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1. ALK F1174S mutation impairs ALK kinase activity in EML4-ALK variant 1 and sensitizes EML4-ALK variant 3 to crizotinib

2. Integrating scRNA and bulk-RNA sequencing develops a cell senescence signature for analyzing tumor heterogeneity in clear cell renal cell carcinoma

3. IGF1R Contributes to Cell Proliferation in ALK-Mutated Neuroblastoma with Preference for Activating the PI3K-AKT Signaling Pathway

4. Extracellular domain shedding of the ALK receptor mediates neuroblastoma cell migration

5. ALK signaling primes the DNA damage response sensitizing ALK-driven neuroblastoma to therapeutic ATR inhibition.

6. Chromosome Imbalances in Neuroblastoma—Recent Molecular Insight into Chromosome 1p-deletion, 2p-gain, and 11q-deletion Identifies New Friends and Foes for the Future

7. Loss of RET Promotes Mesenchymal Identity in Neuroblastoma Cells

8. Sustained Response to Entrectinib in an Infant With a Germline ALKAL2 Variant and Refractory Metastatic Neuroblastoma With Chromosomal 2p Gain and Anaplastic Lymphoma Kinase and Tropomyosin Receptor Kinase Activation

9. Chromosome Imbalances in Neuroblastoma—Recent Molecular Insight into Chromosome 1p-deletion, 2p-gain, and 11q-deletion Identifies New Friends and Foes for the Future

10. Novel Mechanisms of ALK Activation Revealed by Analysis of the Y1278S Neuroblastoma Mutation

11. FAM150A and FAM150B are activating ligands for anaplastic lymphoma kinase

12. BioID-Screening Identifies PEAK1 and SHP2 as Components of the ALK Proximitome in Neuroblastoma Cells

13. Loss of RET promotes mesenchymal identity in neuroblastoma cells

14. ALK ligand ALKAL2 potentiates MYCN‐driven neuroblastoma in the absence of ALK mutation

15. Mapping the Phospho-dependent ALK Interactome to Identify Novel Components in ALK Signaling

16. Extracellular domain shedding of the ALK receptor mediates neuroblastoma cell migration

17. Abstract A36: Targeting anaplastic lymphoma kinase in neuroblastoma

18. Phosphoproteome and gene expression profiling of ALK inhibition in neuroblastoma cell lines reveals conserved oncogenic pathways

19. MEK inhibitor trametinib does not prevent the growth of anaplastic lymphoma kinase (ALK)-addicted neuroblastomas

20. ALKALs are in vivo ligands for ALK family Receptor Tyrosine Kinases in the neural crest and derived cells

21. Novel Mechanisms of ALK Activation Revealed by Analysis of the Y1278S Neuroblastoma Mutation

22. PO-314 ALK inhibitor, ceritinib, abrogates activation of the novel ALK-I1171T mutation in neuroblastoma

24. Abstract B27: Anaplastic lymphoma kinase addicted neuroblastoma cell lines are associated with growth upon treatment with MEK inhibitor trametinib

25. Anaplastic lymphoma kinase L1198F and G1201E mutations identified in anaplastic thyroid cancer patients are not ligand-independent

26. The ALK inhibitor PF-06463922 is effective as a single agent in neuroblastoma driven by expression of ALK and MYCN

27. Abstract 5785: EML4-ALK variant E6a/b;A20 positive NSCLC cell lines are associated with growth upon blocking MEK-ERK pathway

28. Abstract B038: Anaplastic lymphoma kinase addicted neuroblastoma cell lines are associated with growth upon treatment with MEK inhibitor trametinib

29. Abstract B40: A novel activating I1171T ALK mutation in neuroblastoma responds better to ceritinib compare to the first generation inhibitor crizotinib

30. DNAJB13 is a Radial Spoke Protein of Mouse ‘9+2’ Axoneme

31. Cohesin protein SMC1 is a centrosomal protein

33. FAM150A and FAM150B are activating ligands for anaplastic lymphoma kinase

34. Stage-specific and tissue-specific expression characteristics of differentially expressed genes during mouse spermatogenesis

35. Gene Expression Profiles in Different Stages of Mouse Spermatogenic Cells During Spermatogenesis1

36. MEK inhibitor trametinib does not prevent the growth of anaplastic lymphoma kinase (ALK)–addicted neuroblastomas.

37. Abstract B12: The ALK inhibitor PF-06463922 shows significant response as a single agent in ALK/MYCN driven models of neuroblastoma

38. [A simulative biomechanical experiment on different position of none-cement acetabular components influencing the load distribution around acetabulum]

39. A heat-shock protein 40, DNAJB13, is an axoneme-associated component in mouse spermatozoa

40. [A novel orthopaedic biodegradable polymer and its biocompatibility]

41. Stage-specific and tissue-specific expression characteristics of differentially expressed genes during mouse spermatogenesis

42. Gene expression profiles in different stages of mouse spermatogenic cells during spermatogenesis

43. Analysis of gene expression patterns with cDNA microarray during late stage of spermatogenesis in mice

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