Program in Molecular Medicine, University of Massachusetts Medical School, Worcester, Massachusetts.
Guangzhou RiboBio Co., Ltd., Guangzhou, China.
J Cell Physiol. 2019 Dec;234(12):21925-21936. doi: 10.1002/jcp.28756. Epub 2019 May 1.
The intestinal epithelium has a high rate of cell turn over and is an excellent system to study stem cell-mediated tissue homeostasis. The Misshapen subfamily of the Ste20 kinases in mammals consists of misshapen like kinase 1 (MINK1), mitogen-activated protein kinase kinase kinase kinase 4 (MAP4K4), and TRAF2 and NCK interacting kinase (TNIK). Recent reports suggest that this subfamily has a novel function equal to the Hippo/MST subfamily as upstream kinases for Warts/Large tumor suppressor kinase (LATS) to suppress tissue growth. To study the in vivo functions of Mink1, Map4k4, and Tnik, we generated a compound knockout of these three genes in the mouse intestinal epithelium. The intestinal epithelia of the mutant animals were phenotypically normal up to approximately 12 months. The older animals then exhibited mildly increased proliferation throughout the lower GI tract. We also observed that the normally spatially organized Paneth cells in the crypt base became dispersed. The expression of one of the YAP pathway target genes Sox9 was increased while other target genes including CTGF did not show a significant change. Therefore, the Misshapen and Hippo subfamilies may have highly redundant functions to regulate growth in the intestinal epithelium, as illustrated in recent tissue culture models.
肠上皮细胞具有较高的细胞更新率,是研究干细胞介导的组织稳态的理想系统。哺乳动物中的 Ste20 激酶畸形亚家族包括畸形样激酶 1(MINK1)、丝裂原活化蛋白激酶激酶激酶激酶 4(MAP4K4)和 TRAF2 和 NCK 相互作用激酶(TNIK)。最近的研究报告表明,该亚家族具有与 Hippo/MST 亚家族相同的新功能,作为 Warts/Large 肿瘤抑制激酶(LATS)的上游激酶,抑制组织生长。为了研究 Mink1、Map4k4 和 Tnik 的体内功能,我们在小鼠肠上皮细胞中生成了这三种基因的复合敲除。突变动物的肠上皮细胞在大约 12 个月内表型正常。年龄较大的动物随后表现出整个下胃肠道轻度增殖增加。我们还观察到,通常在隐窝底部空间组织的 Paneth 细胞变得分散。YAP 途径靶基因 Sox9 的表达增加,而其他靶基因(包括 CTGF)没有显示出显著变化。因此,畸形和 Hippo 亚家族可能具有高度冗余的功能来调节肠上皮细胞的生长,正如最近的组织培养模型所示。
