Your search keyword '"Namrata D Udeshi"' showing total 119 results

51. The C9orf72-interacting protein Smcr8 is a negative regulator of autoimmunity and lysosomal exocytosis

Author

Sulagna Ghosh, Jin Yuan Wang, Jackson Sandoe, Joanie Mok, Maura Charlton, Steven A. Carr, Namrata D. Udeshi, Aaron Burberry, Yingying Zhang, Quan Zhen Li, Kevin Eggan, Daniel A. Mordes, and Tanya Svinkina

Subjects

0301 basic medicine, Gene isoform, Mutant, Autoimmunity, Biology, Proteomics, Exocytosis, Mice, 03 medical and health sciences, Lysosomal-Associated Membrane Protein 1, C9orf72, Lysosome, Genetics, medicine, Animals, Humans, Protein Isoforms, Secretion, Mice, Knockout, C9orf72 Protein, LAMP1, Protein Stability, Macrophages, Amyotrophic Lateral Sclerosis, Cell biology, 030104 developmental biology, medicine.anatomical_structure, Gene Expression Regulation, Membrane protein, Mutation, Splenomegaly, Lymph Nodes, Carrier Proteins, Lysosomes, Research Paper, Developmental Biology

Abstract

While a mutation in C9ORF72 is the most common genetic contributor to amyotrophic lateral sclerosis (ALS), much remains to be learned concerning the function of the protein normally encoded at this locus. To elaborate further on functions for C9ORF72, we used quantitative mass spectrometry-based proteomics to identify interacting proteins in motor neurons and found that its long isoform complexes with and stabilizes SMCR8, which further enables interaction with WDR41. To study the organismal and cellular functions for this tripartite complex, we generated Smcr8 loss-of-function mutant mice and found that they developed phenotypes also observed in C9orf72 loss-of-function animals, including autoimmunity. Along with a loss of tolerance for many nervous system autoantigens, we found increased lysosomal exocytosis in Smcr8 mutant macrophages. In addition to elevated surface Lamp1 (lysosome-associated membrane protein 1) expression, we also observed enhanced secretion of lysosomal components—phenotypes that we subsequently observed in C9orf72 loss-of-function macrophages. Overall, our findings demonstrate that C9ORF72 and SMCR8 have interdependent functions in suppressing autoimmunity as well as negatively regulating lysosomal exocytosis—processes of potential importance to ALS.

Published

2018

52. Phosphorylation coexists withO-GlcNAcylation in a plant virus protein and influences viral infection

Author

Juan Antonio García, Sergio Ciordia, Marta Hervás, Sandra Martínez-Turiño, Donald F. Hunt, Namrata D. Udeshi, Jeffrey Shabanowitz, José de Jesús Pérez, and Rosana Navajas

Subjects

0301 basic medicine, Potyvirus, Soil Science, Nicotiana benthamiana, Plant Science, Biology, Proteomics, biology.organism_classification, Molecular biology, 03 medical and health sciences, Crosstalk (biology), 030104 developmental biology, Capsid, Biochemistry, Plant virus, Phosphorylation, Target protein, Agronomy and Crop Science, Molecular Biology

Abstract

Phosphorylation and O-GlcNAcylation are two widespread post-translational modifications (PTMs), often affecting the same eukaryotic target protein. Plum pox virus (PPV) is a member of the genus Potyvirus which infects a wide range of plant species. O-GlcNAcylation of the capsid protein (CP) of PPV has been studied extensively, and some evidence of CP phosphorylation has also been reported. Here, we use proteomics analyses to demonstrate that PPV CP is phosphorylated in vivo at the N-terminus and the beginning of the core region. In contrast with the 'yin-yang' mechanism that applies to some mammalian proteins, PPV CP phosphorylation affects residues different from those that are O-GlcNAcylated (serines Ser-25, Ser-81, Ser-101 and Ser-118). Our findings show that PPV CP can be concurrently phosphorylated and O-GlcNAcylated at nearby residues. However, an analysis using a differential proteomics strategy based on iTRAQ (isobaric tags for relative and absolute quantitation) showed a significant enhancement of phosphorylation at Ser-25 in virions recovered from O-GlcNAcylation-deficient plants, suggesting that crosstalk between O-GlcNAcylation and phosphorylation in PPV CP takes place. Although the preclusion of phosphorylation at the four identified phosphotarget sites only had a limited impact on viral infection, the mimicking of phosphorylation prevents PPV infection in Prunus persica and weakens infection in Nicotiana benthamiana and other herbaceous hosts, prompting the emergence of potentially compensatory second mutations. We postulate that the joint action of phosphorylation and O-GlcNAcylation in the N-proximal segment of CP allows a fine-tuning of protein stability, providing the amount of CP required in each step of viral infection.

Published

2018

53. Abstract 960: RNF43 G659fs is an oncogenic mutation in colorectal cancer and sensitizes tumor cells to PI3K/mTOR inhibition

Author

Max Russo, Namrata D. Udeshi, Kimmie Ng, Casey O’Brien, Marios Giannakis, Steven M. Corsello, Maximilien Grandclaudon, Carino Gurjao, Srivatsan Raghavan, Dane Ford-Roshon, Lishan Fang, Ewa Sicinska, and James Berstler

Subjects

Cancer Research, Mutation, Cell growth, Wnt signaling pathway, Cancer, Biology, medicine.disease_cause, medicine.disease, Frameshift mutation, Oncology, Cancer research, medicine, Carcinogenesis, Protein kinase B, PI3K/AKT/mTOR pathway

Abstract

Introduction: RNF43 is a transmembrane E3 ubiquitin ligase and WNT signaling suppressor that is commonly mutated in colorectal cancer (CRC). A C-terminal RNF43 hotspot mutation, RNF43_G659fs, occurs in approximately 36% (55/151) of microsatellite-instability (MSI)-high CRCs, but its underlying mechanism and function remain poorly understood. This study investigated the functional role of RNF43_G659fs in order to evaluate potential novel therapeutic approaches for tumors harboring this mutation. Methods: Isogenic RNF43117mut and RNF43659mut cell line models were generated using the CRISPR/Cas9 system to evaluate CRC tumorigenesis and WNT dependency. RNF43659mut was screened with a novel high-throughput drug repurposing library that employed a set of 5363 small molecules to identify compounds capable of selectively inhibiting RNF43659mut cell growth. Small molecules that selectively killed the RNF43659mut cells were validated in organoid models. Proteomic analysis, RNA-Seq and gene set enrichment analysis (GSEA) were performed to characterize mechanistic interactions and related signaling pathways of RNF43659mut in CRC. Results: Unlike N-terminal RNF43 frameshift mutations, we observed that RNF43659mut conferred a growth advantage over RNF43WT cells independent of WNT signaling. Furthermore, RNF43659mut and RNF43WT exhibited differential drug responses in the high-throughput drug repurposing screen which revealed that RNF43659mut cells were vulnerable to PI3K/AKT/mTOR inhibitors, including BYL-719 (Alpelisib). Enhanced AKT and mTOR activation was observed in RNF43659mut cell and attenuated by BYL-719 treatment in a dose-dependent manner. These results were subsequently validated in patient-derived organoid models. Furthermore, immunoprecipitation and proteomic analysis revealed interactions between RNF43_G659fs and p85, a negative regulator of PI3K. We also demonstrated that the RNF43_G659fs mutant activated PI3K/AKT/mTOR signaling through binding and degradation of p85. Consistent with the role of PI3K in immunomodulation, our RNA-Seq results showed that the RNF43_G659fs mutation was positively related to NF-kB activation (Normalized Enrichment Score=1.842, p Conclusion: This study confirms that RNF43659mut is an essential driver mutation in CRC and provides evidence that patients harboring RNF43_G659fs-mutant tumors may respond favorably to PI3K inhibition. Citation Format: Lishan Fang, Dane Ford-Roshon, Max Russo, Casey O'Brien, Carino Gurjao, Maximilien Grandclaudon, Steven M. Corsello, Srivatsan Raghavan, Namrata Udeshi, James Berstler, Ewa Sicinska, Kimmie Ng, Marios Giannakis. RNF43 G659fs is an oncogenic mutation in colorectal cancer and sensitizes tumor cells to PI3K/mTOR inhibition [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 960.

Published

2021

54. Abstract 1950: A ubiquitination cascade regulates the integrated stress response and epithelial cancer survival

Author

Nolan Bick, Meagan E. Olive, David E. Root, Ashir A. Borah, Joshua M. Dempster, Lisa Leung, Alfredo Gonzalez, Namrata D. Udeshi, Mariya Kazachkova, John M. Krill-Burger, Steven A. Carr, Lisa D. Cervia, Naomi Li, Benjamin Gaeta, Tsukasa Shibue, William C. Hahn, Federica Piccioni, James M. McFarland, Nancy Dumont, and Francisca Vazquez

Subjects

Cancer Research, Oncology, Ubiquitin, biology, Cascade, Chemistry, biology.protein, Integrated stress response, Epithelial cancer, Cell biology

Abstract

Systematic identification of signaling pathways required for the viability of cancer cells will facilitate the development of novel cancer therapies. We used gene essentiality measurements in 726 cancer cell lines to identify selective co-essentiality modules and found a functional ubiquitination cascade containing UBA6, BIRC6, KCMF1 and UBR4, which encode an E1, E2, and two heterodimeric E3 subunits, respectively, as a vulnerability in a subset of epithelial tumors. Suppressing BIRC6 in cancer cell lines that are dependent on this ubiquitination cascade led to a strong reduction in cell fitness in vitro, and to potent tumor regression and metastasis suppression in vivo. Mechanistically, BIRC6 suppression resulted in selective and robust activation of the integrated stress response (ISR) signaling via upregulation of the heme-regulated inhibitor (HRI). Using proteomic profiling, we found that HRI itself is a key degradation target of the UBA6/BIRC6/KCMF1/UBR4 cascade. These observations demonstrate a protein ubiquitination cascade regulating ISR and highlight the potential of this cascade as a novel therapeutic target for a subset of epithelial cancers. Citation Format: Lisa D. Cervia, Tsukasa Shibue, Benjamin Gaeta, Ashir Borah, Lisa Leung, Naomi Li, Nancy Dumont, Alfredo Gonzalez, Nolan Bick, Mariya Kazachkova, Joshua Dempster, John M. Krill-Burger, Namrata Udeshi, Meagan Olive, Steven A. Carr, David E. Root, Federica Piccioni, James M. McFarland, Francisca Vazquez, William C. Hahn. A ubiquitination cascade regulates the integrated stress response and epithelial cancer survival [abstract]. In: Proceedings of the American Association for Cancer Research Annual Meeting 2021; 2021 Apr 10-15 and May 17-21. Philadelphia (PA): AACR; Cancer Res 2021;81(13_Suppl):Abstract nr 1950.

Published

2021

55. Lysine trimethylation regulates 78-kDa glucose-regulated protein proteostasis during endoplasmic reticulum stress

Author

Steven A. Carr, Moran Dvela-Levitt, Nicolas Wieder, Ozan Aygün, Anna Greka, Namrata D. Udeshi, Jonas Sieber, and Mauricio Ostrosky-Frid

Subjects

0301 basic medicine, Lysine, Protein degradation, Methylation, Biochemistry, Cell Line, Mice, 03 medical and health sciences, 0302 clinical medicine, Animals, DNA Modification Methylases, Endoplasmic Reticulum Chaperone BiP, Molecular Biology, Heat-Shock Proteins, biology, Podocytes, Chemistry, Endoplasmic reticulum, STIM1, Cell Biology, Endoplasmic Reticulum Stress, Cell biology, 030104 developmental biology, 78 kDa Glucose-Regulated Protein, Proteostasis, Protein Synthesis and Degradation, Chaperone (protein), Proteolysis, Unfolded Protein Response, Unfolded protein response, biology.protein, 030217 neurology & neurosurgery

Abstract

The up-regulation of chaperones such as the 78-kDa glucose-regulated protein (GRP78, also referred to as BiP or HSPA5) is part of the adaptive cellular response to endoplasmic reticulum (ER) stress. GRP78 is widely used as a marker of the unfolded protein response, associated with sustained ER stress. Here we report the discovery of a proteostatic mechanism involving GRP78 trimethylation in the context of ER stress. Using mass spectrometry–based proteomics, we identified two GRP78 fractions, one homeostatic and one induced by ER stress. ER stress leads to de novo biosynthesis of non-trimethylated GRP78, whereas homeostatic, METTL21A-dependent lysine 585–trimethylated GRP78 is reduced. This proteostatic mechanism, dependent on the posttranslational modification of GRP78, allows cells to differentially regulate specific protein abundance during cellular stress.

Published

2017

56. Antibodies to biotin enable large-scale detection of biotinylation sites on proteins

Author

Vamsi K. Mootha, Dominic Ryan, Karsten Krug, Steven A. Carr, Karl R. Clauser, Tslil Ast, Namrata D. Udeshi, Kayvon Pedram, Tanya Svinkina, Alice Y. Ting, Samuel A. Myers, Shaunt Fereshetian, and Ozan Aygün

Subjects

0301 basic medicine, Streptavidin, Biotin, Peptide, Biology, 010402 general chemistry, Tandem mass spectrometry, Mass spectrometry, 01 natural sciences, Biochemistry, Antibodies, Jurkat Cells, 03 medical and health sciences, chemistry.chemical_compound, Tandem Mass Spectrometry, Humans, Biotinylation, Molecular Biology, chemistry.chemical_classification, Staining and Labeling, Proteins, Cell Biology, 0104 chemical sciences, HEK293 Cells, 030104 developmental biology, chemistry, biology.protein, Antibody, Peptides, Chromatography, Liquid, Biotechnology, Peroxidase

Abstract

Although purification of biotinylated molecules is highly efficient, identifying specific sites of biotinylation remains challenging. We show that anti-biotin antibodies enable unprecedented enrichment of biotinylated peptides from complex peptide mixtures. Live-cell proximity labeling using APEX peroxidase followed by anti-biotin enrichment and mass spectrometry yielded over 1,600 biotinylation sites on hundreds of proteins, an increase of more than 30-fold in the number of biotinylation sites identified compared to streptavidin-based enrichment of proteins.

