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Embryos generated from oocytes lacking complex N- and O-glycans have compromised development and implantation

Female mice generating oocytes lacking complex N- and O-glycans (double mutants (DM)) produce only one small litter before undergoing premature ovarian failure (POF) by 3 months. Here we investigate the basis of the small litter by evaluating ovulation rate and embryo development in DM (Mgat1(F/F)C1...

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Autores principales: Grasa, Patricia, Kaune, Heidy, Williams, Suzannah A
Formato: Online Artículo Texto
Lenguaje:English
Publicado: BioScientifica 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3464042/
https://www.ncbi.nlm.nih.gov/pubmed/22919046
http://dx.doi.org/10.1530/REP-12-0084
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author Grasa, Patricia
Kaune, Heidy
Williams, Suzannah A
author_facet Grasa, Patricia
Kaune, Heidy
Williams, Suzannah A
author_sort Grasa, Patricia
collection PubMed
description Female mice generating oocytes lacking complex N- and O-glycans (double mutants (DM)) produce only one small litter before undergoing premature ovarian failure (POF) by 3 months. Here we investigate the basis of the small litter by evaluating ovulation rate and embryo development in DM (Mgat1(F/F)C1galt1(F/F):ZP3Cre) and Control (Mgat1(F/F)C1galt1(F/F)) females. Surprisingly, DM ovulation rate was normal at 6 weeks, but declined dramatically by 9 weeks. In vitro development of zygotes to blastocysts was equivalent to Controls although all embryos from DM females lacked a normal zona pellucida (ZP) and ∼30% lacked a ZP entirely. In contrast, in vivo preimplantation development resulted in less embryos recovered from DM females compared with Controls at 3.5 days post coitum (dpc) (3.2±1.3 vs 7.0±0.6). Furthermore, only 45% of mated DM females contained embryos at 3.5 dpc. Of the preimplantation embryos collected from DM females, approximately half were morulae unlike Controls where the majority were blastocysts, indicating delayed embryo development in DM females. Post-implantation development in DM females was analysed to determine whether delayed preimplantation development affected subsequent development. In DM females at 5.5 dpc, only ∼40% of embryos found at 3.5 dpc had implanted. However, at 6.5 dpc, implantation sites in DM females corresponded to embryo numbers at 3.5 dpc indicating delayed implantation. At 9.5 dpc, the number of decidua corresponded to embryo numbers 6 days earlier indicating that all implanted embryos progress to midgestation. Therefore, a lack of complex N- and O-glycans in oocytes during development impairs early embryo development and viability in vivo leading to delayed implantation and a small litter.
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spelling pubmed-34640422012-10-04 Embryos generated from oocytes lacking complex N- and O-glycans have compromised development and implantation Grasa, Patricia Kaune, Heidy Williams, Suzannah A Reproduction Research Female mice generating oocytes lacking complex N- and O-glycans (double mutants (DM)) produce only one small litter before undergoing premature ovarian failure (POF) by 3 months. Here we investigate the basis of the small litter by evaluating ovulation rate and embryo development in DM (Mgat1(F/F)C1galt1(F/F):ZP3Cre) and Control (Mgat1(F/F)C1galt1(F/F)) females. Surprisingly, DM ovulation rate was normal at 6 weeks, but declined dramatically by 9 weeks. In vitro development of zygotes to blastocysts was equivalent to Controls although all embryos from DM females lacked a normal zona pellucida (ZP) and ∼30% lacked a ZP entirely. In contrast, in vivo preimplantation development resulted in less embryos recovered from DM females compared with Controls at 3.5 days post coitum (dpc) (3.2±1.3 vs 7.0±0.6). Furthermore, only 45% of mated DM females contained embryos at 3.5 dpc. Of the preimplantation embryos collected from DM females, approximately half were morulae unlike Controls where the majority were blastocysts, indicating delayed embryo development in DM females. Post-implantation development in DM females was analysed to determine whether delayed preimplantation development affected subsequent development. In DM females at 5.5 dpc, only ∼40% of embryos found at 3.5 dpc had implanted. However, at 6.5 dpc, implantation sites in DM females corresponded to embryo numbers at 3.5 dpc indicating delayed implantation. At 9.5 dpc, the number of decidua corresponded to embryo numbers 6 days earlier indicating that all implanted embryos progress to midgestation. Therefore, a lack of complex N- and O-glycans in oocytes during development impairs early embryo development and viability in vivo leading to delayed implantation and a small litter. BioScientifica 2012-10 /pmc/articles/PMC3464042/ /pubmed/22919046 http://dx.doi.org/10.1530/REP-12-0084 Text en © 2012 Society for Reproduction and Fertility http://www.bioscientifica.com/journals/reuselicencerep/ This is an Open Access article distributed under the terms of the Society for Reproduction and Fertility's Re-use Licence (http://www.bioscientifica.com/journals/reuselicencerep/) which permits unrestricted non-commercial use, distribution, and reproduction in any medium, provided the original work is properly cited.
spellingShingle Research
Grasa, Patricia
Kaune, Heidy
Williams, Suzannah A
Embryos generated from oocytes lacking complex N- and O-glycans have compromised development and implantation
title Embryos generated from oocytes lacking complex N- and O-glycans have compromised development and implantation
title_full Embryos generated from oocytes lacking complex N- and O-glycans have compromised development and implantation
title_fullStr Embryos generated from oocytes lacking complex N- and O-glycans have compromised development and implantation
title_full_unstemmed Embryos generated from oocytes lacking complex N- and O-glycans have compromised development and implantation
title_short Embryos generated from oocytes lacking complex N- and O-glycans have compromised development and implantation
title_sort embryos generated from oocytes lacking complex n- and o-glycans have compromised development and implantation
topic Research
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3464042/
https://www.ncbi.nlm.nih.gov/pubmed/22919046
http://dx.doi.org/10.1530/REP-12-0084
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