Your search keyword '"Patrick Reichenbach"' showing total 37 results

1. Structure-based optimization of type III indoleamine 2,3-dioxygenase 1 (IDO1) inhibitors

Author

Ute F. Röhrig, Somi Reddy Majjigapu, Pierre Vogel, Aline Reynaud, Florence Pojer, Nahzli Dilek, Patrick Reichenbach, Kelly Ascenção, Melita Irving, George Coukos, Olivier Michielin, and Vincent Zoete

Subjects

Cancer immunotherapy, structure-based drug design, tryptophan metabolism, X-ray crystallography, Therapeutics. Pharmacology, RM1-950

Abstract

The haem enzyme indoleamine 2,3-dioxygenase 1 (IDO1) catalyses the rate-limiting step in the kynurenine pathway of tryptophan metabolism and plays an essential role in immunity, neuronal function, and ageing. Expression of IDO1 in cancer cells results in the suppression of an immune response, and therefore IDO1 inhibitors have been developed for use in anti-cancer immunotherapy. Here, we report an extension of our previously described highly efficient haem-binding 1,2,3-triazole and 1,2,4-triazole inhibitor series, the best compound having both enzymatic and cellular IC50 values of 34 nM. We provide enzymatic inhibition data for almost 100 new compounds and X-ray diffraction data for one compound in complex with IDO1. Structural and computational studies explain the dramatic drop in activity upon extension to pocket B, which has been observed in diverse haem-binding inhibitor scaffolds. Our data provides important insights for future IDO1 inhibitor design.

Published

2022

2. A cell-based phenotypic library selection and screening approach for the de novo discovery of novel functional chimeric antigen receptors

Author

Julie K. Fierle, Johan Abram-Saliba, Vasileios Atsaves, Matteo Brioschi, Mariastella de Tiani, Patrick Reichenbach, Melita Irving, George Coukos, and Steven M. Dunn

Subjects

Medicine, Science

Abstract

Abstract Anti-tumor therapies that seek to exploit and redirect the cytotoxic killing and effector potential of autologous or syngeneic T cells have shown extraordinary promise and efficacy in certain clinical settings. Such cells, when engineered to express synthetic chimeric antigen receptors (CARs) acquire novel targeting and activation properties which are governed and orchestrated by, typically, antibody fragments specific for a tumor antigen of interest. However, it is becoming increasingly apparent that not all antibodies are equal in this regard, with a growing appreciation that ‘optimal’ CAR performance requires a consideration of multiple structural and contextual parameters. Thus, antibodies raised by classical approaches and intended for other applications often perform poorly or not at all when repurposed as CARs. With this in mind, we have explored the potential of an in vitro phenotypic CAR library discovery approach that tightly associates antibody-driven bridging of tumor and effector T cells with an informative and functionally relevant CAR activation reporter signal. Critically, we demonstrate the utility of this enrichment methodology for ‘real world’ de novo discovery by isolating several novel anti-mesothelin CAR-active scFv candidates.

Published

2022

3. VEGFR-2 redirected CAR-T cells are functionally impaired by soluble VEGF-A competition for receptor binding

Author

George Coukos, Evripidis Lanitis, Melita Irving, Paris Kosti, Catherine Ronet, Elisabetta Cribioli, Giorgia Rota, Aodrenn Spill, Patrick Reichenbach, Vincent Zoete, and Denarda Dangaj Laniti

Subjects

Neoplasms. Tumors. Oncology. Including cancer and carcinogens, RC254-282

Abstract

Background The adoptive transfer of chimeric antigen receptor (CAR)-T cells has emerged as a potent immunotherapy against some hematological malignancies but not yet for epithelial-derived solid tumors. One critical issue is the paucity of broadly expressed solid tumor antigens (TAs), and another is the presence of suppressive mechanisms in the tumor microenvironment (TME) that can impair CAR-T cell homing, extravasation and effector functions. TAs expressed by endothelial cells of the tumor vasculature are of clinical interest for CAR therapy because of their genomic stability and accessibility to circulating T cells, as well as their expression across multiple tumor types. In this study, we sought to explore limitations to the efficacy of second-generation (2G) murine CAR-T cells redirected against the vascular endothelial growth factor receptor-2 (VEGFR-2) with the well-characterized single-chain variable fragment DC101.Methods Primary murine T cells were retrovirally transduced to express a 2G anti-VEGFR-2-CAR, and the in vitro binding to VEGFR-2, as well as reactivity against TA-expressing cells, was evaluated in the absence versus presence of exogenous VEGF-A. The CAR-T cells were further tested in vivo for tumor control alone and in combination with anti-VEGF-A antibody. Finally, we performed ex vivo phenotypic analyses of tumor-infiltrating CAR-T cells for the two treatment groups.Results In line with previous reports, we observed poor control of B16 melanoma by the 2G anti-VEGFR-2 CAR-T cells as a monotherapy. We further showed that VEGFR-2 is not downregulated by B16 melanoma tumors post treatment, but that its soluble ligand VEGF-A is upregulated and furthermore competes in vitro with the CAR-T cells for binding to VEGFR-2. This competition resulted in impaired CAR-T cell adhesion and effector function in vitro that could be restored in the presence of anti-VEGF-A antibody. Finally, we demonstrated that coadministration of anti-VEGF-A antibody in vivo promoted CAR-T cell persistence and tumor control and was associated with reduced frequencies of PD-1+ Ki67- and LAG-3+ Ki67- CAR-T cells in the TME.Conclusions This study represents the first example of impaired function of a vasculature-targeted CAR by an angiogenic ligand and rationalizes the use of combinatorial therapies that target the tumor vasculature and augment CAR-T cell effector function.

Published

2021

4. TCR sequencing and cloning methods for repertoire analysis and isolation of tumor-reactive TCRs

Author

Raphael Genolet, Sara Bobisse, Johanna Chiffelle, Marion Arnaud, Rémy Petremand, Lise Queiroz, Alexandra Michel, Patrick Reichenbach, Julien Cesbron, Aymeric Auger, Petra Baumgaertner, Philippe Guillaume, Julien Schmidt, Melita Irving, Lana E. Kandalaft, Daniel E. Speiser, George Coukos, and Alexandre Harari

Subjects

Genetics, Radiology, Nuclear Medicine and imaging, Biochemistry, Genetics and Molecular Biology (miscellaneous), Biochemistry, Computer Science Applications, Biotechnology

Published

2023

5. CD8 Binding of MHC-Peptide Complexes in cis or trans Regulates CD8+ T-cell Responses

Author

Laurence Goffin, Patrick Reichenbach, Luca Cariolato, Radek Šachl, Philippe Guillaume, Immanuel F. Luescher, Yang Liu, Marek Cebecauer, Michel A. Cuendet, Melita Irving, and George Coukos

Subjects

0303 health sciences, biology, Chemistry, CD3, T cell, T-cell receptor, chemical and pharmacologic phenomena, Major histocompatibility complex, 03 medical and health sciences, 0302 clinical medicine, medicine.anatomical_structure, Förster resonance energy transfer, Structural Biology, Docking (molecular), biology.protein, medicine, Biophysics, Cytotoxic T cell, Antigen-presenting cell, Molecular Biology, 030217 neurology & neurosurgery, 030304 developmental biology

Abstract

The coreceptor CD8αβ can greatly promote activation of T cells by strengthening T-cell receptor (TCR) binding to cognate peptide-MHC complexes (pMHC) on antigen presenting cells and by bringing p56Lck to TCR/CD3. Here, we demonstrate that CD8 can also bind to pMHC on the T cell (in cis) and that this inhibits their activation. Using molecular modeling, fluorescence resonance energy transfer experiments on living cells, biochemical and mutational analysis, we show that CD8 binding to pMHC in cis involves a different docking mode and is regulated by posttranslational modifications including a membrane-distal interchain disulfide bond and negatively charged O-linked glycans near positively charged sequences on the CD8β stalk. These modifications distort the stalk, thus favoring CD8 binding to pMHC in cis. Differential binding of CD8 to pMHC in cis or trans is a means to regulate CD8+ T-cell responses and provides new translational opportunities.

