Subcellular localization and mitotic interactome analyses identify SIRT4 as a centrosomally localized and microtubule associated protein

Bergmann, Laura; Lang, Alexander; Bross, Christoph; Altinoluk-Hambuechen, Simone; Fey, Iris; Overbeck, Nina; Stefanski, Anja; Wiek, Constanze; Verhuelsdonk, Patrick; Mielke, Christian; Sohn, Dennis; Jänicke, Reiner U.; Scheller, Jürgen; Reichert, Andreas S.; Ahmadian, Mohammad Réza; Piekorz, Roland P.

doi:10.1101/2020.02.17.940692

Cited by 5 publications

(8 citation statements)

References 75 publications

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“…Importantly, the N-terminally truncated variant SIRT4 (ΔN28), which cannot translocate into mitochondria, delayed mitotic progression and reduced cell proliferation. Hence, SIRT4 may exert its anti-proliferative role through mitochondrial/metabolism-dependent and mitochondria-independent functions ( 30 ).…”

Section: Structure and Location Of Sirt4mentioning

confidence: 99%

Research Progress of Sirtuin4 in Cancer

et al. 2021

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Sirtuins (SIRTs) are members of the silent information regulator-2 family. They are a conserved family of nicotinamide adenine dinucleotide-dependent protein lysine deacylases. SIRTS are involved in intricate cellular processes. There are seven subtypes of SIRTs (1–7) in mammals. SIRT4 is located mainly in mitochondria and has various catalytic activities. These enzyme activities give it a diverse range of important biologic functions, such as energy metabolism, oxidative stress, and aging. Cancer is characterized as reprogramming of energy metabolism and redox imbalance, and SIRT4 can affect tumorigenesis. Here, we review the structure, localization, and enzyme activity of SIRT4 and its role in various neoplasms.

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Section: Structure and Location Of Sirt4mentioning

confidence: 99%

Research Progress of Sirtuin4 in Cancer

et al. 2021

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“…Also, NAD+ and SIRT3, a mitochondrial NAD+ dependent sirtuin, have been shown to control microtubule dynamics and reduce susceptibility to antimicrotubule agents such as vinblastine and colchicine (Harkcom et al, 2014). Additionally, SIRT4, another mitochondrial NAD+ dependent sirtuin, acts as a novel centrosomal/microtubule‐associated protein in the regulation of cell cycle progression (Bergmann et al, 2020).…”

Section: Resultsmentioning

confidence: 99%

Viewing teratogens through the lens of nicotinamide adenine dinucleotide (NAD+)

Mark

Dunwoodie

2022

Birth Defects Research

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Background Nicotinamide adenine dinucleotide (NAD+) depletion is associated with numerous diseases in humans. Recently it was revealed that genetic blockage of the NAD+ synthesis pathway in humans causes birth defects in multiple organ systems and miscarriage. Additionally, mice with NAD+ deficiency created through dietary restriction of tryptophan and vitamin B3 were shown to have congenital anomalies affecting virtually every organ system along with miscarriage. Perturbations in NAD+/NADH affect mechanisms of teratogenesis presented by Wilson and others, including genetic alterations, altered energy sources, and lack of precursors and substrates needed for biosynthesis. Methods Medical literature was evaluated to demonstrate how perturbations in NAD+/NADH affect mechanisms of teratogenesis. In addition, literature describing several different teratogens of various types (infectious, physical, maternal health factors, drugs) was reviewed showing the impact of these teratogens on NAD+ and NAD+/NADH ratios. Result Many teratogens affect NAD+ by altering its metabolism, decreasing its intracellular availability, or decreasing its production, which in turn is a plausible mechanism for the creation of birth defects. Conclusion Looking at teratogens through the lens of their impact on NAD+ could provide valuable insight into the mechanism by which some teratogens cause birth defects and miscarriage.

