p62/SQSTM1 at the interface of aging, autophagy, and disease

Bitto, Alessandro; Lerner, Chad; Nacarelli, Timothy; Crowe, Elizabeth; Torres, Claudio; Sell, Christian

doi:10.1007/s11357-014-9626-3

Cited by 124 publications

(94 citation statements)

References 150 publications

(225 reference statements)

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“…In addition, several studies have identified changes with age in signaling pathways (i.e. mTOR, SIRT, FOXO) that could contribute to reduced induction of autophagy and autophagosome formation (Bitto et al., 2014; Park et al., 2016; Perluigi, Di Domenico & Butterfield, 2015; Schiavi & Ventura, 2014). Future analysis will be required to explore the molecular requirements that determine the recruitment of motor proteins to AVs and LYS and the potential impact in this process of age‐associated changes in these signaling routes.…”

Section: Discussionmentioning

confidence: 99%

Defective recruitment of motor proteins to autophagic compartments contributes to autophagic failure in aging

et al. 2018

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SummaryInability to preserve proteostasis with age contributes to the gradual loss of function that characterizes old organisms. Defective autophagy, a component of the proteostasis network for delivery and degradation of intracellular materials in lysosomes, has been described in multiple old organisms, while a robust autophagy response has been linked to longevity. The molecular mechanisms responsible for defective autophagic function with age remain, for the most part, poorly characterized. In this work, we have identified differences between young and old cells in the intracellular trafficking of the vesicular compartments that participate in autophagy. Failure to reposition autophagosomes and lysosomes toward the perinuclear region with age reduces the efficiency of their fusion and the subsequent degradation of the sequestered cargo. Hepatocytes from old mice display lower association of two microtubule‐based minus‐end‐directed motor proteins, the well‐characterized dynein, and the less‐studied KIFC3, with autophagosomes and lysosomes, respectively. Using genetic approaches to mimic the lower levels of KIFC3 observed in old cells, we confirmed that reduced content of this motor protein in fibroblasts leads to failed lysosomal repositioning and diminished autophagic flux. Our study connects defects in intracellular trafficking with insufficient autophagy in old organisms and identifies motor proteins as a novel target for future interventions aiming at correcting autophagic activity with anti‐aging purposes.

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Section: Discussionmentioning

confidence: 99%

Defective recruitment of motor proteins to autophagic compartments contributes to autophagic failure in aging

et al. 2018

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“…This may be due to MeHg-induced inhibition of p62 by lysosomal disruption (Daré et al, 2001; Tofighi et al 2011). p62 has multiple domains to regulate cellular events (Bitto et al, 2014; Wang et al 2014), and may trigger nuclear factor-κB (NF-κB) activity to promote cell survival responses (Chen et al 2014). Thus, the significance of enhanced p62 protein by MeHg needs further study.…”

Section: Discussionmentioning

confidence: 99%

Role of autophagy in methylmercury-induced neurotoxicity in rat primary astrocytes

et al. 2014

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Autophagy is an evolutionarily conserved process in which cytoplasmic proteins and organelles are degraded and recycled for reuse. There are numerous reports on the role of autophagy in cell growth and death; however, the role of autophagy in methylmercury (MeHg)-induced neurotoxicity has yet to be identified. We studied the role of autophagy in MeHg-induced neurotoxicity in astrocytes. MeHg reduced astrocytic viability in a concentration- and time-dependent manner, and induced apoptosis. Pharmacological inhibition of autophagy with 3-methyladenine (3-MA) or chloroquine (CQ), as well as the silencing of the autophagy-related protein 5 (Atg5), increased MeHg-induced cytotoxicity and the ratio of apoptotic astrocytes. Conversely, Rapamycin, an autophagy inducer, along with as N-acetyl-L-cysteine (NAC), a precursor of reduced glutathione (GSH), decreased MeHg-induced toxicity and the ratio of apoptotic astrocytes. These results indicated that MeHg-induced neurotoxicity was reduced, at least in part, through the activation of autophagy. Accordingly, modulation of autophagy may offer a new avenue for attenuating MeHg-induced neurotoxicity.

