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2. Synthesis, biological evaluation and docking analysis of a new series of methylsulfonyl and sulfamoyl acetamides and ethyl acetates as potent COX-2 inhibitors.

3. 6-Fluorophenylbenzohydrazides inhibit Mycobacterium tuberculosis growth through alteration of tryptophan biosynthesis.

4. Therapeutic potential for coxibs-nitric oxide releasing hybrids in cystic fibrosis.

5. Mycobacterial tryptophan biosynthesis: A promising target for tuberculosis drug development?

6. SAR analysis of new anti-TB drugs currently in pre-clinical and clinical development.

7. In vivo potent BM635 analogue with improved drug-like properties.

8. Enhancing the pharmacodynamic profile of a class of selective COX-2 inhibiting nitric oxide donors.

9. A class of pyrrole derivatives endowed with analgesic/anti-inflammatory activity.

10. Improving the solubility of a new class of antiinflammatory pharmacodynamic hybrids, that release nitric oxide and inhibit cycloxygenase-2 isoenzyme

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