METHOD FOR THE PRODUCTION OF SUB-MICROMETRIC PARTICLES AND THEIR THERANOSTIC USE IN ONCOLOGY WITH A SPECIFIC APPARATUS

Abstract
The invention relates to a method for producing sub-micrometric particles, which comprises: mechanochemical treatment of homogeneous or heterogeneous magnetic materials until a mass which consists mostly of magnetic nanocrystal aggregates is obtained; selection of aggregates so that the nanocrystals have a Curie temperature within a predefined variation range; functionalization of the aggregates in order to obtain coating thereof with molecules of one or more of the following types of substances: substances for which the tumour cells have a particular metabolic avidity; substances having a biochemical affinity with the tumour cells; substances having an affinity with the acid microenvironment which surrounds the neoplastic cells. In addition to the method the following are claimed: the particles thus produced; their theranostic use which allows the in vivo execution, without interruption, of the diagnosis or monitoring step and the therapy step by means of magnetic hyperthermia of malignant neoplasms, including those localized in the so-called “sanctuary sites” such as the central nervous system and the testicle; an apparatus designed for this use.
Description
FIELD OF THE INVENTION AND EXPLANATORY PREAMBLE

The present invention relates to a method for the production of particles of sub-micrometric size and to theranostic use thereof in oncology, i.e. a use in which the detection of tumours, in particular of malignant neoplasms, and the subsequent medical treatment thereof are closely associated.


As will be seen, the particles according to the present invention comprise nanocrystals, i.e., as defined by current scientific literature, crystallographically ordered agglomerations of a substance with characteristic dimensions in the range typically of less than 100 nm. Such an ordered agglomeration is separated from other nanocrystals by grain boundaries namely may consist of a single particle. The nanocrystals may also take the form of clusters of a certain number of nanocrystals so as to form larger size particles.


STATE OF THE ART

The most widespread therapeutic method used for malignant neoplasms is chemotherapy in which drugs are employed. However, in the case of those types of neoplasms localized in so-called “sanctuary sites” such as the central nervous system (CNS) and the testicle, the penetration of anti-neoplastic drugs is hindered by the presence of the blood-brain barrier or blood-testicle barrier (referred to henceforth herein as BBB and BTB, respectively).


The strategy used nowadays to overcome the obstacle posed by the BBB and BTB essentially consists in using supramaximal doses of said drugs, but this gives rise to a high risk of immediate side effects in the patients, such as a severe and prolonged reduction of the medullar function (with a consequent high risk of haemorrhage or infection), or delayed side effects, such as cognitive, cardiac or gonadal dysfunctions with reduced fertility.


Radiotherapy, namely the use of ionizing radiation, is another well-established method, which is frequently used in synergy with chemotherapy, to induce the necrosis of neoplastic masses. However, a part of the healthy tissues of the patient—which is albeit increasingly smaller with improvements to the method and the equipment for implementing it—is exposed to the radiation, with the well-known side effects.


In oncology for therapeutic purposes, during the last few years, considerable attention has been focussed on a method called magnetic hyperthermia based on obtaining the localized heating of the tumour cells which in particular are less resistant to heat than healthy cells. The method envisages the introduction, generally into the tumour cells themselves, of particles consisting at least partly of materials suitable for being subsequently heated inductively by means of application of an external electromagnetic field.


In this field a fundamental patent is U.S. Pat. No. 4,106,488 which envisages administering to patients affected by malignant neoplasms, ferromagnetic, diamagnetic and paramagnetic particles for which tumour cells have a greater affinity than healthy cells. The magnetic particles, which are encapsulated in materials able to be removed after a predetermined time and kept suspended in suitable physiological solutions, are introduced in vivo and conveyed towards the neoplasms since they have been previously combined with radioisotopes. At the end of a 12-hour period following administration, the application of an external electromagnetic field of suitable intensity results in overheating of the magnetic particles as a result of the inductive currents, which causes melting of the encapsulation materials and raises the temperature of the tumour cells to values such that they are destroyed.


