Filamin A editing in myeloid cells reduces intestinal inflammation and protects from colitis

Riem Gawish; Rajagopal Varada; Florian Deckert; Anastasiya Hladik; Linda Steinbichl; Laura Cimatti; Katarina Milanovic; Mamta Jain; Natalya Torgasheva; Andrea Tanzer; Kim De Paepe; Tom Van de Wiele; Bela Hausmann; Michaela Lang; Martin Pechhacker; Nahla Ibrahim; Ingrid De Vries; Christine Brostjan; Michael Sixt; Christoph Gasche; Louis Boon; David Berry; Michael F. Jantsch; Fatima C. Pereira; Cornelia Vesely

doi:10.1084/jem.20240109

Filamin A editing in myeloid cells reduces intestinal inflammation and protects from colitis

Riem Gawish (Corresponding author), Rajagopal Varada, Florian Deckert, Anastasiya Hladik, Linda Steinbichl, Laura Cimatti, Katarina Milanovic, Mamta Jain, Natalya Torgasheva, Andrea Tanzer, Kim De Paepe, Tom Van de Wiele, Bela Hausmann, Michaela Lang, Martin Pechhacker, Nahla Ibrahim, Ingrid De Vries, Christine Brostjan, Michael Sixt, Christoph GascheLouis Boon, David Berry, Michael F. Jantsch, Fatima C. Pereira (Corresponding author), Cornelia Vesely (Corresponding author)

Department of Microbiology and Ecosystem Science

Publications: Contribution to journal › Article › Peer Reviewed

Abstract

Patho-mechanistic origins of ulcerative colitis are still poorly understood. The actin cross-linker filamin A (FLNA) impacts cellular responses through interaction with cytosolic proteins. Posttranscriptional A-to-I editing generates two forms of FLNA: genome-encoded FLNAQ and FLNAR. FLNA is edited in colon fibroblasts, smooth muscle cells, and endothelial cells. We found that the FLNA editing status determines colitis severity. Editing was highest in healthy colons and reduced during murine and human colitis. Mice that exclusively express FLNAR were highly resistant to DSS-induced colitis, whereas fully FLNAQ animals developed severe inflammation. While the genetic induction of FLNA editing influenced transcriptional states of structural cells and microbiome composition, we found that FLNAR exerts protection specifically via myeloid cells, which are physiologically unedited. Introducing fixed FLNAR did not hamper cell migration but reduced macrophage inflammation and rendered neutrophils less prone to NETosis. Thus, loss of FLNA editing correlates with colitis severity, and targeted editing of myeloid cells serves as a novel therapeutic approach in intestinal inflammation.

Original language	English
Number of pages	34
Journal	The Journal of Experimental Medicine
Volume	222
Issue number	9
DOIs	https://doi.org/10.1084/jem.20240109
Publication status	Published - 5 Jun 2025

Austrian Fields of Science 2012

301902 Immunology
106059 Microbiome research

UN SDGs

This output contributes to the following UN Sustainable Development Goals (SDGs)

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Gawish, R., Varada, R., Deckert, F., Hladik, A., Steinbichl, L., Cimatti, L., Milanovic, K., Jain, M., Torgasheva, N., Tanzer, A., De Paepe, K., Van de Wiele, T., Hausmann, B., Lang, M., Pechhacker, M., Ibrahim, N., De Vries, I., Brostjan, C., Sixt, M., ... Vesely, C. (2025). Filamin A editing in myeloid cells reduces intestinal inflammation and protects from colitis. The Journal of Experimental Medicine, 222(9). https://doi.org/10.1084/jem.20240109

@article{0b2475c70cf1472a8aba33fa9edad058,

title = "Filamin A editing in myeloid cells reduces intestinal inflammation and protects from colitis",

abstract = "Patho-mechanistic origins of ulcerative colitis are still poorly understood. The actin cross-linker filamin A (FLNA) impacts cellular responses through interaction with cytosolic proteins. Posttranscriptional A-to-I editing generates two forms of FLNA: genome-encoded FLNAQ and FLNAR. FLNA is edited in colon fibroblasts, smooth muscle cells, and endothelial cells. We found that the FLNA editing status determines colitis severity. Editing was highest in healthy colons and reduced during murine and human colitis. Mice that exclusively express FLNAR were highly resistant to DSS-induced colitis, whereas fully FLNAQ animals developed severe inflammation. While the genetic induction of FLNA editing influenced transcriptional states of structural cells and microbiome composition, we found that FLNAR exerts protection specifically via myeloid cells, which are physiologically unedited. Introducing fixed FLNAR did not hamper cell migration but reduced macrophage inflammation and rendered neutrophils less prone to NETosis. Thus, loss of FLNA editing correlates with colitis severity, and targeted editing of myeloid cells serves as a novel therapeutic approach in intestinal inflammation.",

