DEXMEDETOMIDINE PREMIX FORM ULATION CROSS-REFERENC[ TO RELATED APPLICATIONS The present application is a divisional application from Australian patent application number 2013201069. The entire disclosure of which is incorporated herein by reference. 1. FIELD OF TIlE INVENTION The present invention relates to patient-ready, premixed formulations of dexmedetornidine, or a pharmaceutically acceptable salt thereof, that can be used, for example, in perioperative care of a patient or for sedation. 2. BAC1KGROUN D OF TI] E INVENTION Racemic 4-[I-(2,3-dimethylphenvl)ethyl]-IH-imi dazole, which is known under the name medetomidine, is a selective and potent U2-adrenoceptor agonist. Medetomidine has been used as an anti hypertensive agent and as a sedative-analgesic agent. It has further been observed that this compound also possesses anxiolytic effects and can therefore be used in the treatment of general anxiety, panic disorder and various types of withdrawal symptoms. The d-enantiomer of medetomidine, the generic name of which is dexmedetomidine, is described in U.S. Pat. No. 4,910,214 as an ur-adrenoceptor agonist for general sedation/analgesia and the treatment of hypertension or anxiety. U.S. Pat. Nos. 5,344,840 and 5,091,402 discuss dexmedetomidine in perioperative and epidural use, respectively. For example, when used in perioperative care, dexmedetomidine can reduce the amount of anesthetic necessary to anesthetize a patient. Additionally, U S Pat. No. 5,304,569 discusses the use of dexmedetomidine in treating glaucoma, and U.S. Pat. No. 5,712,301 discusses the use of dexmedetomidine for preventing neurodegeneration caused by ethanol consumption. Furthermore, U.S. Pat. No. 6,716,867 discloses methods of sedating a patient while in an intensive care unit by administering dexnedetomidine, or a pharmaceutically acceptable salt thereof, to the patient. - I - 077350.0356 Dexmedetomidine can be administered to a patient in a variety of ways. For example, U.S. Pat. Nos. 4,544,664 and 4,910,214 disclose the administration of dexmedetomidine via parenteral, intravenous, and oral routes. U.S. Pat. No. 4,670,455 describes intramuscular and intravenous administration, while U.S. 5 Pat. Nos. 5,124,157 and 5,217,718 describe a method and device for administering dexmedetomidine through the skin. Additionally, U.S. Pat. No. 5,712,301 states that dexmedetomi dine can be administered transmucosally. To date, dexmedetomidine has been provided as a concentrate that must be diluted prior to administration to a patient. The requirement of a dilution step 10 in the preparation of the dexmedetomidine formulation is associated with additional costs and inconvenience, as well as the risk of possible contamination or overdose due to human error. Thus, a dexmedetomidine formulation that avoids the expense, inconvenience, delay and risk of contamination or overdose would provide significant advantages over currently available concentrated formulations. 15 3. SUMMARY OF THE INVENTION The present invention relates to premixed pharmaceutical compositions of dexmedetomidine, or a pharmaceutically acceptable salt thereof, that are formulated for administration to a patient, without the need to reconstitute or dilute 20 the composition prior to administration. Thus, the compositions of the present invention are formulated as a premixed composition comprising dexmedetomidine. In certain non-limiting embodiments, the premixed dexmedetomidine composition is a liquid comprising dexmedetomidine, or a pharmaceutically acceptable salt thereof, at a concentration of between about 0.05 Ig/mL and about 15 25 [ig/mL. In other non-limiting embodiments, the premixed dexnedetomidine composition is a liquid comprising dexmedetomidine at a concentration of about 4 ptg/mL. In other non-limiting embodiments, the premixed dexmedetomidine 30 composition comprises dexmedetomidine mixed or dissolved in a sodium chloride saline solution. In certain embodiments, the premixed dexmedetomidine composition is disposed within a sealed container or vessel. NY02:746896.1 - 2 077350.0356 In certain embodiments, the dexmedetomidine composition is disposed in a container or vessel and is formulated as a premixture. In certain embodiments, the premixed dexmedetomidine composition is disposed within a sealed container as a total volume of about 20 mL, 50 rnL or 100 5 mL. In certain non-limiting embodiments, the premi xed dexmedetornidine composition of the present invention comprises dexm edetomi dine, or a pharmaceutically acceptable salt thereof, at a concentration of between about 0.05 pg/mL. and about 15 pg/mL, and sodium chloride at a concentration of between about 10 0.01 and about 2.0 weight percent. In other non-limiting embodiments, the premixed dexmedetomidine composition of the present invention comprises dexmedetomidine, or a pharnaceutically acceptable salt thereof, at a concentration of about 4 pg/mL and sodium chloride at a concentration of about 0.90 weight percent. 15 In certain embodiments, the compositions of the present invention are formulated as a pharmaceutical composition for administration to a subject for sedation, analgesia or treatment of anxiety or hypertension. The present invention also relates to the perioperative treatment of a patient to reduce the response of the autonomic nervous system to stimuli during an 20 operation by administering a dexmedetomidine composition of the invention. In other non-limiting embodiments, the dexmedetomidine compositions of the present invention can be administered as an anxiolytic analgesic to a patient. In certain embodiments, the composition can be administered as a premedication prior to an operation with or without administration of an amount of an 25 anesthetic effective to achieve a desired level of local or general anesthesia. In other non-limiting embodiments, the dexmedetomidine compositions of the present invention can be administered as a sedative. in certain embodiments, the composition is administered preoperatively to potentiate the effect of an anesthetic, wherein administration of the composition reduces the amount of 30 anesthetic required to achieve a desired level of anesthesia. In certain embodiments of the present invention, the premixed dexmedetomidine composition is administered parenterally as a liquid, orally, transdermally, intravenously, intramuscularly, subcutaneously, or via an implantable pump. NY02:746896.1 -3 - 077350.0356 4. DETAILED DESCRIPTION The present invention is based in part on the discovery that dexmedetomidine prepared in a premixed formulation that does not require 5 reconstitution or dilution prior to administration to a patient, remains stable and active after prolonged storage. Such premixed formulations therefore avoid the cost, inconvenience, and risk of contamination or overdose that can be associated with reconstituting or diluting a concentrated dexmedetonidine formulation prior to administration to a patient. 10 For clarity and not by way of limitation, this detailed description is divided into the following sub-portions: (4.1) Definitions; (4.2) Pharmaceutical formulations; and (4.3) Methods of using premixed dexmedetomidine compositions. 15 4.1 Definitions The terms used in this specification generally have their ordinary meanings in the art, within the context of this invention and in the specific context where each term is used. Certain terms are discussed below, or elsewhere in the 20 specification, to provide additional guidance to the practitioner in describing the compositions and methods of the invention and how to make and use them. According to the present invention, the term "dexmedetomidine" as used herein refers to a substantially pure, optically active dextrorotary stereoisomer of medetomidine, as the free base or pharmaceutically acceptable salt. In one, non 25 limiting embodiment, dexnedetomi dine has the formula (S)-4-[i-(2,3 dimethylphenyl)ethyl]-3H-imidazole. A pharmaceutically acceptable salt of dexmedetomidine can include inorganic acids such as hydrochloric acid, hydrobromic acid, sulfuric acid, nitric acid, phosphoric acid and the like, and organic acids such as acetic acid, propionic acid, glycolic acid, pyruvic acid, oxalic acid, malic acid, 30 malonic acid, succinic acid, maleic acid, fumaric acid, tartaric acid, citric acid, benzoic acid, cinnamic acid, mandelic acid, methanesulfonic acid, ethanesulfonic acid, p-toluenesulfonic acid, and salicylic acid. Preferably, the dexmedetomidine salt NY02:'746896.1 -4- 077350.0356 is dexmedetomidine HCL. In other non-limiting embodiments, dexmedetomidine comprises the structure depicted below in Formula I: CH3 CH CH. N N H Formula I The terms "premix" or "premixture" as used herein refers to a phannaceutical formulation that does not require reconstitution or dilution prior to administration to a patient. For example, in contrast to non-premixed formulations of 10 dexmedetomidine, the premixed compositions provided herein are suitable for administration to a patient without dilution by, for example, a clinician, hospital personnel, caretaker, patient or any other individual. In certain embodiments, the compositions of the present invention can be formulated as "ready to use" compositions which refer to premixed compositions 15 that are suitable for administration to a patient without dilution. For example, in certain embodiments, the compositions of the present invention are "ready to use" upon removing the compositions from a sealed container or vessel. In certain embodiments, the compositions of the present invention can be formulated as a "single use dosage," which refers to a premixed composition that is 20 disposed within a sealed container or vessel as a one dose per container or vessel formulation. According to the invention, a "subject" or "patient" is a human, a non human mammal or a non-human animal. Although the animal subject is preferably a human, the compounds and compositions of the invention