Splice Variants of SmgGDS Control Small GTPase Prenylation and Membrane Localization

SmgGDS is an atypical guanine nucleotide exchange factor (GEF) that promotes both cell proliferation and migration and is up-regulated in several types of cancer. SmgGDS has been previously shown to activate a wide variety of small GTPases, including the Ras family members Rap1a, Rap1b, and K-Ras, as well as the Rho family members Cdc42, Rac1, Rac2, RhoA, and RhoB. In contrast, here we show that SmgGDS exclusively activates RhoA and RhoC among a large panel of purified GTPases. Consistent with the well known properties of GEFs, this activation is catalytic, and SmgGDS preferentially binds to nucleotide-depleted RhoA relative to either GDP-or GTP␥S-bound forms. However, mutational analyses indicate that SmgGDS utilizes a distinct exchange mechanism compared with canonical GEFs and in contrast to known GEFs requires RhoA to retain a polybasic region for activation. A homology model of SmgGDS highlights an electronegative surface patch and a highly conserved binding groove. Mutation of either area ablates the ability of SmgGDS to activate RhoA. Finally, the in vitro specificity of SmgGDS for RhoA and RhoC is retained in cells. Together, these results indicate that SmgGDS is a bona fide GEF that specifically activates RhoA and RhoC through a unique mechanism not used by other Rho family exchange factors.

Section: Discussionmentioning

confidence: 71%

SmgGDS Is a Guanine Nucleotide Exchange Factor That Specifically Activates RhoA and RhoC

Hamel¹,

Monaghan-Benson²,

Rojas³

et al. 2011

“…There are two predominant isoforms of SmgGDS, SmgGDS-607 and SmgGDS-558, which differ by one armadillo domain (5). Recent studies have demonstrated that SmgGDS-558 plays a more significant role than SmgGDS-607 in activating RhoA in breast cancer cells, despite lower levels of endogenous SmgGDS-558 protein (6,7).…”

mentioning

confidence: 99%

“…SmgGDS (Rap1GDS1) is a noncanonical GEF for RhoA and RhoC (4) and also promotes the pro-oncogenic functions of several other small GTPases with C-terminal polybasic regions (PBRs) (5). There are two predominant isoforms of SmgGDS, SmgGDS-607 and SmgGDS-558, which differ by one armadillo domain (5).…”

mentioning

confidence: 99%

The Tumor-suppressive Small GTPase DiRas1 Binds the Noncanonical Guanine Nucleotide Exchange Factor SmgGDS and Antagonizes SmgGDS Interactions with Oncogenic Small GTPases

Bergom

Hauser

Rymaszewski

et al. 2016

Self Cite

The small GTPase DiRas1 has tumor-suppressive activities, unlike the oncogenic properties more common to small GTPases such as K-Ras and RhoA. Although DiRas1 has been found to be a tumor suppressor in gliomas and esophageal squamous cell carcinomas, the mechanisms by which it inhibits malignant phenotypes have not been fully determined. In this study, we demonstrate that DiRas1 binds to SmgGDS, a protein that promotes the activation of several oncogenic GTPases. In silico docking studies predict that DiRas1 binds to SmgGDS in a manner similar to other small GTPases. SmgGDS is a guanine nucleotide exchange factor for RhoA, but we report here that SmgGDS does not mediate GDP/ GTP exchange on DiRas1. Intriguingly, DiRas1 acts similarly to a dominant-negative small GTPase, binding to SmgGDS and inhibiting SmgGDS binding to other small GTPases, including K-Ras4B, RhoA, and Rap1A. DiRas1 is expressed in normal breast tissue, but its expression is decreased in most breast cancers, similar to its family member DiRas3 (ARHI). DiRas1 inhibits RhoA-and Smg-GDS-mediated NF-B transcriptional activity in HEK293T cells. We also report that DiRas1 suppresses basal NF-B activation in breast cancer and glioblastoma cell lines. Taken together, our data support a model in which DiRas1 expression inhibits malignant features of cancers in part by nonproductively binding to SmgGDS and inhibiting the binding of other small GTPases to SmgGDS.

“…Regulation of the prenylation pathway has been largely unexamined, although the recent finding that entry into, and passage through, the prenylation pathway of some small GTPases can be controlled by specific SmgGDS splice variants has highlighted the potential for control of CaaX protein function via this process (28). These recent developments in the prenylation field, coupled with the genetic evidence in plants for demethylation of prenyl proteins (18,19) and our finding of dynamic control of RhoA methylation by CES1, opens new avenues of investigation into the dynamics of prenyl protein processing.…”

Section: Discussionmentioning

confidence: 99%

Control of RhoA Methylation by Carboxylesterase I

Cushman

Potter

et al. 2013

Background: Methylation of Rho proteins by isoprenylcysteine carboxylmethyltransferase impacts their function. Results: RhoA methylation is dynamic and impacted by carboxylesterase 1 activity. Conclusion: Carboxylesterase 1 plays a role in controlling the methylation status and activation of RhoA and impacts cell morphology. Significance: This study demonstrates that C-terminal methylation is under acute control and plays a major role in cell signaling.