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53 research outputs found

Differential exposure and reactivity to interpersonal stress predict sex differences in adolescent depression

Author: Arieti S.
Beck A. T.
Constance L. Hammen
Gore S.
Hankin B. L.
Heubeck B.
Josephine H. Shih
Keeping J. D.
Lai J. C. L.
Leadbeater B. J.
MacKinnon D. P.
Marcotte D.
Mazure C. M.
Nicole K. Eberhart
Patricia A. Brennan
Wells K. B.
Publication venue: 'Informa UK Limited'
Publication date: 01/01/2006
Field of study

This study tested the hypothesis that higher rates of depression in adolescent girls are explained by their greater exposure and reactivity to stress in the interpersonal domain in a large sample of 15-year-olds. Findings indicate that adolescent girls experienced higher levels of total and interpersonal episodic stress, whereas boys experienced higher levels of chronic stress (academic and close friendship domains). Higher rates of depression in girls were explained by their greater exposure to total stress, particularly interpersonal episodic stress. Adolescent girls were also more reactive (more likely to become depressed) to both total and interpersonal episodic stress. The findings suggest that girls experience higher levels of episodic stress and are more reactive to these stressors, increasing their likelihood of becoming depressed compared to boys. Results were discussed in terms of girls' greater interpersonal focus and implications for understanding sex differences in depression

Crossref

University of Queensland eSpace

Design and Implementation of Degenerate Microsatellite Primers for the Mammalian Clade

Author: A Estoup
A Estoup
AJ Hannan
AJ Osborne
B Amos
BC Robertson
C Girod
C Küpper
C Liewlaksaneeyanawin
C Rico
C Schlötterer
C Vanpé
C-H Wu
CR Farber
CR Primmer
CR Primmer
DA Dawson
E Buschiazzo
E Buschiazzo
E Buschiazzo
Emmanuel Buschiazzo
H Ellegren
J Abdelkrim
J Carreras-Carbonell
J Goecks
JC Garza
JD Thompson
Josephine S. Beck
JR Ellis
KA Selkoe
L Zane
M La Rota
M Raveendran
M Raveendran
M Schuelke
MD Gadberry
Neil J. Gemmell
NJ Gemmell
NN FitzSimmons
PA Fujita
PW Walsh
R Sainudiin
RK Varshney
RL Stallings
Robert C. Fleischer
S Kumar
S Rozen
SS Moore
ST Kalinowski
T Barbara
TA Hall
TC Marshall
W Miller
WC Warren
YD Kelkar
Publication venue: Public Library of Science
Publication date: 27/12/2011
Field of study

Microsatellites are popular genetic markers in molecular ecology, genetic mapping and forensics. Unfortunately, despite recent advances, the isolation of de novo polymorphic microsatellite loci often requires expensive and intensive groundwork. Primers developed for a focal species are commonly tested in a related, non-focal species of interest for the amplification of orthologous polymorphic loci; when successful, this approach significantly reduces cost and time of microsatellite development. However, transferability of polymorphic microsatellite loci decreases rapidly with increasing evolutionary distance, and this approach has shown its limits. Whole genome sequences represent an under-exploited resource to develop cross-species primers for microsatellites. Here we describe a three-step method that combines a novel in silico pipeline that we use to (1) identify conserved microsatellite loci from a multiple genome alignments, (2) design degenerate primer pairs, with (3) a simple PCR protocol used to implement these primers across species. Using this approach we developed a set of primers for the mammalian clade. We found 126,306 human microsatellites conserved in mammalian aligned sequences, and isolated 5,596 loci using criteria based on wide conservation. From a random subset of ∼1000 dinucleotide repeats, we designed degenerate primer pairs for 19 loci, of which five produced polymorphic fragments in up to 18 mammalian species, including the distinctly related marsupials and monotremes, groups that diverged from other mammals 120–160 million years ago. Using our method, many more cross-clade microsatellite loci can be harvested from the currently available genomic data, and this ability is set to improve exponentially as further genomes are sequenced

