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{{Infobox_gene}}
{{PBB_Controls
'''Leucine-rich repeat-containing G-protein coupled receptor 5''' ('''LGR5''') also known as '''G-protein coupled receptor 49''' ('''GPR49''') or '''G-protein coupled receptor 67''' ('''GPR67''') is a [[protein]] that in humans is encoded by the LGR5 [[gene]].<ref name="pmid9642114">{{cite journal |vauthors=McDonald T, Wang R, Bailey W, Xie G, Chen F, Caskey CT, Liu Q | title = Identification and cloning of an orphan G protein-coupled receptor of the glycoprotein hormone receptor subfamily | journal = Biochem Biophys Res Commun | volume = 247 | issue = 2 | pages = 266–70 |date=Jul 1998 | pmid = 9642114 | pmc =  | doi = 10.1006/bbrc.1998.8774 }}</ref><ref name="McClanahan_2006">{{cite journal |vauthors=McClanahan T, Koseoglu S, Smith K, Grein J, Gustafson E, Black S, Kirschmeier P, Samatar AA | title = Identification of overexpression of orphan G protein-coupled receptor GPR49 in human colon and ovarian primary tumors | journal = Cancer Biol. Ther. | volume = 5 | issue = 4 | pages = 419–26 |date=April 2006 | pmid = 16575208 | doi = 10.4161/cbt.5.4.2521 }}</ref> It is a member of [[Rhodopsin-like receptors|GPCR class A]] receptor proteins. R-spondin proteins are the biological ligands of LGR5. LGR5 is expressed across a diverse range of tissue such as in the muscle, [[placenta]], spinal cord and brain and particularly as a [[biomarker]] of adult [[stem cell]]s in certain tissues.<ref name="Hsu_1998">{{cite journal |vauthors=Hsu SY, Liang SG, Hsueh AJ | title = Characterization of two LGR genes homologous to gonadotropin and thyrotropin receptors with extracellular leucine-rich repeats and a G protein-coupled, seven-transmembrane region | journal = Mol. Endocrinol. | volume = 12 | issue = 12 | pages = 1830–45 |date=December 1998 | pmid = 9849958 | doi = 10.1210/me.12.12.1830 }}</ref>
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<!-- The GNF_Protein_box is automatically maintained by Protein Box Bot.  See Template:PBB_Controls to Stop updates. -->
== Gene ==
{{GNF_Protein_box
| image =
| image_source =
| PDB =
| Name = Leucine-rich repeat-containing G protein-coupled receptor 5
| HGNCid = 4504
| Symbol = LGR5
| AltSymbols =; FEX; GPR49; GPR67; GRP49; HG38; MGC117008
| OMIM = 606667
| ECnumber = 
| Homologene = 20807
| MGIid = 1341817
| GeneAtlas_image1 = PBB_GE_LGR5_213880_at_tn.png
| GeneAtlas_image2 = PBB_GE_LGR5_210393_at_tn.png
| Function = {{GNF_GO|id=GO:0004872 |text = receptor activity}} {{GNF_GO|id=GO:0005515 |text = protein binding}} {{GNF_GO|id=GO:0016500 |text = protein-hormone receptor activity}}
| Component = {{GNF_GO|id=GO:0005887 |text = integral to plasma membrane}} {{GNF_GO|id=GO:0016020 |text = membrane}} {{GNF_GO|id=GO:0016021 |text = integral to membrane}}
| Process = {{GNF_GO|id=GO:0007165 |text = signal transduction}} {{GNF_GO|id=GO:0007186 |text = G-protein coupled receptor protein signaling pathway}}
| Orthologs = {{GNF_Ortholog_box
    | Hs_EntrezGene = 8549
    | Hs_Ensembl = ENSG00000139292
    | Hs_RefseqProtein = NP_003658
    | Hs_RefseqmRNA = NM_003667
    | Hs_GenLoc_db = 
    | Hs_GenLoc_chr = 12
    | Hs_GenLoc_start = 70120031
    | Hs_GenLoc_end = 70264781
    | Hs_Uniprot = O75473
    | Mm_EntrezGene = 14160
    | Mm_Ensembl = ENSMUSG00000020140
    | Mm_RefseqmRNA = NM_010195
    | Mm_RefseqProtein = NP_034325
    | Mm_GenLoc_db = 
    | Mm_GenLoc_chr = 10
    | Mm_GenLoc_start = 114855736
    | Mm_GenLoc_end = 114991603
    | Mm_Uniprot = Q3V1L2
  }}
}}
'''Leucine-rich repeat-containing G protein-coupled receptor 5''', also known as '''LGR5''', is a human [[gene]].<ref name="entrez">{{cite web | title = Entrez Gene: LGR5 leucine-rich repeat-containing G protein-coupled receptor 5| url = http://www.ncbi.nlm.nih.gov/sites/entrez?Db=gene&Cmd=ShowDetailView&TermToSearch=8549| accessdate = }}</ref>


