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377 results on '"Benkirane, Monsef"'

1. FHL1 is a key player of chikungunya virus tropism and pathogenesis

Author

Meertens, Laurent, Hafirassou, Mohamed Lamine, Couderc, Thérèse, Bonnet-Madin, Lucie, Kril, Vasiliya, Kümmerer, Beate M., Labeau, Athena, Brugier, Alexis, Simon-Loriere, Etienne, Burlaud-Gaillard, Julien, Doyen, Cécile, Pezzi, Laura, Goupil, Thibaud, Rafasse, Sophia, Vidalain, Pierre-Olivier, Legout, Anne Bertrand, Gueneau, Lucie, Juntas-Morales, Raul, Yaou, Rabah Ben, Bonne, Gisèle, de Lamballerie, Xavier, Benkirane, Monsef, Roingeard, Philippe, Delaugerre, Constance, Lecuit, Marc, and Amara, Ali

Subjects
Chikungunya, Four and a Half LIM domains 1 Tropism, Pathogenesis, Virus infection, Biology (General), QH301-705.5
Abstract

Chikungunya is an infectious disease caused by the chikungunya virus (CHIKV), an alphavirus transmitted to humans by Aedes mosquitoes, and for which there is no licensed vaccine nor antiviral treatments. By using a loss-of-function genetic screen, we have recently identified the FHL1 protein as an essential host factor for CHIKV tropism and pathogenesis. FHL1 is highly expressed in muscles cells and fibroblasts, the main CHIKV-target cells. FHL1 interacts with the viral protein nsP3 and plays a critical role in CHIKV genome amplification. Experiments in vivo performed in FHL1-deficient mice have shown that these animals are resistant to infection and do not develop muscular lesions. Altogether these observations, published in the journal Nature [1], show that FHL1 is a key host factor for CHIKV pathogenesis and identify the interaction between FHL1 and nsP3 as a promising target for the development of new antiviral strategies.

Published
2021
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4. International AIDS Society global scientific strategy: towards an HIV cure 2016

Author

Deeks, Steven G, Lewin, Sharon R, Ross, Anna Laura, Ananworanich, Jintanat, Benkirane, Monsef, Cannon, Paula, Chomont, Nicolas, Douek, Daniel, Lifson, Jeffrey D, Lo, Ying-Ru, Kuritzkes, Daniel, Margolis, David, Mellors, John, Persaud, Deborah, Tucker, Joseph D, Barre-Sinoussi, Françoise, Alter, Galit, Auerbach, Judith, Autran, Brigitte, Barouch, Dan H, Behrens, Georg, Cavazzana, Marina, Chen, Zhiwei, Cohen, Éric A, Corbelli, Giulio Maria, Eholié, Serge, Eyal, Nir, Fidler, Sarah, Garcia, Laurindo, Grossman, Cynthia, Henderson, Gail, Henrich, Timothy J, Jefferys, Richard, Kiem, Hans-Peter, McCune, Joseph, Moodley, Keymanthri, Newman, Peter A, Nijhuis, Monique, Nsubuga, Moses Supercharger, Ott, Melanie, Palmer, Sarah, Richman, Douglas, Saez-Cirion, Asier, Sharp, Matthew, Siliciano, Janet, Silvestri, Guido, Singh, Jerome, Spire, Bruno, Taylor, Jeffrey, Tolstrup, Martin, Valente, Susana, van Lunzen, Jan, Walensky, Rochelle, Wilson, Ira, and Zack, Jerome

Subjects
Medical Microbiology, Biomedical and Clinical Sciences, Immunology, Good Health and Well Being, Acquired Immunodeficiency Syndrome, Goals, HIV Infections, Humans, International Cooperation, Organizational Objectives, Research, Societies, Medical, International AIDS Society Towards a Cure Working Group, Medical and Health Sciences, Biomedical and clinical sciences, Health sciences
Abstract

Antiretroviral therapy is not curative. Given the challenges in providing lifelong therapy to a global population of more than 35 million people living with HIV, there is intense interest in developing a cure for HIV infection. The International AIDS Society convened a group of international experts to develop a scientific strategy for research towards an HIV cure. This Perspective summarizes the group's strategy.

Published
2016

5. Hair follicle stem cell replication stress drives IFI16/STING-dependent inflammation in hidradenitis suppurativa

Author

Orvain, Cindy, Lin, Yea-Lih, Jean-Louis, Francette, Hocini, Hakim, Hersant, Barbara, Bennasser, Yamina, Ortonne, Nicolas, Hotz, Claire, Wolkenstein, Pierre, Boniotto, Michele, Tisserand, Pascaline, Lefebvre, Cecile, Lelievre, Jean-Daniel, Benkirane, Monsef, Pasero, Philippe, Levy, Yves, and Hue, Sophie

Subjects
Thermo Fisher Scientific Inc., Skin diseases -- Development and progression, Inflammation -- Development and progression, Skin -- Analysis, Stem cells -- Analysis, Scientific equipment industry -- Analysis, Health care industry
Abstract

