Significant decrease of maternal mitochondria carryover using optimized spindle-chromosomal complex transfer

Mutations in mitochondrial DNA (mtDNA) contribute to a variety of serious multi-organ human diseases, which are strictly inherited from the maternal germline. However, there is currently no curative treatment. Attention has been focused on preventing the transmission of mitochondrial diseases throug...

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Autores principales: Liao, Xiaoyu, Li, Wenzhi, Lin, Kaibo, Jin, Wei, Zhang, Shaozhen, Wang, Yao, Ma, Meng, Xie, Yating, Yu, Weina, Yan, Zhiguang, Gao, Hongyuan, Zhao, Leiwen, Si, Jiqiang, Wang, Yun, Lin, Jiaying, Chen, Chen, Chen, Li, Kuang, Yanping, Lyu, Qifeng
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2023
Materias:
Methods and Resources
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10553349/
https://www.ncbi.nlm.nih.gov/pubmed/37796762
http://dx.doi.org/10.1371/journal.pbio.3002313
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author Liao, Xiaoyu
Li, Wenzhi
Lin, Kaibo
Jin, Wei
Zhang, Shaozhen
Wang, Yao
Ma, Meng
Xie, Yating
Yu, Weina
Yan, Zhiguang
Gao, Hongyuan
Zhao, Leiwen
Si, Jiqiang
Wang, Yun
Lin, Jiaying
Chen, Chen
Chen, Li
Kuang, Yanping
Lyu, Qifeng
author_facet Liao, Xiaoyu
Li, Wenzhi
Lin, Kaibo
Jin, Wei
Zhang, Shaozhen
Wang, Yao
Ma, Meng
Xie, Yating
Yu, Weina
Yan, Zhiguang
Gao, Hongyuan
Zhao, Leiwen
Si, Jiqiang
Wang, Yun
Lin, Jiaying
Chen, Chen
Chen, Li
Kuang, Yanping
Lyu, Qifeng
author_sort Liao, Xiaoyu
collection PubMed
description Mutations in mitochondrial DNA (mtDNA) contribute to a variety of serious multi-organ human diseases, which are strictly inherited from the maternal germline. However, there is currently no curative treatment. Attention has been focused on preventing the transmission of mitochondrial diseases through mitochondrial replacement (MR) therapy, but levels of mutant mtDNA can often unexpectedly undergo significant changes known as mitochondrial genetic drift. Here, we proposed a novel strategy to perform spindle-chromosomal complex transfer (SCCT) with maximal residue removal (MRR) in metaphase II (MII) oocytes, thus hopefully eliminated the transmission of mtDNA diseases. With the MRR procedure, we initially investigated the proportions of mtDNA copy numbers in isolated karyoplasts to those of individual oocytes. Spindle-chromosomal morphology and copy number variation (CNV) analysis also confirmed the safety of this method. Then, we reconstructed oocytes by MRR-SCCT, which well developed to blastocysts with minimal mtDNA residue and normal chromosomal copy numbers. Meanwhile, we optimized the manipulation order between intracytoplasmic sperm injection (ICSI) and SCC transfer and concluded that ICSI-then-transfer was conducive to avoid premature activation of reconstructed oocytes in favor of normal fertilization. Offspring of mice generated by embryos transplantation in vivo and embryonic stem cells derivation further presented evidences for competitive development competence and stable mtDNA carryover without genetic drift. Importantly, we also successfully accomplished SCCT in human MII oocytes resulting in tiny mtDNA residue and excellent embryo development through MRR manipulation. Taken together, our preclinical mouse and human models of the MRR-SCCT strategy not only demonstrated efficient residue removal but also high compatibility with normal embryo development, thus could potentially be served as a feasible clinical treatment to prevent the transmission of inherited mtDNA diseases.