Public Library of Science (PLOS)

Crossref

Directory of Open Access Journals

PubMed Central

The Evolution of Extracellular Matrix

Author: Adamczyk P.
Baldauf S. L.
Beck K.
Bentley A. A.
Bornstein P.
Boute N.
Brower D. L.
Bucior I.
Carafoli F.
Chakravarti R.
Cornillon S.
Cornillon S.
Dacks J. B.
Dehal P.
Doug Kellogg
Ewan R.
Exposito J. Y.
Exposito J. Y.
Fanjul-Fernández M.
Filmus J.
Garrone R.
George E. L.
Gosline J.
Halász K.
Harrington M. J.
Hecht J.
Hughes A. L.
Huhtala M.
Huxley-Jones J.
Hynes R. O.
Jeffery W. R.
Josephine C. Adams
Katsube K.
Kawashima T.
King N.
King N.
Mao Y.
McKenzie P.
Meyer A.
Mueller W.E.G.
Müller W. E.
Nicholson A. C.
Odgren P. R.
Prakash G. Balasubramanian
Ramirez F.
Reber-Müller S.
Reiners J.
Rentz T. J.
Richard P. Tucker
Robson P.
Rokas A.
Ruth Chiquet-Ehrismann
Schierwater B.
Sebé-Pedrós A.
Shalchian-Tabrizi K.
Shoulders M. D.
Silverstein R. L.
Srivastava M.
Suat Özbek
Sun L.
Tucker R. P.
Tucker R. P.
Tucker R. P.
Tucker R. P.
Tucker R. P.
Tulla M.
Tzu J.
Wada H.
Weigel P. H.
Wouters M. A.
Wu H.
Yamada S.
Yoneda M.
Zhang G.
Publication venue: The American Society for Cell Biology
Publication date: 01/12/2010
Field of study

We present a perspective on the molecular evolution of the extracellular matrix (ECM) in metazoa that draws on research publications and data from sequenced genomes and expressed sequence tag libraries. ECM components do not function in isolation, and the biological ECM system or “adhesome” also depends on posttranslational processing enzymes, cell surface receptors, and extracellular proteases. We focus principally on the adhesome of internal tissues and discuss its origins at the dawn of the metazoa and the expansion of complexity that occurred in the chordate lineage. The analyses demonstrate very high conservation of a core adhesome that apparently evolved in a major wave of innovation in conjunction with the origin of metazoa. Integrin, CD36, and certain domains predate the metazoa, and some ECM-related proteins are identified in choanoflagellates as predicted sequences. Modern deuterostomes and vertebrates have many novelties and elaborations of ECM as a result of domain shuffling, domain innovations and gene family expansions. Knowledge of the evolution of metazoan ECM is important for understanding how it is built as a system, its roles in normal tissues and disease processes, and has relevance for tissue engineering, the development of artificial organs, and the goals of synthetic biology

Crossref

PubMed Central

Explore Bristol Research

Understanding the sex difference in vulnerability to adolescent depression: an examination of child and parent characteristics

Author: A. Bedford
A. Bedford
A. E. Grills
A. H. Eagly
A. J. Rose
A. M. Thomas
A. Sund
A. T. Beck
B. Allgood-Merten
B. J. Leadbeater
B. L. Hankin
B. L. Hankin
C. Hammen
C. Hammen
C. L. Hammen
C. M. Ohannessian
C. Z. Garrison
Constance L. Hammen
D. M. Buss
D. Marcotte
D. P. MacKinnon
D. P. MacKinnon
G. C. Armsden
G. H. McClelland
H. Aquinis
H. Hops
H. Hops
H. Orvaschel
J. A. O’Dea
J. C. Coyne
J. D. Keeping
J. M. Cyranowski
J. P. Hill
Josephine H. Shih
K. A. Brennan
K. B. Carnelley
K. Bartholomew
K. D. Rudolph
K. L. Buist
K. Wilhelm
L. A. Slavin
L. Sheeber
M. B. First
M. Dumont
M. E. Kenny
M. E. Kenny
M. E. Sobel
M. H. Boyle
M. P. McCabe
N. C. Andreasen
Nicole K. Eberhart
P. M. Lewinsohn
P. M. Lewinsohn
P. M. Lewinsohn
P. Mallet
P. T. Davies
Patricia A. Brennan
R. C. Kessler
R. E. Roberts
R. H. Moos
R. M. Baron
R. R. Kobak
S. Harter
S. J. Blatt
S. Nolen-Hoeksema
T. E. Joiner
T. J. Wade
T. N. Crawford
U. Rao
V. Phares
W. Furman
W. J. Hagborg
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2006
Field of study

