Berupipam
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| Other names | NNC 22-0010; NNC-22-0010; NNC220010; NNC2210; NNC-2210 |
| Drug class | Dopamine D1 receptor antagonist |
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| Formula | C19H19BrClNO2 |
| Molar mass | 408.72 g·mol−1 |
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Berupipam (INN; developmental code name NNC 22-0010) is a selective dopamine D1 receptor antagonist of the benzazepine group which was under development for the treatment of psychotic disorders but was never marketed.[1][2] It reached phase 1 clinical trials prior to the discontinuation of its development.[1]
Berupipam and closely related dopamine D1 receptor antagonists were reported to have been generally well-tolerated in clinical trials, but side effects included restlessness, drowsiness, other central nervous system-related symptoms, and orthostatic hypotension.[3]
Berupipam, in radiolabeled form, has been studied for use in positron emission tomography (PET) imaging.[4][5][6] The drug was first described in the scientific literature by 1994.[3]
See also
[edit]- Ecopipam (SCH-39166)
- NNC 01-0687 (ADX-10061)
- Odapipam (NNC 01-0756)
- SCH-23390
References
[edit]- ^ a b "BERUPIPAM". Inxight Drugs. Retrieved 21 October 2024.
Berupipam (also known as NNC 22-0010), a dopamine antagonist with a high affinity and selectivity for D1 receptor has been studied for patients with psychotic disorders. Berupipam participated in phase I clinical trials; however, further development of this drug was discontinued
- ^ Zhang J, Xiong B, Zhen X, Zhang A (March 2009). "Dopamine D1 receptor ligands: where are we now and where are we going". Med Res Rev. 29 (2): 272–294. doi:10.1002/med.20130. PMID 18642350.
- ^ a b Hall, Rodger (1994). "Defining new ground for the treatment of schizophrenia". Inpharma Weekly. 953 (953). Springer Science and Business Media LLC: 8–9. doi:10.2165/00128413-199409530-00015. ISSN 1173-8324.
D1-antagonists are an area of active research. Although no results of widespread clinical testing have yet been published. phase I clinical trials presented by Dr M Sloth-Nielson from Novo Nordisk suggest that further investigation of the 3 novel drugs NNC 01-0687, NNC 01-0756 [odapipam] and NNC 22-0010 is warranted. The drugs were generally well tolerated, with restlessness, drowsiness and other CNS-related symptoms being the main effects observed. NNC 22-0010 50mg produced a moderate orthostatic hypotension in 2 volunteers.
- ^ Prante O, Maschauer S, Banerjee A (2013). "Radioligands for the dopamine receptor subtypes". J Labelled Comp Radiopharm. 56 (3–4): 130–148. doi:10.1002/jlcr.3000. PMID 24285319.
- ^ Banerjee A, Prante O (2012). "Subtype-selective dopamine receptor radioligands for PET imaging: current status and recent developments". Curr Med Chem. 19 (23): 3957–3966. doi:10.2174/092986712802002518. PMID 22780960.
- ^ Foged C, Halldin C, Loc'h C, Mazière B, Karlsson P, Mazière M, Swahn CG, Farde L (August 1996). "11C- and 76Br-labelled NNC 22-0010, selective dopamine D1 receptor radioligands for PET". Nucl Med Biol. 23 (6): 837–844. doi:10.1016/0969-8051(96)00083-2. PMID 8940728.
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