139 research outputs found
Long-term results of 32-mm alumina-on-alumina THA for avascular necrosis of the femoral head
- Author
- A Adili
- A Kannan
- AF Brooker
- AJ Hart
- Andrea Piazzolla
- Angela Notarnicola
- BF Wei
- Biagio Moretti
- BJ McGrory
- C Nich
- C Restrepo
- CA Engh
- CJ Ortiguera
- DJ Berry
- E Garcia-Cimbrelo
- E Garcia-Cimbrelo
- E GarcĂa-Rey
- EL Kaplan
- Giuseppe Solarino
- J Livermore
- J Zustin
- JG DeLee
- K Hardinge
- L Massari
- L Savarino
- LM Jazrawi
- Lorenzo Moretti
- M Hamadouche
- ME Steinberg
- NL Millar
- P Bizot
- P Bizot
- P Harvie
- RP Pitto
- S Lazarinis
- Silvana De Giorgi
- Silvio Tafuri
- TA Gruen
- V Eswaramoorthy
- VC Bose
- WH Harris
- WN Capello
- YC Ha
- YH Kim
- YS Park
- Publication venue
- Springer Milan
- Publication date
- 01/01/2012
- Field of study
Get PDFBACKGROUND:
Ceramic bearings in total hip arthroplasty (THA) have been introduced in clinical practice to minimize the problem of polyethylene particle-induced osteolysis. The aim of the study is to report the results of 68 consecutive alumina-on-alumina THAs done in 61 patients for avascular necrosis (AVN) of the femoral head.
MATERIALS AND METHODS:
In all implants a press-fit cup was used; it was combined with a 32-mm alumina head and with titanium-alloy stems. The mean age at surgery was 50 years. At an average follow-up of 13 years two hips have been revised, one for periprosthetic infection and one for excessive abduction of the cup.
RESULTS:
No revision for aseptic loosening is recorded; one anatomical cementless femoral stem had radiological evidence of definite aseptic loosening. No dislocations occurred, and no osteolysis was observed.
CONCLUSIONS:
The results support the application of alumina-alumina THA for long-lasting replacements
Effective Rheology of Bubbles Moving in a Capillary Tube
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- Publication venue
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- Publication date
- 16/03/2012
- Field of study
Full text linkWe calculate the average volumetric flux versus pressure drop of bubbles
moving in a single capillary tube with varying diameter, finding a square-root
relation from mapping the flow equations onto that of a driven overdamped
pendulum. The calculation is based on a derivation of the equation of motion of
a bubble train from considering the capillary forces and the entropy production
associated with the viscous flow. We also calculate the configurational
probability of the positions of the bubbles.Comment: 4 pages, 1 figur
Fundamental limits of repeaterless quantum communications
- Author
- AB Dutta
- AS Holevo
- B Schumacher
- C Ottaviani
- C Ottaviani
- C Weedbrook
- C Weedbrook
- C Weedbrook
- C Weedbrook
- C Weedbrook
- CH Bennett
- CH Bennett
- CH Bennett
- D Dequal
- D Leung
- F Grosshans
- G Bowen
- G Vallone
- H-J Briegel
- H-K Lo
- HJ Kimble
- I Devetak
- I Devetak
- I Devetak
- J Niset
- K Horodecki
- K Modi
- L Banchi
- M Christiandl
- M Horodecki
- M Takeoka
- MA Nielsen
- MM Wolf
- N Gisin
- N Hosseinidehaj
- R Garca-PatrĂłn
- RF Werner
- S Albeverio
- S Bose
- S Lloyd
- S Pirandola
- S Pirandola
- S Pirandola
- S Pirandola
- S Pirandola
- S Pirandola
- S Pirandola
- S Pirandola
- S Scheel
- SL Braunstein
- SL Braunstein
- SL Braunstein
- UL Andersen
- V Scarani
- V Vedral
- V Vedral
- V Vedral
- VC Usenko
- XY Chen
- Z Ji
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- 05/01/2016
- Field of study
