Targeting hypoxia-inducible factors with 32-134D safely and effectively treats diabetic eye disease in mice

Many patients with diabetic eye disease respond inadequately to anti-VEGF therapies, implicating additional vasoactive mediators in its pathogenesis. We demonstrate that levels of angiogenic proteins regulated by HIF-1 and -2 remain elevated in the eyes of people with diabetes despite treatment with...

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Autores principales: Zhang, Jing, Sharma, Deepti, Dinabandhu, Aumreetam, Sanchez, Jaron, Applewhite, Brooks, Jee, Kathleen, Deshpande, Monika, Flores-Bellver, Miguel, Hu, Ming-Wen, Guo, Chuanyu, Salman, Shaima, Hwang, Yousang, Anders, Nicole M., Rudek, Michelle A., Qian, Jiang, Canto-Soler, M. Valeria, Semenza, Gregg L., Montaner, Silvia, Sodhi, Akrit
Formato: Online Artículo Texto
Lenguaje:English
Publicado: American Society for Clinical Investigation 2023
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10313368/
https://www.ncbi.nlm.nih.gov/pubmed/37227777
http://dx.doi.org/10.1172/JCI163290
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author Zhang, Jing
Sharma, Deepti
Dinabandhu, Aumreetam
Sanchez, Jaron
Applewhite, Brooks
Jee, Kathleen
Deshpande, Monika
Flores-Bellver, Miguel
Hu, Ming-Wen
Guo, Chuanyu
Salman, Shaima
Hwang, Yousang
Anders, Nicole M.
Rudek, Michelle A.
Qian, Jiang
Canto-Soler, M. Valeria
Semenza, Gregg L.
Montaner, Silvia
Sodhi, Akrit
author_facet Zhang, Jing
Sharma, Deepti
Dinabandhu, Aumreetam
Sanchez, Jaron
Applewhite, Brooks
Jee, Kathleen
Deshpande, Monika
Flores-Bellver, Miguel
Hu, Ming-Wen
Guo, Chuanyu
Salman, Shaima
Hwang, Yousang
Anders, Nicole M.
Rudek, Michelle A.
Qian, Jiang
Canto-Soler, M. Valeria
Semenza, Gregg L.
Montaner, Silvia
Sodhi, Akrit
author_sort Zhang, Jing
collection PubMed
description Many patients with diabetic eye disease respond inadequately to anti-VEGF therapies, implicating additional vasoactive mediators in its pathogenesis. We demonstrate that levels of angiogenic proteins regulated by HIF-1 and -2 remain elevated in the eyes of people with diabetes despite treatment with anti-VEGF therapy. Conversely, by inhibiting HIFs, we normalized the expression of multiple vasoactive mediators in mouse models of diabetic eye disease. Accumulation of HIFs and HIF-regulated vasoactive mediators in hyperglycemic animals was observed in the absence of tissue hypoxia, suggesting that targeting HIFs may be an effective early treatment for diabetic retinopathy. However, while the HIF inhibitor acriflavine prevented retinal vascular hyperpermeability in diabetic mice for several months following a single intraocular injection, accumulation of acriflavine in the retina resulted in retinal toxicity over time, raising concerns for its use in patients. Conversely, 32-134D, a recently developed HIF inhibitor structurally unrelated to acriflavine, was not toxic to the retina, yet effectively inhibited HIF accumulation and normalized HIF-regulated gene expression in mice and in human retinal organoids. Intraocular administration of 32-134D prevented retinal neovascularization and vascular hyperpermeability in mice. These results provide the foundation for clinical studies assessing 32-134D for the treatment of patients with diabetic eye disease.
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spelling pubmed-103133682023-07-03 Targeting hypoxia-inducible factors with 32-134D safely and effectively treats diabetic eye disease in mice Zhang, Jing Sharma, Deepti Dinabandhu, Aumreetam Sanchez, Jaron Applewhite, Brooks Jee, Kathleen Deshpande, Monika Flores-Bellver, Miguel Hu, Ming-Wen Guo, Chuanyu Salman, Shaima Hwang, Yousang Anders, Nicole M. Rudek, Michelle A. Qian, Jiang Canto-Soler, M. Valeria Semenza, Gregg L. Montaner, Silvia Sodhi, Akrit J Clin Invest Research Article Many patients with diabetic eye disease respond inadequately to anti-VEGF therapies, implicating additional vasoactive mediators in its pathogenesis. We demonstrate that levels of angiogenic proteins regulated by HIF-1 and -2 remain elevated in the eyes of people with diabetes despite treatment with anti-VEGF therapy. Conversely, by inhibiting HIFs, we normalized the expression of multiple vasoactive mediators in mouse models of diabetic eye disease. Accumulation of HIFs and HIF-regulated vasoactive mediators in hyperglycemic animals was observed in the absence of tissue hypoxia, suggesting that targeting HIFs may be an effective early treatment for diabetic retinopathy. However, while the HIF inhibitor acriflavine prevented retinal vascular hyperpermeability in diabetic mice for several months following a single intraocular injection, accumulation of acriflavine in the retina resulted in retinal toxicity over time, raising concerns for its use in patients. Conversely, 32-134D, a recently developed HIF inhibitor structurally unrelated to acriflavine, was not toxic to the retina, yet effectively inhibited HIF accumulation and normalized HIF-regulated gene expression in mice and in human retinal organoids. Intraocular administration of 32-134D prevented retinal neovascularization and vascular hyperpermeability in mice. These results provide the foundation for clinical studies assessing 32-134D for the treatment of patients with diabetic eye disease. American Society for Clinical Investigation 2023-07-03 /pmc/articles/PMC10313368/ /pubmed/37227777 http://dx.doi.org/10.1172/JCI163290 Text en © 2023 Zhang et al. https://creativecommons.org/licenses/by/4.0/This work is licensed under the Creative Commons Attribution 4.0 International License. To view a copy of this license, visit http://creativecommons.org/licenses/by/4.0/ (https://creativecommons.org/licenses/by/4.0/) .
spellingShingle Research Article
Zhang, Jing
Sharma, Deepti
Dinabandhu, Aumreetam
Sanchez, Jaron
Applewhite, Brooks
Jee, Kathleen
Deshpande, Monika
Flores-Bellver, Miguel
Hu, Ming-Wen
Guo, Chuanyu
Salman, Shaima
Hwang, Yousang
Anders, Nicole M.
Rudek, Michelle A.
Qian, Jiang
Canto-Soler, M. Valeria
Semenza, Gregg L.
Montaner, Silvia
Sodhi, Akrit
Targeting hypoxia-inducible factors with 32-134D safely and effectively treats diabetic eye disease in mice
title Targeting hypoxia-inducible factors with 32-134D safely and effectively treats diabetic eye disease in mice
title_full Targeting hypoxia-inducible factors with 32-134D safely and effectively treats diabetic eye disease in mice
title_fullStr Targeting hypoxia-inducible factors with 32-134D safely and effectively treats diabetic eye disease in mice
title_full_unstemmed Targeting hypoxia-inducible factors with 32-134D safely and effectively treats diabetic eye disease in mice
title_short Targeting hypoxia-inducible factors with 32-134D safely and effectively treats diabetic eye disease in mice
title_sort targeting hypoxia-inducible factors with 32-134d safely and effectively treats diabetic eye disease in mice
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10313368/
https://www.ncbi.nlm.nih.gov/pubmed/37227777
http://dx.doi.org/10.1172/JCI163290
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