We estimate the penetrance of LQTS for KCNH2 L15P is 13%. We are unaware of any observations of this variant in individuals. L15P is not present in gnomAD. We have tested the trafficking efficiency of this variant, 64% of WT with a standard error of 14%; in our analysis we used SE < 20% as 'high quality'. Approximately below 50% of WT is considered PS3 moderate and below 30% is PS3 strong. L15P has not been functionally characterized. This residue is located in a Mild_Hotspot region for LQT2. In silico predictions, functional data (if available), and location in structure are equivalent to observing 1 individuals with LQT2 and 9 unaffected individuals.These data combined with observations of carriers lead us to estimate the LQTS penetrance for KCNQ1 L15P around 13% (1/10).

PROVEAN	PolyPhen-2	BLAST-PSSM	REVEL	Penetrance Density (%)
-3.947	1.0	-4	0.874	21

PROVEAN scores less than -2 are considered deleterious. REVEL scores higher than 0.5 or 0.75 are considered likely pathogenic (higher sensitivity with the former cutoff, higher specificity with the latter cutoff). A PolyPhen-2 score of 0.85 or greater is considered likely pathogenic. BLAST-PSSM reflects the evolutionary conservation of residue substitutions, more negative numbers indicate fewer observations of the specific substitution than is expected. Penetrance density is our previously published method to calculate the average LQTS probability density in a shell of residues surrounding a residue of interest (Kroncke et al. 2019).

PubMed ID	Year	Carriers	Unaffected	LQT2	Other Disease
LITERATURE, COHORT, AND GNOMAD:	-	0	0	0	-
VARIANT FEATURES ALONE:	-	10	9	1	-

Summary totals might not agree with the literature table because of duplicate patients, which were excluded from the total counts. We do not distinguish here between multiple missense codons. Missense variants are combined across degenerate codon substitutions since codon-level data were not consistently available for curation.

A residue within a folded protein on average has nearest neighbors that fall roughly into two shells: a "nearest" neighbor around 5-6 angstroms and a second shell around 11 angstroms. NOTE: some residues appear multiple times at different distances since the functional K_V11.1 channel (protein product of KCNH2/hERG) is a homotetramer and occasionally the same residue from multiple subunits is present within the 15A window. All variants shown in the rightmost column have been observed in at least one individual in the literature or gnomAD.

Neighbor	Distance (Angstroms)	Variants Observed in Individuals
15	0	L15V,
14	4
18	6	I18M,
16	6	D16A,
12	6	N12D,
13	6	T13N,
17	6
19	7	I19F,
798	7	I798fsX,
31	8	I31S,
124	8	M124T, M124R,
788	8	E788D, E788D, E788K,
825	8
795	9	V795I,
43	9	Y43C, Y43D,
42	9	I42N,
786	9
115	10	V115M,
797	10	A797T,
11	10	Q11H, Q11L, Q11H,
10	10
126	10
123	10
32	10	A32T,
20	11	R20L, R20G,
33	11	N33T,
22	11	F22Y, F22S,
29	11	F29L, F29L, F29S, F29V, F29L,
21	11
787	11
826	11	T826I, T826A,
796	11	V796L, V796Del, V796L,
799	12	L799sp,
824	12
30	12	I30Del, I30T,
9	12	A9T, A9V,
125	12
800	12
785	12	G785D, G785S, G785fsX,
789	12
790	13
44	13	C44X, C44F, C44W,
794	13	V794D, V794I,
41	13	V41A,
23	13
823	13	R823fsX, R823W, R823T, R823Q,
117	13
114	13	P114S,
113	13	V113Del,
45	13	N45K, N45K, N45D,
34	14	A34T,
116	14	K116Q,
127	14
122	14
40	14
765	14
828	14
60	15	M60T,
793	15	D793N,
766	15
801	15	K801T,
35	15	R35W,
121	15	A121fsX,