Patent Grant
8182836
The invention relates to an abuse-resistant substance, such as an opioid-antagonist, oral dosage form which does not release the opioid antagonist in a therapeutically effective amount when the oral dosage form is orally administered to a human being, but whereby a physical alteration of the oral dosage form results in a release of the opioid antagonist in an amount effective to prevent the abuse. The oral dosage form can further include an abusable substance, such as an opioid agonist, in order to prevent the abuse of the opioid agonist. A preferred embodiment of the invention includes naltrexone as the abuse-resistant substance in an oral dosage form.
Opioid agonists, or opioids, are drugs which are used primarily as analgesics. Opioid agonists act on stereospecific receptor sites in the brain, as well as in other parts of the body, which presumably regulate the feeling and perception of pain. Examples of opioid agonists include, but are not limited to, oxycodone, morphine, hydrocodone and codeine. Although they are effective in reducing the perceived pain by a patient, opioid agonists also have the characteristic of possibly being physically and psychologically addictive to the patient if used repeatedly over an extended period of time. Thus, the potential for addiction to or abuse of such drugs is an issue of concern whenever prescribing such drugs as analgesics.
For example, oxycodone is an opioid agonist which has a high potential for abuse. Oxycodone is most often administered orally, and is commercially available in a controlled-released form known as Oxycontin™ (Purdue Pharma). However, the controlled release aspect of an Oxycontin™ dosage form can be bypassed by an abuser by, for example, crushing or grinding up the dosage form, and then eating or snorting the crushed or ground-up Oxycontin™ dosage form. Thus, in this way the abuser is able to receive a relatively large single dose of the oxycodone, resulting in a euphoric “high” being experienced by the abuser.
Opioid antagonists are those drugs which serve to neutralize or block the euphoric or analgesic effect of an opioid agonist. For example, opioid antagonists are often employed to block the euphoric or analgesic effects in individuals who have overdosed on an opioid agonist, or as a daily treatment drug in individuals who are addicted to an opioid agonist. It is thought that the opioid antagonists act on and compete for the same stereospecific receptor sites in the brain as the opioid agonists, and thereby neutralize or block the resulting-analgesic or euphoric effects of the opioid agonist.
Thus, there have been previous attempts in the prior art to produce formulations and methods concerned with reducing the abuse potential of opioid agonists. For example, U.S. Pat. No. 6,228,863 to Palermo et al. describes a method of preventing the abuse of opioid dosage forms by combining an orally active opioid agonist with an opioid antagonist into an oral dosage form which would require at least a two-step extraction process to separate the opioid antagonist from the opioid agonist. According to Palermo et al., the oral dosage forms described therein had less parenteral and/or oral abuse potential than that of the prior art oral dosage forms.
In addition, U.S. Pat. No. 6,277,384 to Kaiko et al. describes oral dosage forms including combinations of opioid agonists and opioid antagonists in ratios which are analgesically effective when administered orally, but which are aversive in a physically dependent individual. According to Kaiko et al., the oral dosage forms described therein had less oral abuse potential than that of the prior art oral dosage forms.
Furthermore, U.S. Pat. No. 5,236,714 to Lee et al. is directed to an abusable substance dosage form having a reduced abuse potential. Lee et al. disclose compositions and dosage forms for administering abusable substances wherein the therapeutic effect of the abusable substance will not be diminished, although the abuse potential of the abusable substance will be diminished. Specifically, topical compositions for application to a patient's skin or mucosa are disclosed including an abusable substance present in a form which is permeable to the skin or mucosa to which the composition is to be applied, and an antagonist present in a form which is impermeable to the skin or mucosa to which the composition is to be applied, such that if an attempt were made to abuse the composition by administering it through another bodily portal, the antagonist would prevent the occurrence of the abusive effect by producing its antagonistic effect. In addition, Lee et al. disclose dosage forms comprising a drug reservoir composition including an abusable substance and at least one antagonist enclosed within an abusable substance releasing means, wherein the abusable substance is present in a form which is permeable through the releasing means and the antagonist is present in a form which is impermeable to the releasing means. As with the topical composition, Lee et al. disclose that if an attempt were made to abuse the drug reservoir composition by removing it from the dosage form and administering it through another bodily portal, the antagonist would prevent the occurrence of the abusive effect by producing its antagonistic effect. The dosage forms of Lee et al. include a single abusable substance releasing means which controls the release of both the abusable substance and the antagonist.
However, there is still a need in the art for an improved oral dosage form of an opioid antagonist which would reduce the abuse potential of an opioid agonist.
An embodiment of the present invention is directed to an opioid-antagonist oral dosage form wherein the opioid antagonist does not release unless the oral dosage form is crushed or ground up, thereby antagonizing the opioid effect of an opioid agonist.
An embodiment of the oral dosage form of the present invention comprises: a biologically inert pellet; an opioid-antagonist layer coated on the biologically inert pellet, wherein the opioid-antagonist layer comprises a therapeutically effective amount of an opioid antagonist; and a non-releasing membrane coated on the opioid antagonist layer, wherein the non-releasing membrane comprises a water-retardant polymer and may contain a lubricant; wherein the oral dosage form does not release the therapeutically effective amount of the opioid antagonist when the oral dosage form is orally administered to a human being, and wherein a physical alteration of the oral dosage form results in a release of the therapeutically effective amount of the opioid antagonist.
In another embodiment of the invention, the oral dosage form can also include a second pellet comprising an opioid agonist, and/or other pain relievers and anti-inflammatory agents.
In a further embodiment of the invention, the oral dosage form comprises: an opioid-antagonist formulation, wherein the opioid-antagonist formulation comprises a therapeutically effective amount of an opioid antagonist; and a non-releasing membrane coated on the opioid-antagonist formulation, wherein the non-releasing membrane comprises a water-retardant polymer and may contain a lubricant; wherein the oral dosage form does not release the therapeutically effective amount of the opioid antagonist when the oral dosage form is orally administered to a human being, and wherein a physical alteration of the oral dosage form results in a release of the therapeutically effective amount of the opioid antagonist.
The invention is also directed to a method of preventing the abuse of an oral dosage form of an opioid agonist. An embodiment of the method of the invention includes the forming of an oral dosage form by combining: (1) a first type of pellet comprising an opioid agonist; and (2) a second type of pellet comprising: a biologically inert pellet; an opioid-antagonist layer coated on the biologically inert pellet, wherein the opioid-antagonist layer comprises a therapeutically effective amount of an opioid antagonist; and a non-releasing membrane coated on the opioid antagonist layer, wherein the non-releasing membrane comprises a water-retardant polymer. The oral dosage form does not release the therapeutically effective amount of the opioid antagonist when the oral dosage form is orally administered to a human being, and a physical alteration of the oral dosage form results in a release of the therapeutically effective amount of the opioid antagonist.
