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通过转化乳酸菌原位产生和递送CXCL12促进小型猪伤口愈合加速

Accelerated Wound Healing in Minipigs by On-Site Production and Delivery of CXCL12 by Transformed Lactic Acid Bacteria.

作者信息

Öhnstedt Emelie, Lofton Tomenius Hava, Frank Peter, Roos Stefan, Vågesjö Evelina, Phillipson Mia

机构信息

Department of Medical Cell Biology, Uppsala University, 751 23 Uppsala, Sweden.

Ilya Pharma AB, Dag Hammarskjölds Väg, 752 37 Uppsala, Sweden.

出版信息

Pharmaceutics. 2022 Jan 19;14(2):229. doi: 10.3390/pharmaceutics14020229.

Abstract

Non-healing wounds are a growing medical problem and result in considerable suffering. The lack of pharmaceutical treatment options reflects the multistep wound healing process, and the complexity of both translation and assessment of treatment efficacy. We previously demonstrated accelerated healing of full-thickness wounds in mice following topical application of the probiotic bacteria R2LC transformed to express CXCL12. In this study, safety and biological effects of a freeze-dried formulation of CXCL12-producing (ILP100) were investigated in induced full-thickness wounds in minipigs, and different wound healing evaluation methods (macroscopic, planimetry, 2D-photographs, 3D-scanning, ultrasound) were compared. We found that treatment with ILP100 was safe and accelerated healing, as granulation tissue filled wound cavities 1 day faster in treated compared to untreated/placebo-treated wounds. Furthermore, evaluation using planimetry resulted in 1.5 days faster healing than using 2D photographs of the same wounds, whereas the areas measured using 2D photographs were smaller compared to those obtained from 3D scans accounting for surface curvatures, whereas ultrasound imaging enabled detailed detection of thin epithelial layers. In conclusion, topical administration of the drug candidate ILP100 warrants further clinical development as it was proven to be safe and to accelerate healing using different evaluation methods in minipigs.

摘要

难愈合伤口是一个日益严重的医学问题,会导致巨大痛苦。缺乏药物治疗选择反映了伤口愈合的多步骤过程,以及治疗效果转化和评估的复杂性。我们之前证明,在局部应用转化为表达CXCL12的益生菌R2LC后,小鼠的全层伤口愈合加速。在本研究中,我们在小型猪的诱导全层伤口中研究了产生CXCL12的冻干制剂(ILP100)的安全性和生物学效应,并比较了不同的伤口愈合评估方法(宏观观察、平面测量、二维照片、三维扫描、超声)。我们发现,ILP100治疗是安全的且能加速愈合,因为与未治疗/安慰剂治疗的伤口相比,治疗组伤口肉芽组织填充伤口腔的时间快1天。此外,使用平面测量法评估比使用相同伤口的二维照片评估愈合速度快1.5天,而使用二维照片测量的面积比考虑表面曲率的三维扫描获得的面积小,而超声成像能够详细检测薄上皮层。总之,候选药物ILP100的局部给药值得进一步临床开发,因为在小型猪中使用不同评估方法已证明其安全且能加速愈合。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/caf1/8876577/55c7e141c496/pharmaceutics-14-00229-g0A1.jpg

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