Particle formation methods and their products
원문보기
IPC분류정보
국가/구분
United States(US) Patent
등록
국제특허분류(IPC7판)
A61K-009/00
A61K-009/14
출원번호
US-0004522
(2001-11-01)
우선권정보
GB-0027357.3(2000-11-09)
발명자
/ 주소
Hanna,Mazen H.
York,Peter
출원인 / 주소
Nektar Therapeutics UK, Ltd.
대리인 / 주소
Patterson &
인용정보
피인용 횟수 :
5인용 특허 :
13
초록▼
Preparation of particles of an active substance having a layer of an additive at the particle surfaces, by dissolving both the active substance and the additive in a vehicle to form a target solution, and contacting the target solution with an anti-solvent fluid using a SEDS짰 particle formation proc
Preparation of particles of an active substance having a layer of an additive at the particle surfaces, by dissolving both the active substance and the additive in a vehicle to form a target solution, and contacting the target solution with an anti-solvent fluid using a SEDS짰 particle formation process, to cause the active substance and additive to coprecipitate. The additive is typically a protective additive, in particular a taste and/or odour masking agent. Also provided is a particulate coformulation made by the method, which has a finite gradient in the relative additive concentration, which concentration increases radially outwards from the active-rich core to the additive-rich surface of the particles.
대표청구항▼
The invention claimed is: 1. A particulate coformulation of an active substance and an additive, which is a solid dispersion of one component in the other formed from a co-precipitation process containing a supercritical fluid, whererin each particle contains a particle core having a first concentr
The invention claimed is: 1. A particulate coformulation of an active substance and an additive, which is a solid dispersion of one component in the other formed from a co-precipitation process containing a supercritical fluid, whererin each particle contains a particle core having a first concentration by weight of the active substance within a range from about 90% to about 100%, a particle surface having a second concentration by weight of the active substance within a range from about 0% to about 5%, a relative additive concentration increasing radially outwards along a finite gradient and the particles are spherical or approximately spherical particles having a volume mean diameter of less than 100 μm, or needle-like particles having a volume mean length within a range from about 5 μm to about 100 μm and a volume mean thickness within a range from about 0.5 μm to about 5 μm, or plate-like particles having a volume mean thickness within a range from about 0.5 μm to about 5 μm. 2. A particulate coformulation according to claim 1, wherein the particle surface is an additive-rich surface without a distinct boundary between the particle core and the particle surface. 3. A particulate coformulation according to claim 1, wherein the relative additive concentration has a continuous rate of change across the finite gradient. 4. A particulate coformulation according to claim 1, wherein an active substance:additive ratio, at the particle surface, is sufficiently low for the additive to form a protective surface layer around the active substance. 5. A particulate coformulation according to claim 1, wherein the additive is a taste masking agent or an odor masking agent, and wherein an active substance:additive weight ratio, at the particle surface, is sufficiently low for there to be no detectable release of the active substance for at least 30 seconds after the coformulation comes into contact with saliva in a mouth of an individual. 6. A particulate coformulation according to claim 1, wherein the particle surface contains no exposed active substance. 7. A particulate coformulation according to claim 1, which comprises a pharmaceutical agent or a nutriceutical agent or a foodstuff. 8. A particulate coformulation according to claim 1, wherein the additive is an oligomeric material or a polymeric material. 9. A particulate coformulation according to claim 1, wherein the additive is a substance capable of protecting the active substance from at least one external effect selected from the group consisting of heat, light, moisture, oxygen contaminants or chemical contaminants, or reducing incompatibilities between the active substance and another material while processed or stored, or delaying, slowing or targeting the release of the active substance, or masking a flavor or an odor of the active substance. 10. A particulate coformulation according to claim 9, wherein the additive is a taste masking agent or an odor masking agent. 11. A particulate coformulation according to claim 1, wherein the active substance comprises a pharmaceutically active substance. 12. A particulate coformulation according to claim 11, wherein both the active substance and the additive comprise pharmaceutically active substances for co-administration. 13. A particulate coformulation according to claim 1, wherein the active substance is a carrier, diluent or bulking agent for the additive. 14. A particulate coformulation according to claim 1, wherein the active substance is present in a crystalline form and the additive is present in an amorphous form. 15. A particulate coformulation according to claim 14, wherein differential scanning calorimetry or X-ray diffraction analysis indicates an active substance crystallinity is less than an initial crystallinity of the active substance alone. 16. A particulate coformulation according to claim 15, wherein an active substance:additive concentration ratio is such that the active substance crystallinity is within a range from about 20% to about 95% as compared to the active substance alone. 17. A particulate coformulation according to claim 1, wherein the particles are the spherical or approximately spherical particles having a volume mean diameter of at least about 0.5 μm. 18. A particulate coformulation according to claim 1, wherein the active substance concentration is about 70% w/w or greater. 19. A particulate coformulation according claim 18, wherein the active substance concentration is about 80% w/w or greater. 20. A particulate coformulation according to claim 1, wherein the additive concentration is about 10% w/w or greater. 21. A pharmaceutical composition which includes a coformulation as in one of claims 1 to 20. 22. A foodstuff or nutriceutical composition which includes a coformulation as in one of claims 1 to 20. 