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56 research outputs found

Risk of Childhood Cancers Associated with Residence in Agriculturally Intense Areas in the United States

Author: Armstrong BK
Blair A
Bo Li
Bunin GR
Holly EA
Kai Elgethun
Ries LAG
Ryan Whitworth
Settimi L
Simpson EH
Susan E. Carozza
Tiefenbacher JP
U.S. EPA
U.S. EPA
USDA
USDA
Publication venue: National Institute of Environmental Health Sciences
Publication date: 01/04/2008
Field of study

Background: The potential for widespread exposure to agricultural pesticides through drift during application raises concerns about possible health effects to exposed children living in areas of high agricultural activity. Objectives: We evaluated whether residence in a county with greater agricultural activity was associated with risk of developing cancer in children \u3c 15 years of age. Methods: Incidence data for U.S. children 0–14 years of age diagnosed with cancer between 1995 and 2001 were provided by member registries of the North American Association of Central Cancer Registries. We determined percent cropland for each county using agricultural census data, and used the overall study distribution to classify agriculturally intense counties. We estimated odds ratios and 95% confidence intervals for all ages and 5-year age groups for total cancers and selected cancer sites using logistic regression. Results: Our study results showed statistically significant increased risk estimates for many types of childhood cancers associated with residence at diagnosis in counties having a moderate to high level of agricultural activity, with a remarkably consistent dose–response effect seen for counties having ≥ 60% of the total county acreage devoted to farming. Risk for different cancers varied by type of crop. Conclusions: Although interpretation is limited by the ecologic design, in this study we were able to evaluate rarer childhood cancers across a diverse agricultural topography. The findings of this exploratory study support a continued interest in the possible impact of long-term, low-level pesticide exposure in communities located in agriculturally intense areas

Crossref

PubMed Central

Boise State University - ScholarWorks

Detection of brown dwarf-like objects in the core of NGC3603

Author: Abhijit Saha
Alistair R. Walker
Allard
Andersen
Andersen
Baraffe
Basri
Beccari
Braatz
Bradley C. Whitmore
Brandl
Bruce Balick
Burgasser
C. Marcella Carollo
Chabrier
Cristóbal-Hornillos
Cruz
Daniela Calzetti
De Marchi
Dobbs-Dixon
Donald N. B. Hall
Dressel
D’Antona
Erick T. Young
Fossati
Francesco Paresce
Geballe
Giacomo Beccari
Gorlova
Gould
Guido De Marchi
Harayama
Hauschildt
Howard E. Bond
Jay A. Frogel
Jayawardhana
John T. Trauger
Jon A. Holtzman
Joseph I. Silk
Jurić
Kalirai
Kirkpatrick
Konopacky
Kozhurina-Platais
Lada
Lebouteiller
Leggett
Levrard
Loredana Spezzi
Luhman
Mainzer
McLean
Melena
Michael A. Dopita
Michael J. Disney
Moffat
Morten Andersen
Muench
Najita
Nino Panagia
Patrick J. McCarthy
Peimbert
Randy A. Kimble
Reid
Reipurth
Reipurth
Robert W. O'Connell
Rochau
Rogier A. Windhorst
Russell E. Ryan Jr.
Ryan
Schmidt
Schweitzer
Schweitzer
Siess
Sung
Thies
Thompson
Tinney
Tsuji
Vrba
White
Whitworth
Yan
Publication venue: 'IOP Publishing'
Publication date: 28/01/2011
Field of study

We use near-infrared data obtained with the Wide Field Camera 3 (WFC3) on the Hubble Space Telescope to identify objects having the colors of brown dwarfs (BDs) in the field of the massive galactic cluster NGC 3603. These are identified through use of a combination of narrow and medium band filters spanning the J and H bands, and which are particularly sensitive to the presence of the 1.3-1.5{\mu}m H2O molecular band - unique to BDs. We provide a calibration of the relationship between effective temperature and color for both field stars and for BDs. This photometric method provides effective temperatures for BDs to an accuracy of {\pm}350K relative to spectroscopic techniques. This accuracy is shown to be not significantly affected by either stellar surface gravity or uncertainties in the interstellar extinction. We identify nine objects having effective temperature between 1700 and 2200 K, typical of BDs, observed J-band magnitudes in the range 19.5-21.5, and that are strongly clustered towards the luminous core of NGC 3603. However, if these are located at the distance of the cluster, they are far too luminous to be normal BDs. We argue that it is unlikely that these objects are either artifacts of our dataset, normal field BDs/M-type giants or extra-galactic contaminants and, therefore, might represent a new class of stars having the effective temperatures of BDs but with luminosities of more massive stars. We explore the interesting scenario in which these objects would be normal stars that have recently tidally ingested a Hot Jupiter, the remnants of which are providing a short-lived extended photosphere to the central star. In this case, we would expect them to show the signature of fast rotation.Comment: 26 Pages, 8 Figures, Accepted for publication on Ap

arXiv.org e-Print Archive

Crossref

Change in Blood Pressure Variability Among Treated Elderly Hypertensive Patients and Its Association With Mortality

Author: Bear C.
Beckinsale P.
Beilin L.J.
Boyle F.
Brown M.
Bruce A.
Chowdhury Enayet
Cope V.
De Looze F.
DeLooze F.
Dewar E.
Dibben C.
Dickinson J.
Donnan G.
Feneley M.
Fletcher P.
Fraser G.
Gambrill J.
Glasziou P.
Gleave D.
Harrap S.
Jennings G.L.R.
Johnston C.
Joseph P.
MacMahon S.
Marley J.
Marley J.
McDermott B.
McMurchie M.
Moore S.
Morgan T.
Moss J.
Nelson M.R.
Newbury J.
Piterman L.
Primrose J.
Reid Christopher
Ryan P.
Ryan P.
Silagy C.
Thompson J.
Webb P.
Whitworth J.
Willson K.
Wing L.M.H.
Publication venue: 'Ovid Technologies (Wolters Kluwer Health)'
Publication date: 01/01/2019
Field of study

Background: Information is scarce regarding effects of antihypertensive medication on blood pressure variability (BPV) and associated clinical outcomes. We examined whether antihypertensive treatment changes BPV over time and whether such change (decline or increase) has any association with long-term mortality in an elderly hypertensive population. Methods and Results: We used data from a subset of participants in the Second Australian National Blood Pressure study (n=496) aged ≥65 years who had 24-hour ambulatory blood pressure recordings at study entry (baseline) and then after a median of 2 years while on treatment (follow-up). Weighted day-night systolic BPV was calculated for both baseline and follow-up as a weighted mean of daytime and nighttime blood pressure standard deviations. The annual rate of change in BPV over time was calculated from these BPV estimates. Furthermore, we classified both BPV estimates as high and low based on the baseline median BPV value and then classified BPV changes into stable: low BPV, stable: high BPV, decline: high to low, and increase: low to high. We observed an annual decline (mean±SD: −0.37±1.95; 95% CI, −0.54 to −0.19; P<0.001) in weighted day-night systolic BPV between baseline and follow-up. Having constant stable: high BPV was associated with an increase in all-cause mortality (hazard ratio: 3.03; 95% CI, 1.67–5.52) and cardiovascular mortality (hazard ratio: 3.70; 95% CI, 1.62–8.47) in relation to the stable: low BPV group over a median 8.6 years after the follow-up ambulatory blood pressure monitoring. Similarly, higher risk was observed in the decline: high to low group. Conclusions: Our results demonstrate that in elderly hypertensive patients, average BPV declined over 2 years of follow-up after initiation of antihypertensive therapy, and having higher BPV (regardless of any change) was associated with increased long-term mortality