Hidradenitis suppurativa (HS) is a chronic, relapsing, inflammatory skin disease. HS appears to be a primary abnormality in the pilosebaceous-apocrine unit. In this work, we characterized hair follicle stem cells (HFSCs) isolated from HS patients and more precisely the outer root sheath cells (ORSCs). We showed that hair follicle cells from HS patients had an increased number of proliferating progenitor cells and lost quiescent stem cells. Remarkably, we also showed that the progression of replication forks was altered in ORSCs from hair follicles of HS patients, leading to activation of the ATR/CHK1 pathway. These alterations were associated with an increased number of micronuclei and with the presence of cytoplasmic ssDNA, leading to the activation of the IFI16/STING pathway and the production of type I IFNs. This mechanistic analysis of the etiology of HS in the HFSC compartment establishes a formal link between genetic predisposition and skin inflammation observed in HS., Introduction Hidradenitis suppurativa (HS) is a chronic, relapsing, inflammatory skin disease characterized by double comedones; painful, deep, recurrent nodules; and abscesses. It is also known as acne inversa, since it [...]

Published
2020
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7. FHL1 is a major host factor for chikungunya virus infection

Author

Meertens, Laurent, Hafirassou, Mohamed Lamine, Couderc, Thérèse, Bonnet-Madin, Lucie, Kril, Vasiliya, Kümmerer, Beate M., Labeau, Athena, Brugier, Alexis, Simon-Loriere, Etienne, Burlaud-Gaillard, Julien, Doyen, Cécile, Pezzi, Laura, Goupil, Thibaud, Rafasse, Sophia, Vidalain, Pierre-Olivier, Bertrand-Legout, Anne, Gueneau, Lucie, Juntas-Morales, Raul, Ben Yaou, Rabah, Bonne, Gisèle, de Lamballerie, Xavier, Benkirane, Monsef, Roingeard, Philippe, Delaugerre, Constance, Lecuit, Marc, and Amara, Ali

Published
2019
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9. Combined direct/indirect detection allows identification of DNA termini in diverse sequencing datasets and supports a multiple-initiation-site model for HIV plus-strand synthesis

Author

Wang, William, Artiles, Karen L., Machida, Shinichi, Benkirane, Monsef, Jain, Nimit, and Fire, Andrew Z.

Subjects
Article
Abstract

Replication of genetic material involves the creation of characteristic termini. Determining these termini is important to refine our understanding of the mechanisms involved in maintaining the genomes of cellular organisms and viruses. Here we describe a computational approach combining direct and indirect readouts to detect termini from next-generation short-read sequencing. While a direct inference of termini can come from mapping the most prominent start positions of captured DNA fragments, this approach is insufficient in cases where the DNA termini are not captured, whether for biological or technical reasons. Thus, a complementary (indirect) approach to terminus detection can be applied, taking advantage of the imbalance in coverage between forward and reverse sequence reads near termini. A resulting metric (“strand bias”) can be used to detect termini even where termini are naturally blocked from capture or ends are not captured during library preparation (e.g., in tagmentation-based protocols). Applying this analysis to datasets where known DNA termini are present, such as from linear double-stranded viral genomes, yielded distinct strand bias signals corresponding to these termini. To evaluate the potential to analyze a more complex situation, we applied the analysis to examine DNA termini present early after HIV infection in a cell culture model. We observed both the known termini expected based on standard models of HIV reverse transcription (the U5-right-end and U3-left-end termini) as well as a signal corresponding to a previously described additional initiation site for plus-strand synthesis (cPPT [central polypurine tract]). Interestingly, we also detected putative terminus signals at additional sites. The strongest of these are a set that share several characteristics with the previously characterized plus-strand initiation sites (the cPPT and 3’ PPT [polypurine tract] sites): (i) an observed spike in directly captured cDNA ends, an indirect terminus signal evident in localized strand bias, (iii) a preference for location on the plus-strand, (iv) an upstream purine-rich motif, and (v) a decrease in terminus signal at late time points after infection. These characteristics are consistent in duplicate samples in two different genotypes (wild type and integrase-lacking HIV). The observation of distinct internal termini associated with multiple purine-rich regions raises a possibility that multiple internal initiations of plus-strand synthesis might contribute to HIV replication.

