Tesi etd-04032025-213327 |
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Tipo di tesi
Tesi di dottorato di ricerca
Autore
SONAGLIONI, DANIELE
URN
etd-04032025-213327
Titolo
Calorimetry and electron diffraction of molecular compounds of pharmaceutical interest
Settore scientifico disciplinare
PHYS-03/A - Fisica sperimentale della materia e applicazioni
Corso di studi
FISICA
Relatori
tutor Prof. Capaccioli, Simone
correlatore Dott. Gemmi, Mauro
correlatore Dott. Gemmi, Mauro
Parole chiave
- calorimetry
- crystal
- dynamics
- fast calorimetry
- kinetics
- pharmaceuticals
- structure
Data inizio appello
07/04/2025
Consultabilità
Non consultabile
Data di rilascio
07/04/2028
Riassunto
Pharmacology, as a discipline, has existed since ancient times and has as
primary purpose the treatment of human diseases: at the beginning, herbs
were at the basis of this discipline, but, with the evolution of chemistry, it
was possible to isolate the active principle, namely a molecule, useful for
treating illnesses. Nowadays, scientists have developed several ways to treat
diseases: depending on the specific application, it is possible to use as active
principle molecules, proteins, nanoparticles and so on.
This thesis poses its focus on molecular compounds of pharmaceutical interest,
namely molecules with molecular mass of less than 1000 Da. Traditionally,
pharmaceuticals have been prepared in their crystalline state due
to their physical stability upon long term storage. Later on, it has been
discovered that the amorphous state grants a higher water solubility to the
active principle, increasing its bioavailability and speeding up its intake by
the body. However, the use of glassy pharmaceuticals in practical applications
is hampered by the reverse of the material to the crystalline state: since
the glassy state is metastable, reverse to the crystalline state can take from
a couple of hours to months, even if the sample is stored at temperature
far below the glass transition temperature. On top of that, most of the recently
discovered active principles have a poor water solubility, making the
amorphous state desirable for their formulation.
These issues have involved significant efforts in the pharmaceutical sector.
However, they have been addressed on a time-consuming, case-by-case basis,
using different methods and formulation strategies, with an overall slowdown
in the production process. On the other hand, there is lack of a general
understanding of the basic principles ruling the phenomena involving pharmaceutical
materials, making the case-by-case approach the only possible
route. In fact, despite the knowledge of the behaviour of the specific active
ingredient is of utmost importance for the successful development of
the final product, a more general approach is desirable to speed up formulation
and development and formulation of new pharmaceuticals. Indeed, a
thorough understanding of these phenomena would make the development
of new drugs faster and less diffcult, thanks to an approach based on the
use of generalised rules. This thesis is an experimental study of some of
the phenomena associated with pharmaceutical compounds, with the aim of shedding new light on them from a basic science point of view and opening
new perspectives on old questions. The experimental studies have been
carried out mainly with two techniques, differential scanning calorimetry
(conventional and fast) and electron diffraction. The first gives information
about the thermodynamics of the sample under exam, enabling the study of
crystallization kinetics, amorphization, physical ageing and polymorphism,
whereas the latter is about the crystalline structure of the compound, i.e.
the three-dimensional arrangement of the molecules in space. Even though
these information can appear very different in nature, they are closely linked
because the crystalline structure influences the thermodynamic properties of
the specimen and vice versa. Additionally, broadband dielectric spectroscopy
and neutron spectroscopy have been employed to gather information on the
dynamics of the samples under investigation. Indeed, regardless of the phenomenon
being considered, the combination of dynamic (spectroscopic techniques),
thermodynamic (DSC/FDSC) and structural (electron diffraction)
information provides a unified view of the phenomenon, whose interpretation
would be biased or incomplete without at least one of the three perspectives.
This thesis is divided in four chapters, each section discussing a specific topic.
The first chapter gives to the reader the theoretical background of the physical
phenomena investigated. Details about the experimental techniques and
data analysis are provided in the second chapter. The third chapter exposes
and critically discusses the results obtained during my PhD period, highlighting
the future perspectives of the specific study when needed. The last
chapter is devoted to make a summary of the work done, the main achievements
and future perspectives.
primary purpose the treatment of human diseases: at the beginning, herbs
were at the basis of this discipline, but, with the evolution of chemistry, it
was possible to isolate the active principle, namely a molecule, useful for
treating illnesses. Nowadays, scientists have developed several ways to treat
diseases: depending on the specific application, it is possible to use as active
principle molecules, proteins, nanoparticles and so on.
This thesis poses its focus on molecular compounds of pharmaceutical interest,
namely molecules with molecular mass of less than 1000 Da. Traditionally,
pharmaceuticals have been prepared in their crystalline state due
to their physical stability upon long term storage. Later on, it has been
discovered that the amorphous state grants a higher water solubility to the
active principle, increasing its bioavailability and speeding up its intake by
the body. However, the use of glassy pharmaceuticals in practical applications
is hampered by the reverse of the material to the crystalline state: since
the glassy state is metastable, reverse to the crystalline state can take from
a couple of hours to months, even if the sample is stored at temperature
far below the glass transition temperature. On top of that, most of the recently
discovered active principles have a poor water solubility, making the
amorphous state desirable for their formulation.
These issues have involved significant efforts in the pharmaceutical sector.
However, they have been addressed on a time-consuming, case-by-case basis,
using different methods and formulation strategies, with an overall slowdown
in the production process. On the other hand, there is lack of a general
understanding of the basic principles ruling the phenomena involving pharmaceutical
materials, making the case-by-case approach the only possible
route. In fact, despite the knowledge of the behaviour of the specific active
ingredient is of utmost importance for the successful development of
the final product, a more general approach is desirable to speed up formulation
and development and formulation of new pharmaceuticals. Indeed, a
thorough understanding of these phenomena would make the development
of new drugs faster and less diffcult, thanks to an approach based on the
use of generalised rules. This thesis is an experimental study of some of
the phenomena associated with pharmaceutical compounds, with the aim of shedding new light on them from a basic science point of view and opening
new perspectives on old questions. The experimental studies have been
carried out mainly with two techniques, differential scanning calorimetry
(conventional and fast) and electron diffraction. The first gives information
about the thermodynamics of the sample under exam, enabling the study of
crystallization kinetics, amorphization, physical ageing and polymorphism,
whereas the latter is about the crystalline structure of the compound, i.e.
the three-dimensional arrangement of the molecules in space. Even though
these information can appear very different in nature, they are closely linked
because the crystalline structure influences the thermodynamic properties of
the specimen and vice versa. Additionally, broadband dielectric spectroscopy
and neutron spectroscopy have been employed to gather information on the
dynamics of the samples under investigation. Indeed, regardless of the phenomenon
being considered, the combination of dynamic (spectroscopic techniques),
thermodynamic (DSC/FDSC) and structural (electron diffraction)
information provides a unified view of the phenomenon, whose interpretation
would be biased or incomplete without at least one of the three perspectives.
This thesis is divided in four chapters, each section discussing a specific topic.
The first chapter gives to the reader the theoretical background of the physical
phenomena investigated. Details about the experimental techniques and
data analysis are provided in the second chapter. The third chapter exposes
and critically discusses the results obtained during my PhD period, highlighting
the future perspectives of the specific study when needed. The last
chapter is devoted to make a summary of the work done, the main achievements
and future perspectives.
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