Crossref

University of Tasmania Open Access Repository

espace@Curtin

University of Melbourne Institutional Repository

Monash University Research Portal

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A deleterious gene-by-environment interaction imposed by calcium channel blockers in Marfan syndrome

Author: Bachir Suha
Bedja Djahida
Caulfield Mark J
Dietz Harry C
Doyle Alexander J
Doyle Jefferson J
Ehsan Hamid
Farrar Carrie
Habashi Jennifer P
Huso David
Huso Nick
Judge Daniel P
Lindsay Mark E
Myers Loretha
Rusholme Benjamin
Schoenhoff Florian
Squires Oliver
Thomas Craig J
Van Eyk Jennifer E
Whitworth Ryan E
Wilson Nicole K
Publication venue: 'eLife Sciences Publications, Ltd'
Publication date: 01/01/2015
Field of study

Calcium channel blockers (CCBs) are prescribed to patients with Marfan syndrome for prophylaxis against aortic aneurysm progression, despite limited evidence for their efficacy and safety in the disorder. Unexpectedly, Marfan mice treated with CCBs show accelerated aneurysm expansion, rupture, and premature lethality. This effect is both extracellular signal-regulated kinase (ERK1/2) dependent and angiotensin-II type 1 receptor (AT1R) dependent. We have identified protein kinase C beta (PKCβ) as a critical mediator of this pathway and demonstrate that the PKCβ inhibitor enzastaurin, and the clinically available anti-hypertensive agent hydralazine, both normalize aortic growth in Marfan mice, in association with reduced PKCβ and ERK1/2 activation. Furthermore, patients with Marfan syndrome and other forms of inherited thoracic aortic aneurysm taking CCBs display increased risk of aortic dissection and need for aortic surgery, compared to patients on other antihypertensive agents. DOI: http://dx.doi.org/10.7554/eLife.08648.00

Harvard University - DASH

PubMed Central

Bern Open Repository and Information System (BORIS)

Macquarie University ResearchOnline

Inhibition of Dehydration-Induced Water Intake by Glucocorticoids Is Associated with Activation of Hypothalamic Natriuretic Peptide Receptor-A in Rat

Author: A Coons
Bao Deng
C Liu
C Liu
C Liu
Chao Liu
CR Mantyh
CW Simpson
DG Gardner
DG Gardner
E Tarjan
EK Walls
F Laczi
G Katsuura
GE Woodard
GP Chrousos
GW C Paxinos
H Geiger
H Zhang
HE de Wardener
Heming Xiu
J Antunes-Rodrigues
J Antunes-Rodrigues
J Antunes-Rodrigues
J Dananberg
JA Aguirre
JA Whitworth
JD Heiss
Jing Guan
JN Mickerson
JW Jahng
Kunshen Liu
L Laue
LR Potter
MC Ryan
MF Goy
MH Oliveira
MW Radomski
R Garcia
RL Thunhorst
SW Turner
T Wallerath
Timothy Jon Bartness
Ying Chen
Yunxiao Kang
Publication venue: Public Library of Science
Publication date: 01/12/2010
Field of study

Atrial natriuretic peptide (ANP) provides a potent defense mechanism against volume overload in mammals. Its primary receptor, natriuretic peptide receptor-A (NPR-A), is localized mostly in the kidney, but also is found in hypothalamic areas involved in body fluid volume regulation. Acute glucocorticoid administration produces potent diuresis and natriuresis, possibly by acting in the renal natriuretic peptide system. However, chronic glucocorticoid administration attenuates renal water and sodium excretion. The precise mechanism underlying this paradoxical phenomenon is unclear. We assume that chronic glucocorticoid administration may activate natriuretic peptide system in hypothalamus, and cause volume depletion by inhibiting dehydration-induced water intake. Volume depletion, in turn, compromises renal water excretion. To test this postulation, we determined the effect of dexamethasone on dehydration-induced water intake and assessed the expression of NPR-A in the hypothalamus. The rats were deprived of water for 24 hours to have dehydrated status. Prior to free access to water, the water-deprived rats were pretreated with dexamethasone or vehicle. Urinary volume and water intake were monitored. We found that dexamethasone pretreatment not only produced potent diuresis, but dramatically inhibited the dehydration-induced water intake. Western blotting analysis showed the expression of NPR-A in the hypothalamus was dramatically upregulated by dexamethasone. Consequently, cyclic guanosine monophosphate (the second messenger for the ANP) content in the hypothalamus was remarkably increased. The inhibitory effect of dexamethasone on water intake presented in a time- and dose-dependent manner, which emerged at least after 18-hour dexamethasone pretreatment. This effect was glucocorticoid receptor (GR) mediated and was abolished by GR antagonist RU486. These results indicated a possible physiologic role for glucocorticoids in the hypothalamic control of water intake and revealed that the glucocorticoids can act centrally, as well as peripherally, to assist in the normalization of extracellular fluid volume

Public Library of Science (PLOS)

Crossref

Directory of Open Access Journals

PubMed Central

Global patient outcomes after elective surgery: prospective cohort study in 27 low-, middle- and high-income countries.

