Name: rs1050829
Published: September 21, 2022
License: Open Access

Welcome to the Reference SNP (rs) Report

All alleles are reported in the Forward orientation. Click on the Variant Details tab for details on Genomic Placement, Gene, and Amino Acid changes. HGVS names are in the HGVS tab.

Reference SNP (rs) Report

This page reports data for a single dbSNP Reference SNP variation (RefSNP or rs) from the new redesigned dbSNP build.
Top of the page reports a concise summary for the rs, with more specific details included in the corresponding tabs below.
All alleles are reported in the Forward orientation. Use the Genomic View to inspect the nucleotides flanking the variant, and its neighbors.
For more information see Help documentation.

rs1050829

Current Build 156

Released September 21, 2022

Organism: Homo sapiens
Position: chrX:154535277 (GRCh38.p14) Help
The anchor position for this RefSNP. Includes all nucleotides potentially affected by this change, thus it can differ from HGVS, which is right-shifted. See here for details.
Alleles: T>A / T>C
Variation Type: SNV Single Nucleotide Variation
Frequency: C=0.010973 (1435/130772, ALFA)
C=0.0982 (472/4805, 1000G_30x)
C=0.0946 (357/3775, 1000G) (+ 5 more)
C=0.0008 (3/3708, TWINSUK)
C=0.0003 (1/2889, ALSPAC)
C=0.046 (5/108, Qatari)
C=0.00 (0/52, Ancient Sardinia)
T=0.10 (2/20, SGDP_PRJ)

Clinical Significance: Reported in ClinVar
Gene : Consequence: G6PD : Missense Variant
Publications: 45 citations
Genomic View: See rs on genome

ALFA Allele Frequency
The ALFA project provide aggregate allele frequency from dbGaP. More information is available on the project page including descriptions, data access, and terms of use.

Release Version: 20230706150541

Population	Group	Sample Size	Ref Allele	Alt Allele
Total	Global	130772	T=0.989027	A=0.000000, C=0.010973
European	Sub	114918	T=0.999417	A=0.000000, C=0.000583
African	Sub	6124	T=0.7921	A=0.0000, C=0.2079
African Others	Sub	210	T=0.724	A=0.000, C=0.276
African American	Sub	5914	T=0.7946	A=0.0000, C=0.2054
Asian	Sub	3348	T=1.0000	A=0.0000, C=0.0000
East Asian	Sub	2690	T=1.0000	A=0.0000, C=0.0000
Other Asian	Sub	658	T=1.000	A=0.000, C=0.000
Latin American 1	Sub	432	T=0.954	A=0.000, C=0.046
Latin American 2	Sub	908	T=0.990	A=0.000, C=0.010
South Asian	Sub	274	T=1.000	A=0.000, C=0.000
Other	Sub	4768	T=0.9862	A=0.0000, C=0.0138

Frequency tab displays a table of the reference and alternate allele frequencies reported by various studies and populations. Table lines, where Population="Global" refer to the entire study population, whereas lines, where Group="Sub", refer to a study-specific population subgroupings (i.e. AFR, CAU, etc.), if available. Frequency for the alternate allele (Alt Allele) is a ratio of samples observed-to-total, where the numerator (observed samples) is the number of chromosomes in the study with the minor allele present (found in "Sample size", where Group="Sub"), and the denominator (total samples) is the total number of all chromosomes in the study for the variant (found in "Sample size", where Group="Study-wide" and Population="Global").