In addition to the drawbacks due to the use of radioisotopes and the need for disposal of the encapsulating materials from the patient's body, it is necessary to mention also the amount of time which lapses between administration of the magnetic particles and heating thereof, namely when the tumour cells are actually destroyed. In any case it should be noted that this patent does not provide teachings relating to the methods for the production and selection of the magnetic particles, which are instead discussed in more recent documents.


Among the latter, the patent U.S. Pat. No. 5,441,746 describes a complex method for producing particles which have a magnetic, for example ferrite, core which initially comprises the addition in the liquid state of alkalis to bivalent and trivalent metallic hydroxides, followed by a mixing step for obtaining amorphous metallic gels which have a diameter of the order of 100 nm and finally a heating step performed in the presence of oxygen in order to dehydrate the gel and control the dimensions of the resultant crystalline metal oxides. In addition to the magnetic core, the particles comprise a dual coating which not only increases the absorption of the external electromagnetic waves by the core, and therefore overheating thereof, but also allows the particles to pass through specific physiological membranes which in the body protect certain types of cells.


The patent U.S. Pat. No. 7,122,030 refers to a therapeutic method for the treatment of malignant neoplasms by means of hyperthermia where ferroelectric particles are used, namely crystalline dielectric particles which may receive a permanent electrical polarization from a variable electric field. The ferroelectric particles are provided with a coating layer, for example a biocompatible and biodegradable polymer, so that they assume dimensions also of a significant nature (up to 15 μm) and are able to reach tumour cells situated also deep within the patient's body. The method is carried out under the guidance of a control system which comprises the measurement of the temperature of the particles and the parameters of the variable electric field so that the tumour cells reach a temperature (with a variation range of between 41.5 and 50° C.) which results in their destruction, while the healthy cells are not damaged. The patent does not provide any teachings as to the method for producing the ferroelectric particles, in particular their coating.


In addition to the above observations in connection with individual patents, the following may be deduced from examination of a broad and varied cross-section of the prior art on the subject of magnetic hyperthermia:


a) the methods for obtaining particles which are ready for use are most likely unsuitable for production on an industrial scale since they are particularly complex and/or involve particularly long process times: for example, in order to obtain the magnetic cores alone, without considering the subsequent steps where they are coated and/or functionalized, production steps such as synthesis by means of thermal decomposition of organo-metallic compounds in high-boiling organic solvents and methods for hydrothermal synthesis with a duration of up to 72 hours have been proposed;


b) the overall execution of the method for therapeutic purposes envisages that the patient must undergo numerous steps (administration of the particles, viewing of their arrival in the neoplasms to be treated, heating induction of the magnetic particles) which are performed in different locations and at different moments in time, with an increase in the costs for the health cares structure and greater demands, if not inconvenience, for the patient. The prior art includes also the following documents, the author of which is one of the present inventors and the contents of which are cited herein integrally as a reference source: P. MATTEAZZI, Reduction of haematite with carbon by room temperature ball milling, in Materials Science and Engineering, A149 (1991), which demonstrates the feasibility of magnetic nanocrystals in a high-energy mill and the patent application WO2012/085782 relating to a mechanochemical reactor with a high performance also from a technical/economic point of view.


It is pointed out that, in accordance with the scientific literature (for example the aforementioned article), “mechanochemical treatment” is understood as meaning the transformations produced by the impact of masses (milling bodies) which have a high kinetic energy per unit of homogeneous or heterogeneous material (volume, weight) exposed to impact. These mechanochemical transformations involve effects such as variations in the mixing state, structure and size of the crystals, distribution of the phases, state of aggregation or state of chemical combination of the elements and compounds present







OBJECT OF THE INVENTION

The object of the present invention therefore is to overcome the shortcomings and/or drawbacks of that which has been disclosed hitherto with regard to magnetic hyperthermia by proposing a therapeutic method which allows the treatment of all types of malignant neoplasm, even neoplasms localized in “sanctuary sites” such as the central nervous system and testicle, and which is able to replace chemotherapy and other treatment methods established in oncology, or at least reduce the use thereof, essentially by:

    • using sub-micrometric particles produced using methods and apparatus of proven technological and economic efficiency and using substances which, at least in preferred embodiments of the invention, are commonly available;
    • performing theranostics of the malignant neoplasms by means of a material and temporal combination of diagnosis and therapy using an apparatus, which is novel but based on already well-known systems, allowing the reduction of investment and operating costs affecting health care structures as well as the demands and inconveniences for patients.