Published

2017

57. Proximity Biotinylation as a Method for Mapping Proteins Associated with mtDNA in Living Cells

Author

Mark H. Ellisman, Thomas J. Deerinck, Steven A. Carr, Shuo Han, Namrata D. Udeshi, Tanya Svinkina, and Alice Y. Ting

Subjects

APEX2, Proteomics, 0301 basic medicine, Clinical Biochemistry, peroxidase, Mitochondrion, Biochemistry, Drug Discovery, FASTKD1, APEX, mapping, RNA, Small Interfering, mass spectrometry, Mitochondrial nucleoid, Microscopy, RNA-Binding Proteins, Mitochondrial, Mitochondria, Cell biology, Biotinylation, Molecular Medicine, RNA Interference, Mitochondrial DNA, nucleoid, Immunoprecipitation, 1.1 Normal biological development and functioning, Biology, Small Interfering, Electron, DNA, Mitochondrial, Fluorescence, Article, Mitochondrial Proteins, 03 medical and health sciences, proteomics, Underpinning research, Humans, Nucleoid, Molecular Biology, oxphos, Peroxidase, Pharmacology, Messenger RNA, Electron Transport Complex I, 030102 biochemistry & molecular biology, Proteins, DNA, Microscopy, Electron, HEK293 Cells, 030104 developmental biology, Microscopy, Fluorescence, Biocatalysis, RNA, Generic health relevance

Abstract

A recurring challenge in cell biology is to define themolecular components of macromolecular complexes of interest. The predominant method, immunoprecipitation, recovers only strong interaction partners that survive cell lysis and repeated detergent washes. We explored peroxidase-catalyzed proximity biotinylation, APEX, as an alternative, focusing on the mitochondrial nucleoid, the dynamic macromolecular complex that houses the mitochondrial genome. Via 1-min live-cell biotinylation followed by quantitative, ratiometric mass spectrometry, we enriched 37 nucleoid proteins, seven of which had never previously been associated with the nucleoid. The specificity of our dataset was very high, and we validated three hits by follow-up studies. For one novel nucleoid-associated protein, FASTKD1, we discovered a role in downregulation of mitochondrial complex I via specific repression of ND3 mRNA. Our study demonstrates that APEX is a powerful tool for mapping macromolecular complexes in living cells, and can identify proteins and pathways that have been missed by traditional approaches.

Published

2017

58. Cell-Surface Proteomic Profiling in the Fly Brain Uncovers New Wiring Regulators

Author

D. R. Mani, Tanya Svinkina, Shuo Han, Alice Y. Ting, Qijing Xie, Hongjie Li, Pornchai Kaewsapsak, Liqun Luo, Ricardo Guajardo, David J. Luginbuhl, Bing Wu, Steven A. Carr, Anthony Xie, Jiefu Li, Namrata D. Udeshi, Colleen N. McLaughlin, Stephen R. Quake, Chuanyun Xu, and Tongchao Li

Subjects

0303 health sciences, Protein family, Proteomic Profiling, Cell, Biology, LRP1, Cell biology, 03 medical and health sciences, Multicellular organism, 0302 clinical medicine, medicine.anatomical_structure, Proteome, medicine, Receptor, Neural development, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

SUMMARYMolecular interactions at the cellular interface mediate organized assembly of single cells into tissues, and thus govern the development and physiology of multicellular organisms. Here, we developed a cell-type-specific, spatiotemporally-resolved approach to profile cell-surface proteomes in intact tissues. Quantitative profiling of cell-surface proteomes ofDrosophilaolfactory projection neurons (PNs) in pupae and adults revealed a global down-regulation of wiring molecules and an up-regulation of synaptic molecules in the transition from developing to mature PNs. A proteome-instructedin vivoscreen identified 20 new cell-surface molecules regulating neural circuit assembly, many of which belong to evolutionarily conserved protein families not previously linked to neural development. Genetic analysis further revealed that the lipoprotein receptor LRP1 cell-autonomously controls PN dendrite targeting, contributing to the formation of a precise olfactory map. These findings highlight the power of temporally-resolvedin situcell-surface proteomic profiling in discovering new regulators of brain wiring.

Published

2019

59. UbiFast, a rapid and deep-scale ubiquitylation profiling approach for biology and translational research

Author

Steven A. Carr, Shankha Satpathy, Philipp Mertins, Jessica A. Gasser, Deepak Mani, Namrata D. Udeshi, Benjamin L. Ebert, Tanya Svinkina, and Shaunt Fereshetian

Subjects

chemistry.chemical_classification, 0303 health sciences, biology, Peptide, Quantitative accuracy, 3. Good health, Ubiquitin ligase, Cell biology, 03 medical and health sciences, 0302 clinical medicine, Protein ubiquitylation, Ubiquitin, chemistry, 030220 oncology & carcinogenesis, biology.protein, Posttranslational modification, Human breast, 030304 developmental biology

Abstract

Protein ubiquitylation is involved in a plethora of cellular processes. Defects in the ubiquitin system are at the root of many acquired and hereditary diseases. While antibodies directed at ubiquitin remnants (K-ε-GG) have improved the ability to monitor ubiquitylation using mass spectrometry, methods for highly-multiplexed measurement of ubiquitylation in tissues and primary cells using sub-milligram amounts of sample remains a challenge. Here we present a highly-sensitive, rapid and multiplexed protocol for quantifying ∼10,000 ubiquitylation sites from as little as 500 ug peptide per sample from cells or tissue in a TMT10 plex in ca. 5 hr. High-field Asymmetric Ion Mobility Spectrometry (FAIMS) is used to improve quantitative accuracy for posttranslational modification analysis. We use the approach to rediscover substrates of the E3 ligase targeting drug lenalidomide and to identify proteins modulated by ubiquitylation in models of basal and luminal human breast cancer. The sensitivity and speed of the UbiFast method makes it suitable for large-scale studies in primary tissue samples.

Published

2019

60. Glucocorticoids Induce the Expansion of an Immature Human CFU-E Population

Author

John Hale, Sandrina Kinet, Meagan E. Olive, Jeffrey M. Lipton, Christopher D. Hillyer, Naomi Taylor, Brian M. Dulmovits, Nan Wang, Narla Mohandas, Steven A. Carr, Lydie Da Costa, Ryan Ashley, Hongxia Yan, Adrianna Vlachos, Julien Papoin, Namrata D. Udeshi, Anupama Narla, and Lionel Blanc

Subjects

0303 health sciences, medicine.medical_specialty, education.field_of_study, Chemistry, Population, CD34, medicine.disease, 3. Good health, 03 medical and health sciences, 0302 clinical medicine, Endocrinology, 030220 oncology & carcinogenesis, Cord blood, Internal medicine, medicine, Erythropoiesis, Diamond–Blackfan anemia, education, hormones, hormone substitutes, and hormone antagonists, Dexamethasone, 030304 developmental biology, CFU-E, Proto-oncogene tyrosine-protein kinase Src, medicine.drug

Abstract

Despite effective clinical use, the mechanistic bases for the regulation of human erythropoiesis by glucocorticoids remain poorly understood. Here, we employed an erythroid culture system to differentiate primary human CD34+cells isolated from control peripheral blood, cord blood and patients with Diamond Blackfan anemia (DBA), as model of an erythropoietic disorder treated with glucocorticoids. We found that the response to Dexamethasone is dependent on the developmental origin of the source of CD34+cells, specifically increasing the expansion of CD34+cells from peripheral blood but not cord blood. We also demonstrated that Dex treatment leads to the expansion of a novel immature colony-forming unit-erythroid (CFU-E) population in peripheral blood which is uniquely responsible for the proliferative effects observed during human adult erythropoiesis. Dex treatment of peripheral blood CFU-E cells also induced p57Kip2expression while patients with DBA resistant to steroids had altered p57Kip2expression that did not increase with Dex. Furthermore, shRNA knockdown of p57Kip2reduced proliferation and abrogated the effects of Dex. Finally, proteomics of Dex-treated CFU-E from peripheral blood and cord blood additionally revealed novel Dex targets in the erythroid system. Altogether, these results provide novel insights into the regulation of human erythropoiesis by glucocorticoids.Graphical Abstract

Published

2019

61. In Situ Peroxidase Labeling and Mass Spectrometry of Alpha-Synuclein in Rat Cortical Neurons

Author

Ricardo, Sanz, Patrick, Ovando-Roche, Namrata D, Udeshi, Steven A, Carr, Chee Yeun, Chung, and Vikram, Khurana

Subjects

Cerebral Cortex, Data Analysis, Neurons, Proteomics, Staining and Labeling, Fluorescent Antibody Technique, Parkinson Disease, Mass Spectrometry, Rats, alpha-Synuclein, Animals, Humans, Cells, Cultured, In Situ Hybridization, Peroxidase

Abstract

In this chapter, we describe a novel ascorbate peroxidase (APEX)-based labeling method that in combination with mass spectrometry identifies proteins in the immediate vicinity of αSyn in living rat cortical neurons. To isolate these interactions, we transduced primary cortical neurons with a lentivirus encoding APEX2 tagged to the C-terminus of alpha-synuclein (αSyn) and under the control of a synapsin promoter. Neural protein lysates were then incubated with streptavidin magnetic beads, washed, eluted from the beads, and digested overnight. The desalted peptides were then labeled with iTRAQ (4-plex) reagents and analyzed by nanoflow liquid chromatography-tandem mass spectrometry (LC-MS/MS). Collected data were analyzed using Spectrum Mill software, ultimately shedding light on αSyn physiological function and abnormal behavior during pathology.

Published

2019

62. Cell-Surface Proteomic Profiling in the Fly Brain Uncovers New Wiring Regulators

Author

Steven A. Carr, D. R. Mani, Hongjie Li, Namrata D. Udeshi, Shuo Han, David J. Luginbuhl, Bing Wu, Jiefu Li, Qijing Xie, Colleen N. McLaughlin, Pornchai Kaewsapsak, Anthony Xie, Liqun Luo, Ricardo Guajardo, Chuanyun Xu, Tanya Svinkina, Alice Y. Ting, Stephen R. Quake, and Tongchao Li

Subjects

Multicellular organism, medicine.anatomical_structure, Protein family, Proteomic Profiling, Proteome, Cell, medicine, Dendrite, Biology, LRP1, Neural development, Cell biology

Abstract

Molecular interactions at the cellular interface mediate organized assembly of single cells into tissues, and thus govern the development and physiology of multicellular organisms. Here, we developed a cell-type-specific, spatiotemporally-resolved approach to profile cell-surface proteomes in intact tissues. Quantitative profiling of cell-surface proteomes of Drosophila olfactory projection neurons (PNs) in pupae and adults revealed a global down-regulation of wiring molecules and an up-regulation of synaptic molecules in the transition from developing to mature PNs. A proteome-instructed in vivo screen identified 20 new cell-surface molecules regulating neural circuit assembly, many of which belong to evolutionarily conserved protein families not previously linked to neural development. Genetic analysis further revealed that the lipoprotein receptor LRP1 cell-autonomously controls PN dendrite targeting, contributing to the formation of a precise olfactory map. These findings highlight the power of temporally-resolved in situ cell-surface proteomic profiling in discovering new regulators of brain wiring.

Published

2019

63. In Situ Peroxidase Labeling and Mass Spectrometry of Alpha-Synuclein in Rat Cortical Neurons

Author

Ricardo Sanz, Patrick Ovando-Roche, Vikram Khurana, Namrata D. Udeshi, Steven A. Carr, and Chee Yeun Chung

Subjects

Alpha-synuclein, Streptavidin, In situ, 0303 health sciences, Physiological function, biology, Synapsin, Cortical neurons, Mass spectrometry, Cell biology, 03 medical and health sciences, chemistry.chemical_compound, 0302 clinical medicine, chemistry, biology.protein, 030217 neurology & neurosurgery, 030304 developmental biology, Peroxidase

Abstract

In this chapter, we describe a novel ascorbate peroxidase (APEX)-based labeling method that in combination with mass spectrometry identifies proteins in the immediate vicinity of αSyn in living rat cortical neurons. To isolate these interactions, we transduced primary cortical neurons with a lentivirus encoding APEX2 tagged to the C-terminus of alpha-synuclein (αSyn) and under the control of a synapsin promoter. Neural protein lysates were then incubated with streptavidin magnetic beads, washed, eluted from the beads, and digested overnight. The desalted peptides were then labeled with iTRAQ (4-plex) reagents and analyzed by nanoflow liquid chromatography-tandem mass spectrometry (LC-MS/MS). Collected data were analyzed using Spectrum Mill software, ultimately shedding light on αSyn physiological function and abnormal behavior during pathology.