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Study	Population	Group	Sample Size	Ref Allele	Alt Allele
Allele Frequency Aggregator	Total	Global	130772	T=0.989027	A=0.000000, C=0.010973
Allele Frequency Aggregator	European	Sub	114918	T=0.999417	A=0.000000, C=0.000583
Allele Frequency Aggregator	African	Sub	6124	T=0.7921	A=0.0000, C=0.2079
Allele Frequency Aggregator	Other	Sub	4768	T=0.9862	A=0.0000, C=0.0138
Allele Frequency Aggregator	Asian	Sub	3348	T=1.0000	A=0.0000, C=0.0000
Allele Frequency Aggregator	Latin American 2	Sub	908	T=0.990	A=0.000, C=0.010
Allele Frequency Aggregator	Latin American 1	Sub	432	T=0.954	A=0.000, C=0.046
Allele Frequency Aggregator	South Asian	Sub	274	T=1.000	A=0.000, C=0.000
1000Genomes_30x	Global	Study-wide	4805	T=0.9018	C=0.0982
1000Genomes_30x	African	Sub	1328	T=0.6627	C=0.3373
1000Genomes_30x	Europe	Sub	961	T=0.996	C=0.004
1000Genomes_30x	South Asian	Sub	883	T=1.000	C=0.000
1000Genomes_30x	East Asian	Sub	878	T=1.000	C=0.000
1000Genomes_30x	American	Sub	755	T=0.974	C=0.026
1000Genomes	Global	Study-wide	3775	T=0.9054	C=0.0946
1000Genomes	African	Sub	1003	T=0.6620	C=0.3380
1000Genomes	Europe	Sub	766	T=0.996	C=0.004
1000Genomes	East Asian	Sub	764	T=1.000	C=0.000
1000Genomes	South Asian	Sub	718	T=1.000	C=0.000
1000Genomes	American	Sub	524	T=0.971	C=0.029
UK 10K study - Twins	TWIN COHORT	Study-wide	3708	T=0.9992	C=0.0008
The Avon Longitudinal Study of Parents and Children	PARENT AND CHILD COHORT	Study-wide	2889	T=0.9997	C=0.0003
Qatari	Global	Study-wide	108	T=0.954	C=0.046
Ancient Sardinia genome-wide 1240k capture data generation and analysis	Global	Study-wide	52	T=1.00	C=0.00
SGDP_PRJ	Global	Study-wide	20	T=0.10	C=0.90

Variant Details tab shows known variant placements on genomic sequences: chromosomes (NC_), RefSeqGene, pseudogenes or genomic regions (NG_), and in a separate table: on transcripts (NM_) and protein sequences (NP_). The corresponding transcript and protein locations are listed in adjacent lines, along with molecular consequences from Sequence Ontology. When no protein placement is available, only the transcript is listed. Column "Codon[Amino acid]" shows the actual base change in the format of "Reference > Alternate" allele, including the nucleotide codon change in transcripts, and the amino acid change in proteins, respectively, allowing for known ribosomal slippage sites. To view nucleotides adjacent to the variant use the Genomic View at the bottom of the page - zoom into the sequence until the nucleotides around the variant become visible.

Genomic Placements

Sequence name	Change
GRCh38.p14 chr X	NC_000023.11:g.154535277T>A
GRCh38.p14 chr X	NC_000023.11:g.154535277T>C
GRCh37.p13 chr X fix patch HG1497_PATCH	NW_003871103.3:g.1969256T>A
GRCh37.p13 chr X fix patch HG1497_PATCH	NW_003871103.3:g.1969256T>C
G6PD RefSeqGene	NG_009015.2:g.17296A>T
G6PD RefSeqGene	NG_009015.2:g.17296A>G
GRCh37.p13 chr X	NC_000023.10:g.153763492T>A
GRCh37.p13 chr X	NC_000023.10:g.153763492T>C

Gene: G6PD, glucose-6-phosphate dehydrogenase (minus strand)

Molecule type	Change	Amino acid[Codon]	SO Term
G6PD transcript variant 1	NM_000402.4:c.466A>T	N [AAT] > Y [TAT]	Coding Sequence Variant
glucose-6-phosphate 1-dehydrogenase isoform a	NP_000393.4:p.Asn156Tyr	N (Asn) > Y (Tyr)	Missense Variant
G6PD transcript variant 1	NM_000402.4:c.466A>G	N [AAT] > D [GAT]	Coding Sequence Variant
glucose-6-phosphate 1-dehydrogenase isoform a	NP_000393.4:p.Asn156Asp	N (Asn) > D (Asp)	Missense Variant
G6PD transcript variant 3	NM_001360016.2:c.376A>T	N [AAT] > Y [TAT]	Coding Sequence Variant
glucose-6-phosphate 1-dehydrogenase isoform b	NP_001346945.1:p.Asn126Tyr	N (Asn) > Y (Tyr)	Missense Variant
G6PD transcript variant 3	NM_001360016.2:c.376A>G	N [AAT] > D [GAT]	Coding Sequence Variant
glucose-6-phosphate 1-dehydrogenase isoform b	NP_001346945.1:p.Asn126Asp	N (Asn) > D (Asp)	Missense Variant
G6PD transcript variant 2	NM_001042351.3:c.376A>T	N [AAT] > Y [TAT]	Coding Sequence Variant
glucose-6-phosphate 1-dehydrogenase isoform b	NP_001035810.1:p.Asn126Tyr	N (Asn) > Y (Tyr)	Missense Variant
G6PD transcript variant 2	NM_001042351.3:c.376A>G	N [AAT] > D [GAT]	Coding Sequence Variant
glucose-6-phosphate 1-dehydrogenase isoform b	NP_001035810.1:p.Asn126Asp	N (Asn) > D (Asp)	Missense Variant

