Transib

Last updated October 06, 2021

Transib is a superfamily of interspersed repeats DNA transposons. It was named after the Trans-Siberian Express.^[1] It is similar to EnSpm/CACTA.

Transib was first described in 2003, discovered in the Drosophila melanogaster genome. It usually encodes a single protein, DDE transcriptase.^[1] An intact element including terminal inverted repeats (TIR) was found in 2008 in the Helicoverpa zea genome.^[2] Divergent clades of this superfamily has since been discovered and dubbed Transib and TransibSU (for sea urchin); Chapaev and Chapaev3 of the CACTA superfamily are sometimes included too. The differences lie in the domain organization of the core transcriptase; TransibSU is also notable for having RAG2-like proteins.^[3]^{: fig. 2}

Transib is notable as the source of the two Recombination-activating genes. An active transposon with RAG1/2-like genes ("ProtoRAG"; PDB: 6B40 ) has been discovered in B. belcheri (Chinese lancelet). The TIRs are structurally similar to Recombination signal sequences (RSS). The heptamer bears the consensus CACWRTG, while the nonamer is more divergent. Lancelet RAG1L/TIR does not cross-recognize animal RAG1/RSS due to differences in the nonamer.^[4] Psectrotarsia flava (a moth) also has such a transposon. It lacks the nonamer, indicating the nonamer's more recent evolution.^[5]

Related Research Articles

Drosophila is a genus of flies, belonging to the family Drosophilidae, whose members are often called "small fruit flies" or pomace flies, vinegar flies, or wine flies, a reference to the characteristic of many species to linger around overripe or rotting fruit. They should not be confused with the Tephritidae, a related family, which are also called fruit flies ; tephritids feed primarily on unripe or ripe fruit, with many species being regarded as destructive agricultural pests, especially the Mediterranean fruit fly.

A transposable element is a DNA sequence that can change its position within a genome, sometimes creating or reversing mutations and altering the cell's genetic identity and genome size. Transposition often results in duplication of the same genetic material. Barbara McClintock's discovery of them earned her a Nobel Prize in 1983.

Genetic recombination is the exchange of genetic material between different organisms which leads to production of offspring with combinations of traits that differ from those found in either parent. In eukaryotes, genetic recombination during meiosis can lead to a novel set of genetic information that can be passed on from the parents to the offspring. Most recombination is naturally occurring.

A gene family is a set of several similar genes, formed by duplication of a single original gene, and generally with similar biochemical functions. One such family are the genes for human hemoglobin subunits; the ten genes are in two clusters on different chromosomes, called the α-globin and β-globin loci. These two gene clusters are thought to have arisen as a result of a precursor gene being duplicated approximately 500 million years ago.

Retrotransposons are a type of genetic component that copy and paste themselves into different genomic locations (transposon) by converting RNA back into DNA through the process reverse transcription using an RNA transposition intermediate.

Intragenomic conflict refers to the evolutionary phenomenon where genes have phenotypic effects that promote their own transmission in detriment of the transmission of other genes that reside in the same genome. The selfish gene theory postulates that natural selection will increase the frequency of those genes whose phenotypic effects cause their transmission to new organisms, and most genes achieve this by cooperating with other genes in the same genome to build an organism capable of reproducing and/or helping kin to reproduce. The assumption of the prevalence of intragenomic cooperation underlies the organism-centered concept of inclusive fitness. However, conflict among genes in the same genome may arise both in events related to reproduction and altruism.

V(D)J recombination is the mechanism of somatic recombination that occurs only in developing lymphocytes during the early stages of T and B cell maturation. It results in the highly diverse repertoire of antibodies/immunoglobulins and T cell receptors (TCRs) found in B cells and T cells, respectively. The process is a defining feature of the adaptive immune system.

Exon shuffling is a molecular mechanism for the formation of new genes. It is a process through which two or more exons from different genes can be brought together ectopically, or the same exon can be duplicated, to create a new exon-intron structure. There are different mechanisms through which exon shuffling occurs: transposon mediated exon shuffling, crossover during sexual recombination of parental genomes and illegitimate recombination.

