Table 2.

Clinical severity scores based on system adapted from Al Teneiji et al. (2017)

Patient ID	Variant type	Amino acid change	First seizure/movement episode score	GDD/ID score	B6 response score	Severity score sum	Protein effect
Patients reported in this study
1	Homozygous missense	p.Thr116Ile;	3	2	2	Severe (7)	Predicted LOF - variant likely impacts PLP binding
	Homozygous missense	p.His275Asp					Variant of unknown significance: variant likely impacts PLP binding
2	Homozygous missense	p.Arg41Gln	2	0	0	Mild (2)	Predicted to still bind PLP, but stability is reduced
3	Homozygous missense	p.Glu67Lys	3	3	2	Severe (8)	Predicted LOF - variant likely impacts PLP binding
4	Compound heterozygous nonsense and missense	c.320–2A>G;	3	NAa	NAa	Deceased: Severe (9)	LOF - Truncated proteine
		p.Gly224Ala					Predicted LOF - Variant likely disrupts loop 15 structure and orientation of several PLP binding residues
5	Homozygous nonsense	p.Asp124Lys fs*2	3	NAb	NAb	Deceased: Severe (9)	LOF - Truncated protein (band absent as in Supplementary Fig 1)
6	Homozygous missense	p.Thr116Ile	3	2	3	Severe (8)	Predicted LOF - variant likely impacts PLP binding
7	Homozygous missense	p.Ile94Phe	1	1	1	Mild (3)	Predicted LOF? Variant likely impacts PLP binding, but it is possible Phe could still establish aromatic/hydrophobic contacts with PLP;
8	Homozygous missense	p.Arg41Gln	3	0	0	Mild (3)	Predicted to still bind PLP, but stability is reduced
9	Homozygous missense	p.Arg41Gln	3	0	0	Mild (3)	Predicted to still bind PLP, but stability is reduced
10	Homozygous missense	p.Glu67Lys	3	2	2	Severe (7)	Predicted LOF - variant likely impacts PLP binding
11	Homozygous missense	p.Glu67Lys	3	2	2	Severe (7)	Predicted LOF - variant likely impacts PLP binding
12	Homozygous deletion	p.Asp124Lys fs*2	3	NAd	2	NAd	LOF - Truncated protein (band absent as in Supplementary Fig 1)
Patients reported by Darin et al. (2016)
1	Homozygous nonsense	p.Ser78Ter	3	NAc	NAc	Deceased: Severe (9)	LOF - Truncated proteine
2	Homozygous nonsense	p.Ser78Ter	3	2	3	Severe (8)	LOF - Truncated proteine
3	Homozygous nonsense	p.Ser78Ter	3	3	3	Severe (9)	LOF - Truncated proteine
4	Homozygous missense	p.Leu175Pro	3	3	2	Severe (8)	LOF - Misfolded proteine,g
5	Compound heterozygous missense and missense	c.207+1G>A;	3	3	2	Severe (8)	LOF - Truncated proteine; absent band in western blote
		c.320–2A>G;
6	Homozygous nonsense	p.Gln71Ter	3	2	3	Severe (8)	LOF - Truncated proteine
7	Compound heterozygous missense	p.Pro87Leu;	1	1	1	Mild (3)	Lower solubility and some precipitated; folded forms still binds to PLPg
		p.Arg241Gln					LOF - variant abolishes PLP bindingg, drastic reduction in stability (Tm shift −14°C)g
Patients reported by Plecko et al. (2017)
1	Compound heterozygous missense and missense	p.Pro40Leu;	2	0	1	Mild (3)	Reduced stability (Tm shift −6°C); Still binds to PLPg
		p.Arg241Gln					LOF - variant abolishes PLP binding, drastic reduction in stability (Tm shift −14°C)g
2	Compound heterozygous truncating and missense	p.Ser84Cysfs*21;	2	1	1	Moderate (4)	LOF - Truncated proteinf
		p.Arg205Gln					Reduced stability (Tm shift −7°C); Still binds to PLPg
3	Homozygous missense	p.Pro87Leu	3	3	1	Severe (7)	Lower solubility and some precipitated; Folded forms still binds to PLPg
4	Homozygous missense	p.Tyr69Cys	2	0	2	Moderate (4)	Cys forms disulfide bridges, which creates an artificial dimer that hides PLP. Decreased PLP binding in 30%g

Variants are organized by whether seen homozygously versus compound heterozygous, then based on variant type (missense, truncating, splicing). Note that truncating variants are associated with the most severe phenotypes. ^aNA, ^bNA , ^cNA: full clinical scores could not be calculated due to early death of these patients but assumed severe based on lethality. ^dNA full clinical score could not yet be calculated due to early age of patient, so GDD/ID cannot yet be assessed. ^eVariant reported by Darin et al. (2016).^f Variant reported by Plecko et al. (2017). ^gVariant experimentally studied by Tremino et al. (2018). LOF = loss-of-function.