Anticoagulation & Antiplatelet Compounds

Calin is a ~65 kDa glycoprotein that inhibits collagen-mediated platelet adhesion and von Willebrand factor (vWF) binding. Unlike hirudin, which targets thrombin, calin prevents platelets from adhering to damaged tissue in the first place.

Clinical significance: Calin is responsible for the prolonged post-detachment bleeding phase (the "passive bleed") that can last 4 to 24 hours after the leech is removed. This sustained bleeding is therapeutically valuable in venous congestion management.

Apyrase is an ATP-diphosphohydrolase that hydrolyzes ADP (adenosine diphosphate) — a key platelet aggregation agonist released during the coagulation cascade.

By degrading ADP, apyrase blocks ADP-dependent platelet aggregation. It works synergistically with calin: calin prevents initial adhesion, apyrase prevents subsequent aggregation — two distinct targets, same outcome.

Saratin is a ~12 kDa peptide that inhibits platelet-collagen adhesion through a mechanism distinct from calin. While calin targets vWF binding, saratin directly blocks the platelet collagen receptor (GPVI).

Saratin has been investigated as a standalone antiplatelet agent in preclinical research, though no pharmaceutical product has reached clinical trials.

Leech saliva contains antistatin (originally identified in Haementeria leeches, with homologs in Hirudo) — a peptide that blocks factor Xa in the coagulation cascade.

Factor Xa inhibition represents yet another anticoagulation mechanism, complementing the direct thrombin inhibition (hirudin) and platelet-targeted strategies (calin, apyrase, saratin).