Your search keyword '"David C. Martinelli"' showing total 14 results

1. Adhesion Class GPCRs in GtoPdb v.2023.1

Author

Lei Xu, Uwe Wolfrum, Yuri Ushkaryov, Martin Stacey, Kathleen Singer, Helgi Schiöth, Torsten Schöneberg, Simone Prömel, Xianhua Piao, Kelly Monk, David C. Martinelli, Hsi-Hsien Lin, Diana Le Duc, Tobias Langenhan, Arunkumar Krishnan, Barbara Knapp, Christiane Kirchhoff, Henrike Heyne, Breanne Harty, Jörg Hamann, Caroline Formstone, Heike Cappallo-Obermann, Tom I. Bonner, Gabriela Aust, and Demet Arac-Ozkan

Subjects

General Medicine, General Chemistry

Abstract

Adhesion GPCRs are structurally identified on the basis of a large extracellular region, similar to the Class B GPCR, but which is linked to the 7TM region by a GPCR autoproteolysis-inducing (GAIN) domain [10] containing a GPCR proteolysis site (GPS). The N-terminal extracellular region often shares structural homology with adhesive domains (e.g. cadherins, immunolobulin, lectins) facilitating inter- and matricellular interactions and leading to the term adhesion GPCR [104, 418]. Several receptors have been suggested to function as mechanosensors [320, 288, 396, 38]. Cryo-EM structures of the 7-transmembrane domain of several adhesion GPCRs have been determined recently [292, 21, 403, 212, 300, 302, 431, 293]. The nomenclature of these receptors was revised in 2015 as recommended by NC-IUPHAR and the Adhesion GPCR Consortium [125].

Published

2023

2. Adhesion Class GPCRs in GtoPdb v.2021.3

Author

Kathleen Singer, Henrike O. Heyne, Xianhua Piao, Simone Prömel, Jörg Hamann, Uwe Wolfrum, Demet Arac-Ozkan, Diana Le Duc, Breanne L. Harty, Tobias Langenhan, Yuri A. Ushkaryov, Tom I. Bonner, Gabriela Aust, Heike Cappallo-Obermann, Caroline J. Formstone, Torsten Schöneberg, Arunkumar Krishnan, Helgi B. Schiöth, Hsi-Hsien Lin, Martin Stacey, David C. Martinelli, Kelly Monk, Barbara Knapp, Christiane Kirchhoff, and Lei Xu

Subjects

Structural homology, Chemistry, Cadherin, Extracellular, Adhesion, Receptor, hormones, hormone substitutes, and hormone antagonists, Function (biology), G protein-coupled receptor, Cell biology

Abstract

Adhesion GPCRs are structurally identified on the basis of a large extracellular region, similar to the Class B GPCR, but which is linked to the 7TM region by a GPCR autoproteolysis-inducing (GAIN) domain [9] containing a GPCR proteolytic site. The N-terminus often shares structural homology with adhesive domains (e.g. cadherins, immunolobulin, lectins) facilitating inter- and matricellular interactions and leading to the term adhesion GPCR [101, 403]. Several receptors have been suggested to function as mechanosensors [309, 280, 383, 35]. The nomenclature of these receptors was revised in 2015 as recommended by NC-IUPHAR and the Adhesion GPCR Consortium [122].

Published

2021

3. C1QL3 promotes cell‐cell adhesion by mediating complex formation between ADGRB3/BAI3 and neuronal pentraxins

Author

Csaba Földy, Perla Arianna Peña Palomino, Matthew J. Sticco, Brianna L. Thompson, Susanne Ressl, David Lukacsovich, and David C. Martinelli

Subjects

Male, 0301 basic medicine, Nerve Tissue Proteins, Biochemistry, Interactome, Synapse, Mice, 03 medical and health sciences, 0302 clinical medicine, Cell Adhesion, Genetics, Animals, Cell adhesion, Receptor, Molecular Biology, Synapse organization, Neurons, Pentraxins, biology, Chemistry, Complement C1q, Membrane Proteins, Adhesion, Cell biology, C-Reactive Protein, 030104 developmental biology, Multiprotein Complexes, Synapses, Excitatory postsynaptic potential, biology.protein, 030217 neurology & neurosurgery, Biotechnology

