RET proto-oncogene

Ret proto-oncogene

Crystallographic structure of the dimeric tyrosine kinase domain of the human proto-oncogene Ret (rainbow colored cartoon, N-terminus = blue, C-terminus = red).[1]
Identifiers
Symbols RET; PTC; CDHF12; HSCR1; MEN2A; MEN2B; MTC1; RET-ELE1; RET51
External IDs OMIM164761 MGI97902 HomoloGene7517 GeneCards: RET Gene
RNA expression pattern
More reference expression data
Orthologs
Species Human Mouse
Entrez 5979 19713
Ensembl ENSG00000165731 ENSMUSG00000030110
UniProt P07949 P35546
RefSeq (mRNA) NM_020630 NM_001080780
RefSeq (protein) NP_065681 NP_001074249
Location (UCSC) Chr 10:
42.89 – 42.95 Mb
Chr 6:
118.12 – 118.16 Mb
PubMed search [1] [2]

The RET proto-oncogene encodes a receptor tyrosine kinase for members of the glial cell line-derived neurotrophic factor family of extracellular signalling molecules.[2] RET loss of function mutations are associated with the development of Hirschsprung's disease, while gain of function mutations are associated with the development of various types of human cancer, including medullary thyroid carcinoma, multiple endocrine neoplasias type 2A and 2B, phaeochromocytoma and parathyroid hyperplasia.

Contents

Structure

RET is an abbreviation for "rearranged during transfection", as the DNA sequence of this gene was originally found to be rearranged within a 3T3 fibroblast cell line following its transfection with DNA taken from human lymphoma cells.[3] The human gene RET is localized to chromosome 10 (10q11.2) and contains 21 exons.[4]

The natural alternative splicing of the RET gene results in the production of 3 different isoforms of the protein RET. RET51, RET43 and RET9 contain 51, 43 and 9 amino acids in their C-terminal tail respectively.[5] The biological roles of isoforms RET51 and RET9 are the most well studied in-vivo as these are the most common isoforms in which RET occurs.

Common to each isoform is a domain structure. Each protein is divided into three domains: an N-terminal extracellular domain with four cadherin-like repeats and a cysteine-rich region, a hydrophobic transmembrane domain and a cytoplasmic tyrosine kinase domain, which is split by an insertion of 27 amino acids. Within the cytoplasmic tyrosine kinase domain, there are 16 tyrosines (Tyrs) in RET9 and 18 in RET51. Tyr1090 and Tyr1096 are present only in the RET51 isoform.[6]

The extracellular domain of RET contains nine N-glycosylation sites. The fully glycosylated RET protein is reported to have a molecular weight of 170 kDa although it is not clear to which isoform this molecular weight relates.[7]

Kinase activation

RET is the receptor for members of the glial cell line-derived neurotrophic factor (GDNF) family of extracellular signalling molecules or ligands (GFLs).[8]

In order to activate RET GFLs first need to form a complex with a glycosylphosphatidylinositol (GPI)-anchored co-receptor. The co-receptors themselves are classified as members of the GDNF receptor-α (GFRα) protein family. Different members of the GFRα family (GFRα1-GFRα4) exhibit a specific binding activity for a specific GFLs.[9] Upon GFL-GFRα complex formation, the complex then brings together two molecules of RET, triggering trans-autophosphorylation of specific tyrosine residues within the tyrosine kinase domain of each RET molecule. Tyr900 and Tyr905 within the activation loop (A-loop) of the kinase domain have been shown to be autophosphorylation sites by mass spectrometry.[10] Phosphorylation of Tyr905 stabilizes the active conformation of the kinase, which, in turn, results in the autophosphorylation of other tyrosine residues mainly located in the C-terminal tail region of the molecule.[6]

The structure shown to the left was taken from the protein data bank code 2IVT.[2] The structure is that of a dimer formed between two protein molecules each spanning from amino acids 703-1012 of the RET molecule, covering RETs intracellular tyrosine kinase domain. One protein molecule, molecule A is shown in yellow and the other, molecule B in grey. The activation loop is coloured purple and selected tyrosine residues in green. Part of the activation loop from molecule B is absent.

Phosphorylation of Tyr981 and the additional tyrosines Tyr1015, Tyr1062 and Tyr1096 not covered by the above structure, have been shown to be important to the initiation of intracellular signal transduction processes.

