This Non-provisional application claims priority under 35 U.S.C. §119(a) on Patent Application No(s). 098123693 filed in Taiwan, Republic of China on Jul. 14, 2009, the entire contents of which are hereby incorporated by reference.
1. Field of Invention
This invention related to a transportation device which transfers the material to cells by physical method.
2. Related Art
There are lots of ways to deliver bio-materials or medicines into cells even through skin, including using physical theorem, mechanical theorem or both of them. For instances, popular ways to administer bio-materials or medicines includes electroporation, microinjection, and the likes. But these physical injection ways are difficult to operate, and the stability and the rate of success are poor. Therefore, they are not widely used in this field. On the other hand, the research of gene guns reveals the potential for physical bio-materials or medicines transferring technique.
The method of using a gene gun is carrying the vectors (e.g. gold particles) of bio-materials (e.g. DNA) into cells by high-speed shooting for achieving gene transferring. And this technique is already extensively applied into many research fields which include plant system, cells of mammal, gene therapy, and the latest deoxyribonucleic acid (DNA) vaccine study systems as well.
For instance, the gene gun can carry gold particles mixed with DNA, put them on a cartridge, and generate seismic waves by using twinkling high-pressure stream so that the cartridge will accelerate until reaching an obstruction. Because the gold particles in the cartridge will keep moving in a high speed due to inertia, it will enter into cells. However, the drawback of this gene gun is too noisy, and the seismic waves could kill target cells easily. This gene gun also needs to consume a large amount of expensive helium and vectors (usually gold particles).
Besides, there is another way to provide medicine by a gene gun with low pressure vapor acceleration which carries the liquid (suspension liquid with nanometer particles) with DNA to be injected into a converging-diverging nozzle directly or indirectly, and then carries the liquid into human body through the spray nozzle by the instant low pressure vapor. Although this type of gene gun is able to overcome the existing bottleneck, however, as to the existing gene gun, before the sample entering the nozzle, it forms a turbulent flow so the sample may easily have collisions with the wall and be condensed on the wall surface. Additionally, the structure design of the nozzle itself has blind angle. At the same time, low-pressure gas provides the lower kinetic energy, which can not affect the residual sample on the wall to bring it out. For the low-pressure gas accelerating gene gun, its worst drawback is that the liquid is easy to remain in the nozzle which leads to the problems of quantitative and continuous operation.
Therefore, it is an important subjective to provide a transportation device to solve existing bottlenecks encountered.
In view of the foregoing, an objective of the present invention is to provide a transportation device having the physical design of drug delivery systems based on the fluid mechanics theory for delivering the mixed material and carrier fluid to a target.
To achieve the above objective, the present invention discloses a transportation device, which can physically transport a material to a target. The transportation device includes an input module, transmission module and an output module. The input module provides a carrier fluid. The transmission module is coupled to the input module for receiving the carrier fluid in order to disperse/atomize the material. The output module has a first opening, a second opening, and a throat portion positioned between the first and second openings. The aperture of the first opening is larger than that of the second opening. The distance between the throat portion and the second opening is equal to or smaller than the distance between the throat portion and the first opening, and is between three and ten times of the throat portion aperture (d). The second opening has an expending angle which is between half and three times of the throat portion aperture angle (½d°-3d°). The material enters the input module through the first opening and then reaches the target through the second opening. The input module further includes a guiding unit having a length longer than or equal to the distance between the throat portion and the second opening. One end of the guiding unit connects the transmission module, and the size of the end connected to the transmission module is three times larger than the size of the throat portion. The other end of the guiding unit has a guiding corner for connecting to the first opening, and the angle of the guiding corner is between three and fifteen times of the throat portion angle (3d°-15d°).
As mentioned above, the transportation device of the present invention may change the fluid (including: liquid, gas, gel, etc.) size by the atomizing unit. At the same time, through the mixing unit, the atomized material or the solid particles less than 500 microns can be mixed within the carrier fluid. With applying a certain pressure (e.g. 10 kg/cm2) in the output module, a very high-speed fluid can be generated, so that the carrier fluid and the material can be well mixed. At the same time, the temperature inside the output module may down to below zero in a fast moment, so the mixed two-phase samples can be accelerated to high speed and have instantaneous phase change (liquid to solid phase change, which includes ice crystals, ice needles, and the likes). After the solid material is transferred to the second opening, at least a part of the solid material has phase change from solid phase to liquid phase. The liquid phase material can help to reach the surface of the targets, and the solid phase material can make it easier to enter the target (e.g. enter cells through the biological or cell surfaces), thereby achieving the purpose of transmission. Compared with the prior art, this invention not only enhances the use of convenience of those liquid containing biological material (such as DNA, RNA, proteins, viruses, physical, chemical drugs, etc.) or solid state within 500 microns, but also can reduce the difficulty of coping and producing traditional carriers (gold grains) which could reduce the destruction to the biological material and injury to the target (for example: the target cell), and also improve the safety of using and reliable possibility. Moreover, the present invention can also control the amount of the material transferred into the target so as to enhance the dosage control.
