneous), in vitro experiment, in vitro experiments, Muscle, Molecular Medicine, Smooth, Multiple, ATP Binding Cassette Transporter, Subfamily B, Research groups, ATP Binding Cassette Transporter, Guinea Pigs, 3-aryl-4-nitrothiochromans S,S-dioxide, anticancer therapy, multidrug resistance (MDR1), Animals, Antineoplastic Agents, Calcium Channels, Cell Line, Tumor, Cell Proliferation, Chromans, Doxorubicin, Drug Resistance, Neoplasm, Heart Atria, Humans, Inhibitory Concentration 50, Muscle, Smooth, Pyrans, Sulfhydryl Compounds, 3-aryl-4-nitrothiochromans s,s-dioxide, Tumor cells, 3-aryl-4-nitrothiochromans S, Article, Cell Line, lcsh:QD241-441, 03 medical and health sciences, lcsh:Organic chemistry, 3-aryl-4-nitrothiochromans S,S-dioxide, l-Type Calcium Channels (LTCC), anticancer therapy, multidrug resistance (MDR1), in vitro experiments, Anticancer therapy, Cardiovascular activity, In vitro experiments, L-Type Calcium Channels (LTCC), Multidrug resistance (MDR1), Physical and Theoretical Chemistry, l<%2Fspan>-type+calcium+channels+%28ltcc%29%22">l-type calcium channels (ltcc), 030304 developmental biology, 010405 organic chemistry, Aryl, Calcium channel, Organic Chemistry, 0104 chemical sciences, Multiple drug resistance, S-dioxide, chemistry, Neoplasm, Ex vivo

Abstract

Our research groups have been involved for many years in studies aimed at identifying new active organic compounds endowed with pharmacological properties. In this work, we focused our attention on the evaluation of cardiovascular and molecular drug resistance (MDR) reverting activities of some nitrosubstituted sulphur-containing heterocycles. Firstly, we have examined the effects of 4-nitro-3-(4-methylphenyl)-3,6-dihydro-2H-thiopyran S,S-dioxide 5, and have observed no activity. Then we have extended our investigation to the 3-aryl-4-nitrobenzothiochromans S,S-dioxide 6 and 7, and have observed an interesting biological profile. Cardiovascular activities were assessed for all compounds using ex vivo studies, while the MDR reverting effect was evaluated only for selected compounds using tumor cell lines. All compounds were shown to affect cardiovascular parameters. Compound 7i exerted the most effect on negative inotropic activity, while 6d and 6f could be interesting molecules for the development of more active ABCB1 inhibitors. Both 6 and 7 represent structures of large possible biological interest, providing a scaffold for the identification of new ABCB1 inhibitors.

Published

2020

5. Synthesis of fluorescent, triangular gold nanoplates through surface capping by a cationic diacetylene

Author

Maria Isabel Martinez-Espinoza, Sergio Thea, Massimo Ottonelli, Giovanna Dellepiane, Massimo Maccagno, and Marina Alloisio

Subjects

Materials science, Nanoparticle, 02 engineering and technology, Triangularly shaped gold nanoparticles, Cationic diacetylenes, Ligand-exchange reaction, Spectroscopic characterization, Scanning electron microscopy, 010402 general chemistry, Photochemistry, 01 natural sciences, Cationic diacetylenes, chemistry.chemical_compound, symbols.namesake, Ligand-exchange reaction, General Materials Science, Diacetylene, Cationic polymerization, 021001 nanoscience & nanotechnology, Condensed Matter Physics, Fluorescence, 0104 chemical sciences, Monomer, chemistry, Colloidal gold, symbols, Spectroscopic characterization, Triangularly shaped gold nanoparticles, 0210 nano-technology, Raman spectroscopy, Biosensor, Scanning electron microscopy

Abstract

In this work triangular gold nanoplates (AuNTPs) are prepared by spontaneous conversion of spherical-like gold precursors induced by the shape-directing properties of the diacetylene N,N,N-trimethylpentacosa-10,12-diyn-1-ammonium bromide (PCD_ABr), employed as capping agent. In detail, thin AuNTPs with edge length below 200 nm are obtained by incubating premade isotropic gold nanoparticles protected with chitosan (Chit@AuNPs) in PCD_ABr solutions through a standard ligand-exchange reaction (LER) carried out in water at room temperature. Control of the AuNTPs size as well as the reaction shape-yield up to 65% is achieved by simply varying the reagents ratio in the incubation mixture. Because of the high anisotropy of the flat nanoparticles, the AuNTPs-containing hydrosols show intense, well-defined absorptions in the NIR spectral region, which make them excellent candidates as biosensors also for in vivo assays with biological tissues and fluids. When subjected to UV light, both triangular and nearly spherical PCD_ABr-coated gold nanoparticles exhibit fluorescent properties and Raman features typical of disordered, sp2-based carbon nanostructures. The photogeneration of graphite-like moieties within the diacetylene shell instead of expected polydiacetylene skeleton is most likely due to poor alignment of the monomer chains on the gold surfaces and seems to be favored on isotropic nanoparticles.

Published

2020

6. Densely Functionalized 2-Methylideneazetidines from Nitrodienic Building Blocks

Author

Cinzia Tavani, Lara Bianchi, Gianluca Giorgi, Massimo Maccagno, and Giovanni Petrillo

Subjects

010405 organic chemistry, Chemistry, Organic Chemistry, Polymer chemistry, Michael reaction, Physical and Theoretical Chemistry, 010402 general chemistry, Ring (chemistry), Photochemistry, 01 natural sciences, Cycloaddition, Cis–trans isomerism, 0104 chemical sciences

Abstract

Novel, densely functionalized 2-methylideneazetidines can be obtained in high yields and mild conditions from the reaction of nitropentadienoates with primary amines, most likely through an aza-Michael addition followed by a 4-exo-trig cyclization. The initial, selective trans arrangement for the C3 and C4 ring hydrogens undergoes stereomutation due to the presence of an easily enolisable site at C3, eventually leading to mixtures where the cis isomer generally prevails.

Published

2018

7. Sequential Annulations to Interesting Novel Pyrrolo[3,2-c]carbazoles

Author

Cinzia Tavani, Angela Pagano, Lara Bianchi, Alice Benzi, Massimo Maccagno, and Giovanni Petrillo

Subjects

Indoles, Carbazoles, Pharmaceutical Science, Ring (chemistry), Article, Analytical Chemistry, lcsh:QD241-441, chemistry.chemical_compound, nitrobutadienes, lcsh:Organic chemistry, Drug Discovery, Pyrroles, Physical and Theoretical Chemistry, benzannulation, Pyrrole, Indole test, Molecular Structure, Chemistry, Organic Chemistry, Substitution (logic), Combinatorial chemistry, nitroindoles, nitroindoles, nitrobutadienes, benzannulation, Michael addition, Cadogan reaction, Chemistry (miscellaneous), Michael reaction, Molecular Medicine, michael addition, cadogan reaction

Abstract

Herein we report a significant, valuable extension of a recently implemented pyrrole benzannulation methodology that, employing versatile nitrodienes from our lab as useful C4 building blocks, led to indole derivatives characterized by unusual patterns of substitution. The 6-nitro-7-arylindoles resulting from suitably derivatized, non-symmetric dienes are of foreseeable synthetic interest in search for new polyheterocyclic systems. As an example, pyrrolocarbazoles with a rarely reported ring fusion were synthesized with the classical Cadogan protocol. Furthermore, the proven easy reducibility of the nitro group to amine will surely open the way to further interesting elaborations.

Published

2019

8. Nitrobutadienes as powerful benzannulating agents: An unprecedented easy access to rare nitroindoles

Author

Gianluca Giorgi, Angela Pagano, Lara Bianchi, Giovanni Petrillo, Michele Mancinelli, Massimo Maccagno, Cinzia Tavani, Pagano A., Mancinelli M., Bianchi L., Giorgi G., Maccagno M., Petrillo G., and Tavani C.