Published

2019

64. Regulation of purine metabolism connects KCTD13 to a metabolic disorder with autistic features

Author

Clary B. Clish, Sumaiya Iqbal, Dennis Lal, Karen Duong, Namrata D. Udeshi, Arthur J. Campbell, Edward M. Scolnick, Kerry A. Pierce, Feng Zhang, Michael C. Lewis, Jon M. Madison, Antonio S. Gomes, Florence F. Wagner, Randall Jeffrey Platt, Jeffrey R. Cottrell, Morgan Sheng, Ellen F. Vieux, Shaunt Fereshetian, Steven A. Carr, and Elise Requadt

Subjects

Proteomics, 0301 basic medicine, Adenosine monophosphate, Mutant, 02 engineering and technology, Article, 03 medical and health sciences, chemistry.chemical_compound, Ubiquitin, medicine, Metabolomics, lcsh:Science, Purine metabolism, Adenylosuccinate lyase deficiency, chemistry.chemical_classification, DNA ligase, Multidisciplinary, biology, Adenylosuccinate synthase, 021001 nanoscience & nanotechnology, medicine.disease, Ubiquitin ligase, Cell biology, 030104 developmental biology, chemistry, biology.protein, lcsh:Q, Molecular Neuroscience, 0210 nano-technology

Abstract

Summary Genetic variation of the 16p11.2 deletion locus containing the KCTD13 gene and of CUL3 is linked with autism. This genetic connection suggested that substrates of a CUL3-KCTD13 ubiquitin ligase may be involved in disease pathogenesis. Comparison of Kctd13 mutant (Kctd13−/−) and wild-type neuronal ubiquitylomes identified adenylosuccinate synthetase (ADSS), an enzyme that catalyzes the first step in adenosine monophosphate (AMP) synthesis, as a KCTD13 ligase substrate. In Kctd13−/− neurons, there were increased levels of succinyl-adenosine (S-Ado), a metabolite downstream of ADSS. Notably, S-Ado levels are elevated in adenylosuccinate lyase deficiency, a metabolic disorder with autism and epilepsy phenotypes. The increased S-Ado levels in Kctd13−/− neurons were decreased by treatment with an ADSS inhibitor. Lastly, functional analysis of human KCTD13 variants suggests that KCTD13 variation may alter ubiquitination of ADSS. These data suggest that succinyl-AMP metabolites accumulate in Kctd13−/− neurons, and this observation may have implications for our understanding of 16p11.2 deletion syndrome., Graphical abstract, Highlights • KCTD13 deletion leads to decreases in ubiquitination and increases in levels of ADSS • KCTD13 deletion increases S-Ado levels, a metabolite observed in ADSL deficiency • Treatment of KCTD13 deletion neurons with an ADSS inhibitor reduces S-Ado levels • Human KCTD13 variants can alter ubiquitination of ADSS, Molecular Neuroscience; Proteomics; Metabolomics

Published

2021

65. Automating UbiFast for High-throughput and Multiplexed Ubiquitin Enrichment

Author

Meagan E. Olive, Alissa J. Nelson, Kimberly Lee, Namrata D. Udeshi, Erik J. Bergstrom, Keith Rivera, Shankha Satpathy, and Steven A. Carr

Subjects

Proteomics, Computational biology, Tandem mass tag, Multiplexing, Antibodies, Mass Spectrometry, Workflow, Automation, Jurkat Cells, Mice, Protein ubiquitylation, Ubiquitin, Animals, Humans, Throughput (business), biology, Chemistry, Magnetic Phenomena, Sepharose, Ubiquitination, Mammary Neoplasms, Experimental, General Medicine, Ubiquitinated Proteins, High-Throughput Screening Assays, Large sample, Isobaric labeling, biology.protein, Female, Peptides, Automated method

Abstract

Robust methods for deep-scale enrichment and site-specific identification of ubiquitylation sites are necessary for characterizing the myriad roles of protein ubiquitylation. To this end we previously developed UbiFast, a sensitive method for highly multiplexed ubiquitylation profiling where K-ɛ-GG peptides are enriched with anti-K-e-GG antibody and labeled on-antibody with isobaric labeling reagents for sample multiplexing. Here, we present robotic automation of the UbiFast method using a magnetic bead-conjugated K-e-GG antibody (mK-e-GG) and a magnetic particle processor. We report the identification of ∼20,000 ubiquitylation sites from a TMT10-plex with 500 μg input per sample processed in ∼2 hours. Automation of the UbiFast method greatly increased the number of identified and quantified ubiquitylation sites, improved reproducibility and significantly reduced processing time. The automated method also significantly reduced variability across process replicates compared to the manual method. The workflow enables processing of up to 96 samples in a single day making it suitable to study ubiquitylation in large sample sets. Here we demonstrate the applicability of the method to profile small amounts of tissue using breast cancer patient-derived xenograft (PDX) tissue samples.

Published

2021

66. Spatially resolved proteomic mapping in living cells with the engineered peroxidase APEX2

Author

Steven A. Carr, Alice Y. Ting, Kurt James Cox, Stephanie S Lam, Namrata D. Udeshi, Victoria Hung, Kayvon Pedram, and Ken H. Loh

Subjects

Proteomics, 0301 basic medicine, Streptavidin, Proteome, Biotin, Protein Engineering, Mass Spectrometry, Article, General Biochemistry, Genetics and Molecular Biology, Isotopic labeling, 03 medical and health sciences, chemistry.chemical_compound, Stable isotope labeling by amino acids in cell culture, DNA-(Apurinic or Apyrimidinic Site) Lyase, Humans, Biotinylation, Cellular compartment, Hydrogen Peroxide, Protein engineering, Endonucleases, Multifunctional Enzymes, HEK293 Cells, 030104 developmental biology, chemistry, Biochemistry, Isotope Labeling

Abstract

This protocol describes a method to obtain spatially resolved proteomic maps of specific compartments within living mammalian cells. An engineered peroxidase, APEX2, is genetically targeted to a cellular region of interest. Upon the addition of hydrogen peroxide for 1 min to cells preloaded with a biotin-phenol substrate, APEX2 generates biotin-phenoxyl radicals that covalently tag proximal endogenous proteins. Cells are then lysed, and biotinylated proteins are enriched with streptavidin beads and identified by mass spectrometry. We describe the generation of an appropriate APEX2 fusion construct, proteomic sample preparation, and mass spectrometric data acquisition and analysis. A two-state stable isotope labeling by amino acids in cell culture (SILAC) protocol is used for proteomic mapping of membrane-enclosed cellular compartments from which APEX2-generated biotin-phenoxyl radicals cannot escape. For mapping of open cellular regions, we instead use a ‘ratiometric’ three-state SILAC protocol for high spatial specificity. Isotopic labeling of proteins takes 5–7 cell doublings. Generation of the biotinylated proteomic sample takes 1 d, acquiring the mass spectrometric data takes 2–5 d and analysis of the data to obtain the final proteomic list takes 1 week.

Published

2016

67. Cell-Surface Proteomic Profiling in the Fly Brain Uncovers Wiring Regulators

Author

Namrata D. Udeshi, Colleen N McLaughlin, Ricardo Guajardo, Hongjie Li, Tanya Svinkina, D. R. Mani, Alice Y. Ting, Jiefu Li, Shuo Han, David J. Luginbuhl, Bing Wu, Chuanyun Xu, Pornchai Kaewsapsak, Qijing Xie, Tongchao Li, Liqun Luo, Anthony Xie, Steven A. Carr, and Stephen R. Quake

Subjects

Proteomics, Olfactory Nerve, Protein family, Neurogenesis, Biology, Olfactory Receptor Neurons, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, 0302 clinical medicine, Downregulation and upregulation, Animals, Drosophila Proteins, Receptors, Lipoprotein, 030304 developmental biology, 0303 health sciences, Proteomic Profiling, Gene Expression Profiling, Brain, Gene Expression Regulation, Developmental, Membrane Proteins, Dendrites, Olfactory Pathways, LRP1, Axons, Cell biology, Smell, Multicellular organism, Drosophila melanogaster, Proteome, Neural development, 030217 neurology & neurosurgery

Abstract

Summary Molecular interactions at the cellular interface mediate organized assembly of single cells into tissues and, thus, govern the development and physiology of multicellular organisms. Here, we developed a cell-type-specific, spatiotemporally resolved approach to profile cell-surface proteomes in intact tissues. Quantitative profiling of cell-surface proteomes of Drosophila olfactory projection neurons (PNs) in pupae and adults revealed global downregulation of wiring molecules and upregulation of synaptic molecules in the transition from developing to mature PNs. A proteome-instructed in vivo screen identified 20 cell-surface molecules regulating neural circuit assembly, many of which belong to evolutionarily conserved protein families not previously linked to neural development. Genetic analysis further revealed that the lipoprotein receptor LRP1 cell-autonomously controls PN dendrite targeting, contributing to the formation of a precise olfactory map. These findings highlight the power of temporally resolved in situ cell-surface proteomic profiling in discovering regulators of brain wiring.

Published

2020

68. Patterns of substrate affinity, competition, and degradation kinetics underlie biological activity of thalidomide analogs

Author

Mikolaj Slabicki, Eric Kuhn, Quinlan L. Sievers, Namrata D. Udeshi, Jessica A. Gasser, Adam S. Sperling, Rob S. Sellar, Hasmik Keshishian, Michael Burgess, Elyse A. Olesinski, Benjamin L. Ebert, Steven A. Carr, Rohan Sharma, Anthony Letai, Peter Miller, Shruti Bhatt, Max Jan, Brian J. Liddicoat, Mariateresa Fulciniti, Emma C. Fink, Dylan N. Adams, and Nikhil C. Munshi

Subjects

biology, Chemistry, Ubiquitin-Protein Ligases, Immunology, Biological activity, Cell Biology, Hematology, Drug resistance, Protein degradation, Biochemistry, In vitro, Ubiquitin ligase, Substrate Specificity, Thalidomide, Targeted mass spectrometry, In vivo, Hematologic Neoplasms, Proteolysis, biology.protein, medicine, Humans, medicine.drug

Abstract

Pharmacologic agents that modulate ubiquitin ligase activity to induce protein degradation are a major new class of therapeutic agents, active in a number of hematologic malignancies. However, we currently have a limited understanding of the determinants of activity of these agents and how resistance develops. We developed and used a novel quantitative, targeted mass spectrometry (MS) assay to determine the relative activities, kinetics, and cell-type specificity of thalidomide and 4 analogs, all but 1 of which are in clinical use or clinical trials for hematologic malignancies. Thalidomide analogs bind the CRL4CRBN ubiquitin ligase and induce degradation of particular proteins, but each of the molecules studied has distinct patterns of substrate specificity that likely underlie the clinical activity and toxicities of each drug. Our results demonstrate that the activity of molecules that induce protein degradation depends on the strength of ligase-substrate interaction in the presence of drug, the levels of the ubiquitin ligase, and the expression level of competing substrates. These findings highlight a novel mechanism of resistance to this class of drugs mediated by competition between substrates for access to a limiting pool of the ubiquitin ligase. We demonstrate that increased expression of a nonessential substrate can lead to decreased degradation of other substrates that are critical for antineoplastic activity of the drug, resulting in drug resistance. These studies provide general rules that govern drug-dependent substrate degradation and key differences between thalidomide analog activity in vitro and in vivo.

Published

2018

69. Evaluation of Advanced Precursor Determination for Tandem Mass Tag (TMT)-Based Quantitative Proteomics across Instrument Platforms

Author

Susan Klaeger, John C. Rogers, Rosa Viner, Jae Choi, Shankha Satpathy, Namrata D. Udeshi, Samuel A. Myers, Karl R. Clauser, and Steven A. Carr

Subjects

0301 basic medicine, Proteomics, Analyte, Chromatography, Materials science, Staining and Labeling, 010401 analytical chemistry, Quantitative proteomics, General Chemistry, Tandem mass tag, Missing data, 01 natural sciences, Biochemistry, 0104 chemical sciences, Peak detection, 03 medical and health sciences, 030104 developmental biology, Data acquisition, Tandem Mass Spectrometry, Isobaric process, Peptides, Algorithms

Abstract

Tandem mass tag (TMT)-based quantitation is a strong modality for quantitative proteomics, as samples can be multiplexed, creating large-scale data sets with high precision and minimal missing values. However, coisolation/cofragmentation of near isobaric, coeluting precursor peptide analytes has been well-documented to show ratio compression, compromising the accuracy of peptide/protein quantitation. Advanced peak determination (APD) is a new peak-picking algorithm that shows improved identification of peak detection in survey scans (MS1) to increase the number of precursors selected for unimolecular dissociation (MS2). To increase the number of these "features" selected for MS2 APD purposefully selects multiple peptide precursors of very similar m/ z that often derive from different proteins-a major source of ratio compression in TMT quantification. Here, we evaluate the effects of various data acquisition parameters combined with APD on ratio compression. We find that data acquisition with APD enabled results in more coisolated precursors, more mixed spectra, and in turn, fewer peptide spectral matches, especially at standard on-column loads. We conclude that APD should not be utilized for isobaric tagging, MS2-based experiments.

