Has Cristina
Department of Dermatology and Venerology, Medical Center - University of Freiburg, Faculty of Medicine, University of Freiburg, Hauptstrasse 7, DE-79104, Freiburg, Germany.
F1000Res. 2018 Mar 6;7:279. doi: 10.12688/f1000research.12658.1. eCollection 2018.
Skin fragility refers to a large group of conditions in which the ability of the skin to provide protection against trivial mechanical trauma is diminished, resulting in the formation of blisters, erosions, wounds, or scars. Acquired and physiological skin fragility is common; genetic disorders are rare but give insight into the molecular mechanisms ensuring skin stability. The paradigm is represented by inherited epidermolysis bullosa. This review is focused on recent advances in understanding the molecular basis of genetic skin fragility, including emerging concepts, controversies, unanswered questions, and opinions of the author. In spite of the advanced knowledge on the genetic causes of skin fragility, the molecular pathology is still expanding. Open questions in understanding the molecular basis of genetic skin fragility are the following: what are the causes of phenotypes which remain genetically unsolved, and what are the molecular modifiers which might explain phenotypic differences among individuals with similar mutations? New mutational mechanisms and new genes have recently been discovered and are briefly described here. Comprehensive next-generation sequencing-based genetic testing improved mutation detection and facilitated the identification of the genetic basis of unclear and new phenotypes. Characterization of the biochemical and cell biological consequences of the genetic variants is challenging and laborious but may represent the basis for personalized therapeutic approaches. Molecular modifiers of skin fragility have been uncovered in particular animal and genetic models but not in larger cohorts of patients. This scientific progress is the basis for revisions of the epidermolysis bullosa classification and for innovative therapeutic approaches designed for this intractable condition.
皮肤脆弱性指的是一大类病症,即皮肤抵御轻微机械性创伤的能力减弱,从而导致水疱、糜烂、伤口或疤痕的形成。后天性和生理性皮肤脆弱较为常见;遗传性疾病虽罕见,但能让我们深入了解确保皮肤稳定性的分子机制。遗传性大疱性表皮松解症就是典型代表。本综述聚焦于在理解遗传性皮肤脆弱性分子基础方面的最新进展,包括新出现的概念、争议、未解决的问题以及作者的观点。尽管对皮肤脆弱性的遗传病因已有深入了解,但分子病理学仍在不断扩展。在理解遗传性皮肤脆弱性分子基础方面尚未解决的问题如下:那些在遗传上仍未得到解释的表型的病因是什么,以及哪些分子修饰因子可能解释具有相似突变的个体之间的表型差异?最近发现了新的突变机制和新基因,在此简要介绍。基于新一代测序的全面基因检测提高了突变检测能力,并有助于确定不明和新表型的遗传基础。对基因变异的生化和细胞生物学后果进行表征具有挑战性且费力,但可能是个性化治疗方法的基础。皮肤脆弱性的分子修饰因子已在特定动物和遗传模型中被发现,但在更大规模的患者群体中尚未发现。这一科学进展是修订大疱性表皮松解症分类以及为这种难治性疾病设计创新治疗方法的基础。