PITRM1
Pitrilizin-metalopeptidaza 1, znana i kao mitohondrijska presekvencna proteaza, (PreP) i metaloproteaza 1 (MTP-1) je enzim koji je kod ljudi kodiran genom PITRM1.[5][6][7] Ponekad se naziva i metaloproteaza 1 (MP1). PreP olakšava proteostazu korištenjem katalitske komore od ~13300-A (3) za razgradnju toksičnih peptida, uključujući mitohondrijske posljedice i β-amiloid.[8] Nedostatak PreP-a je povezan s Alzheimerovom bolešću. Pokazalo se da smanjeni nivoi PreP-a putem nokdauna posredovane RNK dovode do defektnog sazrijevanja proteina frataksina.[9]
Struktura[uredi | uredi izvor]
Aminokiselinska sekvenca[uredi | uredi izvor]
Dužina polipeptidnog lanca je 1.037 aminokiselina, а molekulska težina 117.413 Da.[10]
| 10 | 20 | 30 | 40 | 50 | ||||
|---|---|---|---|---|---|---|---|---|
| MWRCGGRQGL | CVLRRLSGGH | AHHRAWRWNS | NRACERALQY | KLGDKIHGFT | ||||
| VNQVTSVPEL | FLTAVKLTHD | DTGARYLHLA | REDTNNLFSV | QFRTTPMDST | ||||
| GVPHILEHTV | LCGSQKYPCR | DPFFKMLNRS | LSTFMNAFTA | SDYTLYPFST | ||||
| QNPKDFQNLL | SVYLDATFFP | CLRELDFWQE | GWRLEHENPS | DPQTPLVFKG | ||||
| VVFNEMKGAF | TDNERIFSQH | LQNRLLPDHT | YSVVSGGDPL | CIPELTWEQL | ||||
| KQFHATHYHP | SNARFFTYGN | FPLEQHLKQI | HEEALSKFQK | IEPSTVVPAQ | ||||
| TPWDKPREFQ | ITCGPDSFAT | DPSKQTTISV | SFLLPDITDT | FEAFTLSLLS | ||||
| SLLTSGPNSP | FYKALIESGL | GTDFSPDVGY | NGYTREAYFS | VGLQGIAEKD | ||||
| IETVRSLIDR | TIDEVVEKGF | EDDRIEALLH | KIEIQMKHQS | TSFGLMLTSY | ||||
| IASCWNHDGD | PVELLKLGNQ | LAKFRQCLQE | NPKFLQEKVK | QYFKNNQHKL | ||||
| TLSMRPDDKY | HEKQAQVEAT | KLKQKVEALS | PGDRQQIYEK | GLELRSQQSK | ||||
| PQDASCLPAL | KVSDIEPTIP | VTELDVVLTA | GDIPVQYCAQ | PTNGMVYFRA | ||||
| FSSLNTLPEE | LRPYVPLFCS | VLTKLGCGLL | DYREQAQQIE | LKTGGMSASP | ||||
| HVLPDDSHMD | TYEQGVLFSS | LCLDRNLPDM | MQLWSEIFNN | PCFEEEEHFK | ||||
| VLVKMTAQEL | ANGIPDSGHL | YASIRAGRTL | TPAGDLQETF | SGMDQVRLMK | ||||
| RIAEMTDIKP | ILRKLPRIKK | HLLNGDNMRC | SVNATPQQMP | QTEKAVEDFL | ||||
| RSIGRSKKER | RPVRPHTVEK | PVPSSSGGDA | HVPHGSQVIR | KLVMEPTFKP | ||||
| WQMKTHFLMP | FPVNYVGECI | RTVPYTDPDH | ASLKILARLM | TAKFLHTEIR | ||||
| EKGGAYGGGA | KLSHNGIFTL | YSYRDPNTIE | TLQSFGKAVD | WAKSGKFTQQ | ||||
| DIDEAKLSVF | STVDAPVAPS | DKGMDHFLYG | LSDEMKQAHR | EQLFAVSHDK | ||||
| LLAVSDRYLG | TGKSTHGLAI | LGPENPKIAK | DPSWIIQ |
Gen[uredi | uredi izvor]
Gen PITRM1 nalazi se na hromosomu 10, sekvenca q15.2, a sastoji se od 28 egzona.
