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Here you can see the gene and the variant being analyzed.

We summarize a large amount of clinical data on this gene here. Links are added where available to source information.

Prediction information is summarized here, the percentage shows the likelihood that the variant is pathogenic.

Agreement is a measure (out of 5 stars) of how much our predictors agree between each other. When predictors agree, the prediction is more likely to be correct.

Data quality is a measure (out of 5 stars) of how good the underlying data for this prediction is. This is an assessment of the depth of our alignments and the number of structures available, among other factors.

This table shows literature for this exact position and protein, if it is available.

This table shows literature for this position in homologous proteins, if it is available.

This is a description of our prediction.

This plot illustrates the agreement between different classifiers. If the prediction distributions align on one side it indicates increased certainty in the prediction.

This describes the data quality for this position.

Here are the four factors that contributed most to the prediction. Factors that contributed to a benign prediction are colored blue, pathogenic factors are colored red.

This plot shows all the factors for prediction. Factors that contributed to a benign prediction are colored blue, pathogenic factors are colored red.

This plot shows the conservation on this position.

Here the conservation statistics are described.

This is an interactive structure display. Feel free to play with it after the tour!

This is a list of interactions we found for this position.

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ATM

ENST00000278616 | p.Met1040Val

predicted benign | pathogenicity score: 0%

Summary

ATM - ENST00000278616

Gene ATM - ENSG00000149311 | ENSP00000278616 | ENST00000278616
Ensembl | RefSeq | UniProt
Location GRCh38 11:108222832-108369099 Ensembl UCSC
Description ATM serine/threonine kinase

Serine/threonine protein kinase which activates checkpoint signaling upon double strand breaks (DSBs), apoptosis and genotoxic stresses such as ionizing ultraviolet A light (UVA), thereby acting as a DNA damage sensor. Recognizes the substrate consensus sequence [ST]-Q. Phosphorylates 'Ser-139' of histone variant H2AX/H2AFX at double strand breaks (DSBs), thereby regulating DNA damage response mechanism. Also plays a role in pre-B cell allelic exclusion, a process leading to expression of a single immunoglobulin heavy chain allele to enforce clonality and monospecific recognition by the B-cell antigen receptor (BCR) expressed on individual B-lymphocytes. After the introduction of DNA breaks by the RAG complex on one immunoglobulin allele, acts by mediating a repositioning of the second allele to pericentromeric heterochromatin, preventing accessibility to the RAG complex and recombination of the second allele. Also involved in signal transduction and cell cycle control. May function as a tumor suppressor. Necessary for activation of ABL1 and SAPK. Phosphorylates DYRK2, CHEK2, p53/TP53, FANCD2, NFKBIA, BRCA1, CTIP, nibrin (NBN), TERF1, RAD9 and DCLRE1C. May play a role in vesicle and/or protein transport. Could play a role in T-cell development, gonad and neurological function. Plays a role in replication-dependent histone mRNA degradation. Binds DNA ends. Phosphorylation of DYRK2 in nucleus in response to genotoxic stress prevents its MDM2-mediated ubiquitination and subsequent proteasome degradation. Phosphorylates ATF2 which stimulates its function in DNA damage response. {ECO:0000269|PubMed:10973490, ECO:0000269|PubMed:12556884, ECO:0000269|PubMed:14871926, ECO:0000269|PubMed:15916964, ECO:0000269|PubMed:16086026, ECO:0000269|PubMed:16858402, ECO:0000269|PubMed:17923702, ECO:0000269|PubMed:19431188, ECO:0000269|PubMed:19965871}.;

Condition(s)
  • Ataxia telangiectasia (AT)

    A rare recessive disorder characterized by progressive cerebellar ataxia, dilation of the blood vessels in the conjunctiva and eyeballs, immunodeficiency, growth retardation and sexual immaturity. Patients have a strong predisposition to cancer; about 30% of patients develop tumors, particularly lymphomas and leukemias. Cells from affected individuals are highly sensitive to damage by ionizing radiation and resistant to inhibition of DNA synthesis following irradiation.
    The disease is caused by mutations affecting the gene represented in this entry. OMIM

