Lecture 27- Mechanobiology III Flashcards
Explain how integrins are involved in mechanotransduction
Integrins sense the ECM stiffness and translate this into biochemical signals (specially the activation of focal adhesions kinases, Rho)
What can regulate filamentous actin and YAP/TAZ?
Rho
What does stiffened ECM promote in cells?
Promotes the epithelial to mesenchymal transition
How can the level of epithelial to mesenchymal transition be visualised and what difference would be observed between stiff and soft ECM?
Green immunofluorescene indicating the level of Snail
Snail indicated the epithelial to mesenchymal transition
Soft ECM: low levels of fluorescence, low levels of Snail, low levels of transition
Stiffened ECM: high levels of fluorescence, high levels of Snail, high levels of transition
Why is a lack of epithelial to mesenchymal transition under soft ECM conditions are pre-requisite for tumour progression?
The mesenchymal cells loose their ability to stretch to each other which increases the chance of metastasis
In which ways can inhibitors work to perturb cell-ECM interactions and/or cell signalling?
- Inhibitors aim to delay the formation of epithelial to mesenchymal transition to reduce cancer progression
- Inhibitors can interfere with ECM stiffness and reduce the crosslinking of ECM
- Inhibitors can prevent integrins from binding to ECM or to components which affect the ECM directly and degrade components
- Inhibitors can block the mechanotransduction itself
Give some example of ECM/adhesion signalling inhibitors
- TGF-beta inhibitors
- MMP inhibitors
- Losartan
- LOXL2 inhibitors
- Integrin inhibitors
- Rho inhibitors
- HA inhibitors
- FAK inhibitors
How does the adhesive area vary with differences in ECM stiffness?
Low ECM stiffness: cells don’t spread so occupy a small adhesive area
High ECM stiffness: cells spread and occupy a large adhesive area
The geometry of the cell/size of adhesive area is a physical cue which steers the cells behaviour by dictating its signal transduction
Outline the core cascade of the YAP/TAZ- Hippo pathway
- Mst1/2 positively regulates Lats1/2 which regulates via phosphorylated YAP/TAZ
- Mst1/2 can be regulated by a number of membrane and cytoplasmic regulators
- YAP/TAZ is negatively regulated when phosphorylated
- This is because the phosphorylation leads to increase degradation via the proteasome and the phosphorylation on serine generated a binding site for a 14-3-3 protein
- 14-3-3 protein binds specifically to phosphorylated YAP/TAZ and prevents the transcription regulator entering the nucleus so its retained in the cytoplasm
- When the pathway inactive, YAP/TAZ not phosphorylated so is active in the nucleus so it’s transcription regulator must enter the nucleus to interact with TFs
What does excess YAP activation lead to?
Organ enlargement/over growing phenotypes
What happen if the YAP gene is mutated?
Prevents phosphorylation which is important for degrading YAP
If degradation is prevented, the protein is over expressed which leads to the overgrowing phenotype
What cell or tissue properties regulate the Hippo pathway?
- Apicobasal polarity
- Mechanotransduction
- Cell-cell adhesion
- Contact inhibition
What cellular functions are regulated by the Hippo pathway?
- Proliferation
- Cell survival
- Cell competition
- Stem cell maintenance
- Metastasis
- Regeneration
What regulates YAP nuclear localisation?
YAP/TAZ is mechanosensitive and regulated by ECM stiffness
YAP/TAZ is inhibited at low ECM stiffness and activated at high ECM stiffness
Where is activated and inactivated YAP/TAZ and what causes this?
At high ECM stiffness, YAP/TAZ is activated and localised to the nucleus
At low ECM stiffness, YAP/TAZ is inactivated so will be degraded if found in the cytoplasm
