Your search keyword '"Angela Altomare"' showing total 13 results

1. New Findings on the Crystal Polymorphism of Imepitoin

Author

Giovanna Bruni, Doretta Capsoni, Anna Pellegrini, Angela Altomare, Mauro Coduri, Chiara Ferrara, Pietro Galinetto, and Renato Molteni

Subjects

imepitoin, differential scanning calorimetry, polymorphism, monotropy, X-ray diffraction, Organic chemistry, QD241-441

Abstract

Scientific and industrial reasons dictate the study of the solid state of imepitoin, a highly safe and tolerable anticonvulsant drug used in the therapy of epileptic dogs that was approved in the Europe Union in 2013. Our investigations allowed us to discover the existence of a new polymorph of imepitoin, which finds itself in a monotropic relationship with the crystalline form (polymorph I) already known and present on the market. This form (polymorph II), obtained by crystallization from xylene, remains metastable under ambient conditions for at least 1 year. Both solid forms were characterized by thermal (DSC and TGA), spectroscopic (FT-IR and Raman), microscopic (SEM and HSM), and diffractometric techniques. The thermodynamic relationship between the two polymorphs (monotropic) is such that it is not possible to study the melting of polymorph II, not even by adopting appropriate experimental strategies. Our measurements highlighted that the melting peak of imepitoin actually also includes an onset of melt decomposition. The ab initio structure solution, obtained from synchrotron X-ray powder diffraction data collected at room temperature, allowed us to determine the crystal structure of the new polymorph (II). It crystallizes in the monoclinic crystal structure, P21/c space group (#14), with a = 14.8687(6) Å, b = 7.2434(2) Å, c = 12.5592(4) Å, β = 107.5586(8)°, V = 1289.61(8) Å3, and Z = 4.

Published

2024

2. Solving molecular compounds from powder diffraction data: are results always reliable?

Author

Angela Altomare

Subjects

structure solution, powder diffraction, ambiguous structure determination, low crystallinity, pair distribution function, solid-state nuclear magnetic resonance, Crystallography, QD901-999

Published

2022

3. Crystal structure determination of a lifelong biopersistent asbestos fibre using single-crystal synchrotron X-ray micro-diffraction

Author

Carlotta Giacobbe, Dario Di Giuseppe, Alessandro Zoboli, Magdalena Lassinantti Gualtieri, Paola Bonasoni, Anna Moliterni, Nicola Corriero, Angela Altomare, Jonathan Wright, and Alessandro F. Gualtieri

Subjects

asbestos, micro-diffraction, synchrotrons, fibres, lung diseases, structure determination, Crystallography, QD901-999

Abstract

The six natural silicates known as asbestos may induce fatal lung diseases via inhalation, with a latency period of decades. The five amphibole asbestos species are assumed to be biopersistent in the lungs, and for this reason they are considered much more toxic than serpentine asbestos (chrysotile). Here, we refined the atomic structure of an amosite amphibole asbestos fibre that had remained in a human lung for ∼40 years, in order to verify the stability in vivo. The subject was originally exposed to a blend of chrysotile, amosite and crocidolite, which remained in his parietal pleura for ∼40 years. We found a few relicts of chrysotile fibres that were amorphous and magnesium depleted. Amphibole fibres that were recovered were undamaged and suitable for synchrotron X-ray micro-diffraction experiments. Our crystal structure refinement from a recovered amosite fibre demonstrates that the original atomic distribution in the crystal is intact and, consequently, that the atomic structure of amphibole asbestos fibres remains stable in the lungs for a lifetime; during which time they can cause chronic inflammation and other adverse effects that are responsible for carcinogenesis. The amosite fibres are not iron depleted proving that the iron pool for the formation of the asbestos bodies is biological (haemoglobin/plasma derived) and that it does not come from the asbestos fibres themselves.

