Your search keyword '"Herrero, Melisa"' showing total 7 results

1. Blunted Cardiac Mitophagy in Response to Metabolic Stress Contributes to HFpEF.

Author

Yoshii, Akira, McMillen, Timothy S., Wang, Yajun, Zhou, Bo, Chen, Hongye, Banerjee, Durba, Herrero, Melisa, Wang, Pei, Muraoka, Naoto, Wang, Wang, Murry, Charles E., and Tian, Rong

Published

2024

2. Effective extraction of polyribosomes exposes gene expression strategies in primary astrocytes.

Author

Mandelboum, Shir, Herrero, Melisa, Atzmon, Andrea, Ehrlich, Marcelo, and Elroy-Stein, Orna

Published

2023

3. Oligodendrocytes depend on MCL-1 to prevent spontaneous apoptosis and white matter degeneration.

Author

Cleveland, Abigail H., Romero-Morales, Alejandra, Azcona, Laurent Alfonso, Herrero, Melisa, Nikolova, Viktoriya D., Moy, Sheryl, Elroy-Stein, Orna, Gama, Vivian, and Gershon, Timothy R.

Published

2021

4. eIF2B Mutations Cause Mitochondrial Malfunction in Oligodendrocytes.

Author

Herrero, Melisa, Mandelboum, Shir, and Elroy-Stein, Orna

Abstract

Vanishing white matter (VWM) disease (OMIM#306896) is an autosomal recessive neurodegenerative leukodystrophy caused by hypomorphic mutations in any of the five genes encoding the subunits of eukaryotic translation initiation factor 2B (eIF2B). The disease is manifested by loss of cerebral white matter and progressive deterioration upon exposure to environmental and physiological stressors. "Foamy" oligodendrocytes (OLG), increased numbers of oligodendrocytes precursor cells (OPC), and immature defective astrocytes are major neuropathological denominators. Our recent work using Eif2b5R132H/R132H mice uncovered a fundamental link between eIF2B and mitochondrial function. A decrease in oxidative phosphorylation capacity was observed in mutant astrocytes and fibroblasts. While an adaptive increase in mitochondria abundance corrects the phenotype of mutant fibroblasts, it is not sufficient to compensate for the high-energy demand of astrocytes, explaining their involvement in the disease. To date, astrocytes are marked as central for the disease while eIF2B-mutant OLG are currently assumed to lack a cellular phenotype on their own. Here we show a reduced capacity of eIF2B-mutant OPC isolated from Eif2b5R132H/R132H mice to conduct oxidative respiration despite the adaptive increase in their mitochondrial abundance. We also show their impaired ability to efficiently complete critical differentiation steps towards mature OLG. The concept that defective differentiation of eIF2B-mutant OPC could be a consequence of mitochondrial malfunction is in agreement with numerous studies indicating high dependency of differentiating OLG on accurate mitochondrial performance and ATP availability. [ABSTRACT FROM AUTHOR]

Published

2019

5. Drug Screening Identifies Sigma-1-Receptor as a Target for the Therapy of VWM Leukodystrophy.

Author

Atzmon, Andrea, Herrero, Melisa, Sharet-Eshed, Reut, Gilad, Yocheved, Senderowitz, Hanoch, and Elroy-Stein, Orna

Subjects

DRUG use testing, VANISHING white matter disease, LEUKODYSTROPHY, MITOCHONDRIA, GENETICS, CENTRAL nervous system depressants

Abstract

Vanishing white matter (VWM) disease is an autosomal genetic leukodystrophy caused by mutations in subunits of eukaryotic translation initiation factor 2B (eIF2B). The clinical symptoms exhibit progressive loss of white matter in both hemispheres of the brain, accompanied by motor functions deterioration, neurological deficits, and early death. To date there is no treatment for VWM disease. The aim of this work was to expedite rational development of a therapeutic opportunity. Our approach was to design a computer-aided strategy for an efficient and reliable screening of drug-like molecules; and to use primary cultures of fibroblasts isolated from the Eif2b5R132H/R132H VWM mouse model for screening. The abnormal mitochondria content phenotype of the mutant cells was chosen as a read-out for a simple cell-based fluorescent assay to assess the effect of the tested compounds. We obtained a hit rate of 0.04% (20 hits out of 50,000 compounds from the selected library). All primary hits decreased mitochondria content and brought it closer to WT levels. Structural similarities between our primary hits and other compounds with known targets allowed the identification of three putative cellular pathways/targets: 11β-hydroxysteroid dehydrogenase type 1, Sonic hedgehog (Shh), and Sigma-1-Receptor (S1R). In addition to initial experimental indication of Shh pathway impairment in VWM mouse brains, the current study provides evidence that S1R is a relevant target for pharmaceutical intervention for potential treatment of the disease. Specifically, we found lower expression level of S1R protein in fibroblasts, astrocytes, and whole brains isolated from Eif2b5R132H/R132H compared to WT mice, and confirmed that one of the hits is a direct binder of S1R, acting as agonist. Furthermore, we provide evidence that treatment of mutant mouse fibroblasts and astrocytes with various S1R agonists corrects the functional impairments of their mitochondria and prevents their need to increase their mitochondria content for compensation purposes. Moreover, S1R activation enhances the survival rate of mutant cells under ER stress conditions, bringing it to WT levels. This study marks S1R as a target for drug development toward treatment of VWM disease. Moreover, it further establishes the important connection between white matter well-being and S1R-mediated proper mitochondria/ER function. [ABSTRACT FROM AUTHOR]

