Jump to content

AGR2

From Wikipedia, the free encyclopedia
AGR2
Available structures
PDBOrtholog search: PDBe RCSB
Identifiers
AliasesAGR2, AG2, GOB-4, HAG-2, HEL-S-116, PDIA17, XAG-2, anterior gradient 2, protein disulphide isomerase family member, AG-2, HPC8
External IDsOMIM: 606358; MGI: 1344405; HomoloGene: 4674; GeneCards: AGR2; OMA:AGR2 - orthologs
Orthologs
SpeciesHumanMouse
Entrez
Ensembl
UniProt
RefSeq (mRNA)

NM_006408

NM_011783

RefSeq (protein)

NP_006399

NP_035913

Location (UCSC)Chr 7: 16.79 – 16.83 MbChr 12: 36.04 – 36.05 Mb
PubMed search[3][4]
Wikidata
View/Edit HumanView/Edit Mouse

Anterior gradient protein 2 homolog (AGR-2), also known as secreted cement gland protein XAG-2 homolog, is a protein that in humans is encoded by the AGR2 gene. Anterior gradient homolog 2 was originally discovered in Xenopus laevis.[5] In Xenopus AGR2 plays a role in cement gland differentiation,[6] but in human cancer cell lines high levels of AGR2 correlate with downregulation of the p53 response,[7] cell migration, and cell transformation.[8] However, there have been other observations that AGR2 can repress growth and proliferation.[9]

Discovery in Xenopus laevis

[edit]

The Xenopus laevis anterior gradient genes - XAG-1, XAG-2, and XAG-3 - were discovered through dissection of different-aged embryos.[10] They become expressed in the anterior region of the dorsal ectoderm in late gastrula embryos.[10][11] XAG-2 expression gathers at the anterior region of the dorsal ectoderm, and this region corresponds to the cement gland anlage.[12] Many other homologous proteins have been discovered afterwards in Xenopus.

Tissue distribution

[edit]

AGR2 is the human homolog of XAG-2. It is expressed strongly in tissues that secrete mucus or function as endocrine organs, including the lungs, stomach, colon, prostate and small intestine.[13][14] Its protein expression has been shown to be regulated by both androgens and estrogens.[9][15]

Structure and function

[edit]

AGR2 is a protein disulfide isomerase, with a single CXXS active domain motif for oxidation and reduction reactions.[16][17] AGR2 forms mixed disulfides in substrates, such as intestinal mucin. AGR2 interacts with Mucin 2 through its thioredoxin-like domain forming a heterodisulfide bond with cysteine residues in MUC2.[18] AGR2 is suggested to play a role in protein folding, and it has a KTEL C-terminal motif similar to KDEL and KVEL endoplasmic reticulum retention sequences.[19]

Clinical significance

[edit]

Agr2 is located on chromosome 7p21, a region that has frequent genetic alterations.[20] It was first identified in estrogen receptor-positive breast cancer cells.[14] Later studies showed elevated levels of AGR2 in adenocarcinomas of the esophagus, pancreas, and prostate. In Barrett's esophagus, Agr2 expression is elevated by over 70 times compared to normal esophageal epithelia.[21] Thus, this protein alone is enough to distinguish Barrett's esophagus, which is linked to esophageal adenocarcinoma, from a normal esophagus.[22]

Varying AGR2 levels exist in different cancers. In breast cancer, high AGR2 expression is correlated with low survival rate.[23] AGR2 levels are elevated in the preneoplastic tissue Barrett's oesophagus. AGR2 is also associated with prostate cancer, though lower levels are associated with higher Gleason grades.[24]

In contrast to upregulation of AGR2 in various cancers, downregulation of AGR2 is linked with inflammatory bowel disease and increases in the risk of Crohn's disease and ulcerative colitis. This implies the importance of AGR2 in maintaining epithelial barrier function, which is supported by FOXA1 and FOXA2 molecules (transcription factors for epithelial goblet cells) which can activate the AGR2 promoter.[25]

Breast cancer

[edit]

In breast cancer, AGR2 and estrogen (ER) expression are positively correlated. Approximately 70% of breast cancer patients have breast cancer cells that heavily express ER and progesterone receptors (PgR). These patients are normally treated with endocrine therapy. Tamoxifen, which blocks the binding of estradiol to its receptor, is the standard treatment for ER-positive breast cancer. However, about one third of patients do not respond to this therapy,[26] and increased AGR2 may be one reason.