Published

2018

70. New Approaches for Localization of Proteins and Interaction Partners in Cells with High Spatial Resolution

Author

Steven A. Carr, Namrata D. Udeshi, and Samuel A. Myers

Subjects

Physics, Genetics, High spatial resolution, Biological system, Molecular Biology, Biochemistry, Biotechnology

Published

2018

71. Proteomic mapping in live Drosophila tissues using an engineered ascorbate peroxidase

Author

Norbert Perrimon, Thomas Y. K. Lau, Namrata D. Udeshi, Chiao-Lin Chen, Steven A. Carr, Frederik Wirtz-Peitz, Li He, Yanhui Hu, and Alice Y. Ting

Subjects

Proteomics, Multidisciplinary, Staining and Labeling, biology, fungi, Computational Biology, Biological Sciences, Protein–protein interaction, Apex (geometry), Cell biology, Ascorbate Peroxidases, Mitochondrial matrix, Biotinylation, Proteome, Organelle, biology.protein, Animals, Drosophila, Databases, Protein, Genetic Engineering, Peroxidase

Abstract

Characterization of the proteome of organelles and subcellular domains is essential for understanding cellular organization and identifying protein complexes as well as networks of protein interactions. We established a proteomic mapping platform in live Drosophila tissues using an engineered ascorbate peroxidase (APEX). Upon activation, the APEX enzyme catalyzes the biotinylation of neighboring endogenous proteins that can then be isolated and identified by mass spectrometry. We demonstrate that APEX labeling functions effectively in multiple fly tissues for different subcellular compartments and maps the mitochondrial matrix proteome of Drosophila muscle to demonstrate the power of APEX for characterizing subcellular proteomes in live cells. Further, we generate "MitoMax," a database that provides an inventory of Drosophila mitochondrial proteins with subcompartmental annotation. Altogether, APEX labeling in live Drosophila tissues provides an opportunity to characterize the organelle proteome of specific cell types in different physiological conditions.

Published

2015

72. Building the Connectivity Map of epigenetics: Chromatin profiling by quantitative targeted mass spectrometry

Author

Jeannie T. Lee, Sally E. Peach, Jesse S. Boehm, Amanda L. Creech, Verena K. Maier, Jacob D. Jaffe, Caitlin M. Feeney, Namrata D. Udeshi, Jordan E. Taylor, Steven A. Carr, and Xiaoyun Wu

Subjects

Epigenomics, Proteomics, Genetics, biology, Genomics, Computational biology, Genome, Article, Chromatin, Mass Spectrometry, General Biochemistry, Genetics and Molecular Biology, Histones, Histone, Targeted mass spectrometry, Stable isotope labeling by amino acids in cell culture, biology.protein, Humans, Profiling (information science), Epigenetics, Protein Processing, Post-Translational, Molecular Biology

Abstract

Epigenetic control of genome function is an important regulatory mechanism in diverse processes such as lineage commitment and environmental sensing, and in disease etiologies ranging from neuropsychiatric disorders to cancer. Here we report a robust, high-throughput targeted, quantitative mass spectrometry (MS) method to rapidly profile modifications of the core histones of chromatin that compose the epigenetic landscape, enabling comparisons among cells with differing genetic backgrounds, genomic perturbations, and drug treatments.

Published

2015

73. Directed evolution of TurboID for efficient proximity labeling in living cells and organisms

Author

Tess C. Branon, Justin A. Bosch, Ariana D. Sanchez, Namrata D. Udeshi, Tanya Svinkina, Steven A. Carr, Jessica L. Feldman, Norbert Perrimon, and Alice Y. Ting

Subjects

0301 basic medicine, chemistry.chemical_classification, DNA ligase, biology, Mutant, Yeast display, Directed evolution, Yeast, Cell biology, 03 medical and health sciences, chemistry.chemical_compound, 030104 developmental biology, Enzyme, chemistry, Biotin, Biochemistry, biology.protein, Peroxidase

Abstract

Protein interaction networks and protein compartmentation underlie every signaling process and regulatory mechanism in cells. Recently, proximity labeling (PL) has emerged as a new approach to study the spatial and interaction characteristics of proteins in living cells. However, the two enzymes commonly used for PL come with tradeoffs – BioID is slow, requiring tagging times of 18-24 hours, while APEX peroxidase uses substrates that have limited cell permeability and high toxicity. To address these problems, we used yeast display-based directed evolution to engineer two mutants of biotin ligase, TurboID and miniTurbo, with much greater catalytic efficiency than BioID, and the ability to carry out PL in cells in much shorter time windows (as little as 10 minutes) with non-toxic and easily deliverable biotin. In addition to shortening PL time by 100-fold and increasing PL yield in cell culture, TurboID enabled biotin-based PL in new settings, including yeast, Drosophila, and C. elegans.

Published

2017

74. Proteomic mapping of cytosol-facing outer mitochondrial and ER membranes in living human cells by proximity biotinylation

Author

Vamsi K. Mootha, Steven A. Carr, Gaelen Guzman, Stephanie S Lam, Victoria Hung, Namrata D. Udeshi, Tanya Svinkina, Alice Y. Ting, Broad Institute of MIT and Harvard, Massachusetts Institute of Technology. Department of Chemistry, Hung, Victoria, Lam, Stephanie Shih-Min, Guzman, Gaelen Donnelly, Mootha, Vamsi, Carr, Steven A, and Ting, Alice Y

Subjects

APEX2, 0301 basic medicine, QH301-705.5, Science, promiscuous enzymatic labeling, Biochemistry, mitochondria-ER junctions, General Biochemistry, Genetics and Molecular Biology, mitochondria-associated membrane, 03 medical and health sciences, Mitochondrial membrane transport protein, Biology (General), Endoplasmic reticulum membrane, General Immunology and Microbiology, biology, General Neuroscience, Endoplasmic reticulum, Cell Biology, subcellular regions, General Medicine, Tools and Resources, 3. Good health, Cell biology, Cytosol, 030104 developmental biology, Biotinylation, Proteome, Translocase of the inner membrane, microscopy, biology.protein, Medicine, Signal transduction, Human

Abstract

The cytosol-facing membranes of cellular organelles contain proteins that enable signal transduction, regulation of morphology and trafficking, protein import and export, and other specialized processes. Discovery of these proteins by traditional biochemical fractionation can be plagued with contaminants and loss of key components. Using peroxidase-mediated proximity biotinylation, we captured and identified endogenous proteins on the outer mitochondrial membrane (OMM) and endoplasmic reticulum membrane (ERM) of living human fibroblasts. The proteomes of 137 and 634 proteins, respectively, are highly specific and highlight 94 potentially novel mitochondrial or ER proteins. Dataset intersection identified protein candidates potentially localized to mitochondria-ER contact sites. We found that one candidate, the tail-anchored, PDZ-domain-containing OMM protein SYNJ2BP, dramatically increases mitochondrial contacts with rough ER when overexpressed. Immunoprecipitation-mass spectrometry identified ribosome-binding protein 1 (RRBP1) as SYNJ2BP’s ERM binding partner. Our results highlight the power of proximity biotinylation to yield insights into the molecular composition and function of intracellular membranes., United States. National Institutes of Health (R01 CA186568), United States. National Institutes of Health (R01 GM077465)

Published

2017

75. Author response: Proteomic mapping of cytosol-facing outer mitochondrial and ER membranes in living human cells by proximity biotinylation

Author

Victoria Hung, Stephanie S Lam, Namrata D Udeshi, Tanya Svinkina, Gaelen Guzman, Vamsi K Mootha, Steven A Carr, and Alice Y Ting

Published

2017

76. Probing the lithium-response pathway in hiPSCs implicates the phosphoregulatory set-point for a cytoskeletal modulator in bipolar pathogenesis

Author

Fumio Nakamura, Husseini K. Manji, Namrata D. Udeshi, Hagop S. Akiskal, Jeffrey H. Price, Nikolaos Venizelos, Wen-Ning Zhao, Cordulla Duerr, Ryan W. Logan, Jeffrey S. Nye, Jasmin Lalonde, Steven D. Sheridan, Joseph T. Coyle, Toshio Ohshima, Yoshio Goshima, Michael McCarthy, Shelley Halpain, Barbara Calabrese, Joshua G. Hunsberger, Martin Alda, Yuuka Inoue, Gustavo J. Gutierrez, Stephen J. Haggarty, Brian T. D. Tobe, Cameron D. Pernia, Richard L. Sidman, Moyuka Wada, Hiroko Makihara, Laurence M. Brill, Glenn T. Konopaske, Yang Liu, De-Maw M. Chuang, Ranor C. B. Basa, Alicia M. Winquist, Yang D. Teng, Michelle M. Sidor, Steven A. Carr, Colleen A. McClung, Guy A. Rouleau, Katsuhiko Mikoshiba, Evan Y. Snyder, Laurel Dorsett, Lina Mastrangelo, Guang Chen, Jianxue Li, Haruko Nakamura, Andrew Crain, Philipp Mertins, Michael G. Brandel, Dongmei Wu, Naoya Yamashita, and Biology

Subjects

0301 basic medicine, Genetically modified mouse, Proteomics, Dendritic spine, Bipolar Disorder, Induced Pluripotent Stem Cells, Medical Biotechnology (with a focus on Cell Biology (including Stem Cell Biology), Molecular Biology, Microbiology, Biochemistry or Biopharmacy), Nerve Tissue Proteins, Biology, Lithium, Models, Biological, Psykiatri, 03 medical and health sciences, Mice, 0302 clinical medicine, posttranslational modification, proteomics, psychiatric disease modeling, CRMP2, dendrites, Calcium flux, mental disorders, medicine, Animals, Humans, Induced pluripotent stem cell, Medicinsk bioteknologi (med inriktning mot cellbiologi (inklusive stamcellsbiologi), molekylärbiologi, mikrobiologi, biokemi eller biofarmaci), Cells, Cultured, Brain Chemistry, Psychiatry, Multidisciplinary, Neurosciences, 030104 developmental biology, medicine.anatomical_structure, PNAS Plus, Phosphorylation, Intercellular Signaling Peptides and Proteins, Calcium, Neuron, Collapsin response mediator protein family, Neuroscience, Protein Processing, Post-Translational, 030217 neurology & neurosurgery, Intracellular, Neurovetenskaper

Abstract

The molecular pathogenesis of bipolar disorder (BPD) is poorly understood. Using human-induced pluripotent stem cells (hiPSCs) to unravel such mechanisms in polygenic diseases is generally challenging. However, hiPSCs from BPD patients responsive to lithium offered unique opportunities to discern lithium's target and hence gain molecular insight into BPD. By profiling the proteomics of BDP-hiPSC-derived neurons, we found that lithium alters the phosphorylation state of collapsin response mediator protein-2 (CRMP2). Active non-phosphorylated CRMP2, which binds cytoskeleton, is present throughout the neuron; inactive phosphorylated CRMP2, which dissociates from cytoskeleton, exits dendritic spines. CRMP2 elimination yields aberrant dendritogenesis with diminished spine density and lost lithium responsiveness (LiR). The "set-point" for the ratio of pCRMP2: CRMP2 is elevated uniquely in hiPSC-derived neurons from LiR BPD patients, but not with other psychiatric (including lithium-nonresponsive BPD) and neurological disorders. Lithium (and other pathway modulators) lowers pCRMP2, increasing spine area and density. Human BPD brains show similarly elevated ratios and diminished spine densities; lithium therapy normalizes the ratios and spines. Consistent with such "spine-opathies," human LiR BPD neurons with abnormal ratios evince abnormally steep slopes for calcium flux; lithium normalizes both. Behaviorally, transgenic mice that reproduce lithium's postulated site-of-action in dephosphorylating CRMP2 emulate LiR in BPD. These data suggest that the " lithium response pathway" in BPD governs CRMP2's phosphorylation, which regulates cytoskeletal organization, particularly in spines, modulating neural networks. Aberrations in the posttranslational regulation of this developmentally critical molecule may underlie LiR BPD pathogenesis. Instructively, examining the proteomic profile in hiPSCs of a functional agent-even one whose mechanism-of-action is unknown-might reveal otherwise inscrutable intracellular pathogenic pathways., Funding Agencies:NIH's Library of Integrated Network-based Cellular Signatures Program Viterbi Foundation Neuroscience Initiative Stanley Medical Research Institute R21MH093958 R33MH087896 R01MH095088 Tau Consortium California Institute of Regenerative Medicine training grants University of California, San Diego T32 training grant in psychiatry California Bipolar Foundation International Bipolar Foundation Creation of Innovation Centers for Advanced Interdisciplinary Research Areas Program in the Project for Developing Innovation Systems from the Ministry of Education, Science, Sports and Culture in Japan 42890001 RC2MH090011

Published

2017

77. An Unbiased Approach To Identify Endogenous Substrates of 'Histone' Deacetylase 8

Author

Patrick McCarren, Aravind Subramanian, Noah A. Wolfson, Xiaodong Lu, Fanny Lazzaro, Yan Ling Zhang, Carol Ann Pitcairn, Florence F. Wagner, Ted Natoli, Jennifer P. Gale, Tanya Svinkina, Steven A. Carr, Eric D. Sullivan, Edward B. Holson, Jacob D. Jaffe, Doug Barker, Carol A. Fierke, Joshiawa Paulk, David E. Olson, Eleanor A. Howe, and Namrata D. Udeshi

Subjects

Proteomics, Computational biology, Biology, Biochemistry, Chromatin remodeling, Histone Deacetylases, Substrate Specificity, Transcription (biology), Humans, Letters, Protein Interaction Maps, Nuclear protein, Transcription factor, Genetics, Nuclear Proteins, HDAC8, Acetylation, General Medicine, 3. Good health, DNA-Binding Proteins, Histone Deacetylase Inhibitors, Repressor Proteins, RNA splicing, Molecular Medicine, Transcription Factors

Abstract

Despite being extensively characterized structurally and biochemically, the functional role of histone deacetylase 8 (HDAC8) has remained largely obscure due in part to a lack of known cellular substrates. Herein, we describe an unbiased approach using chemical tools in conjunction with sophisticated proteomics methods to identify novel non-histone nuclear substrates of HDAC8, including the tumor suppressor ARID1A. These newly discovered substrates of HDAC8 are involved in diverse biological processes including mitosis, transcription, chromatin remodeling, and RNA splicing and may help guide therapeutic strategies that target the function of HDAC8.

