Search CORE

7 research outputs found

Pervasive gaps in Amazonian ecological research

Author: Aguiar D.P.P.D.
Aguiar H.J.A.C.D.
Albernaz A.L.
Albuquerque B.W.
Aleixo A.
Alencar L.
Almeida D.D.F.
Almeida M.
Almeida M.R.N.
Almeida R.P.S.
Almeida W.R.D.
Alvarado S.T.
Alverga P.P.D.P.
Alves da Rosa C.
Alves-Martins F.
Alves-Martins F.
Amado L.L.
Amaral D.D.D.
Anacléto M.J.P.
Andrade A.L.
Andrade R.B.D.
Andrade-Silva J.
Andresen E.
Andretti C.B.
Andriolo A.
André T.
Anjos D.V.
Aragão L.
Aragão L.
Arantes C.C.
Arenas E.R.C.
Arrolho S.
Arruda F.V.D.
Assis R.L.D.
Azara L.
Azevêdo C.A.S.D.
Baccaro F.B.
Baccaro F.B.
Baider C.
Baker T.R.
Barbosa E.M.
Barbosa J.F.
Barbosa R.I.
Barbosa T.A.P.
Barlow J.
Barlow J.
Barni P.E.
Barros G.G.
Barroso J.G.
Barthem R.
Bastos D.
Bastos R.C.
Batista A.P.B.
Begot T.O.
Beiroz W.
Benetti C.J.
Benone N.L.
Bentos T.V.
Berenguer E.
Berenguer E.
Bispo P.C.
Boldrini R.
Bonates L.C.D.M.
Borba G.C.
Borges A.
Borges L.H.M.
Borges S.H.
Braga D.D.L.
Braga R.B.
Brando P.
Brasil L.S.
Brejão G.L.
Brito M.T.D.S.
Brito T.D.F.
Brocardo C.R.
Brown I.F.
Brulinger L.F.B.
Bueno A.S.
Cabeceira F.G.
Cabette H.S.R.
Cabral G.S.
Cajaiba R.L.
Callisto M.
Calor A.R.
Calvão L.B.
Camargo J.L.
Camargo P.B.D.
Campana D.R.D.S.
Campos N.
Campos-Filho E.M.
Cardoso M.R.
Carim M.D.J.V.
Carmo G.H.P.D.
Carniello M.A.
Carpanedo R.D.S.
Carreiras J.
Carvalho F.A.
Carvalho F.G.
Carvalho F.R.D.
Carvalho K.S.
Carvalho L.C.D.S.
Carvalho L.N.
Carvalho R.L.
Carvalho R.L.
Casadei-Ferreira A.
Casatti L.
Castello L.
Castello L.
Castilho C.
Castro A.B.
Castro F.S.D.
Castro W.
Catarino M.
Cavalheiro L.
Cerqueira Silva J.C.
Cerqueira P.V.
Cintra B.B.L.
Cochrane M.A.
Coelho de Souza F.
Coelho L.D.S.
Coletti F.
Cordeiro C.L.
Cornelius C.
Correa A.S.A.S.
Costa Batista M.
Costa D.D.S.
Costa F.R.C.
Costa F.R.C.
Costa J.B.P.
Costa J.G.
Costa M.K.S.
Costa M.M.S.D.
Couceiro S.R.M.
Cravo J.S.
Crema L.C.
Cruz P.V.
Cruz W.J.A.D.
Cunha E.J.R.D.
da Rocha M.
da Silva Guimarães J.R.
da Silva Menger J.
da Silva E.R.
da Silva G.C.
da Silva J.S.
da Silva K.D.
da Silva L.F.
da Silva M.J.
da Silva R.R.
Daly D.
Damasco G.
Davis B.
de Abreu J.C.
de Albuquerque E.Z.
de Brito J.G.
de Faria Falcão J.C.
de Lima Alves A.
de Matos L.S.
de Oliveira Melo L.
de Resende B.O.
de Sousa Gorayeb I.
de Toledo J.J.
Delabie J.H.C.
Demarchi L.O.
Desidério G.R.
Deus C.P.D.
Dias M.S.
do Vale J.D.
Domingues T.F.
Doria C.R.D.C.
dos Anjos M.R.
Douglas D.
Duarte Ritter C.
Dumas L.L.
Durgante F.
Dutra D.B.D.S.
