SAGE cohort

Aliases: SAGE, SAGE GWAS, SAGE data, SAGE dataset, SAGE population, SAGE sample, SAGE: phs000092.v1.p1, Serial Analysis of Gene Expression, Study of Addiction: Genetics and Environment, phs000092.v1.p1

Evidence from: primary | all sources

Related entities (61)

Subject	Relation	Object	p-value	Evidence
1000 Genomes Project	interacts_with	SAGE	—	1
AA	associated_with	SAGE	—	1
AA population	associated_with	SAGE	—	1
ADH1B	associated_with	SAGE	—	1
African American	associated_with	SAGE	—	2
alcohol dependence	associated_with	SAGE	—	2
associated SNPs	associated_with	SAGE	—	1
C15orf53	associated_with	SAGE	—	1
cocaine	associated_with	SAGE	—	1
COGEND	associated_with	SAGE	—	1
cognitive ability	associated_with	SAGE	—	1
Collaborative Study on the Genetics of Alcoholism (COGA)	interacts_with	SAGE	—	2
Collaborative Study on the Genetics of Alcoholism (COGA)	associated_with	SAGE	—	3
EA	associated_with	SAGE	—	1
EA population	associated_with	SAGE	—	1
European ancestry	associated_with	SAGE	—	1
FSCD	associated_with	SAGE	—	1
FTND score	associated_with	SAGE	—	1
GCTA	interacts_with	SAGE	—	1
Illumina Human1M array	associated_with	SAGE	—	1
Impute2	associated_with	SAGE	—	1
maxdrinks	associated_with	SAGE	4.3e-08	2
metal	interacts_with	SAGE	—	2
microarray	associated_with	SAGE	—	1
nicotine	associated_with	SAGE	—	1
PLCL1	associated_with	SAGE	—	1
RNA-seq	associated_with	SAGE	—	1
SAGE	associated_with	1000 Genomes Project	—	1
SAGE	associated_with	AA	—	2
SAGE	associated_with	AD diagnosis	—	1
SAGE	associated_with	addiction phenotypes	—	1
SAGE	associated_with	alcohol	—	2
SAGE	associated_with	alcohol dependence	—	5
SAGE	associated_with	Alzheimer's disease	0.00011	3
SAGE	associated_with	associated SNPs	—	1
SAGE	associated_with	cannabis use	—	1
SAGE	associated_with	case-control phenotypes	—	1
SAGE	associated_with	cases	—	1
SAGE	associated_with	cDNA	—	1
SAGE	associated_with	cocaine	—	1
SAGE	associated_with	COGEND	—	3
SAGE	associated_with	Collaborative Study on the Genetics of Alcoholism (COGA)	—	3
SAGE	associated_with	controls	—	1
SAGE	associated_with	DNA	—	1
SAGE	associated_with	DSM-IV alcohol dependence	—	1
SAGE	associated_with	EA	—	2
SAGE	associated_with	FSCD	—	3
SAGE	associated_with	FTND	—	1
SAGE	associated_with	Geneva	—	1
SAGE	associated_with	human genome	—	1
SAGE	associated_with	Illumina Human1M array	—	1
SAGE	associated_with	marijuana use disorder	—	1
SAGE	associated_with	maxdrinks	—	2
SAGE	associated_with	nicotine	—	2
SAGE	associated_with	physical trauma	—	1
SAGE	associated_with	polysubstance dependence	—	1
SAGE	associated_with	principal components	—	1
SAGE	associated_with	RNA	—	1
SAGE	associated_with	sexual trauma	—	1
SAGE	associated_with	trait	—	1
structural connectivity	associated_with	SAGE	—	1

Mentioned in (32)

Papers in which this entity is mentioned.

Alcohol Use Disorder Polygenic Score Compared With Family History and ADH1B. (2024)
Multi-trait genome-wide association study of opioid addiction: OPRM1 and beyond. (2022)
Gene-based polygenic risk scores analysis of alcohol use disorder in African Americans. (2022)
Genome-wide admixture mapping of DSM-IV alcohol dependence, criterion count, and the self-rating of the effects of ethanol in African American populations. (2021)
CYP2A6 is associated with obesity: studies in human samples and a high fat diet mouse model. (2019)
Genome-wide association studies of alcohol dependence, DSM-IV criterion count and individual criteria. (2019)
Genome-wide association study identifies a novel locus for cannabis dependence. (2018)
Genetic studies of alcohol dependence in the context of the addiction cycle. (2017)
Genome-wide Association Study of Cannabis Dependence Severity, Novel Risk Variants, and Shared Genetic Risks. (2016)
KAT2B polymorphism identified for drug abuse in African Americans with regulatory links to drug abuse pathways in human prefrontal cortex. (2016)
Polygenic risk for alcohol dependence associates with alcohol consumption, cognitive function and social deprivation in a population-based cohort. (2016)
Alcohol Dependence Genetics: Lessons Learned From Genome-Wide Association Studies (GWAS) and Post-GWAS Analyses. (2015)
Dissecting ancestry genomic background in substance dependence genome-wide association studies. (2015)
Genomewide Association Study for Maximum Number of Alcoholic Drinks in European Americans and African Americans. (2015)
Clinically relevant genetic biomarkers from the brain in alcoholism with representation on high resolution chromosome ideograms. (2015)
Genome-wide association study of nicotine dependence in American populations: identification of novel risk loci in both African-Americans and European-Americans. (2015)
Genome-wide association study of cocaine dependence and related traits: FAM53B identified as a risk gene. (2014)
Using genetic information from candidate gene and genome-wide association studies in risk prediction for alcohol dependence. (2014)
Common biological networks underlie genetic risk for alcoholism in African- and European-American populations. (2013)
A genome-wide association study of alcohol-dependence symptom counts in extended pedigrees identifies C15orf53. (2013)
The CRHR1 gene, trauma exposure, and alcoholism risk: a test of G × E effects. (2013)
A meta-analysis of two genome-wide association studies to identify novel loci for maximum number of alcoholic drinks. (2013)
Gene expression in the human brain: the current state of the study of specificity and spatiotemporal dynamics. (2013)
The aggregate effect of dopamine genes on dependence symptoms among cocaine users: cross-validation of a candidate system scoring approach. (2012)
Copy number variations in 6q14.1 and 5q13.2 are associated with alcohol dependence. (2012)
Longevity candidate genes and their association with personality traits in the elderly. (2012)
The genetic basis of alcoholism: multiple phenotypes, many genes, complex networks. (2012)
Genome-wide search for replicable risk gene regions in alcohol and nicotine co-dependence. (2012)
Memory for the order of events in specific sequences: contributions of the hippocampus and medial prefrontal cortex. (2011)
Genetics of psychiatric disorders methods: molecular approaches. (2010)
A new statistic to evaluate imputation reliability. (2010)
Neurotoxic hippocampal lesions have no effect on odor span and little effect on odor recognition memory but produce significant impairments on spatial span, recognition, and alternation. (2000)

Merged raw entities (7)

All extracted name/type variants the normalize job merged into this entity. Use this to spot wrong merges, or aliases that should be split off.

Raw name	Type	Papers	Mentions
sage	cohort	28	118
sage	drug	4	5
phs000092.v1.p1	cohort	—	—
sage data	cohort	—	—
sage: phs000092.v1.p1	cohort	—	—
sage population	cohort	—	—
serial analysis of gene expression	cohort	—	—