Author: Ab Majid MA
Ab Rahman AS
Ab Rahman R
Abayasinghe C
Abbott T
Abdullah NH
Abdur-Rahman L
Abeloos J
Abernethy C
Abidin UN
Abrunhosa A
Absar M
Adam S
Adams D
Adams G
Adamson M
Adekola O
Adelaja Y
Ademola A
Adenekan A
Adenike O
Adeolu AA
Adetoye A
Adewale B
Adigun T
Adolfsson A
Aflori L
Africander C
Afshari A
Agarwal V
Agodirin O
Aguero Vera M
Aguzzoli C
Ahmad A
Ahmad N
Ahmad T
Ahmad T
Ahmad Y
Ahmed A
Ahmed J
Ai Y
Aignatoaie M
Aimoniotou-Georgiou E
Akanmu O
Akerman N
Akinwale M
Akring I
Al 'Amri K
Al Anizi M
Al hussaini S
Al-Soudaine Y
Aladin H
Alagbe-Briggs O
Alaman Laguarda G
Albaj S
Alcock D
Alcock L
Aldecoa C
Aldecoa C
Aleixo FB
Alexander H
Alexander M
Alexander-Sefre F
Alherz F
Ali H
Ali M
Ali S
Alias A
Alias AH
Alias RLR
Alit MA
Allen S
Allen SJ
Allison J
Alloj C
Allorto NL
Allsop J
Almeida W
Alonso E
Alphonsus C
Alvares D
Alves MJ
Amador JCB
Ameer Y
Amendola CP
Ami N
Amstrup-Hansen L
Anagnou A
Andersen C
Anderson C
Anderson C
Anderson F
Anderson P
Andreadaki E
Andreou A
Andreou P
Andrew A
Andrews E
Angermair S
Angus K
Anillo V
Antal O
Antill P
Antoniadou E
Antonina W
Apagaki E
Apostolou K
Applewhaite C
Aquino LPG
Ar P
Arawwawala D
Ardern D
Argue R
Arkalaki E
Armaganidis A
Armstrong J
Armstrong R
Arnaoutoglou C
Arnaoutoglou E
Arnold G
Arrandale L
Arrich J
Arrigo M
Arshad H
Arshad MA
Arumugam S
Arustei M
Arvaniti K
Arya A
Arya S
Asimakos A
Asudo F
Athanasakis E
Atiku M
Attrill E
Attwood C
Auer P
Avidan M
Avila Sanchez FJ
Avila EJD
Avis J
Awad H
Axioti E
Ayyaz H
Azam UAA
Azambuja P
Azevedo C
Aziz FZ
Baas P
Baghirzada L
Bai H-P
Bai Y
Baillie S
Baines D
Baio TH
Bairaktari A
Baker G
Baker K-A
Baker P
Balain B
Balaji P
Balajonda N
Balanescu A
Balasubramaniam M
Baldisserotto S
Baldwin J
Baldwin M
Balfoussia D
Bali C
Bandeira ME
Banerjee R
Bankewitz C
Banner-Goodspeed V
Bao Q
Barcraft-Barnes H
Barneto L
Barnett A
Baroselli A
Barraclough J
Barras J-P
Barrett S
Barrett WJ
Basanth S
Batchelor N
Bateman B
Bates A
Bates S
Batista HD
Bauchmuller K
Bauer M
Baumgarten G
Baxter L
Beaton C
Beattie S
Beavis V
Bechan S
Bejia T
Belciu I
Belda MT
Bell G
Bell R
Bell S
Bellandi M
Bello J
Beloeil H
Belskiy V
Ben-Menachem E
Benavent P
Benevento A
Bengeri S
Bennett C
Bennett M
Bennett R
Bennett V
Bentley C
Beretta L
Berg A
Bergin C
Bernard A
Berntsen E
Bertram W
Bester D
Bester M
Bettega F
Bettinelli A
Bhardwaj N
Bhatia K
Bhula C
Bi Y
Biais M
Biccard BM
Bidd H
Bidgoli J
Biffen A
Bignami E
Bilolikar A
Bin Mustapha MT
Birch J
Bishop DG
Biyase T
Bizios C
Blackwell C
Blackwood D
Blaj M
Blakemore SP
Bland M
Blunt M
Blyth K
Bocchino S
Bodansky D
Bodger P
Boer C
Boereboom C
Boggiano V
Bogner G
Bolaji B
Bolton D
Boone M
Boschi L
Boshier P
Botes M
Botis I
Bottini C
Bottrill F
Bouchez S
Boulton K
Bouris V
Bourner L
Boutsikos G
Bouwman A
Bouwman RA
Bowrey S
Boxall L
Boyd C
Bradburn M
Bradley J
Branagan G
Branco T
Brand B
Brandsborg B
Breitenstein S
Brennan A
Brennan E
Brenner L
Brincat M
Briscoe R
Bristogiannis S
Brooke J
Brookes J
Brookes M
Brooks C
Broomby R
Brotto AF
Brown A
Brown CW
Brown G
Brown J
Brown J
Brown L
Brown R
Brown R
Browning J
Bruma D
Brunete T
Brunswicker A
Bryant H
Bua E
Buccimazza I
Buckley S
Buerkle C
Buhre W
Buhre W
Buhrer T
Builu PM
Buise M
Bullock C
Bunwarie B
Burns K
Burrows L
Burrows T
Burston B
Burtenshaw A
Burton M
Busuioc M
Butryn I
Butt G
Byrne K
Cabezuelo E
Cabral R
Cabral TDN
Cabrini L
Cacala S
Cai F
Cai Y
Cain H
Cairns C
Cakova V
Calderwood C
Callaghan M
Campbell D
Campbell D
Campbell D
Campbell G
Campbell G
Campbell K
Campbell M
Campbell T
Campey L
Camsooksai J
Cancho D
Candido K
Cang J
Cannavo M
Cao J
Cao Y
Cao Z
Cardellino S
Cardosa J
Cardoso G
Cardy J
Carmino L
Carp CP
Carr A
Carrera R
Carroll C
Carroll J
Caser E
Castano Moreira B
Castano B
Castle G
Cavanagh S
Cawthorn L
Cernea DD
Chaddock M
Chaloulis P
Chan A
Chan HMH
Chan M
Chan P
Chan V
Chan WK
Chan WKJ
Chan YL
Chande S
Chandler B
Chandra S
Chandrasekharan S
Chang YH
Chaniotaki F
Charitos E
Charlalampidoy A
Charles R
Chatterjee D
Chatterjee J
Chatzimichali CA
Chau S
Chazova E
Cheah C
Cheah S
Cheeseman M
Cheing Y
Chen C
Chen C
Chen F
Chen F
Chen H
Chen J
Chen J
Chen L
Chen L
Chen L-L
Chen P
Chen Q
Chen R
Chen S
Chen S
Chen S
Chen Y
Chen Y
Chen Y
Chen Y
Chen Z
Cheng B
Cheng KH
Cheng Z
Cheong E
Cherian R
Cherrett V
Chetty RR
Chew M
Chhabra A
Chicken D-W
Chilinciuc I
Chin II
Chirkut S
Chisbert Cuenca V
Chlorou D
Choi H-MD
Choi S
Chow L
Christian R
Christiansen IC
Christmas N
Christodoulidis G
Christodoulopoulou T
Christofaki M
Christoforidis D
Chronis C
Chu HM
Chu S
Chua P
Chukkambotla S
Chung CKE
Cifra E
Ciobanu C
Ciobotaru OR
Cirstea E
Clark R
Clarkson A
Clarkson R
Claxton A
Clemmons K
Cloro LM
Clyde A
Cobzaru I
Codita A
Colangelo A
Colangelo C
Colling K
Collins H
Collins M
Collins N
Colvin C
Commey T
Comptaer N
Conde C
Conradie A
Constantin K
Cook T
Cooper L
Cooper L
Cooper M
Cooper R
Cooper S
Copaciu E
Cope J
Copetti E
Copley E
Copotoiu SM
Coppens M
Corneci D
Cornell J
Cornish J
Correia da Silva RFM
Corti D
Costanzo E
Costelloe H
Cotter R
Cotterell S
Cotterill D
Coughlan E
Coulter I
Coulter S
Coutinho F
Cowton A
Cox H
Cozar OI
Craig J
Craven R
Craw N
Craw S
Creary T
Cripps H
Critchley R
Cronje L
Cruickshank R
Cruikshanks A
Cruz S
Cueva A
Cunha P
Curley G
Currow H
Czepanski C
Czeslick E
D'Andrea R
da Costa Fischer BF
Dafnios N
Dai H
Dai Q
Dai Q
Dai SY
Daikou P
Dalamagka M
Dalampini E
Dali-Kemmery L
Dalton E
Damant R
Daniel C
Daniel GD
Daniel H
Daniel H
Daniel S
Dankl D
Darko J
Darwish S
Das S
Dasrath A
Datson A
Daubeny T
Daugaard M
Davari M
Dave T
Davies C
Davies H
Davies K
Davies K
Davies L
Davies Z
Davis E
Davis F
Davis S
Daya B
De Andres Ibanez JA
de Araujo DM
De Baerdemaeker L
de Beer J
de Boer HD
De Bruyne A
de Campos Ferreira MF
de Fretes J
de Gasperi J
De Hert S
De Jongh K
De Kegel D
De Meyer JN
De Oliveira MC
de Rudnicki S
de Swardt M
de Vasconcellos K
de Villiers M
de Wet J
Deacon M
Deblaere I
Dedemadi G
Deen T
Deepak S
Deighton K
Deja M
Delgado Garcia DR
Delgado Navarro C
Della Rocca G
Dempsey G
Dempster A
den Hoedt M
Denham S
Dent K
Dermitzaki D
Desbordes J
Despotidis V
Diaconescu C
Dias F
Dias S
Dickson J
Ditai J
Divatia J
Dixon L
do Nascimento Junior P
Dobson G
Docherty P
Dodiyi-Manuel A
Dodsworth K
Dolan R
Dong B
Donohue R
Donovan A
Douglas J
Doumos R
Downes C
Doyle D
Dragnea D
Dragoescu NA
Drake M
Drimala M
Drinkwater Z
Drummond L
Du F
Du F
Du X
Duarte C
Dube NZ
Duca A
Dudgeon L
Dudson R
Duenser M
Dumitrascu CO
Dumitrescu A
Dunay A
Dunk N
Durant E
Durodola A
Dursin AN
Durst A
Duttchen K
Dutu M
Dwyer H
Dylst D
Dzhamullaev P
Dzulkipli N
Echem R
Edmond H
Edwards J
Edwards M
Edwards M
Efthymiadi A
Egan T
Eggleston C
Eichwalder A
Eikman J
Ekelund K
el Manser D
El-Sayed A
Elabib A
Elena G
Elferink-Vonk R
Elgasim M
Ellis J
Ellis K
Elna C
Emma T
Endersby S
Eneje P
Eng K
English D
English R
Epodoi J
Eskildsen KZ
Esteves S
Ethgen S
Evans A
Evans C
Everingham K
Ewe R
Ezekiel E
Ezike H
Fagerlund MJ
Faina L
Falk E
Fan H
Fan L
Fan Y
Fanfani LC
Faponle F
Faria e Maia D
Faria F
Farid N
Farina Z
Farrell H
Farrow M
Fasina O
Fatungase OM
Faulds M
Fei Y
Fellinger P
Feng Y
Fengas L
Fergey L
Ferguson M
Fernandez S
Ferrando C
Filipescu D
Filippopoulos A
Finch A
Fiorentza K
Fischbach N
Flatt J
Fleischer A
Fleisher L
Fleisher LA
Flores Risco S
Flores AAA
Flores K
Flossos A
Foers W
Foglia J
Foley J
Fonck K
Foord D
Foot H
Foot J
Ford D
Forget P
Forsans E
Forstner K
Foster R
Foubert L
Fouracres A
Fowler A
Fowler C
Fraga JM
Fragandreas G
Francis D
Franklin J
Franks R
Frantzeskos G
Freeman D
Freeman V
Freethy A
Freitas K
Freschini A
Freschini D
Frewer N
Fritsch G
Frost V
Fu K
Fu S
Fu Y
Fuad A
Fuentes I
Fulton G
Funk B
Funk D
Furrer M
Furtado Paiva AA
Futier E
Gaitanakis S
Gall L
Gallacher P
Gallard S
Gallego L
Gama NS
Gambhir R
Ganter DL
Ganter MT
Gao H
Garcia Del Valle S
Garcia J
Garcia-Saiz I
Gardikou VV
Gardiner M
Garg A
Garg S
Garg S
Garrett E
Gastaldi C
Gatke MR
Gatta A
Gaudin C
Gavril L
Gbolahan O
Ge X
Geddoa B
Geddoa E
Geisen M
Geldenhuys J
Geng W
Georgakakis G
George R
Georgiou G
Georgopoulou E
Gercek Y
Germann R
Geromarkaki E
Ghafar FNIA
Ghignone F
Ghosh A
Ghushe N
Giancarlo L
Giannaki C
Gibson-Lapsley H
Gil Manuel G
Giles J
Gill J
Gill S
Gill T
Gille J
Gillespie D
Gillies M
Gilmore J
Gilmour F
Gkini K-P
Gkiokas G
Gkioni P
Glasbey J
Glasgow E
Glister G
Glover L
Goad EHA
Goebel U
Goga IE
Goga R
Goldberg O
Golder K
Gomez Diago L
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Grace A
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Gradwohl-Matis I
Granum SN
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Iloabachie I
Ilyina Y
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Iurin A
Izquierdo Palomares A
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Joseph J
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Kalaitzopoulos I
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Katime A
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Khan RBN
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Kochhar A
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Kong C-C
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Kontis E
Koo EGY
Koompirochana V
Koopman-van Gemert A
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Kottam L
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Koulouras V
Koutelidakis I
Koutsikou A
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Kretov V
Krishnachetty B
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Kuan PX
Kubitzek C
Kuhn WP
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Kulkarni A
Kulkarni A
Kulkarni R
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Kumara P
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Kurasz C
Kurnia A
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Kushakovsky V
Kwok A
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Kwok FY
Kyomugisha E
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Lahiri S
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Lantang EY
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Larsen JR
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Lataniotou O
Lathyris D
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Lavrentieva A
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Lee HS
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Lee YC
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Lewthwaite S
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Lockwood G
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Looseley A
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Lopez del Moral O
Lopez AG
Lopez JCJA
Loumpias C
Lowery T
Lozano A
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Lubach I
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Luisa Garcia-Perez M
Lumsden R
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Martinez Ernesto EP
Martins Costa ACM
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Melbourne S
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Publication venue: 'Oxford University Press (OUP)'
Publication date: 01/01/2016
Field of study