    MedGen: C0950123 C1458155 C0017636 C0677776 C0004135 OrphaNet: 180250 100 360 145

Sequence
MSLVLNDLLI
10		 CCRQLEHDRA
20		 TERKKEVEKF
30		 KRLIRDPETI
40		 KHLDRHSDSK
50		 QGKYLNWDAV
60		 FRFLQKYIQK
70		 ETECLRIAKP
80		 NVSASTQASR
90		 QKKMQEISSL
100
VKYFIKCANR
110		 RAPRLKCQEL
120		 LNYIMDTVKD
130		 SSNGAIYGAD
140		 CSNILLKDIL
150		 SVRKYWCEIS
160		 QQQWLELFSV
170		 YFRLYLKPSQ
180		 DVHRVLVARI
190		 IHAVTKGCCS
200
QTDGLNSKFL
210		 DFFSKAIQCA
220		 RQEKSSSGLN
230		 HILAALTIFL
240		 KTLAVNFRIR
250		 VCELGDEILP
260		 TLLYIWTQHR
270		 LNDSLKEVII
280		 ELFQLQIYIH
290		 HPKGAKTQEK
300
GAYESTKWRS
310		 ILYNLYDLLV
320		 NEISHIGSRG
330		 KYSSGFRNIA
340		 VKENLIELMA
350		 DICHQVFNED
360		 TRSLEISQSY
370		 TTTQRESSDY
380		 SVPCKRKKIE
390		 LGWEVIKDHL
400
QKSQNDFDLV
410		 PWLQIATQLI
420		 SKYPASLPNC
430		 ELSPLLMILS
440		 QLLPQQRHGE
450		 RTPYVLRCLT
460		 EVALCQDKRS
470		 NLESSQKSDL
480		 LKLWNKIWCI
490		 TFRGISSEQI
500
QAENFGLLGA
510		 IIQGSLVEVD
520		 REFWKLFTGS
530		 ACRPSCPAVC
540		 CLTLALTTSI
550		 VPGTVKMGIE
560		 QNMCEVNRSF
570		 SLKESIMKWL
580		 LFYQLEGDLE
590		 NSTEVPPILH
600
SNFPHLVLEK
610		 ILVSLTMKNC
620		 KAAMNFFQSV
630		 PECEHHQKDK
640		 EELSFSEVEE
650		 LFLQTTFDKM
660		 DFLTIVRECG
670		 IEKHQSSIGF
680		 SVHQNLKESL
690		 DRCLLGLSEQ
700
LLNNYSSEIT
710		 NSETLVRCSR
720		 LLVGVLGCYC
730		 YMGVIAEEEA
740		 YKSELFQKAK
750		 SLMQCAGESI
760		 TLFKNKTNEE
770		 FRIGSLRNMM
780		 QLCTRCLSNC
790		 TKKSPNKIAS
800
GFFLRLLTSK
810		 LMNDIADICK
820		 SLASFIKKPF
830		 DRGEVESMED
840		 DTNGNLMEVE
850		 DQSSMNLFND
860		 YPDSSVSDAN
870		 EPGESQSTIG
880		 AINPLAEEYL
890		 SKQDLLFLDM
900
LKFLCLCVTT
910		 AQTNTVSFRA
920		 ADIRRKLLML
930		 IDSSTLEPTK
940		 SLHLHMYLML
950		 LKELPGEEYP
960		 LPMEDVLELL
970		 KPLSNVCSLY
980		 RRDQDVCKTI
990		 LNHVLHVVKN
1000
LGQSNMDSEN
1010		 TRDAQGQFLT
1020		 VIGAFWHLTK
1030		 ERKYIFSVRM
1040		 ALVNCLKTLL
1050		 EADPYSKWAI
1060		 LNVMGKDFPV
1070		 NEVFTQFLAD
1080		 NHHQVRMLAA
1090		 ESINRLFQDT
1100
KGDSSRLLKA
1110		 LPLKLQQTAF
1120		 ENAYLKAQEG
1130		 MREMSHSAEN
1140		 PETLDEIYNR
1150		 KSVLLTLIAV
1160		 VLSCSPICEK
1170		 QALFALCKSV
1180		 KENGLEPHLV
1190		 KKVLEKVSET
1200
FGYRRLEDFM
1210		 ASHLDYLVLE
1220		 WLNLQDTEYN
1230		 LSSFPFILLN
1240		 YTNIEDFYRS
1250		 CYKVLIPHLV
1260		 IRSHFDEVKS
1270		 IANQIQEDWK
1280		 SLLTDCFPKI
1290		 LVNILPYFAY
1300
EGTRDSGMAQ
1310		 QRETATKVYD
1320		 MLKSENLLGK