Another embodiment of the method of the invention includes coating a non-releasing membrane onto an opioid-antagonist formulation, and coating an opioid-agonist layer onto the non-releasing membrane to form an oral dosage form, wherein the opioid-antagonist formulation comprises a therapeutically effective amount of an opioid antagonist, the non-releasing membrane comprises a water-retardant polymer, and the opioid-agonist layer comprises an opioid agonist. The oral dosage form does not release the therapeutically effective amount of the opioid antagonist when the oral dosage form is orally administered to a human being, and a physical alteration of the oral dosage form results in a release of the therapeutically effective amount of the opioid antagonist.
In addition, a further embodiment of the method of the invention also includes adding other pain relievers and/or anti-inflammatory agents when forming the oral dosage form.
The present invention, as disclosed and described herein, provides a novel oral dosage form of a therapeutically effective amount of an opioid antagonist which does not release when orally administered to a human being, but which does release upon a physical alteration of the oral dosage form. That is, if the oral dosage form of the invention is orally administered to a human being, then the therapeutically effective amount of the opioid antagonist is not released from the oral dosage form, and thus an opioid agonist will have its intended analgesic effect on the human being. As used herein, the phrase “a therapeutically effective amount of an opioid antagonist” refers to that amount of the opioid antagonist which is sufficient to antagonize the opioid agonist and thus effectively neutralize the intended analgesic effect of the opioid agonist. Thus, when orally administered to a human being, although the oral dosage form of the invention may release a negligible or inconsequential amount of the opioid antagonist, it will not release an amount to antagonize the opioid agonist and to neutralize its intended analgesic effect.
However, if the oral dosage form of the invention is physically altered in any way, such as by crushing or grinding of the oral dosage form, then the therapeutically effective amount of the opioid antagonist will be released. That is, as the non-releasing membrane of the oral dosage form is rendered ineffective by physical alteration, the opioid antagonist will no longer be effectively coated by the non-releasing membrane and the therapeutically effective amount of the opioid antagonist will thereby be released. Therefore, the opioid agonist will be antagonized by the opioid antagonist and the intended analgesic effect of the opioid agonist will be effectively neutralized, reduced or blocked. Thus, if an individual were to crush and grind up the oral dosage form of the present invention in an attempt to take it parenterally, or orally, or by snorting it through the nose, in order to obtain a euphoric “high,” a sufficient amount of the opioid antagonist would thereby be released to antagonize the opioid agonist and to neutralize or block its intended euphoric, analgesic effect.
Depending upon the specific opioid antagonist(s) present in the embodiment of the oral dosage form of the present invention, the dose of the opioid antagonist(s) will vary. For example, a single 50 mg dose of naltrexone is generally sufficient to block the analgesic effect of an opioid agonist. See, e.g., U.S. Pat. Nos. 6,228,863 and 6,277,384. The dosage amount of any of the opioid antagonists which can be used in accordance with the invention can readily be determined by one of ordinary skill in the art. As mentioned above, the dosage amount of the opioid antagonist will be at least that amount of the opioid antagonist which is sufficient to antagonize the opioid agonist and thus effectively neutralize the intended analgesic effect of the opioid agonist.
The invention provides an oral dosage form which does not release a therapeutically effective amount of an opioid antagonist when the oral dosage form is orally administered to a human being. That is, the oral dosage form of the invention is designed such that when orally administered to a human being, it would not provide effective blood levels of the opioid antagonist for up to about twenty-four (24) hours and beyond, at which time the opioid agonist would have previously been released and would have had its intended analgesic effect on the human being.
According to an embodiment of the invention, the oral dosage form includes a biologically inert pellet (core) coated first by an opioid-antagonist layer, which is then coated by a non-releasing membrane. Many types of inert pellets are suitable for use in forming the core of this embodiment of the oral dosage form, and are commercially available from a number of companies; for example, non-pareils, sugar and/or starch-based pellets are all suitable types of pellets. Sugar spheres of particle size 25 to 30 mesh are particularly preferred, although any inert pellets of mesh size within the range of 14 mesh to 60 mesh are also preferred for use in this invention. In addition, other substrates, including but not limited to, granules, spheroids and beads, may be used in accordance with this embodiment of the invention.
In this embodiment of the invention, an opioid-antagonist layer coats the biologically inert pellet of the oral dosage form. The opioid-antagonist layer comprises a therapeutically effective amount of an opioid antagonist. Any opioid antagonist, or a pharmaceutically acceptable salt thereof, or combinations thereof, may be used in accordance with the invention. Examples of a suitable opioid antagonist, include but are not limited to, naltrexone, naloxone, and nalmephene. Preferably, the opioid antagonist comprises naltrexone.
The opioid-antagonist layer may also include a binder agent to enhance its adherence to the biologically inert pellet. Suitable binder agents for use in the opioid-antagonist layer of the invention include, but are not limited to, hydroxypropylmethyl cellulose (HPMC) (3 to 6 cps, preferably 6 cps), hydroxyethyl cellulose, hydroxypropyl cellulose, methyl cellulose, polyvinyl pyrrolidone and the like. Preferably, hydroxypropylmethyl cellulose, and most preferably, hydroxypropylmethyl cellulose E6 or Opadry® clear is used in accordance with the invention. Preferably, the binder agent is dissolved in water (or any suitable solvent) to form a 5% to 30% (w/w) solution, preferably a 7% to 25% (w/w) solution and most preferably, an approximately 10% (w/w) solution. The solution of binder agent is admixed with a solution or suspension of the opioid antagonist, and then applied onto the biologically inert pellets by conventional spray techniques. For example, the opioid antagonists/binder agent solution or suspension may be applied to the biologically inert pellets by spraying the solution or suspension onto the pellets using a fluid bed processor. Preferably, the amount of binder agent included in the opioid-antagonist layer is in a ratio of binder agent to opioid-antagonist of about 1:10, although any ratio is suitable for use with the present invention.
The opioid-antagonist layer of this embodiment of the oral dosage form of the present invention may also include one or more pharmaceutically acceptable excipients in addition to the opioid antagonist and the optional binder agent. Suitable pharmaceutically acceptable excipients which may be employed in the invention are well known to those of ordinary skill in the art and include any conventional pharmaceutically acceptable excipient, such as an antifoam agent, which is added to aid the formulation process. The opioid-antagonist layer may also include a suitable carrier, diluent, surfactant and/or lubricant.
In another embodiment of the invention, the opioid-antagonist layer is coated with an optional sealing layer. The sealing layer contains a water soluble polymer, which may be the same or different from the binder agent present in the opioid-antagonist layer. For example, the sealing layer may include a water soluble polymer such as hydroxypropylmethyl cellulose (3 to 6 cps, preferably 6 cps), hydroxyethyl cellulose, hydroxypropyl cellulose, methyl cellulose, polyvinylpyrrolidone and the like. Preferably, hydroxypropylmethyl cellulose, and most preferably, hydroxypropylmethyl cellulose-E-6 is employed in the sealing layer. In addition, the sealing layer may optionally contain a lubricant, such as for example, calcium stearate, magnesium stearate, zinc stearate, stearic acid, talc or a combination thereof. The total amount of this optional sealing layer contained in the finally coated pellets is preferably about 0.5% to about 5% of the total weight of the finally coated pellet.