Subjects

Nitroindoles, 010402 general chemistry, Ring (chemistry), 01 natural sciences, Biochemistry, chemistry.chemical_compound, Atom economy, Michael addition, Drug Discovery, Moiety, Pyrrole, Indole test, 2,3-Dinitrobutadienes, Benzannulation, Nitroindoles - dinitroindoles, Stereoselectivity, 010405 organic chemistry, Chemistry, Organic Chemistry, 2,3-Dinitrobutadiene, Nitroindoles, dinitroindoles,2,3-Dinitrobutadienes,Benzannulation,Michael addition,Stereoselectivity, Combinatorial chemistry, 0104 chemical sciences, dinitroindoles, Michael reaction, Nitro, 3-Dinitrobutadienes, Selectivity, Nitroindoles - dinitroindole

Abstract

We report herein an original protocol to the indole nucleus, which could contribute to significantly expand the synthetic access to a heterocyclic moiety of undeniable paramount importance. The protocol consists in the construction of the benzene ring onto a pyrrole (benzannulation) starting from 2,3-dinitro-1,3-butadienes. This appealing, metal-free process characterized by high atom economy and mild reaction conditions allows to synthesize indoles possessing nitro group(s) on the benzene ring: a result which cannot be likewise easily obtained by exploiting most common pathways such as functionalization of a preformed indole or heteroannulation of a suitable benzene derivative. From a mechanistic point of view, a stepwise, ionic process is suggested by the identification of a pivot dihydroindole intermediate whose interception facilitates some selectivity in the preparation of different nitroindoles.

Published

2019

9. Self-assembly and photopolymerization of a novel quaternary-ammonium functionalized diacetylene on noble metal nanoparticles: A comparative study

Author

Maria Isabel Martinez-Espinoza, Marina Alloisio, Sergio Thea, and Massimo Maccagno

Subjects

Materials science, Scanning electron microscopy (SEM), General Physics and Astronomy, Nanoparticle, 02 engineering and technology, Core-shell assembly, engineering.material, 010402 general chemistry, 01 natural sciences, Silver nanoparticle, chemistry.chemical_compound, Organic chemistry, Noble metal nanoparticles, Noble metal nanoparticles, Polydiacetylenes, Core-shell assembly, Spectroscopic characterization, Scanning electron microscopy (SEM), Thermogravimetric analysis (TGA), Diacetylene, Thermogravimetric analysis (TGA), Cationic polymerization, Surfaces and Interfaces, General Chemistry, 021001 nanoscience & nanotechnology, Condensed Matter Physics, 0104 chemical sciences, Surfaces, Coatings and Films, Monomer, Photopolymer, chemistry, Chemical engineering, Polymerization, engineering, Noble metal, Spectroscopic characterization, Polydiacetylenes, 0210 nano-technology

Abstract

Stable hydrosols of gold and silver nanoparticles coated with the quaternary-ammonium group endowed diacetylene DAAMM (N,N,N-trimethyl-3-(pentacosa-10,12-diynamido)propan-1-ammonium) were obtained through a ligand-exchange reaction leaving the morphology of the pristine cores unmodified. Photopolymerization of the chemisorbed diacetylene shell occurred in both red and blue phases thanks to the presence of internal, H-bondable amide functions in the monomer chain, which are supposed to help the formation of a packed bilayer on the metal surfaces. Multidisciplinary characterization of the polymerized samples, including spectroscopic, morphological and thermal techniques, highlighted that differences occur in the polymerization process on gold and silver nanoparticles under different experimental conditions, suggesting a higher affinity of the trimethylammonium headgroup for gold substrates in acidic media. With respect to the extensively investigated PCDA (pentacosa-10,12-diynoic acid), DAAMM showed reduced capability of photogenerating thick polymer shells, especially in the more delocalized blue form, probably because of the inefficiency of the cationic monomer to form the multi-bilayered architecture typical of the highly-performing, carboxyl-terminated diacetylene. On the other end, the inner cross-linked structure gives to poly(DAAMM)-coated nanohybrids increased stability in water with respect to self-assembled counterparts deriving from saturated cationic surfactants, making them a promising sensing platform for rapid and cost effective assays of real samples.

Published

2018

10. Synthesis of poly-functionalized pyrazoles and pyridazines from nitrobutadienes: an interesting dichotomy of practical relevance

Author

Alessandro Carloni-Garaventa, Cinzia Tavani, Marcella Pani, Lara Bianchi, Massimo Maccagno, Carlo Scapolla, and Giovanni Petrillo

Subjects

chemistry.chemical_classification, Nitrobutadienes, Nitrogen heterocycles, Organic Chemistry, Nitrogen heterocycles, Michael additions, Nitrobutadienes, Pyrazoles, Pyridazines, Hydrazone, Biochemistry, Combinatorial chemistry, Acceptor, Pyridazines, Michael additions, Nucleophile, chemistry, Drug Discovery, Michael reaction, Pyrazoles, Moiety, Organic chemistry, Selectivity

Abstract

The initial ring-opening of 3-nitrothiophene and further structural modifications lead to nitrobutadienic building-blocks whose synthetic usefulness in the field of heterocycles has been widely demonstrated. As a further example, the Michael addition of a hydrazone anion to the nitrovinyl moiety of nitrobutadienes generates 1,2-diazaheterocycles as the final result of an overall MIRC process. Depending on the nature of the substituents on the Michael-type acceptor and on the hydrazono nucleophile, an interesting dichotomy is observed that leads to either five-member or six-member N-heterocycles with complete selectivity. The results obtained appear to be both of mechanistic and synthetic interest e.g., in the field of heterocycles endowed with potential pharmacological/biological activity.

Published

2015

11. Ring-Opening/Ring-Closing Protocols from Nitrothiophenes: Easy Access toN-Fused Pyrroles through a Tandem 1,6-H Shift/6π-Electrocyclization

Author

Massimo Maccagno, Lara Bianchi, Cinzia Tavani, Giovanni Petrillo, Carlo Scapolla, and Alessandra Tirocco

Subjects

chemistry.chemical_compound, Tandem, Chemistry, Organic Chemistry, Thiophene, Aromatization, Organic chemistry, Physical and Theoretical Chemistry, Closing (morphology), Ring (chemistry), Combinatorial chemistry

Abstract

The ring opening of 3-nitro-4-(phenylsulfonyl)thiophene with amines and proper modification of the resulting 1,3-diene enables a simple and versatile approach to N-fused pyrroles of both synthetic and biological interest through 1,6-H shift followed by 6π 1,5-electrocyclization. This protocol is effectively driven to the isolated pyrroles by an easy aromatization.

Published

2013

12. Uncommon 1,2-Migration of a Nitro Group Within a β-Nitrostyryl Moiety: Synthetic Scope and Mechanistic Details

Author

Gianluca Giorgi, Giovanni Petrillo, Marco Stenta, Cinzia Tavani, Franco Ghelfi, Domenico Spinelli, Lara Bianchi, and Massimo Maccagno

Subjects

chemistry.chemical_compound, chemistry, Group (periodic table), Stereochemistry, Diazomethane, Organic Chemistry, Nitro, Moiety, Physical and Theoretical Chemistry, Isomerization

Abstract

The unusual migration of a nitro group from the - to the -position of a -aryl--nitroethenyl moiety, following a nitrocyclopropane to isoxazoline N-oxide isomerization, has been studied from a mechanistic and synthetic points of view. As a result, two series of isomeric isoxazoline N-oxides could be obtained under controlled conditions. When reacted with diazomethane, a model transposed isoxazoline cleanly furnished a new, interesting pyrazolylisoxazole.

Published

2013

13. On the behavior of bis(sulfonyl)nitrobutadienes towards primary amines: a convenient access to 1-alkyl-2-aryl-4-(phenylsulfonyl)pyrroles

Author

Cinzia Tavani, Massimo Maccagno, Lara Bianchi, Gianluca Giorgi, Giovanni Petrillo, and Carlo Scapolla

Subjects

Nitrobutadienes, Double bond, Michael additions, Nitrobutadienes, Nitrogen heterocycles, Pyrroles, Vinylic nucleophilic substitutions, Biochemistry, Drug Discovery, Pharmaceutical Science, Organic Chemistry, Pharmaceutical Science, Conjugated system, 010402 general chemistry, 01 natural sciences, Biochemistry, chemistry.chemical_compound, Vinylic nucleophilic substitutions, Drug Discovery, Organic chemistry, Pyrroles, Nitrite, Alkyl, Sulfonyl, chemistry.chemical_classification, 010405 organic chemistry, Aryl, Nitrogen heterocycles, Drug Discovery3003 Pharmaceutical Science, Michael additions, Organic Chemistry, Aromatization, 0104 chemical sciences, chemistry, Yield (chemistry)

Abstract

The conjugated bis(sulfonyl)nitrobutadienes 1 undergo, with primary amines, competitive MeSO2 replacement [vinylic substitution at C(1)] versus aza-Michael addition to the nitroethenyl C(3)–C(4) double bond. The latter pathway eventually leads to the trisubstituted pyrroles 2 and conditions have been optimized in order to maximize the yield of such polyfunctionalized heterocycles. Interestingly, in trifluoroethanol tetrasubstituted pyrroles 7 are also formed, thanks to a final aromatization via oxidation by ‘endogenous’ nitrite.

