Microtubule-severing enzymeskatanin, spastin, fidgetinare related AAA-ATPases that cut microtubules into shorter filaments. These proteins, also called severases, are involved in a wide range of cellular processes including cell division, neuronal development, and tissue morphogenesis. Paradoxically, severases can amplify the microtubule cytoskeleton and not just destroy it. Recent work on spastin and katanin has partially resolved this paradox by showing that these enzymes are strong promoters of microtubule growth. Here, we review recent structural and biophysical advances in understanding the molecular mechanisms of severing and growth promotion that provide insight into how severing enzymes shape microtubule networks. Severing Enzymes Are Multifunctional Microtubule Regulators The structure of the microtubule cytoskeleton is defined by the location, number, length, and orientation of the constituent microtubules. Microtubule organization differs between different cell types, different locations within one cell (e.g., mitotic spindle, membrane cortex, cilium), and different times (e.g., phase of the cell cycle, in response to external signals). The microtubule cytoskeleton is shaped by microtubule-associated proteins (MAPs), a diverse collection of proteins that regulate all aspects of microtubule growth and shrinkage [1-3]. They accelerate or decelerate microtubule polymerization and depolymerization, alter the rates of the transitions between growing and shrinking states known respectively as catastrophe (see Glossary) and rescue [4,5], and nucleate new microtubules [6,7]. Among this wide variety of microtubule regulators are the severing enzymesspastin, katanin, and fidgetinthat cut microtubules into smaller fragments (Box 1). Severases play key roles in many cellular processes: mitosis and meiosis [8,9], ciliogenesis [10], neurodevelopment [11-13], cell migration [14], and cell wall biosynthesis [15] and phototropism [16] in plants [17,18]. These diverse roles, which involve both assembly and disassembly of the cytoskeleton, hint at severases having broader activities than just severing microtubules.
