4.7 Article

ATP signaling in the integrative neural center of Aplysia californica

Journal

SCIENTIFIC REPORTS
Volume 11, Issue 1, Pages -

Publisher

NATURE PORTFOLIO
DOI: 10.1038/s41598-021-84981-5

Keywords

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Funding

  1. Human Frontiers Science Program [RGP0060/2017]
  2. National Science Foundation [1146575, 1557923, 1548121, 1645219]
  3. National Institute of Neurological Disorders and Stroke of the National Institutes of Health [R01NS114491]
  4. Russian Ministry of Science and High Education [075-15-2020-801]
  5. Hungarian Government Balaton Limnological Institute grant

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ATP and its ionotropic P2X receptors are components of the most ancient signaling system, with little known about their distribution and function in invertebrates. This study focuses on the cloning, expression, and pharmacological characterization of P2X receptors in the sea slug Aplysia californica, revealing unique expression patterns and functions, especially in development and homeostasis. The findings provide novel insights into the evolution of neurotransmitters.
ATP and its ionotropic P2X receptors are components of the most ancient signaling system. However, little is known about the distribution and function of purinergic transmission in invertebrates. Here, we cloned, expressed, and pharmacologically characterized the P2X receptors in the sea slug Aplysia californica-a prominent neuroscience model. AcP2X receptors were successfully expressed in Xenopus oocytes and displayed activation by ATP with two-phased kinetics and Na+-dependence. Pharmacologically, they were different from other P2X receptors. The ATP analog, Bz-ATP, was a less effective agonist than ATP, and PPADS was a more potent inhibitor of the AcP2X receptors than the suramin. AcP2X were uniquely expressed within the cerebral F-cluster, the multifunctional integrative neurosecretory center. AcP2X receptors were also detected in the chemosensory structures and the early cleavage stages. Therefore, in molluscs, rapid ATP-dependent signaling can be implicated both in development and diverse homeostatic functions. Furthermore, this study illuminates novel cellular and systemic features of P2X-type ligand-gated ion channels for deciphering the evolution of neurotransmitters.

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