BACKGROUND: As global initiatives increase patient access to surgical treatments, there remains a need to understand the adverse effects of surgery and define appropriate levels of perioperative care. METHODS: We designed a prospective international 7-day cohort study of outcomes following elective adult inpatient surgery in 27 countries. The primary outcome was in-hospital complications. Secondary outcomes were death following a complication (failure to rescue) and death in hospital. Process measures were admission to critical care immediately after surgery or to treat a complication and duration of hospital stay. A single definition of critical care was used for all countries. RESULTS: A total of 474 hospitals in 19 high-, 7 middle- and 1 low-income country were included in the primary analysis. Data included 44 814 patients with a median hospital stay of 4 (range 2-7) days. A total of 7508 patients (16.8%) developed one or more postoperative complication and 207 died (0.5%). The overall mortality among patients who developed complications was 2.8%. Mortality following complications ranged from 2.4% for pulmonary embolism to 43.9% for cardiac arrest. A total of 4360 (9.7%) patients were admitted to a critical care unit as routine immediately after surgery, of whom 2198 (50.4%) developed a complication, with 105 (2.4%) deaths. A total of 1233 patients (16.4%) were admitted to a critical care unit to treat complications, with 119 (9.7%) deaths. Despite lower baseline risk, outcomes were similar in low- and middle-income compared with high-income countries. CONCLUSIONS: Poor patient outcomes are common after inpatient surgery. Global initiatives to increase access to surgical treatments should also address the need for safe perioperative care. STUDY REGISTRATION: ISRCTN5181700

