Synthesis and preliminary PET imaging of 11C and 18F isotopologues of the ROS1/ALK inhibitor lorlatinib

Thomas Lee Collier; Marc D. Normandin; Nickeisha A. Stephenson; Eli Livni; Steven H. Liang; Dustin W. Wooten; Shadi A. Esfahani; Michael G. Stabin; Umar Mahmood; Jianqing Chen; Wei Wang; Kevin Maresca; Rikki N. Waterhouse; Georges El Fakhri; Paul Richardson; Neil Vasdev

doi:10.1038/ncomms15761

Nature Communications (Jun 2017)

Synthesis and preliminary PET imaging of 11C and 18F isotopologues of the ROS1/ALK inhibitor lorlatinib

Thomas Lee Collier,
Marc D. Normandin,
Nickeisha A. Stephenson,
Eli Livni,
Steven H. Liang,
Dustin W. Wooten,
Shadi A. Esfahani,
Michael G. Stabin,
Umar Mahmood,
Jianqing Chen,
Wei Wang,
Kevin Maresca,
Rikki N. Waterhouse,
Georges El Fakhri,
Paul Richardson,
Neil Vasdev

Affiliations

Thomas Lee Collier: Massachusetts General Hospital and Harvard Medical School
Marc D. Normandin: Massachusetts General Hospital and Harvard Medical School
Nickeisha A. Stephenson: Massachusetts General Hospital and Harvard Medical School
Eli Livni: Massachusetts General Hospital and Harvard Medical School
Steven H. Liang: Massachusetts General Hospital and Harvard Medical School
Dustin W. Wooten: Massachusetts General Hospital and Harvard Medical School
Shadi A. Esfahani: Massachusetts General Hospital and Harvard Medical School
Michael G. Stabin: Vanderbilt University
Umar Mahmood: Massachusetts General Hospital and Harvard Medical School
Jianqing Chen: Pfizer Inc., Quantitative Medicine, Worldwide Research and Development
Wei Wang: Pfizer Worldwide Research and Development
Kevin Maresca: Pfizer Inc., Quantitative Medicine, Worldwide Research and Development
Rikki N. Waterhouse: Pfizer Inc., Quantitative Medicine, Worldwide Research and Development
Georges El Fakhri: Massachusetts General Hospital and Harvard Medical School
Paul Richardson: Pfizer Worldwide Research and Development
Neil Vasdev: Massachusetts General Hospital and Harvard Medical School

DOI: https://doi.org/10.1038/ncomms15761
Journal volume & issue: Vol. 8, no. 1
pp. 1 – 12

Abstract

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Lorlatinib—a ROS1/ALK inhibitor—is currently undergoing clinical trials for the treatment of non-small cell lung cancers. Here the authors develop synthetic routes to11C- and 18F-labelled lorlatinib, with subsequent PET imaging showing good blood brain barrier permeability in non-human primates.

Published in Nature Communications

ISSN: 2041-1723 (Online)
Publisher: Nature Portfolio
Country of publisher: United Kingdom
LCC subjects: Science
Website: https://www.nature.com/ncomms/

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