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1. Additional file 19 of Enhancer promoter interactome and Mendelian randomization identify network of druggable vascular genes in coronary artery disease

4. Considerations and consequences of allowing DNA sequence data as types of fungal taxa

5. Considerations and consequences of allowing DNA sequence data as types of fungal taxa

8. Integrative genomic analyses identify candidate causal genes for calcific aortic valve stenosis involving tissue-specific regulation.

9. Enhancer promoter interactome and Mendelian randomization identify network of druggable vascular genes in coronary artery disease.

10. Genome-wide chromatin contacts of super-enhancer-associated lncRNA identify LINC01013 as a regulator of fibrosis in the aortic valve.

11. System Genetics Including Causal Inference Identify Immune Targets for Coronary Artery Disease and the Lifespan.

12. Enhancer-associated aortic valve stenosis risk locus 1p21.2 alters NFATC2 binding site and promotes fibrogenesis.

13. Single-cell expression and Mendelian randomization analyses identify blood genes associated with lifespan and chronic diseases.

14. Enhancer-mediated enrichment of interacting JMJD3-DDX21 to ENPP2 locus prevents R-loop formation and promotes transcription.

15. DNA methylation of a PLPP3 MIR transposon-based enhancer promotes an osteogenic programme in calcific aortic valve disease.

16. Considerations and consequences of allowing DNA sequence data as types of fungal taxa.

17. OxLDL-derived lysophosphatidic acid promotes the progression of aortic valve stenosis through a LPAR1-RhoA-NF-κB pathway.

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