Pharmacological depletion of microglia alleviates neuronal and vascular damage in the diabetic CX3CR1-WT retina but not in CX3CR1-KO or hCX3CR1(I249/M280)-expressing retina

Diabetic retinopathy, a microvascular disease characterized by irreparable vascular damage, neurodegeneration and neuroinflammation, is a leading complication of diabetes mellitus. There is no cure for DR, and medical interventions marginally slow the progression of disease. Microglia-mediated infla...

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Autores principales: Church, Kaira A., Rodriguez, Derek, Mendiola, Andrew S., Vanegas, Difernando, Gutierrez, Irene L., Tamayo, Ian, Amadu, Abdul, Velazquez, Priscila, Cardona, Sandra M., Gyoneva, Stefka, Cotleur, Anne C., Ransohoff, Richard M., Kaur, Tejbeer, Cardona, Astrid E.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Media S.A. 2023
Materias:
Immunology
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10077890/
https://www.ncbi.nlm.nih.gov/pubmed/37033925
http://dx.doi.org/10.3389/fimmu.2023.1130735
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author Church, Kaira A.
Rodriguez, Derek
Mendiola, Andrew S.
Vanegas, Difernando
Gutierrez, Irene L.
Tamayo, Ian
Amadu, Abdul
Velazquez, Priscila
Cardona, Sandra M.
Gyoneva, Stefka
Cotleur, Anne C.
Ransohoff, Richard M.
Kaur, Tejbeer
Cardona, Astrid E.
author_facet Church, Kaira A.
Rodriguez, Derek
Mendiola, Andrew S.
Vanegas, Difernando
Gutierrez, Irene L.
Tamayo, Ian
Amadu, Abdul
Velazquez, Priscila
Cardona, Sandra M.
Gyoneva, Stefka
Cotleur, Anne C.
Ransohoff, Richard M.
Kaur, Tejbeer
Cardona, Astrid E.
author_sort Church, Kaira A.
collection PubMed
description Diabetic retinopathy, a microvascular disease characterized by irreparable vascular damage, neurodegeneration and neuroinflammation, is a leading complication of diabetes mellitus. There is no cure for DR, and medical interventions marginally slow the progression of disease. Microglia-mediated inflammation in the diabetic retina is regulated via CX3CR1-FKN signaling, where FKN serves as a calming signal for microglial activation in several neuroinflammatory models. Polymorphic variants of CX3CR1, hCX3CR1(I249/M280) , found in 25% of the human population, result in a receptor with lower binding affinity for FKN. Furthermore, disrupted CX3CR1-FKN signaling in CX3CR1-KO and FKN-KO mice leads to exacerbated microglial activation, robust neuronal cell loss and substantial vascular damage in the diabetic retina. Thus, studies to characterize the effects of hCX3CR1(I249/M280) -expression in microglia-mediated inflammation in the diseased retina are relevant to identify mechanisms by which microglia contribute to disease progression. Our results show that hCX3CR1(I249/M280) mice are significantly more susceptible to microgliosis and production of Cxcl10 and TNFα under acute inflammatory conditions. Inflammation is exacerbated under diabetic conditions and coincides with robust neuronal loss in comparison to CX3CR1-WT mice. Therefore, to further investigate the role of hCX3CR1(I249/M280) -expression in microglial responses, we pharmacologically depleted microglia using PLX-5622, a CSF-1R antagonist. PLX-5622 treatment led to a robust (~70%) reduction in Iba1(+) microglia in all non-diabetic and diabetic mice. CSF-1R antagonism in diabetic CX3CR1-WT prevented TUJ1(+) axonal loss, angiogenesis and fibrinogen deposition. In contrast, PLX-5622 microglia depletion in CX3CR1-KO and hCX3CR1(I249/M280) mice did not alleviate TUJ1(+) axonal loss or angiogenesis. Interestingly, PLX-5622 treatment reduced fibrinogen deposition in CX3CR1-KO mice but not in hCX3CR1(I249/M280) mice, suggesting that hCX3CR1(I249/M280) expressing microglia influences vascular pathology differently compared to CX3CR1-KO microglia. Currently CX3CR1-KO mice are the most commonly used strain to investigate CX3CR1-FKN signaling effects on microglia-mediated inflammation and the results in this study indicate that hCX3CR1(I249/M280) receptor variants may serve as a complementary model to study dysregulated CX3CR1-FKN signaling. In summary, the protective effects of microglia depletion is CX3CR1-dependent as microglia depletion in CX3CR1-KO and hCX3CR1(I249/M280) mice did not alleviate retinal degeneration nor microglial morphological activation as observed in CX3CR1-WT mice.
