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边界嵴帽细胞基因敲除小鼠揭示皮肤神经纤维瘤的细胞起源、肿瘤进展和发病机制。

Cellular Origin, Tumor Progression, and Pathogenic Mechanisms of Cutaneous Neurofibromas Revealed by Mice with Knockout in Boundary Cap Cells.

机构信息

Ecole Normale Supérieure, PSL Research University, CNRS, Inserm, Institut de Biologie de l'Ecole Normale Supérieure (IBENS), Paris, France.

Institut Cochin, Inserm, CNRS, Université Paris Descartes, Paris, France.

出版信息

Cancer Discov. 2019 Jan;9(1):130-147. doi: 10.1158/2159-8290.CD-18-0156. Epub 2018 Oct 22.

Abstract

Patients carrying an inactive allele develop tumors of Schwann cell origin called neurofibromas (NF). Genetically engineered mouse models have significantly enriched our understanding of plexiform forms of NFs (pNF). However, this has not been the case for cutaneous neurofibromas (cNF), observed in all NF1 patients, as no previous model recapitulates their development. Here, we show that conditional inactivation in -positive boundary cap cells leads to e pNFs and cNFs. This work identifies subepidermal glia as a likely candidate for the cellular origin of cNFs and provides insights on disease mechanisms, revealing a long, multistep pathologic process in which inflammation-related signals play a pivotal role. This new mouse model is an important asset for future clinical and therapeutic investigations of NF1-associated neurofibromas. SIGNIFICANCE: Patients affected by NF1 develop numerous cNFs. We present a mouse model that faithfully recapitulates cNFs, identify a candidate cell type at their origin, analyze the steps involved in their formation, and show that their development is dramatically accelerated by skin injury. These findings have important clinical/therapeutic implications..

摘要

携带无活性等位基因的患者会发展出称为神经纤维瘤(NF)的雪旺细胞来源的肿瘤。基因工程小鼠模型极大地丰富了我们对丛状神经纤维瘤(pNF)形式的理解。然而,对于所有 NF1 患者都观察到的皮肤神经纤维瘤(cNF)并非如此,因为以前没有模型能够重现其发展。在这里,我们表明,在β阳性边界帽细胞中条件性失活会导致 e pNFs 和 cNFs。这项工作确定了表皮下神经胶质细胞可能是 cNF 细胞起源的候选细胞类型,并为疾病机制提供了新的见解,揭示了一个漫长的、多步骤的病理过程,其中炎症相关信号发挥了关键作用。这种新型小鼠模型是未来对 NF1 相关神经纤维瘤进行临床和治疗研究的重要资源。意义:患有 NF1 的患者会发展出许多 cNFs。我们提出了一种能够忠实地重现 cNF 的小鼠模型,确定了其起源的候选细胞类型,分析了其形成所涉及的步骤,并表明皮肤损伤会显著加速其发展。这些发现具有重要的临床/治疗意义。

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