have application in 25 veterinary medicine as well, e.g., for the treatment of domesticated species such as canine, feline, and various other pets; farm animal species such as bovine, equine, ovine, caprine, porcine, etc.; wild animals, e.g., in the wild or in a zoological garden; and avian species, such as chickens, turkeys, quail, songbirds, etc. NY02:746896.1 -5 - 077350.0356 The term "purified" as used herein refers to material that has been isolated under conditions that reduce or eliminate the presence of unrelated materials, i.e., contaminants, including native materials from which the material is obtained. As used herein, the term "substantially free" is used operationally, in the context of 5 analytical testing of the material. Preferably, purified material substantially free of contaminants is at least 95% pure; more preferably, at least 97% pure, and more preferably still at least 99% pure. Purity can be evaluated, for example, by chromatography or any other methods known in the art. In a specific embodiment, purified means that the level of contaminants is below a level acceptable to regulatory 10 authorities for safe administration to a human or non-human animal. The term "pharnaceutically acceptable," when used in connection with the pharmaceutical compositions of the invention, refers to molecular entities and compositions that are physiologically tolerable and do not typically produce untoward reactions when administered to a human. Preferably, as used herein, the term 15 "pharmaceutically acceptable" means approved by a regulatory agency of the Federal or a state government or listed in the U.S. Pharmacopeia or other generally recognized pharmacopeia for use in animals, and more particularly in humans. The term "carrier" refers to a diluent, adjuvant, excipient, dispersing agent or vehicle with which the compound is administered. Such pharmaceutical carriers can be sterile liquids, such as 20 water and oils. For example, water, aqueous solutions, saline solutions, aqueous dextrose or glycerol solutions can be employed as carriers, particularly for injectable solutions. Suitable pharmaceutical carriers are described in, for example, "Remington's Pharmaceutical Sciences" by Philip P. Gerbino, 21st Edition (or previous editions). 25 The term "pharmaceutical composition" as used in accordance with the present invention relates to compositions that can be formulated in any conventional manner using one or more pharmaceutically acceptable carriers or excipients. A "pharmaceutically acceptable" carrier or excipient, as used herein, means approved by a regulatory agency of the Federal or a state government, or as listed in the U.S. 30 Pharmacopoeia or other generally recognized pharmacopoeia for use in mammals, and more particularly in humans. The term "dosage" is intended to encompass a formulation expressed in terms of pg/kg/day, pg/kg/hr, mg/kg/day or mg/kg/hr. The dosage is the amount of an ingredient administered in accordance with a particular dosage regimen. A "dose" NY02:746896.1 -6- 077350.0356 is an amount of an agent administered to a mammal in a unit volume or mass, e.g., an absolute unit dose expressed in mg or ug of the agent. The dose depends on the concentration of the agent in the formulation, e.g., in moles per liter (M), mass per volume (m/v), or mass per mass (m/m). The two terms are closely related, as a 5 particular dosage results from the regimen of administration of a dose or doses of the formulation. The particular meaning in any case will be apparent from context. The terms "therapeutically effective dose," "effective amount," and "therapeutically effective amount" refer to an amount sufficient to produce the desired effect. 10 In some non-limiting embodiments, a "therapeutically effective dose" means an amount sufficient to reduce by at least about 15%, preferably by at least 50%, more preferably by at least 90%, and most preferably prevent, a clinically significant deficit in the activity, function and response of the host. Alternatively, a therapeutically effective amount is sufficient to cause an improvement in a clinically 15 significant condition in the host. These parameters will depend on the severity of the condition being treated, other actions, such as diet modification, that are implemented, the weight, age, and sex of the subject, and other criteria, which can be readily determined according to standard good medical practice by those of skill in the art. In other non-limiting embodiments a therapeutic response may be any 20 response that a user (e.g., a clinician) will recognize as an effective response to the therapy. Thus, a therapeutic response will generally be an induction of a desired effect, such as, for example, sedation or analgesia. The term "about" or "approximately" as used herein means within an acceptable error range for the particular value as determined by one of ordinary skill 25 in the art, which will depend in part on how the value is measured or determined, i.e., the limitations of the measurement system. For example, "about" can mean within 3 or more than 3 standard deviations, per the practice in the art. Alternatively, "about" can mean a range of up to 20%, preferably up to 10%, more preferably up to 5%/0, and more preferably still up to 1% of a given value. Alternatively, particularly with 30 respect to biological systems or processes, the term can mean within an order of magnitude, preferably within 5-fold, and more preferably within 2-fold, of a value. NY02:746896.1 077350.0356 4.2 Pharmaceutical Compositions The compounds and compositions of the invention may be formulated as pharmaceutical compositions by admixture with a pharnaceutically acceptable 5 carrier or excipient. In certain non-limiting embodiments, the compounds or compositions are provided in a therapeutically effective amount to an animal, such as a mammal, preferably a human, in need of treatment therewith for inducing a sedative, anxiolytic, analgesic, or anesthetic effect. In certain non-limiting embodiments, dexm edetomi dine is formulated 10 as a composition, wherein the dexmedetomidine is the only therapeutically active ingredient present in the composition. In another non-limiting embodiments, dexmedetomidine is formulated as a composition, wherein the dexmedetomidine is formulated in combination with at least one or more other therapeutically active ingredient. The formulation is preferably suitable for parenteral administration, 15 including, but not limited to, intravenous, subcutaneous, intramuscular and intraperitoneal administration; however, formulations suitable for other routes of administration such as oral, intranasal, mucosal or transdermal are also contemplated. The pharmaceutical formulations suitable for injectable use, such as, for example, intravenous, subcutaneous, intramuscular and intraperitoneal 20 administration, include sterile aqueous solutions or dispersions and sterile powders for the extemporaneous preparation of sterile injectable solutions or dispersion. In all cases, the form can be sterile and can be fluid to the extent that easy syringability exists. It can be stable under the conditions of manufacture and storage and can be preserved against the contaminating action of microorganisms such as bacteria and 25 fungi. The carrier can be a solvent or dispersion medium containing, for example, water, saline, ethanol, polyol (for example, glycerol, propylene glycol, and polyethylene glycol, and the like), suitable mixtures thereof, and oils. The proper fluidity can be maintained, for example, by the use of a coating such as lecithin, by the maintenance of the required particle size in the case of dispersion and by the use 30 of surfactants. The preventions of the action of microorganisms can be brought about by various antibacterial and antifungal agents, for example, parabens, chliorobutanol, phenol, benzyl alcohol, sorbic acid, and the like. In many cases, it will be preferable to include isotonic agents, for example, sugars or sodium chloride. Prolonged absorption of the injectable NY02:'746896.1 - 8- 077350.0356 compositions can be brought about by the use in the compositions of agents delaying absorption, for example, aluminum monosterate and gelatin. Sterile injectable solutions may be prepared by incorporating the dexmedetomidine in the required amounts in the appropriate solvent with various of the other ingredients enumerated 5 above, as required, followed by filter or terminal sterilization. Generally, dispersions are prepared by incorporating the various sterilized active ingredients into a sterile vehicle which contains the basic dispersion medium and the required other ingredients from those enumerated above. In the case of sterile powders for the preparation of sterile injectable solutions, the preferred methods of preparation are vacuum drying 10 and the freeze-drying technique which yield a powder of the active ingredient plus any additional desired ingredient from previously sterile-filtered solution thereof. Preferably the formulation may contain an excipient. Pharmaceutically acceptable excipients which may be included in the formulation are buffers such as citrate buffer, phosphate buffer, acetate buffer, and bicarbonate buffer; amino acids; 15 urea; alcohols; ascorbic acid; phospholipids; proteins, such as serum albumin, collagen, and gelatin; salts such as EDTA or EGTA, and sodium chloride; liposomes; polyvinylpyrollidone; sugars, such as dextran, mannitol, sorbitol, and glycerol; propylene glycol and polyethylene glycol (e.g., PEG-4000, PEG-6000); glycerol; glycine; lipids; preservatives; suspending agents; stabilizers; and dyes. As used 20 herein, the term "stabilizer" refers to a compound optionally used in the pharmaceutical compositions of the present invention in order to avoid the need for suilphite salts and increase storage life. Non-limiting examples of stabilizers include antioxidants. Buffer systems for use with the formulations include citrate; acetate; bicarbonate; and phosphate buffers. 