The invention will become more fully understood from the detailed description and accompanying drawings, which are given for illustration only, and thus are not limitative of the present invention, and wherein:
The present invention will be apparent from the following detailed description, which proceeds with reference to the accompanying drawings, wherein the same references relate to the same elements.
For enhancing the convenience of using biological material samples and the control of the output, at the same time, to reduce the difficulty of preparing the traditional carriers, the destruction of biological material, and the damage to the target. Besides, to increase the use of the safety and reliability of possibility, this invention presents a transportation device. The text below provides a detailed description and schematic together to help understand the technical features of the present invention.
In addition, guiding unit 18 connects the first opening 161 of the output module 16 to the transmission module 14. In structural design, the opening aperture (diameter) D of the guiding unit 18 is larger than or equal to three times of the throat portion aperture d (D>3d). The length L3 of the guiding unit 18 is greater than or equal to the distance L1 between the second opening 162 and the throat 163 of the output module 16 (L3>L1). There is a guiding corner 181 configured in the conjunction of the guiding unit 18 and the output module 16. The angle A2 of the guiding corner 181 is approximately between three and fifteen times of the throat portion angle d° (3d°≦A2≦15d°). This design helps to promote the dynamic gas source (that is, carrier fluid) and the dispersed/atomized material (including non-solid particles or solid particles suspended) to have the interaction stability in the guiding unit 18. This is because there is a big gap mass density between the carrier fluid and material. Therefore, in the same pressure gradient, the acceleration (or deceleration) of the carrier fluid is more effect than the material. On the other hand, due to the configuration of the guiding corner 181, the two-phase (carrier fluid and material), after a stable interaction, can be guided by the guiding corner 181 and flow into the first opening 161 of the output module 16 without producing the residual on the wall of the guiding unit 18 due to the turbulence.
In addition, the transportation device 1 further includes a control module (not shown), which connects to the input module 12, transmission module 14 and output module 16. More specifically, the control module is electrically connected with all modules. The control module is to control the transfer rate and time of material and carrier fluid in the input module 12, transmission module 14 and output module 16. In this embodiment, the control module is a logic circuit, which controls the transfer rate and time of the carrier fluid in the input module 12, transmission module 14 and output module 16, thereby enhancing the dosage control of transferring the material to the target.
In this embodiment, the input module 12 includes a containing unit 123 (such as gas pressure storage tank) for storing the carrier fluid, and the logic circuit is to control the transfer rate and time of carrier fluid transferred in the input module 12, transmission module 14 and output module 16. More specifically, the input module 12 not only has one set or more containing units 123, but also includes at least one set of filter for filtering impurities in the carrier fluid. In this embodiment, the input module 12 include two sets of filters 121 and 122 (the degree of filtering down to 0.5 microns or less). The control module is composed of several mechanical or electronic control valves and high pressure pipelines. The purpose is to use the sophisticated electronic logic circuit to control various components of the containing unit 123 and the air loop sequence. In the containing unit 123, the power source for driving the gas is provided by the general air compressor, gas manufacture or added high-pressure gas cylinders.
For practical applications, the above-mentioned nozzle is based on the Laval Nozzle which uses very precise line geometry in order to design a converging-diverging channels, so that the flow rate of the carrier fluid can instant access to supersonic speed in the second opening 162, and take advantage of the speed of the carrier fluid to transfer its potential energy into kinetic energy and then make the carrier fluid to get instant access to rapid decline in temperature while flowing into the second opening 162. Moreover, the material may have phase change (e.g. phase change from liquid to solid) in the nozzle. After the solid material is transferred to the second opening 162, at least a part of the solid material has phase change from solid phase to liquid phase. The liquid phase material can help to reach the surface of the targets, and the solid phase material can make it easier to enter the target, thereby achieving the purpose of transmission.
