Approach for targeting Ras with small molecules that activate SOS-mediated nucleotide exchange

Burns, Michael C.; Sun, Qi; Daniels, R. Nathan; Camper, DeMarco V.; Kennedy, J. Phillip; Phan, Jason; Olejniczak, Edward T.; Lee, Taekyu; Waterson, Alex G.; Rossanese, Olivia W.; Fesik, Stephen W.

doi:10.1073/pnas.1315798111

Cited by 174 publications

(223 citation statements)

References 33 publications

Supporting

Mentioning

204

Contrasting

Order By: Relevance

“…Binding site A corresponds to the site recently reported by Burns, et al 11 The three X-ray crystal structures they describe (4NYI, 4NYJ, 4NYM) show minimal side chain movements in site A compared with the unbound structure of SOS, and correspond most closely with our structures of 1 and 2 in complex with HRas:SOS (Figs. 2a & 2b).…”

Section: Fragment Binding Site a On Sossupporting

confidence: 88%

See 1 more Smart Citation

Small Molecule Binding Sites on the Ras:SOS Complex Can Be Exploited for Inhibition of Ras Activation

et al. 2015

View full text Add to dashboard Cite

Constitutively active mutant KRas displays a reduced rate of GTP hydrolysis via both intrinsic and GTPaseactivating protein-catalysed mechanisms, resulting in the perpetual activation of Ras pathways. We describe a fragment screening campaign using X-ray crystallography that led to the discovery of three fragment binding sites on the Ras:SOS complex. The identification of tool compounds binding at each of these sites allowed exploration of two new approaches to Ras pathway inhibition by stabilising or covalently modifying the Ras:SOS complex to prevent the reloading of Ras with GTP. Initially, we identified ligands that bound reversibly to the Ras:SOS complex in two distinct sites, but these compounds were not sufficiently potent inhibitors to validate our stabilisation hypothesis. We conclude by demonstrating that covalent modification of Cys118 on Ras leads to a novel mechanism of inhibition of the SOS-mediated interaction between Ras and Raf, and is effective at inhibiting the exchange of labelled GDP in both mutant (G12C and G12V) and wild type Ras.

show abstract

Section: Fragment Binding Site a On Sossupporting

confidence: 88%

“…10 Compounds have recently been reported by Burns et al which bind to the Ras:SOS complex and increase the rate of SOS-mediated nucleotide exchange. 11 This is the reverse of the desired effect for an oncology therapy but it is notable that a small molecule can affect this pathway.…”

Section: Introductionmentioning

confidence: 99%

Small Molecule Binding Sites on the Ras:SOS Complex Can Be Exploited for Inhibition of Ras Activation

et al. 2015

View full text Add to dashboard Cite

show abstract

“…In other words, there is no requirement to achieve one specific inactive conformation; there may be many inactive conformations that can be achieved with a range of different inhibitor scaffolds targeting the GN-binding pocket and surrounding regions that will likely have the same inhibitory effect on Ras signaling. We therefore speculate that although binding of SML to K-Ras G12C places the protein in a conformation that is known to be inactive, a number of other approaches may also achieve the goal of impairing Ras signaling (41).…”

Section: Discussionmentioning

confidence: 99%

In situ selectivity profiling and crystal structure of SML-8-73-1, an active site inhibitor of oncogenic K-Ras G12C

Hunter¹,

Gurbani²,

Ficarro

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

205

183

View full text Add to dashboard Cite

Significance SML-8-73-1 (SML) is the first example, to our knowledge, of a GTP-competitive inhibitor of V-Ki-ras2 Kirsten rat sarcoma viral oncogene homolog (K-Ras). A high-resolution structure of K-Ras G12C bound to SML shows K-Ras in an inactive conformation. In situ proteomic-based chemical profiling of SML demonstrates that SML is highly selective for K-Ras G12C over other small GTPases. A novel chemosensor-based assay allows measurement of covalent reaction rates between K-Ras G12C and SML and enables characterization of this reaction in the context of millimolar concentrations of GTP and GDP, well in exccss of what is found in living cells. These results demonstrate that even in the presence of high concentrations of GTP and GDP, SML is able to exchange into the GN site.

show abstract

“…However, the potential of this indole scaffold to serve as as tarting point for fragment growing appears to be limited, as compound 19 was also reported to be an activator of SOS-catalyzed nucleotide exchange (EC 50 = 14 mm). [93] Compound 19 binds to ah ydrophobic pocket formed by the CDC25 domain of SOS and increases cellular Ras-GTP levels in ac oncentration-dependent manner,w hereas no effect on the Ras-specific GEF RasGRF-1 was observed. Further investigation of 19 will be required, as it shows ab iphasic response and decreases AKT and ERK activation downstream of Ras through an unknown mode of action, thereby underlining the complexity of the Ras signaling network.…”

Section: Methodsmentioning

confidence: 99%

Direct Modulation of Small GTPase Activity and Function

et al. 2015

View full text Add to dashboard Cite

Small GTPases are a family of GDP-/GTP-binding proteins that serve as biomolecular switches inside cells to control a variety of essential cellular processes. Aberrant function and regulation of small GTPases is associated with a variety of human diseases, thus rendering these proteins highly interesting targets in drug discovery. However, this class of proteins has been considered "undruggable", as intensive decade-long efforts did not yield clinically relevant direct modulators of small GTPases. Recently, the targeting of small GTPases has gained fresh impetus through the discovery of novel transient cavities on the protein surfaces and the application of new targeting strategies. Besides Ras proteins, other small GTPases have attracted increased attention since improved biological insight in combination with novel targeting strategies identified them as promising targets in drug discovery. This Review gives an overview of relevant aspects of the superfamily of small GTPases and summarizes recent progress and perspectives for the direct modulation of these challenging targets.

show abstract

Approach for targeting Ras with small molecules that activate SOS-mediated nucleotide exchange

Cited by 174 publications

References 33 publications

Small Molecule Binding Sites on the Ras:SOS Complex Can Be Exploited for Inhibition of Ras Activation

Small Molecule Binding Sites on the Ras:SOS Complex Can Be Exploited for Inhibition of Ras Activation

In situ selectivity profiling and crystal structure of SML-8-73-1, an active site inhibitor of oncogenic K-Ras G12C

Direct Modulation of Small GTPase Activity and Function

Contact Info

Product

Resources

About