Get PDFQuantum communications promises reliable transmission of quantum information, efficient distribution of entanglement and generation of completely secure keys. For all these tasks, we need to determine the optimal point-to-point rates that are achievable by two remote parties at the ends of a quantum channel, without restrictions on their local operations and classical communication, which can be unlimited and two-way. These two-way assisted capacities represent the ultimate rates that are reachable without quantum repeaters. Here, by constructing an upper bound based on the relative entropy of entanglement and devising a dimension-independent technique dubbed âteleportation stretchingâ, we establish these capacities for many fundamental channels, namely bosonic lossy channels, quantum-limited amplifiers, dephasing and erasure channels in arbitrary dimension. In particular, we exactly determine the fundamental rate-loss tradeoff affecting any protocol of quantum key distribution. Our findings set the limits of point-to-point quantum communications and provide precise and general benchmarks for quantum repeaters
A Zebrafish Model of Roberts Syndrome Reveals That Esco2 Depletion Interferes with Development by Disrupting the Cell Cycle
- Author
- A Musio
- A Pauli
- AR Ball Jr
- B Schule
- B Thisse
- B Xiong
- B Zhang
- B Zhang
- BD Rowland
- CA Schaaf
- Cristin G. Print
- D Dorsett
- D Dorsett
- D Dorsett
- D Dorsett
- D Gerlich
- D Ivanov
- D Schmidt
- DJ Van Den Berg
- E Unal
- ED Rubio
- ET Tonkin
- F Beckouet
- F Hou
- GL Moldovan
- H Vega
- H Vega
- HH Qi
- ID Krantz
- J Herrmann
- J Horsfield
- J Liu
- J Liu
- J Liu
- J Shepard
- J Zhang
- JL Galloway
- JM Craig
- JM Heidinger-Pauli
- JM Rhodes
- Julia A. Horsfield
- Justin Kumar
- K Nasmyth
- KC Lee
- KS Wendt
- M Gause
- M Gause
- M Gordillo
- M Monnich
- M Westerfield
- MA Deardorff
- MA Kenna
- Maren Mönnich
- MB Walker
- MH Kagey
- R Ciosk
- R Kageyama
- RA Rollins
- RD Knight
- RV Skibbens
- S Berghmans
- S Hadjur
- S Kawauchi
- S Schulz
- T Bose
- T Strachan
- T Sutani
- T Vierbuchen
- TR Ben-Shahar
- V Borges
- V Parelho
- VC Seitan
- W Stedman
- Z Misulovin
- Zoë Kuriger
- Publication venue
- Public Library of Science
- Publication date
- 26/05/2011
- Field of study
Get PDFThe human developmental diseases Cornelia de Lange Syndrome (CdLS) and Roberts Syndrome (RBS) are both caused by mutations in proteins responsible for sister chromatid cohesion. Cohesion is mediated by a multi-subunit complex called cohesin, which is loaded onto chromosomes by NIPBL. Once on chromosomes, cohesin binding is stabilized in S phase upon acetylation by ESCO2. CdLS is caused by heterozygous mutations in NIPBL or cohesin subunits SMC1A and SMC3, and RBS is caused by homozygous mutations in ESCO2. The genetic cause of both CdLS and RBS reside within the chromosome cohesion apparatus, and therefore they are collectively known as âcohesinopathiesâ. However, the two syndromes have distinct phenotypes, with differences not explained by their shared ontology. In this study, we have used the zebrafish model to distinguish between developmental pathways downstream of cohesin itself, or its acetylase ESCO2. Esco2 depleted zebrafish embryos exhibit features that resemble RBS, including mitotic defects, craniofacial abnormalities and limb truncations. A microarray analysis of Esco2-depleted embryos revealed that different subsets of genes are regulated downstream of Esco2 when compared with cohesin subunit Rad21. Genes downstream of Rad21 showed significant enrichment for transcriptional regulators, while Esco2-regulated genes were more likely to be involved the cell cycle or apoptosis. RNA in situ hybridization showed that runx1, which is spatiotemporally regulated by cohesin, is expressed normally in Esco2-depleted embryos. Furthermore, myca, which is downregulated in rad21 mutants, is upregulated in Esco2-depleted embryos. High levels of cell death contributed to the morphology of Esco2-depleted embryos without affecting specific developmental pathways. We propose that cell proliferation defects and apoptosis could be the primary cause of the features of RBS. Our results show that mutations in different elements of the cohesion apparatus have distinct developmental outcomes, and provide insight into why CdLS and RBS are distinct diseases
