Your search keyword '"Francesco M. Lasorsa"' showing total 43 results

1. Ketogenic Diet Treatment of Defects in the Mitochondrial Malate Aspartate Shuttle and Pyruvate Carrier

Author

Bigna K. Bölsterli, Eugen Boltshauser, Luigi Palmieri, Johannes Spenger, Michaela Brunner-Krainz, Felix Distelmaier, Peter Freisinger, Tobias Geis, Andrea L. Gropman, Johannes Häberle, Julia Hentschel, Bruno Jeandidier, Daniela Karall, Boris Keren, Annick Klabunde-Cherwon, Vassiliki Konstantopoulou, Raimund Kottke, Francesco M. Lasorsa, Christine Makowski, Cyril Mignot, Ruth O’Gorman Tuura, Vito Porcelli, René Santer, Kuntal Sen, Katja Steinbrücker, Steffen Syrbe, Matias Wagner, Andreas Ziegler, Thomas Zöggeler, Johannes A. Mayr, Holger Prokisch, and Saskia B. Wortmann

Subjects

mitochondrial disease, epilepsy, hepatopathy, aspartate glutamate carrier 1 deficiency, AGC1, citrin deficiency, Nutrition. Foods and food supply, TX341-641

Abstract

The mitochondrial malate aspartate shuttle system (MAS) maintains the cytosolic NAD+/NADH redox balance, thereby sustaining cytosolic redox-dependent pathways, such as glycolysis and serine biosynthesis. Human disease has been associated with defects in four MAS-proteins (encoded by MDH1, MDH2, GOT2, SLC25A12) sharing a neurological/epileptic phenotype, as well as citrin deficiency (SLC25A13) with a complex hepatopathic-neuropsychiatric phenotype. Ketogenic diets (KD) are high-fat/low-carbohydrate diets, which decrease glycolysis thus bypassing the mentioned defects. The same holds for mitochondrial pyruvate carrier (MPC) 1 deficiency, which also presents neurological deficits. We here describe 40 (18 previously unreported) subjects with MAS-/MPC1-defects (32 neurological phenotypes, eight citrin deficiency), describe and discuss their phenotypes and genotypes (presenting 12 novel variants), and the efficacy of KD. Of 13 MAS/MPC1-individuals with a neurological phenotype treated with KD, 11 experienced benefits—mainly a striking effect against seizures. Two individuals with citrin deficiency deceased before the correct diagnosis was established, presumably due to high-carbohydrate treatment. Six citrin-deficient individuals received a carbohydrate-restricted/fat-enriched diet and showed normalisation of laboratory values/hepatopathy as well as age-adequate thriving. We conclude that patients with MAS-/MPC1-defects are amenable to dietary intervention and that early (genetic) diagnosis is key for initiation of proper treatment and can even be lifesaving.

Published

2022

2. Inhibition of the Mitochondrial Glutamate Carrier SLC25A22 in Astrocytes Leads to Intracellular Glutamate Accumulation

Author

Emmanuelle Goubert, Yanina Mircheva, Francesco M. Lasorsa, Christophe Melon, Emanuela Profilo, Julie Sutera, Hélène Becq, Ferdinando Palmieri, Luigi Palmieri, Laurent Aniksztejn, and Florence Molinari

Subjects

mitochondrial glutamate carrier, glutamate transport, epilepsy, astrocytes, glutamate, ATP, Neurosciences. Biological psychiatry. Neuropsychiatry, RC321-571

Abstract

The solute carrier family 25 (SLC25) drives the import of a large diversity of metabolites into mitochondria, a key cellular structure involved in many metabolic functions. Mutations of the mitochondrial glutamate carrier SLC25A22 (also named GC1) have been identified in early epileptic encephalopathy (EEE) and migrating partial seizures in infancy (MPSI) but the pathophysiological mechanism of GC1 deficiency is still unknown, hampered by the absence of an in vivo model. This carrier is mainly expressed in astrocytes and is the principal gate for glutamate entry into mitochondria. A sufficient supply of energy is essential for the proper function of the brain and mitochondria have a pivotal role in maintaining energy homeostasis. In this work, we wanted to study the consequences of GC1 absence in an in vitro model in order to understand if glutamate catabolism and/or mitochondrial function could be affected. First, short hairpin RNA (shRNA) designed to specifically silence GC1 were validated in rat C6 glioma cells. Silencing GC1 in C6 resulted in a reduction of the GC1 mRNA combined with a decrease of the mitochondrial glutamate carrier activity. Then, primary astrocyte cultures were prepared and transfected with shRNA-GC1 or mismatch-RNA (mmRNA) constructs using the Neon® Transfection System in order to target a high number of primary astrocytes, more than 64%. Silencing GC1 in primary astrocytes resulted in a reduced nicotinamide adenine dinucleotide (Phosphate) (NAD(P)H) formation upon glutamate stimulation. We also observed that the mitochondrial respiratory chain (MRC) was functional after glucose stimulation but not activated by glutamate, resulting in a lower level of cellular adenosine triphosphate (ATP) in silenced astrocytes compared to control cells. Moreover, GC1 inactivation resulted in an intracellular glutamate accumulation. Our results show that mitochondrial glutamate transport via GC1 is important in sustaining glutamate homeostasis in astrocytes.Main Points:The mitochondrial respiratory chain is functional in absence of GC1Lack of glutamate oxidation results in a lower global ATP levelLack of mitochondrial glutamate transport results in intracellular glutamate accumulation

Published

2017

3. Supplementary Figure S3 from Statins Reduce Intratumor Cholesterol Affecting Adrenocortical Cancer Growth

Author

Rosa Sirianni, Ivan Casaburi, Vincenzo Pezzi, Antonio M. Lerario, Luigi Palmieri, Simona N. Barile, Francesco M. Lasorsa, Catia Pilon, Raffaele Pezzani, Francesco Fallo, Rocco Malivindi, Marta C. Nocito, Sara Sculco, Arianna De Luca, Vittoria Rago, Adele Chimento, Paola Avena, and Francesca Trotta

Abstract

Supplementary Fig. S3 shows that mevalonate and estradiol prevent simvastatin inhibitory effects.

Published

2023

4. Supplementary methods from Statins Reduce Intratumor Cholesterol Affecting Adrenocortical Cancer Growth

Author

Rosa Sirianni, Ivan Casaburi, Vincenzo Pezzi, Antonio M. Lerario, Luigi Palmieri, Simona N. Barile, Francesco M. Lasorsa, Catia Pilon, Raffaele Pezzani, Francesco Fallo, Rocco Malivindi, Marta C. Nocito, Sara Sculco, Arianna De Luca, Vittoria Rago, Adele Chimento, Paola Avena, and Francesca Trotta

Abstract

Supplementary methods

Published

2023

5. Impaired mitochondrial respiration in neuron progenitor cells from IPSCs of patients affected by AGC1 deficiency

Author

Francesco M. Lasorsa, Maria C. Magnifico, Simona N. Barile, Felix Distelmaier, Luigi Viggiano, Sabrina Petralla, Vito Porcelli, Antonella Pignataro, Eleonora Poeta, Isabella Pisano, Giuseppe Fiermonte, Luigi Palmieri, Stewart A. Anderson, Douglas C. Wallace, Julia Hentschel, and Barbara Monti

Subjects

Biophysics, Cell Biology, Biochemistry

Published

2022

6. Mutations in SLC25A36 (PNC2) associated with the hyperinsulinism/hyperammonemia (HI/HA) syndrome

Author

Luigi Palmieri, Francesco M. Lasorsa, and Orly Elpeleg

Subjects

Biophysics, Cell Biology, Biochemistry

Published

2022

7. KRAS-regulated glutamine metabolism requires UCP2-mediated aspartate transport to support pancreatic cancer growth

Author

Vittoria Rago, Rocco Malivindi, Giuseppe E. De Benedetto, Isabella Pisano, Giuseppe Fiermonte, Francesco M. Lasorsa, Carmela Piazzolla, Christopher L. Riley, Angelo Vozza, Stephan J. Reshkin, Wolfgang Sommergruber, Gennaro Agrimi, Francesca Pezzuto, Rosa Angela Cardone, Simona N. Barile, Yuan Li, Pasquale Scarcia, Carlo M.T. Marobbio, Maria C. Vegliante, Ruggiero Gorgoglione, Edward M. Mills, Luigi Palmieri, Loredana Capobianco, Deborah Fratantonio, Susanna Raho, Maria Raffaella Greco, Francesco De Leonardis, Vincenza Dolce, Raho, Susanna, Capobianco, Loredana, Malivindi, Rocco, Vozza, Angelo, Piazzolla, Carmela, De Leonardis, Francesco, Gorgoglione, Ruggiero, Scarcia, Pasquale, Pezzuto, Francesca, Agrimi, Gennaro, Barile, Simona N., Pisano, Isabella, Reshkin, Stephan J., Greco, Maria R., Cardone, Rosa A., Rago, Vittoria, Li, Yuan, Marobbio, Carlo M. T., Sommergruber, Wolfgang, Riley, Christopher L., Lasorsa, Francesco M., Mills, Edward, Vegliante, Maria C., De Benedetto, Giuseppe E., Fratantonio, Deborah, Palmieri, Luigi, Dolce &amp, Vincenza, Fiermonte, Giuseppe, Raho, S., Capobianco, L., Malivindi, R., Vozza, A., Piazzolla, C., De Leonardis, F., Gorgoglione, R., Scarcia, P., Pezzuto, F., Agrimi, G., Barile, S. N., Pisano, I., Reshkin, S. J., Greco, M. R., Cardone, R. A., Rago, V., Li, Y., Marobbio, C. M. T., Sommergruber, W., Riley, C. L., Lasorsa, F. M., Mills, E., Vegliante, M. C., De Benedetto, G. E., Fratantonio, D., Palmieri, L., Dolce, V., and Fiermonte, G.

Subjects

endocrine system diseases, Endocrinology, Diabetes and Metabolism, Glutamine, Biological Transport, Active, Mice, SCID, Mitochondrion, Proto-Oncogene Proteins p21(ras), chemistry.chemical_compound, Mice, Cytosol, Physiology (medical), Cell Line, Tumor, Internal Medicine, Animals, Humans, Uncoupling Protein 2, oncogenic Kras, mitochondrial carrier, UCP2, human pancreatic ductal adenocarcinoma (PDAC), chemistry.chemical_classification, Reactive oxygen species, Aspartic Acid, Glutaminolysis, Cell growth, Animal, Pancreatic Neoplasm, Cell Biology, Xenograft Model Antitumor Assays, Cell biology, Mitochondria, Pancreatic Neoplasms, chemistry, Glutathione disulfide, Female, Aspartate transport, Reactive Oxygen Species, Reactive Oxygen Specie, Oxidation-Reduction, NADP, Carcinoma, Pancreatic Ductal, Human

Abstract

The oncogenic KRAS mutation has a critical role in the initiation of human pancreatic ductal adenocarcinoma (PDAC) since it rewires glutamine metabolism to increase reduced nicotinamide adenine dinucleotide phosphate (NADPH) production, balancing cellular redox homeostasis with macromolecular synthesis1,2. Mitochondrial glutamine-derived aspartate must be transported into the cytosol to generate metabolic precursors for NADPH production2. The mitochondrial transporter responsible for this aspartate efflux has remained elusive. Here, we show that mitochondrial uncoupling protein 2 (UCP2) catalyses this transport and promotes tumour growth. UCP2-silenced KRASmut cell lines display decreased glutaminolysis, lower NADPH/NADP+ and glutathione/glutathione disulfide ratios and higher reactive oxygen species levels compared to wild-type counterparts. UCP2 silencing reduces glutaminolysis also in KRASWT PDAC cells but does not affect their redox homeostasis or proliferation rates. In vitro and in vivo, UCP2 silencing strongly suppresses KRASmut PDAC cell growth. Collectively, these results demonstrate that UCP2 plays a vital role in PDAC, since its aspartate transport activity connects the mitochondrial and cytosolic reactions necessary for KRASmut rewired glutamine metabolism2, and thus it should be considered a key metabolic target for the treatment of this refractory tumour. UCP2 is shown in yeast and mammalian cells to transport aspartate out of mitochondria, thus enabling KRAS-mutated pancreatic ductal adenocarcinoma cells to perform glutaminolysis to support cancer growth.