Dutra S.L.
Dáttilo W.
d’Horta F.M.
e Gomes J.O.
e Pérez R.E.P.
Edwards D.P.
Elias F.
Elias F.
Emilio T.
Esposito M.C.
Espírito Santo N.B.
Espírito-Santo H.M.V.
Fadini R.F.
Fares A.L.
Faria A.P.J.
Farias E.D.S.
Feitosa R.M.
Feitosa Y.
Feldpausch T.R.
Fernandes I.
Fernandes I.O.
Ferreira A.B.
Ferreira J.
Ferreira J.
Ferreira L.V.
Ferreira N.
Ferreira-Ferreira J.
Firmino V.
Flores B.M.
Florêncio F.P.
Fontenele L.
França F.
França F.M.
Freitas C.
Freitas M.A.B.
Freitas M.G.
Félix N.S.
Galuch A.V.
Gama Neto J.D.L.
Gastauer M.
Geber Filho A.N.D.S.
Ghidini A.R.
Giacomin L.
Giarrizzo T.
Giehl N.F.D.S.
Godoy B.S.
Gomes V.H.F.
Gontijo A.
Gonçalves I.C.
Graça P.M.D.A.
Griffiths H.
Gris D.
Gualberto C.G.
Guedes M.C.
Guedes M.L.
Guedes M.L.
Guerrero J.E.B.
Guilherme E.
Guimaraes A.F.
Guimarães D.P.
Görgens E.B.
Hamada N.
Haugaasen T.
Hawes J.E.
Hercos A.
Hilário R.R.
Holanda de Andrade A.L.R.
Holmgren M.
Householder E.
i Silva P.G.D.
Irume M.V.
Isaac V.
Isaac V.
Ivanauskas N.M.
Izzo T.J.
Jakovac C.C.
Jardim G.A.
Juen L.
Juen L.
Junqueira A.B.
Korasaki V.
Koroiva R.
Krolow T.K.
Kunz S.H.
Landeiro V.L.
Lanna J.
Laranjeiras T.O.
Lasky J.R.
Lasmar C.
Laurance S.
Laurance W.
Leal C.G.
Leal C.G.
Lees A.C.
Lees A.C.
Leitão R.P.
Levis C.
Leão H.
Ligeiro R.
Lima G.R.
Lima J.
Lima Y.G.D.
Lobato C.M.C.
Lopes A.
Lopes M.A.
Lourenço L.D.S.
Louzada J.
Luize B.G.
Luther D.
Machado T.L.D.S.
Maciel R.
Maciel R.
Magalhães J.L.L.
Magnusson W.E.
Mahood S.
Maia L.F.
Maldaner M.E.
Malhi Y.
Manzatto A.G.
Maracahipes L.
Maracahipes-Santos L.
Mariano R.
Marimon B.S.
Marimon-Junior B.H.
Marques E.E.
Marsh C.J.
Martins M.F.D.O.
Martins M.P.
Martins R.T.
Massam M.R.
Matavelli R.
Maximiano M.F.D.A.
Mazzei L.
Medeiros H.
Medeiros M.B.D.
Medeiros N.
Melgaço K.
Melinski R.D.
Melo Lima D.V.
Melo A.W.F.D.
Melo B.S.B.D.
Melo G.D.C.D.
Mendes Aguiar J.J.
Mendes K.R.
Mendes R.N.G.
Mendes T.P.
Mendonça F.P.
Menezes A.S.O.D.
Mestre L.A.M.
Metcalf O.C.
Michelan T.S.
Miguel T.B.
Milheiras S.
Milliken W.
Miranda I.P.D.A.
Miranda P.N.
Montag L.F.D.A.
Monteiro Jr. C.D.S.
Monteiro M.G.T.
Morandi P.S.
Morato E.F.
Moreira F.F.F.
Mormul R.P.
Mortati A.F.
Moser P.
Moura M.R.
Moura M.R.
Muelbert A.E.
Muñoz Gutiérrez J.A.
Naka L.N.
Nascimento H.E.M.
Nascimento M.T.
Nascimento R.O.
Nascimento R.O.
Navarro Paolucci L.
Nelson B.
Nessimian J.L.
Neto F.V.
Nichols E.
Nienow S.
Nogueira D.S.
Nonato F.A.D.S.
Noriega J.A.
Noronha J.C.
Novo E.M.M.D.L.
Nunes C.A.
Nunes C.A.
Nunes L.G.D.O.
o Santos M.P.D.