Published

2018

6. Mutant eIF2B leads to impaired mitochondrial oxidative phosphorylation in vanishing white matter disease.

Author

Raini, Gali, Sharet, Reut, Herrero, Melisa, Atzmon, Andrea, Shenoy, Anjana, Geiger, Tamar, and Elroy‐Stein, Orna

Subjects

TRANSLATION initiation factors (Biochemistry), VANISHING white matter disease, FIBROBLASTS, OXIDATIVE phosphorylation, NEURODEGENERATION

Abstract

Eukaryotic translation initiation factor 2B ( eIF2B) is a master regulator of protein synthesis under normal and stress conditions. Mutations in any of the five genes encoding its subunits lead to vanishing white matter ( VWM) disease, a recessive genetic deadly illness caused by progressive loss of white matter in the brain. In this study we used fibroblasts, which are not involved in the disease, to demonstrate the involvement of eIF2B in mitochondrial function and abundance. Mass spectrometry of total proteome of mouse embryonic fibroblasts ( MEFs) isolated from Eif2b5R132H/R132H mice revealed unbalanced stoichiometry of proteins involved in oxidative phosphorylation and of mitochondrial translation machinery components, among others. Mutant MEFs exhibit 55% decrease in oxygen consumption rate per mt DNA content and 47% increase in mitochondrial abundance ( p < 0.005), reflecting adaptation to energy requirements. A more robust eIF2B-associated oxidative respiration deficiency was found in mutant primary astrocytes, which exhibit > 3-fold lower ATP-linked respiration per cell despite a 2-fold increase in mt DNA content ( p < 0.03). The 2-fold increase in basal and stimulated glycolysis in mutant astrocytes ( p ≤ 0.03), but not in MEFs, demonstrates their higher energetic needs and further explicates their involvement in the disease. The data demonstrate the critical role of eIF2B in tight coordination of expression from nuclear and mitochondrial genomes and illuminates the importance of mitochondrial function in VWM pathology. Further dissection of the signaling network associated with eIF2B function will help generating therapeutic strategies for VWM disease and possibly other neurodegenerative disorders. [ABSTRACT FROM AUTHOR]

Published

2017

7. The Energy Status of Astrocytes Is the Achilles' Heel of eIF2B-Leukodystrophy.

Author

Herrero, Melisa, Daw, Maron, Atzmon, Andrea, and Elroy-Stein, Orna

Subjects

LEUKOENCEPHALOPATHIES, HUNTINGTIN protein, FIBROBLASTS, REACTIVE oxygen species, CHARGE exchange, PROTEIN kinases, ASTROCYTES, GLYCOLYSIS

Abstract

Translation initiation factor 2B (eIF2B) is a master regulator of global protein synthesis in all cell types. The mild genetic Eif2b5(R132H) mutation causes a slight reduction in eIF2B enzymatic activity which leads to abnormal composition of mitochondrial electron transfer chain complexes and impaired oxidative phosphorylation. Previous work using primary fibroblasts isolated from Eif2b5(R132H/R132H) mice revealed that owing to increased mitochondrial biogenesis they exhibit normal cellular ATP level. In contrast to fibroblasts, here we show that primary astrocytes isolated from Eif2b5(R132H/R132H) mice are unable to compensate for their metabolic impairment and exhibit chronic state of low ATP level regardless of extensive adaptation efforts. Mutant astrocytes are hypersensitive to oxidative stress and to further energy stress. Moreover, they show migration deficit upon exposure to glucose starvation. The mutation in Eif2b5 prompts reactive oxygen species (ROS)-mediated inferior ability to stimulate the AMP-activated protein kinase (AMPK) axis, due to a requirement to increase the mammalian target of rapamycin complex-1 (mTORC1) signalling in order to enable oxidative glycolysis and generation of specific subclass of ROS-regulating proteins, similar to cancer cells. The data disclose the robust impact of eIF2B on metabolic and redox homeostasis programs in astrocytes and point at their hyper-sensitivity to mutated eIF2B. Thereby, it illuminates the central involvement of astrocytes in Vanishing White Matter Disease (VWMD), a genetic neurodegenerative leukodystrophy caused by homozygous hypomorphic mutations in genes encoding any of the 5 subunits of eIF2B. [ABSTRACT FROM AUTHOR]

Published

2021