Mice Lacking α-Tubulin Acetyltransferase 1 Are Viable but Display α-Tubulin Acetylation Deficiency and Dentate Gyrus Distortion

Kim, Go-Woon; Li, Lin; Ghorbani, Mohammad; You, Linya; Yang, Xiang-Jiao

doi:10.1074/jbc.m113.464792

Cited by 120 publications

(112 citation statements)

References 84 publications

(129 reference statements)

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“…In agreement with recent work (Kalebic et al. , 2013b; Kim et al. , 2013), no acetylated tubulin was detected in the αTat1-deficient mouse brain, either by immunoblot or immunohistochemistry, suggesting that αTat1 is the sole tubulin acetyltransferase in vivo.…”

Section: Discussionmentioning

confidence: 99%

α-Tubulin K40 acetylation is required for contact inhibition of proliferation and cell–substrate adhesion

Aguilar

Becker

Tedeschi

et al. 2014

MBoC

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Section: Discussionmentioning

confidence: 99%

α-Tubulin K40 acetylation is required for contact inhibition of proliferation and cell–substrate adhesion

Aguilar

Becker

Tedeschi

et al. 2014

MBoC

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“…Furthermore, αTAT1 associates with acetylated MTs in axons and cilia in vivo [65, 66]. Indeed, male mice lacking αTAT1 are less fertile due to altered sperm morphology and motility [65]; however, they do not exhibit obvious behavioral or neurological defects beyond subtle changes in brain architecture [70]. However, in mice without αTAT1 or acetylated MTs, the MTs were more resistant to nocodazole, suggesting increased MT stability [65].…”

Section: Acetylation and Deacetylation Of Tubulinsmentioning

confidence: 99%

Post-translational modifications of tubulin: pathways to functional diversity of microtubules

Song

Brady

2015

Trends in Cell Biology

325

305

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Tubulin and microtubules are subject to a remarkable number of posttranslational modifications. Understanding the roles these modifications play in determining functions and properties of microtubules has presented a major challenge that is only now being met. Many of these modifications are found concurrently, leading to considerable diversity in cellular microtubules, which varies with development, differentiation, cell compartment and cell cycle. We now know that posttranslational modifications of tubulin affect not only the dynamics of the microtubules, but also their organization and interaction with other cellular components. Many early suggestions of how posttranslational modifications affect microtubules have been replaced with new ideas and even new modifications as our understanding of cellular microtubule diversity comes into focus.

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“…However, other studies have shown that αTat1 (α-tubulin K40 acetyltransferase) is a predominant/major α-tubulin acetyltransferases in vivo in mammals and nematodes and fine-tunes hippocampus development (Shida et al, 2010; Kim et al, 2013). As a side note, in D. melanogaster , Naa50 has been shown to acetylate β-tubulin at K252 on soluble tubulin heterodimers but not tubulins in MTs.…”

Section: Mammalsmentioning

confidence: 99%

The biological functions of Naa10 — From amino-terminal acetylation to human disease

Dörfel

Lyon

2015

Gene

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N-terminal acetylation (NTA) is one of the most abundant protein modifications known, and the N-terminal acetyltransferase (NAT) machinery is conserved throughout all Eukarya. Over the past 50 years, the function of NTA has begun to be slowly elucidated, and this includes the modulation of protein–protein interaction, protein-stability, protein function, and protein targeting to specific cellular compartments. Many of these functions have been studied in the context of Naa10/NatA; however, we are only starting to really understand the full complexity of this picture. Roughly, about 40% of all human proteins are substrates of Naa10 and the impact of this modification has only been studied for a few of them. Besides acting as a NAT in the NatA complex, recently other functions have been linked to Naa10, including post-translational NTA, lysine acetylation, and NAT/KAT-independent functions. Also, recent publications have linked mutations in Naa10 to various diseases, emphasizing the importance of Naa10 research in humans. The recent design and synthesis of the first bisubstrate inhibitors that potently and selectively inhibit the NatA/Naa10 complex, monomeric Naa10, and hNaa50 further increases the toolset to analyze Naa10 function.

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Mice Lacking α-Tubulin Acetyltransferase 1 Are Viable but Display α-Tubulin Acetylation Deficiency and Dentate Gyrus Distortion

Cited by 120 publications

References 84 publications

α-Tubulin K40 acetylation is required for contact inhibition of proliferation and cell–substrate adhesion

α-Tubulin K40 acetylation is required for contact inhibition of proliferation and cell–substrate adhesion

Post-translational modifications of tubulin: pathways to functional diversity of microtubules

The biological functions of Naa10 — From amino-terminal acetylation to human disease

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