Immunocal® limits gliosis in mouse models of repetitive mild-moderate traumatic brain injury

Lilia A Koza; Claudia Pena; Madison Russell; Alec C Smith; Jacob Molnar; Maeve Devine; Natalie J Serkova; Daniel A Linseman

doi:10.1016/j.brainres.2023.148338

Immunocal® limits gliosis in mouse models of repetitive mild-moderate traumatic brain injury

Brain Res. 2023 Jun 1:1808:148338. doi: 10.1016/j.brainres.2023.148338. Epub 2023 Mar 24.

Authors

Lilia A Koza¹, Claudia Pena¹, Madison Russell¹, Alec C Smith¹, Jacob Molnar¹, Maeve Devine¹, Natalie J Serkova², Daniel A Linseman³

Affiliations

¹ University of Denver, Department of Biological Sciences, Denver, CO 80208, United States; University of Denver, Knoebel Institute for Healthy Aging, Denver, CO 80208, United States.
² University of Colorado Cancer Center, Department of Radiology, Aurora, CO 80045, United States.
³ University of Denver, Department of Biological Sciences, Denver, CO 80208, United States; University of Denver, Knoebel Institute for Healthy Aging, Denver, CO 80208, United States. Electronic address: daniel.linseman@du.edu.

Abstract

Successive traumatic brain injuries (TBIs) exacerbate neuroinflammation and oxidative stress. No therapeutics exist for populations at high risk of repetitive mild TBIs (rmTBIs). We explored the preventative therapeutic effects of Immunocal®, a cysteine-rich whey protein supplement and glutathione (GSH) precursor, following rmTBI and repetitive mild-moderate TBI (rmmTBI). Populations that suffer rmTBIs largely go undiagnosed and untreated; therefore, we first examined the potential therapeutic effect of Immunocal® long-term following rmTBI. Mice were treated with Immunocal® prior to, during, and following rmTBI induced by controlled cortical impact until analysis at 2 weeks, 2 months, and 6 months following the last rmTBI. Astrogliosis and microgliosis were measured in cortex at each time point and edema and macrophage infiltration by MRI were analyzed at 2 months post-rmTBI. Immunocal® significantly reduced astrogliosis at 2 weeks and 2 months post-rmTBI. Macrophage activation was observed at 2 months post-rmTBI but Immunocal® had no significant effect on this endpoint. We did not observe significant microgliosis or edema after rmTBI. The dosing regimen was repeated in mice subjected to rmmTBI; however, using this experimental paradigm, we examined the preventative therapeutic effects of Immunocal® at a much earlier timepoint because populations that suffer more severe rmmTBIs are more likely to receive acute diagnosis and treatment. Increases in astrogliosis, microgliosis, and serum neurofilament light (NfL), as well as reductions in the GSH:GSSG ratio, were observed 72 h post-rmmTBI. Immunocal® only significantly reduced microgliosis after rmmTBI. In summary, we report that astrogliosis persists for 2 months post-rmTBI and that inflammation, neuronal damage, and altered redox homeostasis present acutely following rmmTBI. Immunocal® significantly limited gliosis in these models; however, its neuroprotection was partially overwhelmed by repetitive injury. Treatments that modulate distinct aspects of TBI pathophysiology, used in combination with GSH precursors like Immunocal®, may show more protection in these repetitive TBI models.

Keywords: Glutathione; Neuroinflammation; Neuroprotection; Oxidative stress; Secondary injury; Traumatic brain injury.

Publication types

Research Support, Non-U.S. Gov't
Research Support, N.I.H., Extramural

MeSH terms

Animals
Brain Concussion*
Brain Injuries, Traumatic* / complications
Dietary Supplements
Disease Models, Animal
Gliosis
Glutathione / metabolism
Mice

Substances

Glutathione

Abstract

Publication types

MeSH terms

Substances

Grants and funding