In a further embodiment of the invention, the oral dosage form includes an opioid-antagonist formulation comprising a therapeutically effective amount of an opioid antagonist, which is then coated by a non-releasing membrane. In this embodiment of the invention, the opioid-antagonist formulation may be produced by any method known in the art, including but not limited to, forming a matrix system of the opioid antagonist which would then be compressed into a tablet. Furthermore, the opioid-antagonist formulation may be provided in any form known in the art, including but not limited to, pellets, granules, spheroids, capsules and tablets. As would be understood by one of ordinary skill in the art, such an opioid-antagonist formulation could further include, for example, binder agents, diluents, carriers, fillers, lubricants and other pharmaceutically acceptable additives and excipients which are used in the formation of the particular form of the formulation, and all such opioid-antagonist formulations are within the scope of the present invention. In further embodiments of the invention, the opioid-antagonist formulation may be coated with an optional sealing layer prior to coating with the non-releasing membrane.
According to the present invention, the oral dosage form also includes a non-releasing membrane which is coated onto the opioid-antagonist layer, the opioid-antagonist formulation, or the optional sealing layer, depending upon the particular embodiment of the oral dosage form. The non-releasing membrane serves to protect the integrity of the biologically inert pellets coated with the opioid-antagonist layer, or the opioid-antagonist formulation, such that the therapeutically effective amount of the opioid antagonist is not released from the oral dosage form when it is orally administered to a human being. At the same time however, if the oral dosage form is physically altered and the non-releasing membrane is rendered ineffective, then the therapeutically effective amount of the opioid antagonist is thereby released from the oral dosage form.
The non-releasing membrane of the invention comprises a water-retardant polymer, such as, for example, an alkyl cellulose, an acrylic acid polymer, an acrylic acid copolymer, a methacrylic acid polymer, a methacrylic acid copolymer, shellac, zein, or hydrogenated vegetable oil. The water-retardant polymer is physiologically acceptable, and it substantially prevents the release of the opioid antagonist. In addition, the water-retardant polymer could optionally be water insoluble. A preferred water-retardant polymer is a poly(meth)acrylate polymer, such as Eudragit NE 30 D or Eudragit NE 40 D, or a combination thereof. Most preferably, the water-retardant polymer comprises the poly(meth)acrylate polymer, Eudragit NE 30 D. Eudragit NE 30 D and Eudragit NE 40 D polymers are available from Rhom Pharma, D-6108 Weiterstadt 1, Dr. Otto-Rohm-Str. 2-4, Germany. Eudragit NE 30 D and Eudragit NE 40 D are pH independent polymers available as 30% or 40% aqueous dispersions, respectively. Furthermore, Eudragit RS 30 D, Eudragit RL 30 D, Eudragit S and Eudragit L 30 D are further examples of suitable water-retardant polymers. When employing Eudragit NE 30 D as the water-retardant polymer, the NE30D solids in the non-releasing membrane generally constitute about 15% to about 80% of the total weight of the solids content of the final oral dosage form, preferably about 25% to about 60%, and most preferably about 30% to about 50% of the total weight of the solids content of the final oral dosage form.
In a preferred embodiment of the present invention, the non-releasing membrane contains in addition to a water-retardant polymer, an amount of a lubricant, such as for example, calcium stearate, magnesium stearate, zinc stearate, stearic acid, talc or a combination thereof, to form the non-releasing membrane. In particular, it is preferred that the non-releasing membrane contains an amount of magnesium stearate, or other lubricant, sufficient to provide non-release of the opioid antagonist for up to about 14-24 hours after administration of the dosage form to a human being. In a most preferred embodiment, the non-releasing membrane contains magnesium stearate admixed with the water-retardant polymer, which is preferably Eudragit NE30D. In embodiments of the invention including opioid-antagonist-coated pellets, the lubricant functions to prevent agglomeration of the opioid-antagonist-coated pellets during processing and also helps to prevent release of the opioid antagonist from the opioid-antagonist-coated pellets. Preferably, the final, dried non-releasing membrane contains about 5% to about 50% magnesium stearate and/or other lubricant(s), and more preferably about 7% to about 30%, and most preferably about 10% to about 25% lubricant(s) based on the total weight of solids content of the total formulation.
In another embodiment of the invention, the non-releasing membrane is coated with an optional sealing layer. This optional sealing layer is similar to the previously described optional sealing layer between, for example, the opioid-antagonist layer and the non-releasing membrane, and in fact may be comprised of the same exact elements. Thus, the sealing layer contains a water soluble polymer, which may be the same or different from the binder agent present in the opioid-antagonist layer. For example, the sealing layer may include a water soluble polymer such as hydroxypropylmethyl cellulose (3 to 6 cps, preferably 6 cps), hydroxyethyl cellulose, hydroxypropyl cellulose, methyl cellulose, polyvinylpyrrolidone and the like. Preferably, hydroxypropylmethyl cellulose, and most preferably, hydroxypropylmethyl cellulose-E-6 is employed in the sealing layer. In addition, the sealing layer may optionally contain a lubricant, such as for example, calcium stearate, magnesium stearate, zinc stearate, stearic acid, talc or a combination thereof. In embodiments of the invention employing pellets, the total amount of this optional sealing layer contained in the finally coated pellets is preferably about 0.5% to about 10% of the total weight of the finally coated pellet. In further embodiments of the invention, the optional sealing layer may also be coated with an enteric layer.
In a further embodiment of the invention, the non-releasing membrane is coated with an enteric layer comprising an enteric coating polymer, and optionally comprising a plasticizer. A preferred enteric coating polymer is Eudragit L 30D. Suitable plasticizers for inclusion in the enteric layer include, for example, triethyl citrate, polyethylene glycol, dibutyl phthalate, diethylphthalate and triacetin. In embodiments of the invention employing pellets, the optional enteric layer, which is pH dependant and resistant to gastric fluids, preferably comprises from about 0.5% to about 10% of the total weight of the finally coated pellet. In further embodiments of the invention, the enteric layer may also be coated with a sealing layer.
In another embodiment of the invention, the non-releasing membrane (optionally coated with an enteric layer and/or a sealing layer) is coated with an opioid-agonist layer comprising an opioid agonist. Any opioid agonist, or a pharmaceutically acceptable salt thereof, may be used in accordance with the invention. Examples of the opioid agonist which may be included in this embodiment of the invention include, but are not limited to, oxycodone, hydrocodone, morphine, hydromorphone, codeine, and mixtures thereof. Preferably, the opioid agonist comprises oxycodone. In further embodiments of the invention, the opioid-agonist layer may also be coated with a sealing layer and/or an enteric layer.