Subject-Matter of the Invention

In order to achieve this object and other objects, a first subject of the present invention consists in a method for producing particles with sub-micrometric dimensions for in vivo oncological use, comprising the following steps:


A. mechanochemical treatment of homogeneous or heterogeneous, powdery, magnetic materials in a controlled atmosphere and, where appropriate, in the presence of a liquid phase of not more than 5% by volume, until a consistent mass comprising at least 80% by volume of magnetic nanocrystal aggregates is obtained. The aggregates have mainly dimensions smaller than 500 nm and are formed by nanocrystals mainly with dimensions smaller than 100 nm.


B. dispersion of said aggregates in a biocompatible fluid;


C. dimensional selection and distribution of the nanocrystal aggregates depending on their Curie temperature within a predefined variation range. (It should be remembered that the Curie temperature is the temperature for transition from the ferromagnetic state to the paramagnetic state and this temperature depends on the dimensions of the crystal). It is carefully selected in order to limit the maximum heating temperature of the magnetic particles so as to cause destruction of the tumour cells, leaving the surrounding zones of healthy tissue undamaged;


D. functionalization of the magnetic nanocrystal aggregates obtained during step C so as to obtain a coating thereof which comprises molecules of one or more of the following types of substances: substances for which the tumour cells have a particular metabolic avidity; substances having a biochemical affinity with the tumour cells; substances having an affinity with the acid microenvironment which surrounds the neoplastic cells. In accordance with the Warburg effect (discovered in 1923 by O. H. Warburg, Nobel Prize winner in 1931), the tumour cells have a high avidity for monosaccharide carbohydrates such as glucose and produce an extra-cellular pH which is more acid than healthy tissues.


In a preferred embodiment, the mechanochemical treatment of step A is performed by loading the powdery materials into a high-energy mill or alternatively into a mechanochemical reactor such as that described in the patent application WO 2012/085782 which, as mentioned above, is herein integrally incorporated by reference.


In a further preferred embodiment of the present invention, in order to achieve functionalization for the metabolic avidity in step D, the aforementioned coating molecules are monosaccharide carbohydrates, preferably glucose, provided at a first end (distal end) with spacers having a substantially linear form. The second end (proximal end) of the spacers is provided with a group having a high affinity towards the nanocrystals (for example chosen from among carboxylates, phosphonates or phosphates). In other words, the aforementioned molecules, for example glucose, form the outermost part of the coating of the magnetic nanocrystal aggregates.


A second subject of the present invention consists in the sub-micrometric particles produced using this method and able to be employed in the treatment of any type of malignant neoplasm, including neoplasms localized in “sanctuary sites” such as the central nervous system and the testicle.


A third subject of the present invention is an in vivo oncological use of the said sub-micrometric particles; this type of use is nowadays commonly referred to as being theranostic since, during it, the diagnosis (and hence also monitoring) and the therapy of the malignant neoplasms are performed immediately one after another, i.e. without interruption. The said use is performed in accordance with the following sequence of steps:


A. by means of a biologically compatible solution the introduction, intravenously, into the patient's body, of sub-micrometric particles comprising magnetic nanocrystal aggregates functionalized with a suitable coating. The nanocrystals are selected so that their Curie temperature is within a predetermined variation range. The coating of the sub-micrometric particles comprises molecules of one or more of the following types of substances: substances for which the tumour cells have a particular metabolic avidity; substances having a biochemical affinity with the said cells; substances having a chemical affinity with the prevalent acidity of the tumoural microenvironment;


