表皮角质形成细胞中活化β-Catenin条件表达的小鼠模型

IF 4.6 Q2 MATERIALS SCIENCE, BIOMATERIALS
Vineet K Maurya, Yan Ying, John P Lydon
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引用次数: 0

摘要

我们报告了 K5:CAT 双基因小鼠的产生和特征,在这种小鼠中,细胞角蛋白-5(K5)阳性表皮角质形成细胞中有条件地表达构成性激活形式的 β-catenin(ΔN89 β-catenin)。在休止期短期摄入强力霉素后,成年 K5: CAT 大鼠会出现增大的皮脂腺单位,并向真皮深层扩展,这种扩展通常在生长期观察到。长期强力霉素治疗会导致 K5:CAT 表皮显著增厚和褶皱。在这一持续诱导期,有明显证据表明角质细胞增殖增加,特别是在表皮基底细胞层和毛囊外根鞘。这种非计划性的细胞增殖可能是K5:CAT小鼠在持续摄入强力霉素后毛发密度下降的原因。在这一治疗期间,还观察到许多增生的子宫内膜样囊肿,这些囊肿的管腔呈粟粒状。值得注意的是,通过停用强力霉素来减少ΔN89 β-catenin的表达会导致皮肤表型的明显逆转,这表明这些形态学变化依赖于β-catenin和/或其下游分子介质的持续信号转导。我们的 K5: CAT 小鼠模型加入了一小群条件性 β-catenin信号转导小鼠模型的行列,它将特别有助于鉴定那些负责启动和维持 K5: CAT 皮肤表型反应的 β-catenin分子介质。预计这些研究将为表皮上皮形态发生、毛囊循环和毛发生长病理中的β-catenin信号转导提供更多的信息。
本文章由计算机程序翻译,如有差异,请以英文原文为准。

A Mouse Model for Conditional Expression of Activated β-Catenin in Epidermal Keratinocytes.

A Mouse Model for Conditional Expression of Activated β-Catenin in Epidermal Keratinocytes.

We report the generation and characterization of the K5: CAT bigenic mouse in which the constitutively activated form of β-catenin (ΔN89 β-catenin) is conditionally expressed in cytokeratin-5 (K5) positive epidermal keratinocytes. Following short-term doxycycline intake during the telogen resting phase, the adult K5: CAT bigenic develops enlarged pilosebaceous units that expand deep into the dermis, an expansion usually observed during the anagen growth phase. Prolonged doxycycline treatment results in significant thickening and folding of the K5: CAT epidermis. During this persistent induction period, there is clear evidence of increased keratinocyte proliferation, particularly in the epidermal basal cell layer and the outer root sheath of the hair follicle. This unscheduled increase in cellular proliferation likely explains the decrease in hair density observed in the K5: CAT mouse following persistent doxycycline intake. Numerous hyperplastic endometrioid cysts, which display cornification toward their lumens, are also observed during this treatment period. Remarkably, de-induction of ΔN89 β-catenin expression through doxycycline withdrawal results in a marked reversal of the skin phenotype, suggesting that these morphological changes are dependent on continued signaling by β-catenin and/or its downstream molecular mediators. Joining a small group of mouse models for conditional β-catenin signaling, our K5: CAT mouse model will be particularly useful in identifying those molecular mediators of β-catenin that are responsible for initiating and maintaining these phenotypic responses in the K5: CAT skin. Such studies are predicted to shed more light on β-catenin signaling in epidermal epithelial morphogenesis, hair follicle cycling, and hair growth pathologies.

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来源期刊
ACS Applied Bio Materials
ACS Applied Bio Materials Chemistry-Chemistry (all)
CiteScore
9.40
自引率
2.10%
发文量
464
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