Published

2020

8. Statins Reduce Intratumor Cholesterol Affecting Adrenocortical Cancer Growth

Author

Ivan Casaburi, Catia Pilon, Raffaele Pezzani, Rosa Sirianni, Arianna De Luca, Antonio M. Lerario, Francesco M. Lasorsa, Rocco Malivindi, Simona N. Barile, Adele Chimento, Francesco Fallo, Vincenzo Pezzi, Marta Claudia Nocito, L. Palmieri, Paola Avena, Sara Sculco, Vittoria Rago, and Francesca Trotta

Subjects

0301 basic medicine, Cancer Research, medicine.medical_specialty, Antineoplastic Agents, Hormonal, Estrogen receptor, 03 medical and health sciences, chemistry.chemical_compound, Mice, 0302 clinical medicine, Internal medicine, medicine, Adrenocortical Carcinoma, Adrenocortical carcinoma, Animals, Humans, Mitotane, Cell growth, Chemistry, Cholesterol, medicine.disease, Adrenal Cortex Neoplasms, 030104 developmental biology, Endocrinology, Oncology, Terminal deoxynucleotidyl transferase, Apoptosis, Simvastatin, 030220 oncology & carcinogenesis, lipids (amino acids, peptides, and proteins), Female, Hydroxymethylglutaryl-CoA Reductase Inhibitors, medicine.drug

Abstract

Mitotane causes hypercholesterolemia in patients with adrenocortical carcinoma (ACC). We suppose that cholesterol increases within the tumor and can be used to activate proliferative pathways. In this study, we used statins to decrease intratumor cholesterol and investigated the effects on ACC growth related to estrogen receptor α (ERα) action at the nuclear and mitochondrial levels. We first used microarray to investigate mitotane effect on genes involved in cholesterol homeostasis and evaluated their relationship with patients' survival in ACC TCGA. We then blocked cholesterol synthesis with simvastatin and determined the effects on H295R cell proliferation, estradiol production, and ERα activity in vitro and in xenograft tumors. We found that mitotane increases intratumor cholesterol content and expression of genes involved in cholesterol homeostasis, among them INSIG, whose expression affects patients' survival. Treatment of H295R cells with simvastatin to block cholesterol synthesis decreased cellular cholesterol content, and this affected cell viability. Simvastatin reduced estradiol production and decreased nuclear and mitochondrial ERα function. A mitochondrial target of ERα, the respiratory complex IV (COXIV), was reduced after simvastatin treatment, which profoundly affected mitochondrial respiration activating apoptosis. Additionally, simvastatin reduced tumor volume and weight of grafted H295R cells, intratumor cholesterol content, Ki-67 and ERα, COXIV expression and activity and increase terminal deoxynucleotidyl transferase dUTP nick end labeling–positive cells. Collectively, these data demonstrate that a reduction in intratumor cholesterol content prevents estradiol production and inhibits mitochondrial respiratory chain–inducing apoptosis in ACC cells. Inhibition of mitochondrial respiration by simvastatin represents a novel strategy to counteract ACC growth.

Published

2019

9. Deficiency of Mitochondrial Aspartate-Glutamate Carrier 1 Leads to Oligodendrocyte Precursor Cell Proliferation Defects Both In Vitro and In Vivo

Author

Ferdinando Palmieri, Francesca Massenzio, Marco Virgili, Miriam Capri, Alberto Danese, Carlotta Giorgi, Sabrina Petralla, Luis Emiliano Peña-Altamira, Barbara Monti, Paolo Pinton, Emanuela Profilo, Luigi Sbano, Simona N. Barile, Francesco M. Lasorsa, Mariangela Corricelli, Eleonora Poeta, Rita Ostan, Petralla S., Pena-Altamira L.E., Poeta E., Massenzio F., Virgili M., Barile S.N., Sbano L., Profilo E., Corricelli M., Danese A., Giorgi C., Ostan R., Capri M., Pinton P., Palmieri F., Lasorsa F.M., and Monti B.

Subjects

Platelet-derived growth factor, Amino Acid Transport Systems, endocrine system diseases, medicine.medical_treatment, Cellular differentiation, Antiporters, lcsh:Chemistry, chemistry.chemical_compound, Mice, Adenosine Triphosphate, Transforming Growth Factor beta, Lateral Ventricles, Receptors, Glutamate aspartate transporter, lcsh:QH301-705.5, Spectroscopy, Membrane Potential, Mitochondrial, Neurons, Platelet-Derived Growth Factor, biology, subventricular zone, growth factor, Cell Differentiation, General Medicine, Mitochondrial, Computer Science Applications, Cell biology, Mitochondria, mitochondrial disease, medicine.anatomical_structure, Lactates, hormones, hormone substitutes, and hormone antagonists, Signal Transduction, AGC1 deficiency, Growth factors, Mitochondrial disease, Mouse model, Subventricular zone, Amino Acid Transport Systems, Acidic, Animals, Cell Line, Cell Proliferation, Down-Regulation, Gene Silencing, Oligodendrocyte Precursor Cells, Reactive Oxygen Species, Receptors, Transforming Growth Factor beta, mouse model, Membrane Potential, Catalysis, Article, NO, Inorganic Chemistry, Precursor cell, Neurosphere, growth factors, medicine, Physical and Theoretical Chemistry, Molecular Biology, Growth factor, Acidic, Organic Chemistry, nutritional and metabolic diseases, Transforming growth factor beta, lcsh:Biology (General), lcsh:QD1-999, chemistry, nervous system, biology.protein

Abstract

Aspartate-Glutamate Carrier 1 (AGC1) deficiency is a rare neurological disease caused by mutations in the solute carrier family 25, member 12 (SLC25A12) gene, encoding for the mitochondrial aspartate-glutamate carrier isoform 1 (AGC1), a component of the malate&ndash, aspartate NADH shuttle (MAS), expressed in excitable tissues only. AGC1 deficiency patients are children showing severe hypotonia, arrested psychomotor development, seizures and global hypomyelination. While the effect of AGC1 deficiency in neurons and neuronal function has been deeply studied, little is known about oligodendrocytes and their precursors, the brain cells involved in myelination. Here we studied the effect of AGC1 down-regulation on oligodendrocyte precursor cells (OPCs), using both in vitro and in vivo mouse disease models. In the cell model, we showed that a reduced expression of AGC1 induces a deficit of OPC proliferation leading to their spontaneous and precocious differentiation into oligodendrocytes. Interestingly, this effect seems to be related to a dysregulation in the expression of trophic factors and receptors involved in OPC proliferation/differentiation, such as Platelet-Derived Growth Factor &alpha, (PDGF&alpha, ) and Transforming Growth Factor &beta, s (TGF&beta, s). We also confirmed the OPC reduction in vivo in AGC1-deficent mice, as well as a proliferation deficit in neurospheres from the Subventricular Zone (SVZ) of these animals, thus indicating that AGC1 reduction could affect the proliferation of different brain precursor cells. These data clearly show that AGC1 impairment alters myelination not only by acting on N-acetyl-aspartate production in neurons but also on OPC proliferation and suggest new potential therapeutic targets for the treatment of AGC1 deficiency.

Published

2019

10. A mutation in the mitochondrial aspartate/glutamate carrier leads to a more oxidizing intramitochondrial environment and an inflammatory myopathy in Dutch shepherd dogs

Author

Antonio M. Persico, James R. Mickelson, G. Diane Shelton, Ruggiero Gorgoglione, Robert K. Naviaux, Ling T. Guo, Peter J. Leegwater, Jane C. Naviaux, Francesco M. Lasorsa, Lin Wang, Elizabeth Guzik, Luigi Palmieri, Jon Monk, Vito Porcelli, Katie M. Minor, and Kefeng Li

Subjects

0301 basic medicine, Research Report, Amino Acid Transport Systems, Amino Acid Transport Systems, Acidic, SLC25A12, Myopathy, Glutamic Acid, Mitochondrion, Polymyositis, mitochondrial transporter, Antiporters, Dermatomyositis, Proinflammatory cytokine, Canine, Inflammatory myopathy, 03 medical and health sciences, 0302 clinical medicine, Dogs, medicine, Glutamate aspartate transporter, Metabolomics, Animals, Humans, Dog Diseases, Mitochondrial transporter, Acidic, Aspartic Acid, Mitochondria, Mutation, Myositis, Oxidation-Reduction, biology, Chemistry, Muscle weakness, medicine.disease, Molecular biology, metabolomics, 030104 developmental biology, Neurology, biology.protein, Neurology (clinical), Inclusion body myositis, medicine.symptom, Canine, Metabolomics, Mitochondrial transporter, Myopathy, SLC25A12, Amino Acid Transport Systems, Acidic, Animals, Antiporters, Aspartic Acid, Dermatomyositis, Dog Diseases, Dogs, Glutamic Acid, Humans, Mitochondria, Mutation, Myositis, Oxidation-Reduction, Polymyositis, 030217 neurology & neurosurgery, myopathy

Abstract

Background Inflammatory myopathies are characterized by infiltration of inflammatory cells into muscle. Typically, immune-mediated disorders such as polymyositis, dermatomyositis and inclusion body myositis are diagnosed. Objective A small family of dogs with early onset muscle weakness and inflammatory muscle biopsies were investigated for an underlying genetic cause. Methods Following the histopathological diagnosis of inflammatory myopathy, mutational analysis including whole genome sequencing, functional transport studies of the mutated and wild-type proteins, and metabolomic analysis were performed. Results Whole genome resequencing identified a pathological variant in the SLC25A12 gene, resulting in a leucine to proline substitution at amino acid 349 in the mitochondrial aspartate-glutamate transporter known as the neuron and muscle specific aspartate glutamate carrier 1 (AGC1). Functionally reconstituting recombinant wild-type and mutant AGC1 into liposomes demonstrated a dramatic decrease in AGC1 transport activity and inability to transfer reducing equivalents from the cytosol into mitochondria. Targeted, broad-spectrum metabolomic analysis from affected and control muscles demonstrated a proinflammatory milieu and strong support for oxidative stress. Conclusions This study provides the first description of a metabolic mechanism in which ablated mitochondrial glutamate transport markedly reduced the import of reducing equivalents into mitochondria and produced a highly oxidizing and proinflammatory muscle environment and an inflammatory myopathy.

