MYBPC3 truncating variants in HCM cohorts

The table below lists the 298 rare (MAF<0.0001 in ExAC) truncating MYBPC3 variants identified in a cohort of 3267 HCM patients. When this rare variant frequency of 0.09122 is compared with a background population rate of 0.00086, there is a statistically significant case excess of 0.09036 (p<0.0001), which suggests that approximately 295 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 (3267)▼	OMGL class	ExAC frequency
1.	c.1458G>A	p.W486X	nonsense	1	Pathogenic	0.000000
2.	c.3697C>T	p.Q1233X	nonsense	4	Likely Pathogenic	0.000008
3.	c.2905C>T	p.Q969X	nonsense	2	Pathogenic	0.000000
4.	c.1303C>T	p.Q435X	nonsense	1	Pathogenic	0.000000
5.	c.932C>A	p.S311X	nonsense	1	Pathogenic	0.000000
6.	c.3357C>A	p.Y1119X	nonsense	1	Pathogenic	0.000000
7.	c.1201C>T	p.Q401X	nonsense	1	Pathogenic	0.000000
8.	c.2065C>T	p.Q689X	nonsense	1	Pathogenic	0.000000
9.	c.2953A>T	p.K985X	nonsense	1	Pathogenic	0.000000
10.	c.3257G>A	p.W1086X	nonsense	1	Pathogenic	0.000021
11.	c.3163A>T	p.K1055X	nonsense	4	Pathogenic	0.000000
12.	c.3129C>A	p.Y1043X	nonsense	3	Pathogenic	0.000000
13.	c.2584C>T	p.Q862X	nonsense	1	Pathogenic	0.000000
14.	c.2748G>A	p.W916X	nonsense	1	Pathogenic	0.000000
15.	c.1457G>A	p.W486X	nonsense	1	Pathogenic	0.000000
16.	c.3408C>A	p.Y1136X	nonsense	3	Pathogenic	0.000000
17.	c.2526C>G	p.Y842X	nonsense	2	Pathogenic	0.000000
18.	c.1273C>T	p.Q425X	nonsense	1	Pathogenic	0.000000
19.	c.711C>A	p.Y237X	nonsense	1	Pathogenic	0.000000
20.	c.2247C>A	p.Y749X	nonsense	1	Pathogenic	0.000000
21.	c.1120C>T	p.Q374X	nonsense	1	Pathogenic	0.000000
22.	c.3811C>T	p.R1271X	nonsense	1	VUS	0.000025
23.	c.3253G>T	p.E1085X	nonsense	1	Pathogenic	0.000000
24.	c.2371C>T	p.Q791X	nonsense	1	Pathogenic	0.000000
25.	c.1405C>T	p.Q469X	nonsense	1	Pathogenic	0.000000
26.	c.747C>A	p.C249X	nonsense	2	Pathogenic	0.000000
27.	c.126G>A	p.W42X	nonsense	2	Pathogenic	0.000000
28.	c.484C>T	p.Q162X	nonsense	4	Pathogenic	0.000000
29.	c.3286G>T	p.E1096X	nonsense	3	Pathogenic	0.000000
30.	c.2827C>T	p.R943X	nonsense	11	Pathogenic	0.000017
31.	c.3181C>T	p.Q1061X	nonsense	3	Pathogenic	0.000016
32.	c.2603-1G>C		essential splice site	1	Pathogenic	0.000000
33.	c.506-1G>A		essential splice site	1	Pathogenic	0.000000
34.	c.1090+2T>C		essential splice site	1	Pathogenic	0.000000
35.	c.25+1G>A		essential splice site	2	Pathogenic	0.000000
36.	c.2905+2dup		essential splice site	2	Likely Pathogenic	0.000000
37.	c.2309-1G>A		essential splice site	3	Pathogenic	0.000000
38.	c.2308+1G>A		essential splice site	2	Pathogenic	0.000000
39.	c.*26+2T>C		essential splice site	1	Likely Pathogenic	0.000000
40.	c.1898-1G>A		essential splice site	1	Pathogenic	0.000000
41.	c.1090+1G>A		essential splice site	1	Pathogenic	0.000000
42.	c.821+2T>G		essential splice site	1	Pathogenic	0.000000