Published

2016

14. Access to 2,3-diaryl-4-nitrothiochroman S,S-dioxides from 3-nitrobenzo[b]thiophene

Author

Domenico Spinelli, Giovanni Petrillo, Fernando Sancassan, Lara Bianchi, Egon Rizzato, Cinzia Tavani, and Massimo Maccagno

Subjects

Ring-opening/ring-closing reactions, Chemistry, Stereochemistry, Ring enlargement, Organic Chemistry, Biological activity, 3-Nitrobenzo[b]thiophene, Thiochromans, 3-Nitrobenzo[b]thiophene, Ring-opening/ring-closing reactions, Ring enlargement, Conformations, Biochemistry, Conformations, chemistry.chemical_compound, Drug Discovery, Proton NMR, Thiophene, Thiochromans, Pharmacophore

Abstract

The base-induced cyclization of ( E )-2-aryl-1-[2-(benzylsulfonyl)phenyl]-1-nitroethenes to polysubstituted thiochroman S , S -dioxides exhibits a diastereoselectivity that can be oriented towards a selected isomer by means of appropriate adjustments of the experimental conditions. The interest of such a result also rests on the promising pharmacological activity of the products, whose structure encompasses different well-acknowledged pharmacophores. A conformational 1 H NMR investigation, backed by molecular-mechanics calculations, has also been accomplished.

Published

2011

15. On resonance interactions in methyl 4-X-benzoates and the effect of 2,6-dimethyl substitution. 13C or 17O NMR chemical shifts as effective indicators of π-electron-density distribution?

Author

Massimo Maccagno, Andrea Mele, Oronzo Sciacovelli, Domenico Spinelli, Fernando Sancassan, Giovanni Petrillo, and Roberta Musio

Subjects

Electron density distribution, Computational chemistry, Chemistry, Chemical shift, Organic Chemistry, Substitution (logic), Resonance, Physical chemistry, Benzoates

Published

2009

16. A new route to thiopyran S,S-dioxide derivatives via an overall ring-enlargement protocol from 3-nitrothiophene

Author

Elda Severi, Domenico Spinelli, Massimo Maccagno, Cinzia Tavani, Andrea Galatini, Lara Bianchi, Egon Rizzato, Marco Stenta, Fernando Sancassan, and Giovanni Petrillo

Subjects

chemistry.chemical_classification, Thiopyran, Ring-opening/ring-closing reactions, Stereochemistry, Ring-enlargement protocol, Organic Chemistry, Nitro compound, chemistry.chemical_element, Ring expansion, Ion calcium, Ring (chemistry), Biochemistry, Combinatorial chemistry, Sulfur, Chemical synthesis, Sulfone, 3-Nitrothiophene, chemistry.chemical_compound, chemistry, Thiopyran S, S-dioxides, Drug Discovery, Moiety, 3-Nitrothiophene, Ring-opening/ring-closing reactions, Ring-enlargement protocol, Sulfur heterocycles, Ring expansion, Thiopyran S,S-dioxides, Sulfur heterocycles

Abstract

(1 E ,3 Z )-1-Aryl-4-methanesulfonyl-2-nitro-1,3-butadienes ( 8 ), derived from the initial ring-opening of 3-nitrothiophene ( 5 ), have been found to undergo a facile base-induced cyclization leading to thiopyran S , S -dioxides ( 9 ), thus furnishing a further example of effective ring-enlargement from 5- to 6-membered sulfur heterocycles. Compounds 9 are obtained as single racemic mixtures in satisfactory yields; they still contain a nitrovinylic moiety, which can be exploited for further modifications targeted to new derivatives endowed with either synthetic or pharmacological potentialities e.g., in the field of L-type Ca 2+ -channel blockers.

Published

2009

17. Butadienic Building Blocks from 2-Nitrothiophene as Precursors of Nitrogen Heterocycles: Intriguing Dichotomic Behavior

Author

Carlo Scapolla, Valeria Rocca, Gianluca Giorgi, Cinzia Tavani, Fernando Sancassan, Elda Severi, Massimo Maccagno, Giovanni Petrillo, and Lara Bianchi

Subjects

chemistry.chemical_classification, Stereochemistry, Diazomethane, Organic Chemistry, Nitro compound, chemistry.chemical_element, Chemical synthesis, Nitrogen, Pyrrolidine, Sulfone, chemistry.chemical_compound, chemistry, Yield (chemistry), Organic chemistry, Methylene

Abstract

With the goal of their exploitation for the synthesis of heterocycles, sulfides 10 and sulfones 11, derived from the initial ring-opening of 2-nitrothiophene (5) with pyrrolidine/AgNO3 in EtOH, were reacted with diazomethane. Interesting dichotomic behavior was found to yield pyrazolines 17 from 10 and isoxazolines 18 (as the main products) from 11. Intriguingly enough, in the latter case, an unexpected apparent C-C methylene insertion was also observed, leading to the homologous cyclopropanes 19 as secondary products.

Published

2007

18. An Unprecedented 'Reverse' 1,2-Migration of a Nitro Group within an α-Aryl-β-nitroethenyl Moiety Driven by Steric and Stereoelectronic Effects

Author

Cinzia Tavani, Giovanni Petrillo, Gianluca Giorgi, Domenico Spinelli, Egon Rizzato, Lara Bianchi, Massimo Maccagno, and Marco Stenta

Subjects

Steric effects, isoxazoline N-oxides, Stereochemistry, Aryl, Organic Chemistry, vinylcyclopropanes, General Medicine, DFT calculations, Biochemistry, chemistry.chemical_compound, chemistry, Nitro group migration, Group (periodic table), Nitro, Moiety, nitroalkenes, Nitro group migration, isoxazoline N-oxides, nitroalkenes, DFT calculations, vinylcyclopropanes

Abstract

Reference EPFL-ARTICLE-150326doi:10.2174/157017807781024165 URL: http://www.bentham.org/loc/contabs/loc4-4.htm#13 Record created on 2010-08-06, modified on 2017-05-12

Published

2007

19. ChemInform Abstract: A Straight Access to Functionalized Carbazoles by Tandem Reaction Between Indole and Nitrobutadienes

Author

Giovanni Petrillo, Carlo Scapolla, Cinzia Tavani, Marcella Pani, Massimo Maccagno, and Lara Bianchi

Subjects

Indole test, Cascade reaction, Chemistry, General Medicine, Combinatorial chemistry

Abstract

The reaction of nitrobutadienes (I) with indole leads to 1,3,4- and 1,2,4-nitrocarbazoles (III) and (IV).

Published

2015

20. A straight access to functionalized carbazoles by tandem reaction between indole and nitrobutadienes

Author

Marcella Pani, Massimo Maccagno, Giovanni Petrillo, Carlo Scapolla, Cinzia Tavani, and Lara Bianchi

Subjects

Indole test, Nitrobutadienes, Chemistry, Nitrogen heterocycles, Organic Chemistry, Aromatization, Carbazoles, Limiting, Ring (chemistry), Biochemistry, Catalysis, Nitrogen heterocycles, Michael additions, Perfluorinated solvents, Carbazoles, Nitrobutadienes, Michael additions, Cascade reaction, Drug Discovery, Organic chemistry, Perfluorinated solvents, Conjugate

Abstract

As a continuation of our research on the synthetic exploitation of the nitrobutadienic building-blocks obtained from the ring-opening of nitrothiophenes, we herein report about their reaction with the π-nucleophilic indole. Thanks to their double Michael-acceptor nature, 2,3-dinitro and 2-nitro-3-phenylsulfonyl substituted 1,3-butadienes produce poly-functionalized carbazoles through a double (inter-+intra-molecular) conjugate addition, followed by aromatization of the newly built ring. Significance is attached to the results obtained in fluorinated solvents such as trifluoroethanol, whereby a mild process, with no need for catalysis, overcomes some practical difficulties otherwise limiting the scope of the reaction. Besides the mechanistic aspects, the reaction encompasses motifs for a synthetic interest, mainly in the field of further-tunable arylcarbazoles endowed with predictable applicative properties, e.g., as fluorescent devices.