Published

2019

11. SLC25A10 biallelic mutations in intractable epileptic encephalopathy with complex I deficiency

Author

Renzo Guerrini, Luna Laera, Sergio Giannattasio, Eleonora Paradies, Carlo M.T. Marobbio, Maria Anna Donati, Luigi Palmieri, Vito Porcelli, Eleonora Lamantea, Alessandra Castegna, Faruk Hossain, Alessio Menga, Anna De Grassi, Ciro Leonardo Pierri, Pasquale Scarcia, Francesco M. Lasorsa, Ruggiero Gorgoglione, Daniele Ghezzi, Isabella Pisano, Valeria Tiranti, Giuseppe Punzi, Matteo Ruggiu, and Ferdinando Palmieri

Subjects

0301 basic medicine, Male, Mitochondrial DNA, Heterozygote, Mitochondrial Diseases, Antioxidants, Brain Diseases, Child, DNA, Mitochondrial, Dicarboxylic Acid Transporters, Humans, Metabolism, Inborn Errors, Mitochondria, Mutation, Oxidative Phosphorylation, Oxidative Stress, Pedigree, RNA Splicing, Mitochondrion, Biology, medicine.disease_cause, 03 medical and health sciences, Genetics, medicine, complex I deficiency, Molecular Biology, Gene, Genetics (clinical), Exome sequencing, encephalopathic epilepsy, Inborn Errors, RNA, Heterozygote advantage, General Medicine, DNA, Articles, Mitochondrial carrier, Mitochondrial, 030104 developmental biology, Metabolism, exome sequencing, slc25a10

Abstract

Mitochondrial diseases are a plethora of inherited neuromuscular disorders sharing defects in mitochondrial respiration, but largely different from one another for genetic basis and pathogenic mechanism. Whole exome sequencing was performed in a familiar trio (trio-WES) with a child affected by severe epileptic encephalopathy associated with respiratory complex I deficiency and mitochondrial DNA depletion in skeletal muscle. By trio-WES we identified biallelic mutations in SLC25A10, a nuclear gene encoding a member of the mitochondrial carrier family. Genetic and functional analyses conducted on patient fibroblasts showed that SLC25A10 mutations are associated with reduction in RNA quantity and aberrant RNA splicing, and to absence of SLC25A10 protein and its transporting function. The yeast SLC25A10 ortholog knockout strain showed defects in mitochondrial respiration and mitochondrial DNA content, similarly to what observed in the patient skeletal muscle, and growth susceptibility to oxidative stress. Albeit patient fibroblasts were depleted in the main antioxidant molecules NADPH and glutathione, transport assays demonstrated that SLC25A10 is unable to transport glutathione. Here, we report the first recessive mutations of SLC25A10 associated to an inherited severe mitochondrial neurodegenerative disorder. We propose that SLC25A10 loss-of-function causes pathological disarrangements in respiratory-demanding conditions and oxidative stress vulnerability.

Published

2017

12. Down-regulation of the mitochondrial aspartate-glutamate carrier isoform 1 AGC1 inhibits proliferation and N-acetylaspartate synthesis in Neuro2A cells

Author

Luigi Palmieri, Alessandra Castegna, Emanuela Profilo, Luis Emiliano Peña-Altamira, Sabrina Petralla, Massimo Zeviani, Mariangela Corricelli, Vito Porcelli, Barbara Monti, Giuseppe Fiermonte, Ferdinando Palmieri, Paolo Pinton, Giulia Giannuzzi, Luigi Sbano, Alberto Danese, Marco Virgili, Carlotta Giorgi, Carlo Viscomi, Francesca Massenzio, Erika M. Palmieri, Francesco M. Lasorsa, Gennaro Agrimi, Profilo, E, Peña-Altamira, Le, Corricelli, M, Castegna, A, Danese, A, Agrimi, G, Petralla, S, Giannuzzi, G, Porcelli, V, Sbano, L, Viscomi, C, Massenzio, F, Palmieri, Em, Giorgi, C, Fiermonte, G, Virgili, M, Palmieri, L, Zeviani, M, Pinton, P, Monti, B, Palmieri, F, and Lasorsa, Fm.

Subjects

0301 basic medicine, medicine.medical_specialty, Mitochondrial Diseases, Amino Acid Transport Systems, Amino Acid Transport Systems, Acidic, AGC1 deficiency, Brain hypomyelination, Mitochondrial aspartate/glutamate carrier, N-Acetylaspartate synthesis, Neurodegenerative disorders, Antiporters, Aspartic Acid, Cell Line, Hereditary Central Nervous System Demyelinating Diseases, Humans, Mitochondrial Proteins, Neurons, Psychomotor Disorders, Cell Proliferation, Down-Regulation, Biology, Mitochondrion, NO, 03 medical and health sciences, Myelin, Downregulation and upregulation, Internal medicine, medicine, Glutamate aspartate transporter, Molecular Medicine, Molecular Biology, brain hypomyelination, Cell growth, Acidic, Glutamate receptor, N-acetylaspartate synthesi, Glutamine, Cytosol, 030104 developmental biology, medicine.anatomical_structure, Endocrinology, nervous system, neurodegenerative disorders, biology.protein

Abstract

The mitochondrial aspartate-glutamate carrier isoform 1 (AGC1) catalyzes a Ca2+-stimulated export of aspartate to the cytosol in exchange for glutamate, and is a key component of the malate-aspartate shuttle which transfers NADH reducing equivalents from the cytosol to mitochondria. By sustaining the complete glucose oxidation, AGC1 is thought to be important in providing energy for cells, in particular in the CNS and muscle where this protein is mainly expressed. Defects in the AGC1 gene cause AGC1 deficiency, an infantile encephalopathy with delayed myelination and reduced brain N-acetylaspartate (NAA) levels, the precursor of myelin synthesis in the CNS. Here, we show that undifferentiated Neuro2A cells with down-regulated AGC1 display a significant proliferation deficit associated with reduced mitochondrial respiration, and are unable to synthesize NAA properly. In the presence of high glutamine oxidation, cells with reduced AGC1 restore cell proliferation, although oxidative stress increases and NAA synthesis deficit persists. Our data suggest that the cellular energetic deficit due to AGC1 impairment is associated with inappropriate aspartate levels to support neuronal proliferation when glutamine is not used as metabolic substrate, and we propose that delayed myelination in AGC1 deficiency patients could be attributable, at least in part, to neuronal loss combined with lack of NAA synthesis occurring during the nervous system development.

Published

2017

13. UCP2 transports C4 metabolites out of mitochondria, regulating glucose and glutamine oxidation

Author

Pasquale Scarcia, Ferdinando Palmieri, Valeria Mariajolanda Calcagnile, Giuseppe Fiermonte, Luigi Palmieri, Francesco De Leonardis, Daniela Amorese, Daniel Ricquier, Alessandra Castegna, Giovanni Parisi, Eleonora Paradies, Raffaele Marmo, Frédéric Bouillaud, Francesco M. Lasorsa, and Angelo Vozza

Subjects

Oxaloacetic Acid, Cellular respiration, Glutamine, Cell Respiration, Citric Acid Cycle, Mitochondrion, Catalysis, Ion Channels, Phosphates, Mitochondrial Proteins, Oxygen Consumption, Humans, Citrate synthase, Uncoupling Protein 2, Gene Silencing, Inner mitochondrial membrane, Membrane Potential, Mitochondrial, Multidisciplinary, Glutaminolysis, biology, Hep G2 Cells, Biological Sciences, Mitochondrial carrier, Carbon, Mitochondria, Cell biology, Oxygen, Citric acid cycle, Glucose, HEK293 Cells, Biochemistry, Liposomes, biology.protein, Energy Metabolism

Abstract

Uncoupling protein 2 (UCP2) is involved in various physiological and pathological processes such as insulin secretion, stem cell differentiation, cancer, and aging. However, its biochemical and physiological function is still under debate. Here we show that UCP2 is a metabolite transporter that regulates substrate oxidation in mitochondria. To shed light on its biochemical role, we first studied the effects of its silencing on the mitochondrial oxidation of glucose and glutamine. Compared with wild-type, UCP2-silenced human hepatocellular carcinoma (HepG2) cells, grown in the presence of glucose, showed a higher inner mitochondrial membrane potential and ATP:ADP ratio associated with a lower lactate release. Opposite results were obtained in the presence of glutamine instead of glucose. UCP2 reconstituted in lipid vesicles catalyzed the exchange of malate, oxaloacetate, and aspartate for phosphate plus a proton from opposite sides of the membrane. The higher levels of citric acid cycle intermediates found in the mitochondria of siUCP2-HepG2 cells compared with those found in wild-type cells in addition to the transport data indicate that, by exporting C4 compounds out of mitochondria, UCP2 limits the oxidation of acetyl-CoA-producing substrates such as glucose and enhances glutaminolysis, preventing the mitochondrial accumulation of C4 metabolites derived from glutamine. Our work reveals a unique regulatory mechanism in cell bioenergetics and provokes a substantial reconsideration of the physiological and pathological functions ascribed to UCP2 based on its purported uncoupling properties.

Published

2014

14. Synthesis, characterization, and in vitro evaluation of new coordination complexes of platinum(<scp>ii</scp>) and rhenium(<scp>i</scp>) with a ligand targeting the translocator protein (TSPO)

Author

Sara Piccinonna, Valentino Laquintana, Giovanni Natile, Nunzio Denora, Francesco M. Lasorsa, Massimo Franco, and Nicola Margiotta

Subjects

Imidazopyridine, Stereochemistry, Apoptosis, Ligands, Inorganic Chemistry, chemistry.chemical_compound, Residue (chemistry), Receptors, GABA, Coordination Complexes, Cell Line, Tumor, Translocator protein, Humans, Moiety, Cytotoxicity, Platinum, biology, Ligand, Valproic Acid, Cell Cycle Checkpoints, In vitro, Mitochondria, Rhenium, Microscopy, Fluorescence, Dipicolylamine, chemistry, biology.protein, Protein Binding

Abstract

The 18 kDa translocator protein (TSPO) is overexpressed in many types of cancers and is also abundant in activated microglial cells occurring in inflammatory neurodegenerative diseases. The TSPO-selective ligand 2-(8-(2-(bis-(pyridin-2-yl-methyl)amino)acetamido)-2-(4-chlorophenyl)H-imidazo[1,2-a]pyridin-3-yl)-N,N-dipropylacetamide (CB256), which fulfills the requirements of a bifunctional chelate approach, has been used to synthesize coordination complexes containing either Pt (1) or Re (3), or both metal ions (2). The new metal complexes showed a cellular uptake markedly greater than that of the precursor metallic compounds and were also able to induce apoptosis in C6 glioma cells. The good cytotoxicity of the free ligand CB256 towards C6, A2780, and A2780cisR tumor cell lines was attenuated after coordination of the dipicolylamine moiety to Pt while coordination of the imidazopyridine residue to Re reduces the affinity towards TSPO. The results of the present investigation are essential for the design of new imidazopyridine bifunctional chelate ligands targeted to TSPO.

