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在经羊膜腔干细胞治疗的健康同基因模型中,供体造血干细胞系的胎儿血行播散。

Fetal hematogenous routing of a donor hematopoietic stem cell line in a healthy syngeneic model of transamniotic stem cell therapy.

机构信息

Department of Surgery, Boston Children's Hospital/ Harvard Medical School, Boston, MA 02115, USA.

Department of Surgery, Boston Children's Hospital/ Harvard Medical School, Boston, MA 02115, USA.

出版信息

J Pediatr Surg. 2021 Jun;56(6):1233-1236. doi: 10.1016/j.jpedsurg.2021.02.035. Epub 2021 Feb 24.

DOI:10.1016/j.jpedsurg.2021.02.035
PMID:33771370
Abstract

BACKGROUND/PURPOSE: In utero administration of hematopoietic stem cells (HSCs) has a variety of actual or potential clinical applications but is hindered by invasive, morbid administration techniques. We sought to determine whether donor HSCs could reach the fetal circulation after simple intra-amniotic delivery in a syngeneic rat model of transamniotic stem cell therapy (TRASCET).

METHODS

Pregnant Lewis rat dams underwent volume-matched intra-amniotic injections in all fetuses (n = 90) on gestational day 17 (E17; term=E21-22) of a suspension of commercially available syngeneic Lewis rat HSCs labeled with luciferase (n = 37 fetuses) or an acellular suspension of recombinant luciferase (n = 53). HSC phenotype was confirmed by flow cytometry. Fetuses were euthanized at term for screening of luciferase activity at select anatomical sites. Statistical comparisons were by Fisher's exact test.

RESULTS

Among survivors (47/90; 52.2%), donor HSCs were identified selectively in the placenta (p = 0.003), umbilical cord (p < 0.001), bone marrow (p < 0.001), thymus (p = 0.009), bowel (p = 0.003), kidney (p = 0.022), and skin (p < 0.001) when compared with acellular luciferase controls.

CONCLUSIONS

Donor hematopoietic stem cells undergo hematogenous routing and can reach the fetal bone marrow after simple intra-amniotic delivery in a syngeneic rat model. Transamniotic stem cell therapy may become a practicable, minimally invasive strategy for the prenatal administration of these cells.

摘要

背景/目的:在子宫内给予造血干细胞(HSCs)具有多种实际或潜在的临床应用,但受到侵入性、病态的给药技术的阻碍。我们试图确定在同种大鼠经羊膜内干细胞治疗(TRASCET)的模型中,单纯经羊膜内递送供体 HSCs 是否可以使供体 HSCs 到达胎儿循环。

方法

妊娠 Lewis 大鼠在妊娠第 17 天(E17;足月=E21-22)对所有胎儿(n=90)进行体积匹配的经羊膜内注射,将含有荧光素酶的商品化同种 Lewis 大鼠 HSCs 悬浮液(n=37 个胎儿)或不含细胞的重组荧光素酶悬浮液(n=53 个胎儿)注射到胎儿羊膜腔中。通过流式细胞术确认 HSC 表型。在足月时处死胎儿,选择解剖部位筛选荧光素酶活性。统计学比较采用 Fisher 确切检验。

结果

在幸存者(47/90;52.2%)中,与不含细胞的荧光素酶对照组相比,供体 HSCs 选择性地存在于胎盘(p=0.003)、脐带(p<0.001)、骨髓(p<0.001)、胸腺(p=0.009)、肠(p=0.003)、肾(p=0.022)和皮肤(p<0.001)中。

结论

在同种大鼠模型中,供体造血干细胞通过血源性途径行进,可以在单纯经羊膜内递送后到达胎儿骨髓。经羊膜内干细胞治疗可能成为一种可行的、微创的产前给药策略。

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