Litcius/Paper detail

Hypoxia induces de novo formation of cerebral collaterals and lessens the severity of ischemic stroke

Hua Zhang, Wojciech Rzechorzek, Amir Aghajanian, James E. Faber

2020Journal of Cerebral Blood Flow & Metabolism58 citationsDOIOpen Access PDF

Abstract

Pial collaterals provide protection in stroke. Evidence suggests their formation late during gestation (collaterogenesis) is driven by reduced oxygen levels in the cerebral watersheds. The purpose of this study was to determine if collaterogenesis can be re-activated in the adult to induce formation of additional collaterals (“neo-collateral formation”, NCF). Mice were gradually acclimated to reduced inspired oxygen (FIO 2 ) and maintained at 12, 10, 8.5 or 7% for two-to-eight weeks. Hypoxemia induced “dose”-dependent NCF and remodeling of native collaterals, and decreased infarct volume after permanent MCA occlusion. In contrast, no formation occurred of addition collateral-like intra-tree anastomoses, PComs, or branches within the MCA tree. Hypoxic NCF, remodeling and infarct protection were durable, i.e. retained for at least six weeks after return to normoxia. Hypoxia increased expression of Hif2α, Vegfa, Rabep2, Angpt2, Tie2 and Cxcr4. Neo-collateral formation was abolished in mice lacking Rabep2, a novel gene involved in VEGFA→Flk1 signaling and required for formation of collaterals during development, and inhibited by knockdown of Vegfa, Flk1 and Cxcr4. Rabep2-dependent NCF was also induced by permanent MCA occlusion. This is the first report that hypoxia induces new pial collaterals to form. Hypoxia- and occlusion-induced neo-collateral formation provide models to study collaterogenesis in the adult.

Topics & Concepts

Hypoxia (environmental)Ischemic strokeCardiologyMedicineStroke (engine)Internal medicineIschemiaChemistryOxygenOrganic chemistryEngineeringMechanical engineeringCancer, Hypoxia, and MetabolismNeurological Disease Mechanisms and TreatmentsAngiogenesis and VEGF in Cancer