TY - JOUR
T1 - The Role of CCL24 in Primary Sclerosing Cholangitis
T2 - Bridging Patient Serum Proteomics to Preclinical Data
AU - Greenman, Raanan
AU - Snir, Tom
AU - Katav, Avi
AU - Aricha, Revital
AU - Mishalian, Inbal
AU - Hay, Ophir
AU - Frankel, Matthew
AU - Lawler, John
AU - Saffioti, Francesca
AU - Pinzani, Massimo
AU - Thorburn, Douglas
AU - Peled, Amnon
AU - Mor, Adi
AU - Vaknin, Ilan
N1 - Publisher Copyright:
© 2024 by the authors.
PY - 2024/1/23
Y1 - 2024/1/23
N2 - Primary sclerosing cholangitis (PSC) is an inflammatory and fibrotic biliary disease lacking approved treatment. We studied CCL24, a chemokine shown to be overexpressed in damaged bile ducts, and its involvement in key disease-related mechanisms. Serum proteomics of PSC patients and healthy controls (HC) were analyzed using the Olink® proximity extension assay and compared based on disease presence, fibrosis severity, and CCL24 levels. Disease-related canonical pathways, upstream regulators, and toxicity functions were elevated in PSC patients compared to HC and further elevated in patients with high CCL24 levels. In vitro, a protein signature in CCL24-treated hepatic stellate cells (HSCs) differentiated patients by disease severity. In mice, CCL24 intraperitoneal injection selectively recruited neutrophils and monocytes. Treatment with CM-101, a CCL24-neutralizing antibody, in an α-naphthylisothiocyanate (ANIT)-induced cholestasis mouse model effectively inhibited accumulation of peribiliary neutrophils and macrophages while reducing biliary hyperplasia and fibrosis. Furthermore, in PSC patients, CCL24 levels were correlated with upregulation of monocyte and neutrophil chemotaxis pathways. Collectively, these findings highlight the distinct role of CCL24 in PSC, influencing disease-related mechanisms, affecting immune cells trafficking and HSC activation. Its blockade with CM-101 reduces inflammation and fibrosis and positions CCL24 as a promising therapeutic target in PSC.
AB - Primary sclerosing cholangitis (PSC) is an inflammatory and fibrotic biliary disease lacking approved treatment. We studied CCL24, a chemokine shown to be overexpressed in damaged bile ducts, and its involvement in key disease-related mechanisms. Serum proteomics of PSC patients and healthy controls (HC) were analyzed using the Olink® proximity extension assay and compared based on disease presence, fibrosis severity, and CCL24 levels. Disease-related canonical pathways, upstream regulators, and toxicity functions were elevated in PSC patients compared to HC and further elevated in patients with high CCL24 levels. In vitro, a protein signature in CCL24-treated hepatic stellate cells (HSCs) differentiated patients by disease severity. In mice, CCL24 intraperitoneal injection selectively recruited neutrophils and monocytes. Treatment with CM-101, a CCL24-neutralizing antibody, in an α-naphthylisothiocyanate (ANIT)-induced cholestasis mouse model effectively inhibited accumulation of peribiliary neutrophils and macrophages while reducing biliary hyperplasia and fibrosis. Furthermore, in PSC patients, CCL24 levels were correlated with upregulation of monocyte and neutrophil chemotaxis pathways. Collectively, these findings highlight the distinct role of CCL24 in PSC, influencing disease-related mechanisms, affecting immune cells trafficking and HSC activation. Its blockade with CM-101 reduces inflammation and fibrosis and positions CCL24 as a promising therapeutic target in PSC.
KW - CCL24
KW - chemokines
KW - cholangitis
KW - fibrosis
KW - hepatic stellate cells
KW - inflammation
KW - monocytes
KW - neutrophils
KW - proteomics
UR - http://www.scopus.com/inward/record.url?scp=85184718414&partnerID=8YFLogxK
U2 - 10.3390/cells13030209
DO - 10.3390/cells13030209
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C2 - 38334601
AN - SCOPUS:85184718414
SN - 2073-4409
VL - 13
JO - Cells
JF - Cells
IS - 3
M1 - 209
ER -