Published

2019

6. VEGFR-2 redirected CAR-T cells are functionally impaired by soluble VEGF-A competition for receptor binding

Author

Aodrenn Spill, Giorgia Rota, George Coukos, Vincent Zoete, Denarda Dangaj Laniti, Catherine Ronet, Melita Irving, Paris Kosti, Patrick Reichenbach, Evripidis Lanitis, and Elisabetta Cribioli

Subjects

Vascular Endothelial Growth Factor A, Cancer Research, Adoptive cell transfer, medicine.medical_treatment, Immunology, receptors, cell engineering, adoptive, Mice, Antigen, antigens, In vivo, Neoplasms, medicine, Animals, Humans, Immunology and Allergy, T-lymphocytes, RC254-282, Pharmacology, Tumor microenvironment, Receptors, Chimeric Antigen, Immune Cell Therapies and Immune Cell Engineering, biology, Chemistry, Neoplasms. Tumors. Oncology. Including cancer and carcinogens, Immunotherapy, Vascular Endothelial Growth Factor Receptor-2, Chimeric antigen receptor, Oncology, chimeric antigen, Cancer research, biology.protein, Molecular Medicine, immunotherapy, Antibody, Ex vivo

Abstract

BackgroundThe adoptive transfer of chimeric antigen receptor (CAR)-T cells has emerged as a potent immunotherapy against some hematological malignancies but not yet for epithelial-derived solid tumors. One critical issue is the paucity of broadly expressed solid tumor antigens (TAs), and another is the presence of suppressive mechanisms in the tumor microenvironment (TME) that can impair CAR-T cell homing, extravasation and effector functions. TAs expressed by endothelial cells of the tumor vasculature are of clinical interest for CAR therapy because of their genomic stability and accessibility to circulating T cells, as well as their expression across multiple tumor types. In this study, we sought to explore limitations to the efficacy of second-generation (2G) murine CAR-T cells redirected against the vascular endothelial growth factor receptor-2 (VEGFR-2) with the well-characterized single-chain variable fragment DC101.MethodsPrimary murine T cells were retrovirally transduced to express a 2G anti-VEGFR-2-CAR, and the in vitro binding to VEGFR-2, as well as reactivity against TA-expressing cells, was evaluated in the absence versus presence of exogenous VEGF-A. The CAR-T cells were further tested in vivo for tumor control alone and in combination with anti-VEGF-A antibody. Finally, we performed ex vivo phenotypic analyses of tumor-infiltrating CAR-T cells for the two treatment groups.ResultsIn line with previous reports, we observed poor control of B16 melanoma by the 2G anti-VEGFR-2 CAR-T cells as a monotherapy. We further showed that VEGFR-2 is not downregulated by B16 melanoma tumors post treatment, but that its soluble ligand VEGF-A is upregulated and furthermore competes in vitro with the CAR-T cells for binding to VEGFR-2. This competition resulted in impaired CAR-T cell adhesion and effector function in vitro that could be restored in the presence of anti-VEGF-A antibody. Finally, we demonstrated that coadministration of anti-VEGF-A antibody in vivo promoted CAR-T cell persistence and tumor control and was associated with reduced frequencies of PD-1+ Ki67- and LAG-3+ Ki67- CAR-T cells in the TME.ConclusionsThis study represents the first example of impaired function of a vasculature-targeted CAR by an angiogenic ligand and rationalizes the use of combinatorial therapies that target the tumor vasculature and augment CAR-T cell effector function.

Published

2021

7. CD8 Binding of MHC-Peptide Complexes in cis or trans Regulates CD8

Author

Yang, Liu, Michel A, Cuendet, Laurence, Goffin, Radek, Šachl, Marek, Cebecauer, Luca, Cariolato, Philippe, Guillaume, Patrick, Reichenbach, Melita, Irving, George, Coukos, and Immanuel F, Luescher

Subjects

Mice, Knockout, Models, Molecular, Protein Conformation, CD8 Antigens, CD8-Positive T-Lymphocytes, Lymphocyte Activation, Models, Biological, Mice, Structure-Activity Relationship, Histocompatibility Antigens, Multiprotein Complexes, Mutation, Animals, Protein Interaction Domains and Motifs, Amino Acid Sequence, Peptides, Protein Binding

Abstract

The coreceptor CD8αβ can greatly promote activation of T cells by strengthening T-cell receptor (TCR) binding to cognate peptide-MHC complexes (pMHC) on antigen presenting cells and by bringing p56

Published

2019

8. 1,2,3-Triazoles as inhibitors of indoleamine 2,3-dioxygenase 2 (IDO2)

Author

Daniela Caldelari, Olivier Michielin, Somi Reddy Majjigapu, Nahzli Dilek, George Coukos, Pierre Vogel, Ute F. Röhrig, Kelly Ascencao, Patrick Reichenbach, Vincent Zoete, and Melita Irving

Subjects

0301 basic medicine, Molecular model, medicine.medical_treatment, Clinical Biochemistry, Pharmaceutical Science, Biochemistry, Inhibitory Concentration 50, 03 medical and health sciences, Cancer immunotherapy, Catalytic Domain, Drug Discovery, medicine, Humans, Indoleamine-Pyrrole 2,3,-Dioxygenase, Enzyme Inhibitors, Indoleamine 2,3-dioxygenase, Molecular Biology, chemistry.chemical_classification, Organic Chemistry, Immune escape, Triazoles, Tryptophan Metabolism, Enzyme Activation, Molecular Weight, 030104 developmental biology, Enzyme, chemistry, Drug Design, Molecular Medicine, Molecular probe

Abstract

Indoleamine 2,3-dioxygenase 2 (IDO2) is a potential therapeutic target for the treatment of diseases that involve immune escape such as cancer. In contrast to IDO1, only a very limited number of inhibitors have been described for IDO2 due to inherent difficulties in expressing and purifying a functionally active, soluble form of the enzyme. Starting from our previously discovered highly efficient 4-aryl-1,2,3-triazole IDO1 inhibitor scaffold, we used computational structure-based methods to design inhibitors of IDO2 which we then tested in cellular assays. Our approach yielded low molecular weight inhibitors of IDO2, the most active displaying an IC 50 value of 51 μM for mIDO2, and twofold selectivity over hIDO1. These compounds could be useful as molecular probes to investigate the biological role of IDO2, and could inspire the design of new IDO2 inhibitors.

Published

2016

9. Author Correction: A computationally designed chimeric antigen receptor provides a small-molecule safety switch for T-cell therapy

Author

Melita Irving, Jaume Bonet, Elise Gray-Gaillard, Patrick Reichenbach, Byung-Ha Oh, George Coukos, Sailan Shui, Angel De Jesus Corria Osorio, Mi Jeong Kwak, Sabrina Vollers, Bruno E. Correia, Pablo Gainza, Greta Giordano-Attianese, Elisabetta Cribioli, and Seong Hoon Kim

Subjects

medicine.anatomical_structure, Chemistry, T cell, Biomedical Engineering, Cancer research, medicine, Molecular Medicine, Bioengineering, Applied Microbiology and Biotechnology, Small molecule, Chimeric antigen receptor, Biotechnology

Published

2020

10. Molecular Dissection of Telomeric Repeat-Containing RNA Biogenesis Unveils the Presence of Distinct and Multiple Regulatory Pathways

Author

Sascha Feuerhahn, Joachim Lingner, Antonio Porro, and Patrick Reichenbach

Subjects

RNA Caps, Identification, Telomeric repeat-containing RNAs, RNA Stability, Telomeric heterochromatin, Expression, Biology, Messenger-Rnas, Cell Line, 03 medical and health sciences, Ends, 0302 clinical medicine, Transcription (biology), Complex, Humans, RNA, Messenger, RNA Processing, Post-Transcriptional, Molecular Biology, 030304 developmental biology, Ribonucleoprotein, Genetics, 0303 health sciences, Base Sequence, Quality-Control, Cell Cycle, RNA, Articles, Cell Biology, Telomere, Subtelomere, Chromatin, Cell biology, Icf Syndrome, Tandem Repeat Sequences, 030220 oncology & carcinogenesis, Transcription, Biogenesis, HeLa Cells, Subcellular Fractions, X-Chromosome Inactivation, Yeast Poly(A) Polymerase

Abstract

Telomeres are transcribed into telomeric repeat-containing RNA (TERRA), large, heterogeneous, noncoding transcripts which form part of the telomeric heterochromatin. Despite a large number of functions that have been ascribed to TERRA, little is known about its biogenesis. Here, we present the first comprehensive analysis of the molecular structure of TERRA. We identify biochemically distinct TERRA complexes, and we describe TERRA regulation during the cell cycle. Moreover, we demonstrate that TERRA 5' ends contain 7-methylguanosine cap structures and that the poly(A) tail, present on a fraction of TERRA transcripts, contributes to their stability. Poly(A)(-) TERRA, but not poly(A)(+) TERRA, is associated with chromatin, possibly reflecting distinct biological roles of TERRA ribonucleoprotein complexes. In support of this idea, poly(A)(-) and poly(A)(+) TERRA molecules end with distinct sequence registers. We also determine that the bulk of 3'-terminal UUAGGG repeats have an average length of 200 bases, indicating that the length heterogeneity of TERRA likely stems from its subtelomeric regions. Finally, we find that TERRA is regulated during the cell cycle, being lowest in late S phase and peaking in early G(1). Our analyses offer the basis for investigating multiple regulatory pathways that affect TERRA synthesis, processing, turnover, and function.