Published

2014

78. Proteomic Mapping of the Human Mitochondrial Intermembrane Space in Live Cells via Ratiometric APEX Tagging

Author

Steven A. Carr, Vamsi K. Mootha, Tanya Svinkina, Alice Y. Ting, Hyun-Woo Rhee, Victoria Hung, Namrata D. Udeshi, Valentin Cracan, Peng Zou, Broad Institute of MIT and Harvard, Massachusetts Institute of Technology. Department of Chemistry, Hung, Victoria, Zou, Peng, Rhee, Hyun-Woo, Carr, Steven A, Mootha, Vamsi, and Ting, Alice Y

Subjects

Proteome, Mitochondrial intermembrane space, Blotting, Western, HEK 293 cells, Cell Biology, Computational biology, Biology, Cell Fractionation, Bioinformatics, Article, Apex (geometry), Mitochondrial Proteins, Cytosol, HEK293 Cells, Isotope Labeling, Stable isotope labeling by amino acids in cell culture, Mitochondrial Membranes, Humans, Molecular Biology, Mitochondrial protein, Function (biology)

Abstract

Obtaining complete protein inventories for subcellular regions is a challenge that often limits our understanding of cellular function, especially for regions that are impossible to purify and are therefore inaccessible to traditional proteomic analysis. We recently developed a method to map proteomes in living cells with an engineered peroxidase (APEX) that bypasses the need for organellar purification when applied to membrane-bound compartments; however, it was insufficiently specific when applied to unbounded regions that allow APEX-generated radicals to escape. Here, we combine APEX technology with a SILAC-based ratiometric tagging strategy to substantially reduce unwanted background and achieve nanometer spatial resolution. This is applied to map the proteome of the mitochondrial intermembrane space (IMS), which can freely exchange small molecules with the cytosol. Our IMS proteome of 127 proteins has >94% specificity and includes nine newly discovered mitochondrial proteins. This approach will enable scientists to map proteomes of cellular regions that were previously inaccessible., United States. National Institutes of Health (DP1 OD003961)

Published

2014

79. Oncogenic Mechanisms of CBL E3 Ubiquitin Ligase Mutations in Myeloid Malignancies

Author

Monica Schenone, Roger Belizaire, Eric Padron, Alexis Vedder, Lei Sun, Namrata D. Udeshi, Steven A. Carr, Benjamin L. Ebert, and Sebastian Koochaki

Subjects

Mutation, biology, Chemistry, Immunology, Cell Biology, Hematology, medicine.disease_cause, environment and public health, Biochemistry, Ubiquitin ligase, Cell biology, enzymes and coenzymes (carbohydrates), LYN, hemic and lymphatic diseases, biology.protein, medicine, Phosphorylation, Src family kinase, biological phenomena, cell phenomena, and immunity, Signal transduction, Protein kinase B, hormones, hormone substitutes, and hormone antagonists, PI3K/AKT/mTOR pathway

Abstract

CBL encodes an E3 ubiquitin ligase and signaling adaptor that acts downstream of cytokine receptors. Recurrent CBL mutations are found in a variety of myeloid disorders, including 10-15% of chronic myelomonocytic leukemia (CMML) cases, and specifically disrupt the protein's RING domain, which is responsible for E3 ligase activity; adaptor domains of CBL, including the tyrosine kinase-binding domain (TKB), proline-rich region (PRR) and C-terminal phosphotyrosine (pY) residues, remain intact in the context of RING mutations. In prior studies, CBL RING mutations were associated with hyperactivation of signaling pathways that drive cell proliferation. However, the precise mechanism by which CBL mutants act remains incompletely understood. Here we combined functional assays and mass spectrometry (MS) to comprehensively define the phosphoproteome, CBL interactome and molecular mechanism of signaling hyperactivation in a panel of cell lines expressing an allelic series of CBL RING mutants. We identified the SRC family kinase LYN as a key driver of signaling by CBL RING mutants; furthermore, we demonstrated in vitro and in vivo efficacy of LYN inhibition by dasatinib in CBL-mutant cell lines and primary CMML patient samples. We generated cell lines expressing wild-type (WT) or RING-mutant CBL using IL3-dependent mouse 32D cells and GM-CSF-dependent human TF1 cells. Cells expressing CBL RING mutants Y371H, C384Y or R420Q had a proliferative advantage over CBL WT or CBL knockout cells. To determine the role of CBL's adaptor domains in the proliferative advantage conferred by CBL RING mutants, we generated double mutants comprising the C384Y RING mutation in cis with mutations in the TKB domain (G306E), PRR (Δ477-688) or pY residues (Y700/731/774F). The proliferative advantage of cells expressing CBL C384Y was significantly reduced with mutation of the TKB domain, PRR or pY residues, indicating that CBL's adaptor domains are critical for the proliferative advantage of cells expressing RING-mutant CBL. To assess the effects of CBL RING mutation on signaling, we used MS to measure global protein phosphorylation in 32D cells expressing CBL WT or CBL C384Y. Activation of LYN and the PI3 kinase (PI3K) pathway were most significantly increased in cells expressing CBL C384Y compared to CBL WT; western blot confirmed increased phosphorylation of LYN, the PI3K p85 subunit and AKT in cells expressing CBL Y371H, C384Y or R420Q. We next employed immunoprecipitation (IP) followed by MS to characterize the global CBL interactome in 32D cells expressing CBL WT or RING mutants Y371H, C384Y or R420Q. In line with the phosphoproteomic analysis, LYN showed significantly increased binding to CBL RING mutants; the PI3K p85 subunit also showed increased binding to CBL RING mutants. Thus, global proteomic analyses revealed that increased binding of LYN and p85 to CBL RING mutants was directly associated with hyperactivation of LYN and PI3K-AKT signaling pathways. Deletion of CBL's PRR reduced interactions with both LYN and p85, and the CBL-p85 interaction required CBL Y731. Genetic ablation or inhibition of LYN by dasatinib decreased binding of p85 to CBL, suggesting that increased CBL Y731 phosphorylation by LYN enabled the CBL-p85 interaction. Indeed, CBL Y731 phosphorylation and AKT activation were diminished by deletion of CBL's PRR, LYN knockout or LYN inhibition by dasatinib. Altogether, these data demonstrated that enhanced LYN activation in cells expressing RING-mutant CBL drives increased CBL phosphorylation, p85 recruitment and downstream AKT signaling. Given the central role of LYN in signaling by CBL RING mutants, we hypothesized that LYN inhibition by dasatinib would abrogate the hyperproliferation of cells expressing CBL RING mutants. Dasatinib blocked the proliferative advantage of 32D and TF1 cells expressing CBL RING mutants. In addition, dasatinib significantly reduced the number of methylcellulose colonies formed by bone marrow mononuclear cells from 2 patients with CBL-mutated CMML; dasatinib treatment of mice xenografted with the same CMML cells resulted in a substantial decrease in leukemia burden compared to vehicle-treated mice. In summary, we have defined a mechanism by which LYN promotes PI3K-AKT signaling through CBL RING mutants. Our data provide rationale for exploring the therapeutic potential of LYN and/or PI3K-AKT inhibition in patients with CBL-mutated myeloid malignancies. Disclosures Ebert: Celgene: Research Funding; Deerfield: Research Funding.

Published

2019

80. Glucocorticoids Induce the Maintenance and Expansion of an Immature CFU-E Erythroid Progenitor Population in Humans

Author

Julien Papoin, Meagan E. Olive, Naomi Taylor, Ryan Ashley, Hongxia Yan, Brian M. Dulmovits, Christopher D. Hillyer, Nan Wang, Lydie Da Costa, Steven A. Carr, Namrata D. Udeshi, Jeffrey M. Lipton, Anupama Narla, Adrianna Vlachos, Lionel Blanc, Sandrina Kinet, Mohandas Narla, and John Hale

Subjects

education.field_of_study, Erythroid progenitor, Immunology, Population, Transferrin receptor, Cell Biology, Hematology, Biology, medicine.disease, Biochemistry, Cell biology, Immunophenotyping, medicine.anatomical_structure, medicine, Bone marrow, Diamond–Blackfan anemia, education, Transcription factor, CFU-E

Abstract

Glucocorticoids are widely used to increase red cell production in a number of hematological disorders including Diamond Blackfan anemia (DBA). Despite their clinical effectiveness we do not fully understand the mechanistic basis for the regulation of human erythropoiesis by glucocorticoids. To improve the clinical management of these patients, we studied the mechanisms of dexamethasone (Dex) on human erythroid progenitors. We employed an erythroid culture system to differentiate primary human CD34+ cells isolated from patients with DBA and healthy controls as well as cord blood samples. We found that Dex increases the proliferation of CD34+ cells derived from peripheral blood but surprisingly not of CD34+ cells from cord blood. Furthermore, by mass spectrometry proteomic analysis, we found that Dex specifically altered the induction of several targets unique to peripheral blood including the transcription factor and cell cycle regulator NR4A1. When examining the cell populations expanded with Dex treatment by immunophenotyping, we detected a specific expansion of CFU-Es. Dex increased the average size of CFU-E colonies in methylcellulose colony forming assays in the presence of Epo alone, suggesting that CFU-Es are the most Dex responsive progenitor in humans. In support of this hypothesis, reticulocyte counts from patients with DBA treated with prednisone were found to increase approximately one week after treatment, consistent with the time course of differentiation of CFU-E to reticulocytes in bone marrow. In order to further resolve the progenitor target of steroid responsive progenitor we developed a new gating scheme that allows for increased resolution of BFU-E and CFU-E subpopulations by monitoring surface expression of CD71 and CD105. Using this system, we found that Dex treatment led to the maintenance of a novel immature transitional progenitor population in peripheral blood-derived cells that we term immature CFU-E. In methylcellulose colony forming assays, these peripheral blood-derived immature CFU-E treated with Dex produced larger colonies than the untreated controls and mature CFU-E. The expansion and proliferation of Dex treated immature CFU-Es derived from peripheral blood was associated with a decreased percentage of cells in the S phase of the cell cycle. No change was noted for either Dex treated BFU-E from peripheral blood or for BFU-E or CFU-E from cord blood. Importantly, Dex responsive peripheral blood-derived CFU-Es divided at a faster rate than untreated CFU-Es, revealing a dissociation in the link between differentiation and proliferation. Mechanistically, we found that Dex treated peripheral blood CFU-E exhibited increased expression of the negative cell cycle regulator p57Kip2. Moreover, this protein was also found to be dysregulated in CD34+ cells from transfusion-dependent patients with DBA, wherein p57Kip2 expression was not significantly altered following Dex treatment, indicating a role for p57Kip2 in the erythroid progenitor defects seen in these patients. To further evaluate the role of p57Kip2 in the Dex dependent alteration in CFU-E proliferation, peripheral blood-derived CD34+ cells were transduced with p57Kip2-specific shRNA lentiviral constructs. shRNA knockdown of p57Kip2 abrogated the effects of Dex on growth and induced a premature EPO-mediated differentiation. In summary, our findings provide new insights into functional heterogeneity of human erythroid progenitors and reveal mechanistic insights into the action of Dex in normal and disordered erythropoiesis. Disclosures Vlachos: Novartis: Other: Steering committee member.

Published

2019

81. EMRE Is an Essential Component of the Mitochondrial Calcium Uniporter Complex

Author

Yasemin Sancak, Namrata D. Udeshi, Sarah E. Calvo, Toshimori Kitami, Andrew L. Markhard, Olga Goldberger, Steven A. Carr, David E. Clapham, Andrew A. Li, Kimberli J. Kamer, Erika Kovács-Bogdán, Dipayan Chaudhuri, and Vamsi K. Mootha

Subjects

Proteomics, Molecular Sequence Data, Mitochondrion, LETM1, Mitochondrial Membrane Transport Proteins, Article, Mitochondrial membrane transport protein, Calcium-binding protein, Humans, Inner membrane, Mitochondrial calcium uptake, Amino Acid Sequence, EF Hand Motifs, Uniporter, Cation Transport Proteins, Phylogeny, Multidisciplinary, biology, Calcium channel, Calcium-Binding Proteins, Cell Membrane, Mitochondria, Protein Structure, Tertiary, Cell biology, HEK293 Cells, Gene Knockdown Techniques, biology.protein, Calcium Channels

Abstract

The mitochondrial uniporter is a highly selective calcium channel in the organelle's inner membrane. Its molecular components include the EF-hand-containing calcium-binding proteins mitochondrial calcium uptake 1 (MICU1) and MICU2 and the pore-forming subunit mitochondrial calcium uniporter (MCU). We sought to achieve a full molecular characterization of the uniporter holocomplex (uniplex). Quantitative mass spectrometry of affinity-purified uniplex recovered MICU1 and MICU2, MCU and its paralog MCUb, and essential MCU regulator (EMRE), a previously uncharacterized protein. EMRE is a 10-kilodalton, metazoan-specific protein with a single transmembrane domain. In its absence, uniporter channel activity was lost despite intact MCU expression and oligomerization. EMRE was required for the interaction of MCU with MICU1 and MICU2. Hence, EMRE is essential for in vivo uniporter current and additionally bridges the calcium-sensing role of MICU1 and MICU2 with the calcium-conducting role of MCU.