Published

2014

15. Inhibition of the Mitochondrial Glutamate Carrier SLC25A22 in Astrocytes Leads to Intracellular Glutamate Accumulation

Author

Emmanuelle, Goubert, Yanina, Mircheva, Francesco M, Lasorsa, Christophe, Melon, Emanuela, Profilo, Julie, Sutera, Hélène, Becq, Ferdinando, Palmieri, Luigi, Palmieri, Laurent, Aniksztejn, and Florence, Molinari

Subjects

ATP, genetic structures, glutamate transport, astrocytes, epilepsy, glutamate, mitochondrial glutamate carrier, Neuroscience, Original Research

Abstract

The solute carrier family 25 (SLC25) drives the import of a large diversity of metabolites into mitochondria, a key cellular structure involved in many metabolic functions. Mutations of the mitochondrial glutamate carrier SLC25A22 (also named GC1) have been identified in early epileptic encephalopathy (EEE) and migrating partial seizures in infancy (MPSI) but the pathophysiological mechanism of GC1 deficiency is still unknown, hampered by the absence of an in vivo model. This carrier is mainly expressed in astrocytes and is the principal gate for glutamate entry into mitochondria. A sufficient supply of energy is essential for the proper function of the brain and mitochondria have a pivotal role in maintaining energy homeostasis. In this work, we wanted to study the consequences of GC1 absence in an in vitro model in order to understand if glutamate catabolism and/or mitochondrial function could be affected. First, short hairpin RNA (shRNA) designed to specifically silence GC1 were validated in rat C6 glioma cells. Silencing GC1 in C6 resulted in a reduction of the GC1 mRNA combined with a decrease of the mitochondrial glutamate carrier activity. Then, primary astrocyte cultures were prepared and transfected with shRNA-GC1 or mismatch-RNA (mmRNA) constructs using the Neon® Transfection System in order to target a high number of primary astrocytes, more than 64%. Silencing GC1 in primary astrocytes resulted in a reduced nicotinamide adenine dinucleotide (Phosphate) (NAD(P)H) formation upon glutamate stimulation. We also observed that the mitochondrial respiratory chain (MRC) was functional after glucose stimulation but not activated by glutamate, resulting in a lower level of cellular adenosine triphosphate (ATP) in silenced astrocytes compared to control cells. Moreover, GC1 inactivation resulted in an intracellular glutamate accumulation. Our results show that mitochondrial glutamate transport via GC1 is important in sustaining glutamate homeostasis in astrocytes. Main Points: The mitochondrial respiratory chain is functional in absence of GC1Lack of glutamate oxidation results in a lower global ATP levelLack of mitochondrial glutamate transport results in intracellular glutamate accumulation

Published

2016

16. Mitochondrial Carriers for Aspartate, Glutamate and Other Amino Acids: A Review

Author

Magnus Monné, Francesco M. Lasorsa, Angelo Vozza, Vito Porcelli, and Ferdinando Palmieri

Subjects

mitochondrial carrier, 0301 basic medicine, Saccharomyces cerevisiae Proteins, Arginine, Mitochondrial translation, membrane transport, Glutamic Acid, glutamate, arginine, Review, Mitochondrial Membrane Transport Proteins, mitochondrial transporter, Catalysis, lcsh:Chemistry, Inorganic Chemistry, 03 medical and health sciences, 0302 clinical medicine, Humans, Nucleotide, Physical and Theoretical Chemistry, Inner mitochondrial membrane, lcsh:QH301-705.5, Molecular Biology, Phylogeny, Spectroscopy, chemistry.chemical_classification, Aspartic Acid, amino acids, aspartate, lysine, Arabidopsis Proteins, Organic Chemistry, Biological Transport, General Medicine, Membrane transport, Mitochondrial carrier, Computer Science Applications, Amino acid, 030104 developmental biology, lcsh:Biology (General), lcsh:QD1-999, chemistry, Biochemistry, Mitochondrial matrix, Mitochondrial Membranes, ornithine, 030217 neurology & neurosurgery, glycine

Abstract

Members of the mitochondrial carrier (MC) protein family transport various molecules across the mitochondrial inner membrane to interlink steps of metabolic pathways and biochemical processes that take place in different compartments; i.e., are localized partly inside and outside the mitochondrial matrix. MC substrates consist of metabolites, inorganic anions (such as phosphate and sulfate), nucleotides, cofactors and amino acids. These compounds have been identified by in vitro transport assays based on the uptake of radioactively labeled substrates into liposomes reconstituted with recombinant purified MCs. By using this approach, 18 human, plant and yeast MCs for amino acids have been characterized and shown to transport aspartate, glutamate, ornithine, arginine, lysine, histidine, citrulline and glycine with varying substrate specificities, kinetics, influences of the pH gradient, and capacities for the antiport and uniport mode of transport. Aside from providing amino acids for mitochondrial translation, the transport reactions catalyzed by these MCs are crucial in energy, nitrogen, nucleotide and amino acid metabolism. In this review we dissect the transport properties, phylogeny, regulation and expression levels in different tissues of MCs for amino acids, and summarize the main structural aspects known until now about MCs. The effects of their disease-causing mutations and manipulation of their expression levels in cells are also considered as clues for understanding their physiological functions.

Published

2019

17. SLC25A22is a novel gene for migrating partial seizures in infancy

Author

Manju A. Kurian, Kutay Deniz Atabay, Jennifer N. Partlow, Emilie Martin, Christopher J. Yuskaitis, Francesco M. Lasorsa, Mustafa A. Salih, Sanjeev V. Kothare, Tommy Stödberg, Salah A. Elmalik, Fahad A. Bashiri, Mohammad M. Kabiraj, Erin L. Heinzen, Ferdinando Palmieri, Radwan M. Zeidan, Annapurna Poduri, Amy McTague, Christopher A. Walsh, P. Christina Elhosary, Robert Sean Hill, Brenda J. Barry, Ingrid E. Scheffer, Vida Chitsazzadeh, Christopher M. LaCoursiere, and A. James Barkovich

Subjects

Genetics, Candidate gene, Mutation, Single-nucleotide polymorphism, Consanguinity, Biology, medicine.disease_cause, Neurology, Genetic linkage, medicine, Neurology (clinical), Exome, Gene, Exome sequencing

Abstract

Objective To identify a genetic cause for migrating partial seizures in infancy (MPSI). Methods We characterized a consanguineous pedigree with MPSI and obtained DNA from affected and unaffected family members. We analyzed single nucleotide polymorphism 500K data to identify regions with evidence of linkage. We performed whole exome sequencing and analyzed homozygous variants in regions of linkage to identify a candidate gene and performed functional studies of the candidate gene SLC25A22. Results In a consanguineous pedigree with 2 individuals with MPSI, we identified 2 regions of linkage, chromosome 4p16.1-p16.3 and chromosome 11p15.4-pter. Using whole exome sequencing, we identified 8 novel homozygous variants in genes in these regions. Only 1 variant, SLC25A22 c.G328C, results in a change of a highly conserved amino acid (p.G110R) and was not present in control samples. SLC25A22 encodes a glutamate transporter with strong expression in the developing brain. We show that the specific G110R mutation, located in a transmembrane domain of the protein, disrupts mitochondrial glutamate transport. Interpretation We have shown that MPSI can be inherited and have identified a novel homozygous mutation in SLC25A22 in the affected individuals. Our data strongly suggest that SLC25A22 is responsible for MPSI, a severe condition with few known etiologies. We have demonstrated that a combination of linkage analysis and whole exome sequencing can be used for disease gene discovery. Finally, as SLC25A22 had been implicated in the distinct syndrome of neonatal epilepsy with suppression bursts on electroencephalogram, we have expanded the phenotypic spectrum associated with SLC25A22. Ann Neurol 2013;74:873–882

Published

2013

18. Targeting of the Translocator Protein 18 kDa (TSPO): A Valuable Approach for Nuclear and Optical Imaging of Activated Microglia

Author

Modesto de Candia, Adriana Trapani, Giuseppe Trapani, Claudio Palazzo, and Francesco M. Lasorsa

Subjects

Pathology, medicine.medical_specialty, Biomedical Engineering, Pharmaceutical Science, Bioengineering, Ligands, Optical imaging, Receptors, GABA, medicine, Radioligand, Translocator protein, Animals, Humans, Pharmacology, medicine.diagnostic_test, biology, Microglia, Chemistry, Optical Imaging, Organic Chemistry, Isoquinolines, medicine.anatomical_structure, Microscopy, Fluorescence, Positron emission tomography, Positron-Emission Tomography, biology.protein, Neuroscience, Biotechnology

Abstract

The aim of the present review is to give a concise and updated analysis of the imaging tools for the visualization of activated microglia. After an overview on the important pathologies where activated microglia are involved, we first describe the role played by the translocator protein-18 kDa (TSPO) as an important target for the visualization of activated microglia. Second, imaging tools based on TSPO ligands radiolabeled for positron emission tomography (PET) are summarized with particular emphasis to the TSPO ligands alternative to the standard radioligand [(11)C]PK11195 or (R)-[(11)C]PK11195. In this regard, an updated list of (11)C- and (18)F-labeled TSPO radioligands is shown. Moreover, a detailed analysis based on TSPO ligands bearing fluorescent probes for fluorescence microscopy is also provided. This last optical imaging technique represents an area of large and increasing interest due to the advantages offered by the use of simple instrumentation and safer experimental conditions. The scope and limitations of the nuclear and optical imaging techniques are discussed. Finally, a perspective on the plausible advances in this area is also presented.

Published

2013

19. Biochemical characterization of a new mitochondrial transporter of dephosphocoenzyme A in Drosophila melanogaster

Author

Susanna Raho, Giovanni Parisi, Eleonora Paradies, Angelo Vozza, Vincenza Dolce, Luigina Muto, Francesco M. Lasorsa, Anna De Grassi, Giuseppe Fiermonte, Carlo M.T. Marobbio, Loredana Capobianco, Ciro Leonardo Pierri, Francesco De Leonardis, Vozza, Angelo, Leonardis, Francesco De, Paradies, Eleonora, Grassi, Anna De, Pierri, Ciro Leonardo, Parisi, Giovanni, Marobbio, Carlo Marya Thoma, Lasorsa, Francesco Massimo, Muto, Luigina, Capobianco, Loredana, Dolce, Vincenza, Raho, Susanna, and Fiermonte, Giuseppe

Subjects

0301 basic medicine, Saccharomyces cerevisiae Proteins, Coenzyme A, Biophysics, Saccharomyces cerevisiae, Bioenergetics, Biology, Mitochondrion, Biochemistry, Mitochondrial Membrane Transport Proteins, 03 medical and health sciences, chemistry.chemical_compound, Cytosol, Biosynthesis, Escherichia coli, Animals, Amino Acid Sequence, Inner mitochondrial membrane, Dephosphocoenzyme A, Coenzyme A, Neurodegenerative disease, Mitochondrial carrier, Transport, 030102 biochemistry & molecular biology, Biological Transport, Cell Biology, Subcellular localization, biology.organism_classification, Mitochondrial carrier, Mitochondria, Kinetics, 030104 developmental biology, Drosophila melanogaster, chemistry, Protein Biosynthesis, Carrier Proteins, Sequence Alignment

Abstract

CoA is an essential cofactor that holds a central role in cell metabolism. Although its biosynthetic pathway is conserved across the three domains of life, the subcellular localization of the eukaryotic biosynthetic enzymes and the mechanism behind the cytosolic and mitochondrial CoA pools compartmentalization are still under debate. In humans, the transport of CoA across the inner mitochondrial membrane has been ascribed to two related genes, SLC25A16 and SLC25A42 whereas in D. melanogaster genome only one gene is present, CG4241, phylogenetically closer to SLC25A42. CG4241 encodes two alternatively spliced isoforms, dPCoAC-A and dPCoAC-B. Both isoforms were expressed in Escherichia coli, but only dPCoAC-A was successfully reconstituted into liposomes, where transported dPCoA and, to a lesser extent, ADP and dADP but not CoA, which was a powerful competitive inhibitor. The expression of both isoforms in a Saccharomyces cerevisiae strain lacking the endogenous putative mitochondrial CoA carrier restored the growth on respiratory carbon sources and the mitochondrial levels of CoA. The results reported here and the proposed subcellular localization of some of the enzymes of the fruit fly CoA biosynthetic pathway, suggest that dPCoA may be synthesized and phosphorylated to CoA in the matrix, but it can also be transported by dPCoAC to the cytosol, where it may be phosphorylated to CoA by the monofunctional dPCoA kinase. Thus, dPCoAC may connect the cytosolic and mitochondrial reactions of the CoA biosynthetic pathway without allowing the two CoA pools to get in contact.