1330		 QIDHLFISNL
1340		 PEIVVELLMT
1350		 LHEPANSSAS
1360		 QSTDLCDFSG
1370		 DLDPAPNPPH
1380		 FPSHVIKATF
1390		 AYISNCHKTK
1400
LKSILEILSK
1410		 SPDSYQKILL
1420		 AICEQAAETN
1430		 NVYKKHRILK
1440		 IYHLFVSLLL
1450		 KDIKSGLGGA
1460		 WAFVLRDVIY
1470		 TLIHYINQRP
1480		 SCIMDVSLRS
1490		 FSLCCDLLSQ
1500
VCQTAVTYCK
1510		 DALENHLHVI
1520		 VGTLIPLVYE
1530		 QVEVQKQVLD
1540		 LLKYLVIDNK
1550		 DNENLYITIK
1560		 LLDPFPDHVV
1570		 FKDLRITQQK
1580		 IKYSRGPFSL
1590		 LEEINHFLSV
1600
SVYDALPLTR
1610		 LEGLKDLRRQ
1620		 LELHKDQMVD
1630		 IMRASQDNPQ
1640		 DGIMVKLVVN
1650		 LLQLSKMAIN
1660		 HTGEKEVLEA
1670		 VGSCLGEVGP
1680		 IDFSTIAIQH
1690		 SKDASYTKAL
1700
KLFEDKELQW
1710		 TFIMLTYLNN
1720		 TLVEDCVKVR
1730		 SAAVTCLKNI
1740		 LATKTGHSFW
1750		 EIYKMTTDPM
1760		 LAYLQPFRTS
1770		 RKKFLEVPRF
1780		 DKENPFEGLD
1790		 DINLWIPLSE
1800
NHDIWIKTLT
1810		 CAFLDSGGTK
1820		 CEILQLLKPM
1830		 CEVKTDFCQT
1840		 VLPYLIHDIL
1850		 LQDTNESWRN
1860		 LLSTHVQGFF
1870		 TSCLRHFSQT
1880		 SRSTTPANLD
1890		 SESEHFFRCC
1900
LDKKSQRTML
1910		 AVVDYMRRQK
1920		 RPSSGTIFND
1930		 AFWLDLNYLE
1940		 VAKVAQSCAA
1950		 HFTALLYAEI
1960		 YADKKSMDDQ
1970		 EKRSLAFEEG
1980		 SQSTTISSLS
1990		 EKSKEETGIS
2000
LQDLLLEIYR
2010		 SIGEPDSLYG
2020		 CGGGKMLQPI
2030		 TRLRTYEHEA
2040		 MWGKALVTYD
2050		 LETAIPSSTR
2060		 QAGIIQALQN
2070		 LGLCHILSVY
2080		 LKGLDYENKD
2090		 WCPELEELHY
2100
QAAWRNMQWD
2110		 HCTSVSKEVE
2120		 GTSYHESLYN
2130		 ALQSLRDREF
2140		 STFYESLKYA
2150		 RVKEVEEMCK
2160		 RSLESVYSLY
2170		 PTLSRLQAIG
2180		 ELESIGELFS
2190		 RSVTHRQLSE
2200
VYIKWQKHSQ
2210		 LLKDSDFSFQ
2220		 EPIMALRTVI
2230		 LEILMEKEMD
2240		 NSQRECIKDI
2250		 LTKHLVELSI
2260		 LARTFKNTQL
2270		 PERAIFQIKQ
2280		 YNSVSCGVSE
2290		 WQLEEAQVFW
2300
AKKEQSLALS
2310		 ILKQMIKKLD
2320		 ASCAANNPSL
2330		 KLTYTECLRV
2340		 CGNWLAETCL
2350		 ENPAVIMQTY
2360		 LEKAVEVAGN
2370		 YDGESSDELR
2380		 NGKMKAFLSL
2390		 ARFSDTQYQR
2400
IENYMKSSEF
2410		 ENKQALLKRA
2420		 KEEVGLLREH
2430		 KIQTNRYTVK
2440		 VQRELELDEL
2450		 ALRALKEDRK
2460		 RFLCKAVENY
2470		 INCLLSGEEH
2480		 DMWVFRLCSL
2490		 WLENSGVSEV
2500
NGMMKRDGMK
2510		 IPTYKFLPLM
2520		 YQLAARMGTK
2530		 MMGGLGFHEV
2540		 LNNLISRISM
2550		 DHPHHTLFII
2560		 LALANANRDE
2570		 FLTKPEVARR
2580		 SRITKNVPKQ
2590		 SSQLDEDRTE
2600
AANRIICTIR
2610		 SRRPQMVRSV
2620		 EALCDAYIIL
2630		 ANLDATQWKT
2640		 QRKGINIPAD
2650		 QPITKLKNLE