Published

2010

11. Protein–RNA and protein–protein interactions mediate association of human EST1A/SMG6 with telomerase

Author

Joachim Lingner, Patrick Reichenbach, and Sophie Redon

Subjects

Telomerase, Nucleic Acid Enzymes, RNA, Context (language use), Plasma protein binding, Biology, Molecular biology, Recombinant Proteins, Cell Line, Protein–protein interaction, Telomerase RNA component, Genetics, Humans, Telomerase reverse transcriptase, Protein Binding, Ribonucleoprotein

Abstract

The human EST1A/SMG6 polypeptide physically interacts with the chromosome end replication enzyme telomerase. In an attempt to better understand hEST1A function, we have started to dissect the molecular interactions between hEST1A and telomerase. Here, we demonstrate that the interaction between hEST1A and telomerase is mediated by protein-RNA and protein-protein contacts. We identify a domain within hEST1A that binds the telomerase RNA moiety hTR while full-length hEST1A establishes in addition RNase-resistant and hTR-independent protein-protein contacts with the human telomerase reverse transcriptase polypeptide (TERT). Conversely, within hTERT, we identify a hEST1A interaction domain, which comprises hTR-binding activity and RNA-independent hEST1A-binding activity. Purified, recombinant hEST1A binds the telomerase RNA moiety (hTR) with high affinity (apparent overall K(d) = 25 nM) but low specificity. We propose that hEST1A assembles specifically with telomerase in the context of the hTR-hTERT ribonucleoprotein, through the high affinity of hEST1A for hTR and specific protein-protein contacts with hTERT.

Published

2007

12. Human Telomerase RNA Accumulation in Cajal Bodies Facilitates Telomerase Recruitment to Telomeres and Telomere Elongation

Author

Emem Adolf, Michael P. Terns, Joachim Lingner, Gaël Cristofari, Rebecca M. Terns, Patrick Reichenbach, and Katarzyna Sikora

Subjects

Cell Extracts, Telomerase, Protein subunit, Coiled Bodies, Biology, 03 medical and health sciences, Telomerase RNA component, 0302 clinical medicine, Humans, Telomerase reverse transcriptase, Molecular Biology, 030304 developmental biology, Ribonucleoprotein, 0303 health sciences, RNA, Cell Biology, Telomere, Molecular biology, Cell biology, Enzyme Activation, Protein Transport, Cajal body, 030220 oncology & carcinogenesis, Mutation, Nucleic Acid Conformation, HeLa Cells

Abstract

Telomerase is required for telomere maintenance and is responsible for the immortal phenotype of cancer cells. How telomerase is assembled and reaches telomeres in the context of nuclear architecture is not understood. Recently, the telomerase RNA subunit (hTR) was shown to accumulate in Cajal bodies (CBs), subnuclear structures implicated in ribonucleoprotein maturation. However, the functional relevance of this localization for telomerase was unknown. hTR localization to CBs requires a short sequence motif called the CAB box. Here, we reconstitute telomerase in human cells and determine the effects of CAB box mutations on telomere biology. We demonstrate that mutant hTR, which fails to accumulate in CBs, is fully capable of forming catalytically active telomerase in vivo but is strongly impaired in telomere extension. The functional deficiency is accompanied by a decreased association of telomerase with telomeres. Collectively, these data identify subnuclear localization as an important regulatory mechanism for telomere length homeostasis in human cells.

Published

2007

13. DNA Binding Specificity of Different STAT Proteins

Author

Patrick Reichenbach, Curt M. Horvath, Philipp Bucher, Stefan Fritz, Markus Nabholz, Georg B. Ehret, and Ulrike Schindler

Subjects

animal structures, biology, food and beverages, Cell Biology, Biochemistry, DNA-binding protein, Molecular biology, DNA binding site, biology.protein, STAT protein, STAT1, Binding site, Molecular Biology, Gene, STAT5, STAT6

Abstract

STAT transcription factors are expressed in many cell types and bind to similar sequences. However, different STAT gene knock-outs show very distinct phenotypes. To determine whether differences between the binding specificities of STAT proteins account for these effects, we compared the sequences bound by STAT1, STAT5A, STAT5B, and STAT6. One sequence set was selected from random oligonucleotides by recombinant STAT1, STAT5A, or STAT6. For another set including many weak binding sites, we quantified the relative affinities to STAT1, STAT5A, STAT5B, and STAT6. We compared the results to the binding sites in natural STAT target genes identified by others. The experiments confirmed the similar specificity of different STAT proteins. Detailed analysis indicated that STAT5A specificity is more similar to that of STAT6 than that of STAT1, as expected from the evolutionary relationships. The preference of STAT6 for sites in which the half-palindromes (TTC) are separated by four nucleotides (N(4)) was confirmed, but analysis of weak binding sites showed that STAT6 binds fairly well to N(3) sites. As previously reported, STAT1 and STAT5 prefer N(3) sites; however, STAT5A, but not STAT1, weakly binds N(4) sites. None of the STATs bound to half-palindromes. There were no specificity differences between STAT5A and STAT5B.

Published

2001

14. Human CD8+ T cells expressing HLA-DR and CD28 show telomerase activity and are distinct from cytolytic effector T cells

Author

Danila Valmori, Immanuel Lüscher, Mikael J. Pittet, Pedro Romero, Ferdy Lejeune, Philippe Guillaume, Marco Migliaccio, Patrick Reichenbach, Danielle Liénard, Daniel E. Speiser, and Jean-Charles Cerottini

Subjects

ZAP70, Immunology, hemic and immune systems, chemical and pharmacologic phenomena, Biology, Natural killer T cell, Molecular biology, Interleukin 21, Immunology and Allergy, Cytotoxic T cell, Telomerase reverse transcriptase, IL-2 receptor, Antigen-presenting cell, Interleukin 3

Abstract

Cycling lymphocytes may express the enzyme telomerase which is involved in maintenance of telomere length and cell proliferation potential. In CD8(+) T cells freshly isolated from peripheral blood, we found that in vivo cycling cells expressed HLA-DR. Furthermore, CD28-positive cells are known to have longer telomeres than CD28-negative T cells. Therefore we used HLA-DR- and CD28-specific antibodies to sort CD8(+) T cells and measure telomerase activity ex vivo. Relatively high levels of telomerase activity were found in HLA-DR/CD28 double-positive cells. In contrast, HLA-DR-negative and CD28-negative cells had almost no telomerase activity. In summary, HLA-DR expression correlates with proliferation, and CD28 expression with proliferative potential. We have previously identified that ex vivo cytolytic CD8(+) T cells are CD56 (NCAM) positive. Here we show that HLA-DR(+) cells were rarely CD56(+) and vice versa. This demonstrates that telomerase-expressing and cytolytic CD8(+) T cells can be separated on the basis of the cell surface markers HLA-DR and CD56. Thus, activated CD8(+) T cells specialize and exert distinct functions correlating with surface molecule expression.

