Sara Johnson Mcphail

Design and synthesis of conformationally-constrained MMP inhibitors

A novel series of conformationally constrained matrix metalloprotease inhibitors was identified. The potencies observed for these inhibitors were highly dependent upon the substitution pattern on the caprolactam ring as well as the succinate moiety.

Genomic expression changes induced by topical N-acetyl glucosamine in skin equivalent cultures in vitro

N‐acetyl glucosamine (NAG) has been shown to be effective in reducing the appearance of hyperpigmented spots. From published in vitro mechanistic testing, glucosamine inhibits enzymatic glycosylation, a required processing step in converting inactive human pro‐tyrosinase to the active tyrosinase, a key enzyme in the production of melanin. There is also published literature discussing the anti‐inflammatory and antioxidant properties of glucosamine compounds. To identify additional mechanisms by which NAG might affect melanin production, an in vitro genomics experiment was conducted in SkinEthic skin equivalent cultures, which were topically dosed with NAG vs. a vehicle control. Relative to vehicle, NAG reduced melanin production, and the expression of several pigmentation‐relevant genes were affected (down‐regulated or up‐regulated) by NAG treatment. Thus, there are several mechanisms that may be operative in the observed pigmentation effects.

Synthesis of potent and selective inhibitors of human plasma kallikrein.

The synthesis and in vitro enzyme inhibition profile of a series of novel trifluoromethylketone (TFMK) inhibitors of human plasma kallikrein (PK) are described. We have developed an efficient method for the construction of peptide TFMKs that provides the final product devoid of compromised stereochemical integrity. Many of these compounds are potent inhibitors of PK and exhibit reduced inhibition of tissue kallikrein (TK) and plasmin (HP).