Published
2023

10. SAMHD1 acts at stalled replication forks to prevent interferon induction

Author

Coquel, Flavie, Silva, Maria-Joao, Técher, Hervé, Zadorozhny, Karina, Sharma, Sushma, Nieminuszczy, Jadwiga, Mettling, Clément, Dardillac, Elodie, Barthe, Antoine, Schmitz, Anne-Lyne, Promonet, Alexy, Cribier, Alexandra, Sarrazin, Amélie, Niedzwiedz, Wojciech, Lopez, Bernard, Costanzo, Vincenzo, Krejci, Lumir, Chabes, Andrei, Benkirane, Monsef, Lin, Yea-Lih, and Pasero, Philippe

Published
2018
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11. A trip down memory lane with Retrovirology

Author

Benkirane, Monsef, Berkhout, Ben, Borrow, Persephone, Fassati, Ariberto, Fujii, Masahiro, Garcia-Martinez, J. Victor, Margolis, D., Nijhuis, Monique, Parent, Leslie, Strebel, Klaus, Venter, François, Kirchhoff, Frank, Lever, Andrew, Ross, Susan, and Mak, Johnson

Published
2019
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15. SAMHD1 is mutated recurrently in chronic lymphocytic leukemia and is involved in response to DNA damage

Author

Clifford, Ruth, Louis, Tania, Robbe, Pauline, Ackroyd, Sam, Burns, Adam, Timbs, Adele T., Wright Colopy, Glen, Dreau, Helene, Sigaux, Francois, Judde, Jean Gabriel, Rotger, Margalida, Telenti, Amalio, Lin, Yea-Lih, Pasero, Philippe, Maelfait, Jonathan, Titsias, Michalis, Cohen, Dena R., Henderson, Shirley J., Ross, Mark T., Bentley, David, Hillmen, Peter, Pettitt, Andrew, Rehwinkel, Jan, Knight, Samantha J.L., Taylor, Jenny C., Crow, Yanick J., Benkirane, Monsef, and Schuh, Anna

Published
2014
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23. Towards an HBV cure: state-of-the-art and unresolved questions—report of the ANRS workshop on HBV cure

Author

Zeisel, Mirjam B, Lucifora, Julie, Mason, William S, Sureau, Camille, Beck, Jürgen, Levrero, Massimo, Kann, Michael, Knolle, Percy A, Benkirane, Monsef, Durantel, David, Michel, Marie-Louise, Autran, Brigitte, Cosset, François-Loïc, Strick-Marchand, Hélène, Trépo, Christian, Kao, Jia-Horng, Carrat, Fabrice, Lacombe, Karine, Schinazi, Raymond F, Barré-Sinoussi, Françoise, Delfraissy, Jean-François, and Zoulim, Fabien

Published
2015
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24. SAMHD1 is the dendritic- and myeloid-cell-specific HIV-1 restriction factor counteracted by Vpx

Author

Laguette, Nadine, Sobhian, Bijan, Casartelli, Nicoletta, Ringeard, Mathieu, Chable-Bessia, Christine, Segeral, Emmanuel, Yatim, Ahmad, Emiliani, Stephane, Schwartz, Olivier, and Benkirane, Monsef

Subjects
Dendritic cells -- Physiological aspects -- Research, HIV infection -- Diagnosis -- Research, Environmental issues, Science and technology, Zoology and wildlife conservation
Abstract

The primate lentivirus auxiliary protein Vpx counteracts an unknown restriction factor that renders human dendritic and myeloid cells largely refractory to HIV-1 infection (1-6). Here we identify SAMHD1 as this restriction factor. SAMHD1 is a protein involved in Aicardi-Goutieres syndrome, a genetic encephalopathy with symptoms mimicking congenital viral infection, that has been proposed to act as a negative regulator of the interferon response (7). We show that Vpx induces proteasomal degradation of SAMHD1. Silencing of SAMHD1 in non-permissive cell lines alleviates HIV-1 restriction and is associated with a significant accumulation of viral DNA in infected cells. Concurrently, overexpression of SAMHD1 in sensitive cells inhibits HIV-1 infection. The putative phosphohydrolase activity of SAMHD1 is probably required for HIV-1 restriction. Vpx-mediated relief of restriction is abolished in SAMHD1-negative cells. Finally, silencing of SAMHD1 markedly increases the susceptibility of monocytic-derived dendritic cells to infection. Our results demonstrate that SAMHD1 is an antiretroviral protein expressed in cells of the myeloid lineage that inhibits an early step of the viral life cycle., Most monocytic cell lines fail to recapitulate the HIV-1 restriction phenotype that is witnessed in primary dendritic cells and to a lesser extent in macrophages. One exception is represented by [...]

Published
2011
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33. SAMHD1 phosphorylation and cytoplasmic relocalization after human cytomegalovirus infection limits its antiviral activity

Author

De Meo, Simone, primary, Dell’Oste, Valentina, additional, Molfetta, Rosa, additional, Tassinari, Valentina, additional, Lotti, Lavinia Vittoria, additional, Vespa, Simone, additional, Pignoloni, Benedetta, additional, Covino, Daniela Angela, additional, Fantuzzi, Laura, additional, Bona, Roberta, additional, Zingoni, Alessandra, additional, Nardone, Ilaria, additional, Biolatti, Matteo, additional, Coscia, Alessandra, additional, Paolini, Rossella, additional, Benkirane, Monsef, additional, Edfors, Fredrik, additional, Sandalova, Tatyana, additional, Achour, Adnane, additional, Hiscott, John, additional, Landolfo, Santo, additional, Santoni, Angela, additional, and Cerboni, Cristina, additional

