Characterization and Dynamics of Intracellular Gene Transfer in Plastid Genomes of Viola (Violaceae) and Order Malpighiales

Functional gene transfer from organelles to the nucleus, known as intracellular gene transfer (IGT), is an ongoing process in flowering plants. The complete plastid genomes (plastomes) of two Ulleung island endemic violets, Viola ulleungdoensis and V. woosanensis, were characterized, revealing a lack of the plastid-encoded infA, rpl32, and rps16 genes. In addition, functional replacement of the three plastid-encoded genes in the nucleus was confirmed within the genus Viola and the order Malpighiales. Three strategies for the acquisition of a novel transit peptide for successful IGT were identified in the genus Viola. Nuclear INFA acquired a novel transit peptide with very low identity between these proteins, whereas the nuclear RPL32 gene acquired an existing transit peptide via fusion with the nuclear-encoded plastid-targeted SOD gene (Cu-Zn superoxide dismutase superfamily) as one exon, and translated both proteins in the cytosol using alternative mRNA splicing. Nuclear RPS16 contains an internal transit peptide without an N-terminal extension. Gene loss or pseudogenization of the plastid-borne rpl32 and rps16 loci was inferred to occur in the common ancestor of the genus Viola based on an infrageneric phylogenetic framework in Korea. Although infA was lost in the common ancestor of the order Malpighiales, the rpl32 and rps16 genes were lost multiple times independently within the order. Our current study sheds additional light on plastid genome composition and IGT mechanisms in the violet genus and in the order Malpighiales.

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Comparative transcriptomics of the venoms of continental and insular radiations of West African cones

Proceedings of The Royal Society B Biological Sciences ◽

10.1098/rspb.2020.0794 ◽

2020 ◽

Vol 287 (1929) ◽

pp. 20200794

Author(s):

Samuel Abalde ◽

Manuel J. Tenorio ◽

Carlos M. L. Afonso ◽

Rafael Zardoya

Keyword(s):

Related Species ◽

Common Ancestor ◽

West African ◽

Generic Level ◽

Closely Related Species ◽

Functional Convergence ◽

Venom Glands ◽

Phylogenetic Framework ◽

The Common ◽

Secreted Peptides

The transcriptomes of the venom glands of 13 closely related species of vermivorous cones endemic to West Africa from genera Africonus and Varioconus were sequenced and venom repertoires compared within a phylogenetic framework using one Kalloconus species as outgroup. The total number of conotoxin precursors per species varied between 108 and 221. Individuals of the same species shared about one-fourth of the total conotoxin precursors. The number of common sequences was drastically reduced in the pairwise comparisons between closely related species, and the phylogenetical signal was totally eroded at the inter-generic level (no sequence was identified as shared derived), due to the intrinsic high variability of these secreted peptides. A common set of four conotoxin precursor superfamilies (T, O1, O2 and M) was expanded in all studied cone species, and thus, they are considered the basic venom toolkit for hunting and defense in the West African vermivorous cone snails. Maximum-likelihood ancestral character reconstructions inferred shared conotoxin precursors preferentially at internal nodes close to the tips of the phylogeny (between individuals and between closely related species) as well as in the common ancestor of Varioconus . Besides the common toolkit, the two genera showed significantly distinct catalogues of conotoxin precursors in terms of type of superfamilies present and the abundance of members per superfamily, but had similar relative expression levels indicating functional convergence. Differential expression comparisons between vermivorous and piscivorous cones highlighted the importance of the A and S superfamilies for fish hunting and defense.

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Portiera Gets Wild: Genome Instability Provides Insights into the Evolution of Both Whiteflies and Their Endosymbionts

Genome Biology and Evolution ◽

10.1093/gbe/evaa216 ◽

2020 ◽

Vol 12 (11) ◽

pp. 2107-2124

Author(s):

Diego Santos-Garcia ◽

Natividad Mestre-Rincon ◽

David Ouvrard ◽

Einat Zchori-Fein ◽

Shai Morin

Keyword(s):

