Assessing gut barrier integrity and reproductive performance following pre-mating oral administration of solid-lipid-nanoparticles designed for drug delivery.

IF 3.6 Q2 TOXICOLOGY Frontiers in toxicology Pub Date : 2025-01-07 eCollection Date: 2024-01-01 DOI:10.3389/ftox.2024.1508598
Valentina Lacconi, Micol Massimiani, Giulia Antonello, Paolo Gasco, Roberta Bernardini, Cristiana Ferrari, Lorenzo Ippoliti, Gina La Sala, Antonio Pietroiusti, Ivana Fenoglio, Chiara Riganti, Luisa Campagnolo
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Abstract

Solid lipid nanoparticles (SLNs) have gained interest as drug delivery carriers due to their efficient cellular internalization and increased therapeutic effect of the loaded drug, with minimal side effects. Although recently several studies have shown the possibility to administer SLNs during pregnancy to vehicle mRNA to the placenta, data about the effect of premating exposure to SLNs on pregnancy outcome are scant. Considering that assumption of drug-delivering nanocarriers in reproductive age may potentially affect women's reproductive health, the aim of the present study was to evaluate whether repeated oral administration of SLNs to female mice prior to mating would influence key pregnancy outcomes. For this purpose, SLNs melatonin loaded (SLN + mlt) or unloaded were orally administered to CD1 female mice at two different dosages-low (7.5 mg/kg) and high (750 mg/kg) -three times a week for 6 weeks. Females mice were mated and pregnancy was monitored from conception to delivery. All the assessed pregnancy parameters, including time to pregnancy, pregnancy duration, litter size, and the presence of any gross anomalies in the pups, and maternal key biochemical parameters were not significantly affected by SLN administration. Embryonic development was also evaluated and no effects on the number of implantation sites, fetus numbers, incidence of fetal resorptions, and measurements of crown-rump length, as well as fetal and placental weights, were observed in the treated mothers. The impact of SLNs on maternal intestinal barrier integrity and inflammation was assessed both in vivo in mice and in vitro using an intestinal epithelial barrier model by qRT-PCR. Results showed that unloaded SLNs, but not the SLN + mlt, affected intestinal barrier integrity. Although variation in the expression of inflammatory cytokines was recorded, this did not reflect in significant histological alterations and the integrity of the intestinal barrier was maintained. The in vitro model further confirmed the biocompatibility of SLNs, showing that both loaded and unloaded SLNs did not affect the integrity of the simulated intestinal epithelial barrier. In conclusion, these data suggest that administering SLNs, as a drug delivery vehicle, prior to conception does not affect either maternal health or fetal development, posing no risk to future pregnancy.

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评估肠道屏障完整性和生殖性能后,预交配口服固体脂质纳米颗粒设计的药物输送。
固体脂质纳米颗粒(sln)由于其有效的细胞内化和负载药物的治疗效果增加而副作用最小,已成为药物递送载体。虽然最近有几项研究表明,在怀孕期间施用sln以将mRNA运送到胎盘是可能的,但关于早产暴露于sln对妊娠结局的影响的数据很少。考虑到育龄期药物递送纳米载体可能潜在影响女性生殖健康的假设,本研究的目的是评估雌性小鼠在交配前多次口服sln是否会影响关键的妊娠结局。为此,将SLN -褪黑素负载(SLN + mlt)或未负载的SLN -褪黑素以两种不同剂量(低(7.5 mg/kg)和高(750 mg/kg)口服给CD1雌性小鼠,每周三次,持续6周。雌性小鼠进行交配,并从受孕到分娩全程监测妊娠情况。所有评估的妊娠参数,包括妊娠时间、妊娠持续时间、产仔数、幼崽是否存在任何明显异常,以及母体的关键生化参数,均未受到SLN的显著影响。胚胎发育也进行了评估,在接受治疗的母亲中,没有观察到对着床部位数量、胎儿数量、胎儿吸收发生率、冠臀长测量以及胎儿和胎盘重量的影响。采用qRT-PCR方法在小鼠体内和体外建立肠上皮屏障模型,评估sln对母体肠道屏障完整性和炎症的影响。结果显示,未加载的SLN影响肠屏障的完整性,而SLN + mlt不影响。虽然记录了炎症细胞因子表达的变化,但这并没有反映在显著的组织学改变上,肠道屏障的完整性得以维持。体外模型进一步证实了sln的生物相容性,表明负载和未负载的sln均不影响模拟肠上皮屏障的完整性。总之,这些数据表明,在受孕前使用sln作为药物递送载体,既不会影响孕产妇健康,也不会影响胎儿发育,对未来妊娠没有风险。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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3.80
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审稿时长
13 weeks
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