In developmental biology, all cellular events are suitably synchronized to
ensure proper growth and development of any multicellular organism. A healthy adult
tissue is often characterized by stem cells that can undergo orchestrated cell division
and differentiation. Disruption of these events often leads to cancer resulting from the
accretion or accumulation of the genetic and epigenetic changes that occur at the
somatic as well as the germ line levels. In the recent years, significant progress has
been made in the early detection, treatment and prevention of cancer. Targeted cancer
therapies include the use of apoptosis inducing drugs and drugs that target microtubules
among others. Over the past few years, drugs that inhibit microtubule dynamics have
been successfully used as anticancer drugs. They can either be microtubule stabilizers
(Vincristine, Vinblastine, Colchicine etc.) or microtubule destabilizers (Paclitaxel,
Docetaxel, Epithilones, Taccalonolides etc.). Recently, new classes of compounds have
been identified that interfere with cell growth and proliferation as a consequence of
binding to tubulin αβ- dimers. Natural compounds like Curcumin have shown to inhibit
tubulin activity. Whereas some antimitotic agents like Aurora A/B, Pentoxifylline,
benzimidazole derivatives, combrestatin, polymeric nanoparticles etc. have been
reported to show significant effect in the treating several types of cancer which were
previously deemed untreatable. The following chapter acknowledges the presence of
these anti-tumor compounds and how they target microtubules and further aid in the
treatment of various cancers afflicting human beings.
Keywords: Antimitotic agents, Aurora A, Apoptosis, Cancer, Combretastatin
analogs, Colchicine, Curcumin, Docetaxel, Epothilones, Microtubules,
Microtubule polymerizers, Microtubule depolymerizers, Paclitaxel,
Pentoxifylline, Taccalonolides, Taxanes, Tubulin, Vinca alkaloids, Vinblastine,
Indexing words: Microtubules, Anti-cancer drug targets, Microtubule stabilizers,
Taxanes, Epothilones, Taccalonolides, Microtubule destabilizers, Vinca alkaloids,
Colchicine, Halichondrin B, Dolostatin 10, Aurora A, Curcumin, Pentoxifylline,
Combretastatin, Benzimidazole derivatives, Casein K2 peptide inhibitor,
Nanoparticles.