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59 research outputs found

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Using Genome Editing to Engineer Universal Platelets

Author: Ghevaert Cedric
Lawrence Moyra
Mueller Annett
Publication venue: Emerging Topics in Life Sciences
Publication date: 31/05/2019
Field of study

Genome editing technologies such as Zinc Finger nucleases, TALENS and CRISPR/Cas9 have recently emerged as tools with the potential to revolutionise cellular therapy. This is particularly exciting for the field of regenerative medicine, where the large-scale, quality controlled editing of large numbers of cells could generate essential cellular products ready to move towards the clinic. This review details recent progress towards generating HLA Class-I null platelets using genome editing technologies for beta-2-microglobulin deletion, generating a universally transfusable cellular product. In addition, we discuss various methods for megakaryocyte (MK) production from human pluripotent stem cells and subsequent platelet production from the MKs. As well as simply producing platelets, differentiating MK cultures can enable us to understand megakaryopoeisis in vivo and take steps towards ameliorating bleeding disorders or deficiencies in MK maturation in patients. Thus by intersecting both these areas of research, we can produce optimised differentiation systems for the production of universal platelets, thus offering a stable supply of platelets for difficult-to-match patients and providing areas with transmissible disease concerns or an unpredictable supply of platelets with a steady supply of quality controlled platelet units.UK Regenerative Medicine Platform and the Pluripotent and Engineered Cell Hub. Research in the laboratory is supported by core funding from Wellcome and MRC to the Wellcome-MRC Cambridge Stem Cell Institut

Apollo (Cambridge)

CCR2 of Tumor Microenvironmental Cells Is a Relevant Modulator of Glioma Biology.

Author: Blank Anne
Brandenburg Susan
Broggini Thomas
Bungert Alexander D
Felsenstein Matthäus
Ghori Adnan
Kremenetskaia Irina
Mueller Annett
Raggatz Jonas
Rung Olga
Scherschinski Lea
Turkowski Kati
Vajkoczy Peter
Publication venue: Cancers (Basel)
Publication date: 01/01/2020
Field of study

Glioblastoma multiforme (GBM) shows a high influx of tumor-associated macrophages (TAMs). The CCR2/CCL2 pathway is considered a relevant signal for the recruitment of TAMs and has been suggested as a therapeutic target in malignant gliomas. We found that TAMs of human GBM specimens and of a syngeneic glioma model express CCR2 to varying extents. Using a Ccr2-deficient strain for glioma inoculation revealed a 30% reduction of TAMs intratumorally. This diminished immune cell infiltration occurred with augmented tumor volumes likely based on increased cell proliferation. Remaining TAMs in Ccr2-/- mice showed comparable surface marker expression patterns in comparison to wildtype mice, but expression levels of inflammatory transcription factors (Stat3, Irf7, Cox2) and cytokines (Ifnβ, Il1β, Il12α) were considerably affected. Furthermore, we demonstrated an impact on blood vessel integrity, while vascularization of tumors appeared similar between mouse strains. The higher stability and attenuated leakiness of the tumor vasculature imply improved sustenance of glioma tissue in Ccr2-/- mice. Additionally, despite TAMs residing in the perivascular niche in Ccr2-/- mice, their pro-angiogenic activity was reduced by the downregulation of Vegf. In conclusion, lacking CCR2 solely on tumor microenvironmental cells leads to enhanced tumor progression, whereby high numbers of TAMs infiltrate gliomas independently of the CCR2/CCL2 signal

Institutional Repository of the Freie Universität Berlin

Apollo (Cambridge)

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Interferon-γ signaling in human iPSC-derived neurons recapitulates neurodevelopmental disorder phenotypes.

