Neuroblastoma RAS viral oncogene homolog

NRAS
	Gene ontology
Molecular function	nucleotide binding; protein-containing complex binding; GTP binding; GTPase activity; protein binding;
Cellular component	Golgi apparatus; membrane; Golgi membrane; plasma membrane; extracellular exosome; tertiary granule membrane;
Biological process	epidermal growth factor receptor signaling pathway; stimulatory C-type lectin receptor signaling pathway; MAPK cascade; axon guidance; Fc-epsilon receptor signaling pathway; Ras protein signal transduction; leukocyte migration; signal transduction; ERBB2 signaling pathway; neutrophil degranulation; positive regulation of endothelial cell proliferation;
	Sources:Amigo / QuickGO

Ensembl


ENSG00000213281


ENSMUSG00000027852

UniProt


P01111


P08556

RefSeq (mRNA)


NM_002524


NM_010937 NM_001368638

RefSeq (protein)


NP_002515


n/a

Location (UCSC)

Chr 1: 114.7 – 114.72 Mb

Chr 3: 102.97 – 102.98 Mb

PubMed search

^[3]

^[4]

Wikidata

View/Edit Human

View/Edit Mouse

NRAS is an

Institute of Cancer Research in London.^[5]^[6] It was the third RAS gene to be discovered, and was named NRAS, for its initial identification in human neuroblastoma

cells.

Function

The N-ras proto-oncogene is a member of the

Ras gene family

. It is mapped on chromosome 1, and it is activated in HL60, a promyelocytic leukemia line. The order of nearby genes is as follows: cen—CD2—NGFB—NRAS—tel.

The mammalian Ras gene family consists of the Harvey and Kirsten Ras genes (HRAS and KRAS), an inactive pseudogene of each (c-Hras2 and c-Kras1) and the N-Ras gene. They differ significantly only in the C-terminal 40 amino acids. These Ras genes have GTP/GDP binding and GTPase activity, and their normal function may be as G-like regulatory proteins involved in the normal control of cell growth.

The N-Ras gene specifies two main transcripts of 2 kb and 4.3 kb. The difference between the two transcripts is a simple extension through the termination site of the 2 kb transcript. The N-Ras gene consists of seven exons (-I, I, II, III, IV, V, VI). The smaller 2 kb transcript contains the VIa exon, and the larger 4.3 kb transcript contains the VIb exon which is just a longer form of the VIa exon. Both transcripts encode identical proteins as they differ only the 3′ untranslated region.^[7]

Mutations

Mutations which change amino acid residues 12, 13 or 61 activate the potential of N-ras to transform cultured cells and are implicated in a variety of human tumors^[7] e.g. melanoma.

As a drug target

Binimetinib (MEK162) has had a phase III clinical trial for NRAS Q61 mutant melanoma.^[8]

References

^ ^a ^b ^c GRCh38: Ensembl release 89: ENSG00000213281 – Ensembl, May 2017
^ ^a ^b ^c GRCm38: Ensembl release 89: ENSMUSG00000027852 – Ensembl, May 2017
^ "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
^ "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.
S2CID 4342747
.

PMID 6300838
.

^ ^a ^b "Entrez Gene: NRAS neuroblastoma RAS viral (v-ras) oncogene homolog".

^ Study Comparing the Efficacy of MEK162 Versus Dacarbazine in Unresectable or Metastatic NRAS Mutation-positive Melanoma

Further reading

McCormick F (1996). "Ras-related proteins in signal transduction and growth control". Mol. Reprod. Dev. 42 (4): 500–6.
S2CID 6507743
.

van Elsas A, Scheibenbogen C, van der Minne C, et al. (1998). "UV-induced N-ras mutations are T-cell targets in human melanoma". Melanoma Res. 7 (Suppl 2): S107–13.
S2CID 19219505
.

Dracopoli NC, Meisler MH (1990). "Mapping the human amylase gene cluster on the proximal short arm of chromosome 1 using a highly informative (CA)n repeat" (PDF). Genomics. 7 (1): 97–102.
PMID 1692298
.

