HEXA
Heksozaminidaza A (alfa polipeptid), znana i kao HEXA, jest enzim koji je kod ljudi kodiran genom HEXA, na hromosomu 15.[5][6]
Heksaozaminidaza A i kofaktor GM2 proteinski aktivator katalizirati razgradnju GM2 gangliozida i drugih molekula koje sadrže terminalne N-acetil heksozamine.[7] Heksozaminidaza A je heterodimer sastavljen od alfa podjedinice (ovaj protein) i beta podjedinice. Polipeptid alfa podjedinice kodiran je genom HEXA, dok je beta podjedinica kodirana genom HEXB . Genske mutacije u genu koji kodira beta podjedinicu (HEXB) često rezultiraju Sandhoffovom bolešću; budući da, mutacije u genu koji kodira alfa podjedinicu (HEXA, ovaj gen) smanjuju hidrolizu GM2 gangliozida, što je glavni uzrok Tay–Sachsove bolesti.[8]
Aminokiselinska sekvenca
[uredi | uredi izvor]Dužina polipeptidnog lanca je 529 aminokiselina, a molekulska težina 60.703 Da.[9].
10 | 20 | 30 | 40 | 50 | ||||
---|---|---|---|---|---|---|---|---|
MTSSRLWFSL | LLAAAFAGRA | TALWPWPQNF | QTSDQRYVLY | PNNFQFQYDV | ||||
SSAAQPGCSV | LDEAFQRYRD | LLFGSGSWPR | PYLTGKRHTL | EKNVLVVSVV | ||||
TPGCNQLPTL | ESVENYTLTI | NDDQCLLLSE | TVWGALRGLE | TFSQLVWKSA | ||||
EGTFFINKTE | IEDFPRFPHR | GLLLDTSRHY | LPLSSILDTL | DVMAYNKLNV | ||||
FHWHLVDDPS | FPYESFTFPE | LMRKGSYNPV | THIYTAQDVK | EVIEYARLRG | ||||
IRVLAEFDTP | GHTLSWGPGI | PGLLTPCYSG | SEPSGTFGPV | NPSLNNTYEF | ||||
MSTFFLEVSS | VFPDFYLHLG | GDEVDFTCWK | SNPEIQDFMR | KKGFGEDFKQ | ||||
LESFYIQTLL | DIVSSYGKGY | VVWQEVFDNK | VKIQPDTIIQ | VWREDIPVNY | ||||
MKELELVTKA | GFRALLSAPW | YLNRISYGPD | WKDFYIVEPL | AFEGTPEQKA | ||||
LVIGGEACMW | GEYVDNTNLV | PRLWPRAGAV | AERLWSNKLT | SDLTFAYERL | ||||
SHFRCELLRR | GVQAQPLNVG | FCEQEFEQT |
- 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
Funkcija
[uredi | uredi izvor]Iako alfa i beta podjedinice heksozaminidaze A mogu obje cijepiti ostatke GalNAc, samo alfa podjedinica je u stanju da hidrolizira GM2 gangliozide. Alfa podjedinica sadrži ključni ostatak, Arg-424, što je neophodno za vezivanje N-acetil-neuraminskog ostatka GM2 gangliozida. Alfa podjedinica može hidrolizirati GM2 gangliozide jer sadrži strukturu petlje koja se sastoji od aminokiselina: Gly-280, Ser-281, Glu-282 i Pro-283. Beta podjedinica nema petlju, ali služi kao idealna struktura za vezivanje proteina aktivatora GM2 (GM2AP) u alfa podjedinici. Kombinacija Arg-424 i aminokiselina koje uzrokuju stvaranje petlje omogućavaju alfa podjedinici da hidrolizuje GM2 gangliozide u GM3 gangliozide, uklanjanjem N-acetilgalaktozaminskih (GalNAc) ostataka iz GM2 gangliozida.[10]
Genske mutacije koje uzrokuju Tay–Sachsovu bolest
[uredi | uredi izvor]Brojne su mutacije koje dovode do nedostatka heksosaminidaze A, uključujući delexciju gena, nonsens i misens mutacije. Tay–Sachsova bolest nastaje kada heksosaminidaza A izgubi sposobnost funkcioniranja. Osobe s Tay–Sachsovom bolešću nisu u stanju ukloniti ostatke GalNAc iz GM2 gangliozida, a kao rezultat toga na kraju skladište 100 do 1.000 puta više gangzioda GM2 u mozgu od normalne osobe. Preko 100 različitih mutacija otkriveno je samo u dojenačkim slučajevima samo Tay–Sachsove bolesti.[11]
Najčešća mutacija, koja se javlja kod preko 80 % pacijenata sa Tay–Sachsovom bolešću, posljedica je dodavanja četiri para baza (TATC) u egzonu 11 gena Hex A. Ova insercija dovodi do ranog stop kodona, što uzrokuje nedostatak hex A.[12]
