Direct Regulation of Alternative Splicing by SMAD3 through PCBP1 Is Essential to the Tumor-Promoting Role of TGF-β

Tripathi, Veenu; Sixt, Katherine M.; Gao, Shaojian; Xu, Xuan; Huang, Jing; Weigert, Roberto; Zhou, Ming; Zhang, Ying E.

doi:10.1016/j.molcel.2016.09.013

Cited by 79 publications

(54 citation statements)

References 38 publications

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“…6 We also found that a nonphosphorytable T179V mutant of SMAD3 while still retaining its transcriptional activity was nevertheless inept in restoring the mesenchymal gene expression, TGF-b-mediated invasion, and formation of lung metastasis to SMAD3-depleted cells. These experimental clues suggested that phosphorylation at T179 could contribute to the contextual cue of cancer progression and prompted us to seek nontranscriptional mechanism of SMAD3 in mediating TGF-b-induced mesenchymal gene expression and cell invasion and metastasis.…”

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confidence: 68%

“…In searching for proteins that confer regulation of the key TGF-b pathway transcription effector SMAD3 via phosphorylation of threonine 179 (T179) in the linker region, we identified an RNA-binding protein poly(RC) binding protein 1 (PCBP1, also known as hnRNP E1), and serendipitously discovered that by partnering with PCBP1, SMAD3 is brought onto the pre-mRNA of a cancer stem cell marker gene CD44 to regulate its alternative splicing. 6 In addition to CD44, our global RNA-seq study revealed a plethora of cancers genes whose splicing patterns are altered by the SMAD3-PCBP1 interaction in favor of tumor progression. These findings let us to propose that regulation of alternative splicing by the concerted action of receptor-activated SMAD3 and PCBP1 is a key mechanism that propels TGF-b to a tumor promoter (Fig.…”

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confidence: 93%

“…Against this backdrop, PCBP1 was identified as a SMAD3-binding partner. 6 The notable features of this new interaction include phosphorylation-induced binding and colocalization of both proteins in the nuclear antigen serine and arginine-rich splicing factor 2 (SRSF2, also known as SC35) positive speckles that are intimately involved in RNA splicing. Modeling on a heavily spliced CD44 gene, we demonstrated that SMAD3 indeed participates directly in the splicing of CD44 mRNA isoforms that are preferentially expressed in association with EMT.…”

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Redirecting RNA splicing by SMAD3 turns TGF-β into a tumor promoter

Tripathi

Zhang

2016

Molecular & Cellular Oncology

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Transforming growth factor b (TGF-b) is a well-known growth inhibitor of normal epithelial cells, but it is also secreted by solid tumors to promote cancer progression. Our recent discovery of SMAD3-PCBP1 complex with direct RNA-binding properties has shed light on how this conversion is implemented by controlling pre-mRNA splicing patterns. Transforming growth factor b (TGF-b) is well known to be a potent growth inhibitor and tumor suppressor; however, at the time when TGF-b was discovered, it was first identified as an activity that transformed normal fibroblasts to form colonies in soft-agar in cooperation with epidermal growth factor (EGF) or TGF-a, both of which are ligands of EGF receptors (EGFR). 1 Fast forward 35 y to present time, it has been appreciated that the two seemingly opposing functions of TGF-b are cell-contextual dependent: in normal epithelial, endothelial, and hematopoietic cells. TGF-b strongly inhibits growth, but this inhibition is lost in late stages of carcinomas with elevated levels of signaling from the mitogen-activated protein kinase (MAPK) pathway sustained by oncogenic mutations. 2,3 Multiple mechanisms by which TGF-b inhibits cell growth have been unraveled, chief among them are transcriptional induction of cyclin dependent kinase (CDK) inhibitors and suppression of proto-oncogene MYC and apoptosis inducer B-cell lymphoma 2 (BCL2). On the other hand, advanced tumors are frequently found with high levels of TGF-b that promotes tumor progression by inducing epithelial to mesenchymal transition (EMT) and invasion. 4,5 Several key transcriptional targets of TGF-b including Snail Family Zinc Finger 1 (SNAl1), Zinc finger E-box binding homeobox 1 (ZEB1), high mobility group AT-Hook 2 (HMGA2), and forkhead box A1 (FOXA1) have been shown to play important roles in TGF-b-induced EMT, while other nontranscriptional mechanisms have also been reported. Despite a vast body of the literature on the nuts and bolts of how TGF-b signals, the mechanism that underpins the switch of TGF-b from a growth inhibitor to a tumor promoter still remains elusive. In searching for proteins that confer regulation of the key TGF-b pathway transcription effector SMAD3 via phosphorylation of threonine 179 (T179) in the linker region, we identified an RNA-binding protein poly(RC) binding protein 1 (PCBP1, also known as hnRNP E1), and serendipitously discovered that by partnering with PCBP1, SMAD3 is brought onto the pre-mRNA of a cancer stem cell marker gene CD44 to regulate its alternative splicing. 6 In addition to CD44, our global RNA-seq study revealed a plethora of cancers genes whose splicing patterns are altered by the SMAD3-PCBP1 interaction in favor of tumor progression. These findings let us to propose that regulation of alternative splicing by the concerted action of receptor-activated SMAD3 and PCBP1 is a key mechanism that propels TGF-b to a tumor promoter (Fig. 1).According to the current paradigm of TGF-b signaling, SMAD3 is activated by phosphorylation at the carboxyl terminus SSXS motif b...