Yuasa Y, Kamiyama T, Kato M, et al. (1990). "Transforming genes from familial adenomatous polyposis patient cells detected by a tumorigenicity assay". Oncogene. 5 (4): 589–96.
PMID 1970154
.

Hancock JF, Magee AI, Childs JE, Marshall CJ (1989). "All ras proteins are polyisoprenylated but only some are palmitoylated". Cell. 57 (7): 1167–77.
S2CID 19292550
.

Hall A, Brown R (1985). "Human N-ras: cDNA cloning and gene structure". Nucleic Acids Res. 13 (14): 5255–68.
PMID 2991860
.

Hirai H, Tanaka S, Azuma M, et al. (1986). "Transforming genes in human leukemia cells". Blood. 66 (6): 1371–8.
PMID 2998510
.

Neri A, Knowles DM, Greco A, et al. (1988). "Analysis of RAS oncogene mutations in human lymphoid malignancies". Proc. Natl. Acad. Sci. U.S.A. 85 (23): 9268–72.
PMID 3057505
.

Nitta N, Ochiai M, Nagao M, Sugimura T (1987). "Amino-acid substitution at codon 13 of the N-ras oncogene in rectal cancer in a Japanese patient". Jpn. J. Cancer Res. 78 (1): 21–6.
PMID 3102434
.

Raybaud F, Noguchi T, Marics I, et al. (1988). "Detection of a low frequency of activated ras genes in human melanomas using a tumorigenicity assay". Cancer Res. 48 (4): 950–3.
PMID 3276402
.

Hirai H, Kobayashi Y, Mano H, et al. (1987). "A point mutation at codon 13 of the N-ras oncogene in myelodysplastic syndrome". Nature. 327 (6121): 430–2.
S2CID 4270769
.

Gambke C, Hall A, Moroni C (1985). "Activation of an N-ras gene in acute myeloblastic leukemia through somatic mutation in the first exon". Proc. Natl. Acad. Sci. U.S.A. 82 (3): 879–82.
PMID 3856237
.

Padua RA, Barrass NC, Currie GA (1985). "Activation of N-ras in a human melanoma cell line". Mol. Cell. Biol. 5 (3): 582–5.
PMID 3887133
.

Brown R, Marshall CJ, Pennie SG, Hall A (1984). "Mechanism of activation of an N-ras gene in the human fibrosarcoma cell line HT1080". EMBO J. 3 (6): 1321–6.
PMID 6086315
.

Yuasa Y, Gol RA, Chang A, et al. (1984). "Mechanism of activation of an N-ras oncogene of SW-1271 human lung carcinoma cells". Proc. Natl. Acad. Sci. U.S.A. 81 (12): 3670–4.
PMID 6587382
.

Taparowsky E, Shimizu K, Goldfarb M, Wigler M (1983). "Structure and activation of the human N-ras gene". Cell. 34 (2): 581–6.
S2CID 39787991
.

Mitchell EL, Jones D, White GR, et al. (1995). "Determination of the gene order of the three loci CD2, NGFB, and NRAS at human chromosome band 1p13 and refinement of their localisation at the subband level by fluorescence in situ hybridisation". Cytogenet. Cell Genet. 70 (3–4): 183–5.
PMID 7789166
.

Kodaki T, Woscholski R, Hallberg B, et al. (1995). "The activation of phosphatidylinositol 3-kinase by Ras". Curr. Biol. 4 (9): 798–806.
S2CID 20836474
.

Rodriguez-Viciana P, Warne PH, Vanhaesebroeck B, et al. (1996). "Activation of phosphoinositide 3-kinase by interaction with Ras and by point mutation". EMBO J. 15 (10): 2442–51.
PMID 8665852
.