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spelling pubmed-100778902023-04-07 Pharmacological depletion of microglia alleviates neuronal and vascular damage in the diabetic CX3CR1-WT retina but not in CX3CR1-KO or hCX3CR1(I249/M280)-expressing retina Church, Kaira A. Rodriguez, Derek Mendiola, Andrew S. Vanegas, Difernando Gutierrez, Irene L. Tamayo, Ian Amadu, Abdul Velazquez, Priscila Cardona, Sandra M. Gyoneva, Stefka Cotleur, Anne C. Ransohoff, Richard M. Kaur, Tejbeer Cardona, Astrid E. Front Immunol Immunology Diabetic retinopathy, a microvascular disease characterized by irreparable vascular damage, neurodegeneration and neuroinflammation, is a leading complication of diabetes mellitus. There is no cure for DR, and medical interventions marginally slow the progression of disease. Microglia-mediated inflammation in the diabetic retina is regulated via CX3CR1-FKN signaling, where FKN serves as a calming signal for microglial activation in several neuroinflammatory models. Polymorphic variants of CX3CR1, hCX3CR1(I249/M280) , found in 25% of the human population, result in a receptor with lower binding affinity for FKN. Furthermore, disrupted CX3CR1-FKN signaling in CX3CR1-KO and FKN-KO mice leads to exacerbated microglial activation, robust neuronal cell loss and substantial vascular damage in the diabetic retina. Thus, studies to characterize the effects of hCX3CR1(I249/M280) -expression in microglia-mediated inflammation in the diseased retina are relevant to identify mechanisms by which microglia contribute to disease progression. Our results show that hCX3CR1(I249/M280) mice are significantly more susceptible to microgliosis and production of Cxcl10 and TNFα under acute inflammatory conditions. Inflammation is exacerbated under diabetic conditions and coincides with robust neuronal loss in comparison to CX3CR1-WT mice. Therefore, to further investigate the role of hCX3CR1(I249/M280) -expression in microglial responses, we pharmacologically depleted microglia using PLX-5622, a CSF-1R antagonist. PLX-5622 treatment led to a robust (~70%) reduction in Iba1(+) microglia in all non-diabetic and diabetic mice. CSF-1R antagonism in diabetic CX3CR1-WT prevented TUJ1(+) axonal loss, angiogenesis and fibrinogen deposition. In contrast, PLX-5622 microglia depletion in CX3CR1-KO and hCX3CR1(I249/M280) mice did not alleviate TUJ1(+) axonal loss or angiogenesis. Interestingly, PLX-5622 treatment reduced fibrinogen deposition in CX3CR1-KO mice but not in hCX3CR1(I249/M280) mice, suggesting that hCX3CR1(I249/M280) expressing microglia influences vascular pathology differently compared to CX3CR1-KO microglia. Currently CX3CR1-KO mice are the most commonly used strain to investigate CX3CR1-FKN signaling effects on microglia-mediated inflammation and the results in this study indicate that hCX3CR1(I249/M280) receptor variants may serve as a complementary model to study dysregulated CX3CR1-FKN signaling. In summary, the protective effects of microglia depletion is CX3CR1-dependent as microglia depletion in CX3CR1-KO and hCX3CR1(I249/M280) mice did not alleviate retinal degeneration nor microglial morphological activation as observed in CX3CR1-WT mice. Frontiers Media S.A. 2023-03-22 /pmc/articles/PMC10077890/ /pubmed/37033925 http://dx.doi.org/10.3389/fimmu.2023.1130735 Text en Copyright © 2023 Church, Rodriguez, Mendiola, Vanegas, Gutierrez, Tamayo, Amadu, Velazquez, Cardona, Gyoneva, Cotleur, Ransohoff, Kaur and Cardona https://creativecommons.org/licenses/by/4.0/This is an open-access article distributed under the terms of the Creative Commons Attribution License (CC BY). The use, distribution or reproduction in other forums is permitted, provided the original author(s) and the copyright owner(s) are credited and that the original publication in this journal is cited, in accordance with accepted academic practice. No use, distribution or reproduction is permitted which does not comply with these terms.
spellingShingle Immunology
Church, Kaira A.
Rodriguez, Derek
Mendiola, Andrew S.
Vanegas, Difernando
Gutierrez, Irene L.
Tamayo, Ian
Amadu, Abdul
Velazquez, Priscila
Cardona, Sandra M.
Gyoneva, Stefka
Cotleur, Anne C.
Ransohoff, Richard M.
Kaur, Tejbeer
Cardona, Astrid E.
Pharmacological depletion of microglia alleviates neuronal and vascular damage in the diabetic CX3CR1-WT retina but not in CX3CR1-KO or hCX3CR1(I249/M280)-expressing retina
title Pharmacological depletion of microglia alleviates neuronal and vascular damage in the diabetic CX3CR1-WT retina but not in CX3CR1-KO or hCX3CR1(I249/M280)-expressing retina
title_full Pharmacological depletion of microglia alleviates neuronal and vascular damage in the diabetic CX3CR1-WT retina but not in CX3CR1-KO or hCX3CR1(I249/M280)-expressing retina
title_fullStr Pharmacological depletion of microglia alleviates neuronal and vascular damage in the diabetic CX3CR1-WT retina but not in CX3CR1-KO or hCX3CR1(I249/M280)-expressing retina
title_full_unstemmed Pharmacological depletion of microglia alleviates neuronal and vascular damage in the diabetic CX3CR1-WT retina but not in CX3CR1-KO or hCX3CR1(I249/M280)-expressing retina
title_short Pharmacological depletion of microglia alleviates neuronal and vascular damage in the diabetic CX3CR1-WT retina but not in CX3CR1-KO or hCX3CR1(I249/M280)-expressing retina
title_sort pharmacological depletion of microglia alleviates neuronal and vascular damage in the diabetic cx3cr1-wt retina but not in cx3cr1-ko or hcx3cr1(i249/m280)-expressing retina
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10077890/
https://www.ncbi.nlm.nih.gov/pubmed/37033925
http://dx.doi.org/10.3389/fimmu.2023.1130735
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