<!-- The PBB_Summary template is automatically maintained by Protein Box Bot. See Template:PBB_Controls to Stop updates. -->
Prior to its current naming designation, LGR5 was also known as FEX, HG38, GPR49, and GPR67.<ref name="entrez">{{cite web | title =LGR5 leucine-rich repeat-containing G protein-coupled receptor 5 | url = https://www.ncbi.nlm.nih.gov/sites/entrez?Db=gene&Cmd=ShowDetailView&TermToSearch=8549 | work = Entrez Gene }}</ref> The Human LGR5 gene is 144,810 [[nucleobase|bases]] long and located at [[chromosome 12]] at position 12q22-q23.<ref name="entrez"/> Both human, rat and mouse homologs contain 907 [[amino acid]]s and seven [[transmembrane domain]]s.<ref name="iupharLGR5">{{cite web | title = LGR5 leucine-rich repeat containing G protein-coupled receptor 5 | url = http://www.iuphar-db.org/DATABASE/ObjectDisplayForward?familyId=16&objectId=148 | work = IUPHAR Database}}</ref>  After [[Translation (biology)|translation]], the [[signal peptide]] (amino acids 1-21) is cleaved off and the mature [[peptide]] (amino acids 22-907) inserts its transmembrane domain into the [[translocon]] membrane prior to packaging towards the plasma membrane.
{{PBB_Summary
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| summary_text =  
}}


==References==
==Protein structure==
{{reflist|2}}
 
==Further reading==
LGR5 is highly conserved within the [[mammal| mammalian clade]]. [[sequence analysis|Sequence analyses]] showed that the transmembrane regions and [[cysteine]]-flanked junction between TM1 and the [[ectodomain|extracellular domain]] were highly conserved in sea anemone (''[[Anthopleura elegantissima]]''), fly (''[[Drosophila melanogaster]]''), worm (''[[Caenorhabditis elegans]]''), snail (''[[Lymnaea stagnalis]]''), rat (''[[Rattus rattus]]'') and human (''[[Homo sapiens]]'').<ref name="Hsu_1998"/> Homology amongst the metazoan suggests that it has been conserved across animals and was hypothesised as a chimeric fusion of an ancestral GPCR and a leucine-rich repeat motif.
{{refbegin | 2}}
 
{{PBB_Further_reading
Sheau Hsu, Shan Liang and Aaron Hsueh first identified LGR5, together with LGR4, in 1998 at the University Medical School Stanford, California using [[gene expression|expression sequence tag]]s based on putative [[glycoprotein]] hormone receptors in ''Drosophila''.<ref name="Hsu_1998"/>
| citations =  
 
*{{cite journal | author=McDonald T, Wang R, Bailey W, ''et al.'' |title=Identification and cloning of an orphan G protein-coupled receptor of the glycoprotein hormone receptor subfamily. |journal=Biochem. Biophys. Res. Commun. |volume=247 |issue= 2 |pages= 266-70 |year= 1998 |pmid= 9642114 |doi= 10.1006/bbrc.1998.8774 }}
Experimental evidence show that the mature receptor protein contains up to 17 leucine-rich repeats, each composed of 24 amino acids spanning the extracellular domain flanked by the cysteine-rich [[N-terminus|N-terminal]] and [[C-terminus|C-terminal]] regions. In contrast, other glycoprotein hormone receptors such as [[Luteinizing hormone]], [[Follicle-stimulating hormone]] and [[Thyroid-stimulating hormone]] contain only 9 repeats.<ref name="Hsu_1998"/> Sequence alignment showed that the second [[N-glycosylation]] site in LGR5 ([[asparagine|Asn]] 208) aligns with that on the sixth repeat of [[gonadotropin]] and TSH receptors. The cysteine residues flanking the ectodomain form stabilising [[disulfide bond]]s that support the secondary structure of the leucine-rich repeats.
*{{cite journal | author=Hsu SY, Liang SG, Hsueh AJ |title=Characterization of two LGR genes homologous to gonadotropin and thyrotropin receptors with extracellular leucine-rich repeats and a G protein-coupled, seven-transmembrane region. |journal=Mol. Endocrinol. |volume=12 |issue= 12 |pages= 1830-45 |year= 1999 |pmid= 9849958 |doi= }}
 
*{{cite journal | author=Hsu SY, Kudo M, Chen T, ''et al.'' |title=The three subfamilies of leucine-rich repeat-containing G protein-coupled receptors (LGR): identification of LGR6 and LGR7 and the signaling mechanism for LGR7. |journal=Mol. Endocrinol. |volume=14 |issue= 8 |pages= 1257-71 |year= 2001 |pmid= 10935549 |doi= }}
==Function==
*{{cite journal | author=Strausberg RL, Feingold EA, Grouse LH, ''et al.'' |title=Generation and initial analysis of more than 15,000 full-length human and mouse cDNA sequences. |journal=Proc. Natl. Acad. Sci. U.S.A. |volume=99 |issue= 26 |pages= 16899-903 |year= 2003 |pmid= 12477932 |doi= 10.1073/pnas.242603899 }}
 