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University of Groningen

Archivio istituzionale della ricerca - Università dell'Insubria

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Repositório do Centro Hospitalar de Lisboa Central, EPE

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Guidelines for the use and interpretation of assays for monitoring autophagy (3rd edition)

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Publication venue
Publication date: 22/09/2015
Field of study

In 2008 we published the first set of guidelines for standardizing research in autophagy. Since then, research on this topic has continued to accelerate, and many new scientists have entered the field. Our knowledge base and relevant new technologies have also been expanding. Accordingly, it is important to update these guidelines for monitoring autophagy in different organisms. Various reviews have described the range of assays that have been used for this purpose. Nevertheless, there continues to be confusion regarding acceptable methods to measure autophagy, especially in multicellular eukaryotes. For example, a key point that needs to be emphasized is that there is a difference between measurements that monitor the numbers or volume of autophagic elements (e.g., autophagosomes or autolysosomes) at any stage of the autophagic process versus those that measure fl ux through the autophagy pathway (i.e., the complete process including the amount and rate of cargo sequestered and degraded). In particular, a block in macroautophagy that results in autophagosome accumulation must be differentiated from stimuli that increase autophagic activity, defi ned as increased autophagy induction coupled with increased delivery to, and degradation within, lysosomes (inmost higher eukaryotes and some protists such as Dictyostelium ) or the vacuole (in plants and fungi). In other words, it is especially important that investigators new to the fi eld understand that the appearance of more autophagosomes does not necessarily equate with more autophagy. In fact, in many cases, autophagosomes accumulate because of a block in trafficking to lysosomes without a concomitant change in autophagosome biogenesis, whereas an increase in autolysosomes may reflect a reduction in degradative activity. It is worth emphasizing here that lysosomal digestion is a stage of autophagy and evaluating its competence is a crucial part of the evaluation of autophagic flux, or complete autophagy. Here, we present a set of guidelines for the selection and interpretation of methods for use by investigators who aim to examine macroautophagy and related processes, as well as for reviewers who need to provide realistic and reasonable critiques of papers that are focused on these processes. These guidelines are not meant to be a formulaic set of rules, because the appropriate assays depend in part on the question being asked and the system being used. In addition, we emphasize that no individual assay is guaranteed to be the most appropriate one in every situation, and we strongly recommend the use of multiple assays to monitor autophagy. Along these lines, because of the potential for pleiotropic effects due to blocking autophagy through genetic manipulation it is imperative to delete or knock down more than one autophagy-related gene. In addition, some individual Atg proteins, or groups of proteins, are involved in other cellular pathways so not all Atg proteins can be used as a specific marker for an autophagic process. In these guidelines, we consider these various methods of assessing autophagy and what information can, or cannot, be obtained from them. Finally, by discussing the merits and limits of particular autophagy assays, we hope to encourage technical innovation in the field

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Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)

Author: A. -G. Wu
A. C. Ma
A. K. Au
Abdel-Aziz A. K.
Abdelfatah S.
Abdellatif M.
Abdoli A.
Abel S.
Abeliovich H.
Abildgaard M. H.
Abudu Y. P.
Acevedo-Arozena A.
Adamopoulos I. E.
Adeli K.
Adolph T. E.
Adornetto A.
Aflaki E.
Agam G.
Agarwal A.
Aggarwal B. B.
Agnello M.
Agostinis P.
Agrewala J. N.
Agrotis A.
Aguilar P. V.
Ahmad S. T.
Ahmed Z. M.
Ahumada-Castro U.
Aits S.
Aizawa S.
Akkoc Y.
Akoumianaki T.
Akpinar H. A.
Al-Abd A. M.
Al-Akra L.
Al-Gharaibeh A.
Alaoui-Jamali M. A.
Alberti S.
Alcocer-Gomez E.
Alessandri C.
Ali M.
Alim Al-Bari M. A.
Aliwaini S.
Alizadeh J.
Almacellas E.
Almasan A.
Alonso A.
Alonso G. D.
Altan-Bonnet N.
Altieri D. C.
Alvarez E. M. C.
Alves da Costa C.
Alves S.
Alzaharna M. M.
Amadio M.
Amantini C.
Amaral C.
Ambrosio S.
Amer A. O.
Ammanathan V.
An Z.
Andersen S. U.
Andrabi S. A.
Andrade-Silva M.
Andres A. M.
Angelini S.
Ann D.
Anozie U. C.
Ansari M. Y.
Antas P.
Antebi A.
Anton Z.
Anwar T.
Apetoh L.
Apostolova N.
Araki T.
Araki Y.
Arasaki K.
Araujo W. L.
Araya J.
Arden C.
Arevalo M. -A.
Arguelles S.
Arias E.
Arikkath J.
Arimoto H.
Ariosa A. R.
Armstrong-James D.
Arnaune-Pelloquin L.
Aroca A.
Arroyo D. S.
Arsov I.
Artero R.
Asaro D. M. L.
Aschner M.
Ashrafizadeh M.
Ashur-Fabian O.
Atanasov A. G.
Auberger P.
Auner H. W.
Aurelian L.
Autelli R.
Avagliano L.
Avalos Y.
Aveic S.
Aveleira C. A.
Avin-Wittenberg T.
Aydin Y.
Ayton S.
Ayyadevara S.
Azzopardi M.
B. C. B. Ko
Baba M.
Backer J. M.
Backues S. K.
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Bae O. -N.
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Publication venue: 'Informa UK Limited'
Publication date: 01/01/2021
Field of study

Institutional Research Information System University of Turin

Guidelines for the use and interpretation of assays for monitoring autophagy (4th edition)1.

