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1. Potent cyclic antagonists of the complement C5a receptor on human polymorphonuclear leukocytes. Relationships between structures and activity.

2. Synthesis and activity of analogues of the isoleucyl tRNA synthetase inhibitor SB-203207.

4. Multi-component assembly of the bicyclic core associated with the tRNA synthetase inhibitors SB-203207 and SB-203208. Application to the synthesis of biologically active analogues.

5. Analogues of SB-203207 as inhibitors of tRNA synthetases.

6. Synthesis, stability, antiviral activity, and protease-bound structures of substrate-mimicking constrained macrocyclic inhibitors of HIV-1 protease.

7. Conformational selection of inhibitors and substrates by proteolytic enzymes: implications for drug design and polypeptide processing.

8. Molecular recognition of macrocyclic peptidomimetic inhibitors by HIV-1 protease.

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