Your search keyword '"Colin H. Lipper"' showing total 7 results

1. Redox-dependent gating of VDAC by mitoNEET

Author

Rachel Nechushtai, Colin H. Lipper, Ron Mittler, Fang Bai, Patricia A. Jennings, Susmita Roy, José N. Onuchic, Sohn Yang-Sung, and Jason T. Stofleth

Subjects

0301 basic medicine, Iron-Sulfur Proteins, Secondary, 2'-Disulfonic Acid, Protein Conformation, 2-Disulfonic Acid, Mitochondria, Liver, Apoptosis, Gating, Mitochondrion, 4,4'-Diisothiocyanostilbene-2,2'-Disulfonic Acid, Protein Structure, Secondary, chemistry.chemical_compound, 0302 clinical medicine, Protein Interaction Mapping, Homeostasis, chemistry.chemical_classification, Multidisciplinary, biology, Neurodegeneration, Biological Sciences, Recombinant Proteins, Cell biology, Mitochondria, CISD1, VDAC1, Liver, DIDS, Mitochondrial Membranes, Dimyristoylphosphatidylcholine, Oxidation-Reduction, Protein Structure, Voltage-dependent anion channel, Iron, Mitochondrial Proteins, 03 medical and health sciences, direct coupling, medicine, Animals, Humans, Ferroptosis, Reactive oxygen species, Sheep, Binding Sites, 4-Diisothiocyanostilbene-2, Voltage-Dependent Anion Channel 1, medicine.disease, Oxygen, Cytosol, Biophysics and Computational Biology, Kinetics, 030104 developmental biology, chemistry, mitoNEET, biology.protein, 4'-Diisothiocyanostilbene-2, Protein Multimerization, 030217 neurology & neurosurgery

Abstract

Significance This work demonstrates that the outer mitochondrial-anchored [2Fe-2S] mitoNEET is able to bind within the central cavity of the voltage-dependent anion channel (VDAC) and regulate its gating in a redox-dependent manner. These findings have implications for ferroptosis, apoptosis, and iron metabolism by linking VDAC function, mitoNEET, and the redox environment of the cell. Furthermore, these findings introduce a potential player to the many mechanisms that may alter VDAC’s governance in times of homeostasis or strife., MitoNEET is an outer mitochondrial membrane protein essential for sensing and regulation of iron and reactive oxygen species (ROS) homeostasis. It is a key player in multiple human maladies including diabetes, cancer, neurodegeneration, and Parkinson’s diseases. In healthy cells, mitoNEET receives its clusters from the mitochondrion and transfers them to acceptor proteins in a process that could be altered by drugs or during illness. Here, we report that mitoNEET regulates the outer-mitochondrial membrane (OMM) protein voltage-dependent anion channel 1 (VDAC1). VDAC1 is a crucial player in the cross talk between the mitochondria and the cytosol. VDAC proteins function to regulate metabolites, ions, ROS, and fatty acid transport, as well as function as a “governator” sentry for the transport of metabolites and ions between the cytosol and the mitochondria. We find that the redox-sensitive [2Fe-2S] cluster protein mitoNEET gates VDAC1 when mitoNEET is oxidized. Addition of the VDAC inhibitor 4,4′-diisothiocyanatostilbene-2,2′-disulfonate (DIDS) prevents both mitoNEET binding in vitro and mitoNEET-dependent mitochondrial iron accumulation in situ. We find that the DIDS inhibitor does not alter the redox state of MitoNEET. Taken together, our data indicate that mitoNEET regulates VDAC in a redox-dependent manner in cells, closing the pore and likely disrupting VDAC’s flow of metabolites.

