Neutrophils insert elastase into hepatocytes to regulate calcium signaling in alcohol-associated hepatitis
Noriyoshi Ogino, … , Barbara E. Ehrlich, Michael H. Nathanson
Noriyoshi Ogino, … , Barbara E. Ehrlich, Michael H. Nathanson
Published June 25, 2024
Citation Information: J Clin Invest. 2024;134(16):e171691. https://doi.org/10.1172/JCI171691.
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Research Article Hepatology

Neutrophils insert elastase into hepatocytes to regulate calcium signaling in alcohol-associated hepatitis

Abstract

Neutrophil infiltration occurs in a variety of liver diseases, but it is unclear how neutrophils and hepatocytes interact. Neutrophils generally use granule proteases to digest phagocytosed bacteria and foreign substances or neutralize them in neutrophil extracellular traps. In certain pathological states, granule proteases play a destructive role against the host as well. More recently, nondestructive actions of neutrophil granule proteins have been reported, such as modulation of tissue remodeling and metabolism. Here, we report a completely different mechanism by which neutrophils act nondestructively, by inserting granules directly into hepatocytes. Specifically, elastase-containing granules were transferred to hepatocytes where elastase selectively degraded intracellular calcium channels to reduce cell proliferation without cytotoxicity. In response, hepatocytes increased expression of Serpin E2 and A3, which inhibited elastase activity. Elastase insertion was seen in patient specimens of alcohol-associated hepatitis, and the relationship between elastase-mediated ITPR2 degradation and reduced cell proliferation was confirmed in mouse models. Moreover, neutrophils from patients with alcohol-associated hepatitis were more prone to degranulation and more potent in reducing calcium channel expression than neutrophils from healthy individuals. This nondestructive and reversible action on hepatocytes defines a previously unrecognized role for neutrophils in the transient regulation of epithelial calcium signaling mechanisms.

Authors

Noriyoshi Ogino, M. Fatima Leite, Mateus T. Guerra, Emma Kruglov, Hiromitsu Asashima, David A. Hafler, Takeshi Ito, João P. Pereira, Brandon J. Peiffer, Zhaoli Sun, Barbara E. Ehrlich, Michael H. Nathanson

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Figure 9

Neutrophils from patients with alcohol-associated hepatitis (AAH) are more capable than healthy controls of degrading ITPR2.

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Neutrophils from patients with alcohol-associated hepatitis (AAH) are mo...
(AD) Kinetics of ITPR2 loss in HepG2 cells cocultured with control or AAH neutrophils. (A) Representative immunoblots of ITPR2 levels in HepG2 cells cocultured with neutrophils for 20 hours from (A) healthy volunteers or (B) patients with AAH. (C) Quantification of data from 7 healthy volunteers and 7 AAH patients shows a significant difference in measured ITPR2/GAPDH levels when 0.025 × 106 or 0.05 × 106 neutrophils were administered. (D) First-order rate constant K is higher for AAH neutrophils than for controls. (EG) MPO and elastase content is similar in control and AAH neutrophils. (E) Representative immunoblots and (F and G) quantitation of MPO and elastase protein levels in neutrophils from 7 healthy volunteers and 7 AAH patients. (H and I) ERK signaling is more active in AAH neutrophils. (H) Representative immunoblots and (I) quantitation of p-ERK and ERK after stimulation of neutrophils isolated from blood of 8 healthy volunteers (Ctrl) or 7 AAH patients with fMLP (100 nM) for 5 minutes. Data are shown as mean ± SEM (C and D) or mean ± SD (F, G, and I). NS, not significant. *P < 0.05, **P < 0.01 by unpaired, 2-tailed Student’s t test.