PARK2

Razlikovati: Parkin (čvor).

Parkin je protein koji je kod ljudi kodiran genom PARK2. To je E3 ubikvitin-ligaza od 465 ostataka koji ima kritičnu ulogu u ubikvitinaciji – procesu kojim su molekule kovalentno povezane sa ubikvitinom (Ub) i usmjerene prema razgradnji u proteasomima ili lizosomima. Ubikvitinacija uključuje uzastopno djelovanje tri enzima. E1 enzim koji aktivira ubikvitin u eukariotskim ćelijama veže se za neaktivni Ub putem tioesterskih veza i mobilizira ga u procesu ovisnom o ATP-u. (2) Ub se zatim prenosi u E2 enzim koji konjuguje ubikvitin prije nego što se konjugira sa ciljnim proteinom preko E3 ubikvitin-ligaza.^[5] Postoji mnoštvo E3 ligaza, koje se razlikuju po strukturi i specifičnosti supstrat, kako bi omogućile selektivno ciljanje proteina za unutarćelijsku degradaciju.

PRKN
Dostupne strukture PDB Pretraga ortologa: PDBe RCSB Spisak PDB ID kodova 1IYF, 2JMO, 4I1F, 4I1H, 4BM9, 5C1Z, 5C23, 5C9V
Identifikatori
Aliasi	PRKN
Vanjski ID-jevi	OMIM: 602544 MGI: 1355296 HomoloGene: 3355 GeneCards: PRKN
Lokacija gena (čovjek) Hrom. Hromosom 6 (čovjek)[1] Bend 6q26 Početak 161,347,417 bp[1] Kraj 162,727,775 bp[1]
Lokacija gena (miš) Hrom. Hromosom 17 (miš)[2] Bend 17 A1|17 7.8 cM Početak 11,059,271 bp[2] Kraj 12,282,248 bp[2]
Obrazac RNK ekspresije Više referentnih podataka o ekspresiji
Ontologija gena Molekularna funkcija • phospholipase binding • GO:0001131, GO:0001151, GO:0001130, GO:0001204 DNA-binding transcription factor activity • SH3 domain binding • histone deacetylase binding • vezivanje tubulina • cullin family protein binding • PDZ domain binding • heat shock protein binding • vezivanje iona metala • Hsp70 protein binding • kinase binding • vezivanje enzima • beta-catenin binding • vezivanje iona cinka • GO:0001948, GO:0016582 vezivanje za proteine • ubiquitin conjugating enzyme binding • protein kinase binding • chaperone binding • GO:0000975 transcription cis-regulatory region binding • GO:0050372 aktivnost sa transferazom ubikvitina • F-box domain binding • ubiquitin binding • vezivanje identičnih proteina • actin binding • ubiquitin-specific protease binding • G protein-coupled receptor binding • ubiquitin protein ligase binding • aktivnost sa transferazom • GO:1904264, GO:1904822, GO:0090622, GO:0090302 ubiquitin protein ligase activity • GO:0001078, GO:0001214, GO:0001206 DNA-binding transcription repressor activity, RNA polymerase II-specific • GO:0032403 protein-containing complex binding Ćelijska komponenta • citoplazma • citosol • mitohondrija • perinuklearno područje citoplazme • jedro • Lewy body • SCF ubiquitin ligase complex • aggresome • Endoplazmatski retikulum • Golđijev aparat • Parkin-FBXW7-Cul1 ubiquitin ligase complex • kompleks ubikvitin-ligaze • LUBAC complex • presynapse • neuron projection • mitochondrion-derived vesicle • nuclear speck • GO:0009327 makromolekulani kompleks Biološki proces • GO:1904089 negative regulation of neuron apoptotic process • protein K29-linked ubiquitination • negative regulation of insulin secretion • ERAD pathway • positive regulation of mitochondrial fission • positive regulation of mitophagy in response to mitochondrial depolarization • GO:1903364 positive regulation of protein catabolic process • synaptic transmission, glutamatergic • positive regulation of tumor necrosis factor-mediated signaling pathway • neuron cellular homeostasis • regulation of protein ubiquitination • cellular response to toxic substance • modulation of chemical synaptic transmission • regulation of synaptic vesicle transport • Učenje • protein monoubiquitination • synaptic transmission, dopaminergic • positive regulation of neurotransmitter uptake • regulation of glucose metabolic process • protein K6-linked ubiquitination • negative regulation of intrinsic apoptotic signaling pathway by p53 class mediator • negative regulation of spontaneous neurotransmitter secretion • negative regulation by host of viral genome replication • positive regulation of DNA binding • macroautophagy • negative regulation of canonical Wnt signaling pathway • Unfolded Protein Response • aggresome