Functional and topological diversity of LOV domain photoreceptors

Spencer T. Glantz; Eric J. Carpenter; Michael Melkonian; Kevin H. Gardner; Edward S. Boyden; Gane Ka Shu Wong; Brian Y. Chow

doi:10.1073/pnas.1509428113

Functional and topological diversity of LOV domain photoreceptors

Spencer T. Glantz, Eric J. Carpenter, Michael Melkonian, Kevin H. Gardner, Edward S. Boyden, Gane Ka Shu Wong, Brian Y. Chow

Research output: Contribution to journal › Article › peer-review

111 Scopus citations

Abstract

Light-oxygen-voltage sensitive (LOV) flavoproteins are ubiquitous photoreceptors that mediate responses to environmental cues. Photosensory inputs are transduced into signaling outputs via structural rearrangements in sensor domains that consequently modulate the activity of an effector domain or multidomain clusters. Establishing the diversity in effector function and sensor-effector topology will inform what signaling mechanisms govern light-responsive behaviors across multiple kingdoms of life and how these signals are transduced. Here, we report the bioinformatics identification of over 6,700 candidate LOV domains (including over 4,000 previously unidentified sequences from plants and protists), and insights from their annotations for ontological function and structural arrangements. Motif analysis identified the sensors from ∼42 million ORFs, with strong statistical separation from other flavoproteins and non-LOV members of the structurally related Per-aryl hydrocarbon receptor nuclear translocator (ARNT)-Sim family. Conserved-domain analysis determined putative light-regulated function and multidomain topologies. We found that for certain effectors, sensor-effector linker length is discretized based on both phylogeny and the preservation of α-helical heptad repeats within an extended coiled-coil linker structure. This finding suggests that preserving sensor-effector orientation is a key determinant of linker length, in addition to ancestry, in LOV signaling structure-function.We found a surprisingly high prevalence of effectors with functions previously thought to be rare among LOV proteins, such as regulators of G protein signaling, and discovered several previously unidentified effectors, such as lipases. This work highlights the value of applying genomic and transcriptomic technologies to diverse organisms to capture the structural and functional variation in photosensory proteins that are vastly important in adaptation, photobiology, and optogenetics.

Original language	English (US)
Pages (from-to)	E1442-E1451
Journal	Proceedings of the National Academy of Sciences of the United States of America
Volume	113
Issue number	11
DOIs	https://doi.org/10.1073/pnas.1509428113
State	Published - Mar 15 2016

Keywords

Flavoproteins
LOV
Optogenetics
Photoreceptors

ASJC Scopus subject areas

General

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10.1073/pnas.1509428113

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title = "Functional and topological diversity of LOV domain photoreceptors",

abstract = "Light-oxygen-voltage sensitive (LOV) flavoproteins are ubiquitous photoreceptors that mediate responses to environmental cues. Photosensory inputs are transduced into signaling outputs via structural rearrangements in sensor domains that consequently modulate the activity of an effector domain or multidomain clusters. Establishing the diversity in effector function and sensor-effector topology will inform what signaling mechanisms govern light-responsive behaviors across multiple kingdoms of life and how these signals are transduced. Here, we report the bioinformatics identification of over 6,700 candidate LOV domains (including over 4,000 previously unidentified sequences from plants and protists), and insights from their annotations for ontological function and structural arrangements. Motif analysis identified the sensors from ∼42 million ORFs, with strong statistical separation from other flavoproteins and non-LOV members of the structurally related Per-aryl hydrocarbon receptor nuclear translocator (ARNT)-Sim family. Conserved-domain analysis determined putative light-regulated function and multidomain topologies. We found that for certain effectors, sensor-effector linker length is discretized based on both phylogeny and the preservation of α-helical heptad repeats within an extended coiled-coil linker structure. This finding suggests that preserving sensor-effector orientation is a key determinant of linker length, in addition to ancestry, in LOV signaling structure-function.We found a surprisingly high prevalence of effectors with functions previously thought to be rare among LOV proteins, such as regulators of G protein signaling, and discovered several previously unidentified effectors, such as lipases. This work highlights the value of applying genomic and transcriptomic technologies to diverse organisms to capture the structural and functional variation in photosensory proteins that are vastly important in adaptation, photobiology, and optogenetics.",