Obermuller F.A.
Oliveira Pes A.M.
Oliveira A.A.D.
Oliveira A.B.D.S.D.
Oliveira C.P.D.
Oliveira E.A.D.
Oliveira F.F.D.
Oliveira J.M.B.
Oliveira M.A.D.
Oliveira M.V.N.D.
Oliveira R.L.C.D.
Oliveira S.A.V.D.
Oliveira V.C.D.
Oliveira V.H.F.
Oliveira W.L.D.
Olivo Neto A.M.
Pansonato M.P.
Passos M.I.S.
Paula W.S.D.
Pauletto D.
Pedroza D.
Peixoto U.
Penagos C.C.M.
Perdiz R.D.O.
Pereira J.L.D.S.
Peres C.A.
Peruquetti P.S.F.
Phillips O.L.
Phillips O.L.
Piedade A.R.D.
Piedade M.T.F.
Pombo M.M.
Pompeu P.D.S.
Pontes-Lopes A.
Pozzobom U.M.
Prado L.P.D.
Prance G.T.
Pringle E.G.
Prist P.
Prudente B.D.S.
Puker A.
Pérez-Mayorga M.A.
Quaresma A.
Queiroz A.C.M.
Queiroz H.L.D.
r Costa Neto S.V.D.
Raseira M.B.
Rechetelo J.
Reis F.
Reis L.P.
Resende A.F.
Resende A.F.
Revilla J.D.C.
Ribas C.R.
Ribeiro J.M.F.
Ribeiro R.A.B.
Ribeiro S.C.
Ribeiro S.P.
Ribeiro V.S.
Rodrigues D.D.J.
Rodrigues S.B.
Rodrigues T.H.A.
Roque F.D.O.
Rosa D.C.P.
Rosalino L.M.D.C.
Rousseau G.X.
Ruschel A.
Rutt C.L.
s de Lima R.B.
Salcedo A.K.M.
Sales F.M.D.S.
Salles F.F.
Salomão R.P.
Salomão R.P.
Santana E.C.C.D.
Santana F.D.
Santiago W.T.V.
Santos Ferreira V.R.
Santos Neto C.R.D.
Santos A.P.M.D.
Santos B.B.
Santos C.A.D.
Santos C.R.M.D.
Santos D.C.D.
Santos E.A.D.
Santos I.C.S.
Santos J.C.
Santos T.F.D.
Sarmento P.S.D.M.
Schietti J.
Schietti J.
Schmidt F.A.
Schmidt F.A.
Schwartz G.
Schöngart J.
Scudeller V.V.
Shimabukuro Y.E.
Shimano Y.
Shutt J.
Shutt J.
Silva Brito J.
Silva C.A.
Silva C.V.J.
Silva D.A.S.D.
Silva D.R.D.
Silva F.A.B.
Silva J.O.D.A.
Silva O.G.M.D.
Silva R.D.C.
Silva R.D.S.A.D.
Silva R.J.D.
Silva S.S.D.
Silva T.S.F.
Silva V.D.N.G.
Silva W.C.D.
Silva W.F.M.D.
Silvano R.A.M.
Silveira J.M.
Silveira J.M.
Silveira L.F.
Silveira M.
Silveira M.A.P.D.A.
Silvério D.V.
Simon M.F.
Siqueira E.L.S.D.
Solar R.
Sousa S.A.D.
Sousa T.
Souto P.
Souza F.K.S.D.
Souza J.L.P.D.
Souza M.F.D.
Souza M.R.D.
Souza P.
Stegmann L.
Stegmann L.
Storck-Tonon D.
Stropp J.
Targhetta N.
ter Steege H.
ter Steege H.
Todeschini F.
Triana S.P.
Uehara-Prado M.
van den Berg E.
Vasconcelos H.L.
Vaz-de-Mello F.
Vaz-de-Mello F.
Vedovato L.B.
Venticinque E.M.
Venticinque E.M.
Veras D.S.
Vicente R.E.
Vicentini A.
Vidal E.
Vieira D.L.M.
Vieira I.C.G.
Vieira I.C.G.
Vieira L.
Vieira S.A.
Villa B.
Vital M.J.S.
Vulinec K.
Wilker I.
Williamson B.
Wittmann F.
Wolfe J.
Yamamoto K.C.
Zanetti R.
Zanzini A.C.D.S.
Zanzini L.P.
Zuanon J.
Zuanon J.
Publication venue: Elsevier
Publication date: 21/08/2023
Field of study