*{{cite journal | author=Yamamoto Y, Sakamoto M, Fujii G, ''et al.'' |title=Overexpression of orphan G-protein-coupled receptor, Gpr49, in human hepatocellular carcinomas with beta-catenin mutations. |journal=Hepatology |volume=37 |issue= 3 |pages= 528-33 |year= 2003 |pmid= 12601349 |doi= 10.1053/jhep.2003.50029 }}
LGR5 is a member of the [[Wnt signaling pathway]]. Although its ligand remains elusive, it has been shown that costimulation with [[RSPO1|R-spondin 1]] and [[WNT3A|Wnt-3a]] induce increased internalization of LGR5. LGR5 also cointernalizes with [[LRP6]] and [[FZD5]] via a [[clathrin]]-dependent pathway to form a ternary complex upon Wnt ligand binding. Moreover, the rapid cointernalization of LRP6 by LGR5 induces faster rates of degradation for the former. It has been shown that the [[C-terminal]] region of LGR5 is crucial for both dynamic internalization and degradation to occur, although C-terminal truncation does not inhibit LRP6 interaction and internalization, but rather, heightens receptor activity. Thus, only the initial interaction with its unknown ligand and other membrane bound receptors is crucial in its role in Wnt signalling and not the internalization itself.<ref name="Carmon_2012">{{cite journal |vauthors=Carmon KS, Lin Q, Gong X, Thomas A, Liu Q | title = LGR5 interacts and cointernalizes with Wnt receptors to modulate Wnt/β-catenin signaling | journal = Mol. Cell. Biol. | volume = 32 | issue = 11 | pages = 2054–64 |date=June 2012 | pmid = 22473993 | pmc = 3372227 | doi = 10.1128/MCB.00272-12 }}</ref> LGR5 is  crucial during embryogenesis as LGR null studies in mice incurred 100% neonatal mortality accompanied by several craniofacial distortions such as ankyloglossia and gastrointestinal dilation.<ref name="morita2004">{{cite journal |vauthors=Morita H, Mazerbourg S, Bouley DM, Luo CW, Kawamura K, Kuwabara Y, Baribault H, Tian H, Hsueh AJ | title = Neonatal lethality of LGR5 null mice is associated with ankyloglossia and gastrointestinal distension | journal = Mol. Cell. Biol. | volume = 24 | issue = 22 | pages = 9736–43 |date=November 2004 | pmid = 15509778 | pmc = 525477 | doi = 10.1128/MCB.24.22.9736-9743.2004 }}</ref>
*{{cite journal | author=McClanahan T, Koseoglu S, Smith K, ''et al.'' |title=Identification of overexpression of orphan G protein-coupled receptor GPR49 in human colon and ovarian primary tumors. |journal=Cancer Biol. Ther. |volume=5 |issue= 4 |pages= 419-26 |year= 2007 |pmid= 16575208 |doi= }}
 
