MYO15A

MYO15A
Identifikatori
Aliasi	MYO15A
Vanjski ID-jevi	OMIM: 602666 MGI: 1261811 HomoloGene: 56504 GeneCards: MYO15A
Lokacija gena (čovjek)
Hrom.	Hromosom 17 (čovjek)
Kraj	18,179,802 bp
Lokacija gena (miš)
Hrom.	Hromosom 11 (miš)
Kraj	60,419,195 bp
Obrazac RNK ekspresije
	Više referentnih podataka o ekspresiji
Ontologija gena
Molekularna funkcija	• nucleotide binding; • actin binding; • cytoskeletal motor activity; • ATP binding; • calmodulin binding;
Ćelijska komponenta	• citoplazma; • stereocilium bundle; • projekcija ćelije; • Egzosom; • citoskelet; • myosin complex; • stereocilium;
Biološki proces	• sluh; • inner ear morphogenesis; • locomotory behavior;
	Izvori:Amigo / QuickGO
Ortolozi
	51168
	17910
	ENSG00000091536
	ENSMUSG00000042678
	Q9UKN7
	Q9QZZ4
	NM_016239
	NM_001103171; NM_010862; NM_182698
	NP_057323
	NP_001096641; NP_034992; NP_874357
	Wikipodaci
Pogledaj/uredi – čovjek	Pogledaj/uredi – miš

Miozin-XV je protein koji je kod ljudi kodiran genom MYO15A.^[5]^[6]

Identificirani su i pročitani transkript koji sadrži uzvodni i ovaj gen, ali se smatra da oni ne kodiraju fuzijski protein. Opisano je nekoliko alternativno prerađenih varijanti transkripta, ali njihove sekvence pune dužine nisu određene.^[6]

Wang el al. (1998) izolirali su djelimičnu cDNK MYO15A iz biblioteke ljudske cDNK specifičnoe za ljudski hromosom. Izvedeni parcijalni protein od 1.585 aminokiselina dijeli 99% aminokiselinskog identiteta s dijelom proteina miša. MYO15A sadrži N-terminalni motorni domen, dva IQ motiva koja vezuju lahki lanac i repnu regiju koja sadrži MyTH4 i domin sličan talinu. Opseg divergencije sekvence motornog domena MYO15A od ostalih prijavljenih miozina kvalifikovao je MYO15A kao novu granu miozinske superporodice. Northern blot analiza otkrila je ekspresiju MYO15A u ljudskom muzgu fetusa i odraslih, a RT-PCR analiza otkrila je ekspresiju u ljudskoj fetusnoj pužnici. RNK dot-blot analiza pokazala je ekspresiju u jajnicima, sjemenicima, bubrezima i hipofizi.

