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The evolutionary origins and ancestral features of septins.

Publication ,  Journal Article
Delic, S; Shuman, B; Lee, S; Bahmanyar, S; Momany, M; Onishi, M
Published in: Frontiers in cell and developmental biology
January 2024

Septins are a family of membrane-associated cytoskeletal guanine-nucleotide binding proteins that play crucial roles in various cellular processes, such as cell division, phagocytosis, and organelle fission. Despite their importance, the evolutionary origins and ancestral function of septins remain unclear. In opisthokonts, septins form five distinct groups of orthologs, with subunits from multiple groups assembling into heteropolymers, thus supporting their diverse molecular functions. Recent studies have revealed that septins are also conserved in algae and protists, indicating an ancient origin from the last eukaryotic common ancestor. However, the phylogenetic relationships among septins across eukaryotes remained unclear. Here, we expanded the list of non-opisthokont septins, including previously unrecognized septins from glaucophyte algae. Constructing a rooted phylogenetic tree of 254 total septins, we observed a bifurcation between the major non-opisthokont and opisthokont septin clades. Within the non-opisthokont septins, we identified three major subclades: Group 6 representing chlorophyte green algae (6A mostly for species with single septins, 6B for species with multiple septins), Group 7 representing algae in chlorophytes, heterokonts, haptophytes, chrysophytes, and rhodophytes, and Group 8 representing ciliates. Glaucophyte and some ciliate septins formed orphan lineages in-between all other septins and the outgroup. Combining ancestral-sequence reconstruction and AlphaFold predictions, we tracked the structural evolution of septins across eukaryotes. In the GTPase domain, we identified a conserved GAP-like arginine finger within the G-interface of at least one septin in most algal and ciliate species. This residue is required for homodimerization of the single Chlamydomonas septin, and its loss coincided with septin duplication events in various lineages. The loss of the arginine finger is often accompanied by the emergence of the α0 helix, a known NC-interface interaction motif, potentially signifying the diversification of septin-septin interaction mechanisms from homo-dimerization to hetero-oligomerization. Lastly, we found amphipathic helices in all septin groups, suggesting that membrane binding is an ancestral trait. Coiled-coil domains were also broadly distributed, while transmembrane domains were found in some septins in Group 6A and 7. In summary, this study advances our understanding of septin distribution and phylogenetic groupings, shedding light on their ancestral features, potential function, and early evolution.

Duke Scholars

Published In

Frontiers in cell and developmental biology

DOI

EISSN

2296-634X

ISSN

2296-634X

Publication Date

January 2024

Volume

12

Start / End Page

1406966

Related Subject Headings

  • 32 Biomedical and clinical sciences
  • 31 Biological sciences
 

Citation

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Delic, S., Shuman, B., Lee, S., Bahmanyar, S., Momany, M., & Onishi, M. (2024). The evolutionary origins and ancestral features of septins. Frontiers in Cell and Developmental Biology, 12, 1406966. https://doi.org/10.3389/fcell.2024.1406966
Delic, Samed, Brent Shuman, Shoken Lee, Shirin Bahmanyar, Michelle Momany, and Masayuki Onishi. “The evolutionary origins and ancestral features of septins.Frontiers in Cell and Developmental Biology 12 (January 2024): 1406966. https://doi.org/10.3389/fcell.2024.1406966.
Delic S, Shuman B, Lee S, Bahmanyar S, Momany M, Onishi M. The evolutionary origins and ancestral features of septins. Frontiers in cell and developmental biology. 2024 Jan;12:1406966.
Delic, Samed, et al. “The evolutionary origins and ancestral features of septins.Frontiers in Cell and Developmental Biology, vol. 12, Jan. 2024, p. 1406966. Epmc, doi:10.3389/fcell.2024.1406966.
Delic S, Shuman B, Lee S, Bahmanyar S, Momany M, Onishi M. The evolutionary origins and ancestral features of septins. Frontiers in cell and developmental biology. 2024 Jan;12:1406966.

Published In

Frontiers in cell and developmental biology

DOI

EISSN

2296-634X

ISSN

2296-634X

Publication Date

January 2024

Volume

12

Start / End Page

1406966

Related Subject Headings

  • 32 Biomedical and clinical sciences
  • 31 Biological sciences