A Tale of 12 Tails: Katanin Severing Activity Affected by Carboxy-Terminal Tail Sequences

In cells, microtubule location, length, and dynamics are regulated by a host of microtubule-associated proteins and enzymes that read where to bind and act based on the microtubule "tubulin code," which is predominantly encoded in the tubulin carboxy-terminal tail (CTT). Katanin is a highl...

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Published inBiomolecules (Basel, Switzerland) Vol. 13; no. 4; p. 620
Main Authors Lindsay, K Alice, Abdelhamid, Nedine, Kahawatte, Shehani, Dima, Ruxandra I, Sackett, Dan L, Finegan, Tara M, Ross, Jennifer L
Format Journal Article
LanguageEnglish
Published Switzerland MDPI AG 30.03.2023
MDPI
Subjects
Carboxylases
Cell division
Hydrophobicity
katanin
Katanin - analysis
Katanin - chemistry
Katanin - metabolism
microtubule-associated protein
Microtubule-associated proteins
Microtubule-Associated Proteins - metabolism
microtubule-severing enzyme
Microtubules
Microtubules - metabolism
Peptides
Physiological aspects
Polymers
post-translational modifications
Proteins
Tubulin
Tubulin - metabolism
tubulin code
tubulin isotypes
United States
katanin
microtubule-associated protein
post-translational modifications
tubulin code
tubulin isotypes
microtubule-severing enzyme
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Summary:In cells, microtubule location, length, and dynamics are regulated by a host of microtubule-associated proteins and enzymes that read where to bind and act based on the microtubule "tubulin code," which is predominantly encoded in the tubulin carboxy-terminal tail (CTT). Katanin is a highly conserved AAA ATPase enzyme that binds to the tubulin CTTs to remove dimers and sever microtubules. We have previously demonstrated that short CTT peptides are able to inhibit katanin severing. Here, we examine the effects of CTT sequences on this inhibition activity. Specifically, we examine CTT sequences found in nature, alpha1A (TUBA1A), detyrosinated alpha1A, Δ2 alpha1A, beta5 (TUBB/TUBB5), beta2a (TUBB2A), beta3 (TUBB3), and beta4b (TUBB4b). We find that these natural CTTs have distinct abilities to inhibit, most noticeably beta3 CTT cannot inhibit katanin. Two non-native CTT tail constructs are also unable to inhibit, despite having 94% sequence identity with alpha1 or beta5 sequences. Surprisingly, we demonstrate that poly-E and poly-D peptides are capable of inhibiting katanin significantly. An analysis of the hydrophobicity of the CTT constructs indicates that more hydrophobic polypeptides are less inhibitory than more polar polypeptides. These experiments not only demonstrate inhibition, but also likely interaction and targeting of katanin to these various CTTs when they are part of a polymerized microtubule filament.
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ISSN:2218-273X
2218-273X
DOI:10.3390/biom13040620