This study examined sex differences in risk factors associated with adolescent depression in a large sample of boys and girls. Moderation and mediation explanatory models of the sex difference in likelihood of depression were examined. Findings indicate that the factors associated with depression in adolescent boys and girls are quite similar. All of the variables considered were associated with depression, but sex did not moderate the impact of vulnerability factors on likelihood of depression diagnosis. However, negative self-perceptions in the domains of achievement, global self-worth, and physical appearance partially mediated the relationship between sex and depression. Further, girls had higher levels of positive self-perceptions in interpersonal domains that acted as suppressors and reduced the likelihood of depression in girls. These findings suggest that girls' higher incidence of depression is due in part to their higher levels of negative self-perceptions, whereas positive interpersonal factors serve to protect them from depressive episodes

CiteSeerX

Crossref

University of Queensland eSpace

A communal catalogue reveals Earth's multiscale microbial diversity

Author: Aaron Clauset
Aaron R. Jex
Alexandra H. Campbell
Alexandra M. Linz
Allison Berry
Allison E. Williams
Alyssa Cochran
Amnon Amir
Amy Apprill
Andaine Seguin-Orlando
Anders Karlsson
Andrew P. Rees
Andrew Whitehead
Anna Forsman
Anni Moore
Anson V. Koehler
Antje Gittel
Antonio González
Antonio M. Martín-Platero
Anupriya Tripathi
Asha Rani
Ashish Bhatnagar
Ashley Shade
Aurora MacRae-Crerar
Baddr Shakhsheer
Bazartseren Boldgiv
Beck Wehrle
Benjamin B. Crary
Benjamin D. Shogan
Benjamin L. Turner
Bharath Prithiviraj
Bonnie Laverock
Brenda B. Casper
Brent Stephens
Byron C. Crump
Caitlin Potter
Carol Robinson
Catherine M. Spirito
Catherine Pfister
Cesar Cardona
Chia L. Tan
Chris Freeman
Christopher Quince
Colin J. Brislawn
Colleen T. E. Kellogg
Congcong Shen
D. Lee Taylor
Daniel A. Cristol
Daniel McDonald
Daniel P. Smith
Daniel van der Lelie
Daniela Vargas-Robles
Danielle C. Claar
Danilo Ercolini
Dave Shutler
David A. Lipson
David A. Mills
David Armitage
David Garshelis
David Myrold
Diogo Jurelevicius
Dionysios A. Antonopoulos
Donal M. Boyer
Donald A. Walker
Donglai Gong
Donna Berg-Lyons
Douglas C. Woodhams
Duoying Cui
Elizabeth Pilon-Smits
Elliot S. Friedman
Embriette Hyde
Emily M. Landon
Eric A. Dubinsky
Eric Bottos
Eric R. Johnston
Eske Willerslev
Evguenia Kopylova
Ezequiel M. Marzinelli
F. Joseph Pollock
Fabian Michelangeli
Folker Meyer
Forest Rohwer
Francis Q. Brearley
Frédéric Delsuc
Gabriela M. Sheets
Gail Ackermann
Gary M. King
Gavin Collins
George W. Kling
Giancarlo Galindo
Glida Hidalgo
Graeme W. Nicol
Gregory D. Mayer
Gregory Humphrey
Gunnar Gerdts
Haiyan Chu
Hakdong Shin
Hans-Peter Grossart
Hebe M. Dionisi
Helen S. Findlay
Hongxia Zhao
Ina Timling
Iratxe Zarraonaindia
Iris I. Levin
Irma D. Fleming
Isaac Gifford
J. Gregory Caporaso
Jack A. Gilbert
Jacob Parnell
Jad Kanbar
James E. McDonald
James T. Morton
Jamie M. McDevitt-Irwin
Janet K. Jansson
Jarrad Hampton-Marcell