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Redirecting RNA splicing by SMAD3 turns TGF-β into a tumor promoter

Tripathi

Zhang

2016

Molecular & Cellular Oncology

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“…Alternative splicing induced by Smad3 linker phosphorylation is now extended to occur in a large number of genes required for TGF‐β‐induced EMT and metastasis. Upon binding of either Pin1, Nedd4L, Smurf2, or PCBP1 to phosphorylated linker sites of Smad3, phosphorylation at the T179 residue has been determined to play a pivotal role in eliciting biological activities …”

Section: Linker Region‐phosphorylated Smad3 Recruits Functional Molecmentioning

confidence: 99%

“…Upon binding of either Pin1, Nedd4L, Smurf2, or PCBP1 to phosphorylated linker sites of Smad3, phosphorylation at the T179 residue has been determined to play a pivotal role in eliciting biological activities. 35…”

Section: Although Egf Phosphorylates Smad3 Linker Serine/threonine Rementioning

confidence: 99%

Phosphorylation status at Smad3 linker region modulates transforming growth factor‐β‐induced epithelial‐mesenchymal transition and cancer progression

2019

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Smad3, a major transcription factor in transforming growth factor‐β (TGF‐β) signaling, plays critical roles in both tumor‐suppressive and pro‐oncogenic functions. Upon TGF‐β stimulation, the C‐terminal tail of Smad3 undergoes phosphorylation that is essential for canonical TGF‐β signaling. The Smad3 linker region contains serine/threonine phosphorylation sites and can be phosphorylated by intracellular kinases, such as the MAPK family, cyclin‐dependent kinase (CDK) family and glycogen synthase kinase‐3β (GSK‐3β). Previous reports based on cell culture studies by us and others showed that mutation of Smad3 linker phosphorylation sites dramatically intensifies TGF‐β responses as well as growth‐inhibitory function and epithelial‐mesenchymal transition (EMT), suggesting that Smad3 linker phosphorylation suppresses TGF‐β transcriptional activities. However, recent discoveries of Smad3‐interacting molecules that preferentially bind phosphorylated Smad3 linker serine/threonine residues have shown a multitude of signal transductions that either enhance or suppress TGF‐β responses associated with Smad3 turnover or cancer progression. This review aims at providing new insight into the perplexing mechanisms of TGF‐β signaling affected by Smad3 linker phosphorylation and further attempts to gain insight into elimination and protection of TGF‐β‐mediated oncogenic and growth‐suppressive signals, respectively.

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Alternative Splicing of Pre-messenger RNA

Arfelli

Archangelo

2022

Transcriptomics in Health and Disease

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Direct Regulation of Alternative Splicing by SMAD3 through PCBP1 Is Essential to the Tumor-Promoting Role of TGF-β

Cited by 79 publications

References 38 publications

Redirecting RNA splicing by SMAD3 turns TGF-β into a tumor promoter

Redirecting RNA splicing by SMAD3 turns TGF-β into a tumor promoter

Phosphorylation status at Smad3 linker region modulates transforming growth factor‐β‐induced epithelial‐mesenchymal transition and cancer progression

Alternative Splicing of Pre-messenger RNA

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