A Comprehensive Survey of Ras Mutations in Cancer

Prior, Ian A.; Lewis, Paul D.; Mattos, Carla

doi:10.1158/0008-5472.can-11-2612

Cited by 1,619 publications

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“…Activating mutations occur at codons 12, 13, and 61, which are within the GTPase catalytic domain, in all three RAS isoforms [14] . Approximately 80% of KRAS mutations are found in codon 12, whereas approximately 60% of NRAS mutations are found in codon 61, with 35% in codon 12 [2,14] .…”

Section: Wwwnaturecom/aps Guin S Et Almentioning

confidence: 99%

The RAS-RAL axis in cancer: evidence for mutation-specific selectivity in non-small cell lung cancer

Guin

Theodorescu

2015

Acta Pharmacol Sin

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Activating RAS mutations are common in human tumors. These mutations are often markers for resistance to therapy and subsequent poor prognosis. So far, targeting the RAF-MEK-ERK and PI3K-AKT signaling pathways downstream of RAS is the only promising approach in the treatment of cancer patients harboring RAS mutations. RAL GTPase, another downstream effector of RAS, is also considered as a therapeutic option for the treatment of RAS-mutant cancers. The RAL GTPase family comprises RALA and RALB, which can have either divergent or similar functions in different tumor models. Recent studies on non-small cell lung cancer (NSCLC) have showed that different RAS mutations selectively activate specific effector pathways. This observation requires broader validation in other tumor tissue types, but if true, will provide a new approach to the treatment of RAS-mutant cancer patients by targeting specific downstream RAS effectors according to the type of RAS mutation. It also suggests that RAL GTPase inhibition will be an important treatment strategy for tumors harboring RAS glycine to cysteine (G12C) or glycien to valine (G12V) mutations, which are commonly found in NSCLC and pancreatic cancer. Review RAS GTPase overviewRAS is the most extensively studied GTPase [1] . It is known to regulate various cellular functions, including proliferation, survival, growth, migration, differentiation and cytoskeletal dynamics [2][3][4] (Figure 1). Not coincidentally, increased activities of all of these processes are required by tumor cells to promote tumor growth. Activating oncogenic RAS mutations lead to treatment resistance in various tumor models and poor patient outcomes [3,[5][6][7][8][9] . Three human RAS genes have been identified: HRAS, KRAS, and NRAS [1,2] . These encode the related proteins HRAS, KRAS and NRAS, respectively, of 189 amino acids in length [1,4] . KRAS exists as two isoforms, 4A and 4B, which are generated by alternative exon splicing [10] . These different RAS genes are well known to have differential cellular specificities and intrinsic transforming potentials [3,4,10] .In normal cells, RAS proteins act as molecular switches for critical cellular functions. RAS proteins are activated by upstream receptors such as receptor tyrosine kinases * To whom correspondence should be addressed. E-mail dan.theodorescu@ucdenver.edu Received 2014-08-07 Accepted 2014-10-30 Figure 1. RAS GTPase activation and downstream signaling. The cartoon shows the mechanism of RAS GTPase activation by upstream stimuli and numerous downstream effectors stimulated by activated RAS. RAS regulates critical cellular functions through these effectors. Constitutive RAS activation due to mutations leads to protumorigenic signaling through these effectors.

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Section: Wwwnaturecom/aps Guin S Et Almentioning

confidence: 99%

The RAS-RAL axis in cancer: evidence for mutation-specific selectivity in non-small cell lung cancer

Guin

Theodorescu

2015

Acta Pharmacol Sin

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“…Ras must be membrane bound to promote signal transduction, and altering the normal time scale and details of this interaction dramatically affects signal output, leading to a multitude of disease states, including some of the most aggressive forms of cancers (5). For example, about 60% of pancreatic cancers have a point mutation at residue G12 in K-Ras, whereas about 30% of melanomas are found with mutations at residue Q61 in N-Ras (5).…”

Section: Disease Implications Of the Ras-membrane Interactionmentioning

confidence: 99%

“…K-Ras is by far the most oncogenic isoform, showing extensive prominence in pancreatic and colorectal cancers, while melanomas have a high incidence of N-Ras mutations (5). Codon mutation bias among the isoforms at 100% conserved effector lobe sites indicates that the allosteric features of Ras cannot be ignored.…”

Section: Disease Implications Of the Ras-membrane Interactionmentioning

confidence: 99%

“…Here, many effector and regulator proteins interact with the effector lobe (residues 1-86) of GTP-bound Ras to promote signaling cascades that translate to changes in gene expression, controlling cellular outcomes, such as cell proliferation, differentiation, and apoptosis (4). Point mutations occur most frequently at residue positions 12, 13, and 61, leading to constitutive Ras activation and hyperproliferation traditionally associated with cancer and developmental disorders (5). Although GAPs stimulate GTP hydrolysis by stabilizing both switch regions and inserting a positively charged arginine finger to neutralize negative charges that develop during the transition state of the reaction, oncogenic mutations often promote insensitivity to this regulation (6).…”

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confidence: 99%

“…1). Interestingly, although the effector lobe containing G12, G13, and Q61 is 100% conserved across the three isoforms, an isoform-specific codon mutation profile indicates allosteric lobe influence over oncogenicity (5).…”

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The Ras–Membrane Interface: Isoform-Specific Differences in the Catalytic Domain

Parker

Mattos

2015

Molecular Cancer Research

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The small GTPase Ras is mutated in about 20% of human cancers, primarily at active site amino acid residues G12, G13, and Q61. Thus, structural biology research has focused on the active site, impairment of GTP hydrolysis by oncogenic mutants, and characterization of protein-protein interactions in the effector lobe half of the protein. The C-terminal hypervariable region has increasingly gained attention due to its importance in H-Ras, N-Ras, and K-Ras differences in membrane association. A highresolution molecular view of the Ras-membrane interaction involving the allosteric lobe of the catalytic domain has lagged behind, although evidence suggests that it contributes to isoform specificity. The allosteric lobe has recently gained interest for harboring potential sites for more selective targeting of this elusive "undruggable" protein. The present review reveals critical insight that isoform-specific differences appear prominently at these potentially targetable sites and integrates these differences with knowledge of Ras plasma membrane localization, with the intent to better understand the structure-function relationships needed to design isoform-specific Ras inhibitors. Mol Cancer Res; 13(4); 595-603. Ó2015 AACR.

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Selumetinib Plus Docetaxel Compared With Docetaxel Alone and Progression-Free Survival in Patients With KRAS-Mutant Advanced Non–Small Cell Lung Cancer

Jänne

Heuvel

Barlési

et al. 2017

JAMA

285

205

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A Comprehensive Survey of Ras Mutations in Cancer

Cited by 1,619 publications

References 63 publications

The RAS-RAL axis in cancer: evidence for mutation-specific selectivity in non-small cell lung cancer

The RAS-RAL axis in cancer: evidence for mutation-specific selectivity in non-small cell lung cancer

The Ras–Membrane Interface: Isoform-Specific Differences in the Catalytic Domain

Selumetinib Plus Docetaxel Compared With Docetaxel Alone and Progression-Free Survival in Patients With KRAS-Mutant Advanced Non–Small Cell Lung Cancer

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