Published

2001

15. Ectopic Human Telomerase Catalytic Subunit Expression Maintains Telomere Length But Is Not Sufficient for CD8+ T Lymphocyte Immortalization

Author

Jean-Charles Cerottini, Tom Just, Pedro Romero, Markus Nabholz, Danila Valmori, Marco Migliaccio, Patrick Reichenbach, and Mario Amacker

Subjects

Adoptive cell transfer, Telomerase, Somatic cell, Immunology, Cell Culture Techniques, Cell Separation, CD8-Positive T-Lymphocytes, Biology, Lymphocyte Activation, Transduction, Genetic, Catalytic Domain, Humans, Immunology and Allergy, Telomerase reverse transcriptase, Cell Line, Transformed, Telomere, Molecular biology, DNA-Binding Proteins, Retroviridae, Cell culture, RNA, Ectopic expression, Cell Division, CD8, T-Lymphocytes, Cytotoxic

Abstract

Like most somatic human cells, T lymphocytes have a limited replicative life span. This phenomenon, called senescence, presents a serious barrier to clinical applications that require large numbers of Ag-specific T cells such as adoptive transfer therapy. Ectopic expression of hTERT, the human catalytic subunit of the enzyme telomerase, permits fibroblasts and endothelial cells to avoid senescence and to become immortal. In an attempt to immortalize normal human CD8+ T lymphocytes, we infected bulk cultures or clones of these cells with a retrovirus transducing an hTERT cDNA clone. More than 90% of transduced cells expressed the transgene, and the cell populations contained high levels of telomerase activity. Measuring the content of total telomere repeats in individual cells (by flowFISH) we found that ectopic hTERT expression reversed the gradual loss of telomeric DNA observed in control populations during long term culture. Telomere length in transduced cells reached the levels observed in freshly isolated normal CD8+ lymphocytes. Nevertheless, all hTERT-transduced populations stopped to divide at the same time as nontransduced or vector-transduced control cells. When kept in IL-2 the arrested cells remained alive. Our results indicate that hTERT may be required but is not sufficient to immortalize human T lymphocytes.

Published

2000

16. Elf-1 Contributes to the Function of the Complex Interleukin (IL)-2–responsive Enhancer in the Mouse IL-2 Receptor α Gene

Author

Anne Wilson, M. Pla, Patrick Reichenbach, Jonathan Freeman, Markus Nabholz, Irina Serdobova, Peter Sperisen, and Jacques Ghysdael

Subjects

T-Lymphocytes, Molecular Sequence Data, Immunology, Cooperativity, Plasma protein binding, Biology, DNA-binding protein, Article, Mice, Proto-Oncogene Proteins, Tumor Cells, Cultured, Transcriptional regulation, Animals, Immunology and Allergy, Nuclear protein, Binding site, Enhancer, Transcription factor, Binding Sites, Base Sequence, Proto-Oncogene Proteins c-ets, Ephrin-A2, Nuclear Proteins, Receptors, Interleukin-2, Molecular biology, DNA-Binding Proteins, Enhancer Elements, Genetic, DNA-Binding Proteins/genetics, DNA-Binding Proteins/metabolism, Interleukin-2/pharmacology, Mutation, Nuclear Proteins/metabolism, Protein Binding, Proto-Oncogene Proteins/genetics, Receptors, Interleukin-2/genetics, T-Lymphocytes/metabolism, Transcription Factors/genetics, Transcription Factors/metabolism, Interleukin-2, Transcription Factors

Abstract

Lymphocytes regulate their responsiveness to IL-2 through the transcriptional control of the IL-2Rα gene, which encodes a component of the high affinity IL-2 receptor. In the mouse IL-2Rα gene this control is exerted via two regulatable elements, a promoter proximal region, and an IL-2–responsive enhancer (IL-2rE) 1.3 kb upstream. In vitro and in vivo functional analysis of the IL-2rE in the rodent thymic lymphoma-derived, CD4−CD8− cell line PC60 demonstrated that three separate elements, sites I, II, and III, were necessary for IL-2 responsiveness; these three sites demonstrate functional cooperation. Site III contains a consensus binding motif for members of the Ets family of transcription factors. Here we demonstrate that Elf-1, an Ets-like protein, binds to site III and participates in IL-2 responsiveness. In vitro site III forms a complex with a protein constitutively present in nuclear extracts from PC60 cells as well as from normal CD4−CD8− thymocytes. We have identified this molecule as Elf-1 according to a number of criteria. The complex possesses an identical electrophoretic mobility to that formed by recombinant Elf-1 protein and is super-shifted by anti–Elf-1 antibodies. Biotinylated IL-2rE probes precipitate Elf-1 from PC60 extracts provided site III is intact and both recombinant and PC60-derived proteins bind with the same relative affinities to different mutants of site III. In addition, by introducing mutations into the core of the site III Ets-like motif and comparing the corresponding effects on the in vitro binding of Elf-1 and the in vivo IL-2rE activity, we provide strong evidence that Elf-1 is directly involved in IL-2 responsiveness. The nature of the functional cooperativity observed between Elf-1 and the factors binding sites I and II remains unresolved; experiments presented here however suggest that this effect may not require direct interactions between the proteins binding these three elements.

Published

1997

17. Telomerase inhibitors from cyanobacteria: isolation and synthesis of sulfoquinovosyl diacylglycerols from Microcystis aeruguinosa PCC 7806

Author

Karl Gademann, Tom M. Woods, Joachim Lingner, Danilo D’Ambrosio, Cyril Portmann, Patrick Reichenbach, Damiano Banfi, Gerardo Turcatti, Emilie Baudat, Laeticia Da Silva, and Malika Makhlouf Brahmi

Subjects

Cyanobacteria, Telomerase, Microcystis, Phencyclidine, Tandem mass spectrometry, 01 natural sciences, Catalysis, Diglycerides, 03 medical and health sciences, Structure-Activity Relationship, Tandem Mass Spectrometry, Structure–activity relationship, Enzyme Inhibitors, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Chromatography, biology, 010405 organic chemistry, Organic Chemistry, Biological activity, General Chemistry, biology.organism_classification, 0104 chemical sciences, Enzyme, Biochemistry, chemistry, Glycolipids, Two-dimensional nuclear magnetic resonance spectroscopy

Abstract

By using the Telospot assay, 27 different extracts of cyanobacteria were evaluated for telomerase inhibition. All extracts showed varying, but significant activity. We selected Microcystis aeruguinosa PCC 7806 to identify the active compound and a bioassay guided fractionation led us to isolate mixtures of sulfoquinovosyl diacylglycerols (SQDGs), which were identified by 2D NMR and MS/MS experiments. Pure SQDG derivatives were then synthesized. The IC(50) values of pure synthetic sulfoquinovosyl dipalmitoylglycerol and the monopalmitoylated derivative against telomerase were determined to be 17 and 40 μM, respectively. A structure-activity relationship study allowed the identification of compounds with modified lipophilic acyl groups that display improved activity.

Published

2013

18. Mouse Interleukin-2 Receptor α Gene Expression

Author

Corinne Rusterholz, Markus Nabholz, Peter Sperisen, Elisabetta Soldaini, San Ming Wang, Patrick Reichenbach, Patricia Corthesy, M. Pla, and Philipp Bucher

Subjects

SCN3A, Retinoic acid receptor alpha, Interleukin 5 receptor alpha subunit, Interleukin, Liver X receptor alpha, Cell Biology, Biology, Enhancer, Molecular Biology, Biochemistry, Molecular biology, G alpha subunit, Interleukin 10 receptor, alpha subunit

Abstract

We have shown that interleukin-1 (IL-1) and IL-2 control IL-2 receptor alpha (IL-2R alpha) gene transcription in CD4-CD8- murine T lymphocyte precursors. Here we map the cis-acting elements that mediate interleukin responsiveness of the mouse IL-2R alpha gene using a thymic lymphoma-derived hybridoma (PC60). The transcriptional response of the IL-2R alpha gene to stimulation by IL-1 + IL-2 is biphasic. IL-1 induces a rapid, protein synthesis-independent appearance of IL-2R alpha mRNA that is blocked by inhibitors of NF-kappa B activation. It also primes cells to become IL-2 responsive and thereby prepares the second phase, in which IL-2 induces a 100-fold further increase in IL-2R alpha transcripts. Transient transfection experiments show that several elements in the promoter-proximal region of the IL-2R alpha gene contribute to IL-1 responsiveness, most importantly an NF-kappa B site conserved in the human and mouse gene. IL-2 responsiveness, on the other hand, depends on a 78-nucleotide segment 1.3 kilobases upstream of the major transcription start site. This segment functions as an IL-2-inducible enhancer and lies within a region that becomes DNase I hypersensitive in normal T cells in which IL-2R alpha expression has been induced. IL-2 responsiveness requires three distinct elements within the enhancer. Two of these are potential binding sites for STAT proteins.