Published

2021

4. Structural Characterization of Low-Sr-Doped Hydroxyapatite Obtained by Solid-State Synthesis

Author

Francesco Baldassarre, Angela Altomare, Ernesto Mesto, Maria Lacalamita, Bujar Dida, Altin Mele, Elvira Maria Bauer, Massimo Puzone, Emanuela Tempesta, Davide Capelli, Dritan Siliqi, and Francesco Capitelli

Subjects

hydroxyapatite, strontium, solid-state synthesis, PXRD, FTIR, Raman, Crystallography, QD901-999

Abstract

Strontium-substituted Ca10(PO4)6(OH)2 hydroxyapatite (HAp) powders, with Sr wt% concentrations of 2.5, 5.6 and 10%, were prepared by a solid-state synthesis method. The chemical composition of the samples was accurately evaluated by using inductively coupled plasma (ICP) spectroscopy. The morphology of the samples was analyzed via optical microscopy, while structural characterization was achieved through powder X-ray diffraction (PXRD) and infrared (FTIR) and Raman spectroscopy. The PXRD structural characterization showed the presence of the Sr dopant in the Ca1 structural site for HAp with a lower Sr concentration and in the Ca2 site for the sample with a higher Sr concentration. FTIR and Raman spectra showed slight band shifts and minor modifications of the (PO4) bands with increasing the Sr doping rate.

Published

2023

5. Dynamic Phenomena and Complexation Effects in the α-Lithiation and Asymmetric Functionalization of Azetidines

Author

Pantaleo Musci, Marco Colella, Angela Altomare, Giuseppe Romanazzi, Nadeem S. Sheikh, Leonardo Degennaro, and Renzo Luisi

Subjects

azetidines, organolithiums, nitrogen dynamics, heterocyclic chemistry, computational chemistry, Organic chemistry, QD241-441

Abstract

In this work it is demonstrated that enantiomerically enriched N-alkyl 2-oxazolinylazetidines undergo exclusive α-lithiation, and that the resulting lithiated intermediate is chemically stable but configurationally labile under the given experimental conditions that afford enantioenriched N-alkyl-2,2-disubstituted azetidines. Although this study reveals the configurational instability of the diastereomeric lithiated azetidines, it points out an interesting stereoconvergence of such lithiated intermediates towards the thermodynamically stable species, making the overall process highly stereoselective (er > 95:5, dr > 85:15) after trapping with electrophiles. This peculiar behavior has been rationalized by considering the dynamics at the azetidine nitrogen atom, the inversion at the C-Li center supported by in situ FT-IR experiments, and DFT calculations that suggested the presence of η3-coordinated species for diastereomeric lithiated azetidines. The described situation contrasted with the demonstrated stability of the smaller lithiated aziridine analogue. The capability of oxazolinylazetidines to undergo different reaction patterns with organolithium bases supports the model termed “dynamic control of reactivity” of relevance in organolithium chemistry. It has been demonstrated that only 2,2-substituted oxazolinylazetidines with suitable stereochemical requirements could undergo C=N addition of organolithiums in non-coordinating solvents, leading to useful precursors of chiral (er > 95:5) ketoazetidines.

Published

2022

6. Stereo- and Enantioselective Addition of Organolithiums to 2-Oxazolinylazetidines as a Synthetic Route to 2-Acylazetidines

Author

Pantaleo Musci, Marco Colella, Flavio Fanelli, Angela Altomare, Luisa Pisano, Claudia Carlucci, Renzo Luisi, and Leonardo Degennaro

Subjects

azetidine, lithiation, oxazoline, stereoselectivity, NMR calculations, oxazolidine, Chemistry, QD1-999

Abstract

A new synthetic route to N-alkyl-2-acylazetidines was developed through a highly stereoselective addition of organolithiums to N-alkyl-2-oxazolinylazetidines followed by acidic hydrolysis of the resulting oxazolidine intermediates. This study revealed an unusual reactivity of the C=N bond of the oxazoline group when reacted with organolithiums in a non-polar solvent such as toluene. The observed reactivity has been explained considering the role of the nitrogen lone pair of the azetidine ring as well as of the oxazolinyl group in promoting a complexation of the organolithium, thus ending up with the addition to the C=N double bond. The high level of stereoselectivity in this addition is supported by DFT calculations and NMR investigations, and a model is proposed for the formation of the oxazolidine intermediates, that have been isolated and fully characterized. Upon acidic conditions, the oxazolidine moieties were readily converted into 2-acylazetidines. This synthetic approach has been applied for the preparation of highly enantioenriched 2-acylazetidines starting from chiral not racemic N-alkyl-2-oxazolinylazetidines.

