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可溶性P-选择素糖蛋白配体1在小鼠过敏性模型中抑制眼部炎症。

Soluble P-selectin glycoprotein ligand 1 inhibits ocular inflammation in a murine model of allergy.

作者信息

Strauss E C, Larson K A, Brenneise I, Foster C S, Larsen G R, Lee N A, Lee J J

机构信息

Department of Biochemistry and Molecular Biology, Mayo Clinic Scottsdale, Arizona 85259, USA.

出版信息

Invest Ophthalmol Vis Sci. 1999 Jun;40(7):1336-42.

Abstract

PURPOSE

To assess the anti-inflammatory modality of a soluble extracellular form of P-selectin glycoprotein ligand 1 (sPSGL-1) in a mouse model of ocular allergic response.

METHODS

Potential anti-inflammatory effects of sPSGL-1 were investigated in SWR/J mice sensitized by topical application of short ragweed pollen to the nasal mucosa followed by a challenge of the ocular mucosa with the same allergen. Five experimental groups were included in these studies: A, mice neither sensitized nor challenged with pollen (control group 1); B, animals sensitized but not challenged (control group 2); C, animals not sensitized but challenged (control group 3); D, animals sensitized and challenged; and E, sensitized animals treated with sPSGL-1 before pollen challenge. All experimental groups were evaluated for gross morphologic ocular changes, and histologic assessments were made to determine the onset/progression of inflammatory reactions and to look for evidence of eosinophil infiltration.

RESULTS

Mice sensitized and challenged with pollen developed clinical signs consistent with human allergic conjunctivitis. These signs correlate with histologic changes in the conjunctival epithelium and stroma (e.g., edema and extensive eosinophil infiltration). Moreover, the ocular changes also correlated with evidence of eosinophil degranulation. However, sensitized and challenged mice concurrently treated with sPSGL-1 displayed no inflammatory ocular changes associated with a ragweed-induced type-1 hypersensitivity reaction. The lack of ocular changes included the absence of histologic late-phase inflammatory changes of the conjunctiva and a 97% reduction in the induced eosinophil infiltrate.

CONCLUSIONS

The antagonistic intervention of cell- cell interactions through the blockade of selectin-dependent leukocyte adhesion may offer novel therapeutic strategies to modulate inflammatory responses. The potent inhibitory effects on eosinophil recruitment and late-phase inflammation suggest a role for sPSGL-1 in the treatment of ocular allergic diseases.

摘要

目的

在小鼠眼部过敏反应模型中评估可溶性细胞外形式的P-选择素糖蛋白配体1(sPSGL-1)的抗炎方式。

方法

通过将短豚草花粉局部应用于鼻黏膜使SWR/J小鼠致敏,随后用相同变应原刺激眼黏膜,研究sPSGL-1的潜在抗炎作用。这些研究包括五个实验组:A组,既未用花粉致敏也未用花粉刺激的小鼠(对照组1);B组,致敏但未受刺激的动物(对照组2);C组,未致敏但受刺激的动物(对照组3);D组,致敏并受刺激的动物;E组,在花粉刺激前用sPSGL-1治疗的致敏动物。对所有实验组进行眼部大体形态变化评估,并进行组织学评估以确定炎症反应的发生/进展,并寻找嗜酸性粒细胞浸润的证据。

结果

用花粉致敏并刺激的小鼠出现了与人类过敏性结膜炎一致的临床体征。这些体征与结膜上皮和基质的组织学变化相关(如水肿和广泛的嗜酸性粒细胞浸润)。此外,眼部变化也与嗜酸性粒细胞脱颗粒的证据相关。然而,同时用sPSGL-1治疗的致敏和刺激小鼠未出现与豚草诱导的I型超敏反应相关的眼部炎症变化。眼部变化的缺乏包括结膜组织学晚期炎症变化的缺失以及诱导的嗜酸性粒细胞浸润减少97%。

结论

通过阻断选择素依赖性白细胞黏附来拮抗细胞间相互作用可能为调节炎症反应提供新的治疗策略。对嗜酸性粒细胞募集和晚期炎症的强效抑制作用表明sPSGL-1在眼部过敏性疾病治疗中具有作用。

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