Abstract

Synapses are the fundamental structural unit by which neurons communicate. An orchestra of proteins regulates diverse synaptic functions, including synapse formation, maintenance, and elimination-synapse homeostasis. Some proteins of the larger C1q super-family are synaptic organizers involved in crucial neuronal processes in various brain regions. C1Q-like (C1QL) proteins bind to the adhesion G protein-coupled receptor B3 (ADGRB3) and act at synapses in a subset of circuits. To investigate the hypothesis that the secreted C1QL proteins mediate tripartite trans-synaptic adhesion complexes, we conducted an in vivo interactome study and identified new binding candidates. We demonstrate that C1QL3 mediates a novel cell-cell adhesion complex involving ADGRB3 and two neuronal pentraxins, NPTX1 and NPTXR. Analysis of single-cell RNA-Seq data from the cerebral cortex shows that C1ql3, Nptx1, and Nptxr are highly co-expressed in the same excitatory neurons. Thus, our results suggest the possibility that in vivo the three co-expressed proteins are presynaptically secreted and form a complex capable of binding to postsynaptically localized ADGRB3, thereby creating a novel trans-synaptic adhesion complex. Identifying new binding partners for C1QL proteins and deciphering their underlying molecular principles will accelerate our understanding of their role in synapse organization.

Published

2020

4. Anatomical and Behavioral Investigation of C1ql3 in the Mouse Suprachiasmatic Nucleus

Author

Samer Hattar, Diego C. Fernandez, Thomas C. Südhof, David C. Martinelli, and Kylie S. Chew

Subjects

Male, 0301 basic medicine, Physiology, Photoperiod, Period (gene), Nerve Tissue Proteins, Biology, Article, Synapse, Mice, 03 medical and health sciences, Glutamatergic, 0302 clinical medicine, Physiology (medical), Animals, Circadian rhythm, Mice, Knockout, Neurons, Suprachiasmatic nucleus, Complement C1q, Period Circadian Proteins, Circadian Rhythm, 030104 developmental biology, nervous system, Light effects on circadian rhythm, Synapses, Knockout mouse, Excitatory postsynaptic potential, Suprachiasmatic Nucleus, sense organs, Neuroscience, 030217 neurology & neurosurgery, Signal Transduction

Abstract

Many biochemical, physiological, and behavioral processes such as glucose metabolism, body temperature, and sleep-wake cycles show regular daily rhythms. These circadian rhythms are adjusted to the environmental light-dark cycle by a central pacemaker located in the suprachiasmatic nucleus (SCN) in order for the processes to occur at appropriate times of day. Here, we investigated the expression and function of a synaptic organizing protein, C1QL3, in the SCN. We found that C1ql3 is robustly expressed in the SCN. C1ql3 knockout mice have a reduced density of excitatory synapses in the SCN. In addition, these mice exhibited less consolidated activity to the active portions of the day and period lengthening following a 15-minute phase-delaying light pulse. These data identify C1QL3 as a signaling molecule that is highly expressed in SCN neurons, where it contributes to the formation and/or maintenance of glutamatergic synapses and plays a role in circadian behaviors, which may include circadian aftereffects.

Published

2017

5. Adhesion Class GPCRs (version 2019.4) in the IUPHAR/BPS Guide to Pharmacology Database

Author

Torsten Schöneberg, Diana Le Duc, Breanne L. Harty, Christiane Kirchhoff, Simone Prömel, Heike Cappallo-Obermann, Demet Arac-Ozkan, Xianhua Piao, Gabriela Aust, Lei Xu, Helgi B. Schiöth, Hsi-Hsien Lin, Kathleen Singer, Barbara Knapp, Uwe Wolfrum, Jörg Hamann, Arunkumar Krishnan, Martin Stacey, Henrike O. Heyne, Tobias Langenhan, David C. Martinelli, Caroline J. Formstone, Yuri A. Ushkaryov, Tom I. Bonner, and Kelly Monk

Subjects

Structural homology, Cadherin, Chemistry, Computational biology, Adhesion, Receptor, hormones, hormone substitutes, and hormone antagonists, Function (biology), G protein-coupled receptor

Abstract

Adhesion GPCRs are structurally identified on the basis of a large extracellular region, similar to the Class B GPCR, but which is linked to the 7TM region by a GPCR autoproteolysis-inducing (GAIN) domain [8] containing a GPCR proteolytic site. The N-terminus often shares structural homology with adhesive domains (e.g. cadherins, immunolobulin, lectins) facilitating inter- and matricellular interactions and leading to the term adhesion GPCR [82, 332]. Several receptors have been suggested to function as mechanosensors [254, 234, 315, 32]. The nomenclature of these receptors was revised in 2015 as recommended by NC-IUPHAR and the Adhesion GPCR Consortium [100].