Gout and risk of chronic kidney disease and nephrolithiasis: meta-analysis of observational studies
- Author
- AK Bello
- B Bose
- C Hsu
- C Kuo
- C Padang
- C Scales
- CA Sarawate
- CF Kuo
- CF Kuo
- Christian D Mallen
- D Khanna
- DH Solomon
- E Krishnan
- E Pascual
- E Roddy
- E Roddy
- E Roddy
- E Roddy
- Edward Roddy
- EN Taylor
- EN Taylor
- ES Johnson
- F Liote
- FP Cappuccio
- G Trifiro
- H El-Zawawy
- HJ Kramer
- HK Choi
- HM Kramer
- JB OâSullivan
- JB Rosenfeld
- JH Kellgren
- John Belcher
- JPT Higgins
- K Matsushita
- KH Yu
- L Berger
- L Cea Soriano
- LG Glynn
- LR Harrold
- M Jin
- Matthew J Roughley
- MJ Fuldeore
- MS Parmar
- MY Lin
- N Chen
- National Institute for Health and Care Excellence
- National Kidney Foundation
- OB Schaffalitzky De Muckadell
- P Soltész
- PE Stevens
- PH Bennett
- R Ando
- RT Keenan
- S Lusignan de
- SE Liebman
- SL Wallace
- TF YĂŒ
- TF YĂŒ
- TR Mikuls
- VC Kok
- WJ Currie
- WJ Currie
- WJ Fessel
- Y Zhu
- Publication venue
- 'Springer Science and Business Media LLC'
- Publication date
- Field of study
Get PDFAlignment of the ALICE Inner Tracking System with cosmic-ray tracks
- Author
- Aamodt K
- Abel N
- Abeysekara U
- Adamova D
- Aggarwal M
- Agocs AG
- Ahammed Z
- Ahmad A
- Ahmad N
- Ahn SU
- Akimoto R
- Akindinov A
- Aleksandrov D
- Alessandro B
- Alici A
- Alme J
- Alt T
- Altini V
- Altinpinar S
- Andrei C
- Andronic A
- Anelli G
- Angelov V
- Anson C
- Anticic T
- Antinori F
- Antinori S
- Antipin K
- Antonczyk D
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- Appelshauser H
- Arcelli S
- Arceo R
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- Arsene IC
- Asryan A
- Augustinus A
- Averbeck R
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- Awes TC
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- Azmi MD
- Bablok S
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- Biolcati E
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- Busch O
- Buthelezi Z
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- Cahuantzi MR
- Cai X
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- Zagreev B
- Zalite A
- Zampolli C
- Zanevsky Y
- Zaporozhets S
- Zarochentsev A
- Zavada P
- Zbroszczyk H
- Zelnicek P
- Zenin A
- Zepeda A
- Zetina LM
- Zgura I
- Zhalov M
- Zhang X
- Zhou D
- Zhou S
- Zhu J
- Zichichi A
- Zinchenko A
- Zinovjev G
- Zoccarato Y
- Zychacek V
- Zynovyev M
- Publication venue
- Publication date
- 01/01/2010
- Field of study
Get PDF37 pages, 15 figures, revised version, accepted by JINSTALICE (A Large Ion Collider Experiment) is the LHC (Large Hadron Collider) experiment devoted to investigating the strongly interacting matter created in nucleus-nucleus collisions at the LHC energies. The ALICE ITS, Inner Tracking System, consists of six cylindrical layers of silicon detectors with three different technologies; in the outward direction: two layers of pixel detectors, two layers each of drift, and strip detectors. The number of parameters to be determined in the spatial alignment of the 2198 sensor modules of the ITS is about 13,000. The target alignment precision is well below 10 micron in some cases (pixels). The sources of alignment information include survey measurements, and the reconstructed tracks from cosmic rays and from proton-proton collisions. The main track-based alignment method uses the Millepede global approach. An iterative local method was developed and used as well. We present the results obtained for the ITS alignment using about 10^5 charged tracks from cosmic rays that have been collected during summer 2008, with the ALICE solenoidal magnet switched off.Peer reviewe
Global burden of 369 diseases and injuries in 204 countries and territories, 1990-2019: a systematic analysis for the Global Burden of Disease Study 2019
