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CL 218872
shows specific action on benzodiazepine receptors; structure
Also Known As:
3-methyl-6-(3-(trifluoromethyl)phenyl)-1,2,4-triazolo(4,2-b)pyridazine; CL 218,872; CL-218872; CL218,872; 1,2,4-Triazolo(4,3-b)pyridazine, 3-methyl-6-(3-(trifluoromethyl)phenyl)-
Networked:
9
relevant articles (
0
outcomes,
1
trials/studies)
Bio-Agent Context: Research Results
Heterocyclic Compounds: 198
1-Ring Heterocyclic Compounds
Pyridazines: 11
CL 218872: 9
Experts
1.
Bonnie, K E
: 1 article (12/2003)
2.
Duran, P
: 1 article (12/2003)
3.
Galler, Janina R
: 1 article (12/2003)
4.
Hudson, J L
: 1 article (12/2003)
5.
Shultz, P L
: 1 article (12/2003)
6.
Tonkiss, J
: 1 article (12/2003)
Related Diseases
1.
Seizures (Absence Seizure)
09/01/1993 - "
CL 218,872 retarded the development of kindled seizures in a linear dose-dependent manner; rats treated with 5, 10, and 20 mg/kg, but not 1 mg/kg, of CL 218,872 required a greater number of afterdischarges (ADs) to develop generalized seizures than controls.
"
09/01/1993 - "
Together, these data suggest that CL 218,872 is a potent anticonvulsant, implicating the BZ1 receptor subtype in seizure development and in the expression of kindled seizures.
"
09/01/1993 - "
CL 218,872 also dose-dependently depressed kindled seizures and this was attenuated by flumazenil, which had little effect on kindled seizures by itself.
"
04/01/1985 - "
At high doses (20-60 mg kg-1) CL 218,872 counteracted seizures caused by pentetrazol but not those caused by picrotoxin.
"
09/01/1993 - "
Additionally, we assessed the effects of flumazenil (10 mg/kg), a non-specific benzodiazepine receptor antagonist, on kindling and the expression of kindled seizures alone or concomitantly with CL 218,872 (20 mg/kg).
"
2.
Ataxia (Dyssynergia)
02/01/1983 - "
A new chemical series was discovered, triazolopyridazines (TPZ, prototype CL 218,872), which showed anticonflict activity in rats and monkeys without sedation or ataxia and inhibited 3H-BDZ binding in brain membranes with kinetic characteristics suggesting the presence of multiple BDZ receptors.
"
07/01/1984 - "
The only qualitative difference between the compounds that could be detected was in the mouse where large doses of CL218,872 did not produce the marked degree of motor incoordination seen after diazepam.
"
3.
Malnutrition (Nutritional Deficiencies)
12/01/2003 - "
Spatial learning deficits induced by muscimol and CL218,872: lack of effect of prenatal malnutrition.
"
4.
Shock
11/01/1985 - "
The benzodiazepines midazolam, chlordiazepoxide, diazepam and N-desmethyldiazepam, the cyclopyrrolone zopiclone and the triazolopyridazine CL 218,872 had qualitatively similar stimulus effects regardless of the type of consequence (food presentation or stimulus-shock termination) that maintained responding.
"
5.
Hyperphagia (Overeating)
08/01/1985 - "
Benzodiazepine-induced hyperphagia in the nondeprived rat: comparisons with CL 218,872, zopiclone, tracazolate and phenobarbital.
"
Related Drugs and Biologics
1.
GABA-A Receptors (GABA(A) Receptor)
2.
Anticonvulsants (Antiepileptic Drugs)
3.
Bicuculline
4.
Allylglycine
5.
Diazepam (Valium)
6.
Benzodiazepines
7.
zopiclone (Zop)
8.
Picrotoxin
9.
Phenobarbital (Luminal)
10.
Muscimol