Altered meningeal immunity contributing to the autism-like behavior of BTBR T+ Itpr3tf/J mice

https://doi.org/10.1016/j.bbih.2022.100563Get rights and content
Under a Creative Commons license
open access

Highlights

  • BTBR mice have higher level of immune cell meningeal deposition compared to C57BL/6 (B6) mice.

  • Meningeal T cells and B cells of BTBR mice express a higher level of CD25 and MHCII, respectively, than B6 mice.

  • BTBR mice have a higher level of serum autoantibodies to dsDNA, Aquaporin-4, NMDAR1, Pentraxin/SAP and Caspr2 than B6 mice.

  • BTBR mice have reduced level of T regulatory (Treg) cells in the meninges and brain draining lymph nodes and produce less IL-10.

  • Fewer Treg cells, more activated meningeal T and B cells, and higher autoantibody levels contribute to the autism-like development of BTBR mice.

Abstract

Autism spectrum disorder (ASD) is a complicated neurodevelopmental disorder, which is categorized by deficiency of social contact and communication, and stereotyped forms of performance. Meningeal immunity conditions the immune reflection and immune defense in the meningeal area involving meningeal lymphatic organization, glymphatic structure, immune cells, and cytokines. The development of meningeal immunity dysfunction might be the leading cause for many neural diseases including ASD. The inbred mouse strain BTBRT + Itpr3tf/J (BTBR) shows multiple ASD-like behavioral phenotypes, thus making this strain a widely used animal model for ASD. In our previous study, we reported an altered peripheral immune profile in BTBR mice. Herein, we are investigating immunological and neural interactions associated with the aberrant behavior of BTBR mice. BTBR mice have an increased level of immune cell deposition in the meninges along with a higher level of CD4+ T cells expressing CD25 and of B and myeloid cells expressing more MHCII than C57BL/6 (B6) mice, which have normal behaviors. BTBR mice also have higher levels of autoantibodies to dsDNA, Aquaporin-4, NMDAR1, Pentraxin/SAP and Caspr2 than B6 mice, which may affect neural functions. Interestingly, the T regulatory (Treg) cell population and their function was significantly reduced in the meninges and brain draining lymph nodes, which may explain the increased level of activated B and T cells in the meninges of BTBR mice. A low level of Treg cells, less IL-10 production by Treg, and activated T and B cells in meninges together with higher autoantibody levels might contribute to the development of autism-like behavior through neuroinflammation, which is known to be increased in BTBR mice.

Keywords

Autism
BTBR
Meninges
T regulatory cell
Interleukin-10
Autoantibodies

Data availability

Data will be made available on request.

Cited by (0)