assembly • proteasome-mediated ubiquitin-dependent protein catabolic process • regulation of dopamine secretion • zinc ion homeostasis • free ubiquitin chain polymerization • GO:0009373 regulation of transcription, DNA-templated • locomotory behavior • norepinephrine metabolic process • negative regulation of endoplasmic reticulum stress-induced neuron intrinsic apoptotic signaling pathway • adult locomotory behavior • GO:0044267 protein metabolic process • negative regulation of cell death • GO:0001306 response to oxidative stress • protein K27-linked ubiquitination • negative regulation of gene expression • transcription, DNA-templated • response to endoplasmic reticulum stress • protein K11-linked ubiquitination • central nervous system development • negative regulation of oxidative stress-induced cell death • positive regulation of mitochondrial fusion • protein localization to mitochondrion • proteasomal protein catabolic process • cellular response to manganese ion • negative regulation of mitochondrial fusion • protein autoubiquitination • negative regulation of neuron death • GO:0033128 negative regulation of protein phosphorylation • negative regulation of endoplasmic reticulum stress-induced intrinsic apoptotic signaling pathway • negative regulation of primary amine oxidase activity • startle response • mitochondrial fission • regulation of mitochondrion organization • regulation of canonical Wnt signaling pathway • negative regulation of release of cytochrome c from mitochondria • protein stabilization • mitochondrion organization • protein polyubiquitination • GO:1901227 negative regulation of transcription by RNA polymerase II • GO:1904489 regulation of reactive oxygen species metabolic process • regulation of neurotransmitter secretion • positive regulation of protein linear polyubiquitination • protein K48-linked ubiquitination • dopamine uptake involved in synaptic transmission • regulation of autophagy • regulation of protein targeting to mitochondrion • protein destabilization • negative regulation of glucokinase activity • positive regulation of proteasomal protein catabolic process • protein K63-linked ubiquitination • cellular response to dopamine • regulation of lipid transport • negative regulation of actin filament bundle assembly • regulation of dopamine metabolic process • regulation of mitochondrial membrane potential • Autofagija • negative regulation of JNK cascade • dopamine metabolic process • GO:1901313 positive regulation of gene expression • positive regulation of I-kappaB kinase/NF-kappaB signaling • positive regulation of dendrite extension • negative regulation of reactive oxygen species metabolic process • GO:0003257, GO:0010735, GO:1901228, GO:1900622, GO:1904488 positive regulation of transcription by RNA polymerase II • mitophagy • protein ubiquitination • parkin-mediated stimulation of mitophagy in response to mitochondrial depolarization • positive regulation of proteasomal ubiquitin-dependent protein catabolic process • protein deubiquitination • regulation of protein stability • positive regulation of protein binding • mitochondrion to lysosome transport • regulation of cellular response to oxidative stress • negative regulation of exosomal secretion • positive regulation of retrograde transport, endosome to Golgi • negative regulation of intralumenal vesicle formation • positive regulation of protein localization to membrane • autophagy of mitochondrion • negative regulation of oxidative stress-induced neuron intrinsic apoptotic signaling pathway • positive regulation of autophagy of mitochondrion • ubiquitin-dependent protein catabolic process • regulation of apoptotic process Izvori:Amigo / QuickGO
Ortolozi
Vrste	Čovjek	Miš
Entrez	5071	50873
Ensembl	ENSG00000185345	ENSMUSG00000023826
UniProt	O60260	Q9WVS6
RefSeq (mRNK)	NM_004562 NM_013987 NM_013988	NM_016694 NM_001317726
RefSeq (bjelančevina)	NP_004553 NP_054642 NP_054643	NP_001304655 NP_057903
Lokacija (UCSC)	Chr 6: 161.35 – 162.73 Mb	Chr 17: 11.06 – 12.28 Mb
PubMed pretraga	[3]	[4]
Wikipodaci
Pogledaj/uredi – čovjek Pogledaj/uredi – miš