B. the localization of the tumour cells by means of a magnetic resonance imaging (MRI) system which uses the tracing effect of the magnetic nanocrystals. In fact, the latter, owing to mutual attraction between tumour cells (and the tumoural microenvironment) and the coating molecules of the sub-micrometric particles, agglomerate (i.e. are concentrated in a substantially significant manner) in the tumoural tissues namely not only inside the tumour cells, but also in contact with them and in any case in the immediate vicinity thereof, for example in the region of the BBB and the BTB. Therefore, during this step B, owing to the present invention, the neoplasms may be diagnosed and monitored with extreme precision;


C. the application to the patient's body, immediately following, i.e. without interruption after the preceding step B, of an external, variable, electromagnetic field with a predetermined intensity and frequency. The field is located on the tumoural masses defined in step B. According to a preferred embodiment of the present invention, the electromagnetic field is generated by means known per se which are added to a machine, also known per se, of the magnetic resonance imaging (MRI) system, with which the preceding step B of this method is performed;


D. the electromagnetic field generates in the magnetic nanocrystals the inductive currents which cause overheating thereof and consequently heating of the magnetic nanocrystals concentrated in the region of the tumour cells with temperatures limited by the Curie temperature range. According to the present invention, this step is performed in a very precise manner by means of detection of the attenuation of the response which is provided by the tracer and which corresponds to the fact that the magnetic nanocrystals reach the Curie temperatures with the consequent necrosis of the tumour cells. As soon as the temperature of the magnetic nanocrystals exceeds the maximum value (Tmax) of the predefined variation range of the Curie temperature, the generation of the electromagnetic field is interrupted, preventing damage to the surrounding healthy tissue in which, as already mentioned, the magnetic nanocrystals are present in a significantly smaller concentration.


A last subject of the present invention is an apparatus suitable for the use described above, for implementing this method.


The above reveals two kinds of advantages offered by the present invention which clearly provides an effective theranostic approach. The first advantage is that the posture of the patient remains unchanged from start to finish, with obvious less inconvenience. The second which favours the health care establishment where this approach is adopted, consists in: lower investment costs for the machinery used in the oncology department, together with a smaller space occupied; reduction in the amount of time spent by the patient in the health care structure.


EMBODIMENTS OF THE INVENTION

Hereinbelow a number of preferred embodiments are described in detail in order to highlight better the characteristic features and advantages of the present invention compared to the prior art. It is understood, however, that other embodiments thereof may be provided and realized and/or variants thereof may be developed within the scope of protection defined in the claims below.


Firstly the three main steps of the method for the production of sub-micrometric particles for oncological use are described below with the aid of a number of examples.


Step A—Mechanochemical Treatment of Cowdery Materials

According to experiments carried out on the second embodiment of the mechanochemical reactor described in the already mentioned patent application. WO 2012/085782 the feasibility of the following treatments has been demonstrated.


Direct Conversion


Magnetic materials consisting of oxide powders (e.g. iron oxides), or carbides (e.g. iron carbides), intermetallic compounds or other compounds or magnetic alloys are treated, namely ground, in the solid state in a neutral atmosphere and without addition of heat. The duration of the treatment is the time needed to obtain a mass which consists principally (at least 80% by volume) of aggregates with dimensions smaller than 500 nm, the aggregates being in turn formed by magnetic nanocrystals, the dimensions of which are smaller than 100 nm and typically included within the range of 10-50 nm. In certain circumstances, in order to obtain the desired result, it may be required to introduce into the mill also suitable process agents (such as alcohols, stearates, hydrocarbons, water, although any liquid phase present during treatment is not greater than 5% by volume) or integrate the milled product into the reactor with a conventional disintegration treatment by means of ultrasound or the like.