}}
===Ligand===
 
LGR5 belongs to a class of class A GPCR [[orphan receptor]]s. Thus its ligands remain elusive. However, it has been shown that Lgr2, the fly orthologue of mammalian LGR5, binds with "high affinity and specificity" with [[bursicon]], an insect heterodimeric, neurohormone that belongs in the same class as FSH, LH and TSH, which in turn are homologous to mammalian bone morphogenetic factors (BMPs) such  as [[gremlin (protein)|gremlin]] and [[cerberus (protein)|cerberus]]. Therefore, LGR5 might be a receptor for a member of the large family of [[bone morphogenetic protein]] antagonists.<ref name="Barker_2010">{{cite journal |vauthors=Barker N, Clevers H | title = Leucine-rich repeat-containing G-protein-coupled receptors as markers of adult stem cells | journal = Gastroenterology | volume = 138 | issue = 5 | pages = 1681–96 |date=May 2010 | pmid = 20417836 | doi = 10.1053/j.gastro.2010.03.002 }}</ref> Moreover, R-spondin proteins were shown to interact with the extracellular domain of LRG5.<ref name="Ruffner_2012">{{cite journal |vauthors=Ruffner H, Sprunger J, Charlat O, Leighton-Davies J, Grosshans B, Salathe A, Zietzling S, Beck V, Therier M, Isken A, Xie Y, Zhang Y, Hao H, Shi X, Liu D, Song Q, Clay I, Hintzen G, Tchorz J, Bouchez LC, Michaud G, Finan P, Myer VE, Bouwmeester T, Porter J, Hild M, Bassilana F, Parker CN, Cong F | display-authors = 6 | title = R-Spondin potentiates Wnt/β-catenin signaling through orphan receptors LGR4 and LGR5 | journal = PLoS ONE | volume = 7 | issue = 7 | pages = e40976 | year = 2012 | pmid = 22815884 | pmc = 3397969 | doi = 10.1371/journal.pone.0040976 }}</ref> The LGR5 / R-spondin complex acts by binding and subsequently internalizing [[RNF43]] and [[ZNF3|ZNRF3]]. RNF43 and ZNRF3 are transmembrane E3 ligases that negatively regulate wnt signaling by ubiquitinating frizzled receptors.<ref>{{cite journal | vauthors = Koo BK, Spit M, Jordens I, Low TY, Stange DE, van de Wetering M, van Es JH, Mohammed S, Heck AJ, Maurice MM, Clevers H | title = Tumour suppressor RNF43 is a stem-cell E3 ligase that induces endocytosis of Wnt receptors | language = En | journal = Nature | volume = 488 | issue = 7413 | pages = 665–9 | date = August 2012 | pmid = 22895187 | doi = 10.1038/nature11308 | url = http://www.nature.com/articles/nature11308 }}</ref><ref>{{cite journal | vauthors = Hao HX, Xie Y, Zhang Y, Charlat O, Oster E, Avello M, Lei H, Mickanin C, Liu D, Ruffner H, Mao X, Ma Q, Zamponi R, Bouwmeester T, Finan PM, Kirschner MW, Porter JA, Serluca FC, Cong F | title = ZNRF3 promotes Wnt receptor turnover in an R-spondin-sensitive manner | language = En | journal = Nature | volume = 485 | issue = 7397 | pages = 195–200 | date = April 2012 | pmid = 22575959 | doi = 10.1038/nature11019 }}</ref> Thereby, R-spondin binding to LGR5 potentiates wnt signaling.<ref>{{cite journal | vauthors = de Lau W, Peng WC, Gros P, Clevers H | title = The R-spondin/Lgr5/Rnf43 module: regulator of Wnt signal strength | journal = Genes & Development | volume = 28 | issue = 4 | pages = 305–16 | date = February 2014 | pmid = 24532711 | pmc = 3937510 | doi = 10.1101/gad.235473.113 }}</ref>
 
==Clinical relevance==
 
LGR5 are well-established stem cell markers in certain types of tissue, wholly due to the fact that they are highly enriched in truly, [[Hematopoietic stem cell|multipotent stem cells]] compared to their immediate progeny, the transit-amplifying cells.
 
===Intestines===
 
[[File:Small intestine low mag.jpg|200px|thumb | Intestinal crypt structure. LGR5 stem cells are located at the bottom of the crypt]]
[[Fate mapping|Tracing]] has revealed that LGR5 is a marker of adult intestinal stem cells. The high turnover rate of the intestinal lining is due to a dedicated population of stem cells found at the base of the intestinal crypt. In the small intestines, these LGR5<sup>+ve</sup> crypt base columnar cells (CBC cells) have broad basal surfaces and very little cytoplasm and organelles and are located interspersed among the terminally differentiated Paneth cells.<ref name="Barker_2010"/> These CBC cells generate the plethora of functional cells in the intestinal tissue: Paneth cells, enteroendocrine cells, goblet cells, tuft cells, columnar cells and the M cells over an adult’s entire lifetime. Similarly, LGR5 expression in the colon resembles faithfully that of the small intestine.<ref name="Barker_2010"/>
 
===Kidney===
 
In vivo lineage tracing showed that LGR5 is expressed in nascent [[nephron]] cell cluster within the developing [[kidney]]. Specifically, the LGR5<sup>+ve</sup> stem cells contribute into the formation of the thick ascending limb of [[Loop of Henle|Henle’s loop]] and the [[distal convoluted tubule]]. However, expression is eventually truncated after postnatal day 7, a stark contrast to the facultative expression of LGR5 in actively renewing tissues such as in the intestines.<ref name="Barker_2012">{{cite journal |vauthors=Barker N, Rookmaaker MB, Kujala P, Ng A, Leushacke M, Snippert H, van de Wetering M, Tan S, Van Es JH, Huch M, Poulsom R, Verhaar MC, Peters PJ, Clevers H | title = Lgr5<sup>+ve</sup> stem/progenitor cells contribute to nephron formation during kidney development | journal = Cell Rep | volume = 2 | issue = 3 | pages = 540–52 |date=September 2012 | pmid = 22999937 | doi = 10.1016/j.celrep.2012.08.018 }}</ref>
 