Published

2016

20. Rapamycin reduces oxidative stress in frataxin-deficient yeast cells

Author

L. Palmieri, Isabella Pisano, Francesco M. Lasorsa, Carlo M.T. Marobbio, and Vito Porcelli

Subjects

Saccharomyces cerevisiae, Mitochondrion, medicine.disease_cause, Antioxidants, Stress, Physiological, Iron-Binding Proteins, Mitophagy, medicine, Idebenone, Molecular Biology, Sirolimus, chemistry.chemical_classification, Reactive oxygen species, biology, Autophagy, Cell Biology, Flow Cytometry, Cell biology, Oxidative Stress, Biochemistry, chemistry, Frataxin, biology.protein, Molecular Medicine, TOR Serine-Threonine Kinases, Reactive Oxygen Species, Gene Deletion, Oxidative stress, medicine.drug

Abstract

Friedreich ataxia (FRDA) is a common form of ataxia caused by decreased expression of the mitochondrial protein frataxin. Oxidative damage of mitochondria is thought to play a key role in the pathogenesis of the disease. Therefore, a possible therapeutic strategy should be directed to an antioxidant protection against mitochondrial damage. Indeed, treatment of FRDA patients with the antioxidant idebenone has been shown to improve neurological functions. The yeast frataxin knock-out model of the disease shows mitochondrial iron accumulation, iron-sulfur cluster defects and high sensitivity to oxidative stress. By flow cytometry analysis we studied reactive oxygen species (ROS) production of yeast frataxin mutant cells treated with two antioxidants, N-acetyl-L-cysteine and a mitochondrially-targeted analog of vitamin E, confirming that mitochondria are the main site of ROS production in this model. Furthermore we found a significant reduction of ROS production and a decrease in the mitochondrial mass in mutant cells treated with rapamycin, an inhibitor of TOR kinases, most likely due to autophagy of damaged mitochondria.

Published

2012

21. A new Caucasian case of neonatal intrahepatic cholestasis caused by citrin deficiency (NICCD): A clinical, molecular, and functional study

Author

Giuliano Torre, Alessia Saccari, Ciro Leonardo Pierri, Carlo Dionisi-Vici, Giuseppe Fiermonte, Francesco De Leonardis, Francesco M. Lasorsa, Diego Martinelli, Angelo Vozza, Giovanni Parisi, and Ferdinando Palmieri

Subjects

Male, Models, Molecular, medicine.medical_specialty, Endocrinology, Diabetes and Metabolism, Molecular Sequence Data, Mutation, Missense, Citrin deficiency, Mitochondrial Membrane Transport Proteins, Biochemistry, White People, Endocrinology, Cholestasis, Internal medicine, Genetics, Glutamate aspartate transporter, medicine, Humans, Missense mutation, Amino Acid Sequence, Molecular Biology, Conserved Sequence, Genetic Association Studies, Citrullinemia, Binding Sites, Base Sequence, biology, business.industry, Homozygote, Infant, Sequence Analysis, DNA, Jaundice, medicine.disease, Recombinant Proteins, Protein Structure, Tertiary, Citrin, Galactosuria, biology.protein, medicine.symptom, business, Protein Binding

Abstract

Citrin is the liver-specific isoform of the mitochondrial aspartate/glutamate carrier (AGC2). AGC2 deficiency is an autosomal recessive disorder with two age related phenotypes: neonatal intrahepatic cholestasis (NICCD, OMIM#605814) and adult-onset type II citrullinemia (CTLN2, OMIM#603471). NICCD arises within the first few weeks of life resulting in prolonged cholestasis and metabolic abnormalities including aminoacidemia and galactosuria. Usually symptoms disappear within the first year of life, thus making a diagnosis difficult after this time. In this study we report a new Caucasian case of NICCD, a seven week old Romanian boy with prolonged jaundice. Sequencing of the AGC2 gene showed a novel homozygous missense double-nucleotide (doublet) mutation, which produces the change of the glycine at position 437 into glutamate. Functional studies, carried out on the recombinant mutant protein, for the first time demonstrated, that NICCD is caused by a reduced transport activity of AGC2. The presence of AGC2 deficiency in other ethnic groups besides Asian population suggests further consideration for NICCD diagnosis of any neonate with an unexplained cholestasis; a prompt diagnosis is crucial to resolve the metabolic decompensation with an appropriate dietary treatment.

Published

2011

22. The Insulin-like Growth Factor-I–mTOR Signaling Pathway Induces the Mitochondrial Pyrimidine Nucleotide Carrier to Promote Cell Growth

Author

Edmund R.S. Kunji, Dirk Jan Slotboom, Rosemary O'Connor, Giuseppe Trigiante, Suzanne Floyd, Ferdinando Palmieri, Cedric Favre, Gary Loughran, Madeline Leahy, Alexander Marx, Francesco M. Lasorsa, Katie O'Callaghan, Carlo M.T. Marobbio, and Philipp Stroebel

Subjects

medicine.medical_treatment, Molecular Sequence Data, Uridine Triphosphate, Mitochondrion, Biology, Receptor, IGF Type 1, Mitochondrial Proteins, Mice, Cell Line, Tumor, medicine, Animals, Humans, Insulin, Amino Acid Sequence, Insulin-Like Growth Factor I, RNA, Small Interfering, Molecular Biology, Protein kinase B, PI3K/AKT/mTOR pathway, Cell Line, Transformed, Cell Proliferation, Cell Size, RECEPTOR, IDENTIFICATION, Cell growth, TOR Serine-Threonine Kinases, Growth factor, TRANSPORTER, RPTOR, Biological Transport, Articles, Cell Biology, Fibroblasts, Mitochondrial carrier, CANCER, GENE, Mitochondria, Cell biology, Enzyme Activation, Gene Expression Regulation, Neoplastic, Nucleotide Transport Proteins, Signal transduction, Reactive Oxygen Species, Protein Kinases, Signal Transduction

Abstract

The insulin/insulin-like growth factor (IGF) signaling pathway to mTOR is essential for the survival and growth of normal cells and also contributes to the genesis and progression of cancer. This signaling pathway is linked with regulation of mitochondrial function, but how is incompletely understood. Here we show that IGF-I and insulin induce rapid transcription of the mitochondrial pyrimidine nucleotide carrier PNC1, which shares significant identity with the essential yeast mitochondrial carrier Rim2p. PNC1 expression is dependent on PI-3 kinase and mTOR activity and is higher in transformed fibroblasts, cancer cell lines, and primary prostate cancers than in normal tissues. Overexpression of PNC1 enhances cell size, whereas suppression of PNC1 expression causes reduced cell size and retarded cell cycle progression and proliferation. Cells with reduced PNC1 expression have reduced mitochondrial UTP levels, but while mitochondrial membrane potential and cellular ATP are not altered, cellular ROS levels are increased. Overall the data indicate that PNC1 is a target of the IGF-I/mTOR pathway that is essential for mitochondrial activity in regulating cell growth and proliferation.

Published

2007

23. Inulin‑D‑α-Tocopherol Succinate (INVITE) Nanomicelles as a Platform for Effective Intravenous Administration of Curcumin

Author

Francesco M. Lasorsa, Giuseppe Tripodo, Delia Mandracchia, Anna Mero, Adriana Trapani, Gianfranco Pasut, Giuseppe Trapani, and Theodora Chlapanidas

Subjects

Erythrocytes, Polymers and Plastics, alpha-Tocopherol, Inulin, Bioengineering, Pharmacology, Micelle, Biomaterials, Mice, chemistry.chemical_compound, Drug delivery, curcumin, Pharmacokinetics, In vivo, micelle, Materials Chemistry, Animals, Humans, Vitamin E, pharmacokinetic, Micelles, Drug Carriers, Mice, Inbred BALB C, Chemistry, cell uptake, HEK293 Cells, Biopharmaceutical, Curcumin, Nanoparticles, Administration, Intravenous, Female, Nanocarriers

Abstract

The aim of this work was to evaluate the potential of INVITE-based nanomicelles, an amphiphilic polymer constituted by inulin (INU) and vitamin E (VITE), as a platform for improving the biopharmaceutical properties of hydrophobic drugs. For this purpose, curcumin was selected as a model and curcumin-INVITE nanomicelles were prepared. This drug delivery system was characterized both in vitro for what concerns the physicochemical properties, blood compatibility, and cellular uptake, and in vivo for the evaluation of the pharmacokinetic profile. It was found that these nanomicelles released curcumin in a controlled manner, and they were able to penetrate cellular membrane. Moreover, they showed an improved pharmacokinetic profile after intravenous administration. In conclusion, INVITE micelles might constitute promising nanocarriers for improving the biopharmaceutical performance of hydrophobic drugs.

Published

2015

24. Identification of the Mitochondrial ATP-Mg/Pi Transporter

Author

Ferdinando Palmieri, Simona Todisco, Luigi Palmieri, Giuseppe Fiermonte, Francesco De Leonardis, and Francesco M. Lasorsa

Subjects

chemistry.chemical_classification, Cell Biology, Mitochondrion, Biology, Mitochondrial carrier, Biochemistry, Cell biology, Transport protein, Mitochondrial membrane transport protein, chemistry, Adenine nucleotide, Cytoplasm, Translocase of the inner membrane, biology.protein, Nucleotide, Molecular Biology

Abstract

The mitochondrial carriers are a family of transport proteins that, with a few exceptions, are found in the inner membranes of mitochondria. They shuttle metabolites, nucleotides, and cofactors through this membrane and thereby connect and/or regulate cytoplasm and matrix functions. ATP-Mg is transported in exchange for phosphate, but no protein has ever been associated with this activity. We have isolated three human cDNAs that encode proteins of 458, 468, and 489 amino acids with 66–75% similarity and with the characteristic features of the mitochondrial carrier family in their C-terminal domains and three EF-hand Ca2+-binding motifs in their N-terminal domains. These proteins have been overexpressed in Escherichia coli and reconstituted into phospholipid vesicles. Their transport properties and their targeting to mitochondria demonstrate that they are isoforms of the ATP-Mg/Pi carrier described in the past in whole mitochondria. The tissue specificity of the three isoforms shows that at least one isoform was present in all of the tissues investigated. Because phosphate recycles via the phosphate carrier in mitochondria, the three isoforms of the ATP-Mg/Pi carrier are most likely responsible for the net uptake or efflux of adenine nucleotides into or from the mitochondria and hence for the variation in the matrix adenine nucleotide content, which has been found to change in many physiopathological situations.

