AUTHOR=Rosin Diane L. , Hall J. Perry , Zheng Shuqiu , Huang Liping , Campos-Bilderback Silvia , Sandoval Ruben , Bree Andrea , Beaumont Kevin , Miller Emily , Larsen Jennifer , Hariri Ghazal , Kaila Neelu , Encarnacion Iain M. , Gale Jeremy D. , van Elsas Andrea , Molitoris Bruce A. , Okusa Mark D. 

TITLE=Human Recombinant Alkaline Phosphatase (Ilofotase Alfa) Protects Against Kidney Ischemia-Reperfusion Injury in Mice and Rats Through Adenosine Receptors

JOURNAL=Frontiers in Medicine

VOLUME=9

YEAR=2022

URL=https://www.frontiersin.org/journals/medicine/articles/10.3389/fmed.2022.931293

DOI=10.3389/fmed.2022.931293

ISSN=2296-858X

ABSTRACT=<p>Adenosine triphosphate (ATP) released from injured or dying cells is a potent pro-inflammatory “danger” signal. Alkaline phosphatase (AP), an endogenous enzyme that de-phosphorylates extracellular ATP, likely plays an anti-inflammatory role in immune responses. We hypothesized that ilofotase alfa, a human recombinant AP, protects kidneys from ischemia-reperfusion injury (IRI), a model of acute kidney injury (AKI), by metabolizing extracellular ATP to adenosine, which is known to activate adenosine receptors. Ilofotase alfa (iv) with or without ZM241,385 (sc), a selective adenosine A<sub>2A</sub> receptor (A<sub>2A</sub>R) antagonist, was administered 1 h before bilateral IRI in WT, A<sub>2A</sub>R KO (<italic>Adora2a<sup>–/–</sup></italic>) or <italic>CD73<sup>–/–</sup></italic> mice. In additional studies recombinant alkaline phosphatase was given after IRI. In an AKI-on-chronic kidney disease (CKD) ischemic rat model, ilofotase alfa was given after the three instances of IRI and rats were followed for 56 days. Ilofotase alfa in a dose dependent manner decreased IRI in WT mice, an effect prevented by ZM241,385 and partially prevented in <italic>Adora2a<sup>–/–</sup></italic> mice. Enzymatically inactive ilofotase alfa was not protective. Ilofotase alfa rescued <italic>CD73<sup>–/–</sup></italic> mice, which lack a 5′-ectonucleotidase that dephosphorylates AMP to adenosine; ZM241,385 inhibited that protection. In both rats and mice ilofotase alfa ameliorated IRI when administered after injury, thus providing relevance for therapeutic dosing of ilofotase alfa following established AKI. In an AKI-on-CKD ischemic rat model, ilofotase alfa given after the third instance of IRI reduced injury. These results suggest that ilofotase alfa promotes production of adenosine from liberated ATP in injured kidney tissue, thereby amplifying endogenous mechanisms that can reverse tissue injury, in part through A<sub>2A</sub>R-and non-A<sub>2A</sub>R-dependent signaling pathways.</p>