===Stomach ===
 
The [[stomach]] lining also possess populations of LGR5<sup>+ve</sup> stem cells, although there are two conflicting theories: one is that LGR5<sup>+ve</sup> stem cells reside in the isthmus, the region between the pit cells and gland cells, where most cellular proliferation takes place. However, lineage tracing had revealed LGR5<sup>+ve</sup> stem cells at the bottom of the gland,<ref name="Barker_Clevers_2010">{{cite journal |vauthors=Barker N, Huch M, Kujala P, van de Wetering M, Snippert HJ, van Es JH, Sato T, Stange DE, Begthel H, van den Born M, Danenberg E, van den Brink S, Korving J, Abo A, Peters PJ, Wright N, Poulsom R, Clevers H | title = Lgr5<sup>+ve</sup> stem cells drive self-renewal in the stomach and build long-lived gastric units in vitro | journal = Cell Stem Cell | volume = 6 | issue = 1 | pages = 25–36 |date=January 2010 | pmid = 20085740 | doi = 10.1016/j.stem.2009.11.013 }}</ref> architecture reminiscent to that of the intestinal arrangement. This suggests that LGR5 stem cells give rise to transit-amplifying cells, which migrate towards the isthmus where they proliferate and maintain the stomach [[epithelium]].<ref name="Barker_2010"/>
 
===Ear===
 
LGR5<sup>+ve</sup> stem cells were pinpointed as the precursor for sensory hair cells that line the [[cochlea]].<ref name="Ruffner_2012"/>
 
===Hair follicle===
[[File:Hair follicle-en.svg|200px|thumb | Hair follicle structure where LGR5 stem cells are found in the bulge region]]
[[Hair follicle]] renewal is governed by Wnt signalling that act upon hair follicle stem cells located in the follicle bulge. Although these cells are well characterised by CD34 and cytokeratin markers, there is a growing body of agreement that LGR5 is a putative hair follicle stem cell marker.<ref name="Haegebarth_2009">{{cite journal |vauthors=Haegebarth A, Clevers H | title = Wnt signaling, lgr5, and stem cells in the intestine and skin | journal = Am. J. Pathol. | volume = 174 | issue = 3 | pages = 715–21 |date=March 2009 | pmid = 19197002 | pmc = 2665733 | doi = 10.2353/ajpath.2009.080758 | url = }}</ref> LGR5 in conjunction with LRG6, is expressed in a remarkable fashion: LRG6<sup>+ve</sup> stem cells maintain the upper sebaceous gland whilst LRG5<sup>+ve</sup> stem cells fuel the actual hair follicle shaft upon migration of transit-amplifying cells into the dermal papilla. In between these two distinct populations of stem cells are the multipotent LRG5/6<sup>+ve</sup> stem cells that ultimately maintain the epidermal hair follicle in adults.<ref name="Barker_2010"/>
 
==Cancer==
 
The [[Cancer stem cell| cancer stem cell hypothesis]] states that a dedicated small population of cancerous stem cells<ref name="Kleist_2011">{{cite journal |vauthors=Kleist B, Xu L, Li G, Kersten C | title = Expression of the adult intestinal stem cell marker Lgr5 in the metastatic cascade of colorectal cancer | journal = Int J Clin Exp Pathol | volume = 4 | issue = 4 | pages = 327–35 |date=April 2011 | pmid = 21577318 | pmc = 3093057 | doi = }}</ref> that manages to evade anti-cancer therapy maintains benign and malignant tumours. This explains recurring malignancies even after surgical removal of the [[tumor|tumour]]s.<ref name="McClanahan_2006" /> LGR5<sup>+ve</sup> stem cells were identified to fuel stem cell activity in murine intestinal adenomas via erroneous activation of the pro-cell cycle Wnt signalling pathway as a result of successive mutations, such as formation of adenoma via [[Adenomatous polyposis coli]] (APC) mutation.<ref name="Schepers_2012">{{cite journal |vauthors=Schepers AG, Snippert HJ, Stange DE, van den Born M, van Es JH, van de Wetering M, Clevers H | title = Lineage tracing reveals Lgr5<sup>+</sup> stem cell activity in mouse intestinal adenomas | journal = Science | volume = 337 | issue = 6095 | pages = 730–5 |date=August 2012 | pmid = 22855427 | doi = 10.1126/science.1224676 }}</ref> Studies on LGR5 in colorectal cancer revealed a rather perplexing mechanism: loss of LGR5 actually increased tumourigenicity and invasion whereas overexpression results a reduction in tumourigenicity and clonogenicity. This implies that LGR5 is not an [[oncogene]] but a [[tumor suppressor gene]], and that its main role is delimiting stem cell expansion in their respective niches.<ref name="Walker_2011">{{cite journal |vauthors=Walker F, Zhang HH, Odorizzi A, Burgess AW | title = LGR5 is a negative regulator of tumourigenicity, antagonizes Wnt signalling and regulates cell adhesion in colorectal cancer cell lines | journal = PLoS ONE | volume = 6 | issue = 7 | pages = e22733 | year = 2011 | pmid = 21829496 | pmc = 3145754 | doi = 10.1371/journal.pone.0022733 }}</ref> Varying expression profile of LGR5 was also observed in different stages of gastrointestinal cancers, which suggests that the histoanatomical distribution of LGR5<sup>+ve</sup> stem cells determine how the cancer advances.<ref name="Petke_2012">{{cite journal |vauthors=Simon E, Petke D, Böger C, Behrens HM, Warneke V, Ebert M, Röcken C | title = The spatial distribution of LGR5<sup>+</sup> cells correlates with gastric cancer progression | journal = PLoS ONE | volume = 7 | issue = 4 | pages = e35486 | year = 2012 | pmid = 22530031 | pmc = 3329462 | doi = 10.1371/journal.pone.0035486  }}</ref> Densitometry results of LGR5 expression by western blotting in the different cell lines showed that high LGR5 expression levels were apparent in BHK, AGS, VERO and NIH3T3 cell lines compared with the other cell lines.<ref name=" Alizadeh-Navaei _2011">{{cite journal | vauthors = Alizadeh-Navaei R, Rafiei A, Abedian-Kenari S, Asgarian-Omran H, Valadan R, Hedayatizadeh-Omran A | title = Comparison of leucine-rich repeat-containing G protein-coupled receptor 5 expression in different cancer and normal cell lines | journal = Biomedical Reports | volume = 5 | issue = 1 | pages = 130–132 | date = July 2016 | pmid = 27347416 | pmc = 4907073 | doi = 10.3892/br.2016.684 }}</ref>
 