Published
2020
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35. SAMHD1 enhances chikungunya and zika virus replication in human skin fibroblasts

Author

Wichit, Sineewanlaya, Hamel, Rodolphe, Zanzoni, Andreas, Diop, Fode, Cribier, Alexandra, Talignani, Loïc, Diack, Abibatou, Ferraris, Pauline, Liegeois, Florian, Urbach, Serge, Ekchariyawat, Peeraya, Merits, Andres, Yssel, Hans, Benkirane, Monsef, Missé, Dorothée, Mahidol University [Bangkok], Interhuman Arbovirus Transmission (MIVEGEC-iHAT), Biologie des infections virales: Emergence, DIFfusion, Impact, Contrôle, Elimination (EDIFICE), Maladies infectieuses et vecteurs : écologie, génétique, évolution et contrôle (MIVEGEC), Université de Montpellier (UM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche pour le Développement (IRD [France-Sud])-Université de Montpellier (UM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche pour le Développement (IRD [France-Sud])-Maladies infectieuses et vecteurs : écologie, génétique, évolution et contrôle (MIVEGEC), Université de Montpellier (UM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche pour le Développement (IRD [France-Sud])-Université de Montpellier (UM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche pour le Développement (IRD [France-Sud]), Theories and Approaches of Genomic Complexity (TAGC), Aix Marseille Université (AMU)-Institut National de la Santé et de la Recherche Médicale (INSERM), Université de Montpellier (UM)-Centre National de la Recherche Scientifique (CNRS)-Institut de Recherche pour le Développement (IRD [France-Sud]), Institut de génétique humaine (IGH), Université de Montpellier (UM)-Centre National de la Recherche Scientifique (CNRS), Virostyle (MIVEGEC-Virostyle), Perturbations, Evolution, Virulence (PEV), Zoonoses virales et MTN (MIVEGEC-VIROZ), Institut de Génomique Fonctionnelle (IGF), Université de Montpellier (UM)-Université Montpellier 1 (UM1)-Institut National de la Santé et de la Recherche Médicale (INSERM)-Université Montpellier 2 - Sciences et Techniques (UM2)-Centre National de la Recherche Scientifique (CNRS), University of Tartu, Centre d'Immunologie et de Maladies Infectieuses (CIMI), Institut National de la Santé et de la Recherche Médicale (INSERM)-Sorbonne Université (SU)-Centre National de la Recherche Scientifique (CNRS), ANR-14-CE14-0029,TIMTAMDEN,Rôle des récepteurs TIM et TAM dans l'infection des cellules cibles par le virus de la dengue(2014), ANR-16-IDEX-0006,MUSE,MUSE(2016), European Project: 734548,ZIKAlliance(2016), Institut National de la Santé et de la Recherche Médicale (INSERM)-Université de Montpellier (UM)-Centre National de la Recherche Scientifique (CNRS), and Centre d'Immunologie et des Maladies Infectieuses (CIMI)

Subjects
viruses, Virus Replication, SILAC, Article, Cell Line, SAM Domain and HD Domain-Containing Protein 1, lcsh:Chemistry, Zika, [SDV.MHEP.MI]Life Sciences [q-bio]/Human health and pathology/Infectious diseases, Humans, [SDV.BBM]Life Sciences [q-bio]/Biochemistry, Molecular Biology, Viral Regulatory and Accessory Proteins, Protein Interaction Maps, lcsh:QH301-705.5, Skin, [SDV.MHEP.ME]Life Sciences [q-bio]/Human health and pathology/Emerging diseases, Zika Virus Infection, IFIT, virus diseases, Molecular Sequence Annotation, Zika Virus, Fibroblasts, SAMHD1, Up-Regulation, arbovirus, lcsh:Biology (General), lcsh:QD1-999, Proteolysis, Chikungunya Fever, Chikungunya, Chikungunya virus
Abstract

International audience; Chikungunya virus (CHIKV) and Zika virus (ZIKV) are emerging arboviruses that pose a worldwide threat to human health. Currently, neither vaccine nor antiviral treatment to control their infections is available. As the skin is a major viral entry site for arboviruses in the human host, we determined the global proteomic profile of CHIKV and ZIKV infections in human skin fibroblasts using Stable Isotope Labelling by Amino acids in Cell culture (SILAC)-based mass-spectrometry analysis. We show that the expression of the interferon-stimulated proteins MX1, IFIT1, IFIT3 and ISG15, as well as expression of defense response proteins DDX58, STAT1, OAS3, EIF2AK2 and SAMHD1 was significantly up-regulated in these cells upon infection with either virus. Exogenous expression of IFITs proteins markedly inhibited CHIKV and ZIKV replication which, accordingly, was restored following the abrogation of IFIT1 or IFIT3. Overexpression of SAMHD1 in cutaneous cells, or pretreatment of cells with the virus-like particles containing SAMHD1 restriction factor Vpx, resulted in a strong increase or inhibition, respectively, of both CHIKV and ZIKV replication. Moreover, silencing of SAMHD1 by specific SAMHD1-siRNA resulted in a marked decrease of viral RNA levels. Together, these results suggest that IFITs are involved in the restriction of replication of CHIKV and ZIKV and provide, as yet unreported, evidence for a proviral role of SAMHD1 in arbovirus infection of human skin cells.

