Targeting the innate repair receptor axis via erythropoietin or pyroglutamate helix B surface peptide attenuates hemolytic-uremic syndrome in mice

Dennhardt, Sophie; Pirschel, Wiebke; Wissuwa, Bianka; Imhof, Diana; Daniel, Christoph; Kielstein, Jan T.; Hennig-Pauka, Isabel; Amann, Kerstin; Gunzer, Florian; Coldewey, Sina M.

doi:10.3389/fimmu.2022.1010882

Cited by 2 publications

(2 citation statements)

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“…In fact, the level of EPOR in P KO IR kidneys was still significantly higher than that in the WT control (1.7 0.8 vs. 0.1 0.0, P<0.05) after HBSP treatment. In addition, the expression of the heterodimer EPOR/bcR was greatly increased by IR injury in both genotypes and furthered by P KO (7.6×10 6 1.8×10 6 vs. 3.2×10 6 8.0×10 5 , P<0.05, Figure 2B). HBSP treatment significantly decreased the level of EPOR/bcR in the kidneys of P KO mice, but not in WT mice after IR.…”

Section: Hbsp Protected 72-h Ir Kidneys In Both Genotype Micementioning

confidence: 92%

“…Erythropoietin (EPO) receptors include the homodimer (EPOR) 2 initiating erythropoiesis and the heterodimer EPOR/bcR that delivers tissue protection only, thus also known as the innate repair receptor, without role in erythropoiesis (5). The function of EPOR/bcR was mainly discovered via its specific ligand EPOderived helix B surface peptide (HBSP) (6). HBSP attenuated cell death, inflammation and prevented progression of chronic fibrosis after kidney IR injury through multiple signaling pathways, including caspase 9/3, HSP70 and PI3K/Akt/FoxO3a signaling (7)(8)(9).…”

Section: Introductionmentioning

confidence: 99%

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HBSP improves kidney ischemia-reperfusion injury and promotes repair in properdin deficient mice via enhancing phagocytosis of tubular epithelial cells

Huang

Sai

et al. 2023

Front. Immunol.

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Phagocytosis plays vital roles in injury and repair, while its regulation by properdin and innate repair receptor, a heterodimer receptor of erythropoietin receptor (EPOR)/β common receptor (βcR), in renal ischaemia-reperfusion (IR) remains unclear. Properdin, a pattern recognition molecule, facilitates phagocytosis by opsonizing damaged cells. Our previous study showed that the phagocytic function of tubular epithelial cells isolated from properdin knockout (PKO) mouse kidneys was compromised, with upregulated EPOR in IR kidneys that was further raised by PKO at repair phase. Here, helix B surface peptide (HBSP), derived from EPO only recognizing EPOR/βcR, ameliorated IR-induced functional and structural damage in both PKO and wild-type (WT) mice. In particular, HBSP treatment led to less cell apoptosis and F4/80+ macrophage infiltration in the interstitium of PKO IR kidneys compared to the WT control. In addition, the expression of EPOR/βcR was increased by IR in WT kidneys, and furthered increased in IR PKO kidneys, but greatly reduced by HBSP in the IR kidneys of PKO mice. HBSP also increased PCNA expression in IR kidneys of both genotypes. Moreover, iridium-labelled HBSP (HBSP-Ir) was localized mainly in the tubular epithelia after 17-h renal IR in WT mice. HBSP-Ir also anchored to mouse kidney epithelial (TCMK-1) cells treated by H2O2. Both EPOR and EPOR/βcR were significantly increased by H2O2 treatment, while further increased EPOR was showed in cells transfected with small interfering RNA (siRNA) targeting properdin, but a lower level of EPOR was seen in EPOR siRNA and HBSP-treated cells. The number of early apoptotic cells was increased by EPOR siRNA in H2O2-treated TCMK-1, but markedly reversed by HBSP. The phagocytic function of TCMK-1 cells assessed by uptake fluorescence-labelled E.coli was enhanced by HBSP dose-dependently. Our data demonstrate for the first time that HBSP improves the phagocytic function of tubular epithelial cells and kidney repair post IR injury, via upregulated EPOR/βcR triggered by both IR and properdin deficiency.

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Section: Hbsp Protected 72-h Ir Kidneys In Both Genotype Micementioning

confidence: 92%