Published

1995

19. Specific binding of telomeric G-quadruplexes by hydrosoluble perylene derivatives inhibits repeat addition processivity of human telomerase

Author

Joachim Lingner, Patrick Reichenbach, Emanuela Micheli, Antonello Alvino, Danilo D’Ambrosio, Marco Franceschin, and Maria Savino

Subjects

Telomerase, Spectrometry, Mass, Electrospray Ionization, Inhibitor, Cells, Compound, Biology, G-quadruplex, Ligands, Imides, Biochemistry, 03 medical and health sciences, chemistry.chemical_compound, medicine, Humans, Telospot, Dna Structures, Mass-Spectrometry, Polymorphism, Perylene, 030304 developmental biology, Cancer, Telomere-binding protein, 0303 health sciences, telomerase, g-quadruplex, telospot, perylene diimide, telomere, inhibitor, Coronene Derivatives, Circular Dichroism, 030302 biochemistry & molecular biology, General Medicine, Processivity, Telomere, Reverse-Transcriptase, Reverse transcriptase, G-Quadruplexes, Mechanism of action, chemistry, Perylene diimide, Different Side-Chains, medicine.symptom, DNA

Abstract

Telomerase is responsible for the immortal phenotype of cancer cells and telomerase inhibition may specifically target cancer cell proliferation. Ligands able to selectively bind to G-quadruplex telomeric DNA have been considered as telomerase inhibitors but their mechanisms of action have often been deduced from a non-quantitative telomerase activity assay (TRAP assay) that involves a PCR step and that does not provide insight on the mechanism of inhibition. Furthermore, quadruplex ligands have also been shown to exert their effects by affecting association of telomere binding proteins with telomeres. Here, we use quantitative direct telomerase activity assays to evaluate the strength and mechanism of action of hydrosoluble perylene diimides (HPDIs). HPDIs contain a perylene moiety and different numbers of positively charged side chains. Side chain features vary with regard to number and distances of the charges. IC50 values of HPDIs were in the low micromolar (0.5-5 mu M) range depending on the number and features of the side chains. HPDIs having four side chains emerged as the best compounds of this series. Analysis of primer elongation products demonstrated that at low HPDI concentrations, telomerase inhibition involved formation of telomeric G-quadruplex structures, which inhibited further elongation by telomerase. At high HPDI concentrations, telomerase inhibition occurred independently of G-quadruplex formation of the substrate. The mechanism of action of HPDIs and their specific binding to G-quadruplex DNA was supported by PAGE analysis, CD spectroscopy and ESI-MS. Finally, competition Telospot experiments with duplex DNA indicated specific binding of HPDIs to the single-stranded telomeric substrates over double stranded DNA, a result supported by competitive ESI-MS. Altogether, our results indicate that HPDIs act by stabilizing G-quadruplex structures in single-stranded telomeric DNA, which in turn prevents repeat addition processivity of telomerase. (C) 2011 Elsevier Masson SAS. All rights reserved.

Published

2011

20. The non-coding RNA TERRA is a natural ligand and direct inhibitor of human telomerase

Author

Patrick Reichenbach, Joachim Lingner, and Sophie Redon

Subjects

Telomerase, Telomeric repeat-containing RNAs, RNA, Untranslated, Chromosome Ends, Telomeric heterochromatin, Repeat-Containing Rna, Biology, Ligands, Cell Line, Association, 03 medical and health sciences, Telomerase RNA component, 0302 clinical medicine, Transcription (biology), Hnrnp A1, Genetics, Humans, Telomerase reverse transcriptase, 030304 developmental biology, Repetitive Sequences, Nucleic Acid, Cell Nucleus, 0303 health sciences, Nucleic Acid Enzymes, Anchor Site, Immortal Cells, Templates, Genetic, Dna, Telomere, Non-coding RNA, Molecular biology, Reverse-Transcriptase, Mammalian Telomeres, In-Vitro, 030220 oncology & carcinogenesis, Peptides

Abstract

Telomeres, the physical ends of eukaryotes chromosomes are transcribed into telomeric repeat containing RNA (TERRA), a large non-coding RNA of unknown function, which forms an integral part of telomeric heterochromatin. TERRA molecules resemble in sequence the telomeric DNA substrate as they contain 5'-UUAGGG-3' repeats near their 3'-end which are complementary to the template sequence of telomerase RNA. Here we demonstrate that endogenous TERRA is bound to human telomerase in cell extracts. Using in vitro reconstituted telomerase and synthetic TERRA molecules we demonstrate that the 5'-UUAGGG-3' repeats of TERRA base pair with the RNA template of the telomerase RNA moiety (TR). In addition TERRA contacts the telomerase reverse transcriptase (TERT) protein subunit independently of hTR. In vitro studies further demonstrate that TERRA is not used as a telomerase substrate. Instead, TERRA acts as a potent competitive inhibitor for telomeric DNA in addition to exerting an uncompetitive mode of inhibition. Our data identify TERRA as a telomerase ligand and natural direct inhibitor of human telomerase. Telomerase regulation by the telomere substrate may be mediated via its transcription.

Published

2010

21. TIN2-tethered TPP1 recruits human telomerase to telomeres in vivo

Author

Michael P. Terns, Rebecca M. Terns, Joachim Lingner, Gaël Cristofari, Elena Aritonovska, Patrick Reichenbach, Eladio Abreu, and Brad Culp

Subjects

Telomerase, Chromatin Immunoprecipitation, Human Cancer-Cells, Length Homeostasis, Telomere-Binding Proteins, Dysfunctional Telomeres, Dna-Damage Response, Biology, Protein Structure, Secondary, Shelterin Complex, 03 medical and health sciences, Telomerase RNA component, 0302 clinical medicine, Cajal Bodies, Oligosaccharide binding, Humans, Telomerase reverse transcriptase, Molecular Biology, Pot1, 030304 developmental biology, Telomere-binding protein, 0303 health sciences, End-Binding Protein, Dyskeratosis-Congenita, Cell Biology, Articles, Telomere, Shelterin, Molecular biology, Reverse-Transcriptase, 3. Good health, Protein Transport, Cajal body, 030220 oncology & carcinogenesis, Rna, DNA Damage, HeLa Cells, Protein Binding

Abstract

Recruitment to telomeres is a pivotal step in the function and regulation of human telomerase; however, the molecular basis for recruitment is not known. Here, we have directly investigated the process of telomerase recruitment via fluorescence in situ hybridization (FISH) and chromatin immunoprecipitation (ChIP). We find that depletion of two components of the shelterin complex that is found at telomeres--TPP1 and the protein that tethers TPP1 to the complex, TIN2--results in a loss of telomerase recruitment. On the other hand, we find that the majority of the observed telomerase association with telomeres does not require POT1, the shelterin protein that links TPP1 to the single-stranded region of the telomere. Deletion of the oligonucleotide/oligosaccharide binding fold (OB-fold) of TPP1 disrupts telomerase recruitment. In addition, while loss of TPP1 results in the appearance of DNA damage factors at telomeres, the DNA damage response per se does not account for the telomerase recruitment defect observed in the absence of TPP1. Our findings indicate that TIN2-anchored TPP1 plays a major role in the recruitment of telomerase to telomeres in human cells and that recruitment does not depend on POT1 or interaction of the shelterin complex with the single-stranded region of the telomere.

