DCC

DCC
Dostupne strukture
PDB	Pretraga ortologa: PDBe RCSB
Spisak PDB ID kodova
	2ED7, 2ED8, 2ED9, 2EDB, 2EDD, 2EDE, 3AU4, 4URT
Identifikatori
Aliasi	DCC
Vanjski ID-jevi	OMIM: 120470 MGI: 94869 HomoloGene: 21081 GeneCards: DCC
Lokacija gena (čovjek)
Hrom.	Hromosom 18 (čovjek)
Kraj	53,535,903 bp
Lokacija gena (miš)
Hrom.	Hromosom 18 (miš)
Kraj	72,484,140 bp
Ontologija gena
Molekularna funkcija	• GO:0001948, GO:0016582 vezivanje za proteine; • netrin receptor activity; • transmembrane signaling receptor activity;
Ćelijska komponenta	• integral component of membrane; • citosol; • membrana; • ćelijska membrana; • Akson; • Schaffer collateral - CA1 synapse; • integral component of postsynaptic density membrane;
Biološki proces	• dorsal/ventral axon guidance; • negative regulation of neuron projection development; • axonogenesis; • netrin-activated signaling pathway; • neuron migration; • nervous system development; • negative regulation of dendrite development; • axon guidance; • multicellular organism development; • negative regulation of collateral sprouting; • regulation of neuron death; • extrinsic apoptotic signaling pathway in absence of ligand; • spinal cord ventral commissure morphogenesis; • anterior/posterior axon guidance; • GO:0097285 apoptoza; • negative regulation of netrin-activated signaling pathway; • postsynaptic modulation of chemical synaptic transmission;
	Izvori:Amigo / QuickGO
Ortolozi
	1630
	13176
	ENSG00000187323
	ENSMUSG00000060534
	P43146
	P70211
	NM_005215
	NM_007831
	NP_005206
	NP_031857
	Wikipodaci
Pogledaj/uredi – čovjek	Pogledaj/uredi – miš

Deletirani protein kolorektumskog karcinoma, znan i kao DCC, je protein koji je kod ljudi kodiran genom DCC. Odavno je uplitan u rak debelog crijeva.^[5]

Odkad je prvi put otkriven u studiji kolorektumskog karcinoma 1990,^[6] bio je u fokusu značajnog broja istraživanja. DCC je godinama imao kontroverzno mjesto kao gen supresije tumora i dobro je poznat kao receptor provodljivost aksona, koji reagira na netrin-1.^[7]

U novije vrijeme DCC je okarakteriziran kao receptor ovisnosti, a iznesene su mnoge hipoteze koje su oživile interes za kandidaturu DCC kao gena za supresiju tumora, jer to može biti ovisno o ligandu koji se često epigenetički utišava.^[8]

Gen DCC nalazi se na lokusu 18q21.3 i ima ukupno 57 mogućih egzona i 43 moguća introna. Ovo teorijski rezultira sa 13 pravilno prerađenih, navodno dobrih proteina. Dužina polipeptidnog lanca je 1.447 aminokiselina, a molekulska težina — 158.457.^[9]^[10] Tipskii DCC protein ima jedan signalni motiv peptida i jedanaest domena, uključujući višestruke domene slične imunoglobulinu, transmembranski domen i nekoliko domena fibronektina tipa 3.^[11]

DCC ima vanćelijska mjesta vezanja i za netrin-1 i za heparin. Smatra se da je heparin-sulfat takođe prisutan tokom nevrnog rasta, kao tip kofaktora za aksonsko provođenje.^[12]^[13] Pokazano je da DCC unutarćelijski ima mjesto proteolize kaspaze-3 na Asp 1290.

