Search

Your search keyword '"Kramer, Nicholas J."' showing total 36 results
Start Over Author "Kramer, Nicholas J."
36 results on '"Kramer, Nicholas J."'

3. A versatile system to record cell-cell interactions

Author

Tang, Rui, Murray, Christopher W, Linde, Ian L, Kramer, Nicholas J, Lyu, Zhonglin, Tsai, Min K, Chen, Leo C, Cai, Hongchen, Gitler, Aaron D, Engleman, Edgar, Lee, Wonjae, and Winslow, Monte M

Subjects
Biochemistry and Cell Biology, Biological Sciences, Cancer, 1.1 Normal biological development and functioning, 2.1 Biological and endogenous factors, Generic health relevance, Animals, Cell Communication, Cell Line, Coculture Techniques, Green Fluorescent Proteins, Humans, Lentivirus, Mice, Microscopy, Protein Transport, cancer biology, cancer-stromal, cell biology, cell-cell interaction, human, mouse, nanobody, tumor microenvironment, Biological sciences, Biomedical and clinical sciences, Health sciences
Abstract

Cell-cell interactions influence all aspects of development, homeostasis, and disease. In cancer, interactions between cancer cells and stromal cells play a major role in nearly every step of carcinogenesis. Thus, the ability to record cell-cell interactions would facilitate mechanistic delineation of the role of the cancer microenvironment. Here, we describe GFP-based Touching Nexus (G-baToN) which relies upon nanobody-directed fluorescent protein transfer to enable sensitive and specific labeling of cells after cell-cell interactions. G-baToN is a generalizable system that enables physical contact-based labeling between various human and mouse cell types, including endothelial cell-pericyte, neuron-astrocyte, and diverse cancer-stromal cell pairs. A suite of orthogonal baToN tools enables reciprocal cell-cell labeling, interaction-dependent cargo transfer, and the identification of higher order cell-cell interactions across a wide range of cell types. The ability to track physically interacting cells with these simple and sensitive systems will greatly accelerate our understanding of the outputs of cell-cell interactions in cancer as well as across many biological processes.

Published
2020

4. Interception of the Bycroft–Gowland Intermediate in the Enzymatic Macrocyclization of Thiopeptides

Author

Bogart, Jonathan W, Kramer, Nicholas J, Turlik, Aneta, Bleich, Rachel M, Catlin, Daniel S, Schroeder, Frank C, Nair, Satish K, Williamson, R Thomas, Houk, KN, and Bowers, Albert A

Subjects
Organic Chemistry, Chemical Sciences, Biocatalysis, Cycloaddition Reaction, Lyases, Protein Conformation, Thiostrepton, General Chemistry, Chemical sciences, Engineering
Abstract

Thiopeptides are a broad class of macrocyclic, heavily modified peptide natural products that are unified by the presence of a substituted, nitrogen-containing heterocycle core. Early work indicated that this core might be fashioned from two dehydroalanines by an enzyme-catalyzed aza-[4 + 2] cycloaddition to give a cyclic-hemiaminal intermediate. This common intermediate could then follow a reductive path toward a dehydropiperidine, as in the thiopeptide thiostrepton, or an aromatization path to yield the pyridine groups observed in many other thiopeptides. Although several of the enzymes proposed to perform this cycloaddition have been reconstituted, only pyridine products have been isolated and any hemiaminal intermediates have yet to be observed. Here, we identify the conditions and substrates that decouple the cycloaddition from subsequent steps and allow interception and characterization of this long hypothesized intermediate. Transition state modeling indicates that the key amide-iminol tautomerization is the major hurdle in an otherwise energetically favorable cycloaddition. An anionic model suggests that deprotonation and polarization of this amide bond by TbtD removes this barrier and provides a sufficient driving force for facile (stepwise) cycloaddition. This work provides evidence for a mechanistic link between disparate cyclases in thiopeptide biosynthesis.