The recombination-activating genes (RAGs) encode parts of a protein complex that plays important roles in the rearrangement and recombination of the genes encoding immunoglobulin and T cell receptor molecules. There are two recombination-activating genes RAG1 and RAG2, whose cellular expression is restricted to lymphocytes during their developmental stages. The enzymes encoded by these genes, RAG-1 and RAG-2, are essential to the generation of mature B cells and T cells, two types of lymphocyte that are crucial components of the adaptive immune system.

Piwi-interacting RNA (piRNA) is the largest class of small non-coding RNA molecules expressed in animal cells. piRNAs form RNA-protein complexes through interactions with piwi-subfamily Argonaute proteins. These piRNA complexes are mostly involved in the epigenetic and post-transcriptional silencing of transposable elements and other spurious or repeat-derived transcripts, but can also be involved in the regulation of other genetic elements in germ line cells.

The mobilome is the entire set of mobile genetic elements in a genome. Mobilomes are found in eukaryotes, prokaryotes, and viruses. The compositions of mobilomes differ among lineages of life, with transposable elements being the major mobile elements in eukaryotes, and plasmids and prophages being the major types in prokaryotes. Virophages contribute to the viral mobilome.

Helitrons are one of the three groups of eukaryotic class 2 transposable elements (TEs) so far described. They are the eukaryotic rolling-circle transposable elements which are hypothesized to transpose by a rolling circle replication mechanism via a single-stranded DNA intermediate. They were first discovered in plants and in the nematode Caenorhabditis elegans, and now they have been identified in a diverse range of species, from protists to mammals. Helitrons make up a substantial fraction of many genomes where non-autonomous elements frequently outnumber the putative autonomous partner. Helitrons seem to have a major role in the evolution of host genomes. They frequently capture diverse host genes, some of which can evolve into novel host genes or become essential for Helitron transposition.

Transposons are semi-parasitic DNA sequences which can replicate and spread through the host's genome. They can be harnessed as a genetic tool for analysis of gene and protein function. The use of transposons is well-developed in Drosophila and in Thale cress and bacteria such as Escherichia coli.

Miniature Inverted-repeat Transposable Elements (MITEs) are a group of non-autonomous Class II transposable elements. Being non-autonomous, MITEs cannot code for their own transposase. They exist within the genomes of animals, plants, fungi and bacteria. MITEs are generally short elements with terminal inverted repeats and two flanking target site duplications (TSDs). Like other transposons, MITEs are inserted predominantly in gene-rich regions and this can be a reason that they affect gene expression and play important roles in accelerating eukaryotic evolution. Their high copy number in spite of small sizes has been a topic of interest.

A transpoviron is a plasmid-like genetic element found in the genomes of giant DNA viruses.

DNA transposons are DNA sequences, sometimes referred to "jumping genes", that can move and integrate to different locations within the genome. They are class II transposable elements (TEs) that move through a DNA intermediate, as opposed to class I TEs, retrotransposons, that move through an RNA intermediate. DNA transposons can move in the DNA of an organism via a single-or double-stranded DNA intermediate. DNA transposons have been found in both prokaryotic and eukaryotic organisms. They can make up a significant portion of an organism's genome, particularly in eukaryotes. In prokaryotes, TE's can facilitate the horizontal transfer of antibiotic resistance or other genes associated with virulence. After replicating and propagating in a host, all transposon copies become inactivated and are lost unless the transposon passes to a genome by starting a new life cycle with horizontal transfer. It is important to note that DNA transposons do not randomly insert themselves into the genome, but rather show preference for specific sites.

Tc1/mariner is a class and superfamily of interspersed repeats DNA transposons. The elements of this class are found in all animals, including humans. They can also be found in protists and bacteria.

Metavirus is a genus of viruses in the family Metaviridae. They are retrotransposons that invade a eukaryotic host genome and may only replicate once the virus has infected the host. These genetic elements exist to infect and replicate in their host genome and are derived from ancestral elements unrelated from their host. Metavirus may use several different hosts for transmission, and has been found to be transmissible through ovule and pollen of some plants.

hAT transposons are a superfamily of DNA transposons, or Class II transposable elements, that are common in the genomes of plants, animals, and fungi.

