Cell Biology Program, Memorial Sloan-Kettering Cancer Center, 1274 York Ave., New York, NY 10065, USA.
Mol Cell Biol. 2011 Jan;31(1):81-91. doi: 10.1128/MCB.01001-10. Epub 2010 Oct 25.
Rho GTPases regulate multiple signaling pathways to control a number of cellular processes during epithelial morphogenesis. To investigate the downstream pathways through which Rho regulates epithelial apical junction formation, we screened a small interfering RNA (siRNA) library targeting 28 known Rho target proteins in 16HBE human bronchial epithelial cells. This led to the identification of the serine-threonine kinase PRK2 (protein kinase C-related kinase 2, also called PKN2). Depletion of PRK2 does not block the initial formation of primordial junctions at nascent cell-cell contacts but does prevent their maturation into apical junctions. PRK2 is recruited to primordial junctions, and this localization depends on its C2-like domain. Rho binding is essential for PRK2 function and also facilitates PRK2 recruitment to junctions. Kinase-dead PRK2 acts as a dominant-negative mutant and prevents apical junction formation. We conclude that PRK2 is recruited to nascent cell-cell contacts through its C2-like and Rho-binding domains and promotes junctional maturation through a kinase-dependent pathway.
Rho GTPases 调节多种信号通路,在上皮形态发生过程中控制许多细胞过程。为了研究 Rho 调节上皮顶端连接形成的下游途径,我们在 16HBE 人支气管上皮细胞中筛选了针对 28 种已知 Rho 靶蛋白的小干扰 RNA(siRNA)文库。这导致了丝氨酸-苏氨酸激酶 PRK2(蛋白激酶 C 相关激酶 2,也称为 PKN2)的鉴定。PRK2 的缺失不会阻断原代连接在新生细胞-细胞接触处的初始形成,但确实阻止了它们向顶端连接的成熟。PRK2 被募集到原始连接,这种定位依赖于其 C2 样结构域。Rho 结合对于 PRK2 的功能是必需的,并且还促进 PRK2 募集到连接。激酶失活的 PRK2 作为显性负突变体,防止顶端连接形成。我们得出结论,PRK2 通过其 C2 样和 Rho 结合结构域被募集到新生细胞-细胞接触处,并通过激酶依赖途径促进连接成熟。
