Variant ID	Name	Type	Effect	Location	cDNA Change	Protein Change	Cases Reported	MAF*	Legacy Nomenclature	Comments	Known Phenotypic effect
											In vivo	In vitro
992	rs510317	Point	Promoter	Flanking (5')	c.-402A>G		1	0.2326	0	Comparison of PrASE and Pyrosequencing for SNP Genotyping	The rare c.-402A allele was associated with significantly higher FVII:C and FVII:Ag levels than subjects homozygous for the common c.-402G allele (p<0.05) (16038716)"	The rare c.-402A allele confers increased transcriptional activity and is associated with increased plasma FVII:C level (10233895). The allelic variant c.-402A showed a statistically significant increase in expression levels (increase of 50.99%) (17292373)"
991	rs510335	Point	Promoter	Flanking (5')	c.-401G>T		1	0.2041	0	In complete allelic association with c.-325_-324ins10 and c.-122C	No variant-specific in vivo studies as the c.-401T variant is in complete association with c.-325_-324ins10 (10233895)"	The allelic variant c.-401T showed an increase of 39.04% when analyzed alone. By contrast, this effect disappeared when combined with c.-325_-324ins10 (17292373)"
996	rs5742910	Insertion	Promoter	Flanking (5')	c.-325_-324insCCTATATCCT		80	0.23	0	In linkage disequilibrium with p.Arg413Gln	Genetic variation associated with the c.-325_-324ins10 polymorphism contributes to 26% and 23% of the variance of FVII:C and FVII:Ag respectively (8548429)"	Decanucleotide insert at c.-325 is shown to reduce promoter activity by 33% compared with wild type (reporter gene constructs in HepG2) (8576177). This was confirmed in both individual and combined allelic variants experiments) (17292373)
995	rs561241	Point	Promoter	Flanking (5')	c.-122T>C		5	0.1436	0	In complete allelic association with c.-325_-324ins10 and c.-401T (possible exceptions)	No in vivo studies as the c.-122C variant is in complete association with c.-325_-324ins10	The allelic variant c.-122C caused a statistically significant reduction in expression level at 39.90% (reporter plasmids containing individual allelic variant) (17292373)"
993	rs6039	Point	Intronic	Intron (1)	c.64+9G>A		7	0.2096	0	In linkage disequilibrium with p.Arg413Gln	Due to the linkage disequilibrium, they could not establish whether the c.64+9G>A allele variant contributed per se to lowering FVII:C levels study (10691850)"	There is no in vitro study
999	rs6042	Point	Silent	Exon (6)	c.525C>T	p.His175=	64	0.1419	0
988	VNTR[8]	Indel	Intronic	Exon (8)	c.795_805+26[8]		1		0	VNTR[6] is the Wild Type	Due to the low frequency of this allele, no large studies were published. Subjects carring an H8 allele showed a high FVIIa level	A quantitative analysis of transcripts indicated a parallel decrease of the IVS7 repeat number and mRNA relative expression (VNTR[6] being considered as a reference). VNTR[8] showed higher values than VNTR[6] (10828024)"
989	VNTR[5]	Indel	Intronic	Exon (8)	c.795_805+26[5]		0		0	VNTR[6] is the Wild Type	Due to the low frequency of this allele, no large studies were published. Subjects with the H5 allele (without c.-325ins10 neither p.413Gln) showed lower FVII levels than controls.	A quantitative analysis of transcripts indicated a parallel decrease of the IVS7 repeat number and mRNA relative expression (VNTR[6] being considered as a reference). VNTR[5] showed lower values than VNTR[6] (10828024)"
990	VNTR[7]	Indel	Intronic	Exon (8)	c.795_805+26[7]		89	0.31	0	VNTR[6] is the Wild Type	Genetic variation associated with the c.795_805+26[7] polymorphism contributes to 17% and 13% of the variance of FVII:C and FVII:Ag respectively (8548429)"	A quantitative analysis of transcripts indicated a parallel decrease of the IVS7 repeat number and mRNA relative expression (VNTR[6] being considered as a reference). VNTR[7] showed higher values than VNTR[6] (10828024)"
994	rs6041	Point	Intronic	Intron (8)	c.806-20G>A		45	0.1342	0	Ischemic stroke is associated with the ABO locus: the EuroCLOT study.
998	rs6046	Point	Missense	Exon (9)	c.1238G>A	p.Arg413Gln	116	0.1341	0	In linkage disequilibrium with the c.-401T/c.-325_-324ins10/c.-122C haplotype	Genetic variation associated with the p.Arg413Gln polymorphism contributes to 30% and 23% of the variance of FVII:C and FVII:Ag respectively (8548429; 9409261)"	Transient transfection assays with a F7 cDNA containing the base substitution resulting in Gln413 showed a FVII secretion decrease to 74% compared to wild type (9409261)"

^*MAF - Minor Allele Frequency (according to 1000 Genomes database).