Mechanochemical Synthesis


Iron in powder form (pure element) is treated, namely ground, in the solid state and without addition of heat inside a mechanochemical reactor where an atmosphere with an adjustable oxygen content is maintained for the time needed to obtain the reaction Fe+O→FeOx, namely to obtain bivalent or trivalent magnetic oxides depending on the oxygen content inside the reactor. The duration of the treatment is the time needed to obtain a mass which consists principally (at least 80% by volume) of aggregates with dimensions smaller than 500 nm, the aggregates being in turn formed by magnetic nanocrystals, the dimensions of which are smaller than 100 nm and typically within the range of 10-50 nm. In the same way a large variety of compounds and magnetic alloys of iron or other metals may be produced.


Mechanochemical Synthesis and Transformation


Powdery magnetic materials consisting of oxides (e.g. iron oxides) or carbides (e.g. iron carbides), intermetallic compounds or other compounds or metallic alloys may be obtained in forms, also of a mixed nature, with a combination of the treatments described above so as to obtain magnetic systems which may also be complex in nature. In a mechanochemical reactor transformation such as those indicated below by way of example are obtained:


Fe2O3+Crx→Fe2CrxO3 and Fe2O3+Cr2O3→FexCryOz (mixed iron and chromium oxides)


Fe+C+Cr→FexCryCz (complex chromium carbide)


Co+C→CoCr (cobalt-chromium alloy).


In this case also the duration of the treatment is the time needed to obtain a mass which consists principally (at least 80% by volume) of aggregates with dimensions smaller than 500 nm, the aggregates being in turn formed by magnetic nanocrystals, the dimensions of which are mainly less then 100 nm and typically included within the range of 10-50 nm.


Step C—Magnetic Selection of the Nanocrystals

For the purposes of the intended oncological use of the particles it is of fundamental importance to select a dimensional category of the nanocrystals corresponding to a correct Curie temperature, namely a temperature able to induce the necrosis of the tumour cells without damaging the healthy cells. For this purpose it is preferable that the Curie temperature of the magnetic nanocrystals should be in a range having a minimum value Tmin=38° C. and a maximum value Tmax=42° C.


The aggregates obtained for example in accordance with one of the aforementioned examples are dispersed in a liquid phase so as to obtain a dispersion of nanocrystal aggregates (Step B). Obviously, a biocompatible liquid phase, for example an aqueous solution, must be used, namely one such as not to cause any modification of the chemical composition of the nanocrystals and not alter their magnetic properties.


In order to select, for the purposes of the intended oncological use, all and only the magnetic nanocrystal aggregates which have a Curie temperature within the desired range, according to the present invention the procedure below is adopted. Firstly the solution is brought to the temperature Tmax which is kept thermostatically controlled while, by means of a first magnetic filter immersed in the solution, all the magnetic nanocrystals which have a Curie temperature higher than the said value Tmax are removed therefrom. The temperature of the solution is then lowered down to the temperature Tmin which is kept under thermostatic control, while, with the aid of a second magnetic filter, the nanocrystal aggregates with a Curie temperature within the range Tmin÷Tmax are extracted for the subsequent oncological use.


Step D—Functionalization of the Nanocrystal Aggregates

In the present invention, the primary aim of functionalization of the nanocrystal aggregates obtained and selected during the preceding steps is to produce a coating of the aggregates which maximizes the mutual attraction between tumoural masses in vivo and sub-micrometric particles.


According to the present invention, molecules of various types may be used in order to obtain the coating of the magnetic nanocrystal aggregates: substances for which the tumour cells have a particular metabolic avidity (for example monosaccharide carbohydrates, in particular glucose); substances having a biochemical affinity with the tumour cells (for example monoclonal anti-bodies); substances having an affinity with the acid microenvironment which surrounds the neoplastic cells (for example linear polysaccharides such as chitosan).


For example in the case of a coating with monosaccharide carbohydrates, the present invention envisages making use of standard organic synthesis procedures in order to form the biocompatible spacers with a linear form of varying length. A first end (distal end) of each spacer is provided with molecules, for example glucose, while the other end (proximal end) is provided with a group having a high affinity towards the magnetic properties of the nanocrystals (such as carboxylates, phosphonates and phosphates).