keywords = "Flavoproteins, LOV, Optogenetics, Photoreceptors",

author = "Glantz, {Spencer T.} and Carpenter, {Eric J.} and Michael Melkonian and Gardner, {Kevin H.} and Boyden, {Edward S.} and Wong, {Gane Ka Shu} and Chow, {Brian Y.}",

note = "Funding Information: The authors thank Ben Voight, Danielle Bassett, Arjun Raj, Daniel Schmidt, and all members of the B.Y.C. laboratory for helpful discussions. The authors also thank Stuart Levine and Huiming Ding of the MIT Broad Institute for early technical support and the Hibberd laboratory for access to the TransRate software. S.T.G. is supported by the National Science Foundation (NSF) Graduate Research Fellowship Program. B.Y.C. was funded by NSF Biophotonics (CBET 126497), the W. W. Smith Charitable Trust for the Heart, the Brain Research Foundation Fay Frank Program, the Penn Medicine Neuroscience Center, and the NIH/National Institute on Drug Abuse Grant 1R21 DA040434-01. B.Y.C. and E.S.B. were funded by Defense Advanced Research Projects Agency Living Foundries HR0011-12-C-0068. The 1000 Plants (1KP) initiative, led by G.K.-S.W., is funded by the Alberta Ministry of Innovation and Advanced Education, Alberta Innovates Technology Futures, Innovates Centres of Research Excellence, Musea Ventures, BGI-Shenzhen, and China National Genebank. E.S.B. was funded by the MIT Media Lab, Office of the Assistant Secretary of Defense for Research and Engineering, Harvard/MIT Joint Grants in Basic Neuroscience, NSF (especially CBET 1053233 and EFRI 0835878), NIH (especially 1DP2OD002002, 1R01NS067199, 1R01DA029639, 1R01GM104948, 1RC1MH088182, and 1R01NS075421), the Wallace H. Coulter Foundation, Alfred P. Sloan Foundation, Human Frontiers Science Program, New York Stem Cell Foundation Robertson Neuroscience Investigator Award, Institution of Engineering and Technology A. F. Harvey Prize, and Skolkovo Institute of Science and Technology. K.H.G. was funded by NIH Grant R01 GM106239 and Cancer Prevention Research Institute of Texas Grant RP130312.",

year = "2016",

month = mar,

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doi = "10.1073/pnas.1509428113",

language = "English (US)",

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T1 - Functional and topological diversity of LOV domain photoreceptors

AU - Glantz, Spencer T.

AU - Carpenter, Eric J.

AU - Melkonian, Michael

AU - Gardner, Kevin H.

AU - Boyden, Edward S.

AU - Wong, Gane Ka Shu

AU - Chow, Brian Y.

N1 - Funding Information: The authors thank Ben Voight, Danielle Bassett, Arjun Raj, Daniel Schmidt, and all members of the B.Y.C. laboratory for helpful discussions. The authors also thank Stuart Levine and Huiming Ding of the MIT Broad Institute for early technical support and the Hibberd laboratory for access to the TransRate software. S.T.G. is supported by the National Science Foundation (NSF) Graduate Research Fellowship Program. B.Y.C. was funded by NSF Biophotonics (CBET 126497), the W. W. Smith Charitable Trust for the Heart, the Brain Research Foundation Fay Frank Program, the Penn Medicine Neuroscience Center, and the NIH/National Institute on Drug Abuse Grant 1R21 DA040434-01. B.Y.C. and E.S.B. were funded by Defense Advanced Research Projects Agency Living Foundries HR0011-12-C-0068. The 1000 Plants (1KP) initiative, led by G.K.-S.W., is funded by the Alberta Ministry of Innovation and Advanced Education, Alberta Innovates Technology Futures, Innovates Centres of Research Excellence, Musea Ventures, BGI-Shenzhen, and China National Genebank. E.S.B. was funded by the MIT Media Lab, Office of the Assistant Secretary of Defense for Research and Engineering, Harvard/MIT Joint Grants in Basic Neuroscience, NSF (especially CBET 1053233 and EFRI 0835878), NIH (especially 1DP2OD002002, 1R01NS067199, 1R01DA029639, 1R01GM104948, 1RC1MH088182, and 1R01NS075421), the Wallace H. Coulter Foundation, Alfred P. Sloan Foundation, Human Frontiers Science Program, New York Stem Cell Foundation Robertson Neuroscience Investigator Award, Institution of Engineering and Technology A. F. Harvey Prize, and Skolkovo Institute of Science and Technology. K.H.G. was funded by NIH Grant R01 GM106239 and Cancer Prevention Research Institute of Texas Grant RP130312.