Published

2015

21. Novel quaternary ammonium-functionalized diacetylenes: their synthesis and photopolymerization

Author

Sergio Thea, Massimo Maccagno, Marina Alloisio, and Maria Isabel Martinez-Espinoza

Subjects

inorganic chemicals, chemistry.chemical_compound, symbols.namesake, Synthesis, Amide, Polymer chemistry, Materials Chemistry, chemistry.chemical_classification, Quaternary-ammonium surfactants, Diacetylene, Mechanical Engineering, technology, industry, and agriculture, Metals and Alloys, Polymer, Condensed Matter Physics, Electronic, Optical and Magnetic Materials, Photopolymer, chemistry, Polymerization, Mechanics of Materials, symbols, Spectroscopic characterization, Counterion, Raman spectroscopy, Cationic polydiacetylenes, Polydiacetylenes, Quaternary-ammonium surfactants, Cationic polydiacetylenes, Synthesis, Spectroscopic characterization

Abstract

In this paper, we report the synthesis of novel diacetylenes bearing trimethylammonium end groups, their photochemical polymerization and the spectroscopic characterization of the polymers by different techniques (UV–vis, fluorescence, FT-IR, Raman). The obtained results shed light on the role of the trimethylammonium head group (and its counterions) in the polymerization process. It is also demonstrated that the presence of an internal, H-bondable amide function in the diacetylene tail favors the photopolymerization process as well as the formation of the polydiacetylene in its blue, highly-conjugated form. Moreover, the corresponding polymer in the less-conjugated red phase, typical of polydiacetylenes in solution, shows significantly enhanced emission properties with respect to its counterparts carrying all-saturated lateral chains.

Published

2015

22. From β-Nitrothiophenes to Ring-Fused Nitrobenzenes: An Overall Ring-Enlargement Process via a Facile, Aromatization-Driven, Thermal 6π Electrocyclization1

Author

Carlo Dell'Erba, Elda Severi, G. Petrillo, L. Bianchi, C. Tavani, Massimo Maccagno, Fernando Sancassan, and Egon Rizzato

Subjects

chemistry.chemical_classification, Electrocyclic reaction, Concerted reaction, Aryl, Organic Chemistry, Aromatization, Nitro compound, Ring (chemistry), Photochemistry, Combinatorial chemistry, Nitrobenzene, chemistry.chemical_compound, chemistry, Nitro

Abstract

[reaction: see text] In prosecution of previous work on the thermal cyclization of 1-aryl-4-methanesulfonyl-2-nitro-3-phenylsulfonyl-1,3-butadienes (7), the 3-unsubstituted derivatives 8, deriving from the initial ring opening of 3-nitrothiophene (2), have been likewise found herein to undergo cyclization, followed by aromatization, in analogous mild experimental conditions, leading to the ring-fused homo- or heteroaromatic nitro derivatives 10. The concerted electrocyclic nature of the process is strongly supported by the outcome of tests based on the variation of the polarity of the solvent or of the electron density on the aryl of 8. Thus, the successful application of the process to the non-phenylsulfonyl-activated 8 significantly widens the scope of a synthetically valuable overall ring-opening/ring-closing procedure from nitrothiophenes. Support to the recently renewed interest in thermal 6pi electrocyclizations as a tool for the construction of the benzene ring is furthermore provided.

Published

2005

23. The Reaction of 3,4-Dinitrothiophene with Grignard Reagents: Formation of 2-(3-Amino-4-nitrothiophen-2-yl)phenols

Author

Lara Bianchi, Angelo Mugnoli, Elda Severi, Cinzia Tavani, Massimo Maccagno, Marino Novi, Carlo Dell'Erba, and Giovanni Petrillo

Subjects

Grignard reagents, Stereochemistry, Aryl, Organic Chemistry, Nitrothiophenes, General Medicine, Ring (chemistry), 3.4-Dinitrothiophene, Medicinal chemistry, Claisen-like rearrangements, chemistry.chemical_compound, chemistry, Nucleophile, Intramolecular force, Reagent, Nitro, Reactivity (chemistry), Phenols, Physical and Theoretical Chemistry, Nitrothiophenes, 3.4-Dinitrothiophene, Grignard reagents, Claisen-like rearrangements

Abstract

The treatment of 3,4-dinitrothiophene with an aryl Grignard reagent results in the reduction of one nitro group accompanied by the ipso-substitution of a hydrogen atom by an ortho-phenolic group on the ring carbon adjacent to the reduced nitro group. A Claisen-type intramolecular rearrangement is proposed as the pivotal step of a rather complex mechanism, followed by proton-transfer aromatizing steps. This work shows yet another facet of the variegated reactivity of 3,4-dinitrothiophene towards nucleophiles. (© Wiley-VCH Verlag GmbH & Co. KGaA, 69451 Weinheim, Germany, 2004)

Published

2004

24. Access to Ring-Fused Homo- and Heteroaromatic Derivatives via an Initial Ring-Opening of 3-Nitro-4-(phenylsulfonyl)thiophene1

Author

Massimo Maccagno, Carlo Dell'Erba, Cinzia Tavani, Angelo Mugnoli, Lara Bianchi, Marino Novi, Fernando Sancassan, and Giovanni Petrillo

Subjects

chemistry.chemical_classification, Stereochemistry, Organic Chemistry, Nitro compound, Benzothiophene, Ring (chemistry), Medicinal chemistry, Chemical synthesis, Pyrrolidine, Sulfone, chemistry.chemical_compound, chemistry, Thiophene, Nitro

Abstract

Within an overall ring-opening/ring-forming protocol, the (E,E)-4-methylthio-2-nitro-3-phenylsulfonyl-1-pyrrolidino-1,3-butadiene (7) [derived from the initial opening of 3-nitro-4-(phenylsulfonyl)thiophene (6) with pyrrolidine and silver nitrate in EtOH] is revealed to be an excellent precursor of nitro(phenylsulfonyl) derivatives of ring-fused aromatic (naphthalene, phenanthrene) or heteroaromatic (benzothiophene) compounds whose substitution pattern cannot be easily achieved by conventional methods. The key step is represented by a thermal electrocyclic rearrangement of (E,E)-1-aryl-4-methylsulfonyl-2-nitro-3-phenylsulfonyl-1,3-butadienes (9), which, thanks to proper geometric and electronic factors, occurs in unprecedentedly mild conditions and is followed by an irreversible, concerted syn β-elimination of methanesulfinic acid to aromatize the newly formed cyclohexadienic ring.

Published

2003

25. ChemInform Abstract: Ring-Opening/Ring-Closing Protocols from Nitrothiophenes: Easy Access to N-Fused Pyrroles Through a Tandem 1,6-H Shift/6π-Electrocyclization

Author

Carlo Scapolla, Giovanni Petrillo, Lara Bianchi, Massimo Maccagno, Cinzia Tavani, and Alessandra Tirocco

Subjects

chemistry.chemical_compound, Tandem, chemistry, Aromatization, Thiophene, General Medicine, Closing (morphology), Ring (chemistry), Combinatorial chemistry

Abstract

The ring opening of 3-nitro-4-(phenylsulfonyl)thiophene with amines and proper modification of the resulting 1,3-diene enables a simple and versatile approach to N-fused pyrroles of both synthetic and biological interest through 1,6-H shift followed by 6π 1,5-electrocyclization. This protocol is effectively driven to the isolated pyrroles by an easy aromatization.

Published

2014

26. Synthesis of a disulfide functionalized diacetylenic derivative of carbazole as building-block of polymerizable self-assembled monolayers

Author

Massimo Maccagno and Sushilkumar A. Jadhav

Subjects

Diacetylene, Carbazole, General Chemical Engineering, Metallic nanostructures, Disulfide bond, Self-assembled monolayer, General Chemistry, sodium hydrosulfide, Block (periodic table), Biochemistry, Fluorescence, Industrial and Manufacturing Engineering, chemistry.chemical_compound, chemistry, symmetrical disulfide, diacetylene, sodium hydrosulfide, Monolayer, Polymer chemistry, Materials Chemistry, Organic chemistry, diacetylene, symmetrical disulfide

Abstract

A new symmetrical disulfide containing a diacetylenic unit and bearing a fluorescent carbazolyl end-group forming polymerizable self-assembled monolayers on metallic nanostructures has been synthesized. Suitable modifications of the synthetic steps involved in the synthesis of such derivatives were made in order to assure better synthetic pathway. Conversion of the tosylated derivative into the final symmetrical disulfide is carried out using sodium hydrosulfide (NaSH).

