4.7 Review

Antitubulin sulfonamides: The successful combination of an established drug class and a multifaceted target

Journal

MEDICINAL RESEARCH REVIEWS
Volume 39, Issue 3, Pages 775-830

Publisher

WILEY
DOI: 10.1002/med.21541

Keywords

molecular mechanisms; sulfonamides; tubulin binding drugs; tubulin binding sites

Funding

  1. Consejeria de Educacion de la Junta de Castilla y Leon
  2. EU's European Regional Development Fund - FEDER [SA030U16]

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Tubulin, the microtubules and their dynamic behavior are amongst the most successful antitumor, antifungal, antiparasitic, and herbicidal drug targets. Sulfonamides are exemplary drugs with applications in the clinic, in veterinary and in the agrochemical industry. This review summarizes the actual state and recent progress of both fields looking from the double point of view of the target and its drugs, with special focus onto the structural aspects. The article starts with a brief description of tubulin structure and its dynamic assembly and disassembly into microtubules and other polymers. Posttranslational modifications and the many cellular means of regulating and modulating tubulin's biology are briefly presented in the tubulin code. Next, the structurally characterized drug binding sites, their occupying drugs and the effects they induce are described, emphasizing on the structural requirements for high potency, selectivity, and low toxicity. The second part starts with a summary of the favorable and highly tunable combination of physical-chemical and biological properties that render sulfonamides a prototypical example of privileged scaffolds with representatives in many therapeutic areas. A complete description of tubulin-binding sulfonamides is provided, covering the different species and drug sites. Some of the antimitotic sulfonamides have met with very successful applications and others less so, thus illustrating the advances, limitations, and future perspectives of the field. All of them combine in a mechanism of action and a clinical outcome that conform efficient drugs.

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