NO-IL-6/10-IL-1β axis: a new pathway in steatotic and non-steatotic liver grafts from brain-dead donor rats

Araní Casillas-Ramírez; Marc Micó-Carnero; Alfredo Sánchez-González; Cristina Maroto-Serrat; Andrés Trostchansky; Carmen Peralta

doi:10.3389/fimmu.2023.1178909

NO-IL-6/10-IL-1β axis: a new pathway in steatotic and non-steatotic liver grafts from brain-dead donor rats

Front Immunol. 2023 Aug 1:14:1178909. doi: 10.3389/fimmu.2023.1178909. eCollection 2023.

Authors

Araní Casillas-Ramírez^{1

2}, Marc Micó-Carnero³, Alfredo Sánchez-González¹, Cristina Maroto-Serrat³, Andrés Trostchansky⁴, Carmen Peralta³

Affiliations

¹ Department of Teaching and Research Sub-Direction, Hospital Regional de Alta Especialidad de Ciudad Victoria "Bicentenario 2010", Ciudad Victoria, Mexico.
² Facultad de Medicina e Ingeniería en Sistemas Computacionales de Matamoros, Universidad Autónoma de Tamaulipas, Matamoros, Mexico.
³ Department of Liver, Digestive System and Metabolism, Institut d'Investigacions Biomèdiques August Pi i Sunyer, Barcelona, Spain.
⁴ Departamento de Bioquímica and Centro de Investigaciones Biomédicas (CEINBIO), Facultad de Medicina, Universidad de la República, Montevideo, Uruguay.

Abstract

Introduction: Brain death (BD) and steatosis are both risk factors for organ dysfunction or failure in liver transplantation (LT).

Material and methods: Here, we examine the role of interleukin 6 (IL- 6) and IL-10 in LT of both non-steatotic and steatotic liver recovered from donors after brain death (DBDs), as well as the molecular signaling pathways underlying the effects of such cytokines.

Results: BD reduced IL-6 levels only in nonsteatotic grafts, and diminished IL-10 levels only in steatotic ones. In both graft types, BD increased IL-1β, which was associated with hepatic inflammation and damage. IL-6 administration reduced IL-1β only in non-steatotic grafts and protected them against damage and inflammation. Concordantly, IL-1β inhibition via treatment with an IL-1 receptor antagonist caused the same benefits in non-steatotic grafts. Treatment with IL-10 decreased IL-1β only in steatotic grafts and reduced injury and inflammation specifically in this graft type. Blockading the IL-1β effects also reduced damage and inflammation in steatotic grafts. Also, blockade of IL-1β action diminished hepatic cAMP in both types of livers, and this was associated with a reduction in liver injury and inflammation, then pointing to IL-1β regulating cAMP generation under LT and BD conditions. Additionally, the involvement of nitric oxide (NO) in the effects of interleukins was evaluated. Pharmacological inhibition of NO in LT from DBDs prompted even more evident reductions of IL-6 or IL-10 in non-steatotic and steatotic grafts, respectively. This exacerbated the already high levels of IL-1β seen in LT from DBDs, causing worse damage and inflammation in both graft types. The administration of NO donors to non-steatotic grafts potentiated the beneficial effects of endogenous NO, since it increased IL-6 levels, and reduced IL-1β, inflammation, and damage. However, treatment with NO donors in steatotic grafts did not modify IL-10 or IL-1β levels, but induced more injurious effects tan the induction of BD alone, characterized by increased nitrotyrosine, lipid peroxidation, inflammation, and hepatic damage.

Conclusion: Our study thus highlights the specificity of new signaling pathways in LT from DBDs: NO-IL-6-IL-1β in non-steatotic livers and NO-IL-10-IL-1β in steatotic ones. This opens up new therapeutic targets that could be useful in clinical LT.

Keywords: IL-1; IL-10; IL-6; brain death; ischemia-reperfusion; liver transplantation; nitric oxide; steatotic liver grafts.

Publication types

Research Support, Non-U.S. Gov't

MeSH terms

Animals
Brain
Brain Death
Fatty Liver*
Inflammation
Interleukin-6
Nitric Oxide Donors
Nitric Oxide*
Rats

Substances

Interleukin-6
Nitric Oxide
Nitric Oxide Donors

Grants and funding

The Spanish Ministerio de Ciencia supported this research (PID2021-123123OB-100) as did the European Union (via the European Regional Development Fund “Una manera de hacer Europa”).