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1. CCL22 mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk

2. Orthogonal Enzyme–Substrate Design Strategy for Discovery of Human Protein Palmitoyltransferase Substrates

6. CLL-156: Novel CCL22 Mutations Drive Chronic Lymphoproliferative Disorder of NK Cells Through Biased GPCR Signaling

7. Poster: CLL-156: Novel CCL22 Mutations Drive Chronic Lymphoproliferative Disorder of NK Cells Through Biased GPCR Signaling

10. Recurrent Mutations of the C-C Motif Chemokine Ligand 22 (CCL22) Define a Distinct Subgroup of Chronic Lymphoproliferative Disorder of NK Cells (CLPD-NK)

11. Bivalent recognition of fatty acyl-CoA by a human integral membrane palmitoyltransferase.

14. CCL22mutations drive natural killer cell lymphoproliferative disease by deregulating microenvironmental crosstalk

17. The molecular mechanism of DHHC protein acyltransferases.

18. In vitro reconstitution of Wnt acylation reveals structural determinants of substrate recognition by the acyltransferase human Porcupine.

19. Hydrogen-Exposed Welded Specimens in Bending and Rotational Bending Fatigue

20. Assessment of Chemical and Physical Characteristics of Bottom, Cyclone, and Baghouse Ashes from the Combustion of Manure

24. Component D of chicken hemoglobin and the hemoglobin of the embryonic Tammar wallaby ( Macropus eugenii) self-associate upon deoxygenation: Effect on oxygen binding.

25. Recurrent Mutations of the C-C Motif Chemokine Ligand 22(CCL22) Define a Distinct Subgroup of Chronic Lymphoproliferative Disorder of NK Cells (CLPD-NK)

26. Deoxygenation-dependent self-association of avian hemoglobins

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