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羊水来源的干细胞:先天性畸形自然及模拟策略的潜在工厂

Amniotic fluid-derived stem cells: potential factories of natural and mimetic strategies for congenital malformations.

作者信息

Fonteles Cristiane S R, Enterria-Rosales Julia, Lin Ying, Steele John W, Villarreal-Leal Ramiro A, Xiao Jing, Idowu Daniel I, Burgelin Beck, Wlodarczyk Bogdan J, Finnell Richard H, Corradetti Bruna

机构信息

Departamento de Clínica Odontológica. Faculdade de Farmácia, Odontologia E Enfermagem, Universidade Federal Do Ceara. Rua Monsenhor Furtado, S/N-Rodolfo Teófilo, Fortaleza, Brazil.

Center for Precision Environmental Health, Baylor College of Medicine, One Baylor Plaza, Houston, TX, USA.

出版信息

Stem Cell Res Ther. 2024 Dec 5;15(1):466. doi: 10.1186/s13287-024-04082-8.

Abstract

BACKGROUND

Mesenchymal stem cells (MSCs) derived from gestational tissues offer a promising avenue for prenatal intervention in congenital malformations although their application is hampered by concerns related to cellular plasticity and the need for invasive, high-risk surgical procedures. Here, we present naturally occurring exosomes (EXOs) isolated from amniotic fluid-derived MSCs (AF-MSCs) and their mimetic analogs (MIMs) as viable, reproducible, and stable alternatives. These nanovesicles present a minimally invasive therapeutic option, addressing the limitations of MSC-based treatments while retaining therapeutic efficacy.

METHODS

MIMs were generated from AF-MSCs by combining sequential filtration steps through filter membranes with different porosity and size exclusion chromatography columns. A physicochemical, structural, and molecular comparison was conducted with exosomes (EXOs) released from the same batch of cells. Additionally, their distribution patterns in female mice were evaluated following in vivo administration, along with an assessment of their safety profile throughout gestation in a mouse strain predisposed to neural tube defects (NTDs). The possibility to exploit both formulations as mRNA-therapeutics was explored by evaluating cell uptake in two different cell types(fibroblasts, and macrophages) and mRNA functionality overtime in an in vitro experimental setting as well as in an ex vivo, whole embryo culture using pregnant C57BL6 dams.

RESULTS

Molecular and physiochemical characterization showed no differences between EXOs and MIMs, with MIMs determining a threefold greater yield. Biodistribution patterns following intraperitoneal administration were comparable between the two particle types, with the uterus being among targeted organs. No toxic effects were observed in the dams during gestation, nor were there any malformations or significant differences in the number of viable versus dead fetuses detected. MIMs delivered a more intense and prolonged expression of mRNA encoding for green fluorescent protein in macrophages and fibroblasts. An ex-vivo whole embryo culture demonstrated that MIMs mainly accumulate at the level of the yolk sac, while EXOs reach the embryo.

CONCLUSIONS

The present data confirms the potential application of EXOs and MIMs as suitable tools for prevention and treatment of NTDs and proposes MIMs as prospective vehicles to prevent congenital malformations caused by in utero exposure to drugs.

摘要

背景

源自妊娠组织的间充质干细胞(MSCs)为先天性畸形的产前干预提供了一条有前景的途径,尽管其应用受到细胞可塑性相关问题以及侵入性、高风险外科手术需求的阻碍。在此,我们展示了从羊水来源的间充质干细胞(AF-MSCs)中分离出的天然存在的外泌体(EXOs)及其模拟类似物(MIMs),它们是可行、可重复且稳定的替代物。这些纳米囊泡提供了一种微创治疗选择,解决了基于MSC治疗的局限性,同时保留了治疗效果。

方法

通过将不同孔隙率的滤膜和尺寸排阻色谱柱的连续过滤步骤相结合,从AF-MSCs生成MIMs。对同一批细胞释放的外泌体(EXOs)进行了物理化学、结构和分子比较。此外,在体内给药后评估了它们在雌性小鼠中的分布模式,并在易患神经管缺陷(NTDs)的小鼠品系的整个妊娠期评估了它们的安全性。通过评估两种不同细胞类型(成纤维细胞和巨噬细胞)中的细胞摄取以及在体外实验环境中以及使用怀孕的C57BL6母鼠进行的离体全胚胎培养中mRNA随时间的功能,探索了将这两种制剂用作mRNA治疗剂的可能性。

结果

分子和物理化学表征显示EXOs和MIMs之间没有差异,MIMs的产量提高了三倍。两种颗粒类型腹腔给药后的生物分布模式相当,子宫是靶向器官之一。在妊娠期母鼠中未观察到毒性作用,也未检测到任何畸形或存活与死亡胎儿数量的显著差异。MIMs在巨噬细胞和成纤维细胞中使编码绿色荧光蛋白的mRNA表达更强烈且持续时间更长。离体全胚胎培养表明,MIMs主要积聚在卵黄囊水平,而EXOs到达胚胎。

结论

目前的数据证实了EXOs和MIMs作为预防和治疗NTDs的合适工具的潜在应用,并提出MIMs作为预防子宫内接触药物引起的先天性畸形的前瞻性载体。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/01a2/11622670/73f4e2b1bbba/13287_2024_4082_Fig1_HTML.jpg

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