In the case of malignant neoplasms localized in so-called “sanctuary sites” such as the central nervous system (CNS) and the testicle, where the blood-brain barrier and the blood-testicle barrier are respectively present, the coating therefore has the effect of bringing the magnetic nanocrystals into direct contact with, even though not inside, the tumour cells. In other words, a concentration of the magnetic nanocrystals in the region around the tumour cells is obtained.


An example of implementation of the method illustrated above is provided below solely by way of a non-limiting example.


Step A—Mechanochemical Treatment


According to a possible embodiment of step A, a mechanochemical reactor of the type described in the already mentioned patent application WO2012/085782 provided with milling balls with a weight of 15 kg and operating with an oscillating frequency of 15 Hz, may be used. The powdery magnetic material introduced into the reactor for treatment may have an overall weight of 1.5 kg and may be magnetite (Fe3O4) with a mean distribution of the particles of 35 μm: consequently the ratio between material to be treated and milling means is 1:10. After being subjected to a vacuum, the milling chamber of the reactor may be filled for example with 99.99% pure argon with 2% of added oxygen.


The treatment may last 4 hours and may give rise to about 1 kg of aggregates with dimensions of less than 400 nm. Then the aggregates may undergo characterization with X-ray diffraction and evaluation using the Scherrer equation. Advantageously, the aggregates may be formed by magnetite crystals with an average size smaller than 10 nm (magnetic nanocrystals).


Step B—Dispersion (Disaggregation) of the Aggregates


For this step a conventional grinding mill for example of the type commercially distributed by Union Process Inc. (USA) and provided with milling balls made of zirconium oxide with a diameter of 300μ and overall weight of 2 kg, filled with 2 litres of water and operating at a speed of rotation of 100 rpm, may be used. 300 g of powder (aggregates of magnetite nanocrystals obtained in Step A) may be loaded into the grinding mill. At the end of a process time of 2 hours an aqueous dispersion of particles may be obtained, the weight distribution thereof consisting 90% of particles with a size smaller than 60 nm which may be advantageously measured using a laser diffractometer, for example of the type commercially distributed by Malvern Instruments Ltd (UK). Using a set of filters with dimensions ranging from 8 μm to 50 nm it is possible to obtain a liquid which consists of about 2 litres of water and in which a solid dispersion of aggregate particles of magnetite nanocrystals with an average size of 10 nm for about 100 g is formed.


Step C—Magnetic Selection of the Nanocrystals


The solution obtained at the end of Step B and temperature-controlled at 42° C. may be passed through a first magnetic filter which is also kept at 42° C. so as to capture the particles having a Curie temperature higher than this value. After lowering the temperature to 38° C., the solution thus selected may be passed through a second, different, magnetic filter kept at 38° C. so as to capture the particles with a Curie temperature greater than 38° C. and therefore inside the desired range, i.e. between 38° C. (Tmin) and 42° C. (Tmin) for subsequent theranostic use. The “useful” particles of magnetite, namely those selected in this way, may total about 30 g in weight (10% compared to the initial 300 g).


The fluid selected with particles having a Curie temperature of less than 38° C. may also be replenished, in the same weight proportion, with the selected particles in the temperature range 38-42° C., so as to form a system comprising the superparametric fraction at a body temperature (useful for basic imaging) supplemented with the particles useful for the treatment.


Step D—Functionalization


In the present invention, the primary aim of functionalization of the nanocrystal aggregates obtained and selected during the preceding steps is to produce a coating of the aggregates which maximizes the mutual attraction between tumoural masses in vivo and sub-micrometric particles, which could be for example glucose. In the case of magnetic oxide particles, as in this example, it may be particularly useful, for example, to use a coating of the particles with silanes (silanization) which allows both the attachment of various carrier substances and the dispersion of the particles in water, facilitating their stability in an aqueous solution.


