T Masukawa, M Sai, Y Tochino
Index: Life Sci. 44(6) , 417-24, (1989)
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To search for a technique to deplete reduced glutathione (GSH) in brain, the influence of various types of compounds on brain GSH levels was investigated in mice. Of the compounds tested, cyclohexene-1-one, cycloheptene-1-one and diethyl maleate were shown to be potent GSH depletors in brain as well as in liver. The depletion of cerebral GSH ranged about 40-60% of control levels at 1 and 3 hr after intraperitoneal injection. Cyclohexene, cycloheptene, phorone, acetaminophen, and benzyl chloride caused mild depletion of cerebral GSH, but buthionine sulfoximine did not alter cerebral GSH levels. Further, intracerebroventricular injection of cyclohexene-1-one and cycloheptene-1-one caused depletion of brain GSH to about 60-80% of control levels at 1 hr after injection, and the effects persisted for at least 6 hr. Under these conditions, hepatic GSH was not altered. These results demonstrated that cyclohexene-1-one and cycloheptene-1-one can cause not only a marked depletion of brain GSH by systemic administration, but also depletion of cerebral GSH by intracerebroventricular injection by virtue of being water-soluble compounds. Thus, methods for depleting brain GSH employing both compounds are available for exploring possible functions of cerebral GSH in in vivo systems.
| Structure | Name/CAS No. | Molecular Formula | Articles | 
|---|---|---|---|
                        ![]()  | 
                    2-cycloheptenone
                     CAS:1121-66-0  | 
                    C7H10O | 
| 
                                
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                                 1980-05-01 [J. Pharm. Sci. 69(5) , 527-31, (1980)]  | 
                        
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                                 2006-03-01 [Spectrochim. Acta. A. Mol. Biomol. Spectrosc. 63(3) , 709-13, (2006)]  | 
                        
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                                 [Tetrahedron Lett. 42(1) , 37-39, (2001)]  | 
                        
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