Published
2020

5. CRISPR–Cas9 screens in human cells and primary neurons identify modifiers of C9ORF72 dipeptide-repeat-protein toxicity

Author

Kramer, Nicholas J, Haney, Michael S, Morgens, David W, Jovičić, Ana, Couthouis, Julien, Li, Amy, Ousey, James, Ma, Rosanna, Bieri, Gregor, Tsui, C Kimberly, Shi, Yingxiao, Hertz, Nicholas T, Tessier-Lavigne, Marc, Ichida, Justin K, Bassik, Michael C, and Gitler, Aaron D

Subjects
Biochemistry and Cell Biology, Biological Sciences, Brain Disorders, Rare Diseases, Human Genome, Genetics, Frontotemporal Dementia (FTD), Biotechnology, ALS, Dementia, Acquired Cognitive Impairment, Stem Cell Research, Neurodegenerative, Neurosciences, 2.1 Biological and endogenous factors, Aetiology, Neurological, Active Transport, Cell Nucleus, Amyotrophic Lateral Sclerosis, Animals, C9orf72 Protein, CRISPR-Cas Systems, DNA Repeat Expansion, Endoplasmic Reticulum Stress, Frontotemporal Dementia, Gene Knockout Techniques, HeLa Cells, Humans, K562 Cells, Membrane Proteins, Mice, Microsatellite Repeats, Motor Neurons, Thioredoxins, rab GTP-Binding Proteins, rab7 GTP-Binding Proteins, Hela Cells, Medical and Health Sciences, Developmental Biology, Agricultural biotechnology, Bioinformatics and computational biology
Abstract

Hexanucleotide-repeat expansions in the C9ORF72 gene are the most common cause of amyotrophic lateral sclerosis and frontotemporal dementia (c9ALS/FTD). The nucleotide-repeat expansions are translated into dipeptide-repeat (DPR) proteins, which are aggregation prone and may contribute to neurodegeneration. We used the CRISPR-Cas9 system to perform genome-wide gene-knockout screens for suppressors and enhancers of C9ORF72 DPR toxicity in human cells. We validated hits by performing secondary CRISPR-Cas9 screens in primary mouse neurons. We uncovered potent modifiers of DPR toxicity whose gene products function in nucleocytoplasmic transport, the endoplasmic reticulum (ER), proteasome, RNA-processing pathways, and chromatin modification. One modifier, TMX2, modulated the ER-stress signature elicited by C9ORF72 DPRs in neurons and improved survival of human induced motor neurons from patients with C9ORF72 ALS. Together, our results demonstrate the promise of CRISPR-Cas9 screens in defining mechanisms of neurodegenerative diseases.

Published
2018

7. RPS25 is required for efficient RAN translation of C9orf72 and other neurodegenerative disease-associated nucleotide repeats

Author

Yamada, Shizuka B., Gendron, Tania F., Niccoli, Teresa, Genuth, Naomi R., Grosely, Rosslyn, Shi, Yingxiao, Glaria, Idoia, Kramer, Nicholas J., Nakayama, Lisa, Fang, Shirleen, Dinger, Tai J. I., Thoeng, Annora, Rocha, Gabriel, Barna, Maria, Puglisi, Joseph D., Partridge, Linda, Ichida, Justin K., Isaacs, Adrian M., Petrucelli, Leonard, and Gitler, Aaron D.

Published
2019
Full Text
View/download PDF

11. Parkinson’s Disease Genes VPS35 and EIF4G1 Interact Genetically and Converge on α-Synuclein

Author

Dhungel, Nripesh, primary, Eleuteri, Simona, additional, Li, Ling-bo, additional, Kramer, Nicholas J., additional, Chartron, Justin W., additional, Spencer, Brian, additional, Kosberg, Kori, additional, Fields, Jerel Adam, additional, Stafa, Klodjan, additional, Adame, Anthony, additional, Lashuel, Hilal, additional, Frydman, Judith, additional, Shen, Kang, additional, Masliah, Eliezer, additional, and Gitler, Aaron D., additional

Published
2023
Full Text
View/download PDF

12. Spt4 selectively regulates the expression of C9orf72 sense and antisense mutant transcripts

Author

Kramer, Nicholas J., Carlomagno, Yari, Zhang, Yong-Jie, Almeida, Sandra, Cook, Casey N., Gendron, Tania F., Prudencio, Mercedes, Van Blitterswijk, Marka, Belzil, Veronique, Couthouis, Julien, Paul, Joseph West, Goodman, Lindsey D., Daughrity, Lillian, Chew, Jeannie, Garrett, Aliesha, Pregent, Luc, Jansen-West, Karen, Tabassian, Lilia J., Rademakers, Rosa, Boylan, Kevin, Graff-Radford, Neill R., Josephs, Keith A., Parisi, Joseph E., Knopman, David S., Petersen, Ronald C., Boeve, Bradley F., Deng, Ning, Feng, Yanan, Cheng, Tzu-Hao, Dickson, Dennis W., Cohen, Stanley N., Bonini, Nancy M., Link, Christopher D., Gao, Fen-Biao, Petrucelli, Leonard, and Gitler, Aaron D.