Published
2019

37. Publisher Correction: LifeTime and improving European healthcare through cell-based interceptive medicine

Author

Rajewsky, Nikolaus, Almouzni, Geneviève, Clevers, Hans, Heutink, Peter, Heymans, Stephane R B, Heyn, Holger, Huch, Meritxell, Huitinga, Inge, Jackowiak, Paulina, Jongsma, Karin R, Journot, Laurent, Junker, Jan Philipp, Katz, Shauna, De Strooper, Bart, Kehren, Jeanne, Kempa, Stefan, Kirchhof, Paulus, Klein, Christine, Koralewska, Natalia, Korbel, Jan O, Kühnemund, Malte, Lamond, Angus I, Lauwers, Elsa, Le Ber, Isabelle, Eggert, Angelika, Leinonen, Ville, López-Tobón, Alejandro, Lundberg, Emma, Lunkes, Astrid, Maatz, Henrike, Mann, Matthias, Marelli, Luca, Matser, Vera, Matthews, Paul M, Mechta-Grigoriou, Fatima, Ellenberg, Jan, Menon, Radhika, Nielsen, Anne F, Pagani, Massimiliano, Pasterkamp, R Jeroen, Pitkänen, Asla, Popescu, Valentin, Pottier, Cyril, Puisieux, Alain, Rademakers, Rosa, Reiling, Dory, Fernández, Xosé M, Reiner, Orly, Remondini, Daniel, Ritchie, Craig, Rohrer, Jonathan D, Saliba, Antoine-Emmanuel, Sanchez-Valle, Raquel, Santosuosso, Amedeo, Sauter, Arnold, Scheltema, Richard A, Scheltens, Philip, Figlerowicz, Marek, Schiller, Herbert B, Schneider, Anja, Seibler, Philip, Sheehan-Rooney, Kelly, Shields, David J, Sleegers, Kristel, Smit, August B, Smith, Kenneth G C, Smolders, Ilse, Synofzik, Matthis, Gasser, Susan M, Tam, Wai Long, Teichmann, Sarah A, Thom, Maria, Turco, Margherita Y, van Beusekom, Heleen M M, Vandenberghe, Rik, Van den Hoecke, Silvie, van de Poel, Ibo, van der Ven, Andre, van der Zee, Julie, Hubner, Norbert, van Lunzen, Jan, van Minnebruggen, Geert, van Oudenaarden, Alexander, Van Paesschen, Wim, van Swieten, John C, van Vught, Remko, Verhage, Matthijs, Verstreken, Patrik, Villa, Carlo Emanuele, Vogel, Jörg, Kjems, Jørgen, von Kalle, Christof, Walter, Jörn, Weckhuysen, Sarah, Weichert, Wilko, Wood, Louisa, Ziegler, Anette-Gabriele, Zipp, Frauke, Knoblich, Jürgen A, Gorski, Stanislaw A, Krabbe, Grietje, Lichter, Peter, Linnarsson, Sten, Marine, Jean-Christophe, Marioni, John C, Marti-Renom, Marc A, Netea, Mihai G, Nickel, Dörthe, Nollmann, Marcelo, Novak, Halina R, Aerts, Stein, Parkinson, Helen, Piccolo, Stefano, Pinheiro, Inês, Pombo, Ana, Popp, Christian, Reik, Wolf, Roman-Roman, Sergio, Rosenstiel, Philip, Schultze, Joachim L, Stegle, Oliver, Amit, Ido, Tanay, Amos, Testa, Giuseppe, Thanos, Dimitris, Theis, Fabian J, Torres-Padilla, Maria-Elena, Valencia, Alfonso, Vallot, Céline, Vidal, Marie, Voet, Thierry, Bertero, Michela G, Groups, LifeTime Community Working, Alberi, Lavinia, Alexander, Stephanie, Alexandrov, Theodore, Arenas, Ernest, Bagni, Claudia, Balderas, Robert, Bandelli, Andrea, Becher, Burkhard, Becker, Matthias, Bock, Christoph, Beerenwinkel, Niko, Benkirane, Monsef, Beyer, Marc, Bickmore, Wendy A, Biessen, Erik E A L, Blomberg, Niklas, Blumcke, Ingmar, Bodenmiller, Bernd, Borroni, Barbara, Boumpas, Dimitrios T, Bredenoord, Annelien L, Bourgeron, Thomas, Bowers, Sarion, Braeken, Dries, Brooksbank, Catherine, Brose, Nils, Bruining, Hilgo, Bury, Jo, Caporale, Nicolo, Cattoretti, Giorgio, Chabane, Nadia, Cavalli, Giacomo, Chneiweiss, Hervé, Cook, Stuart A, Curatolo, Paolo, de Jonge, Marien I, Deplancke, Bart, de Witte, Peter, Dimmeler, Stefanie, Draganski, Bogdan, Drews, Anna, Chiocca, Susanna, Dumbrava, Costica, Engelhardt, Stefan, Gasser, Thomas, Giamarellos-Bourboulis, Evangelos J, Graff, Caroline, Grün, Dominic, Gut, Ivo G, Hansson, Oskar, Henshall, David C, and Herland, Anna

