The small molecule AUTEN-99 (autophagy enhancer-99) prevents the progression of neurodegenerative symptoms

Kovács, Tibor; Billes, Viktor; Komlós, Marcell; Hotzi, Bernadette; Manzéger, Anna; Tarnóci, Anna; Papp, Diána; Szikszai, Fanni; Szinyákovics, Janka; Rácz, Anita; Noszál, Béla; Veszelka, Szilvia; Walter, Fruzsina R.; Deli, Mária A.; Hackler, László; Alföldi, Róbert; Huzián, Orsolya; Puskás, László G.; Liliom, Hanna; Tárnok, Krisztián; Schlett, Katalin; Borsy, Adrienn; Welker, Ervin; Kovács, Attila; Pádár, Zsolt; Erdős, Attila; Legradi, Adam; Bjelik, Annamária; Gulya, Károly; Gulyás, Balázs; Vellai, Tibor

doi:10.1038/srep42014

Cited by 45 publications

(56 citation statements)

References 61 publications

Supporting

Mentioning

Contrasting

Unclassified

Order By: Relevance

“…Other studies show an important role for MTMRs in autophagy‐dependent clearance of dysfunctional proteins, making them attractive targets for neurodegenerative disorders such as Alzheimer’s, Parkinson’s, and Huntington’s disease. For instance, inhibiting MTMR14/Jumpy using the small molecules such as autophagy enhancer 67 and autophagy enhancer 99 restores autophagic flux and reduces symptoms in Drosophila models for Parkinson’s and Huntington’s diseases (Table ).…”

Section: Understanding the Phosphoinositides Function In The Pathophymentioning

confidence: 99%

Phosphoinositides in autophagy: current roles and future insights

2019

View full text Add to dashboard Cite

Today, the importance of autophagy in physiological processes and pathological conditions is undeniable. Initially, autophagy merely was described as an evolutionarily conserved mechanism to maintain metabolic homeostasis in times of starvation; however, in recent years it is now apparent that autophagy is a powerful regulator of many facets of cellular metabolism, that its deregulation contributes to various human pathologies, including cancer and neurodegeneration, and that its modulation has considerable potential as a therapeutic approach. Different lipid species, including sphingolipids, sterols, and phospholipids, play important roles in the various steps of autophagy. In particular, there is accumulating evidence indicating the minor group of phospholipids called the phosphoinositides as key modulators of autophagy, including the signaling processes underlying autophagy initiation, autophagosome biogenesis and maturation. In this review, we discuss the known functions to date of the phosphoinositides in autophagy and attempt to summarize the kinases and phosphatases that regulate them as well as the proteins that bind to them throughout the autophagy program. We will also provide examples of how the control of phosphoinositides and their metabolizing enzymes is relevant to understanding many human diseases.Abbreviations ALR, autophagic lysosome reformation; CMT4J, Charcot-Marie-Tooth type 4J; ESI, electron spray ionization; FYCO1, FYVE and coiled-coiled domain-containing 1; GABARAP, gamma-aminobutyric acid receptor-associated protein; HOPS, homotypic fusion and protein sorting; HPLC, high performance liquid chromatography; KO, knockout; MS, mass spectrometry; MS/MS, tandem mass spectrometry; MTM1, Myotubular myopathy 1; MTMRs, myotubularin family of phosphatases; mTORC1, mammalian target of rapamycin complex 1; OCRL, OculoCerebroRenal of Lowe; PDK1, phosphoinositide-dependent kinase-1; PH, pleckstrin homology; PI, phosphatidylinositol; PI-3,5-P 2 , phosphatidylinositol 3,5-bisphosphate; PI-3-P, phosphatidylinositol 3-monophosphate; PI-4,5-P 2 , phosphatidylinositol 4,5-bisphosphate; PI4P5K, phosphatidylinositol-4-phosphate 5-kinase; PI-5-P, phosphatidylinositol 5-monophosphate; PI5P4K, phosphatidylinositol-5-phosphate 4-kinase; PLCd1-PH, PH domain of phospholipase C d1; PLEKHM1, pleckstrin homology domain-containing protein family member 1; PM, plasma membrane; SynJ1, synaptojanin 1; TFEB, transcription factor EB; WIPI, WD-repeat protein interacting with phosphoinositides.

show abstract

Section: Understanding the Phosphoinositides Function In The Pathophymentioning

confidence: 99%

Phosphoinositides in autophagy: current roles and future insights

2019

View full text Add to dashboard Cite

show abstract

“…These observations suggest a role for EDTP in the regulation of autophagy. This is indeed supported by the findings that PtdIns3P stimulates autophagy in human HT-29 cells [10], that MTMR14 negatively controls the autophagosome formation and maturation in mammalian cells [11], and that the EDTP/MTMR14 inhibitor, AUTEN-99, activates autophagy in human HeLa cells and mouse tissues [12]. Interestingly, the latter group also shows that overexpression of a modified EDTP (by skipping the first exon) in the fat body antagonizes the effect of AUTEN-67 in inducing autophagy [13].…”