Published

2004

25. UCP2 exports C4 metabolites out of mitochondria in exchange for phosphate

Author

Francesco De Leonardis, Daniela Amorese, Luigi Palmieri, Francesco M. Lasorsa, Angelo Vozza, Alessandra Castegna, Pasquale Scarcia, Frédéric Bouillaud, Daniel Ricquier, Giovanni Parisi, Giuseppe Fiermonte, Ferdinando Palmieri, and Eleonora Paradies

Subjects

chemistry.chemical_compound, Biochemistry, Chemistry, Biophysics, Cell Biology, Mitochondrion, Phosphate

Published

2014

26. Erratum to: AGC1 Deficiency Causes Infantile Epilepsy, Abnormal Myelination, and Reduced N-Acetylaspartate

Author

Giulia Giannuzzi, Cuiping Hou, Ferdinando Palmieri, Cecilia E. Kim, Yiran Guo, Emily Place, Xiaowu Gai, Marni J. Falk, Lifeng Tian, Lyam Vazquez, Nada Abdel-Magid, Hui Jiang, Elizabeth M. McCormick, Hakon Hakonarson, Francesco M. Lasorsa, Jinlong Liang, Rosetta M. Chiavacci, Frederick G. Otieno, Frank D. Mentch, Dong Li, Eric D. Marsh, and Xuanzhu Liu

Subjects

Pediatrics, medicine.medical_specialty, AGC1 Deficiency, business.industry, Published Erratum, Abnormal myelination, MEDLINE, Infantile epilepsy, Data science, Human genetics, Article, Medicine, business, N-acetylaspartate

Abstract

Whole exome sequencing (WES) offers a powerful diagnostic tool to rapidly and efficiently sequence all coding genes in individuals presenting for consideration of phenotypically and genetically heterogeneous disorders such as suspected mitochondrial disease. Here, we report results of WES and functional validation in a consanguineous Indian kindred where two siblings presented with profound developmental delay, congenital hypotonia, refractory epilepsy, abnormal myelination, fluctuating basal ganglia changes, cerebral atrophy, and reduced N-acetylaspartate (NAA).Whole blood DNA from one affected and one unaffected sibling was captured by Agilent SureSelect Human All Exon kit and sequenced on the Illumina HiSeq2000. Mutations were validated by Sanger sequencing in all family members. Protein from wild-type and mutant fibroblasts was isolated to assess mutation effects on protein expression and enzyme activity.A novel SLC25A12 homozygous missense mutation, c.1058GA; p.Arg353Gln, segregated with disease in this kindred. SLC25A12 encodes the neuronal aspartate-glutamate carrier 1 (AGC1) protein, an essential component of the neuronal malate/aspartate shuttle that transfers NADH and H(+) reducing equivalents from the cytosol to mitochondria. AGC1 activity enables neuronal export of aspartate, the glial substrate necessary for proper neuronal myelination. Recombinant mutant p.Arg353Gln AGC1 activity was reduced to 15% of wild type. One prior reported SLC25A12 mutation caused complete loss of AGC1 activity in a child with epilepsy, hypotonia, hypomyelination, and reduced brain NAA.These data strongly suggest that SLC25A12 disease impairs neuronal AGC1 activity. SLC25A12 sequencing should be considered in children with infantile epilepsy, congenital hypotonia, global delay, abnormal myelination, and reduced brain NAA.

Published

2014

27. Translocator protein ligand-PLGA conjugated nanoparticles for 5-fluorouracil delivery to glioma cancer cells

Author

Francesco M. Lasorsa, Valentino Laquintana, Giulia Agostino, Nunzio Denora, Annalisa Cutrignelli, Angela Lopedota, Antonio Lopalco, and Massimo Franco

Subjects

Drug, Antimetabolites, Antineoplastic, media_common.quotation_subject, Pharmaceutical Science, Apoptosis, macromolecular substances, Conjugated system, chemistry.chemical_compound, Drug Delivery Systems, Polylactic Acid-Polyglycolic Acid Copolymer, Drug Discovery, Translocator protein, Tumor Cells, Cultured, Distribution (pharmacology), Humans, Tissue Distribution, Lactic Acid, media_common, Cell Proliferation, Drug Carriers, biology, Calorimetry, Differential Scanning, Chemistry, technology, industry, and agriculture, Glioma, Receptors, GABA-A, PLGA, Biochemistry, Targeted drug delivery, Microscopy, Fluorescence, Drug delivery, Cancer cell, biology.protein, Biophysics, Molecular Medicine, Nanoparticles, Fluorouracil, Carrier Proteins, Polyglycolic Acid

Abstract

Translocator protein 18 kDa (TSPO) is a promising target for molecular imaging and for targeted drug delivery to tumors overexpressing TSPO. In our previous work, new macromolecular conjugates with a high affinity and selectivity for TSPO were prepared by conjugating the biodegradable poly(d,l-lactic-co-glycolic acid) (PLGA) polymer with two potent and selective TSPO ligands, namely, compounds 1 and 2. Based on this, nanoparticle delivery systems (NPs), employing TSPO ligand-PLGA conjugated (PLGA-TSPO) polymers, were prepared. Furthermore, to evaluate the ability of the new NPs to be used as a drug delivery systems for anticancer therapy, PLGA-TSPO NPs were loaded with 5-fluorouracil (5-FU), chosen as a model hydrophilic anticancer drug. The main goal of this work was to investigate the synergistic potential of using NP conjugates PLGA-TSPO, TSPO ligands being pro-apoptotic agents, to simultaneously deliver a cytotoxic anticancer drug. To better highlight the occurrence of synergistic effects, dual drug loaded PLGA NPs (PLGA NPs/5-FU/1) and dual drug loaded PLGA-TSPO NPs (PLGA-TSPO NPs/5-FU/1), with 5-FU and TSPO ligand 1 physically incorporated together, were also prepared and characterized. The particle size and size distribution, surface morphology, and drug encapsulation efficiency, as well as the drug release kinetics, were investigated. In vitro cytotoxicity studies were carried out on C6 glioma cells overexpressing TSPO, and to evaluate the potential uptake of these nanoparticulate systems, the internalization of fluorescent labeled PLGA-TSPO NPs (FITC-PLGA-TSPO NPs) was also investigated by fluorescence microscopy. Results demonstrated that PLGA-TSPO NPs/5-FU and dual drug loaded PLGA NPs/5-FU/1 and PLGA-TSPO NPs/5-FU/1 could significantly enhance toxicity against human cancer cells due to the synergistic effect of the TSPO ligand 1 with the anticancer drug 5-FU.

Published

2014

28. AGC1 Deficiency Causes Infantile Epilepsy, Abnormal Myelination, and Reduced N-Acetylaspartate

Author

Cecilia E. Kim, Xiaowu Gai, Ferdinando Palmieri, Cuiping Hou, Lyam Vazquez, Eric D. Marsh, Rosetta M. Chiavacci, Nada Abdel-Magid, Jinlong Liang, Frederick G. Otieno, Marni J. Falk, Giulia Giannuzzi, Xuanzhu Liu, Guo Yiran, Hakon Hakonarson, Elizabeth M. McCormick, Francesco M. Lasorsa, Hui Jiang, Dong Li, Frank D. Mentch, Emily Place, and Lifeng Tian

Subjects

Cerebral atrophy, AGC1 Deficiency, Genetic heterogeneity, medicine.medical_treatment, Mitochondrial disease, Basal ganglia, Abnormal myelination, medicine, Biology, medicine.disease, Bioinformatics, Exome sequencing, Ketogenic diet

Abstract

Background: Whole exome sequencing (WES) offers a powerful diagnostic tool to rapidly and efficiently sequence all coding genes in individuals presenting for consideration of phenotypically and genetically heterogeneous disorders such as suspected mitochondrial disease. Here, we report results of WES and functional validation in a consanguineous Indian kindred where two siblings presented with profound developmental delay, congenital hypotonia, refractory epilepsy, abnormal myelination, fluctuating basal ganglia changes, cerebral atrophy, and reduced N-acetylaspartate (NAA).

Published

2014

29. Perturbed mitochondrial Ca2+ signals as causes or consequences of mitophagy induction

Author

Paolo Pinton, Simone Patergnani, Saverio Marchi, Massimo Bonora, Alessandro Rimessi, Carlo M.T. Marobbio, and Francesco M. Lasorsa

Subjects

Membrane Potential, Mitochondrial, Endoplasmic reticulum, Autophagy, Mitophagy, Cell Biology, Mitochondrion, Biology, Endoplasmic Reticulum, Yeast, Cell biology, Mitochondria, Crosstalk (biology), mitochondrial fusion, DNAJA3, Animals, Humans, Mitochondrial fission, Mitochondrial membrane potential, Calcium Signaling, Mitochondrial structure, Reactive Oxygen Species, Molecular Biology, Reactive oxygen species

Abstract

Mitophagy is an essential process that maintains mitochondrial quality and number, thus limiting cellular degeneration. Along with apoptosis, mitophagy participates in cellular fate decisions by eliminating damaged mitochondria. A variety of mitochondrial parameters, such as structure, membrane potential, and reactive oxygen species, are key determinants in triggering the mitophagic machinery. These parameters are also important regulators of the mitochondrial capacity for calcium (Ca (2+)) uptake. Rapid Ca (2+) accumulation in the mitochondrial matrix allows for prompt stimulation of the organelle. This process requires a close morphofunctional coupling between mitochondria and the main intracellular Ca (2+) stores. In mitophagy, the role of Ca (2+) remains obscure. What role does mitochondrial Ca (2+) play in metabolic sensing or in mitochondrial remodeling? Is endoplasmic reticulum (ER)-Ca (2+) crosstalk involved? These are some of the questions that we address in this review.

Published

2013

30. Down-regulation of mitochondrial aspartate/glutamate carrier isoform 1 in Neuro2A cells inhibits cell proliferation and N-acetyl-aspartate synthesis

Author

Alberto Danese, Luigi Sbano, Sabrina Petralla, Paolo Pinton, Carlotta Giorgi, Luigi Palmieri, Carlo Viscomi, Alessandra Castegna, Gennaro Agrimi, Vito Porcelli, Luis Emiliano Peña-Altamira, Barbara Monti, Emanuela Profilo, Giulia Giannuzzi, Ferdinando Palmieri, Mariangela Corricelli, Massimo Zeviani, and Francesco M. Lasorsa

Subjects

Gene isoform, Downregulation and upregulation, biology, Biochemistry, Cell growth, Chemistry, Biophysics, Glutamate aspartate transporter, biology.protein, Cell Biology, N acetyl aspartate

Published

2016

31. Mitochondrial Glutamate Carrier GC1 as a Newly Identified Player in the Control of Glucose-stimulated Insulin Secretion*

Author

Marina Shamini Casimir, Blanca Rubi, Dorothée Caille, Francesco M. Lasorsa, Paolo Meda, Ferdinando Palmieri, and Pierre Maechler

Subjects

genetic structures, medicine.medical_treatment, Membrane Transport Proteins/metabolism/physiology, Mitochondrion, RNA, Small Interfering/metabolism, Biochemistry, Mitochondrial Membrane Transport Proteins, Mice, Insulin-Secreting Cells, Insulin Secretion, Glucose/metabolism, Insulin, REGULATED ANAPLEROSIS, RNA, Small Interfering, Inner mitochondrial membrane, TISSUE DISTRIBUTION, biology, Membrane transport protein, Glutamate receptor, Immunohistochemistry, Mitochondria, Metabolism and Bioenergetics, Insulin/metabolism/secretion, Glutamate dehydrogenase 1, Glutamic Acid/metabolism, endocrine system, Glutamic Acid, Models, Biological, Cell Line, Mitochondrial Proteins/metabolism/physiology, Mitochondrial Proteins, Mitochondrial membrane transport protein, Insulin-Secreting Cells/metabolism, Mitochondria/metabolism, medicine, Animals, Humans, Gene Silencing, ddc:612, Molecular Biology, Membrane Transport Proteins, Cell Biology, Glutamic acid, Molecular biology, PANCREATIC BETA-CELLS, FUNCTIONAL-CHARACTERIZATION, Rats, Kinetics, BACTERIAL EXPRESSION, Glucose, biology.protein