Subjects
Male, medicine.medical_specialty, Legislation, Medical, Cell- and Tissue-Based Therapy, MEDLINE, Diseases, Artificial Intelligence, Health care, Pathology, medicine, Humans, Medical physics, Multidisciplinary, Education, Medical, business.industry, Published Erratum, Publisher Correction, Europe, Early Diagnosis, Health, Medicine, Female, ddc:500, Single-Cell Analysis, Systems biology, business, Delivery of Health Care, Biomarkers, Cell based
Abstract

Here we describe the LifeTime Initiative, which aims to track, understand and target human cells during the onset and progression of complex diseases, and to analyse their response to therapy at single-cell resolution. This mission will be implemented through the development, integration and application of single-cell multi-omics and imaging, artificial intelligence and patient-derived experimental disease models during the progression from health to disease. The analysis of large molecular and clinical datasets will identify molecular mechanisms, create predictive computational models of disease progression, and reveal new drug targets and therapies. The timely detection and interception of disease embedded in an ethical and patient-centred vision will be achieved through interactions across academia, hospitals, patient associations, health data management systems and industry. The application of this strategy to key medical challenges in cancer, neurological and neuropsychiatric disorders, and infectious, chronic inflammatory and cardiovascular diseases at the single-cell level will usher in cell-based interceptive medicine in Europe over the next decade.

Published
2021

40. A trip down memory lane with Retrovirology

Author

MMB Research line 3a, Infection & Immunity, Benkirane, Monsef, Berkhout, Ben, Borrow, Persephone, Fassati, Ariberto, Fujii, Masahiro, Garcia-Martinez, J Victor, Margolis, D, Nijhuis, Monique, Parent, Leslie, Strebel, Klaus, Venter, François, Kirchhoff, Frank, Lever, Andrew, Ross, Susan, Mak, Johnson, MMB Research line 3a, Infection & Immunity, Benkirane, Monsef, Berkhout, Ben, Borrow, Persephone, Fassati, Ariberto, Fujii, Masahiro, Garcia-Martinez, J Victor, Margolis, D, Nijhuis, Monique, Parent, Leslie, Strebel, Klaus, Venter, François, Kirchhoff, Frank, Lever, Andrew, Ross, Susan, and Mak, Johnson

Published
2019

41. SAMHD1 restricts HIV-1 reverse transcription in quiescent CD4+ T-cells

Author

Descours Benjamin, Cribier Alexandra, Chable-Bessia Christine, Ayinde Diana, Rice Gillian, Crow Yanick, Yatim Ahmad, Schwartz Olivier, Laguette Nadine, and Benkirane Monsef

Subjects
SAMHD1, Quiescent CD4+ T-cell, HIV-1, Reverse transcription, Restriction, Immunologic diseases. Allergy, RC581-607
Abstract

Abstract Background Quiescent CD4+ T lymphocytes are highly refractory to HIV-1 infection due to a block at reverse transcription. Results Examination of SAMHD1 expression in peripheral blood lymphocytes shows that SAMHD1 is expressed in both CD4+ and CD8+ T cells at levels comparable to those found in myeloid cells. Treatment of CD4+ T cells with Virus-Like Particles (VLP) containing Vpx results in the loss of SAMHD1 expression that correlates with an increased permissiveness to HIV-1 infection and accumulation of reverse transcribed viral DNA without promoting transcription from the viral LTR. Importantly, CD4+ T-cells from patients with Aicardi-Goutières Syndrome harboring mutation in the SAMHD1 gene display an increased susceptibility to HIV-1 infection that is not further enhanced by VLP-Vpx-treatment. Conclusion Here, we identified SAMHD1 as the restriction factor preventing efficient viral DNA synthesis in non-cycling resting CD4+ T-cells. These results highlight the crucial role of SAMHD1 in mediating restriction of HIV-1 infection in quiescent CD4+ T-cells and could impact our understanding of HIV-1 mediated CD4+ T-cell depletion and establishment of the viral reservoir, two of the HIV/AIDS hallmarks.