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“…The beads were mixed with Laemmli loading buffer and co-immunoprecipitation of SIRT4-Flag and endogenous C-RAF proteins was analyzed by SDS-PAGE and immunoblotting. Co-immunoprecipitation of SIRT4-eGFP and endogenous C-RAF using the anti-eGFP nanobody protocol was performed essentially as previously described (33).…”

Section: Co-immunoprecipitation Analysismentioning

confidence: 99%

“…In particular, SIRT4 inhibits, as a tumor suppressor, the metabolic gate-keepers pyruvate dehydrogenase (PDH) and glutamate dehydrogenase (GDH) (31,32), with particular significance for the regulation of glutamine metabolism in tumor cells. Recent findings uncovered novel extra-mitochondrial roles of SIRT4 in microtubule dynamics and regulation of mitotic cell cycle progression, WNT/-Catenin and Hippo signaling, and SNARE complex formation required for autophagosome-lysosome fusion (33)(34)(35)(36). Interestingly, proteomic analysis of the SIRT4 interactome identified C-RAF as a potential binding partner of SIRT4, indicating a novel role of SIRT4 in the regulation of the RAF-MAPK signaling pathway (33).…”

Section: Introductionmentioning

confidence: 99%

“…Recent findings uncovered novel extra-mitochondrial roles of SIRT4 in microtubule dynamics and regulation of mitotic cell cycle progression, WNT/-Catenin and Hippo signaling, and SNARE complex formation required for autophagosome-lysosome fusion (33)(34)(35)(36). Interestingly, proteomic analysis of the SIRT4 interactome identified C-RAF as a potential binding partner of SIRT4, indicating a novel role of SIRT4 in the regulation of the RAF-MAPK signaling pathway (33). Consistent with this idea, recent studies have demonstrated that (i) the tumor suppressor SIRT4 is downregulated in most human solid tumor types and cell lines (37)(38)(39), and (ii) ectopic expression of SIRT4 downregulates pERK1/2 levels and hence inhibits MAPK signaling and cell proliferation (37)(38)(39)(40)(41)(42).…”

Section: Introductionmentioning

confidence: 99%

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Identification of SIRT4 as a novel paralog-specific interactor and candidate suppressor of C-RAF kinase in MAPK signaling

Mehrabipour,

Dvorsky,

Nakhaei-Rad

et al. 2023

Preprint

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Cellular responses leading to development, proliferation, and differentiation rely on RAF/MEK/ERK signaling that integrates and amplifies signals from various stimuli to cellular downstream responses. The clinical significance of C-RAF activation has been reported in many types of tumor cell proliferation and developmental disorders, which requires the discovery of potential C-RAF protein regulators. Here, we identify a novel and specific protein interaction between C-RAF, among the RAF kinase paralogs, and SIRT4 among the mitochondrial sirtuin family members SIRT3, SIRT4, and SIRT5. Structurally, C-RAF binds to SIRT4 through the N-terminal cysteine-rich domain (CRD; a.a. 136-187), and on the other side, SIRT4 requires predominantly the C-terminus (a.a. 255-314) for full interaction with C-RAF. Interestingly, SIRT4 interacts specifically with C-RAF in a pre-signaling inactive (serine 259 phosphorylated) state. Consistent with this finding, ectopic expression of SIRT4 in HEK293 cells results in upregulation of pS259-C-RAF levels and concomitant reduction of MAPK signaling as evidenced by strongly decreased phospho-ERK signals. Thus, our findings propose another extra-mitochondrial role of SIRT4 and suggest that SIRT4 functions as a cytosolic tumor suppressor of C-RAF-MAPK signaling, besides its known metabolic tumor suppressor role towards glutamate dehydrogenase and glutamine levels in mitochondria.

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Subcellular localization and mitotic interactome analyses identify SIRT4 as a centrosomally localized and microtubule associated protein

Cited by 5 publications

References 75 publications

Research Progress of Sirtuin4 in Cancer

Research Progress of Sirtuin4 in Cancer

Viewing teratogens through the lens of nicotinamide adenine dinucleotide (NAD+)

Identification of SIRT4 as a novel paralog-specific interactor and candidate suppressor of C-RAF kinase in MAPK signaling

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