2660		 DVVVPTMEIK
2670		 VDHTGEYGNL
2680		 VTIQSFKAEF
2690		 RLAGGVNLPK
2700
IIDCVGSDGK
2710		 ERRQLVKGRD
2720		 DLRQDAVMQQ
2730		 VFQMCNTLLQ
2740		 RNTETRKRKL
2750		 TICTYKVVPL
2760		 SQRSGVLEWC
2770		 TGTVPIGEFL
2780		 VNNEDGAHKR
2790		 YRPNDFSAFQ
2800
CQKKMMEVQK
2810		 KSFEEKYEVF
2820		 MDVCQNFQPV
2830		 FRYFCMEKFL
2840		 DPAIWFEKRL
2850		 AYTRSVATSS
2860		 IVGYILGLGD
2870		 RHVQNILINE
2880		 QSAELVHIDL
2890		 GVAFEQGKIL
2900
PTPETVPFRL
2910		 TRDIVDGMGI
2920		 TGVEGVFRRC
2930		 CEKTMEVMRN
2940		 SQETLLTIVE
2950		 VLLYDPLFDW
2960		 TMNPLKALYL
2970		 QQRPEDETEL
2980		 HPTLNADDQE
2990		 CKRNLSDIDQ
3000
SFNKVAERVL
3010		 MRLQEKLKGV
3020		 EEGTVLSVGG
3030		 QVNLLIQQAI
3040		 DPKNLSRLFP
3050		 GWKAWV
3056
PDB and PDB position 5np1 1040 (Explore)
gnomAD Exome Allele Frequency: 0.003072148
Genome Allele Frequency: 0.01136725
gnomAD
Pathogenicity benign according to VKGL
Older predictions
Helix v3 Helix v4.0.1 Helix v4.2.0 Helix v4.2.1 Helix v4.4.1 (selected)

Literature

Helix classification

Classification: benign according to VKGL

This variant was found in the VKGL dataset. According to this authoritative source this variant is classified as benign. A prediction is available for this variant, but this source takes precedence in our classification.

Helix prediction details

Prediction: benign 0%

The Met1040Val mutation in the protein has been classified as benign by our ensemble classifier system, with very high confidence. There is a 99% agreement between all subclassifiers.

Data quality

Data quality for this region is considered good. This means that structural data is present, alignments are deep and the species in those alignments are diverse.

Assistant summary

This is an automatically generated assessment, it is not reviewed by humans and only has partial access to the information contained in the report. Generating this may take some time.

Evolutionary pressure

Conservation

The wildtype was observed in 52.98% of the 168 sequences analyzed. The variant type was observed in 21.43% of observed sequences.

Structure

Toggle interactions

This residue is involved in 2 Hydrophobic interactions.

Interaction statistics were calculated using advanced molecular optimization techniques and may not be visible in the plain PDB file. Please download the YASARA scene to explore the interactions in more detail.