RAS subfamily | Enzymes | IUPHAR/BPS Guide to PHARMACOLOGY

GtoPdb is requesting financial support from commercial users. Please see our sustainability page for more information.

RAS subfamily C

Unless otherwise stated all data on this page refer to the human proteins. Gene information is provided for human (Hs), mouse (Mm) and rat (Rn).

Overview

Show »« Hide More detailed introduction go icon to follow link

The RAS proteins (HRAS, NRAS and KRAS) are small membrane-localised G protein-like molecules of 21 kd. They act as an on/off switch linking receptor and non-receptor tyrosine kinase activation to downstream cytoplasmic or nuclear events. Binding of GTP activates the switch, and hydrolysis of the GTP to GDP inactivates the switch.

The RAS proto-oncogenes are the most frequently mutated class of proteins in human cancers. Common mutations compromise the GTP-hydrolysing ability of the proteins causing constitutive activation [5], which leads to increased cell proliferation and decreased apoptosis [10]. Because of their importance in oncogenic transformation these proteins have become the targets of intense drug discovery effort [1].

Enzymes

HRAS Show summary »« Hide summary More detailed page go icon to follow link

Target Id

2822

Nomenclature

HRAS

Previous and unofficial names

Genes

HRAS (Hs), Hras (Mm), Hras (Rn)

Ensembl ID

ENSG00000174775 (Hs), ENSMUSG00000025499 (Mm), ENSRNOG00000016611 (Rn)

UniProtKB AC

P01112 (Hs), Q61411 (Mm), P20171 (Rn)

Inhibitors

lonafarnib pIC₅₀ 8.7 [4]

NRAS Show summary »« Hide summary More detailed page go icon to follow link

Target Id	2823
Nomenclature	NRAS
Previous and unofficial names	N-ras \| neuroblastoma ras oncogene \| neuroblastoma RAS viral (v-ras) oncogene homolog \| neuroblastoma RAS viral oncogene homolog \| NRAS proto-oncogene, GTPase \| NRAS proto-oncogene
Genes	NRAS (Hs), Nras (Mm), Nras (Rn)
Ensembl ID	ENSG00000213281 (Hs), ENSMUSG00000027852 (Mm), ENSRNOG00000023079 (Rn)
UniProtKB AC	P01111 (Hs), P08556 (Mm), Q04970 (Rn)

KRAS Show summary »« Hide summary More detailed page go icon to follow link

Target Id

2824

Nomenclature

KRAS

Previous and unofficial names

Genes

KRAS (Hs), Kras (Mm), Kras (Rn)

Ensembl ID

ENSG00000133703 (Hs), ENSMUSG00000030265 (Mm), ENSRNOG00000009338 (Rn)

UniProtKB AC

P01116 (Hs), P32883 (Mm), P08644 (Rn)

Inhibitors

sotorasib [2]

ARF GTPase 6 Show summary »« Hide summary

Target Id

3324

Nomenclature

ARF GTPase 6

Previous and unofficial names

ADP ribosylation factor 6

Genes

ARF6 (Hs), Arf6 (Mm), Arf6 (Rn)

Ensembl ID

ENSG00000165527 (Hs), ENSMUSG00000044147 (Mm), ENSRNOG00000004791 (Rn)

UniProtKB AC

P62330 (Hs), P62331 (Mm), ARF6_RAT (Rn)

Allosteric modulators

NAV2729 (Inhibition) pIC₅₀ 6.0 [8]

Comment

ARF6 is a RAS superfamily small GTPase that acts as a guanyl ribonucleotide exchange factor. It is involved in signaling pathways that lead to actin remodeling and it regulates vesicular trafficking. Like other RAS GTPases it has oncogenic potential [3,6-7,9,11].

References

Show »« Hide

1. Baines AT, Xu D, Der CJ. (2011) Inhibition of Ras for cancer treatment: the search continues. Future Med Chem, 3 (14): 1787-808. [PMID:22004085]

2. Lanman BA, Allen JR, Allen JG, Amegadzie AK, Ashton KS, Booker SK, Chen JJ, Chen N, Frohn MJ, Goodman G et al.. (2020) Discovery of a Covalent Inhibitor of KRAS^G12C (AMG 510) for the Treatment of Solid Tumors. J Med Chem, 63 (1): 52-65. [PMID:31820981]

3. Li Q, Xie K, Lin B, Gong Y. (2025) TBC1D24 promotes the progression of the breast cancer cells via ARF6/PLD axis under hypoxia. Sci Prog, 108 (3): 368504251367649. [PMID:40790967]

4. Liu M, Bryant MS, Chen J, Lee S, Yaremko B, Lipari P, Malkowski M, Ferrari E, Nielsen L, Prioli N et al.. (1998) Antitumor activity of SCH 66336, an orally bioavailable tricyclic inhibitor of farnesyl protein transferase, in human tumor xenograft models and wap-ras transgenic mice. Cancer Res, 58 (21): 4947-56. [PMID:9810004]

5. Stanley LA. (1995) Molecular aspects of chemical carcinogenesis: the roles of oncogenes and tumour suppressor genes. Toxicology, 96 (3): 173-94. [PMID:7900159]

6. Xu H, Chen D, Lu J, Zhong L, Wang L, Ge J. (2025) ARF6 Promotes AML Progression via Activation of PI3K/AKT/mTOR Signaling. Cancer Med, 14 (9): e70872. [PMID:40275490]

7. Yang Y, Qing L, You C, Li Q, Xu W, Dong Z. (2025) Methuosis key gene ARF6 as a diagnostic, prognostic and immunotherapeutic marker for prostate cancer: based on a comprehensive pan-cancer multi-omics analysis. Discov Oncol, 16 (1): 882. [PMID:40410613]

8. Yoo JH, Shi DS, Grossmann AH, Sorensen LK, Tong Z, Mleynek TM, Rogers A, Zhu W, Richards JR, Winter JM et al.. (2016) ARF6 Is an Actionable Node that Orchestrates Oncogenic GNAQ Signaling in Uveal Melanoma. Cancer Cell, 29 (6): 889-904. [PMID:27265506]

9. Zhang C, Liu Y, Yuan X, Yang X, Yang B, Huang Y, Wang F, He Z, Li Y. (2025) Identification and validation of ARF6 for a potential prognostic biomarker of acute myeloid leukemia. Cancer Cell Int, 25 (1): 218. [PMID:40542378]

10. Zhang J, Lodish HF. (2007) Endogenous K-ras signaling in erythroid differentiation. Cell Cycle, 6 (16): 1970-3. [PMID:17721087]

11. Zhao HG, Cruz-Rodriguez N, Johnson KC, Pomicter AD, Bates B, Bateman B, Haferlach T, Gu T, Ahmann J, Yan D et al.. (2025) The small GTPase ARF6 regulates sphingolipid homeostasis and supports proliferation in acute myeloid leukemia. Haematologica, [Epub ahead of print]. [PMID:40637748]

Citation information

Database page citation (select format):

Concise Guide to PHARMACOLOGY citation:

Alexander SPH, Fabbro D, Kelly E, Mathie AA, Peters JA, Veale EL, Armstrong JF, Faccenda E, Harding SD, Davies JA et al. (2023) The Concise Guide to PHARMACOLOGY 2023/24: Enzymes. Br J Pharmacol. 180 Suppl 2:S289-373.

RAS subfamily C

Overview

Enzymes

Further reading

References

Citation information