Jason Andras
Jed A. Fuhrman
Jeff Hooker
Jeffrey J. Werner
Jeffrey Siegel
Jenni Hultman
Jennifer Defazio
Jennifer F. Biddle
Jeremiah Minich
Jesse Zaneveld
Jessica L. Metcalf
Jirˇí Bárta
John Alverdy
JoLynn Carroll
Jon G. Sanders
Jonathan B. Clayton
Jonathan E. Hickman
Jordan Kueneman
Jose A. Navas-Molina
Jose C. Clemente
Jose L. Agosto Rivera
Joseph R. Mendelson
Josephine Braun
Josh D. Neufeld
Joshua Ladau
Joshua Lefler
Jozef I. Nissimov
Juan Diego Ibáñez-Álamo
Juan J. Soler
Juan M. Peralta-Sánchez
Julia K. Baum
Julie D. Jastrow
Julie LaRoche
Karen Noyce
Karen Tait
Karl J. Rockne
Kate Ballantine
Katherine D. McMahon
Katherine R. Amato
Katherine S. Pollard
Kefeng Niu
Kelly D. Goodwin
Kelly Lane-deGraaf
Kenneth J. Locey
Kim M. Handley
Kim Miller
Kirsten S. Hofmockel
Krista L. McGuire
Kristin West
Kristina Guyton
L. Margarita Martínez
L. Scott Johnson
Largus T. Angenent
Lauren M. Seyler
Lee J. Kerkhof
Liliana Davalos
Linda A. Whittingham
Lingjing Jiang
Lisa Al-Moosawi
Liza Garcia
Lucas Moitinho-Silva
Lucie Bittner
Lucy Seldin
Ludovic Orlando
Lukas van Zwieten
Luke K. Ursell
Luke R. Thompson
Magda Magris
Manuel E. Lladser
Manuel Martín-Vivaldi
Manuel Martínez-Bueno
Maria Alexandra Garcia-Amado
Maria Gloria Dominguez-Bello
Mariana Lozada
Mark D. Schrenzel
Martin Sperling
Matthew J. Nolan
Matthew Schrenk
Maureen L. Coleman
Melita A. Stevens
Miguel Lentino
Miles Richardson
Mohamed F. Haroon
Molly K. Gibson
Monica Bhatnagar
Monika Krezalek
Mónica Contreras
Mónica Medina
Naseer Sangwan
Nathalie Fenner
Neslihan Tas¸
Nicholas A. Bokulich
Nicole M. Scott
Nicole S. Webster
Noah Fierer
Noriko Okamoto
null null
Nur A. Hasan
Olayinka Osuolale
Olivia U. Mason
Pamela Weisenhorn
Paola Piombino
Paola Vitaglione
Paul Munroe
Peter D. Steinberg
Peter Golyshin
Peter Larsen
Peter O. Dunn
Peter Petraitis
Pierre Liancourt
Qikun Zhang
Qiyun Zhu
Rachael M. Morgan-Kiss
Ravi Ranjan
Rebecca J. Safran
Rebecca Vega Thurber
Regina Lamendella
Rick L. Stevens
Rita L. Seger
Rita R. Colwell
Rob Knight
Robert E. Espinoza
Robert G. Clark
Robert J. Prill
Robin B. Gasser
Robin Dowell
Roger Karlsson
Ross Stephen Hall
Russell D. Dawson
Ryan McMinds
Ryan T. Gill
S. Craig Cary
Safiyh Taghavi
Sara Sjöling
Sarah E. Daly
Sarah L. O’Brien
Sarah M. Owens
Sarah-Jane Haig
Se Jin Song
Sean M. Gibbons
Selena Marie Rodriguezl
Seth Kauppinen
Shane R. Haydon
Shaun Nielsen
Shi Wang
Siavash Mirarab
Simon Creer
Simon Lax
Sophie Weiss
Stefan Hulth
Stefan Janssen
Stefano Mocali
Stephanie D. Jurburg
Stephen A. Wood
Stephen B. Pointing
Stephen Joseph
Steve Simmons
Steven J. Hallam
Subramanya Rao
Susan R. Whitehead
Suzanne J. Kennedy
Tao Wang
Tim Urich
Tom Weaver
Tomasz Kosciolek
Torsten Thomas
Trevor C. Charles
Tugrul Giray
Ulf Riebesell
Valerie McKenzie
Vanessa Ezenwa
Vanessa Hale
Vera Tai
Vincenzo Fogliano
Virginia Sanz
Walter P. MacCormack
Wayne Roundstone
Wenju Liang
William A. Walters
William Brazelton
William Van Treuren
Wyatt Oswald
Yadira Ortiz Castellano
Yeqin Yang
Yingying Ni
Yongqin Liu
Yoshiki Vázquez-Baeza
Yu Shi
Zhenjiang Zech Xu
Publication venue
Publication date: 01/01/2017
Field of study

