High-DNA Stainability Is Not Related to Embryonic Development and Clinical Outcomes on In Vitro Fertilization Cycles: A Retrospective Study Using a Propensity Score-Matching Analysis
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Abstract
The high-DNA stainability (HDS) might be an indicator for the detection of sperm chromatin decondensation structure resulting from the incomplete histone-to-protamine exchange. The aim of our study was to investigate the association of HDS with embryonic development and clinical outcomes after in vitro fertilization (IVF) treatment. Couples underwent IVF cycles from January 2016 to December 2020 were retrospectively studied, including a total of 2,604 target couples undergoing IVF treatment and 628 couples undergoing fresh IVF-embryo transplantation (IVF-ET) treatment. Couples were divided into HDS > 15% group and HDS ≤ 15% group according to HDS levels. After controlling the bias between groups using the propensity score-matching method, data of embryonic development, and clinical outcomes were analyzed. No significant differences were observed between HDS > 15% group and HDS ≤ 15% group regarding fertilization rate (83.33% vs. 84.62%, P = 0.349), two pronuclei rate (81.82% vs. 83.33%, P = 0.613), cleavage rate (100.00% vs. 100.00%, P = 0.172), and high-quality embryo rate (60.00% vs. 60.00%, P = 0.961). Linear regression analysis showed that HDS was negatively associated with fertilization rate (B value = −0.094, 95% CI: −0.184 to −0.005, P = 0.039), whereas no correlation (adjusted B value = −0.081, 95% CI: −0.170 to 0.008, P = 0.074) was observed after adjusting potential confounding factors. The clinical pregnancy rate (62.11% vs. 60.39%, P = 0.699), ongoing pregnancy rate (52.17% vs. 53.10%, P = 0.838), early miscarriage rate (9.94% vs. 7.28%, P = 0.283), late miscarriage rate (0.62% vs. 2.14%, P = 0.305), and live birth rate (51.55% vs. 50.96%, P = 0.838) were not significantly different between groups. Binary logistic regression analysis showed that HDS levels did not affect clinical outcomes after fresh IVF-ET treatments. HDS was not significantly associated with embryonic development and clinical outcomes of IVF. Our findings suggested that HDS evaluation before IVF treatment might be with limited potential to predict embryo development and clinical outcomes.
高dna染色率(HDS)可能是检测精子染色质去浓缩结构的一个指标,这是由于历史蛋白与鱼精蛋白交换不完全引起的。本研究的目的是探讨HDS与体外受精(IVF)治疗后胚胎发育和临床结局的关系。回顾性研究2016年1月至2020年12月接受试管婴儿周期的夫妇,包括2,604对接受试管婴儿治疗的目标夫妇和628对接受新鲜IVF-胚胎移植(IVF- et)治疗的夫妇。按HDS水平分为HDS & 15%组和HDS≤15%组。在使用倾向评分匹配法控制组间偏差后,对胚胎发育数据和临床结果进行分析。HDS >; 15%组与HDS≤15%组受精率(83.33%比84.62%,P = 0.349)、双原核率(81.82%比83.33%,P = 0.613)、卵裂率(100.00%比100.00%,P = 0.172)、优质胚率(60.00%比60.00%,P = 0.961)差异均无统计学意义。线性回归分析显示,HDS与受精率呈负相关(B值= - 0.094,95% CI: - 0.184 ~ - 0.005, P = 0.039),而调整潜在混杂因素后,HDS与受精率无相关性(调整后的B值= - 0.081,95% CI: - 0.170 ~ 0.008, P = 0.074)。临床妊娠率(62.11% vs. 60.39%, P = 0.699)、妊娠持续率(52.17% vs. 53.10%, P = 0.838)、早期流产率(9.94% vs. 7.28%, P = 0.283)、晚期流产率(0.62% vs. 2.14%, P = 0.305)、活产率(51.55% vs. 50.96%, P = 0.838)组间差异无统计学意义。二元logistic回归分析显示HDS水平不影响新鲜IVF-ET治疗后的临床结果。HDS与胚胎发育和体外受精临床结果无显著相关性。我们的研究结果表明,体外受精治疗前HDS评估可能预测胚胎发育和临床结果的潜力有限。
期刊介绍:
Andrologia provides an international forum for original papers on the current clinical, morphological, biochemical, and experimental status of organic male infertility and sexual disorders in men. The articles inform on the whole process of advances in andrology (including the aging male), from fundamental research to therapeutic developments worldwide. First published in 1969 and the first international journal of andrology, it is a well established journal in this expanding area of reproductive medicine.
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