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在使用干细胞衍生的平滑肌细胞祖细胞治疗后的盆腔手术损伤大鼠模型中,阴道前壁的功能结局

Functional outcome of the anterior vaginal wall in a pelvic surgery injury rat model after treatment with stem cell-derived progenitors of smooth muscle cells.

作者信息

Wang Yiting, Wen Yan, Kim Kayla, Wu Hugo, Zhang Jerry, Dobberfuhl Amy D, Chen Bertha

机构信息

Stanford University School of Medicine.

出版信息

Res Sq. 2024 Jun 11:rs.3.rs-4172308. doi: 10.21203/rs.3.rs-4172308/v1.

Abstract

BACKGROUND

Stem-cell-derived therapy is a promising option for tissue regeneration. Human iPSC-derived progenitors of smooth muscle cells (pSMCs) have limited proliferation and differentiation, which may minimize the risk of tumor formation while restoring smooth muscle cell deficiencies. Up to 30 % of women who suffer from recurrence of vaginal prolapse after prolapse surgery are faced with reoperation. Therefore, there is an unmet need for therapies that can restore vaginal tissue function. We hypothesize that human pSMCs can restore vaginal function in a vaginal-injury rat model.

METHODS

Female immune-compromised RNU rats were divided into 5 groups: intact controls (n=12), VSHAM (surgery + saline injection, n=33), and cell-injection group (surgery + cell injection using three patient pSMCs lines, n=14/cell line). The surgery, similar to what is done in vaginal prolapse surgery, involved ovariectomy, urethrolysis, and vagina injury. The vagina, urethra, bladder dome and trigone were harvested 10 weeks after surgery (5 weeks after injection). Organ bath myography was performed to evaluate the contractile function of vagina, and smooth muscle thickness was examined by tissue immunohistochemistry. Collagen I, collagen III, and elastin mRNA and protein expressions in tissues were assessed.

RESULTS

When compared to the VSHAM group, cell-injection groups showed significantly increased vaginal smooth muscle contractions induced by carbachol (groups A and C) and by KCl (group C), and significantly higher collagen I protein expression in the vagina (groups A and B). Elastin mRNA and protein expressions in the vagina did not correlate with injection group. In the urethra, mRNA expressions of collagen I, collagen III, and elastin were all significantly higher in the cell-injection groups compared to the VSHAM group. Collagen I protein expression of the urethra was also higher in the cell-injection group compared to the VSHAM group. Elastin protein expression in the urethra did not correlate with injection group.

CONCLUSIONS

Human iPSC-derived pSMCs improved contractile function of the post-surgery vagina. Additionally, pSMC injection modulated collagen I, collagen III and elastin mRNA and protein expressions in the vagina and urethra. These findings suggest that pSMCs may be a possible therapy for vaginal prolapse recurrence after surgical intervention.

摘要

背景

干细胞衍生疗法是组织再生的一个有前景的选择。人诱导多能干细胞衍生的平滑肌细胞祖细胞(pSMCs)增殖和分化有限,这在恢复平滑肌细胞缺陷的同时可能将肿瘤形成风险降至最低。高达30%的女性在脱垂手术后出现阴道脱垂复发,面临再次手术。因此,对于能够恢复阴道组织功能的疗法存在未满足的需求。我们假设人pSMCs可以在阴道损伤大鼠模型中恢复阴道功能。

方法

将雌性免疫缺陷RNU大鼠分为5组:完整对照组(n = 12)、VSHAM组(手术 + 注射生理盐水,n = 33)和细胞注射组(手术 + 使用三种患者pSMCs系进行细胞注射,每个细胞系n = 14)。手术类似于阴道脱垂手术,包括卵巢切除术、尿道松解术和阴道损伤。在手术后10周(注射后5周)采集阴道、尿道、膀胱穹窿和三角区。进行器官浴肌电图检查以评估阴道的收缩功能,并通过组织免疫组化检查平滑肌厚度。评估组织中I型胶原、III型胶原和弹性蛋白的mRNA和蛋白表达。

结果

与VSHAM组相比,细胞注射组显示由卡巴胆碱(A组和C组)和氯化钾(C组)诱导的阴道平滑肌收缩显著增加,并且阴道中I型胶原蛋白表达显著更高(A组和B组)。阴道中弹性蛋白的mRNA和蛋白表达与注射组无关。在尿道中,与VSHAM组相比,细胞注射组中I型胶原、III型胶原和弹性蛋白的mRNA表达均显著更高。与VSHAM组相比,细胞注射组尿道中I型胶原蛋白表达也更高。尿道中弹性蛋白蛋白表达与注射组无关。

结论

人诱导多能干细胞衍生的pSMCs改善了手术后阴道的收缩功能。此外,pSMC注射调节了阴道和尿道中I型胶原、III型胶原和弹性蛋白的mRNA和蛋白表达。这些发现表明pSMCs可能是手术干预后阴道脱垂复发的一种可能治疗方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/1438/11213168/5c4ea06cf083/nihpp-rs4172308v1-f0001.jpg

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