25 The formulation also may contain a non-ionic detergent. Preferred non ionic detergents include Polysorbate 20, Polysorbate 80, Triton X-100, Triton X-i 14, Nonidet P-40, Octyl ca-glucoside, Octyl -glucoside, Brij 35, Pluronic, and Tween 20. The parenteral formulations of the present invention can be sterilized. Non-limiting examples of sterilization techniques include filtration through a 30 bacterial-retaining filter, terminal sterilization, incorporation of sterilizing agents, irradiation, and heating. The route of administration may be oral or parenteral, including intravenous, subcutaneous, intra-arterial, intraperitoneal, ophthalmic, intramuscular, buccal, rectal, vaginal, intraorbital, intracerebral, intradermal, intracranial, intraspinal, NY02:746896.1 -9- 077350.0356 intraventricular, intrathecal, intracisternal, intracapsular, intrapulmonary, intranasal, transmucosal, transdermal, or via inhalation. Administration of the above-described parenteral formulations may be by periodic injections of a bolus of the preparation, or may be administered by 5 intravenous or intraperitoneal administration from a reservoir which is external (e.g., an intravenous bag) or internal (e.g., a bioerodabl e implant, a bioartificial or organ). See, eg., U S. Pat. Nos. 4,407,957 and 5,798,113, each incorporated herein by reference in their entireties. Intrapulmonary delivery methods and apparatus are described, for example, in U.S. Pat. Nos. 5,654,007, 5,780,014, and 5,814,607, each 10 incorporated herein by reference in their entireties. Other useful parenteral delivery systems include ethylene-vinyl acetate copolymer particles, osmotic pumps, implantable infusion systems, pump delivery, encapsulated cell delivery, liposomal delivery, needle-delivered injection., needle-less injection, nebulizer, aeorosolizer, electroporation, and transdermal patch. Needle-less injector devices are described in 15 U.S. Pat. Nos. 5,879,327; 5,520,639; 5,846,233 and 5,704,911, the specifications of which are herein incorporated herein by reference in their entireties. Any of the formulations described herein can be administered in these methods. In yet another non-limiting embodiment, the therapeutic compound can be delivered in a controlled or sustained release system. For example, a compound or 20 composition may be administered using intravenous infusion, an implantable osmotic pump, a transdermal patch, liposomes, or other modes of administration. In one embodiment, a pump may be used (see Sefton, 1987, CRC Crit. Ref. Biomed. Eng. 14:201; Buchwald et al., 1980, Surgery 88:507; Saudek et al., 1989, N. Engl. J. Med. 321:574). In another embodiment, polymeric materials can be used (see Langer and 25 Wise eds., 1974, Medical Applications of Controlled Release, CRC Press: Boca Raton, Fla; Smolen and Ball eds., 1984, Controlled Drug Bioavailability, Drug Product Design and Performance, Wiley, N.Y.; Ranger and Peppas, 1983, J. Macromol. Sci. Rev. Macromol. Chem., 23:61; Levy et al., 1985, Science 228:190; During et al., 1989, Ann. Neurol., 25:351; Howard et al., 9189, J.Neurosurg. 71:105). 310 In yet another embodiment, a controlled release system can be placed in proximity of the therapeutic target, i.e., the brain, thus requiring only a fraction of the systemic dose (see, e.g., Goodson, 1984, in Medical Applications of Controlled Release, Vol. 2, pp. 115-138). NY02:746896.1 - 10 - 077350.0356 In certain non-limiting embodiments, the premixed dexmedetomidine composition comprises dexmedetomidine, or a pharmaceutically acceptable salt thereof, at a concentration of between about 0.005 pg/mL and about 100 pg/mL, or between about 0.005 pg/mL and about 50 pg/mL, or between about 0.005 pg/mL and 5 about 25 pg/mL, or between about 0.005 pg/mL and about 15 pg/mL, or between about 0.005 pg/mL and about 10 pg/mi, or between about 0.005 pg/mL and about 7 pg/mL, or between about 0.005 pg/mL. and about 5 pg/mL, or between about 0.005 pg/mL and about 4 pg/mL, or between about 0.005 pg/mL and about 3 pg/mL, or between about 0.005 pg/mL and about 2 ug/mL, or between about 0.005 pg/mL and 10 about I pg/mL, or between about 0.005 pg/mL and about 0.5 pg/mL, or between about 0.005 pg/mL and about 0.05 pg/mi.. In certain non-limiting embodiments, the premixed dexmedetomidine composition comprises dexmedetornidine, or a pharmaceutically acceptable salt thereof, at a concentration of between about 3.5 pg/mL and about 4.5 pg/mL, or 15 between about 3 pg/mL and about 5 pg/mL, or between about 2.5 pg/mL and about 5.5 g/mL, or between about 2 pg/mL and about 6 g/mL, or between about 1.5 pg/mL and about 6.5 pg/mL, or between about I pg/mL and about 7 pg/mL, or between about 0.5 pg/mL and about 10 pg/mL. In certain non-limiting embodiments, the premixed dexmedetomidine 20 composition comprises dexmedetomidine at a concentration of about 0.5 pg/mL, or about I pg/mL, or about 1.5 pg/mL, or about 2 pg/mL, or about 2.5 g/mL, or about 3 pg/mi., or about 3.5 pg/mi, or about 4 pg/mi., or about 4.5 pg/mL, or about 5 pg/mL, or about 5.5 pg/mL, or about 6 pg/mL, or about 6.5 pg/mL, or about 7 pg/mL, or about 7.5 pg/m, or about 8 pg/mL, or about 8.5 pg/nL, or about 9 25 pg/mL, or about 9.5 p g/mL, or about 10 pg/mL, or about 10. 5 pg/mL, or about II pg/mL, or about 11.5 pg/mL, or about 12 pg/mL, or about 12.5 pg/mL, or about 13 pg/mL., or about 13.5 pg/mL., or about 14 pg/mL, or about 14.5 pg/m L, or about 15 pg/mL, or about 15.5 pg/mL, or about 16 pg/mL, or about 16.5 pg/mL, or about 17 pg/mL, or about 17.5 pg/mL, or about 18 pg/mL., or about 18.5 pg/mL. or about 19 3 g/mL, or about 19.5 g/mL, or about 20 pg/mi. In certain non-limiting embodiments, the premixed dexnedetomidine composition comprises dexmedetomidine at a concentration of about 4 pg/mL. In certain non-limiting embodiments, the premixed dexmedetomidine composition is formulated as a liquid. NY02:746896.1 - 11 - 077350.0356 In certain non-limiting embodiments, the premixed dexmedetomidine composition is formulated at a p1- of between about I and about 10, or between about 1 and about 8, or between about I and about 6, or between about I and about 4, or between about I and about 2. In other non-limiting embodiments, the premixed 5 dexmedetomidine composition is formulated at a pH of between about 2 and about 10, or between about 4 and about 8, or between about 4 and about 7. In other non limiting embodiments, the premixed dexmedetomidine composition is formulated at a pH of between about 4.7 and about 6.2. In a preferred non-limiting embodiment, the premixed dexmedetomidine composition is formulated at a p-I of between about 4.5 10 and about 7.0. In other non-limiting embodiments, the premixed dexmedetomidine composition comprises dexmedetomidine mixed or dissolved in a sodium chloride saline solution. The saline solution can comprise sodium chloride present at a concentration of between about 0.05 weight percent and about 10 weight percent, or 15 between about 0.05 weight percent and about 5 weight percent, or between about 0.05 weight percent and about 3 weight percent, or between about 0.05 weight percent and about 2 weight percent, or between about 0.05 weight percent and about I weight percent. In one preferred, non-limiting embodiment, the sodium chloride is present at a concentration of about 0.9 weight percent. 20 In certain embodiments, the weight percent of the saline solution is a percent weight/weight of the premix composition. In certain embodiments, the weight percent of the saline solution is a percent weight/volume of the premix composition. In certain non-limiting embodiments, the premi xed dexmedetornidine 25 composition of the present invention comprises dexmedetomidine, or a pharmaceutically acceptable salt thereof, at a concentration of between about 0.05 pg/mL and about 15 pg/mL, and sodium chlorde at a concentration of between about 0.01 and about 2.0 weight percent. In other non-limiting embodiments, the premixed dexmedetomidine 30 composition of the present invention comprises dexmedetomidine, or a pharnaceutically acceptable salt thereof, at a concentration of about 4 ttg/mL and sodium chloride at a concentration of about 0.90 weight percent. In one non-limiting example, the 0.9% NaCl solution is formulated by mixing 9.0 g NaCl / 1000 mL of water. In certain embodiments, the premix NY02:746896.1 - 12 - 077350.0356 compositions of the present invention are formulated by adding 0.118 g dexmedetomidine [HCA plus 9.0 g NaCi into the same 1000 ml- of water. The solution can then be mixed with addition 0.9% NaCl solution to achieve a desired concentration of dexmedetomidine, for example, 4 pg/mL. 5 In certain non-limiting embodiments, the premixed dexmedetomidine composition of the present invention is disposed in a container or vessel that can maintain the sterility of, or prevent the contamination of, a premixed dexmedetomidine composition that is purified or substantially free of any contaminants. In certain non-limiting embodiments, the container or vessel is a sealed 10 container or vessel. In certain non-limiting embodiments, the dexmedetomidine composition of the present invention is disposed in a container or vessel and is formulated as a premixture. In certain non-limiting embodiments, the premixed dexmedetomidine 15 composition of the present invention is disposed in a container or vessel and is formulated as a single use dosage. In certain non-limiting embodiments, the premixed dexmedetomidine composition of the present invention is disposed in a container or vessel and is formulated as a dosage for multiple use. In certain non-limiting embodiments, the container or vessel includes, 20 but is not limited to, glass vials (for example, but not limited to, flint glass vials), ampoules, plastic flexible containers, for example, but not limited to, PVC (polyvinyl chloride) containers, VisIVTh plastic containers (Hospira, Inc., Lake Forest, IL), and CR3 elastomer copolyester ether containers (Hospira, Inc., Lake Forest, IL), CZ resin containers, poly propylene containers and syringes. 