Our growing awareness of the microbial world's importance and diversity contrasts starkly with our limited understanding of its fundamental structure. Despite recent advances in DNA sequencing, a lack of standardized protocols and common analytical frameworks impedes comparisons among studies, hindering the development of global inferences about microbial life on Earth. Here we present a meta-analysis of microbial community samples collected by hundreds of researchers for the Earth Microbiome Project. Coordinated protocols and new analytical methods, particularly the use of exact sequences instead of clustered operational taxonomic units, enable bacterial and archaeal ribosomal RNA gene sequences to be followed across multiple studies and allow us to explore patterns of diversity at an unprecedented scale. The result is both a reference database giving global context to DNA sequence data and a framework for incorporating data from future studies, fostering increasingly complete characterization of Earth's microbial diversity.Peer reviewe

LAReferencia - Red Federada de Repositorios Institucionales de Publicaciones Científicas Latinoamericanas

University of Groningen

Plymouth Marine Science Electronic Archive (PlyMSEA)

Warwick Research Archives Portal Repository

UNSWorks

USC Research Bank - University of the Sunshine Coast

Aquila Digital Community

Proceedings - University of Groningen

CONICET Digital

Publications at Bielefeld University

Bangor University Research Portal

University of Melbourne Institutional Repository

OceanRep

E-space: Manchester Metropolitan University's Research Repository

Louisiana State University

EUSpace

Helsingin yliopiston digitaalinen arkisto

HAL-CIRAD

Repository for Publications and Research Data

Archivio della ricerca - Università degli studi di Napoli Federico II

Crossref

ARTS repository - University of Groningen

eScholarship - University of California

University of East Anglia digital repository

Dissertations of the University of Groningen

A communal catalogue reveals Earth’s multiscale microbial diversity

Author: Thompson L R
Sanders Jon G
McDonald Daniel
Amir Amnon
Ladau Joshua
Locey Kenneth J
Prill Robert J
Tripathi Anupriya
Gibbons Sean M
Ackermann Gail
Navas-Molina Jose A
Janssen Stefan
Kopylova Evguenia
Vázquez-Baeza Yoshiki