External links

GeneReviews/NCBI/NIH/UW entry on Noonan syndrome

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PDB gallery

121p: STRUKTUR UND GUANOSINTRIPHOSPHAT-HYDROLYSEMECHANISMUS DES C-TERMINAL VERKUERZTEN MENSCHLICHEN KREBSPROTEINS P21-H-RAS

1aa9: HUMAN C-HA-RAS(1-171)(DOT)GDP, NMR, MINIMIZED AVERAGE STRUCTURE

1agp: THREE-DIMENSIONAL STRUCTURES AND PROPERTIES OF A TRANSFORMING AND A NONTRANSFORMING GLY-12 MUTANT OF P21-H-RAS

1bkd: COMPLEX OF HUMAN H-RAS WITH HUMAN SOS-1

1clu: H-RAS COMPLEXED WITH DIAMINOBENZOPHENONE-BETA,GAMMA-IMIDO-GTP

1crp: THE SOLUTION STRUCTURE AND DYNAMICS OF RAS P21. GDP DETERMINED BY HETERONUCLEAR THREE AND FOUR DIMENSIONAL NMR SPECTROSCOPY

1crq: THE SOLUTION STRUCTURE AND DYNAMICS OF RAS P21. GDP DETERMINED BY HETERONUCLEAR THREE AND FOUR DIMENSIONAL NMR SPECTROSCOPY

1crr: THE SOLUTION STRUCTURE AND DYNAMICS OF RAS P21. GDP DETERMINED BY HETERONUCLEAR THREE AND FOUR DIMENSIONAL NMR SPECTROSCOPY

1ctq: STRUCTURE OF P21RAS IN COMPLEX WITH GPPNHP AT 100 K

1gnp: X-RAY CRYSTAL STRUCTURE ANALYSIS OF THE CATALYTIC DOMAIN OF THE ONCOGENE PRODUCT P21H-RAS COMPLEXED WITH CAGED GTP AND MANT DGPPNHP

1gnq: X-RAY CRYSTAL STRUCTURE ANALYSIS OF THE CATALYTIC DOMAIN OF THE ONCOGENE PRODUCT P21H-RAS COMPLEXED WITH CAGED GTP AND MANT DGPPNHP

1gnr: X-RAY CRYSTAL STRUCTURE ANALYSIS OF THE CATALYTIC DOMAIN OF THE ONCOGENE PRODUCT P21H-RAS COMPLEXED WITH CAGED GTP AND MANT DGPPNHP

1he8: RAS G12V - PI 3-KINASE GAMMA COMPLEX

1iaq: C-H-RAS P21 PROTEIN MUTANT WITH THR 35 REPLACED BY SER (T35S) COMPLEXED WITH GUANOSINE-5'-[B,G-IMIDO] TRIPHOSPHATE

1ioz: Crystal Structure of the C-HA-RAS Protein Prepared by the Cell-Free Synthesis

1jah: H-RAS P21 PROTEIN MUTANT G12P, COMPLEXED WITH GUANOSINE-5'-[BETA,GAMMA-METHYLENE] TRIPHOSPHATE AND MAGNESIUM

1jai: H-RAS P21 PROTEIN MUTANT G12P, COMPLEXED WITH GUANOSINE-5'-[BETA,GAMMA-METHYLENE] TRIPHOSPHATE AND MANGANESE

1k8r: Crystal structure of Ras-Bry2RBD complex

1lf0: Crystal Structure of RasA59G in the GTP-bound form

1lf5: Crystal Structure of RasA59G in the GDP-bound Form

1lfd: CRYSTAL STRUCTURE OF THE ACTIVE RAS PROTEIN COMPLEXED WITH THE RAS-INTERACTING DOMAIN OF RALGDS

1nvu: Structural evidence for feedback activation by RasGTP of the Ras-specific nucleotide exchange factor SOS

1nvv: Structural evidence for feedback activation by RasGTP of the Ras-specific nucleotide exchange factor SOS

1nvw: Structural evidence for feedback activation by RasGTP of the Ras-specific nucleotide exchange factor SOS

1nvx: Structural evidence for feedback activation by RasGTP of the Ras-specific nucleotide exchange factor SOS

1p2s: H-Ras 166 in 50% 2,2,2 triflouroethanol

1p2t: H-Ras 166 in Aqueous mother liquor, RT

1p2u: H-Ras in 50% isopropanol

1p2v: H-RAS 166 in 60 % 1,6 hexanediol

1plj: CRYSTALLOGRAPHIC STUDIES ON P21H-RAS USING SYNCHROTRON LAUE METHOD: IMPROVEMENT OF CRYSTAL QUALITY AND MONITORING OF THE GTPASE REACTION AT DIFFERENT TIME POINTS