There is a positive correlation for a higher level of AGR2 expression with poor therapeutic results in ERα-positive breast cancer patients.[27][28] Agr2 mRNA expression is elevated in in vitro and in vivo studies responding to tamoxifen adjuvant therapy, so AGR2 is likely provides an agonistic effect on tamoxifen.[27][29] Therefore, AGR2 is a possible predictive biomarker when selecting patients with ER-positive breast cancer to participate this therapy.[30] Although Agr2 mRNA levels are correlated with the tamoxifen therapy response, AGR2 protein levels have yet to be statistically associated with the therapy. A combinatorial therapy using the anastrozole and fulvestrant has been shown to prevent binding of the ER to the Agr2 promoter, and there has been improved prognosis in the patients receiving it, possibly because AGR2 expression in the tumors have been reduced.[31][unreliable medical source]

What AGR2 does in cancers is poorly understood. In breast cancer, HSP90 is a molecular chaperone expressed in tumor cells when there exists an excess of unfolded protein, and its co-chaperone has been reported to induce expression of AGR2,[32][33] so AGR2 may be used by the endoplasmic reticulum to assist with protein folding to alleviate proteotoxic stress. AGR2 may help regulate the protein and mRNA levels in a cell overall as well. During late pregnancy and lactation, AGR2 levels peak when milk proteins are produced, and mammary-specific Agr2 knockout mice had downregulated milk protein mRNA expression.[34]

Prostate cancer

[edit]

AGR2 is expressed in relatively high levels for prostate cancer patients. Urine sediment tests determined Agr2 transcript levels to be elevated.[9] AGR2 expression was increased in metastatic prostate cancer cells cultured in a bone marrow microenvironment, where intense levels of Agr2 mRNA were detected, suggesting AGR2 is required for bone metastasis of prostate cancer cells.[35] AGR2 transcript levels were lower in metastatic lesions compared to the primary tumor, however.[24] A greater chance of prostate cancer recurrence is linked to relatively lower levels of AGR2.[24]

AGR2 depletion through gene knockdown was shown to result in accumulation of prostate cancer cell lines at the G0/G1 phase of the cell cycle, while forced expression of AGR led to an increase in cell proliferation.[36] AGR2 was determined to be involved in cell adhesion. Agr2-silenced prostate cancer cells had a large decrease in association with fibronectin, lost expression of integrin, and reduced tumor cell migration.[35] In addition to these studies, AGR2 was among a set of genes consistently associated with prostate tumour visibility on MRI in a bioinformatic analysis, the analysis found that more visible tumours harboured more aggressive genetic characteristics.[37] The study also found genes involved with cell-ECM interactions to be altered in aggressive MRI-visible tumours,[37] potentially reflecting AGR2's association with cellular adhesion ans integrin signalling.[35]

Pancreatic cancer

[edit]

AGR2 mRNA was discovered to be increased in precancerous lesions and neoplastic cells of pancreatic tumors and cancer cell lines.[38] Transient silencing of AGR2 by small interfering RNA and short hairpin RNA significantly reduces cell proliferation and invasion while increasing the effectiveness of gemcitabine treatment in pancreatic cancer cell lines in vitro,[38][39] indicating that AGR2 can help pancreatic cancer cells survive and protect tumors from chemotherapeutic treatments for pancreatic cancer. This is critical because pancreatic cancer is well recognized as being highly resistant to therapeutics, and five-year survival rates for pancreatic cancer are extremely low.

Protein interactions

[edit]

AGR2 protein has been demonstrated to interact with C4.4A and DAG-1 proteins which are associated with metastasis formation since these transmembrane proteins are involved in cell and matrix interactions between cancer and normal cells.[40] AGR2 is able to suppress p53 activity by preventing phosphorylation after DNA damage.[7] AGR2 has been shown to bind to Reptin, a tumor repressor, in the nucleus.[41]

