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Vineeta B. Tripathi

Medical Research Council
Other affiliations: University of Cambridge, King's College, University of London  ...read more
Bio: Vineeta B. Tripathi is an academic researcher from Medical Research Council. The author has contributed to research in topics: Amyotrophic lateral sclerosis & TARDBP. The author has an hindex of 6, co-authored 7 publications receiving 4773 citations. Previous affiliations of Vineeta B. Tripathi include University of Cambridge & King's College.
Topics: Amyotrophic lateral sclerosis, TARDBP, Neurodegeneration, C9orf72, UBQLN2
Papers
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Journal ArticleDOI
TDP-43 Mutations in Familial and Sporadic Amyotrophic Lateral Sclerosis

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Jemeen Sreedharan1, Ian P. Blair2, Vineeta B. Tripathi1, Xun Hu1, Caroline Vance1, Boris Rogelj1, Steven Ackerley1, Steven Ackerley3, Jennifer C Durnall, Kelly L. Williams, Emanuele Buratti4, Francisco E. Baralle4, Jacqueline de Belleroche5, J. Douglas Mitchell, P. Nigel Leigh1, Ammar Al-Chalabi1, Christopher C.J. Miller3, Christopher C.J. Miller1, Garth A. Nicholson6, Garth A. Nicholson2, Christopher Shaw1 
Medical Research Council1, University of Sydney2, King's College London3, International Centre for Genetic Engineering and Biotechnology4, Imperial College London5, Concord Repatriation General Hospital6
21 Mar 2008-Science
TL;DR: The evidence suggests a pathophysiological link between TDP-43 and ALS, and neighboring mutations in a highly conserved region of TARDBP in sporadic and familial ALS cases.
Abstract: Amyotrophic lateral sclerosis (ALS) is a fatal motor neuron disorder characterized pathologically by ubiquitinated TAR DNA binding protein (TDP-43) inclusions. The function of TDP-43 in the nervous system is uncertain, and a mechanistic role in neurodegeneration remains speculative. We identified neighboring mutations in a highly conserved region of TARDBP in sporadic and familial ALS cases. TARDBPM337V segregated with disease within one kindred and a genome-wide scan confirmed that linkage was restricted to chromosome 1p36, which contains the TARDBP locus. Mutant forms of TDP-43 fragmented in vitro more readily than wild type and, in vivo, caused neural apoptosis and developmental delay in the chick embryo. Our evidence suggests a pathophysiological link between TDP-43 and ALS.

2,425 citations

Journal ArticleDOI
Mutations in FUS, an RNA Processing Protein, Cause Familial Amyotrophic Lateral Sclerosis Type 6

[...]

Caroline Vance1, Boris Rogelj1, Tibor Hortobágyi1, Kurt J. De Vos2, Agnes L. Nishimura1, Jemeen Sreedharan1, Xun Hu1, Bradley N. Smith1, Deborah Ruddy1, Paul Wright1, Jeban Ganesalingam1, Kelly L. Williams, Vineeta B. Tripathi1, Safa Al-Saraj1, Ammar Al-Chalabi1, P. Nigel Leigh1, Ian P. Blair3, Garth A. Nicholson4, Garth A. Nicholson3, Jackie de Belleroche5, Jean-Marc Gallo1, Christopher C.J. Miller2, Christopher C.J. Miller1, Christopher Shaw1 
Medical Research Council1, King's College London2, University of Sydney3, Concord Hospital4, Imperial College London5
27 Feb 2009-Science
TL;DR: A missense mutation in the gene encoding fused in sarcoma (FUS) in a British kindred, linked to ALS6, is identified, which suggests that a common mechanism may underlie motor neuron degeneration.
Abstract: Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease that is familial in 10% of cases. We have identified a missense mutation in the gene encoding fused in sarcoma (FUS) in a British kindred, linked to ALS6. In a survey of 197 familial ALS index cases, we identified two further missense mutations in eight families. Postmortem analysis of three cases with FUS mutations showed FUS-immunoreactive cytoplasmic inclusions and predominantly lower motor neuron degeneration. Cellular expression studies revealed aberrant localization of mutant FUS protein. FUS is involved in the regulation of transcription and RNA splicing and transport, and it has functional homology to another ALS gene, TARDBP, which suggests that a common mechanism may underlie motor neuron degeneration.

2,373 citations

Journal ArticleDOI
Variants of the elongator protein 3 (ELP3) gene are associated with motor neuron degeneration

[...]

