The Anticoagulant Activity of 3.3’-(p-Alkylthio-Benzylidene)-Bis-4-Hydroxycoumarins and Their Oxidation Products

 

 Buy Article Permissions and Reprints

Summary

The anticoagulant activity of 3.3’-(benzylidene)-bis-4-hydroxycoumarin derivatives has been estimated by one step Quick’s method. The derivatives contained the following groups in the para position of benzylidene residue: NCS- (I), CH₃-S- (II), CH₃-SO-(III), CH₃-S0₂- (IV), C₂H₅-S- (V), C₂H₅-SO- (VI), C₂H₅-S0₂- (VII). All these compounds were much more active than 3.3’-(benzylidene)-bis-4-hydroxycoumarin itself.

Compounds possessing the ethyl chain at the sulphur atom (V, VI, VII) were more active than methyl homologues (II, III, IV). Comparison of the activity of the series of thio-, sulphoxy-, and sulphonyl-derivatives showed that among methyl- and ethyl-derivatives those with the sulphoxy grouping (III, VI) displayed the greatest anticoagulant activity. The action of sulphonyl (IV, VII) and thio-derivatives (II, V) was weaker and shortest. The derivative with the NCS-group (I) possessed a relatively the lowest activity among the investigated compounds. 3.3’-(p-Ethylsulphoxybenzyl-idene)-bis-4-hydroxycoumarin (VI), with distinct biological activity reached about ½ of dicoumarol activity.

• References

• 1 Eckstein M, Cwynar J. Studies of compounds with anticoagulant activity from the group of 4-hydroxycoumarin derivatives. Part IV. Condensation products of 4-hydroxycoumarin with halogen derivatives of aromatic aldehydes. Dissert. Pharmaceuticae (Krakow) 14: 29 1962;
  PubMedGoogle Scholar
• 2 Gori E, Molteni L. Nuovi anticoagulanti ad attivity prothrombinopenica. Parte I. Seria dicumarolica. Bend. 1st. Lombardo Sci. e Lett 86: III 551 1953;
  PubMedGoogle Scholar
• 3 Gori E. Attività, tossicità ed antidotismo di un nuovo anticoagulante a struttura dicumarolica: la 3.3’-metil-tiopropiliden-bis-(4-idrossicumarina). Rend. 1st. Lombardo Sci. e Lett 56: 111 607 1953;
  PubMedGoogle Scholar
• 4 Gumińska M, Eckstein M. The anticoagulant actien of some derivatives of 3.3’-(arylidene)-bis-4-hydroxycoumarin. J. med. pharm. Chem 3: 583 1961;
  CrossrefPubMedGoogle Scholar
• 5 Maj J, Przegalinski E. Wlasnosci farmakologiczne aktywnych przeciwzakrzepowo 3.3’-(chlorobenzylideno)-bis-4-hydroksykumaryn. Dissert. Pharmaceuticae (Kraków) 17: 163 1965;
  PubMedGoogle Scholar
• 6 Overman R. S, Stahmann M. A, Huebner Ch. F, Sullivan W. R, Spero L, Doherty D. G, Ikawa M, Graf L, Roseman S, Link K. Studies on the hemorrhagic sweet clover disease. XIII. Anticoagulant activity and structure in the 4-hydroxycoumarin group. J. biol. Chem 153: 5 1944;
  PubMedGoogle Scholar
• 7 Quick A. J. On various properties of thromboplastin (aqueous tissue extracts). Amer. J. Physiol 214: 282 1936;
  PubMedGoogle Scholar
• 8 Quick A. J. The coagulation defect in sweet clover disease and in the hemorrhagic chick disease of dietary origin. Amer. J. Physiol 118: 260 1937;
  PubMedGoogle Scholar
• 9 Sulko J, Eckstein M. Badania nad pochodnymi 4-hydroksykumaryny. LX. 3.3’-(p-Alkilo-tiobenzylideno)-bis-4-hydroksykumaryny i produkty ich utlenienia. Dissert. Pharm. Pharmacol. (Krakow) (In press.) (1967).
  PubMedGoogle Scholar
• 10 Trcka V. Activity of some new types of coumarin anticoagulants and related substances, p. 231. Pharmacotherapeutica 1950–1959. Statni Zdravotnickë Nakl. Praha 1961.
  PubMed
• 11 Trčka V. Ucinnost nëkolika typu antikoagulancii N odvosenych od 4-hydroxykumarinu. Čs. Farm 12: 65 1963;
  PubMedGoogle Scholar
• 12 Witte S, Heinkel K, Drinberger P. Untersuchungen über die Wirkung von Vitamin K auf die Gerinnungsstörungen bei der Äthioninpankreatitis der Ratte. Z. ges. exp. Med 122: 249 1953;
  CrossrefPubMedGoogle Scholar