Published

2010

22. Reevaluation of telomerase inhibition by quadruplex ligands and their mechanisms of action

Author

David Monchaud, Jean-Louis Mergny, Patrick Reichenbach, Kazuo Shin-ya, Laurent Lacroix, Elsa De Lemos, Marie-Paule Teulade-Fichou, Anne De Cian, Joachim Lingner, Gaël Cristofari, Sciences pour l'environnement (SPE), Centre National de la Recherche Scientifique (CNRS)-Université Pascal Paoli (UPP), Istituto di Ricerca per la Protezione Idrogeologica [Perugia] (IRPI), Consiglio Nazionale delle Ricerche [Roma] (CNR), Régulation et dynamique des génomes, Institut National de la Santé et de la Recherche Médicale (INSERM)-Centre National de la Recherche Scientifique (CNRS), Institut de Chimie Moléculaire de l'Université de Bourgogne [Dijon] (ICMUB), and Université de Bourgogne (UB)-Institut de Chimie du CNRS (INC)-Centre National de la Recherche Scientifique (CNRS)

Subjects

Telomerase, Molecular Sequence Data, Biology, Ligands, 010402 general chemistry, G-quadruplex, 01 natural sciences, Telomeric repeat, Substrate Specificity, Inhibitory Concentration 50, 03 medical and health sciences, heterocyclic compounds, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Inhibitory effect, ComputingMilieux_MISCELLANEOUS, 030304 developmental biology, 0303 health sciences, Multidisciplinary, Base Sequence, Telomerase inhibition, [CHIM.ORGA]Chemical Sciences/Organic chemistry, Biological activity, Processivity, Biological Sciences, 0104 chemical sciences, G-Quadruplexes, Biochemistry, Telomeric dna

Abstract

Quadruplex ligands are often considered as telomerase inhibitors. Given the fact that some of these molecules are present in the clinical setting, it is important to establish the validity of this assertion. To analyze the effects of these compounds, we used a direct assay with telomerase-enriched extracts. The comparison of potent ligands from various chemical families revealed important differences in terms of effects on telomerase initiation and processivity. Although most quadruplex ligands may lock a quadruplex-prone sequence into a quadruplex structure that inhibits the initiation of elongation by telomerase, the analysis of telomerase-elongation steps revealed that only a few molecules interfered with the processivity of telomerase (i.e., inhibit elongation once one or more repeats have been incorporated). The demonstration that these molecules are actually more effective inhibitors of telomeric DNA amplification than extension by telomerase contributes to the already growing suspicion that quadruplex ligands are not simple telomerase inhibitors but, rather, constitute a different class of biologically active molecules. We also demonstrate that the popular telomeric repeat amplification protocol is completely inappropriate for the determination of telomerase inhibition by quadruplex ligands, even when PCR controls are included. As a consequence, the inhibitory effect of many quadruplex ligands has been overestimated.

Published

2007

23. Telomeric repeat containing RNA and RNA surveillance factors at mammalian chromosome ends

Author

Lela Khoriauli, Claus M. Azzalin, Elena Giulotto, Joachim Lingner, and Patrick Reichenbach

Subjects

Telomere Recombination, Telomerase, Telomeric repeat-containing RNAs, Transcription, Genetic, Molecular Sequence Data, Telomeric heterochromatin, Biology, Mice, Tumor Cells, Cultured, Animals, Chromosomes, Human, Humans, Amino Acid Sequence, Cells, Cultured, In Situ Hybridization, Fluorescence, Repetitive Sequences, Nucleic Acid, Genetics, Multidisciplinary, RNA, Proteins, Telomere, Subtelomere, Blotting, Northern, Chromosomes, Mammalian, Eukaryotic chromosome fine structure, HeLa Cells

Abstract

Telomeres, the DNA-protein complexes located at the end of linear eukaryotic chromosomes, are essential for chromosome stability. Until now, telomeres have been considered to be transcriptionally silent. We demonstrate that mammalian telomeres are transcribed into telomeric repeat–containing RNA (TERRA). TERRA molecules are heterogeneous in length, are transcribed from several subtelomeric loci toward chromosome ends, and localize to telomeres. We also show that suppressors with morphogenetic defects in genitalia (SMG) proteins, which are effectors of nonsense-mediated messenger RNA decay, are enriched at telomeres in vivo, negatively regulate TERRA association with chromatin, and protect chromosome ends from telomere loss. Thus, telomeres are actively transcribed into TERRA, and SMG factors represent a molecular link between TERRA regulation and the maintenance of telomere integrity.

Published

2007

24. Low- to high-throughput analysis of telomerase modulators with Telospot

Author

Marc Chambon, Damiano Banfi, Joachim Lingner, Patrick Reichenbach, Gaël Cristofari, Pierre-Olivier Regamey, and Gerardo Turcatti

Subjects

Genetics, Human telomerase, Telomerase, Chemical biology, Antineoplastic Agents, Cell Biology, Computational biology, Biology, Biochemistry, High throughput analysis, chemistry.chemical_compound, chemistry, Humans, Molecular Biology, Throughput (business), DNA, Biotechnology

Abstract

We designed a method termed Telospot to discover and characterize telomerase modulators as anticancer drugs or chemical biology tools. Telospot is based on a highly efficient human telomerase expression system and the detection of telomerase DNA reaction products in macroarray format. Telospot offers a highly scalable, cost- and time-effective alternative to presently available telomerase assays, which are limited by the requirement for PCR, telomerase purification or technologies not amenable to high throughput.

Published

2007

25. Methods for the ex vivo characterization of human CD8+ T subsets based on gene expression and replicative history analysis

Author

Nathalie, Rufer, Patrick, Reichenbach, and Pedro, Romero

Subjects

Reverse Transcriptase Polymerase Chain Reaction, T-Lymphocyte Subsets, Gene Expression, Humans, CD8-Positive T-Lymphocytes, Fibroblasts, Telomere, Flow Cytometry, Cell Division, In Situ Hybridization, Fluorescence

Abstract

The generation of an antigen-specific T-lymphocyte response is a complex multi-step process. Upon T-cell receptor-mediated recognition of antigen presented by activated dendritic cells, naive T-lymphocytes enter a program of proliferation and differentiation, during the course of which they acquire effector functions and may ultimately become memory T-cells. A major goal of modern immunology is to precisely identify and characterize effector and memory T-cell subpopulations that may be most efficient in disease protection. Sensitive methods are required to address these questions in exceedingly low numbers of antigen-specific lymphocytes recovered from clinical samples, and not manipulated in vitro. We have developed new techniques to dissect immune responses against viral or tumor antigens. These allow the isolation of various subsets of antigen-specific T-cells (with major histocompatibility complex [MHC]-peptide multimers and five-color FACS sorting) and the monitoring of gene expression in individual cells (by five-cell reverse transcription-polymerase chain reaction [RT-PCR]). We can also follow their proliferative life history by flow-fluorescence in situ hybridization (FISH) analysis of average telomere length. Recently, using these tools, we have identified subpopulations of CD8+ T-lymphocytes with distinct proliferative history and partial effector-like properties. Our data suggest that these subsets descend from recently activated T-cells and are committed to become differentiated effector T-lymphocytes.

Published

2004

26. Methods for the Ex Vivo Characterization of Human CD8+ T Subsets Based on Gene Expression and Replicative History Analysis

Author

Patrick Reichenbach, Pedro Romero, and Nathalie Rufer

Subjects

Immune system, Antigen, biology, Effector, Gene expression, biology.protein, In situ hybridization, Major histocompatibility complex, CD8, Telomere, Cell biology

Abstract

The generation of an antigen-specific T-lymphocyte response is a complex multi-step process. Upon T-cell receptor-mediated recognition of antigen presented by activated dendritic cells, naive T-lymphocytes enter a program of proliferation and differentiation, during the course of which they acquire effector functions and may ultimately become memory T-cells. A major goal of modern immunology is to precisely identify and characterize effector and memory T-cell subpopulations that may be most efficient in disease protection. Sensitive methods are required to address these questions in exceedingly low numbers of antigen-specific lymphocytes recovered from clinical samples, and not manipulated in vitro. We have developed new techniques to dissect immune responses against viral or tumor antigens. These allow the isolation of various subsets of antigen-specific T-cells (with major histocompatibility complex [MHC]-peptide multimers and five-color FACS sorting) and the monitoring of gene expression in individual cells (by five-cell reverse transcription-polymerase chain reaction [RT-PCR]). We can also follow their proliferative life history by flow-fluorescence in situ hybridization (FISH) analysis of average telomere length. Recently, using these tools, we have identified subpopulations of CD8+ T-lymphocytes with distinct proliferative history and partial effector-like properties. Our data suggest that these subsets descend from recently activated T-cells and are committed to become differentiated effector T-lymphocytes.