Published
2012
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42. Role of SAMHD1 nuclear localization in restriction of HIV-1 and SIVmac

Author

Brandariz-Nuñez Alberto, Valle-Casuso Jose, White Tommy E, Laguette Nadine, Benkirane Monsef, Brojatsch Jurgen, and Diaz-Griffero Felipe

Subjects
SAMHD, Restriction, Nuclear localization, Vpx, HIV-1, SIV, Degradation, Immunologic diseases. Allergy, RC581-607
Abstract

Abstract Background SAMHD1 is a nuclear protein that blocks lentiviral infection before reverse transcription in macrophages and dendritic cells. The viral accessory protein Vpx overcomes the SAMHD1-mediated lentiviral block by inducing its proteasomal degradation. Results Here, we identified the nuclear localization signal (NLS) of SAMHD1, and studied its contribution to restriction of HIV-1 and SIVmac. By studying the cellular distribution of different SAMHD1 variants, we mapped the nuclear localization of SAMHD1 to residues 11KRPR14. Mutagenesis of these residues changed the cellular distribution of SAMHD1 from the nucleus to the cytoplasm. SAMHD1 mutants that lost nuclear localization restricted HIV-1 and SIV as potently as the wild type protein. Interestingly, SAMHD1 mutants that localized to the cytoplasm were not degraded by nuclear Vpx alleles. Therefore, nuclear Vpx alleles require nuclear localization of SAMHD1 in order to induce its degradation. In agreement, SIVmac viruses encoding Vpx did not overcome the restriction imposed by the cytoplasmic variants of SAMHD1. Conclusions We mapped the NLS of SAMHD1 to residues 11KRPR14 and studied the contribution of SAMHD1 nuclear localization to restriction of HIV-1 and SIV. These experiments demonstrate that cytoplasmic variants of SAMHD1 potently block lentiviral infection and are resistant to Vpx-mediated degradation. The nuclear Vpx alleles studied here are only capable of degrading a nuclearly localized SAMHD1 suggesting that Vpx-mediated degradation of SAMHD1 is initiated in the nucleus.

Published
2012
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44. Posttranscriptional Regulation of HIV-1 Gene Expression during Replication and Reactivation from Latency by Nuclear Matrix Protein MATR3

Author

Sarracino, Ambra, primary, Gharu, Lavina, additional, Kula, Anna, additional, Pasternak, Alexander O., additional, Avettand-Fenoel, Veronique, additional, Rouzioux, Christine, additional, Bardina, Maryana, additional, De Wit, Stéphane, additional, Benkirane, Monsef, additional, Berkhout, Ben, additional, Van Lint, Carine, additional, and Marcello, Alessandro, additional

Published
2018
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46. Suppression of HIV-1 replication by microRNA effectors

Author

Levy Yves, Reynes Jacques, Jacquet Jean-Marc, Wagschal Alexandre, Zamborlini Alessia, Robinson Robinson, Latreille Daniel, Meziane Oussama, Chable-Bessia Christine, Saib Ali, Bennasser Yamina, and Benkirane Monsef

Subjects
Immunologic diseases. Allergy, RC581-607
Abstract

Abstract The rate of HIV-1 gene expression is a key step that determines the kinetics of virus spread and AIDS progression. Viral entry and gene expression were described to be the key determinants for cell permissiveness to HIV. Recent reports highlighted the involvement of miRNA in regulating HIV-1 replication post-transcriptionally. In this study we explored the role of cellular factors required for miRNA-mediated mRNA translational inhibition in regulating HIV-1 gene expression. Here we show that HIV-1 mRNAs associate and co-localize with components of the RNA Induced Silencing Complex (RISC), and we characterize some of the proteins required for miRNA-mediated silencing (miRNA effectors). RCK/p54, GW182, LSm-1 and XRN1 negatively regulate HIV-1 gene expression by preventing viral mRNA association with polysomes. Interestingly, knockdown of RCK/p54 or DGCR8 resulted in virus reactivation in PBMCs isolated from HIV infected patients treated with suppressive HAART.

Published
2009
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47. Small non-coding RNAs, mammalian cells, and viruses: regulatory interactions?

Author

Benkirane Monsef, Jeang Kuan-Teh, and Yeung Man

Subjects
Immunologic diseases. Allergy, RC581-607
Abstract

Abstract Recent findings suggest that mammalian cells can use small non-coding RNAs (ncRNA) to regulate physiological viral infections. Here, we comment on several lines of evidence that support this concept. We discuss how viruses may in turn protect, suppress, evade, modulate, or adapt to the host cell's ncRNA regulatory schema.

Published
2007
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48. Posttranscriptional Regulation of HIV-1 Gene Expression during Replication and Reactivation from Latency by Nuclear Matrix Protein MATR3.