References

[edit]
  1. ^ a b c GRCh38: Ensembl release 89: ENSG00000106541Ensembl, May 2017
  2. ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000020581Ensembl, 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.
  5. ^ "Entrez Gene: AGR2 anterior gradient homolog 2 (Xenopus laevis)".
  6. ^ Aberger F, Weidinger G, Grunz H, Richter K (March 1998). "Anterior specification of embryonic ectoderm: the role of the Xenopus cement gland-specific gene XAG-2". Mech. Dev. 72 (1–2): 115–30. doi:10.1016/S0925-4773(98)00021-5. PMID 9533957. S2CID 15262006.
  7. ^ a b Pohler E, Craig AL, Cotton J, Lawrie L, Dillon JF, Ross P, Kernohan N, Hupp TR (June 2004). "The Barrett's antigen anterior gradient-2 silences the p53 transcriptional response to DNA damage". Mol. Cell. Proteomics. 3 (6): 534–47. doi:10.1074/mcp.M300089-MCP200. PMID 14967811.
  8. ^ Wang Z, Hao Y, Lowe AW (January 2008). "The adenocarcinoma-associated antigen, AGR2, promotes tumor growth, cell migration, and cellular transformation". Cancer Res. 68 (2): 492–7. doi:10.1158/0008-5472.CAN-07-2930. PMID 18199544.
  9. ^ a b c Bu H, Bormann S, Schäfer G, Horninger W, Massoner P, Neeb A, Lakshmanan VK, Maddalo D, Nestl A, Sültmann H, Cato AC, Klocker H (May 2011). "The anterior gradient 2 (AGR2) gene is overexpressed in prostate cancer and may be useful as a urine sediment marker for prostate cancer detection". Prostate. 71 (6): 575–87. doi:10.1002/pros.21273. PMID 20945500. S2CID 1861353.
  10. ^ a b Sive HL, Hattori K, Weintraub H (July 1989). "Progressive determination during formation of the anteroposterior axis in Xenopus laevis". Cell. 58 (1): 171–80. doi:10.1016/0092-8674(89)90413-3. PMID 2752418. S2CID 40970928.
  11. ^ Sive H, Bradley L (March 1996). "A sticky problem: the Xenopus cement gland as a paradigm for anteroposterior patterning". Dev. Dyn. 205 (3): 265–80. doi:10.1002/(SICI)1097-0177(199603)205:3<265::AID-AJA7>3.0.CO;2-G. PMID 8850563. S2CID 22326745.
  12. ^ Aberger F, Weidinger G, Grunz H, Richter K (March 1998). "Anterior specification of embryonic ectoderm: the role of the Xenopus cement gland-specific gene XAG-2". Mech. Dev. 72 (1–2): 115–30. doi:10.1016/S0925-4773(98)00021-5. PMID 9533957. S2CID 15262006.
  13. ^ "Anterior gradient 2 homolog (Xenopus laevis)". Gene/Protein. The Human Protein Atlas. Retrieved 28 February 2014.
  14. ^ a b Thompson DA, Weigel RJ (October 1998). "hAG-2, the human homologue of the Xenopus laevis cement gland gene XAG-2, is coexpressed with estrogen receptor in breast cancer cell lines". Biochem. Biophys. Res. Commun. 251 (1): 111–6. doi:10.1006/bbrc.1998.9440. PMID 9790916.
  15. ^ Vanderlaag KE, Hudak S, Bald L, Fayadat-Dilman L, Sathe M, Grein J, Janatpour MJ (2010). "Anterior gradient-2 plays a critical role in breast cancer cell growth and survival by modulating cyclin D1, estrogen receptor-alpha and survivin". Breast Cancer Res. 12 (3): R32. doi:10.1186/bcr2586. PMC 2917027. PMID 20525379.
  16. ^ Galligan JJ, Petersen DR (July 2012). "The human protein disulfide isomerase gene family". Human Genomics. 6 (1): 6. doi:10.1186/1479-7364-6-6. PMC 3500226. PMID 23245351.
  17. ^ Persson S, Rosenquist M, Knoblach B, Khosravi-Far R, Sommarin M, Michalak M (September 2005). "Diversity of the protein disulfide isomerase family: identification of breast tumor induced Hag2 and Hag3 as novel members of the protein family". Mol. Phylogenet. Evol. 36 (3): 734–40. doi:10.1016/j.ympev.2005.04.002. PMID 15935701.