Konkretno, parkin prepoznaje proteine na vanjskoj membrani mitohondrija nakon povede ćelija i posreduje u čišćenju oštećenih mitohondrija putem autofagije i proteasomskih mehanizama.^[6] Parkin također poboljšava preživljavanje ćelija suzbijanjem mitohondrijski ovisnih i neovisnih apoptoza. Mutacije povezane su s mitohondrijskom disfunkcijom, što dovodi do neuronske smrti u Parkinsonovoj bolesti ^[7] iporemećenog metabolizma i tumorigenezi.^[8]

Aminokiselinska sekvenca

Dužina polipeptidnog lanca je 465 aminokiselina, а molekulska težina 51.641 Da.^[9]

• 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
MIVFVRFNSS		HGFPVEVDSD		TSIFQLKEVV		AKRQGVPADQ		LRVIFAGKEL
RNDWTVQNCD		LDQQSIVHIV		QRPWRKGQEM		NATGGDDPRN		AAGGCEREPQ
SLTRVDLSSS		VLPGDSVGLA		VILHTDSRKD		SPPAGSPAGR		SIYNSFYVYC
KGPCQRVQPG		KLRVQCSTCR		QATLTLTQGP		SCWDDVLIPN		RMSGECQSPH
CPGTSAEFFF		KCGAHPTSDK		ETSVALHLIA		TNSRNITCIT		CTDVRSPVLV
FQCNSRHVIC		LDCFHLYCVT		RLNDRQFVHD		PQLGYSLPCV		AGCPNSLIKE
LHHFRILGEE		QYNRYQQYGA		EECVLQMGGV		LCPRPGCGAG		LLPEPDQRKV
TCEGGNGLGC		GFAFCRECKE		AYHEGECSAV		FEASGTTTQA		YRVDERAAEQ
ARWEAASKET		IKKTTKPCPR		CHVPVEKNGG		CMHMKCPQPQ		CRLEWCWNCG
CEWNRVCMGD		HWFDV

Struktura

Parkin je protein koji čiji se genski lokus (PARK2) kod ljudi nalazi na hromosomu 6.^[10][11] Tačna funkcija ovog proteina nije poznata; međutim, zna se da je komponenta kompleksa multiproteina E3-ubikvitin ligaze koji je pak dio ubikvitin-proteasomskog sistema, koji posreduje u ciljanju proteina za razgradnju . Poznato je da mutacije u ovom genu uzrokuju porodični oblik Parkinsonove bolesti, poznate kao autosomno recesivna maloljetnička Parkinsonova bolest (AR-JP). Štaviše, opisano je da je parkin neophodan za mitofagiju (autofagiju mitohondrija).

Međutim, nije jasno kako gubitak funkcije parkinskog proteina dovodi do smrti dopaminergijskih ćelija) u ovoj bolesti. Prevladavajuća hipoteza je da parkin pomaže u razgradnji jednog ili više proteina toksičnih za dopaminergične neurone. Putativni supstrati parkina uključuju sinfilin-1, CDC-rel1 , ciklin E, p38 tRNK sitazu, Pael-R, sinaptotagmin XI, sp22 i sam parkin (vidi takođe ubikvitin-ligaza). Osim toga, parkin sadrži C-terminalni motiv koji veže PDZ-domene. Pokazalo se da se parkin povezuje na PDZ ovisan način sa domenom PDZ, koji sadrži proteine CASK i PICK1.

 

A: Dijagram rasporeda funkcionalnih domena parkina.
B: RING0, RING1, IBR i RING2 svaki koordiniraju dva Zn iona (približna lokacija označena sivim krugovima) za strukturnu stabilnost, što dovodi do stehiometrijske konformacije od 8 Zn2+/parkin.

Kao i drugi članovi porodice R3-RING-RING (RBR) E3 ligaza, parkin posjeduje dva RING-domena prstiju i jedan između RING (IBR) regije. RING1 formira mjesto vezanja za E2 Ub-konjugirajući enzim, dok RING2 sadrži katalitski cisteinski ostatak (Cys431) koji cijepa Ub iz E2 i privremeno ga veže za E3 tioesterskom vezom.^[6] Prijenosu Ub pomažu susjedni ostaci histidina His433, koji prihvata proton iz Cys431 da ga aktivira, i glutamat Glu444, koji je uključen u autoubikvitaciju.^[12] Zajedno tvore katalitsku trijadu, čije je sklapanje potrebno za aktivaciju parkina.^[13] Parkin također sadrži N-terminalni Ub-sličan domen (Ubl) za specifično prepoznavanje podloge, jedinstvenog domen RING0 i represorske (REP) regije koja tonski potiskuje aktivnost ligaza.