== References ==
{{Reflist|35em}}
 
== Further reading ==
{{refbegin|35em}}
* {{cite journal |vauthors=Hsu SY, Kudo M, Chen T, Nakabayashi K, Bhalla A, van der Spek PJ, van Duin M, Hsueh AJ | title = The three subfamilies of leucine-rich repeat-containing G protein-coupled receptors (LGR): identification of LGR6 and LGR7 and the signaling mechanism for LGR7 | journal = Mol. Endocrinol. | volume = 14 | issue = 8 | pages = 1257–71 |date=August 2000 | pmid = 10935549 | doi = 10.1210/me.14.8.1257 }}
* {{cite journal |vauthors=Yamamoto Y, Sakamoto M, Fujii G, Tsuiji H, Kenetaka K, Asaka M, Hirohashi S | title = Overexpression of orphan G-protein-coupled receptor, Gpr49, in human hepatocellular carcinomas with beta-catenin mutations | journal = Hepatology | volume = 37 | issue = 3 | pages = 528–33 |date=March 2003 | pmid = 12601349 | doi = 10.1053/jhep.2003.50029 }}
{{refend}}
{{refend}}


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{{NLM content}}
{{G protein-coupled receptors}}
{{G protein-coupled receptors}}
[[Category:G protein coupled receptors]]
 
{{WikiDoc Sources}}
[[Category:G protein-coupled receptors]]

Latest revision as of 18:01, 24 September 2018

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Identifiers
Aliases
External IDsGeneCards: [1]
Orthologs
SpeciesHumanMouse
Entrez
Ensembl
UniProt
RefSeq (mRNA)

n/a

n/a

RefSeq (protein)

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Location (UCSC)n/an/a
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Leucine-rich repeat-containing G-protein coupled receptor 5 (LGR5) also known as G-protein coupled receptor 49 (GPR49) or G-protein coupled receptor 67 (GPR67) is a protein that in humans is encoded by the LGR5 gene.[1][2] It is a member of GPCR class A receptor proteins. R-spondin proteins are the biological ligands of LGR5. LGR5 is expressed across a diverse range of tissue such as in the muscle, placenta, spinal cord and brain and particularly as a biomarker of adult stem cells in certain tissues.[3]

Gene

Prior to its current naming designation, LGR5 was also known as FEX, HG38, GPR49, and GPR67.[4] The Human LGR5 gene is 144,810 bases long and located at chromosome 12 at position 12q22-q23.[4] Both human, rat and mouse homologs contain 907 amino acids and seven transmembrane domains.[5] After translation, the signal peptide (amino acids 1-21) is cleaved off and the mature peptide (amino acids 22-907) inserts its transmembrane domain into the translocon membrane prior to packaging towards the plasma membrane.

Protein structure

LGR5 is highly conserved within the mammalian clade. Sequence analyses showed that the transmembrane regions and cysteine-flanked junction between TM1 and the extracellular domain were highly conserved in sea anemone (Anthopleura elegantissima), fly (Drosophila melanogaster), worm (Caenorhabditis elegans), snail (Lymnaea stagnalis), rat (Rattus rattus) and human (Homo sapiens).[3] Homology amongst the metazoan suggests that it has been conserved across animals and was hypothesised as a chimeric fusion of an ancestral GPCR and a leucine-rich repeat motif.

Sheau Hsu, Shan Liang and Aaron Hsueh first identified LGR5, together with LGR4, in 1998 at the University Medical School Stanford, California using expression sequence tags based on putative glycoprotein hormone receptors in Drosophila.[3]

Experimental evidence show that the mature receptor protein contains up to 17 leucine-rich repeats, each composed of 24 amino acids spanning the extracellular domain flanked by the cysteine-rich N-terminal and C-terminal regions. In contrast, other glycoprotein hormone receptors such as Luteinizing hormone, Follicle-stimulating hormone and Thyroid-stimulating hormone contain only 9 repeats.[3] Sequence alignment showed that the second N-glycosylation site in LGR5 (Asn 208) aligns with that on the sixth repeat of gonadotropin and TSH receptors. The cysteine residues flanking the ectodomain form stabilising disulfide bonds that support the secondary structure of the leucine-rich repeats.