Role of RET signalling during development

Mice deficient in GDNF, GFRα1 or the RET protein itself exhibit severe defects in kidney and enteric nervous system development. This implicates RET signal transduction as key to the development of normal kidneys and the enteric nervous system.[6]

Clinical relevance

Activating point mutations in RET can give rise to the hereditary cancer syndrome known as multiple endocrine neoplasia type 2 (MEN 2).[11] There are three subtypes based on clinical presentation: MEN 2A, MEN 2B, and familial medullary thyroid carcinoma (FMTC).[12] There is a high degree of correlation between the position of the point mutation and the phenotype of the disease.

Chromosomal rearrangements that generate a fusion gene resulting in the juxtaposition of the C-terminal region of the RET protein with an N-terminal portion of another protein, can also lead to constitutive activation of the RET kinase. These types of mutations are associated with papillary thyroid carcinoma (PTC), and the fusion oncoproteins generated are termed RET/PTC proteins.

Disease Database

RET gene variant database

Interactions

RET proto-oncogene has been shown to interact with GRB10,[13] STAT3,[14][15][16] DOK5,[17][18] Grb2,[19][13] GRB7,[20] DOK1,[21] SHC1[22][19] and GDNF family receptor alpha 1.[23][24]

References

  1. ^ PDB 2ivs; Knowles PP, Murray-Rust J, Kjaer S, Scott RP, Hanrahan S, Santoro M, Ibáñez CF, McDonald NQ (November 2006). "Structure and chemical inhibition of the RET tyrosine kinase domain". J. Biol. Chem. 281 (44): 33577–87. doi:10.1074/jbc.M605604200. PMID 16928683. 
  2. ^ a b Knowles PP, Murray-Rust J. et al. (2006). "Structure and chemical inhibition of the RET tyrosine kinase domain". J. Biol. Chem. 281 (44): 33577–87. doi:10.1074/jbc.M605604200. PMID 16928683. 
  3. ^ Takahashi M, Ritz J, Cooper GM. (1985). "Activation of a novel human transforming gene, ret, by DNA rearrangement.". Cell 42 (2): 581–8. doi:10.1016/0092-8674(85)90115-1. PMID 2992805. 
  4. ^ Ceccherini I, Bocciardi R. et al. (1993). "Exon structure and flanking intronic sequences of the human RET proto-oncogene". Biochem. Biophys. Res. Commun. 196 (3): 1288–1295. doi:10.1006/bbrc.1993.2392. PMID 7902707. 
  5. ^ Myers SM, Eng C. et al. (1995). "Characterization of RET proto-oncogene 3' splicing variants and polyadenylation sites: a novel C-terminus for RET". Oncogene 11 (10): 2039–2045. PMID 7478523. 
  6. ^ a b c Arighi E, Borrello MG, Sariola H. (2005). "RET tyrosine kinase signaling in development and cancer". Cytokine Growth Factor Rev. 16 (4–5): 441–67. doi:10.1016/j.cytogfr.2005.05.010. PMID 15982921. 
  7. ^ Takahashi M, Asai N. et al. (1993). "Characterization of the ret proto-oncogene products expressed in mouse L cells". Oncogene 8 (11): 2925–2929. PMID 8414495. 
  8. ^ Baloh RH, Enomoto H. et al. (2000). "The GDNF family ligands and receptors - implications for neural development". Curr. Opin. Neurobiol. 10 (1): 103–10. doi:10.1016/S0959-4388(99)00048-3. PMID 10679429. 
  9. ^ Airaksinen MS, Titievsky A, Saarma M. (1999). "GDNF family neurotrophic factor signaling: four masters, one servant?". Mol. Cell Neurosci. 13 (5): 313–25. doi:10.1006/mcne.1999.0754. PMID 10356294. 
  10. ^ Kawamoto Y, Takeda K. et al. (2004). "Identification of RET autophosphorylation sites by mass spectrometry". J. Biol. Chem. 279 (14): 14213–24. doi:10.1074/jbc.M312600200. PMID 14711813. 
  11. ^ Online 'Mendelian Inheritance in Man' (OMIM) MULTIPLE ENDOCRINE NEOPLASIA, TYPE IIA; MEN2A -171400
  12. ^ Qi XP, Ma JM, Du ZF, Ying RB, Fei J, Jin HY, Han JS, Wang JQ, Chen XL, Chen CY, Liu WT, Lu JJ, Zhang JG, Zhang XN (2011). "RET germline mutations identified by exome sequencing in a Chinese multiple endocrine neoplasia type 2A/familial medullary thyroid carcinoma family". PLoS ONE 6 (5): e20353. doi:10.1371/journal.pone.0020353. PMC 3105051. PMID 21655256. http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pmcentrez&artid=3105051. 