Abstract

The SLC25 carrier family mediates solute transport across the inner mitochondrial membrane, a process that is still poorly characterized regarding both the mechanisms and proteins implicated. This study investigated mitochondrial glutamate carrier GC1 in insulin-secreting beta-cells. GC1 was cloned from insulin-secreting cells, and sequence analysis revealed hydropathy profile of a six-transmembrane protein, characteristic of mitochondrial solute carriers. GC1 was found to be expressed at the mRNA and protein levels in INS-1E beta-cells and pancreatic rat islets. Immunohistochemistry showed that GC1 was present in mitochondria, and ultrastructural analysis by electron microscopy revealed inner mitochondrial membrane localization of the transporter. Silencing of GC1 in INS-1E beta-cells, mediated by adenoviral delivery of short hairpin RNA, reduced mitochondrial glutamate transport by 48% (p < 0.001). Insulin secretion at basal 2.5 mM glucose and stimulated either by intermediate 7.5 mM glucose or non-nutrient 30 mM KCl was not modified by GC1 silencing. Conversely, insulin secretion stimulated with optimal 15 mM glucose was reduced by 23% (p < 0.005) in GC1 knocked down cells compared with controls. Adjunct of cell-permeant glutamate (5 mM dimethyl glutamate) fully restored the secretory response at 15 mM glucose (p < 0.005). Kinetics of insulin secretion were investigated in peri-fused isolated rat islets. GC1 silencing in islets inhibited the secretory response induced by 16.7 mM glucose, both during first (-25%, p < 0.05) and second (-33%, p < 0.05) phases. This study demonstrates that insulin-secreting cells depend on GC1 for maximal glucose response, thereby assigning a physiological function to this newly identified mitochondrial glutamate carrier.

Published

2009

32. Peroxisomes as novel players in cell calcium homeostasis

Author

Luigi Palmieri, Hanspeter Rottensteiner, Pasquale Scarcia, Francesco M. Lasorsa, Paolo Pinton, Rosario Rizzuto, and Ferdinando Palmieri

Subjects

Vacuolar Proton-Translocating ATPases, peroxisome, calcium homeostasis, Aequorin, Green Fluorescent Protein, mithocondria, ENDOPLASMIC-RETICULUM, GREEN FLUORESCENT PROTEINS, Biology, Biochemistry, TARGETED RECOMBINANT AEQUORIN, Chlorocebus aethiops, Peroxisomes, Animals, Homeostasis, Humans, Molecular Biology, Ion transporter, Ion Transport, Peroxisomal matrix, Endoplasmic reticulum, Sodium, Mechanisms of Signal Transduction, Cell Biology, Intracellular Membranes, Peroxisome, Cell biology, Cytosol, MITOCHONDRIAL CA2+ HOMEOSTASIS, COS Cells, biology.protein, Calcium, Protons, Intracellular, perossisomes

Abstract

Ca2+ concentration in peroxisomal matrix ([Ca2+](perox)) has been monitored dynamically in mammalian cells expressing variants of Ca2+-sensitive aequorin specifically targeted to peroxisomes. Upon stimulation with agonists that induce Ca2+ release from intracellular stores, peroxisomes transiently take up Ca2+ reaching peak values in the lumen as high as 50-100 microm, depending on cell types. Also in resting cells, peroxisomes sustain a Ca2+ gradient, [Ca2+](perox) being approximately 20-fold higher than [Ca2+] in the cytosol ([Ca2+](cyt)). The properties of Ca2+ traffic across the peroxisomal membrane are different from those reported for other subcellular organelles. The sensitivity of peroxisomal Ca2+ uptake to agents dissipating H+ and Na+ gradients unravels the existence of a complex bioenergetic framework including V-ATPase, Ca2+/H+, and Ca2+/Na+ activities whose components are yet to be identified at a molecular level. The different [Ca2+](perox) of resting and stimulated cells suggest that Ca2+ could play an important role in the regulation of peroxisomal metabolism.

Published

2008

33. Identification of the human mitochondrial S adenosylmethionine transporter: bacterial expression, reconstitution, functional characterization and tissue distribution

Author

Ferdinando Palmieri, Gennaro Agrimi, Francesco M. Lasorsa, Carlo M.T. Marobbio, Giuseppe Fiermonte, and M. A. Di Noia

Subjects

mitochondrial carrier, S-Adenosylmethionine, Amino Acid Transport Systems, Mitochondrion, Biochemistry, chemistry.chemical_compound, Cytosol, Cricetinae, Bromcresol Purple, Cloning, Molecular, Phylogeny, Expressed Sequence Tags, biology, S-Adenosylhomocysteine, Hydrolyzable Tannins, Transport protein, Cell biology, mitochondria, Organ Specificity, Research Article, DNA, Complementary, Recombinant Fusion Proteins, Molecular Sequence Data, Nerve Tissue Proteins, CHO Cells, Mitochondrial Proteins, Mitochondrial membrane transport protein, proteomics, Complementary DNA, Membrane Transport Modulators, Escherichia coli, Animals, Humans, Amino Acid Sequence, RNA, Messenger, Molecular Biology, Brain Chemistry, Sequence Homology, Amino Acid, Calcium-Binding Proteins, RNA, Membrane Transport Proteins, Biological Transport, Cell Biology, Mitochondrial carrier, S-adenosylmethionine carrier, chemistry, Genes, transport, biology.protein, Sequence Alignment, DNA

Abstract

The mitochondrial carriers are a family of transport proteins that, with a few exceptions, are found in the inner membranes of mitochondria. They shuttle metabolites and cofactors through this membrane, and connect cytoplasmic functions with others in the matrix. SAM (S-adenosylmethionine) has to be transported into the mitochondria where it is converted into S-adenosylhomocysteine in methylation reactions of DNA, RNA and proteins. The transport of SAM has been investigated in rat liver mitochondria, but no protein has ever been associated with this activity. By using information derived from the phylogenetically distant yeast mitochondrial carrier for SAM and from related human expressed sequence tags, a human cDNA sequence was completed. This sequence was overexpressed in bacteria, and its product was purified, reconstituted into phospholipid vesicles and identified from its transport properties as the human mitochondrial SAM carrier (SAMC). Unlike the yeast orthologue, SAMC catalysed virtually only countertransport, exhibited a higher transport affinity for SAM and was strongly inhibited by tannic acid and Bromocresol Purple. SAMC was found to be expressed in all human tissues examined and was localized to the mitochondria. The physiological role of SAMC is probably to exchange cytosolic SAM for mitochondrial S-adenosylhomocysteine. This is the first report describing the identification and characterization of the human SAMC and its gene.

Published

2004

34. The yeast peroxisomal adenine nucleotide transporter: characterization of two transport modes and involvement inƒn„ÁpH formation across peroxisomal membranes

Author

Pasquale Scarcia, Ralf Erdmann, Luigi Palmieri, Ferdinando Palmieri, Hanspeter Rottensteiner, and Francesco M. Lasorsa

Subjects

microscopic fluorescence imaging, Saccharomyces cerevisiae Proteins, Saccharomyces cerevisiae, Biological Transport, Active, Accelerated Publication, Biology, bioenergetics, Biochemistry, Green fluorescent protein, Cytosol, Adenine nucleotide, Peroxisomes, Nucleotide, peroxisome, Molecular Biology, chemistry.chemical_classification, Adenine Nucleotides, Chemiosmosis, Proton-Motive Force, Intracellular Membranes, Cell Biology, Hydrogen-Ion Concentration, Peroxisome, biology.organism_classification, Nucleotide Transport Proteins, chemistry, adenine nucleotide transport, mitochondrial carrier family

Abstract

The yeast peroxisomal adenine nucleotide carrier, Ant1p, was shown to catalyse unidirectional transport in addition to exchange of substrates. In both transport modes, proton movement occurs. Nucleotide hetero-exchange is H+-compensated and electroneutral. Furthermore, microscopic fluorescence imaging of a pH-sensitive green fluorescent protein targeted to peroxisomes shows that Ant1p is involved in the formation of a ΔpH across the peroxisomal membrane, acidic inside.

Published

2004

35. Recombinant expression of the Ca(2+)-sensitive aspartate/glutamate carrier increases mitochondrial ATP production in agonist-stimulated Chinese hamster ovary cells

Author

Rosario Rizzuto, Paolo Pinton, Luigi Palmieri, Giuseppe Fiermonte, Francesco M. Lasorsa, and Ferdinando Palmieri

Subjects

Blotting, Western, Molecular Sequence Data, Glutamic Acid, Organic Anion Transporters, CHO Cells, Mitochondrion, Transfection, Biochemistry, Mitochondrial Membrane Transport Proteins, Mitochondrial Proteins, Mitochondrial membrane transport protein, Adenosine Triphosphate, Aequorin, Cytosol, Cricetinae, Glutamate aspartate transporter, Animals, Humans, Luciferases, Molecular Biology, Aspartic Acid, Binding Sites, biology, Chinese hamster ovary cell, Calcium-Binding Proteins, Cell Membrane, Membrane Transport Proteins, Cell Biology, Recombinant Proteins, Mitochondria, Protein Structure, Tertiary, Oxygen, Spectrometry, Fluorescence, Citrin, Microscopy, Fluorescence, Mitochondrial matrix, Luminescent Measurements, biology.protein, Calcium, Plasmids

Abstract

The Ca(2+)-sensitive dehydrogenases of the mitochondrial matrix are, so far, the only known effectors to allow Ca2+ signals to couple the activation of plasma membrane receptors to the stimulation of aerobic metabolism. In this study, we demonstrate a novel mechanism, based on Ca(2+)-sensitive metabolite carriers of the inner membrane. We expressed in Chinese hamster ovary cells aralar1 and citrin, aspartate/glutamate exchangers that have Ca(2+)-binding sites in their sequence, and measured mitochondrial Ca2+ and ATP levels as well as cytosolic Ca2+ concentration with targeted recombinant probes. The increase in mitochondrial ATP levels caused by cell stimulation with Ca(2+)-mobilizing agonists was markedly larger in cells expressing aralar and citrin (but not truncated mutants lacking the Ca(2+)-binding site) than in control cells. Conversely, the cytosolic and the mitochondrial Ca2+ signals were the same in control cells and cells expressing the different aralar1 and citrin variants, thus ruling out an indirect effect through the Ca(2+)-sensitive dehydrogenases. Together, these data show that the decoding of Ca2+ signals in mitochondria depends on the coordinate activity of mitochondrial enzymes and carriers, which may thus represent useful pharmacological targets in this process of major pathophysiological interest.