Author: Couch Amalie
Duarte Rodrigo RR
Evans Amanda L
Ghevaert Cédric
Loth Eva
McAlonan Grainne
Mueller Annett
Murphy Declan
Nagy Roland
Perfect Leo
Powell Timothy R
Price Jack
Raval Pooja
Reid Matthew J
Srivastava Deepak P
Vernon Anthony C
Warre-Cornish Katherine
Publication venue: Sci Adv
Publication date: 01/08/2020
Field of study

Maternal immune activation increases the risk of neurodevelopmental disorders. Elevated cytokines, such as interferon-γ (IFN-γ), in offspring's brains play a central role. IFN-γ activates an antiviral cellular state, limiting viral entry and replication. Moreover, IFN-γ is implicated in brain development. We tested the hypothesis that IFN-γ signaling contributes to molecular and cellular phenotypes associated with neurodevelopmental disorders. Transient IFN-γ treatment of neural progenitors derived from human induced pluripotent stem cells increased neurite outgrowth. RNA sequencing analysis revealed that major histocompatibility complex class I (MHCI) genes were persistently up-regulated through neuronal differentiation-an effect that was mediated by IFN-γ-induced promyelocytic leukemia protein (PML) nuclear bodies. Critically, IFN-γ-induced neurite outgrowth required both PML and MHCI. We also found evidence that IFN-γ disproportionately altered the expression of genes associated with schizophrenia and autism, suggesting convergence between genetic and environmental risk factors. Together, these data implicate IFN-γ signaling in neurodevelopmental disorder etiology

Apollo (Cambridge)

King's Research Portal

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DNA methylation-based classification of central nervous system tumours.

Author: Aronica Eleonora
Becker Albert
Benner Axel
Beschorner Rudi
Bewerunge-Hudler Melanie
Bjerkvig Rolf
Braczynski Anne K
Brehmer Stefanie
Brück Wolfgang
Calaminus Gabriele
Capper David
Chavez Lukas
Coras Roland
Cryan Jane
Deckert Martina
Dohmen Hildegard
Driever Pablo Hernáiz
Engel Nils W
Farrell Michael
Fischer Roger
Fleischhack Gudrun
Frank Stephan
Frühwald Michael C
Garvalov Boyan K
Geisenberger Christoph
Giangaspero Felice
Gnekow Astrid
Gottardo Nicholas G
Haberler Christine
Hans Volkmar
Hansford Jordan R
Harter Patrick N
Hench Jürgen
Heppner Frank
Hewer Ekkehard
Hofer Silvia
Hovestadt Volker
Huang Kristin
Hänggi Daniel
Hölsken Annett
Jones Chris
Jones David TW
Jouvet Anne
Kannan Kasthuri
Keohane Catherine
Ketter Ralf
Khatib Ziad
Koch Arend
Koelsche Christian
Kohlhof Patricia
Kramm Christof M
Kratz Annekathrin
Kristensen Bjarne W
Kulozik Andreas
Lechner Matt
Lindenberg Kerstin
Lohmann Dietmar
Lopes Beatriz
Mawrin Christian
Milde Till
Monoranu Camelia-Maria
Mueller Wolf
Mühleisen Helmut
Müller Hermann L
Olar Adriana
Pages Melanie
Pajtler Kristian W
Perry Arie
Plate Karl H
Pohl Ute
Preusser Matthias
Prinz Marco
Reuss David E
Rodriguez Fausto J
Rozsnoki Stephanie
Rushing Elisabeth
Rutkowski Stefan
Sahm Felix
Scheurlen Wolfram
Schick Matthias
Schittenhelm Jens
Schrimpf Daniel
Schweizer Leonille
Seiz-Rosenhagen Marcel
Selt Florian
Serrano Jonathan
Sill Martin
Staszewski Ori
Stichel Damian
Sturm Dominik
Temming Petra
Tippelt Stephan
Tsirigos Aristotelis
Varlet Pascale
von Hoff Katja
Wani Khalida
Wefers Annika K
Witt Hendrik
Witt Olaf
Zapatka Marc
Publication venue: eScholarship, University of California
Publication date: 01/03/2018
Field of study