1plk: CRYSTALLOGRAPHIC STUDIES ON P21H-RAS USING SYNCHROTRON LAUE METHOD: IMPROVEMENT OF CRYSTAL QUALITY AND MONITORING OF THE GTPASE REACTION AT DIFFERENT TIME POINTS

1pll: CRYSTALLOGRAPHIC STUDIES ON P21H-RAS USING SYNCHROTRON LAUE METHOD: IMPROVEMENT OF CRYSTAL QUALITY AND MONITORING OF THE GTPASE REACTION AT DIFFERENT TIME POINTS

1q21: CRYSTAL STRUCTURES AT 2.2 ANGSTROMS RESOLUTION OF THE CATALYTIC DOMAINS OF NORMAL RAS PROTEIN AND AN ONCOGENIC MUTANT COMPLEXED WITH GSP

1qra: STRUCTURE OF P21RAS IN COMPLEX WITH GTP AT 100 K

1rvd: H-RAS COMPLEXED WITH DIAMINOBENZOPHENONE-BETA,GAMMA-IMIDO-GTP

1wq1: RAS-RASGAP COMPLEX

1xcm: Crystal structure of the GppNHp-bound H-Ras G60A mutant

1xd2: Crystal Structure of a ternary Ras:SOS:Ras*GDP complex

1xj0: Crystal Structure of the GDP-bound form of the RasG60A mutant

1zvq: Structure of the Q61G mutant of Ras in the GDP-bound form

1zw6: Crystal Structure of the GTP-bound form of RasQ61G

221p: THREE-DIMENSIONAL STRUCTURES OF H-RAS P21 MUTANTS: MOLECULAR BASIS FOR THEIR INABILITY TO FUNCTION AS SIGNAL SWITCH MOLECULES

2c5l: STRUCTURE OF PLC EPSILON RAS ASSOCIATION DOMAIN WITH HRAS

2ce2: CRYSTAL STRUCTURE ANALYSIS OF A FLUORESCENT FORM OF H-RAS P21 IN COMPLEX WITH GDP

2cl0: CRYSTAL STRUCTURE ANALYSIS OF A FLUORESCENT FORM OF H-RAS P21 IN COMPLEX WITH GPPNHP

2cl6: CRYSTAL STRUCTURE ANALYSIS OF A FLUORESCENT FORM OF H-RAS P21 IN COMPLEX WITH S-CAGED GTP

2cl7: CRYSTAL STRUCTURE ANALYSIS OF A FLUORESCENT FORM OF H-RAS P21 IN COMPLEX WITH GTP

2clc: CRYSTAL STRUCTURE ANALYSIS OF A FLUORESCENT FORM OF H-RAS P21 IN COMPLEX WITH GTP (2)

2cld: CRYSTAL STRUCTURE ANALYSIS OF A FLUORESCENT FORM OF H-RAS P21 IN COMPLEX WITH GDP (2)

2evw: Crystal structure analysis of a fluorescent form of H-Ras p21 in complex with R-caged GTP

421p: THREE-DIMENSIONAL STRUCTURES OF H-RAS P21 MUTANTS: MOLECULAR BASIS FOR THEIR INABILITY TO FUNCTION AS SIGNAL SWITCH MOLECULES

521p: THREE-DIMENSIONAL STRUCTURES OF H-RAS P21 MUTANTS: MOLECULAR BASIS FOR THEIR INABILITY TO FUNCTION AS SIGNAL SWITCH MOLECULES

5p21: REFINED CRYSTAL STRUCTURE OF THE TRIPHOSPHATE CONFORMATION OF H-RAS P21 AT 1.35 ANGSTROMS RESOLUTION: IMPLICATIONS FOR THE MECHANISM OF GTP HYDROLYSIS

