Transforming Growth Factor-β Receptor-associated Protein 1 Is a Smad4 Chaperone

Würthner, Jens U.; Frank, David B.; Felici, Angelina; Green, Harry M.; Cao, Zhouhong; Schneider, Michael; McNally, James G.; Lechleider, Robert J.; Roberts, Anita B.

doi:10.1074/jbc.m006473200

Cited by 89 publications

(75 citation statements)

References 39 publications

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“…TRAP1 plays a role in the Smad-mediated signal transduction pathway, interacting with the common mediator Smad4 in a ligand-dependent fashion. While TRAP1 has only a small stimulatory effect on TGF-b signaling in functional assays, deletion of TRAP1 inhibits TGF-b signaling and impairs the interaction between Smad4 and Smad2 [49]. However, TRAP1 does not affect the phosphorylation of Smad2.…”

Section: Discussionmentioning

confidence: 94%

MicroRNA‐181a Regulates Local Immune Balance by Inhibiting Proliferation and Immunosuppressive Properties of Mesenchymal Stem Cells

et al. 2012

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Section: Discussionmentioning

confidence: 94%

MicroRNA‐181a Regulates Local Immune Balance by Inhibiting Proliferation and Immunosuppressive Properties of Mesenchymal Stem Cells

et al. 2012

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“…TGFBRAP1 to VPS39 exchange might further be regulated by proteins such as MON1-CCZ1 (Fig. 6B), which are recruited by CORVET, interact with VPS39, and act as activators of RAB7 (44 -46) and signaling pathways such as the TGF␤ pathway, which has been shown to intersect with TGFBRAP1 and VPS39 function (47)(48)(49).…”

Section: Discussionmentioning

confidence: 99%

Characterization of the Mammalian CORVET and HOPS Complexes and Their Modular Restructuring for Endosome Specificity

Kant

Jonker

Wijdeven

et al. 2015

Journal of Biological Chemistry

117

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Background:The CORVET and HOPS complexes regulate endosomal cargo trafficking but have not been well characterized in mammals. Results: A detailed analysis of subunit interactions within the mammalian CORVET, HOPS, and VIPAS39/VPS33B complexes. Conclusion: Tethering complexes have adapted to the higher complexity of trafficking in mammalian cells. Significance: This work provides a detailed architectural insight into the mammalian endosomal tethering complexes.

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“…Interestingly, TGF-b receptor-associated protein-1 (TRAP-1) was found to speci®cally interact with Smad4 and to aid in the recruitment of Smad4 to the TGF-b and activin receptor complex (Wurthner et al, 2001). TRAP-1 associates with the inactive TGF-b receptor complex, and upon receptor activation, TRAP-1 dissociates from the receptor complex and associates with Smad4.…”

Section: Regulation Of Smad Activation Tgf-b Receptor-induced Smad Acmentioning

confidence: 99%

“…The TRAP-1/Smad4 interaction is transient and disrupted by activated R-Smads. Wurthner et al (2001) suggested that TRAP-1 may function as a chaperone to reduce the auto-inhibitory interactions between N-and C-terminal domains of Smad4 and thereby facilitate the interaction of Smad4 with activated R-Smads.…”

Section: Regulation Of Smad Activation Tgf-b Receptor-induced Smad Acmentioning

confidence: 99%

Regulation of cell proliferation by Smad proteins

Dijke

Goumans

Itoh

2002

Journal Cellular Physiology

398

278

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Transforming growth factor-b (TGF-b) family members which include TGF-bs, activins, and bone morphogenetic proteins (BMPs) regulate a broad spectrum of biological responses on a large variety of cell types. TGF-b family members initiate their cellular responses by binding to distinct receptors with intrinsic serine/ threonine kinase activity and activation of speci®c downstream intracellular effectors termed Smad proteins. Smads relay the signal from the cell membrane to the nucleus, where they affect the transcription of target genes. Smad activation, subcellular distribution, and stability have been found to be intricately regulated and a broad array of transcription factors have been identi®ed as Smad partners. Important activities of TGF-b are its potent anti-mitogenic and pro-apoptotic effects that, at least in part, are mediated via Smad proteins. Escape from TGF-b/ Smad-induced growth inhibition and apoptosis is frequently observed in tumors. Certain Smads have been found to be mutated in speci®c types of cancer and gene ablation of particular Smads in mice has revealed increased rate of tumorigenesis. In late stage tumors, TGF-b has been shown to function as a tumor promoter. TGFb can stimulate the de-differentiation of epithelial cells to malignant invasive and metastatic ®broblastic cells. Interestingly, TGF-b may mediate these effects directly on tumor cells via subverted Smad-dependent and/or Smad-independent pathways.

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Transforming Growth Factor-β Receptor-associated Protein 1 Is a Smad4 Chaperone

Cited by 89 publications

References 39 publications

MicroRNA‐181a Regulates Local Immune Balance by Inhibiting Proliferation and Immunosuppressive Properties of Mesenchymal Stem Cells

MicroRNA‐181a Regulates Local Immune Balance by Inhibiting Proliferation and Immunosuppressive Properties of Mesenchymal Stem Cells

Characterization of the Mammalian CORVET and HOPS Complexes and Their Modular Restructuring for Endosome Specificity

Regulation of cell proliferation by Smad proteins

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