U uvjetima mirovanja, čvrsto namotana konformacija parkina čini ga neaktivnim, jer je pristup katalitskom ostatku RING2 sterno blokiran pomoću RING0, dok domen vezanja E2 na RING1 zaklanjaju Ubl i REP.^[6] Aktiviranje stimulusa remeti ove međudomenske interakcije i izaziva kolaps parkina duž sučelja RING1-RING0.^[13] Aktivno mjesto RING2 je povučeno prema E2-Ub vezanom za RING1, olakšavajući stvaranje međuproizvoda Ub-tioestera. Aktivacija parkina zahtijeva fosforilaciju serina Ser65 u Ubl-u pomoću serin/treonin-kinaza, PINK1. Dodavanje nabijenog fosfata destabilizira hidrofobne interakcije između Ubl i susjednih podregija, smanjujući autoinhibitorne efekte ovog domena N-kraja.^[14] Utvrđeno je da misens mutacije Ser65Ala desabliziraju vezivanje Ub-parkina, a istovremeno inhibiraju regrutovanje parkina u oštećene mitohondrije.^[15] PINK1 također fosforilira Ub na Ser65, ubrzavajući njegovo otpuštanje iz E2 i povećavajući njegov afinitet za parkin.^[14]

Iako su strukturne promjene nakon fosforilacije neizvjesne, kristalizacija parkina otkrila je kationski džep formiran u RING0-u od lizinskih i argininskih ostataka Lys161, Arg163 i Lys211 koji tvore navodno mjesto vezivanja fosfata.^[16] S obzirom na to da je domen RING0 jedinstven za parkin i da njegovo hidrofobno sučelje s RING1 zatrpava Cys431 u neaktivnom parkinu,^[15] ciljanje fosforiliranog Ub i/ili Ubl prema ovoj veznoj niši moglo bi biti kritično u uklanjanju autoinhibitornih kompleksa tokom aktivacije parkina.

Funkcija

Mitofagija

Parkin ima ključnu ulogu u mitofagiji i čišćenju reaktivnih vrsta kisika.^[17] Mitofagija je uklanjanje oštećenih mitohondrija u autofagosomima i ovisi o ciklusu pozitivne povrtne sprege koji uključuje sinergijsko djelovanje parkina i PINK1. Nakon teške ćelijake povrede, zaostajanje mitohondrijskog membranskog potencijala sprječava unos PINK1 u mitohondrijski matriks i uzrokuje njegovo nakupljanje na vanjskoj mitohondrijskoj membrani (OMM).^[18] Parkin se regrutira u mitohondrije, nakon depolarizacije i fosforilira PINK1, koji istovremeno fosforilira Ub. prethodno konjugiran na proteine mitohondrijske membrane. Fosforilacija PINK1 i Ub olakšava aktivaciju parkina i daljnje sklapanje mono- i poli-Ub lanaca.^[14] S obzirom na blizinu ovih lanaca PINK1, daljnja fosforilacija Ub na Ser65 vjerojatna je, pojačavajući mobilizaciju parkina i supstratnu sveprisutnost u ciklusu samopojačavanja.^[6]

Parkinski supstrati uključuju mitofusine Mfn1 i Mfn2, koji su velike GTPaze koji promoviraju fuziju mitohondrija u dinamične, cjevaste komplekse koji povećavaju učinkovitost oksidativne fosforilacije.^[19] Međutim, nakon mitohondrijskog oštećenja, nužna je degradacija fuzijskih proteina kako bi se odvojili od mreže putem mitohondrijskih fisija i spriječili kvarenje zdravih mitohondrija.[^[20] Parkin je stoga potreban prije mitofagije, jer ubikvitinizira Mfn1/2, označavajući ga za proteasomsku degradaciju. Proteomske studije identificirale su dodatne OMM proteine kao supstrate za parkin, uključujući fisijski protein FIS, njegov adapter TBC1D15 i translokaze TOMM20 i TOMM70, koje olakšavaju kretanje proteina poput PINK1 preko OMM-a.^[21] Miro (ili RHOT1/RHOT2) je OMM protein koji je kritičan za aksonsdki transport, a mogu biti sveprisutni i usmjereni prema proteasomskoj degradaciji putem parkina.^[22] Kvar miro-a izaziva značajno smanjenje migracije ugroženih mitohondrija duž mišjih aksona u hipokampusnim neuronima,^[23] pojačavajući važnost parkina u odvajanju defektnih mitohondrija od njihovih funkcionalnih parnjaka i ograničavajući prostorno širenje mitohondrijske disfunkcije, prije autofagije.

