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Evolutionary history and origin of Tre1 superfamily shed light on its role in regulating blood brain barrier

Norwin Kubick, Pavel Klimovich, Irmina Bieńkowska, Mariusz Sacharczuk, Michel-Edwar Mickael
doi: https://doi.org/10.1101/2021.04.29.441935
Norwin Kubick
1Department of Biochemistry and Molecular Cell Biology (IBMZ), University Medical Center Hamburg-Eppendorf, Martinistraße 52, 20246 Hamburg, Germany
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Pavel Klimovich
2Department of Immunology, PM Forskningscentreum, 17854 Ekerö Stockholm, Sweden
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Irmina Bieńkowska
1Department of Biochemistry and Molecular Cell Biology (IBMZ), University Medical Center Hamburg-Eppendorf, Martinistraße 52, 20246 Hamburg, Germany
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Mariusz Sacharczuk
1Department of Biochemistry and Molecular Cell Biology (IBMZ), University Medical Center Hamburg-Eppendorf, Martinistraße 52, 20246 Hamburg, Germany
4Department of Pharmacodynamics, Faculty of Pharmacy, Warsaw Medical University, l Banacha 1, 02-697 Warsaw, Poland
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Michel-Edwar Mickael
2Department of Immunology, PM Forskningscentreum, 17854 Ekerö Stockholm, Sweden
3Department of Experimental Genomics, Institute of Animal Biotechnology and Genetics, Polish Academy of Science, Postepu 36A, 05-552 Jastrzebiec, Poland
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  • For correspondence: Michel.edwar77@gmail.com
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Abstract

Understanding how the evolutionary relationship between immune cells and the blood-brain is important to devise therapeutic strategies that can regulate their critical function. In vertebrates, immune cells follow either a paracellular or transcellular pathway to infiltrate the BBB. In drosophila glial cells form the BBB that regulates the access of immune-like cells to the drosophila brain. However, it is still not known which route immune-like cells follow to infiltrate the drosophila brain. In vertebrates, paracellular migration is dependent on PECAM1, while transcellular migration is dependent on the expression of CAV1. Interestingly drosophila genome lacks both genes. Tre1 superfamily (Tre1, Moody, and Dmel_CG4313) play a diverse role in regulating transepithelial migration in drosophila. However, its evolutionary history and origin are not yet known. We performed phylogenetic analysis, together with HH search, positive selection, and ancestral reconstruction to investigate the Tre1 family Interestingly we found that Tre1 exists in mollusks, insects, ambulacria, and sclaidphora. Moody is shown to be a more ancient protein and it existed since cnidaria emergence and has a homolog (GPCR84) in mammals. The third family member (Dmel_CG4313) only exists in insects. The origin of the family seems to be related to the rhodopsin-like family and in particular family α. We found that opsin is the nearest receptor to have a common ancestor with the Tre1 superfamily that seems to have diverged in sponges. We investigated the positive selection of the Tre1 family using PAML. Tre1 seems to have evolved under negative selection, whereas Moody has evolved during positive selection. The sites that we found under positive selection are Likely to play a role in the speciation of function in the case of Moody. We have identified an SH3, in Tre1 and, moody and Dmel_CG4313. Sh3 is known to play a fundamental role in regulating actin movement in a Rho-dependent manner. We suggest that Tre1 could be playing an important role in paracellular diapedesis in drosophila.

Competing Interest Statement

The authors have declared no competing interest.

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Posted April 30, 2021.
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Evolutionary history and origin of Tre1 superfamily shed light on its role in regulating blood brain barrier
Norwin Kubick, Pavel Klimovich, Irmina Bieńkowska, Mariusz Sacharczuk, Michel-Edwar Mickael
bioRxiv 2021.04.29.441935; doi: https://doi.org/10.1101/2021.04.29.441935
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Evolutionary history and origin of Tre1 superfamily shed light on its role in regulating blood brain barrier
Norwin Kubick, Pavel Klimovich, Irmina Bieńkowska, Mariusz Sacharczuk, Michel-Edwar Mickael
bioRxiv 2021.04.29.441935; doi: https://doi.org/10.1101/2021.04.29.441935

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