Developmental ablation of mature oligodendrocytes exacerbates adult CNS demyelination

Ahdeah Pajoohesh-Ganji; Molly Karl; Eric Garrison; Nana Adwoa Osei-Bonsu; Cheryl Clarkson-Paredes; Julie Ahn; Robert H Miller

doi:10.1016/j.bbih.2020.100110

Developmental ablation of mature oligodendrocytes exacerbates adult CNS demyelination

Brain Behav Immun Health. 2020 Jul 26:7:100110. doi: 10.1016/j.bbih.2020.100110. eCollection 2020 Aug.

Authors

Ahdeah Pajoohesh-Ganji¹, Molly Karl¹, Eric Garrison¹, Nana Adwoa Osei-Bonsu¹, Cheryl Clarkson-Paredes¹, Julie Ahn¹, Robert H Miller¹

Affiliation

¹ Department of Anatomy and Cell Biology, The George Washington University, School of Medicine and Health Sciences, Washington, DC, United States.

Abstract

Multiple sclerosis (MS) is a CNS neurodegenerative autoimmune disease characterized by loss of oligodendrocytes and myelin in the brain and the spinal cord that results in localized functional deficits. Several risk factors have been associated with MS, however none fully explain the enhanced susceptibility seen in older individuals. Epidemiological data, based on geographical prevalence studies suggest that susceptibility is established early in life and frequently long before the diagnosis of disease raising the possibility that developmental events influence adult disease onset and progression. Here we test the hypothesis that selective loss of mature oligodendrocytes during postnatal development results in enhanced susceptibility to a demyelinating insult to the mature CNS. A transgenic mouse model was utilized to specifically induce apoptotic cell death in a subset of mature oligodendrocytes (MBP-iCP9) during the first 2 postnatal weeks followed by either a local LPC spinal cord injection or the induction of EAE in the adult animal. Immunostaining, immunoblotting, behavioral testing, and electron microscopy were utilized to examine the differences in the response between animals with developmental loss of oligodendrocytes and controls. We show that during development, oligodendrocyte apoptosis results in transient reductions in myelination and functional deficits that recover after 10-14 days. Compared to animals in which oligodendrocyte development was unperturbed, animals subjected to postnatal oligodendrocyte loss showed delayed recovery from an LPC lesion to the mature spinal cord. Unexpectedly, the induction and severity of MOG induced EAE was not significantly altered in animals following oligodendrocyte developmental loss even though there was a substantial increase in spinal cord tissue damage and CNS inflammation. It is unclear why the elevated glial responses seen in developmentally compromised animals were not reflected in enhanced functional deficits. These observations suggest that developmental loss of oligodendrocytes results in long lasting tissue changes that alter its response to subsequent insults and the capacity for repair in the adult.

Keywords: EAE; Inflammation; LPC; Multiple sclerosis; Priming.