Published

2019

2. The Fe-S cluster-containing NEET proteins mitoNEET and NAF-1 as chemotherapeutic targets in breast cancer

Author

Yuting Luo, Merav Darash-Yahana, Faruck Morcos, Sagi Tamir, Sarah H. Holt, Luhua Song, Ron Mittler, Celso O. Rezende, Rachel Nechushtai, Mark L. Paddock, Emmanuel A. Theodorakis, Patricia A. Jennings, Yang Sung Sohn, Fang Bai, José N. Onuchic, and Colin H. Lipper

Subjects

Iron-Sulfur Proteins, animal structures, Cell Survival, Xanthones, Molecular Conformation, Drug design, Antineoplastic Agents, Breast Neoplasms, Biology, Mitochondrion, Bioinformatics, Mitochondrial Proteins, Small hairpin RNA, Breast cancer, Cell Line, Tumor, medicine, Cluster Analysis, Humans, Molecular Targeted Therapy, Cell Proliferation, Multidisciplinary, Cell growth, Endoplasmic reticulum, Autophagy, Biological Sciences, medicine.disease, Molecular Docking Simulation, Ribonucleoproteins, Drug Design, Cancer cell, MCF-7 Cells, Cancer research, Female, Software

Abstract

Identification of novel drug targets and chemotherapeutic agents is a high priority in the fight against cancer. Here, we report that MAD-28, a designed cluvenone (CLV) derivative, binds to and destabilizes two members of a unique class of mitochondrial and endoplasmic reticulum (ER) 2Fe-2S proteins, mitoNEET (mNT) and nutrient-deprivation autophagy factor-1 (NAF-1), recently implicated in cancer cell proliferation. Docking analysis of MAD-28 to mNT/NAF-1 revealed that in contrast to CLV, which formed a hydrogen bond network that stabilized the 2Fe-2S clusters of these proteins, MAD-28 broke the coordinative bond between the His ligand and the cluster's Fe of mNT/NAF-1. Analysis of MAD-28 performed with control (Michigan Cancer Foundation; MCF-10A) and malignant (M.D. Anderson-metastatic breast; MDA-MB-231 or MCF-7) human epithelial breast cells revealed that MAD-28 had a high specificity in the selective killing of cancer cells, without any apparent effects on normal breast cells. MAD-28 was found to target the mitochondria of cancer cells and displayed a surprising similarity in its effects to the effects of mNT/NAF-1 shRNA suppression in cancer cells, causing a decrease in respiration and mitochondrial membrane potential, as well as an increase in mitochondrial iron content and glycolysis. As expected, if the NEET proteins are targets of MAD-28, cancer cells with suppressed levels of NAF-1 or mNT were less susceptible to the drug. Taken together, our results suggest that NEET proteins are a novel class of drug targets in the chemotherapeutic treatment of breast cancer, and that MAD-28 can now be used as a template for rational drug design for NEET Fe-S cluster-destabilizing anticancer drugs.

Published

2015

3. Structure of the human monomeric NEET protein MiNT and its role in regulating iron and reactive oxygen species in cancer cells

Author

Rachel Nechushtai, Amy Liu, José N. Onuchic, Yang Sung Sohn, Merav Darash-Yahana, Ron Mittler, Colin H. Lipper, Luhua Song, Patricia A. Jennings, Heiko Lammert, and Ola Karmi

Subjects

0301 basic medicine, Iron-Sulfur Proteins, Protein Folding, 1.1 Normal biological development and functioning, Iron, Mitochondrion, Molecular Dynamics Simulation, Crystallography, X-Ray, Cell Line, Mitochondrial Proteins, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, Protein Domains, Underpinning research, Cell Line, Tumor, Neoplasms, cancer, Humans, Gene, chemistry.chemical_classification, Reactive oxygen species, Gene knockdown, Multidisciplinary, Tumor, Crystallography, Endoplasmic reticulum, Cell biology, mitochondria, Cytosol, Kinetics, 030104 developmental biology, Monomer, chemistry, Cancer cell, Physical Sciences, Mitochondrial Membranes, Mutation, X-Ray, iron homeostasis, RNA Interference, Generic health relevance, NEET proteins, Reactive Oxygen Species, 030217 neurology & neurosurgery