Biodiversity loss is one of the main challenges of our time, and attempts to address it require a clear understanding of how ecological communities respond to environmental change across time and space. While the increasing availability of global databases on ecological communities has advanced our knowledge of biodiversity sensitivity to environmental changes, vast areas of the tropics remain understudied. In the American tropics, Amazonia stands out as the world's most diverse rainforest and the primary source of Neotropical biodiversity, but it remains among the least known forests in America and is often underrepresented in biodiversity databases. To worsen this situation, human-induced modifications may eliminate pieces of the Amazon's biodiversity puzzle before we can use them to understand how ecological communities are responding. To increase generalization and applicability of biodiversity knowledge, it is thus crucial to reduce biases in ecological research, particularly in regions projected to face the most pronounced environmental changes. We integrate ecological community metadata of 7,694 sampling sites for multiple organism groups in a machine learning model framework to map the research probability across the Brazilian Amazonia, while identifying the region's vulnerability to environmental change. 15%–18% of the most neglected areas in ecological research are expected to experience severe climate or land use changes by 2050. This means that unless we take immediate action, we will not be able to establish their current status, much less monitor how it is changing and what is being lost

White Rose Research Online

Whole-genome sequencing reveals host factors underlying critical COVID-19

Author: Abd Elghafar M.S.
Abdel-Aziz M.
Abdelrazik M.
Abdollahi H.
Abdullah T.
Abecasis G.R.
Abecasis G.R.
Abedalthagafi M.
Abel L.
Abernathy C.
Abraheem A.
Abul-Husn N.S.
Acquilini D.
Adams C.
Adams E.L.
Adams K.
Adamsara A.
Adanini O.
Adeleye O.
Adra D.
Afilalo J.
Afilalo M.
Afolabi D.
Afrasiabi Z.
Agasou A.
Agrawal S.
Agüero D.
Ahmad N.
Ahmadi S.
Ahmed A.
Ahmed C.
Akeroyd L.
Akhtar M.N.
Akinkugbe O.
Aksentijevich A.
Al Harthi F.
Al Mutairi A.
Al-Afghani H.
Al-Awdah L.
Alaamery M.
Alahmadey Z.Z.
Alaverdian D.
Alavere H.
Albader A.
Albaiceta G.M.
Albakri J.K.
AlBardis H.
Albeladi M.
Albesher N.
Albrich W.
AlDhawi N.
Aldridge J.
Aleagha A.E.
Alexander P.
Alfonso J.
Alghamdi B.
Alghamdi J.
Ali A.
Ali A.
Ali I.A.M.
Ali S.
Aliannejad R.
Aljawini N.
AlJohani S.
Alkwai S.
Allan A.
Allan E.
Allan J.
Alldis Z.
Allen L.
Allen M.
Allen S.
Allibone S.
Allison K.S.
Allos R.
Almaden-Boyle C.
AlMalik A.
Almalki F.
Almohammed I.
Almutairi M.
Alotaibi S.
Alowayn A.M.
Alqahtani S.
Alqubaishi F.
Alrashed M.
Alshareef A.
Alsolm E.
Alswailm M.
Altabaibeh A.
Alvaro A.
AlZahrani D.
Amin V.
Amirsavadkouhi A.
Amitrano S.
Anastasescu E.
Anderson F.
Anderson J.
Anderson M.
Anderson P.
Anderson S.
Anderson S.
Anderson T.
Andolfo I.
Andretta F.
Andreucci E.
Andrew A.
Andrew B.
Andrew G.
Andrews E.
Andrews S.J.
Anedda F.
Anemoli V.
Annis A.
Antcliffe D.
Antinori A.
Antoni M.D.
Anumakonda V.
Apetri E.
Aquino M.
Arabi Y.M.
Aravindan L.
Arbane G.
Archer K.
Arden T.
Arias S.S.
Arif S.
Armstrong J.
Armstrong L.
Armstrong R.
Arning N.
Arnold S.
Arranz M.J.
Arribas E.
Artuso R.
Arumugam P.
Arumugam P.
Ascolillo S.
Ashraf S.
Ashton L.