Evolutionary History ◽

Common Ancestor ◽

Genome Instability ◽

Rare Event ◽

Essential Amino Acids ◽

Phylogenetic Framework ◽

The Common ◽

Phloem Feeding ◽

New Framework ◽

Time Point

Abstract Whiteflies (Hemiptera: Sternorrhyncha: Aleyrodidae) are a superfamily of small phloem-feeding insects. They rely on their primary endosymbionts "Candidatus Portiera aleyrodidarum" to produce essential amino acids not present in their diet. Portiera has been codiverging with whiteflies since their origin and therefore reflects its host’s evolutionary history. Like in most primary endosymbionts, the genome of Portiera stays stable across the Aleyrodidae superfamily after millions of years of codivergence. However, Portiera of the whitefly Bemisia tabaci has lost the ancestral genome order, reflecting a rare event in the endosymbiont evolution: the appearance of genome instability. To gain a better understanding of Portiera genome evolution, identify the time point in which genome instability appeared and contribute to the reconstruction of whitefly phylogeny, we developed a new phylogenetic framework. It targeted five Portiera genes and determined the presence of the DNA polymerase proofreading subunit (dnaQ) gene, previously associated with genome instability, and two alternative gene rearrangements. Our results indicated that Portiera gene sequences provide a robust tool for studying intergenera phylogenetic relationships in whiteflies. Using these new framework, we found that whitefly species from the Singhiella, Aleurolobus, and Bemisia genera form a monophyletic tribe, the Aleurolobini, and that their Portiera exhibit genome instability. This instability likely arose once in the common ancestor of the Aleurolobini tribe (at least 70 Ma), drawing a link between the appearance of genome instability in Portiera and the switch from multibacteriocyte to a single-bacteriocyte mode of inheritance in this tribe.

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Plastid Genomes and Proteins Illuminate the Evolution of Eustigmatophyte Algae and Their Bacterial Endosymbionts

Genome Biology and Evolution ◽

10.1093/gbe/evz004 ◽

2019 ◽

Vol 11 (2) ◽

pp. 362-379 ◽

Cited By ~ 7

Author(s):

Tereza Ševčíková ◽

Tatiana Yurchenko ◽

Karen P Fawley ◽

Raquel Amaral ◽

Hynek Strnad ◽

...

Keyword(s):

Gene Transfer ◽

Horizontal Gene Transfer ◽

Evolutionary History ◽

Common Ancestor ◽

Acyl Carrier Protein ◽

Phylogenomic Analysis ◽

Plastid Gene ◽

Plastid Genomes ◽

Bacterial Endosymbionts ◽

Gains And Losses

Abstract Eustigmatophytes, a class of stramenopile algae (ochrophytes), include not only the extensively studied biotechnologically important genus Nannochloropsis but also a rapidly expanding diversity of lineages with much less well characterized biology. Recent discoveries have led to exciting additions to our knowledge about eustigmatophytes. Some proved to harbor bacterial endosymbionts representing a novel genus, Candidatus Phycorickettsia, and an operon of unclear function (ebo) obtained by horizontal gene transfer from the endosymbiont lineage was found in the plastid genomes of still other eustigmatophytes. To shed more light on the latter event, as well as to generally improve our understanding of the eustigmatophyte evolutionary history, we sequenced plastid genomes of seven phylogenetically diverse representatives (including new isolates representing undescribed taxa). A phylogenomic analysis of plastid genome-encoded proteins resolved the phylogenetic relationships among the main eustigmatophyte lineages and provided a framework for the interpretation of plastid gene gains and losses in the group. The ebo operon gain was inferred to have probably occurred within the order Eustigmatales, after the divergence of the two basalmost lineages (a newly discovered hitherto undescribed strain and the Pseudellipsoidion group). When looking for nuclear genes potentially compensating for plastid gene losses, we noticed a gene for a plastid-targeted acyl carrier protein that was apparently acquired by horizontal gene transfer from Phycorickettsia. The presence of this gene in all eustigmatophytes studied, including representatives of both principal clades (Eustigmatales and Goniochloridales), is a genetic footprint indicating that the eustigmatophyte–Phycorickettsia partnership started no later than in the last eustigmatophyte common ancestor.

