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FoxP3 expression by retinal pigment epithelial cells : transcription factor with potential relevance for the pathology of age-related macular degeneration

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Alfaar_2-11sk6rps1f7tx0.pdf
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2022

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Alfaar, Ahmad Samir
Stürzbecher, Lucas
Diedrichs-Möhring, Maria
Lam, Marion
Roubeix, Christophe
Ritter, Julia
Annamalai, Balasubramaniam
Wildner, Gerhild
Strauß, Olaf
et al.

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http://nbn-resolving.de/urn:nbn:de:bsz:352-2-11sk6rps1f7tx0
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https://doi.org/10.1186/s12974-022-02620-w
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CC BY 4.0

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Journal of Neuroinflammation. Springer. 2022, 19(1), 260. eISSN 1742-2094. Verfügbar unter: doi: 10.1186/s12974-022-02620-w

Zusammenfassung

Background Forkhead-Box-Protein P3 (FoxP3) is a transcription factor and marker of regulatory T cells, converting naive T cells into Tregs that can downregulate the effector function of other T cells. We previously detected the expression of FoxP3 in retinal pigment epithelial (RPE) cells, forming the outer blood–retina barrier of the immune privileged eye.

Methods We investigated the expression, subcellular localization, and phosphorylation of FoxP3 in RPE cells in vivo and in vitro after treatment with various stressors including age, retinal laser burn, autoimmune inflammation, exposure to cigarette smoke, in addition of IL-1β and mechanical cell monolayer destruction. Eye tissue from humans, mouse models of retinal degeneration and rats, and ARPE-19, a human RPE cell line for in vitro experiments, underwent immunohistochemical, immunofluorescence staining, and PCR or immunoblot analysis to determine the intracellular localization and phosphorylation of FoxP3. Cytokine expression of stressed cultured RPE cells was investigated by multiplex bead analysis. Depletion of the FoxP3 gene was performed with CRISPR/Cas9 editing.

Results RPE in vivo displayed increased nuclear FoxP3-expression with increases in age and inflammation, long-term exposure of mice to cigarette smoke, or after laser burn injury. The human RPE cell line ARPE-19 constitutively expressed nuclear FoxP3 under non-confluent culture conditions, representing a regulatory phenotype under chronic stress. Confluently grown cells expressed cytosolic FoxP3 that was translocated to the nucleus after treatment with IL-1β to imitate activated macrophages or after mechanical destruction of the monolayer. Moreover, with depletion of FoxP3, but not of a control gene, by CRISPR/Cas9 gene editing decreased stress resistance of RPE cells.

Conclusion Our data suggest that FoxP3 is upregulated by age and under cellular stress and might be important for RPE function.

Zusammenfassung in einer weiteren Sprache

Fachgebiet (DDC)
570 Biowissenschaften, Biologie

Schlagwörter

IL-1β, Ca-channels, CRISPR/Cas9, Phosphorylation, RPE, Age-related macular degeneration, FoxP3, Immune barrier, Immune privilege of the retina

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ISO 690ALFAAR, Ahmad Samir, Lucas STÜRZBECHER, Maria DIEDRICHS-MÖHRING, Marion LAM, Christophe ROUBEIX, Julia RITTER, Kathrin SCHUMANN, Balasubramaniam ANNAMALAI, Gerhild WILDNER, Olaf STRAUSS, 2022. FoxP3 expression by retinal pigment epithelial cells : transcription factor with potential relevance for the pathology of age-related macular degeneration. In: Journal of Neuroinflammation. Springer. 2022, 19(1), 260. eISSN 1742-2094. Verfügbar unter: doi: 10.1186/s12974-022-02620-w
BibTex
@article{Alfaar2022-10-22FoxP3-75127,
  title={FoxP3 expression by retinal pigment epithelial cells : transcription factor with potential relevance for the pathology of age-related macular degeneration},
  year={2022},
  doi={10.1186/s12974-022-02620-w},
  number={1},
  volume={19},
  journal={Journal of Neuroinflammation},
  author={Alfaar, Ahmad Samir and Stürzbecher, Lucas and Diedrichs-Möhring, Maria and Lam, Marion and Roubeix, Christophe and Ritter, Julia and Schumann, Kathrin and Annamalai, Balasubramaniam and Wildner, Gerhild and Strauß, Olaf},
  note={Article Number: 260}
}
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Forkhead-Box-Protein P3 (FoxP3) is a transcription factor and marker of regulatory T cells, converting naive T cells into Tregs that can downregulate the effector function of other T cells. We previously detected the expression of FoxP3 in retinal pigment epithelial (RPE) cells, forming the outer blood–retina barrier of the immune privileged eye.

Methods
We investigated the expression, subcellular localization, and phosphorylation of FoxP3 in RPE cells in vivo and in vitro after treatment with various stressors including age, retinal laser burn, autoimmune inflammation, exposure to cigarette smoke, in addition of IL-1β and mechanical cell monolayer destruction. Eye tissue from humans, mouse models of retinal degeneration and rats, and ARPE-19, a human RPE cell line for in vitro experiments, underwent immunohistochemical, immunofluorescence staining, and PCR or immunoblot analysis to determine the intracellular localization and phosphorylation of FoxP3. Cytokine expression of stressed cultured RPE cells was investigated by multiplex bead analysis. Depletion of the FoxP3 gene was performed with CRISPR/Cas9 editing.

Results
RPE in vivo displayed increased nuclear FoxP3-expression with increases in age and inflammation, long-term exposure of mice to cigarette smoke, or after laser burn injury. The human RPE cell line ARPE-19 constitutively expressed nuclear FoxP3 under non-confluent culture conditions, representing a regulatory phenotype under chronic stress. Confluently grown cells expressed cytosolic FoxP3 that was translocated to the nucleus after treatment with IL-1β to imitate activated macrophages or after mechanical destruction of the monolayer. Moreover, with depletion of FoxP3, but not of a control gene, by CRISPR/Cas9 gene editing decreased stress resistance of RPE cells.

Conclusion
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    <dc:contributor>Strauß, Olaf</dc:contributor>
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