  13. ^ a b Pandey, A; Duan H, Di Fiore P P, Dixit V M (Sep. 1995). "The Ret receptor protein tyrosine kinase associates with the SH2-containing adapter protein Grb10". J. Biol. Chem. (UNITED STATES) 270 (37): 21461–3. doi:10.1074/jbc.270.37.21461. ISSN 0021-9258. PMID 7665556. 
  14. ^ Yuan, Zheng-Long; Guan Ying-Jie, Wang Lijuan, Wei Wenyi, Kane Agnes B, Chin Y Eugene (Nov. 2004). "Central role of the threonine residue within the p+1 loop of receptor tyrosine kinase in STAT3 constitutive phosphorylation in metastatic cancer cells". Mol. Cell. Biol. (United States) 24 (21): 9390–400. doi:10.1128/MCB.24.21.9390-9400.2004. ISSN 0270-7306. PMC 522220. PMID 15485908. http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pmcentrez&artid=522220. 
  15. ^ Hwang, Jung Hwan; Kim Dong Wook, Suh Jae Mi, Kim Ho, Song Jung Hun, Hwang Eun Suk, Park Ki Cheol, Chung Hyo Kyun, Kim Jin Man, Lee Tae-Hoon, Yu Dae-Yeul, Shong Minho (Jun. 2003). "Activation of signal transducer and activator of transcription 3 by oncogenic RET/PTC (rearranged in transformation/papillary thyroid carcinoma) tyrosine kinase: roles in specific gene regulation and cellular transformation". Mol. Endocrinol. (United States) 17 (6): 1155–66. doi:10.1210/me.2002-0401. ISSN 0888-8809. PMID 12637586. 
  16. ^ Schuringa, J J; Wojtachnio K, Hagens W, Vellenga E, Buys C H, Hofstra R, Kruijer W (Aug. 2001). "MEN2A-RET-induced cellular transformation by activation of STAT3". Oncogene (England) 20 (38): 5350–8. doi:10.1038/sj.onc.1204715. ISSN 0950-9232. PMID 11536047. 
  17. ^ Crowder, Robert J; Enomoto Hideki, Yang Mao, Johnson Eugene M, Milbrandt Jeffrey (Oct. 2004). "Dok-6, a Novel p62 Dok family member, promotes Ret-mediated neurite outgrowth". J. Biol. Chem. (United States) 279 (40): 42072–81. doi:10.1074/jbc.M403726200. ISSN 0021-9258. PMID 15286081. 
  18. ^ Grimm, J; Sachs M, Britsch S, Di Cesare S, Schwarz-Romond T, Alitalo K, Birchmeier W (Jul. 2001). "Novel p62dok family members, dok-4 and dok-5, are substrates of the c-Ret receptor tyrosine kinase and mediate neuronal differentiation". J. Cell Biol. (United States) 154 (2): 345–54. doi:10.1083/jcb.200102032. ISSN 0021-9525. PMC 2150770. PMID 11470823. http://www.pubmedcentral.nih.gov/articlerender.fcgi?tool=pmcentrez&artid=2150770. 
  19. ^ a b Borrello, M G; Pelicci G, Arighi E, De Filippis L, Greco A, Bongarzone I, Rizzetti M, Pelicci P G, Pierotti M A (Jun. 1994). "The oncogenic versions of the Ret and Trk tyrosine kinases bind Shc and Grb2 adaptor proteins". Oncogene (ENGLAND) 9 (6): 1661–8. ISSN 0950-9232. PMID 8183561. 
  20. ^ Pandey, A; Liu X, Dixon J E, Di Fiore P P, Dixit V M (May. 1996). "Direct association between the Ret receptor tyrosine kinase and the Src homology 2-containing adapter protein Grb7". J. Biol. Chem. (UNITED STATES) 271 (18): 10607–10. doi:10.1074/jbc.271.18.10607. ISSN 0021-9258. PMID 8631863. 
  21. ^ Murakami, Hideki; Yamamura Yumiko, Shimono Yohei, Kawai Kumi, Kurokawa Kei, Takahashi Masahide (Sep. 2002). "Role of Dok1 in cell signaling mediated by RET tyrosine kinase". J. Biol. Chem. (United States) 277 (36): 32781–90. doi:10.1074/jbc.M202336200. ISSN 0021-9258. PMID 12087092. 
  22. ^ Arighi, E; Alberti L, Torriti F, Ghizzoni S, Rizzetti M G, Pelicci G, Pasini B, Bongarzone I, Piutti C, Pierotti M A, Borrello M G (Feb. 1997). "Identification of Shc docking site on Ret tyrosine kinase". Oncogene (ENGLAND) 14 (7): 773–82. doi:10.1038/sj.onc.1200896. ISSN 0950-9232. PMID 9047384. 
  23. ^ Klein, R D; Sherman D, Ho W H, Stone D, Bennett G L, Moffat B, Vandlen R, Simmons L, Gu Q, Hongo J A, Devaux B, Poulsen K, Armanini M, Nozaki C, Asai N, Goddard A, Phillips H, Henderson C E, Takahashi M, Rosenthal A (Jun. 1997). "A GPI-linked protein that interacts with Ret to form a candidate neurturin receptor". Nature (ENGLAND) 387 (6634): 717–21. doi:10.1038/42722. ISSN 0028-0836. PMID 9192898. 
  24. ^ Cik, M; Masure S, Lesage A S, Van Der Linden I, Van Gompel P, Pangalos M N, Gordon R D, Leysen J E (Sep. 2000). "Binding of GDNF and neurturin to human GDNF family receptor alpha 1 and 2. Influence of cRET and cooperative interactions". J. Biol. Chem. (UNITED STATES) 275 (36): 27505–12. doi:10.1074/jbc.M000306200. ISSN 0021-9258. PMID 10829012. 

