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1. Structure of the M. tuberculosis DnaK−GrpE complex reveals how key DnaK roles are controlled

2. The Rip1 intramembrane protease contributes to iron and zinc homeostasis in Mycobacterium tuberculosis

3. Distinctive roles of translesion polymerases DinB1 and DnaE2 in diversification of the mycobacterial genome through substitution and frameshift mutagenesis

4. Diisonitrile Lipopeptides Mediate Resistance to Copper Starvation in Pathogenic Mycobacteria

5. Gastrointestinal microbiota composition predicts peripheral inflammatory state during treatment of human tuberculosis

7. Rifamycin congeners kanglemycins are active against rifampicin-resistant bacteria via a distinct mechanism

8. Antibiotic treatment for Tuberculosis induces a profound dysbiosis of the microbiome that persists long after therapy is completed

9. Longitudinal profiling reveals a persistent intestinal dysbiosis triggered by conventional anti-tuberculosis therapy

10. Two Accessory Proteins Govern MmpL3 Mycolic Acid Transport in Mycobacteria

11. The Microbiome and Tuberculosis: Early Evidence for Cross Talk

12. Genome-wide mapping of the distribution of CarD, RNAP σA, and RNAP β on the Mycobacterium smegmatis chromosome using chromatin immunoprecipitation sequencing

14. Single-Cell Transcriptional Profiling Reveals Signatures of Helper, Effector, and Regulatory MAIT Cells during Homeostasis and Activation

15. Roles for mycobacterial DinB2 in frameshift and substitution mutagenesis

17. Data from BCG-Induced Tumor Immunity Requires Tumor-Intrinsic CIITA Independent of MHC-II

22. Data from The Canonical Wnt Pathway Drives Macropinocytosis in Cancer

23. Combined supplementary figures from The Canonical Wnt Pathway Drives Macropinocytosis in Cancer

24. Supplementary Data from Oncogenic Activation of Pak1-Dependent Pathway of Macropinocytosis Determines BCG Entry into Bladder Cancer Cells

25. Supplementary Methods, Figures 1 - 6 from Oncogenic Activation of Pak1-Dependent Pathway of Macropinocytosis Determines BCG Entry into Bladder Cancer Cells

26. Division of labor between SOS and PafBC in mycobacterial DNA repair and mutagenesis

28. The C-terminal acid phosphatase module of the RNase HI enzyme RnhC controls rifampicin sensitivity and light-dependent colony pigmentation ofMycobacterium smegmatis

29. A multilayered repair system protects the mycobacterial chromosome from endogenous and antibiotic-induced oxidative damage

30. Determinants of COVID-19 disease severity in patients with cancer

31. BCG-Induced Tumor Immunity Requires Tumor-Intrinsic CIITA Independent of MHC-II

33. TOX is a critical regulator of tumour-specific T cell differentiation

34. Division of Labor between SOS and PafBC in mycobacterial DNA Repair and Mutagenesis

36. The DnaK Chaperone System Buffers the Fitness Cost of Antibiotic Resistance Mutations in Mycobacteria

37. Gastrointestinal microbiota composition predicts peripheral inflammatory state during treatment of human tuberculosis

38. Efficient 5-OP-RU-Induced Enrichment of Mucosa-Associated Invariant T Cells in the Murine Lung Does Not Enhance Control of Aerosol Mycobacterium tuberculosis Infection

39. H. Mucosal-Associated Invariant and Vγ9Vδ2 T Cells

40. Integrated sensing of host stresses by inhibition of a cytoplasmic two-component system controls

41. Inherited PD-1 deficiency underlies tuberculosis and autoimmunity in a child

42. Single cell transcriptional profiling reveals helper, effector, and regulatory MAIT cell populations enriched during homeostasis and activation

43. Efficient 5-OP-RU-induced enrichment of Mucosal-associated invariant T cells in the murine lung does not enhance control of aerosol Mycobacterium tuberculosis infection

44. Intestinal microbiome composition influences the peripheral inflammatory state during treatment of human tuberculosis

45. Bacterial immunotherapy for cancer induces CD4-dependent tumor-specific immunity through tumor-intrinsic interferon-γ signaling

46. Structural basis for aggregate dissolution and refolding by the Mycobacterium tuberculosis ClpB-DnaK bi-chaperone system

47. The Canonical Wnt Pathway Drives Macropinocytosis in Cancer

48. Defining innate immune training potential as a predictor of Bacillus Calmette-Guérin immunotherapy response in nonmuscle-invasive bladder cancer

49. Peripheral inflammatory response in human tuberculosis treatment is predicted by a combination of pathogen sterilization and microbiome dysbiosis

50. Mycobacterium tuberculosis protease MarP activates a peptidoglycan hydrolase during acid stress

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