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Your search keyword '"Shikha Nayar"' showing total 21 results

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21 results on '"Shikha Nayar"'

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1. Single‐cell transcriptomics reveals conserved cell identities and fibrogenic phenotypes in zebrafish and human liver

2. From single-target to cellular niche targeting in Crohn's disease: intercepting bad communications

3. Glycemic index of wheat and rice are similar when consumed as part of a North Indian mixed meal

4. Zebrafish modeling of intestinal injury, bacterial exposures and medications defines epithelial in vivo responses relevant to human inflammatory bowel disease

5. MPI depletion enhances O-GlcNAcylation of p53 and suppresses the Warburg effect

6. NOX1 is essential for TNFα-induced intestinal epithelial ROS secretion and inhibits M cell signatures

7. Inflamed Ulcerative Colitis Regions Associated With MRGPRX2-Mediated Mast Cell Degranulation and Cell Activation Modules, Defining a New Therapeutic Target

8. A Role for CXCR3 Ligands as Biomarkers of Post-Operative Crohn's Disease Recurrence

9. Single-cell transcriptomic profiling of healthy and fibrotic adult zebrafish liver reveals conserved cell identities and stellate cell activation phenotypes with human liver

10. A myeloid–stromal niche and gp130 rescue in NOD2-driven Crohn’s disease

11. Machine learning identifies novel blood protein predictors of penetrating and stricturing complications in newly diagnosed paediatric Crohn's disease

13. 374 INFLAMED ULCERATIVE COLITIS REGIONS ASSOCIATED TO MRGPRX2-MEDIATED MAST CELL DEGRANULATION AND CELL ACTIVATION MODULES, DEFINING A NEW THERAPEUTIC TARGET

14. trappc11is required for protein glycosylation in zebrafish and humans

15. Single-cell analysis of Crohn’s disease lesions identifies a pathogenic cellular module associated with resistance to anti-TNF therapy

17. Zebrafish modeling of intestinal injury, bacterial exposures and medications defines epithelial

20. MPI depletion enhances O-GlcNAcylation of p53 and suppresses the Warburg effect

21. Single-Cell Analysis of Crohn’s Disease Lesions Identifies a Pathogenic Cellular Module Associated with Resistance to Anti-TNF Therapy

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