Pd-catalysed general access to 7-membered N/O-heterocyclic compounds as potential agents against inflammation

B. Thirupataiah; Gangireddy Sujeevan Reddy; Guntipally Mounika; Jetta Sandeep Kumar; Kazi Amirul Hossain; Jayesh Mudgal; Jessy E. Mathew; Gautham G. Shenoy; Marina Rajadurai; Kishore V. L. Parsa; Manojit Pal

doi:10.1039/D1CC04140A

Pd-catalysed general access to 7-membered N/O-heterocyclic compounds as potential agents against inflammation†

B. Thirupataiah,^ab Gangireddy Sujeevan Reddy,^ab Guntipally Mounika,^a Jetta Sandeep Kumar,^ab Kazi Amirul Hossain,^a Jayesh Mudgal,^b Jessy E. Mathew,^b Gautham G. Shenoy,

^b Marina Rajadurai,^a Kishore V. L. Parsa^a and Manojit Pal

*^a

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* Corresponding authors

^a Dr. Reddy's Institute of Life Sciences, University of Hyderabad Campus, Gachibowli, Hyderabad 500 046, India
E-mail: manojitpal@rediffmail.com

^b Manipal College of Pharmaceutical Sciences, Manipal Academy of Higher Education, Madhav Nagar, Manipal 576 104, Karnataka, India

Abstract

A Pd-catalysed regioselective synthesis of 4,5-disubstituted 7-membered N/O-heterocycles was achieved via the 7-endo-dig cyclization followed by C–C bond formation of 2-(1-alkynyl)phenylacetamide. The ligand/additive free cascade reaction proceeded in the presence of PdCl₂ in aqueous MeCN when the separate and individual use of methyl vinyl ketone and allyl bromide generally afforded an O- and N-heterocycle, respectively. The pharmacological assay was performed to identify the first example of a 1H-benzo[d]azepin-2(3H)-one based novel inhibitor of PDE4B.

Chemical Communications

Pd-catalysed general access to 7-membered N/O-heterocyclic compounds as potential agents against inflammation†

Abstract

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