621p: THREE-DIMENSIONAL STRUCTURES OF H-RAS P21 MUTANTS: MOLECULAR BASIS FOR THEIR INABILITY TO FUNCTION AS SIGNAL SWITCH MOLECULES

6q21: MOLECULAR SWITCH FOR SIGNAL TRANSDUCTION: STRUCTURAL DIFFERENCES BETWEEN ACTIVE AND INACTIVE FORMS OF PROTOONCOGENIC RAS PROTEINS

721p: THREE-DIMENSIONAL STRUCTURES OF H-RAS P21 MUTANTS: MOLECULAR BASIS FOR THEIR INABILITY TO FUNCTION AS SIGNAL SWITCH MOLECULES

821p: THREE-DIMENSIONAL STRUCTURES AND PROPERTIES OF A TRANSFORMING AND A NONTRANSFORMING GLYCINE-12 MUTANT OF P21H-RAS

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Hydrolases: acid anhydride hydrolases (EC 3.6)
3.6.1

Pyrophosphatase
Inorganic

Thiamine

Apyrase

Thiamine-triphosphatase

3.6.2

Adenylylsulfatase

Phosphoadenylylsulfatase

3.6.3-4: ATPase
3.6.3
Cu++ (3.6.3.4)

Menkes/ATP7A

Wilson/ATP7B

Ca+ (3.6.3.8)

SERCA
ATP2A1

ATP2A2

ATP2A3

Plasma membrane
ATP2B1

ATP2B2

ATP2B3

ATP2B4

SPCA
ATP2C1

ATP2C2

Na+/K+
(3.6.3.9)

ATP1A1

ATP1A2

ATP1A3

ATP1A4

ATP1B1

ATP1B2

ATP1B3

ATP1B4

H+/K+ (3.6.3.10)

ATP4A

Other P-type ATPase

ATP8B1

ATP10A

ATP11B

ATP12A

ATP13A2

ATP13A3

3.6.4

Dynein

Kinesin

Myosin

Katanin

3.6.5: GTPase
3.6.5.1: Heterotrimeric G protein

G_αs
G_olf

G_αi
GNAI1

GNAI2

GNAI3

Transducin
GNAT1

GNAT2

Gustducin
GNAT3

G_αq/11
GNAQ

GNA11

G_α12/13
GNA12

GNA13

3.6.5.2: Small GTPase > Ras superfamily

Rho family of GTPases: Cdc42
CDC42

TC10

TCL

RhoUV
RhoU

RhoV

Rac
Rac1

2

3

RhoG

RhoBTB
1

2

RhoH

Rho
A

B

C

Rnd
1

2

3

RhoDF
RhoF

RhoD

other:
Ras

HRAS

KRAS

NRAS

Rab
RAB23

RAB27

Arf
ARF6

SAR1B

ARL13B

ARL6

Ran

Rheb

Rap

RGK

3.6.5.3: Protein-synthesizing GTPase

Prokaryotic

IF-2

EF-Tu

EF-G

Eukaryotic

3.6.5.5-6: Polymerization motors

dynamin superfamily
Dynamin

Guanylate-binding protein

Mitofusin-1

MX1 and MX2

OPA1

Tubulin

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Retrieved from "https://en.wikipedia.org/w/index.php?title=Neuroblastoma_RAS_viral_oncogene_homolog&oldid=1191281881"

[refGRCh38Ensembl-1] GRCh38: Ensembl release 89: ENSG00000213281 – Ensembl, May 2017

[refGRCm38Ensembl-2] GRCm38: Ensembl release 89: ENSMUSG00000027852 – Ensembl, May 2017

[3] "Human PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.

[4] "Mouse PubMed Reference:". National Center for Biotechnology Information, U.S. National Library of Medicine.

[pmid6287287-5] S2CID 4342747
.

[pmid6300838-6] PMID 6300838
.

[entrez-7] "Entrez Gene: NRAS neuroblastoma RAS viral (v-ras) oncogene homolog".

[NCT01763164-8] Study Comparing the Efficacy of MEK162 Versus Dacarbazine in Unresectable or Metastatic NRAS Mutation-positive Melanoma

[3]

[4]

[5]

[6]

[7]

[8]