在成熟和发育中的瘢痕疙瘩中定义独特的基因表达谱

Yuan O. Zhu , Scott MacDonnell , Theodore Kaplan , Chien Liu , Yasmeen Ali , Stephanie M. Rangel , Matthew F. Wipperman , Madeleine Belback , Daphne S. Sun , Ziyou Ren , Xiaolong Alan Zhou , Gabor Halasz , Lori Morton , Roopal V. Kundu
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引用次数: 0

摘要

瘢痕疙瘩是一种良性的纤维增生性真皮肿瘤,通常是由于伤口愈合异常而形成的。目前的护理标准通常是无效的,不能防止复发。为了表征瘢痕疙瘩并更好地了解其形成机制,我们对来自不同种族和民族的25名受试者的瘢痕疙瘩活检进行了转录组学分析,其中15人提供了配对的非活体样本、纵向样本或两者兼有。瘢痕疙瘩受试者的非残留皮肤活检的转录组学特征与基线时的对照皮肤相似,但在真皮创伤后转移到与瘢痕疙瘩皮肤非常匹配。外周瘢痕疙瘩皮肤和正常皮肤周围复发均显示上皮-间充质过渡标记物、细胞外基质组织和胶原基因上调。这些瘢痕疙瘩的特征与健康伤口愈合研究的特征强烈重叠,通常具有更大的扰动,这加强了我们对瘢痕疙瘩是失调和旺盛的伤口愈合的理解。此外,还鉴定了219个在瘢痕疙瘩中唯一调控的基因,但在正常受伤或未受伤的皮肤中没有。这项研究为成熟和发展中的瘢痕疙瘩特征提供了见解,可以作为寻找变革性瘢痕疙瘩治疗方法的进一步验证和靶点识别的基础。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

Defining a Unique Gene Expression Profile in Mature and Developing Keloids

Defining a Unique Gene Expression Profile in Mature and Developing Keloids

Defining a Unique Gene Expression Profile in Mature and Developing Keloids

Defining a Unique Gene Expression Profile in Mature and Developing Keloids

Keloids are benign, fibroproliferative dermal tumors that typically form owing to abnormal wound healing. The current standard of care is generally ineffective and does not prevent recurrence. To characterize keloid scars and better understand the mechanism of their formation, we performed transcriptomic profiling of keloid biopsies from a total of 25 subjects of diverse racial and ethnic origins, 15 of whom provided a paired nonlesional sample, a longitudinal sample, or both. The transcriptomic signature of nonlesional skin biopsies from subjects with keloids resembled that of control skin at baseline but shifted to closely match that of keloid skin after dermal trauma. Peripheral keloid skin and rebiopsied surrounding normal skin both showed upregulation of epithelial–mesenchymal transition markers, extracellular matrix organization, and collagen genes. These keloid signatures strongly overlapped those from healthy wound healing studies, usually with greater perturbations, reinforcing our understanding of keloids as dysregulated and exuberant wound healing. In addition, 219 genes uniquely regulated in keloids but not in normal injured or uninjured skin were also identified. This study provides insights into mature and developing keloid signatures that can act as a basis for further validation and target identification in the search for transformative keloid treatments.

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