NMR and EPR-DEER Structure of a Dimeric Guanylate Cyclase Activator Protein-5 from Zebrafish Photoreceptors

Cudia, Diana; Roseman, Graham; Assafa, Tufa E.; Shahu, Manisha Kumari; Scholten, Alexander; Menke-Sell, Sarah-Karina; Yamada, Hiroaki; Koch, Karl‐Wilhelm; Milhauser, Glenn; Ames, James B.

doi:10.1021/acs.biochem.1c00612

Cited by 4 publications

(35 citation statements)

References 55 publications

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“…GCAP1 and GCAP5 both form homodimers in solution in the absence of RetGC1 ( Figures 3C,D ). The dimerization of GCAP1 and GCAP5 are both Ca 2+ -independent and have a dimerization dissociation constant in the micromolar range ( Lim et al, 2018 ; Boni et al, 2020 ; Cudia et al, 2021 ). Structural models of GCAP1 and GCAP5 dimers were both determined previously by measuring intermolecular DEER distances that served as restraints for molecular docking ( Lim et al, 2018 ; Cudia et al, 2021 ; Figures 3C,D ).…”

Section: Molecular Structure and Function Of Guanylate Cyclase Activa...mentioning

confidence: 99%

“…The dimerization of GCAP1 and GCAP5 are both Ca 2+ -independent and have a dimerization dissociation constant in the micromolar range ( Lim et al, 2018 ; Boni et al, 2020 ; Cudia et al, 2021 ). Structural models of GCAP1 and GCAP5 dimers were both determined previously by measuring intermolecular DEER distances that served as restraints for molecular docking ( Lim et al, 2018 ; Cudia et al, 2021 ; Figures 3C,D ). The overall structures of both dimers are fairly similar (RMSD = 2.4 Å) and residues at the dimer interface are highly conserved (see red residues in Figure 3 ).…”

Section: Molecular Structure and Function Of Guanylate Cyclase Activa...mentioning

confidence: 99%

“…The overall structures of both dimers are fairly similar (RMSD = 2.4 Å) and residues at the dimer interface are highly conserved (see red residues in Figure 3 ). An important structural difference is that the GCAP5 dimer forms an intermolecular salt bridge between R22 and D71 that is not seen in the GCAP1 dimer, and the GCAP5 mutation R22A abolishes dimerization ( Cudia et al, 2021 ). The dimer structures of GCAP1 and GCAP5 are both stabilized by hydrophobic contacts at the dimer interface ( Figures 3C,D ).…”

Section: Molecular Structure and Function Of Guanylate Cyclase Activa...mentioning

confidence: 99%

“…The most prominent intermolecular contacts involve conserved hydrophobic residues, H19, Y22, M26, F73, V77, and W94 in GCAP1 ( Figure 3 ). In particular, the methyl side-chain atoms of V77 (V76 in GCAP5) each contact one another at the dimer interface and therefore explain why the V77E (or V76E in GCAP5) mutation significantly weakens protein dimerization for both GCAP1 and GCAP5 ( Lim et al, 2016 ; Cudia et al, 2021 ). Individual point mutations at the dimer interface in GCAP1 (H19A, Y22A, F73A, V77E, and W94A) or GCAP5 (H18A, Y21A, F72A, V76E, and W93E) each weaken the dimerization dissociation constant and completely abolish the activation of RetGC1 by GCAP1 ( Lim et al, 2018 ) or GCAP5 ( Cudia et al, 2021 ).…”

Section: Molecular Structure and Function Of Guanylate Cyclase Activa...mentioning

confidence: 99%

“…In this review, I provide an overview of previous atomic-resolution structures of GCAP1 ( Stephen et al, 2007 ; Lim et al, 2016 ), GCAP5 ( Cudia et al, 2021 ) and RD3 ( Peshenko et al, 2019 ), and propose a molecular mechanism for how RetGC1 might be regulated by GCAP1 and RD3.…”

Section: Introductionmentioning

confidence: 99%

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Structural basis of retinal membrane guanylate cyclase regulation by GCAP1 and RD3

Ames

2022

Front. Mol. Neurosci.