Aslibekyan S.
Astin-Chamberlain R.
Atkinson E.G.
Attwood B.
Aucella F.
Auld D.
Auld F.
Austin K.
Austin P.
Auton A.
Ayers A.
Azarzar S.
Bachetti T.
Baikady R.R.
Baillie J.K.
Baillie J.K.
Baillie J.K.
Baines B.
Baines D.
Baines K.
Baird Y.
Bakthavatsalam D.
Balaconis M.K.
Baldassarri M.
Ball C.A.
Baltzell A.H.
Bamford A.
Bamford P.
Banach D.
Bancroft H.
Band G.
Bandini M.
Bandla N.
Bano S.
Baptista D.
Barakeh D.
Baras A.
Baras A.
Baratti S.
Barber R.
Barberis L.
Barberis L.
Barbieri C.
Barclay L.
Bargagli E.
Barhoush E.
Barker J.
Barnes K.C.
Baroni S.
Barrett F.
Barron A.
Barry P.
Bartels M.
Bartley S.
Baruah R.
Bashyal A.
Basikolo C.
Bassetti M.
Bastion V.
Bates H.
Bates M.
Batini C.
Battle C.
Bauchmuller K.
Baxter N.
Baya N.
Bayo L.-A.
Beadle J.
Bean S.
Beaumont K.
Beavis S.
Beck A.
Beckmann N.D.
Bedini J.L.
Bee C.E.
Beech E.
Beech V.
Beekes M.
Beesley K.
Begg C.
Beguin Y.
Behan T.
Beith C.M.
Belagodu Z.
Belbin G.M.
Belfield H.
Belhaj Y.
Beligni G.
Belisle A.
Bell D.
Bell G.
Bell M.
Bell S.
Bellamy M.
Belli M.A.
Bellini A.
Bellwood R.
Below J.
Bemand T.
Benetti E.
Benham L.
Bennett D.
Bennett S.
Bentley D.
Bentley M.
Benyon S.
Beranova E.
Bercades G.
Bergantini L.
Bergomi P.
Berkowitz N.
Bernardo D.
Bevan E.
Bewley J.
Bhatia N.
Bhatterjee R.
Bhuie P.
Bi R.
Bianchi F.
Bibert S.
Bibi F.
Biddle J.
Biggs H.
Birch J.
Birch J.
Birch S.
Birchall K.
Birchall K.
Bird S.
Birkinshaw I.
Birt M.
Biscarini F.
Black E.
Black K.
Blackledge B.
Blackledge B.
Blackman H.
Blakemore H.
Blay N.
Blow S.
Blunt M.
Board S.
Bochud P.-Y.
Bociek A.
Boezen M.
Boillat N.
Bokhari M.
Bolton M.
Bolton R.
Bonner S.
Booker L.
Borislavova B.
Borra C.
Botello A.
Botfield L.
Bottà G.
Bouab M.
Bough L.
Boughton A.P.
Bowes A.
Bowles R.
Boyle P.
Boyle R.
Boz C.
Bradford Y.
Bradley C.
Bradley P.
Bradley-Potts J.
Bradshaw Z.
Brady A.
Brady M.
Brady R.
Brandwood C.
Branney D.
Brantwood C.
Brassard N.
Brayne A.
Brealey D.
Brealey D.
Bremmer P.
Brenner B.
Bretherick A.D.
Brett M.
Brett S.
Brickell K.
Bridgett V.
Brimfield L.
Brinkworth E.
Briton K.
Britvan B.
Bromley M.
Brooke H.
Brooks S.
Brown A.
Brown A.
Brown A.
Brown E.
Brown J.
Bruce M.
Brumpton B.M.
Bruno R.
Brunton M.
Bruttini M.
Bryant J.
Bryant S.
Buckley C.
Buckley S.
Bunni L.
Burda D.
Buring J.E.
Burn I.
Burnett C.
Burns K.
Burt K.
Burtenshaw A.
Burton M.
Busani S.
Bussotti M.
Butcher D.
Butler A.
Butler J.
Butler S.
Butler-Laporte G.
Butterworth A.S.
Butterworth-Cowin N.
Button H.
Buxbaum J.D.
Cabrelli L.
Cagova L.
Caldarelli G.P.
Callaghan M.
Callier S.
Cameli P.
Campbell A.
Campbell A.
Campbell H.
Campbell R.
Campbell R.
Campbell S.
Campos S.
Camsooksai J.
Canaccini A.
Cantarini L.
Cantor M.N.
Capasso M.
Capitani K.
Cappelli S.
Capps N.
Carbral-Ortega L.
Carella M.
Carey D.J.
Carmody M.
Carmody S.
Carnahan M.
Carreras A.
Carriero M.L.
Carter A.
Carter D.
Carter E.
Carter J.
Carter S.
Carungcong J.
Casey M.
Castaño-Vinyals G.
Castelli F.
Castle K.
Castori M.
Caswell M.
Catena E.
Caterson J.
Cathcart S.
Catlow L.
Caulfield M.J.
Caulfield M.J.
Cavazza A.
Cawley K.
Cawthron K.
Ceri S.
Chablani M.
Chadbourn I.
Chamnanphon M.
Chan G.
Chan G.
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Zheng C.
Zhou W.
Zitter L.
Zlatopolsky M.
Zongo O.
Zucchi P.
Zyndorf M.
Zöllner S.
Åsvold B.O.
Publication venue: Springer Science and Business Media LLC
Publication date: 07/07/2022
Field of study