25 In certain non-limiting embodiments, the premixed dexmedetomidine composition of the present invention can be stored as a liquid in an aliquot having a total volume of between about I and 500 mL, or between about I and 250 mL, or between about I and 200 mL, or between about I and 150 mL, or between about I and 125 mL, or between about I and 120 mL, or between about I and 110 mL., or 30 between about I and 100 mL, or between about I and 90 mL, or between about 1 and 80 n L, or between about I and 70 ml, or between about I and 60 n L, or between about 1 and 50 mL, or between about 1 and 40 mL, or between about 1 and 30 mL, or between about I and 20 mL, or between about I and 10 mL, or between about I and 5 mL. NYO2:746 896.1 - 13 - 077350.0356 In certain non-limiting embodiments, the premixed dexmedetomidine composition of the present invention can be stored as a liquid in an aliquot having a total volume of about 5 mL, or about 10 mL, or about 15 mL, or about 20 mL, or about 25 ml, or about 30 mL, or about 35 nL, or about 40 nL, or about 45 mL, or 5 about 50 mL, or about 55 mL, or about 60 mL, or about 65 mL, or about 70 mL, or about 75 nL, or about 80 mL, or about 85 mL, or about 90 mL, or about 95 mL, or about 100 mL, or about 105 m L, or about 110 n L, or about 115i mL, or about 120 mL, or about 125 mL, or about 130 mL, or about 135 mL, or about 140 mL, or about 145 mL, or about 150 mL, or about 200 nL, or about 250 mL, or about 500 rnL 10 In certain non-limiting embodiments, the premixed dexmedetomidine composition of the present invention can be stored as a liquid in an aliquot having a total volume of about 20 mL. In certain non-limiting embodiments, the premixed dexnedetomidine composition of the present invention can be stored as a liquid in an aliquot having a 15 total volume of about 50 mL. In certain non-limiting embodiments, the premixed dexmedetomidine composition of the present invention can be stored as a liquid in an aliquot having a total volume of about 100 mL. 20 4.3 Methods of Using Premixed Dexmedetomidine Comp ositions In accordance with the invention, there are provided methods of using a premixed dexmedetonidine composition. In certain non-limiting embodiments, the present invention provides for preoperative treatment of a patient to reduce the response of the autonomic nervous system to stimuli during an operation by 25 administering a dexmedetomidine composition of the invention, as described in U S Pat. No. 5,344,840. In other non-limiting embodiments, the dexmedetomidine compositions of the present invention can be administered as a sedative. in certain embodiments, the composition is administered preoperatively to potentiate the effect of an anesthetic, wherein administration of the composition reduces the amount of 30 anesthetic required to achieve a desired level of anesthesia. In certain embodiments, the dexmedetomidine compositions of the present invention can be administered as an anxiolytic analgesic premedication prior to the operation with or without administration of an amount of an anesthetic effective to achieve a desired level of local or general anesthesia. In certain embodiments, the dexm edetomi dine NY02:7468996.1 - 14 - 077350.0356 compositions of the present invention are formulated as a pharmaceutical composition for use in a method of sedation, analgesia or treatment of anxiety or hypertension. In certain non-limiting embodiments, the patient treated with the premixed dexmedetomidine composition of the invention is intubated. The patient 5 may be intubated prior to, during, or after administration of the premixed dexmedetonidine composition. The patient may be intubated by the nasotracheal, endotracheal, direct oral laryngoscopy or by fibreoptic routes, or via tracheotomy, for example, while being treated in an intensive care unit (ICU), which, as used herein refers to any setting that provides intensive care, as described, for example, in U S. 10 Pat. No. 6,716,867. For example, the compositions of the invention can be used for sedating a patient in an intensive care unit which means rendering a patient calm and treating conditions that affect patient comfort, such as pain and anxiety, in any setting that provides intensive care. In other non-limiting embodiments, the premixed dexmedetomidine 15 compositions of the present invention can be administered to a patient as a perioperative treatment. In certain embodiments, the composition can be administered as a premedication prior to an operation. In certain embodiments, the premixed dexmedetomidine compositions of the present invention can be used in the manufacture of a medicament for perioperative treatment of mammals to reduce the 20 responses of the autonomic nervous system to stressful stimuli during an operation, for example, as described in U.S. Pat. No. 5,344,840. In other non-limiting embodiments, the premixed dexmnedetomidine compositions of the present invention can be administered to a patient as an adjunct anesthesia. For example, the composition can be administered with or without an 25 amount of an anesthetic effective to achieve a desired level of local or general anesthesia, for example, as described in U.S. Pat. No. 5,344,840. In certain embodiments, administration of the compositions of the present invention reduces the amount of anesthetic required to achieve a desired level of anesthesia. In other non-limiting embodiments, the patient treated with the 30 premixed dexmedetomidine composition is critically ill. In one embodiment, the patient suffers from one or more medical conditions. In certain embodiments, the medical condition is a lung problem, brain problem, heart problem, liver problem, kidney problem, eye or ear problem, gastrointestinal problem, or skin problem. Non limiting examples of lung problems include respiratory distress syndrome, NY02:746896.1 - 15 - 077350.0356 pneumonia, bronchopulmonary dysplasia, apnea of prematurity, and pneumothorax. Non-limiting examples of brain problems include intraventricular hemorrhage, and cerebral palsy. Non-limiting examples of liver problems include jaundice. Non limiting examples of heart problems include patent ductus arteriosus. Non-limiting 5 examples of eye problems include retinopathy of prematurity, myopia, and strabismus. Non-limiting examples of other medical conditions includes heroin withdrawal, cocaine withdrawal, alcohol fetal syndrome, HIV-positive status, and Tay Sachs disease. In one embodiment, the patient has undergone surgery. The patient 10 may undergo surgery prior to, during, or after administration of the premixed dexmedetonidine composition. Non-limiting examples of surgery include cardiopulmonary bypass. In other non-limiting embodiments, the premixed dexrnedetomidine compositions of the present invention can be administered to a patient as an anxiolytic 15 or analgesic agent, for example, as described in U.S. Pat. Nos. 5,344,840 and 6,716,867. In one non-limiting example, the method comprises local epidural or intraspinal administration of the premixed dexmedetomidine composition of the invention. In other non-limiting embodiments, the premixed dexmedetomidine 20 compositions of the present invention can be administered to a patient to lower intraocular pressure, for example, in the treatment of glaucoma, as described in U.S. Pat. No. 5,304,569. In certain embodiments, the premixed dexmedetomidine compositions of the present invention do not include any other active ingredient, or therapeutic 25 agent, other than dexmedetomidine. In certain non-limiting embodiments of the present invention, the premixed dexmedetomidine composition can be administered as a single continuous dose over a period of time. For example, the premixed dexmedetomidine composition can be administered intravenously for a period of time of between about I and about 30 10 minutes, or between about 1 and about 20 minutes, or between about 1 and about 30 minutes, or between about I and about 2 hours, or between about I and about 3 hours, or between about I and about 4 hours, or between about I and about 5 hours, or between about I and about 6 hours, or between about I and about 7 hours, or between about I and about 8 hours, or between about I and about 9 hours, or between about I NY02:746896.1 - 16 - 077350.0356 and about 10 hours, or between about I and about 11 hours, or between about I and about 12 hours, or between about I and about 13 hours, or between about I and about 14 hours, or between about 1 and about 15 hours, or between about I and about 16 hours, or between about I and about 17 hours, or between about I and about 18 hours, 5 or between about I and about 19 hours, or between about 1 and about 20 hours, or between about I and about 21 hours, or between about 1 and about 22 hours, or between about I and about 23 hours, or between about I and about 24 hours, and administered at a dosage of between about 0.005 ptg/kg/hr and about 5 pig/kg/hr, or between about 0.005 tg/kg/hr and about 4.5 pg/kg/hr, or between about 0.005 10 pg/kg/hr and about 3 pg/kg/hr, or between about 0.005 pg/kg/hr and about 2.5 pg/kg/hr, or between about 0.005 pg/kg/hr and about 2 g/kg/hr, or between about 0.005 pg/kg/hr and about 1.5 pg/kg/hr, or between about 0.005 pg/kg/hr and about I pg/kg/hr, or between about 0.005 pg/kg/hr and about 0.5 pg/kg/hr, or between about 0.005 pg/kg/hr and about 0.25 pg/kg/hr. 15 In other non-limiting embodiments of the present invention, the premixed dexrnedetomi dine composition can be administered as a loading dose followed by a maintenance dose over a period of time. For example, the loading dose can comprise administration of the premixed dexmedetomidine composition at a first dosage amount for a first period of time, followed by administration of the 20 maintenance dose at a second dosage amount for a second period of time. The loading dose can be administered for a period of time of between about I and about 5 minutes, or between about I and about 10 minutes, or between about I and about 15 minutes, or between about I and about 20 minutes, or between about I and about 25 minutes, or between about 1 and about 30 minutes, or between about 1 and about 45 25 minutes, or between about I and about 60 minutes. Following the loading dose, the maintenance dose can be administered for a period of time as described above for a single continuous dose. In certain non-limiting embodiments, the premixed dexmedetomidine composition, when administered as a single continuous, loading or maintenance dose, 30 is administered for a period of time of about 1 hour to about 7 days, or about 1 hour to about 4 days, or about I hour to about 48 hours, or about I hour to about 36 hours, or about 1 hour to about 24 hours, or about 1 hour to about 12 hours. In certain non-limiting embodiments, the premixed dexmedetomidine composition, when administered as a single continuous, loading or maintenance dose, NY02:746896.1 - 17 - 077350.0356 is administered for a period of time of about 24 hours to about 120 hours, or about 24 hours to about 108 hours, or about 24 hours to about 96 hours, or about 24 hours to about 72 hours, or about 24 hours to about 48 hours, or about 24 hours to about 36 hours. 