Abstract

The NEET family is a relatively new class of three related [2Fe-2S] proteins (CISD1–3), important in human health and disease. While there has been growing interest in the homodimeric gene products of CISD1 (mitoNEET) and CISD2 (NAF-1), the importance of the inner mitochondrial CISD3 protein has only recently been recognized in cancer. The CISD3 gene encodes for a monomeric protein that contains two [2Fe-2S] CDGSH motifs, which we term mitochondrial inner NEET protein (MiNT). It folds with a pseudosymmetrical fold that provides a hydrophobic motif on one side and a relatively hydrophilic surface on the diametrically opposed surface. Interestingly, as shown by molecular dynamics simulation, the protein displays distinct asymmetrical backbone motions, unlike its homodimeric counterparts that face the cytosolic side of the outer mitochondrial membrane/endoplasmic reticulum (ER). However, like its counterparts, our biological studies indicate that knockdown of MiNT leads to increased accumulation of mitochondrial labile iron, as well as increased mitochondrial reactive oxygen production. Taken together, our study suggests that the MiNT protein functions in the same pathway as its homodimeric counterparts (mitoNEET and NAF-1), and could be a key player in this pathway within the mitochondria. As such, it represents a target for anticancer or antidiabetic drug development.

Published

2017

4. The NEET Proteins Mediate Iron-Sulfur Cluster Transport from the Mitochondria to Cytosolic Proteins

Author

Patricia A. Jennings, Mark L. Paddock, Rachel Nechushtai, and Colin H. Lipper

Subjects

Crystallography, Cytosol, Membrane, Protein family, Chemistry, Microscale thermophoresis, Biophysics, Mitochondrion, Iron-sulfur cluster transport, VDAC1, Biogenesis

Abstract

Mitochondria have an essential role in the production and export of iron-sulfur clusters. The NEET protein family members mitoNEET (mNT) and nutrient-deprivation autophagy factor-1 (NAF-1) are the only known iron-sulfur proteins at the interface of the outer-mitochondrial membrane (OMM) and the cytosol, with mNT localized to the OMM and NAF-1 on the mitochondria-associated ER membrane. Each has a similar homodimeric structure coordinating two 2Fe-2S clusters. We have shown previously that the NEETs have the ability to transfer 2Fe-2S clusters to a standard acceptor protein [1,2]. Additionally, mNT has been reported to acquire 2Fe-2S clusters from the mitochondria [3]; this is also likely the case for NAF-1. The localization, transfer ability and 2Fe-2S source suggest that these proteins act as conduits, transporting 2Fe-2S clusters from the mitochondria to cytosolic proteins. In this study we identify Anamorsin as the first known physiological acceptor of 2Fe-2S clusters from each of the NEET proteins [4]. Anamorsin is required for cytosolic iron-sulfur cluster biogenesis. We analyzed the kinetics of this reaction using UV-Vis spectroscopy and determined transfer rates that are similar to those of known human cluster transfer proteins. We also show by biolayer interferometry that these proteins form a direct protein-protein interaction, which is required for the transfer. Furthermore we found via microscale thermophoresis that mNT interacts with VDAC1, a pore protein in the OMM. We propose that the NEETs acquire 2F-2S clusters through VDAC1 and transfer them to the essential Anamorsin.[1] Zuris JA, et al. (2011) Proc Natl Acad Sci USA 108(32):13047-52.[2] Tamir S, et al. (2013) PLoS ONE 8(5):e61202.[3] Ferecatu I, et al. (2014) J Biol Chem 289(41):28070-86.[4] Lipper CH, et al. (2015) PLoS ONE (In press).

Published

2016

5. Structure-function analysis of NEET proteins uncovers their role as key regulators of iron and ROS homeostasis in health and disease

Author

Dorit Michaeli, Merav Darash-Yahana-Baram, Faruck Morcos, Colin H. Lipper, Sagi Tamir, Ioav Cabantchik, Jason T. Stofleth, Yang Sung Sohn, Mark L. Paddock, José N. Onuchic, Ron Mittler, Lily Agranat, Patricia A. Jennings, Sarah H. Holt, and Rachel Nechushtai