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- Abbafati C
- Abbas KM
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- Pangaribuan HU
- Park E-K
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- Rahman MA
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- Rajati F
- Rakovac I
- Ram P
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- Ranabhat CL
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- Rao PC
- Rao SJ
- Rasella D
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- Renjith V
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- Resnikoff S
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- Ribeiro ALP
- Ribeiro D
- Ribeiro DC
- Rickard J
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- Rivera JA
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- Roberts S
- Robinson SR
- Rodriguez-Ramirez S
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- Rolfe S
- Romoli M
- Ronfani L
- Room R
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- Roth GA
- Rothenbacher D
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- Rumisha SF
- Rwegerera GM
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- Sabour S
- Sachdev PS
- Saddik B
- Sadeghi E
- Sadeghi M
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- Schutte AE
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- Schwendicke F
- Section MPA
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- Serdar B
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- Sha F
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- Siabani S
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- Sigfusdottir ID
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- Silva DAS
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- Simpson KE
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- Skou ST
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- Smith A
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- Sobngwi E
- Soheili A
- Sokhan A
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- Somefun OD
- Soofi M
- Sorensen RJD
- Soriano JB
- Sorrie MB
- Soshnikov S
- Soyiri IN
- Spencer CN
- Spotin A
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- Sreeramareddy CT
- Srinivasan V
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- Stanaway JD
- Stark BA
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- Stein DJ
- Steiner C
- Steiner TJ
- Steuben KM
- Stockfelt L
- Stokes MA
- Stovner LJ
- Straif K
- Stranges S
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- Suchdev PS
- Sudaryanto A
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- Suleria HAR
- Sulo G
- Sultan I
- Swope CB
- Sykes BL
- Sylte DO
- Szocska M
- Szumowski L
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- Tabb KM
- Tabuchi T
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- Taddele BW
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- Troeger CE
- Truelsen TC
- Tsai AC
- Tsatsakis A
- Tyrovolas S
- Uddin R
- Ullah I
- Ullah S
- Umeokonkwo CD
- Undurraga EA
- Unnikrishnan B
- Upadhyay E
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- Valdez PR
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- Vardavas C
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- Venketasubramanian N
- Vidale S
- Violante FS
- Vlassov V
- Vollset SE
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- Vukovic A
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- Wallin MT
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- Wickramasinghe ND
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- Wijeratne T
- Wilner LB
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- Wojtyniak B
- Woldu G
- Wolfe CDA
- Wondmeneh TG
- Wondmieneh AB
- Wool EE
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- Wu A-M
- Wu C
- Wu J
- Wunrow HY
- Xie Y
