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1. Opportunities and challenges of low-dose radiation to enable immunotherapy efficacy

3. The Impact of Neutrophil Recruitment to the Skin on the Pathology Induced by Leishmania Infection

4. Survival Mechanisms Used by Some Leishmania Species to Escape Neutrophil Killing

6. NLRP1-dependent activation of Gasdermin D in neutrophils controls cutaneous leishmaniasis.

7. Strategies for overcoming tumour resistance to immunotherapy: harnessing the power of radiation therapy.

8. Opportunities and challenges of low-dose radiation to enable immunotherapy efficacy.

9. The C5a-C5aR1 complement axis is essential for neutrophil recruitment to draining lymph nodes via high endothelial venules in cutaneous leishmaniasis.

10. The c-MET receptor tyrosine kinase contributes to neutrophil-driven pathology in cutaneous leishmaniasis.

11. The Impact of Neutrophil Recruitment to the Skin on the Pathology Induced by Leishmania Infection.

12. TLR7 Sensing by Neutrophils Is Critical for the Control of Cutaneous Leishmaniasis.

13. M2-like, dermal macrophages are maintained via IL-4/CCL24-mediated cooperative interaction with eosinophils in cutaneous leishmaniasis.

14. TLR2 Signaling in Skin Nonhematopoietic Cells Induces Early Neutrophil Recruitment in Response to Leishmania major Infection.

15. Deletion of Interleukin-4 Receptor Alpha-Responsive Keratinocytes in BALB/c Mice Does Not Alter Susceptibility to Cutaneous Leishmaniasis.

16. Survival Mechanisms Used by Some Leishmania Species to Escape Neutrophil Killing.

17. IL-4Rα Signaling in Keratinocytes and Early IL-4 Production Are Dispensable for Generating a Curative T Helper 1 Response in Leishmania major -Infected C57BL/6 Mice.

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