DCC i neogenin, dva od netrin-1 receptora, nedavno su pokazali da imaju mjesta za fosforilaciju tirozina (na Y1420 na DCC) i vjerovatno stupaju u interakciju sa porodicom Src kinaze u regulaciji odgovora na netrin-1.^[14]

Aminokiselinska sekvenca: Simboli

C: Cistein
D: Asparaginska kiselina
E: Glutaminska kiselina
F: Fenilalanin
G: Glicin
H: Histidin
I: Izoleucin
K: Lizin
L: Leucin
M: Metionin
N: Asparagin
P: Prolin
Q: Glutamin
R: Arginin
S: Serin
T: Treonin
V: Valin
W: Triptofan
Y: Tirozin

10	20	30	40	50
MENSLRCVWV	PKLAFVLFGA	SLFSAHLQVT	GFQIKAFTAL	RFLSEPSDAV
TMRGGNVLLD	CSAESDRGVP	VIKWKKDGIH	LALGMDERKQ	QLSNGSLLIQ
NILHSRHHKP	DEGLYQCEAS	LGDSGSIISR	TAKVAVAGPL	RFLSQTESVT
AFMGDTVLLK	CEVIGEPMPT	IHWQKNQQDL	TPIPGDSRVV	VLPSGALQIS
RLQPGDIGIY	RCSARNPASS	RTGNEAEVRI	LSDPGLHRQL	YFLQRPSNVV
AIEGKDAVLE	CCVSGYPPPS	FTWLRGEEVI	QLRSKKYSLL	GGSNLLISNV
TDDDSGMYTC	VVTYKNENIS	ASAELTVLVP	PWFLNHPSNL	YAYESMDIEF
ECTVSGKPVP	TVNWMKNGDV	VIPSDYFQIV	GGSNLRILGV	VKSDEGFYQC
VAENEAGNAQ	TSAQLIVPKP	AIPSSSVLPS	APRDVVPVLV	SSRFVRLSWR
PPAEAKGNIQ	TFTVFFSREG	DNRERALNTT	QPGSLQLTVG	NLKPEAMYTF
RVVAYNEWGP	GESSQPIKVA	TQPELQVPGP	VENLQAVSTS	PTSILITWEP
PAYANGPVQG	YRLFCTEVST	GKEQNIEVDG	LSYKLEGLKK	FTEYSLRFLA
YNRYGPGVST	DDITVVTLSD	VPSAPPQNVS	LEVVNSRSIK	VSWLPPPSGT
QNGFITGYKI	RHRKTTRRGE	METLEPNNLW	YLFTGLEKGS	QYSFQVSAMT
VNGTGPPSNW	YTAETPENDL	DESQVPDQPS	SLHVRPQTNC	IIMSWTPPLN
PNIVVRGYII	GYGVGSPYAE	TVRVDSKQRY	YSIERLESSS	HYVISLKAFN
NAGEGVPLYE	SATTRSITDP	TDPVDYYPLL	DDFPTSVPDL	STPMLPPVGV
QAVALTHDAV	RVSWADNSVP	KNQKTSEVRL	YTVRWRTSFS	ASAKYKSEDT
TSLSYTATGL	KPNTMYEFSV	MVTKNRRSST	WSMTAHATTY	EAAPTSAPKD
LTVITREGKP	RAVIVSWQPP	LEANGKITAY	ILFYTLDKNI	PIDDWIMETI
SGDRLTHQIM	DLNLDTMYYF	RIQARNSKGV	GPLSDPILFR	TLKVEHPDKM
ANDQGRHGDG	GYWPVDTNLI	DRSTLNEPPI	GQMHPPHGSV	TPQKNSNLLV
IIVVTVGVIT	VLVVVIVAVI	CTRRSSAQQR	KKRATHSAGK	RKGSQKDLRP
PDLWIHHEEM	EMKNIEKPSG	TDPAGRDSPI	QSCQDLTPVS	HSQSETQLGS
KSTSHSGQDT	EEAGSSMSTL	ERSLAARRAP	RAKLMIPMDA	QSNNPAVVSA
IPVPTLESAQ	YPGILPSPTC	GYPHPQFTLR	PVPFPTLSVD	RGFGAGRSQS
VSEGPTTQQP	PMLPPSQPEH	SSSEEAPSRT	IPTACVRPTH	PLRSFANPLL
PPPMSAIEPK	VPYTPLLSQP	GPTLPKTHVK	TASLGLAGKA	RSPLLPVSVP
TAPEVSEESH	KPTEDSANVY	EQDDLSEQMA	SLEGLMKQLN	AITGSAF

Uloga u raku

Jedna od najčešćih genetičkih abnormalnosti koja se javlja u uznapredovalom raku debelog crijeva je gubitak heterozigotnosti (LOH) DCC u regiji 18q21.

