13 research outputs found
The Chinese military system : an organizational study of the Chinese People's Liberation Army
xiv,266p. : ill., maps ; 24cm
Simultaneous homoharringtonine and interferon-α in the treatment of patients with chronic-phase chronic myelogenous leukemia
Activity of camptothecin, harringtonin, cantharidin and curcumae in the human tumor stem cell assay
Assessing factors influencing vegetation coverage calculation with remote sensing imagery
Additional file 1 of The hepato-ovarian axis: genetic evidence for a causal association between non-alcoholic fatty liver disease and polycystic ovary syndrome
Additional file 1: Table S1. Key characteristics of participating studies. Table S2. GWAS significant SNPs used as genetic instruments for fasting insulin and fasting glucose. Table S3. GWAS significant SNPs used as genetic instruments for serum SHBG levels and bioavailable testosterone levels in women. Table S4. Direct causal effects of NAFLD, fasting insulin, fasting glucose, serum SHBG levels, and serum bioavailable testosterone levels on PCOS risk via multivariable MR analysis. Table S5. Direct causal effects of NAFLD, fasting insulin, fasting glucose, and serum SHBG levels on serum bioavailable testosterone levels via multivariable MR analysis. Table S6. Direct causal effects of NAFLD, fasting insulin, and fasting glucose on serum SHBG levels via multivariable MR analysis. Table S7. Obesity-related genome-wide significant genetic variants. Table S8. Directional pleiotropy test using MR-Egger intercepts. Table S9. Horizontal pleiotropy test using MR-PRESSO. Table S10. Linkage disequilibrium score regression results on genetic correlations between NAFLD, fasting insulin, fasting glucose, SHBG, BT, and PCOS. Table S11. Indirect causal effects between NAFLD and PCOS via fasting insulin, serum SHBG levels, and serum bioavailable testosterone levels through step-wise MR analysis