Different states of synaptotagmin regulate evoked versus spontaneous release

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作者
Hua Bai
Renhao Xue
Huan Bao
Leili Zhang
Arun Yethiraj
Qiang Cui
Edwin R. Chapman
机构
[1] University of Wisconsin,Howard Hughes Medical Institute and Department of Neuroscience
[2] University of Wisconsin,Department of Chemistry and Theoretical Chemistry Institute
[3] Present address: Department of Biochemistry,undefined
[4] University of Washington,undefined
[5] Seattle,undefined
[6] Washington 98195,undefined
[7] USA,undefined
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The tandem C2-domains of synaptotagmin 1 (syt) function as Ca2+-binding modules that trigger exocytosis; in the absence of Ca2+, syt inhibits spontaneous release. Here, we used proline linkers to constrain and alter the relative orientation of these C2-domains. Short poly-proline helices have a period of three, so large changes in the relative disposition of the C2-domains result from changing the length of the poly-proline linker by a single residue. The length of the linker was varied one residue at a time, revealing a periodicity of three for the ability of the linker mutants to interact with anionic phospholipids and drive evoked synaptic transmission; syt efficiently drove exocytosis when its tandem C2-domains pointed in the same direction. Analysis of spontaneous release revealed a reciprocal relationship between the activation and clamping activities of the linker mutants. Hence, different structural states of syt underlie the control of distinct forms of synaptic transmission.
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