) Hereditary hemorrhagic telangiectasia (HHT) is an autosomal dominant genetic disorder characterized by the development of systemic and potentially life-threatening vascular anomalies called arteriovenous malformations (AVMs). HHT mutations are mostly found in the ALK1 and ENG genes and lead to a loss-of-function of BMP9/10- ALK1-ENG signaling in endothelial cells (ECs). Recent evidence suggests that HHT pathogenesis and AVM development require the aberrant overactivation of the endothelial mTOR and VEGFR2 pathways. The overall goal of this program is to characterize the precise mechanisms of mTOR and VEGFR2 overactivations upon ALK1-ENG loss-of-function, and determine whether targeting of these mechanisms has disease-modifying properties and therapeutic potential in cell and mouse models of HHT. Using whole-transcriptome interrogation, our preliminary investigation has shown that combined pharmacological inhibition of mTOR and VEGFR2 demonstrated a remarkable synergy and efficacy in correcting a pathological gene expression signature in the BMP9/10-immunoblocked (BMP9/10ib) mouse model of HHT. Strikingly, dual mTOR-VEGFR2 inhibition blocked vascular pathology and AVMs in the retina, liver, lungs, and mucosa to avert bleeding and anemia in BMP9/10ib mice. Mechanistically, our preliminary data revealed that, downstream of ALK1-ENG inhibition, changes in angiopoietin-2 (ANG2)/Tie2 receptor signaling were important triggers for mTOR-VEGFR2 activation and AVM development in HHT mice. Therefore, our data support the working model that HHT pathogenesis is caused by defective ANG2-mTOR-VEGFR2 pathways, and that interventions targeting these mechanistic defects might provide therapeutic benefit in HHT. Based on these results, we propose in Aim 1 to assess whether endothelial mTOR and VEGFR2 are independently activated and whether they are both required for AVM development in HHT mice. To this end, pharmacological and gene deletion approaches independently targeting mTOR and VEGFR2 will be employed in two HHT mouse models: the BMP9/10ib mice and a newly generated knockin (KI) mouse expressing a HHT-causing ALK1 mutation.
In Aim 2, we will delineate the precise mechanism of mTOR and VEGFR2 overactivation by ANG2/Tie2 signaling, both in vivo in HHT mice and in vitro in primary ECs, including in HHT patient blood outgrowth ECs. Lastly in Aim 3, we will determine whether Tie2 derepression blocks vascular pathology in HHT mice.
ATTACHMENT) Hereditary hemorrhagic telangiectasia (HHT) is a highly debilitating genetic bleeding disorder, for which no effective cure is currently available. In this application, we propose to determine whether interventions targeting a newly identified pathological mechanism could have disease-modifying properties in HHT models. This strategy has the potential to pave the way for new clinical investigations in HHT.