DCC u receptoru za netrin-1 i za neke druge, vjeruje se da je uslovni gen za supresiju tumora, što znači da normalno sprečava rast ćelija u odsustvu netrina-1. Vjeruje se da eliminacija DCC nije ključna genetička promjena u stvaranju tumora, već jedna od mnogih koje mogu promovirati postojeći rast tumora. Moguća uloga DCC-a u migraciji ćelija karcinoma je u procesu karakterizacije.

Iako nedavni rezultati čine prilično vjerojatnim da je DCC uključen u biologiju nekoliko karcinoma, opseg njegove uključenosti i detalji o tome kako djeluju još uvijek se proučavaju.

Normalna funkcija u supresiji i apoptozi tumora

Kada nije vezan za netrin-1, unutarćelijski domen DCC-a se cijepa pomoću kaspaza i inducira apoptozu na putu koji ovisi o kaspazi-9. Ovaj domen ne odgovara poznatom motivu regrutiranja kaspaze ili domenu sekvence ćelijke smrti, ali je potreban za iniciranje apoptoze. Teoretizirano je da domen djeluje kao skela za angažiranje i aktiviranje kaspaze-9 i kaspaze-3. Ovaj put DCC-apoptoze ne ovisi ni o putu mitohondrijske apoptoze, ni o putu receptora ćelijske smrti/kaspaze-8.^[15] U nedostatku liganda, DCC stupa u interakciju sa kaspazom-9 (vjerovatno putem neidentificiranog proteinskog adaptera) i promovira skup kompleksa koji aktivira kaspazu. To uzrokuje aktivaciju kaspaze-3, preko kaspazu-9 i pokreće apoptozu bez stvaranja apoptosoma ili oslobađanja citohroma c. To implicira da DCC regulira novi put za aktivaciju kaspaze i da je onaj koji je nezavisan od apoptosoma.

Da bi se ovo stavilo u kontekst bioloških sistema, potrebna je određena fiziologija. U gastrointestinalnom traktu, epitelne ćelije se umnožavaju i brzo umiru. Podjela ovih ćelija događa se u osnovi resica, a one se potiskuju prema gore, naknadnim diobama, do vrha, gdje ulaze u apoptozu i odlijevaju se u lumen. Netrin-1 se proizvodi u osnovi resica, pa je prisutan njegov gradijent, koji je najslabiji na vrhu. U normalnom fiziološkom procesu, prisustvo netrina-1 inhibira DCC-posredovanu ćelijsku smrt dok epitelna ćelija ne dođe do vrha resice, gdje tada nevezani DCC pokreće apoptozu. U stanju karcinoma, odsustvo DCC sprečava gradijent da djeluje na ćeliju, što čini vjerovatnijim da će i dalje opstati.

Uloga DCC-a kao supresora tumora vezana je za karakteristike zavisnosti receptora. Kada nije vezan netrin-1, DCC inducira ćelijsku smrt epitelnih ćelija. Pored gubitka heterozigotnosti DCC-a, ovaj mehanizam apoptoze može se izbjeći i u malignim procesima prekomjernom ekspresijom netrina.