PY - 2016/3/15

Y1 - 2016/3/15

N2 - Light-oxygen-voltage sensitive (LOV) flavoproteins are ubiquitous photoreceptors that mediate responses to environmental cues. Photosensory inputs are transduced into signaling outputs via structural rearrangements in sensor domains that consequently modulate the activity of an effector domain or multidomain clusters. Establishing the diversity in effector function and sensor-effector topology will inform what signaling mechanisms govern light-responsive behaviors across multiple kingdoms of life and how these signals are transduced. Here, we report the bioinformatics identification of over 6,700 candidate LOV domains (including over 4,000 previously unidentified sequences from plants and protists), and insights from their annotations for ontological function and structural arrangements. Motif analysis identified the sensors from ∼42 million ORFs, with strong statistical separation from other flavoproteins and non-LOV members of the structurally related Per-aryl hydrocarbon receptor nuclear translocator (ARNT)-Sim family. Conserved-domain analysis determined putative light-regulated function and multidomain topologies. We found that for certain effectors, sensor-effector linker length is discretized based on both phylogeny and the preservation of α-helical heptad repeats within an extended coiled-coil linker structure. This finding suggests that preserving sensor-effector orientation is a key determinant of linker length, in addition to ancestry, in LOV signaling structure-function.We found a surprisingly high prevalence of effectors with functions previously thought to be rare among LOV proteins, such as regulators of G protein signaling, and discovered several previously unidentified effectors, such as lipases. This work highlights the value of applying genomic and transcriptomic technologies to diverse organisms to capture the structural and functional variation in photosensory proteins that are vastly important in adaptation, photobiology, and optogenetics.

AB - Light-oxygen-voltage sensitive (LOV) flavoproteins are ubiquitous photoreceptors that mediate responses to environmental cues. Photosensory inputs are transduced into signaling outputs via structural rearrangements in sensor domains that consequently modulate the activity of an effector domain or multidomain clusters. Establishing the diversity in effector function and sensor-effector topology will inform what signaling mechanisms govern light-responsive behaviors across multiple kingdoms of life and how these signals are transduced. Here, we report the bioinformatics identification of over 6,700 candidate LOV domains (including over 4,000 previously unidentified sequences from plants and protists), and insights from their annotations for ontological function and structural arrangements. Motif analysis identified the sensors from ∼42 million ORFs, with strong statistical separation from other flavoproteins and non-LOV members of the structurally related Per-aryl hydrocarbon receptor nuclear translocator (ARNT)-Sim family. Conserved-domain analysis determined putative light-regulated function and multidomain topologies. We found that for certain effectors, sensor-effector linker length is discretized based on both phylogeny and the preservation of α-helical heptad repeats within an extended coiled-coil linker structure. This finding suggests that preserving sensor-effector orientation is a key determinant of linker length, in addition to ancestry, in LOV signaling structure-function.We found a surprisingly high prevalence of effectors with functions previously thought to be rare among LOV proteins, such as regulators of G protein signaling, and discovered several previously unidentified effectors, such as lipases. This work highlights the value of applying genomic and transcriptomic technologies to diverse organisms to capture the structural and functional variation in photosensory proteins that are vastly important in adaptation, photobiology, and optogenetics.

KW - Flavoproteins

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KW - Optogenetics

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Functional and topological diversity of LOV domain photoreceptors

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