Published
2016

15. G-baToN: a versatile cell-cell interaction reporter system

Author

Tang, Rui, Murray, Christopher W., Linde, Ian, Kramer, Nicholas J., Tsai, Min K., Chen, Leo, Cai, Hongchen, Gitler, Aaron D., Engleman, Edgar, and Winslow, Monte M.

Abstract

Cell-cell interactions influence all aspects of development, homeostasis, and disease. Here, we describe GFP-based Touching Nexus (G-baToN) which relies upon fluorescent protein transfer driven by nanobody-mediated recognition to enable sensitive and specific labeling of cells after cell-cell interactions. A suite of orthogonal baToN tools enables reciprocal cell-cell labeling, interaction-dependent cargo transfer, and the identification of higher order cell-cell interactions across a wide range of cell types.

Published
2020
Full Text
View/download PDF

16. The exploration of aza-quinolines as hematopoietic prostaglandin D synthase (H-PGDS) inhibitors with low brain exposure

Author

Cadilla, Rodolfo, primary, Deaton, David N., additional, Do, Young, additional, Elkins, Patricia A., additional, Ennulat, Daniela, additional, Guss, Jeffrey H., additional, Holt, Jason, additional, Jeune, Michael R., additional, King, Andrew G., additional, Klapwijk, Jan C., additional, Kramer, H. Fritz, additional, Kramer, Nicholas J., additional, Laffan, Susan B., additional, Masuria, Paresh I., additional, McDougal, Alan V., additional, Mortenson, Paul N., additional, Musetti, Caterina, additional, Peckham, Gregory E., additional, Pietrak, Beth L., additional, Poole, Chuck, additional, Price, Daniel J., additional, Rendina, Alan R., additional, Sati, Girish, additional, Saxty, Gordon, additional, Shearer, Barry G., additional, Shewchuk, Lisa M., additional, Sneddon, Helen F., additional, Stewart, Eugene L., additional, Stuart, J. Darren, additional, Thomas, Dean N., additional, Thomson, Stephen A., additional, Ward, Paris, additional, Wilson, Joseph W., additional, Xu, Tiahshun, additional, and Youngman, Mark A., additional

Published
2020
Full Text
View/download PDF

17. A versatile system to record cell-cell interactions

Author

Tang, Rui, primary, Murray, Christopher W, additional, Linde, Ian L, additional, Kramer, Nicholas J, additional, Lyu, Zhonglin, additional, Tsai, Min K, additional, Chen, Leo C, additional, Cai, Hongchen, additional, Gitler, Aaron D, additional, Engleman, Edgar, additional, Lee, Wonjae, additional, and Winslow, Monte M, additional

Published
2020
Full Text
View/download PDF

18. Author response: A versatile system to record cell-cell interactions

Author

Tang, Rui, primary, Murray, Christopher W, additional, Linde, Ian L, additional, Kramer, Nicholas J, additional, Lyu, Zhonglin, additional, Tsai, Min K, additional, Chen, Leo C, additional, Cai, Hongchen, additional, Gitler, Aaron D, additional, Engleman, Edgar, additional, Lee, Wonjae, additional, and Winslow, Monte M, additional

Published
2020
Full Text
View/download PDF

24. LRRK2 modifies α-syn pathology and spread in mouse models and human neurons.

Author

Brahic, Michel, Couthouis, Julien, Ma, Rosanna, Nakayama, Lisa, Bieri, Gregor, Kramer, Nicholas J., Gitler, Aaron D., Bousset, Luc, Melki, Ronald, Monbureau, Marie, Defensor, Erwin, Shamloo, Mehrdad, and Schüle, Birgitt