Tokom mitofagije, parkin cilja VDAC1, anionski kanal pod naponom koji prolazi kroz konformacijske promjene. nakon depolarizacije mitohondrijske membrane, izlažući citosolni domen za sveprisutnu primjenu.^[18] Utišavanje ekspresija VDAC1 u HeLa ćelijama značajno je smanjilo regrutiranje parkina u depolarizane mitohondrije i njihov naknadni klirens,^[24] ističući kritičnu ulogu VDAC1 kao selektivnog markera mitohondrijskog oštećenja i izazivača mitofagije. Nakon konjugacije Ub, parkin regrutira receptore autofagije, kao što su p62, TAX1BP1 i CALCOCO2, olakšavajući sastavljanje autofagosoma koji probavljaju defektne mitohondrije.^[21]

Ćelijsko preživljavanje

Aktivacijom signalizacije NF-κB, parkin povećava preživljavanje i štiti ćelije od apoptoze izazvane stresom. Nakon ćelijske povrede, parkin aktivira katalitski HOIP podjedinice druge E3 ligaze LUBAC. HOIP pokreće sklapanje linearnog Ub polimera na NF-κB esencijalnom modulatoru (NEMO), potencirajući transkripciju mitohondrijske GTPaze OPA1.^[25] Povećana translacija OPA1 održava strukturu krista i smanjuje oslobađanje citohroma C iz mitohondrija, inhibirajući kaspazom posredovanu apoptozu. ]Ono što je važno, parkin aktivira HOIP sa većom potencijom od ostalih faktora povezanih s LUBAC-om HOIL-1 i oštrinom,^[26] što znači da mobilizacija parkina značajno povećava toleranciju na umjerenu stresora.

Parkin ima afinitet vezanja za DNK i proizvode ovisne o dozi, smanjenje transkripcije i aktivnosti proapoptotskog faktora p53. Transfekcija p53 promotora sa skraćenim verzijama parkina u SH-SY5Y neurone otkrila je da se parkin direktno veže za promotor p53, preko svog RING1-domena.^[27] Nasupot tome, parkin može biti transkripcijski cilj p53-a u plućnim H460, gdje posreduje tumour-supresorsku aktivnost p53-a.^[8] S obzirom na njegovu ulogu u mitohondrijskoj homeostazi, parkin pomaže p53 u održavanju mitohondrijskog disanja, dok ograničava unos glukoze i proizvosnju laktata, sprječavajući tako nastanak Warburgovog učinka tokom tumourigeneze.^[28] Parkin dodatno podiže nivo citosolnog glutationa i štiti od oksidativnog stresa, okarakterizirajući ga kao kritičnog supresora tumora sa anti-glikolitskim i antioksidativnim sposobnostima.^[8]

Klinički značaj

Pokazano je da su gen PARK2 i parkin vezani za više porfemećaja:

• Parkinsonova bolest (OMIM)^[29] i
• Tumourigeneza^[30]

Interakcije

Parkin (ligaza) pokazao je interakcije sa:

• Alfa-sinukleinom,^[31][32]
• CASK,^[33]
• CUL1,^[34]
• FBXW7^[34] and
• GPR37,^[35][36]
• HSPA1A,^[35]
• HSPA8,^[35]
• Kompleksom komponente p38,^[37]
• PDCD2,^[38]
• SEPT5,^[39][40]
• SNCAIP,
• STUB1,^[35]
• SYT11,^[41] i
• Ubikvitinom C.^[32][42]

Reference

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2. GRCm38: Ensembl release 89: ENSMUSG00000023826 - 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.
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Vanjski linkovi

• GeneReviews/NCBI/NIH/UW entry on Parkin Type of Juvenile Parkinson Disease
• parkin protein na US National Library of Medicine Medical Subject Headings (MeSH)

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