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Original Articles

Diorganotin(IV) Derivatives of Dipeptides Containing at Least One Essential Amino Acid Residue: Synthesis, Characteristic Spectral Data, Cardiovascular, and Anti‐inflammatory Activities

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Pages 1689-1708 | Received 13 Sep 2003, Accepted 02 Jun 2004, Published online: 16 Nov 2010
 

Abstract

New diphenyltin(IV) derivatives of the formula Ph2SnL, where L is the dianion of glycyltryptophan (Gly‐Trp), glycylphenylalanine (Gly‐Phe), valylvaline (Val‐Val), alanylvaline (Ala‐Val), and leucylalanine (Leu‐Ala), have been synthesized by the reaction of Ph2SnCl2 and the disodium salt of the respective dipeptides. The bonding and coordination behaviour in these derivatives are discussed on the basis of IR, multinuclear 1H, 13C, and 119Sn NMR and 119Sn Mössbauer spectroscopic studies. These investigations suggest that all the dipeptides in Ph2SnL act as dianionic tridentate ligands coordinating through the COO, NH2, and Npeptide groups. The 119Sn Mössbauer studies, together with the NMR data, suggest a trigonal‐bipyramidal geometry around tin in Ph2SnL with the phenyl groups and Npeptide in the equatorial positions, whereas a carboxylic oxygen and the amino nitrogen atom occupy the axial positions. The anti‐inflammatory and cardiovascular activities, and toxicity of all the synthesized diphenyltin(IV) derivatives of dipeptides and of n‐dibutyltin(IV) derivatives of dipeptides (synthesized and characterized earlier) viz. Gly‐Trp, Val‐Val, Ala‐Val, glycyltyrosine (Gly‐Tyr), leucyltyrosine (Leu‐Tyr), and leucylleucine (Leu‐Leu) are discussed. The n‐dibutyltin(IV) derivatives exhibit better cardiovascular and anti‐inflammatory activities than the diphenyltin(IV) analogues.

Acknowledgments

This work was a part of a major research project sponsored by the Department of Science and Technology (DST) (Grant No. SP/S1/F‐07/2000), New Delhi, India. M. Nath is thankful to the DST, New Delhi, India. Financial support for the Mössbauer work from the National Institute of Health, Minority Biomedical Research Support Programs MBRS/SCORE, GM08005, is gratefully acknowledged. Thanks are also due to the Head, Regional Sophisticated Instrumentation Centre, Central Drug Research Institute, Lucknow, India, for elemental analyses and NMR spectral measurements, and to the Head, Department of Chemistry, Indian Institute of Technology, Delhi, India, for 119Sn NMR spectral studies. One of the authors (S. Pokharia) is thankful to the Council for Scientific and Industrial Research, New Delhi, for a Senior Research fellowship during the period of writing this manuscript.

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