Critical COVID-19 is caused by immune-mediated inflammatory lung injury. Host genetic variation influences the development of illness requiring critical care1 or hospitalization2,3,4 after infection with SARS-CoV-2. The GenOMICC (Genetics of Mortality in Critical Care) study enables the comparison of genomes from individuals who are critically ill with those of population controls to find underlying disease mechanisms. Here we use whole-genome sequencing in 7,491 critically ill individuals compared with 48,400 controls to discover and replicate 23 independent variants that significantly predispose to critical COVID-19. We identify 16 new independent associations, including variants within genes that are involved in interferon signalling (IL10RB and PLSCR1), leucocyte differentiation (BCL11A) and blood-type antigen secretor status (FUT2). Using transcriptome-wide association and colocalization to infer the effect of gene expression on disease severity, we find evidence that implicates multiple genes—including reduced expression of a membrane flippase (ATP11A), and increased expression of a mucin (MUC1)—in critical disease. Mendelian randomization provides evidence in support of causal roles for myeloid cell adhesion molecules (SELE, ICAM5 and CD209) and the coagulation factor F8, all of which are potentially druggable targets. Our results are broadly consistent with a multi-component model of COVID-19 pathophysiology, in which at least two distinct mechanisms can predispose to life-threatening disease: failure to control viral replication; or an enhanced tendency towards pulmonary inflammation and intravascular coagulation. We show that comparison between cases of critical illness and population controls is highly efficient for the detection of therapeutically relevant mechanisms of disease

White Rose Research Online

Infarto Intestinale

Author: F.G. MAZZEI
GRASSI R
L. VOLTERRANI
M.A. MAZZEI
Publication venue
Publication date
Field of study

Archivio Istituzionale della Ricerca - Università degli Studi della Campania "Luigi Vanvitelli"

Preoperative MDCT assessment for lymphatic gastric cancer spread in the era of neoadjuvant treatment

Author: A.V. Parrinello
C. Pozzessere
F.G. Mazzei
L. Volterrani
M.A. Mazzei
N. Cioffi Squitieri
P. Mercuri
S. Guerrini
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2013
Field of study

Purpose: To validate the feasibility and accuracy of MDCT for the preoperative lymphatic gastric cancer spread. Material and Methods: 104 patients with primary gastric cancer (mean age 68.67 years) who consecutively underwent MDCT scan followed by radical surgical treatment were prospectively evaluated. Regional lymph nodes were considered involved when the short-axis diameter was >5mm for the lymph nodes of group 1 and >8mm for the lymph nodes of other group according to the Japanese Classification of Gastric Carcinoma. All patients underwent a radical lymph node dissection (D2-D3) according to Japanese Research Society for Gastric Cancer (JRSGC) guidelines. The removal of nodal stations was always preceded by Indian-ink injection in the lesser and greater curvature of the stomach; after operation, single lymph nodes were retrieved on the fresh specimen by the surgeon, and classified in JRSGC nodal stations for pathological examination. Results: Lymph node invasion was found in 85 cases (81.73%) with a MDCT sensitivity and specificity of 89% and 85%, respectively. The rate of understaging was higher (15%) than that of overstaging (8%). Lymph node status of early forms was correctly staged in all cases. Furthermore, all N3 cases were correctly staged. Conclusion: MDCT is a useful technique in the preoperative assessment of lymphatic cancer spread and could have a positive impact in clinical decision making in the era of neoadjuvant treatment

Archivio della Ricerca - Università degli Studi di Siena

Light and electron microscopic findings in five cases of cryoglobulinemic glomerulonephritis

Author: A. Lupo
C. Parolini
C.G. Cochrane
D. Cordonnier
D. Golde
D. Mazzei
D.A. Mathison
D.S. Baldwin
F.G. Germuth
G. Mazzucco
G. Monga
G. Previato
G. Riethmuller
G.W. Miller
H. Feiner
H.A. Bogaars
H.H. Zinnemann
J. Spalluto Lo
J.C. Brouet
L. Morel-Maroger
M. Meltzer
M.C. Gelfand
P. Verroust
R.L. Vernier
S. Muller
T. Faraggiana
V. Marinozzi
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/1979
Field of study

