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1. SND1 binds to ERG and promotes tumor growth in genetic mouse models of prostate cancer

2. Genomic attributes of homology-directed DNA repair deficiency in metastatic prostate cancer

6. Aberrant CREB1 activation in prostate cancer disrupts normal prostate luminal cell differentiation

7. Notch3 promotes prostate cancer-induced bone lesion development via MMP-3

8. Selective androgen receptor modulators activate the canonical prostate cancer androgen receptor program and repress cancer growth

9. Human stroma and epithelium co-culture in a microfluidic model of a human prostate gland

10. Supraphysiological androgens suppress prostate cancer growth through androgen receptor–mediated DNA damage

11. Application of a Microfluidic-Based Model of a Human Prostate Gland for Cancer Research

12. Recent advances in prostate cancer research: large-scale genomic analyses reveal novel driver mutations and DNA repair defects

13. Transient Induction of ING4 by Myc Drives Prostate Epithelial Cell Differentiation and Its Disruption Drives Prostate Tumorigenesis

14. A streamlined method for the design and cloning of shRNAs into an optimized Dox-inducible lentiviral vector

15. Abstract B031: CREB1 and ATF1 differentially regulate terminal prostate luminal differentiation by controlling the timing of ING4 expression, while CREB1 prevents ING4 expression upon PTEN loss in prostate cancer

16. Receptor tyrosine kinase Met promotes cell survival via kinase-independent maintenance of integrin α3β1

17. Human prostate luminal cell differentiation requires NOTCH3 induction by p38-MAPK and MYC

18. Disruption of Prostate Epithelial Differentiation Pathways and Prostate Cancer Development

19. Abstract B18: Myc governs a prostate epithelial differentiation program involving chromatin remodeling protein ING4 and Notch3: Disruption of which is necessary for human prostate cancer development

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