We estimate the penetrance of LQTS for SCN5A F1596I around 16% and the Brugada syndrome penetrance around 2%. SCN5A F1596I was found in a total of 37 carriers in 9 papers and/or in gnomAD: 0 had Brugada syndrome, 6 had LQTS. F1596I is present in 30 alleles in gnomAD. F1596I has been functionally characterized in 11 papers. This residue is located in a Non_Hotspot region for Brugada syndrome and a Mild_Hotspot region for LQTS. In silico predictions, functional data (if available), and location in structure are equivalent to phenotyping 10 individuals for Brugada syndrome (0 diagnosed with Brugada syndrome) and 5 individuals for LQTS (0 with LQTS). These data combined with observations of carriers lead us to estimate the LQTS penetrance for SCN5A F1596I around 16% (6/47) and the Brugada syndrome penetrance around 2% (0/47).

PROVEAN	PolyPhen-2	BLAST-PSSM	REVEL	Penetrance Density BrS (%)	Penetrance Density LQT3 (%)
-4.26	0.289	-0.89	0.936	1	22

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 BrS/LQTS probability density in a shell of residues surrounding a residue of interest (Kroncke et al. 2019).

PubMed ID	Year	Carriers	Unaffected	LQT3	BrS1	Other	Other Disease
23631430	2013	1		1	0	0
24144883	2014	1		0	0	1	AF
24606995	2014	1		1	0	0
25051102	2014	1		0	0	1	VF
25163546	2015	1		0	0	1	DCM
26746457	2016	1		0	0	0
27566755	2016	5		5	0	0
22685113	2012	1		0	0	1	AF
19716085	2009	2		2	0	0
LITERATURE, COHORT, AND GNOMAD:	-	37	31	6	0		-
VARIANT FEATURES ALONE:	-	15	15	0	0	-	-

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.

Peak and late/persistent current are relative to wildtype (100% being no different from wildtype). V_0.5 act/inact are the voltages at which half of the maximal current is reached during an activation and inactivation protocol, each is in units of mV and relative to wildtype.

PubMed ID	Year	Cell Type	Peak Current (%WT)	V1/2 Act. (mV)	V1/2 Inact. (mV)	Late/Persistent Current (%WT)
23631430	2013
24144883	2014
24606995	2014
25051102	2014
25163546	2015
29017927	2017
26746457	2016
21051419	2011	CHO	120	0	0
27566755	2016
22685113	2012	HEK
19716085	2009

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. 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
1569	14	A1569P,
1586	7
1568	12
1587	7	F1587V,
1602	10
1534	15
1601	9	L1601H,
1575	7	C1575S,
1600	5
1571	11	F1571C,
1572	10
1570	15	I1570V, p.I1570dup, p.1570_F1571insI,
1599	6
1583	13	R1583H, R1583C,
1580	13
1626	13	R1626H, R1626P, R1626C, R1626L,
1603	10	I1603F,
1625	11
1585	15	Y1585C,
1576	11
1596	0	F1596C, F1596I,
1628	13
1589	11
1584	13
1632	13	R1632C, R1632L, R1632H,
1597	5	V1597M,
1573	11
1594	8	F1594S,
1588	12	T1588I,
1581	14	A1581S,
1591	12	W1591X,
1593	6	I1593M,
1595	6
1629	11	R1629Q, R1629G, R1629X,
1605	15	G1605D, c.4813+5insTGGG, c.4813+3_4813+6dupGGGT, G1605C, c.4813+2_4813+5dupTGGG,
1574	10	E1574K, c.4719C>T,
1592	8
1578	10	c.4732_4733dupAA,
1617	14	p.F1617del,
1590	11
1604	12	c.4810+3_4810+6dupGGGT, V1604M,
1622	13
1582	12	L1582P,
1621	15
1579	8	L1579fsX53,
1598	7	V1598A,
1577	13