Crossref

Light and electron microscopic findings in five cases of cryoglobulinemic glomerulonephritis

Author: A. Lupo
C. Parolini
C.G. Cochrane
D. Cordonnier
D. Golde
D. Mazzei
D.A. Mathison
D.S. Baldwin
F.G. Germuth
G. Mazzucco
G. Monga
G. Previato
G. Riethmuller
G.W. Miller
H. Feiner
H.A. Bogaars
H.H. Zinnemann
J. Spalluto Lo
J.C. Brouet
L. Morel-Maroger
M. Meltzer
M.C. Gelfand
P. Verroust
R.L. Vernier
S. Muller
T. Faraggiana
V. Marinozzi
Publication venue
Publication date: 01/01/1979
Field of study

Renal tissue from five patients with cryoglobulinemia was studied by light and electron microscopy and immunofluorescence. None of the histologic features observed at the light microscopic level seems to be specific for cryoglobulinemia. Electron microscopic investigations have shown very large electron dense deposits in almost every examined lobule in all cases. The deposits displayed two main patterns; a homogeneous texture in two cases and tubular or annular structures in three cases. The patients with typically structured deposits had IgG-IgM cryoglobulinemia (2 cases) or monoclonal IgM cryoglobulinemia (1 case). The presence of IgM in cryoglobulinemia may be the cause of the peculiar structure of the deposits

Crossref

Catalogo dei prodotti della ricerca

Whole-genome sequencing reveals host factors underlying critical COVID-19

Author: Abd Elghafar Mohamed S.
Abdel-Aziz Mahmoud
Abdelrazik Marwa
Abdollahi Hamed
Abdullah T.
Abecasis Goncalo
Abedalthagafi M.
Abel Lynn
Abernathy C.
Abraheem Azmeralde
Abul-Husn Noura S.
Acquilini D.
Adams C.
Adams Emma L.
Adams K.
Adamsara Alireza
Adanini Olurenke
Adeleye O.
Adra D.
Afilalo J.
Afilalo M.
Afolabi D.
Afrasiabi Z.
Agasou A.
Agrawal Shruti
Agüero D.
Ahmad N.
Ahmadi Saeideh
Ahmed A.
Ahmed Cecilia
Akeroyd L.
Akhtar M.N.
Akinkugbe O.
Aksentijevich Alexandra
Al-Afghani H.
Al-Awdah L.
Alaamery M.
Alahmadey Z.Z.
Alaverdian D.
Alavere H.
Albader A.
Albaiceta G.M.
Albakri J.K.
AlBardis H.
Albeladi M.
Albesher N.
Albrich W.
AlDhawi N.
Aldridge J.
Aleagha Afshar Etemadi
Alexander Peter.
Alfonso J.
Alghamdi B.
Alghamdi J.
Ali A.
Ali Altaf
Ali I.A.M.
Ali Syamlan
Aliannejad Rasoul
Aljawini N.
AlJohani S.
Alkwai S.
Allan A.
Allan E.
Allan J.
Alldis Zoe
Allen L.
Allen Meryem
Allen Schvearn
Allibone S.
Allison K.S.
Allos R.
Ally S.M.
AlMalik A.
Almalki F.
Almohammed I.
Almutairi M.
Alotaibi S.
Alowayn A.M.
Alqahtani S.
Alqubaishi F.
Alrashed M.
Alshareef A.
Alsolm E.
Alswailm M.
Altabaibeh A.
Alvaro A.
AlZahrani D.
Amin V.
Amirsavadkouhi Ali
Amitrano Sara
Anastasescu E.
Anderson F.
Anderson J.
Anderson Madeleine
Anderson Peter
Anderson S.
Anderson S.
Anderson T.
Andolfo I.
Andretta F.
Andreucci E.
Andrew Angela
Andrew B.
Andrew Gratrix
Andrews E.
Andrews Shea J.
Anedda F.
Anemoli V.
Annis A.
Antcliffe David
Antinori Andrea
Antoni M.D.
Anumakonda V.
Apetri E.
Aquino Maia
Arabi Y.M.
Aravindan Latha
Arbane Gill
Archer Katie
Arden T.
Arias Sonia Sousa
Arif S.
Armstrong Jacob
Armstrong Lisa
Armstrong Ruth
Arning N.
Arnold Sophie
Arranz María Jesús
Arribas E.
Artuso R.
Arumugam Prabhu
Ascolillo Steven
Ashraf Saima
Ashton L.
Aslibekyan S.
Astin-Chamberlain Raine
Atkinson E.G.
Attwood B.
Aucella F.
Auld D.
Auld F.
Austin Karen
Austin Pauline
Auton A.
Ayers A.
Azarzar S.
Bachetti T.
Baikady R.R.
Baillie John Kenneth
Baines Balvinder
Baines D.
Baines K.
Baird Yolanda
Bakthavatsalam Dhanalakshmi
Balaconis Mary K.
Baldassarri M.
Ball C.A.
Baltzell A.H.
Bamford A.
Bamford Peter
Banach Dorota
Bancroft Hollie
Band G.
Bandini M.
Bandla Nageswar
Bano S.
Baptista David
Barakeh D.
Baras Aris
Baratti S.
Barber R.
Barberis L.
Barbieri C.
Barclay Lucy
Bargagli E.
Barhoush E.
Barker J.
Barnes K.C.
Baroni S.
Barrett F.
Barron A.
Barry P.
Bartels M.
Bartley Shauna
Baruah R.
Bashyal Archana
Basikolo C.
Bassetti M.
Bastion V.
Bates H.
Bates Michelle
Batini Chiara
Battle Ceri
Bauchmuller K.
Baxter N.
Baya N.
Bayo L.A.
Beadle Jane
Bean S.
Beaumont K.
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Publication venue
Publication date: 01/01/2022
Field of study

