Therapeutic application of anti-arthritis, pain-releasing, and anti-cancer effects of bee venom and its constituent compounds

Dong Ju Son, … Jin Tae Hong, in Pharmacology & Therapeutics, 2007

https://doi.org/10.1016/j.pharmthera.2007.04.004Get rights and content

Bee venom (BV) therapy (BVT) is the therapeutic application of honeybee venom (HBV) to the treatment of various diseases. BVT has been used as a traditional medicine to treat a variety of conditions, such as arthritis, rheumatism, back pain, cancerous tumors, and skin diseases (Hider, 1988). BV contains at least 18 active components, including enzymes, peptides, and biogenic amines, which have a wide variety of pharmaceutical properties. BV might modify the immune system functions in the body and contribute to the increased production of cortisol (Vick et al., 1972). The healing potency of BV in the treatment of arthritis and rheumatism is initiated after stimulating the production of cortisol in the adrenal glands, which in turn has anti-inflammatory activity (Vick & Shipman, 1972). Recent studies have reported a variety of mechanisms for the anti-arthritis and/or anti-inflammatory effects of BV and its constituents. The decrease in cyclooxygenase (COX)-2 and phospholipase (PL) A₂ expression and the decrease in the levels of tumor necrosis factor alpha (TNF-α), interleukin (IL)-1, IL-6, nitric oxide (NO) and oxygen reactive species (ROS) are suggested to be associated with the anti-arthritis effect of melittin (Murakami et al., 1997; Pelletier et al., 1998; Yang et al., 1999; Amin et al., 1999; Cernanec et al., 2002). Adolapin also has anti-inflammatory activity in carrageenan-, prostaglandin (PG)-, and adjuvant-induced rat hind paw edema and adjuvant polyarthritis. The effects of adolapin are presumably due to its ability to inhibit the PG synthesis system through COX inhibitory properties (Shkenderov & Koburova, 1982; Koburova et al., 1985). Apamin, a small conductance Ca²⁺-activated K⁺ channel blocker, significantly inhibited both ovalumine-induced tracheal contraction and histamine release from lung tissues, suggesting that this compound reduces allergic airway inflammation through a mast cell stabilizing effect (Ichinose et al., 1995). The mast-cell-degranulating (MCD) peptide has an anti-allergic activity by inhibiting the release of histamine from mast cells (Buku, 1999). The MCD peptide binds to the mast cell receptors in a dose–response manner and has been found to partially inhibit the binding of IgE to this receptor (Buku et al., 2001). Recently, it was found that melittin inhibited the DNA-binding activity of NF-κB, a critical transcriptional factor regulating inflammatory gene expression, by inhibiting IκB phosphorylation (Park et al., 2004, 2007). This result may be critical to understanding the anti-inflammatory and anti-arthritis mechanisms of BV and melittin, its major constituent.