In the present invention, the opioid agonist is preferably present in an amount which will provide for effective blood levels of the opioid agonist in a human being. That is, when the oral dosage form of the invention is orally administered to a human being, the opioid agonist will be released from the oral dosage form, and it can thus have its intended analgesic effect upon the human being. This is because, as described above, upon oral administration of the oral dosage form of the invention, the opioid antagonist will not be sufficiently released from the oral dosage form, thereby enabling the opioid agonist to have its intended analgesic effect. At the same time, however, if the oral dosage form of the invention is physically altered in any way, such as by grinding or crushing, then the therapeutically effective amount of the opioid antagonist will be released from the oral dosage form, thereby antagonizing the opioid agonist and thus effectively neutralizing the intended analgesic effect of the opioid agonist. Thus, the formation of the oral dosage form of the invention is an effective method of preventing the abuse of an oral dosage form of an opioid agonist. For example, if an individual were to crush and grind up the oral dosage form of the present invention in an attempt to take it parenterally, orally, or by snorting it through the nose, in order to obtain a euphoric “high”, a sufficient amount of the opioid antagonist would thereby be released to antagonize the opioid agonist and to neutralize or block its intended euphoric, analgesic effect.
In addition, the opioid-agonist layer of this embodiment may further include, for example, binder agents, diluents, carriers, fillers, lubricants and other pharmaceutically acceptable additives and excipients which may or may not effect the rate of release of the opioid agonist from the oral dosage form of this embodiment. Thus, any type of release profile known in the art, including but not limited to, immediate and sustained release formulations, may be used in accordance with the opioid-agonist layer of this embodiment.
The opioid-antagonist layer, the opioid-antagonist formulation, and/or the non-releasing membrane of the invention may each further comprise diluents, carriers, fillers and other pharmaceutical additives which may or may not effect the rate of release of the opioid antagonist from the oral dosage form of the invention. For example, the non-releasing membrane preferably contains a lubricant and the opioid-antagonist layer may optionally contain a surfactant. The opioid-antagonist layer, the opioid-antagonist formulation, and/or the non-releasing membrane may also further contain pharmaceutically acceptable excipients such as anti-adherents, and pharmaceutically acceptable pigments such as titanium dioxide, iron oxide and various color pigments including vegetable dyes, and the like.
In embodiments of the invention employing pellets, the opioid-antagonist loaded pellets preferably provide in total a potency of about 6% to about 70% (w/w) based upon the total weight of the layered pellets, although the potency can be adjusted as desired. For example, when the opioid antagonist employed in the invention is naltrexone, it is preferred that the layered pellets be formulated at about 60% potency (w/w). However, the skilled practitioner can formulate the oral dosage forms of the invention to have any desired total potency of opioid antagonist.
The non-release, oral dosage form of the invention, as disclosed herein, is designed such that it does not provide for effective blood levels of the opioid antagonist for at least 24 hours after oral administration of the oral dosage form. In addition, the non-release, oral dosage form provides a dissolution rate of the opioid antagonist, when measured in vitro by the U.S. Pharmacopeia XXVI basket method of 100 rpm in 900 ml of water at 37° C., wherein the therapeutically effective amount of the opioid antagonist is not released from the dosage form after about 14 to 24 hours.
The process for making an embodiment of the oral dosage form of the invention includes coating at least one layer of an opioid antagonist onto the surface of a biologically inert pellet (e.g., a non-pareil pellet (sugar and/or starch-based pellets)) to form opioid-antagonist loaded pellets. The opioid-antagonist loaded pellets are then coated with a non-releasing membrane.
In preparing an embodiment of the oral dosage form of the invention, the opioid-antagonist layer may be applied by spraying the opioid-antagonist suspension onto sugar spheres or other biologically inert pellets that have been suspended in a fluidized bed, for example. Other conventional spray techniques such as pan coating may also be used. The opioid-antagonist loaded pellets can also be prepared by an extruder/marumerizer. After the sugar spheres or pellets are coated with the opioid-antagonist layer, they may optionally be dried by air exposure, or other methods known in the art (although drying may occur spontaneously from air flow in the fluid bed processor).
In this embodiment, the non-releasing membrane including the water-retardant polymer is next coated onto the opioid-antagonist loaded pellets. The water-retardant polymer comprising the non-releasing membrane is generally prepared as a dispersion and sprayed onto the opioid-antagonist loaded pellets. The total amount of water-retardant polymer in the pellets is in the range of from about 15% to about 80% of the total weight of the prepared pellets, preferably about 30% to about 55% of the total weight of the prepared pellets. By varying the amount of water-retardant polymer within this range, the desired non-release of the opioid antagonist is achieved.
At the final stage in preparing this embodiment, the coated pellets may optionally be subjected to a curing process. For example, the coated pellets may be cured at a temperature in the range of from about 30° to about 50° C., preferably from about 35° to about 45° C., and most preferably about 40° C., for a period of about 5 to about 10 days and, preferably, about 7 days. A further example of a suitable curing process could be performed in a fluid bed processor for about 1 to about 5 hours at about 40° to about 80° C., preferably for about 3 hours at about 55° to about 65° C., and most preferably for about 1 hour at about 60° C.
The coated pellets may then be weighed out according to the total dose of opioid antagonist to be administered to patients. Diluent may be added, such as, for example, dextrose, sorbitol, mannitol, microcrystalline cellulose, methocel ether, lactose, glyceryl palmitostearate, glyceryl stearate, glyceryl behenate, and combinations thereof, among other commonly used pharmaceutical diluents, and the mixture of coated pellets and diluents pressed into tablets. Alternatively, the coated pellets, with or without diluents, can be encapsulated in a capsule, such as a hard gelatin capsule. Furthermore, in an embodiment of the invention, the opioid agonist(s) can also be added to a tablet or capsule containing the opioid-antagonist loaded pellets.
It is often desirable to add inert diluent when formulating the coated pellets into tablet form. The presence of pharmaceutical diluents, such as microcrystalline cellulose, methocel ether, glyceryl palmitostearate, glyceryl stearate, and/or glyceryl behemate, for example, in the coated pellet mixture serves to cushion the pellets so that they are not significantly ruptured during compression. In addition, pharmaceutical diluents can be added to enhance the non-releasing property of the oral dosage form of the present invention.
In general, the release rate of opioid antagonist from the coated pellets is dependent upon a number of factors including, inter alia, the overall structure and design of the coated pellet, the potency of the coated pellet, the type and amount of water-retardant polymer present in the non-releasing membrane, and when present in the coated pellets, the type and amount of lubricant. The coated pellets may be formulated into tablets or encapsulated in the desired dosage amount. Typical unit dosage amounts for the opioid antagonist of the oral dosage form of the invention include any dosage between about 1 and 200 mg, although dosages outside of this range may also be employed in the present invention.
In another embodiment of the oral dosage form of the invention, in addition to the coated pellets described above which are coated with an opioid antagonist, the oral dosage form may include an opioid-agonist formulation including an opioid agonist. The opioid-agonist formulation may be produced by any method known in the art, including the method described above wherein pellets are coated by use of a fluid bed processor. In addition, the opioid-agonist formulation may be provided in any form known in the art, including but not limited to, pellets, granules, spheroids, capsules and tablets, with any type of release profile, including but not limited to, immediate and sustained release formulations. Any opioid agonist, combinations thereof, or a pharmaceutically acceptable salt thereof, may be used in accordance with the invention. Examples of the opioid agonist which may be included in the oral dosage form of the invention include, but are not limited to, oxycodone, hydrocodone, morphine, hydromorphone, codeine, and mixtures thereof. Preferably, the opioid agonist comprises oxycodone.