Aminokiselinska sekvenca

10	20	30	40	50
MAKEEDEEKK	AKKGKKGKKA	PEPEKPKRSL	KGTSRLFMGF	RDRTPKISKK
GQFRSASAFF	WGLHTGPQKT	KRKRKARTVL	KSTSKLMTQM	RMGKKKRAMK
GKKPSFMVIR	FPGRRGYGRL	RPRARSLSKA	STAINWLTKK	FLLKKAEESG
SEQATVDAWL	QRSSSRMGSR	KLPFPSGAEI	LRPGGRLRRF	PRSRSIYASG
EPLGFLPFED	EAPFHHSGSR	KSLYGLEGFQ	DLGEYYDYHR	DGDDYYDRQS
LHRYEEQEPY	LAGLGPYSPA	WPPYGDHYYG	YPPEDPYDYY	HPDYYGGPFD
PGYTYGYGYD	DYEPPYAPPS	GYSSPYSYHD	GYEGEAHPYG	YYLDPYAPYD
APYPPYDLPY	HTPYDVPYFD	PYGVHYTVPY	AEGVYGGGDE	AIYPPEVPYF
YPEESASAFV	YPWVPPPIPS	PHNPYAHAMD	DIAELEEPED	AGVERQGTSF
RLPSAAFFEQ	QGMDKPARSK	LSLIRKFRLF	PRPQVKLFGK	EKLEVPLPPS
LDIPLPLGDA	DEEEDEEELP	PVSAVPYGHP	FWGFLTPRQR	NLQRALSAFG
AHRGLGFGPE	FGRPVPRPAT	SLARFLKKTL	SEKKPIARLR	GSQKARAGGP
AVREAAYKRF	GYKLAGMDPE	KPGTPIVLRR	AQPRARSSND	ARRPPAPQPA
PRTLSHWSAL	LSPPVPPRPP	SSGPPPAPPL	SPALSGLPRP	ASPYGSLRRH
PPPWAAPAHV	PPAPQASWWA	FVEPPAVSPE	VPPDLLAFPG	PRPSFRGSRR
RGAAFGFPGA	SPRASRRRAW	SPLASPQPSL	RSSPGLGYCS	PLAPPSPQLS
LRTGPFQPPF	LPPARRPRSL	QESPAPRRAA	GRLGPPGSPL	PGSPRPPSPP
LGLCHSPRRS	SLNLPSRLPH	TWRRLSEPPT	RAVKPQVRLP	FHRPPRAGAW
RAPLEHRESP	REPEDSETPW	TVPPLAPSWD	VDMPPTQRPP	SPWPGGAGSR
RGFSRPPPVP	ENPFLQLLGP	VPSPTLQPED	PAADMTRVFL	GRHHEPGPGQ
LTKSAGPTPE	KPEEEATLGD	PQLPAETKPP	TPAPPKDVTP	PKDITPPKDV
LPEQKTLRPS	LSYPLAACDQ	TRATWPPWHR	WGTLPQAAAP	LAPIRAPEPL
PKGGERRQAA	PGRFAVVMPR	VQKLSSFQRV	GPATLKPQVQ	PIQDPKPRAC
SLRWSCLWLR	ADAYGPWPRV	HTHPQSCHLG	PGAACLSLRG	SWEEVGPPSW
RNKMHSIRNL	PSMRFREQHG	EDGVEDMTQL	EDLQETTVLS	NLKIRFERNL
IYTYIGSILV	SVNPYQMFGI	YGPEQVQQYN	GRALGENPPH	LFAVANLAFA
KMLDAKQNQC	IIISGESGSG	KTEATKLILR	YLAAMNQKRE	VMQQIKILEA
TPLLESFGNA	KTVRNDNSSR	FGKFVEIFLE	GGVISGAITS	QYLLEKSRIV
FQAKNERNYH	IFYELLAGLP	AQLRQAFSLQ	EAETYYYLNQ	GGNCEIAGKS
DADDFRRLLA	AMEVLGFSSE	DQDSIFRILA	SILHLGNVYF	EKYETDAQEV
ASVVSAREIQ	AVAELLQISP	EGLQKAITFK	VTETMREKIF	TPLTVESAVD
ARDAIAKVLY	ALLFSWLITR	VNALVSPRQD	TLSIAILDIY	GFEDLSFNSF
EQLCINYANE	NLQYLFNKIV	FQEEQEEYIR	EQIDWQEITF	ADNQPCINLI
SLKPYGILRI	LDDQCCFPQA	TDHTFLQKCH	YHHGANPLYS	KPKMPLPEFT
IKHYAGKVTY	QVHKFLDKNH	DQVRQDVLDL	FVRSRTRVVA	HLFSSHAPQA
APQRLGKSSS	VTRLYKAHTV	AAKFQQSLLD	LVEKMERCNP	LFMRCLKPNH
KKEPGLFEPD	VVMAQLRYSG	VLETVRIRKE	GFPVRLPFQG	FIDRYCCLVA
LKHDLPANGD	MCVSVLSRLC	KVMPNMYRVG	VSKLFLKEHL	YQLLESMREH
VLNLAALTLQ	RCLRGFFIKR	RFRSLRHKII	LLQSRARGYL	ARQRYQQMRR
SLVKFRSLVH	AYVSRRRYLK	LRAEWRCQVE	GALLWEQEEL	SKREVVAVGH
LEVPAELAGL	LQAVAGLGLA	QVPQVAPVRT	PRLQAEPRVT	LPLDINNYPM
AKFVQCHFKE	PAFGMLTVPL	RTPLTQLPAE	HHAEAVSIFK	LILRFMGDPH
LHGARENIFG	NYIVQKGLAV	PELRDEILAQ	LANQVWHNHN	AHNAERGWLL
LAACLSGFAP	SPCFNKYLLK	FVSDYGRNGF	QAVCQHRLMQ	AMGRAQQQGS
GAARTLPPTQ	LEWTATYEKA	SMALDVGCFN	GDQFSCPVHS	WSTGEEVAGD
ILRHRGLADG	WRGWTVAMKN	GVQWAELAGH	DYVLDLVSDL	ELLRDFPRQK
SYFIVGTEGP	AASRGGPKVV	FGNSWDSDED	MSTRPQPQEH	MPKVLDSDGY
SSHNQDGTNG	ETEAQRGTAT	HQESDSLGEP	AVPHKGLDCY	LDSLFDPVLS
YGDADLEKPT	AIAYRMKGGG	QPGGGSSSGT	EDTPRRPPEP	KPIPGLDAST
LALQQAFIHK	QAVLLAREMT	LQATALQQQP	LSAALRSLPA	EKPPAPEAQP
TSVGTGPPAK	PVLLRATPKP	LAPAPLAKAP	RLPIKPVAAP	VLAQDQASPE
TTSPSPELVR	YSTLNSEHFP	QPTQQIKNIV	RQYQQPFRGG	RPEALRKDGG
KVFMKRPDPH	EEALMILKGQ	MTHLAAAPGT	QVSREAVALV	KPVTSAPRPS
MAPTSALPSR	SLEPPEELTQ	TRLHRLINPN	FYGYQDAPWK	IFLRKEVFYP
KDSYSHPVQL	DLLFRQILHD	TLSEACLRIS	EDERLRMKAL	FAQNQLDTQK
PLVTESVKRA	VVSTARDTWE	VYFSRIFPAT	GSVGTGVQLL	AVSHVGIKLL
RMVKGGQEAG	GQLRVLRAYS	FADILFVTMP	SQNMLEFNLA	SEKVILFSAR
AHQVKTLVDD	FILELKKDSD	YVVAVRNFLP	EDPALLAFHK	GDIIHLQPLE
PPRVGYSAGC	VVRRKVVYLE	ELRRRGPDFG	WRFGTIHGRV	GRFPSELVQP
AAAPDFLQLP	TEPGRGRAAA	VAAAVASAAA	AQEVGRRREG	PPVRARSADH
GEDALALPPY	TMLEFAQKYF	RDPQRRPQDG	LRLKSKEPRE	SRTLEDMLCF
TKTPLQESLI	ELSDSSLSKM	ATDMFLAVMR	FMGDAPLKGQ	SDLDVLCNLL
KLCGDHEVMR	DECYCQVVKQ	ITDNTSSKQD	SCQRGWRLLY	IVTAYHSCSE
VLHPHLTRFL	QDVSRTPGLP	FQGIAKACEQ	NLQKTLRFGG	RLELPSSIEL
RAMLAGRSSK	RQLFLLPGGL	ERHLKIKTCT	VALDVVEEIC	AEMALTRPEA
FNEYVIFVVT	NRGQHVCPLS	RRAYILDVAS	EMEQVDGGYM	LWFRRVLWDQ
PLKFENELYV	TMHYNQVLPD	YLKGLFSSVP	ASRPSEQLLQ	QVSKLASLQH
RAKDHFYLPS	VREVQEYIPA	QLYRTTAGST	WLNLVSQHRQ	QTQALSPHQA
RAQFLGLLSA	LPMFGSSFFF	IQSCSNIAVP	APCILAINHN	GLNFLSTETH
ELMVKFPLKE	IQSTRTQRPT	ANSSYPYVEI	ALGDVAAQRT	LQLQLEQGLE
LCRVVAVHVE	NLLSAHEKRL	TLPPSEITLL

