The role of Rac in tumor susceptibility and disease progression: from biochemistry to the clinic

Casado‐Medrano, Victoria; Baker, Martin J.; López‐Haber, Cynthia; Cooke, Mariana; Wang, Shaofei; Caloca, María J.; Kazanietz, Marcelo G.

doi:10.1042/bst20170519

Cited by 28 publications

(29 citation statements)

References 106 publications

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“…P-Rex1 is activated by human epidermal growth factor receptor (HER2) and GPCRs, such as the chemokine receptor CXCR4 in breast cancer, and overexpressed in ER and HER2 positive luminal A and B breast cancer tissues compared to normal breast tissue. P-Rex1 expression was actually low in triple-negative primary tumors but was upregulated in distant metastases (Marotti et al, 2017;Casado-Medrano et al, 2018;Kazanietz et al, 2018). Furthermore, demethylation in the PREX promoter has been associated with breast cancer mortality (Montero et al, 2011).…”

Section: Targeting Vav1/2/3mentioning

confidence: 99%

“…The pivotal role of Rac and Cdc42 in multiple cancers has been extensively reviewed by us and others (Pai et al, 2010;Mack et al, 2011;Stengel and Zheng, 2011;Wertheimer et al, 2012;Bid et al, 2013;Kazanietz and Caloca, 2017;Casado-Medrano et al, 2018;Maldonado and Dharmawardhane, 2018;De et al, 2019). In addition, the related Rho GTPase Rho has also been implicated in tumorigenesis and cancer progression.…”

Section: Introductionmentioning

confidence: 99%

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Targeting Rac and Cdc42 GEFs in Metastatic Cancer

Maldonado

Medina

Velázquez

et al. 2020

Front. Cell Dev. Biol.

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The Rho family GTPases Rho, Rac, and Cdc42 have emerged as key players in cancer metastasis, due to their essential roles in regulating cell division and actin cytoskeletal rearrangements; and thus, cell growth, migration/invasion, polarity, and adhesion. This review will focus on the close homologs Rac and Cdc42, which have been established as drivers of metastasis and therapy resistance in multiple cancer types. Rac and Cdc42 are often dysregulated in cancer due to hyperactivation by guanine nucleotide exchange factors (GEFs), belonging to both the diffuse B-cell lymphoma (Dbl) and dedicator of cytokinesis (DOCK) families. Rac/Cdc42 GEFs are activated by a myriad of oncogenic cell surface receptors, such as growth factor receptors, G-protein coupled receptors, cytokine receptors, and integrins; consequently, a number of Rac/Cdc42 GEFs have been implicated in metastatic cancer. Hence, inhibiting GEF-mediated Rac/Cdc42 activation represents a promising strategy for targeted metastatic cancer therapy. Herein, we focus on the role of oncogenic Rac/Cdc42 GEFs and discuss the recent advancements in the development of Rac and Cdc42 GEF-interacting inhibitors as targeted therapy for metastatic cancer, as well as their potential for overcoming cancer therapy resistance.

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Section: Targeting Vav1/2/3mentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Targeting Rac and Cdc42 GEFs in Metastatic Cancer

Maldonado

Medina

Velázquez

et al. 2020

Front. Cell Dev. Biol.

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“…In summary, our work identified Rac1 and Cdc42 hyperactivation in aggressive androgen-insensitive DU145 and PC3 prostate cancer cell lines. These proteins and their regulators are known to play important roles in the progression of cancer and are therefore of interest as potential therapeutic targets [3]. We have also demonstrated that targeting P-Rex1, a previously identified therapeutic target candidate, is unlikely to have an impact on Rac1 activation status, migration or invasion in prostate cancer cells.…”

Section: Discussionmentioning

confidence: 67%

“…One is that multiple GEFs are required for maintaining Rac1-GTP and Cdc42-GTP in these cells, and thus silencing single GEFs is insufficient to cause an effect. We cannot rule out that a Rac-GEF not included in our screen could be involved, albeit a less likely possibility because our analysis encompasses the majority of known Rac-GEFs [3]. However, it is quite remarkable that no Dbl or DOCK family GEFs were identified in our proteomics analysis using a nucleotide free Rac1 bait, which is designed to pull-down Rac1 associated GEFs.…”

Section: Discussionmentioning

confidence: 97%

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P-REX1-Independent, Calcium-Dependent RAC1 Hyperactivation in Prostate Cancer

Baker

Abba

Garcı́a-Mata

et al. 2020

Cancers

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The GTPase Rac1 is a well-established master regulator of cell motility and invasiveness contributing to cancer metastasis. Dysregulation of the Rac1 signaling pathway, resulting in elevated motile and invasive potential, has been reported in multiple cancers. However, there are limited studies on the regulation of Rac1 in prostate cancer. Here, we demonstrate that aggressive androgen-independent prostate cancer cells display marked hyperactivation of Rac1. This hyperactivation is independent of P-Rex1 activity or its direct activators, the PI3K product PIP3 and Gβγ subunits. Furthermore, we demonstrate that the motility and invasiveness of PC3 prostate cancer cells is independent of P-Rex1, supporting the analysis of publicly available datasets indicating no correlation between high P-Rex1 expression and cancer progression in patients. Rac1 hyperactivation was not related to the presence of activating Rac1 mutations and was insensitive to overexpression of a Rac-GAP or the silencing of specific Rac-GEFs expressed in prostate cancer cells. Interestingly, active Rac1 levels in these cells were markedly reduced by elevations in intracellular calcium or by serum stimulation, suggesting the presence of an alternative means of Rac1 regulation in prostate cancer that does not involve previously established paradigms.

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Development of an Improved Guanidine‐Based Rac1 Inhibitor with in vivo Activity against Non‐Small Cell Lung Cancer

et al. 2021

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The Rho GTPase Rac1 is involved in the control of cytoskeleton reorganization and other fundamental cellular functions. Aberrant activity of Rac1 and its regulators is common in human cancer. In particular, deregulated expression/activity of Rac GEFs, responsible for Rac1 activation, has been associated to a metastatic phenotype and drug resistance. Thus, the development of novel Rac1‐GEF interaction inhibitors is a promising strategy for finding new preclinical candidates. Here, we studied structure–activity relationships within a new family of N,N’‐disubstituted guanidine as Rac1 inhibitors. We found that compound 1D‐142, presents superior antiproliferative activity in human cancer cell lines and higher potency as Rac1‐GEF interaction inhibitor in vitro than parental compounds. In addition, 1D‐142 reduces Rac1‐mediated TNFα‐induced NF‐κB nuclear translocation during cell proliferation and migration in NSCLC. Notably, 1D‐142 allowed us to show for the first time the application of a Rac1 inhibitor in a lung cancer animal model.

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The role of Rac in tumor susceptibility and disease progression: from biochemistry to the clinic

Cited by 28 publications

References 106 publications

Targeting Rac and Cdc42 GEFs in Metastatic Cancer

Targeting Rac and Cdc42 GEFs in Metastatic Cancer

P-REX1-Independent, Calcium-Dependent RAC1 Hyperactivation in Prostate Cancer

Development of an Improved Guanidine‐Based Rac1 Inhibitor with in vivo Activity against Non‐Small Cell Lung Cancer

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