Clinical Significance tab shows a list of clinical significance entries from ClinVar associated with the variation, per allele. Click on the RCV accession (i.e. RCV000001615.2) or Allele ID (i.e. 12274) to access full ClinVar report.

Allele: A (allele ID: 1526181 )

ClinVar Accession	Disease Names	Clinical Significance
RCV002170707.3	Anemia, nonspherocytic hemolytic, due to G6PD deficiency	Likely-Benign

Allele: C (allele ID: 25399 )

ClinVar Accession	Disease Names	Clinical Significance
RCV000011073.8	G6PD A+	Other
RCV000011075.16	G6PD deficiency	Pathogenic
RCV000011109.5	G6PD SANTAMARIA	Other
RCV000079405.24	not provided	Conflicting-Interpretations-Of-Pathogenicity
RCV000178823.18	Anemia, nonspherocytic hemolytic, due to G6PD deficiency	Conflicting-Interpretations-Of-Pathogenicity
RCV000307631.4	G6PD deficiency	Likely-Benign
RCV000477820.2	Anemia, nonspherocytic hemolytic, due to G6PD deficiency,Malaria, susceptibility to	Pathogenic
RCV000761430.2	Bone mineral density quantitative trait locus 18	Benign
RCV000999876.4	not specified	Likely-Benign
RCV001095678.2	Anemia, nonspherocytic hemolytic, due to G6PD deficiency,G6PD deficiency	Pathogenic
RCV001267359.2	Inborn genetic diseases	Pathogenic
RCV001375611.2	Anemia, nonspherocytic hemolytic, due to G6PD deficiency	Pathogenic

Aliases tab displays HGVS names representing the variant placements and allele changes on genomic, transcript and protein sequences, per allele. HGVS name is an expression for reporting sequence accession and version, sequence type, position, and allele change. The column "Note" can have two values: "diff" means that there is a difference between the reference allele (variation interval) at the placement reported in HGVS name and the reference alleles reported in other HGVS names, and "rev" means that the sequence of this variation interval at the placement reported in HGVS name is in reverse orientation to the sequence(s) of this variation in other HGVS names not labeled as "rev".

Placement	T=	A	C
GRCh38.p14 chr X	NC_000023.11:g.154535277=	NC_000023.11:g.154535277T>A	NC_000023.11:g.154535277T>C
GRCh37.p13 chr X fix patch HG1497_PATCH	NW_003871103.3:g.1969256=	NW_003871103.3:g.1969256T>A	NW_003871103.3:g.1969256T>C
G6PD RefSeqGene	NG_009015.2:g.17296=	NG_009015.2:g.17296A>T	NG_009015.2:g.17296A>G
G6PD transcript variant 1	NM_000402.4:c.466=	NM_000402.4:c.466A>T	NM_000402.4:c.466A>G
G6PD transcript variant 1	NM_000402.3:c.466=	NM_000402.3:c.466A>T	NM_000402.3:c.466A>G
G6PD transcript variant 2	NM_001042351.3:c.376=	NM_001042351.3:c.376A>T	NM_001042351.3:c.376A>G
G6PD transcript variant 2	NM_001042351.2:c.376=	NM_001042351.2:c.376A>T	NM_001042351.2:c.376A>G
G6PD transcript variant 2	NM_001042351.1:c.376=	NM_001042351.1:c.376A>T	NM_001042351.1:c.376A>G
G6PD transcript variant 3	NM_001360016.2:c.376=	NM_001360016.2:c.376A>T	NM_001360016.2:c.376A>G
G6PD transcript variant 1	NM_001360016.1:c.376=	NM_001360016.1:c.376A>T	NM_001360016.1:c.376A>G
GRCh37.p13 chr X	NC_000023.10:g.153763492=	NC_000023.10:g.153763492T>A	NC_000023.10:g.153763492T>C
glucose-6-phosphate 1-dehydrogenase isoform a	NP_000393.4:p.Asn156=	NP_000393.4:p.Asn156Tyr	NP_000393.4:p.Asn156Asp
glucose-6-phosphate 1-dehydrogenase isoform b	NP_001035810.1:p.Asn126=	NP_001035810.1:p.Asn126Tyr	NP_001035810.1:p.Asn126Asp
glucose-6-phosphate 1-dehydrogenase isoform b	NP_001346945.1:p.Asn126=	NP_001346945.1:p.Asn126Tyr	NP_001346945.1:p.Asn126Asp