Published

2013

82. Integrated proteomic analysis of post-translational modifications by serial enrichment

Author

Karl R. Clauser, Namrata D. Udeshi, Michael A. Gillette, Jacob D. Jaffe, Jana W. Qiao, Michael Burgess, Steven A. Carr, Jinal Patel, Philipp Mertins, and D. R. Mani

Subjects

Proteome, Gene Expression Profiling, Systems biology, Ubiquitination, Saccharomyces cerevisiae, Cell Biology, Biology, Proteomics, Ubiquitinated Proteins, Biochemistry, Article, Mass Spectrometry, Cell biology, Fungal Proteins, Gene expression profiling, Ubiquitin, Acetylation, Protein Interaction Mapping, biology.protein, Phosphorylation, Protein Processing, Post-Translational, Molecular Biology, Quantitative analysis (chemistry), Biotechnology

Abstract

We report a mass spectrometry–based method for the integrated analysis of protein expression, phosphorylation, ubiquitination and acetylation by serial enrichments of different post-translational modifications (SEPTM) from the same biological sample. this technology enabled quantitative analysis of nearly 8,000 proteins and more than 20,000 phosphorylation, 15,000 ubiquitination and 3,000 acetylation sites per experiment, generating a holistic view of cellular signal transduction pathways as exemplified by analysis of bortezomib-treated human leukemia cells.

Published

2013

83. Proteomic Analysis of Unbounded Cellular Compartments: Synaptic Clefts

Author

Emily K. Lehrman, Philipp Stawski, Mark H. Ellisman, Beth Stevens, Austin S. Draycott, Thomas J. Deerinck, Daniel K. Wilton, Ken H. Loh, Tanya Svinkina, Alice Y. Ting, Steven A. Carr, and Namrata D. Udeshi

Subjects

0301 basic medicine, Proteomics, Proteome, Neuronal, Bioinformatics, Medical and Health Sciences, Mice, GABA, Thalamus, Receptors, GABAergic Neurons, Receptor, Neural Cell Adhesion Molecules, Membrane Glycoproteins, Biological Sciences, CD, Neurological, Excitatory postsynaptic potential, Biotechnology, Cell Adhesion Molecules, Neuronal, Recombinant Fusion Proteins, 1.1 Normal biological development and functioning, Synaptic Membranes, Glutamic Acid, Immunoglobulins, Nerve Tissue Proteins, Biology, Inhibitory postsynaptic potential, Article, General Biochemistry, Genetics and Molecular Biology, 03 medical and health sciences, Receptors, GABA, Antigens, CD, Underpinning research, Animals, Humans, Antigens, Cellular compartment, Peroxidase, HEK 293 cells, Neurosciences, Rats, 030104 developmental biology, HEK293 Cells, MDGA2, Neuroscience, Cell Adhesion Molecules, Developmental Biology

Abstract

Cellular compartments that cannot be biochemically isolated are challenging to characterize. Here we demonstrate the proteomic characterization of the synaptic clefts that exist at both excitatory and inhibitory synapses. Normal brain function relies on the careful balance of these opposing neural connections, and understanding how this balance is achieved relies on knowledge of their protein compositions. Using a spatially restricted enzymatic tagging strategy, we mapped the proteomes of two of the most common excitatory and inhibitory synaptic clefts in living neurons. These proteomes reveal dozens of synaptic candidates, and assign numerous known synaptic proteins to a specific cleft type. The molecular differentiation of each cleft allowed us to identify Mdga2 as a potential specificity factor influencing Neuroligin-2's recruitment of presynaptic neurotransmitters at inhibitory synapses.

Published

2016

84. Identification and Origin of N-Linked β-<scp>d</scp>-N-Acetylglucosamine Monosaccharide Modifications on Arabidopsis Proteins

Author

Bruce A. Witthuhn, Matthew D. Stone, Donald F. Hunt, Young Cheon Kim, Jeffrey Shabanowitz, Namrata D. Udeshi, Neil E. Olszewski, Todd W. Markowski, and Neal Jahren

Subjects

Glycan, Physiology, Endoplasmic reticulum, Plant Science, Biology, Golgi apparatus, biology.organism_classification, carbohydrates (lipids), Serine, Electron-transfer dissociation, chemistry.chemical_compound, symbols.namesake, chemistry, Biochemistry, Arabidopsis, Genetics, N-Acetylglucosamine, symbols, biology.protein, Threonine

Abstract

Many plant proteins are modified with N-linked oligosaccharides at asparagine-X-serine/threonine sites during transit through the endoplasmic reticulum and the Golgi. We have identified a number of Arabidopsis (Arabidopsis thaliana) proteins with modifications consisting of an N-linked N-acetyl-d-glucosamine monosaccharide (N-GlcNAc). Electron transfer dissociation mass spectrometry analysis of peptides bearing this modification mapped the modification to asparagine-X-serine/threonine sites on proteins that are predicted to transit through the endoplasmic reticulum and Golgi. A mass labeling method was developed and used to study N-GlcNAc modification of two thioglucoside glucohydrolases (myrosinases), TGG1 and TGG2 (for thioglucoside glucohydrolase). These myrosinases are also modified with high-mannose (Man)-type glycans. We found that N-GlcNAc and high-Man-type glycans can occur at the same site. It has been hypothesized that N-GlcNAc modifications are generated when endo-β-N-acetylglucosaminidase (ENGase) cleaves N-linked glycans. We examined the effects of mutations affecting the two known Arabidopsis ENGases on N-GlcNAc modification of myrosinase and found that modification of TGG2 was greatly reduced in one of the single mutants and absent in the double mutant. Surprisingly, N-GlcNAc modification of TGG1 was not affected in any of the mutants. These data support the hypothesis that ENGases hydrolyze high-Man glycans to produce some of the N-GlcNAc modifications but also suggest that some N-GlcNAc modifications are generated by another mechanism. Since N-GlcNAc modification was detected at only one site on each myrosinase, the production of the N-GlcNAc modification may be regulated.

Published

2012

85. Quantitative Assessment of Chromatin Immunoprecipitation Grade Antibodies Directed against Histone Modifications Reveals Patterns of Co-occurring Marks on Histone Protein Molecules

Author

Steven A. Carr, Emily L. Rudomin, Jacob D. Jaffe, Sally E. Peach, and Namrata D. Udeshi

Subjects

Chromatin Immunoprecipitation, Biology, Methylation, Biochemistry, Antibodies, Chromatin remodeling, Analytical Chemistry, Histones, Histone H3, Histone H1, Antibody Specificity, Histone H2A, Cluster Analysis, Humans, Histone code, Histone octamer, Phosphorylation, Molecular Biology, Research, Acetylation, Molecular biology, Cell biology, Histone methyltransferase, Protein Processing, Post-Translational, Chromatin immunoprecipitation, HeLa Cells, Protein Binding

Abstract

The defining step in most chromatin immunoprecipitation (ChIP) assays is the use of an antibody to enrich for a particular protein or histone modification state associated with segments of chromatin. The specificity of the antibody is critical to the interpretation of the experiment, yet this property is rarely reported. Here, we present a quantitative method using mass spectrometry to characterize the specificity of key histone H3 modification-targeting antibodies that have previously been used to characterize the “histone code.” We further extend the use of these antibody reagents to the observation of long range correlations among disparate histone modifications. Using purified human histones representing the mixture of chromatin states present in living cells, we were able to quantify the degree of target enrichment and the specificity of several commonly used, commercially available ChIP grade antibodies. We found significant differences in enrichment efficiency among various reagents directed against four frequently studied chromatin marks: H3K4me2, H3K4me3, H3K9me3, and H3K27me3. For some antibodies, we also detected significant off target enrichment of alternate modifications at the same site (i.e., enrichment of H3K4me2 by an antibody directed against H3K4me3). Through cluster analysis, we were able to recognize patterns of co-enrichment of marks at different sites on the same histone protein. Surprisingly, these co-enrichments corresponded well to “canonical” chromatin states that are exemplary of activated and repressed regions of chromatin. Altogether, our findings suggest that 1) the results of ChIP experiments need to be evaluated with caution given the potential for cross-reactivity of the commonly used histone modification recognizing antibodies, 2) multiple marks with consistent biological interpretation exist on the same histone protein molecule, and 3) some components of the histone code may be transduced on single proteins in living cells.

Published

2012

86. Deep, Quantitative Coverage of the Lysine Acetylome Using Novel Anti-acetyl-lysine Antibodies and an Optimized Proteomic Workflow

Author

Jana Qiao, Eric Kuhn, Tanya Svinkina, Shaunt Fereshetian, Jacob D. Jaffe, Steven A. Carr, Hongbo Gu, Philipp Mertins, Namrata D. Udeshi, and Jeffrey C. Silva

Subjects

Proteomics, Special Issue Articles, Lysine, Peptide, Mass spectrometry, Biochemistry, Mass Spectrometry, Analytical Chemistry, Workflow, Jurkat Cells, Mice, Ubiquitin, Stable isotope labeling by amino acids in cell culture, Animals, Humans, Molecular Biology, chemistry.chemical_classification, Chromatography, biology, Chemistry, Antibodies, Monoclonal, Mammary Neoplasms, Experimental, Acetylation, Liver, biology.protein, Phosphorylation, Female, Protein Processing, Post-Translational

Abstract

Introduction of antibodies specific for acetylated lysine has significantly improved the detection of endogenous acetylation sites by mass spectrometry. Here, we describe a new, commercially available mixture of anti-lysine acetylation (Kac) antibodies and show its utility for in-depth profiling of the acetylome. Specifically, seven complementary monoclones with high specificity for Kac were combined into a final anti-Kac reagent which results in at least a twofold increase in identification of Kac peptides over a commonly used Kac antibody. We outline optimal antibody usage conditions, effective offline basic reversed phase separation, and use of state-of-the-art LC-MS technology for achieving unprecedented coverage of the acetylome. The methods were applied to quantify acetylation sites in suberoylanilide hydroxamic acid-treated Jurkat cells. Over 10,000 Kac peptides from over 3000 Kac proteins were quantified from a single stable isotope labeling by amino acids in cell culture labeled sample using 7.5 mg of peptide input per state. This constitutes the deepest coverage of acetylation sites in quantitative experiments obtained to-date. The approach was also applied to breast tumor xenograft samples using isobaric mass tag labeling of peptides (iTRAQ4, TMT6 and TMT10-plex reagents) for quantification. Greater than 6700 Kac peptides from over 2300 Kac proteins were quantified using 1 mg of tumor protein per iTRAQ 4-plex channel. The novel reagents and methods we describe here enable quantitative, global acetylome analyses with depth and sensitivity approaching that obtained for other well-studied post-translational modifications such as phosphorylation and ubiquitylation, and should have widespread application in biological and clinical studies employing mass spectrometry-based proteomics.

Published

2015

87. Pomalidomide-Based Homo-Protacs for the Chemical Knockdown of Cereblon

Author

Jan Krönke, Steven A. Carr, Namrata D. Udeshi, Hannes Kehm, Stefanie Lindner, Michael Gütschow, Christian Steinebach, Deepak Mani, and Simon Köpff

Subjects

biology, Chemistry, Cereblon, Immunology, Cell Biology, Hematology, Pomalidomide, Biochemistry, Ubiquitin ligase, Cell biology, DDB1, biology.protein, Proteasome inhibitor, medicine, Neddylation, CUL4A, Cullin, medicine.drug

Abstract

The immunomodulatory drugs (IMiDs) thalidomide, lenalidomide, and pomalidomide are all approved for the treatment of multiple myeloma. IMiDs bind cereblon (CRBN), a substrate adaptor for the CRL4 E3 ubiquitin ligase (CRL4CRBN). In multiple myeloma, IMiDs enhance the binding of the lymphoid transcription factors Ikaros (IKZF1) and Aiolos (IKZF3) to CRL4CRBN, leading to their ubiquitination and degradation. Depletion of IKZF1 and IKZF3 results in growth inhibition in multiple myeloma cells. In addition, IMiDs can block the physiologic function of CRBN what has been shown to contribute to the anti-proliferative effects as well as other properties of the drug. Recently, IMiDs were exploited for the generation of Proteolysis Targeting Chimeras (PROTACs). These molecules link the IMiD structure to another small molecule that binds a protein of interest (POI). Such IMiD-based PROTACs are capable to guide the CRBN-CRL4 E3 ligase to the POI, resulting in its ubiquitination and degradation. Here, we designed pomalidomide-based homobifunctional PROTACs and investigated their ability to induce self-directed CRBN ubiquitination and degradation (Figure 1A). We evaluated different attachment strategies, modifications and linker lengths and tested the effect of a series of homo-dimeric compounds on their potency to deplete CRBN protein levels. The homodimeric compound 15a with a linker length of 8 atoms was identified as the most potent CRBN degrader with a minimal remaining effect on IKZF1 (Figure 1B). Homodimeric PROTACs with longer linkers exhibited a weaker capability for CRBN degradation and had a more potent effect on IKZF1 protein levels. The effect of compound 15a on CRBN was blocked after pre-treatment with a proteasome inhibitor or MLN4924, a neddylation activating enzyem inhibitor that blocks Cullin E3 ligases. Co-immunoprecipitation revealed that 15a induces interaction of two CRBN molecules. The homo-PROTAC 15a was active at low concentrations below 100 nM and had long-lasting effects on the intracellular CRBN level (Figure 1B). Applying global proteome analyses in the multiple myeloma cell line MM1.S demonstrated that PROTAC 15a specifically induced degradation of CRBN and had only weak effects on IKZF1 and IKZF3 and no effect on the other members of the CRL4 ligase family, including DDB1 and CUL4A which are in close proximity to CRBN in the CRL4CRBN complex. CRBN inactivation by our compounds had no effect on proliferation of different multiple myeloma cell lines. Pre-treatment with Homo-PROTAC 15a prevented pomalidomide-induced degradation of IKZF1 and IKZF3, and antagonized the effects of pomalidomide and lenalidomide on multiple myeloma cell growth. This was consistent with genetic inactivation of CRBN by CRISPR/Cas9. In conclusion, we generated the first chemical inhibitors of CRBN that can serve as a useful tool for future biomedical investigations on CRBN-related signaling. These compounds will also help to discriminate whether an IMiD effect depends on CRBN-mediated targeted degradation of neo-substrates or from blocking the physiologic function of CRBN. Furthermore, our data confirm the essential role of CRBN in IMiD activity in multiple myeloma. Figure 1. Figure 1. Disclosures No relevant conflicts of interest to declare.