Mehanizam delecije

Prvobitno se vjerovalo da postoje dva glavna puta u stvaranju kolorektumskog karcinoma. Prvi je bio put hromosomske nestabilnosti, za koji se mislilo da je odgovoran za napredovanje adenoma do karcinoma, koji je karakteriziran gubitkom heterozigotnosti (LOH) na hromosomskim pozicijama 5q, 17p i 18q. Smatralo se da je drugi put mikrosatelitska nestabilnost, koji karakterizira povećanje ili smanjenje broja tandemskih ponavljanja jednostavnih sekvenci DNK. Ovaj tip nestabilnosti povezan je sa nekim specifičnim mutacijama, uključujući gene koji su uključeni u neusklađenosti DNK i, začudo, transformišući faktor rasta-beta. U novije vrijeme, u oblasti kolorektalnog karcinoma priznali su da je stvaranje raka mnogo složenije, ali geni povezani sa rakom i dalje imaju tendenciju da se kategoriziraju kao hromosomski ili mikrosatelitski geni nestabilnosti.^[16]

DCC bi spadao u kategoriju hromosomske nestabilnosti. Hromosomsko područje 18q pokazuje postojani LOH gotovo dvadeset godina. Otprilike 70% primarnih karcinoma debelog crijeva pokazuje LOH u ovoj regiji, a procenat se povećava kada se porede rani sa uznapredovalim karcinomima. Ovaj porast gubitka DCC u uznapredovalom raku može ukazati na to da je gubitak DCC važniji za progresiju tumora nego formiranje tumora. Međutim, regija 18q nije samo mjesto DCC-a, a mnoge su studije u sukobu kada izvještavaju da li se 18q LOH može pripisati DCC-u ili drugim kandidatima za supresore tumora u susjednim područjima. Mnoge recenzije odbijaju komentirati DCC zbog njegove povijesti sukobljenih informacija, navodeći da je potrebno dodatno proučavanje.

LOH hromosoma 18 ima tendenciju da se javlja u klasterima. Jedna od glavnih grupa nalazi se na 18q21, što se slaže s lokacijom DCC-a. Ova skupina uključuje marker D18S51, a uz nju su lokusi D18S1109 i D18S68. Ovaj segment obuhvata 7,64 kb, što je relativno velik dio DNK koji lahko može obuhvatiti više od jednog gena za supresiju tumora.^[17]

Značajna razlika između ekspresije DCC i 18q21 LOH otkrivena je 1997. Studije su otkrile da više tumora ima smanjenu ekspresiju DCC nego što se može objasniti LOH ili MSI, što ukazuje da je na djelu drugi mehanizam.^[18] Ovo zapažanje je vjerovatno objašnjeno kada je izvedena epigenetička analiza.

Epigenetika

Gubitak DCC u raku debelog crijeva prvenstveno se javlja hromosomskom nestabilnošću, a samo mali procenat uključuje epigenetičko prigušivanje.

Epigenetičko utišavanje DCC-a hipermetilacijom promotora pokazalo se značajnim faktorom u drugim tipovima karcinoma. U karcinomu skvamoznih ćelija glave i vrata, 77,3% uzoraka tumora ispoljilo je hipermetilaciju DCC promotora u odnosu na 0,8% u uzorcima nekancerozne pljuvačke.^[19] Slični rezultati viđeni su kod raka dojke, akutne limfoblastne leukemije i nekoliko drugih.

Metastaze

Povećanje procenta gubitka heterozigotnosti hromosomskog srgmenta 18q21 već dugo sugerira da bi DCC mogao biti uključen u napredovanje benignih adenoma u maligne karcinome.^[20] Nedavno je utvrđeno da DCC suzbija metastaze u eksperimentalnom okruženju, ali mehanizam za to još nije predložen.^[21]

Farmakologija

Na ovom spoju, DCC nije farmaceutska meta. Kako DCC nije prekomjerno izražen u raku i prisutan je u cijelom tijelu, tako se ne smatra dobrom metom za većinu vrsta lijekova protiv raka.