Submissions tab displays variations originally submitted to dbSNP, now supporting this RefSNP cluster (rs). We display Submitter handle, Submission identifier, Date and Build number, when the submission appeared for the first time. Direct submissions to dbSNP have Submission ID in the form of an ss-prefixed number (ss#). Other supporting variations are listed in the table without ss#.

65 SubSNP, 16 Frequency, 13 ClinVar submissions

No	Submitter	Submission ID	Date (Build)
1	LEE	ss1525831	Oct 05, 2000 (86)
2	WICVAR	ss3177126	Aug 15, 2001 (102)
3	SC_JCM	ss3526371	Sep 28, 2001 (100)
4	LEE	ss4416360	May 29, 2002 (106)
5	CSHL-HAPMAP	ss18052006	Feb 27, 2004 (120)
6	SEQUENOM	ss24796045	Sep 20, 2004 (123)
7	ABI	ss43577126	Mar 13, 2006 (126)
8	CORNELL	ss86241800	Mar 23, 2008 (129)
9	SNP500CANCER	ss105436778	Feb 04, 2009 (130)
10	1000GENOMES	ss115337861	Jan 25, 2009 (130)
11	SEATTLESEQ	ss159746045	Dec 01, 2009 (131)
12	COMPLETE_GENOMICS	ss165817158	Jul 04, 2010 (132)
13	OMICIA	ss244239872	Aug 29, 2012 (137)
14	OMIM-CURATED-RECORDS	ss289479822	Jan 06, 2011 (133)
15	1000GENOMES	ss341909269	May 09, 2011 (134)
16	NHLBI-ESP	ss342562465	May 09, 2011 (134)
17	1000GENOMES	ss491206105	May 04, 2012 (137)
18	EXOME_CHIP	ss491580926	May 04, 2012 (137)
19	ILLUMINA	ss535323435	Sep 11, 2015 (146)
20	TISHKOFF	ss567108039	Apr 25, 2013 (138)
21	JMKIDD_LAB	ss1067612240	Apr 09, 2015 (144)
22	1000GENOMES	ss1556698416	Apr 09, 2015 (144)
23	EVA_UK10K_ALSPAC	ss1641785229	Apr 09, 2015 (144)
24	EVA_UK10K_TWINSUK	ss1684779262	Apr 09, 2015 (144)
25	EVA_EXAC	ss1694662810	Apr 09, 2015 (144)
26	EVA_EXAC	ss1694662811	Apr 09, 2015 (144)
27	WEILL_CORNELL_DGM	ss1939852051	Feb 17, 2016 (147)
28	ILLUMINA	ss1945981458	Feb 17, 2016 (147)
29	ILLUMINA	ss1958229242	Feb 17, 2016 (147)
30	ILLUMINA	ss1958229243	Feb 17, 2016 (147)
31	HUMAN_LONGEVITY	ss2321325427	Dec 20, 2016 (150)
32	ILLUMINA	ss2634991674	Oct 13, 2018 (152)
33	ILLUMINA	ss2711191349	Oct 13, 2018 (152)
34	GNOMAD	ss2745625036	Oct 13, 2018 (152)
35	GNOMAD	ss2746166238	Oct 13, 2018 (152)
36	GNOMAD	ss2984756196	Oct 13, 2018 (152)
37	AFFY	ss2985493628	Oct 13, 2018 (152)
38	AFFY	ss2986139339	Oct 13, 2018 (152)
39	ILLUMINA	ss3023047875	Oct 13, 2018 (152)
40	ILLUMINA	ss3626004428	Oct 13, 2018 (152)
41	ILLUMINA	ss3630501801	Oct 13, 2018 (152)
42	ILLUMINA	ss3645020372	Oct 13, 2018 (152)
43	ILLUMINA	ss3653606143	Oct 13, 2018 (152)
44	ILLUMINA	ss3654261379	Oct 13, 2018 (152)
45	ILLUMINA	ss3726710870	Jul 14, 2019 (153)
46	ILLUMINA	ss3744335273	Jul 14, 2019 (153)
47	KHV_HUMAN_GENOMES	ss3823525347	Jul 14, 2019 (153)
48	EVA	ss3825516080	Apr 27, 2020 (154)
49	SGDP_PRJ	ss3892536823	Apr 27, 2020 (154)
50	FSA-LAB	ss3984446471	Apr 27, 2021 (155)
51	EVA	ss3985974748	Apr 27, 2021 (155)
52	EVA	ss3986888537	Apr 27, 2021 (155)
53	GNOMAD	ss4381199084	Apr 27, 2021 (155)
54	GNOMAD	ss4381199085	Apr 27, 2021 (155)
55	TOPMED	ss5141613329	Apr 27, 2021 (155)
56	TOPMED	ss5141613330	Apr 27, 2021 (155)
57	1000G_HIGH_COVERAGE	ss5314364529	Oct 17, 2022 (156)
58	HUGCELL_USP	ss5505716667	Oct 17, 2022 (156)
59	EVA	ss5512474065	Oct 17, 2022 (156)
60	1000G_HIGH_COVERAGE	ss5623703419	Oct 17, 2022 (156)
61	SANFORD_IMAGENETICS	ss5624741787	Oct 17, 2022 (156)