Author: Abdel-Aziz AK
Abdelfatah S
Abdellatif M
Abdoli A
Abel S
Abeliovich H
Abildgaard MH
Abudu YP
Acevedo-Arozena A
Adamopoulos IE
Adeli K
Adolph TE
Adornetto A
Aflaki E
Agam G
Agarwal A
Aggarwal BB
Agnello M
Agostinis P
Agrewala JN
Agrotis A
Aguilar PV
Ahmad ST
Ahmed ZM
Ahumada-Castro U
Aits S
Aizawa S
Akkoc Y
Akoumianaki T
Akpinar HA
Al-Abd AM
Al-Akra L
Al-Gharaibeh A
Alaoui-Jamali MA
Alberti S
Alcocer-Gómez E
Alessandri C
Ali M
Alim Al-Bari MA
Aliwaini S
Alizadeh J
Almacellas E
Almasan A
Alonso A
Alonso GD
Altan-Bonnet N
Altieri DC
Alves da Costa C
Alves S
Alzaharna MM
Amadio M
Amantini C
Amaral C
Ambrosio S
Amer AO
Ammanathan V
An Z
Andersen SU
Andrabi SA
Andrade-Silva M
Andres AM
Angelini S
Ann D
Anozie UC
Ansari MY
Antas P
Antebi A
Antón Z
Anwar T
Apetoh L
Apostolova N
Araki T
Araki Y
Arasaki K
Araya J
Araújo WL
Arden C
Arguelles S
Arias E
Arikkath J
Arimoto H
Ariosa AR
Armstrong-James D
Arnauné-Pelloquin L
Aroca A
Arroyo DS
Arsov I
Artero R
Arévalo M-A
Asaro DML
Aschner M
Ashrafizadeh M
Ashur-Fabian O
Atanasov AG
Au AK
Auberger P
Auner HW
Aurelian L
Autelli R
Avagliano L
Aveic S
Aveleira CA
Avin-Wittenberg T
Aydin Y
Ayton S
Ayyadevara S
Azzopardi M
Baba M
Backer JM
Backues SK
Bae D-H
Bae O-N
Bae SH
Baehrecke EH
Baek A
Baek S-H
Baek SH
Bagetta G
Bagniewska-Zadworna A
Bai H
Bai J
Bai X
Bai Y
Bairagi N
Baksi S
Balazadeh S
Balbi T
Baldari CT
Balduini W
Ballabio A
Ballester M
Balzan R
Bandopadhyay R
Banerjee S
Banerjee S
Bao Y
Baptista MS
Baracca A
Barbati C
Bargiela A
Barilà D
Barlow PG
Barmada SJ
Barreiro E
Barreto GE
Bartek J
Bartel B
Bartolome A
Barve GR
Basagoudanavar SH
Bassham DC
Bast RC
Basu A
Batoko H
Batten I
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Baumgarner BL
Bayry J
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Beau I
Beaumatin F
Bechara LRG
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Berchtold MW
Berezowska S
Bergamaschi D
Bergami M
Bergmann A
Berliocchi L
Berlioz-Torrent C
Bernard A
Berthoux L
Besirli CG
Besteiro S
Betin VM
Beyaert R
Bezbradica JS
Bhaskar K
Bhatia-Kissova I
Bhattacharya R
Bhattacharya S
Bhattacharyya S
Bhuiyan MS
Bhutia SK
Bi L
Bi X
Biden TJ
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Blum JS
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Boban M
Boesze-Battaglia K
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Bomont P
Bonaldo P
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Brodsky JL
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Buckingham EM
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Buitrago-Molina LE
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Burón MI
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Camara NO
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Campbell EM
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Candido de Almeida D
Canesi L
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Cao B
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Carosi JM
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Castro-Obregon S
Catz SD
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Cechowska-Pasko M
Cenci S
Ceperuelo-Mallafré V
Cerqueira JJ
Cerutti JM
Cervia D
Cetintas VB
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Chae H-J
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Chan HYE
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Chan YS
Chandra PK
Chang C
Chang C-P
Chang H-C
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Chao J
Chapman T
Charlet-Berguerand N
Chatterjee S
Chaube SK
Chaudhary A
Chauhan S
Chaum E
Checler F
Cheetham ME
Chen C-S
Chen G-C
Chen J-F
Chen L
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Chen LL
Chen M
Chen M-K
Chen N
Chen Q
Chen R-H
Chen S
Chen W
Chen W
Chen X
Chen X-M
Chen X-W
Chen Y
Chen Y
Chen Y
Chen Y-G
Chen Y-J
Chen Y-Q
Chen Z
Chen Z
Chen Z
Chen Z-H
Chen ZJ
Chen ZS
Cheng H
Cheng J
Cheng S-Y
Cheng W
Cheng X
Cheng X-T
Cheng Y
Cheng Z
Cheong H
Cheong JK
Chernyak BV
Cherry S
Cheung CFR
Cheung CHA
Cheung K-H
Chevet E
Chi RJ
Chiang AKS
Chiaradonna F
Chiarelli R
Chiariello M
Chica N
Chiocca S
Chiong M
Chiou S-H
Chiramel AI
Chiurchiù V
Cho D-H
Choe S-K
Choi AMK
Choi ME
Choudhury KR
Chow NS
Chu CT
Chua JJE
Chua JP
Chung H
Chung KP
Chung S
Chung S-H
Chung Y-L
Cianfanelli V
Ciechomska IA
Cifuentes M
Cinque L
Cirak S
Cirone M
Clague MJ
Clarke R
Clementi E
Coccia EM
Codogno P
Cohen E
Cohen MM
Colasanti T
Colasuonno F
Colbert RA
Colell A
Coll NS
Collins MO
Colombo MI
Colón-Ramos DA
Combaret L
Comincini S
Cominetti MR
Consiglio A
Conte A
Conti F
Contu VR
Cookson MR
Coombs KM
Coppens I
Corasaniti MT
Cordes N
Corkery DP
Cortese K
Costa MDC
Costantino S
Costelli P
Coto-Montes A
Crack PJ
Crespo JL
Criollo A
Crippa V
Cristofani R
Csizmadia T
Cuadrado A
Cui B
Cui J
Cui Y
Cui Y
Culetto E
Cumino AC
Cybulsky AV
Czaja MJ
Czuczwar SJ
D'Adamo S
D'Amelio M
D'Arcangelo D
D'Lugos AC
D'Orazi G
da Silva JA
Dafsari HS
Dagda RK
Dagdas Y
Daglia M
Dai X
Dai Y
Dai Y
Dal Col J
Dalhaimer P
Dalla Valle L
Dallenga T
Dalmasso G
Damme M
Dando I
Dantuma NP
Darling AL
Das H
Dasarathy S
Dasari SK
Dash S
Daumke O
Dauphinee AN
Davies JS
Davis RJ
Davis T
Dayalan Naidu S
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De Bosscher K
De Felice F
De Franceschi L
De Leonibus C
de Mattos Barbosa MG
De Meyer GRY
De Milito A
De Nunzio C
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De Zio D
Debnath J
DeBosch BJ
Decuypere J-P
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Deflorian G
DeGregori J
Dehay B
Del Rio G
Delaney JR
Delbridge LMD
Delorme-Axford E
Delpino MV
Demarchi F
Dembitz V
Demers ND
Deng H
Deng Z
Dengjel J
Dent P
Denton D
DePamphilis ML
Der CJ
Deretic V
Descoteaux A
Devis L
Devkota S
Devuyst O
Dewson G
Dharmasivam M
Dhiman R
di Bernardo D
Di Cristina M
Di Domenico F
Di Fazio P
Di Fonzo A
Di Guardo G
Di Guglielmo GM
Di Leo L
Di Malta C
Di Nardo A
Di Rienzo M
Di Sano F
Diallinas G
Diao J
Diaz-Araya G
Dickinson JM
Diederich M
Dieudé M
Dikic I
Ding S
Ding W-X
Dini L
Dinic M
Dinić J
Dinkova-Kostova AT
Dionne MS
Distler JHW
Diwan A
Dixon IMC
Djavaheri-Mergny M
Dobrinski I
Dobrovinskaya O
Dobrowolski R
Dobson RCJ
Dokmeci Emre S
Donadelli M
Dong B
Dong X
Dong XC
Dong Z
Dorn Ii GW
Dotsch V
Dou H
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Dowaidar M
Dridi S
Drucker L
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Du A
Du C
Du G
Du H-N
Du L-L
Duan S-B
Duan X
Duarte SP
Dubrovska A
Dunlop EA
Dupont N
Durán RV
Dwarakanath BS
Dyshlovoy SA
Dávila VA
Díaz-Laviada I
Ebrahimi-Fakhari D
Eckhart L
Edelstein CL
Efferth T
Eftekharpour E
Eichinger L
Eid N
Eisenberg T
Eissa NT
Eissa S
Ejarque M
El Andaloussi A
El-Hage N
El-Naggar S
El-Shafey ES
Eleuteri AM
Elgendy M
Eliopoulos AG
Elizalde MM
Elks PM
Elsasser H-P
Elsherbiny ES
Emerling BM
Emre NCT
Eng CH
Engedal N
Engelbrecht A-M
Engelsen AST
Enserink JM
Escalante R
Esclatine A
Escobar-Henriques M
Eskelinen E-L
Espert L
Eusebio M-O
Fabrias G
Fabrizi C
Facchiano A
Facchiano F
Fadeel B
Fader C
Faesen AC
Fairlie WD
Falcó A
Falkenburger BH
Fan D
Fan J
Fan Y
Fang EF
Fang Y
Fang Y
Fanto M
Farfel-Becker T
Faure M
Fazeli G
Fedele AO
Feldman AM
Feng D
Feng J
Feng L
Feng W
Feng Y
Feng Y
Fenz Araujo T
Ferguson TA
Fernandez-Checa JC
Fernie AR
Fernández ÁF
Fernández-Veledo S
Ferrante AW
Ferraresi A
Ferrari MF
Ferreira JCB
Ferro-Novick S
Figueras A
Filadi R
Filigheddu N
Filippi-Chiela E
Filomeni G
Fimia GM
Fineschi V
Finetti F
Finkbeiner S
Fisher EA
Fisher PB
Flamigni F
Fliesler SJ
Flo TH
Florance I
Florey O
Florio T
Fodor E
Follo C
Fon EA
Forlino A
Fornai F
Fortini P
Fracassi A
Fraldi A
Franco B
Franco R
Franconi F
Frankel LB
Friedman SL
Fröhlich LF
Frühbeck G
Fuentes JM
Fujiki Y
Fujita N
Fujiwara Y
Fukuda M
Fulda S
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Furuya N
Fusco C
Gack MU
Gaffke L
Galadari S
Galasso A
Galindo MF
Gallolu Kankanamalage S
Galluzzi L
Galy V
Gammoh N
Gan B
Ganley IG
Gao F
Gao H
Gao M
Gao P
Gao S-J
Gao W
Gao X
Garcera A
Garcia MN
Garcia VE
Garcia-Escudero V
Garcia-Garcia A
Garcia-Macia M
Garcia-Ruiz C
García-Del Portillo F
García-Moreno D
García-Sanz P
Garg AD
Gargini R
Garofalo T
Garry RF
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Gatica D
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Geiss-Friedlander R
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Gentle IE
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Gerhardt C
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Gewirtz DA
Ghasemipour Afshar E
Ghavami S
Ghigo A
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Giamas G
Giampietri C
Giatromanolaki A
Gibson GE
Gibson SB
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Giniger E
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Girao H
Girardin SE
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Giulivi C
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Goder V
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Golab J
Goldstone DC
Golebiewska A
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Gonzalez-Hernandez T
Gonzalez-Polo RA
Gonzalez-Reyes JA
González-Gallego J
González-Rodríguez P
Goping IS
Gorbatyuk MS
Gorbunov NV
Gorojod RM
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Goruppi S
Gotor C
Gottlieb RA
Gozes I
Gozuacik D
Graef M
Granatiero V
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Green DR
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Gräler MH
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Guan J-L
Guardia CM
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Gustafsson AB
Gutterman DD
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Görgülü K
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Hasegawa T
Hasima Nagoor N
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Hayrabedyan SB
Hays TS
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Heakal Y
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Hejtmancik JF
Helgason GV
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Hernandez C
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Hernandez-Gea V
Hernández A
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Hervás JH
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Heussler VT
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Ho S-L
Ho WY
Hobbs GA
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Hoet PHM
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Holmberg CI
Hombrebueno JR
Hooper LV
Hoppe T
Horos R
Hoshida Y
Hsin I-L
Hsu H-Y
Hu B
Hu D
Hu L-F
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Hu R
Hu W
Hu Y-C
Hu Z-W
Hua F
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Hua Y
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Huang YJ
Huber TB
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Irazoqui JE
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Iyer AKV
Izquierdo JM
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Jimenez-Sanchez M
Jin E-J
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Johansen T
Johnson GVW
Johnston SA
Jokitalo E
Jolly MK
Joosten LAB
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Kapuy O
Karamouzis MV
Karim MR
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Kaufmann SHE
Kauppinen A
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Keulers TG
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Khandelwal VKM
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Killackey SA
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Kinsey CG
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Kirshenbaum LA
Kiselev SL
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Koh YH
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Korkmaz G
Korolchuk VI
Korsnes MS
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Kotler ML
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Kunnumakkara AB
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Laface I
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Lima TRR
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Lin K-H
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Zhou Y
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Zhu B
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Zhu H
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Zhu H
Zhu W-G
Zhu Y
Zhu Y
Zhuang H
Zhuang X
Zientara-Rytter K
Zimmermann CM
Ziviani E
Zoladek T
Zong W-X
Zorov DB
Zorzano A
Zou W
Zou Z
Zou Z
Zuryn S
Zwerschke W
Álvarez ÉMC
Ávalos Y
Önal G
Üstün S
Čolić M
Đokić J
Žerovnik E
Publication venue: 'Informa UK Limited'
Publication date: 01/01/2021
Field of study