Published

2014

27. Identification of thiol from 11-(9-Carbazolyl)-1-undecyldisulfide by NMR spectroscopy and single step coating of gold nanoparticles

Author

Massimo Maccagno and Sushilkumar A. Jadhav

Subjects

chemistry.chemical_classification, disulfide, Inorganic chemistry, long-chain thiol, Disulfide bond, thiol, General Chemistry, Nuclear magnetic resonance spectroscopy, thiol, long-chain thiol, disulfide, NMR spectroscopy, gold nanoparticles, engineering.material, NMR spectroscopy, chemistry, Coating, Colloidal gold, gold nanoparticles, Polymer chemistry, Monolayer, Thiol, Proton NMR, engineering, Spectroscopy

Abstract

Disulfide-functionalized fluorescent derivative of carbozole named 11-(9-carbazolyl)-1-undecyl disulfide (CBZDS) has been synthesized. Proton nuclear magnetic resonance spectroscopy was used to distinguish thiol from its corresponding symmetrical disulfide. Single step synthesis of gold nanoparticles coated with CBZDS was carried out which resulted in stable monolayers of CBZDS on gold nanoparticles.

Published

2014

28. ChemInform Abstract: Highly Substituted Pyrazoles and Pyridazines by MIRC Reactions of Hydrazone Anions and Nitrobutadienic Fragments

Author

Massimo Maccagno, Lara Bianchi, Alessandro Carloni-Garaventa, Carlo Scapolla, Cinzia Tavani, and Giovanni Petrillo

Subjects

chemistry.chemical_classification, Chemistry, Organic chemistry, Hydrazone, General Medicine

Abstract

Different approaches are investigated to the pharmaceutically interesting heterocyclic systems.

Published

2013

29. ChemInform Abstract: An Original Route to Newly-Functionalized Indoles and Carbazoles Starting from the Ring-Opening of Nitrothiophenes

Author

Cinzia Tavani, Gianluca Giorgi, Giovanni Petrillo, Carlo Scapolla, Massimo Maccagno, and Lara Bianchi

Subjects

Indole test, Addition reaction, Nucleophilic addition, Chemistry, Organic chemistry, General Medicine, Ring (chemistry), Medicinal chemistry, Adduct

Abstract

Nucleophilic addition of indole to nitroolefins gives the expected Michael-type adducts (III) and (VI) as well as the carbazoles (IX) and (X).

Published

2012

30. Highly-substituted pyrazoles and pyridazines by MIRC reactions of hydrazone anions and nitrobutadienic fragments

Author

Cinzia Tavani, Massimo Maccagno, Carlo Scapolla, Lara Bianchi, Alessandro Carloni-Garaventa, and Giovanni Petrillo

Subjects

chemistry.chemical_classification, Michael-type additions, Nitrobutadienes, Indoles, Diene, Nitrogen heterocycles, Organic Chemistry, Carbazoles, Hydrazone, Biological activity, Biochemistry, Combinatorial chemistry, Acceptor, chemistry.chemical_compound, chemistry, Drug Discovery, Reactivity (chemistry), Nitrobutadienes, Nitrogen heterocycles, Indoles, Carbazoles, Michael-type additions, Selectivity

Abstract

In prosecution of the synthetic exploitation of nitrobutadienes deriving from the initial ring-opening of nitrothiophenes, their multifaceted behavior finds a further clear-cut example in their Michael-type acceptor reactivity toward the anions of α-oxohydrazones. Thus, depending on the starting diene, new poly-functionalized pyrazoles are obtained. Furthermore, most interestingly, in one occasion a dichotomy has been observed, depending on the nature of the Michael-type donor, leading with complete selectivity to either 5-member or 6-member N-heterocycles. The outcome encompasses motifs for both mechanistic and synthetic interest, for example, in the field of heterocycles endowed with possible pharmacological/biological activity.

Published

2012

31. An Original Route to Newly-Functionalized Indoles and Carbazoles Starting from the Ring-Opening of Nitrothiophenes

Author

Carlo Scapolla, Gianluca Giorgi, Massimo Maccagno, Lara Bianchi, Giovanni Petrillo, and Cinzia Tavani

Subjects

Indole test, Michael-type additions, Nitrobutadienes, Indoles, Diene, Chemistry, Nitrogen heterocycles, Organic Chemistry, Carbazoles, Ring (chemistry), Biochemistry, Combinatorial chemistry, Acceptor, chemistry.chemical_compound, Drug Discovery, Moiety, Reactivity (chemistry), Nitrobutadienes, Nitrogen heterocycles, Indoles, Carbazoles, Michael-type additions

Abstract

The multifaceted behavior of nitrobutadienes deriving from the initial ring-opening of nitrothiophenes finds a further clear-cut example in their Michael-type acceptor reactivity towards indole. Thus, depending on the starting diene, either newly-functionalized indoles or carbazoles are produced, the latter as the result of an appealing double (intermolecular + intramolecular) Michael-type addition to a nitrovinylic moiety. The outcome encompasses motifs for both mechanistic and synthetic interest in the field of heterocycles endowed with possible pharmacological activity.

Published

2012

32. Sensitivity of different resistant tumour cell lines to the two novel compounds (2Z,4E)-2-methylsulfanyl-5-(1-naphthyl)-4-nitro-2,4-pentadienoate and (1E,3E)-1,4-bis(2-naphthyl)-2,3-dinitro-1,3-butadiene

Author

Domenico Spinelli, Cinzia Cordazzo, Massimo Maccagno, Sushilkumar A. Jadhav, Giuseppe Leto, Maria A. Mariggiò, Cinzia Aiello, Patrizio Castagnola, Maurizio Viale, Giovanni Petrillo, Egon Rizzato, Alessandro Poggi, and Lara Bianchi

Subjects

Mechanism of resistance, Nitro compound, Fluorescent Antibody Technique, Tetrazolium Salts, Antineoplastic Agents, Biology, Naphthalenes, Microtubules, Cell Line, Tumor, Drug-resistance, 1-Naph-NMCB, 2-Naph-DNB, Mechanism of resistance, medicine, Butadienes, Cytotoxic T cell, Humans, 2-Naph-DNB, Cell Proliferation, Drug-resistance, Pharmacology, Cisplatin, chemistry.chemical_classification, Cell growth, Cell Cycle, In vitro, Thiazoles, Biochemistry, Mechanism of action, chemistry, Cell culture, Drug Resistance, Neoplasm, Fatty Acids, Unsaturated, 1-Naph-NMCB, medicine.symptom, Immunostaining, medicine.drug

Abstract

The inhibition of cell proliferation by methyl (2Z,4E)-2-methylsulfanyl-5-(1-naphthyl)-4-nitro-2,4-pentadienoate (1-Naph-NMCB) and (1E,3E)-1,4-bis(2-naphthyl)-2,3-dinitro-1,3-butadiene (2-Naph-DNB) has been studied in vitro against four cell lines selected for their resistance to doxorubicin, cisplatin, taxol and 5-fluorouracil. In previous experiments both compounds showed good in vitro antiproliferative, cytotoxic and pro-apoptotic activities against cell lines of different histologic origin. The results of the experiments presented here suggest that 1-Naph-NMCB is able to overcome all of the different mechanisms of resistance showed by the resistant cell lines used for our experiments. On the contrary, when we used the taxol-resistant A549-T12 cell line, characterized by a mechanism of resistance due to a mutation of the target site of taxol on microtubules, it displayed a partial but significant cross-resistance to 2-Naph-DNB. Although the actual mechanism of this cross-resistance has not yet been definitively elucidated, our results from immunostaining of microtubules suggest that it may be linked to the presence of a shared target site for taxol and 2-Naph-DNB on microtubules.