Further reading

  • Eng C, Mulligan LM (1997). "Mutations of the RET proto-oncogene in the multiple endocrine neoplasia type 2 syndromes, related sporadic tumours, and hirschsprung disease". Hum. Mutat. 9 (2): 97–109. doi:10.1002/(SICI)1098-1004(1997)9:2<97::AID-HUMU1>3.0.CO;2-M. PMID 9067749. 
  • Hofstra RM, Osinga J, Buys CH (1998). "Mutations in Hirschsprung disease: when does a mutation contribute to the phenotype". Eur. J. Hum. Genet. 5 (4): 180–5. PMID 9359036. 
  • Nikiforov YE (2002). "RET/PTC rearrangement in thyroid tumors". Endocr. Pathol. 13 (1): 3–16. doi:10.1385/EP:13:1:03. PMID 12114746. 
  • Santoro M, Melillo RM, Carlomagno F, et al. (2004). "Minireview: RET: normal and abnormal functions". Endocrinology 145 (12): 5448–5451. doi:10.1210/en.2004-0922. PMID 15331579. 
  • Santoro M, Carlomagno F, Melillo RM, Fusco A (2005). "Dysfunction of the RET receptor in human cancer". Cell. Mol. Life Sci. 61 (23): 2954–2964. doi:10.1007/s00018-004-4276-8. PMID 15583857. 
  • Niccoli-Sire P, Conte-Devolx B, (2005). "[RET mutations and preventive treatment of medullary thyroid cancer]". Ann. Endocrinol. (Paris) 66 (3): 168–75. PMID 15988377. 
  • Lantieri F, Griseri P, Ceccherini I (2006). "Molecular mechanisms of RET-induced Hirschsprung pathogenesis". Ann. Med. 38 (1): 11–9. doi:10.1080/07853890500442758. PMID 16448984. 
  • Ciampi R, Nikiforov YE (2007). "RET/PTC rearrangements and BRAF mutations in thyroid tumorigenesis". Endocrinology 148 (3): 936–41. doi:10.1210/en.2006-0921. PMID 16946010. 
  • Plaza-Menacho I, Burzynski GM, de Groot JW, et al. (2007). "Current concepts in RET-related genetics, signaling and therapeutics". Trends Genet. 22 (11): 627–36. doi:10.1016/j.tig.2006.09.005. PMID 16979782. 

External links