Function

LGR5 is a member of the Wnt signaling pathway. Although its ligand remains elusive, it has been shown that costimulation with R-spondin 1 and Wnt-3a induce increased internalization of LGR5. LGR5 also cointernalizes with LRP6 and FZD5 via a clathrin-dependent pathway to form a ternary complex upon Wnt ligand binding. Moreover, the rapid cointernalization of LRP6 by LGR5 induces faster rates of degradation for the former. It has been shown that the C-terminal region of LGR5 is crucial for both dynamic internalization and degradation to occur, although C-terminal truncation does not inhibit LRP6 interaction and internalization, but rather, heightens receptor activity. Thus, only the initial interaction with its unknown ligand and other membrane bound receptors is crucial in its role in Wnt signalling and not the internalization itself.[6] LGR5 is crucial during embryogenesis as LGR null studies in mice incurred 100% neonatal mortality accompanied by several craniofacial distortions such as ankyloglossia and gastrointestinal dilation.[7]

Ligand

LGR5 belongs to a class of class A GPCR orphan receptors. Thus its ligands remain elusive. However, it has been shown that Lgr2, the fly orthologue of mammalian LGR5, binds with "high affinity and specificity" with bursicon, an insect heterodimeric, neurohormone that belongs in the same class as FSH, LH and TSH, which in turn are homologous to mammalian bone morphogenetic factors (BMPs) such as gremlin and cerberus. Therefore, LGR5 might be a receptor for a member of the large family of bone morphogenetic protein antagonists.[8] Moreover, R-spondin proteins were shown to interact with the extracellular domain of LRG5.[9] The LGR5 / R-spondin complex acts by binding and subsequently internalizing RNF43 and ZNRF3. RNF43 and ZNRF3 are transmembrane E3 ligases that negatively regulate wnt signaling by ubiquitinating frizzled receptors.[10][11] Thereby, R-spondin binding to LGR5 potentiates wnt signaling.[12]

Clinical relevance

LGR5 are well-established stem cell markers in certain types of tissue, wholly due to the fact that they are highly enriched in truly, multipotent stem cells compared to their immediate progeny, the transit-amplifying cells.

Intestines

File:Small intestine low mag.jpg
Intestinal crypt structure. LGR5 stem cells are located at the bottom of the crypt

Tracing has revealed that LGR5 is a marker of adult intestinal stem cells. The high turnover rate of the intestinal lining is due to a dedicated population of stem cells found at the base of the intestinal crypt. In the small intestines, these LGR5+ve crypt base columnar cells (CBC cells) have broad basal surfaces and very little cytoplasm and organelles and are located interspersed among the terminally differentiated Paneth cells.[8] These CBC cells generate the plethora of functional cells in the intestinal tissue: Paneth cells, enteroendocrine cells, goblet cells, tuft cells, columnar cells and the M cells over an adult’s entire lifetime. Similarly, LGR5 expression in the colon resembles faithfully that of the small intestine.[8]

Kidney

In vivo lineage tracing showed that LGR5 is expressed in nascent nephron cell cluster within the developing kidney. Specifically, the LGR5+ve stem cells contribute into the formation of the thick ascending limb of Henle’s loop and the distal convoluted tubule. However, expression is eventually truncated after postnatal day 7, a stark contrast to the facultative expression of LGR5 in actively renewing tissues such as in the intestines.[13]

Stomach

The stomach lining also possess populations of LGR5+ve stem cells, although there are two conflicting theories: one is that LGR5+ve stem cells reside in the isthmus, the region between the pit cells and gland cells, where most cellular proliferation takes place. However, lineage tracing had revealed LGR5+ve stem cells at the bottom of the gland,[14] architecture reminiscent to that of the intestinal arrangement. This suggests that LGR5 stem cells give rise to transit-amplifying cells, which migrate towards the isthmus where they proliferate and maintain the stomach epithelium.[8]

Ear

LGR5+ve stem cells were pinpointed as the precursor for sensory hair cells that line the cochlea.[9]

Hair follicle

File:Hair follicle-en.svg
Hair follicle structure where LGR5 stem cells are found in the bulge region

Hair follicle renewal is governed by Wnt signalling that act upon hair follicle stem cells located in the follicle bulge. Although these cells are well characterised by CD34 and cytokeratin markers, there is a growing body of agreement that LGR5 is a putative hair follicle stem cell marker.[15] LGR5 in conjunction with LRG6, is expressed in a remarkable fashion: LRG6+ve stem cells maintain the upper sebaceous gland whilst LRG5+ve stem cells fuel the actual hair follicle shaft upon migration of transit-amplifying cells into the dermal papilla. In between these two distinct populations of stem cells are the multipotent LRG5/6+ve stem cells that ultimately maintain the epidermal hair follicle in adults.[8]

