Drugging the undruggable RAS: Mission Possible?

Cox, Adrienne D.; Fesik, Stephen W.; Kimmelman, Alec C.; Luo, Ji; Der, Channing J.

doi:10.1038/nrd4389

Cited by 1,612 publications

(1,862 citation statements)

References 228 publications

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“…Three publications reported low-frequency KRAS mutations (10-20%) also in pNET (Yuan et al 2014, Vijayvergia et al 2016, Kimura et al 2016. Although targeting RAS directly is a mission impossible (Cox et al 2014), new options arouse from targeting RAS downstream effectors and cell cycle checkpoint control. In NRAS mutant melanomas (Ascierto et al 2016), inhibition of MEK produced a partial response in a subset of patients.…”

Section: Impact Of Genomic Profiling On Therapymentioning

confidence: 99%

WOMEN IN CANCER THEMATIC REVIEW: Systemic therapies in neuroendocrine tumors and novel approaches toward personalized medicine

Pavel¹,

Sers²

2016

Endocrine-Related Cancer

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Neuroendocrine tumors (NETs) are a group of heterogenous neoplasms. Evidencebased treatment options for antiproliferative therapy include somatostatin analogues, the mTOR inhibitor everolimus, the multiple tyrosine kinase inhibitor sunitinib and peptide receptor radionuclide therapy with 177-Lu-octreotate. In the absence of definite predictive markers, therapeutic decision making follows clinical and pathological criteria. As objective response rates with targeted drugs are rather low, and response duration is limited in most patients, numerous combination therapies targeting multiple pathways have been explored in the field. Upfront combination of drugs, however, is associated with increasing toxicity and has shown little benefit. Major advancements in the molecular understanding of NET based on genomic, epigenomic and transcriptomic analysis have been achieved with prognostic and therapeutic impact. New insight into molecular alterations has paved the way to biomarker-driven clinical trials and may facilitate treatment stratification toward personalized medicine in the near future. However, an improved understanding of the complexity of pathway interactions is required for successful treatment. A systems biology approach is one of the tools that may help to achieve this endeavor.

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Section: Impact Of Genomic Profiling On Therapymentioning

confidence: 99%

WOMEN IN CANCER THEMATIC REVIEW: Systemic therapies in neuroendocrine tumors and novel approaches toward personalized medicine

Pavel¹,

Sers²

2016

Endocrine-Related Cancer

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“…However, these drugs failed to increase survival in clinical trials of patients with K-Ras mutated pancreatic cancer (12). N-Ras and K-Ras become substrates for geranylgeranyltransferase I, resulting in alternative prenylation and membrane targeting (9,13). By contrast, H-Ras has no alternative prenylation for membrane targeting.…”

Section: Introductionmentioning

confidence: 99%

Farnesyl transferase inhibitor FTI-277 inhibits breast cell invasion and migration by blocking H-Ras activation

2016

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Abstract. Hyperactive Ras promotes proliferation and malignant phenotypic conversion of cells in cancer. Ras protein must be associated with cellular membranes for its oncogenic activities through post-translational modifications, including farnesylation. Farnesyltransferase (FTase) is essential for H-Ras membrane targeting, and H-Ras, but not N-Ras, has been demonstrated to cause an invasive phenotype in MCF10A breast epithelial cells. In the present study, it was observed that an FTase inhibitor (FTI), FTI-277, blocked epidermal growth factor (EGF)-induced H-Ras activation, but not N-Ras activation in MDA-MB-231 cells, which express wild-type H-Ras and N-Ras. FTI-277 exerted a more potent inhibitory effect on the proliferation of H-Ras-MCF10A cells and Hs578T breast cancer cells expressing an active mutant of H-Ras than that of MDA-MB-231 cells. The invasive/migratory phenotypes of the H-Ras-MCF10A and Hs578T cells were effectively inhibited by FTI-277 treatment. By contrast, FTI-277 did not affect the invasive/migratory phenotypes of MDA-MB-231 cells. However, the EGF-induced invasion of MDA-MB-231 cells was decreased by FTI-277, implicating that FTI-277 inhibits breast cell invasion and migration by blocking H-Ras activation. Taken together, the results of the present study suggest that FTase inhibition by FTI-277 may be an effective strategy for targeting H-Ras-mediated proliferation, migration and invasion of breast cells.

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“…KRAS targeting represents a particularly important opportunity for impacting cancer therapy, given that KRAS mutations are involved in the development of several types of cancers (3). Attempts at targeting point-mutated KRAS have consisted of siRNAs directly targeting this oncogene and associated pathways.…”

Section: Discussionmentioning

confidence: 99%

“…Specifically, Kras, a GTPase protein, is frequently mutated in codon 12 of its coding sequence (CDS) in large fractions of specific human cancer types (2,3). For example, the G12S mutation, in which a single nucleotide modification leads to the substitution of a glycine (Gly) for a serine (Ser), confers constitutive activation of KRAS, inducing cell proliferation (4)(5)(6).…”

mentioning

confidence: 99%

Selective targeting of point-mutated KRAS through artificial microRNAs

Acunzo

Romano

Nigita

et al. 2017

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

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Mutated protein-coding genes drive the molecular pathogenesis of many diseases, including cancer. Specifically, mutated KRAS is a documented driver for malignant transformation, occurring early during the pathogenesis of cancers such as lung and pancreatic adenocarcinomas. Therapeutically, the indiscriminate targeting of wild-type and point-mutated transcripts represents an important limitation. Here, we leveraged on the design of miRNA-like artificial molecules (amiRNAs) to specifically target point-mutated genes, such as KRAS, without affecting their wild-type counterparts. Compared with an siRNA-like approach, the requirement of perfect complementarity of the microRNA seed region to a given target sequence in the microRNA/target model has proven to be a more efficient strategy, accomplishing the selective targeting of point-mutated KRAS in vitro and in vivo

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Drugging the undruggable RAS: Mission Possible?

Cited by 1,612 publications

References 228 publications

WOMEN IN CANCER THEMATIC REVIEW: Systemic therapies in neuroendocrine tumors and novel approaches toward personalized medicine

WOMEN IN CANCER THEMATIC REVIEW: Systemic therapies in neuroendocrine tumors and novel approaches toward personalized medicine

Farnesyl transferase inhibitor FTI-277 inhibits breast cell invasion and migration by blocking H-Ras activation

Selective targeting of point-mutated KRAS through artificial microRNAs

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