Accurate pathological diagnosis is crucial for optimal management of patients with cancer. For the approximately 100 known tumour types of the central nervous system, standardization of the diagnostic process has been shown to be particularly challenging-with substantial inter-observer variability in the histopathological diagnosis of many tumour types. Here we present a comprehensive approach for the DNA methylation-based classification of central nervous system tumours across all entities and age groups, and demonstrate its application in a routine diagnostic setting. We show that the availability of this method may have a substantial impact on diagnostic precision compared to standard methods, resulting in a change of diagnosis in up to 12% of prospective cases. For broader accessibility, we have designed a free online classifier tool, the use of which does not require any additional onsite data processing. Our results provide a blueprint for the generation of machine-learning-based tumour classifiers across other cancer entities, with the potential to fundamentally transform tumour pathology

eScholarship - University of California

Glyphosate targets fish monoaminergic systems leading to oxidative stress and anxiety

Author: Aitbali
Annett
Authority
Babin
Bai
Battaglin
Bridi
Brunello
Casarejos
Cattani
Cattani
da Costa Chaulet
de Souza
Edge
Faria
Faria
Faria
Faria
Faria
Faria
Filippi
Friard
Gallegos
Godefroy
Gordon
Guyton
Hamilton
Hermida-Ameijeiras
Horzmann
Joerss
Johnson
Kalueff
Kellner
Kysil
Kyzar
Livak
Martínez
Maximino
Maximino
Mayol-Cabré
Meshalkina
Moratalla
Motta
Mueller
Myers
Pereira
Pu
Reis
Roffler-Tarlov
Roy
Steinrücken
Tingaud-Sequeira
Vandenberg
Vencill
Wang
Webster
Westerink
White
Yamamoto
Zweifel
Publication venue: 'Elsevier BV'
Publication date: 18/11/2020
Field of study

Artículo científico indizadoGlyphosate is the active ingredient of some of the most highly produced and used herbicides worldwide. The intensive applications of glyphosate-based herbicides and its half-life in water lead to its presence in many aquatic ecosystems. Whereas recent studies have reported neurotoxic effects of glyphosate including autism- related effects, most of them used extremely high (mg/L to g/L) concentrations, so it is still unclear if chronic, low environmentally relevant concentrations of this compound (ng/L to μg/L) can induce neurotoxicity. In this study we analyzed the neurotoxicity of glyphosate in adult zebrafish after waterborne exposure to environmentally relevant concentrations (0.3 and 3 μg/L) for two weeks. Our data showed that exposed fish presented a significant impairment of exploratory and social behaviors consistent with increased anxiety. The anterior brain of the exposed fish presented a significant increase in dopamine and serotonin levels, as well as in the DOPAC/dopamine and homovanillic acid/dopamine turnover ratios. Moreover, the expression of genes involved in the dopaminergic system, as th1, th2, comtb, and scl6a3 was downregulated. Finally, the brain of exposed fish presented a significant increase in the catalase and superoxide dismutase activities, with a concomitant decrease of glutathione stores. These changes in the antioxidant defense system are consistent with the observed increase in oxidative stress, reflected by the increase in the levels of lipid peroxidation in the brain. The presented results show that current glyphosate concentrations commonly found in many aquatic ecosystems may have detrimental consequences on fish survival by decreasing exploration of the environment or altering social interactions. Furthermore, as zebrafish is also a vertebrate model widely used in human neurobehavioral studies, these results are relevant not only for environmental risk assessment, but also for understanding the risk of chronic low-dose exposures on human health.This work was supported by the Spanish Government with FEDER Funds (CTM2017-83242-R; D.R.) and the network of recognized research groups by the Catalan Government (2017 SGR_902). J.B. was supported by a Spanish fellowship PRE2018-083513. Mention of spe- cific products or trade names does not indicate endorsement by the US federal government

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Repositorio Institucional de la Universidad Autónoma del Estado de México

Digital.CSIC

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CRLF3 plays a key role in the final stage of platelet genesis and is a potential therapeutic target for thrombocythemia.

