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Duration‐dependent effects of IH‐stimulated Hif1a signaling on adult hippocampal neurogenesis
Author(s) -
Nallamothu Thara,
Khuu Maggie A.,
Garcia Alfredo J.
Publication year - 2019
Publication title -
the faseb journal
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 1.709
H-Index - 277
eISSN - 1530-6860
pISSN - 0892-6638
DOI - 10.1096/fasebj.2019.33.1_supplement.551.21
Subject(s) - neurogenesis , hif1a , intermittent hypoxia , hippocampal formation , neural stem cell , endocrinology , medicine , hypoxia (environmental) , biology , stem cell , andrology , neuroscience , chemistry , angiogenesis , microbiology and biotechnology , obstructive sleep apnea , oxygen , organic chemistry
Intermittent hypoxia (IH), is a hallmark consequence of sleep apnea, a common untreated disorder associated with impaired neurological health. We have recently demonstrated that thirty days of IH impairs long term potentiation and reduced the proportion of neurons generated during adult neurogenesis. Hypoxia Inducible Factor 1a (HIF1a) is a transcription factor important to stem cell development that is regulated by the state of oxygenation. The objective of this on‐going study is to characterize how the duration of IH exposure influences the generation of adult‐born neurons and to determine the role of IH‐dependent HIF1a signaling in the generation of adult‐born neurons in the hippocampus. We hypothesize that IH has duration dependent influence over neurons generated through adult neurogenesis and involves HIF1a dependent signaling. We used a cre‐loxP transgenic strategy to birth label a discrete cohort of stem cells that experience room air for 30 days (control), 10 days of IH +20 days of recovery in room air (IH 10+20RA ), or 30 days of IH (IH 30 ) in wild‐type reporter mice (Ai27) and in Ai27‐HIF1a +/flox mice. In wild‐type mice, exposure to IH 10+20RA led to higher proportion of birth‐labelled neurons compared to the control (+19% ± 5%, n=6) while the proportion of neurons following IH 30 decreased (−40% ± 10%, n=4). In Ai27‐HIF1a +/− mice, the proportion of birth‐labeled neurons was similar between control and IH 10+20RA groups. However, following IH 30 the proportion of birth‐labeled neurons was markedly decreased when compared to control in Ai27‐Hif1a +/− and to the IH 30 wild‐type group. Dendritic complexity, as determined by Sholl analysis, was similar among labeled neurons in both wild‐type and Ai27‐HIF1a +/− groups suggesting that neither IH nor IH‐dependent HIF1a signaling influences dendritic complexity. These findings indicate that exposure duration is factor impacting how IH affects the generation of adult‐born neurons through a HIF1a signaling shaping how IH influences, associated with sleep apnea affects the generation of adult‐born neurons. Support or Funding Information This work was supported by NIH R01 NS10742101 (AJG). This abstract is from the Experimental Biology 2019 Meeting. There is no full text article associated with this abstract published in The FASEB Journal .