Chemistry:Cytochalasin

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Short description: Group of chemical compounds

Cytochalasins are fungal metabolites that have the ability to bind to actin filaments and block polymerization and the elongation of actin. As a result of the inhibition of actin polymerization, cytochalasins can change cellular morphology, inhibit cellular processes such as cell division, and even cause cells to undergo apoptosis.[1] Cytochalasins have the ability to permeate cell membranes, prevent cellular translocation and cause cells to enucleate.[2] Cytochalasins can also have an effect on other aspects of biological processes unrelated to actin polymerization. For example, cytochalasin A and cytochalasin B can also inhibit the transport of monosaccharides across the cell membrane,[2] cytochalasin H has been found to regulate plant growth,[3] cytochalasin D inhibits protein synthesis[4] and cytochalasin E prevents angiogenesis.[5]

Binding to actin filaments

Cytochalasins are known to bind to the barbed, fast growing plus ends of microfilaments, which then blocks both the assembly and disassembly of individual actin monomers from the bound end. Once bound, cytochalasins essentially cap the end of the new actin filament. One cytochalasin will bind to one actin filament.[2] Studies done with cytochalasin D (CD) have found that CD-actin dimers contain ATP-bound actin upon formation.[6] These CD-actin dimers are reduced to CD-actin monomers as a result of ATP hydrolysis. The resulting CD-actin monomer can bind ATP-actin monomer to reform the CD-actin dimer.[2] CD is very effective; only low concentrations (0.2 μM) are needed to prevent membrane ruffling and disrupt treadmilling.[7] The effects of many different cytochalasins on actin filaments were analyzed and higher concentrations (2-20 μM) of CD were found to be needed to remove stress fibers.[7]

In contrast, latrunculin inhibits actin filament polymerization by binding to actin monomers.

Uses and applications of cytochalasins

Actin microfilaments have been widely studied using cytochalasins. Due to their chemical nature, cytochalasins can help researchers understand the importance of actin in various biological processes. The use of cytochalasins has allowed researchers to better understand actin polymerization, cell motility, ruffling, cell division, contraction, and cell stiffness. The use of cytochalasins has been so important to understanding cytoskeletal movement and many other biological processes, researchers have created two synthetic cytochalasins.[1]

Cytochalasin has found practical application in thromboelastometry (TEM) whole blood assays for the assessment of fibrinogen and fibrin polymerization disorders in the FIBTEM assay on ROTEM. This test is based on the principle that cytochalasin D very effectively inhibits platelet function by inhibition of the contractile elements.[8] The platelet inhibition is more effective than when platelets are blocked by GPIIb/IIIa antagonists.[9] In vitro and clinical data indicate that the clot strength in FIBTEM increases in a fibrinogen concentration-dependent manner independent of platelet count.[10] Therefore, fibrinogen deficiency or fibrin polymerization disorders can be rapidly detected.

Chemical structures

See also

References

  1. 1.0 1.1 Haidle, A. M.; Myers, A. G. (2004). "An Enantioselective, Modular, and General Route to the Cytochalasins: Synthesis of L-696,474 and Cytochalasin B". Proceedings of the National Academy of Sciences 101 (33): 12048–12053. doi:10.1073/pnas.0402111101. PMID 15208404. PMC 514432. http://www.pnas.org/content/101/33/12048.full.pdf. 
  2. 2.0 2.1 2.2 2.3 Cooper, J. A. (1987). "Effects of Cytochalasin and Phalloidin on Actin". Journal of Cell Biology 105 (4): 1473–1478. doi:10.1083/jcb.105.4.1473. PMID 3312229. PMC 2114638. http://jcb.rupress.org/content/105/4/1473.full.pdf. 
  3. Cox, R. H.; Cutler, H. G.; Hurd, R. E.; Cole, R. J. (1983). "Proton and Carbon-13 Nuclear Magnetic Resonance Studies of the Conformation of Cytochalasin H Derivatives and Plant Growth Regulating Effects of Cytochalasins". Journal of Agricultural and Food Chemistry 31 (2): 405–408. doi:10.1021/jf00116a055. 
  4. Ornelles, D. A.; Fey, E. G.; Penman, S. (1986). "Cytochalasin Releases mRNA from the Cytoskeletal Framework and Inhibits Protein Synthesis". Molecular and Cellular Biology 6 (5): 1650–1662. doi:10.1128/mcb.6.5.1650. PMID 3785175. 
  5. Udagawa, T.; Yuan, J.; Panigrahy, D.; Chang, Y.-H.; Shah, J.; D’Amato, R. J. (2000). "Cytochalasin E, an Epoxide Containing Aspergillus-Derived Fungal Metabolite, Inhibits Angiogenesis and Tumor Growth". Journal of Pharmacology and Experimental Therapeutics 294 (2): 421–427. PMID 10900214. http://jpet.aspetjournals.org/content/294/2/421.full.pdf. 
  6. Goddette, D. W.; Frieden, C. (1987). "Actin Polymerization - The Mechanism of Action of Cytochalasin D". Journal of Biological Chemistry 261 (34): 15974–15980. doi:10.1016/S0021-9258(18)66662-1. PMID 3023337. http://www.jbc.org/content/261/34/15974.full.pdf. 
  7. 7.0 7.1 Yahara, I.; Harada, F.; Sekita, S.; Yoshihira, K.; Natori, S. (1982). "Correlation between effects of 24 different cytochalasins on cellular structures and cellular events and those on actin in vitro". Journal of Cell Biology 92 (1): 69–78. doi:10.1083/jcb.92.1.69. PMID 7199054. 
  8. May, J. A.; Ratan, H.; Glenn, J. R.; Lösche, W.; Spangenberg, P.; Heptinstall, S. (1998). "GPIIb-IIIa antagonists cause rapid disaggregation of platelets pretreated with cytochalasin D. Evidence that the stability of platelet aggregates depends on normal cytoskeletal assembly". Platelets 9 (3–4): 227–232. doi:10.1080/09537109876744. PMID 16793707. 
  9. Lang, T.; Toller, W.; Gütl, M.; Mahla, E.; Metzler, H.; Rehak, P.; März, W.; Halwachs-Baumann, G. (2004). "Different effects of abciximab and cytochalasin D on clot strength in thrombelastography". Journal of Thrombosis and Haemostasis 2 (1): 147–153. doi:10.1111/j.1538-7836.2004.00555.x. PMID 14717978. 
  10. Lang, T.; Johanning, K.; Metzler, H.; Piepenbrock, S.; Solomon, C.; Rahe-Meyer, N.; Tanaka, K. A. (2009). "The effects of fibrinogen levels on thromboelastometric variables in the presence of thrombocytopenia". Anesthesia and Analgesia 108 (3): 751–758. doi:10.1213/ane.0b013e3181966675. PMID 19224779. http://www.anesthesia-analgesia.org/content/108/3/751.full.pdf.