Published

2003

36. A novel mutation in the SLC25A12 gene causing mitochondrial aspartate/glutamate carrier 1 (AGC1) deficiency

Author

Marni J. Falk, Frederick G. Otieno, Lyam Vazquez, Emily Place, Elizabeth M. McCormick, Rosetta M. Chiavacci, Xiaowu Gai, Lifeng Tian, Frank D. Mentch, Hui Jiang, Nada Abdel-Magid, Eric D. Marsh, Ferdinando Palmieri, Cecilia E. Kim, Yiran Guo, Giuseppe Fiermonte, Dong Li, Giulia Giannuzzi, Francesco M. Lasorsa, Xuanzhu Liu, Hakon Hakonarson, Jinlong Liang, and Cuiping Hou

Subjects

AGC1 Deficiency, biology, Chemistry, Biophysics, Glutamate aspartate transporter, biology.protein, Cell Biology, Biochemistry, Novel mutation, Molecular biology, Gene

Published

2014

37. Erratum to 'The Saccharomyces cerevisiae gene YPR011c encodes a mitochondrial transporter of adenosine 5′-phosphosulfate and 3′-phospho-adenosine 5′-phosphosulfate' [Biochim. Biophys. Acta Bioenerg. (2014): 326, 334]

Author

Eleonora Paradies, Ferdinando Palmieri, Simona Todisco, Maria Antonietta Di Noia, Francesco M. Lasorsa, and Alessandra Castegna

Subjects

Biochemistry, biology, Bioenergetics, Saccharomyces cerevisiae, Biophysics, medicine, Transporter, Cell Biology, biology.organism_classification, Adenosine, Gene, medicine.drug

Published

2014

38. Citrin and aralar1 are Ca(2+)-stimulated aspartate/glutamate transporters in mitochondria

Author

Ferdinando Palmieri, Jorgina Satrústegui, Mikio Iijima, Beatriz Pardo, Michael J. Runswick, Takeyori Saheki, A. del Arco, Keiko Kobayashi, Luigi Palmieri, John E. Walker, and Francesco M. Lasorsa

Subjects

endocrine system diseases, Amino Acid Transport Systems, Acidic, Proteolipids, Malate-aspartate shuttle, Organic Anion Transporters, Transfection, Mitochondrial Membrane Transport Proteins, General Biochemistry, Genetics and Molecular Biology, Antiporters, Article, Cell Line, Mitochondrial Proteins, Mitochondrial membrane transport protein, Glutamate aspartate transporter, Escherichia coli, Humans, Inner mitochondrial membrane, Molecular Biology, Citrullinemia, General Immunology and Microbiology, biology, General Neuroscience, Calcium-Binding Proteins, Glutamate receptor, nutritional and metabolic diseases, Membrane Transport Proteins, Mitochondrial carrier, Mitochondria, Aspartate carbamoyltransferase, Kinetics, Citrin, Biochemistry, Models, Chemical, biology.protein, Calcium, Carrier Proteins, hormones, hormone substitutes, and hormone antagonists

Abstract

The mitochondrial aspartate/glutamate carrier catalyzes an important step in both the urea cycle and the aspartate/malate NADH shuttle. Citrin and aralar1 are homologous proteins belonging to the mitochondrial carrier family with EF-hand Ca(2+)-binding motifs in their N-terminal domains. Both proteins and their C-terminal domains were overexpressed in Escherichia coli, reconstituted into liposomes and shown to catalyze the electrogenic exchange of aspartate for glutamate and a H(+). Overexpression of the carriers in transfected human cells increased the activity of the malate/aspartate NADH shuttle. These results demonstrate that citrin and aralar1 are isoforms of the hitherto unidentified aspartate/glutamate carrier and explain why mutations in citrin cause type II citrullinemia in humans. The activity of citrin and aralar1 as aspartate/glutamate exchangers was stimulated by Ca(2+) on the external side of the inner mitochondrial membrane, where the Ca(2+)-binding domains of these proteins are localized. These results show that the aspartate/glutamate carrier is regulated by Ca(2+) through a mechanism independent of Ca(2+) entry into mitochondria, and suggest a novel mechanism of Ca(2+) regulation of the aspartate/malate shuttle.

Published

2001

39. Identification and functions of new transporters in yeast mitochondria

Author

John E. Walker, Francesco M. Lasorsa, Luigi Palmieri, Ferdinando Palmieri, Angelo Vozza, Gennaro Agrimi, Michael J. Runswick, and Giuseppe Fiermonte

Subjects

Overexpression, Saccharomyces cerevisiae, Biophysics, Transport, Mitochondrion, medicine.disease_cause, Gene, Genome, Biochemistry, Antiporters, Mitochondrial membrane transport protein, Bacterial Proteins, medicine, Escherichia coli, Animals, Humans, Cloning, Molecular, Caenorhabditis elegans, Dicarboxylic Acid Transporters, biology, Escherichia coli Proteins, Membrane Proteins, Membrane Transport Proteins, Cell Biology, Intracellular Membranes, biology.organism_classification, Mitochondrial carrier, Yeast, Mitochondria, Metabolism, Carnitine Acyltransferases, biology.protein, Amino Acid Transport Systems, Basic, Carrier, Carrier Proteins

Abstract

The genome of Saccharomyces cerevisiae encodes 35 putative members of the mitochondrial carrier family. Known members of this family transport substrates and products across the inner membranes of mitochondria. We are attempting to identify the functions of the yeast mitochondrial transporters via high-yield expression in Escherichia coli and/or S. cerevisiae, purification and reconstitution of their protein products into liposomes, where their transport properties are investigated. With this strategy, we have already identified the functions of seven S. cerevisiae gene products, whose structural and functional properties assigned them to the mitochondrial carrier family. The functional information obtained in the reconstituted system and the use of knock-out yeast strains can be usefully exploited for the investigation of the physiological role of individual transporters. Furthermore, the yeast carrier sequences can be used to identify the orthologous proteins in other organisms, including man.

Published

2000

40. Identification of the mitochondrial carnitine carrier in Saccharomyces cerevisiae

Author

Luigi Palmieri, Michael J. Runswick, Francesco M. Lasorsa, Ferdinando Palmieri, Vito Iacobazzi, and John E. Walker

Subjects

Saccharomyces cerevisiae Proteins, Time Factors, Amino Acid Transport Systems, Saccharomyces cerevisiae, Molecular Sequence Data, Biophysics, Transport, Mitochondrion, Biochemistry, Chromatography, Affinity, Substrate Specificity, Mitochondrial Proteins, Affinity chromatography, Structural Biology, Carnitine, Genetics, medicine, Acetylcarnitine, Molecular Biology, Mitochondrial transport, CRC1 gene, biology, YOR100c, Cell Biology, Mitochondrial carrier, biology.organism_classification, Yeast, Recombinant Proteins, Mitochondria, Kinetics, Carrier Proteins, Carnitine carrier, medicine.drug

Abstract

The mitochondrial carrier protein for carnitine has been identified in Saccharomyces cerevisiae. It is encoded by the gene CRC1 and is a member of the family of mitochondrial transport proteins. The protein has been over-expressed with a C-terminal His-tag in S. cerevisiae and isolated from mitochondria by nickel affinity chromatography. The purified protein has been reconstituted into proteoliposomes and its transport characteristics established. It transports carnitine, acetylcarnitine, propionylcarnitine and to a much lower extent medium- and long-chain acylcarnitines.

Published

2000

41. Identification of the yeast ACR1 gene product as a succinate-fumarate transporter essential for growth on ethanol or acetate

Author

Annalisa De Palma, Ferdinando Palmieri, Luigi Palmieri, Michael J. Runswick, Francesco M. Lasorsa, and John E. Walker

Subjects

Recombinant Fusion Proteins, Saccharomyces cerevisiae, Genetic Vectors, Biophysics, Succinic Acid, Transport, Acetates, medicine.disease_cause, Biochemistry, Yeast mitochondrion, Substrate Specificity, Fungal Proteins, Fumarates, Structural Biology, Genetics, medicine, Escherichia coli, Molecular Biology, Expression vector, biology, Ethanol, Succinate-fumarate exchange, Cell Biology, Isocitrate lyase, Fumarate reductase, biology.organism_classification, Yeast, Cytosol, Kinetics, Mitochondrial matrix, ACR1 gene, Carrier Proteins

Abstract

The protein encoded by the ACR1 gene in Saccharomyces cerevisiae belongs to a family of 35 related membrane proteins that are encoded in the fungal genome. Some of them are known to transport various substrates and products across the inner membranes of mitochondria, but the functions of 28 members of the family are unknown. The yeast ACR1 gene was introduced into Escherichia coli on an expression plasmid. The protein was over-produced as inclusion bodies, which were purified and solubilised in the presence of sarkosyl. The solubilised protein was reconstituted into liposomes and shown to transport fumarate and succinate. Its physiological role in S. cerevisiae is probably to transport cytoplasmic succinate, derived from isocitrate by the action of isocitrate lyase in the cytosol, into the mitochondrial matrix in exchange for fumarate. This exchange activity and the subsequent conversion of fumarate to oxaloacetate in the cytosol would be essential for the growth of S. cerevisiae on ethanol or acetate as the sole carbon source.

Published

1997

42. The Saccharomyces cerevisiae gene YPR011c encodes a mitochondrial transporter of adenosine 5′-phosphosulfate and 3′-phospho-adenosine 5′-phosphosulfate

Author

Maria Antonietta Di Noia, Francesco M. Lasorsa, Ferdinando Palmieri, Eleonora Paradies, Alessandra Castegna, and Simona Todisco

Subjects

Thermotolerance, Mitochondrial carrier, Saccharomyces cerevisiae Proteins, Coenzyme A, Mutant, Saccharomyces cerevisiae, Genes, Fungal, Phosphoadenosine Phosphosulfate, Biophysics, Mitochondrion, Biology, Transporter, Biochemistry, Substrate Specificity, chemistry.chemical_compound, Methionine, Adenosine 5′-phosphosulfate, medicine, Escherichia coli, Mitochondrial transport, Genetic Complementation Test, Temperature, Biological Transport, Cell Biology, biology.organism_classification, Adenosine, Adaptation, Physiological, Glutathione, Recombinant Proteins, Adenosine Phosphosulfate, Mitochondria, Kinetics, chemistry, Mutant Proteins, medicine.drug

Abstract

The genome of Saccharomyces cerevisiae contains 35 members of the mitochondrial carrier family, nearly all of which have been functionally characterized. In this study, the identification of the mitochondrial carrier for adenosine 5′-phosphosulfate (APS) is described. The corresponding gene (YPR011c) was overexpressed in bacteria. The purified protein was reconstituted into phospholipid vesicles and its transport properties and kinetic parameters were characterized. It transported APS, 3′-phospho-adenosine 5′-phosphosulfate, sulfate and phosphate almost exclusively by a counter-exchange mechanism. Transport was saturable and inhibited by bongkrekic acid and other inhibitors. To investigate the physiological significance of this carrier in S. cerevisiae, mutants were subjected to thermal shock at 45°C in the presence of sulfate and in the absence of methionine. At 45°C cells lacking YPR011c, engineered cells (in which APS is produced only in mitochondria) and more so the latter cells, in which the exit of mitochondrial APS is prevented by the absence of YPR011cp, were less thermotolerant. Moreover, at the same temperature all these cells contained less methionine and total glutathione than wild-type cells. Our results show that S. cerevisiae mitochondria are equipped with a transporter for APS and that YPR011cp-mediated mitochondrial transport of APS occurs in S. cerevisiae under thermal stress conditions.

43. S8.6 Role of peroxisomes in cell calcium homeostasis

Author

Rosario Rizzuto, Francesco M. Lasorsa, Paolo Pinton, Ferdinando Palmieri, Luigi Palmieri, and Pasquale Scarcia

Subjects

Calcium metabolism, Chemistry, Biophysics, Cell Biology, Peroxisome, Human homeostasis, Biochemistry, Cell biology