González Antonio
Morton James T
Mirarab Siavash
Zech Xu Zhenjiang
Jiang Lingjing
Haroon Mohamed F
Kanbar Jad
Zhu Qiyun
Jin Song Se
Kosciolek Tomasz
Bokulich Nicholas A
Lefler Joshua
Brislawn Colin J
Humphrey Gregory
Owens Sarah M
Hampton-Marcell Jarrad
Berg-Lyons Donna
McKenzie Valerie
Fierer Noah
Fuhrman Jed A
Clauset Aaron
Stevens Rick L
Shade Ashley
Pollard Katherine S
Goodwin Kelly D
Jansson Janet K
Gilbert Jack A
Knight Rob
Rivera Jose L Agosto
Al-Moosawi Lisa
Alverdy John
Amato Katherine R
Andras Jason
Angenent Largus T
Antonopoulos Dionysios A
Apprill Amy
Armitage David
Ballantine Kate
Bárta Jirˇí
Baum Julia K
Berry Allison
Bhatnagar Ashish
Bhatnagar Monica
Biddle Jennifer F
Bittner Lucie
Boldgiv Bazartseren
Bottos Eric
Boyer Donal M
Braun Josephine
Brazelton William
Brearley Francis Q
Campbell Alexandra H
Caporaso J Gregory
Cardona Cesar
Carroll JoLynn
Cary S Craig
Casper Brenda B
Charles Trevor C
Chu Haiyan
Claar Danielle C
Clark Robert G
Clayton Jonathan B
Clemente Jose C
Cochran Alyssa
Coleman Maureen L
Collins Gavin
Colwell Rita R
Contreras Mónica
Crary Benjamin B
Creer Simon
Cristol Daniel A
Crump Byron C
Cui Duoying
Daly Sarah E
Davalos Liliana
Dawson Russell D
Defazio Jennifer
Delsuc Frédéric
Dionisi Hebe M
Dominguez-Bello Maria Gloria
Dowell Robin
Dubinsky Eric A
Dunn Peter O
Ercolini Danilo
Espinoza Robert E
Ezenwa Vanessa
Fenner Nathalie
Findlay Helen S
Fleming Irma D
Fogliano Vincenzo
Forsman Anna
Freeman Chris
Friedman Elliot S
Galindo Giancarlo
Garcia Liza
Garcia-Amado Maria Alexandra
Garshelis David
Gasser Robin B
Gerdts Gunnar
Gibson Molly K
Gifford Isaac
Gill Ryan T
Giray Tugrul
Gittel Antje
Golyshin Peter
Gong Donglai
Grossart Hans-Peter
Guyton Kristina
Haig Sarah-Jane
Hale Vanessa
Hall Ross Stephen
Hallam Steven J
Handley Kim M
Hasan Nur A
Haydon Shane R
Hickman Jonathan E
Hidalgo Glida
Hofmockel Kirsten S
Hooker Jeff
Hulth Stefan
Hultman Jenni
Hyde Embriette
Ibáñez-Álamo Juan Diego
Jastrow Julie D
Jex Aaron R
Johnson L Scott
Johnston Eric R
Joseph Stephen
Jurburg Stephanie D
Jurelevicius Diogo
Karlsson Anders
Karlsson Roger
Kauppinen Seth
Kellogg Colleen T E
Kennedy Suzanne J
Kerkhof Lee J
King Gary M
Kling George W
Koehler Anson V
Krezalek Monika
Kueneman Jordan
Lamendella Regina
Landon Emily M
Lane-deGraaf Kelly
LaRoche Julie
Larsen Peter
Laverock Bonnie
