Dataset
All samples in this dataset are included in the "DIAMANTE (European) T2D GWAS" dataset.
Dataset phenotypes
Phase 1 analysis:
- type 2 diabetes
- type 2 diabetes adjusted for BMI
- fasting glucose
- fasting glucose adjusted for BMI
- fasting insulin
- fasting insulin adjusted for BMI
Phase 2 analysis:
- diastolic blood pressure
- urinary creatinine
- LDL cholesterol
- HDL cholesterol
- BMI
- systolic blood pressure
Dataset subjects
| Cases | Controls | Cohort | Ancestry |
|---|---|---|---|
| 884 | 797 | Finland-United States Investigation of NIDDM Genetics Study (FUSION) | European |
Project
The FUSION (Finland-United States Investigation of NIDDM Genetics) Study seeks to to map and identify genetic variants that predispose to type 2 diabetes mellitus (T2D) or are responsible for variability in diabetes-related quantitative traits.
Acknowledgments
This study was funded by NIH grants R01-DK062370 and R01-DK072193; intramural project number 1Z01-HG000024; and FNIH grant BOEH15AMP2.
Experiment summary
The FUSION (Finland–United States Investigation of Non–Insulin-Dependent Diabetes Mellitus Genetics) study is a long-term effort to identify genetic variants affecting risk of type 2 diabetes (T2D) or impacting T2D-related quantitative traits. This case-control study initially involved linkage analysis of affected-sibling-pair families based on over 5,000 individuals living in Finland; additional T2D cases and controls were subsequently included.
Individual-level genotype data from 4,233 unique samples, generated on four different arrays, was received by the Analysis Team at the Accelerating Medicines Partnership Data Coordinating Center (AMP-DCC) and subjected to quality control. Since the samples analyzed with the CIDR exome chip consisted of related pairs, they were removed from further analysis. Association analysis was then performed for the three remaining arrays: the Broad exome chip (resulting dataset termed "FUSION exome chip analysis" in the T2DKP); the HumanHap300 chip (resulting dataset termed "FUSION GWAS" in the T2DKP); and the Metabochip (resulting dataset termed "FUSION Metabochip" in the T2DKP).
Data were analyzed by the Analysis Team at the Accelerating Medicines Partnership Data Coordinating Center (AMP-DCC), Broad Institute, using Loamstream software and the AMP-DCC Data Analysis Pipeline. Results are summarized below; see the Quality Control and Analysis Reports (links below) for full details.
Overview of analysis and results
No T2D associations reached genome-wide significance in either the BMI-unadjusted or BMI-adjusted models. In both models, one of the top 20 associations had been identified previously.
No fasting glucose or fasting insulin associations reached genome-wide significance in either the BMI-unadjusted or BMI-adjusted models, and none of the top 20 associations for either phenotype or model had been identified previously.
No associations with diastolic blood pressure, systolic blood pressure, urinary creatinine, or BMI reached genome-wide significance, and none of the top 20 associations had been identified previously.
No LDL cholesterol associations reached genome-wide significance; one association among the top 20 had been identified previously.
One HDL cholesterol association reached genome-wide significance: rs3764261 in the region of the CETP gene, with a p-value of 2.16 × 10−11. This association and one other among the top 20 had been identified previously.
Detailed reports
Genotype Data Quality Control Report (download PDF)
AMP-DCC Phase 1 Data Analysis Report (download PDF)
AMP-DCC Phase 2 Data Analysis Report (download PDF)