Cancer

The cancer stem cell hypothesis states that a dedicated small population of cancerous stem cells[16] that manages to evade anti-cancer therapy maintains benign and malignant tumours. This explains recurring malignancies even after surgical removal of the tumours.[2] LGR5+ve stem cells were identified to fuel stem cell activity in murine intestinal adenomas via erroneous activation of the pro-cell cycle Wnt signalling pathway as a result of successive mutations, such as formation of adenoma via Adenomatous polyposis coli (APC) mutation.[17] Studies on LGR5 in colorectal cancer revealed a rather perplexing mechanism: loss of LGR5 actually increased tumourigenicity and invasion whereas overexpression results a reduction in tumourigenicity and clonogenicity. This implies that LGR5 is not an oncogene but a tumor suppressor gene, and that its main role is delimiting stem cell expansion in their respective niches.[18] Varying expression profile of LGR5 was also observed in different stages of gastrointestinal cancers, which suggests that the histoanatomical distribution of LGR5+ve stem cells determine how the cancer advances.[19] Densitometry results of LGR5 expression by western blotting in the different cell lines showed that high LGR5 expression levels were apparent in BHK, AGS, VERO and NIH3T3 cell lines compared with the other cell lines.[20]

References

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  3. 3.0 3.1 3.2 3.3 Hsu SY, Liang SG, Hsueh AJ (December 1998). "Characterization of two LGR genes homologous to gonadotropin and thyrotropin receptors with extracellular leucine-rich repeats and a G protein-coupled, seven-transmembrane region". Mol. Endocrinol. 12 (12): 1830–45. doi:10.1210/me.12.12.1830. PMID 9849958.
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  10. Koo BK, Spit M, Jordens I, Low TY, Stange DE, van de Wetering M, van Es JH, Mohammed S, Heck AJ, Maurice MM, Clevers H (August 2012). "Tumour suppressor RNF43 is a stem-cell E3 ligase that induces endocytosis of Wnt receptors". Nature. 488 (7413): 665–9. doi:10.1038/nature11308. PMID 22895187.
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  13. Barker N, Rookmaaker MB, Kujala P, Ng A, Leushacke M, Snippert H, van de Wetering M, Tan S, Van Es JH, Huch M, Poulsom R, Verhaar MC, Peters PJ, Clevers H (September 2012). "Lgr5+ve stem/progenitor cells contribute to nephron formation during kidney development". Cell Rep. 2 (3): 540–52. doi:10.1016/j.celrep.2012.08.018. PMID 22999937.
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  15. Haegebarth A, Clevers H (March 2009). "Wnt signaling, lgr5, and stem cells in the intestine and skin". Am. J. Pathol. 174 (3): 715–21. doi:10.2353/ajpath.2009.080758. PMC 2665733. PMID 19197002.
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  18. Walker F, Zhang HH, Odorizzi A, Burgess AW (2011). "LGR5 is a negative regulator of tumourigenicity, antagonizes Wnt signalling and regulates cell adhesion in colorectal cancer cell lines". PLoS ONE. 6 (7): e22733. doi:10.1371/journal.pone.0022733. PMC 3145754. PMID 21829496.
  19. Simon E, Petke D, Böger C, Behrens HM, Warneke V, Ebert M, Röcken C (2012). "The spatial distribution of LGR5+ cells correlates with gastric cancer progression". PLoS ONE. 7 (4): e35486. doi:10.1371/journal.pone.0035486. PMC 3329462. PMID 22530031.
  20. Alizadeh-Navaei R, Rafiei A, Abedian-Kenari S, Asgarian-Omran H, Valadan R, Hedayatizadeh-Omran A (July 2016). "Comparison of leucine-rich repeat-containing G protein-coupled receptor 5 expression in different cancer and normal cell lines". Biomedical Reports. 5 (1): 130–132. doi:10.3892/br.2016.684. PMC 4907073. PMID 27347416.

Further reading

  • Hsu SY, Kudo M, Chen T, Nakabayashi K, Bhalla A, van der Spek PJ, van Duin M, Hsueh AJ (August 2000). "The three subfamilies of leucine-rich repeat-containing G protein-coupled receptors (LGR): identification of LGR6 and LGR7 and the signaling mechanism for LGR7". Mol. Endocrinol. 14 (8): 1257–71. doi:10.1210/me.14.8.1257. PMID 10935549.
  • Yamamoto Y, Sakamoto M, Fujii G, Tsuiji H, Kenetaka K, Asaka M, Hirohashi S (March 2003). "Overexpression of orphan G-protein-coupled receptor, Gpr49, in human hepatocellular carcinomas with beta-catenin mutations". Hepatology. 37 (3): 528–33. doi:10.1053/jhep.2003.50029. PMID 12601349.

This article incorporates text from the United States National Library of Medicine, which is in the public domain.