In 2008, we published the first set of guidelines for standardizing research in autophagy. Since then, this topic has received increasing attention, and many scientists have entered the field. Our knowledge base and relevant new technologies have also been expanding. Thus, it is important to formulate on a regular basis updated guidelines for monitoring autophagy in different organisms. Despite numerous reviews, there continues to be confusion regarding acceptable methods to evaluate autophagy, especially in multicellular eukaryotes. Here, we present a set of guidelines for investigators to select and interpret methods to examine autophagy and related processes, and for reviewers to provide realistic and reasonable critiques of reports that are focused on these processes. These guidelines are not meant to be a dogmatic set of rules, because the appropriateness of any assay largely depends on the question being asked and the system being used. Moreover, no individual assay is perfect for every situation, calling for the use of multiple techniques to properly monitor autophagy in each experimental setting. Finally, several core components of the autophagy machinery have been implicated in distinct autophagic processes (canonical and noncanonical autophagy), implying that genetic approaches to block autophagy should rely on targeting two or more autophagy-related genes that ideally participate in distinct steps of the pathway. Along similar lines, because multiple proteins involved in autophagy also regulate other cellular pathways including apoptosis, not all of them can be used as a specific marker for bona fide autophagic responses. Here, we critically discuss current methods of assessing autophagy and the information they can, or cannot, provide. Our ultimate goal is to encourage intellectual and technical innovation in the field

