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1. Selection of Explants and Optimization of Culture Conditions for Tissue Culture of Pholidota chinensis Lindl.

3. Integrated transcriptomic and metabolomic analysis reveals the metabolic programming of GM-CSF- and M-CSF- differentiated mouse macrophages

4. Targeted therapeutics and novel signaling pathways in non-alcohol-associated fatty liver/steatohepatitis (NAFL/NASH)

5. Bioactive compound C498-0670 alleviates LPS-induced sepsis via JAK/STAT and NFκB signaling pathways

6. Identifying gene variants underlying the pathogenesis of diabetic retinopathy based on integrated genomic and transcriptomic analysis of clinical extreme phenotypes

7. The Culture Dish Surface Influences the Phenotype and Dissociation Strategy in Distinct Mouse Macrophage Populations

8. Association Between Metabolic Syndrome and Risk of Renal Cell Cancer: A Meta-Analysis

9. Inhibition of Histone H3 Lysine-27 Demethylase Activity Relieves Rheumatoid Arthritis Symptoms via Repression of IL6 Transcription in Macrophages

10. Unfolded Protein Response Differentially Regulates TLR4-Induced Cytokine Expression in Distinct Macrophage Populations

11. A novel synthetic analog of 5, 8-disubstituted quinazolines blocks mitosis and induces apoptosis of tumor cells by inhibiting microtubule polymerization.

14. Effects of Residual Composition and Distribution on the Structural Characteristics of the Protein

15. Integrated transcriptomic and metabolomic analysis reveals the metabolic programming of GMCSF- and M-CSF- differentiated mouse macrophages.

16. Small-Molecule Inhibitors Targeting the Canonical WNT Signaling Pathway for the Treatment of Cancer

17. Transmissible ER stress between macrophages and tumor cells configures tumor microenvironment

18. Type I interferon signaling facilitates resolution of acute liver injury by priming macrophage polarization

19. Short-term exposure to air pollution and occurrence of emergency stroke in Chongqing, China

20. Inhibition of Histone H3 Lysine-27 Demethylase Activity Relieves Rheumatoid Arthritis Symptoms

21. The phagocytic receptors of β-glucan

23. C644-0303, a small-molecule inhibitor of the Wnt/β-catenin pathway, suppresses colorectal cancer growth

24. Discovery and evaluation of Atopaxar hydrobromide, a novel JAK1 and JAK2 inhibitor, selectively induces apoptosis of cancer cells with constitutively activated STAT3

25. Morphological control of inverted MgO-SiO2 composite catalysts for efficient conversion of ethanol to 1,3-butadiene

26. E2F is required for STAT3-mediated upregulation of cyclin B1 and Cdc2 expressions and contributes to G2–M phase transition

27. Scaffold compound L971 exhibits anti-inflammatory activities through inhibition of JAK/STAT and NFκB signalling pathways

28. A virus-induced conformational switch of STAT1-STAT2 dimers boosts antiviral defenses

29. Synthesis of Biotinylated 2-methoxystypandrone and Identification of JAK2 and IKK as its Targets

30. Support effect of Ag/ZnO catalysts for partial oxidation of methanol

31. Cucurbitacin I inhibits STAT3, but enhances STAT1 signaling in human cancer cells in vitro through disrupting actin filaments

32. Boosting CO2 methanation activity on Ru/TiO2 catalysts by exposing (001) facets of anatase TiO2

33. A β-1,3/1,6-glucan from Durvillaea Antarctica inhibits tumor progression in vivo as an immune stimulator

34. Zelnorm, an agonist of 5-Hydroxytryptamine 4-receptor, acts as a potential antitumor drug by targeting JAK/STAT3 signaling

35. Concomitant inhibition of receptor tyrosine kinases and downstream AKT synergistically inhibited growth of KRAS/BRAF mutant colorectal cancer cells

36. The influence of zinc loadings on the selectivity control of bio-ethanol transformation over MgO-SiO2 catalysts

37. Axl inhibitor R428 induces apoptosis of cancer cells by blocking lysosomal acidification and recycling independent of Axl inhibition

38. Scaffold compound L971 exhibits anti-inflammatory activities through inhibition of JAK/STAT and NFκB signalling pathways.

39. Virtual Screening Guided Design, Synthesis and Bioactivity Study of Benzisoselenazolones (BISAs) on Inhibition of c-Met and Its Downstream Signalling Pathways

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