Facile entry to an efficient and practical enantioselective synthesis of a polycyclic cholesteryl ester transfer protein inhibitor.

نویسندگان

  • Zhengxu S Han
  • Yibo Xu
  • Daniel R Fandrick
  • Sonia Rodriguez
  • Zhibin Li
  • Bo Qu
  • Nina C Gonnella
  • Sanjit Sanyal
  • Jonathan T Reeves
  • Shengli Ma
  • Nelu Grinberg
  • Nizar Haddad
  • Dhileep Krishnamurthy
  • Jinhua J Song
  • Nathan K Yee
  • Waldemar Pfrengle
  • Markus Ostermeier
  • Jürgen Schnaubelt
  • Zeno Leuter
  • Sonja Steigmiller
  • Jürgen Däubler
  • Emanuel Stehle
  • Lukas Neumann
  • Thomas Trieselmann
  • Patrick Tielmann
  • Annette Buba
  • Rainer Hamm
  • Gunter Koch
  • Svenja Renner
  • Juan R Dehli
  • Florian Schmelcher
  • Christian Stange
  • Jürgen Mack
  • Rainer Soyka
  • Chris H Senanayake
چکیده

An efficient enantioselective synthesis of the chiral polycyclic cholesteryl ester transfer protein (CETP) inhibitor 1 has been developed. The synthesis was rendered practical for large scale via the development of a modified Hantzsch-type reaction to prepare the sterically hindered pyridine ring, enantioselective hydrogenation of hindered ketone 6 utilizing novel BIBOP-amino-pyridine derived Ru complex, efficient ICl promoted lactone formation, and a BF3 mediated hydrogenation process for diastereoselective lactol reduction. This efficient route was successfully scaled to produce multikilogram quantities of challenging CETP drug candidate 1.

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عنوان ژورنال:
  • Organic letters

دوره 16 16  شماره 

صفحات  -

تاریخ انتشار 2014