5 When administered as a loading dose followed by a maintenance dose, the loading dose and/or maintenance dose can be a dose of between about 0.005 pg/kg/hr and about 5 tg/kg/hr, or between about 0.005 ig/kg/hr and about 4.5 pg/kg/hr, or between about 0.005 pig/kg/hr and about 3 pig/kg/hr, or between about 0.005 pg/kg/hr and about 2.5 pag/kg/hr, or between about 0.005 ptg/kg/hr and about 2 10 pag/kg/hr, or between about 0.005 jag/kg/hr and about 1.5 ptg/kg/hr, or between about 0.005 pg/kg/hr and about I pg/kg/hr, or between about 0.005 pg/kg/hr and about 0.5 [tg/kg/hr, or between about 0.005 jag/kg/hr and about 0.25 jag/kg/hr. In a preferred non-limiting embodiment, the premi xed dexmedetomidine composition is administered as a loading dose followed by a 15 maintenance dose, wherein the loading dose is about I pg/kg/hr for a period of about 10 minutes, followed by a maintenance dose of between about 0.2 pg/kg/hr to about I pg/kg/hr, more preferably, between about 0.2 pg/kg/hr to about 0.7 pg/kg/hr. In other preferred non-limiting embodiments, the premixed dexmedetomidine composition is administered as a loading dose followed by a 20 maintenance dose, wherein the loading dose is about 0.5 pg/kg/hr for a period of about 10 minutes, followed by a maintenance dose of between about 0.2 pg/kg/hr to about I pg/kg/hr, more preferably, between about 0.2 pg/kg/hr to about 0.7 pg/kg/hr. In certain non-limiting embodiments, the dosage of premixed dexmedetonidine composition administered as a single continuous, loading or 25 maintenance dose, is titrated until a desired effect is achieved. In some patients, the quality of the sedation achieved by administering the premixed dexmedetomidine composition of the present invention can be unique. In one non-limiting example, a patient sedated by the premixed dexmedetomidine composition is arousable and oriented. The patient can be awakened and is able to 30 respond to questions. The patient is aware and can tolerate an endotracheal tube. Should a deeper level of sedation be required or desired, an increase in dose of the composition of the invention can be administered to transit the patient into a deeper level of sedation. NY02:746896.1 - 18 - 077350.0356 In certain non-limiting embodiments, the compositions of the invention can be administered to non-ventilated patients who require sedation, anxiolysis, analgesia, or hemodynamic stability in an amount to achieve a sedative, anxiolytic, analgesic or hemodynamic stabilizing effect in the patient. 5 5. EXAMPLES The following examples are merely illustrative of the presently disclosed subject matter and they should not be considered as limiting the scope of the 10 invention in any way. EXAMPLE 1: Selection of Packaging Components for the Premixed Dexmedetomidine Pharmaceutical Composition In order to identify suitable primary packaging components for the 4 15 pg/mL premixed dexmedetomidine composition in 0.9%NaCl, stability studies were conducted in various configurations including glass vials, ampoules, plastic flexible containers (CR3 elastomer copolyester ether containers (Hospira, Inc., Lake Forest, IL), PVC and VisIVTM plastic containers (Hospira, Inc., Lake Forest, IL)), and Ansyr@ syringes (H-ospira, Inc., Lake Forest, IL). A batch of premixed 20 dexmedetomidine composition was prepared at the premix concentration of 4 pg/mL, in 0.9% NaCl. Solution was filled into 20 mL ampoules, 50 mL glass vials, 100 mL PVC flexible containers, 100 mL CR3 elastomer copolyester ether flexible containers (Hospira, Inc., Lake Forest, IL), 50 mL VisIVTM plastic (Hospira, Inc., Lake Forest, IL) flexible containers, and 10 mL Ansyr@ syringes (Hospira, Inc., Lake Forest, IL), 25 and all configurations were autoclaved. The pH and potency (using HPLC method) of the sterilized samples were determined. The stability of the autoclaved samples under accelerated conditions (40'C/75%RH) was also evaluated over a period of 5 months (Table 1). Potency was evaluated using a HPLC method. Post sterilization 30 potency values ranged from 73-88%. The solution pHs varied from 4.7-6.2 following an in-process result of 6.0. Two weeks samples stored under ambient conditions were tested for pH, potency and related substances. The two weeks potency results were considered as time zero results because the 4 pg/mnL formulation remains stable at room temperature for more than 2 weeks. Comparison of potency results at time zero NY02:'746896.1 - 19 - 077350.0356 in different configurations indicated a drop in potency of premixed dexmedetomidine composition filled in CR3 elastomer copolyester ether bags (Hospira, Inc., Lake Forest, IL) and VisIV T 1 plastic bags (Hospira, Inc., Lake Forest, IL), after sterilization (Table 1). 5 The stability of the autoclaved samples under accelerated conditions (40'C/75%RFI) was also evaluated over a period of 5 months (Table 1). After five months under accelerated conditions the potency of the premixed dexmedetomidine composition in glass ampoules and vials remained at about 98% while that in the syringe was found to be about 90%. In PVC and CR3 elastomer copolyester ether 10 bags (Hospira, Inc., Lake Forest, IL), after the initial potency loss no further loss of potency was observed during the five month period. Table 1: 4 pg/mL Premixed Dexmedetomidine Composition in Normal Saline Formulation Stability 2 1 2 3 5 Week/2 Month/ Month/ Month/ Month/ 5"C 40"C 40"C 40"C 40"C Avg Avg Avg Avg Avg P otency Potency Potency Potency P otency (%) pH (%) pH (%) (%) (%) Ampoule 99.0 5.0 99.0 5.6 97.7 98.3 987 Vial 8. 2 6.7 99.4 6.3 98.0 98.3 98.6 Syringe 95.0 5.5 94.6 5.7 92.2 89.5 90.8 CR3 80.2 4.7 79.5 4.8 NT 753 792 PVC 79.9 4.8 81.4 4.6 NT 790 767 Vis-IV
T
M 95.8 5.9 92.8 5.8 NT 94.0 NT 15 NT - Not tested NY02:746896.1 -20- 077350.0356 The cause of potency loss in PVC bags and CR3 elastomer copolyester ether bags (Hospira, Inc., Lake Forest, IL) during autocl having was investigated. Related substances testing on autoclaved premixed dexmedetomidine composition filled in PVC and CR3 elastomer copolyester ether bags (Hospira, Inc., Lake Forest, 5 IL) revealed that potency drop did not occur due to degradation, because the total percent of impurities was much less than 20% (Table 2). Loss of potency may be due to either adsorption (restricted to the surface of the flex bag) and /or absorption (not restricted to the surface) of the drug in to the flex bags. To confirm the absorption/adsorption phenomena, the CR3 elastomer copolyester ether bags 10 (Hospira, Inc., Lake Forest, IL) and PVC bags that showed 20% potency loss were emptied and rinsed with MeOH. The rinse solvent was tested for dexrmedetomidine. Nearly all the drug was recovered from CR3 elastomer copolyester ether bags (Hospira, Inc., Lake Forest, IL) - indicating adsorption and only 1 % of the drug was recovered from PVC bags - indicating absorption, since drug dissolves in DEM3. 15 The related substances results indicated that premixed dexmedetomidine composition in VisIVTM plastic bags (Hospira, Inc., Lake Forest, IL) had high impurity levels (Table 2), higher than levels observed in ampoules, vials, syringes, PVC bags and CR3 elastomer copolyester ether bags (Hospira, Inc., Lake Forest, IL). 20 Table 2: Impurity Results for 4 [tg/mL Premixed Dexmedetomidine Composition 2 week/25"C I Month/40"C Total impurity (%) Total impurity (%) Ampoule 0.66% 0.54% Vial 0.02% N1 Syringe 0.49% 1.48% CR3 2.61% 5.88% PVC 2.26% NT VisIV TM 19. 08 % 7.02% EXAMPLE 2: Development in ADDVantage@ PVC (Hospira, Inc., Lake Forest, IL) Admixture System 25 In this study three 250 ml- ADDVantage@ PVC bags (Hospira, Inc., Lake Forest, IL) were spiked with 10 mL of dexmedetomidine concentrate (100 NY02:746896.1 -21 - 077350.0356 ptg/mL) to obtain a final concentration of 4 pg/mL. As a control, a glass bottle was spiked in the same manner. Upon thorough mixing of the samples, an aliquot was withdrawn for subsequent potency analysis. The bag was then allowed to sit on the bench top for various interval testing. The results showed that there is a drop in 5 potency after the initial mixing period and a slight decrease thereafter (Table 3). Table 3: 4 .Lg/mL Premixed Dexmedetomidine Composition ADDVantage@ PVC bag (Hospira, Inc., Lake Forest, IL) Admixture Study Time Following Admixture % Loss from Control* Immediately 5.3 4 Hours 5.6 8 Hours 6.0 24 Hours 5.5 48 Hours 5.8 72 Hours 6.0 7 Days 6.1 Average of three spiked bags compared to glass bottle. 10 EXAMPLE 3: Modification of the Premixed Dexmedetomidine Composition Formulation The pH of the premixed dexmedetomidine composition formulation 15 can affect the adsorption of dexmedetomidine molecule. The free base form of dexmedetomidine is more adsorptive. At lower p-I -- 4.0, most of the dexmedetomidine is in the ionized form, which minimized adsorption and thereby loss in potency. Buffered formulations were tested to detennine whether loss of potency in flex bags can be minimized. NY02:'746896.1 - 22 - 077350.0356
