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L6 结构域四跨膜蛋白 4(Tm4sf4)调控内分泌胰腺的分化和定向细胞迁移。

The L6 domain tetraspanin Tm4sf4 regulates endocrine pancreas differentiation and directed cell migration.

机构信息

Molecular Biology Program, University of Colorado Denver, Aurora, CO 80045, USA.

出版信息

Development. 2011 Aug;138(15):3213-24. doi: 10.1242/dev.058693.

Abstract

The homeodomain transcription factor Nkx2.2 is essential for pancreatic development and islet cell type differentiation. We have identified Tm4sf4, an L6 domain tetraspanin family member, as a transcriptional target of Nkx2.2 that is greatly upregulated during pancreas development in Nkx2.2(-/-) mice. Tetraspanins and L6 domain proteins recruit other membrane receptors to form active signaling centers that coordinate processes such as cell adhesion, migration and differentiation. In this study, we determined that Tm4sf4 is localized to the ductal epithelial compartment and is prominent in the Ngn3(+) islet progenitor cells. We also established that pancreatic tm4sf4 expression and regulation by Nkx2.2 is conserved during zebrafish development. Loss-of-function studies in zebrafish revealed that tm4sf4 inhibits α and β cell specification, but is necessary for ε cell fates. Thus, Tm4sf4 functional output opposes that of Nkx2.2. Further investigation of how Tm4sf4 functions at the cellular level in vitro showed that Tm4sf4 inhibits Rho-activated cell migration and actin organization in a ROCK-independent fashion. We propose that the primary role of Nkx2.2 is to inhibit Tm4sf4 in endocrine progenitor cells, allowing for delamination, migration and/or appropriate cell fate decisions. Identification of a role for Tm4sf4 during endocrine differentiation provides insight into islet progenitor cell behaviors and potential targetable regenerative mechanisms.

摘要

同源域转录因子 Nkx2.2 对于胰腺发育和胰岛细胞类型分化是必不可少的。我们已经确定 Tm4sf4 是 Nkx2.2 的转录靶标,它是 L6 结构域四跨膜蛋白家族成员,在 Nkx2.2(-/-) 小鼠的胰腺发育过程中被极大地上调。四跨膜蛋白和 L6 结构域蛋白招募其他膜受体形成活跃的信号中心,协调细胞黏附、迁移和分化等过程。在这项研究中,我们确定 Tm4sf4 定位于导管上皮细胞区室,在 Ngn3(+)胰岛祖细胞中表现突出。我们还确定了胰腺 tm4sf4 的表达和 Nkx2.2 的调节在斑马鱼发育过程中是保守的。斑马鱼的功能丧失研究表明,tm4sf4 抑制 α 和 β 细胞的特化,但对于 ε 细胞命运是必要的。因此,Tm4sf4 的功能输出与 Nkx2.2 相反。进一步研究 Tm4sf4 在体外细胞水平上的功能表明,Tm4sf4 以 ROCK 非依赖性方式抑制 Rho 激活的细胞迁移和肌动蛋白组织。我们提出,Nkx2.2 的主要作用是抑制内分泌祖细胞中的 Tm4sf4,允许分层、迁移和/或适当的细胞命运决定。在内分泌分化过程中鉴定出 Tm4sf4 的作用,为胰岛祖细胞行为和潜在的可靶向再生机制提供了深入的了解。

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