The particles selected in Step C may be dispersed in water in a concentration of 5% and the silanization may be performed using 3-aminopropyltriethoxysilane, leaving for example the dispersion at 40° C. for 3 hours. By subsequently heating the same dispersion to 70° C. with glucose in a concentrated aqueous solution, a fructosamine Rp—NH—CH2—CO—(CHOH)3—CH2OH which coats the single particle may be obtained according to the Amadori reaction. The stable dispersion thus obtained may be used directly for intravenous injection in the amount of 30 micromol Fe/kg of bodyweight.


According to the present invention, a preferred form of oncological use of the sub-micrometric particles is performed with a novel apparatus which is based on a conventional magnetic resonance imaging (MRI) system, substantially all the parts of which are maintained, and which further comprises one or more induction coils for generating an oscillating electromagnetic field, as well as means for regulating the parameters of the field and directing it towards the zone of the patient's body where the neoplasm is assumed to be present.


With this apparatus it is possible to perform both the diagnosis (and monitoring) as well as the treatment of the neoplasms, without interruption, i.e. in a continuous manner, while keeping the posture of the patient unchanged.


The diagnosis step is per se conventional in that it ascertains the location of the magnetic aggregates (present in the sub-micrometric particles previously introduced into the patient's body intravenously) in the region of the tumour cells, owing to the “attraction” which the latter exert on the molecules of their coating.


During therapy, the electromagnetic field generated by the induction coils results in heating of the nanocrystals which, following selection thereof, as already described above, remain with certainty within the predefined variation range of the Curie temperature. The heating is interrupted instantaneously while, at the same time, the nanocrystals are no longer “viewable” by the diagnostic means owing to the fact that they have lost their magnetic properties. As a result it is possible to establish a principle which ensures the specific and selective destruction of the tumour cells, without damaging the healthy tissues, including those which are in the immediate vicinity of the neoplasms.


More particularly, the theranostic method may be carried out for example on a visible mass traced in conventional MRI (magnetic resonance imaging). After prior treatment with cortisones and anti-histamines, the previously mentioned dispersion from step D selected within the Curie temperature range 38-43° C. may be injected intravenously. An induction coil with an induced field of 7 KA/m at the frequency of 100 KHZ may be used, for example, for the treatment, having been placed inside a magnetic resonance machine. The part to be treated is inserted inside the coil after anaesthesia. Before application of the field, the MRI causes a reduction in the signal in the region of the mass owing to the accumulation of the magnetic particles caused by the glucose carrier. Following application of the induced field, as described above, after about 5 minutes, the image in the region of the tumoural mass may be seen highlighted. This is due to the gradual entry into the super-paramagnetic field of the particles within the temperature range of 38-43° C. The zones surrounding the tumoural mass, during the treatment which may last one hour in total, are stable in the MRI signal, with no substantial thermal alteration being detected therein. Advantageously, an analysis of the tumoural mass and the surrounding tissue may reveal a considerable degree of cellular necrosis of the tumoural mass without damage to the healthy tissue.


It is understood that other variations and embodiments are included within the scope of protection defined by the accompanying claims.