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

Ovaj gen kodira nekonvencijski miozin. Ovaj protein razlikuje se od ostalih miozina po tome što ima dugi N-terminalni produžetak koji prethodi konzerviranom motornom domenu. Studije na miševima sugeriraju da je ovaj protein neophodan za organizaciju aktina u trepljastim ćelijama pužnice.^[6]

Klinički značaj

Mutacije u ovom genu povezane su s dubokom, urođenom, neurosenzornom, nesindromnom gluhoćom.^[7] Lociran je unutar regije za Smith–Magenisov sindrom, na hromosomu 17.^[6]

Reference

^ ^a ^b ^c GRCh38: Ensembl release 89: ENSG00000091536 - Ensembl, maj 2017
^ ^a ^b ^c GRCm38: Ensembl release 89: ENSMUSG00000042678 - 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.
^ Wang A, Liang Y, Fridell RA, Probst FJ, Wilcox ER, Touchman JW, Morton CC, Morell RJ, Noben-Trauth K, Camper SA, Friedman TB (Jun 1998). "Association of unconventional myosin MYO15 mutations with human nonsyndromic deafness DFNB3". Science. 280 (5368): 1447–51. doi:10.1126/science.280.5368.1447. PMID 9603736.
^ ^a ^b ^c ^d "Entrez Gene: MYO15A myosin XVA".
^ Riahi, Z; Bonnet, C; Zainine, R; Louha, M; Bouyacoub, Y; Laroussi, N; Chargui, M; Kefi, R; Jonard, L; Dorboz, I; Hardelin, J. P.; Salah, S. B.; Levilliers, J; Weil, D; McElreavey, K; Boespflug, O. T.; Besbes, G; Abdelhak, S; Petit, C (2014). "Whole Exome Sequencing Identifies New Causative Mutations in Tunisian Families with Non-Syndromic Deafness". PLOS ONE. 9 (6): e99797. doi:10.1371/journal.pone.0099797. PMC 4057390. PMID 24926664.