Published

2004

27. Induction of interleukin-2 receptor alpha (IL-2Ralpha) expression by interleukin-2: important role of the interleukin-2 receptor beta chain region between the two Stat5 docking sites

Author

Véronique, Imbert, Roger, Rezzonico, Patrick, Reichenbach, and Markus, Nabholz

Subjects

Base Sequence, Blotting, Western, Interleukin-2 Receptor alpha Subunit, Electrophoretic Mobility Shift Assay, Receptors, Interleukin, Milk Proteins, Precipitin Tests, Cell Line, DNA-Binding Proteins, Interleukin-2 Receptor beta Subunit, Mice, STAT5 Transcription Factor, Trans-Activators, Animals, Interleukin-2, DNA Primers, Protein Binding

Abstract

The interleukin-2 receptor alpha (IL-2Ralpha) forms, together with IL-2Rbeta and gammac chains, a high affinity IL-2 receptor that is important for IL-2 responsiveness and normal T cell function. Expression of the IL-2Ralpha gene by T cells is regulated mainly at the transcription level which is transiently activated by antigen and upregulated and then prolonged by stimulation with IL-2. The effect of IL-2 on the IL-2Ralpha gene depends on the activation of the transcription factor Stat5, which acts on an IL-2- responsive enhancer that consists of two Stat5 and an Elf1 binding site. To identify the functional domains of the IL-2 receptor required for the stimulation of IL-2Ralpha gene expression, we introduced, into the CTL44 T cell line, receptor chimeras between the extracellular domain of the IL-9 receptor and the cytoplasmic region of IL-2Rbeta. Analyzing the effect of mutations in the intracellular IL-2Rbeta segment, we found that a minimal receptor containing the Jak boxes and one intact Stat5 docking site (i.e. tyrosine 392 or 510) can, as expected, mediate Stat5 activation, but is unable to stimulate IL-2Ralpha expression. However, when this minimal receptor includes the region between the two tyrosines, its capacity to mediate IL-2Ralpha cell surface expression is restored. These data suggest that the segment between the two Stat5 docking sites of the IL-2Rbeta chain mediates signaling events that, together with Stat5 activation, are essential for the stimulation of IL-2Ralpha gene transcription.

Published

2002

28. Interaction of STAT5 dimers on two low affinity binding sites mediates interleukin 2 (IL-2) stimulation of IL-2 receptor alpha gene transcription

Author

Markus Nabholz, Patrick Reichenbach, Elisabetta Soldaini, Ulrike Schindler, and Wolfram K.-H. Meyer

Subjects

Transcription, Genetic, Molecular Sequence Data, Enhancer RNAs, Plasma protein binding, Biochemistry, Cell Line, Mice, Transcription (biology), STAT5 Transcription Factor, Animals, Binding site, Enhancer, Molecular Biology, STAT5, Binding Sites, biology, Base Sequence, Receptors, Interleukin-2, Cell Biology, DNA, Milk Proteins, Molecular biology, DNA binding site, DNA-Binding Proteins, biology.protein, STAT protein, Trans-Activators, Interleukin-2, Dimerization, Protein Binding

Abstract

Stimulation of the interleukin 2 receptor alpha (IL-2Ralpha) gene by IL-2 is important for the proliferation of antigen-activated T lymphocytes. IL-2 regulates IL-2Ralpha transcription via a conserved 51-nucleotide IL-2 responsive enhancer. Mouse enhancer function depends on cooperative activity of three distinct sites. Two of these are weak binding sites for IL-2-activated STAT5 (signal transducer and activator of transcription) proteins, and mutational analysis indicates that binding of STAT5 to both sites is required for IL-2 responsiveness of the enhancer. The STAT5 dimers interact to form a STAT5 tetramer. The efficiency of tetramerization depends on the relative rotational orientation of the two STAT motifs on the DNA helix. STAT5 tetramerization on enhancer mutants correlates well with the IL-2 responsiveness of these mutants. This provides strong evidence that interactions between STAT dimers binding to a pair of weak binding sites play a biological role by controlling the activity of a well characterized, complex cytokine-responsive enhancer.

Published

1998

29. The cis-acting elements controlling mouse IL-2R alpha transcription

Author

Peter Sperisen, H. R. Macdonald, Patrick Reichenbach, Elisabetta Soldaini, Markus Nabholz, San Ming Wang, Philipp Bucher, Friedrich Beermann, and M. Pla

Subjects

Regulation of gene expression, Transcription, Genetic, Immunology, Receptors, Interleukin-2, Hematology, Biology, Regulatory Sequences, Nucleic Acid, Cell biology, Mice, Gene Expression Regulation, Transcription (biology), Immunology and Allergy, Animals, Cis-regulatory element

Abstract

Note: Swiss Institute of Experimental Cancer Research (ISREC), Epalinges, Switzerland. Reference GR-BUCHER-ARTICLE-1995-003 Record created on 2007-12-17, modified on 2017-05-12

Published

1995

30. Interleukins (IL)-1 and IL-2 control IL-2 receptor alpha and beta expression in immature thymocytes

Author

H R MacDonald, Patrick Reichenbach, Anne Wilson, Markus Nabholz, and Patricia Corthesy

Subjects

Interleukin 2, medicine.medical_specialty, medicine.medical_treatment, Cellular differentiation, Immunology, Alpha (ethology), Thymus Gland, Biology, Mice, Cell surface receptor, T-Lymphocyte Subsets, Internal medicine, medicine, Immunology and Allergy, Animals, RNA, Messenger, Autocrine signalling, Beta (finance), Cells, Cultured, In Situ Hybridization, Ionomycin, Receptors, Interleukin-2, Flow Cytometry, Cell biology, Mice, Inbred C57BL, Thymocyte, Cytokine, Endocrinology, Gene Expression Regulation, Interleukin-2, Tetradecanoylphorbol Acetate, Female, medicine.drug, Interleukin-1

Abstract

Functional high-affinity interleukin-2 receptors (IL-2R) contain three transmembrane proteins, IL-2R alpha, beta and gamma. We have investigated the expression of IL-2R alpha and beta genes in immature mouse thymocytes. Previous work has shown that during differentiation these cells transiently express IL-2R alpha on their surface. Stimulation of IL-2R alpha+ and IL-2R alpha- immature thymocytes with phorbol 12-myristate 13-acetate and calcium ionophore induces synthesis of IL-2R alpha and IL-2R beta mRNA. Most of this response depends on autocrine stimulation by IL-2. IL-1 synergizes with IL-2 to induce a 120-fold increase in IL-2R alpha mRNA and a 14-fold increase in IL-2R beta mRNA levels. A large proportion of the stimulated cells contains both transcripts. These interleukins do not induce any differentiation to more mature phenotypes. Collectively, these results show that IL-2 plays a major role in the regulation of IL-2R expression in normal immature thymocyte. We suggest that this response to interleukins may be part of a homeostatic mechanism to increase the production of immature thymocytes during stress.

Published

1994

31. A PCR-based assay for reporter gene expression

Author

Markus Nabholz, San Ming Wang, Peter Sperisen, and Patrick Reichenbach

Subjects

Reporter gene, Messenger RNA, Base Sequence, Molecular Sequence Data, Gene Expression, GUS reporter system, DNA, Biology, Transfection, Molecular biology, Polymerase Chain Reaction, Sensitivity and Specificity, Globins, Exon, Complementary DNA, Gene expression, Genetics, Animals, Luciferase, RNA, Messenger, Rabbits, Chromosome Deletion, Gene, Genetics (clinical), Plasmids

Abstract

Transient transfection is a widely used tool for the identification of cis-acting regulatory elements. These elements are detected by their effect on the expression of a reporter gene, which is quantified by measuring the reporter gene product in the form of mRNA, protein (hGH), or enzymes (CAT, luciferase). Measurements of mRNA levels have several advantages over enzyme or protein assays. However, mRNA quantification by RNase protection or S1 mapping has considerably lower signal-to-background ratio than protein assays and is therefore less sensitive. In this paper we report the development of a system that takes advantage of the polymerase chain reaction (PCR) to quantify rabbit beta-globin reporter gene expression. Cells are co-transfected with constructs whose activity is to be tested and a reference plasmid with a small deletion in the second exon of the beta-globin gene. We show that the ratio of the two amplified cDNA signals is a highly reliable measure of test gene expression. The sensitivity of this assay is at least 1000-fold higher than RNase protection.