Section: Introductionmentioning

confidence: 55%

“…EDTP/MTMR14 has two main functions: negative regulation of autophagy and disease-causing effect if deficient in the muscles [1,[11][12][13][14][15]. Drosophila EDTP has two peaks of expression, one Motoneurons are highly specialized and terminally differentiated with reduced function of global genome repair [32,33].…”

Section: Discussionmentioning

confidence: 99%

Drosophilaegg-derived tyrosine phosphatase (EDTP): a novel target for improved survivorship to prolonged anoxia and cellular protein aggregates

Xiao

Qiu

et al. 2018

Preprint

View full text Add to dashboard Cite

Drosophila egg-derived tyrosine phosphatase (EDTP), a lipid phosphatase that removes 3position phosphate at the inositol ring, has dual functions in the oogenesis and the muscle performance during adult stages. A mammalian homologous gene MTMR14, which encodes the myotubularin-related protein 14, negatively regulates autophagy. Mutation of EDTP/MTMR14, however, causes at least three deleterious consequences: (1) lethality in the early embryogenesis in Drosophila; (2) "jumpy" phenotype with apparently impaired motor functions; and (3) association with a rare genetic disorder called centronuclear myopathy. Here we show that flies carrying a heterozygous EDTP mutation had increased survivorship to prolonged anoxia; tissuespecific downregulation of EDTP in non-muscle tissues, particularly motoneurons, extended the lifespan; and tissue-specific downregulation of EDTP in motoneurons improved the survivorship to beta-amyloid peptides (Aβ42) and polyglutamine (polyQ) protein aggregates. MTMR14 expression was evident in the hippocampus and cortex in C57BL/6J and APP/PS1 mice.Compared with C57BL/6J mice, APP/PS1 mice had reduced MTMR14 in the cortex but not in the hippocampus. Hippocampal expression of MTMR14 was increased and plateaued at 9-17 months compared with 2-6 months in C57BL/6J mice. Aβ42 treatment increased the expression of MTMR14 in the primarily cultured hippocampal neurons of Sprague/Dawley rats and mouse Neuro2a neuroblasts. We demonstrated a novel approach of tissue-specific manipulation of the disease-associated gene EDTP/MTMR14 for lifespan extension and the improvement of survivorship to cellular protein aggregates.

show abstract

“…This observation suggests a role for EDTP in the regulation of autophagy. This is indeed supported by the findings that PtdIns3P stimulates autophagy in human HT-29 cells 9 , that mJUMPY negatively controls autophagosome formation and maturation in mammalian cells 10 , and that EDTP/JUMPY inhibitors, AUTEN-67 and AUTEN-99, activate autophagy in human cell lines and mouse tissues 11,12 .…”

Section: Introductionmentioning

confidence: 62%

Tissue-specific downregulation ofEDTPsuppresses polyglutamine protein aggregates and extends lifespan inDrosophila

Xiao

Qiu

Robertson

et al. 2017

Preprint

View full text Add to dashboard Cite

Drosophila egg-derived tyrosine phosphatase (EDTP, also called JUMPY) is a lipid phosphatase essential in oogenesis and muscle function in the adult stage. Although mammalian JUMPY negatively regulates autophagy, loss-of-JUMPY causes muscle dysfunction and is associated with a rare genetic disorder called centronuclear myopathy. Here we show that tissue-specific downregulation of EDTP in Drosophila non-muscle tissues, particularly glial cells, suppresses the expression of polyglutamine (polyQ) protein aggregates in the same cells and improves survival. Additionally, tissue-specific downregulation of EDTP in glial cells or motoneurons extends lifespan. We demonstrate an approach to fine-tune the expression of a disease-associated gene EDTP for the removal of polyQ protein aggregate and lifespan extension in Drosophila.

show abstract

The small molecule AUTEN-99 (autophagy enhancer-99) prevents the progression of neurodegenerative symptoms

Cited by 45 publications

References 61 publications

Phosphoinositides in autophagy: current roles and future insights

Phosphoinositides in autophagy: current roles and future insights

Drosophilaegg-derived tyrosine phosphatase (EDTP): a novel target for improved survivorship to prolonged anoxia and cellular protein aggregates

Tissue-specific downregulation ofEDTPsuppresses polyglutamine protein aggregates and extends lifespan inDrosophila

Contact Info

Product

Resources

About