Abstract

BackgroundThe amino acid neurotransmitter GABA is abundant in the central nervous system (CNS) of both invertebrates and vertebrates. Receptors of this neurotransmitter play a key role in important processes such as learning and memory. Yet, little is known about the mode and tempo of evolution of the receptors of this neurotransmitter. Here, we investigate the phylogenetic relationships of GABA receptor subunits across the chordates and detail their mode of evolution among mammals.Principal FindingsOur analyses support two major monophyletic clades: one clade containing GABAA receptor α, γ, and ε subunits, and another one containing GABAA receptor ρ, β, δ, θ, and π subunits. The presence of GABA receptor subunits from each of the major clades in the Ciona intestinalis genome suggests that these ancestral duplication events occurred before the divergence of urochordates. However, while gene divergence proceeded at similar rates on most receptor subunits, we show that the mammalian-specific subunits θ and ε experienced an episode of positive selection and of relaxed constraints, respectively, after the duplication event. Sites putatively under positive selection are placed on a three-dimensional model obtained by homology-modeling.ConclusionsOur results suggest an early divergence of the GABA receptor subunits, before the split from urochordates. We show that functional changes occurred in the lineages leading to the mammalian-specific subunit θ, and we identify the amino acid sites putatively responsible for the functional divergence. We discuss potential consequences for the evolution of mammals and of their CNS.

Highlights

  • Gene duplication followed by gene divergence is one of the major mechanisms responsible for the evolution of new functions [1]

  • There are three major classes of GABA receptors identified in the mammalian central nervous system (CNS): GABAA, GABAB and GABAC

  • Our estimate of the GABAA receptor phylogeny shows two major monophyletic clades (Fig. 1), which is consistent with previous studies [3,23,24,25]

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Summary

Introduction

Gene duplication followed by gene divergence is one of the major mechanisms responsible for the evolution of new functions [1]. There are three major classes of GABA receptors identified in the mammalian CNS: GABAA, GABAB and GABAC. These are distinguished according to their composition, pharmacology and localization. Ionotropic GABAC receptors are composed of r subunits that are highly expressed in the vertebrate retina and preferentially localized to bipolar cells [17] but are found in the spinal cord and pituitary [18] Both spatial and temporal regulation of GABA receptor subunit expression provide functional diversity to the GABA receptor family. The amino acid neurotransmitter GABA is abundant in the central nervous system (CNS) of both invertebrates and vertebrates Receptors of this neurotransmitter play a key role in important processes such as learning and memory. We discuss potential consequences for the evolution of mammals and of their CNS

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