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2. Detecting past and ongoing natural selection among ethnically Tibetan women at high altitude in Nepal.

3. Colonic transcriptional response to 1α,25(OH) 2 vitamin D 3 in African- and European-Americans.

4. Mapping Variation in Cellular and Transcriptional Response to 1,25-Dihydroxyvitamin D3 in Peripheral Blood Mononuclear Cells.

5. Long-term genetic stability and a high-altitude East Asian origin for the peoples of the high valleys of the Himalayan arc.

6. Patterns of Transcriptional Response to 1,25-Dihydroxyvitamin D3 and Bacterial Lipopolysaccharide in Primary Human Monocytes.

7. Admixture facilitates genetic adaptations to high altitude in Tibet.

8. Genetic mapping with multiple levels of phenotypic information reveals determinants of lymphocyte glucocorticoid sensitivity.

9. Genetic, functional and molecular features of glucocorticoid receptor binding.

10. Reconstructing Native American population history.

11. SNP discovery, expression and cis-regulatory variation in the UGT2B genes.

12. The genetic architecture of adaptations to high altitude in Ethiopia.

13. A signature of balancing selection in the region upstream to the human UGT2B4 gene and implications for breast cancer risk.

14. A reduced representation approach to population genetic analyses and applications to human evolution.

15. Interactions between glucocorticoid treatment and cis-regulatory polymorphisms contribute to cellular response phenotypes.

16. Natural selection and functional genetic variation in the p53 pathway.

17. Adaptations to climate-mediated selective pressures in humans.

18. Allele-specific down-regulation of RPTOR expression induced by retinoids contributes to climate adaptations.

19. Adaptations to new environments in humans: the role of subtle allele frequency shifts.

20. Colloquium paper: human adaptations to diet, subsistence, and ecoregion are due to subtle shifts in allele frequency.

21. Allelic imbalance (AI) identifies novel tissue-specific cis-regulatory variation for human UGT2B15.

22. Adaptations to climate in candidate genes for common metabolic disorders.

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