Published

2019

7. Crystal Structure Characterization by Powder Diffraction

Author

Rosanna Rizzi and Angela Altomare

Subjects

n/a, Crystallography, QD901-999

Abstract

The important role played by powder diffraction in the last twenty-five years both in its earlier fields of application (e [...]

Published

2020

8. Crystal Chemistry and Luminescence Properties of Eu-Doped Polycrystalline Hydroxyapatite Synthesized by Chemical Precipitation at Room Temperature

Author

Francesco Baldassarre, Angela Altomare, Nicola Corriero, Ernesto Mesto, Maria Lacalamita, Giovanni Bruno, Alberto Sacchetti, Bujar Dida, Dafina Karaj, Giancarlo Della Ventura, Francesco Capitelli, and Dritan Siliqi

Subjects

hydroxyapatite, europium, chemical precipitation method, PXRD, FTIR, Raman and PL spectroscopy, Crystallography, QD901-999

Abstract

Europium-doped hydroxyapatite Ca10(PO4)6(OH)2 (3% mol) powders were synthesized by an optimized chemical precipitation method at 25 °C, followed by drying at 120 °C and calcination at 450 °C and 900 °C. The obtained nanosized crystallite samples were investigated by means of a combination of inductively coupled plasma (ICP) spectroscopy, powder X-ray diffraction (PXRD), Fourier Transform Infrared (FTIR), Raman and photoluminescence (PL) spectroscopies. The Rietveld refinement in the hexagonal P63/m space group showed europium ordered at the Ca2 site at high temperature (900 °C), and at the Ca1 site for lower temperatures (120 °C and 450 °C). FTIR and Raman spectra showed slight band shifts and minor modifications of the (PO4) bands with increasing annealing temperature. PL spectra and decay curves revealed significant luminescence emission for the phase obtained at 900 °C and highlighted the migration of Eu from the Ca1 to Ca2 site as a result of increasing calcinating temperature.

Published

2020

9. Solving a Structure in the Reciprocal Space, Real Space and Both by Using the EXPO Software

Author

Angela Altomare, Nicola Corriero, Corrado Cuocci, Aurelia Falcicchio, and Rosanna Rizzi

Subjects

powder structure solution, expo software, reciprocal-space methods, real-space methods, Crystallography, QD901-999

Abstract

The solution of crystal structures from X-ray powder diffraction data has undergone an intense development in the last 25 years. Overlapping, background estimate, preferred orientation are the main difficulties met in the process of determining the crystal structure from the analysis of the one-dimensional powder diffraction pattern. EXPO is a well known computer program that, designed for solving structures, organic, inorganic, as well as metal-organic by powder diffraction data, employs the two most widely used kinds of solution methods: Direct Methods proceeding in the reciprocal space and Simulated Annealing proceeding in the real space. EXPO allows also to suitably combine these two approaches for validating the structure solution. In this paper, we give examples of structure characterization by EXPO with the aim of suggesting a solution strategy leading towards the application of reciprocal-space methods or real-space methods or both.

Published

2019

10. New Ca2.90(Me2+)0.10(PO4)2 β-tricalcium Phosphates with Me2+ = Mn, Ni, Cu: Synthesis, Crystal-Chemistry, and Luminescence Properties

Author

Angela Altomare, Rosanna Rizzi, Manuela Rossi, Asmaa El Khouri, Mohammed Elaatmani, Veronica Paterlini, Giancarlo Della Ventura, and Francesco Capitelli

Subjects

TCP, SEM-EDS, PXRD and Rietveld refinement, FTIR, luminescence spectroscopy, Crystallography, QD901-999

