Isoform Positions

Isoform Protein Position Transcript Position Chromosomal Position (HG38) Chromosomal Position (HG19)
IC892827007;27008;27009 chr2:178713352;178713351;178713350chr2:179578079;179578078;179578077
N2AB861126056;26057;26058 chr2:178713352;178713351;178713350chr2:179578079;179578078;179578077
N2A768423275;23276;23277 chr2:178713352;178713351;178713350chr2:179578079;179578078;179578077
N2BNoneNone chr2:Nonechr2:None
Novex-1NoneNone chr2:Nonechr2:None
Novex-2NoneNone chr2:Nonechr2:None
Novex-3NoneNone chr2:Nonechr2:None

Information

  • RefSeq wild type amino acid: F
  • RefSeq wild type transcript codon: TTC
  • RefSeq wild type template codon: AAG
  • Domain: Ig-75
  • Domain position: 3
  • Structural Position: 3
  • Q(SASA): 0.1618
  • Predicted PPI site: N

Reported SAVs

SNV RS
DUET
PolyPhen-2
Condel
Rhapsody
REVEL
MVP
Source
MAF
Disease
Zygosity
Site annotation
mCSM PPI
Predicted PPI site
Comments
AFR
AMR
AMS
ASJ
EAS
EUR
FIN
MDE
NFE
SAS
OTH
F/L None None 0.999 N 0.665 0.681 0.584023569625 gnomAD-4.0.0 1.20032E-06 None None None None N None 0 0 None 0 0 None 0 0 1.3125E-06 0 0

Saturation Mutagenesis

SAV
AlphaMissense (IC)
AlphaMissense Class (IC)
AlphaMissense (N2AB)
AlphaMissense Class (N2AB)
mCSM
mCSM class
PolyPhen-2
PolyPhen-2 Class
Rhapsody
Rhapsody Class
Condel
Condel Score
Site annotation
mCSM PPI
Predicted PPI site
F/A 0.9949 likely_pathogenic 0.997 pathogenic -2.716 Highly Destabilizing 1.0 D 0.807 deleterious None None None None N
F/C 0.9779 likely_pathogenic 0.9883 pathogenic -1.731 Destabilizing 1.0 D 0.824 deleterious D 0.559503653 None None N
F/D 0.9993 likely_pathogenic 0.9995 pathogenic -2.864 Highly Destabilizing 1.0 D 0.843 deleterious None None None None N
F/E 0.9993 likely_pathogenic 0.9995 pathogenic -2.813 Highly Destabilizing 1.0 D 0.843 deleterious None None None None N
F/G 0.9982 likely_pathogenic 0.9989 pathogenic -3.019 Highly Destabilizing 1.0 D 0.839 deleterious None None None None N
F/H 0.9927 likely_pathogenic 0.9953 pathogenic -1.3 Destabilizing 1.0 D 0.8 deleterious None None None None N
F/I 0.8008 likely_pathogenic 0.8652 pathogenic -1.775 Destabilizing 1.0 D 0.783 deleterious N 0.491799304 None None N
F/K 0.9987 likely_pathogenic 0.9993 pathogenic -1.477 Destabilizing 1.0 D 0.845 deleterious None None None None N
F/L 0.9886 likely_pathogenic 0.9946 pathogenic -1.775 Destabilizing 0.999 D 0.665 neutral N 0.516201117 None None N
F/M 0.9522 likely_pathogenic 0.9712 pathogenic -1.545 Destabilizing 1.0 D 0.786 deleterious None None None None N
F/N 0.9966 likely_pathogenic 0.998 pathogenic -1.553 Destabilizing 1.0 D 0.851 deleterious None None None None N
F/P 0.9994 likely_pathogenic 0.9996 pathogenic -2.088 Highly Destabilizing 1.0 D 0.855 deleterious None None None None N
F/Q 0.9983 likely_pathogenic 0.9989 pathogenic -1.83 Destabilizing 1.0 D 0.853 deleterious None None None None N
F/R 0.9961 likely_pathogenic 0.9976 pathogenic -0.628 Destabilizing 1.0 D 0.854 deleterious None None None None N
F/S 0.9943 likely_pathogenic 0.9968 pathogenic -2.175 Highly Destabilizing 1.0 D 0.837 deleterious D 0.570352979 None None N
F/T 0.9958 likely_pathogenic 0.9977 pathogenic -2.031 Highly Destabilizing 1.0 D 0.834 deleterious None None None None N
F/V 0.8442 likely_pathogenic 0.8875 pathogenic -2.088 Highly Destabilizing 1.0 D 0.774 deleterious N 0.521694846 None None N
F/W 0.9522 likely_pathogenic 0.9628 pathogenic -0.831 Destabilizing 1.0 D 0.787 deleterious None None None None N
F/Y 0.793 likely_pathogenic 0.8383 pathogenic -1.029 Destabilizing 0.999 D 0.633 neutral D 0.547729274 None None N

Titin has multiple isoforms, the longest being the theoretical IC (inferred complete) isoform which contains all 363 in-frame titin exons. Here all isoform positions have been mapped onto the IC sequence, with an exception being the C-terminal of the much shorter novex-3 isoform. This contains the out of frame exon 48 which cannot be mapped to the other isoforms.