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在鼻中隔软骨细胞(NSC)来源的基质上预处理的人鼻中隔软骨细胞(NSCs)可提高其软骨形成潜能。

Human nasal septal chondrocytes (NSCs) preconditioned on NSC-derived matrix improve their chondrogenic potential.

作者信息

Noh Yong Kwan, Kim Sung Won, Kim Ik-Hwan, Park Kwideok

机构信息

Center for Biomaterials, Korea Institute of Science and Technology (KIST), 02792, Seoul, Republic of Korea.

Department of Biotechnology, Korea University, 02841, Seoul, Republic of Korea.

出版信息

Biomater Res. 2021 Apr 6;25(1):10. doi: 10.1186/s40824-021-00211-z.

Abstract

BACKGROUND

Extracellular matrix (ECM) has a profound effect on cell behaviors. In this study, we prepare a decellularized human nasal septal chondrocyte (NSC)-derived ECM (CHDM), as a natural (N-CHDM) or soluble form (S-CHDM), and investigate their impact on NSCs differentiation.

METHODS

N-CHDM, S-CHDM were obtained from NSC. To evaluate function of NSC cultured on each substrate, gene expression using chondrogenic marker, and chondrogenic protein expression were tested. Preconditioned NSCs-loaded scaffolds were transplanted in nude mice for 3 weeks and analyzed.

RESULTS

When cultivated on each substrate, NSCs exhibited similar cell spread area but showed distinct morphology on N-CHDM with significantly lower cell circularity. They were highly proliferative on N-CHDM than S-CHDM and tissue culture plastic (TCP), and showed more improved cell differentiation, as assessed via chondrogenic marker (Col2, Sox9, and Aggrecan) expression and immunofluorescence of COL II. We also investigated the effect of NSCs preconditioning on three different 2D substrates while NSCs were isolated from those substrates, subsequently transferred to 3D mesh scaffold, then cultivated them in vitro or transplanted in vivo. The number of cells in the scaffolds was similar to each other at 5 days but cell differentiation was notably better with NSCs preconditioned on N-CHDM, as assessed via real-time q-PCR, Western blot, and immunofluorescence. Moreover, when those NSCs-loaded polymer scaffolds were transplanted subcutaneously in nude mice for 3 weeks and analyzed, the NSCs preconditioned on the N-CHDM showed significantly advanced cell retention in the scaffold, more cells with a chondrocyte lacunae structure, and larger production of cartilage ECM (COL II, glycosaminoglycan).

CONCLUSIONS

Taken together, a natural form of decellularized ECM, N-CHDM would present an advanced chondrogenic potential over a reformulated ECM (S-CHDM) or TCP substrate, suggesting that N-CHDM may hold more diverse signaling cues, not just limited to ECM component.

摘要

背景

细胞外基质(ECM)对细胞行为有深远影响。在本研究中,我们制备了脱细胞人鼻中隔软骨细胞(NSC)来源的ECM(CHDM),其有天然形式(N-CHDM)或可溶性形式(S-CHDM),并研究它们对NSC分化的影响。

方法

从NSC获得N-CHDM、S-CHDM。为评估在每种基质上培养的NSC的功能,检测了使用软骨生成标志物的基因表达和软骨生成蛋白表达。将预处理的负载NSC的支架移植到裸鼠体内3周并进行分析。

结果

当在每种基质上培养时,NSC表现出相似的细胞铺展面积,但在N-CHDM上呈现出明显不同的形态,细胞圆形度显著更低。与S-CHDM和组织培养塑料(TCP)相比,它们在N-CHDM上具有更高的增殖能力,并且通过软骨生成标志物(Col2、Sox9和聚集蛋白聚糖)表达以及COL II免疫荧光评估显示出更好的细胞分化。我们还研究了NSC预处理对三种不同二维基质的影响,在从这些基质分离NSC后,随后将其转移到三维网状支架上,然后在体外培养或体内移植。在第5天时,支架中的细胞数量彼此相似,但通过实时定量PCR、蛋白质印迹和免疫荧光评估,在N-CHDM上预处理的NSC的细胞分化明显更好。此外,当将那些负载NSC的聚合物支架皮下移植到裸鼠体内3周并进行分析时,在N-CHDM上预处理的NSC在支架中显示出明显更高的细胞保留率,更多具有软骨细胞腔隙结构的细胞,以及更大的软骨ECM(COL II、糖胺聚糖)产生量。

结论

综上所述,天然形式的脱细胞ECM,即N-CHDM,相较于重新配制的ECM(S-CHDM)或TCP基质,具有更高的软骨生成潜力,这表明N-CHDM可能拥有更多样化的信号线索,而不仅限于ECM成分。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/bf2f/8025325/faecd3fe485c/40824_2021_211_Fig1_HTML.jpg

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