IPSE, a parasite-derived host immunomodulatory protein, is a potential therapeutic for hemorrhagic cystitis.

We report that H-IPSEH03, like M-IPSE and H-IPSEH06, activates IgE-bearing basophils in an NFAT reporter assay, indicating activation of the cytokine pathway. Further, H-IPSEH03 attenuates ifosfamide-induced increases in bladder wet weight in an IL-4-dependent fashion. H-IPSEH03 relieves hemorrhagic cystitis-associated allodynia and modulates voiding patterns in mice. Finally, H-IPSEH03 drives increased urothelial cell proliferation suggesting that IPSE induces bladder repair mechanisms. Taken together, H-IPSEH03 may be a potential novel therapeutic to treat hemorrhagic cystitis by basophil activation, attenuation of allodynia and promotion of urothelial cell proliferation. PMID: 30785353 [PubMed - as supplied by publisher]

https://www.ncbi.nlm.nih.gov/pubmed/30785353?dopt=Abstract

Source: American Journal of Physiology. Renal Physiology - February 20, 2019 Category: Physiology Authors: Zee RS, Mbanefo EC, Le LH, Pennington LF, Odegaard J, Jardetzky TS, Alouffi A, Akinwale J, Falcone FH, Hsieh MH Tags: Am J Physiol Renal Physiol Source Type: research