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Computational Analysis of the Potential Impact of MTC Complex Missenses SNPs Associated with Male Infertility

Meiotic chromosomes endure rapid prophase movements that ease the formation of interhomologue recombination intermediates that drive synapsis, crossing over, and segregation process. To generate these fast moves, the meiotic telomere complex (MTC) enables telomere-inner nuclear membrane attachment d...

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Autores principales: Harmak, Houda, Charoute, Hicham, Redouane, Salaheddine, Filali, Ouafaa Aniq, Barakat, Abdelhamid, Rouba, Hassan
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Hindawi 2022
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8956405/
https://www.ncbi.nlm.nih.gov/pubmed/35342767
http://dx.doi.org/10.1155/2022/1664825
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author Harmak, Houda
Charoute, Hicham
Redouane, Salaheddine
Filali, Ouafaa Aniq
Barakat, Abdelhamid
Rouba, Hassan
author_facet Harmak, Houda
Charoute, Hicham
Redouane, Salaheddine
Filali, Ouafaa Aniq
Barakat, Abdelhamid
Rouba, Hassan
author_sort Harmak, Houda
collection PubMed
description Meiotic chromosomes endure rapid prophase movements that ease the formation of interhomologue recombination intermediates that drive synapsis, crossing over, and segregation process. To generate these fast moves, the meiotic telomere complex (MTC) enables telomere-inner nuclear membrane attachment during meiotic prophase I and transfers cytoskeletal signals via another complex: the LINC complex. Furthermore, disruption or mutations of any of the MTC genes (TERB1, TERB2, and MAJIN) alters telomere association with the nuclear envelope leading to impairment of homologous pairing and synapsis, a meiotic arrest, and consequently to male infertility. To decipher the effect of TERB1, TERB2, and MAJIN missense mutations on protein structure, stability, and function, different bioinformatic tools were used in this study including VEP, Mutabind2, Haddock, Prodigy, Ligplot, ConSurf, DUET and MusiteDeep. In total, thirty mutations were predicted to be deleterious using VEP web server: seventeen for TERB1, eleven for TERB2, and two for MAJIN. All these single nucleotide polymorphisms were further analyzed and only 11 SNPs (W8R, G25R, P649A, I624T, C618R, F607V, S604G, C592Y, C592R, G187W, and R53C) were found to be the most damaging by at least six software tools and exert deleterious effect on the TERB1, TERB2, and MAJIN protein structures and likely functions. They revealed high conservation, less stability, and having a role in posttranslational modifications. This in silico approach provides information to gain further insights about variants that might affect stability, change binding affinity, and edit protein-protein interactions to facilitate their identification and functional characterization associated with male infertility.
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spelling pubmed-89564052022-03-26 Computational Analysis of the Potential Impact of MTC Complex Missenses SNPs Associated with Male Infertility Harmak, Houda Charoute, Hicham Redouane, Salaheddine Filali, Ouafaa Aniq Barakat, Abdelhamid Rouba, Hassan Biomed Res Int Research Article Meiotic chromosomes endure rapid prophase movements that ease the formation of interhomologue recombination intermediates that drive synapsis, crossing over, and segregation process. To generate these fast moves, the meiotic telomere complex (MTC) enables telomere-inner nuclear membrane attachment during meiotic prophase I and transfers cytoskeletal signals via another complex: the LINC complex. Furthermore, disruption or mutations of any of the MTC genes (TERB1, TERB2, and MAJIN) alters telomere association with the nuclear envelope leading to impairment of homologous pairing and synapsis, a meiotic arrest, and consequently to male infertility. To decipher the effect of TERB1, TERB2, and MAJIN missense mutations on protein structure, stability, and function, different bioinformatic tools were used in this study including VEP, Mutabind2, Haddock, Prodigy, Ligplot, ConSurf, DUET and MusiteDeep. In total, thirty mutations were predicted to be deleterious using VEP web server: seventeen for TERB1, eleven for TERB2, and two for MAJIN. All these single nucleotide polymorphisms were further analyzed and only 11 SNPs (W8R, G25R, P649A, I624T, C618R, F607V, S604G, C592Y, C592R, G187W, and R53C) were found to be the most damaging by at least six software tools and exert deleterious effect on the TERB1, TERB2, and MAJIN protein structures and likely functions. They revealed high conservation, less stability, and having a role in posttranslational modifications. This in silico approach provides information to gain further insights about variants that might affect stability, change binding affinity, and edit protein-protein interactions to facilitate their identification and functional characterization associated with male infertility. Hindawi 2022-03-18 /pmc/articles/PMC8956405/ /pubmed/35342767 http://dx.doi.org/10.1155/2022/1664825 Text en Copyright © 2022 Houda Harmak et al. https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research Article
Harmak, Houda
Charoute, Hicham
Redouane, Salaheddine
Filali, Ouafaa Aniq
Barakat, Abdelhamid
Rouba, Hassan
Computational Analysis of the Potential Impact of MTC Complex Missenses SNPs Associated with Male Infertility
title Computational Analysis of the Potential Impact of MTC Complex Missenses SNPs Associated with Male Infertility
title_full Computational Analysis of the Potential Impact of MTC Complex Missenses SNPs Associated with Male Infertility
title_fullStr Computational Analysis of the Potential Impact of MTC Complex Missenses SNPs Associated with Male Infertility
title_full_unstemmed Computational Analysis of the Potential Impact of MTC Complex Missenses SNPs Associated with Male Infertility
title_short Computational Analysis of the Potential Impact of MTC Complex Missenses SNPs Associated with Male Infertility
title_sort computational analysis of the potential impact of mtc complex missenses snps associated with male infertility
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8956405/
https://www.ncbi.nlm.nih.gov/pubmed/35342767
http://dx.doi.org/10.1155/2022/1664825
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