In this embodiment of the invention, the opioid agonist is preferably present in an amount which will provide for effective blood levels of the opioid agonist in a human being. That is, when this embodiment of the oral dosage form of the invention is orally administered to a human being, the opioid agonist will be released from the oral dosage form, and it can thus have its intended analgesic effect upon the human being. This is because, as described above, upon oral administration of the oral dosage form of the invention, the opioid antagonist will not be sufficiently released from the oral dosage form, thereby enabling the opioid agonist to have its intended analgesic effect. At the same time, however, if this embodiment of the oral dosage form of the invention is physically altered in any way, such as by grinding or crushing, then the therapeutically effective amount of the opioid antagonist will be released from the oral dosage form, thereby antagonizing the opioid agonist and thus effectively neutralizing the intended analgesic effect of the opioid agonist. Thus, the formation of the oral dosage form of this embodiment is an effective method of preventing the abuse of an oral dosage form of an opioid agonist. For example, if an individual were to crush and grind up the oral dosage form of the present invention in an attempt to take it parenterally, orally, or by snorting it through the nose, in order to obtain a euphoric “high”, a sufficient amount of the opioid antagonist would thereby be released to antagonize the opioid agonist and to neutralize or block its intended euphoric, analgesic effect.
The following examples are illustrative of the invention, and are not to be construed as limiting the invention in any way.
In these examples, embodiments of the oral dosage form of the invention were prepared as follows.
Step 1: Applying an Opioid Antagonist Layer to a Biologically Inert Pellet
An opioid-antagonist suspension was prepared by mixing the methocel E6 10% solution (binder agent), the naltrexone hydrochloride (opioid antagonist), the simethicone 30% emulsion (antifoam agent) and the purified water (in the amounts listed above for each example). This opioid-antagonist suspension was then sprayed onto the 25/30 mesh sugar spheres using a fluid bed processor, resulting in biologically inert pellets coated with an opioid-antagonist layer. In Example 1, these coated pellets have a naltrexone (opioid antagonist) potency of 6.2%, and in Example 2, these coated pellets have a naltrexone (opioid antagonist) potency of 53%.
Step 2: Applying a Non-Releasing Membrane to the Coated Pellets of Example 1 from Step 1
Next, the Eudragit NE 30D 30% dispersion and the magnesium stearate 15% suspension (in the amounts listed above) were added together and mixed to form a non-releasing suspension. This non-releasing suspension was then sprayed onto 650 grams of the coated pellets of Example 1 from step 1 using a fluid bed processor. These twice-coated pellets were then cured in the fluid bed processor for about 6 hours at 60° C.
Step 3: Filling into Capsules
The coated pellets from step 2 were then filled into capsules to give an effective dose of 50 mg naltrexone hydrochloride.
Step 4: In-Vitro Dissolution Testing
Dissolution testing was then performed on the capsules prepared in step 3 as described above. In this example, the Eudragit NE 30D solids coating constituted 42.48% of the final formulation (i.e., the capsule), and the total solids coating constituted 59% of the final formulation (i.e., the capsule). As used herein, the “total solids coating” refers to the Eudragit NE 30D and the magnesium stearate, as described above in step 2. The conditions for testing were those of the USP Basket Method of 100 rpm in 900 ml of de-ionized water at 37° C., with the results shown below in Table 1. A graph of these in vitro dissolution testing results can be seen in
As can be seen from Table 1 above, in this embodiment of the oral dosage form of the invention, the therapeutically effective amount of the naltrexone is still not released from the dosage form after about 14 to 24 hours, as only 5.7% of the naltrexone has been released from the dosage form after about 24 hours. Thus, in this example, 5.7% of the 50 mg naltrexone (i.e., about 2.85 mg) has been released after about 24 hours, which is insufficient to block or neutralize the intended analgesic effect of an opioid agonist.
It should be understood that some modification, alteration and substitution is anticipated and expected from those skilled in the art without departing from the teachings of the invention. Accordingly, it is appropriate that the following claims be construed broadly and in a manner consistent with the scope and spirit of the invention.
This application is a continuation application of U.S. patent application Ser. No. 10/409,992 filed Apr. 8, 2003, the content of which is herein incorporated by reference in its entirety.
| Number | Name | Date | Kind |
|---|---|---|---|
| 2770569 | Fromherz et al. | Nov 1956 | A |
| 3332950 | Blumberg et al. | Jul 1967 | A |
