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1. Functional characterisation of cis-regulatory elements governing dynamic Eomes expression in the early mouse embryo

2. Combinatorial Smad2/3 Activities Downstream of Nodal Signaling Maintain Embryonic/Extra-Embryonic Cell Identities during Lineage Priming

3. The transcriptional repressor Blimp1 is expressed in rare luminal progenitors and is essential for mammary gland development

4. BALB/c invariant chain mutant mice display relatively efficient maturation of CD4+ T cells in the periphery and secondary proliferative responses elicited upon peptide challenge

6. Mice lacking Bmp6 function

8. Distinct peptide loading pathways for MHC class II molecules associated with alternative Ii chain isoforms

9. MHC class II expression in double mutant mice lacking invariant chain and DM functions

12. The zinc-finger transcription factor Blimp1/Prdm1 is required for uterine remodelling and repair in the mouse.

13. A degron-based approach to manipulate Eomes functions in the context of the developing mouse embryo.

16. The T-box transcription factor Eomesodermin governs haemogenic competence of yolk sac mesodermal progenitors.

17. The transcriptional repressor Blimp1/PRDM1 regulates the maternal decidual response in mice.

18. Genetic dissection of Nodal and Bmp signalling requirements during primordial germ cell development in mouse.

20. Combinatorial Smad2/3 Activities Downstream of Nodal Signaling Maintain Embryonic/Extra-Embryonic Cell Identities during Lineage Priming.

21. Blimp-1/PRDM1 is a critical regulator of Type III Interferon responses in mammary epithelial cells.

22. Long-lived unipotent Blimp1-positive luminal stem cells drive mammary gland organogenesis throughout adult life.

23. Mapping the chromatin landscape and Blimp1 transcriptional targets that regulate trophoblast differentiation.

24. The transcriptional repressor Blimp1 is expressed in rare luminal progenitors and is essential for mammary gland development.

25. Single-cell RNA-seq reveals cell type-specific transcriptional signatures at the maternal-foetal interface during pregnancy.

26. Lhx1 functions together with Otx2, Foxa2, and Ldb1 to govern anterior mesendoderm, node, and midline development.

27. Blimp1/Prdm1 Functions in Opposition to Irf1 to Maintain Neonatal Tolerance during Postnatal Intestinal Maturation.

28. The PR/SET domain zinc finger protein Prdm4 regulates gene expression in embryonic stem cells but plays a nonessential role in the developing mouse embryo.

29. Technical Advance: Fluorescent reporter reveals insights into eomesodermin biology in cytotoxic lymphocytes.

30. The nonconventional MHC class II molecule DM governs diabetes susceptibility in NOD mice.

31. Progenitor and terminal subsets of CD8+ T cells cooperate to contain chronic viral infection.

32. Blimp1/Prdm1 governs terminal differentiation of endovascular trophoblast giant cells and defines multipotent progenitors in the developing placenta.

33. Alternative splicing regulates Prdm1/Blimp-1 DNA binding activities and corepressor interactions.

34. The T-box transcription factor Eomesodermin acts upstream of Mesp1 to specify cardiac mesoderm during mouse gastrulation.

35. The transcriptional repressor Blimp1/Prdm1 regulates postnatal reprogramming of intestinal enterocytes.

36. Blimp-1/Prdm1 alternative promoter usage during mouse development and plasma cell differentiation.

37. Smad4-dependent pathways control basement membrane deposition and endodermal cell migration at early stages of mouse development.

38. An expanding job description for Blimp-1/PRDM1.

39. The T-box transcription factor Eomes/Tbr2 regulates neurogenesis in the cortical subventricular zone.

41. Ventral closure, headfold fusion and definitive endoderm migration defects in mouse embryos lacking the fibronectin leucine-rich transmembrane protein FLRT3.

42. An MHC class II restriction bias in CD4 T cell responses toward I-A is altered to I-E in DM-deficient mice.

43. Pivotal roles for eomesodermin during axis formation, epithelium-to-mesenchyme transition and endoderm specification in the mouse.

44. Blimp1 regulates development of the posterior forelimb, caudal pharyngeal arches, heart and sensory vibrissae in mice.

45. Mice develop normally in the absence of Smad4 nucleocytoplasmic shuttling.

46. Loss of invariant chain protects nonobese diabetic mice against type 1 diabetes.

47. Dose-dependent Smad1, Smad5 and Smad8 signaling in the early mouse embryo.

48. DM peptide-editing function leads to immunodominance in CD4 T cell responses in vivo.

49. BMP4 substitutes for loss of BMP7 during kidney development.

50. The zinc finger transcriptional repressor Blimp1/Prdm1 is dispensable for early axis formation but is required for specification of primordial germ cells in the mouse.

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