CH
3
CH
3 CH 3
CH
3 N OH 3 N CH 3 N pKa - N H2+ H Buffered formulations were prepared at different pHs 3.0, 3.4, 4.0, and 4.5 using acetate, citrate, lactate and ascorbate buffer. Since the pKa for dexmedetomidine is about 7.1, at this pH the molecule might be protonated 5 sufficiently to retard adsorption. Post-autoclave potency values dropped approximately 10% in all instances; this was an improvement from the 20% decrease observed in the unbuffered formulation in Example 1. In a second study, additives were formulated with the premixed dexmedetomidine composition to prevent adsorption of the dexmedetomidine to CR3 10 elastomer copolvester ether (-lospira, Inc., Lake Forest, IL). The following additives were tested: ethyl alcohol, benzyl alcohol, methyl paraben, propyl paraben, PEG 1000, polysorbate 20 and 80, propylene glycol. Formulations prepared included additives in both buffered and unbuffered premixed dexmedetomidine composition. Both these reformulation strategies reduced potency loss. 15 Stability testing of the 4 pig/mL premixed dexmedetomidine composition (unbuffered saline formulation), in glass vials and ampoules stored at 25 C, after 9 months was performed. Potency remained relatively unchanged from initial measurements. Additionally., the largest single impurity detected in the samples was present at a concentration of 0.06%. 20 EXAMPLE 4: Stability of the Premixed Dexmedetomidine Composition The stability of dexnedetomi dine hydrochloride to acidic, basic, oxidative and photolytic stress was examined. In order to demonstrate the resiliency 25 of dexnedetomidine, even when present in extremely low levels (ppm or ptg/mL levels), dilute solutions of dexmedetomidine (approx. 13.3 [tg/mL) were separately subjected to acidic, basic, oxidative and photolytic stress and then diluted with 0.9% Sodium Chloride to a final nominal concentration of 4 pag/mL and assayed by [IPLC NY02:7468596.1 - 23 - 077350.0356 with a photodiode array (PDA) detector for spectral peak purity analysis. Each sample was injected in duplicate. The stress conditions are listed in Table 4. Table 4: Stress Conditions Stress Condition Description 5.0 mL of a 40 pg/mL stock Dexmedetomidine Hydrochloride solution* and 10 mL of 5N Hydrochloric Acid were added to 20 mL scintillation vial. The vial was placed in an oven at 60'C for 8 Acid hours. The solution was then diluted with 0.9% NaCI to 4 pg/mi.. 5.0 mL of a 40 pg/mL stock Dexmedetomidine Hydrochloride solution* and 5 niL of 2N Sodim Hydroxide were added to 20 mL scintillation vial. The vial was placed in an oven at 60'C for 4 Base hours. The solution was then diluted with 0.9% NaC to 4 ptg/mL. 5.0 mL. of a 40 pg/mL stock Dexmedetomidine Hydrochloride solution* was added to 20 mL scintillation vial. The vial was placed in an oven at 60'C for 8 hours. The solution was then diluted with Thermal 0.9% NaCl to 4 [tg/mL. 5.0 mL of a 40 pg/mL stock Dexmedetomidine Hydrochloride solution* and 5 mL of 0.3% Hydrogen Peroxide were added to 20 mL scintillation vial. The vial was placed in an oven at 60'C for 8
H
2 0 2 hours. The solution was then diluted with 0.9% NaCi to 4 pag/mL. 5.0 mL of a 40 pg/mL stock Dexmedetomidine Hydrochloride solution* were added to 20 mL scintillation vial and placed into a photochemical reaction unit for 24 hours. The solution was then Light diluted with 0.9% NaCl to 4 p g/mL. 5.0 mL of a 40 ptg/mL stock Dexmedetomi dine Hydrochloride solution* was added to 20 mL scintillation vial. The vial was not subjected to any stress condition. The solution was then diluted Control with 0.9% NaCI to 4 ug/mL. 5 * Stock solution of dexnedetomidine -ICI was prepared in 0.9% NaCi solution. NY02:'746896.1 - 24 - 077350.0356 The peak purity analysis shows that under all stress conditions the parent peak were spectrally pure, attesting to the assay being performed under conditions of specificity. See Table 5 for Potency Results. Under oxidative conditions, the sample showed highest amount of 5 degradation (12.7%) compared to the control sample. Appropriate precautions are taken during manufacturing and packaging to prevent oxidative stress. Thermal stress studies indicate that the premixed dexmedetomidine composition is stable at high temperature. It is also confirmed by accelerated stability studies, wherein potency values remained within shelf life specifications over a period 10 of 6 months. Moreover the premixed dexmedetomidine composition is a terminally sterilized product. Hence, it is expected that premixed dexmedetomidine composition would remain stable if exposed to temperature excursions during transportation or storage. 15 Table 5: Forced Degradation Results Samples ID Assay Control Sample 98.4% Acid Sample 95.2% Base Sample 93.8% Heat Sample 98.4% Oxidation Sample 85.7% Light Sample 92.0% EXAMPLE 5: Manufacture of the Premixed Dexmedetomidine Composition Formulation 20 A 4 ig/mL premixed dexmedetomidine composition can be manufactured according to the following process: Water for Injection is added to a mixing tank to approximately 110% of the final volume and heated to 80'C. Nitrogen sparging in the tank is started and maintained throughout the manufacturing process. 25 Water for Injection is then cooled and a sufficient amount of water is withdrawn from the tank to leave approximately 90%/0 of the final volume in the mix tank. NY02:746896.1 - 25 - 077350.0356 Dexmedetomidine HCI is then added to the tank and mixed for not less than 15 minutes. Sodium chloride is then added and mixed. The solution is then divided into batch size. An in-process sample is then evaluated for pH and potency. The nitrogen protection is maintained. 5 Filteri ng of dexmedetomidine composition The dexmedetomidine solution is filtered prior to filling in a clinician useable container. For the 20 mL batches, solution is filtered through Pall NIylon 66, 0.45 im filter membrane with a pre filter. For 50 and 100 mL batches, solution is 10 filtered through Nylon 66, 0.22 pm filter membrane with a pre filter. A filter compatibility study was performed using Pall Nylon 66 0.45 pum filter. It was determined that filters had little to no impact on the premixed dexmedetomidine composition product after 52 hours of recirculation. The prolonged exposure of these filter materials did not produce any significant potency or pH changes in the drug 15 product (See Table 6). Additionally, there was no change in bubble point for the filters before and after exposure. Table 6: Filter compatibility testing Time Sample Tested Pall Nylon 66 filter (Pall Corp., Port Washington, NY) Potency (%) pH Pre-filtration Tank (0 hr) 99.8 6.30 5 minute static filter hold 97.3 6.01 sample One hour tank 994 6.17 Six hour tank 99 1 6.18 Eight hour tank 99.2 6.23 25 hour tank 98.9 6.24 52 hour tank 993 6.17 Nitrogen protection during filling 20 The transfer line from solution manufacturing to filling is optionally flushed with filtered nitrogen gas prior to filling. The filling equipment, including all lines are purged with nitrogen before starting to fill the product. An atmosphere of NY02:746896.1 - 26 - 077350.0356 filtered nitrogen gas is maintained in the headspace of the surge bottle. After filling, the headspace of the container is gassed with nitrogen to achieve not more than 5% of oxygen in the headspace. Hold Time 5 The following time limits will be applied to manufacture of the subject drug product: Total time for filtration and filling: NMT (Not More Than) 16 hours Total time for manufacturing (from compounding to end of filling): NMT 24 hours 10 Sterilization The premixed dexmedetomidine composition is terminally sterilized. Vials filled with the composition are autoclaved using 15 - 30 minutes exposure at 121 - 1240C. Container closure system 15 The 4 ug/mL premixed dexmedetomidine composition can be manufactured in three configurations: 20 mL fill in 20 mL vial, 50 mL fill in 50 mL vial and 100 mL. fill in 100 mL vial. Examples of packaging components for the 20 mL, 50 mL and 100 mL configurations are listed in Tables 7, 8, and 9 below. 20 Table 7: Container Closure System for 4 ug/mL Premixed Dexmedetomidine Composition, 20 mL Primary Packaging Materials Kimble USP Type 1, Clear Tubing Glass Vial, Sulfur-Treated, 20 mm, 20 mL (Kimble Chase, Vineland, NJ) West 4432/50 Teflon 2 coated Gray rubber Closure (Stopper), 20 mm (West Pharmaceutical Services, Inc.) Seal, Flip-Off@ (Blue or Gray) elastomer stoppers, 20 mm (West Pharmaceutical Services, Inc., Lionville, PA) Table 8: Container Closure System for 4 pg/mL Premixed Dexmedetomidine Composition, 50 mL Primary Packaging Materials Gerresheimer USP Type 1, Glass Vial (Bottle), Sulfur-Treated, 28 mm, 50 mL NY02746896.1 - 27 - 077350.0356 (Gerresheimer Glass Inc., Vineland, NJ) Helvolet FM 259/0 Gray with OmniflexPlus@ Fluoropolyier coating Rubber Closure (Stopper), 28 mm (Helvoet Pharma, Datwyler USA, Pennsauken, NJ) Aluminum Seal, Overseal Assembly, 3 piece, 28 mm Table 9: Container Closure System for 4 pg/mL Premixed Dexmedetomidine Composition, 100 mL Primary Packaging Materials Gerresheimer USP Type 1, Glass Bottle, Sulfur-Treated, 100 mL (Gerresheimer Glass Inc., Vineland, NJ) Helvolet FM 259/0 Gray with OmniflexPlus@ Fluoropolymer coating Rubber Closure (Stopper), 28 mm (Helvoet Pharma, Datwyler USA, Pennsauken, NJ) Aluminum Seal, Overseal Assembly, 3 piece, 28 mm 5 Batch Formula Examples of qualitative and quantitative batch formula for a registration batch and a commercial batch for a 4 p.g/mL premixed dexmedetomidine (dexmedetomi dine hydrochloride) composition, for a 20, 50, and 100 mL presentation are presented in Tables 10 and II below. 