Djeca rođena s Tay–Sachsvom bolešću obično umiru između dvije i šest godina, od aspiracije i upale pluća. Tay–Sachsova bolest uzrokuje cerebralnu degeneraciju i sljepoću. Pacijenti također imaju mlitave ekstremitete i napade. Još ne postoji lijek za ovu bolest.[11]
Genske terapije za Tay-Sachsovu bolest
[uredi | uredi izvor]Gen HEXA je gen koji kodira protein za lizosomski enzim beta-heksosaminidazu. Ovaj enzim, u kombinaciji s GM2 proteinskim aktivatorom, odgovoran je za razgradnju gangliozida GM2 unutar lizosoma. Defekti gena HEXA, međutim, sprečavaju ovu degradaciju, što dovodi do nakupljanja toksina u ćelijama mozga i kičmene moždine. Ovaj fatalni genetički poremećaj naziva se Tay-Sachsova bolest. Budući da defekt odgovsrsjućrg gena uglavnom pogađa živčane ćelije, pacijent s mutacijom HEXA doživjet će brzo pogoršanje motorne i mentalne funkcije prije nego što umre oko treće ili četvrte godine života.
Model nokaut-miša, koji je genetički modificiran kako bi se promatrali efekti inaktivacije ili oštećenja određenih gena, otkrio je da su miševi kojima je primijenjen HEXA gen imali mnoge iste simptome Tay-Sachsove bolesti, uz jedan izuzetak: nakupljanje GM2 distribuirano je drugačije u mozgu miševa nego u mozgu tiskog ljudskog Tay-Sachsovog pacijenta. Ovaj model omogućio je istraživnje genske terapije za HEXA defekte. Jedna studija, rađena na miševima, uspješno je ponovo uspostavila nivo beta-heksoaminidaze i uklonila nakupljanje toksičnih ćelija, upotrebom nerepliciranog Herpes simplex vektora za kodiranje gena koji nedostaje.
Reference
[uredi | uredi izvor]- ^ a b c GRCh38: Ensembl release 89: ENSG00000213614 - Ensembl, maj 2017
- ^ a b c GRCm38: Ensembl release 89: ENSMUSG00000025232 - 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.
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- ^ Mark BL, Mahuran DJ, Cherney MM, Zhao D, Knapp S, James MN (april 2003). "Crystal structure of human beta-hexosaminidase B: understanding the molecular basis of Sandhoff and Tay-Sachs disease". Journal of Molecular Biology. 327 (5): 1093–109. doi:10.1016/S0022-2836(03)00216-X. PMC 2910754. PMID 12662933.
- ^ "UniProt, P06865". Pristupljeno 14. 7. 2021.
- ^ Lemieux MJ, Mark BL, Cherney MM, Withers SG, Mahuran DJ, James MN (juni 2006). "Crystallographic structure of human beta-hexosaminidase A: interpretation of Tay-Sachs mutations and loss of GM2 ganglioside hydrolysis". Journal of Molecular Biology. 359 (4): 913–29. doi:10.1016/j.jmb.2006.04.004. PMC 2910082. PMID 16698036.
- ^ a b Ozand PT, Nyhan WL, Barshop BA (2005). "Part Thirteen Lipid Storage Disorders: Tay-Sachs disease/hexosaminidase A deficiency". Atlas of metabolic diseases. London: Hodder Arnold. str. 539–546. ISBN 0-340-80970-1.
- ^ Boles DJ, Proia RL (mart 1995). "The molecular basis of HEXA mRNA deficiency caused by the most common Tay-Sachs disease mutation". American Journal of Human Genetics. 56 (3): 716–24. PMC 1801160. PMID 7887427.
Dopunska literatura
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Vanjski linkovi
[uredi | uredi izvor]- Hexosaminidase A na US National Library of Medicine Medical Subject Headings (MeSH)
- EC 3.2.1.52
- National Tay-Sach’s Disease Site