62	SANFORD_IMAGENETICS	ss5666098068	Oct 17, 2022 (156)
63	EVA	ss5848241670	Oct 17, 2022 (156)
64	EVA	ss5848748608	Oct 17, 2022 (156)
65	EVA	ss5979247997	Oct 17, 2022 (156)
66	1000Genomes	NC_000023.10 - 153763492	Oct 13, 2018 (152)
67	1000Genomes_30x	NC_000023.11 - 154535277	Oct 17, 2022 (156)
68	The Avon Longitudinal Study of Parents and Children	NC_000023.10 - 153763492	Oct 13, 2018 (152)
69	ExAC Submission ignored due to conflicting rows: Row 10174658 (NC_000023.10:153763491:T:T 85203/87430, NC_000023.10:153763491:T:C 2227/87430) Row 10174659 (NC_000023.10:153763491:T:T 87422/87430, NC_000023.10:153763491:T:A 8/87430)	-	Oct 13, 2018 (152)
70	ExAC Submission ignored due to conflicting rows: Row 10174658 (NC_000023.10:153763491:T:T 85203/87430, NC_000023.10:153763491:T:C 2227/87430) Row 10174659 (NC_000023.10:153763491:T:T 87422/87430, NC_000023.10:153763491:T:A 8/87430)	-	Oct 13, 2018 (152)
71	gnomAD - Genomes Submission ignored due to conflicting rows: Row 594566002 (NC_000023.11:154535276:T:A 2/103967) Row 594566003 (NC_000023.11:154535276:T:C 10202/103956)	-	Apr 27, 2021 (155)
72	gnomAD - Genomes Submission ignored due to conflicting rows: Row 594566002 (NC_000023.11:154535276:T:A 2/103967) Row 594566003 (NC_000023.11:154535276:T:C 10202/103956)	-	Apr 27, 2021 (155)
73	gnomAD - Exomes Submission ignored due to conflicting rows: Row 14954572 (NC_000023.10:153763491:T:T 183346/183378, NC_000023.10:153763491:T:A 32/183378) Row 14954573 (NC_000023.10:153763491:T:T 178674/183378, NC_000023.10:153763491:T:C 4704/183378)	-	Jul 14, 2019 (153)
74	gnomAD - Exomes Submission ignored due to conflicting rows: Row 14954572 (NC_000023.10:153763491:T:T 183346/183378, NC_000023.10:153763491:T:A 32/183378) Row 14954573 (NC_000023.10:153763491:T:T 178674/183378, NC_000023.10:153763491:T:C 4704/183378)	-	Jul 14, 2019 (153)
75	Ancient Sardinia genome-wide 1240k capture data generation and analysis	NC_000023.10 - 153763492	Apr 27, 2021 (155)
76	Qatari	NC_000023.10 - 153763492	Apr 27, 2020 (154)
77	SGDP_PRJ	NC_000023.10 - 153763492	Apr 27, 2020 (154)
78	TopMed Submission ignored due to conflicting rows: Row 705219686 (NC_000023.11:154535276:T:A 24/264690) Row 705219687 (NC_000023.11:154535276:T:C 27207/264690)	-	Apr 27, 2021 (155)
79	TopMed Submission ignored due to conflicting rows: Row 705219686 (NC_000023.11:154535276:T:A 24/264690) Row 705219687 (NC_000023.11:154535276:T:C 27207/264690)	-	Apr 27, 2021 (155)
80	UK 10K study - Twins	NC_000023.10 - 153763492	Oct 13, 2018 (152)
81	ALFA	NC_000023.11 - 154535277	Apr 27, 2021 (155)
82	ClinVar	RCV000011073.8	Oct 17, 2022 (156)
83	ClinVar	RCV000011075.16	Oct 17, 2022 (156)
84	ClinVar	RCV000011109.5	Oct 17, 2022 (156)
85	ClinVar	RCV000079405.24	Oct 17, 2022 (156)
86	ClinVar	RCV000178823.18	Oct 17, 2022 (156)
87	ClinVar	RCV000307631.4	Oct 17, 2022 (156)
88	ClinVar	RCV000477820.2	Oct 17, 2022 (156)
89	ClinVar	RCV000761430.2	Oct 17, 2022 (156)
90	ClinVar	RCV000999876.4	Oct 17, 2022 (156)
91	ClinVar	RCV001095678.2	Oct 17, 2022 (156)
92	ClinVar	RCV001267359.2	Oct 17, 2022 (156)
93	ClinVar	RCV001375611.2	Oct 17, 2022 (156)
94	ClinVar	RCV002170707.3	Oct 17, 2022 (156)

