in
Sandwip displaying signs of rigor mortis After
death, aerobic respiration in an organism ceases, depleting the source of oxygen used in the making of
adenosine triphosphate (ATP). ATP is required to cause separation of the
actin-myosin cross-bridges during relaxation of muscle. When oxygen is no longer present, the body may continue to produce ATP via anaerobic
glycolysis. When the body's
glycogen is depleted, the ATP concentration diminishes, and the body enters rigor mortis because it is unable to break those bridges. Calcium enters the
cytosol after death. Calcium is released into the cytosol due to the deterioration of the
sarcoplasmic reticulum. Also, the breakdown of the
sarcolemma causes additional calcium to enter the cytosol. The calcium activates the formation of actin-myosin cross-bridging. Once calcium is introduced into the cytosol, it binds to the troponin of thin filaments, which causes the troponin-tropomyosin complex to change shape and allow the myosin heads to bind to the active sites of actin proteins. In rigor mortis,
myosin heads continue binding with the active sites of actin proteins via
adenosine diphosphate (ADP), and the muscle is unable to relax until further enzyme activity degrades the complex. Normal relaxation would occur by replacing ADP with ATP, which would destabilize the myosin-actin bond and break the cross-bridge. However, as ATP is absent, there must be a breakdown of muscle
tissue by
enzymes (endogenous or bacterial) during
decomposition. As part of the process of decomposition, the myosin heads are degraded by the enzymes, allowing the muscle contraction to release and the body to relax. Decomposition of the myofilaments occurs between 48 and 60 hours after the peak of rigor mortis, which occurs approximately 13 hours after death. == Nysten's rule ==