The equations relates to the isentropic flow in the nozzle are briefly described hereinbelow:
Wherein, “exit” represents the second opening, “throat” represents the throat portion, M represents a Mach number, which is a ratio compared with the speed of sound, Mexit≧1, A represents the sectional area, P represents the pressure (P0 represents the pressure at the first opening), and γ represents the isentropic exponent. According to the equation (1), Athroat can be calculated by specifically selected Mach number and Aexit. According to the equation (2), Pexit is 1 atm (normal state), so that the pressure P0 of the first opening can be calculated. According to the equation (3), the pressure in the throat portion can be estimated based on the selected Mach number inside the throat portion. Consequently, the pressure values under different conditions can be obtained. To be noted, the design of the nozzle may be modified according to the actual conditions. In addition, the mass change of the material under various pressures at the throat portion can still be calculated according to the equation (4).
The temperature gradient of the output module 16 is as the curve shown in
In addition, in the contraction section of the nozzle, which is located between the first opening 161 and the throat portion 163, the pressure gradient is positive, the acceleration of the carrier fluid is larger than the material, and, therefore, the movement velocity of the carrier fluid will be higher than that of the material. On the contrary, in the expansion section of the nozzle, which is located between the throat portion 163 and the second opening 162, the pressure gradient is the opposite direction of the flow direction. The deceleration of the carrier fluid will enable the movement velocity of the carrier fluid less than the speed of the material. Especially when having waves in the expansion section of the throat portion 163, this deceleration will become more obvious.
Therefore, when designing the output module 16, the interaction between two fluids is considered so that the pressure and speed in the throat portion 163 can respectively reach the minimum and maximum values. When the carrier fluid in the flow field gradually accelerates to the critical state, the throat portion 163 will have choking phenomenon, and the pressure and the speed of two-phase mixture (including the carrier fluid and material) will no longer change before the throat portion 163. And when the carrier fluid flows through the throat portion 163 and enters the expansion section, the speed will still be increased instead of being decreased. It will reach its maximum, possibly over the supersonic state, at the downstream of the throat portion 163, so that the material can be dispersed/atomized into small-sized particles. Because, the dispersed/atomized material has the advantages of high speed and small size, it can penetrate through the surface of organisms or cells, and reaches the dermis or inside the cells. The transportation device of the invention can be applied to the transdermal therapeutic system, gene gun, nutrition supply device, cosmetic device, anti-aging device, etc.
The transmission module 14 will be different according to the phase of the input material, and the described material could be in solid-state, non-solid state or combination of both. The following will present a description by embodiments of the solid-state material and non-solid material.
Take a solid material (e.g. the powder of chemical compound) as an example first with reference to
To be noted, the mixing unit 141 not only can mix the solid-state material and the carrier fluid, but also can make these materials homogenously suspended in the carrier fluid, so that the solution of the solid-state material and carrier fluid can keep the suspension state in the mixing unit 141 without forming precipitation at the bottom of mixing unit 141 before outputting. The way to output the mixed solid-state material and carrier fluid from the mixing unit 141 can be carried out by mechanical or electronic control valve.
Alternatively, if the material is a non-solid-state material, such as a liquid or gel material, the transportation device of another embodiment is shown in
In addition, based on the liquid atomization mechanism of the twin-fluid atomizer 142b, the containers for storing the non-solid material can be divided into parallel type and vertical type.
To sum up, the transportation device of the present invention may change the fluid (including: liquid, gas, gel, etc.) size by the atomizing unit. At the same time, through the mixing unit, the atomized material or the solid particles less than 500 microns can be mixed within the carrier fluid. With applying a certain pressure (e.g. 10 kg/cm2) in the output module, a very high-speed fluid can be generated, so that the carrier fluid and the material can be well mixed. At the same time, the temperature inside the output module may down to below zero in a fast moment, so the mixed two-phase samples can be accelerated to high speed and have instantaneous phase change (liquid to solid phase change, which includes ice crystals, ice needles, and the likes). After the solid material is transferred to the second opening, at least a part of the solid material has phase change from solid phase to liquid phase. The liquid phase material can help to reach the surface of the targets, and the solid phase material can make it easier to enter the target (e.g. enter cells through the biological or cell surfaces), thereby achieving the purpose of transmission. Compared with the prior art, this invention not only enhances the use of convenience of those liquid containing biological material (such as DNA, RNA, proteins, viruses, physical, chemical drugs, etc.) or solid state within 500 microns, but also can reduce the difficulty of coping and producing traditional carriers (gold grains) which could reduce the destruction to the biological material and injury to the target (for example: the target cell), and also improve the safety of using and reliable possibility. Moreover, the present invention can also control the amount of the material transferred into the target so as to enhance the dosage control.
Although the invention has been described with reference to specific embodiments, this description is not meant to be construed in a limiting sense. Various modifications of the disclosed embodiments, as well as alternative embodiments, will be apparent to persons skilled in the art. It is, therefore, contemplated that the appended claims will cover all modifications that fall within the true scope of the invention.
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