Subjects

Senescence, Protein Conformation, Iron, Molecular Sequence Data, Mitochondrion, Biology, Mitochondrial Proteins, 03 medical and health sciences, 0302 clinical medicine, medicine, Glucose homeostasis, Homeostasis, Humans, Genetic Predisposition to Disease, Amino Acid Sequence, Gene, Molecular Biology, 030304 developmental biology, Wolfram Syndrome 2, Cancer, Genetics, 0303 health sciences, 2Fe–2S cluster, Obesity and diabetes, Sequence Homology, Amino Acid, Cluster donor/acceptor protein, Autophagy, Genetic disorder, Cell Biology, medicine.disease, Cell biology, Mitochondria, Reactive Oxygen Species, 030217 neurology & neurosurgery, Function (biology), Biogenesis

Abstract

A novel family of 2Fe–2S proteins, the NEET family, was discovered during the last decade in numerous organisms, including archea, bacteria, algae, plant and human; suggesting an evolutionary-conserved function, potentially mediated by their CDGSH Iron–Sulfur Domain. In human, three NEET members encoded by the CISD1–3 genes were identified. The structures of CISD1 (mitoNEET, mNT), CISD2 (NAF-1), and the plant At-NEET uncovered a homodimer with a unique “NEET fold”, as well as two distinct domains: a beta-cap and a 2Fe–2S cluster-binding domain. The 2Fe–2S clusters of NEET proteins were found to be coordinated by a novel 3Cys:1His structure that is relatively labile compared to other 2Fe–2S proteins and is the reason of the NEETs' clusters could be transferred to apo-acceptor protein(s) or mitochondria. Positioned at the protein surface, the NEET's 2Fe–2S's coordinating His is exposed to protonation upon changes in its environment, potentially suggesting a sensing function for this residue. Studies in different model systems demonstrated a role for NAF-1 and mNT in the regulation of cellular iron, calcium and ROS homeostasis, and uncovered a key role for NEET proteins in critical processes, such as cancer cell proliferation and tumor growth, lipid and glucose homeostasis in obesity and diabetes, control of autophagy, longevity in mice, and senescence in plants. Abnormal regulation of NEET proteins was consequently found to result in multiple health conditions, and aberrant splicing of NAF-1 was found to be a causative of the neurological genetic disorder Wolfram Syndrome 2. Here we review the discovery of NEET proteins, their structural, biochemical and biophysical characterization, and their most recent structure–function analyses. We additionally highlight future avenues of research focused on NEET proteins and propose an essential role for NEETs in health and disease. This article is part of a Special Issue entitled: Fe/S proteins: Analysis, structure, function, biogenesis and diseases.

Published

2014

6. Nutrient-deprivation autophagy factor-1 (NAF-1): biochemical properties of a novel cellular target for anti-diabetic drugs

Author

Rachel Nechushtai, Andrea R. Conlan, Zvi Ioav Cabantchik, Dorit Michaeli, Lily Agranat, Colin H. Lipper, Sagi Tamir, Yael Harir, John A. Zuris, Patricia A. Jennings, Ron Mittler, and Mark L. Paddock

Subjects

Macromolecular Assemblies, Cell, lcsh:Medicine, Mitochondrion, Resveratrol, Biochemistry, chemistry.chemical_compound, 0302 clinical medicine, Protein structure, Drug Delivery Systems, Drug Discovery, Molecular Cell Biology, Thiazolidinedione, Biomacromolecule-Ligand Interactions, lcsh:Science, Cells, Cultured, 0303 health sciences, Multidisciplinary, Physics, 3. Good health, Cell biology, Mitochondria, Chemistry, medicine.anatomical_structure, Ribonucleoproteins, 030220 oncology & carcinogenesis, Oxidation-Reduction, Research Article, Biotechnology, medicine.drug_class, Protein subunit, Iron, Biophysics, Biology, Protein Chemistry, Small Molecule Libraries, 03 medical and health sciences, Chemical Biology, medicine, Humans, Hypoglycemic Agents, 030304 developmental biology, Endoplasmic reticulum, Autophagy, lcsh:R, Proteins, Protein Subunits, chemistry, Small Molecules, Thiazolidinediones, lcsh:Q

