SOD1 Lysine 123 Acetylation in the Adult Central Nervous System

Kaliszewski, Michael; Kennedy, Austin K.; Blaes, Shelby L; Shaffer, Robert; Knott, Andrew B.; Song, Wenjun; Hauser, Henry A.; Bossy, Blaise; Huang, Ting‐Ting; Bossy‐Wetzel, Ella

doi:10.3389/fncel.2016.00287

Cited by 10 publications

(8 citation statements)

References 45 publications

(51 reference statements)

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“…Glutathionylation, palmitoylation, succinylation and acetylation are among the PTMs of SOD1. Lysine 123 acetylation is a reversible PTM that regulates the interaction, subcellular localization, folding and activity of many proteins [ 48 ]. Specific conditions, such as H 2 O 2 and superoxide concentration, appear to favor SOD activity [ 49 ].…”

Section: Discussionmentioning

confidence: 99%

Metallothionein and Superoxide Dismutase—Antioxidative Protein Status in Fullerene-Doxorubicin Delivery to MCF-7 Human Breast Cancer Cells

Kępińska

Kizek²,

Milnerowicz³

2018

IJMS

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Doxorubicin (DOX) is one of the most frequently used anticancer drugs in breast cancer treatment. However, clinical applications of DOX are restricted, largely due to the fact that its action disturbs the pro/antioxidant balance in both cancerous and non-cancerous cells. The aim of this study was to investigate the influence of fullerene (C60) in cell treatment by DOX on the proliferation of human breast cancer cells (MCF-7), concentration of metallothionein (MT) and superoxide dismutase (SOD), and SOD activity in these cells. The use of C60 in complexes with DOX causes a change in the level of cell proliferation of about 5% more than when caused by DOX alone (from 60–65% to 70%). The use of C60 as a DOX nanotransporter reduced the MT level increase induced by DOX. C60 alone caused an increase of SOD1 concentration. On the other hand, it led to a decrease of SOD activity. C60 in complex with DOX caused a decrease of the DOX-induced SOD activity level. Exposure of MCF-7 cells to DOX-C60 complexes results in a decrease in viable cells and may become a new therapeutic approach to breast cancer. The effects of C60 in complexes with DOX on MCF-7 cells included a decreased enzymatic (SOD activity) and nonenzymatic (MT) antioxidant status, thus indicating their prooxidant role in MCF-7 cells.

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Section: Discussionmentioning

confidence: 99%

Metallothionein and Superoxide Dismutase—Antioxidative Protein Status in Fullerene-Doxorubicin Delivery to MCF-7 Human Breast Cancer Cells

Kępińska

Kizek²,

Milnerowicz³

2018

IJMS

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“…Sirtuin-1 is known to act as a deacetylase for SOD1 Lys70 and restores activation by hCCS (Lin et al ., 2015). Acetylation of Lys122, on the N-terminus of the electrostatic loop, does not change SOD1 activity but is found only in specific cell types and regions within the CNS indicating functional importance (Kaliszewski et al ., 2016). Non-specific lysine acetylation of wild-type, Asp90Ala and Ala4Val SOD1 with aspirin in vitro inhibited the nucleation rate and extension of aggregates overall.…”

Section: Secondary Sod1 Post-translational Modificationsmentioning

confidence: 99%

The biophysics of superoxide dismutase-1 and amyotrophic lateral sclerosis

Wright

Antonyuk

Hasnain

2019

Quart. Rev. Biophys.

