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Mast cell hyperactivity underpins the development of oxygen-induced retinopathy
Kenshiro Matsuda, … , Akane Tanaka, Hiroshi Matsuda
Kenshiro Matsuda, … , Akane Tanaka, Hiroshi Matsuda
Published October 9, 2017
Citation Information: J Clin Invest. 2017;127(11):3987-4000. https://doi.org/10.1172/JCI89893.
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Research Article Angiogenesis Inflammation

Mast cell hyperactivity underpins the development of oxygen-induced retinopathy

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Abstract

Mast cells are classically thought to play an important role in protection against helminth infections and in the induction of allergic diseases; however, recent studies indicate that these cells also contribute to neovascularization, which is critical for tissue remodeling, chronic inflammation, and carcinogenesis. Here, we demonstrate that mast cells are essential for sprouting angiogenesis in a murine model of oxygen-induced retinopathy (OIR). Although mouse strains lacking mast cells did not exhibit retinal neovascularization following hypoxia, these mice developed OIR following infusion of mast cells or after injection of mast cell tryptase (MCT). Relative hypoxia stimulated mast cell degranulation via transient receptor potential ankyrin 1. Subsequent surges in MCT stimulated retinal endothelial cells to produce monocyte chemotactic protein-1 (MCP1) and angiogenic factors, leading to sprouting angiogenesis. Mast cell stabilizers as well as specific tryptase and MCP1 inhibitors prevented the development of OIR in WT mice. Preterm infants with early retinopathy of prematurity had markedly higher plasma MCT levels than age-matched infants without disease, suggesting mast cells contribute to human disease. Together, these results suggest therapies that suppress mast cell activity should be further explored as a potential option for preventing eye diseases and subsequent blindness induced by neovascularization.

Authors

Kenshiro Matsuda, Noriko Okamoto, Masatoshi Kondo, Peter D. Arkwright, Kaoru Karasawa, Saori Ishizaka, Shinichi Yokota, Akira Matsuda, Kyungsook Jung, Kumiko Oida, Yosuke Amagai, Hyosun Jang, Eiichiro Noda, Ryota Kakinuma, Koujirou Yasui, Uiko Kaku, Yasuo Mori, Nobuyuki Onai, Toshiaki Ohteki, Akane Tanaka, Hiroshi Matsuda

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Figure 3

Injection of mast cells restored retinal neovascularization in mast cell–deficient DA/Ham-KitWs/Ws rats.

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Injection of mast cells restored retinal neovascularization in mast cell...
(A) Whole-mount analysis of the rat ROP model was conducted on P17. Neovascular tufts are shown as white areas. Yellow areas indicate avascular areas. (B–D) Quantification of whole-mount analysis showed that neovascularization was rescued in KitWs/Ws pups injected with 1 × 106 peritoneal mast cells (PMC) freshly isolated from WT rats. n = 8 in each group. **P < 0.01 versus saline-injected KitWs/Ws rats, Dunnett’s test. (E) ERG analysis was performed on P19. (F) Chloroacetate esterase–positive mast cells were observed in the dorsal skin, but not in the retina. Arrows and arrowheads indicate degranulated and nondegranulated mast cells, respectively. Results are representative of 3 independent experiments. Scale bars: 500 μm (A); 100 μm (F). Results are shown as mean ± SEM of values determined from 4 independent experiments (B–D).

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ISSN: 0021-9738 (print), 1558-8238 (online)

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