MYH7 non-truncating variants in DCM cohorts


The table below lists the 44 rare (MAF<0.0001 in ExAC) non-truncating MYH7 variants identified in a cohort of 756 DCM patients. When this rare variant frequency of 0.05820 is compared with a background population rate of 0.01350, there is a statistically significant case excess of 0.04470 (p<0.0001), which suggests that approximately 34 of these variants may be pathogenic.


Variant Type:      All protein-altering variants     -     Truncating variants     -     Non-Truncating variants
Source:      Combined (OMGL + LMM)     -     OMGL     -     LMM



No. Variant (CDS) Variant (Protein) Variant Type Cases (756)LMM class ExAC frequency
1. c.1106G>A p.R369Qmissense 2Likely Pathogenic0.000000
2. c.2711G>A p.R904Hmissense 2Likely Pathogenic0.000000
3. c.2678C>T p.A893Vmissense 2VUS favour pathogenic0.000000
4. c.3856G>A p.E1286Kmissense 2Likely Pathogenic0.000016
5. c.1405G>T p.D469Ymissense 2Likely Pathogenic0.000000
6. c.1597A>G p.I533Vmissense 2Likely Pathogenic0.000000
7. c.2710C>T p.R904Cmissense 1Pathogenic0.000008
8. c.734G>A p.G245Emissense 1Likely Pathogenic0.000000
9. c.2683C>G p.Q895Emissense 1VUS0.000000
10. c.1630A>G p.T544Amissense 1VUS0.000016
11. c.4030C>T p.R1344Wmissense 1VUS favour pathogenic0.000016
12. c.2171T>A p.I724Nmissense 1VUS favour pathogenic0.000000
13. c.1573G>A p.E525Kmissense 1Likely Pathogenic0.000000
14. c.4720C>T p.R1574Wmissense 1Likely Pathogenic0.000000
15. c.3578G>A p.R1193Hmissense 1Likely Pathogenic0.000000
16. c.709C>T p.R237Wmissense 1VUS0.000008
17. c.1402T>C p.F468Lmissense 1VUS favour pathogenic0.000000
18. c.5740G>A p.E1914Kmissense 1Likely Pathogenic0.000000
19. c.1892T>C p.I631Tmissense 1VUS0.000016
20. c.1700G>A p.R567Hmissense 1Likely Pathogenic0.000016
21. c.3455A>T p.E1152Vmissense 1Likely Pathogenic0.000000
22. c.3982G>A p.A1328Tmissense 1VUS favour pathogenic0.000043
23. c.742A>T p.I248Fmissense 1Likely Pathogenic0.000000
24. c.4985G>A p.R1662Hmissense 1VUS favour pathogenic0.000057
25. c.3734T>A p.L1245Qmissense 1VUS0.000000
26. c.184G>A p.E62Kmissense 1VUS0.000008
27. c.4348G>A p.D1450Nmissense 1Likely Pathogenic0.000008
28. c.1570A>G p.I524Vmissense 1Likely Pathogenic0.000000
29. c.2348G>C p.R783Pmissense 1Likely Pathogenic0.000000
30. c.5401G>A p.E1801Kmissense 1Likely Pathogenic0.000000
31. c.602T>C p.I201Tmissense 1Likely Pathogenic0.000000
32. c.1791C>A p.N597Kmissense 1Likely Pathogenic0.000000
33. c.4408T>C p.S1470Pmissense 1VUS favour pathogenic0.000000
34. c.835G>A p.A279Tmissense 1VUS favour pathogenic0.000000
35. c.5380C>G p.Q1794Emissense 1Likely Pathogenic0.000000
36. c.1888C>T p.P630Smissense 1VUS0.000016
37. c.2973G>T p.K991Nmissense 1VUS favour pathogenic0.000000

References

1. Roddy Walsh, Kate L. Thomson, James S. Ware, Birgit H. Funke, Jessica Woodley, Karen J. McGuire, Francesco Mazzarotto, Edward Blair, Anneke Seller, Jenny C. Taylor, Eric V. Minikel, Exome Aggregation Consortium, Daniel G. MacArthur, Martin Farrall, Stuart A. Cook and Hugh Watkins. Reassessment of Mendelian gene pathogenicity using 7,855 cardiomyopathy cases and 60,706 reference samples. Genet Med. 2016 doi:10.1038/gim.2016.90.

2. Pugh TJ, Kelly MA, Gowrisankar S, Hynes E, Seidman MA, Baxter SM, Bowser M, Harrison B, Aaron D, Mahanta LM, Lakdawala NK, McDermott G, White ET, Rehm HL, Lebo M, Funke BH. The landscape of genetic variation in dilated cardiomyopathy as surveyed by clinical DNA sequencing. Genet Med. 2014 Aug;16(8):601-8.