一种通过组织分层对急性伤口愈合进行时空多变量基因组分析的方法:猪负压治疗的初步研究

Frontiers in molecular medicine Pub Date : 2023-08-31 eCollection Date: 2023-01-01 DOI:10.3389/fmmed.2023.1195822
Jacob G Hodge, Sumedha Gunewardena, Richard A Korentager, David S Zamierowski, Jennifer L Robinson, Adam J Mellott
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引用次数: 0

摘要

简介:伤口治疗能够调节组织再生的复杂分子信号谱。然而,传统的大块组织分析结果是非特异性的表达谱和缺乏时空信息的稀释信号。方法:在负压伤口治疗(NPWT)的背景下,建立猪急性切口伤口模型。将敷料插入有或没有NPWT暴露的伤口,并在8小时内进行评估。伤口外植后,将组织分层并解剖成表皮、真皮层或皮下层,或作为大样本不解剖,所有组均进行RNAseq处理。分层层的RNAseq提供了定义组织区域内表达变化的空间定位,包括血管生成、炎症和基质重塑。结果:在单个创面组中,不同组织层之间相对于其他组织层之间以及相对于整体分析中,不同组织层之间存在不同的表达谱。组织分层鉴定了在批量分析中隐藏的特定组织层内独特的差异表达基因,以及在同一伤口的两层之间微弱信号的放大和/或信号反转,这表明两层皮肤可以抵消批量分析方法中的信号。讨论:本研究中独特的伤口分层和空间RNAseq方法提供了一种新的方法,可以更精确地观察组织内可能无法检测到的表达模式。总之,这些实验数据为伤口愈合途径中组织层内部和组织层之间的早期表达模式和基因组图谱提供了新的见解,可能有助于指导临床决策和改善伤口结局。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
A method for temporal-spatial multivariate genomic analysis of acute wound healing via tissue stratification: a porcine negative pressure therapy pilot study.

Introduction: Wound therapies are capable of modulating the complex molecular signaling profile of tissue regeneration. However traditional, bulk tissue analysis results in nonspecific expressional profiles and diluted signaling that lacks temporal-spatial information. Methods: An acute incisional porcine wound model was developed in the context of negative pressure wound therapy (NPWT). Dressing materials were inserted into wounds with or without NPWT exposure and evaluated over 8-hours. Upon wound explantation, tissue was stratified and dissected into the epidermis, dermis, or subcutaneous layer, or left undissected as a bulk sample and all groups processed for RNAseq. RNAseq of stratified layers provided spatial localization of expressional changes within defined tissue regions, including angiogenesis, inflammation, and matrix remodeling. Results: Different expressional profiles were observed between individual tissue layers relative to each other within a single wound group and between each individual layer relative to bulk analysis. Tissue stratification identified unique differentially expressed genes within specific layers of tissue that were hidden during bulk analysis, as well as amplification of weak signals and/or inversion of signaling between two layers of the same wound, suggesting that two layers of skin can cancel out signaling within bulk analytical approaches. Discussion: The unique wound stratification and spatial RNAseq approach in this study provides a new methodology to observe expressional patterns more precisely within tissue that may have otherwise not been detectable. Together these experimental data offer novel insight into early expressional patterns and genomic profiles, within and between tissue layers, in wound healing pathways that could potentially help guide clinical decisions and improve wound outcomes.

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