{{Rsnum
|rsid=12608932
|Gene=UNC13A
|Chromosome=19
|position=17641880
|Orientation=plus
|GMAF=0.4325
|Assembly=GRCh38
|GenomeBuild=38.1
|dbSNPBuild=141
|geno1=(A;A)
|geno2=(A;C)
|geno3=(C;C)
|Gene_s=UNC13A
}}{{ population diversity
| geno1=(A;A)
| geno2=(A;C)
| geno3=(C;C)
| CEU | 43.4 | 44.2 | 12.4
| HCB | 7.4 | 38.2 | 54.4
| JPT | 5.3 | 34.5 | 60.2
| YRI | 40.8 | 43.5 | 15.6
| ASW | 42.1 | 45.6 | 12.3
| CHB | 7.4 | 38.2 | 54.4
| CHD | 9.2 | 41.3 | 49.5
| GIH | 27.7 | 47.5 | 24.8
| LWK | 56.9 | 37.6 | 5.5
| MEX | 48.3 | 39.7 | 12.1
| MKK | 54.5 | 38.5 | 7.1
| TSI | 46.1 | 44.1 | 9.8
| HapMapRevision=28
}}{{PMID Auto GWAS
|PMID=19734901
|Trait=Amyotrophic lateral sclerosis
|Title=Genome-wide association study identifies 19p13.3 (UNC13A) and 9p21.2 as susceptibility loci for sporadic amyotrophic lateral sclerosis
|RiskAllele=
|Pval=3E-14
|OR=1.25
|ORtxt=[NR]
}}

{{omim
|id=105400
|rsnum=12608932
}}

rs12608932 is a SNP located in an intron of the UNC13A gene which encodes UNC13A, a protein involved with regulation of neurotransmitters like glutamate at central and neuromuscular synpases.  

rs12608932(C, reference allele: A) was identified as a risk allele associated with sporadic amyotrophic lateral sclerosis (sALS) or Lou Gehrig’s disease in a two-stage association study with individuals of European ancestry. An initial genome-wide study (2,323 case and 9,013 control subjects) identified SNPs that exhibited P-values less than 1.0x10-4, including rs12608932 (P =1.30x10-9, OR=1.25).  These SNPs were further evaluated in a second, independent cohort of individuals (2,532 affected individuals and 5,940 controls). This SNP exhibited significant association in the replication round (P=1.86x10-6, OR=1.20 replication round) with an overall combined P=2.50x10-14. {{PMID|19734901}}
	
Two replication studies examining the association of including rs12608932 did not identify any significant association with sALS. The first of these studies was performed with patients from France (285 cases and 285 controls) were genotyped for rs12608932 exhibited P=0.85. {{PMID|20385924}} The second examined two separate populations of Japanese (1179 cases/1645 controls) and Chinese (684 cases/830 controls) ancestry and found no significant association of rs12608932 with sALS (P=0.67 OR=1.02 for Japanese and P=0.73 OR=1.02 for Chinese). {{PMID|21295378}} Additionally, the allele frequencies differ between the Eastern Asian population (MAF in Japanese controls: 0.741, cases: 0.746; in Chinese controls: 0.675, cases: 0.681) and the European ancestry population in the initial GWA study that identified rs12608932 as associated with sALS. The minor allele frequency in this study was 0.395 in patients and 0.342 in controls in the first GWAS stage and 0.369 in patients and 0.337 in controls in the second-stage of the study.  {{PMID|19734901}}  In both the French and East Asian replication studies, the sample sizes may have been too small to exclude rs12608932(C) as a risk allele for sALS. For example, the power of the Chinese population study was only 63%.  

A more recent smaller-scale replication study did identify an association of rs12608932 with sALS in patients of Dutch ancestry (P=0.001). Additionally, the authors collected data on the survivability of patients with sALS and control individuals (of Dutch, Swedish, and Belgian descent) from the previous GWAS which initially associated rs12608932 with ALS {{PMID|19734901}}. This study showed a weak association with survivability and rs12608932 (P<0.001) when fit to a recessive model. Patients homozygous for the minor allele of rs12608932 (CC) exhibited shorter survival after ALS onset than patients AC or AA by 5 and 10 months in the Dutch population and GWAS cohort, respectively.  {{PMID|22118904}}

{{PMID Auto
|PMID=22118904
|Title=UNC13A is a modifier of survival in amyotrophic lateral sclerosis
}}

{{PMID Auto
|PMID=22509407
|Title=Mapping of Gene Expression Reveals CYP27A1 as a Susceptibility Gene for Sporadic ALS
|OA=1
}}

{{GET Evidence
|impact=pathogenic
|qualified_impact=Insufficiently evaluated pathogenic
|inheritance=unknown
|quality_scores=Array
|dbsnp_id=rs12608932
|overall_frequency_n=44
|overall_frequency_d=128
|overall_frequency=0.34375
|n_genomes=28
|n_genomes_annotated=0
|n_haplomes=40
|n_articles=0
|n_articles_annotated=0
|in_gwas=Y
|autoscore=1
|webscore=N
}}

{{PMID Auto GWAS
  |PMID=22959728
  |Trait=Amyotrophic lateral sclerosis
  |Title=Age of onset of amyotrophic lateral sclerosis is modulated by a locus on 1p34.1.
  |RiskAllele=C
  |Pval=5E-8
  |OR=1.37
  |ORtxt=[1.21-1.56]
  |OA=1
}}

{{PMID Auto
|PMID=22921269
|Title=UNC13A influences survival in Italian amyotrophic lateral sclerosis patients: a population-based study.
|OA=1
}}

{{PMID Auto GWAS
  |PMID=24256812
  |Trait=Amyotrophic lateral sclerosis (sporadic)
  |Title=A genome-wide association meta-analysis identifies a novel locus at 17q11.2 associated with sporadic amyotrophic lateral sclerosis.
  |RiskAllele=
  |Pval=6E-6
  |OR=NR
  |ORtxt=NR
  }}
{{on chip | 23andMe v1}}
{{on chip | 23andMe v2}}
{{on chip | 23andMe v3}}
{{on chip | 23andMe v4}}
{{on chip | HumanOmni1Quad}}
{{on chip | Illumina Human 1M}}