Lax Simon
Lentino Miguel
Levin Iris I
Liancourt Pierre
Liang Wenju
Linz Alexandra M
Lipson David A
Liu Yongqin
Lladser Manuel E
Lozada Mariana
Spirito Catherine M
MacCormack Walter P
MacRae-Crerar Aurora
Magris Magda
Martín-Platero Antonio M
Martín-Vivaldi Manuel
Martínez L Margarita
Martínez-Bueno Manuel
Marzinelli Ezequiel M
Mason Olivia U
Mayer Gregory D
McDevitt-Irwin Jamie M
McDonald James E
McGuire Krista L
McMahon Katherine D
McMinds Ryan
Medina Mónica
Mendelson Joseph R
Metcalf Jessica L
Meyer Folker
Michelangeli Fabian
Miller Kim
Mills David A
Minich Jeremiah
Mocali Stefano
Moitinho-Silva Lucas
Moore Anni
Morgan-Kiss Rachael M
Munroe Paul
Myrold David
Neufeld Josh D
Ni Yingying
Nicol Graeme W
Nielsen Shaun
Nissimov Jozef I
Niu Kefeng
Nolan Matthew J
Noyce Karen
O’Brien Sarah L
Okamoto Noriko
Orlando Ludovic
Castellano Yadira Ortiz
Osuolale Olayinka
Oswald Wyatt
Parnell Jacob
Peralta-Sánchez
Juan M
Petraitis Peter
Pfister Catherine
Pilon-Smits Elizabeth
Piombino Paola
Pointing Stephen B
Pollock F Joseph
Potter Caitlin
Prithiviraj Bharath
Quince Christopher
Rani Asha
Ranjan Ravi
Rao Subramanya
Rees Andrew P
Richardson Miles
Riebesell Ulf
Robinson Carol
Rockne Karl J
Rodriguezl Selena Marie
Rohwer Forest
Roundstone Wayne
Safran Rebecca J
Sangwan Naseer
Sanz Virginia
Schrenk Matthew
Schrenzel Mark D
Scott Nicole M
Seger Rita L
Seguin-Orlando Andaine
Seldin Lucy
Seyler Lauren M
Shakhsheer Baddr
Sheets Gabriela M
Shen Congcong
Shi Yu
Shin Hakdong
Shogan Benjamin D
Shutler Dave
Siegel Jeffrey
Simmons Steve
Sjöling Sara
Smith Daniel P
Soler Juan J
Sperling Martin
Steinberg Peter D
Stephens Brent
Stevens Melita A
Taghavi Safiyh
Tai Vera
Tait Karen
Tan Chia L
Tas Neslihan
Taylor D Lee
Thomas Torsten
Timling Ina
Turner Benjamin L
Urich Tim
Ursell Luke K
van der Lelie Daniel
Van Treuren William
van Zwieten Lukas
Vargas-Robles Daniela
Thurber Rebecca Vega
Vitaglione Paola
Walker Donald A
Walters William A
Wang Shi
Wang Tao
Weaver Tom
Webster Nicole S
Wehrle Beck
Weisenhorn Pamela
Weiss Sophie
Werner Jeffrey J
West Kristin
Whitehead Andrew
Whitehead Susan R
Whittingham Linda A
Willerslev Eske
Williams Allison E
Wood Stephen A
Woodhams Douglas C
Yang Yeqin
Zaneveld Jesse
Zarraonaindia Iratxe
Zhang Qikun
Zhao Hongxia
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 22/09/2000
Field of study