Claire L. Simpson1, Robin Lemmens2, Robin Lemmens3, Katarzyna Miskiewicz2, Katarzyna Miskiewicz3, Wendy J. Broom4, Valerie K. Hansen1, Paul W.J. van Vught5, John Landers4, Peter C. Sapp4, Peter C. Sapp6, Ludo Van Den Bosch2, Ludo Van Den Bosch3, Joanne Knight1, Benjamin M. Neale1, Martin R Turner1, Jan H. Veldink5, Roel A. Ophoff5, Roel A. Ophoff7, Vineeta B. Tripathi1, Ana Beleza1, Meera N. Shah1, Petroula Proitsi1, Annelies Van Hoecke3, Annelies Van Hoecke2, Peter Carmeliet2, H. Robert Horvitz6, P. Nigel Leigh1, Christopher Shaw1, Leonard H. van den Berg, Pak C. Sham8, John Powell1, Patrik Verstreken3, Patrik Verstreken2, Robert H. Brown4, Wim Robberecht3, Wim Robberecht2, Ammar Al-Chalabi1 
University of London1, Flanders Institute for Biotechnology2, Katholieke Universiteit Leuven3, Harvard University4, University of Groningen5, Massachusetts Institute of Technology6, University of California, Los Angeles7, University of Hong Kong8
01 Feb 2009-Human Molecular Genetics
TL;DR: In this article, the RNA polymerase II component, ELP3, was found to be associated with ALS in three human populations comprising 1483 people (P=1.96 x 10(-9)).
Abstract: Amyotrophic lateral sclerosis (ALS) is a spontaneous, relentlessly progressive motor neuron disease, usually resulting in death from respiratory failure within 3 years. Variation in the genes SOD1 and TARDBP accounts for a small percentage of cases, and other genes have shown association in both candidate gene and genome-wide studies, but the genetic causes remain largely unknown. We have performed two independent parallel studies, both implicating the RNA polymerase II component, ELP3, in axonal biology and neuronal degeneration. In the first, an association study of 1884 microsatellite markers, allelic variants of ELP3 were associated with ALS in three human populations comprising 1483 people (P=1.96 x 10(-9)). In the second, an independent mutagenesis screen in Drosophila for genes important in neuronal communication and survival identified two different loss of function mutations, both in ELP3 (R475K and R456K). Furthermore, knock down of ELP3 protein levels using antisense morpholinos in zebrafish embryos resulted in dose-dependent motor axonal abnormalities [Pearson correlation: -0.49, P=1.83 x 10(-12) (start codon morpholino) and -0.46, P=4.05 x 10(-9) (splice-site morpholino), and in humans, risk-associated ELP3 genotypes correlated with reduced brain ELP3 expression (P=0.01). These findings add to the growing body of evidence implicating the RNA processing pathway in neurodegeneration and suggest a critical role for ELP3 in neuron biology and of ELP3 variants in ALS.

274 citations

Supporting Online Material for Mutations in FUS, an RNA Processing Protein, Cause Familial Amyotrophic Lateral Sclerosis Type 6

[...]

Caroline Vance, Boris Rogelj, Tibor Hortobágyi, Kurt J. De Vos, Agnes L. Nishimura, Jemeen Sreedharan, Xun Hu, Bradley N. Smith, Deborah Ruddy, Paul Wright, Jeban Ganesalingam, Kelly L. Williams, Vineeta B. Tripathi, Safa Al-Saraj, Ammar Al-Chalabi, P. Nigel Leigh, Ian P. Blair, Garth A. Nicholson, Jackie de Belleroche, Jean-Marc Gallo, Christopher C.J. Miller, Christopher Shaw1 
King's College London1
01 Jan 2009
TL;DR: The authors identified a missense mutation in the gene encoding fused in sarcoma (FUS) in a British kindred, linked to ALS6, and two further missense mutations in eight families.
Abstract: Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease that is familial in 10% of cases. We have identified a missense mutation in the gene encoding fused in sarcoma (FUS) in a British kindred, linked to ALS6. In a survey of 197 familial ALS index cases, we identified two further missense mutations in eight families. Postmortem analysis of three cases with FUS mutations showed FUS-immunoreactive cytoplasmic inclusions and predominantly lower motor neuron degeneration. Cellular expression studies revealed aberrant localization of mutant FUS protein. FUS is involved in the regulation of transcription and RNA splicing and transport, and it has functional homology to another ALS gene, TARDBP, which suggests that a common mechanism may underlie motor neuron degeneration.

125 citations

Journal ArticleDOI
Tar DNA-binding protein-43 (TDP-43) regulates axon growth in vitro and in vivo

[...]

Vineeta B. Tripathi1, Vineeta B. Tripathi2, Pranetha Baskaran2, Christopher Shaw1, Sarah Guthrie2 
King's College1, University of Cambridge2
01 May 2014-Neurobiology of Disease
TL;DR: The capacity of spinal motor neurons to produce and maintain an axon is compromised by dysregulation of TDP-43 and that the disruption of cytoskeletal integrity may play a role in the pathogenesis of ALS and FTD-TDP.