Author

Sarracino, Ambra, Gharu, Lavina, Kula, Anna, Pasternak, Alexander, Avettand-Fenoel, Veronique, Rouzioux, Christine, Bardina, Maryana, De Wit, Stéphane, Benkirane, Monsef, Berkhout, Ben, Van Lint, Carine, Marcello, Alessandro, Sarracino, Ambra, Gharu, Lavina, Kula, Anna, Pasternak, Alexander, Avettand-Fenoel, Veronique, Rouzioux, Christine, Bardina, Maryana, De Wit, Stéphane, Benkirane, Monsef, Berkhout, Ben, Van Lint, Carine, and Marcello, Alessandro

Abstract

Posttranscriptional regulation of HIV-1 replication is finely controlled by viral and host factors. Among the former, Rev controls the export of partially spliced and unspliced viral RNAs from the nucleus and their translation in the cytoplasm or incorporation into new virions as genomic viral RNA. To investigate the functional role of the Rev cofactor MATR3 in the context of HIV infection, we modulated its expression in Jurkat cells and primary peripheral blood lymphocytes (PBLs). We confirmed that MATR3 is a positive regulator of HIV-1 acting at a posttranscriptional level. By applying the same approach to J-lat cells, a well-established model for the study of HIV-1 latency, we observed that MATR3 depletion did not affect transcriptional reactivation of the integrated provirus, but caused a reduction of Gag production. Following these observations, we hypothesized that MATR3 could be involved in the establishment of HIV-1 posttranscriptional latency. Indeed, mechanisms acting at the posttranscriptional level have been greatly overlooked in favor of transcriptional pathways. MATR3 was almost undetectable in resting PBLs, but could be promptly upregulated upon cellular stimulation with PHA. However, HIV latency-reversing agents were poor inducers of MATR3 levels, providing a rationale for their inability to fully reactivate the virus. These data have been confirmed ex vivo in cells derived from patients under suppressive ART. Finally, in the context of MATR3-depleted J-lat cells, impaired reactivation by SAHA could be fully rescued by MATR3 reconstitution, demonstrating a direct role of MATR3 in the posttranscriptional regulation of HIV-1 latency.IMPORTANCE The life cycle of HIV-1 requires integration of a DNA copy into the genome of the host cell. Transcription of the viral genes generates RNAs that are exported to the cytoplasm with the contribution of viral and cellular factors to get translated or incorporated in the newly synthesized virions. It has been observ, SCOPUS: ar.j, info:eu-repo/semantics/published

Published
2018

49. Changes in microRNA expression profiles in HIV-1-transfected human cells

Author

Benkirane Monsef, Jiang Guojian, Myers Timothy G, Bennasser Yamina, Yeung Man Lung, and Jeang Kuan-Teh

Subjects
Immunologic diseases. Allergy, RC581-607
Abstract

Abstract MicroRNAs (miRNAs) are small RNAs of 18–25 nucleotides (nt) in length that play important roles in regulating a variety of biological processes. Recent studies suggest that cellular miRNAs may serve to control the replication of viruses in cells. If such is the case, viruses might be expected to evolve the ability to modulate the expression of cellular miRNAs. To ask if expression of HIV-1 genes changes the miRNA profiles in human cells, we employed a high throughput microarray method, termed the RNA-primed Array-based Klenow Enzyme (RAKE) assay. Here, we describe the optimization of this assay to quantify the expression of miRNAs in HIV-1 transfected human cells. We report distinct differences in miRNA profiles in mock-transfected HeLa cells versus HeLa cells transfected with an infectious HIV-1 molecular clone, pNL4-3.

Published
2005
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50. Exploring histone loading on HIV DNA reveals a dynamic nucleosome positioning between unintegrated and integrated viral genome.

Author

Shinichi Machida, Depierre, David, Heng-Chang Chen, Thenin-Houssier, Suzie, Petitjean, Gaël, Doyen, Cecile M., Motoki Takaku, Cuvier, Olivier, and Benkirane, Monsef

Subjects
VIRAL genomes, DNA, NUCLEAR DNA, HIV, HISTONES
Abstract

The aim of the present study was to understand the biology of unintegrated HIV-1 DNA and reveal the mechanisms involved in its transcriptional silencing. We found that histones are loaded on HIV-1 DNA after its nuclear import and before its integration in the host genome. Nucleosome positioning analysis along the unintegrated and integrated viral genomes revealed major differences in nucleosome density and position. Indeed, in addition to the wellknown nucleosomes Nuc0, Nuc1, and Nuc2 loaded on integrated HIV-1 DNA, we also found NucDHS, a nucleosome that covers the DNase hypersensitive site, in unintegrated viral DNA. In addition, unintegrated viral DNA-associated Nuc0 and Nuc2 were positioned slightly more to the 5' end relative to their position in integrated DNA. The presence of NucDHS in the proximal region of the long terminal repeat (LTR) promoter was associated with the absence of RNAPII and of the active histone marks H3K4me3 and H3ac at the LTR. Conversely, analysis of integrated HIV-1 DNA showed a loss of NucDHS, loading of RNAPII, and enrichment in active histone marks within the LTR. We propose that unintegrated HIV-1 DNA adopts a repressive chromatin structure that competes with the transcription machinery, leading to its silencing. [ABSTRACT FROM AUTHOR]

Published
2020
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