Fakih Dalia, Pilecki Bartosz, Schlosser Anders, Jepsen Christine S, Thomsen Laura K, Ormhøj Maria, Watson Alastair, Madsen Jens, Clark Howard W, Barfod Kenneth K, Hansen Soren, Marcussen Niels, Jounblat Rania, Chamat Soulaima, Holmskov Uffe, Sorensen Grith L
Department of Cancer and Inflammation Research, Institute of Molecular Medicine, University of Southern Denmark, Odense, Denmark; Department of Biology, Faculty of Sciences II, Lebanese University, Fanar, Lebanon; Laboratory of Immunology, Faculty of Public Health, Lebanese University, Fanar, Lebanon;
Department of Cancer and Inflammation Research, Institute of Molecular Medicine, University of Southern Denmark, Odense, Denmark;
Am J Physiol Lung Cell Mol Physiol. 2015 Dec 1;309(11):L1333-43. doi: 10.1152/ajplung.00090.2015. Epub 2015 Oct 2.
Surfactant protein D (SP-D) is a pulmonary collectin important in lung immunity. SP-D-deficient mice (Sftpd(-/-)) are reported to be susceptible to ovalbumin (OVA)- and fungal allergen-induced pulmonary inflammation, while treatment with exogenous SP-D has therapeutic effects in such disease models. β-Glucans are a diverse group of polysaccharides previously suggested to serve as fungal ligands for SP-D. We set out to investigate if SP-D could interact with 1,3-β-glucan and attenuate allergic pulmonary inflammation in the presence of 1,3-β-glucan. Allergic airway disease was induced in Sftpd(-/-) and Sftpd(+/+) mice by OVA sensitization and subsequent challenge with OVA, 1,3-β-glucan, or OVA/1,3-β-glucan together. Mice in the combined treatment group were further treated with a high dose of recombinant fragment of human SP-D (rfhSP-D). We demonstrated direct interaction between SP-D and 1,3-β-glucan. OVA-induced mucous cell metaplasia was increased in Sftpd(-/-) mice, supporting previously reported protective effects of endogenous SP-D in allergy. OVA-induced parenchymal CCL11 levels and eosinophilic infiltration in bronchoalveolar lavage were unaffected by 1,3-β-glucan, but were reversed with rfhSP-D treatment. 1,3-β-Glucan treatment did, however, induce pulmonary neutrophilic infiltration and increased TNF-α levels in bronchoalveolar lavage, independently of OVA-induced allergy. This infiltration was also reversed by treatment with rfhSP-D. 1,3-β-Glucan reduced OVA-induced mucous cell metaplasia, T helper 2 cytokines, and IFN-γ production. rfhSP-D treatment further reduced mucous metaplasia and T helper 2 cytokine secretion to background levels. In summary, rfhSP-D treatment resulted in attenuation of both allergic inflammation and 1,3-β-glucan-mediated neutrophilic inflammation. Our data suggest that treatment with high-dose SP-D protects from mold-induced exacerbations of allergic asthma.
表面活性蛋白D(SP-D)是一种在肺部免疫中起重要作用的肺凝集素。据报道,SP-D缺陷小鼠(Sftpd(-/-))易患卵清蛋白(OVA)和真菌过敏原诱导的肺部炎症,而外源性SP-D治疗在这些疾病模型中具有治疗作用。β-葡聚糖是一类多样的多糖,先前被认为可作为SP-D的真菌配体。我们着手研究SP-D是否能与1,3-β-葡聚糖相互作用,并在存在1,3-β-葡聚糖的情况下减轻过敏性肺部炎症。通过OVA致敏并随后用OVA、1,3-β-葡聚糖或OVA/1,3-β-葡聚糖联合攻击,在Sftpd(-/-)和Sftpd(+/+)小鼠中诱导过敏性气道疾病。联合治疗组的小鼠进一步用高剂量的人SP-D重组片段(rfhSP-D)进行治疗。我们证明了SP-D与1,3-β-葡聚糖之间的直接相互作用。OVA诱导的黏液细胞化生在Sftpd(-/-)小鼠中增加,这支持了先前报道的内源性SP-D在过敏中的保护作用。OVA诱导的实质CCL11水平和支气管肺泡灌洗中的嗜酸性粒细胞浸润不受1,3-β-葡聚糖的影响,但rfhSP-D治疗可使其逆转。然而,1,3-β-葡聚糖治疗确实诱导了肺部中性粒细胞浸润,并增加了支气管肺泡灌洗中的TNF-α水平,这与OVA诱导的过敏无关。这种浸润也可通过rfhSP-D治疗逆转。1,3-β-葡聚糖减少了OVA诱导的黏液细胞化生、辅助性T细胞2细胞因子和IFN-γ的产生。rfhSP-D治疗进一步将黏液化生和辅助性T细胞2细胞因子分泌降低至背景水平。总之,rfhSP-D治疗导致过敏性炎症和1,3-β-葡聚糖介导的中性粒细胞炎症均减轻。我们的数据表明,高剂量SP-D治疗可预防霉菌诱导的过敏性哮喘加重。
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