10 Table 10: Batch Formula for 4 pg/mL Premixed Dexmedetomidine Hydrochloride Composition, 20 mL Registration Maximum Component Stability Batch Commercial Batch Size: Size: Dexmedetomidine HCl 2.832 mg 25.96 mug Sodium Chloride 5.4 g 49.5 g Water for Injection USP q.s. to 600 Liters q.s. to 5500 Liters Nitrogen NF 3 A R. A.R. 15 q.s. = Quantity sufficient NY02:'746896.1 - 28 - 077350.0356 A.R. = As required Factored to 100% basis. The final pH range of the finished product is 4.5 - 7.0. Nitrogen is used to displace air during manufacturing (i.e. to blanket the formulation and to fill the vial headspace). Table 11: Batch Formula for 4 pg/mL Premixed Dexmedetomidine Hydrochloride Composition, 50 & 100 mL Registration Maximum Component Stability Batch Commercial Batch Size: Size: Dexmedetomidine HCl 4.72 mg 33.04 mg Sodium Chloride 9 g 63 g Water for Injection USP q.s. to 1000 Liters q s to 7000 Liters Nitrogen NF A R. A.R. q.s. = Quantity sufficient A.R. = As required 10 Factored to 100% basis. The final pH range of the finished drug product is 4.5 - 7.0. Nitrogen is used to displace air during manufacturing (i.e. to blanket the forimiulation and to fill the vial headspace). 15 In-Process Specification Examples of in-process controls during the manufacturing process for the 4 Pg/mL premixed dexmedetomidine composition are presented in Table 12. NY02:'746896.1 - 29 - 077350.0356 Table 12: In-Process Specification In-Process In-Process Unit Operation Control/Test Procedures or Methods Limit Solution Preparation pH USP <791> 4.5-7.0 (Compounding) Assay HPLC 94 - 106/ Perform fill Weight/volume weigh t/volume checks per Meets Filling Process control SOP requirements An example of final product limits for physical, chemical, and biological testing of 4 pg/mL premixed dexmedetomidine composition are listed in the Table 13. 5 Table 13 Premixed Dexmedetomidine Composition Specifications Test Acceptance Criteria Solution is clear. Solution does not contain one or more Clarity particles visible upon attentive inspection 90.0% - 110.0% Assay (9.00 mg/mL - 1.10 mg/mL) Color Colorless pH 4.5 - 7.0 Label Claim Acceptable Range 20 mL 20.5 - 22.5 mL 50 mL 50.0 - 54.5 mL Volume 100 mL 102.0 - 10.8.0 mL Optical Purity NMT 1.0% Related Substances: A. Individual A. NMT 0.5% B. Total B. NMT 1.0% 90.0% - 110.0% Sodium Chloride (8.1 mg/mL - 9.9 mg/mL) NMT 25/mL 3 10 mm Particulate Matter NMT 3/m L 3 25 mm Sterility Meets USP requirements Bacterial Endotoxin NMT 0.08 EU/mL NY02:746896.1 - 30 - 077350.0356 EXAMPLE 6: Stopper Selection for Glass Vials The objective was to have three presentations of Precedex@ (dexmedetomidine hydrochloride, Hospira, Inc., Lake Forest, IL) premix Injection 4 ug/mL: 20 mL, 50 mL and 100 mL. Precedex) concentrate Injection 100 ig/mL is currently marketed in 2mL glass vial with West 4416 Teflon coated elastomer stopper (West Pharmaceutical Services, Inc., Lionville, PA). Uncoated infusion stoppers, were evaluated. 28 mm Helvoet 5330 10 rubber stopper (1-lelvoet Pharma, Datwyler USA, Pennsauken, NJ), EDPM rubber stoppers (EPSI, Franksville, WI) and West 4432 elastomer stoppers (West Pharmaceutical Services, Inc.) were investigated. During feasibility testing loss of potency and stopper extractables were observed. The performance of coated stoppers was compared with that of uncoated stoppers (West 4432 and Helvoet 5330) by 15 conducting feasibility studies on West 4588/40 FluroTec) elastomer stoppers (West Pharmaceutical Services, Inc., Lionville, PA). Results showed a clear benefit to using a coated stopper vs. the uncoated stopper. The potency remained stable with the coated stopper. Hence for Precedex@ Injection, it was planned to implement coated stoppers in order to mimic the current product and prevent any drug adsorption. 20 Helvoet FM 259/0 OmniflexPlus@ fluoropolymer coated rubber stoppers (Helvoet Pharma, Datwyler USA, Pennsauken, NJ) were evaluated. Chemical compatibility testing was favorable; upon autoclave no change in potency or pH1 was observed and no significant amount of impurities detected. The OmniflexPlus@ coated stopper from Helvoet, was examined for determining the self 25 sealing characteristics of the stopper when penetrated multiple times with hypodermic needle. This is a dye ingress test. The new stopper/vial/3-piece overseal combination passed this test. Helvoet OmniflexPlus@ coated stopper passed the Rocky Mount pressure test at the required 80 psi criterion. These stoppers, vials and overseals were also evaluated by Tech Ops for functional testing to confirm that the stoppers can be 30 pierced without being pushed into the vial. All testing indicated that the stoppers are acceptable for use. Feasibility stability studies were conducted by preparing a batch of Precedex@ Injection 4 ig/mL and filling into 50 mL vials with the Helvoet OmniflexPlus@ stoppers followed by autoclaving. Samples were stored under NY02:746896.1 -31- 077350.0356 accelerated (40 C/75% relative humidity, inverted) and long term (25C/60% relative humidity) conditions. Initial testing showed no loss in potency, no change in pH-, and virtually no measurable impurities. The I month stability testing of samples stored inverted at 40C showed slight drop in potency (2%). This trend in potency drop 5 continued at 2 months under accelerated conditions with further 2% drop in potency. After 3 months under accelerated conditions the potency values remain unchanged as compared to that of 2 months, indicating that potency values have leveled off. Similar trend in drop of potency during the first three months of storage was observed for long term stability conditions (25 0 C/60% relative humidity) but the percent drop was 10 less. The total percent drop in potency over three months under long term conditions was 1.1%. Stability testing at 4 and 5 months for samples stored under accelerated and long term conditions confirmed that potency values had almost leveled off, with small drop in potency values. During I month impurity testing numerous small impurity peaks that totaled over 0.5% of the drug peak were observed. A placebo batch was 15 prepared to confirm whether the peaks are related to the stopper or the drug. Results indicated that impurities were related to the stopper. Plastic vials were also evaluated for Precedex@V premix Injection 4 meg/mI. Two types of plastic vials were used: CZ resin and poly propylene vials. West 4432 Teflon coated 20 mm elastomer stopper (West Pharmaceutical Services, 20 Inc.) was used for both the plastic vials. The pH, potency and impurities of Precedex@7 Injection 4 mcg/mL filled in plastic vials and stored under accelerated conditions over a period of 3 months was determined. Similar trend in potency drop was observed. The total % impurities were found to increase over a period of 3 months for both CZ resin vials and polypropylene vials, but the total % of impurities of CZ resin vials was 25 less than that of polypropylene vials. CZ resin vials were found to better as compared to polypropylene vials in terms of drop in potency and total impurities. Since the drug is present at such a low concentration 4 pg/mL, even ppb levels of impurities would have a significant contribution toward the impurity limit. Moreover the Precedex@ related substances method was developed to detect 30 organic impurities at ppb levels. This method requires detection at non-discriminating low wavelength of 210 nm and high injection volume of 500 1., which render it highly sensitive to detect any organic impurity, including stopper extractables. NY02:746896.1 - 32 - 077350.0356 Extractables West 4432/50 Teflon 2 coated elastomer stoppers (West Pharmaceutical Services, Inc.) 5 The West 4432/50 Teflon 2 coated elastomer stopper, 20 mm is used for Precedex@ Injection 4 pg/mL, 20 mL presentation. The stoppers have been qualified for use based on the results of compendial biological, physiochemical and other characterization tests. The related substance testing of Precedex@ Injection has not shown any unidentified peaks that exceed the specification of NMT 0.2%, 10 suggesting that extractables are not an issue for Precedex@ Injection in this container closure system. Helvoet FM 259/0 Omniflex@ fluoropolymer coated rubber stoppers (Helvoet Pharma, Datwyler USA, Pennsauken, NJ) 15 The Helvoet Omniflex@ fluoropolymer coated FM259/0 gray bromobutyl 28 mm rubber stoppers (Helvoet Pharma, Datwyler USA, Pennsauken, NJ) (ready-to-use) are used for Precedex@ Injection 4 pg/mL, 50 and 100 mL presentations. The stoppers have been qualified for use based on the results of compendial biological, physiochemical and other characterization tests performed 20 During related substances analysis of the exhibit batches of Precedex@ 4 g/rnL Injection, unidentified impurity peaks were observed in chromatograms of 50 and 100 mL presentation samples. During investigation of the source of chemical constituents responsible for the 'unidentified impurity peaks', it was found that these peaks also appeared in chromatograms of 0.9% NaCl placebo formulation filled into 25 50 mL vials with 1-elvoet FM259/O rubber stoppers (Helvoet Phanna, Datwyler USA, Pennsauken, NJ), but were absent in those of 0.9% NaCl placebo formulation filled into glass ampoules. Additionally identical peaks were observed in chromatograms of Helvoet FM259/O rubber stopper (Helvoet Pharma, Datwyler USA, Pennsauken, NJ) extract solution analyzed by Precedex@ related substances 30 method. The extract was prepared by autoclaving (12 VC for 60 minutes) 30 stoppers in 300 mL purified water, yielding an extract of 2 cm2 stopper surface area per mL water. The results from these investigative studies confirmed that 'unidentified impurity peaks' observed at specific relative retention times were not dexmedetomi dine HCI related, but were extractables from Helvoet rubber stoppers NY02:746896.1 - 33 - 077350.0356 used in the container/closure system. It was expected that stopper extractables would be detected at such low limits of detection, i.e. ppb levels, as a highly sensitive LC UV 210 nm related substances method was used for a highly potent very low concentration (4 ptg/mL) product. 