The role of Neuregulin-1 in steatotic and non-steatotic liver transplantation from donors after cardiocirculatory death

Araní Casillas-Ramírez, Cristina Maroto-Serrat, Carlos Rojano-Alfonso, Francisco Sanus, Marc Micó-Carnero, Margalida Cabrer, Hadassa Yuef Martínez-Padrón, Carmen Peralta
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Abstract

Liver grafts from donors after cardiocirculatory death (DCDs) are sometimes not considered for liver transplantation (LT). Plasma Neuregulin-1 (NRG1) is altered in cardiac abnormalities and the liver is one of the most important targets of NRG1. We study the role of NRG1 in DCD LT. Under these conditions, NRG1 was pharmacologically modulated and their pathways were characterized. NRG1 levels were increased in steatotic and non-steatotic grafts from DCDs; NRG1 was derived from adipose tissue. When NRG1 was inhibited, injury and inflammation were exacerbated. The benefits of endogenous NRG1 in DCD grafts were associated with increased hepatic accumulation of adipocyte-derived vascular endothelial growth factor-A (VEGFA). The Id1-Wnt2 signaling pathway was involved in the action mechanisms of endogenous VEGFA. Exogenous NRG1 exacerbated damage and inflammation. Here differential role of NRG1 (endogenous versus exogenous) was demonstrated and VEGFA treatment was proposed as a highly protective strategy in steatotic and non-steatotic DCD LT.

Abstract Image

Neuregulin-1 在脂肪肝和非脂肪肝肝移植中的作用
心脏循环死亡(DCD)后的供体的肝脏移植物有时不被考虑用于肝移植(LT)。血浆Neuregulin-1(NRG1)在心脏异常时会发生改变,而肝脏是NRG1最重要的靶点之一。我们研究了 NRG1 在 DCD LT 中的作用。在这些条件下,我们对 NRG1 进行了药理调控,并对其通路进行了表征。在来自 DCD 的脂肪性移植物和非脂肪性移植物中,NRG1 水平均有所增加;NRG1 来自脂肪组织。当抑制 NRG1 时,损伤和炎症会加剧。DCD移植物中内源性NRG1的益处与脂肪细胞衍生的血管内皮生长因子-A(VEGFA)的肝积聚增加有关。Id1-Wnt2信号通路参与了内源性血管内皮生长因子的作用机制。外源性 NRG1 会加剧损伤和炎症。在这里,NRG1(内源性与外源性)的不同作用得到了证实,VEGFA治疗被认为是一种对脂肪性和非脂肪性DCD LT具有高度保护作用的策略。
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