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=== Binding ===
=== Binding ===
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In its resting state, VKOR is in its <scene name='90/904322/Open_conformation/2'>open conformation</scene>. The Vitamin K epoxide enters through the <scene name='90/904322/Tunnel/7'>isoprenyl-chain tunnel</scene>. The tunnel is located between <scene name='90/904322/Tunnel/8'>TM2 and TM3</scene>.<ref name="Li">PMID:20110994</ref> The carbonyls on the VK epoxide bind to <scene name='90/904322/Vko_binding/2'>Asn80 and Tyr139</scene> on VKOR. With Vitamin K epoxide bound, the cysteines of VKOR are partially oxidized, and concurrently reduce the substrate. A disulfide bond then forms between Cys51 and Cys132, resulting in the closed conformation. This leaves the sulfur on Cys43 and the sulfur on Cys135 protonated. The available hydrogens on these cysteines are utilized in reducing the epoxide. First, the free sulfur on Cys43 attacks Cys51 to form a new disulfide bond. With the loss of hydrogen from Cys43 in the formation of the new disulfide bond, an electron transfer is made to VKO. Next, the sulfur on Cys132 and the sulfur on Cys135 form a new disulfide bond. The hydrogen that was present on Cys135 is lost in the formation of the disulfide bond, allowing for an electron transfer to the oxygen of the epoxide. With these cysteine pairs formed, VKOR is left in an open conformation. The end products are Vitamin K/quinone and water.
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In its resting state, VKOR is in its <scene name='90/904322/Open_conformation/2'>open conformation</scene>. The Vitamin K epoxide enters through the <scene name='90/904322/Tunnel/7'>isoprenyl-chain tunnel</scene>. The tunnel is located between <scene name='90/904322/Tunnel/8'>TM2 and TM3</scene>.<ref name="Li">PMID:20110994</ref> The carbonyls on the VK epoxide bind to <scene name='90/904322/Vko_binding/2'>Asn80 and Tyr139</scene> on VKOR. With Vitamin K epoxide bound, the conformation transitions from open to closed, where the catalytic process will begin.

Revision as of 12:35, 19 April 2022

Structure of Closed Vitamin K Epoxide Reductase (PDB entry 6wv3)

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