5 The chemical constituents responsible for peaks in specific relative retention times were determined to be extractables from 28 mm Helvoet FM259/O rubber stoppers (Helvoet Pharma, Datwyler USA, Pennsauken, NJ), part of container closure system for Precedex@ Injection 50 and 100 mL. Moreover no peaks were found in these specific relative retention times in chromatograms of forced 10 degradation samples of dexmedetomidine HCI or Precedex@ Injection filled in ampoules. Hence in the calculation of single largest related substance and total related substances, peaks in relative retention time ranges: 0.71-0.80, 1.10-1.30, 1.50-1.80 are excluded. In an effort to quantify the highest levels of observed individual 15 extractable and total extractable, dexmedetomidine HCI was used as a surrogate standard for all stopper extractables. Since, the Helvoet FM259/O rubber stopper (Helvoet Pharma, Datwyler USA, Pennsauken, NJ) extractables responsible for the peaks in Precedex@ related substances profile could not be identified. Through 6 months stability testing the highest % of extractables was observed in Precedex@ 20 stability samples stored at 30C/65% relative humidity for 3 months. The largest individual extractable % peak area was found to be 0.95% or 38 ppb and total extractable % peak area, calculated by adding the % peak areas of all the peaks in the RRT of 0.71 - 0.80, 1.10 - 1.30, 1.55 - 1.80, was found to be 2.7% or 108 ppb. Helvoet FM259/O rubber stoppers (Helvoet Pharma, Datwyler USA, 25 Pennsauken, NJ) passed the 'Elastomeric Closures for Injections' testing. As per Helvoet technical documentation the total amount of extractables was determine to be 0.8 mg/100 mL or 8 ppm for a total surface area of 100 cm> The surface area of a 28 mm Helvoet stopper is approximately 6.45 cm2 , the total acceptable amount of extractable for each 28 mm Helvoet FM259/O rubber stopper (Helvoet Pharma, 30 Datwyler USA, Pennsauken, NJ) on an average would be 0.05 mg/100 mL or 500 ppb. Additionally as per SP the total organic content of purified water should not exceed 0.5 mg/L or 500 ppb. The highest levels of observed extractables in Precedex® Injection are at least 5 times lower than the acceptable levels of NY02:746896.1 - 34 - 077350.0356 extractable in purified water and acceptable levels of extractable in the qualified [Helvoet stoppers. USP 'In vitro cytotoxicity test' and USP 'Intracutaneous test and systemic injection test' were performed on Helvoet stopper extracts. The results show 5 that stoppers meet the requirements of these tests, confirming the safety of the stoppers and any stopper related extractables. The 'In vitro cytotoxicity test' was repeated for Helvoet 28 mm stoppers that were used in the exhibit batch to demonstrate the safety of the stoppers. The stopper extract was prepared by autoclaving the stoppers at 121 0 C for I hour in 0.9% NaCl yielding an extract of 2 10 cm2 stopper surface area per mL water. This extraction condition closely mimics Precedex@ Injection manufacturing conditions and also meets the extraction requirements of USP 'In vitro cytotoxicity test' testing . Precedex@ injection is formulated in 0.9% NaCl and the final product i.e. Precedex@ Injection in container closure is autoclaved at 121 C for 20 --- 40 minutes. Additionally while investigating 15 the source of 'unidentified impurity peaks' Helvoet FM259/O rubber stopper (Helvoet Pharma, Datwyler USA, Pennsauken, NJ) aqueous extracts were prepared by autoclaving the stoppers at 121 C for one hour and then tested by the Precedex@ related substances method. The results demonstrated that the chemical constituents responsible for the peaks were also present in the Helvoet FM259/O rubber stopper 20 (1elvoet Pharma, Datwyler USA, Pennsauken, NJ) aqueous extracts. The stoppers passed the USP 87 testing indicating that the stopper extractables are non cytotoxic. According to Helvoet Pharma, 1-lelvoet FIM259/O Omniflex@ fluoropolymer coated rubber stoppers (Helvoet Pharma, Datwyler U SA, Pennsauken, NJ) have been used for other marketed products, and there have been no reported 25 cases of toxicity issues arising due to stopper extractables. Identification of extractables Diligent efforts were made to characterize and identify the 30 extractables. Helvoet's extractables report lists a number of potential extractable compounds. From Helvoet's list, the most likely to be responsible for the peaks observed in the Precedex® chromatograms were selected: - BHT Irganox- 1076 NY02:746896.1 -35 - 077350.0356 - Irganox-1010 - Stearic Acid - Palmitic Acid - Sulphur 5 Samples of these compounds were obtained, and solutions were prepared and injected into an HPLC using the Precedex@ related substances method. None of these compounds matched the relative retention time of the stopper extractable peaks in Precedex@ sample chromatograms. In general, the substances listed above are all too hydrophobic (retained too long on the C1 column with the 10 isocratic mobile phase that is used for the method, 40% aqueous phosphate buffer pH 7.0 /60% inethanol). Since these peaks were also observed in the chromatograms of Helvoet FM259/O rubber stopper (Helvoet Pharma, Datwyler USA, Pennsauken, NJ) extract solution, a concentrated stopper extract solution was prepared by first by autoclaving 15 a large number of stoppers in purified water, and then concentrating the extract by liquid-liquid extraction into dichloromethane and then rotovaping and re-suspending the residue into a small volume of methanol/water. LC-UV analysis of this concentrated stopper extract show the same peaks of interest as observed in Precedex@ chromatogram, but at much higher levels (approx 100 times larger peak 20 size). This concentrated extract solution was then analyzed by LC-MS using the Waters Q-TOF instrument with the electrospray source in positive ion mode and observed at least one of the peaks of interest in the mass spec TIC chromatogram; the mass spectrum of the peak has been obtained and appears to have what might be the molecular ion peak at m/z 158; exact mass analysis of this peak and its pattern of 25 isotope peaks predicts some empirical formulas. Compounds with these empirical formula and known usage in the rubber industry were tested but without success. Solvent extracts of the stoppers were prepared and analyzed by gas chromatography-mass spectrometry. Analysis revealed the presence of two low molecular weight rubber oligomers previously reported by Helvoet. These oligomers 30 are not commercially available for identification confirmation; however, their hydrophobic character makes it unlikely that they would elute near dexmedetomi dine in the related substances HPLC method. A pure extractable sample was isolated by combining multiple fractions collected from repeated -PLC separations of a stopper extract. Attempts to NY02:746896.1 - 36 - 077350.0356 obtain an EI+ mass spectrum by direct probe mass spectrometry and gas chromatography-mass spectrometry were unsuccessful, suggesting that the stopper extractable is nonvolatile and possibly thermally labile. The pure extractable sample was analyzed by IR. and elemental 5 analysis. Both of these techniques suggested that the extractable contains only carbon, oxygen and hydrogen. No indication of nitrogen, sulfur or any other heteroatom was observed. The chemical additives that perform variety of functions, including plasticizers, fillers, etc are the most significant source of chemical entities observed as 10 extractables. There are several reasons which makes identifying the extractables challenging and at times impossible. Each functional additive category contains representatives from several molecular structures. For example, consider the category of antidegradants, subcategory antioxidants, which includes aromatic arines, sterically hindered phenols, phosphites, phosphonites, and thioethers. To further 15 complicate the picture, chemical additives are often not pure compounds but mixtures of related structures. For examples "Abietic Acid" which is an organic chemical filler used in certain types of rubber, in reality is a complex mixture of chemical entities, all of which could appear as extractables/leachables. Chemical additives can also react and degrade within the rubber/polymer matrix during or subsequent to compounding 20 process. As an example of this consider, the trivalent phosphorus, or phosphate antioxidant, a common tradename for which is lrgafos 168. This compound reacts with and thereby destroys oxidizing agents, such as hydroperoxides, to form the corresponding pentavalent phosphorus species, or phosphate. In addition to the foregoing, the following must also be considered 25 when analyzing extractables/leachables: -Monomers and high molecular weight oligomers derived from incomplete polymerization reactions. - Surface residues, such as heavy oils and degreasing agents on the surface of metal canisters and containers. 30 - Chemical additives on the surfaces of container closure component fabrication machinery, such as mould release agents, antistatic and antislip agents, etc. * * * NY02:'746896.1 - 37 - 077350.0356 The present invention is not to be limited in scope by the specific embodiments described herein. Indeed, various modifications of the invention in addition to those described herein will become apparent to those skilled in the art from the foregoing description. Such modifications are intended to fall within the 5 scope of the appended claims. Patents, patent applications, publications, product descriptions, and protocols are cited throughout this application, the disclosures of which are incorporated herein by reference in their entireties for all purposes. 10 NY02:'746896.1 - 38 -