Published

2019

6. International Union of Basic and Clinical Pharmacology. XCIV. Adhesion G Protein–Coupled Receptors

Author

Thue W. Schwartz, Uwe Wolfrum, Xianhua Piao, Robert Fredriksson, Yuri A. Ushkaryov, Jörg Hamann, Simone Prömel, Hsi-Hsien Lin, Torsten Schöneberg, Helgi B. Schiöth, Ines Liebscher, Felix B. Engel, Gabriela Aust, Kathleen Singer, Tobias Langenhan, Miriam C. Peeters, Barbara Knapp, Arunkumar Krishnan, Martin Stacey, Caroline J. Formstone, David C. Martinelli, Mario Vallon, Breanne L. Harty, Kelly Monk, Randy A. Hall, Demet Araç, Mathew W. Wright, Christiane Kirchhoff, and Lei Xu

Subjects

Models, Molecular, Societies, Scientific, Subfamily, Computational biology, Biology, GPR110, Pharmacology, Ligands, GPR113, Second Messenger Systems, Receptors, G-Protein-Coupled, Cell Movement, Terminology as Topic, Cell Adhesion, Cyclic AMP, Animals, Humans, Protein Isoforms, Receptor, Nomenclature, G protein-coupled receptor, Cell Membrane, International Agencies, Adhesion, QP, GPR56, Pharmacology, Clinical, IUPHAR Nomenclature Reports, Molecular Medicine, QP517, Cell Adhesion Molecules, Signal Transduction

Abstract

The Adhesion family forms a large branch of the pharmacologically important superfamily of G protein-coupled receptors (GPCRs). As Adhesion GPCRs increasingly receive attention from a wide spectrum of biomedical fields, the Adhesion GPCR Consortium, together with the International Union of Basic and Clinical Pharmacology Committee on Receptor Nomenclature and Drug Classification, proposes a unified nomenclature for Adhesion GPCRs. The new names have ADGR as common dominator followed by a letter and a number to denote each subfamily and subtype, respectively. The new names, with old and alternative names within parentheses, are: ADGRA1 (GPR123), ADGRA2 (GPR124), ADGRA3 (GPR125), ADGRB1 (BAI1), ADGRB2 (BAI2), ADGRB3 (BAI3), ADGRC1 (CELSR1), ADGRC2 (CELSR2), ADGRC3 (CELSR3), ADGRD1 (GPR133), ADGRD2 (GPR144), ADGRE1 (EMR1, F4/80), ADGRE2 (EMR2), ADGRE3 (EMR3), ADGRE4 (EMR4), ADGRE5 (CD97), ADGRF1 (GPR110), ADGRF2 (GPR111), ADGRF3 (GPR113), ADGRF4 (GPR115), ADGRF5 (GPR116, Ig-Hepta), ADGRG1 (GPR56), ADGRG2 (GPR64, HE6), ADGRG3 (GPR97), ADGRG4 (GPR112), ADGRG5 (GPR114), ADGRG6 (GPR126), ADGRG7 (GPR128), ADGRL1 (latrophilin-1, CIRL-1, CL1), ADGRL2 (latrophilin-2, CIRL-2, CL2), ADGRL3 (latrophilin-3, CIRL-3, CL3), ADGRL4 (ELTD1, ETL), and ADGRV1 (VLGR1, GPR98). This review covers all major biologic aspects of Adhesion GPCRs, including evolutionary origins, interaction partners, signaling, expression, physiologic functions, and therapeutic potential.

Published

2015

7. Gas1 is a modifier for holoprosencephaly and genetically interacts with sonic hedgehog

Author

Maisa Seppala, Martyn T. Cobourne, Chen-Ming Fan, Michael J. Depew, Paul T. Sharpe, and David C. Martinelli

Subjects

Male, Craniofacial abnormality, Cell Cycle Proteins, GPI-Linked Proteins, Craniofacial Abnormalities, Mice, Holoprosencephaly, Pregnancy, medicine, Animals, Humans, Hedgehog Proteins, Sonic hedgehog, Craniofacial, Mice, Knockout, Genetics, biology, Membrane Proteins, General Medicine, medicine.disease, Phenotype, Hedgehog signaling pathway, Cell biology, Mice, Inbred C57BL, Somite, medicine.anatomical_structure, Forebrain, biology.protein, Female, Research Article, Signal Transduction

