TY - JOUR
T1 - Neonatal hyperoxia in mice triggers long-term cognitive deficits via impairments in cerebrovascular function and neurogenesis
AU - Lithopoulos, Marissa A.
AU - Toussay, Xavier
AU - Zhong, Shumei
AU - Xu, Liqun
AU - Mustafa, Shamimunisa B.
AU - Ouellette, Julie
AU - Freitas-Andrade, Moises
AU - Comin, Cesar H.
AU - Bassam, Hayam A.
AU - Baker, Adam N.
AU - Sun, Yiren
AU - Wakem, Michael
AU - Moreira, Alvaro G.
AU - Blanco, Cynthia L.
AU - Vadivel, Arul
AU - Tsilfidis, Catherine
AU - Seidner, Steven R.
AU - Slack, Ruth S.
AU - Lagace, Diane C.
AU - Wang, Jing
AU - Lacoste, Baptiste
AU - Thébaud, Bernard
N1 - Publisher Copyright:
© 2022 American Society for Clinical Investigation. All rights reserved.
PY - 2022/11/15
Y1 - 2022/11/15
N2 - Preterm birth is the leading cause of death in children under 5 years of age. Premature infants who receive life-saving oxygen therapy often develop bronchopulmonary dysplasia (BPD), a chronic lung disease. Infants with BPD are at a high risk of abnormal neurodevelopment, including motor and cognitive difficulties. While neural progenitor cells (NPCs) are crucial for proper brain development, it is unclear whether they play a role in BPD-associated neurodevelopmental deficits. Here, we show that hyperoxia-induced experimental BPD in newborn mice led to lifelong impairments in cerebrovascular structure and function as well as impairments in NPC self-renewal and neurogenesis. A neurosphere assay utilizing nonhuman primate preterm baboon NPCs confirmed impairment in NPC function. Moreover, gene expression profiling revealed that genes involved in cell proliferation, angiogenesis, vascular autoregulation, neuronal formation, and neurotransmission were dysregulated following neonatal hyperoxia. These impairments were associated with motor and cognitive decline in aging hyperoxia-exposed mice, reminiscent of deficits observed in patients with BPD. Together, our findings establish a relationship between BPD and abnormal neurodevelopmental outcomes and identify molecular and cellular players of neonatal brain injury that persist throughout adulthood that may be targeted for early intervention to aid this vulnerable patient population.
AB - Preterm birth is the leading cause of death in children under 5 years of age. Premature infants who receive life-saving oxygen therapy often develop bronchopulmonary dysplasia (BPD), a chronic lung disease. Infants with BPD are at a high risk of abnormal neurodevelopment, including motor and cognitive difficulties. While neural progenitor cells (NPCs) are crucial for proper brain development, it is unclear whether they play a role in BPD-associated neurodevelopmental deficits. Here, we show that hyperoxia-induced experimental BPD in newborn mice led to lifelong impairments in cerebrovascular structure and function as well as impairments in NPC self-renewal and neurogenesis. A neurosphere assay utilizing nonhuman primate preterm baboon NPCs confirmed impairment in NPC function. Moreover, gene expression profiling revealed that genes involved in cell proliferation, angiogenesis, vascular autoregulation, neuronal formation, and neurotransmission were dysregulated following neonatal hyperoxia. These impairments were associated with motor and cognitive decline in aging hyperoxia-exposed mice, reminiscent of deficits observed in patients with BPD. Together, our findings establish a relationship between BPD and abnormal neurodevelopmental outcomes and identify molecular and cellular players of neonatal brain injury that persist throughout adulthood that may be targeted for early intervention to aid this vulnerable patient population.
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U2 - 10.1172/JCI146095
DO - 10.1172/JCI146095
M3 - Article
C2 - 36136598
AN - SCOPUS:85141936088
SN - 0021-9738
VL - 132
JO - Journal of Clinical Investigation
JF - Journal of Clinical Investigation
IS - 22
M1 - e146095
ER -