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首页> 外文期刊>Journal of diabetes research. >Atypical Diabetic Foot Ulcer Keratinocyte Protein Signaling Correlates with Impaired Wound Healing
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Atypical Diabetic Foot Ulcer Keratinocyte Protein Signaling Correlates with Impaired Wound Healing

机译:非典型糖尿病足溃疡角质形成细胞蛋白信号转导与伤口愈合受损相关

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Diabetes mellitus is associated with chronic diabetic foot ulcers (DFUs) and wound infections often resulting in lower extremity amputations. The protein signaling architecture of the mechanisms responsible for impaired DFU healing has not been characterized. In this preliminary clinical study, the intracellular levels of proteins involved in signal transduction networks relevant to wound healing were non-biasedly measured using reverse-phase protein arrays (RPPA) in keratinocytes isolated from DFU wound biopsies. RPPA allows for the simultaneous documentation and assessment of the signaling pathways active in each DFU. Thus, RPPA provides for the accurate mapping of wound healing pathways associated with apoptosis, proliferation, senescence, survival, and angiogenesis. From the study data, we have identified potential diagnostic, or predictive, biomarkers for DFU wound healing derived from the ratios of quantified signaling protein expressions within interconnected pathways. These biomarkers may allow physicians to personalize therapeutic strategies for DFU management on an individual basis based upon the signaling architecture present in each wound. Additionally, we have identified altered, interconnected signaling pathways within DFU keratinocytes that may help guide the development of therapeutics to modulate these dysregulated pathways, many of which parallel the therapeutic targets which are the hallmarks of molecular therapies for treating cancer.
机译:糖尿病与慢性糖尿病足溃疡(DFU)有关,伤口感染常导致下肢截肢。尚未阐明导致DFU修复受损的机制的蛋白质信号传导结构。在这项初步的临床研究中,在从DFU伤口活检组织中分离出的角质形成细胞中,使用反相蛋白质阵列(RPPA)对与伤口愈合相关的信号转导网络中涉及的蛋白质的细胞内水平进行了无偏测量。 RPPA允许同时记录和评估每个DFU中活跃的信号通路。因此,RPPA提供了与细胞凋亡,增殖,衰老,存活和血管生成相关的伤口愈合途径的准确定位。从研究数据中,我们已经确定了DFU伤口愈合的潜在诊断或预测生物标志物,这些标志物是由相互连接的途径中定量的信号蛋白表达比例得出的。这些生物标记物可以允许医生基于每个伤口中存在的信号传导结构,个性化个性化DFU管理的治疗策略。此外,我们已经确定了DFU角质形成细胞内相互联系的信号通路已改变,这可能有助于指导治疗剂的开发以调节这些失调的途径,其中许多与治疗靶点平行,而这些靶点是治疗癌症的分子疗法的标志。

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