Subjects
PARKINSON'S disease, ALPHA-synuclein, GENDER mainstreaming
Abstract

Progressive aggregation of the protein alpha-synuclein (α-syn) and loss of dopaminergic neurons in the substantia nigra pars compacta (SNpc) are key histopathological hallmarks of Parkinson's disease (PD). Accruing evidence suggests that α-syn pathology can propagate through neuronal circuits in the brain, contributing to the progressive nature of the disease. Thus, it is therapeutically pertinent to identify modifiers of α-syn transmission and aggregation as potential targets to slow down disease progression. A growing number of genetic mutations and risk factors has been identified in studies of familial and sporadic forms of PD. However, how these genes affect α-syn aggregation and pathological transmission, and whether they can be targeted for therapeutic interventions, remains unclear. We performed a targeted genetic screen of risk genes associated with PD and parkinsonism for modifiers of α-syn aggregation, using an α-syn preformed-fibril (PFF) induction assay. We found that decreased expression of Lrrk2 and Gba modulated α-syn aggregation in mouse primary neurons. Conversely, α-syn aggregation increased in primary neurons from mice expressing the PD-linked LRRK2 G2019S mutation. In vivo, using LRRK2 G2019S transgenic mice, we observed acceleration of α-syn aggregation and degeneration of dopaminergic neurons in the SNpc, exacerbated degeneration-associated neuroinflammation and behavioral deficits. To validate our findings in a human context, we established a novel human α-syn transmission model using induced pluripotent stem cell (iPS)-derived neurons (iNs), where human α-syn PFFs triggered aggregation of endogenous α-syn in a time-dependent manner. In PD subject-derived iNs, the G2019S mutation enhanced α-syn aggregation, whereas loss of LRRK2 decreased aggregation. Collectively, these findings establish a strong interaction between the PD risk gene LRRK2 and α-syn transmission across mouse and human models. Since clinical trials of LRRK2 inhibitors in PD are currently underway, our findings raise the possibility that these may be effective in PD broadly, beyond cases caused by LRRK2 mutations. [ABSTRACT FROM AUTHOR]

Published
2019
Full Text
View/download PDF

29. Modifiers of C9orf72 dipeptide repeat toxicity connect nucleocytoplasmic transport defects to FTD/ALS

Author

Jovičić, Ana, primary, Mertens, Jerome, additional, Boeynaems, Steven, additional, Bogaert, Elke, additional, Chai, Noori, additional, Yamada, Shizuka B, additional, Paul, Joseph W, additional, Sun, Shuying, additional, Herdy, Joseph R, additional, Bieri, Gregor, additional, Kramer, Nicholas J, additional, Gage, Fred H, additional, Van Den Bosch, Ludo, additional, Robberecht, Wim, additional, and Gitler, Aaron D, additional

Published
2015
Full Text
View/download PDF

30. Parkinson’s Disease Genes VPS35 and EIF4G1 Interact Genetically and Converge on α-Synuclein

Author

Dhungel, Nripesh, primary, Eleuteri, Simona, additional, Li, Ling-bo, additional, Kramer, Nicholas J., additional, Chartron, Justin W., additional, Spencer, Brian, additional, Kosberg, Kori, additional, Fields, Jerel Adam, additional, Stafa, Klodjan, additional, Adame, Anthony, additional, Lashuel, Hilal, additional, Frydman, Judith, additional, Shen, Kang, additional, Masliah, Eliezer, additional, and Gitler, Aaron D., additional

Published
2015
Full Text
View/download PDF

31. CRISPR–Cas9 screens in human cells and primary neurons identify modifiers of C9ORF72dipeptide-repeat-protein toxicity

Author

Kramer, Nicholas J., Haney, Michael S., Morgens, David W., Jovičić, Ana, Couthouis, Julien, Li, Amy, Ousey, James, Ma, Rosanna, Bieri, Gregor, Tsui, C. Kimberly, Shi, Yingxiao, Hertz, Nicholas T., Tessier-Lavigne, Marc, Ichida, Justin K., Bassik, Michael C., and Gitler, Aaron D.