Plymouth Electronic Archive and Research Library

Large-scale phenotyping of patients with long COVID post-hospitalization reveals mechanistic subtypes of disease

Author: Abel K.
Adamali H.
Adeloye D.
Adeniji K.
Adeyemi O.
Adrego R.
Agranoff D.
Agwuh K.
Ahmad S.
Ahmed K.A.
Ahmed R.
Ahwireng N.
Ail D.
Ainsworth M.
Al-Sheklly B.
Alamoudi A.
Aldera E.L.
Alegria A.
Alex B.
Ali M.
Aljaroof M.
Allan L.
Allen R.
Allen S.
Allerton L.
Allsop L.
Allt A.M.
Almeida P.
Altmann D.
Amoils S.
Anderson D.
Andrikopoulos P.
Angus B.
Antoniades C.
Arbane G.
Arias A.M.
Armour C.
Armstrong J.A.
Armstrong L.
Armstrong N.
Arnold D.
Arnold H.
Ascough S.
Ashish A.
Ashish A.
Ashworth A.
Ashworth M.
Ashworth M.
Asiimwe I.G.
Aslani S.
Assefa-Kebede H.
Atkin C.
Atkin P.
Atkinson D.
Aul R.
Aung H.
Austin L.
Avram C.
Avramidis N.
Ayoub A.
Babores M.
Bach B.
Baggott R.
Bagshaw J.
Baguley D.
Bailey E.
Baillie J.K.
Baillie J.K.
Baillie J.K.
Bain S.
Bakali M.
Bakau M.
Bakshi S.
Baldry E.
Baldwin D.
Baldwin M.
Ballard C.
Banerjee A.
Bang D.
Barclay W.S.
Bari S.
Barker R.E.
Barlow G.
Barlow S.L.
Barman L.
Barnass S.
Barran P.
Barratt S.
Barrett F.
Barrett N.
Basire D.
Bassford C.
Basu N.
Basude S.
Bates A.
Bates M.
Batterham R.
Baxendale H.
Baxter D.
Baxter G.
Bayes H.
Beadsworth M.
Beadsworth M.
Beckett P.
Beggs M.
Begum M.
Beirne P.
Bell M.
Bell R.
Bennett K.
Beranova E.
Bermperi A.
Bernatoniene J.
Berridge A.
Berridge J.
Berry C.
Berry C.
Best N.
Betts S.
Bevan E.
Bhui K.
Bingham M.
Birchall K.
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Valabhji J.
Vallotton N.
van Tonder L.
Vancheeswaran R.
Ventura M.
Vere J.
Vickers C.
Vincent R.
Vincent-Smith L.
Vinson B.
Visuvanathan S.
Vogiatzis I.
Vuylsteke A.
Waddy S.
Wade E.
Wade P.
Wain L.V.
Wainwright T.
Wajero L.
Wake R.
Walden A.
Walder S.
Walker S.
Walker S.
Wall E.
Wallis T.
Walmsley S.
Walsh J.A.
Walsh S.
Warburton L.
Ward T.J.C.
Warwick K.
Wassall H.
Waterson S.
Watson E.
Watson J.
Watson L.
Webster M.
Welch C.
Welch H.
Welsh B.
Welters I.
Wessely S.
West S.
Weston H.
Wham M.
Wheeler H.
White S.
Whitehead V.
Whitehouse T.
Whitney J.
Whittaker P.
Whittaker S.
Whittam B.
Whittington A.
Whitworth V.
Wight A.
Wijesinghe M.
Wilcock E.
Wild J.
Wilkins M.
Wilkinson D.
Williams B.
Williams J.
Williams M.
Williams N.
Williams N.
Williams-Howard S.A.
Willicombe M.
Willis G.
Willoughby J.
Wilson A.
Wilson D.
Wilson I.
Wilson L.
Winchester S.
Window N.
Wiselka M.
Witham M.
Wolf-Roberts R.
Wolverson A.
Wood C.
Woodhead F.
Woods J.
Wootton D.
Wootton D.G.
Wootton D.G.
Workman A.
Wormleighton J.
Worsley J.
Wraith D.
Wright C.
Wright L.
Wright S.
Wrobel N.
Wyles J.
Wynter I.
Xie C.
Xu M.
Yasmin N.
Yasmin S.
Yates B.
Yates T.
Yip K.P.
Young A.
Young B.
Young P.
Young S.
Yousuf A.J.
Zambon M.
Zawia A.
Zeidan L.
Zhang J.E.
Zhao B.
Zheng B.
Zongo O.
Publication venue: Springer Science and Business Media LLC
Publication date: 01/04/2024
Field of study

One in ten severe acute respiratory syndrome coronavirus 2 infections result in prolonged symptoms termed long coronavirus disease (COVID), yet disease phenotypes and mechanisms are poorly understood1. Here we profiled 368 plasma proteins in 657 participants ≥3 months following hospitalization. Of these, 426 had at least one long COVID symptom and 233 had fully recovered. Elevated markers of myeloid inflammation and complement activation were associated with long COVID. IL-1R2, MATN2 and COLEC12 were associated with cardiorespiratory symptoms, fatigue and anxiety/depression; MATN2, CSF3 and C1QA were elevated in gastrointestinal symptoms and C1QA was elevated in cognitive impairment. Additional markers of alterations in nerve tissue repair (SPON-1 and NFASC) were elevated in those with cognitive impairment and SCG3, suggestive of brain–gut axis disturbance, was elevated in gastrointestinal symptoms. Severe acute respiratory syndrome coronavirus 2-specific immunoglobulin G (IgG) was persistently elevated in some individuals with long COVID, but virus was not detected in sputum. Analysis of inflammatory markers in nasal fluids showed no association with symptoms. Our study aimed to understand inflammatory processes that underlie long COVID and was not designed for biomarker discovery. Our findings suggest that specific inflammatory pathways related to tissue damage are implicated in subtypes of long COVID, which might be targeted in future therapeutic trials

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