Structural and Functional Analyses Explain Pea KAI2 Receptor Diversity and Reveal Stereoselective Catalysis During Signal Perception

Guercio, Angelica M.; Torabi, Salar; Cornu, David; Bendahmane, Abdelhafid; Signor, Christine Le; Pillot, Jean‐Paul; Bris, Philippe Le; Boyer, François‐Didier; Rameau, Catherine; Gutjahr, Caroline; Germain, Alexandre de Saint; Shabek, Nitzan

doi:10.1101/2021.01.06.425465

Cited by 5 publications

(17 citation statements)

References 101 publications

(235 reference statements)

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“…Previous literature on the nature of the covalent modification include mass spectrometry showing a D-ring bound to H247 9 , a crystal structure of a CLIM species 4 , reanalysis of the CLIM structure suggesting that the electron density fits will with an intact D-ring 13 , and a crystal structure showing a D-ring on the catalytic serine in KAI2, a homolog of D14 with the same catalytic triad 37 . While these all initially appear to be competing views, our simulations show that all of these covalent modifications are likely to be present in some quantity.…”

Section: Discussionmentioning

confidence: 99%

Multiple modes of substrate hydrolysis-induced covalent modification of strigolactone receptors

Chen

Shukla

2022

Preprint

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The strigolactone signaling pathway in plants is unconventional among plant hormone signaling pathways in that the receptor also acts as an enzyme that hydrolyzes the strigolactone substrate. While the canonical view of strigolactone hydrolysis is that it occurs via a nucleophilic attack on the butenolide ring of strigolactone, an alternative Michael addition mechanism in which hydrolysis occurs via a nucleophilic attack on the enol-ether bridge has been proposed. Furthermore, while it is known that a hydrolysis-induced covalent modification to the receptor promotes strigolactone receptor activation, the nature of this covalent modification has been disputed. Here, we employ QM/MM string method simulations to determine the favored pathway of strigolactone hydrolysis and the nature of the covalent modification that acts as a promoter of strigolactone receptor activation. Our simulations show that strigolactone hydrolysis occurs via an acyl substitution pathway beginning with nucleophilic attack on the butenolide ring, which is well corroborated by previous experimental literature. Additionally, we show that multiple possible modes of covalent modifications to the catalytic residues by the butenolide ring are able to form and interconvert, reconciling several seemingly conflicting views on the hydrolysis-induced covalent modification to strigolactone receptors.

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Section: Discussionmentioning

confidence: 99%

Multiple modes of substrate hydrolysis-induced covalent modification of strigolactone receptors

Chen

Shukla

2022

Preprint

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“…Here, we present the crystal structure of A. thaliana DLK2, which, as a major difference to its paralogs AtD14 and AtKAI2, features a significantly smaller substrate binding pocket. Previous structures of strigolactone receptors or KAI2 clade proteins have shown that not only the substitution of amino acids inside the substrate binding pocket determines its size or ligand specificity (Guercio et al, 2022; Toh et al, 2015) but that also interactions between residues located in different secondary structure elements can influence the volume and shape of the pocket. This has been observed in a hydrogen bond between helices αD1 and αD3 in hyposensitive to light proteins from Striga hermonthica (ShHTL) (Xu et al, 2018) and in a loop region between helices αE and αF in KAI2‐like proteins from Physcomitrium patens (Bürger et al, 2019).…”

Section: Discussionmentioning

confidence: 99%

Crystal structure of Arabidopsis DWARF14‐LIKE2 (DLK2) reveals a distinct substrate binding pocket architecture

et al. 2022

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In Arabidopsis thaliana, the Sigma factor B regulator RsbQ-like family of α/β hydrolases contains the strigolactone (SL) receptor DWARF14 (AtD14), the karrikin receptor KARRIKIN INSENSITIVE2 (AtKAI2), and DWARF14-LIKE2 (AtDLK2), a protein of unknown function. Despite very similar protein folds, AtD14 and AtKAI2 differ in size and architecture of their ligand binding pockets, influencing their substrate specificity. We present the 1.5 Å crystal structure of AtDLK2, revealing the smallest ligand binding pocket in the protein family, bordered by two unique glycine residues. We identified a gatekeeper residue in the protein's lid domain and present a pyrroloquinoline-dione compound that inhibits AtDLK2's enzymatic activity.

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“…Neither structure shows the dramatic conformational change found in the homologous SL receptor DWARF14 (D14) when it is in a putatively active complex with MAX2/DWARF3 (D3) (Yao et al, 2016). Finally, the chemistry of KARs is incompatible with the ligand hydrolysis model proposed for PsKAI2B in pea (Pisum sativum) (Guercio et al, 2022), because KARs do not have a suitable leaving group and would likely re-close upon nucleophilic attack (Scaffidi et al, 2012). However, this last point may be moot if ligand hydrolysis is not essential for signal transduction by KAI2, as has been hypothesised for D14 (Seto et al, 2019).…”

Section: Kai2 Is Probably Not a Karrikin Receptormentioning

confidence: 92%

“…KAI2 proteins that are putatively KL-responsive can be activated by synthetic molecules with hydrolysable, 2 0 S-configured butenolide rings, such as GR24 ent-5DS (Waters et al, 2015b;Carbonnel et al, 2020b;Sun et al, 2020;Wang et al, 2020b;Yao et al, 2021). The KAI2 catalytic triad undergoes a similar modification with the cleaved butenolide ring as DWARF14 (D14) does during SL hydrolysis (Guercio et al, 2022). This suggests KL may have some structural similarity to SLs.…”

Section: Kai2 Is Probably Not a Karrikin Receptormentioning

confidence: 99%

Karrikin perception and signalling

Waters

Nelson

2022

New Phytologist

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Summary Karrikins (KARs) are a class of butenolide compounds found in smoke that were first identified as seed germination stimulants for fire‐following species. Early studies of KARs classified the germination and postgermination responses of many plant species and investigated crosstalk with plant hormones that regulate germination. The discovery that Arabidopsis thaliana responds to KARs laid the foundation for identifying mutants with altered KAR responses. Genetic analysis of KAR signalling revealed an unexpected link to strigolactones (SLs), a class of carotenoid‐derived plant hormones. Substantial progress has since been made towards understanding how KARs are perceived and regulate plant growth, in no small part due to advances in understanding SL perception. KAR and SL signalling systems are evolutionarily related and retain a high degree of similarity. There is strong evidence that KARs are natural analogues of an endogenous signal(s), KAI2 ligand (KL), which remains unknown. KAR/KL signalling regulates many developmental processes in plants including germination, seedling photomorphogenesis, and root and root hair growth. KAR/KL signalling also affects abiotic stress responses and arbuscular mycorrhizal symbiosis. Here, we summarise the current knowledge of KAR/KL signalling and discuss current controversies and unanswered questions in this field.

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Structural and Functional Analyses Explain Pea KAI2 Receptor Diversity and Reveal Stereoselective Catalysis During Signal Perception

Cited by 5 publications

References 101 publications

Multiple modes of substrate hydrolysis-induced covalent modification of strigolactone receptors

Multiple modes of substrate hydrolysis-induced covalent modification of strigolactone receptors

Crystal structure of Arabidopsis DWARF14‐LIKE2 (DLK2) reveals a distinct substrate binding pocket architecture

Karrikin perception and signalling

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