Abstract

Hexanucleotide-repeat expansions in the C9ORF72gene are the most common cause of amyotrophic lateral sclerosis and frontotemporal dementia (c9ALS/FTD). The nucleotide-repeat expansions are translated into dipeptide-repeat (DPR) proteins, which are aggregation prone and may contribute to neurodegeneration. We used the CRISPR–Cas9 system to perform genome-wide gene-knockout screens for suppressors and enhancers of C9ORF72DPR toxicity in human cells. We validated hits by performing secondary CRISPR–Cas9 screens in primary mouse neurons. We uncovered potent modifiers of DPR toxicity whose gene products function in nucleocytoplasmic transport, the endoplasmic reticulum (ER), proteasome, RNA-processing pathways, and chromatin modification. One modifier, TMX2, modulated the ER-stress signature elicited by C9ORF72DPRs in neurons and improved survival of human induced motor neurons from patients with C9ORF72ALS. Together, our results demonstrate the promise of CRISPR–Cas9 screens in defining mechanisms of neurodegenerative diseases.

Published
2018
Full Text
View/download PDF

33. Altered lymphopoiesis and immunodeficiency in miR-142null mice

Author

Kramer, Nicholas J., Wang, Wei-Le, Reyes, Estefany Y., Kumar, Bijender, Chen, Ching-Cheng, Ramakrishna, Chandran, Cantin, Edouard M., Vonderfecht, Steven L., Taganov, Konstantin D., Chau, Nelson, and Boldin, Mark P.

Abstract

MicroRNAs (miRNAs) are a class of powerful posttranscriptional regulators implicated in the control of diverse biological processes, including regulation of hematopoiesis and the immune response. To define the biological functions of miR-142, which is preferentially and abundantly expressed in immune cells, we created a mouse line with a targeted deletion of this gene. Our analysis of miR-142−/−mice revealed a critical role for this miRNA in the development and homeostasis of lymphocytes. Marginal zone B cells expand in the knockout spleen, whereas the number of T and B1 B cells in the periphery is reduced. Abnormal development of hematopoietic lineages in miR-142−/−animals is accompanied by a profound immunodeficiency, manifested by hypoimmunoglobulinemia and failure to mount a productive immune response to soluble antigens and virus. miR-142−/−B cells express elevated levels of B-cell–activating factor (BAFF) receptor (BAFF-R) and as a result proliferate more robustly in response to BAFF stimulation. Lowering the BAFF-Rgene dose in miR-142−/−mice rescues the B-cell expansion defect, suggesting that BAFF-Ris a bona fide miR-142target through which it controls B-cell homeostasis. Collectively, our results uncover miR-142as an essential regulator of lymphopoiesis, and suggest that lesions in this miRNA gene may lead to primary immunodeficiency.

Published
2015
Full Text
View/download PDF

34. Tissue-Nonspecific Alkaline Phosphatase Acts Redundantly with PAP and NT5E to Generate Adenosine in the Dorsal Spinal Cord.

Author

Street, Sarah E., Kramer, Nicholas J., Walsh, Paul L., Taylor-Blake, Bonnie, Yadav, Manisha C., King, Ian F., Vihko, Pirkko, Wightman, R. Mark, Millán, José Luis, and Zylka, Mark J.

Subjects
*ALKALINE phosphatase, *ADENOSINE synthesis, *THORACIC vertebrae, *SPINAL cord, *PAP test, *NUCLEOTIDASES, *ANATOMY
Abstract

Prostatic acid phosphatase (PAP) and ecto-5'-nucleotidase (NT5E) hydrolyze extracellular AMP to adenosine in dorsal root ganglia (DRG) neurons and in the dorsal spinal cord. Previously, we found that adenosine production was reduced, but not eliminated, in Pap-/- INt5e-/- double knock-out (dKO) mice, suggesting that a third AMP ectonucleotidase was present in these tissues. Here, we found that tissue-nonspecific alkaline phosphatase (TNAP, encoded by the Alpl gene) is expressed and functional in DRG neurons and spinal neurons. Using a cell-based assay, we found that TNAP rapidly hydrolyzed extracellular AMP and activated adenosine receptors. This activity was eliminated by MLS-0038949, a selective pharmacological inhibitor of TNAP. In addition, MLS-0038949 eliminated AMP hydrolysis in DRG and spinal lamina II of dKO mice. Using fast-scan-cyclic voltammetry, we found that adenosine was rapidly produced from AMP in spinal cord slices from dKO mice, but virtually no adenosine was produced in spinal cord slices from dKO mice treated with MLS-0038949. Last, we found that AMP inhibited excitatory neurotransmission via adenosine A! receptor activation in spinal cord slices from wild-type, Pap-/- Nt5e-/- and dKO mice, but failed to inhibit neurotransmission in slices from dKO mice treated with MLS-0038949. These data suggest that triple elimination of TNAP, PAP, and NT5E is required to block AMP hydrolysis to adenosine in DRG neurons and dorsal spinal cord. Moreover, our data reveal that TNAP, PAP, and NT5E are the main AMP ectonucleotidases in primary somatosensory neurons and regulate physiology by metabolizing extracellular purine nucleotides. [ABSTRACT FROM AUTHOR]