Author: Adams David J
Akbari Parsa
Baig Ayesha
Ballester-Beltrán Jose
Bender Markus
Bennett Cavan
Couzens Amber L
Erber Wendy N
Evans Amanda L
Ghevaert Cedric
Guerrero Jose A
Hoffman Gary J
Lawrence Moyra
Mayer Louisa
Mifsud Richard W
Mookerjee Souradip
Moreau Thomas
Mueller Annett
Nieswandt Bernhard
Penkett Christopher J
Read Randy J
Saeb-Parsy Kourosh
Stritt Simon
Waller Amie K
Warland James
Yan Yahui
Publication venue: Blood
Publication date: 07/04/2022
Field of study

The process of platelet production has so far been understood to be a 2-stage process: megakaryocyte maturation from hematopoietic stem cells followed by proplatelet formation, with each phase regulating the peripheral blood platelet count. Proplatelet formation releases into the bloodstream beads-on-a-string preplatelets, which undergo fission into mature platelets. For the first time, we show that preplatelet maturation is a third, tightly regulated, critical process akin to cytokinesis that regulates platelet count. We show that deficiency in cytokine receptor-like factor 3 (CRLF3) in mice leads to an isolated and sustained 25% to 48% reduction in the platelet count without any effect on other blood cell lineages. We show that Crlf3-/- preplatelets have increased microtubule stability, possibly because of increased microtubule glutamylation via the interaction of CRLF3 with key members of the Hippo pathway. Using a mouse model of JAK2 V617F essential thrombocythemia, we show that a lack of CRLF3 leads to long-term lineage-specific normalization of the platelet count. We thereby postulate that targeting CRLF3 has therapeutic potential for treatment of thrombocythemia

Apollo (Cambridge)

Dynamic Maize Responses to Aphid Feeding Are Revealed by a Time Series of Transcriptomic and Metabolomic Assays

Author: Ahern Kevin R.
Degenhardt Joerg
Fernández-Pozo Noé
Huffaker Alisa
Jander Georg
Kaur Harleen
Meihls Lisa N.
Mori Naoki
Mueller Lukas A.
Richter Annett
Schmelz Eric A.
Schoettner Matthias
Schäfer Martin
Tzin Vered
Publication venue
Publication date: 16/09/2015
Field of study

As a response to insect attack, maize (Zea mays) has inducible defenses that involve large changes in gene expression and metabolism. Piercing/sucking insects such as corn leaf aphid (Rhopalosiphum maidis) cause direct damage by acquiring phloem nutrients as well as indirect damage through the transmission of plant viruses. To elucidate the metabolic processes and gene expression changes involved in maize responses to aphid attack, leaves of inbred line B73 were infested with corn leaf aphids for 2 to 96 h. Analysis of infested maize leaves showed two distinct response phases, with the most significant transcriptional and metabolic changes occurring in the first few hours after the initiation of aphid feeding. After 4 d, both gene expression and metabolite profiles of aphid-infested maize reverted to being more similar to those of control plants. Although there was a predominant effect of salicylic acid regulation, gene expression changes also indicated prolonged induction of oxylipins, although not necessarily jasmonic acid, in aphid-infested maize. The role of specific metabolic pathways was confirmed using Dissociator transposon insertions in maize inbred line W22. Mutations in three benzoxazinoid biosynthesis genes, Bx1, Bx2, and Bx6, increased aphid reproduction. In contrast, progeny production was greatly decreased by a transposon insertion in the single W22 homolog of the previously uncharacterized B73 terpene synthases TPS2 and TPS3. Together, these results show that maize leaves shift to implementation of physical and chemical defenses within hours after the initiation of aphid feeding and that the production of specific metabolites can have major effects in maize-aphid interactions.Peer reviewe

Digital.CSIC

Can Budget Institutions Counteract Political Indiscipline?

Author: Acemoglu
Aghion
Alesina
Alesina
Allen
Alt
Annett
Baltagi
Benoit
Besley
Blanchard
Blanchard
Bohn
Bruno
Cukierman
Eichengreen
Franzese
Gleich
Hahm
Hallerberg
Hallerberg
Hallerberg
Knight
Kontopoulos
Lijphart
Milesi-Ferretti
Mueller
Perotti
Persson
Persson
Persson
Persson
Persson
Poterba
Poterba
Potter
Roubini
Shepsle
Stein
Velasco
Velasco
von Hagen
Weingast
Wyplosz
Yläoutinen
Publication venue: 'International Monetary Fund (IMF)'
Publication date: 01/01/2006
Field of study

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