History tab displays RefSNPs (Associated ID) from previous builds (Build) that now support the current RefSNP, and the dates, when the history was updated for each Associated ID (History Updated).

Associated ID	History Updated (Build)
rs2230035	Jan 04, 2002 (102)
rs3191189	Jul 03, 2002 (106)

Added to this RefSNP Cluster:

Submission IDs	Observation SPDI	Canonical SPDI	Source RSIDs
ss1694662811, ss2745625036, ss5512474065	NC_000023.10:153763491:T:A	NC_000023.11:154535276:T:A	(self)
RCV002170707.3, 12014791718, ss4381199084, ss5141613329	NC_000023.11:154535276:T:A	NC_000023.11:154535276:T:A	(self)
ss115337861, ss165817158	NC_000023.9:153416685:T:C	NC_000023.11:154535276:T:C	(self)
84651633, 46612239, 1200675, 21893973, 44553803, 46612239, ss341909269, ss342562465, ss491206105, ss491580926, ss535323435, ss567108039, ss1067612240, ss1556698416, ss1641785229, ss1684779262, ss1694662810, ss1939852051, ss1945981458, ss1958229242, ss1958229243, ss2634991674, ss2711191349, ss2745625036, ss2746166238, ss2984756196, ss2985493628, ss2986139339, ss3023047875, ss3626004428, ss3630501801, ss3645020372, ss3653606143, ss3654261379, ss3744335273, ss3825516080, ss3892536823, ss3984446471, ss3985974748, ss3986888537, ss5512474065, ss5624741787, ss5666098068, ss5848241670, ss5848748608, ss5979247997	NC_000023.10:153763491:T:C	NC_000023.11:154535276:T:C	(self)
RCV000011073.8, RCV000011075.16, RCV000011109.5, RCV000079405.24, RCV000178823.18, RCV000307631.4, RCV000477820.2, RCV000761430.2, RCV000999876.4, RCV001095678.2, RCV001267359.2, RCV001375611.2, 111229354, 12014791718, ss244239872, ss289479822, ss2321325427, ss3726710870, ss3823525347, ss4381199085, ss5141613330, ss5314364529, ss5505716667, ss5623703419	NC_000023.11:154535276:T:C	NC_000023.11:154535276:T:C	(self)
ss18052006	NT_025965.12:1115113:T:C	NC_000023.11:154535276:T:C	(self)
ss1525831, ss3177126, ss3526371, ss4416360, ss24796045, ss43577126, ss86241800, ss105436778, ss159746045	NT_167198.1:4681429:T:C	NC_000023.11:154535276:T:C	(self)

Publications tab displays PubMed articles citing the variation as a listing of PMID, Title, Author, Year, Journal, ordered by Year, descending.