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spelling pubmed-105533492023-10-06 Significant decrease of maternal mitochondria carryover using optimized spindle-chromosomal complex transfer Liao, Xiaoyu Li, Wenzhi Lin, Kaibo Jin, Wei Zhang, Shaozhen Wang, Yao Ma, Meng Xie, Yating Yu, Weina Yan, Zhiguang Gao, Hongyuan Zhao, Leiwen Si, Jiqiang Wang, Yun Lin, Jiaying Chen, Chen Chen, Li Kuang, Yanping Lyu, Qifeng PLoS Biol Methods and Resources Mutations in mitochondrial DNA (mtDNA) contribute to a variety of serious multi-organ human diseases, which are strictly inherited from the maternal germline. However, there is currently no curative treatment. Attention has been focused on preventing the transmission of mitochondrial diseases through mitochondrial replacement (MR) therapy, but levels of mutant mtDNA can often unexpectedly undergo significant changes known as mitochondrial genetic drift. Here, we proposed a novel strategy to perform spindle-chromosomal complex transfer (SCCT) with maximal residue removal (MRR) in metaphase II (MII) oocytes, thus hopefully eliminated the transmission of mtDNA diseases. With the MRR procedure, we initially investigated the proportions of mtDNA copy numbers in isolated karyoplasts to those of individual oocytes. Spindle-chromosomal morphology and copy number variation (CNV) analysis also confirmed the safety of this method. Then, we reconstructed oocytes by MRR-SCCT, which well developed to blastocysts with minimal mtDNA residue and normal chromosomal copy numbers. Meanwhile, we optimized the manipulation order between intracytoplasmic sperm injection (ICSI) and SCC transfer and concluded that ICSI-then-transfer was conducive to avoid premature activation of reconstructed oocytes in favor of normal fertilization. Offspring of mice generated by embryos transplantation in vivo and embryonic stem cells derivation further presented evidences for competitive development competence and stable mtDNA carryover without genetic drift. Importantly, we also successfully accomplished SCCT in human MII oocytes resulting in tiny mtDNA residue and excellent embryo development through MRR manipulation. Taken together, our preclinical mouse and human models of the MRR-SCCT strategy not only demonstrated efficient residue removal but also high compatibility with normal embryo development, thus could potentially be served as a feasible clinical treatment to prevent the transmission of inherited mtDNA diseases. Public Library of Science 2023-10-05 /pmc/articles/PMC10553349/ /pubmed/37796762 http://dx.doi.org/10.1371/journal.pbio.3002313 Text en © 2023 Liao et al https://creativecommons.org/licenses/by/4.0/This is an open access article distributed under the terms of the Creative Commons Attribution License (https://creativecommons.org/licenses/by/4.0/) , which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Methods and Resources
Liao, Xiaoyu
Li, Wenzhi
Lin, Kaibo
Jin, Wei
Zhang, Shaozhen
Wang, Yao
Ma, Meng
Xie, Yating
Yu, Weina
Yan, Zhiguang
Gao, Hongyuan
Zhao, Leiwen
Si, Jiqiang
Wang, Yun
Lin, Jiaying
Chen, Chen
Chen, Li
Kuang, Yanping
Lyu, Qifeng
Significant decrease of maternal mitochondria carryover using optimized spindle-chromosomal complex transfer
title Significant decrease of maternal mitochondria carryover using optimized spindle-chromosomal complex transfer
title_full Significant decrease of maternal mitochondria carryover using optimized spindle-chromosomal complex transfer
title_fullStr Significant decrease of maternal mitochondria carryover using optimized spindle-chromosomal complex transfer
title_full_unstemmed Significant decrease of maternal mitochondria carryover using optimized spindle-chromosomal complex transfer
title_short Significant decrease of maternal mitochondria carryover using optimized spindle-chromosomal complex transfer
title_sort significant decrease of maternal mitochondria carryover using optimized spindle-chromosomal complex transfer
topic Methods and Resources
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10553349/
https://www.ncbi.nlm.nih.gov/pubmed/37796762
http://dx.doi.org/10.1371/journal.pbio.3002313
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