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异源三聚体和同源三聚体转化生长因子-β受体在上皮细胞中表现出不同的信号传导和内吞反应。

Heteromeric and homomeric transforming growth factor-beta receptors show distinct signaling and endocytic responses in epithelial cells.

作者信息

Doré J J, Edens M, Garamszegi N, Leof E B

机构信息

Thoracic Disease Research Unit and Department of Biochemistry and Molecular Biology, Mayo Clinic, Rochester, Minnesota 55905, USA.

出版信息

J Biol Chem. 1998 Nov 27;273(48):31770-7. doi: 10.1074/jbc.273.48.31770.

Abstract

Transforming growth factor-beta (TGF-beta) induces distinct responses dependent upon the cellular context. It is unclear whether the initial receptor interactions identified in one cell type will be operative in another. Utilizing a chimeric receptor strategy we have examined the signaling and endocytic activity of both heteromeric (type I/type II) and homomeric (type I/type I or type II/type II) TGF-betaR interactions in Mv1Lu epithelial cells. In agreement with that observed in mesenchymal cells, all TGF-betaR signaling in Mv1Lu cells required the formation of a heteromeric type I-type II receptor complex. However, the initial endocytic response to TGF-betaR oligomerization was distinctly regulated in the two cell types. While heteromeric TGF-beta receptors were internalized and down-regulated, homomeric TGF-betaR interactions showed diminished endocytic activity in Mv1Lu cells. This contrasts to that observed in mesenchymal cultures where ligand bound to TGF-betaR homomers was internalized, yet the receptors were not down-regulated. Moreover, while previous reports have suggested that mutations at serine 172 or threonine 176 in the type I TGF-betaR separated transcriptional from proliferative responses, we found no separation of pathways or effect on initial endocytic activity when the analogous mutations were made in the chimeric receptors.

摘要

转化生长因子-β(TGF-β)根据细胞环境诱导不同的反应。目前尚不清楚在一种细胞类型中鉴定出的初始受体相互作用在另一种细胞类型中是否起作用。利用嵌合受体策略,我们研究了Mv1Lu上皮细胞中异源二聚体(I型/II型)和同源二聚体(I型/I型或II型/II型)TGF-β受体相互作用的信号传导和内吞活性。与在间充质细胞中观察到的一致,Mv1Lu细胞中的所有TGF-β受体信号传导都需要形成异源二聚体I型-II型受体复合物。然而,对TGF-β受体寡聚化的初始内吞反应在两种细胞类型中受到明显调节。虽然异源二聚体TGF-β受体被内化并下调,但同源二聚体TGF-β受体相互作用在Mv1Lu细胞中显示出内吞活性降低。这与在间充质培养物中观察到的情况形成对比,在间充质培养物中,与TGF-β受体同聚体结合的配体被内化,但受体未被下调。此外,虽然先前的报告表明I型TGF-β受体中丝氨酸172或苏氨酸176处的突变将转录反应与增殖反应分开,但我们发现在嵌合受体中进行类似突变时,途径没有分开,对初始内吞活性也没有影响。

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