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1. The Homeobox Transcription Factor NKX3.1 Displays an Oncogenic Role in Castration-Resistant Prostate Cancer Cells.

2. Targeting unique ligand binding domain structural features downregulates DKK1 in Y537S ESR1 mutant breast cancer cells.

3. Androgen receptor monomers and dimers regulate opposing biological processes in prostate cancer cells.

4. NR0B2 re-educates myeloid immune cells to reduce regulatory T cell expansion and progression of breast and other solid tumors.

5. Development of NR0B2 as a therapeutic target for the re-education of tumor associated myeloid cells.

6. Targeting Unique Ligand Binding Domain Structural Features Downregulates DKK1 in Y537S ESR1 Mutant Breast Cancer Cells.

7. Targeting Unique Ligand Binding Domain Structural Features Downregulates DKK1 in Y537S ESR1 Mutant Breast Cancer Cells.

8. Estrogen Receptor Alpha Mutations, Truncations, Heterodimers, and Therapies.

9. Editorial: Hormone resistance in cancer.

10. Re-education of myeloid immune cells to reduce regulatory T cell expansion and impede breast cancer progression.

11. Targeting MYC with modular synthetic transcriptional repressors derived from bHLH DNA-binding domains.

12. ESR1 activating mutations: From structure to clinical application.

13. Unconventional isoquinoline-based SERMs elicit fulvestrant-like transcriptional programs in ER+ breast cancer cells.

14. Labeling of a mutant estrogen receptor with an Affimer in a breast cancer cell line.

15. A New Chemotype of Chemically Tractable Nonsteroidal Estrogens Based on a Thieno[2,3- d ]pyrimidine Core.

16. Stereospecific lasofoxifene derivatives reveal the interplay between estrogen receptor alpha stability and antagonistic activity in ESR1 mutant breast cancer cells.

17. Defining the Energetic Basis for a Conformational Switch Mediating Ligand-Independent Activation of Mutant Estrogen Receptors in Breast Cancer.

18. A small-molecule activator of the unfolded protein response eradicates human breast tumors in mice.

19. Lasofoxifene as a potential treatment for therapy-resistant ER-positive metastatic breast cancer.

20. Rapid Induction of the Unfolded Protein Response and Apoptosis by Estrogen Mimic TTC-352 for the Treatment of Endocrine-Resistant Breast Cancer.

21. The Structure-Function Relationship of Angular Estrogens and Estrogen Receptor Alpha to Initiate Estrogen-Induced Apoptosis in Breast Cancer Cells.

22. Versatile Peptide Macrocyclization with Diels-Alder Cycloadditions.

23. Next-Generation ERα Inhibitors for Endocrine-Resistant ER+ Breast Cancer.

24. The SERM/SERD bazedoxifene disrupts ESR1 helix 12 to overcome acquired hormone resistance in breast cancer cells.

25. Endoxifen, 4-Hydroxytamoxifen and an Estrogenic Derivative Modulate Estrogen Receptor Complex Mediated Apoptosis in Breast Cancer.

26. Specific stereochemistry of OP-1074 disrupts estrogen receptor alpha helix 12 and confers pure antiestrogenic activity.

27. A "cross-stitched" peptide with improved helicity and proteolytic stability.

28. Stapled Peptides with γ-Methylated Hydrocarbon Chains for the Estrogen Receptor/Coactivator Interaction.

29. Estrogen receptor alpha somatic mutations Y537S and D538G confer breast cancer endocrine resistance by stabilizing the activating function-2 binding conformation.

30. Structural basis of an engineered dual-specific antibody: conformational diversity leads to a hypervariable loop metal-binding site.

31. Mutations in the coat protein-binding cis-acting RNA motifs debilitate RNA recombination of Brome mosaic virus.

32. A combinatorial histidine scanning library approach to engineer highly pH-dependent protein switches.

33. An anti-hapten camelid antibody reveals a cryptic binding site with significant energetic contributions from a nonhypervariable loop.

34. A combinatorial approach to engineering a dual-specific metal switch antibody.

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