Our growing awareness of the microbial world’s importance and diversity contrasts starkly with our limited understanding of its fundamental structure. Despite recent advances in DNA sequencing, a lack of standardized protocols and common analytical frameworks impedes comparisons among studies, hindering the development of global inferences about microbial life on Earth. Here we present a meta-analysis of microbial community samples collected by hundreds of researchers for the Earth Microbiome Project. Coordinated protocols and new analytical methods, particularly the use of exact sequences instead of clustered operational taxonomic units, enable bacterial and archaeal ribosomal RNA gene sequences to be followed across multiple studies and allow us to explore patterns of diversity at an unprecedented scale. The result is both a reference database giving global context to DNA sequence data and a framework for incorporating data from future studies, fostering increasingly complete characterization of Earth’s microbial diversity

Convalescent plasma in patients admitted to hospital with COVID-19 (RECOVERY): a randomised controlled, open-label, platform trial

Author: Abani Obbina
Abbas Ali
Abbas Fatima
Abbas Mustafa
Abbasi Sadia
Abbass Hakam
Abbott Alfie
Abdallah Nabeel
Abdelaziz Ashraf
Abdelfattah Mohamed
Abdelqader Bushra
Abdo David
Abdul Rasheed Althaf
Abdul Basir
Abdul-Kadir Rezan
Abdul-Raheem Rasheed
Abdulakeem Ajibode
Abdulle Amina
Abdulmumeen Abdulfatahi
Abdulshukkoor Niyaz
Abdusamad Kula
Abed El Khaleq Yazeed
Abedalla Mai
Abeer Ul Amna Abeer Ul Amna
Abernethy Katrina
Abo-Leyah Hani
Aboaba Adebanke
Abou-Haggar Ahmed
Abouibrahim Mahmoud
Abraham Miriam
Abraham Tizzy
Abraheem Abraheem
Abrams Judith
Abu Hyacinth-John
Abu-Arafeh Ahmed
Abubacker Syed M
Abung Akata
Aceampong Yaa
Achara Amaka
Acharya Devikumar
Acheampong Sarah
Acheson Janet
Acosta Andres
Acton Catherine
Adabie-Ankrah Jacqueline
Adair Sara
Adam Fiona
Adam Matthew
Adamali Huzaifa
Adams Carol
Adams Charlotte
Adams Kate
Adams Lisa
Adams Richard
Adams Tim
Adcock Kirsty
Addai Jemaimah
Adebiyi Ade
Adegoke Ken
Adell Vicki
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Butler Peter
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Publication venue: 'Elsevier BV'
Publication date: 13/02/2021
Field of study

SummaryBackground Azithromycin has been proposed as a treatment for COVID-19 on the basis of its immunomodulatoryactions. We aimed to evaluate the safety and efficacy of azithromycin in patients admitted to hospital with COVID-19.Methods In this randomised, controlled, open-label, adaptive platform trial (Randomised Evaluation of COVID-19Therapy [RECOVERY]), several possible treatments were compared with usual care in patients admitted to hospitalwith COVID-19 in the UK. The trial is underway at 176 hospitals in the UK. Eligible and consenting patients wererandomly allocated to either usual standard of care alone or usual standard of care plus azithromycin 500 mg once perday by mouth or intravenously for 10 days or until discharge (or allocation to one of the other RECOVERY treatmentgroups). Patients were assigned via web-based simple (unstratified) randomisation with allocation concealment andwere twice as likely to be randomly assigned to usual care than to any of the active treatment groups. Participants andlocal study staff were not masked to the allocated treatment, but all others involved in the trial were masked to theoutcome data during the trial. The primary outcome was 28-day all-cause mortality, assessed in the intention-to-treatpopulation. The trial is registered with ISRCTN, 50189673, and ClinicalTrials.gov, NCT04381936.Findings Between April 7 and Nov 27, 2020, of 16 442 patients enrolled in the RECOVERY trial, 9433 (57%) wereeligible and 7763 were included in the assessment of azithromycin. The mean age of these study participants was65·3 years (SD 15·7) and approximately a third were women (2944 [38%] of 7763). 2582 patients were randomlyallocated to receive azithromycin and 5181 patients were randomly allocated to usual care alone. Overall,561 (22%) patients allocated to azithromycin and 1162 (22%) patients allocated to usual care died within 28 days(rate ratio 0·97, 95% CI 0·87–1·07; p=0·50). No significant difference was seen in duration of hospital stay (median10 days [IQR 5 to >28] vs 11 days [5 to >28]) or the proportion of patients discharged from hospital alive within 28 days(rate ratio 1·04, 95% CI 0·98–1·10; p=0·19). Among those not on invasive mechanical ventilation at baseline, nosignificant difference was seen in the proportion meeting the composite endpoint of invasive mechanical ventilationor death (risk ratio 0·95, 95% CI 0·87–1·03; p=0·24).Interpretation In patients admitted to hospital with COVID-19, azithromycin did not improve survival or otherprespecified clinical outcomes. Azithromycin use in patients admitted to hospital with COVID-19 should be restrictedto patients in whom there is a clear antimicrobial indication

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