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The Possible Common Origin of tRNA and 5S rRNA

Zeitschrift für Naturforschung C ◽

10.1515/znc-1983-5-633 ◽

1983 ◽

Vol 38 (5-6) ◽

pp. 501-504 ◽

Cited By ~ 2

Author(s):

Mária Ujhelyi

Keyword(s):

Common Ancestor ◽

Common Origin ◽

5S Rrna ◽

Mitochondrial Trna ◽

Trna Molecule ◽

The Common

Seryl tRNA (anticodon GCU) from mammalian mitochondria shows in comparison to other mitochondrial tRNAs additional special features differing from the generalized tRNA model. When arranged in the traditional cloverleaf form, eight bases fall within the TΨC loop, and the entire dihydrouridine loop is lacking. This seryl tRNA molecule is therefore shorter than other tRNAs. It was originally thought to represent a mitochondrial analogon of 5 S rRNA and its precise classification is still disputed. The present studies suggest that this mitochondrial tRNA represents a fossil molecule which is related to the common ancestor of the present tRNA and 5 S rRNA molecules.

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Role of the Digestive Gland in Ink Production in Four Species of Sea Hares: An Ultrastructural Comparison

Journal of Marine Biology ◽

10.1155/2013/209496 ◽

2013 ◽

Vol 2013 ◽

pp. 1-5 ◽

Cited By ~ 3

Author(s):

Jeffrey S. Prince ◽

Paul Micah Johnson

Keyword(s):

Digestive Gland ◽

Common Ancestor ◽

Aplysia Californica ◽

Digestive Cell ◽

Digestive Cells ◽

Sea Hare ◽

Red Algal ◽

The Common ◽

Algal Chloroplast

The ultrastructure of the digestive gland of several sea hare species that produce different colored ink (Aplysia californicaproduces purple ink,A. julianawhite ink,A. parvulaboth white and purple ink, whileDolabrifera dolabriferaproduces no ink at all) was compared to determine the digestive gland’s role in the diet-derived ink production process. Rhodoplast digestive cells and their digestive vacuoles, the site of digestion of red algal chloroplast (i.e., rhodoplast) inA. californica, were present and had a similar ultrastructure in all four species. Rhodoplast digestive cell vacuoles either contained a whole rhodoplast or fragments of one or were empty. These results suggest that the inability to produce colored ink in some sea hare species is not due to either an absence of appropriate digestive machinery, that is, rhodoplast digestive cells, or an apparent failure of rhodoplast digestive cells to function. These results also propose that the digestive gland structure described herein occurred early in sea hare evolution, at least in the common ancestor to the generaAplysiaandDolabrifera. Our data, however, do not support the hypothesis that the loss of purple inking is a synapomorphy of the white-ink-producing subgenusAplysia.

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Sexual reproduction and genetic exchange in parasitic protists

Parasitology ◽

10.1017/s0031182014001693 ◽

2014 ◽

Vol 142 (S1) ◽

pp. S120-S127 ◽

Cited By ~ 29

Author(s):

GARETH D. WEEDALL ◽

NEIL HALL

Keyword(s):

Life Cycle ◽

Genome Sequencing ◽

Common Ancestor ◽

Life Cycles ◽

Animal Disease ◽

Eukaryotic Evolution ◽

Sequencing Technology ◽

Parasite Reproduction ◽

The Common ◽

Higher Eukaryotes

SUMMARYA key part of the life cycle of an organism is reproduction. For a number of important protist parasites that cause human and animal disease, their sexuality has been a topic of debate for many years. Traditionally, protists were considered to be primitive relatives of the ‘higher’ eukaryotes, which may have diverged prior to the evolution of sex and to reproduce by binary fission. More recent views of eukaryotic evolution suggest that sex, and meiosis, evolved early, possibly in the common ancestor of all eukaryotes. However, detecting sex in these parasites is not straightforward. Recent advances, particularly in genome sequencing technology, have allowed new insights into parasite reproduction. Here, we review the evidence on reproduction in parasitic protists. We discuss protist reproduction in the light of parasitic life cycles and routes of transmission among hosts.

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Whole-genome analysis-based phylogeographic investigation of Streptococcus pneumoniae serotype 19A sequence type 320 isolates in Japan.