45 citations for rs1050829

PMID	Title	Author	Year	Journal
5448	Genetic variants of human erythrocyte glucose-6-phosphate dehydrogenase. Kinetic and thermodynamic parameters of variants A, B, and A- in relation to quaternary structure.	Babalola AO et al.	1976	The Journal of biological chemistry
669721	A variant glucose-6-phosphate dehydrogenase Gd(-) Chiapas associated with moderate enzyme deficiency and occasional hemolytic anemia.	Lisker R et al.	1978	Human genetics
903703	A glucose 6-phosphate dehydrogenase Gd (-) Castilla variant characterized by mild deficiency associated with drug-induced hemolytic anemia.	Lisker R et al.	1977	The Journal of laboratory and clinical medicine
1303173	Both mutations in G6PD A- are necessary to produce the G6PD deficient phenotype.	Town M et al.	1992	Human molecular genetics
1631957	The molecular basis of glucose-6-phosphate dehydrogenase deficiency.	Vulliamy T et al.	1992	Trends in genetics
1978554	The NT 1311 polymorphism of G6PD: G6PD Mediterranean mutation may have originated independently in Europe and Asia.	Beutler E et al.	1990	American journal of human genetics
2253938	Genetic heterogeneity at the glucose-6-phosphate dehydrogenase locus in southern Italy: a study on a population from the Matera district.	Calabrò V et al.	1990	Human genetics
2503817	G6PD mahidol, a common deficient variant in South East Asia is caused by a (163)glycine----serine mutation.	Vulliamy TJ et al.	1989	Nucleic acids research
2572288	Molecular heterogeneity of glucose-6-phosphate dehydrogenase A-.	Beutler E et al.	1989	Blood
2836867	Molecular cloning and nucleotide sequence of cDNA for human glucose-6-phosphate dehydrogenase variant A(-).	Hirono A et al.	1988	Proceedings of the National Academy of Sciences of the United States of America
2912886	Chronic nonspherocytic hemolytic anemia (CNSHA) and glucose 6 phosphate dehydrogenase (G6PD) deficiency in a patient with familial amyloidotic polyneuropathy (FAP). Molecular study of a new variant (G6PD Clinic) with markedly acidic pH optimum.	Vives-Corrons JL et al.	1989	Human genetics
3393536	Diverse point mutations in the human glucose-6-phosphate dehydrogenase gene cause enzyme deficiency and mild or severe hemolytic anemia.	Vulliamy TJ et al.	1988	Proceedings of the National Academy of Sciences of the United States of America
3446582	A single nucleotide base transition is the basis of the common human glucose-6-phosphate dehydrogenase variant A (+).	Takizawa T et al.	1987	Genomics
4388132	Human glucose 6-phosphate dehydrogenase: purification and characterization of Negro type variant (A+) and comparison with normal enzyme (B+).	Yoshida A et al.	1967	Biochemical genetics
5492291	Amino acid substitution (histidine to tyrosine) in a glucose-6-phosphate dehydrogenase variant (G6PD Hektoen) associated with over-production.	Yoshida A et al.	1970	Journal of molecular biology
6433630	A glucose-6-phosphate dehydrogenase variant, Gd(-) Santamaria found in Costa Rica.	Sáenz GF et al.	1984	Acta haematologica
7106752	Heterogeneity of "Mediterranean type" glucose-6-phosphate dehydrogenase (G6PD) deficiency in Spain and description of two new variants associated with favism.	Vives Corrons JL et al.	1982	Human genetics
7291768	[Federal District glucose-6-phosphate dehydrogenase Gd(-). A new variant associated with moderate enzyme deficiency and occasional hemolytic anemia].	Lisker R et al.	1981	Revista de investigacion clinica; organo del Hospital de Enfermedades de la Nutricion
7949118	G6PD deficiency.	Beutler E et al.	1994	Blood
10734064	Structural defects underlying protein dysfunction in human glucose-6-phosphate dehydrogenase A(-) deficiency.	Gómez-Gallego F et al.	2000	The Journal of biological chemistry
12367584	Molecular heterogeneity of G6PD deficiency in an Amazonian population and description of four new variants.	Hamel AR et al.	2002	Blood cells, molecules & diseases
14278484	FUNCTIONALLY ABNORMAL GLUCOSE-6-PHOSPHATE DEHYDROGENASES.	KIRKMAN HN et al.	1964	Cold Spring Harbor symposia on quantitative biology
19223928	Allelic heterogeneity of G6PD deficiency in West Africa and severe malaria susceptibility.	Clark TG et al.	2009	European journal of human genetics