Published

2008

33. Design, synthesis, and in vitro evaluation of new naphthylnitrobutadienes with potential antiproliferative activity: toward a structure/activity correlation

Author

Claudia Prevosto, Cinzia Tavani, Cinzia Aiello, Carla Fenoglio, Domenico Spinelli, Stefano Morganti, Michela Croce, Massimo Maccagno, Maria A. Mariggiò, Maurizio Viale, Egon Rizzato, Lara Bianchi, Cinzia Cordazzo, and Giovanni Petrillo

Subjects

Naphthylnitrobutadienes, Antiproliferative activit, Mechanism of action, Molecular-simplification strategy, Molecular-simplification strategy, Stereochemistry, Clinical Biochemistry, Nitro compound, Pharmaceutical Science, Antineoplastic Agents, Apoptosis, Mechanism of action, Naphthalenes, Biochemistry, Chemical synthesis, Inhibitory Concentration 50, Structure-Activity Relationship, Cell Line, Tumor, Drug Discovery, medicine, Butadienes, Moiety, Humans, Cytotoxicity, Molecular Biology, Interphase, Cell Proliferation, chemistry.chemical_classification, Chemistry, Cell growth, Organic Chemistry, Antiproliferative activit, DNA, In vitro, Cell culture, Drug Design, Molecular Medicine, medicine.symptom, Drug Screening Assays, Antitumor, Tumor Suppressor Protein p53, Naphthylnitrobutadienes

Abstract

On the grounds of previous encouraging results on the antitumor activity of (1 E ,3 E )-1,4-bis(1-naphthyl)-2,3-dinitro-1,3-butadiene ( 1 ), we have designed and synthesized two new molecules [(1 E ,3 E )-1,4-bis(4-carboxy-1-naphthyl)-2,3-dinitro-1,3-butadiene ( 2 ) and methyl (2 Z ,4 E )-2-methylsulfanyl-5-(1-naphthyl)-4-nitro-2,4-pentadienoate ( 3 )] characterized by a common naphthylnitrobutadiene array but with different structural properties, with the aim of approaching to some structure–activity correlation. When 2 and 3 were analyzed in vitro for their inhibition of cell proliferation and pro-apoptotic properties, the carboxyderivative 2 did not furnish appreciable results. In contrast, 3 (which contains only one of the two naphthylnitroethenyl moieties of the original compound 1 ) showed remarkable activities in the range of micromolar concentrations (in six over eight cell lines its IC 50 s are in the 1–3 μM range), with a significant improvement compared to 1 . In particular, 3 proved able to bind to DNA, to upregulate p53, to block cells in the G2/M phase of their cycle, and to induce apoptosis. Thus, very interestingly, the performance of 3 with respect to 1 shows that a single 1-(1-naphthyl)-2-nitroethene moiety is able to ensure better (on four out of eight of the cell lines tested) or comparable levels of activity. This result suggests that the ‘molecular-simplification strategy’ could furnish a useful instrument for future design in our antitumor research.

Published

2007

34. Naphthylnitrobutadienes as pharmacologically active molecules: evaluation of the in vivo antitumour activity

Author

Cinzia Aiello, Carla Fenoglio, Emanuela Ognio, Stefano Morganti, Maria A. Mariggiò, Maurizio Viale, Massimo Maccagno, Domenico Spinelli, Giovanni Petrillo, and Cinzia Cordazzo

Subjects

Colorectal cancer, Pharmacology toxicology, Mice, Nude, Antitumour activity, Antineoplastic Agents, Pharmacology, Naphthalenes, Mice, In vivo, Toxicity Tests, medicine, Butadienes, Nitrobutadiene derivatives, Molecule, Animals, Pharmacology (medical), In vivo pharmacological activity, Fibrosarcoma, Mice, Inbred BALB C, Chemistry, Melanoma, Lewis lung carcinoma, medicine.disease, Xenograft Model Antitumor Assays, In vitro, Mice, Inbred C57BL, Antitumour activity, Nitrobutadiene derivatives, In vivo pharmacological activity, Oncology, Fatty Acids, Unsaturated, Female

Abstract

On the basis of our previous interesting results in vitro on the antiproliferative activity of (1E,3E)-1,4-bis(1-naphthyl)-2,3-dinitro-1,3-butadiene (1-Naph-DNB) we have designed and synthesized the new molecule methyl (2Z,4E)-2-methylsulphanyl-5-(1-naphthyl)-4-nitro-2,4-pentadienoate (1-Naph-NMCB) characterized by the same naphthylnitrobutadiene array but with a different functional group at one end of the diene system. This new molecule showed an in vitro antiproliferative activity more significant than that found for the original 1-Naph-DNB. In order to verify in vivo our in vitro results we have tested the antitumour activity of 1-Naph-DNB and 1-Naph-NMCB in several murine tumour models, namely the myelomonocytic P388 and the Lewis lung carcinoma 3LL in BDF1 mice, the melanoma B16 in C57Bl mice, the fibrosarcoma WEHI 164 in nude mice and, finally, the C51 colon cancer in Balb/c mice. In the case of 1-Naph-NMCB the analysis of the antitumour activity has been preceded by toxicological experiments on CD-1 mice, in order to determine the lethal (LD) and the maximal tolerated (MTD) doses together with the spectrum of histological alterations caused by its iv administration. The results obtained show that the modification of the original structure of 1-Naph-DNB according to the molecular-simplification strategy has led to an asymmetric nitrobutadiene array, i.e. that of 1-Naph-NMCB, endowed with an antitumour activity which is in some cases even better than that showed by the parental compound itself, together with differences in tumour selectivity and negligible histological toxic effects. A promising, versatile route to new, more active and/or safe nitrobutadiene derivatives has thus been positively tested.

Published

2007

35. Synthesis, in vitro activity and in vivo toxicity of the new 2,3-dinitrobutadiene derivative (1E,3E)-1,4-bis(2-naphthyl)-2,3-dinitro-1,3-butadiene

Author

Egon Rizzato, Claudia Prevosto, Rita Vaccarone, Maurizio Viale, Maria A. Mariggiò, Giovanni Petrillo, Cinzia Cordazzo, Amalia Cassano, Domenico Spinelli, Cinzia Aiello, Carla Fenoglio, Lara Bianchi, Emanuela Ognio, and Massimo Maccagno

Subjects

Stereochemistry, Blotting, Western, Stereoisomerism, Antineoplastic Agents, Apoptosis, Antiproliferative activity, Biology, Naphthalenes, Kidney, chemistry.chemical_compound, Mice, In vivo, Cell Line, Tumor, Butadienes, Animals, Humans, Cell Proliferation, Pharmacology, Toxicity, Cell growth, Cell Cycle, DNA, Naphthylnitrobutadienes, Antiproliferative activity, Apoptosis, Cell cycle, In vitro, Up-Regulation, Cross-Linking Reagents, Biochemistry, chemistry, Liver, Cell culture, Female, Tumor Suppressor Protein p53, Naphthylnitrobutadienes, Lead compound, Spleen

Abstract

Our interesting results on the antiproliferative (in vitro) and antitumour (in vivo) activities of (1E,3E)-1,4-bis(1-naphthyl)-2,3-dinitro-1,3-butadiene (1-Naph-DNB) have more recently induced us to design and synthesize some new 1,4-diaryl-2,3-dinitro-1,3-butadienes characterized by a common arylnitrobutadiene array but with different geometric and/or functional properties. This task was undertaken with the aim to obtain new compounds with an enhanced antiproliferative activity and, possibly, a different specificity with respect to the original (lead) compound. (1E,3E)-1,4-Bis(2-naphthyl)-2,3-dinitro-1,3-butadiene (2-Naph-DNB) is one of the molecules so obtained, a structural isomer of 1-Naph-DNB provided with a different spatial arrangement. When analyzed in vitro for its inhibition of cell proliferation 2-Naph-DNB showed a remarkable activity in the range of micromolar concentrations, with significant differences, with respect to 1-Naph-DNB, against some cell lines. Furthermore, it was able to significantly trigger apoptosis, to up-regulate p53, to block cells in the G2/M phase of the cell cycle and, finally, to slightly bind to DNA forming interstrand cross-links (ISCL). 2-Naph-DNB was then analyzed for its toxic activity in vivo in CD1 mice. This allowed the determination of toxicity parameters such as the lethal doses (LD) and the maximal tolerated dose (MTD) together with the definition of the spectrum of tissue alterations due to its administration i.v. Altogether our data suggest that the idea of modifying the geometry of the lead compound 1-Naph-DNB deserves further investigation aimed at synthesizing new molecules with similar chemical functionalities but with different spatial requirements, hopefully characterized by still enhanced activities in terms of inhibition of cell proliferation and apoptosis.