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Few proteins have come under such intense scrutiny as superoxide dismutase-1 (SOD1). For almost a century, scientists have dissected its form, function and then later its malfunction in the neurodegenerative disease amyotrophic lateral sclerosis (ALS). We now know SOD1 is a zinc and copper metalloenzyme that clears superoxide as part of our antioxidant defence and respiratory regulation systems. The possibility of reduced structural integrity was suggested by the first crystal structures of human SOD1 even before deleterious mutations in thesod1gene were linked to the ALS. This concept evolved in the intervening years as an impressive array of biophysical studies examined the characteristics of mutant SOD1 in great detail. We now recognise how ALS-related mutations perturb the SOD1 maturation processes, reduce its ability to fold and reduce its thermal stability and half-life. Mutant SOD1 is therefore predisposed to monomerisation, non-canonical self-interactions, the formation of small misfolded oligomers and ultimately accumulation in the tell-tale insoluble inclusions found within the neurons of ALS patients. We have also seen that several post-translational modifications could push wild-type SOD1 down this toxic pathway. Recently we have come to view ALS as a prion-like disease where both the symptoms, and indeed SOD1 misfolding itself, are transmitted to neighbouring cells. This raises the possibility of intervention after the initial disease presentation. Several small-molecule and biologic-based strategies have been devised which directly target the SOD1 molecule to change the behaviour thought to be responsible for ALS. Here we provide a comprehensive review of the many biophysical advances that sculpted our view of SOD1 biology and the recent work that aims to apply this knowledge for therapeutic outcomes in ALS.

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“…Figure 5B shows the increase in endogenous SOD1 succinylation at K122 in SIRT5-depleted cells. Although acetylation of K122 clearly occurs on endogenous SOD1 (21,26,28,30; also our proteomics data), our attempts to generate site-specific acetyl-K122 antibodies had only limited success: the antibodies showed marginal specificity to the acetylation. This complication, combined with the fact that K122E showed a slightly more robust effect in inhibiting the antirespiration function of SOD1 than K122Q, led us to focus primarily on K122 succinylation.…”

Section: Figmentioning

confidence: 77%

“…A study by Lin et al found that SIRT5 desuccinylates K122, and it was proposed to affect SOD1 antioxidant activity (29). In addition, a recent study using a site-specific antibody demonstrated that K122 is acetylated on endogenous SOD1 in multiple cell types throughout the murine nervous system (30), although the impact of the acetyl modification on SOD1 function was not demonstrated. With this background, we investigated the functional impact of K122 acylation on SOD1.…”

Section: Resultsmentioning

confidence: 99%

Acylation of Superoxide Dismutase 1 (SOD1) at K122 Governs SOD1-Mediated Inhibition of Mitochondrial Respiration

Banks

Rodriguez

Gashler

et al. 2017

Molecular and Cellular Biology

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In this study, we employed proteomics to identify mechanisms of posttranslational regulation on cell survival signaling proteins. We focused on Cu-Zn superoxide dismutase (SOD1), which protects cells from oxidative stress. We found that acylation of K122 on SOD1, while not impacting SOD1 catalytic activity, suppressed the ability of SOD1 to inhibit mitochondrial metabolism at respiratory complex I. We found that deacylase depletion increased K122 acylation on SOD1, which blocked the suppression of respiration in a K122-dependent manner. In addition, we found that acyl-mimicking mutations at K122 decreased SOD1 accumulation in mitochondria, initially hinting that SOD1 may inhibit respiration directly within the intermembrane space (IMS). However, surprisingly, we found that forcing the K122 acyl mutants into the mitochondria with an IMS-targeting tag did not recover their ability to suppress respiration. Moreover, we found that suppressing or boosting respiration levels toggled SOD1 in or out of the mitochondria, respectively. These findings place SOD1-mediated inhibition of respiration upstream of its mitochondrial localization. Lastly, deletion-rescue experiments show that a respiration-defective mutant of SOD1 is also impaired in its ability to rescue cells from toxicity caused by SOD1 deletion. Together, these data suggest a previously unknown interplay between SOD1 acylation, metabolic regulation, and SOD1-mediated cell survival.

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SOD1 Lysine 123 Acetylation in the Adult Central Nervous System

Cited by 10 publications

References 45 publications

Metallothionein and Superoxide Dismutase—Antioxidative Protein Status in Fullerene-Doxorubicin Delivery to MCF-7 Human Breast Cancer Cells

Metallothionein and Superoxide Dismutase—Antioxidative Protein Status in Fullerene-Doxorubicin Delivery to MCF-7 Human Breast Cancer Cells

The biophysics of superoxide dismutase-1 and amyotrophic lateral sclerosis

Acylation of Superoxide Dismutase 1 (SOD1) at K122 Governs SOD1-Mediated Inhibition of Mitochondrial Respiration

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