31 citations

Cited by
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Journal ArticleDOI
Expanded GGGGCC hexanucleotide repeat in noncoding region of C9ORF72 causes chromosome 9p-linked FTD and ALS

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Mariely DeJesus-Hernandez1, Ian R. A. Mackenzie2, Bradley F. Boeve1, Adam L. Boxer3, Matt Baker1, Nicola J. Rutherford1, Alexandra M. Nicholson1, Ni Cole A. Finch1, Heather C. Flynn1, Jennifer Adamson1, Naomi Kouri1, Aleksandra Wojtas1, Pheth Sengdy2, Ging-Yuek Robin Hsiung2, Anna Karydas3, William W. Seeley3, Keith A. Josephs1, Giovanni Coppola4, Daniel H. Geschwind4, Zbigniew K. Wszolek1, Howard Feldman5, Howard Feldman2, David S. Knopman1, Ronald C. Petersen1, Bruce L. Miller3, Dennis W. Dickson1, Kevin B. Boylan1, Neill R. Graff-Radford1, Rosa Rademakers1 
Mayo Clinic1, University of British Columbia2, University of California, San Francisco3, Semel Institute for Neuroscience and Human Behavior4, Bristol-Myers Squibb5
20 Oct 2011-Neuron
TL;DR: It is found that repeat expansion in C9ORF72 is a major cause of both FTD and ALS, suggesting multiple disease mechanisms.

4,153 citations

Journal ArticleDOI
A hexanucleotide repeat expansion in C9ORF72 is the cause of chromosome 9p21-linked ALS-FTD

[...]

Alan E. Renton1, Elisa Majounie1, Adrian James Waite2, Javier Simón-Sánchez3, Javier Simón-Sánchez4, Sara Rollinson5, J. Raphael Gibbs1, J. Raphael Gibbs6, Jennifer C. Schymick1, Hannu Laaksovirta7, John C. van Swieten4, John C. van Swieten3, Liisa Myllykangas7, Hannu Kalimo7, Anders Paetau7, Yevgeniya Abramzon1, Anne M. Remes8, Alice Kaganovich1, Sonja W. Scholz1, Sonja W. Scholz9, Sonja W. Scholz10, Jamie Duckworth1, Jinhui Ding1, Daniel W. Harmer11, Dena G. Hernandez6, Dena G. Hernandez1, Janel O. Johnson6, Janel O. Johnson1, Kin Y. Mok6, Mina Ryten6, Danyah Trabzuni6, Rita Guerreiro6, Richard W. Orrell6, James Neal2, Alexandra Murray12, J. P. Pearson2, Iris E. Jansen3, David Sondervan3, Harro Seelaar4, Derek J. Blake2, Kate Young5, Nicola Halliwell5, Janis Bennion Callister5, Greg Toulson5, Anna Richardson5, Alexander Gerhard5, Julie S. Snowden5, David M. A. Mann5, David Neary5, Mike A. Nalls1, Terhi Peuralinna7, Lilja Jansson7, Veli-Matti Isoviita7, Anna-Lotta Kaivorinne8, Maarit Hölttä-Vuori7, Elina Ikonen7, Raimo Sulkava13, Michael Benatar14, Joanne Wuu14, Adriano Chiò15, Gabriella Restagno, Giuseppe Borghero16, Mario Sabatelli17, David Heckerman18, Ekaterina Rogaeva19, Lorne Zinman19, Jeffrey D. Rothstein9, Michael Sendtner20, Carsten Drepper20, Evan E. Eichler21, Can Alkan21, Ziedulla Abdullaev1, Svetlana Pack1, Amalia Dutra1, Evgenia Pak1, John Hardy6, Andrew B. Singleton1, Nigel Williams2, Peter Heutink3, Stuart Pickering-Brown5, Huw R. Morris22, Huw R. Morris12, Huw R. Morris2, Pentti J. Tienari7, Bryan J. Traynor1, Bryan J. Traynor9 
National Institutes of Health1, Cardiff University2, VU University Amsterdam3, Erasmus University Rotterdam4, University of Manchester5, University College London6, University of Helsinki7, University of Oulu8, Johns Hopkins University9, Georgetown University10, Illumina11, University Hospital of Wales12, University of Eastern Finland13, University of Miami14, University of Turin15, University of Cagliari16, The Catholic University of America17, Microsoft18, University of Toronto19, University of Würzburg20, University of Washington21, Aneurin Bevan University Health Board22
20 Oct 2011-Neuron
TL;DR: The chromosome 9p21 amyotrophic lateral sclerosis-frontotemporal dementia (ALS-FTD) locus contains one of the last major unidentified autosomal-dominant genes underlying these common neurodegenerative diseases, and a large hexanucleotide repeat expansion in the first intron of C9ORF72 is shown.

3,784 citations

Journal ArticleDOI
Mechanisms underlying inflammation in neurodegeneration.

