Multimediator transporter inhibitors for use in treatment of central nervous system disorders
A technology of inhibitors and transporters, applied in nervous system diseases, data processing applications, metabolic diseases, etc., can solve problems such as side effects, intolerance, inability to prevent or cure
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[0159] Dosage form matrices can be prepared by methods known in the polymer art. In one method of preparation, 3-5 or more casting compositions are prepared independently, wherein each casting composition contains increasing doses of drug covering each composition from low to high doses. This produces a series of layers that together form a unit polymer matrix with a concentration gradient. In another method of preparation, higher doses are prepared first, followed by layering with layers of decreasing doses, resulting in a polymer matrix with a drug concentration gradient. An example of preparing a dosage form includes mixing a pharmaceutically acceptable carrier such as polyethylene glycol with a known dose of inhibitor, incorporating it into a silicone rubber medical grade elastomer with a crosslinking agent such as stannous octoate, followed by casting in a mold. Repeat this step for subsequent layers.
[0160] The system is allowed to run, for example, for 1 hour, resul...
Embodiment 1
[0314] Example 1: Antagonism and functional activity of dopamine receptors or transporters
[0315] The functional activity of compounds is determined in vitro in cellular assays using recombinant human cell lines. According to the method of Gu et al. (J.Biol.Chem.269:27124, 1994), the functional activity of serotonin uptake inhibition was determined in human HEK-293 cell line, with fluoxetine (EC 50 =57nM) was used as a reference compound. According to the method of Galli et al. (J.Exp.Biol.198:2197,1995), the functional activity of norepinephrine uptake inhibition was determined with MDCK cell line, and desipramine (EC 50 =7nM) was used as a reference compound. To determine dopamine functional activity, the hDAT cell line was used as described by Giros et al. (Mol. Pharmacol. 42:383, 1992), with nomifensine (EC 50 =11 nM) was the reference compound.
[0316] Table 1, human (h) and rat (r) in vitro functional absorption distribution profiles
[0317] compound
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Embodiment 2
[0335] Example 2: In vivo potency of several exemplary dopamine transporter inhibitors
[0336] The in vivo potency of several exemplary inhibitors (1), (3) and (4) of the invention was determined using a standard forced swim test model in rats. The aim of this study was to evaluate the antidepressant effect of test compounds in a behavioral despair assay in rats using a modified method described in: Porsolt R.D.etal.in Behavioral despair in rats: a new model sensitive to antidepressanttreatment, Eur.J Pharmacol., 47:379-391, 1978; Porsolt et al., Nature 266:730-732, 1977; and Porsolt et al., in Psychopharmacology, Olivier, Mos, and Slangen (eds) Birkhauser Verlag, Basel, pp. .137-159, 1991. In simple terms, when mice (or rats) are forced to swim within a cylinder from which escape is impossible, they readily adopt a characteristic immobility posture and no longer attempt to escape, except for requiring small movements to remain afloat. Immobility has been suggested to refle...
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