TAZ激活驱动成纤维细胞球体生长、促纤维化旁分泌信号的表达以及依赖于环境的细胞外基质基因表达。
TAZ activation drives fibroblast spheroid growth, expression of profibrotic paracrine signals, and context-dependent ECM gene expression.
作者信息
Jorgenson Amy J, Choi Kyoung Moo, Sicard Delphine, Smith Karry M J, Hiemer Samantha E, Varelas Xaralabos, Tschumperlin Daniel J
机构信息
Department of Physiology and Biomedical Engineering, College of Medicine, Mayo Clinic, Rochester, Minnesota; and.
Department of Biochemistry, Boston University School of Medicine, Boston, Massachusetts.
出版信息
Am J Physiol Cell Physiol. 2017 Mar 1;312(3):C277-C285. doi: 10.1152/ajpcell.00205.2016. Epub 2016 Nov 23.
Recent studies have implicated the Hippo pathway and its transcriptional effectors YAP and TAZ as necessary for fibroblast activation and tissue fibrosis. To test the specific and sufficient roles for TAZ in driving autonomous fibroblast activation, we cultured NIH3T3 fibroblasts expressing a doxycycline-inducible nuclear-localized mutant of TAZ (TAZ4SA) in scaffold-free 3D hanging drop spheroids, or on matrices of specified mechanical rigidity. Control NIH3T3 fibroblasts formed spheroids in hanging drop culture that remained stable and neither increased nor decreased in size significantly over 15 days. In contrast, TAZ4SA-transduced fibroblasts grew robustly in spheroid culture, and expressed enhanced levels of genes encoding profibrotic soluble factors connective tissue growth factor (CTGF), endothelin-1 (Et-1), and plasminogen activator inhibitor 1 (PAI-1). However, TAZ4SA expression was unable to enhance expression of extracellular matrix (ECM)-encoding genes , or in spheroid culture. Micromechanical testing indicated that spheroids composed of either control or TAZ4SA-expressing cells were highly compliant and indistinguishable in mechanical properties. In fibroblasts cultured on 2D matrices of compliance similar to spheroids, TAZ4SA expression was able to enhance contractile force generation, but was unable to enhance ECM gene expression. In contrast, culture on stiff hydrogels potentiated TAZ4SA enhancement of ECM expression. TAZ4SA enhancement of expression on soft matrices was potentiated by TGF-β1, while on stiff matrices it was abrogated by inhibition of myocardin-related transcription factor, demonstrating context-dependent crosstalk of TAZ with these pathways. These findings demonstrate sufficiency of TAZ activation for driving fibroblast proliferation, contraction, and soluble profibrotic factor expression, and mechanical context-dependent crosstalk of TAZ with other pathways in regulating expression.
近期研究表明,河马通路及其转录效应因子YAP和TAZ是成纤维细胞激活和组织纤维化所必需的。为了测试TAZ在驱动自主成纤维细胞激活中的特定且充分的作用,我们在无支架的三维悬滴球体中,或在具有特定机械刚性的基质上,培养了表达强力霉素诱导型核定位TAZ突变体(TAZ4SA)的NIH3T3成纤维细胞。对照NIH3T3成纤维细胞在悬滴培养中形成球体,这些球体保持稳定,在15天内大小既没有显著增加也没有显著减少。相比之下,转导了TAZ4SA的成纤维细胞在球体培养中强劲生长,并表达了更高水平的编码促纤维化可溶性因子的基因,即结缔组织生长因子(CTGF)、内皮素-1(Et-1)和纤溶酶原激活物抑制剂1(PAI-1)。然而,TAZ4SA的表达无法增强细胞外基质(ECM)编码基因的表达,在球体培养中也是如此。微机械测试表明,由对照细胞或表达TAZ4SA的细胞组成的球体具有高度的顺应性,机械性能无法区分。在与球体顺应性相似的二维基质上培养的成纤维细胞中,TAZ4SA的表达能够增强收缩力的产生,但无法增强ECM基因的表达。相比之下,在刚性水凝胶上培养可增强TAZ4SA对ECM表达的促进作用。TGF-β1增强了TAZ4SA在软基质上对表达的促进作用,而在刚性基质上,通过抑制心肌相关转录因子可消除这种促进作用, 这表明TAZ与这些通路存在依赖于环境的相互作用。这些发现证明了TAZ激活足以驱动成纤维细胞增殖、收缩和可溶性促纤维化因子表达,以及TAZ与其他通路在调节表达中的机械环境依赖性相互作用。
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