DCC se eksprimira na vrlo niskim nivoima kroz veći dio tijela, ali na višim u mnogim dijelovima mozga, posebno u dopaminskim neuronima. Nedavno je pokazano da režim senzibilizacije amfetamina uzrokuje izrazito povećane nivoe ekspresije DCC i UNC-5 na tijelima neuronskih ćelija. To može ukazivati na to da su receptori za netrin-1 uključeni u trajne efekte izloženosti stimulativnim lijekovima poput amfetamina i mogu imati neku terapeutsku vrijednost na polju tolerancije na lijekove.^[22]

Interakcije

Pokazalo se da deletirani protein u kolorektumskom karcinomu ima interakcije sa:

Reference

^ ^a ^b ^c GRCh38: Ensembl release 89: ENSG00000187323 - Ensembl, maj 2017
^ ^a ^b ^c GRCm38: Ensembl release 89: ENSMUSG00000060534 - Ensembl, maj 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.
^ NCBI Website for DCC
^ Fearon ER, Cho KR, Nigro JM, Kern SE, Simons JW, Ruppert JM, Hamilton SR, Preisinger AC, Thomas G, Kinzler KW (januar 1990). "Identification of a chromosome 18q gene that is altered in colorectal cancers". Science. 247 (4938): 49–56. doi:10.1126/science.2294591. PMID 2294591.
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^ "UniProt, P43146". Pristupljeno 12. 9. 2017.
^ AceView: Homo sapiens complex locus DCC, encoding deleted in colorectal carcinoma
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^ "Human Protein Reference Database: DCC". Arhivirano s originala, 2. 6. 2021. Pristupljeno 2. 6. 2021.
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^ Rodrigues S, De Wever O, Bruyneel E, Rooney RJ, Gespach C (august 2007). "Opposing roles of netrin-1 and the dependence receptor DCC in cancer cell invasion, tumor growth and metastasis". Oncogene. 26 (38): 5615–25. doi:10.1038/sj.onc.1210347. PMID 17334389.
^ Yetnikoff L, Labelle-Dumais C, Flores C (decembar 2007). "Regulation of netrin-1 receptors by amphetamine in the adult brain". Neuroscience. 150 (4): 764–73. doi:10.1016/j.neuroscience.2007.09.069. PMC 4880477. PMID 17996376.
^ Liu J, Yao F, Wu R, Morgan M, Thorburn A, Finley RL, Chen YQ (Jul 2002). "Mediation of the DCC apoptotic signal by DIP13 alpha". J. Biol. Chem. 277 (29): 26281–5. doi:10.1074/jbc.M204679200. PMID 12011067.
^ Wafa LA, Cheng H, Rao MA, Nelson CC, Cox M, Hirst M, Sadowski I, Rennie PS (Oct 2003). "Isolation and identification of L-dopa decarboxylase as a protein that binds to and enhances transcriptional activity of the androgen receptor using the repressed transactivator yeast two-hybrid system". Biochem. J. 375 (Pt 2): 373–83. doi:10.1042/BJ20030689. PMC 1223690. PMID 12864730.
^ Forcet C, Ye X, Granger L, Corset V, Shin H, Bredesen DE, Mehlen P (Mar 2001). "The dependence receptor DCC (deleted in colorectal cancer) defines an alternative mechanism for caspase activation". Proc. Natl. Acad. Sci. U.S.A. 98 (6): 3416–21. doi:10.1073/pnas.051378298. PMC 30668. PMID 11248093.
^ Ugai H, Li HO, Komatsu M, Tsutsui H, Song J, Shiga T, Fearon E, Murata T, Yokoyama KK (Sep 2001). "Interaction of Myc-associated zinc finger protein with DCC, the product of a tumor-suppressor gene, during the neural differentiation of P19 EC cells". Biochem. Biophys. Res. Commun. 286 (5): 1087–97. doi:10.1006/bbrc.2001.5469. PMID 11527412.
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Vanjski linkovi

[refGRCh38Ensembl-1] GRCh38: Ensembl release 89: ENSG00000187323 - Ensembl, maj 2017

[refGRCm38Ensembl-2] GRCm38: Ensembl release 89: ENSMUSG00000060534 - Ensembl, maj 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] NCBI Website for DCC

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