23. The particulate coformulation of claim 1, wherein the particles are the spherical particles having a volume mean diameter within a range from about 0.5 μm to about 20 μm. 24. The particulate coformulation of claim 23, wherein the particles are the spherical particles having a volume mean diameter within a range from about 0.5 μm to about 10 μm. 25. The particulate coformulation of claim 1, wherein the particles are the spherical particles having a volume mean diameter of less than about 5 μm. 26. The particulate coformulation of claim 1, wherein the additive is a taste masking agent and the particles are the spherical particles having a volume mean diameter within a range from about 0.5 μ m to about 20 μm. 27. The particulate coformulation of claim 23, wherein the particles are the spherical particles having a volume mean diameter within a range from about 0.5 μm to about 10 μm. 28. The particulate coformulation of claim 1, wherein the additive is a taste masking agent and the particles are the spherical particles having a volume mean diameter of less than about 5 μm. 29. A particulate coformulation, comprising: an active substance and an additive contained within particulate formed from a co-precipitation process containing a supercritical fluid, wherein each particle contains a particle core having a first concentration by weight of the active substance within a range from about 90% to about 100%, a particle surface having a second concentration by weight of the active substance within a range from about 0% to about 5 %, an additive concentration having a finite gradient increasing radially from a center towards the particle surface and the particles are spherical or substantially spherical particles having a volume mean diameter of less than 100 μm. 30. A particulate coformulation, comprising: an active substance and a taste masking agent contained within particulate formed from a co-precipitation process containing a supercritical fluid, wherein each particle contains a particle core having a first concentration by weight of the active substance within a range from about 90% to about 100%, a particle surface having a second concentration by weight of the active substance within a range from about 0% to about 5%, an additive concentration having a finite gradient increasing radially from a center towards the particle surface and the particles are spherical or substantially spherical particles having a volume mean diameter of about 20 μm or less. 31. A particulate coformulation, comprising: an active substance and an additive contained within particulate formed from a co-precipitation process containing a supercritical fluid; and an additive concentration having a finite gradient increasing radially towards a particle surface of each particle within the particulate, wherein each particle contains a particle core having a first concentration by weight of the active substance within a range from about 90% to about 100% and the particle surface having a second concentration by weight of the active substance within a range from about 0% to about 5%. 32. The particulate coformulation of claim 31, wherein the particle surface is an additive-rich surface without a distinct physical boundary between the particle core and the particle surface. 33. The particulate coformulation of claim 31, wherein the additive concentration has a continuous rate of change across a radius of the particle. 34. The particulate coformulation of claim 31, wherein an active substance:additive ratio on the particle surface is sufficiently low to form a protective surface layer of the additive around the particle. 35. The particulate coformulation of claim 34, wherein the additive is a taste masking agent or an odor masking agent and the protective surface layer provides no detectable release of the active substance for at least 30 seconds after the coformulation comes into contact with saliva in a mouth of an individual. 36. The particulate coformulation of claim 34, wherein the particle surface contains no exposed active substance. 37. The particulate coformulation of claim 31, which comprises a pharmaceutical agent or a nutriceutical agent or a foodstuff. 38. The particulate coformulation of claim 31, wherein the additive is an oligomeric material or a polymeric material. 39. The particulate coformulation of claim 31, wherein the additive is a substance capable of protecting the active substance from at least one external effect selected from the group consisting of heat, light, moisture, oxygen contaminants and chemical contaminants. 40. The particulate coformulation of claim 31, wherein the additive is a substance capable of reducing incompatibilities between the active substance and another material during processing or storage. 41. The particulate coformulation of claim 31, wherein the additive is a substance capable of delaying, slowing or targeting release of the active substance. 42. The particulate coformulation of claim 31, wherein the additive is a taste masking agent or an odor masking agent. 43. The particulate coformulation of claim 31, wherein the active substance contains a pharmaceutically active substance. 44. The particulate coformulation of claim 43, wherein the additive contains another pharmaceutically active substance for co-administration. 45. The particulate coformulation of claim 31, wherein the active substance is a carrier, a diluent or a bulking agent for the additive. 46. The particulate coformulation of claim 31, wherein the active substance is in a crystalline state and the additive is in an amorphous state. 47. The particulate coformulation of claim 46, wherein a crystallinity of the active substance within the particulate is less than an initial crystallinity of the active substance alone. 48. The particulate coformulation of claim 47, wherein an active substance:additive concentration ratio is such that the crystallinity of the active substance is within a range from about 20% to about 95% as compared to the active substance alone. 49. The particulate coformulation of claim 31, wherein the particles are spherical or approximately spherical particles having a volume mean diameter within a range from about 0.5 μm to about 100 μ m. 50. The particulate coformulation of claim 31, wherein the particles are needle-like particles having a volume mean length within a range from about 5 μm to about 100 μm and a volume mean thickness within a range from about 0.5 μm to about 5 μm. 51. The particulate coformulation of claim 31, wherein the particles are plate-like particles having a volume mean thickness within a range from about 0.5 μm to about 5 μm. 52. The particulate coformulation of claim 31, wherein an active substance concentration is about 70% w/w or greater. 53. The particulate coformulation of claim 52, wherein the active substance concentration is about 80% w/w or greater. 54. The particulate coformulation of claim 31, wherein the additive concentration is about 10% w/w or greater. 55. The particulate coformulation of claim 49, wherein the volume mean diameter is within a range from about 0.5 μm to about 20 μm. 56. The particulate coformulation of claim 55, wherein the volume mean diameter is within a range from about 0.5 μm to about 10 μm. 57. The particulate coformulation of claim 31, wherein the volume mean diameter is about 5 μm or less. 58. The particulate coformulation of claim 31, wherein the additive is a taste masking agent and the particles are spherical particles having a volume mean diameter within a range from about 0.5 μ m to about 20 μm. 59. The particulate coformulation of claim 58, wherein the volume mean diameter is within a range from about 0.5 μm to about 10 μm. 60. The particulate coformulation of claim 31, wherein the additive is a taste masking agent and the particles are spherical particles having a volume mean diameter of about 5 μm or less.
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