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Series GSE190085 Query DataSets for GSE190085
Status Public on Dec 05, 2021
Title Electrospun scaffold micro-architecture induces an activated transcriptional phenotype within tendon fibroblasts. Bulk RNA-seq data.
Organism Homo sapiens
Experiment type Expression profiling by high throughput sequencing
Summary Biomaterial augmentation of surgically repaired rotator cuff tendon tears aims to improve the high failure rates (~40%) of traditional repairs. Biomaterials that can alter cellular phenotypes through the provision of microscale topographical cues are now under development. We aimed to systematically evaluate the effect of topographic architecture on the cellular phenotype of fibroblasts from healthy and diseased tendons. Electrospun polydioxanone scaffolds with fiber diameters ranging from 300 to 4000 nm, in either a highly aligned or random configuration, were produced. Healthy tendon fibroblasts cultured for 7 days on scaffolds with highly aligned fibers demonstrated a distinctive elongated morphology, whilst those cultured on randomly configured fibers demonstrated a flattened and spread morphology. The effect of scaffold micro-architecture on the transcriptome of both healthy and diseased tendon fibroblasts was assessed with bulk RNA-seq. Both healthy (n=3) and diseased tendon cells (n=3) demonstrated a similar transcriptional response to architectural variants. Gene set enrichment analysis revealed that large diameter (≥ 2000 nm) aligned scaffolds induced an upregulation of genes involved in cellular replication and a downregulation of genes defining inflammatory responses and cell adhesion. Similarly, PDPN and CD248, markers of inflammatory or ‘activated’ fibroblasts, were downregulated during culture of both healthy and diseased fibroblasts on aligned scaffolds with large (≥ 2000 nm) fiber diameters. In conclusion scaffold architectures resembling that of disordered type III collagen, typically present during the earlier phases of wound healing, resulted in tendon fibroblast activation. Conversely, scaffolds mimicking aligned diameter collagen I fibrils, present during tissue remodelling, did not activate tendon derived fibroblasts. This has implications for the design of scaffolds used during rotator cuff repair augmentation.
 
Overall design 8 unique conditions (scaffold architectural variants), in biological triplicate (n= 3 donors). 2 cell types (Healthy tendon fibroblasts [Hamstring derived] and diseased tendon fibroblasts [massive (>5cm in AP diameter, rotator cuff tears]). Single time point (7 days). 48 samples total.
 
Contributor(s) Baldwin M, Cribbs A, Snelling S, Mimpen J
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Submission date Dec 03, 2021
Last update date Dec 05, 2021
Contact name Adam Cribbs
E-mail(s) adam.cribbs@ndorms.ox.ac.uk
Organization name University of Oxford
Department NDORMS
Street address Windmill Road
City Oxford
ZIP/Postal code OX37LD
Country United Kingdom
 
Platforms (1)
GPL18573 Illumina NextSeq 500 (Homo sapiens)
Samples (48)
GSM5712943 i01-Disease1-Aligned-300_S15
GSM5712944 i02-Disease1-Aligned-1000_S17
GSM5712945 i03-Disease1-Aligned-2000_S24
Relations
BioProject PRJNA785809
SRA SRP349101

Download family Format
SOFT formatted family file(s) SOFTHelp
MINiML formatted family file(s) MINiMLHelp
Series Matrix File(s) TXTHelp

Supplementary file Size Download File type/resource
GSE190085_diseased_counts.tsv.gz 672.1 Kb (ftp)(http) TSV
GSE190085_healthy_counts.tsv.gz 671.7 Kb (ftp)(http) TSV
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Raw data are available in SRA
Processed data are available on Series record
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