Kentson Lam scite author profile

Salinosporamide A (1, NPI-0052) is a potent proteasome inhibitor in development for treating cancer. In this study, a series of analogues was assayed for cytotoxicity, proteasome inhibition, and inhibition of NF-kappaB activation. Marked reductions in potency in cell-based assays accompanied replacement of the chloroethyl group with unhalogenated substituents. Halogen exchange and cyclohexene ring epoxidation were well tolerated, while some stereochemical modifications significantly attenuated activity. These findings provide insights into structure-activity relationships within this novel series.

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Discovery of novel metabolites from marine actinomycetes

Lam¹

2006

Current Opinion in Microbiology

461

231

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Discovery and development of the anticancer agent salinosporamide A (NPI-0052)

Fenical

Jensen

Palladino³

et al. 2009

Bioorganic & Medicinal Chemistry

258

195

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The discovery of the anticancer agent salinosporamide A (NPI-0052) resulted from the exploration of new marine environments and a commitment to the potential of the ocean to yield new natural products for drug discovery and development. Driving the success of this process was the linkage of academic research together with the ability and commitment of industry to undertake drug development and provide the resources and expertise to advance the entry of salinosporamide A (NPI-0052) into human clinical trials. This paper offers a chronicle of the important events that facilitated the rapid clinical development of this exciting molecule.

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Kentson Lam

New aspects of natural products in drug discovery

Structure−Activity Relationship Studies of Salinosporamide A (NPI-0052), a Novel Marine Derived Proteasome Inhibitor

Discovery of novel metabolites from marine actinomycetes

Discovery and development of the anticancer agent salinosporamide A (NPI-0052)

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