Table 2 Potentially pathogenic variants identified by whole-exome sequencing in 18 EA patients.

From: Genetic Variants Associated with Episodic Ataxia in Korea

Patient No	Family History	Gene	Exon	mRNA	Protein	Variant effect	SIFT	LRT	Polyphen	Mutation taster	GERP	MAF	Pathogenic
1	+	CACNA1A	16	c.2030 G > A	p.Gly677Glu	missense	D	D	B	D	4.58	—	possible
2	+	CACNA1A	40	c.5956 C > T	p.Gln1986*	nonsense	—	—	—	—	—	—	probable
		UBR4	100	c.14630 A > G	p.Tyr4877Cys	missense	D	D	D	D	5.75	—	possible
3	+	CACNA1A	23	c.3871_3873delGAG	p.Glu1294 DEL	deletion	—	—	—	—	—	—	probable
		SLC1A3	7	c.985 G > A	p.Ala329Thr	missense	D	D	P	D	5.71	0.0003^†	probable
4	+	CACNA1A	5	c.742 T > A	p.Tyr248Asn	missense	D	D	D	D	5.55	—	possible
5	+	CACNA1A	32	c.5005 C > T	p.Arg1669*	nonsense	—	—	—	—	—	—	probable
		CACNA1A	19	c.2992 G > C	p.Glu998Gln	missense	T	N	B	D	1.91	—	possible
		UBR4	83	c.12332 G > A	p.Arg4111His	missense	T	D	P	D	5.25	0.0001^†	possible
6	+	SLC1A3	8	c.1177 G > A	p.Val393Ile	missense	T	D	P	D	5.8	—	probable
11	+	TTBK2	15	c.3467 G > A	p.Arg1156Gln	missense	D	D	D	D	5.13	0.00002^†	possible
12	+	TGM6	10	c.1478 C > T	p.Pro493Leu	missense	T	N	D	D	4.67	0.0001^†	possible
15	−	CACNA1A	20	c.3321_3322insC	p.Gly1108Argfs40*	insertion	—	—	—	—	—	—	probable
		CACNA1A	46	c.6605_6616delACC AGGAGCGGG	p.Asp2202_Arg2205DEL	deletion	—	—	—	—	—	0.0005^†	possible
16	−	CACNA1A	29	c.4645 C > T	p.Arg1549*	nonsense	—	—	—	—	—	—	probable
19	−	ATP1A2	6	c.586 C > T	p.Arg196Cys	missense	D	D	D	D	5.11	0.00003^†	possible
22	−	SCN1A	26	c.5516 T > G	p.Ile1839Ser	missense	D	D	D	D	5.6	0.000008^†	possible
23	−	SLC1A3	7	c.952 A > G	p.Thr318Ala	missense	T	D	B	D	6.07	0.0002^†	possible
26	−	UBR4	103	c.15125 C > T	p.Ala5042Val	missense	T	D	D	D	5.39	0.0002^‡	possible
28	−	UBR4	52	c.7742 C > T	p.Ala2581Val	missense	D	D	D	D	5.95	—	possible
30	−	SCN1A	11	c.1688T > A	p.Leu563Gln	missense	D	D	D	D	5.59	—	possible
32	−	FGF14	1	c.31 A > G	p.Thr11Ala	missense	D	N	B	D	4.73	—	possible
33	−	KCND3	4	c.1291 C > T	p.Arg431Cys	missense	D	D	D	D	5.25	0.000009^†	possible

Transcript ID: ATP1A2, NM_000702.3 (NP_000693.1); CACNA1A, NM_023035.2 (NP_075461.2); FGF14, NM_175959.2 (NP_787125.1); KCND3, NM_004890.4(NP_004971.2); SCN1A, NM_006920.4 (NP_008851.3); SLC1A3, NM_004172.4 (NP_00416.3); TGM6, NM_198994.2 (NP_945345.2); TTBK2, NM_173500.3 (NP_775771.3); UBR4, NM_020765.2 (NP_065816.2). SIFT- D (damaging), T (tolerated); LRT- D (deleterious), N (neutral); Polyphen- D (probably damaging), P (possibly damaging), B (benign); MutationTaster- D (disease_causing). ^†MAF based on the Exome Aggregation Consortium (ExAC), ^‡MAF based on the 1000 Genomes Project.

Back to article page

Table 2 Potentially pathogenic variants identified by whole-exome sequencing in 18 EA patients.

Search

Quick links