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Christopher K. Glass1, Kaoru Saijo1, Beate Winner2, Maria C. Marchetto2, Fred H. Gage2 
University of California, San Diego1, Salk Institute for Biological Studies2
19 Mar 2010-Cell
TL;DR: There is evidence for a remarkable convergence in the mechanisms responsible for the sensing, transduction, and amplification of inflammatory processes that result in the production of neurotoxic mediators in neurodegenerative diseases.

2,838 citations

Journal ArticleDOI
Mutations in the FUS/TLS gene on chromosome 16 cause familial amyotrophic lateral sclerosis.

[...]

Thomas J. Kwiatkowski1, D. A. Bosco1, D. A. Bosco2, A. L. LeClerc2, A. L. LeClerc1, Eric Tamrazian1, Charles R. Vanderburg1, Carsten Russ3, Carsten Russ1, A. Davis1, James M. Gilchrist4, E. J. Kasarskis5, Theodore L. Munsat6, Paul N. Valdmanis7, Guy A. Rouleau7, Betsy A. Hosler1, Pietro Cortelli8, P. J. De Jong9, Yuko Yoshinaga9, Jonathan L. Haines10, Margaret A. Pericak-Vance, Jianhua Yan11, Nicola Ticozzi1, Nicola Ticozzi12, Nicola Ticozzi2, Teepu Siddique11, Diane McKenna-Yasek1, Peter C. Sapp3, Peter C. Sapp1, H R Horvitz3, John Landers1, John Landers2, Robert H. Brown2, Robert H. Brown1 
Harvard University1, University of Massachusetts Medical School2, Massachusetts Institute of Technology3, Rhode Island Hospital4, University of Kentucky5, Tufts University6, Université de Montréal7, University of Bologna8, Children's Hospital Oakland Research Institute9, Vanderbilt University10, Northwestern University11, University of Milan12
27 Feb 2009-Science
TL;DR: Neuronal cytoplasmic protein aggregation and defective RNA metabolism thus appear to be common pathogenic mechanisms involved in ALS and possibly in other neurodegenerative disorders.
Abstract: Amyotrophic lateral sclerosis (ALS) is a fatal degenerative motor neuron disorder Ten percent of cases are inherited; most involve unidentified genes We report here 13 mutations in the fused in sarcoma/translated in liposarcoma (FUS/TLS) gene on chromosome 16 that were specific for familial ALS The FUS/TLS protein binds to RNA, functions in diverse processes, and is normally located predominantly in the nucleus In contrast, the mutant forms of FUS/TLS accumulated in the cytoplasm of neurons, a pathology that is similar to that of the gene TAR DNA-binding protein 43 (TDP43), whose mutations also cause ALS Neuronal cytoplasmic protein aggregation and defective RNA metabolism thus appear to be common pathogenic mechanisms involved in ALS and possibly in other neurodegenerative disorders

2,387 citations

Journal ArticleDOI
Mutations in FUS, an RNA Processing Protein, Cause Familial Amyotrophic Lateral Sclerosis Type 6

[...]

Caroline Vance1, Boris Rogelj1, Tibor Hortobágyi1, Kurt J. De Vos2, Agnes L. Nishimura1, Jemeen Sreedharan1, Xun Hu1, Bradley N. Smith1, Deborah Ruddy1, Paul Wright1, Jeban Ganesalingam1, Kelly L. Williams, Vineeta B. Tripathi1, Safa Al-Saraj1, Ammar Al-Chalabi1, P. Nigel Leigh1, Ian P. Blair3, Garth A. Nicholson3, Garth A. Nicholson4, Jackie de Belleroche5, Jean-Marc Gallo1, Christopher C.J. Miller1, Christopher C.J. Miller2, Christopher Shaw1 
Medical Research Council1, King's College London2, University of Sydney3, Concord Hospital4, Imperial College London5
27 Feb 2009-Science
TL;DR: A missense mutation in the gene encoding fused in sarcoma (FUS) in a British kindred, linked to ALS6, is identified, which suggests that a common mechanism may underlie motor neuron degeneration.
Abstract: Amyotrophic lateral sclerosis (ALS) is a fatal neurodegenerative disease that is familial in 10% of cases. We have identified a missense mutation in the gene encoding fused in sarcoma (FUS) in a British kindred, linked to ALS6. In a survey of 197 familial ALS index cases, we identified two further missense mutations in eight families. Postmortem analysis of three cases with FUS mutations showed FUS-immunoreactive cytoplasmic inclusions and predominantly lower motor neuron degeneration. Cellular expression studies revealed aberrant localization of mutant FUS protein. FUS is involved in the regulation of transcription and RNA splicing and transport, and it has functional homology to another ALS gene, TARDBP, which suggests that a common mechanism may underlie motor neuron degeneration.

2,373 citations