Adenosine receptors differentially mediate enteric glial cell death induced by Clostridioides difficile Toxins A and B

Deiziane V S Costa; Jae H Shin; Sophia M Goldbeck; David T Bolick; Flavio S Mesquita; Andrea V Loureiro; Mônica J Rodrigues-Jesus; Gerly A C Brito; Cirle A Warren

doi:10.3389/fimmu.2022.956326

Adenosine receptors differentially mediate enteric glial cell death induced by Clostridioides difficile Toxins A and B

Front Immunol. 2023 Jan 16:13:956326. doi: 10.3389/fimmu.2022.956326. eCollection 2022.

Authors

Deiziane V S Costa¹, Jae H Shin¹, Sophia M Goldbeck¹, David T Bolick¹, Flavio S Mesquita², Andrea V Loureiro³, Mônica J Rodrigues-Jesus¹, Gerly A C Brito³, Cirle A Warren¹

Affiliations

¹ Division of Infectious Diseases and International Health, University of Virginia, Charlottesville, VA, United States.
² Department of Microbiology, University of Sao Paulo, Sao Paulo, Brazil.
³ Department of Morphology, Faculty of Medicine, Federal University of Ceará, Fortaleza, Ceará, Brazil.

Abstract

Increased risk of intestinal dysfunction has been reported in patients after Clostridioides difficile infection (CDI). Enteric glial cells (EGCs), a component of the enteric nervous system (ENS), contribute to gut homeostasis. Previous studies showed that adenosine receptors, A2A and A2B, modulate inflammation during CDI. However, it is unknown how these receptors can modulate the EGC response to the C. difficile toxins (TcdA and TcdB). We investigated the effects of these toxins on the expression of adenosine receptors in EGCs and the role of these receptors on toxin-induced EGC death. Rat EGCs line were incubated with TcdA or TcdB alone or in combination with adenosine analogues 1h prior to toxins challenge. After incubation, EGCs were collected to evaluate gene expression (adenosine receptors and proinflammatory markers) and cell death. In vivo, WT, A2A, and A2B KO mice were infected with C. difficile, euthanized on day 3 post-infection, and cecum tissue was processed. TcdA and TcdB increased A2A and A3 transcripts, as well as decreased A2B. A2A agonist, but not A2A antagonist, decreased apoptosis induced by TcdA and TcdB in EGCs. A2B blocker, but not A2B agonist, diminished apoptosis in EGCs challenged with both toxins. A3 agonist, but not A3 blocker, reduced apoptosis in EGCs challenged with TcdA and TcdB. Inhibition of protein kinase A (PKA) and CREB, both involved in the main signaling pathway driven by activation of adenosine receptors, decreased EGC apoptosis induced by both toxins. A2A agonist and A2B antagonist decreased S100B upregulation induced by C. difficile toxins in EGCs. In vivo, infected A2B KO mice, but not A2A, exhibited a decrease in cell death, including EGCs and enteric neuron loss, compared to infected WT mice, reduced intestinal damage and decreased IL-6 and S100B levels in cecum. Our findings indicate that upregulation of A2A and A3 and downregulation of A2B in EGCs and downregulation of A2B in intestinal tissues elicit a protective response against C. difficile toxins. Adenosine receptors appear to play a regulatory role in EGCs death and proinflammatory response induced by TcdA and TcdB, and thus may be potential targets of intervention to prevent post-CDI intestinal dysmotility.

Keywords: Clostridioides difficile; Clostridioides difficile infection; adenosine receptors; cell death; enteric glia.

Publication types

Research Support, N.I.H., Extramural

MeSH terms

Animals
Apoptosis
Bacterial Proteins / genetics
Bacterial Toxins* / metabolism
Clostridioides difficile* / physiology
Clostridium Infections* / metabolism
Mice
Neuroglia / metabolism
Rats
Receptors, Purinergic P1 / metabolism

Substances

Bacterial Toxins
trimethylaminocarboxyldihydroboran
Bacterial Proteins
Receptors, Purinergic P1

Grants and funding

R21 AI119418/AI/NIAID NIH HHS/United States