Published

1992

32. Telomerase and telomeric repeat containing RNA at chromosome ends

Author

S. Redon, A. Panza, K. Sikora, Gaël Cristofari, M. Chang, Patrick Reichenbach, C. Azzalin, V. Machluf, B. Luke, and Joachim Lingner

Subjects

Genetics, Cancer Research, Telomerase, Telomeric repeat-containing RNAs, Oncology, Web of science, Chromosome, Biology, Molecular biology

Abstract

Reference EPFL-CONF-160760View record in Web of Science Record created on 2010-11-30, modified on 2017-05-12

Published

2008

33. Mouse IL-2Rα gene regulation by IL-1 and IL-2

Author

C. Rusterholz, Patrick Reichenbach, Elisabetta Soldaini, P. Corthesy, Peter Sperisen, Anne Wilson, F. Beermann, M. Nabholz, San Ming Wang, and M. Pla

Subjects

Regulation of gene expression, Immunology, Immunology and Allergy, Hematology, Biology, RBBP7, Molecular Biology, Biochemistry, Cell biology

Published

1994

34. Azole-Based Indoleamine 2,3-Dioxygenase 1 (IDO1) Inhibitors

Author

Ute F. Röhrig, Vincent Zoete, Olivier Michielin, Nahzli Dilek, Kelly Ascencao, Patrick Reichenbach, Florence Pojer, Melita Irving, Pierre Vogel, George Coukos, Somi Reddy Majjigapu, and Aline Reynaud

Subjects

Azoles, Kynurenine pathway, Heme binding, Quantitative Structure-Activity Relationship, Molecular Dynamics Simulation, 01 natural sciences, imidazole, 03 medical and health sciences, chemistry.chemical_compound, Drug Discovery, Humans, Indoleamine-Pyrrole 2,3,-Dioxygenase, Enzyme Inhibitors, Indoleamine 2,3-dioxygenase, Heme, 030304 developmental biology, chemistry.chemical_classification, 0303 health sciences, Molecular Structure, Orders of magnitude (mass), 0104 chemical sciences, 010404 medicinal & biomolecular chemistry, HEK293 Cells, Enzyme, chemistry, Biochemistry, Molecular Medicine, Azole, Function (biology), Protein Binding

Abstract

The heme enzyme indoleamine 2,3-dioxygenase 1 (IDO1) plays an essential role in immunity, neuronal function, and aging through catalysis of the rate-limiting step in the kynurenine pathway of tryptophan metabolism. Many IDO1 inhibitors with different chemotypes have been developed, mainly targeted for use in anti-cancer immunotherapy. Lead optimization of direct heme iron-binding inhibitors has proven difficult due to the remarkable selectivity and sensitivity of the heme-ligand interactions. Here, we present experimental data for a set of closely related small azole compounds with more than 4 orders of magnitude differences in their inhibitory activities, ranging from millimolar to nanomolar levels. We investigate and rationalize their activities based on structural data, molecular dynamics simulations, and density functional theory calculations. Our results not only expand the presently known four confirmed chemotypes of sub-micromolar heme binding IDO1 inhibitors by two additional scaffolds but also provide a model to predict the activities of novel scaffolds.

35. Characterization of a new tissue-specific transcription factor binding to the simian virus 40 enhancer TC-II (NF-kappa B) element

Author

P Baeuerle, Markus Nabholz, A L Lattion, Alain Israël, N R Rice, Enric Espel, Philipp Bucher, C. Fromental, and Patrick Reichenbach

Subjects

Lymphocyte, Cellular differentiation, Molecular Sequence Data, Simian virus 40, Biology, Proto-Oncogene Proteins, Consensus Sequence, Consensus sequence, medicine, Animals, Humans, Lymphocytes, Binding site, Enhancer, Transcription factor, Molecular Biology, Binding Sites, Base Sequence, NF-kappa B, food and beverages, Cell Differentiation, DNA, Cell Biology, NFKB1, Molecular biology, Proto-Oncogene Proteins c-rel, medicine.anatomical_structure, Enhancer Elements, Genetic, Chromatography, Gel, Research Article, Transcription Factors

Abstract

We have biochemically and functionally characterized a new transcription factor, NP-TCII, which is present in nuclei from unstimulated T and B lymphocytes but is not found in nonhematopoietic cells. This factor has a DNA-binding specificity similar to that of NF-kappa B but is unrelated to this or other Rel proteins by functional and biochemical criteria. It can also be distinguished from other previously described lymphocyte-specific DNA-binding proteins.

36. A computationally designed chimeric antigen receptor provides a small-molecule safety switch for T-cell therapy

Author

Sabrina Vollers, Melita Irving, Patrick Reichenbach, Byung-Ha Oh, Angel De Jesus Corria Osorio, Greta Giordano-Attianese, George Coukos, Bruno E. Correia, Mi Jeong Kwak, Sailan Shui, Jaume Bonet, Seong Hoon Kim, Pablo Gainza, Elisabetta Cribioli, and Elise Gray-Gaillard

Subjects

binding, T-Lymphocytes, T cell, Receptors, Antigen, T-Cell, Biomedical Engineering, Bioengineering, Plasma protein binding, system, Lymphocyte Activation, Protein Engineering, b-cell, Immunotherapy, Adoptive, Applied Microbiology and Biotechnology, Jurkat cells, Small Molecule Libraries, Jurkat Cells, 03 medical and health sciences, 0302 clinical medicine, Antigen, medicine, Humans, Cell Engineering, Cells, Cultured, B cell, 030304 developmental biology, 0303 health sciences, Receptors, Chimeric Antigen, prostate, Chemistry, Protein engineering, Chimeric antigen receptor, bh3-only proteins, 3. Good health, Cell biology, inhibitor, medicine.anatomical_structure, PC-3 Cells, Molecular Medicine, Protein Multimerization, Signal transduction, membrane antigen, 030217 neurology & neurosurgery, Protein Binding, Signal Transduction, Biotechnology

Abstract

The activity of CAR-T cells is reversibly halted with a small-molecule drug. Approaches to increase the activity of chimeric antigen receptor (CAR)-T cells against solid tumors may also increase the risk of toxicity and other side effects. To improve the safety of CAR-T-cell therapy, we computationally designed a chemically disruptable heterodimer (CDH) based on the binding of two human proteins. The CDH self-assembles, can be disrupted by a small-molecule drug and has a high-affinity protein interface with minimal amino acid deviation from wild-type human proteins. We incorporated the CDH into a synthetic heterodimeric CAR, called STOP-CAR, that has an antigen-recognition chain and a CD3 zeta- and CD28-containing endodomain signaling chain. We tested STOP-CAR-T cells specific for two antigens in vitro and in vivo and found similar antitumor activity compared to second-generation (2G) CAR-T cells. Timed administration of the small-molecule drug dynamically inactivated the activity of STOP-CAR-T cells. Our work highlights the potential for structure-based design to add controllable elements to synthetic cellular therapies.

37. Structure-based optimization of type III indoleamine 2,3-dioxygenase 1 (IDO1) inhibitors

Author

Ute F. Röhrig, Somi Reddy Majjigapu, Pierre Vogel, Aline Reynaud, Florence Pojer, Nahzli Dilek, Patrick Reichenbach, Kelly Ascenção, Melita Irving, George Coukos, Olivier Michielin, and Vincent Zoete

Subjects

Pharmacology, cancer immunotherapy, tryptophan degradation, biological evaluation, rational design, General Medicine, Heme, Triazoles, highly potent, Enzyme Inhibitors/chemistry, Enzyme Inhibitors/pharmacology, Indoleamine-Pyrrole 2,3,-Dioxygenase, Triazoles/chemistry, Triazoles/pharmacology, Cancer immunotherapy, X-ray crystallography, structure-based drug design, tryptophan metabolism, Drug Discovery, Enzyme Inhibitors, imidazoleisoindole derivatives, protein, potent inhibitors, x-ray crystallography, discovery, cycloaddition, crystal-structures

Abstract

The haem enzyme indoleamine 2,3-dioxygenase 1 (IDO1) catalyses the rate-limiting step in the kynurenine pathway of tryptophan metabolism and plays an essential role in immunity, neuronal function, and ageing. Expression of IDO1 in cancer cells results in the suppression of an immune response, and therefore IDO1 inhibitors have been developed for use in anti-cancer immunotherapy. Here, we report an extension of our previously described highly efficient haem-binding 1,2,3-triazole and 1,2,4-triazole inhibitor series, the best compound having both enzymatic and cellular IC 50 values of 34 nM. We provide enzymatic inhibition data for almost 100 new compounds and X-ray diffraction data for one compound in complex with IDO1. Structural and computational studies explain the dramatic drop in activity upon extension to pocket B, which has been observed in diverse haem-binding inhibitor scaffolds. Our data provides important insights for future IDO1 inhibitor design.