| 3493657 | Lewenstein et al. | Feb 1970 | A |
| 3676557 | Lachman et al. | Jul 1972 | A |
| 3773955 | Pachter et al. | Nov 1973 | A |
| 3879555 | Pachter et al. | Apr 1975 | A |
| 3965256 | Leslie | Jun 1976 | A |
| 3966940 | Pachter et al. | Jun 1976 | A |
| 4176186 | Goldberg | Nov 1979 | A |
| 4237140 | Dudzinski | Dec 1980 | A |
| 4366310 | Leslie | Dec 1982 | A |
| 4401672 | Portoghese et al. | Aug 1983 | A |
| 4443428 | Oshlack et al. | Apr 1984 | A |
| 4451470 | Ganti | May 1984 | A |
| 4457933 | Gordon et al. | Jul 1984 | A |
| 4464378 | Hussain et al. | Aug 1984 | A |
| 4469827 | Pusineri et al. | Sep 1984 | A |
| 4573995 | Chen et al. | Mar 1986 | A |
| 4582835 | Lewis et al. | Apr 1986 | A |
| 4608376 | Pasternak | Aug 1986 | A |
| 4661492 | Lewis et al. | Apr 1987 | A |
| 4668685 | Shami | May 1987 | A |
| 4719215 | Goldberg | Jan 1988 | A |
| 4722928 | Boswell et al. | Feb 1988 | A |
| 4730048 | Portoghese et al. | Mar 1988 | A |
| 4760069 | Rzeszotarski et al. | Jul 1988 | A |
| 4769372 | Kreek et al. | Sep 1988 | A |
| 4774230 | Tuttle et al. | Sep 1988 | A |
| 4785000 | Kreek et al. | Nov 1988 | A |
| 4803208 | Pasternak | Feb 1989 | A |
| 4806341 | Chien et al. | Feb 1989 | A |
| 4806543 | Choi | Feb 1989 | A |
| 4806558 | Wuest et al. | Feb 1989 | A |
| 4828836 | Elger et al. | May 1989 | A |
| 4834965 | Martani et al. | May 1989 | A |
| 4834984 | Goldie et al. | May 1989 | A |
| 4834985 | Elger et al. | May 1989 | A |
| 4844907 | Elger et al. | Jul 1989 | A |
| 4844909 | Goldie et al. | Jul 1989 | A |
| 4844910 | Leslie et al. | Jul 1989 | A |
| 4861598 | Oshlack et al. | Aug 1989 | A |
| 4861781 | Goldberg | Aug 1989 | A |
| 4867985 | Heafield et al. | Sep 1989 | A |
| 4873076 | Fishman et al. | Oct 1989 | A |
| 4882335 | Sinclair | Nov 1989 | A |
| 4889860 | Rzeszotarski et al. | Dec 1989 | A |
| 4935428 | Lewis | Jun 1990 | A |
| 4940587 | Jenkins et al. | Jul 1990 | A |
| 4970075 | Oshlack | Nov 1990 | A |
| 4987136 | Kreek et al. | Jan 1991 | A |
| 4990341 | Goldie et al. | Feb 1991 | A |
| 5071646 | Malkowska et al. | Dec 1991 | A |
| 5075341 | Mendelson et al. | Dec 1991 | A |
| 5086058 | Sinclair et al. | Feb 1992 | A |
| 5091189 | Heafield et al. | Feb 1992 | A |
| 5096715 | Sinclair | Mar 1992 | A |
| 5102887 | Goldberg | Apr 1992 | A |
| 5122127 | Stanley | Jun 1992 | A |
| 5149538 | Granger et al. | Sep 1992 | A |
| 5215758 | Krishnamurthy | Jun 1993 | A |
| 5225440 | London et al. | Jul 1993 | A |
| 5226331 | Thompson et al. | Jul 1993 | A |
| 5228497 | Romanowski | Jul 1993 | A |
| 5236714 | Lee et al. | Aug 1993 | A |
| 5256669 | Askanazi et al. | Oct 1993 | A |
| 5273760 | Oshlack et al. | Dec 1993 | A |
| 5286493 | Oshlack et al. | Feb 1994 | A |
| 5288498 | Stanley et al. | Feb 1994 | A |
| 5316759 | Rose et al. | May 1994 | A |
| 5317022 | Borsodi et al. | May 1994 | A |
| 5321012 | Mayer et al. | Jun 1994 | A |
| 5324351 | Oshlack et al. | Jun 1994 | A |
| 5336691 | Raffa et al. | Aug 1994 | A |
| 5352680 | Portoghese et al. | Oct 1994 | A |
| 5352683 | Mayer et al. | Oct 1994 | A |
| 5356467 | Oshlack et al. | Oct 1994 | A |
| 5356900 | Bihari et al. | Oct 1994 | A |
| 5376662 | Ockert | Dec 1994 | A |
| 5411745 | Oshlack et al. | May 1995 | A |
| 5411965 | Reid et al. | May 1995 | A |
| 5426112 | Zagon et al. | Jun 1995 | A |
| 5457208 | Portoghese et al. | Oct 1995 | A |
| 5460826 | Merrill et al. | Oct 1995 | A |
| 5464841 | Portoghese et al. | Nov 1995 | A |
| 5472712 | Oshlack et al. | Dec 1995 | A |
| 5472943 | Crain et al. | Dec 1995 | A |
| 5478577 | Sackler et al. | Dec 1995 | A |
| 5486362 | Kitchell et al. | Jan 1996 | A |
| 5500227 | Oshlack et al. | Mar 1996 | A |
| 5502058 | Mayer et al. | Mar 1996 | A |
| 5506257 | MacLeod et al. | Apr 1996 | A |
| 5508042 | Oshlack et al. | Apr 1996 | A |
| 5508043 | Krishnamurthy | Apr 1996 | A |
| 5512578 | Crain et al. | Apr 1996 | A |
| 5514680 | Weber et al. | May 1996 | A |
| 5534492 | Aston et al. | Jul 1996 | A |
| 5549912 | Oshlack et al. | Aug 1996 | A |
| 5552422 | Gauthier et al. | Sep 1996 | A |
| 5556838 | Mayer et al. | Sep 1996 | A |
| 5574052 | Rose et al. | Nov 1996 | A |
| 5578725 | Portoghese et al. | Nov 1996 | A |
| 5580578 | Oshlack et al. | Dec 1996 | A |
| 5580876 | Crain et al. | Dec 1996 | A |
| 5585348 | Crain et al. | Dec 1996 | A |
| 5591452 | Miller et al. | Jan 1997 | A |
| 5601845 | Buxton et al. | Feb 1997 | A |
| 5616601 | Khanna et al. | Apr 1997 | A |
| 5622722 | Knott et al. | Apr 1997 | A |
| 5624932 | Qin et al. | Apr 1997 | A |
| 5631263 | Portoghese et al. | May 1997 | A |
| 5633259 | Qin et al. | May 1997 | A |
| 5639476 | Oshlack et al. | Jun 1997 | A |
| 5656295 | Oshlack et al. | Aug 1997 | A |
| 5670172 | Buxton et al. | Sep 1997 | A |
| 5672360 | Sackler et al. | Sep 1997 | A |
| 5681585 | Oshlack et al. | Oct 1997 | A |
| 5709883 | Drizen et al. | Jan 1998 | A |
| 5732717 | Watanabe et al. | Mar 1998 | A |
| 5763452 | Miller et al. | Jun 1998 | A |
| 5767125 | Crain et al. | Jun 1998 | A |
| 5780479 | Kim | Jul 1998 | A |
| 5785989 | Stanley et al. | Jul 1998 | A |
| 5811126 | Krishnamurthy | Sep 1998 | A |