Abstract

Holoprosencephaly (HPE) is a clinically heterogeneous developmental anomaly affecting the CNS and face, in which the embryonic forebrain fails to divide into distinct halves. Numerous genetic loci and environmental factors are implicated in HPE, but mutation in the sonic hedgehog (Shh) gene is an established cause in both humans and mice. As growth arrest-specific 1 (Gas1) encodes a membrane glycoprotein previously identified as a Shh antagonist in the somite, we analyzed the craniofacial phenotype of mice harboring a targeted Gas1 deletion. Gas1(-/-) mice exhibited microform HPE, including midfacial hypoplasia, premaxillary incisor fusion, and cleft palate, in addition to severe ear defects; however, gross integrity of the forebrain remained intact. These defects were associated with partial loss of Shh signaling in cells at a distance from the source of transcription, suggesting that Gas1 can potentiate hedgehog signaling in the early face. Loss of a single Shh allele in a Gas1(-/-) background significantly exacerbated the midline craniofacial phenotype, providing genetic evidence that Shh and Gas1 interact. As human GAS1 maps to chromosome 9q21.3-q22, a region previously associated with nonsyndromic cleft palate and congenital deafness, our results establish GAS1 as a potential locus for several human craniofacial malformations.

Published

2007

8. Gas1 is a receptor for sonic hedgehog to repel enteric axons

Author

Marc Tessier-Lavigne, Shiying Jin, Xiaobin Zheng, David C. Martinelli, and Chen-Ming Fan

Subjects

Cell Cycle Proteins, GPI-Linked Proteins, Enteric Nervous System, Receptors, G-Protein-Coupled, Mice, Neurosphere, Animals, Hedgehog Proteins, Sonic hedgehog, Hedgehog, Myenteric plexus, Multidisciplinary, biology, Smoothened Receptor, Axons, GTP-Binding Protein alpha Subunits, Gut Epithelium, Intestines, nervous system, PNAS Plus, Mutation, biology.protein, Axon guidance, Enteric nervous system, Smoothened, Neuroscience

Abstract

The myenteric plexus of the enteric nervous system controls the movement of smooth muscles in the gastrointestinal system. They extend their axons between two peripheral smooth muscle layers to form a tubular meshwork arborizing the gut wall. How a tubular axonal meshwork becomes established without invading centrally toward the gut epithelium has not been addressed. We provide evidence here that sonic hedgehog (Shh) secreted from the gut epithelium prevents central projections of enteric axons, thereby forcing their peripheral tubular distribution. Exclusion of enteric central projections by Shh requires its binding partner growth arrest specific gene 1 (Gas1) and its signaling component smoothened (Smo) in enteric neurons. Using enteric neurons differentiated from neurospheres in vitro, we show that enteric axon growth is not inhibited by Shh. Rather, when Shh is presented as a point source, enteric axons turn away from it in a Gas1-dependent manner. Of the Gαi proteins that can couple with Smo, G protein α Z (Gnaz) is found in enteric axons. Knockdown and dominant negative inhibition of Gnaz dampen the axon-repulsive response to Shh, and Gnaz mutant intestines contain centrally projected enteric axons. Together, our data uncover a previously unsuspected mechanism underlying development of centrifugal tubular organization and identify a previously unidentified effector of Shh in axon guidance.

Published

2014

9. Structures of C1q-like proteins reveal unique features among the C1q/TNF superfamily

Author

Thomas C. Südhof, Axel T. Brunger, Brandon Vu, Sandro Vivona, David C. Martinelli, and Susanne Ressl

Subjects

Mutation, Protein Stability, Complement C1q, Molecular Sequence Data, Trimer, Plasma protein binding, Protomer, Biology, medicine.disease_cause, Protein Structure, Tertiary, Protein structure, Biochemistry, Structural Biology, medicine, Biophysics, Calcium, Adiponectin, Amino Acid Sequence, Protein Multimerization, Receptor, Molecular Biology, Peptide sequence, Actin, Protein Binding

