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      Recent Progress in the Discovery of Next Generation Inhibitors of Aromatase from the Structure–Function Perspective

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      Journal of medicinal chemistry

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          Abstract

          Human aromatase catalyzes the synthesis of estrogen from androgen with high substrate specificity. For the past 40 years, aromatase has been a target of intense inhibitor discovery research for the prevention and treatment of estrogen-dependent breast cancer. The so-called third generation aromatase inhibitors (AIs) letrozole, anastrozole, and the steroidal exemestane were approved in the U.S. in the late 1990s for estrogen-dependent postmenopausal breast cancer. Efforts to develop better AIs with higher selectivity and lower side effects were handicapped by the lack of an experimental structure of this unique P450. The year 2009 marked the publication of the crystal structure of aromatase purified from human placenta, revealing an androgen-specific active site. The structure has reinvigorated research activities on this fascinating enzyme and served as the catalyst for next generation AI discovery research. Here, we present an account of recent developments in the AI field from the perspective of the enzyme’s structure–function relationships.

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          Journal
          9716531
          4938
          J Med Chem
          J. Med. Chem.
          Journal of medicinal chemistry
          0022-2623
          1520-4804
          7 June 2016
          19 January 2016
          9 June 2016
          09 June 2017
          : 59
          : 11
          : 5131-5148
          Affiliations
          Department of Pharmacology, State University of New York Upstate Medical University, 750 East Adams Street, Syracuse, New York 13210, United States
          Author notes
          [* ]Corresponding Author: ghoshd@ 123456upstate.edu . Phone: 315-464-9677
          Article
          PMC4915572 PMC4915572 4915572 nihpa792373
          10.1021/acs.jmedchem.5b01281
          4915572
          26689671
          4e94adc7-989f-41d3-b578-ccbd1c4574c2
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