Table 1.

Demographic characteristics of 1563 cardiomyopathy probands in the 100,000 Genome Project (100KGP)

		All probands (n = 1563)	Paediatric probands (n = 273)	Adult probands (n = 1290)
		n (%)	n (%)	n (%)
Sex	Female	589 (38)	115 (42)	474 (37)
	Male	974 (62)	158 (58)	816 (63)
Ancestry (self-reported)	Asian	105 (7)	32 (14a)	73 (7a)
	Black	53 (3)	10 (4a)	43 (4a)
	White	1070 (68)	180 (77a)	890 (85a)
	Mixed	21 (1)	< 10	< 20
	Other	30 (2)	< 10	< 30
	Not stated	284 (18)	39 (14)	245 (19)
Family history	Yes	659 (42)	95 (35)	564 (44)
	No	904 (58)	178 (65)	726 (56)
Primary CM	ARVC	126 (8)	9 (3)	117 (9)
	DCM	383 (25)	54 (20)	329 (26)
	HCM	794 (51)	92 (34)	702 (54)
	LVNC	50 (3)	19 (7)	31 (2)
	Mixed_CM	< 20	< 10	< 10
	Mixed_other	< 20	< 10	< 10
Complex CM		195 (12)	93 (34)	102 (8)

Primary CM: probands recruited under a specific cardiomyopathy disease category

Complex CM: probands recruited under a non-cardiomyopathy disease category with a human phenotype ontology (HPO) term containing ‘cardiomyopathy’

Counts <5 must be masked when exporting data from the 100KGP research environment. Smaller values are therefore given as ranges, e.g. <5, and percentages in these instances are not reported

Family history is recorded as ‘Yes’ if either a parent or a sibling is recorded as affected with the same condition as the proband

ARVC Arrhythmogenic right ventricular cardiomyopathy, DCM Dilated cardiomyopathy, HCM Hypertrophic cardiomyopathy, LVNC Left ventricular non-compaction cardiomyopathy, Mixed_CM, probands recruited under more than one cardiomyopathy specific category, e.g. hypertrophic cardiomyopathy and left ventricular non-compaction cardiomyopathy, Mixed_other, participants recruited under a cardiomyopathy disease category and at least one other non-cardiomyopathy category, e.g. hypertrophic cardiomyopathy and corneal abnormalities

^a% of known self-reported ancestry, excluding those where ancestry is not stated