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  4. Dependency of mitochondrial quantity on blastocyst timeline obscures its actual effect to pregnancy outcomes.
 
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Dependency of mitochondrial quantity on blastocyst timeline obscures its actual effect to pregnancy outcomes.

Journal
Frontiers in endocrinology
Journal Volume
15
ISSN
1664-2392
Date Issued
2024
Author(s)
Chuang, Tzu-Hsuan
Chou, Hsin-Hua
Kuan, Chin-Sheng
Liu, Shu-Cheng
Kao, Chia-Wei
Wu, Yi-Hsin
Lai, Hsing-Hua
Hsieh, Chia-Lin
Liang, Yi-Ting
Chen, Chien-Yu
SHEE-UAN CHEN  
DOI
10.3389/fendo.2024.1415865
URI
https://scholars.lib.ntu.edu.tw/handle/123456789/720179
Abstract
Objectives: To explore the correlation between mitochondrial quantity and the blastocyst development timeline as well as their respective contributions to early pregnancy. Methods: A retrospective study was conducted using a dataset comprising 2,633 embryos that underwent preimplantation genetic testing for aneuploidy (PGT-A) between January 2016 and December 2023. The study was divided into three subsets to address distinct aspects: the representativeness of a single trophectoderm (TE) biopsy for mitochondrial quantity (n=43), the correlation between morphokinetic features and mitochondrial quantity (n=307), and the association analysis among mitochondrial quantity, blastocyst timeline factor, and reproductive outcomes (n=2,283). Distribution assessment of mitochondrial quantity across an individual blastocyst involved the identification within multiple biopsies and spent culture media. Timeline evaluation included correlating mitochondrial quantity with time-lapse datasets. Finally, multivariate logistic regression models, incorporating potential effectors alongside mitochondrial quantity, were employed to analyze their respective contributions to early pregnancy endpoints. Results: Of distribution assessment, mitochondrial quantity exhibited an even distribution across the entire trophectoderm (Spearman’s ρ=0.82), while no detectable mtDNAs in the corresponding spent culture media. Then the timeline correlation study revealed significant association between mitochondrial quantity and blastocyst features of both the day of expanded blastocyst formation (95% Confidence intervals, CIs: 0.27~4.89, p=0.03) and the timing of expanded blastocyst formation (tEB) (95% CIs: -0.24~-0.01, p=0.04) in the regression model, indicating a strong dependency between mitochondrial quantity and the blastocyst development timeline. For the contribution to early pregnancy, multivariate logistic regression models showed that the day of expanded blastocyst formation contributed to four endpoints persistently: positive for HCG (odd ratio, OR: 0.71, p=0.006), gestational sac (OR: 0.78, p=0.04), fetal heartbeat (OR: 0.71, p=0.004), and progression to 14 weeks (OR: 0.69, p=0.002). Contrastingly, no notable correlation was observed between the mitochondrial quantity and these endpoints. Conclusions: Strong interaction was observed between mitochondrial quantity and the blastocyst timeline, particularly the timing of expanded blastocyst formation. It suggests that the primary determinant influencing pregnancy outcomes lies in the time-dependent parameter of blastocyst rather than in the specific mitochondrial quantity.
Subjects
blastocyst timeline
mitochondria
morphokinetics
next-generation sequencing
single euploid embryo transfer
SDGs

[SDGs]SDG3

Type
journal article

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