Published

2018

88. A PGC-1α-O-GlcNAc Transferase Complex Regulates FoxO Transcription Factor Activity in Response to Glucose

Author

Gerald W. Hart, Michael P. Housley, Pere Puigserver, Donald F. Hunt, Joseph T. Rodgers, Jeffrey Shabanowitz, and Namrata D. Udeshi

Subjects

Transcription, Genetic, Acylation, Response element, E-box, Transcription coregulator, N-Acetylglucosaminyltransferases, Biochemistry, Acetylglucosamine, Cell Line, Sp3 transcription factor, Multienzyme Complexes, Humans, Molecular Biology, Transcription factor, Heat-Shock Proteins, General transcription factor, biology, Forkhead Box Protein O1, Mechanisms of Signal Transduction, Forkhead Transcription Factors, Promoter, Cell Biology, Peroxisome Proliferator-Activated Receptor Gamma Coactivator 1-alpha, Activating transcription factor 2, biology.protein, Energy Metabolism, Protein Processing, Post-Translational, Transcription Factors

Abstract

Metabolic and stress response gene regulation is crucial for the survival of an organism to a changing environment. Three key molecules that sense nutrients and broadly affect gene expression are the FoxO transcription factors, the transcriptional co-activator PGC-1alpha, and the dynamic post-translational modification, O-linked beta-N-acetylglucosamine (O-GlcNAc). Here we identify novel post-translational modifications of PGC-1alpha, including O-GlcNAc, and describe a novel mechanism for how PGC-1alpha co-activates transcription by FoxOs. In liver, in cultured cells, and in vitro with recombinant proteins, PGC-1alpha binds to O-GlcNAc transferase and targets the enzyme to FoxOs, resulting in their increased GlcNAcylation and increased transcriptional activity. Furthermore, glucose-enhanced activation of FoxO1 occurs via this PGC-1alpha-O-GlcNAc transferase-mediated GlcNAcylation. Therefore, one mechanism by which PGC-1alpha can serve as a co-activator of transcription is by targeting the O-GlcNAc transferase to increase GlcNAcylation of specific transcription factors important to nutrient/stress sensing and energy metabolism.

Published

2009

89. Analysis of proteins and peptides on a chromatographic timescale by electron-transfer dissociation MS

Author

Kristie L. Rose, Namrata D. Udeshi, Donald F. Hunt, and Jeffrey Shabanowitz

Subjects

Electron-transfer dissociation, Chromatography, Protein mass spectrometry, Fragmentation (mass spectrometry), Chemistry, Cell Biology, Quadrupole ion trap, Mass spectrometry, Top-down proteomics, Tandem mass spectrometry, Molecular Biology, Biochemistry, Peptide sequence

Abstract

Peptide and protein sequence analysis using a combination of gas-phase ion-ion chemistry and tandem MS is described. Samples are converted to multiply charged ions by ESI and then allowed to react with fluoranthene radical anions in a quadrupole linear ion trap mass spectrometer. Electron transfer from the radical anion to the multiply charged peptide or protein promotes random fragmentation along the amide backbone that is independent of peptide or protein size, sequence, or the presence of post-translational modifications. Examples are provided that demonstrate the utility of electron-transfer dissociation for characterizing post-translational modifications and for identifying proteins in mixtures on a chromatographic timescale (500 ms/protein).

Published

2007

90. In Situ Peroxidase Labeling and Mass-Spectrometry Connects Alpha-Synuclein Directly to Endocytic Trafficking and mRNA Metabolism in Neurons

Author

Yelena Freyzon, David E. Hill, Pavan K. Auluck, Marc Vidal, Vikram Khurana, Alice Y. Ting, Song Yi, Valeriya Baru, Namrata D. Udeshi, Nidhi Sahni, Susan Lindquist, Chee Yeun Chung, Steven A. Carr, and Ken H. Loh

Subjects

0301 basic medicine, Histology, animal diseases, Cell, Endocytic cycle, Biology, Mass Spectrometry, Article, Pathology and Forensic Medicine, 03 medical and health sciences, chemistry.chemical_compound, Ascorbate Peroxidases, medicine, Animals, Humans, RNA, Messenger, Cells, Cultured, Neurons, Synucleinopathies, Alpha-synuclein, HEK 293 cells, Parkinson Disease, Hydrogen Peroxide, Cell Biology, Rats, nervous system diseases, Transport protein, Cell biology, Retromer complex, Protein Transport, HEK293 Cells, 030104 developmental biology, medicine.anatomical_structure, Endocytic vesicle, nervous system, Biochemistry, chemistry, alpha-Synuclein

Abstract

Summary Synucleinopathies, including Parkinson's disease (PD), are associated with the misfolding and mistrafficking of alpha-synuclein (α-syn). Here, using an ascorbate peroxidase (APEX)-based labeling method combined with mass spectrometry, we defined a network of proteins in the immediate vicinity of α-syn in living neurons to shed light on α-syn function. This approach identified 225 proteins, including synaptic proteins, proteins involved in endocytic vesicle trafficking, the retromer complex, phosphatases and mRNA binding proteins. Many were in complexes with α-syn, and some were encoded by genes known to be risk factors for PD and other neurodegenerative diseases. Endocytic trafficking and mRNA translation proteins within this spatial α-syn map overlapped with genetic modifiers of α-syn toxicity, developed in an accompanying study (Khurana et al., this issue of Cell Systems ). Our data suggest that perturbation of these particular pathways is directly related to the spatial localization of α-syn within the cell. These approaches provide new avenues to systematically examine protein function and pathology in living cells.

Published

2017

91. Lenalidomide induces ubiquitination and degradation of CK1α in del(5q) MDS

Author

Hon-Wah Man, Namrata D. Udeshi, D. R. Mani, Marie McConkey, Anita Gandhi, Lars Bullinger, Emma C. Fink, Steven A. Carr, Slater N. Hurst, Brian E. Cathers, Elizabeth A. Griffiths, Tanya Svinkina, Rebekka K. Schneider, Meir Wetzler, Jan Krönke, Rajesh Chopra, Marcus Järås, Philip P Chamberlain, Kyle J. MacBeth, Benjamin L. Ebert, and Paul W. Hollenbach

Subjects

Ubiquitin-Protein Ligases, Molecular Sequence Data, Cell Line, Jurkat Cells, Mice, Ubiquitin, Species Specificity, medicine, Animals, Humans, Immunologic Factors, Amino Acid Sequence, Lenalidomide, Sequence Deletion, Multidisciplinary, biology, Casein Kinase I, Cereblon, Ubiquitination, IKZF3, 3. Good health, Ubiquitin ligase, Thalidomide, HEK293 Cells, Biochemistry, Gene Expression Regulation, Myelodysplastic Syndromes, Proteolysis, biology.protein, Cancer research, Casein kinase 1, Haploinsufficiency, K562 Cells, Sequence Alignment, medicine.drug, Peptide Hydrolases

Abstract

Lenalidomide is a highly effective treatment for myelodysplastic syndrome (MDS) with deletion of chromosome 5q (del(5q)). Here, we demonstrate that lenalidomide induces the ubiquitination of casein kinase 1A1 (CK1α) by the E3 ubiquitin ligase CUL4-RBX1-DDB1-CRBN (known as CRL4(CRBN)), resulting in CK1α degradation. CK1α is encoded by a gene within the common deleted region for del(5q) MDS and haploinsufficient expression sensitizes cells to lenalidomide therapy, providing a mechanistic basis for the therapeutic window of lenalidomide in del(5q) MDS. We found that mouse cells are resistant to lenalidomide but that changing a single amino acid in mouse Crbn to the corresponding human residue enables lenalidomide-dependent degradation of CK1α. We further demonstrate that minor side chain modifications in thalidomide and a novel analogue, CC-122, can modulate the spectrum of substrates targeted by CRL4(CRBN). These findings have implications for the clinical activity of lenalidomide and related compounds, and demonstrate the therapeutic potential of novel modulators of E3 ubiquitin ligases.

Published

2014

92. Ubiquitylome analysis identifies dysregulation of effector substrates in SPOP-mutant prostate cancer

Author

Levi A. Garraway, Mirjam Blattner, Namrata D. Udeshi, Mark A. Rubin, Anna C. Groner, Sylvan C. Baca, Marius S. Pop, Wesley J. Errington, Tanya Svinkina, Holger Moch, Gilbert G. Privé, Jean Philippe Theurillat, Peter J. Wild, and Steven A. Carr

Subjects

Male, Proteasome Endopeptidase Complex, Carcinogenesis, Chromosomal Proteins, Non-Histone, Ubiquitin-Protein Ligases, Molecular Sequence Data, SPOP, medicine.disease_cause, Article, Ubiquitin, Cell Line, Tumor, medicine, Humans, Neoplasm Invasiveness, Nuclear protein, Poly-ADP-Ribose Binding Proteins, Genetics, Oncogene Proteins, Mutation, Multidisciplinary, Binding Sites, biology, Base Sequence, Effector, Ubiquitination, Nuclear Proteins, Prostatic Neoplasms, Chromoplexy, 3. Good health, Ubiquitin ligase, Cell biology, Repressor Proteins, stomatognathic diseases, biology.protein, Carrier Proteins

Abstract

Mutant protein in tumors hits the DEK Cancer genome sequencing projects have uncovered a multitude of mutations in human tumors. Understanding whether and how these mutations contribute to tumor development and progression could ultimately lead to new therapies. Theurillat et al. studied the protein product of a gene that is recurrently mutated in prostate cancer. Normally this protein helps attach a biochemical tag to cellular proteins that marks them for degradation. The new work shows that the tumor-associated mutant protein loses this tagging ability, which results in the stabilization of a handful of cellular proteins that would otherwise be degraded. One of the most intriguing of these proteins was DEK, which helps prostate cancer cells invade into surrounding tissue. Science , this issue p. 85

Published

2014

93. Opposing therapeutic efficacy of BET inhibitors is determined by cancer type-specific SPOP mutants

Author

Hana Janouskova, Namrata D. Udeshi, Steven A. Carr, Andrea Rinaldi, G. El Tekle, Anna Ulbricht, Matthias Peter, Jean-Philippe Theurillat, Levi A. Garraway, Carlo V. Catapano, and Gianluca Civenni

Subjects

Cancer Research, Oncology, business.industry, Cancer type, Mutant, Cancer research, Medicine, SPOP, business

Published

2016

94. Lenalidomide Causes Selective Degradation of IKZF1 and IKZF3 in Multiple Myeloma Cells

Author

Anupama Narla, Emily C. Hartman, Nikhil C. Munshi, Peter V. Grauman, Slater N. Hurst, Namrata D. Udeshi, Benjamin L. Ebert, Stuart L. Schreiber, Jan Krönke, Marie McConkey, Monica Schenone, Xiaoyu Li, Eamon Comer, Dirk Heckl, Steven A. Carr, Tanya Svinkina, and Christie Ciarlo

Subjects

Ubiquitin-Protein Ligases, Antineoplastic Agents, Article, Ikaros Transcription Factor, Ubiquitin, medicine, Humans, Transcription factor, Lenalidomide, Multiple myeloma, Adaptor Proteins, Signal Transducing, Multidisciplinary, biology, Cereblon, Proteolysis targeting chimera, medicine.disease, Ubiquitin ligase, Thalidomide, Teratogens, Mechanism of action, Immunology, biology.protein, Cancer research, medicine.symptom, Multiple Myeloma, medicine.drug, Peptide Hydrolases

Abstract

Drug With a (Re)Purpose Thalidomide, once infamous for its deleterious effects on fetal development, has re-emerged as a drug of great interest because of its beneficial immunomodulatory effects. A derivative drug called lenalidomide significantly extends the survival of patients with multiple myeloma, but the molecular mechanisms underlying its efficacy remain unclear (see the Perspective by Stewart ). Building on a previous observation that thalidomide binds to cereblon, a ubiquitin ligase, Lu et al. (p. 305 , published online 28 November) and Krönke et al. (p. 301 , published online 28 November) show that in the presence of lenalidomide, cereblon selectively targets two B cell transcription factors (Ikaros family members, IKZF1 and IKZF3) for degradation. In myeloma cell lines and patient cells, down-regulation of IKZF1 and IKZF3 was necessary and sufficient for the drug's anticancer activity. Thus, lenalidomide may act, at least in part, by “grepurposing” a ubiquitin ligase.