Published

2007

36. Oxidative nucleophilic substitution of hydrogen versus ring-opening in the reaction of 4-R-2-nitrothiophenes with amines. The crucial effect of 4-alkyl groups

Author

Stefano Morganti, Domenico Spinelli, Fernando Sancassan, Cinzia Tavani, Massimo Maccagno, Lara Bianchi, Egon Rizzato, and Giovanni Petrillo

Subjects

chemistry.chemical_classification, Hydrogen, Stereochemistry, Organic Chemistry, Nitro compound, chemistry.chemical_element, Ring (chemistry), Chemical synthesis, Medicinal chemistry, Adduct, chemistry, Nucleophilic substitution, Aliphatic compound, Alkyl

Abstract

4-Alkyl-2-nitrothiophenes [10: R = CH3, CH(OH)CH3, CH(OCH3)CH3] react with secondary aliphatic amines, in the presence of AgNO3, to give 3-alkyl-2-amino-5-nitrothiophenes (12) through an oxidative nucleophilic substitution of hydrogen (ONSH) of synthetic interest. This behavior is in striking contrast with that of the parent 2-nitrothiophene (6), which was found to undergo ring-opening in analogous reaction conditions. A possible rationale for the crucial effect of alkyl groups is suggested, grounded also on a study of the corresponding Meisenheimer-like adducts.

Published

2007

37. Nitrobutadienes from β-Nitrothiophenes: Valuable Building Blocks in the Overall Ring Opening/Ring Closure Protocol to Homo- or Heterocycles

Author

Stefano Morganti, Lara Bianchi, Domenico Spinelli, Carlo Dell'Erba, Elda Severi, Cinzia Tavani, Massimo Maccagno, Egon Rizzato, Giovanni Petrillo, and Fernando Sancassan

Subjects

Stereochemistry, Chemistry, Closure (topology), General Medicine, Ring (chemistry), Combinatorial chemistry

Published

2006

38. Synthetic Exploitation of the Ring-Opening of Nitrothiophenes. Part 17. From β-Nitrothiophenes to Ring-Fused Nitrobenzenes: An Overall Ring-Enlargement Process via a Facile, Aromatization-Driven, Thermal 6π Electrocyclization

Author

Lara Bianchi, Fernando Sancassan, Egon Rizzato, Cinzia Tavani, Elda Severi, Massimo Maccagno, Carlo Dell'Erba, and Giovanni Petrillo

Subjects

Nitrobenzene, chemistry.chemical_compound, Chemistry, Scientific method, Thermal, Aromatization, General Medicine, Ring (chemistry), Photochemistry

Published

2006

39. From β-nitrothiophenes to ring-fused nitrobenzenes: an overall ring-enlargement process via a facile, aromatization-driven, thermal 6π electrocyclization

Author

Lara, Bianchi, Carlo, Dell'Erba, Massimo, Maccagno, Giovanni, Petrillo, Egon, Rizzato, Fernando, Sancassan, Elda, Severi, and Cinzia, Tavani

Abstract

[reaction: see text] In prosecution of previous work on the thermal cyclization of 1-aryl-4-methanesulfonyl-2-nitro-3-phenylsulfonyl-1,3-butadienes (7), the 3-unsubstituted derivatives 8, deriving from the initial ring opening of 3-nitrothiophene (2), have been likewise found herein to undergo cyclization, followed by aromatization, in analogous mild experimental conditions, leading to the ring-fused homo- or heteroaromatic nitro derivatives 10. The concerted electrocyclic nature of the process is strongly supported by the outcome of tests based on the variation of the polarity of the solvent or of the electron density on the aryl of 8. Thus, the successful application of the process to the non-phenylsulfonyl-activated 8 significantly widens the scope of a synthetically valuable overall ring-opening/ring-closing procedure from nitrothiophenes. Support to the recently renewed interest in thermal 6pi electrocyclizations as a tool for the construction of the benzene ring is furthermore provided.

Published

2005

40. 1,4-bis(1-naphthyl)-2,3-dinitro-1,3-butadiene a novel anticancer compound effective against tumor cell lines characterized by different mechanisms of resistance

Author

Marino Novi, Federica Barbieri, Maurizio Viale, Carlo Dell'Erba, Massimo Maccagno, Barbara Chiavarina, and Massimo Ottone

Subjects

Cancer Research, Paclitaxel, medicine.drug_class, Cell, Antineoplastic Agents, 4-bis(1-naphthyl)-2, Biology, Toxicology, Cell Line, Tumor, Butadienes, medicine, Humans, MTT assay, A549 cell, 3-butadiene, drug resistance, Cell growth, 3-dinitro-1, General Medicine, Cell cycle, Drug Resistance, Multiple, 1,4-bis(1-naphthyl)-2,3-dinitro-1,3-butadiene, drug resistance, mechanisms of resistance, Kinetics, medicine.anatomical_structure, Oncology, Mechanism of action, Biochemistry, Doxorubicin, Drug Resistance, Neoplasm, mechanisms of resistance, Cell culture, Fluorouracil, Cisplatin, medicine.symptom, Cell Division, Topoisomerase inhibitor

Abstract

The inhibition of cell proliferation by 1,4-bis (1-naphthyl)-2,3-dinitro-1,3-butadiene (Naph-DNB) was evaluated in vitro against 4 cell lines (L1210/DDP, A2780/DX3, HCT-8/FU7dR, A549-T12) selected for their resistance to cisplatin, doxorubicin, 5-fluorouracil and taxol, and their wild-type counterparts. Naph-DNB is a novel anti-cancer compound obtained years ago within a research project of Organic Chemistry aimed at synthesizing 2,3-dinitrobutadiene derivatives. Because of its chemical structure, Naph-DNB was suggested to interact with nucleic acids, in particular DNA, and the other cellular macromolecules. This hypothesis made us consider Naph-DNB as a candidate for studies concerning its antitumour activity. We used the MTT assay to test the inhibition of cell proliferation after incubation of the cell lines with Naph-DNB for 72 h. For comparison, resistant and wild-type cell lines were also tested against those anticancer drugs used in vitro for their selection. In these culture conditions Naph-DNB retained its inhibiting activity against all resistant cells with IC50 values similar to those obtained in corresponding wild-type cell lines. Moreover, Naph-DNB was twice as effective as 5-fluorouracil against wild-type HCT-8 cells. Our previous findings about the interaction of Naph-DNB with DNA through the formation of interstrand cross-links suggested a mechanism of action similar to that of platinum/alkylating agents or topoisomerase inhibitors (intercalating agents). Our present data obtained by the K-SDS precipitation assay in A2780 and A549 cells showed that Naph-DNB is not able to form a stable topoisomerase-DNA complex as is the case for topoisomerase inhibitors. In conclusion, our results indicate that Naph-DNB is able to overcome some of the classical mechanisms of resistance selected by some anticancer drugs mainly used in clinical setting.

Published

2004

41. α-Oxohydrazones as Imine Component in the Synthesis of 4-Functionalized Azetidinones by the Staudinger Reaction

Author

Fernando Sancassan, Carlo Dell'Erba, Cinzia Tavani, Angelo Mugnoli, Marino Novi, Lara Bianchi, Giovanni Petrillo, and Massimo Maccagno

Subjects

alpha-hydrazono-amides, alpha-hydrazono-ketones, Stereochemistry, Organic Chemistry, Imine, azetidinones, General Medicine, Magnesium monoperoxyphthalate, Ring (chemistry), Cleavage (embryo), Biochemistry, Medicinal chemistry, Cycloaddition, azetidinones, Staudinger reaction, alpha-hydrazono-ketones, alpha-hydrazono-amides, alpha-hydrazono-esters, chemistry.chemical_compound, chemistry, Drug Discovery, Surface modification, Stereoselectivity, Staudinger reaction, alpha-hydrazono-esters

Abstract

1-(Methyl-p-tolyl-amino)-3-phenoxy-2-azetidinones 4-COX and 4-R substituted (COX: X=Me, Et, Ph, NMe2, NEt2, OBut; R=Me, Et, Ph) were smoothly prepared from the corresponding α-(methyl-p-tolyl)hydrazonylated ketones, amides and esters via [2+2] cycloaddition with phenoxyketene. The reaction was generally high-yielding and diastereoselective, leading to β-lactams with a cis relationship between the PhO and the COX moieties, except for R=Ph, where an opposite stereoselectivity was instead observed. The azetidinones represent interesting intermediates which couple protection at N(1) and functionalization at position 4 of the ring. Deprotection of N(1) can be easily attained by oxidative N–N cleavage with magnesium monoperoxyphthalate.