Altres ajuts: Department of Health and Social Care (DHSC); Illumina; LifeArc; Medical Research Council (MRC); UKRI; Sepsis Research (the Fiona Elizabeth Agnew Trust); the Intensive Care Society, Wellcome Trust Senior Research Fellowship (223164/Z/21/Z); BBSRC Institute Program Support Grant to the Roslin Institute (BBS/E/D/20002172, BBS/E/D/10002070, BBS/E/D/30002275); UKRI grants (MC_PC_20004, MC_PC_19025, MC_PC_1905, MRNO2995X/1); UK Research and Innovation (MC_PC_20029); the Wellcome PhD training fellowship for clinicians (204979/Z/16/Z); the Edinburgh Clinical Academic Track (ECAT) programme; the National Institute for Health Research, the Wellcome Trust; the MRC; Cancer Research UK; the DHSC; NHS England; the Smilow family; the National Center for Advancing Translational Sciences of the National Institutes of Health (CTSA award number UL1TR001878); the Perelman School of Medicine at the University of Pennsylvania; National Institute on Aging (NIA U01AG009740); the National Institute on Aging (RC2 AG036495, RC4 AG039029); the Common Fund of the Office of the Director of the National Institutes of Health; NCI; NHGRI; NHLBI; NIDA; NIMH; NINDS.Critical COVID-19 is caused by immune-mediated inflammatory lung injury. Host genetic variation influences the development of illness requiring critical care or hospitalization after infection with SARS-CoV-2. The GenOMICC (Genetics of Mortality in Critical Care) study enables the comparison of genomes from individuals who are critically ill with those of population controls to find underlying disease mechanisms. Here we use whole-genome sequencing in 7,491 critically ill individuals compared with 48,400 controls to discover and replicate 23 independent variants that significantly predispose to critical COVID-19. We identify 16 new independent associations, including variants within genes that are involved in interferon signalling (IL10RB and PLSCR1), leucocyte differentiation (BCL11A) and blood-type antigen secretor status (FUT2). Using transcriptome-wide association and colocalization to infer the effect of gene expression on disease severity, we find evidence that implicates multiple genes-including reduced expression of a membrane flippase (ATP11A), and increased expression of a mucin (MUC1)-in critical disease. Mendelian randomization provides evidence in support of causal roles for myeloid cell adhesion molecules (SELE, ICAM5 and CD209) and the coagulation factor F8, all of which are potentially druggable targets. Our results are broadly consistent with a multi-component model of COVID-19 pathophysiology, in which at least two distinct mechanisms can predispose to life-threatening disease: failure to control viral replication; or an enhanced tendency towards pulmonary inflammation and intravascular coagulation. We show that comparison between cases of critical illness and population controls is highly efficient for the detection of therapeutically relevant mechanisms of disease

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