author = "Riem Gawish and Rajagopal Varada and Florian Deckert and Anastasiya Hladik and Linda Steinbichl and Laura Cimatti and Katarina Milanovic and Mamta Jain and Natalya Torgasheva and Andrea Tanzer and {De Paepe}, Kim and {Van de Wiele}, Tom and Bela Hausmann and Michaela Lang and Martin Pechhacker and Nahla Ibrahim and {De Vries}, Ingrid and Christine Brostjan and Michael Sixt and Christoph Gasche and Louis Boon and David Berry and Jantsch, {Michael F.} and Pereira, {Fatima C.} and Cornelia Vesely",

note = "Publisher Copyright: {\textcopyright} 2025 Gawish et al.",

year = "2025",

month = jun,

day = "5",

doi = "10.1084/jem.20240109",

language = "English",

volume = "222",

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Gawish, R, Varada, R, Deckert, F, Hladik, A, Steinbichl, L, Cimatti, L, Milanovic, K, Jain, M, Torgasheva, N, Tanzer, A, De Paepe, K, Van de Wiele, T, Hausmann, B, Lang, M, Pechhacker, M, Ibrahim, N, De Vries, I, Brostjan, C, Sixt, M, Gasche, C, Boon, L, Berry, D, Jantsch, MF, Pereira, FC & Vesely, C 2025, 'Filamin A editing in myeloid cells reduces intestinal inflammation and protects from colitis', The Journal of Experimental Medicine, vol. 222, no. 9. https://doi.org/10.1084/jem.20240109

TY - JOUR

T1 - Filamin A editing in myeloid cells reduces intestinal inflammation and protects from colitis

AU - Gawish, Riem

AU - Varada, Rajagopal

AU - Deckert, Florian

AU - Hladik, Anastasiya

AU - Steinbichl, Linda

AU - Cimatti, Laura

AU - Milanovic, Katarina

AU - Jain, Mamta

AU - Torgasheva, Natalya

AU - Tanzer, Andrea

AU - De Paepe, Kim

AU - Van de Wiele, Tom

AU - Hausmann, Bela

AU - Lang, Michaela

AU - Pechhacker, Martin

AU - Ibrahim, Nahla

AU - De Vries, Ingrid

AU - Brostjan, Christine

AU - Sixt, Michael

AU - Gasche, Christoph

AU - Boon, Louis

AU - Berry, David

AU - Jantsch, Michael F.

AU - Pereira, Fatima C.

AU - Vesely, Cornelia

PY - 2025/6/5

Y1 - 2025/6/5

N2 - Patho-mechanistic origins of ulcerative colitis are still poorly understood. The actin cross-linker filamin A (FLNA) impacts cellular responses through interaction with cytosolic proteins. Posttranscriptional A-to-I editing generates two forms of FLNA: genome-encoded FLNAQ and FLNAR. FLNA is edited in colon fibroblasts, smooth muscle cells, and endothelial cells. We found that the FLNA editing status determines colitis severity. Editing was highest in healthy colons and reduced during murine and human colitis. Mice that exclusively express FLNAR were highly resistant to DSS-induced colitis, whereas fully FLNAQ animals developed severe inflammation. While the genetic induction of FLNA editing influenced transcriptional states of structural cells and microbiome composition, we found that FLNAR exerts protection specifically via myeloid cells, which are physiologically unedited. Introducing fixed FLNAR did not hamper cell migration but reduced macrophage inflammation and rendered neutrophils less prone to NETosis. Thus, loss of FLNA editing correlates with colitis severity, and targeted editing of myeloid cells serves as a novel therapeutic approach in intestinal inflammation.

AB - Patho-mechanistic origins of ulcerative colitis are still poorly understood. The actin cross-linker filamin A (FLNA) impacts cellular responses through interaction with cytosolic proteins. Posttranscriptional A-to-I editing generates two forms of FLNA: genome-encoded FLNAQ and FLNAR. FLNA is edited in colon fibroblasts, smooth muscle cells, and endothelial cells. We found that the FLNA editing status determines colitis severity. Editing was highest in healthy colons and reduced during murine and human colitis. Mice that exclusively express FLNAR were highly resistant to DSS-induced colitis, whereas fully FLNAQ animals developed severe inflammation. While the genetic induction of FLNA editing influenced transcriptional states of structural cells and microbiome composition, we found that FLNAR exerts protection specifically via myeloid cells, which are physiologically unedited. Introducing fixed FLNAR did not hamper cell migration but reduced macrophage inflammation and rendered neutrophils less prone to NETosis. Thus, loss of FLNA editing correlates with colitis severity, and targeted editing of myeloid cells serves as a novel therapeutic approach in intestinal inflammation.

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U2 - 10.1084/jem.20240109

DO - 10.1084/jem.20240109

M3 - Article

C2 - 40471139

AN - SCOPUS:105008426130

SN - 0022-1007

VL - 222

JO - The Journal of Experimental Medicine

JF - The Journal of Experimental Medicine

IS - 9

ER -

Filamin A editing in myeloid cells reduces intestinal inflammation and protects from colitis

Abstract

Austrian Fields of Science 2012

UN SDGs

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