Exploration of mitotic poisons from plants a detailed investigation on the anticancer and antimitotic activities of securinine and zerumbone
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Abstract
Microtubules are a key component of the cytoskeleton that plays a crucial role in cell
newlinedivision and many other vital cellular processes. They are highly dynamic in nature and
newlineundergo polymerization and depolymerization in a short span of time.
newlineAll the cellular functions of microtubules are highly dependent on their polymerization
newlinedynamics. Molecules that target polymerization dynamics of microtubules are also
newlineknown as mitotic poisons. And they inhibit the metaphase-anaphase transition in the
newlinedividing cells. Prolonged mitotic arrest leads to apoptosis through various signaling
newlinepathways. Several small molecules that target microtubules have been developed with
newlinedifferent aims such as anticancer drugs, pesticides, anthelmintic and antifungal drugs
newlinesince it is vital for cell division and other important cellular processes. Antimitotic
newlinedrugs that disrupt the normal functioning of mitotic spindle have proven to be the most
newlineeffective chemotherapeutic drugs and most of them are derived from natural sources.
newlineChemotherapeutic drugs like vincristine, vinblastine, paclitaxel, podophyllotoxin,
newlinecamptothecin, and combretastatin are good examples of clinically successful antimitotic
newlineagents. Securinine and zerumbone are two plant-derived molecules that are proven to
newlinepossess strong anticancer activity against different cancer cell lines. However, the
newlinemechanism behind their cytotoxicity is not investigated in detail.
newlineSecurinine is a plant-derived alkaloid present in the roots of the Securinega suffruticosa.
newlineSecurinine effectively prevented the proliferation of cervical, breast, and lung cancer
newlinecells with an IC50 of 6, 10, and 11 and#956;M respectively and induced minimal toxicity in
newlinenormal HEK cell lines. Securinine at concentrations higher than IC50 induced
newlinesignificant depolymerization in interphase and mitotic microtubules. It effectively
newlinesuppressed the migration of HeLa cells indicating its potential as an anticancer drug.