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Structure of SOQ1 lumenal domains identifies potential disulfide exchange for negative regulation of photoprotection, qH

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AbstractNon-photochemical quenching (NPQ) plays an important role for phototrophs in decreasing photo-oxidative damage. qH is a sustained component of NPQ and depends on the plastid lipocalin (LCNP). A thylakoid membrane-anchored protein SUPPRESSOR OF QUENCHING1 (SOQ1) prevents qH formation by inhibiting LCNP. SOQ1 suppresses qH with its lumen-located C-terminal Trx-like and NHL domains. Here we report crystal structures and biochemical characterization of SOQ1 lumenal domains. Our results show that the Trx-like and NHL domains are stably associated, with the potential redox-active motif located at their interface. Residue E859 essential for SOQ1 function is pivotal for mediating the inter-domain interaction. Moreover, the C-terminal region of SOQ1 forms an independent β-stranded domain, which possibly interacts with the Trx-like domain through disulfide exchange. Furthermore, SOQ1 is susceptible to cleavage at the loops connecting the neighboring domains both in vitro and in vivo, which could be a regulatory process for its suppression function of qH.
Title: Structure of SOQ1 lumenal domains identifies potential disulfide exchange for negative regulation of photoprotection, qH
Description:
AbstractNon-photochemical quenching (NPQ) plays an important role for phototrophs in decreasing photo-oxidative damage.
qH is a sustained component of NPQ and depends on the plastid lipocalin (LCNP).
A thylakoid membrane-anchored protein SUPPRESSOR OF QUENCHING1 (SOQ1) prevents qH formation by inhibiting LCNP.
SOQ1 suppresses qH with its lumen-located C-terminal Trx-like and NHL domains.
Here we report crystal structures and biochemical characterization of SOQ1 lumenal domains.
Our results show that the Trx-like and NHL domains are stably associated, with the potential redox-active motif located at their interface.
Residue E859 essential for SOQ1 function is pivotal for mediating the inter-domain interaction.
Moreover, the C-terminal region of SOQ1 forms an independent β-stranded domain, which possibly interacts with the Trx-like domain through disulfide exchange.
Furthermore, SOQ1 is susceptible to cleavage at the loops connecting the neighboring domains both in vitro and in vivo, which could be a regulatory process for its suppression function of qH.

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