43.	c.1224-1G>T		essential splice site	1	Pathogenic	0.000000
44.	c.3627+1G>T		essential splice site	2	Pathogenic	0.000000
45.	c.3190+2T>G		essential splice site	7	Pathogenic	0.000016
46.	c.821+2T>C		essential splice site	4	Pathogenic	0.000000
47.	c.2603-2_2603-1delinsGA		essential splice site	1	Pathogenic	0.000000
48.	c.3330+1G>C		essential splice site	1	Pathogenic	0.000000
49.	c.655-2del		essential splice site	1	Pathogenic	0.000000
50.	c.2905+1G>A		essential splice site	3	Pathogenic	0.000000
51.	c.2995-1G>A		essential splice site	1	Pathogenic	0.000000
52.	c.927-2A>G		essential splice site	8	Pathogenic	0.000000
53.	c.1351+1G>A		essential splice site	1	Pathogenic	0.000000
54.	c.772+1G>A		essential splice site	1	Pathogenic	0.000000
55.	c.2738-2A>G		essential splice site	1	Pathogenic	0.000000
56.	c.1223+2T>C		essential splice site	1	Pathogenic	0.000000
57.	c.3627+1G>A		essential splice site	6	Pathogenic	0.000000
58.	c.1624+1G>A		essential splice site	1	Pathogenic	0.000000
59.	c.2304_2308+2delCATCGGT		essential splice site	1	Pathogenic	0.000000
60.	c.3490+1G>A		essential splice site	1	Pathogenic	0.000000
61.	c.821+1G>A		essential splice site	1	Pathogenic	0.000043
62.	c.1090+1G>T		essential splice site	1	Pathogenic	0.000000
63.	c.1928-2A>G		essential splice site	10	Pathogenic	0.000000
64.	c.3316del	p.Asp1106Thrfs*83	frameshift	1	Pathogenic	0.000000
65.	c.2789del	p.Leu930Argfs*2	frameshift	1	Pathogenic	0.000000
66.	c.2490_2491insT	p.His831SerfsTer2	frameshift	7	Pathogenic	0.000024
67.	c.2188del	p.Thr730Profs*24	frameshift	1	Pathogenic	0.000000
68.	c.1266_1267insTGAT	p.Ile423*	frameshift	1	Pathogenic	0.000000
69.	c.2429_2503delins23	p.Arg810Profs*10	frameshift	1	Pathogenic	0.000000
70.	c.611_618delinsT	p.Gly204Valfs*94	frameshift	1	Pathogenic	0.000000
71.	c.211_212delinsTA	p.Val71*	frameshift	1	Pathogenic	0.000000
72.	c.1359del	p.Val454Cysfs*12	frameshift	1	Pathogenic	0.000000
73.	c.3226_3227insT		frameshift	12	Pathogenic	0.000000
74.	c.2534_2538delGCGTC		frameshift	1	Pathogenic	0.000000
75.	c.3600_3609delCTGCTGTGCT		frameshift	3	Pathogenic	0.000000
76.	c.2096delC		frameshift	15	Pathogenic	0.000000
77.	c.833delG	p.Gly278GlufsX22	frameshift	2	Pathogenic	0.000000
78.	c.2558delG		frameshift	1	Pathogenic	0.000000
79.	c.2690_2696del	p.Gly897Glufs*25	frameshift	1	Pathogenic	0.000000
80.	c.743_746delACTG		frameshift	1	Pathogenic	0.000000
81.	c.2524dup	p.Tyr842Leufs*42	frameshift	2	Pathogenic	0.000000
82.	c.1569dup	p.His524Alafs*7	frameshift	1	Pathogenic	0.000000
83.	c.2149_2737del	p.Leu717Alafs*11	frameshift	1	Pathogenic	0.000000
84.	c.351_352del	p.Gly118Argfs*8	frameshift	1	Pathogenic	0.000000
85.	c.1404del	p.Gln469Serfs*19	frameshift	1	Pathogenic	0.000000
86.	c.731del	p.Lys244Argfs*56	frameshift	1	Pathogenic	0.000000
87.	c.121dup	p.Arg41Profs*8	frameshift	1	Pathogenic	0.000000
