• 作者：Enkhbaatar Ulziikhishig ; Kang Kwang Lee ; Quazi Sohel Hossain ; Yumiko Higa ; Naoki Imaizumi ; Yoko Aniya
• 关键词：Mitochondria ; Glutathione transferase ; Mitochondrial permeability transition ; Cyclosporin A ; Cyclophilin D ; Adenine nucleotide translocator
• 刊名：Life Sciences
• 出版年：2010
• 出版时间：8 May 2010
• 年：2010
• 卷：86
• 期：19-20
• 页码：726-732
• 全文大小：498 K

Aims

Main methods

When mitochondria were incubated with MPT inhibitors, mtMGST1 activity was decreased dose dependently and their 50 % inhibition concentration (IC₅₀) were 1.2 μM (cyclosporin A; CsA), 31 μM (bongkrekic acid; BKA), 1.8 mM (ADP), and 3.2 mM (ATP). The decrease of mtMGST1 activity by the MPT inhibitors was not observed in the presence of detergent Triton X-100. On the contrary, mtMGST1 inhibition by GST inhibitors such as cibacron blue (IC₅₀, 4.2 μM) and S-hexylglutathione (IC₅₀, 480 μM) was not affected in the presence of detergent. Although mtMGST1 resides in both the inner (IMM) and outer mitochondrial membranes (OMM), only mtMGST1 in the IMM was inhibited by the MPT inhibitors in the absence of detergent. GST inhibitors decreased mtMGST1 activity both in the IMM and OMM regardless of the presence or absence of detergent. Cytosolic GSTs and microsomal MGST1 were not inhibited by the MPT inhibitors.

Key findings

These results indicate that mtMGST1 is inhibited by MPT inhibitors through membrane components, not directly by the inhibitors.

Significance

Since CsA binds to cyclophilin D (Cyp-D) in the mitochondrial matrix whereas BKA or ADP binds to adenine nucleotide translocator (ANT) in the IMM, it was suggested that mtMGST1 in the IMM interacts with Cyp-D/ANT and the binding of MPT inhibitors to Cyp-D or ANT causes their conformational change followed by an alteration of mtMGST1 conformation, resulting in decreasing mtMGST1 activity.