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1. Cardiotoxicity of Chemotherapy: A Multi-OMIC Perspective.

2. Recent Advances in Peptide Drug Discovery: Novel Strategies and Targeted Protein Degradation.

3. Multi-Omic Approaches in Cancer-Related Micropeptide Identification.

4. K128 ubiquitination constrains RAS activity by expanding its binding interface with GAP proteins.

5. Relevance of Carcinogen-Induced Preclinical Cancer Models.

6. Spatial Mechano-Signaling Regulation of GTPases through Non-Degradative Ubiquitination.

8. Multi-Omics Integration for the Design of Novel Therapies and the Identification of Novel Biomarkers.

9. Novel Therapeutic Approaches Targeting Post-Translational Modifications in Lung Cancer.

10. Loss-of-Function Mutations in TRAF7 and KLF4 Cooperatively Activate RAS-Like GTPase Signaling and Promote Meningioma Development.

11. Loss of 9p21 Regulatory Hub Promotes Kidney Cancer Progression by Upregulating HOXB13.

12. The Noonan Syndrome Gene Lztr1 Controls Cardiovascular Function by Regulating Vesicular Trafficking.

13. Cracking the Monoubiquitin Code of Genetic Diseases.

14. PDZRN3 destabilizes endothelial cell-cell junctions through a PKCζ-containing polarity complex to increase vascular permeability.

15. Kif26b controls endothelial cell polarity through the Dishevelled/Daam1-dependent planar cell polarity-signaling pathway.

16. The ubiquitin ligase PDZRN3 is required for vascular morphogenesis through Wnt/planar cell polarity signalling.

17. Heterozygous deletion of a 2-Mb region including the dystroglycan gene in a patient with mild myopathy, facial hypotonia, oral-motor dyspraxia and white matter abnormalities.

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