ADReCS

Pharmaceutical Information

Drug Name	Rotigotine hydrochloride
Drug ID	BADD_D01974
Description	Rotigotine (Neupro) is a non-ergoline dopamine agonist indicated for the treatment of Parkinson's disease (PD) and restless legs syndrome (RLS) in Europe and the United States. It is formulated as a once-daily transdermal patch which provides a slow and constant supply of the drug over the course of 24 hours. Like other dopamine agonists, rotigotine has been shown to possess antidepressant effects and may be useful in the treatment of depression as well. Rotigotine was developed by Aderis Pharmaceuticals. In 1998 Aderis licensed worldwide development and commercialization rights to Schwarz Pharma of Germany. It was approved by the European Medicines Agency in 2006 and by the FDA in 2007. However, all Neupro patches in the United States and some of Europe were recalled in 2008 due to delivery mechanism issues. Rotigotine has been authorized as a treatment for RLS since August 2008.
Indications and Usage	For use/treatment in neurologic disorders and parkinson's disease as well as moderate-to-severe primary Restless Legs Syndrome.
Marketing Status	approved
ATC Code	N04BC09
DrugBank ID	DB05271
KEGG ID	D05768
MeSH ID	C047508
PubChem ID	180335
TTD Drug ID	D0E4JL
NDC Product Code	17337-0078
UNII	6Q1W9573L2
Synonyms	rotigotine \| 2-(N-n-propyl-N-2-thienylethylamino)-5-hydroxytetralin \| N 0437, hydrochloride, (S)-isomer \| N 0923 \| N-0923 \| N 0924 \| N-0924 \| rotigotine, (+)- \| (+)-5,6,7,8-tetrahydro-6-(propyl(2-(2-thienyl)ethyl)amino)-1-naphthol \| Neupro \| N 0437 \| N-0437 \| N 0437, (+-)-isomer \| N 0437, (-)-isomer \| N 0437, hydrochloride, (R)-isomer \| rotigotine, (+--)- \| racemic N-0437 \| rotigotine (+-)-form \| 1-naphthalenol, 5,6,7,8-tetrahydro-6-(propyl(2-(2-thienyl)ethyl)amino)- \| (+--)-5,6,7,8-tetrahydro-6-(propyl(2-(2-thienyl)ethyl)amino)-1-naphthol \| N 0437, (R)-isomer \| Rotigotine CDS

Chemical Information

Molecular Formula	C19H26ClNOS
CAS Registry Number	125572-93-2
SMILES	CCCN(CCC1=CC=CS1)C2CCC3=C(C2)C=CC=C3O.Cl
Chemical Structure

ADRs Induced by Drug

*The priority for ADR severity classification is based on FAERS assessment, followed by the most severe level in CTCAE rating. If neither is available, it will be displayed as 'Not available'.
**The 'Not Available' level is hidden by default and can be restored by clicking on the legend twice..

ADR Term	ADReCS ID	ADR Frequency (FAERS)	ADR Severity Grade (FAERS)	ADR Severity Grade (CTCAE)
Abnormal dreams	19.02.03.001; 17.15.02.001	-	-	Not Available
Aggression	19.05.01.001	-	-	Not Available
Agitation	19.06.02.001; 17.02.05.012	-	-
Angioedema	22.04.02.008; 23.04.01.001; 10.01.05.009	-	-	Not Available
Application site reaction	12.07.01.006; 08.02.01.006	-	-	Not Available
Arthralgia	15.01.02.001	-	-
Asthenia	08.01.01.001	-	-	Not Available
Binge eating	19.09.01.001	-	-	Not Available
Compulsions	19.06.05.003	-	-	Not Available
Confusional state	19.13.01.001; 17.02.03.005	-	-
Constipation	07.02.02.001	-	-
Cough	22.02.03.001	-	-
Depression	19.15.01.001	-	-
Dermatitis	23.03.04.002	-	-	Not Available
Diarrhoea	07.02.01.001	-	-
Discomfort	08.01.08.003	-	-	Not Available
Disorientation	19.13.01.002; 17.02.05.015	-	-	Not Available
Dizziness	02.11.04.006; 24.06.02.007; 17.02.05.003	-	-
Dizziness postural	17.02.05.004; 02.11.04.008; 24.06.02.008	-	-	Not Available
Dry mouth	07.06.01.002	-	-
Dysaesthesia	23.03.03.077; 17.02.06.003	-	-
Dyskinesia	17.01.02.006	-	-
Dyspepsia	07.01.02.001	-	-
Ear disorder	04.03.01.001	-	-	Not Available
Eating disorder	19.09.01.008; 14.03.01.008	-	-	Not Available
Eczema	23.03.04.006	-	-
Erythema	23.03.06.001	-	-	Not Available
Fall	12.01.08.002	-	-
Fatigue	08.01.01.002	-	-
Feeling abnormal	08.01.09.014	-	-	Not Available

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