Heg1 and Ccm1/2 proteins control endocardial mechanosensitivity during zebrafish valvulogenesis.
Stefan DonatMarta LourençoAlessio PaoliniCécile OttenMarc RenzSalim Abdelilah-SeyfriedPublished in: eLife (2018)
Endothelial cells respond to different levels of fluid shear stress through adaptations of their mechanosensitivity. Currently, we lack a good understanding of how this contributes to sculpting of the cardiovascular system. Cerebral cavernous malformation (CCM) is an inherited vascular disease that occurs when a second somatic mutation causes a loss of CCM1/KRIT1, CCM2, or CCM3 proteins. Here, we demonstrate that zebrafish Krit1 regulates the formation of cardiac valves. Expression of heg1, which encodes a binding partner of Krit1, is positively regulated by blood-flow. In turn, Heg1 stabilizes levels of Krit1 protein, and both Heg1 and Krit1 dampen expression levels of klf2a, a major mechanosensitive gene. Conversely, loss of Krit1 results in increased expression of klf2a and notch1b throughout the endocardium and prevents cardiac valve leaflet formation. Hence, the correct balance of blood-flow-dependent induction and Krit1 protein-mediated repression of klf2a and notch1b ultimately shapes cardiac valve leaflet morphology.
Keyphrases
- blood flow
- aortic valve
- mitral valve
- poor prognosis
- binding protein
- left ventricular
- endothelial cells
- transcription factor
- transcatheter aortic valve replacement
- aortic stenosis
- aortic valve replacement
- copy number
- genome wide
- gene expression
- long non coding rna
- amino acid
- living cells
- antiretroviral therapy
- vascular endothelial growth factor
- blood brain barrier
- cerebral ischemia
- hiv testing