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Intranasal Delivery of Mesenchymal Stromal Cells Protects against Neonatal Hypoxic–Ischemic Brain Injury

by Miller, Suzanne L. , Penny, Tayla R. , Castillo-Melendez, Margie , Novak, Iona , Jenkin, Graham , Paton, Madison C. B. , Djuliannisaa, Zlatikha , Sutherland, Amy E. , Fahey, Michael C. , McDonald, Courtney A. , Petraki, Maria

in Bone marrow / Cerebral palsy / Clinical trials / Cytokines / Gene expression / Hypothermia / Hypoxia / Ischemia / Neurons / Proteins / Traumatic brain injury / Tumor necrosis factor-TNF / Umbilical cord

2019

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Intranasal Delivery of Mesenchymal Stromal Cells Protects against Neonatal Hypoxic–Ischemic Brain Injury

2019

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Intranasal Delivery of Mesenchymal Stromal Cells Protects against Neonatal Hypoxic–Ischemic Brain Injury

2019

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Journal Article

Intranasal Delivery of Mesenchymal Stromal Cells Protects against Neonatal Hypoxic–Ischemic Brain Injury

Miller, Suzanne L.,

Penny, Tayla R.,

Castillo-Melendez, Margie,

Novak, Iona,

Jenkin, Graham,

Paton, Madison C. B.,

Djuliannisaa, Zlatikha,

Sutherland, Amy E.,

Fahey, Michael C.,

McDonald, Courtney A.,

Petraki, Maria

2019

Overview

Cerebral palsy (CP) is a permanent motor disorder that results from brain injury and neuroinflammation during the perinatal period. Mesenchymal stromal cells (MSCs) have been explored as a therapy in multiple adult neuroinflammatory conditions. Our study examined the therapeutic benefits of intranasal delivery of human umbilical cord tissue (UC) derived-MSCs in a rat model of neonatal hypoxic–ischemic (HI) brain injury. To do this, HI was performed on postnatal day 10 Sprague-Dawley rat pups via permanent ligation of the left carotid artery, followed by a hypoxic challenge of 8% oxygen for 90 min. A total of 200,000 UC-MSCs (10 million/kg) were administered intranasally 24 h post-HI. Motor control was assessed after seven days, followed by post-mortem. Analysis included brain immunohistochemistry, gene analysis and serum cytokine measurement. Neonatal HI resulted in brain injury with significant loss of neurons, particularly in the hippocampus. Intranasal administration of UC-MSCs significantly reduced the loss of brain tissue and increased the number of hippocampal neurons. HI significantly upregulated brain inflammation and expression of pro-inflammatory cytokines, while intranasal UC-MSCs significantly reduced markers of neuroinflammation. This study demonstrated that a clinically relevant dose (10 million/kg) of UC-MSCs was neuroprotective following HI by restoring neuronal cell numbers and reducing brain inflammation. Therefore, intranasal delivery of UC-MSCs may be an effective therapy for neonatal brain injury.

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Publisher

MDPI AG,MDPI

Subject

/ Hypoxia