| 5834477 | Mioduszewski | Nov 1998 | A |
| 5843480 | Miller et al. | Dec 1998 | A |
| 5846974 | Kallman et al. | Dec 1998 | A |
| 5849240 | Miller et al. | Dec 1998 | A |
| 5856332 | Dante | Jan 1999 | A |
| 5858017 | Demopulos et al. | Jan 1999 | A |
| 5860950 | Demopulos et al. | Jan 1999 | A |
| 5866164 | Kuczynski et al. | Feb 1999 | A |
| 5869097 | Wong et al. | Feb 1999 | A |
| 5879705 | Heafield et al. | Mar 1999 | A |
| 5880132 | Hill | Mar 1999 | A |
| 5891471 | Miller et al. | Apr 1999 | A |
| 5908848 | Muller et al. | Jun 1999 | A |
| 5931809 | Gruber et al. | Aug 1999 | A |
| 5942241 | Chasin et al. | Aug 1999 | A |
| 5958452 | Oshlack et al. | Sep 1999 | A |
| 5958459 | Chasin et al. | Sep 1999 | A |
| 5965161 | Oshlack et al. | Oct 1999 | A |
| 5965163 | Miller et al. | Oct 1999 | A |
| 5968547 | Reder et al. | Oct 1999 | A |
| 5968551 | Oshlack et al. | Oct 1999 | A |
| 5968824 | Spruce et al. | Oct 1999 | A |
| 5972954 | Foss | Oct 1999 | A |
| 5980882 | Eichman | Nov 1999 | A |
| 5980927 | Nelson et al. | Nov 1999 | A |
| 5985856 | Stella et al. | Nov 1999 | A |
| 5998434 | Mitch et al. | Dec 1999 | A |
| 6008258 | Inturrisi | Dec 1999 | A |
| 6024982 | Oshlack et al. | Feb 2000 | A |
| 6034091 | Dante | Mar 2000 | A |
| 6068855 | Leslie et al. | May 2000 | A |
| 6077532 | Malkowska et al. | Jun 2000 | A |
| 6077533 | Oshlack et al. | Jun 2000 | A |
| 6096756 | Crain et al. | Aug 2000 | A |
| 6103258 | Simon | Aug 2000 | A |
| 6103261 | Chasin et al. | Aug 2000 | A |
| 6143322 | Sackler et al. | Nov 2000 | A |
| 6143328 | Heafield et al. | Nov 2000 | A |
| 6153621 | Hamann | Nov 2000 | A |
| 6159501 | Skinhoj | Dec 2000 | A |
| 6162467 | Miller et al. | Dec 2000 | A |
| 6194382 | Crain et al. | Feb 2001 | B1 |
| 6203813 | Gooberman | Mar 2001 | B1 |
| 6210714 | Oshlack et al. | Apr 2001 | B1 |
| 6221339 | Akehurst et al. | Apr 2001 | B1 |
| 6228863 | Palermo et al. | May 2001 | B1 |
| 6254887 | Miller et al. | Jul 2001 | B1 |
| 6261599 | Oshlack et al. | Jul 2001 | B1 |
| 6264981 | Zhang et al. | Jul 2001 | B1 |
| 6277384 | Kaiko et al. | Aug 2001 | B1 |
| 6284268 | Mishra et al. | Sep 2001 | B1 |
| 6294195 | Oshlack et al. | Sep 2001 | B1 |
| 6299901 | DiSanto et al. | Oct 2001 | B1 |
| 6306438 | Oshlack et al. | Oct 2001 | B1 |
| 6310072 | Smith et al. | Oct 2001 | B1 |
| 6316502 | Lai et al. | Nov 2001 | B1 |
| 6319954 | DiSanto | Nov 2001 | B1 |
| 6326027 | Miller et al. | Dec 2001 | B1 |
| 6335033 | Oshlack et al. | Jan 2002 | B2 |
| 6342246 | Johnson et al. | Jan 2002 | B2 |
| 6362194 | Crain et al. | Mar 2002 | B1 |
| 6375957 | Kaiko et al. | Apr 2002 | B1 |
| 6387404 | Oshlack et al. | May 2002 | B2 |
| 6395705 | Crain et al. | May 2002 | B2 |
| 6399096 | Miller et al. | Jun 2002 | B1 |
| 6419959 | Walter et al. | Jul 2002 | B1 |
| 6420433 | DiSanto | Jul 2002 | B2 |
| 6436438 | Momberger et al. | Aug 2002 | B1 |
| 6458795 | Bergeron, Jr. | Oct 2002 | B1 |
| 6475494 | Kaiko et al. | Nov 2002 | B2 |
| 6476046 | Wu | Nov 2002 | B1 |
| 6491949 | Faour et al. | Dec 2002 | B2 |
| 6558708 | Lin | May 2003 | B1 |
| 6559159 | Carroll et al. | May 2003 | B2 |
| 6562364 | DiSanto et al. | May 2003 | B2 |
| 6569449 | Stinchcomb et al. | May 2003 | B1 |
| 6572638 | Dae et al. | Jun 2003 | B1 |
| 6589991 | Lai et al. | Jul 2003 | B1 |
| 6599529 | Skinhøj et al. | Jul 2003 | B1 |
| 6627635 | Palermo et al. | Sep 2003 | B2 |
| 6635661 | Cuny et al. | Oct 2003 | B2 |
| 6645980 | Cuny et al. | Nov 2003 | B1 |
| 6664270 | Bergeron, Jr. | Dec 2003 | B2 |
| 6677332 | Cuny et al. | Jan 2004 | B1 |
| 6696066 | Kaiko et al. | Feb 2004 | B2 |
| 6696088 | Oshlack et al. | Feb 2004 | B2 |
| 6713089 | Bertelsen et al. | Mar 2004 | B1 |
| 6716449 | Oshlack et al. | Apr 2004 | B2 |
| 6734188 | Rhodes et al. | May 2004 | B1 |
| 6753011 | Faour | Jun 2004 | B2 |
| 6762202 | Marek et al. | Jul 2004 | B2 |
| 6765010 | Crain et al. | Jul 2004 | B2 |
| 6818656 | Bergeron, Jr. | Nov 2004 | B2 |
| 6825205 | Kyle | Nov 2004 | B2 |
| 6858580 | Ekwuribe et al. | Feb 2005 | B2 |
| 20010006967 | Crain et al. | Jul 2001 | A1 |
| 20010018069 | Johnson et al. | Aug 2001 | A1 |
| 20010041688 | Waeber et al. | Nov 2001 | A1 |
| 20010046471 | Marek et al. | Nov 2001 | A1 |
| 20020022048 | Bromberg et al. | Feb 2002 | A1 |
| 20020039599 | Lin et al. | Apr 2002 | A1 |
| 20020052351 | Hagan et al. | May 2002 | A1 |
| 20020058673 | Kaiko et al. | May 2002 | A1 |
| 20020065506 | Gruber et al. | May 2002 | A1 |
| 20020094947 | Crain et al. | Jul 2002 | A1 |
| 20020099013 | Piccariello et al. | Jul 2002 | A1 |
| 20020106329 | Leslie | Aug 2002 | A1 |
| 20020119192 | Vishwanathan et al. | Aug 2002 | A1 |
| 20020132005 | Faour | Sep 2002 | A1 |
| 20020132828 | Carroll et al. | Sep 2002 | A1 |
| 20020137761 | Crain et al. | Sep 2002 | A1 |
| 20020156056 | Johnson et al. | Oct 2002 | A1 |
| 20020156092 | Wu | Oct 2002 | A1 |
| 20020160043 | Coleman | Oct 2002 | A1 |
| 20020160991 | Shao | Oct 2002 | A1 |
| 20020173466 | Crain et al. | Nov 2002 | A1 |
| 20030003113 | Lewandowski | Jan 2003 | A1 |
| 20030004177 | Kao et al. | Jan 2003 | A1 |
| 20030022909 | Moss et al. | Jan 2003 | A1 |