Published

2004

42. Easy access to 4-nitrothiochroman S,S-dioxides via ring-enlargement from 3-nitrobenzo[b]thiophene

Author

Fernando Sancassan, Elda Severi, Cinzia Tavani, Lara Bianchi, Domenico Spinelli, Carlo Dell'Erba, Marino Novi, Massimo Maccagno, Egon Rizzato, Giovanni Petrillo, Stefano Morganti, L. BIANCHI, C. DELL'ERBA, M. MACCAGNO, S. MORGANTI, M. NOVI, G. PETRILLO, E. RIZZATO, F. SANCASSAN, E. SEVERI, SPINELLI D., and C. TAVANI

Subjects

Steric effects, Thiochromans, Nitrothiophenes, 3-Nitrobenzo[b]thiophene, Ring-opening/ring-closure reactions, Ring enlargement, Conformations, Trimethylsilyl, Stereochemistry, Ring enlargement, Organic Chemistry, Nitrothiophenes, 3-Nitrobenzo[b]thiophene, Ring (chemistry), Biochemistry, Medicinal chemistry, chemistry.chemical_compound, chemistry, Amide, Intramolecular force, Drug Discovery, Michael reaction, Thiophene, Moiety, Thiochromans, Ring-opening/ring-closure reactions

Abstract

The (E)-2-aryl-1-[2-(methylthio)phenyl]-1-nitroethylenes 5 can easily be oxidized to the relevant sulfones 6 and effectively subjected to cyclization via an intramolecular Michael addition after metallation with lithium bis(trimethylsilyl)amide in THF. After quenching with ammonium chloride the 3-aryl-4-nitrothiochroman S,S-dioxides 2 are obtained as diastereomeric mixtures in good to excellent yields. Both yields and stereochemistry of the ring-closure step appear to be influenced by steric effects of the 3-aryl moiety. As sulfides 5 derive from an initial ring opening of 3-nitrobenzo[b]thiophene ( 1 ), the overall 1 to 2 process can be considered as an effective 5 to 6 ring enlargement of the sulfur heterocycle. A conformational 1H NMR and molecular-mechanics investigation on the isolated diastereomeric 2 has also been accomplished.

Published

2004

43. Synthetic Exploitation of the Ring-Opening of Nitrothiophenes. Part 15. Access to Ring-Fused Homo- and Heteroaromatic Derivatives via an Initial Ring-Opening of 3-Nitro-4-(phenylsulfonyl)thiophene

Author

Massimo Maccagno, Angelo Mugnoli, Marino Novi, Fernando Sancassan, Lara Bianchi, Cinzia Tavani, Carlo Dell'Erba, and Giovanni Petrillo

Subjects

chemistry.chemical_compound, Chemistry, Stereochemistry, Nitro, Thiophene, General Medicine, Ring (chemistry), Medicinal chemistry

Published

2003

44. Access to ring-fused homo- and hetero-aromatic derivatives via an initial ring-opening of 3-nitro-4-(phenylsulphonyl)thiophene

Author

Lara, Bianchi, Carlo, Dell'Erba, Massimo, Maccagno, Angelo, Mugnoli, Marino, Novi, Giovanni, Petrillo, Fernando, Sancassan, and Cinzia, Tavani

Abstract

Within an overall ring-opening/ring-forming protocol, the (E,E)-4-methylthio-2-nitro-3-phenylsulfonyl-1-pyrrolidino-1,3-butadiene (7) [derived from the initial opening of 3-nitro-4-(phenylsulfonyl)thiophene (6) with pyrrolidine and silver nitrate in EtOH] is revealed to be an excellent precursor of nitro(phenylsulfonyl) derivatives of ring-fused aromatic (naphthalene, phenanthrene) or heteroaromatic (benzothiophene) compounds whose substitution pattern cannot be easily achieved by conventional methods. The key step is represented by a thermal electrocyclic rearrangement of (E,E)-1-aryl-4-methylsulfonyl-2-nitro-3-phenylsulfonyl-1,3-butadienes (9), which, thanks to proper geometric and electronic factors, occurs in unprecedentedly mild conditions and is followed by an irreversible, concerted syn beta-elimination of methanesulfinic acid to aromatize the newly formed cyclohexadienic ring.

Published

2003

45. Strategies for improving the water solubility of new antitumour nitronaphthylbutadiene derivatives

Author

Domenico Spinelli, Carla Gasbarri, Susanna Guernelli, Massimo Maccagno, Silvano Ferrini, Maurizio Viale, Giovanni Petrillo, Antonella Fontana, Cinzia Aiello, Egon Rizzato, A. Fontana, M. Viale, S. Guernelli, C. Gasparri, E. Rizzato, M. Maccagno, G. Petrillo, C. Aiello, S. Ferrini, and D. Spinelli

Subjects

Liposome, Aqueous solution, Molecular Structure, Chemistry, Organic Chemistry, Water, Antineoplastic Agents, Nitro Compounds, Biochemistry, In vitro, Solubility, Cell Line, Tumor, Butadienes, Humans, Cytotoxic T cell, Organic chemistry, Physical and Theoretical Chemistry, Cancer cell lines, Cell Proliferation

Abstract

Different nitronaphthylbutadienes have been previously proved to have antitumour activity. The main drawback of these derivatives is their low water solubility. With the aim of facilitating the administration of these new drugs we have synthesized the hexyl (2Z,4E)-2-methylsulfanyl-5-(1-naphthyl)-4-nitro-2,4-pentadienoate analogue (1-Naph-NHCB) which is demonstrated to be easily included into cyclodextrins and/or entrapped into liposomes. Its antitumour activity was revealed to be almost comparable with that of the previously studied methyl analogue ester (1-Naph-NMCB). On the other hand, in vitro studies with different cancer cell lines showed that the cytotoxic activity of both 1-Naph-NMCB and 1-Naph-NHCB were fully preserved and in some cases also enhanced when entrapped into liposomal carriers.

Published

2010

46. Crystal structure of (1E,3E)-4-methylthio-2-nitro-3-phenylsulfonyl-1- pyrrolidino-1,3-butadiene, C15H18N2C 4S2

Author

Cinzia Tavani, P Fossa, Giovanni Petrillo, Massimo Maccagno, Angelo Mugnoli, and Lara Bianchi

Subjects

Inorganic Chemistry, chemistry.chemical_compound, Crystallography, QD901-999, Chemistry, Nitro, Organic chemistry, Molecule, 1,3-Butadiene, General Materials Science, Crystal structure, Condensed Matter Physics, Sulfone

Abstract

C15H18N2O4S2, monoclinic, P121/c1 (No. 14), a = 8.754(3) Å, b = 12.499(2) Å, c = 15.599(3) Å, β = 95.09(2)°, V = 1700.1Å3, Z = 4, Rgt(F) = 0.049, wRref(F2) = 0.128, T = 294 K.

47. Ring-Opening/Ring-Closing Protocols from Nitrothiophenes: Six-Membered versus Unusual Eight-Membered Sulfur Heterocycles through Michael-Type Addition on Nitrobutadienes

Author

Fernando Sancassan, Marco Stenta, Domenico Spinelli, Massimo Maccagno, Lara Bianchi, Giovanni Petrillo, Cinzia Tavani, Gianluca Giorgi, and Elda Severi

Subjects

Thiopyran, fused-ring systems, medium-ring compounds, nitrothiophenes, ring expansion, sulfur heterocycles, Stereochemistry, Organic Chemistry, chemistry.chemical_element, nitrothiophenes, medium-ring compounds, General Chemistry, Ring (chemistry), Sulfur, Catalysis, sulfur heterocycles, fused-ring systems, chemistry.chemical_compound, chemistry, ring expansion, Moiety

Abstract

When Ar is a low-aromaticity homo- or heterosystem, the sulfonyl-stabilized anion of nitrobutadienes 4 (which derive from the initial ring opening of 3-nitrothiophene) undergoes a rather surprising addition onto the aromatic ring itself, thereby leading to the construction of an unusual eight-membered sulfur heterocycle condensed with the original Ar ring. The competitiveness of such a pathway with respect to the formation of the thiopyran ring (i.e., addition onto the nitrovinyl moiety) is favored at low temperatures, thus revealing its nature as a kinetically controlled process.

48. Nitrobutadienes from β-nitrothiophenes: Valuable building-blocks in the overall ring-opening/ring-closure protocol to homo- or hetero-cycles

Author

Bianchi, L., Erba, C., Massimo Maccagno, Morganti, S., Petrillo, G., Rizzato, E., Sancassan, F., Severi, E., Spinelli, D., and Tavania, C.