Drosophila NUAK functions with Starvin/BAG3 in autophagic protein turnover

Brooks, David; Naeem, Fawwaz; Stetsiv, Marta; Goetting, Samantha C.; Bawa, Simranjot; Green, Nicole M.; Clark, Cheryl; Bashirullah, Arash; Geisbrecht, Erika R.

doi:10.1371/journal.pgen.1008700

Cited by 22 publications

(28 citation statements)

References 84 publications

(133 reference statements)

Supporting

Mentioning

Contrasting

Order By: Relevance

“…In Drosophila, the serine/threonine kinase NUAK interacts with Starvin, the fly orthologue of BAG3 (Brooks et al , 2020 ). Starvin and NUAK mutant flies exhibit muscle degeneration and muscle contraction defects, and similar phenotypes are also observed following a depletion of Drosophila HSC70 and the autophagic membrane marker ATG8 (Arndt et al , 2010 ; Brooks et al , 2020 ). Moreover, muscle degeneration is accompanied by the accumulation of protein aggregates that contain filamin.…”

Section: Mechanical Stress Signallingmentioning

confidence: 99%

Maintaining proteostasis under mechanical stress

et al. 2021

View full text Add to dashboard Cite

Cell survival, tissue integrity and organismal health depend on the ability to maintain functional protein networks even under conditions that threaten protein integrity. Protection against such stress conditions involves the adaptation of folding and degradation machineries, which help to preserve the protein network by facilitating the refolding or disposal of damaged proteins. In multicellular organisms, cells are permanently exposed to stress resulting from mechanical forces. Yet, for long time mechanical stress was not recognized as a primary stressor that perturbs protein structure and threatens proteome integrity. The identification and characterization of protein folding and degradation systems, which handle force‐unfolded proteins, marks a turning point in this regard. It has become apparent that mechanical stress protection operates during cell differentiation, adhesion and migration and is essential for maintaining tissues such as skeletal muscle, heart and kidney as well as the immune system. Here, we provide an overview of recent advances in our understanding of mechanical stress protection.

show abstract

Section: Mechanical Stress Signallingmentioning

confidence: 99%

Maintaining proteostasis under mechanical stress

et al. 2021

View full text Add to dashboard Cite

show abstract

“…in Drosophila S2 cell culture and eye tissue, which consists mostly of photoreceptor neurons (Carra et al, 2010). Several studies on stv have focused on embryonic and larval muscle (Brooks et al, 2020;Coulson et al, 2005) and stv colocalizes with HspB8/Hsp67Bc in the larval muscle (Carra et al, 2010). However, in the adult flight muscle stv has only been characterized by an interaction with a CASA complex including HspB8/CG14207 (Arndt et al, 2010).…”

Section: Discussionmentioning

confidence: 99%

“…In adult Drosophila muscle, the CASA complex has been reported to consist of the Hsp70 homologue Hsc70-4, the HspB8 homologue CG14207 and the BAG-3 homologue starvin (stv) (Arndt et al, 2010). stv is a nucleotide exchange factor that binds to both Hsp70 and HspB8 as well as a variety of target proteins that need refolding (Brooks et al, 2020;Carra et al, 2008;Doong et al, 2002;Gamerdinger et al, 2011;Guilbert et al, 2018;Gupta et al, 2019;Ulbricht et al, 2013). As stv has been shown to be required for muscle functions (Arndt et al, 2010;Brooks et al, 2020;Coulson et al, 2005), we tested if p38Kb and stv colocalizes and find that they colocalize at both the Z-disk and M-line (Figure 3a,b).…”

Section: P38kb Colocalizes and Physically Interacts With Starvin In The Adult Flight Musclementioning

confidence: 99%

“…stv is a nucleotide exchange factor that binds to both Hsp70 and HspB8 as well as a variety of target proteins that need refolding (Brooks et al, 2020;Carra et al, 2008;Doong et al, 2002;Gamerdinger et al, 2011;Guilbert et al, 2018;Gupta et al, 2019;Ulbricht et al, 2013). As stv has been shown to be required for muscle functions (Arndt et al, 2010;Brooks et al, 2020;Coulson et al, 2005), we tested if p38Kb and stv colocalizes and find that they colocalize at both the Z-disk and M-line (Figure 3a,b). We next tested if p38Kb physically interacts with stv in the adult muscle.…”