  18. ^ Park SW, Zhen G, Verhaeghe C, Nakagami Y, Nguyenvu LT, Barczak AJ, Killeen N, Erle DJ (April 2009). "The protein disulfide isomerase AGR2 is essential for production of intestinal mucus". Proc. Natl. Acad. Sci. U.S.A. 106 (17): 6950–5. Bibcode:2009PNAS..106.6950P. doi:10.1073/pnas.0808722106. PMC 2678445. PMID 19359471.
  19. ^ Gupta A, Dong A, Lowe AW (2012). "AGR2 gene function requires a unique endoplasmic reticulum localization motif". J. Biol. Chem. 287 (7): 4773–82. doi:10.1074/jbc.M111.301531. PMC 3281655. PMID 22184114.
  20. ^ Petek E, Windpassinger C, Egger H, Kroisel PM, Wagner K (2000). "Localization of the human anterior gradient-2 gene (AGR2) to chromosome band 7p21.3 by radiation hybrid mapping and fluorescencein situ hybridisation". Cytogenet. Cell Genet. 89 (3–4): 141–2. doi:10.1159/000015594. PMID 10965104. S2CID 19307750.
  21. ^ Hao Y, Triadafilopoulos G, Sahbaie P, Young HS, Omary MB, Lowe AW (September 2006). "Gene expression profiling reveals stromal genes expressed in common between Barrett's esophagus and adenocarcinoma". Gastroenterology. 131 (3): 925–33. doi:10.1053/j.gastro.2006.04.026. PMC 2575112. PMID 16952561.
  22. ^ Maley CC, Rustgi AK (April 2006). "Barrett's esophagus and its progression to adenocarcinoma". J Natl Compr Canc Netw. 4 (4): 367–74. doi:10.6004/jnccn.2006.0031. PMID 16569389.
  23. ^ Barraclough DL, Platt-Higgins A, de Silva Rudland S, Barraclough R, Winstanley J, West CR, Rudland PS (November 2009). "The metastasis-associated anterior gradient 2 protein is correlated with poor survival of breast cancer patients". Am. J. Pathol. 175 (5): 1848–57. doi:10.2353/ajpath.2009.090246. PMC 2774050. PMID 19834055.
  24. ^ a b c Maresh EL, Mah V, Alavi M, Horvath S, Bagryanova L, Liebeskind ES, Knutzen LA, Zhou Y, Chia D, Liu AY, Goodglick L (2010). "Differential expression of anterior gradient gene AGR2 in prostate cancer". BMC Cancer. 10: 680. doi:10.1186/1471-2407-10-680. PMC 3009682. PMID 21144054.
  25. ^ Zheng W, Rosenstiel P, Huse K, Sina C, Valentonyte R, Mah N, Zeitlmann L, Grosse J, Ruf N, Nürnberg P, Costello CM, Onnie C, Mathew C, Platzer M, Schreiber S, Hampe J (January 2006). "Evaluation of AGR2 and AGR3 as candidate genes for inflammatory bowel disease". Genes Immun. 7 (1): 11–8. doi:10.1038/sj.gene.6364263. PMID 16222343. S2CID 10046565.
  26. ^ "Scientists Unravel Resistance to Breast Cancer Treatment". Artemis. Retrieved 26 February 2014.
  27. ^ a b Hrstka R, Nenutil R, Fourtouna A, Maslon MM, Naughton C, Langdon S, Murray E, Larionov A, Petrakova K, Muller P, Dixon MJ, Hupp TR, Vojtesek B (August 2010). "The pro-metastatic protein anterior gradient-2 predicts poor prognosis in tamoxifen-treated breast cancers". Oncogene. 29 (34): 4838–47. doi:10.1038/onc.2010.228. PMID 20531310. S2CID 21135835.
  28. ^ Innes HE, Liu D, Barraclough R, Davies MP, O'Neill PA, Platt-Higgins A, de Silva Rudland S, Sibson DR, Rudland PS (April 2006). "Significance of the metastasis-inducing protein AGR2 for outcome in hormonally treated breast cancer patients". Br. J. Cancer. 94 (7): 1057–65. doi:10.1038/sj.bjc.6603065. PMC 2361240. PMID 16598187.
  29. ^ Hengel SM, Murray E, Langdon S, Hayward L, O'Donoghue J, Panchaud A, Hupp T, Goodlett DR (October 2011). "Data-independent proteomic screen identifies novel tamoxifen agonist that mediates drug resistance". J. Proteome Res. 10 (10): 4567–78. doi:10.1021/pr2004117. PMC 3242698. PMID 21936522.
  30. ^ Hrstka R, Brychtova V, Fabian P, Vojtesek B, Svoboda M (2013). "AGR2 predicts tamoxifen resistance in postmenopausal breast cancer patients". Dis. Markers. 35 (4): 207–12. doi:10.1155/2013/761537. PMC 3776368. PMID 24167368.