20459687	Candidate malaria susceptibility/protective SNPs in hospital and population-based studies: the effect of sub-structuring.	Eid NA et al.	2010	Malaria journal
21515823	Genetic predictors for stroke in children with sickle cell anemia.	Flanagan JM et al.	2011	Blood
21867552	Host candidate gene polymorphisms and clearance of drug-resistant Plasmodium falciparum parasites.	Diakite M et al.	2011	Malaria journal
21931645	An exhaustive, non-euclidean, non-parametric data mining tool for unraveling the complexity of biological systems--novel insights into malaria.	Loucoubar C et al.	2011	PloS one
21931771	Path to facilitate the prediction of functional amino acid substitutions in red blood cell disorders--a computational approach.	B R et al.	2011	PloS one
22438807	HMOX1 gene promoter alleles and high HO-1 levels are associated with severe malaria in Gambian children.	Walther M et al.	2012	PLoS pathogens
22957039	Candidate polymorphisms and severe malaria in a Malian population.	Toure O et al.	2012	PloS one
23144702	Candidate human genetic polymorphisms and severe malaria in a Tanzanian population.	Manjurano A et al.	2012	PloS one
23757202	Free the data: one laboratory's approach to knowledge-based genomic variant classification and preparation for EMR integration of genomic data.	Bean LJ et al.	2013	Human mutation
24934404	Association of candidate gene polymorphisms and TGF-beta/IL-10 levels with malaria in three regions of Cameroon: a case-control study.	Apinjoh TO et al.	2014	Malaria journal
24944790	Screening for 392 polymorphisms in 141 pharmacogenes.	Kim JY et al.	2014	Biomedical reports
25741868	Standards and guidelines for the interpretation of sequence variants: a joint consensus recommendation of the American College of Medical Genetics and Genomics and the Association for Molecular Pathology.	Richards S et al.	2015	Genetics in medicine
27413522	Molecular Heterogeneity of Glucose-6-Phosphate Dehydrogenase Deficiency in Burkina Faso: G-6-PD Betica Selma and Santamaria in People with Symptomatic Malaria in Ouagadougou.	Ouattara AK et al.	2016	Mediterranean journal of hematology and infectious diseases
27767381	The effect of SNPs in CYP450 in chloroquine/primaquine Plasmodium vivax malaria treatment.	Sortica VA et al.	2016	Pharmacogenomics
28067620	Characterisation of the opposing effects of G6PD deficiency on cerebral malaria and severe malarial anaemia.	Clarke GM et al.	2017	eLife
30819192	An update on glucose-6-phosphate dehydrogenase deficiency in children from Brazzaville, Republic of Congo.	Gampio Gueye NS et al.	2019	Malaria journal
32936528	Important Pharmacogenetic Information for Drugs Prescribed During the SARS-CoV-2 Infection (COVID-19).	Zubiaur P et al.	2020	Clinical and translational science
33170161	Genetic test for the prescription of diets in support of physical activity.	Naureen Z et al.	2020	Acta bio-medica
33875422	Pharmacogene Sequencing of a Gabonese Population with Severe Plasmodium falciparum Malaria Reveals Multiple Novel Variants with Putative Relevance for Antimalarial Treatment.	Pernaute-Lau L et al.	2021	Antimicrobial agents and chemotherapy
33897764	G6PD Polymorphisms and Hemolysis After Antimalarial Treatment With Low Single-Dose Primaquine: A Pooled Analysis of Six African Clinical Trials.	Sepúlveda N et al.	2021	Frontiers in genetics
34577605	Clinical Application of Pharmacogenetic Markers in the Treatment of Dermatologic Pathologies.	Membrive Jiménez C et al.	2021	Pharmaceuticals (Basel, Switzerland)
35283964	Differences in the genotype frequencies of genes related to blood pressure regulation - a comparative study between South-West Europe and Peri-equatorial Africa.	Aguiar L et al.	2021	African health sciences

The Flanks tab provides retrieving flanking sequences of a SNP on all molecules that have placements.

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Genomic regions, transcripts, and products
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dbSNP Short Genetic Variations

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Reference SNP (rs) Report

rs1050829