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含成纤维细胞的胶原凝胶收缩:初始胶原浓度调节收缩程度和细胞存活。

Contraction of fibroblast-containing collagen gels: initial collagen concentration regulates the degree of contraction and cell survival.

作者信息

Zhu Y K, Umino T, Liu X D, Wang H J, Romberger D J, Spurzem J R, Rennard S I

机构信息

Department of Pulmonary Disease, Jincheng Hospital, Lan Zhou, China.

出版信息

In Vitro Cell Dev Biol Anim. 2001 Jan;37(1):10-6. doi: 10.1290/1071-2690(2001)037<0010:COFCCG>2.0.CO;2.

Abstract

Remodeling of extracellular matrix involves a number of steps including the recruitment, accumulation, and eventual apoptosis of parenchymal cells as well as the production, organization, and rearrangement of extracellular matrix produced by these cells. The culture of fibroblasts in three-dimensional gels made of type I collagen has been used as a model of tissue contraction which characterizes both wound repair and fibrosis. The current study was designed to determine the effect of initial collagen concentration on the ability of fibroblasts to contract collagen gels and on cell survival. Native type I collagen was extracted from rat tail tendons and used to prepare collagen gels with varying collagen concentrations (0.75-2.0 mg/ml). Human lung fibroblasts (HFL-1) were cast into the gels and cultured in Dulbecco modified Eagle medium with 0.1% fetal calf serum for 2 wk. The gel size, collagen content, and deoxyribonucleic acid (DNA) content were determined. Gels prepared with an initial concentration of 0.75 mg/ml contracted more rapidly and to a smaller final size than gels prepared from 2 mg/ml initial collagen concentration (final size 7.1 versus 36.4% of initial size, P < 0.01). There was no significant degradation of the collagen in the gels under either condition. Hence, the dramatically increased contraction of the lower density gels resulted in a higher final density (P < 0.01). Cell density was estimated from DNA content. In low initial density gels, the final DNA content was significantly less than that in higher initial density gels (0.73 versus 1.88 microg/gel, P < 0.05). This was accompanied by an increased percentage of apoptotic cells at day 14 (43.3 versus 34.1%, P < 0.05). If the gels were maintained in the attached state which largely prevents contraction, apoptosis was significantly reduced, suggesting that contraction rather than matrix composition was a requirement for the increased apoptosis. In summary, these findings indicate that the initial matrix composition can lead to differing outcomes during fibroblast-mediated wound contraction.

摘要

细胞外基质的重塑涉及多个步骤,包括实质细胞的募集、积聚及最终凋亡,以及这些细胞产生的细胞外基质的生成、组织和重排。在由I型胶原制成的三维凝胶中培养成纤维细胞,已被用作组织收缩的模型,该模型可表征伤口修复和纤维化过程。本研究旨在确定初始胶原浓度对成纤维细胞收缩胶原凝胶能力及细胞存活的影响。从大鼠尾腱中提取天然I型胶原,用于制备具有不同胶原浓度(0.75 - 2.0 mg/ml)的胶原凝胶。将人肺成纤维细胞(HFL - 1)接种到凝胶中,并在含0.1%胎牛血清的杜尔贝科改良伊格尔培养基中培养2周。测定凝胶大小、胶原含量和脱氧核糖核酸(DNA)含量。初始浓度为0.75 mg/ml制备的凝胶比初始胶原浓度为2 mg/ml制备的凝胶收缩更快,最终尺寸更小(最终尺寸分别为初始尺寸的7.1%和36.4%,P < 0.01)。在两种条件下,凝胶中的胶原均无明显降解。因此,低密度凝胶显著增加的收缩导致最终密度更高(P < 0.01)。通过DNA含量估算细胞密度。在低初始密度凝胶中,最终DNA含量显著低于高初始密度凝胶(0.73对1.88 μg/凝胶,P < 0.05)。这伴随着第14天凋亡细胞百分比的增加(43.3%对34.1%,P < 0.05)。如果凝胶保持附着状态,这在很大程度上可防止收缩,凋亡则显著减少,表明收缩而非基质组成是凋亡增加的必要条件。总之,这些发现表明初始基质组成可导致成纤维细胞介导的伤口收缩过程出现不同结果。

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