Induced Regenerative Elastic Matrix Repair in LOXL1 Knockout Mouse Cell Cultures: Towards Potential therapy for Pelvic Organ Prolapse.

Journal of tissue science & engineering Pub Date : 2012-01-01 Epub Date: 2012-09-28 DOI:10.4172/2157-7552.1000120
L Venkataraman, A T Lenis, B M Couri, M S Damaser, A Ramamurthi
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引用次数: 9

Abstract

Impaired elastic matrix remodeling occurs in reproductive tissues after vaginal delivery. This has been linked to development of pelvic organ prolapse (POP) for which there currently is no pharmacologic therapy. Hyaluronan oligomers and transforming growth factor beta 1 (termed elastogenic factors, EFs) have been shown to significantly enhance tropoelastin synthesis, elastic fiber assembly, and crosslinking by adult vascular smooth muscle cells (SMCs). The goal of this study was to ascertain if these factors similarly improve the quantity and quality of elastic matrix deposition by vaginal SMCs (VSMCs) isolated from lysyl oxidase like-1 knock out (LOXL1 KO) mouse model of POP. Cells isolated from whole vagina of a LOXL1 KO mouse (multiparous, stage 3 prolapse) were cultured and identified as SMCs by their expression of various SMC markers. Passage 2 vaginal SMCs (VSMCs; 3×104/10 cm2) were cultured for 21 days with EFs. Cell layers and spent medium aliquots were assessed for elastin content and quality. EF-treated VSMCs proliferated at a similar rate to untreated controls but synthesized more total elastin primarily in the form of soluble matrix elastin. Elastin mRNA was also increased compared to controls. The elastic matrix was significantly denser in EF-treated cultures, which was composed of more mature, non-interrupted elastic fibers that were absent in controls. The results are promising towards development of a therapy to enhance regenerative elastic matrix repair in post-partum female pelvic floor tissues.

LOXL1敲除小鼠细胞培养诱导再生弹性基质修复:骨盆器官脱垂的潜在治疗方法。
阴道分娩后生殖组织弹性基质重塑受损。这与骨盆器官脱垂(POP)的发展有关,目前尚无药物治疗方法。透明质酸低聚物和转化生长因子β 1(称为弹性因子,EFs)已被证明可以显著促进成年血管平滑肌细胞(SMCs)的对流层弹性蛋白合成、弹性纤维组装和交联。本研究的目的是确定这些因素是否同样改善了从赖氨酸氧化酶样-1敲除(LOXL1 KO)小鼠模型中分离的阴道SMCs (VSMCs)弹性基质沉积的数量和质量。从LOXL1 KO小鼠(多产,3期脱垂)的全阴道中分离细胞进行培养,并通过其各种SMC标记的表达鉴定为SMCs。阴道SMCs (VSMCs;3×104/10 cm2)用EFs培养21 d。评估细胞层和废培养基的弹性蛋白含量和质量。ef处理的VSMCs增殖速度与未处理的对照组相似,但主要以可溶性基质弹性蛋白的形式合成了更多的总弹性蛋白。与对照组相比,弹性蛋白mRNA也有所增加。在ef处理的培养物中,弹性基质明显更致密,由更成熟、不间断的弹性纤维组成,而在对照组中则不存在。这一结果有望发展一种增强产后女性盆底组织再生弹性基质修复的治疗方法。
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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