Abstract

C1q-like (C1QL) -1, -2, and -3 proteins are encoded by homologous genes that are highly expressed in brain. C1QLs bind to brain-specific angiogenesis inhibitor 3 (BAI3), an adhesion-type G-protein coupled receptor that may regulate dendritic morphology by organizing actin filaments. To begin to understand the function of C1QLs, we determined high-resolution crystal structures of the globular C1q-domains of C1QL1, C1QL2, and C1QL3. Each structure is a trimer, with each protomer forming a jelly-roll fold consisting of 10 β strands. Moreover, C1QL trimers may assemble into higher-order oligomers similar to adiponectin and contain four Ca(2+)-binding sites along the trimeric symmetry axis, as well as additional surface Ca(2+)-binding sites. Mutation of Ca(2+)-coordinating residues along the trimeric symmetry axis lowered the Ca(2+)-binding affinity and protein stability. Our results reveal unique structural features of C1QLs among C1q/TNF superfamily proteins that may be associated with their specific brain functions.

Published

2014

10. Presynaptic neurexin-3 alternative splicing trans-synaptically controls postsynaptic AMPA receptor trafficking

Author

Thomas C. Südhof, Katsuhiko Tabuchi, Robert C. Malenka, David C. Martinelli, and Jason Aoto

Subjects

Long-Term Potentiation, Neurexin, Nerve Tissue Proteins, AMPA receptor, Biology, Hippocampus, General Biochemistry, Genetics and Molecular Biology, Article, 03 medical and health sciences, Mice, 0302 clinical medicine, Postsynaptic potential, Animals, Gene Knock-In Techniques, Receptors, AMPA, Receptor, 030304 developmental biology, Neurons, 0303 health sciences, integumentary system, Biochemistry, Genetics and Molecular Biology(all), Alternative splicing, fungi, Long-term potentiation, Endocytosis, Cell biology, Alternative Splicing, Biochemistry, Synapses, NMDA receptor, Postsynaptic density, 030217 neurology & neurosurgery

Abstract

Neurexins are essential presynaptic cell-adhesion molecules that are linked to schizophrenia and autism, and are subject to extensive alternative splicing. Here, we used a novel genetic approach to test the physiological significance of neurexin alternative splicing. We generated knock-in mice in which alternatively spliced sequence #4 (SS4) of neurexin-3 is constitutively included, but can be selectively excised by cre-recombination. SS4 of neurexin-3 was chosen because it is highly regulated and controls neurexin-binding to neuroligins, LRRTMs, and other ligands. Unexpectedly, constitutive inclusion of SS4 in presynaptic neurexin-3 decreased postsynaptic AMPA- but not NMDA-receptor levels and enhanced postsynaptic AMPA-receptor endocytosis. Moreover, constitutive inclusion of SS4 in presynaptic neurexin-3 abrogated postsynaptic AMPA-receptor recruitment during NMDA-receptor-dependent LTP. These phenotypes were fully rescued by constitutive excision of SS4 in neurexin-3. Thus, alternative splicing of presynaptic neurexin-3 controls postsynaptic AMPA-receptor trafficking, revealing an unanticipated alternative splicing mechanism for trans-synaptic regulation of synaptic strength and long-term plasticity.

Published

2013

11. Cerebellins meet neurexins (Commentary on MatsudaYuzaki)

Author

David C, Martinelli and Thomas C, Südhof

Subjects

Receptors, Glutamate, Synapses, Protein Isoforms, Nerve Tissue Proteins

Published

2011

12. Primary cilia regulate Shh activity in the control of molar tooth number

Author

Courtney J. Haycraft, Hervé Lesot, Paul T. Sharpe, Maisa Seppala, James Blackburn, Sarah Ghafoor, Chen-Ming Fan, Atsushi Ohazama, Martyn T. Cobourne, Renata Peterkova, Bradley K. Yoder, and David C. Martinelli

Subjects

Molar, Mesenchyme, Context (language use), Cell Cycle Proteins, Mice, Transgenic, Biology, GPI-Linked Proteins, Mice, Downregulation and upregulation, stomatognathic system, Intraflagellar transport, medicine, Animals, Hedgehog Proteins, Cilia, Molecular Biology, Cilium, Diastema, Gene Expression Regulation, Developmental, Membrane Proteins, Research Reports, Anatomy, Epithelium, Cell biology, stomatognathic diseases, medicine.anatomical_structure, Phenotype, Mutation, Tooth, Developmental Biology

