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1. CD2 expressing innate lymphoid and T cells are critical effectors of immunopathogenesis in hidradenitis suppurativa.

2. Heavy Metal Exposure-Mediated Dysregulation of Sphingolipid Metabolism.

3. Small Extracellular Vesicle Signaling and Mitochondrial Transfer Reprograms T Helper Cell Function in Human Asthma.

4. NK and NKT cells in the pathogenesis of Hidradenitis suppurativa: Novel therapeutic strategy through targeting of CD2.

5. Altered sphingolipid pathway in SARS-CoV-2 infected human lung tissue.

6. Mitochondrial transfer from cancer-associated fibroblasts increases migration in aggressive breast cancer.

7. Ex Vivo Culture Models of Hidradenitis Suppurativa for Defining Molecular Pathogenesis and Treatment Efficacy of Novel Drugs.

8. Local SARS-CoV-2 Peptide-Specific Immune Responses in Lungs of Convalescent and Uninfected Human Subjects.

9. Sphingolipids in Lung Pathology in the Coronavirus Disease Era: A Review of Sphingolipid Involvement in the Pathogenesis of Lung Damage.

10. Extracellular Vesicle Mediated Tumor-Stromal Crosstalk Within an Engineered Lung Cancer Model.

11. Moving Immune Therapy Forward Targeting TME.

12. Mechanical strain induces phenotypic changes in breast cancer cells and promotes immunosuppression in the tumor microenvironment.

14. Energetic regulation of coordinated leader-follower dynamics during collective invasion of breast cancer cells.

15. Methods to Evaluate Cell Growth, Viability, and Response to Treatment in a Tissue Engineered Breast Cancer Model.

16. Flow-perfusion bioreactor system for engineered breast cancer surrogates to be used in preclinical testing.

17. A recapitulative three-dimensional model of breast carcinoma requires perfusion for multi-week growth.

18. Preparation and Analysis of In Vitro Three Dimensional Breast Carcinoma Surrogates.

19. The presence of primary cilia in cancer cells does not predict responsiveness to modulation of smoothened activity.

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