AI Article Synopsis

  • * In the study, researchers identified three unique nitric oxide synthase (NOS) genes in the placozoans Trichoplax and Hoilungia and confirmed their functional presence by measuring NO-related compounds using advanced techniques.
  • * The findings reveal a more complex signaling system in placozoans than previously thought, with diverse NOSs and NO receptors that suggest significant evolutionary adaptations in their cellular mechanisms compared to more complex animals.

Article Abstract

Nitric oxide (NO) is a ubiquitous gaseous messenger, but we know little about its early evolution. Here, we analyzed NO synthases (NOS) in four different species of placozoans-one of the early-branching animal lineages. In contrast to other invertebrates studied, Trichoplax and Hoilungia have three distinct NOS genes, including PDZ domain-containing NOS. Using ultra-sensitive capillary electrophoresis assays, we quantified nitrites (products of NO oxidation) and L-citrulline (co-product of NO synthesis from L-arginine), which were affected by NOS inhibitors confirming the presence of functional enzymes in Trichoplax. Using fluorescent single-molecule in situ hybridization, we showed that distinct NOSs are expressed in different subpopulations of cells, with a noticeable distribution close to the edge regions of Trichoplax. These data suggest both the compartmentalized release of NO and a greater diversity of cell types in placozoans than anticipated. NO receptor machinery includes both canonical and novel NIT-domain containing soluble guanylate cyclases as putative NO/nitrite/nitrate sensors. Thus, although Trichoplax and Hoilungia exemplify the morphologically simplest free-living animals, the complexity of NO-cGMP-mediated signaling in Placozoa is greater to those in vertebrates. This situation illuminates multiple lineage-specific diversifications of NOSs and NO/nitrite/nitrate sensors from the common ancestor of Metazoa and the preservation of conservative NOS architecture from prokaryotic ancestors.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC7400543PMC
http://dx.doi.org/10.1038/s41598-020-69851-wDOI Listing

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