Abstract

Primary cilia mediate Hh signalling and mutations in their protein components affect Hh activity. We show that in mice mutant for a cilia intraflagellar transport (IFT) protein, IFT88/polaris, Shh activity is increased in the toothless diastema mesenchyme of the embryonic jaw primordia. This results in the formation of ectopic teeth in the diastema, mesial to the first molars. This phenotype is specific to loss of polaris activity in the mesenchyme since loss of Polaris in the epithelium has no detrimental affect on tooth development. To further confirm that upregulation of Shh activity is responsible for the ectopic tooth formation, we analysed mice mutant for Gas1, a Shh protein antagonist in diastema mesenchyme. Gas1mutants also had ectopic diastema teeth and accompanying increased Shh activity. In this context, therefore, primary cilia exert a specific negative regulatory effect on Shh activity that functions to repress tooth formation and thus determine tooth number. Strikingly, the ectopic teeth adopt a size and shape characteristic of premolars, a tooth type that was lost in mice around 50-100 million years ago.

Published

2009

13. The role of Gas1 in embryonic development and its implications for human disease

Author

David C. Martinelli and Chen-Ming Fan

Subjects

Genetics, Patched, Cell growth, Cell Cycle, Membrane Proteins, Cell Cycle Proteins, Cell Biology, Cell cycle, Biology, GPI-Linked Proteins, Ligands, Embryonic stem cell, Transmembrane protein, Cell biology, Neoplasms, Animals, Humans, Hedgehog Proteins, Disease Susceptibility, Stem cell, Molecular Biology, Intracellular, Embryonic Stem Cells, Developmental Biology, Morphogen

Abstract

Growth Arrest Specific Gene 1 (Gas1) has long been regarded as a cell cycle inhibitor of the G(0) to S phase transition. How GAS1, a GPI-anchored plasma membrane protein, directs intracellular changes without an extracellular ligand or a transmembrane protein partner has been puzzling. A recent series of biochemical and molecular genetic studies assigned the mammalian Hedgehog (HH) growth factor to be a ligand for GAS1 in vitro and in vivo. HH has enjoyed considerable attention for its profound role in embryonic patterning as a classic morphogen, i.e. inducing various cell types in a concentration-dependent manner. GAS1 appears to help transform the HH concentration gradient into its morphogenic activity gradient by acting cooperatively with the HH receptor, the 12-transmembrane protein Patched 1 (PTC1). These findings provoke intriguing thoughts on how HH and GAS1 may coordinate cell proliferation and differentiation to create biological patterns. The role of HH extends to human genetic diseases, stem cell renewal, and cancer growth, and we consider the possibility of GAS1's involvement in these processes as well.

Published

2007

14. Gas1 extends the range of hedgehog action by facilitating its signaling

Author

Chen-Ming Fan and David C. Martinelli

Subjects

Patched Receptors, Neural Tube, Cell signaling, animal structures, Blotting, Western, Cell, Regulator, Embryonic Development, Cell Cycle Proteins, Receptors, Cell Surface, Biology, GPI-Linked Proteins, Cell Line, Mice, Genetics, medicine, Animals, Hedgehog Proteins, RNA, Small Interfering, Molecular Biology, Hedgehog, In Situ Hybridization, DNA Primers, Electroporation, Membrane Proteins, Extremities, Cell Biology, Molecular biology, Hedgehog signaling pathway, Cell biology, Patched-1 Receptor, medicine.anatomical_structure, Membrane protein, embryonic structures, Smoothened, Research Paper, Signal Transduction, Developmental Biology, Morphogen

Abstract

Cellular signaling initiated by Hedgehog binding to Patched1 has profound importance in mammalian embryogenesis, genetic disease, and cancer. Hedgehog acts as a morphogen to specify distinctive cell fates using different concentration thresholds, but our knowledge of how the concentration gradient is interpreted into the activity gradient is incomplete. The membrane protein Growth Arrest-Specific Gene 1 (GAS1) was thought to be a negative regulator of the Hedgehog concentration gradient. Here, we report unexpected genetic evidence that Gas1 positively regulates Hedgehog signaling in multiple developmental contexts, an effect particularly noticeable at regions where Hedgehog acts at low concentration. Using a combination of in vitro cell culture and in ovo electroporation assays, we demonstrate that GAS1 acts cooperatively with Patched1 for Hedgehog binding and enhances signaling activity in a cell-autonomous manner. Our data support a model in which GAS1 helps transform the Hedgehog protein gradient into the observed activity gradient. We propose that Gas1 is an evolutionarily novel, vertebrate-specific Hedgehog pathway regulator.

Published

2007