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“…As p62 appears to play an important role in maintaining mitochondrial quality control through mitophagy, it is possible that the loss of p62 in pancreatic β cells may cause mitochondrial dysfunction and thus result in impaired glucose tolerance [5]. Normal β-cell function and mass in β-cell-specific p62-deficient mice suggested redundant autophagy receptors; for instance, NBR1, which shares similar functional domains with p62, may have a compensatory role in mitophagy when p62 is deficient [26].…”

Section: Discussionmentioning

confidence: 99%

“…Therefore, elucidating the molecular mechanisms underlying pancreatic β-cell dysfunction is a key to understanding the pathology of diabetes [3,4]. Sequestosome 1 (SQSTM1, referred to hereafter as p62) is a multifunctional scaffold protein that can interact with several signaling pathways through its functional subdomains, including the Phox and Bem1 (PB1) domain, zinc-finger domain, TNF receptor-associated factor 6 (TRAF6)-binding domain, and Kelch-like ECHassociated protein 1 (Keap1) interacting region (KIR) [5][6][7]. p62/SQSTM1 can activate the antioxidant response by interacting with the Keap1-Nrf2 pathway [8][9][10].…”

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confidence: 99%

“…p62 -/-mice have a reduced lifespan and show premature aging phenotypes with increased mitochondrial damage and dysfunction [21]. Given the importance of p62 in maintaining mitochondrial homeostasis through the autophagic degradation of damaged mitochondria, or so called mitophagy, it is possible that loss of p62 in pancreatic β cells contributes to mitochondrial dysfunction and thereby reduces insulin release, resulting in impaired glucose tolerance [5]. On the other hand, a recent study reported that in contrast to what has been reported for ubiquitin-induced pexophagy and xenophagy, p62 appears to be dispensable for mitophagy [22].…”

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confidence: 99%

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Normal pancreatic β-cell function in mice with <i>RIP-Cre</i>-mediated inactivation of p62/SQSTM1

et al. 2018

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Abstract. Recent studies have suggested that decreased pancreatic β-cell function and mass are common features of patients with type 2 diabetes mellitus. Pancreatic β-cell homeostasis is regulated by various types of signaling molecules and stress responses. Sequestosome 1/p62 (SQSTM1, hereafter referred to as p62) is a ubiquitin-binding adaptor protein involved in cell signaling, oxidative stress, and autophagy. Because p62 appears to play an important role in maintaining mitochondrial quality control, it is possible that the loss of p62 in pancreatic β cells contributes to mitochondrial dysfunction, and thus leading to impaired glucose tolerance. In this study we investigated the physiological roles of p62 by inactivating p62 in a β-cell specific manner. We found that firstly, rat insulin-2 promoter-Cre (RIP-Cre)-mediated p62 inactivation did not cause body weight gain, although ubiquitous inactivation of p62 was previously shown to result in severe obesity. Secondly, we found no gross structural disorganization of the islets of p62-deficient mice. Consistent with normal islet morphology, no impairment in glucose tolerance was observed in mice with RIP-Cre-mediated p62 deletion. These results suggest that p62 is dispensable for normal islet organization and β-cell function.Key words: Islets, β cell, Diabetes, p62, Sequestosome 1 TYPE 2 DIABETES MELLITUS is a metabolic disorder characterized by hyperglycemia resulting from the complex interplay of multiple genetic and environmental factors, resulting in both decreased insulin action on target tissues and defective pancreatic β-cell insulin secretion in response to glucose [1]. The natural history of diabetes is strongly associated with the disability of pan-

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p62/SQSTM1 at the interface of aging, autophagy, and disease

Cited by 124 publications

References 150 publications

Defective recruitment of motor proteins to autophagic compartments contributes to autophagic failure in aging

Defective recruitment of motor proteins to autophagic compartments contributes to autophagic failure in aging

Role of autophagy in methylmercury-induced neurotoxicity in rat primary astrocytes

Normal pancreatic β-cell function in mice with <i>RIP-Cre</i>-mediated inactivation of p62/SQSTM1

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