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Retinal membrane guanylate cyclases (RetGC1 and RetGC2) are expressed in photoreceptor rod and cone cells, where they promote the onset of visual recovery during phototransduction. The catalytic activity of RetGCs is regulated by their binding to regulatory proteins, guanylate cyclase activating proteins (GCAP1-5) and the retinal degeneration 3 protein (RD3). RetGC1 is activated by its binding to Ca2+-free/Mg2+-bound GCAP1 at low cytosolic Ca2+ levels in light-activated photoreceptors. By contrast, RetGC1 is inactivated by its binding to Ca2+-bound GCAP1 and/or RD3 at elevated Ca2+ levels in dark-adapted photoreceptors. The Ca2+ sensitive cyclase activation helps to replenish the cytosolic cGMP levels in photoreceptors during visual recovery. Mutations in RetGC1, GCAP1 or RD3 that disable the Ca2+-dependent regulation of cyclase activity are genetically linked to rod/cone dystrophies and other inherited forms of blindness. Here I review the structural interaction of RetGC1 with GCAP1 and RD3. I propose a two-state concerted model in which the dimeric RetGC1 allosterically switches between active and inactive conformational states with distinct quaternary structures that are oppositely stabilized by the binding of GCAP1 and RD3. The binding of Ca2+-free/Mg2+-bound GCAP1 is proposed to activate the cyclase by stabilizing RetGC1 in an active conformation (R-state), whereas Ca2+-bound GCAP1 and/or RD3 inhibit the cyclase by locking RetGC1 in an inactive conformation (T-state). Exposed hydrophobic residues in GCAP1 (residues H19, Y22, M26, F73, V77, W94) are essential for cyclase activation and could be targeted by rational drug design for the possible treatment of rod/cone dystrophies.

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Section: Molecular Structure and Function Of Guanylate Cyclase Activa...mentioning

confidence: 99%

Section: Molecular Structure and Function Of Guanylate Cyclase Activa...mentioning

confidence: 99%

Section: Molecular Structure and Function Of Guanylate Cyclase Activa...mentioning

confidence: 99%

Section: Molecular Structure and Function Of Guanylate Cyclase Activa...mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

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Structural basis of retinal membrane guanylate cyclase regulation by GCAP1 and RD3

Ames

2022

Front. Mol. Neurosci.

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Chemical shift assignments of retinal guanylyl cyclase activating protein 5 (GCAP5) with a mutation (R22A) that abolishes dimerization and enhances cyclase activation

2023

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Retinal membrane guanylyl cyclases (RetGCs) in vertebrate rod and cone photoreceptors are activated by a family of neuronal Ca2+ sensor proteins called guanylyl cyclase activating proteins (GCAP1-7). GCAP5 from zebrafish photoreceptors binds to RetGC and confers Ca2+/Fe2+-dependent regulation of RetGC enzymatic activity that promotes the recovery phase of visual phototransduction. We report NMR chemical shift assignments of GCAP5 with a R22A mutation (called GCAP5R22A) that abolishes protein dimerization and activates RetGC with 3-fold higher activity than that of wild type GCAP5 (BMRB No. 51,783).

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Molecular tuning of calcium dependent processes by neuronal calcium sensor proteins in the retina

Koch

2023

Biochimica et Biophysica Acta (BBA) - Molecular Cell Research

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NMR and EPR-DEER Structure of a Dimeric Guanylate Cyclase Activator Protein-5 from Zebrafish Photoreceptors

Cited by 4 publications

References 55 publications

Structural basis of retinal membrane guanylate cyclase regulation by GCAP1 and RD3

Structural basis of retinal membrane guanylate cyclase regulation by GCAP1 and RD3

Chemical shift assignments of retinal guanylyl cyclase activating protein 5 (GCAP5) with a mutation (R22A) that abolishes dimerization and enhances cyclase activation

Molecular tuning of calcium dependent processes by neuronal calcium sensor proteins in the retina

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