Gene transfer of master autophagy regulator TFEB results in clearance of toxic protein and correction of hepatic disease in alpha‐1‐anti‐trypsin deficiency

Pastore, Nunzia; Blomenkamp, Keith; Annunziata, Fabio; Piccolo, Pasquale; Mithbaokar, Pratibha; Sepe, Rosa Maria; Vetrini, Francesco; Palmer, D. Jason; Ng, Philip; Polishchuk, Elena; Iacobacci, Simona; Polishchuk, Roman; Teckman, Jeffrey; Ballabio, Andrea; Brunetti‐Pierri, Nicola

doi:10.1002/emmm.201202046

Cited by 134 publications

(116 citation statements)

References 67 publications

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“…TFEB overexpression has also shown therapeutic effects in mouse models of α1-antitrypsin deficiency, the most common genetic cause of liver disease (Pastore et al, 2013). In this case as well, enhanced intracellular clearance represents the major therapeutic mechanism, as induction of autophagy by TFEB reduces the levels of α1-antitrypsin accumulation and ameliorates liver injury.…”

Section: Tfeb As a Therapeutic Target For Diseasesmentioning

confidence: 99%

TFEB at a glance

Napolitano

Ballabio

2016

Journal of Cell Science

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The transcription factor EB (TFEB) plays a pivotal role in the regulation of basic cellular processes, such as lysosomal biogenesis and autophagy. The subcellular localization and activity of TFEB are regulated by mechanistic target of rapamycin (mTOR)-mediated phosphorylation, which occurs at the lysosomal surface. Phosphorylated TFEB is retained in the cytoplasm, whereas dephosphorylated TFEB translocates to the nucleus to induce the transcription of target genes. Thus, a lysosome-to-nucleus signaling pathway regulates cellular energy metabolism through TFEB. Recently, in vivo studies have revealed that TFEB is also involved in physiological processes, such as lipid catabolism. TFEB has attracted a lot of attention owing to its ability to induce the intracellular clearance of pathogenic factors in a variety of murine models of disease, such as Parkinson's and Alzheimer's, suggesting that novel therapeutic strategies could be based on the modulation of TFEB activity. In this Cell Science at a Glance article and accompanying poster, we present an overview of the latest research on TFEB function and its implication in human diseases.

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Section: Tfeb As a Therapeutic Target For Diseasesmentioning

confidence: 99%

TFEB at a glance

Napolitano

Ballabio

2016

Journal of Cell Science

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608

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“…For instance, overexpression of TFEB rescues toxicity of α-synuclein and protects dopaminergic neurons in a rat model of Parkinson's disease that is induced by viral overexpression of α-synuclein (Decressac et al, 2013); it also ameliorates toxicity by enhancing the clearance of misfolded polyglutamine-expanded ( polyQ) huntingtin protein (Tsunemi et al, 2012) and the mutant androgen receptor that causes X-linked spinal and bulbar muscular atrophy (Cortes et al, 2014). Gene transfer of TFEB alleviates pathology in a mouse model of alpha-1-anti-trypsin deficiency (Pastore et al, 2013). Moreover, activation of autophagy and lysosomal activity by TFEB attenuates the pathological phenotype in mouse models of Pompe disease (Spampanato et al, 2013).…”

Section: Tfeb and Zkscan3 -The Master Autophagy Regulatorsmentioning

confidence: 99%

Transcriptional regulation of mammalian autophagy at a glance

Füllgrabe

Ghislat

Cho

et al. 2016

Journal of Cell Science

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Macroautophagy, hereafter referred to as autophagy, is a catabolic process that results in the lysosomal degradation of cytoplasmic contents ranging from abnormal proteins to damaged cell organelles. It is activated under diverse conditions, including nutrient deprivation and hypoxia. During autophagy, members of the core autophagy-related (ATG) family of proteins mediate membrane rearrangements, which lead to the engulfment and degradation of cytoplasmic cargo. Recently, the nuclear regulation of autophagy, especially by transcription factors and histone modifiers, has gained increased attention. These factors are not only involved in rapid responses to autophagic stimuli, but also regulate the long-term outcome of autophagy. Now there are more than 20 transcription factors that have been shown to be linked to the autophagic process. However, their interplay and timing appear enigmatic as several have been individually shown to act as major regulators of autophagy. This Cell Science at a Glance article and the accompanying poster highlights the main cellular regulators of transcription involved in mammalian autophagy and their target genes.

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“…9 The problem of applying gene therapy to treat diseases associated with protein misfolding and aggregation has now been addressed, in part, by a study concerning liver disease. 10 Andrea Ballabio and colleagues previously described the coordinated lysosomal expression and regulation (CLEAR) network, 11 which is controlled through the transcription factor TFEB, and demonstrated that it regulates macroautophagy in an MTOR-dependent manner. [12][13][14] The possibility of manipulating TFEB to treat a disease by upregulating macroautophagy was seen with the finding that overexpression of TFEB, or its upstream regulator PPARGC1A/ PGC-1α, rescues the neurodegenerative effects resulting from HTT toxicity.…”

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confidence: 99%

“…15 Now, a paper from Nicola BrunettiPierri and colleagues has advanced this knowledge by using TFEB-based gene therapy to treat a mouse model of α 1 -antitrypsin deficiency. 10 In this disease, a mutant form of SERPINA1/A1AT accumulates in particular in liver cells, the site of its synthesis, and can lead to cirrhosis. In addition, a deficiency of SERPIN1A in the lungs can lead to emphysema.…”

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confidence: 99%

“…16,17 Of course, there are problems associated with the long-term use of systemic drugs. Hence, this is one reason why the study by Pastore et al 10,18 holds great promise. In this case, the authors relied on overexpression of liver-directed TFEB to upregulate macroautophagy and promote clearance of the altered SERPIN1A protein, suppressing the disease phenotype.…”

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confidence: 99%

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