. 2018 Jan 20;6(2):160–170. doi: 10.1002/mgg3.342

Table 1.

CBS analysis—pathogenic mutations found in patients with classical homocystinuria (n = 35)

Patient	Sex	Origin (Brazilian region)	Allele 1		Allele 2		Cons.	Age at inclusion (years)	Age of onset (years)	B6 response found	B6 response expecteda
Patient	Sex	Origin (Brazilian region)	cDNA	Protein	cDNA	Protein	Cons.	Age at inclusion (years)	Age of onset (years)	B6 response found	B6 response expecteda
1a	M	S	c.253G>Ac	p.Gly85Arg	c.253G>A	p.Gly85Arg	Y	36	6	N	N
1b	F	S	c.253G>Ac	p.Gly85Arg	c.253G>A	p.Gly85Arg	Y	27	NA	N	N
1c	F	S	c.253G>Ac	p.Gly85Arg	c.253G>A	p.Gly85Arg	Y	31	7	N	N
2	M	S	c.833T>C	p.Ile278Thr	c.833T>C	p.Ile278Thr	Y	35	0.2	Y	Y
3	M	S	c.833T>C	p.Ile278Thr	c.833T>C	p.Ile278Thr	N	35	7	Y	Y
4	F	SE	c.833T>Cc	p.Ile278Thr	c.833T>Cd	p.Ile278Thr	Y	18	15	Y	Y
5	M	SE	c.833T>C	p.Ile278Thr	c.28delG	p.Val10 fs	N	26	1	Y	Y/Nb
6	M	SE	c.833T>C	p.Ile278Thr	c.451G>A	p.Gly151Arg	N	23	4	Y	Y/Nb
7	F	S	c.833T>C	p.Ile278Thr	c.989_991delAGG	p.(Glu330del)	N	28	20	N	Y/Nb
8	M	NE	c.833T>C	p.Ile278Thr	c.828+1G>A	p.?	N	16	4	N	Nb
9	F	S	c.828+1G>Ac	p.?	c.1126G>A	p.Asp376Asn	N	23	5	N	Nb
10	M	SE	c.828+1G>Ad	p.?	c.2T>C c	p.?	N	13	1	N	Nb
11	F	S	c.828+1G>A	p.?	c.691G>C	p.Ala231Leu	N	13	1	N	Nb
12	M	NE	c.828+1G>A	p.?	c.828+1G>A	p.?	Y	8	1	N	Nb
13	M	SE	c.572C>T	p.Thr191Met	c.572C>T	p.Thr191Met	Y	26	19	N	N
14	M	SE	c.572C>T	p.Thr191Met	c.572C>T	p.Thr191Met	Y	10	5	N	N
15	F	S	c.572C>T	p.Thr191Met	c.572C>T	p.Thr191Met	Y	18	5	N	N
16	M	SE	c.572C>T	p.Thr191Met	c.572C>T	p.Thr191Met	Y	19	4	N	N
17	M	S	c.572C>T	p.Thr191Met	c.209+1delG c	p.?	N	14	8	N	Nb
18a	M	SE	c.969G>Ac	p.Trp323Ter	c.969G>Ad	p.Trp323Ter	Y	17	6	N	NA
18b	M	SE	c.969G>Ac	p.Trp323Ter	c.969G>Ad	p.Trp323Ter	Y	6	1	N	NA
19	M	NE	c.969G>A	p.Trp323Ter	c.969G>A	p.Trp323Ter	N	15	1	N	NA
20	M	NE	c.969G>A	p.Trp323Ter	c.969G>A	p.Trp323Ter	N	10	7	N	NA
21a	M	SE	c.451G>A	p.Gly151Arg	c.451G>A	p.Gly151Arg	Y	15	7.5	N	N
21b	F	SE	c.451G>A	p.Gly151Arg	c.451G>A	p.Gly151Arg	Y	14	NA	N	N
22	F	SE	c.451G>A	p.Gly151Arg	c.451G>A	p.Gly151Arg	Y	17	3	N	N
23	M	S	c.284T>C c	p.Ile95Thr	c.284T>C	p.Ile95Thr	Y	18	1	N	NA
24	M	S	c.1058C>Tc	p.Thr353Met	c.146C>T	p.Pro49Leu	N	19	3	Y	Yb
25	F	S	c.1126G>Ac	p.Asp376Asn	c.1126G>Ad	p.Asp376Asn	Y	14	1.5	N	N
26	M	S	c.444delG c	p.(Asn149 fs )	c.444delG	p.(Asn149 fs )	Y	22	1.5	N	NA
27	M	NE	c.329A>T	p.Glu110Val	c.770C>T	p.Thr257Met	N	16	3	N	Nb
28a	F	NE	c.1223+5G>T	p.?	c.1223+5G>T	p.?	Y	5	3	NA	NA
28b	F	NE	c.1223+5G>T	p.?	c.1223+5G>T	p.?	Y	7	3	NA	NA
29	F	CW	c.864_868delGAG	p.(Glu289del)	c.864_868delGAG	p.(Glu289del)	Y	17	6	N	NA
30	M	SE	c.209+1G>A	p.?	NI	NI	N	37	6	N	Nb

Novel mutations are set in bold. Patients represented by the same number belong to the same family. M, male; F, female; S, south; SE, southeast; NE, northeast; CW, central‐west; Cons, consanguinity; Y, yes; N, no; B6, pyridoxine; NA, not available; NI, not identified.

According to previously described cases in the literature (Kraus, 2017), all partially responsive patients were considered as nonresponsive.

Estimated; no identical genotype reported previously.

Mother heterozygous for mutation.

Father heterozygous for mutation.