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1. Imprinting control regions (ICRs) are marked by mono-allelic bivalent chromatin when transcriptionally inactive

5. Additional file 2: of Placenta-specific epimutation at H19-DMR among common pregnancy complications: its frequency and effect on the expression patterns of H19 and IGF2

6. Additional file 1: of Placenta-specific epimutation at H19-DMR among common pregnancy complications: its frequency and effect on the expression patterns of H19 and IGF2

7. Characterization of parent-of-origin methylation using the Illumina Infinium MethylationEPIC array platform

8. Imprinting control regions (ICRs) are marked by mono-allelic bivalent chromatin when transcriptionally inactive

9. Human Oocyte-Derived Methylation Differences Persist in the Placenta Revealing Widespread Transient Imprinting

10. Human Oocyte-Derived Methylation Differences Persist in the Placenta Revealing Widespread Transient Imprinting

11. Human Oocyte-Derived Methylation Differences Persist in the Placenta Revealing Widespread Transient Imprinting

12. Absence of Maternal Methylation in Biparental Hydatidiform Moles from Women with NLRP7 Maternal-Effect Mutations Reveals Widespread Placenta-Specific Imprinting

13. Imprinting control regions (ICRs) are marked by mono-allelic bivalent chromatin when transcriptionally inactive

14. Integration of transcriptome and methylome analysis of aldosterone-producing adenomas

15. Genomic, Epigenomic, and Transcriptomic Profiling towards Identifying Omics Features and Specific Biomarkers That Distinguish Uterine Leiomyosarcoma and Leiomyoma at Molecular Levels

16. Genome-wide parent-of-origin DNA methylation analysis reveals the intricacies of human imprinting and suggests a germline methylation-independent mechanism of establishment

17. Molecular and Clinical Studies in 138 Japanese Patients with Silver-Russell Syndrome

18. HBx induces hypomethylation of distal intragenic CpG islands required for active expression of developmental regulators.

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