Antimicrobial Agents and Chemotherapy ◽

10.1128/aac.01395-21 ◽

2021 ◽

Author(s):

Satoshi Nakano ◽

Takao Fujisawa ◽

Bin Chang ◽

Yutaka Ito ◽

Hideki Akeda ◽

...

Keyword(s):

Common Ancestor ◽

Sampling Bias ◽

Health Concern ◽

Recent Common Ancestor ◽

Whole Genome ◽

Whole Genome Analysis ◽

Identification Rate ◽

Most Recent Common Ancestor ◽

The Common ◽

The U.S

After the introduction of the seven-valent pneumococcal conjugate vaccine, the global spread of multidrug resistant serotype 19A-ST320 strains became a public health concern. In Japan, the main genotype of serotype 19A was ST3111, and the identification rate of ST320 was low. Although the isolates were sporadically detected in both adults and children, their origin remains unknown. Thus, by combining pneumococcal isolates collected in three nationwide pneumococcal surveillance studies conducted in Japan between 2008 and 2020, we analyzed 56 serotype 19A-ST320 isolates along with 931 global isolates, using whole-genome sequencing to uncover the transmission route of the globally distributed clone in Japan. The clone was frequently detected in Okinawa Prefecture, where the U.S. returned to Japan in 1972. Phylogenetic analysis demonstrated that the isolates from Japan were genetically related to those from the U.S.; therefore, the common ancestor may have originated in the U.S. In addition, Bayesian analysis suggested that the time to the most recent common ancestor of the isolates form Japan and the U.S. was approximately the 1990s to 2000, suggesting the possibility that the common ancestor could have already spread in the U.S. before the Taiwan 19F-14 isolate was first identified in a Taiwanese hospital in 1997. The phylogeographical analysis supported the transmission of the clone from the U.S. to Japan, but the analysis could be influenced by sampling bias. These results suggested the possibility that the serotype 19A-ST320 clone had already spread in the U.S. before being imported into Japan.

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The Common Ancestor of Man and Apes

Science ◽

10.1126/science.59.1530.xii-s ◽

1924 ◽

Vol 59 (1530) ◽

Keyword(s):

Common Ancestor ◽

The Common

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From the Common Ancestor of all Living Organisms to Protoeukaryotic Cell

Thermophiles ◽

10.1201/9781482273045-33 ◽

1998 ◽

pp. 307-316

Keyword(s):

Common Ancestor ◽

The Common ◽

Living Organisms

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Comparing the folding landscapes of evolutionarily divergent procaspase-3

10.1101/2022.01.12.476064 ◽

2022 ◽

Author(s):

Liqi Yao ◽

Clay Clark

Keyword(s):

Conformational Change ◽

Common Ancestor ◽

Folding Pathway ◽

Free Energies ◽

Folding Intermediates ◽

Effector Caspases ◽

The Common ◽

Ph Dependent ◽

Species Specific ◽

Dimeric Intermediate

All caspases evolved from a common ancestor and subsequently developed into two general classes, inflammatory or apoptotic caspases. The caspase-hemoglobinase fold has been conserved throughout nearly one billion years of evolution and is utilized for both the monomeric and dimeric subfamilies of apoptotic caspases, called initiator and effector caspases, respectively. We compared the folding and assembly of procaspase-3b from zebrafish to that of human effector procaspases in order to examine the conservation of the folding landscape. Urea-induced equilibrium folding/unfolding of procaspase-3b showed a minimum three-state folding pathway, where the native dimer isomerizes to a partially folded dimeric intermediate, which then unfolds. A partially folded monomeric intermediate observed in the folding landscape of human procaspase-3 is not well-populated in zebrafish procaspase-3b. By comparing effector caspases from different species, we show that the effector procaspase dimer undergoes a pH-dependent conformational change, and that the conformational species in the folding landscape exhibit similar free energies. Together, the data show that the landscape for the caspase-hemoglobinase fold is conserved, yet it provides flexibility for species-specific stabilization or destabilization of folding intermediates resulting in changes in stability. The common pH-dependent conformational change in the native dimer, which yields an enzymatically inactive species, may provide an additional, albeit reversible, mechanism for controlling caspase activity in the cell.

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