Published

2013

95. Refined preparation and use of anti-diglycine remnant (K-ε-GG) antibody enables routine quantification of 10,000s of ubiquitination sites in single proteomics experiments

Author

Namrata D. Udeshi, Philipp Mertins, D. R. Mani, Tanya Svinkina, Eric Kuhn, Jana W. Qiao, and Steven A. Carr

Subjects

Proteomics, Proteasome Endopeptidase Complex, Proteome, Leupeptins, Peptide, Biology, Cysteine Proteinase Inhibitors, Mass spectrometry, Tandem mass spectrometry, Biochemistry, Antibodies, Analytical Chemistry, Jurkat Cells, Tandem Mass Spectrometry, Stable isotope labeling by amino acids in cell culture, Diglycine, Humans, Binding site, Amino Acids, Molecular Biology, chemistry.chemical_classification, Binding Sites, Glycylglycine, Ubiquitination, Technological Innovation and Resources, Reproducibility of Results, Ubiquitinated Proteins, Cross-Linking Reagents, chemistry, Isotope Labeling, Chromatography, Liquid

Abstract

Detection of endogenous ubiquitination sites by mass spectrometry has dramatically improved with the commercialization of anti-di-glycine remnant (K-e-GG) antibodies. Here, we describe a number of improvements to the K-e-GG enrichment workflow, including optimized antibody and peptide input requirements, antibody cross-linking, and improved off-line fractionation prior to enrichment. This refined and practical workflow enables routine identification and quantification of ∼20,000 distinct endogenous ubiquitination sites in a single SILAC experiment using moderate amounts of protein input.

Published

2012

96. Proteomic Mapping of Mitochondria in Living Cells via Spatially Restricted Enzymatic Tagging

Author

Namrata D. Udeshi, Peng Zou, Jeffrey D. Martell, Alice Y. Ting, Vamsi K. Mootha, Steven A. Carr, Hyun-Woo Rhee, Massachusetts Institute of Technology. Department of Chemistry, Martell, Jeffrey Daniel, Ting, Alice Y., Rhee, Hyun-Woo, and Zou, Peng

Subjects

Proteomics, Multidisciplinary, HEK 293 cells, Mitochondrion, Biology, Mass Spectrometry, Article, Mitochondria, Cell biology, Ascorbate Peroxidases, HEK293 Cells, Biochemistry, Mitochondrial matrix, Biotinylation, COS Cells, Chlorocebus aethiops, Gene Targeting, Animals, Humans, Inner membrane, Genetic Engineering, Bacterial outer membrane, Intermembrane space

Abstract

Microscopy and mass spectrometry (MS) are complementary techniques: The former provides spatiotemporal information in living cells, but only for a handful of recombinant proteins at a time, whereas the latter can detect thousands of endogenous proteins simultaneously, but only in lysed samples. Here, we introduce technology that combines these strengths by offering spatially and temporally resolved proteomic maps of endogenous proteins within living cells. Our method relies on a genetically targetable peroxidase enzyme that biotinylates nearby proteins, which are subsequently purified and identified by MS. We used this approach to identify 495 proteins within the human mitochondrial matrix, including 31 not previously linked to mitochondria. The labeling was exceptionally specific and distinguished between inner membrane proteins facing the matrix versus the intermembrane space (IMS). Several proteins previously thought to reside in the IMS or outer membrane, including protoporphyrinogen oxidase, were reassigned to the matrix by our proteomic data and confirmed by electron microscopy. The specificity of peroxidase-mediated proteomic mapping in live cells, combined with its ease of use, offers biologists a powerful tool for understanding the molecular composition of living cells., National Institutes of Health (U.S.) (Grant DP1 OD003961), Camille & Henry Dreyfus Foundation, American Chemical Society

Published

2012

97. iTRAQ labeling is superior to mTRAQ for quantitative global proteomics and phosphoproteomics

Author

D. R. Mani, Philipp Mertins, Namrata D. Udeshi, Shao En Ong, Jacob D. Jaffe, Karl R. Clauser, Jinal Patel, and Steven A. Carr

Subjects

chemistry.chemical_classification, Proteomics, Chromatography, Epidermal Growth Factor, Proteome, Chemistry, Phosphoproteomics, Technological Innovation and Resources, Peptide, Tandem mass spectrometry, Mass spectrometry, Phosphoproteins, Biochemistry, Peptide Fragments, Analytical Chemistry, Isobaric labeling, Tandem Mass Spectrometry, Isotope Labeling, Humans, Regression Analysis, Egfr signaling, Molecular Biology, HeLa Cells

Abstract

Labeling of primary amines on peptides with reagents containing stable isotopes is a commonly used technique in quantitative mass spectrometry. Isobaric labeling techniques such as iTRAQ™ or TMT™ allow for relative quantification of peptides based on ratios of reporter ions in the low m/z region of spectra produced by precursor ion fragmentation. In contrast, nonisobaric labeling with mTRAQ™ yields precursors with different masses that can be directly quantified in MS1 spectra. In this study, we compare iTRAQ- and mTRAQ-based quantification of peptides and phosphopeptides derived from EGF-stimulated HeLa cells. Both labels have identical chemical structures, therefore precursor ion- and fragment ion-based quantification can be directly compared. Our results indicate that iTRAQ labeling has an additive effect on precursor intensities, whereas mTRAQ labeling leads to more redundant MS2 scanning events caused by triggering on the same peptide with different mTRAQ labels. We found that iTRAQ labeling quantified nearly threefold more phosphopeptides (12,129 versus 4,448) and nearly twofold more proteins (2,699 versus 1,597) than mTRAQ labeling. Although most key proteins in the EGFR signaling network were quantified with both techniques, iTRAQ labeling allowed quantification of twice as many kinases. Accuracy of reporter ion quantification by iTRAQ is adversely affected by peptides that are cofragmented in the same precursor isolation window, dampening observed ratios toward unity. However, because of tighter overall iTRAQ ratio distributions, the percentage of statistically significantly regulated phosphopeptides and proteins detected by iTRAQ and mTRAQ was similar. We observed a linear correlation of logarithmic iTRAQ to mTRAQ ratios over two orders of magnitude, indicating a possibility to correct iTRAQ ratios by an average compression factor. Spike-in experiments using peptides of defined ratios in a background of nonregulated peptides show that iTRAQ quantification is less accurate but not as variable as mTRAQ quantification.

Published

2012

98. O-GlcNAcylation of the Plum pox virus capsid protein catalyzed by SECRET AGENT: characterization of O-GlcNAc sites by electron transfer dissociation mass spectrometry

Author

Young Cheon Kim, Jeffrey Shabanowitz, Neil E. Olszewski, Namrata D. Udeshi, Jeremy L. Balsbaugh, and Donald F. Hunt

Subjects

Glycosylation, Clinical Biochemistry, Mutant, Molecular Sequence Data, Mutagenesis (molecular biology technique), medicine.disease_cause, Proteomics, N-Acetylglucosaminyltransferases, Biochemistry, Peptide Mapping, Mass Spectrometry, Article, Acetylglucosamine, medicine, Transferase, Deletion mapping, Amino Acid Sequence, Mutation, Chemistry, Arabidopsis Proteins, Organic Chemistry, Molecular biology, Electron-transfer dissociation, Capsid, Plum Pox Virus, Biocatalysis, Capsid Proteins

Abstract

The capsid protein of Plum pox virus (PPV-CP) is modified with O-linked β-N-acetylglucosamine (O-GlcNAc). In Arabidopsis thaliana this modification is made by an O-GlcNAc transferase named SECRET AGENT (SEC). Modification of PPV-CP by SEC is hypothesized to have a direct role in the infection process, because virus titer and rate of spread are reduced in SEC mutants. Previous studies used deletion mapping and site-directed mutagenesis to identify four O-GlcNAc sites on the capsid protein that are modified by Escherichia coli-expressed SEC. The infection process was not affected when two of these sites were mutated suggesting that O-GlcNAcylation of these sites does not have a significant role in the infection process or that a subset of the modifications is sufficient. Since it is possible that the mutational mapping approach missed or incorrectly identified O-GlcNAc sites, the modifications produced by E. coli-expressed SEC were characterized using mass spectrometry. O-GlcNAcylated peptides were enzymatically tagged with galactose, the products were enriched on immobilized Ricinus communis agglutinin I and sequenced by electron transfer dissociation (ETD) mass spectrometry. Five O-GlcNAc sites on PPV-CP were identified. Two of these sites were not identified in by the previous mutational mapping. In addition, one site previously predicted by mutation mapping was not detected, but modification of this site was not supported when the mutation mapping was repeated. This study suggests that mapping modification sites by ETD mass spectrometry is more comprehensive and accurate than mutational mapping.

Published

2010

99. Extensive crosstalk between O-GlcNAcylation and phosphorylation regulates cytokinesis

Author

Jeffrey Shabanowitz, Chad Slawson, Zihao Wang, Gerald W. Hart, Kaoru Sakabe, Win D. Cheung, Namrata D. Udeshi, Philip D. Compton, and Donald F. Hunt

Subjects

Proteomics, Glycosylation, Blotting, Western, Molecular Sequence Data, Cell Cycle Proteins, Spindle Apparatus, Biology, N-Acetylglucosaminyltransferases, Biochemistry, environment and public health, Models, Biological, Article, Phosphorylation cascade, Acetylglucosamine, Nuclear Matrix-Associated Proteins, CDC2 Protein Kinase, Humans, Amino Acid Sequence, Phosphorylation, Molecular Biology, Cytokinesis, Centrosome, Cyclin-dependent kinase 1, Binding Sites, Reverse Transcriptase Polymerase Chain Reaction, Nuclear Proteins, Antigens, Nuclear, Cell Biology, Cell cycle, Neoplasm Proteins, Nuclear Pore Complex Proteins, Repressor Proteins, Midbody, enzymes and coenzymes (carbohydrates), Signal transduction, HeLa Cells, Protein Binding, Signal Transduction

Abstract

Like phosphorylation, the addition of O-linked beta-N-acetylglucosamine (O-GlcNAcylation) is a ubiquitous, reversible process that modifies serine and threonine residues on nuclear and cytoplasmic proteins. Overexpression of the enzyme that adds O-GlcNAc to target proteins, O-GlcNAc transferase (OGT), perturbs cytokinesis and promotes polyploidy, but the molecular targets of OGT that are important for its cell cycle functions are unknown. Here, we identify 141 previously unknown O-GlcNAc sites on proteins that function in spindle assembly and cytokinesis. Many of these O-GlcNAcylation sites are either identical to known phosphorylation sites or in close proximity to them. Furthermore, we found that O-GlcNAcylation altered the phosphorylation of key proteins associated with the mitotic spindle and midbody. Forced overexpression of OGT increased the inhibitory phosphorylation of cyclin-dependent kinase 1 (CDK1) and reduced the phosphorylation of CDK1 target proteins. The increased phosphorylation of CDK1 is explained by increased activation of its upstream kinase, MYT1, and by a concomitant reduction in the transcript for the CDK1 phosphatase, CDC25C. OGT overexpression also caused a reduction in both messenger RNA expression and protein abundance of Polo-like kinase 1, which is upstream of both MYT1 and CDC25C. The data not only illustrate the crosstalk between O-GlcNAcylation and phosphorylation of proteins that are regulators of crucial signaling pathways but also uncover a mechanism for the role of O-GlcNAcylation in regulation of cell division.

Published

2010

100. Enrichment and Site Mapping of O-Linked N-Acetylglucosamine by a Combination of Chemical/Enzymatic Tagging, Photochemical Cleavage, and Electron Transfer Dissociation Mass Spectrometry*

Author

Gerald W. Hart, Jeffrey Shabanowitz, Meaghan O'Malley, Namrata D. Udeshi, Donald F. Hunt, and Zihao Wang

Subjects

Proteomics, Methyl-CpG-Binding Protein 2, Photochemistry, Synucleins, tau Proteins, Mass spectrometry, Cleavage (embryo), Biochemistry, Chromatography, Affinity, Mass Spectrometry, Analytical Chemistry, Acetylglucosamine, Affinity chromatography, Animals, Protein phosphorylation, Biotinylation, Amino Acid Sequence, alpha-Crystallins, Molecular Biology, Peptide sequence, Glycoproteins, Binding Sites, Molecular Structure, Chemistry, Research, Brain, Proteins, Rats, Electron-transfer dissociation, Peptides

Abstract

Numerous cellular processes are regulated by the reversible addition of either phosphate or O-linked beta-N-acetylglucosamine (O-GlcNAc) to nuclear and cytoplasmic proteins. Although sensitive methods exist for the enrichment and identification of protein phosphorylation sites, those for the enrichment of O-GlcNAc-containing peptides are lacking. Reported here is highly efficient methodology for the enrichment and characterization of O-GlcNAc sites from complex samples. In this method, O-GlcNAc-modified peptides are tagged with a novel biotinylation reagent, enriched by affinity chromatography, released from the solid support by photochemical cleavage, and analyzed by electron transfer dissociation mass spectrometry. Using this strategy, eight O-GlcNAc sites were mapped from a tau-enriched sample from rat brain. Sites of GlcNAcylation were characterized on important neuronal proteins such as tau, synucleins, and methyl CpG-binding protein 2.

Published

2009