Protein[uredi | uredi izvor]
PreP je 117 kDa M16C enzim koji je široko eksprimiran u ljudskim tkivima.[11] PreP se sastoji od PreP-N (aa 33-509) i PreP-C (aa 576-1037) domena, koji su povezani produženim spiralom ukosnica (aa 510 -575). Njegova struktura pokazuje da je odabir supstrata isključivanjem veličine konzervirani mehanizam u M16C proteazama.[8]
Funkcija[uredi | uredi izvor]
PreP je Zn2+-ovisna i ATP-neovisna metaloproteaza, it doesn’t select substrates on the basis of post-translational modifications or embedded degradation tags.[12][13][14] Umjesto toga, koristi negativno nabijenu katalitsku komoru, kako bi zahvatio supstrate peptida do ~65 ostataka, isključujući veće, savijene proteine.[15][16] Primarno je lokaliziran u mitohondrijskom matriksu, gdje cijepa peptide u reciklibilne fragmente.[17][18] Ne bira podloge na temelju posttranslacijskih modifikacija ili ugrađenih oznaka razgradnje.[19][20] Stoga delecija PRTRM1 dovodi do odgođenog fenotipa rasta.[21][22] Značajno je da PreP razgrađuje nekoliko funkcionalno relevantnih tipova β, čiji su agregati toksični za neurone i imaju ključnu ulogu u patogenezi Alzheimerove bolesti (AD).[15][23][24]
Klinički značaj[uredi | uredi izvor]
PreP je proteaza koja razgrađuje Aβ u mitohondrijama. Imuno-iscrpljivanje PreP-a u moždanim mitohondrijama sprječava razgradnju mitohondrijskog Ap, a utvrđeno je da je aktivnost PreP-a smanjena kod pacijenata s AD.[8] Prijavljeno je da je gubitak PreP aktivnosti posljedica oksidacije metionina i ovo istraživanje pruža racionalnu osnovu za terapijsku intervenciju u stanjima karakteriziranim prekomjernom oksidacijom PreP-a.[25] Nedavna studija također sugerira da PreP regulira amiloidne polipeptidne otočiće u beta-ćelijama.[26] Za dva brata i sestre koji nose homozigotnu PITRM1 misens mutaciju (c.548G> A, p.Arg183Gln) prijavljeno je da su povezani s autosomno recesivnim, sporo progresivnim sindromom. Kliničke značajke uključuju mentalnu retardaciju, spinocerebelarnu ataksiju, kognitivni pad i psihozu.[27] Hemizigotni model miša za PITRM1 pokazao je progresivnu ataksiju za koju se pretpostavljalo da je povezana s degenerativnim lezijama mozga, uključujući nakupljanje Aβ-pozitivnih amiloidnih naslaga. Nedavno je pokazano da dva brata iz srodničke porodice sa recesivnom cerebelumskom patologijom u djetinjstvu nose homozigotnu mutaciju u PITRM1 (c.2795C > T, p.T931M). Ova mutacija je rezultirala je smanjenjem proteina PITRM1 za 95%.[28] Pokazalo se da nokdaun PITRM1 dovodi do smanjenja nivoa zrelog proteina frataksina,[29] protein čiji nedostatk uzrokuje Friedreichovu ataksiju i može biti uključen u patološke promjene kod pacijenata koji nose PITRM1 mutacije.
Interakcije[uredi | uredi izvor]
Pokazano je da PITRM1 stupa u interakciju sa sljedećim proteinima: CCL22, CGB2, DDX41, DEFB104A, HDHD3, MRPL12, NDUFV2, PRDX6, PRKCSH, RARS2, RIF1, SUCLG2, TEKT3 , TERF2 i VAPB.[30]
Modelni organizmi[uredi | uredi izvor]
U proučavanju funkcije PITRM1 korišteni su i modelni organizmi. Uslovna linija nokaut-miša pod nazivom Pitrm1tm1a(KOMP)Wtsi generirana je u Wellcome Trust Sanger Institute.[31] Mužjaci i ženke podvrgnuti su standardiziranom fenotipskom pregledu[32] to determine the effects of deletion.[33][34][35][36] Izvršeni su dodatni pregledi: dubinsko imunsko fenotipiziranje.[37]
| Svojstvo | Fenotip |
|---|---|
| Svi podaci raspoloživi su na linku.[32][37] | |
| Limfociti periferne krvi 6 sedmica | Normalan |
| Hematologija 6 sedmica | Nenormalan |
| Insulin | Normalan |
| Vijabilnost homozigota na P14 | Nenormalan |
| Studija recesivne letalnosti | Nenormalan |
| Tjelesna težina | Normalan |
| Neurološka procjena | Normalan |
| Snaga stiska | Normalan |
| Dismorfologija | Normalan |
| Indirektna kalorimetrija | Normalan |
| Test tolerancije glukoze | Normalan |
| Slušni odgovor možanog stabla | Normalan |
| DEXA | Normalan |
| Radiografija | Normalan |
| Morfologija oka | Normalan |
| Klinička hemija | Normalan |
| Hematologija 16 sedmica | Normalan |
| Leukociti periferne krvi 16 sedmica | Normalan |
| Težina srca | Normalan |
| Salmonella infekcija | Normalan |
| Funkcija citotoksičnih T-ćelija | Normalan |
| Slezena | Normalan |
| Imunofenotipizacija mezenternih limfnih čvorova | Normalna |
| Imunofenotipizacija koštane srži | Normalan |
| Epidermni imunski sastav | Normalan |
| Trichuris-ni izazov | Normalan |
Reference[uredi | uredi izvor]
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- ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000021193 - Ensembl, maj 2017
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Dopunska literatura[uredi | uredi izvor]
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