| 20030026838 | Farrell | Feb 2003 | A1 |
| 20030031712 | Kaiko et al. | Feb 2003 | A1 |
| 20030044458 | Wright, IV et al. | Mar 2003 | A1 |
| 20030049317 | Lindsay | Mar 2003 | A1 |
| 20030054030 | Gordon | Mar 2003 | A1 |
| 20030055075 | Rubsamen | Mar 2003 | A1 |
| 20030059471 | Compton et al. | Mar 2003 | A1 |
| 20030064099 | Oshlack et al. | Apr 2003 | A1 |
| 20030065002 | Caruso et al. | Apr 2003 | A1 |
| 20030068370 | Sackler | Apr 2003 | A1 |
| 20030068371 | Oshlack et al. | Apr 2003 | A1 |
| 20030068375 | Wright et al. | Apr 2003 | A1 |
| 20030068392 | Sackler | Apr 2003 | A1 |
| 20030069263 | Breder et al. | Apr 2003 | A1 |
| 20030069418 | Aquila et al. | Apr 2003 | A1 |
| 20030073714 | Breder et al. | Apr 2003 | A1 |
| 20030082225 | Mason | May 2003 | A1 |
| 20030096019 | Currie et al. | May 2003 | A1 |
| 20030103972 | Pasternak et al. | Jun 2003 | A1 |
| 20030104976 | Davar et al. | Jun 2003 | A1 |
| 20030118641 | Maloney et al. | Jun 2003 | A1 |
| 20030124061 | Roberts | Jul 2003 | A1 |
| 20030124086 | Bentley et al. | Jul 2003 | A1 |
| 20030124185 | Oshlack et al. | Jul 2003 | A1 |
| 20030133951 | Coe et al. | Jul 2003 | A1 |
| 20030143269 | Oshlack et al. | Jul 2003 | A1 |
| 20030144271 | Shulman | Jul 2003 | A1 |
| 20030148941 | Crain et al. | Aug 2003 | A1 |
| 20030152623 | Bromberg et al. | Aug 2003 | A1 |
| 20030153582 | Bergeron, Jr. | Aug 2003 | A1 |
| 20030157168 | Breder et al. | Aug 2003 | A1 |
| 20030166670 | Brooks-Korn | Sep 2003 | A1 |
| 20030180357 | Martino et al. | Sep 2003 | A1 |
| 20030190362 | Sackler et al. | Oct 2003 | A1 |
| 20030191147 | Sherman et al. | Oct 2003 | A1 |
| 20030194420 | Holl et al. | Oct 2003 | A1 |
| 20030203055 | Rao et al. | Oct 2003 | A1 |
| 20030209240 | Hale et al. | Nov 2003 | A1 |
| 20030211123 | Shukla et al. | Nov 2003 | A1 |
| 20030211136 | Kulkarni et al. | Nov 2003 | A1 |
| 20030211157 | Simon | Nov 2003 | A1 |
| 20030228275 | Ekwuribe et al. | Dec 2003 | A1 |
| 20030232744 | Crain et al. | Dec 2003 | A1 |
| 20030235589 | Demopulos et al. | Dec 2003 | A1 |
| 20030235595 | Chen et al. | Dec 2003 | A1 |
| 20030235617 | Martino et al. | Dec 2003 | A1 |
| 20040024003 | Asmussen et al. | Feb 2004 | A1 |
| 20040024004 | Sherman et al. | Feb 2004 | A1 |
| 20040024434 | Yang et al. | Feb 2004 | A1 |
| 20040033255 | Baker et al. | Feb 2004 | A1 |
| 20040062778 | Shefer et al. | Apr 2004 | A1 |
| 20040072864 | Bergeron, Jr. | Apr 2004 | A1 |
| 20040086561 | Kaiko et al. | May 2004 | A1 |
| 20040087561 | Gonzalez et al. | May 2004 | A1 |
| 20040087607 | Crain et al. | May 2004 | A1 |
| 20040091529 | Edgren et al. | May 2004 | A1 |
| 20040092542 | Oshlack et al. | May 2004 | A1 |
| 20040109894 | Shefer et al. | Jun 2004 | A1 |
| 20040110781 | Harmon et al. | Jun 2004 | A1 |
| 20040115262 | Jao et al. | Jun 2004 | A1 |
| 20040115287 | Chen et al. | Jun 2004 | A1 |
| 20040122022 | Gonzales et al. | Jun 2004 | A1 |
| 20040126323 | Shevchuk et al. | Jul 2004 | A1 |
| 20040131552 | Boehm | Jul 2004 | A1 |
| 20040142958 | Herzberg et al. | Jul 2004 | A1 |
| 20040146547 | Marcenyac et al. | Jul 2004 | A1 |
| 20040151774 | Pauletti et al. | Aug 2004 | A1 |
| 20040156826 | Dangond et al. | Aug 2004 | A1 |
| 20040156903 | Abrams et al. | Aug 2004 | A1 |
| 20040161382 | Yum, II et al. | Aug 2004 | A1 |
| 20040170567 | Sackler | Sep 2004 | A1 |
| 20040176274 | Davar et al. | Sep 2004 | A1 |
| 20040176402 | Oshlack et al. | Sep 2004 | A1 |
| 20040180834 | Lin | Sep 2004 | A1 |
| 20040180916 | Levine | Sep 2004 | A1 |
| 20040186121 | Oshlack et al. | Sep 2004 | A1 |
| 20040192715 | Chasin et al. | Sep 2004 | A1 |
| 20040202717 | Mehta | Oct 2004 | A1 |
| 20040209846 | Cuny et al. | Oct 2004 | A1 |
| 20040209850 | Babul | Oct 2004 | A1 |
| 20040213828 | Smith | Oct 2004 | A1 |
| 20040224020 | Schoenhard | Nov 2004 | A1 |
| 20040228802 | Chang et al. | Nov 2004 | A1 |
| 20040228924 | Oshlack et al. | Nov 2004 | A1 |
| 20040247646 | Ivory et al. | Dec 2004 | A1 |
| 20040247647 | Ivory et al. | Dec 2004 | A1 |
| 20040259899 | Sanghvi et al. | Dec 2004 | A1 |
| 20040266806 | Sanghvi et al. | Dec 2004 | A1 |
| 20050002997 | Howard et al. | Jan 2005 | A1 |
| 20050004155 | Boyd et al. | Jan 2005 | A1 |
| 20050008702 | Faour et al. | Jan 2005 | A1 |
| 20050014693 | Lin | Jan 2005 | A1 |
| 20050020613 | Boehm et al. | Jan 2005 | A1 |
| 20050031546 | Bartholomaus et al. | Feb 2005 | A1 |
| 20050038062 | Burns et al. | Feb 2005 | A1 |
| 20050042281 | Singh et al. | Feb 2005 | A1 |
| 20050043280 | Geisslinger et al. | Feb 2005 | A1 |
| 20050063909 | Wright, IV et al. | Mar 2005 | A1 |
| 20050074493 | Mehta et al. | Apr 2005 | A1 |
| 20050080012 | Mickle et al. | Apr 2005 | A1 |
| 20050080271 | Persons et al. | Apr 2005 | A1 |
| 20050095291 | Oshlack et al. | May 2005 | A1 |
| 20050106249 | Hwang et al. | May 2005 | A1 |
| Number | Date | Country |
|---|---|---|
| WO 03013525 | Feb 2003 | WO |
| Number | Date | Country | |
|---|---|---|---|
| 20090238868 A1 | Sep 2009 | US |
| Number | Date | Country | |
|---|---|---|---|
| Parent | 10409992 | Apr 2003 | US |
| Child | 12478952 | US |