  31. ^ Mehta RS, Barlow WE, Albain KS, Vandenberg TA, Dakhil SR, Tirumali NR, Lew DL, Hayes DF, Gralow JR, Livingston RB, Hortobagyi GN (2012). "Combination anastrozole and fulvestrant in metastatic breast cancer". N. Engl. J. Med. 367 (5): 435–44. doi:10.1056/NEJMoa1201622. PMC 3951300. PMID 22853014.
  32. ^ Whitesell L, Lindquist SL (2005). "HSP90 and the chaperoning of cancer" (PDF). Nat. Rev. Cancer. 5 (10): 761–72. doi:10.1038/nrc1716. PMID 16175177. S2CID 22098282. Archived from the original (PDF) on 2014-03-27. Retrieved 2019-09-27.
  33. ^ Simpson NE, Lambert WM, Watkins R, Giashuddin S, Huang SJ, Oxelmark E, Arju R, Hochman T, Goldberg JD, Schneider RJ, Reiz LF, Soares FA, Logan SK, Garabedian MJ (2010). "High levels of Hsp90 cochaperone p23 promote tumor progression and poor prognosis in breast cancer by increasing lymph node metastases and drug resistance". Cancer Res. 70 (21): 8446–56. doi:10.1158/0008-5472.CAN-10-1590. PMC 3007122. PMID 20847343.
  34. ^ Verma S, Salmans ML, Geyfman M, Wang H, Yu Z, Lu Z, Zhao F, Lipkin SM, Andersen B (2012). "The estrogen-responsive Agr2 gene regulates mammary epithelial proliferation and facilitates lobuloalveolar development". Dev. Biol. 369 (2): 249–60. doi:10.1016/j.ydbio.2012.06.030. PMC 3465459. PMID 22819674.
  35. ^ a b c Chanda D, Lee JH, Sawant A, Hensel JA, Isayeva T, Reilly SD, Siegal GP, Smith C, Grizzle W, Singh R, Ponnazhagan S (2014). "Anterior gradient protein-2 is a regulator of cellular adhesion in prostate cancer". PLOS ONE. 9 (2): e89940. Bibcode:2014PLoSO...989940C. doi:10.1371/journal.pone.0089940. PMC 3937391. PMID 24587138.
  36. ^ Hu Z, Gu Y, Han B, Zhang J, Li Z, Tian K, Young CY, Yuan H (2012). "Knockdown of AGR2 induces cellular senescence in prostate cancer cells". Carcinogenesis. 33 (6): 1178–86. doi:10.1093/carcin/bgs141. PMID 22467239.
  37. ^ a b Norris, Joseph M.; Simpson, Benjamin S.; Parry, Marina A.; Allen, Clare; Ball, Rhys; Freeman, Alex; Kelly, Daniel; Kim, Hyung L.; Kirkham, Alex; You, Sungyong; Kasivisvanathan, Veeru (2020-07-01). "Genetic Landscape of Prostate Cancer Conspicuity on Multiparametric Magnetic Resonance Imaging: A Systematic Review and Bioinformatic Analysis". European Urology Open Science. 20: 37–47. doi:10.1016/j.euros.2020.06.006. ISSN 2666-1683. PMC 7497895. PMID 33000006.
  38. ^ a b Ramachandran V, Arumugam T, Wang H, Logsdon CD (October 2008). "Anterior gradient 2 is expressed and secreted during the development of pancreatic cancer and promotes cancer cell survival". Cancer Res. 68 (19): 7811–8. doi:10.1158/0008-5472.CAN-08-1320. PMC 4429896. PMID 18829536.
  39. ^ Iacobuzio-Donahue CA, Ashfaq R, Maitra A, Adsay NV, Shen-Ong GL, Berg K, Hollingsworth MA, Cameron JL, Yeo CJ, Kern SE, Goggins M, Hruban RH (December 2003). "Highly expressed genes in pancreatic ductal adenocarcinomas: a comprehensive characterization and comparison of the transcription profiles obtained from three major technologies". Cancer Res. 63 (24): 8614–22. PMID 14695172.
  40. ^ Fletcher GC, Patel S, Tyson K, Adam PJ, Schenker M, Loader JA, Daviet L, Legrain P, Parekh R, Harris AL, Terrett JA (February 2003). "hAG-2 and hAG-3, human homologues of genes involved in differentiation, are associated with oestrogen receptor-positive breast tumours and interact with metastasis gene C4.4a and dystroglycan". Br. J. Cancer. 88 (4): 579–85. doi:10.1038/sj.bjc.6600740. PMC 2377166. PMID 12592373.
  41. ^ Maslon MM, Hrstka R, Vojtesek B, Hupp TR (2010). "A divergent substrate-binding loop within the pro-oncogenic protein anterior gradient-2 forms a docking site for Reptin". J. Mol. Biol. 404 (3): 418–38. doi:10.1016/j.jmb.2010.09.035. hdl:1842/6477. PMID 20888340.
[edit]

Further reading

[edit]