AI Article Synopsis

  • The study focuses on strain FS406-22, a heat-loving methanogen that can fix nitrogen using a minimal set of genes, including just four main structural genes and a homolog found elsewhere in its genome.
  • The absence of a key gene necessary for forming the nitrogenase cofactor in related organisms, coupled with the discovery of novel proteins, raises questions about how nitrogen fixation evolved in FS406-22.
  • Researchers developed genetic tools to manipulate FS406-22, demonstrating that the deletion of one gene affected growth and suggesting a cooperative role with another gene in nitrogen fixation processes.

Article Abstract

sp. strain FS406-22, a hyperthermophilic methanogen, fixes nitrogen with a minimal set of known genes. Only four structural genes, , , , and are present in a cluster, and a homolog is present elsewhere in the genome. , essential for the final synthesis of the iron-molybdenum cofactor of nitrogenase in well-characterized diazotrophs, is absent from FS406-22. In addition, FS406-22 encodes four novel hypothetical proteins, and a ferredoxin, in the cluster. Here, we develop a set of genetic tools for FS406-22 and test the functionality of genes in the cluster by making markerless in-frame deletion mutations. Deletion of the gene for one hypothetical protein, designated Hp4, delayed the initiation of diazotrophic growth and decreased the growth rate, an effect we confirmed by genetic complementation. NifE also appeared to play a role in diazotrophic growth, and the encoding of Hp4 and NifE in a single operon suggested they may work together in some way in the synthesis of the nitrogenase cofactor. No role could be discerned for any of the other hypothetical proteins, nor for the ferredoxin, despite the presence of these genes in a variety of related organisms. Possible pathways and evolutionary scenarios for the synthesis of the nitrogenase cofactor in an organism that lacks are discussed. has been considered a model genus, but genetic tools have not been forthcoming until recently. Here, we develop and illustrate the utility of positive selection with either of two selective agents (simvastatin and neomycin), negative selection, generation of markerless in-frame deletion mutations, and genetic complementation. These genetic tools should be useful for a variety of related species. We address the question of the minimal set of genes, which has implications for how nitrogen fixation evolved.

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Source
http://www.ncbi.nlm.nih.gov/pmc/articles/PMC8809328PMC
http://dx.doi.org/10.1128/spectrum.02093-21DOI Listing

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