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微粒状转化生长因子β1和全反式维甲酸的口服给药可减轻炎症性肠病小鼠模型的肠道炎症。

Oral Delivery of Particulate Transforming Growth Factor Beta 1 and All-Trans Retinoic Acid Reduces Gut Inflammation in Murine Models of Inflammatory Bowel Disease.

作者信息

Conway Thomas F, Hammer Laura, Furtado Stacia, Mathiowitz Edith, Nicoletti Ferdinando, Mangano Katia, Egilmez Nejat K, Auci Dominick L

机构信息

TherapyX , Buffalo, NY, USA State University of New York, at Buffalo, NY, USA.

TherapyX , Buffalo, NY, USA.

出版信息

J Crohns Colitis. 2015 Aug;9(8):647-58. doi: 10.1093/ecco-jcc/jjv089. Epub 2015 May 18.

Abstract

BACKGROUND AND AIMS

We investigated oral delivery of transforming growth factor beta 1 [TGFβ]- and all-trans retinoic acid [ATRA]-loaded microspheres as therapy for gut inflammation in murine models of inflammatory bowel disease [IBD].

METHODS

ATRA and TGFβ were separately encapsulated in poly [lactic-co-glycolic] acid or polylactic acid microspheres [respectively]. TGFβ was encapsulated using proprietary phase-inversion nanoencapsulation [PIN] technology.

RESULTS

PIN particles provided sustained release of bioactive protein for at least 4 days and were stable for up to 52 weeks when stored at either 4(0)C or -20(0)C. In the SCID mouse CD4 + CD25- T cell transfer model of IBD, oral treatment starting at disease onset prevented weight loss, significantly reduced average disease score [~ 50%], serum amyloid A levels [~ 5-fold], colon weight-to-length ratio [~ 50%], and histological score [~ 5-fold].

CONCLUSIONS

Both agents given together outperformed either separately. Highest TGFβ doses and most frequent dose schedule were most effective. Activity was associated with a significant increase [45%] in Foxp3 expression by colonic lamina propria CD4+ CD25+ T-cells. Activity was also demonstrated in dextran sulphate sodium-induced colitis. The data support development of the combination product as a novel, targeted immune based therapy for treatment for IBD.

摘要

背景与目的

我们研究了口服负载转化生长因子β1(TGFβ)和全反式维甲酸(ATRA)的微球作为炎性肠病(IBD)小鼠模型肠道炎症治疗方法的效果。

方法

分别将ATRA和TGFβ包裹于聚乳酸-乙醇酸共聚物或聚乳酸微球中(分别包裹)。使用专利相转化纳米包封(PIN)技术包裹TGFβ。

结果

PIN颗粒能够使生物活性蛋白持续释放至少4天,在4℃或-20℃储存时长达52周都保持稳定。在IBD的SCID小鼠CD4+CD25-T细胞转移模型中,疾病发作时开始口服治疗可防止体重减轻,显著降低平均疾病评分(约50%)、血清淀粉样蛋白A水平(约5倍)、结肠重量与长度比(约50%)以及组织学评分(约5倍)。

结论

两种药物联合使用的效果优于单独使用。最高的TGFβ剂量和最频繁的给药方案最为有效。活性与结肠固有层CD4+CD25+T细胞中Foxp3表达显著增加(45%)相关。在葡聚糖硫酸钠诱导的结肠炎中也证实了其活性。这些数据支持开发该联合产品作为一种新型的、基于靶向免疫的IBD治疗方法。

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