A requirement for astrocyte IP3R2 signaling for whisker experience-dependent depression and homeostatic upregulation in the mouse barrel cortex

John B. Butcher; John B. Butcher; Robert E. Sims; Neville M. Ngum; Amjad H. Bazzari; Stuart I. Jenkins; Marianne King; Eric J. Hill; David A. Nagel; Kevin Fox; H. Rheinallt Parri; Stanislaw Glazewski

doi:10.3389/fncel.2022.905285

Frontiers in Cellular Neuroscience (Aug 2022)

A requirement for astrocyte IP3R2 signaling for whisker experience-dependent depression and homeostatic upregulation in the mouse barrel cortex

John B. Butcher,
John B. Butcher,
Robert E. Sims,
Neville M. Ngum,
Amjad H. Bazzari,
Stuart I. Jenkins,
Marianne King,
Eric J. Hill,
David A. Nagel,
Kevin Fox,
H. Rheinallt Parri,
Stanislaw Glazewski

Affiliations

John B. Butcher: School of Life Sciences, Keele University, Keele, United Kingdom
John B. Butcher: College of Health and Life Sciences, Aston University, Birmingham, United Kingdom
Robert E. Sims: College of Health and Life Sciences, Aston University, Birmingham, United Kingdom
Neville M. Ngum: College of Health and Life Sciences, Aston University, Birmingham, United Kingdom
Amjad H. Bazzari: College of Health and Life Sciences, Aston University, Birmingham, United Kingdom
Stuart I. Jenkins: Neural Tissue Engineering Group, Institute for Science and Technology in Medicine (ISTM), Keele University, Keele, United Kingdom
Marianne King: College of Health and Life Sciences, Aston University, Birmingham, United Kingdom
Eric J. Hill: College of Health and Life Sciences, Aston University, Birmingham, United Kingdom
David A. Nagel: Aston Medical School, Aston Medical Research Institute, Aston University, Birmingham, United Kingdom
Kevin Fox: School of Biosciences, Cardiff University, Cardiff, United Kingdom
H. Rheinallt Parri: College of Health and Life Sciences, Aston University, Birmingham, United Kingdom
Stanislaw Glazewski: School of Life Sciences, Keele University, Keele, United Kingdom

DOI: https://doi.org/10.3389/fncel.2022.905285
Journal volume & issue: Vol. 16

Abstract

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Changes to sensory experience result in plasticity of synapses in the cortex. This experience-dependent plasticity (EDP) is a fundamental property of the brain. Yet, while much is known about neuronal roles in EDP, very little is known about the role of astrocytes. To address this issue, we used the well-described mouse whiskers-to-barrel cortex system, which expresses a number of forms of EDP. We found that all-whisker deprivation induced characteristic experience-dependent Hebbian depression (EDHD) followed by homeostatic upregulation in L2/3 barrel cortex of wild type mice. However, these changes were not seen in mutant animals (IP3R2–/–) that lack the astrocyte-expressed IP3 receptor subtype. A separate paradigm, the single-whisker experience, induced potentiation of whisker-induced response in both wild-type (WT) mice and IP3R2–/– mice. Recordings in ex vivo barrel cortex slices reflected the in vivo results so that long-term depression (LTD) could not be elicited in slices from IP3R2–/– mice, but long-term potentiation (LTP) could. Interestingly, 1 Hz stimulation inducing LTD in WT paradoxically resulted in NMDAR-dependent LTP in slices from IP3R2–/– animals. The LTD to LTP switch was mimicked by acute buffering astrocytic [Ca2+]i in WT slices. Both WT LTD and IP3R2–/– 1 Hz LTP were mediated by non-ionotropic NMDAR signaling, but only WT LTD was P38 MAPK dependent, indicating an underlying mechanistic switch. These results demonstrate a critical role for astrocytic [Ca2+]i in several EDP mechanisms in neocortex.

Published in Frontiers in Cellular Neuroscience

ISSN: 1662-5102 (Online)
Publisher: Frontiers Media S.A.
Country of publisher: Switzerland
LCC subjects: Medicine: Internal medicine: Neurosciences. Biological psychiatry. Neuropsychiatry
Website: http://www.frontiersin.org/cellular-neuroscience

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