Published
2013
Full Text
View/download PDF

35. Parkinson's Disease Genes VPS35 and EIF4G1 Interact Genetically and Converge on α-Synuclein

Author

Dhungel, Nripesh, Eleuteri, Simona, Li, Ling-Bo, Kramer, Nicholas J, Chartron, Justin W, Spencer, Brian, Kosberg, Kori, Fields, Jerel Adam, Stafa, Klodjan, Adame, Anthony, Lashuel, Hilal, Frydman, Judith, Shen, Kang, Masliah, Eliezer, and Gitler, Aaron D

Abstract

Parkinson's disease (PD) is a common neurodegenerative disorder. Functional interactions between some PD genes, like PINK1 and parkin, have been identified, but whether other ones interact remains elusive. Here we report an unexpected genetic interaction between two PD genes, VPS35 and EIF4G1. We provide evidence that EIF4G1 upregulation causes defects associated with protein misfolding. Expression of a sortilin protein rescues these defects, downstream of VPS35, suggesting a potential role for sortilins in PD. We also show interactions between VPS35, EIF4G1, and α-synuclein, a protein with a key role in PD. We extend our findings from yeast to an animal model and show that these interactions are conserved in neurons and in transgenic mice. Our studies reveal unexpected genetic and functional interactions between two seemingly unrelated PD genes and functionally connect them to α-synuclein pathobiology in yeast, worms, and mouse. Finally, we provide a resource of candidate PD genes for future interrogation.

36. Genome-wide screens for mitonuclear co-regulators uncover links between compartmentalized metabolism and mitochondrial gene expression.

Author

Kramer NJ, Prakash G, Choquet K, Soto I, Petrova B, Merens HE, Kanarek N, and Churchman LS

Abstract

Mitochondrial oxidative phosphorylation (OXPHOS) complexes are assembled from proteins encoded by both nuclear and mitochondrial DNA. These dual-origin enzymes pose a complex gene regulatory challenge for cells, in which gene expression must be coordinated across organelles using distinct pools of ribosomes. How cells produce and maintain the accurate subunit stoichiometries for these OXPHOS complexes remains largely unknown. To identify genes involved in dual-origin protein complex synthesis, we performed FACS-based genome-wide screens analyzing mutant cells with unbalanced levels of mitochondrial- and nuclear-encoded subunits of cytochrome c oxidase (Complex IV). We identified novel genes involved in OXPHOS biogenesis, including two uncharacterized genes: PREPL and NME6 . We found that PREPL specifically regulates Complex IV biogenesis by interacting with mitochondrial protein synthesis machinery, while NME6, an uncharacterized nucleoside diphosphate kinase (NDPK), controls OXPHOS complex biogenesis through multiple mechanisms reliant on its NDPK domain. First, NME6 maintains local mitochondrial pyrimidine triphosphate levels essential for mitochondrial RNA abundance. Second, through stabilizing interactions with RCC1L, NME6 modulates the activity of mitoribosome regulatory complexes, leading to disruptions in mitoribosome assembly and mitochondrial RNA pseudouridylation. Taken together, we propose that NME6 acts as a link between compartmentalized mitochondrial metabolites and mitochondrial gene expression. Finally, we present these screens as a resource, providing a catalog of genes involved in mitonuclear gene regulation and OXPHOS biogenesis.

Published
2023
Full Text
View/download PDF

Catalog

Books, media, physical & digital resources
See catalog results