Claims
  • 1. Method for the production of sub-micrometric particles for the in vivo treatment of tumour cells, comprising the steps of: A. mechanochemical treatment of homogeneous or heterogeneous, powdery, magnetic materials in a controlled atmosphere, and in the presence of a liquid phase of not more than 5% by volume, until a consistent mass with at least 80% by volume of magnetic aggregates mainly with dimensions smaller than 500 nm is obtained, said aggregates being formed by magnetic nanocrystals mainly with dimensions smaller than 100 nm;B. dispersion of the magnetic aggregates in a fluid;C. dimensional selection and distribution of the magnetic aggregates present in the said fluid depending on their Curie temperature within a predefined variation range (Tmin-Tmax);D. functionalization by coating the aggregates with substances designed to generate a mutual attraction between the tumour cells and the nanocrystals of the magnetic aggregates.
  • 2. Method according to claim 1, wherein the mechanochemical treatment takes place, in a high-energy mill or, alternatively, in a mechanochemical reactor, where an atmosphere with a controlled oxygen content is maintained.
  • 3. Method according to claim 1 or claim 2, wherein the dimensional selection and distribution of the magnetic nanocrystal aggregates dispersed in a biocompatible fluid comprises in succession: a) heating and keeping the fluid at the maximum temperature of the predefined variation range Tmax;b) removing from the fluid by means of a first magnetic filter the aggregates having a Curie temperature greater than Tmax c) cooling the fluid from which the said aggregates have been removed to the minimum temperature within the predefined variation range Tmin and keeping the fluid at said temperature;d) removing from the fluid by means of a second magnetic filter the aggregates having a Curie temperature within the range Tmin-Tmax with a view to subsequent oncological use.
  • 4. Method according to any one of claims 1 to 3, wherein functionalization of the aggregates is performed using molecules of substances for which the tumour cells have a particular metabolic avidity, such as monosaccharide carbohydrates, in particular glucose.
  • 5. Method according to any one of claims 1 to 3, wherein the functionalization of the aggregates is performed using molecules of substances having a biochemical affinity with the tumour cells such as monoclonal antibodies.
  • 6. Method according to any one of claims 1 to 3, wherein functionalization of the aggregates is performed using molecules of substances having an affinity with the acid microenvironment which surrounds the tumour cells such as linear polysaccharides, in particular chitosan.
  • 7. Sub-micrometric particles for theranostic use in the treatment of neoplasms, obtained according to the methods of any one of the preceding claims, comprising: an aggregate of nanocrystals of at least one of the following magnetic materials: iron oxides, also of a mixed and complex nature; intermetallic compounds and iron-containing magnetic alloys; magnetic systems consisting of iron with other metals.a coating of the said aggregate of magnetic nanocrystals comprising molecules of at least one of the following types of substances: substances for which the tumour cells have a particular metabolic avidity; substances having a biochemical affinity with the tumour cells; substances having an affinity with the acid microenvironment which surrounds the neoplastic cells.
  • 8. Theranostic use in oncology of sub-micrometric particles produced with the method according to any one of claims 1 to 6 and/or claim 7, comprising in succession and without interruption the steps of: A. introducing intravenously the sub-micrometric particles into the patient's body using a compatible physiological solution;B. diagnosis and/or monitoring of tumour cells by means of location of the magnetic nanocrystal aggregates concentrated in the vicinity or inside the said cells as a result of attraction of the molecules of the coating of the magnetic nanocrystal aggregates by means of a magnetic resonance imaging system known per se;C. localized heating, inductively, of the magnetic nanocrystals to a temperature within a predefined variation range of the Curie temperature having, as an effect, the destruction of the tumour cells by means magnetic hyperthermia;D. detection of the loss of the magnetic properties of the nanocrystals upon reaching the Curie temperature by means of the said imaging system known per se; andE. simultaneous stoppage of said heating operation so as to ensure that the healthy tissue surrounding the tumour cells remains undamaged, since it is at a lower temperature.
  • 9. Apparatus for implementing a theranostic use in oncology according to claim 8, the apparatus being based on a magnetic resonance imaging (MRI) system known per se and also comprising means for generating an electromagnetic field designed to heat inductively, to a value within a predefined variation range of the Curie temperature, the magnetic nanocrystal aggregates forming part of the sub-micrometric particles previously introduced intravenously into the patient's body.
  • 10. Apparatus for implementing a theranostic use in oncology according to claim 9, characterized in that said heating means are designed to stop following the loss of the magnetic properties of the nanoparticles.
  • 11. Apparatus according to either one of claims 9 to 10, wherein the means for generating a variable electromagnetic field comprise one or more induction coils and means for varying the parameters of the said field and directing it towards the zone of the patient's body where a neoplasm is assumed to be present.
Priority Claims (1)
Number Date Country Kind
TV2013A000027 Feb 2013 IT national
PCT Information
Filing Document Filing Date Country Kind
PCT/IB2014/059337 2/28/2014 WO 00