Dopunska literatura

Kalay E, Uzumcu A, Krieger E, et al. (2007). "MYO15A (DFNB3) mutations in Turkish hearing loss families and functional modeling of a novel motor domain mutation". Am. J. Med. Genet. A. 143 (20): 2382–9. doi:10.1002/ajmg.a.31937. PMID 17853461. S2CID 26797020.
Nal N, Ahmed ZM, Erkal E, et al. (2007). "Mutational spectrum of MYO15A: the large N-terminal extension of myosin XVA is required for hearing". Hum. Mutat. 28 (10): 1014–9. doi:10.1002/humu.20556. PMID 17546645. S2CID 27597330.
La Rosa S, Capella C, Lloyd RV (2002). "Localization of myosin XVA in endocrine tumors of gut and pancreas". Endocr. Pathol. 13 (1): 29–37. doi:10.1385/EP:13:1:29. PMID 12114748. S2CID 20356974.
Bi W, Yan J, Stankiewicz P, et al. (2002). "Genes in a Refined Smith-Magenis Syndrome Critical Deletion Interval on Chromosome 17p11.2 and the Syntenic Region of the Mouse". Genome Res. 12 (5): 713–28. doi:10.1101/gr.73702. PMC 186594. PMID 11997338.
Liburd N, Ghosh M, Riazuddin S, et al. (2001). "Novel mutations of MYO15A associated with profound deafness in consanguineous families and moderately severe hearing loss in a patient with Smith-Magenis syndrome". Hum. Genet. 109 (5): 535–41. doi:10.1007/s004390100604. PMID 11735029. S2CID 20812371.
Lloyd RV, Vidal S, Jin L, et al. (2001). "Myosin XVA Expression in the Pituitary and in Other Neuroendocrine Tissues and Tumors". Am. J. Pathol. 159 (4): 1375–82. doi:10.1016/S0002-9440(10)62524-2. PMC 1850513. PMID 11583965.
Anderson DW, Probst FJ, Belyantseva IA, et al. (2000). "The motor and tail regions of myosin XV are critical for normal structure and function of auditory and vestibular hair cells". Hum. Mol. Genet. 9 (12): 1729–38. doi:10.1093/hmg/9.12.1729. PMID 10915760.
Liang Y, Wang A, Belyantseva IA, et al. (2000). "Characterization of the human and mouse unconventional myosin XV genes responsible for hereditary deafness DFNB3 and shaker 2". Genomics. 61 (3): 243–58. doi:10.1006/geno.1999.5976. PMID 10552926.
Friedman TB, Liang Y, Weber JL, et al. (1995). "A gene for congenital, recessive deafness DFNB3 maps to the pericentromeric region of chromosome 17". Nat. Genet. 9 (1): 86–91. doi:10.1038/ng0195-86. PMID 7704031. S2CID 33397422.

[refGRCh38Ensembl-1] GRCh38: Ensembl release 89: ENSG00000091536 - Ensembl, maj 2017

[refGRCm38Ensembl-2] GRCm38: Ensembl release 89: ENSMUSG00000042678 - 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.

[pmid9603736-5] Wang A, Liang Y, Fridell RA, Probst FJ, Wilcox ER, Touchman JW, Morton CC, Morell RJ, Noben-Trauth K, Camper SA, Friedman TB (Jun 1998). "Association of unconventional myosin MYO15 mutations with human nonsyndromic deafness DFNB3". Science. 280 (5368): 1447–51. doi:10.1126/science.280.5368.1447. PMID 9603736.

[entrez-6] "Entrez Gene: MYO15A myosin XVA".

[7] Riahi, Z; Bonnet, C; Zainine, R; Louha, M; Bouyacoub, Y; Laroussi, N; Chargui, M; Kefi, R; Jonard, L; Dorboz, I; Hardelin, J. P.; Salah, S. B.; Levilliers, J; Weil, D; McElreavey, K; Boespflug, O. T.; Besbes, G; Abdelhak, S; Petit, C (2014). "Whole Exome Sequencing Identifies New Causative Mutations in Tunisian Families with Non-Syndromic Deafness". PLOS ONE. 9 (6): e99797. doi:10.1371/journal.pone.0099797. PMC 4057390. PMID 24926664.

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