Section: P38kb Colocalizes and Physically Interacts With Starvin In The Adult Flight Musclementioning

confidence: 99%

“…Those substrates that cannot be refolded by the complex are poly-ubiquitinated and targeted to the autophagosome through a handover between BAG-3/stv and the autophagy adaptor protein p62 (ref(2)p in flies), and subsequently degraded through the autophagosome-lysosome system (Behl, 2011;Carra et al, 2008;Gamerdinger et al, 2009;Kettern et al, 2010;Min et al, 2008;Selcen et al, 2009;Terman et al, 2007). Furthermore, stv has been shown to play a role in regulating protein homeostasis in fly muscle (Arndt et al, 2010;Brooks et al, 2020).…”

mentioning

confidence: 99%

See 2 more Smart Citations

Drosophila p38 MAPK interacts with BAG‐3/starvin to regulate age‐dependent protein homeostasis

et al. 2021

View full text Add to dashboard Cite

Protein turnover is critical for maintaining tissue health as many proteins become damaged or misfolded during normal tissue functions. Therefore, the cell utilizes a variety of protein quality control mechanisms to refold or degrade these damaged proteins, including the ubiquitin proteasome system and autophagy. During aging, protein quality control mechanisms become less efficient leading to the accumulation of damaged or misfolded proteins that begin to form protein aggregates (Taylor & Dillin, 2011). It has been hypothesized that these aggregates are toxic and may lead to the deleterious phenotypes associated with normal aging, such as impaired tissue function (Taylor & Dillin, 2011). Furthermore, decreased protein aggregation has been associated with longevity. For example, over-expression of Foxo leads to an increased lifespan but also a concordant decrease in protein aggregation in C. elegans, Drosophila, and mice (Ben-Zvi et al.,

show abstract

UNC‐82/NUAK kinase is required by myosin A, but not myosin B, to assemble and function in the thick filament arms of C. elegans striated muscle

Schiller,

Almuhanna,

Hoppe

2023

Cytoskeleton

View full text Add to dashboard Cite

The mechanisms that ensure proper assembly, activity, and turnover of myosin II filaments are fundamental to a diverse range of cellular processes. In Caenorhabditis elegans striated muscle, thick filaments contain two myosins that are functionally distinct and spatially segregated. Using transgenic double mutants, we demonstrate that the ability of increased myosin A expression to restore muscle structure and movement in myosin B mutants requires UNC‐82/NUAK kinase activity. Myosin B function appears unaffected in the kinase‐impaired unc‐82(e1220) mutant: the recessive antimorphic effects on early assembly of paramyosin and myosin A in this mutant are counteracted by increased myosin B expression and exacerbated by loss of myosin B. Using chimeric myosins and motility assays, we mapped the region of myosin A that requires UNC‐82 activity to a 531‐amino‐acid region of the coiled‐coil rod. This region includes the 264‐amino‐acid Region 1, which is sufficient in chimeric myosins to rescue the essential filament‐initiation function of myosin A, as well as two sites that interact with myosin head domains in the Interacting Heads Motif. A specific physical interaction between myosin A and UNC‐82::GFP is supported by GFP labeling of ectopic myosin A filaments but not thin filaments. We hypothesize that UNC‐82 regulates assembly competence of myosin A during parallel assembly in the filament arms.

show abstract

Drosophila NUAK functions with Starvin/BAG3 in autophagic protein turnover

Cited by 22 publications

References 84 publications

Maintaining proteostasis under mechanical stress

Maintaining proteostasis under mechanical stress

Drosophila p38 MAPK interacts with BAG‐3/starvin to regulate age‐dependent protein homeostasis

UNC‐82/NUAK kinase is required by myosin A, but not myosin B, to assemble and function in the thick filament arms of C. elegans striated muscle

Contact Info

Product

Resources

About