Helicoverpa zea nudivirus 2 is an enveloped, rod-shaped, nonoccluded, double stranded DNA (dsDNA) sexually transmitted virus whose natural host is the corn earworm moth. At about 440 by 90 nm, it is the causative agent of the only sexually transmitted viral disease of any insect. It was originally identified in a colony of corn earworm moths established and maintained in Stoneville, Mississippi, U.S. and was found to be responsible for the sterility of those infected.

References

1 2 Kapitonov, V. V.; Jurka, J. (12 May 2003). "Molecular paleontology of transposable elements in the Drosophila melanogaster genome". Proceedings of the National Academy of Sciences. 100 (11): 6569–6574. Bibcode:2003PNAS..100.6569K. doi: 10.1073/pnas.0732024100 . PMC 164487 . PMID 12743378.
↑ Chen, S; Li, X (31 January 2008). "Molecular characterization of the first intact Transib transposon from Helicoverpa zea". Gene. 408 (1–2): 51–63. doi:10.1016/j.gene.2007.10.015. PMID 18031956.
↑ Kapitonov VV, Koonin EV (2015-04-28). "Evolution of the RAG1-RAG2 locus: both proteins came from the same transposon". Biology Direct. 10 (1): 20. doi:10.1186/s13062-015-0055-8. PMC 4411706 . PMID 25928409.
↑ Huang, S; Tao, X; Yuan, S; Zhang, Y; Li, P; Beilinson, HA; Zhang, Y; Yu, W; Pontarotti, P; Escriva, H; Le Petillon, Y; Liu, X; Chen, S; Schatz, DG; Xu, A (30 June 2016). "Discovery of an Active RAG Transposon Illuminates the Origins of V(D)J Recombination". Cell. 166 (1): 102–14. doi:10.1016/j.cell.2016.05.032. PMC 5017859 . PMID 27293192.
↑ Morales Poole, Jose Ricardo; Huang, Sheng Feng; Xu, Anlong; Bayet, Justine; Pontarotti, Pierre (28 April 2017). "The RAG transposon is active through the deuterostome evolution and domesticated in jawed vertebrates". Immunogenetics. 69 (6): 391–400. bioRxiv 10.1101/100735 . doi:10.1007/s00251-017-0979-5. PMID 28451741. S2CID 11192471.

This page is based on this Wikipedia article
Text is available under the CC BY-SA 4.0 license; additional terms may apply.
Images, videos and audio are available under their respective licenses.

[Kapitonov_2003-1] 1 2 Kapitonov, V. V.; Jurka, J. (12 May 2003). "Molecular paleontology of transposable elements in the Drosophila melanogaster genome". Proceedings of the National Academy of Sciences. 100 (11): 6569–6574. Bibcode:2003PNAS..100.6569K. doi: 10.1073/pnas.0732024100 . PMC 164487 . PMID 12743378.

[2] Chen, S; Li, X (31 January 2008). "Molecular characterization of the first intact Transib transposon from Helicoverpa zea". Gene. 408 (1–2): 51–63. doi:10.1016/j.gene.2007.10.015. PMID 18031956.

[Kapitonov_2015-3] Kapitonov VV, Koonin EV (2015-04-28). "Evolution of the RAG1-RAG2 locus: both proteins came from the same transposon". Biology Direct. 10 (1): 20. doi:10.1186/s13062-015-0055-8. PMC 4411706 . PMID 25928409.

[pmid27293192-4] Huang, S; Tao, X; Yuan, S; Zhang, Y; Li, P; Beilinson, HA; Zhang, Y; Yu, W; Pontarotti, P; Escriva, H; Le Petillon, Y; Liu, X; Chen, S; Schatz, DG; Xu, A (30 June 2016). "Discovery of an Active RAG Transposon Illuminates the Origins of V(D)J Recombination". Cell. 166 (1): 102–14. doi:10.1016/j.cell.2016.05.032. PMC 5017859 . PMID 27293192.

[5] Morales Poole, Jose Ricardo; Huang, Sheng Feng; Xu, Anlong; Bayet, Justine; Pontarotti, Pierre (28 April 2017). "The RAG transposon is active through the deuterostome evolution and domesticated in jawed vertebrates". Immunogenetics. 69 (6): 391–400. bioRxiv 10.1101/100735 . doi:10.1007/s00251-017-0979-5. PMID 28451741. S2CID 11192471.

[1]

[2]

[3]

[4]

[5]