Abstract

Nutrient-deprivation autophagy factor-1 (NAF-1) (synonyms: Cisd2, Eris, Miner1, and Noxp70) is a [2Fe-2S] cluster protein immune-detected both in endoplasmic reticulum (ER) and mitochondrial outer membrane. It was implicated in human pathology (Wolfram Syndrome 2) and in BCL-2 mediated antagonization of Beclin 1-dependent autophagy and depression of ER calcium stores. To gain insights about NAF-1 functions, we investigated the biochemical properties of its 2Fe-2S cluster and sensitivity of those properties to small molecules. The structure of the soluble domain of NAF-1 shows that it forms a homodimer with each protomer containing a [2Fe-2S] cluster bound by 3 Cys and one His. NAF-1 has shown the unusual abilities to transfer its 2Fe-2S cluster to an apo-acceptor protein (followed in vitro by spectrophotometry and by native PAGE electrophoresis) and to transfer iron to intact mitochondria in cell models (monitored by fluorescence imaging with iron fluorescent sensors targeted to mitochondria). Importantly, the drug pioglitazone abrogates NAF-1's ability to transfer the cluster to acceptor proteins and iron to mitochondria. Similar effects were found for the anti-diabetes and longevity-promoting antioxidant resveratrol. These results reveal NAF-1 as a previously unidentified cell target of anti-diabetes thiazolidinedione drugs like pioglitazone and of the natural product resveratrol, both of which interact with the protein and stabilize its labile [2Fe-2S] cluster.

Published

2013

7. Cancer-Related NEET Proteins Transfer 2Fe-2S Clusters to Anamorsin, a Protein Required for Cytosolic Iron-Sulfur Cluster Biogenesis

Author

Colin H. Lipper, Mark L. Paddock, Rachel Nechushtai, José N. Onuchic, Ron Mittler, and Patricia A. Jennings

Subjects

Spectrometry, Mass, Electrospray Ionization, lcsh:Medicine, Iron–sulfur cluster, Plasma protein binding, Mitochondrion, Electron Transport, Mitochondrial Proteins, chemistry.chemical_compound, Electron transfer, Protein structure, Neoplasms, Humans, Protein Interaction Domains and Motifs, lcsh:Science, Ribonucleoprotein, Binding Sites, Multidisciplinary, Chemistry, lcsh:R, Intracellular Signaling Peptides and Proteins, Protein Structure, Tertiary, Cell biology, Kinetics, Cytosol, Interferometry, Ribonucleoproteins, Biochemistry, Spectrophotometry, Ultraviolet, lcsh:Q, Apoproteins, Dimerization, Biogenesis, Protein Binding, Research Article

Abstract

Iron-sulfur cluster biogenesis is executed by distinct protein assembly systems. Mammals have two systems, the mitochondrial Fe-S cluster assembly system (ISC) and the cytosolic assembly system (CIA), that are connected by an unknown mechanism. The human members of the NEET family of 2Fe-2S proteins, nutrient-deprivation autophagy factor-1 (NAF-1) and mitoNEET (mNT), are located at the interface between the mitochondria and the cytosol. These proteins have been implicated in cancer cell proliferation, and they can transfer their 2Fe-2S clusters to a standard apo-acceptor protein. Here we report the first physiological 2Fe-2S cluster acceptor for both NEET proteins as human Anamorsin (also known as cytokine induced apoptosis inhibitor-1; CIAPIN-1). Anamorsin is an electron transfer protein containing two iron-sulfur cluster-binding sites that is required for cytosolic Fe-S cluster assembly. We show, using UV-Vis spectroscopy, that both NAF-1 and mNT can transfer their 2Fe-2S clusters to apo-Anamorsin with second order rate constants similar to those of other known human 2Fe-2S transfer proteins. A direct protein-protein interaction of the NEET proteins with apo-Anamorsin was detected using biolayer interferometry. Furthermore, electrospray mass spectrometry of holo-Anamorsin prepared by cluster transfer shows that it receives both of its 2Fe-2S clusters from the NEETs. We propose that mNT and NAF-1 can provide parallel routes connecting the mitochondrial ISC system and the CIA. 2Fe-2S clusters assembled in the mitochondria are received by NEET proteins and when needed transferred to Anamorsin, activating the CIA.

Published

2015