Tamm-Horsfall protein augments neutrophil NETosis during urinary tract infection
Vicki Mercado-Evans, … , Victor Nizet, Kathryn A. Patras
Vicki Mercado-Evans, … , Victor Nizet, Kathryn A. Patras
Published November 26, 2024
Citation Information: JCI Insight. 2025;10(1):e180024. https://doi.org/10.1172/jci.insight.180024.
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Research Article Immunology Infectious disease

Tamm-Horsfall protein augments neutrophil NETosis during urinary tract infection

Abstract

Urinary neutrophils are a hallmark of urinary tract infection (UTI), yet the mechanisms governing their activation, function, and efficacy in controlling infection remain incompletely understood. Tamm-Horsfall glycoprotein (THP), the most abundant protein in urine, uses terminal sialic acids to bind an inhibitory receptor and dampen neutrophil inflammatory responses. We hypothesized that neutrophil modulation is an integral part of THP-mediated host protection. In a UTI model, THP-deficient mice showed elevated urinary tract bacterial burdens, increased neutrophil recruitment, and more severe tissue histopathological changes compared with WT mice. Furthermore, THP-deficient mice displayed impaired urinary NETosis during UTI. To investigate the effect of THP on NETosis, we coupled in vitro fluorescence-based NET assays, proteomic analyses, and standard and imaging flow cytometry with peripheral human neutrophils. We found that THP increases proteins involved in respiratory chain, neutrophil granules, and chromatin remodeling pathways; enhances NETosis in an ROS-dependent manner; and drives NET-associated morphologic features including nuclear decondensation. These effects were observed only in the presence of a NETosis stimulus and could not be solely replicated with equivalent levels of sialic acid alone. We conclude that THP is a critical regulator of NETosis in the urinary tract, playing a key role in host defense against UTI.

Authors

Vicki Mercado-Evans, Holly Branthoover, Claude Chew, Camille Serchejian, Alexander B. Saltzman, Marlyd E. Mejia, Jacob J. Zulk, Ingrid Cornax, Victor Nizet, Kathryn A. Patras

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Figure 1

THP deficiency increases urinary tract bacterial burdens and tissue pathology.

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THP deficiency increases urinary tract bacterial burdens and tissue path...
(AC) Time course of urine (A), bladder (B), and kidney (C) UPEC burdens from WT and THP-KO mice. Urine samples were collected from mice at multiple time points up until tissue collection. (D and E) Bladder (D) and kidney (E) pathology scores on 1 and 3 dpi. (F and G) Representative H&E images of day 1 bladders (F) and day 3 kidneys (G) from UPEC-infected or mock-infected mice. Scale bars: 110 μm (F) and 210 μm (G). Arrowheads point to polymorphonuclear cell infiltration (black) and polymorphonuclear cell aggregates (blue). Experiments were performed at least twice with data combined. n = 18–46/time point (A), n = 11–31 (B and C), or n = 5–15 (D and E). Box-and-whisker plots show median, all points, and 25–75th percentiles (AC). Points represent individual samples; lines indicate medians with interquartile ranges (D and E). Data were analyzed by Mann-Whitney U test (AC) and Fisher’s exact test (D and E). *P < 0.05; **P < 0.01.