88.	c.443dup	p.Ala149Serfs*4	frameshift	2	Pathogenic	0.000000
89.	c.3624delC		frameshift	1	Pathogenic	0.000000
90.	c.2610delC		frameshift	5	Pathogenic	0.000000
91.	c.1377delC		frameshift	1	Pathogenic	0.000000
92.	c.811_817delTTCCGCC		frameshift	1	Pathogenic	0.000000
93.	c.2373_2374insG	p.Trp792ValfsTer41	frameshift	40	Pathogenic	0.000037
94.	c.3297dup	p.Tyr1100Valfs*49	frameshift	1	Pathogenic	0.000000
95.	c.2161_2168del	p.Thr721Profs*23	frameshift	1	Pathogenic	0.000000
96.	c.2502del	p.Arg835Alafs*2	frameshift	1	Pathogenic	0.000000
97.	c.177dup	p.Glu60Argfs*53	frameshift	1	Pathogenic	0.000000
98.	c.553_562del	p.Lys185Trpfs*12	frameshift	1	Pathogenic	0.000000
99.	c.1038_1042dupCGGCA		frameshift	1	Pathogenic	0.000008
100.	c.3605delG		frameshift	1	Pathogenic	0.000000
101.	c.2864_2865delCT		frameshift	8	Pathogenic	0.000000
102.	c.2556_2557delinsTCT	p.Gly853fs	frameshift	4	Pathogenic	0.000000
103.	c.459delC		frameshift	1	Pathogenic	0.000000
104.	c.1999_2000delinsG	p.Leu667AspfsX15	frameshift	1	Pathogenic	0.000000
105.	c.2807dup	p.Ala938Glyfs*113	frameshift	1	Pathogenic	0.000000
106.	c.1352_1353del	p.Glu451Alafs*23	frameshift	1	Pathogenic	0.000000
107.	c.2512dup	p.Glu838Glyfs*46	frameshift	1	Pathogenic	0.000000
108.	c.1523_1525delinsT	p.Gln508Leufs*22	frameshift	1	Pathogenic	0.000000
109.	c.2718_2719dup	p.Glu907Glyfs*18	frameshift	1	Pathogenic	0.000000
110.	c.255del	p.Ser86Profs*10	frameshift	1	Pathogenic	0.000000
111.	c.1376_1377del	p.Pro459Leufs*15	frameshift	1	Pathogenic	0.000000
112.	c.391dup	p.Ala131Glyfs*22	frameshift	1	Pathogenic	0.000000
113.	c.100_110dup	p.Val38Serfs*5	frameshift	1	Pathogenic	0.000000
114.	c.3617delG		frameshift	1	Pathogenic	0.000000
115.	c.2267delC		frameshift	5	Pathogenic	0.000000
116.	c.2604_2605delinsA	p.S871fs	frameshift	8	Pathogenic	0.000000
117.	c.3043dup	p.Ala1015Glyfs*36	frameshift	1	Pathogenic	0.000000
118.	c.982delG		frameshift	1	Pathogenic	0.000000
119.	c.3792_3793del	p.Cys1264*	frameshift	1	Likely Pathogenic	0.000000
120.	c.1797del	p.His599Glnfs*3	frameshift	1	Pathogenic	0.000000
121.	c.3271del	p.Asp1091Metfs*98	frameshift	2	Pathogenic	0.000000
122.	c.2545del	p.Val849Serfs*30	frameshift	3	Pathogenic	0.000000
123.	c.2054_2067+11del	p.Lys685Argfs*3	frameshift	1	Pathogenic	0.000000
124.	c.1021_1028del	p.Gly341*	frameshift	1	Pathogenic	0.000000
125.	c.177_187del	p.Glu60AlafsX49	frameshift	2	Pathogenic	0.000000

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. Alfares AA, Kelly MA, McDermott G, Funke BH, Lebo MS, Baxter SB, Shen J, McLaughlin HM, Clark EH, Babb LJ, Cox SW, DePalma SR, Ho CY, Seidman JG, Seidman CE, Rehm HL. Results of clinical genetic testing of 2,912 probands with hypertrophic cardiomyopathy: expanded panels offer limited additional sensitivity. Genet Med. 2015 Nov;17(11):880-8.