Abstract

C a 2.90 M e 0.10 2 + ( P O 4 ) 2 (with Me = Mn, Ni, Cu) β-tricalcium phosphate (TCP) powders were synthesized by solid-state reaction at T = 1200 °C and investigated by means of a combination of scanning electron microscopy (SEM) equipped with energy dispersive X-ray spectroscopy (EDS), powder X-ray diffraction (PXRD), Fourier transform infrared (FTIR) spectroscopy, and luminescence spectroscopy. SEM morphological analysis showed the run products to consist of sub spherical microcrystalline aggregates, while EDS semi-quantitative analysis confirmed the nominal Ca/Me composition. The unit cell and the space group were determined by X-ray powder diffraction data showing that all the compounds crystallize in the rhombohedral R3c whitlockite-type structure, with the following unit cell constants: a = b = 10.41014(19) Å, c = 37.2984(13) Å, and cell volume V = 3500.53(15) Å3 (Mn); a = b = 10.39447(10) Å, c = 37.2901(8) Å; V = 3489.22(9) Å3 (Ni); a = b = 10.40764(8) Å, c = 37.3158(6) Å, V = 3500.48(7) Å3 (Cu). The investigation was completed with the structural refinement by the Rietveld method. The FTIR spectra are similar to those of the end-member Ca β-tricalcium phosphate (TCP), in agreement with the structure determination, and show minor band shifts of the (PO4) modes with the increasing size of the replacing Me2+ cation. Luminescence spectra and decay curves revealed significant luminescence properties for Mn and Cu phases.

Published

2019

11. The Rietveld Refinement in the EXPO Software: A Powerful Tool at the End of the Elaborate Crystal Structure Solution Pathway

Author

Angela Altomare, Francesco Capitelli, Nicola Corriero, Corrado Cuocci, Aurelia Falcicchio, Anna Moliterni, and Rosanna Rizzi

Subjects

powder structure solution, EXPO software, Rietveld refinement, Crystallography, QD901-999

Abstract

The Rietveld method is the most reliable and powerful tool for refining crystal structure when powder diffraction data are available. It requires that the structure model to be adjusted is as close as possible to the true structure. The Rietveld method usually represents the final step of the powder solution process, in particular when a new structure is going to be determined and published. EXPO is a software able to execute all the steps of the solution process in a mostly automatic way, by starting from the chemical formula and the experimental diffraction pattern, passing through computational methods for locating the structure model and optimizing it, and ending to the Rietveld refinement. In this contribution, we present the most recent solution strategies in EXPO, both in reciprocal and direct space, aiming at obtaining models suitable to be refined by the Rietveld method. Examples of Rietveld refinements are described, whose results are related to different solution procedures and types of compounds (organic and inorganic).

Published

2018

12. Crystallographic study of PET radiotracers in clinical evaluation for early diagnosis of Alzheimers

Author

Angela Altomare, Elena Capparelli, Antonio Carrieri, Nicola A. Colabufo, Anna Moliterni, Rosanna Rizzi, and Dritan Siliqi

Subjects

crystal structure, ligands, P-glycoprotein inhibitor, PET radiotracer, hydrogen bonds, Crystallography, QD901-999

Abstract

The title compound, C24H25NO3·2CH3OH, which crystallized as a methanol disolvate, has applications as a PET radiotracer in the early diagnosis of Alzheimer's disease. The dihedral angle between the biphenyl rings is 8.2 (2)° and the heterocyclic ring adopts a half-chair conformation with the N atom adopting a pyramidal geometry (bond-angle sum = 327.6°). The C atoms of both methoxy groups lie close to the plane of their attached ring [deviations = 0.107 (6) and 0.031 (6) Å]. In the crystal, the components are linked by O—H...O and O—H...N hydrogen bonds, generating [010] chains. C—H...O interactions are also observed.

Published

2014

13. In-situ X-ray powder diffraction studies of hydrothermal and thermal decomposition reactions of basic bismuth(iii) nitrates in the temperature range 20–650 °C.

Author

Axel Nørlund Christensen, Torben René Jensen, Nicola V. Y. Scarlett, Ian C. Madsen, Jonathan C. Hanson, and Angela Altomare

Published

2003