Shear stress upregulates regeneration-related immediate early genes in liver progenitors in 3D ECM-like microenvironments.
Kenichiro NishiiErik BrodinTaylor RenshawRachael WeesnerEmma MoranShay SokerJessica L SparksPublished in: Journal of cellular physiology (2017)
The role of fluid stresses in activating the hepatic stem/progenitor cell regenerative response is not well understood. This study hypothesized that immediate early genes (IEGs) with known links to liver regeneration will be upregulated in liver progenitor cells (LPCs) exposed to in vitro shear stresses on the order of those produced from elevated interstitial flow after partial hepatectomy. The objectives were: (1) to develop a shear flow chamber for application of fluid stress to LPCs in 3D culture; and (2) to determine the effects of fluid stress on IEG expression in LPCs. Two hours of shear stress exposure at ∼4 dyn/cm2 was applied to LPCs embedded individually or as 3D spheroids within a hyaluronic acid/collagen I hydrogel. Results were compared against static controls. Quantitative reverse transcriptase polymerase chain reaction was used to evaluate the effect of experimental treatments on gene expression. Twenty-nine genes were analyzed, including IEGs and other genes linked to liver regeneration. Four IEGs (CFOS, IP10, MKP1, ALB) and three other regeneration-related genes (WNT, VEGF, EpCAM) were significantly upregulated in LPCs in response to fluid mechanical stress. LPCs maintained an early to intermediate stage of differentiation in spheroid culture in the absence of the hydrogel, and addition of the gel initiated cholangiocyte differentiation programs which were abrogated by the onset of flow. Collectively the flow-upregulated genes fit the pattern of an LPC-mediated proliferative/regenerative response. These results suggest that fluid stresses are potentially important regulators of the LPC-mediated regeneration response in liver.
Keyphrases
- stem cells
- hyaluronic acid
- wound healing
- genome wide
- gene expression
- genome wide identification
- bioinformatics analysis
- tissue engineering
- drug delivery
- genome wide analysis
- dna methylation
- transcription factor
- poor prognosis
- public health
- endothelial cells
- high resolution
- circulating tumor cells
- cell proliferation
- long non coding rna