- Xu G
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- Yaminfirooz M
- Yano Y
- Yaya S
- Yazdi-Feyzabadi V
- Yearwood JA
- Yeheyis TY
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- Yilgwan CS
- Yilma MT
- Yip P
- Yonemoto N
- Yoon S-J
- York HW
- Younis MZ
- Younker TP
- Yousefi B
- Yousefi Z
- Yousefifard M
- Yousefinezhadi T
- Yousuf AY
- Yu C
- Yu Y
- Yuan C-W
- Yuce D
- Yusefzadeh H
- Zadey S
- Zahabi SS
- Zaidi SS
- Zaki L
- Zaki MES
- Zakzuk J
- Zamani M
- Zamanian M
- Zandian H
- Zangeneh A
- Zarafshan H
- Zastrozhin MS
- Zewdie KA
- Zhang J
- Zhang Y
- Zhang Z-J
- Zhao JT
- Zhao X-JG
- Zhao Y
- Zheleva B
- Zheng P
- Zhou M
- Zhu C
- Ziapour A
- Zimsen SRM
- Zlavog BS
- Zodpey S
- Publication venue
- 'Elsevier BV'
- Publication date
- 17/10/2020
- Field of study
Get PDFFive insights from the Global Burden of Disease Study 2019
- Author
- Abbafati C
- Abbas KM
- Abbasi M
- Abbasi-Kangevari M
- Abbasifard M
- Abbastabar H
- Abd El Razek HM
- Abd El Razek MM
- Abd-Allah F
- Abdelalim A
- Abdollahi M
- Abdollahpour I
- Abdulkader RS
- Abdullah KH
- Abedi A
- Abedi P
- Abegaz KH
- Abolhassani H
- Abosetugn AE
- Aboyans V
- Abrams EM
- Abreu LG
- Abrigo MRM
- Abu Haimed AK
- Abu-Gharbieh E
- Abu-Raddad LJ
- Abualhasan A
- Abushouk AI
- Acebedo A
- Ackerman IN
- Adabi M
- Adair T
- Adamu AA
- Adebayo OM
- Adedeji IA
- Adekanmbi V
- Adelson JD
- Adeoye AM
- Adetokunboh OO
- Adham D
- Advani SM
- Afarideh M
- Afshari M
- Afshin A
- Agardh EE
- Agarwal G
- Agasthi P
- Agesa KM
- Aghaali M
- Aghamir SMK
- Agrawal A
- Ahmad T
- Ahmadi A
- Ahmadi K
- Ahmadi M
- Ahmadieh H
- Ahmadpour E
- Ahmed MB
- Aji B
- Akalu TY
- Akinyemi RO
- Akinyemiju T
- Akombi B
- Akunna CJ
- Al-Aly Z
- Al-Mekhlafi HM
- Al-Raddadi RM
- Alahdab F
- Alam K
- Alam N
- Alam S
- Alam T
- Alanezi FM
- Alanzi TM
- Albertson SB
- Alcalde-Rabanal JE
- Alema NM
- Alemu BW
- Alemu YM
- Alhabib KF
- Alhassan RK
- Ali M
- Ali S
- Alicandro G
- Alijanzadeh M
- Alinia C
- Alipour V
- Alizade H
- Aljunid SM
- Alla F
- Allebeck P
- Almadi MAH
- Almasi A
- Almasi-Hashiani A
- Almasri NA
- Almulhim AM
- Alonso J
- Altirkawi KA
- Alumran AK
- Alvis-Guzman N
- Alvis-Zakzuk NJ
- Amare AT
- Amare B
- Amini S
- Amini-Rarani M
- Aminorroaya A
- Amiri F
- Amit AML
- Amugsi DA
- Amul GGH
- Anbesu EW
- Ancuceanu R
- Anderlini D
- Anderson JA
- Andrei CL
- Andrei T
- Androudi S
- Angus C
- Anjomshoa M
- Ansari F
- Ansari I
- Ansari-Moghaddam A
- Antonazzo IC
- Antonio CAT
- Antony CM
- Antriyandarti E
- Anvari D
- Anwer R
- Appiah SCY
- Arab-Zozani M
- Arabloo J
- Aravkin AY
- Arba AAK
- Aremu O
- Ariani F
- Aripov T
- Armoon B
- Arnlov J
- Arowosegbe OO
- Aryal KK
- Arzani A
- Asaad M
- Asadi-Aliabadi M
- Asadi-Pooya AA
- Asgari S
- Asghari B
- Ashbaugh C
- Assmus M
- Atafar Z
- Athari SS
- Atnafu DD
- Atout MMW
- Atre SR
- Atteraya MS
- Ausloos F
- Ausloos M
- Avila-Burgos L
- Avokpaho EFGA
- Ayano G
- Ayanore MA
- Aynalem GL
- Aynalem YA
- Ayza MA
- Azari S
- Azarian G
- Azene ZN
- Azhar G
- Azzopardi PS
- Babaee E
- Badawi A
- Badiye AD
- Bagherzadeh M
- Bagli E
- Bahrami MA
- Baig AA
- Bairwa M
- Bakhshaei MH
- Bakhtiari A
- Bakkannavar SM
- Balachandran A
- Balakrishnan S
- Balalla S
- Balassyano S
- Baldasseroni A
- Bali AO
- Ball K
- Ballew SH
- Balzi D
- Banach M
- Bandpei MAM
- Banerjee SK
- Banik PC
- Bannick MS
- Bante AB
- Bante SA
- Baraki AG
- Barboza MA
- Barker-Collo SL
- Barnighausen TW
- Barrero LH
- Barthelemy CM
- Barua L
- Barzegar A
- Basaleem H
- Bassat Q
- Basu S
- Baune BT
- Bayati M
- Baye BA
- Bazmandegan G
- Becker JS
- Bedi N
- Beghi E
- Behzadifar M
- Bejot Y
- Bekuma TTT
- Bell ML
- Bello AK
- Ben L
- Bender RG
- Bennett DA
- Bennitt FB
- Bensenor IM
- Benziger CP
- Berhe K
- Berman AE
- Bernabe E
- Bernstein RS
- Bertolacci GJ
- Bhagavathula AS
- Bhageerathy R
- Bhala N
- Bhandari D
- Bhardwaj P
- Bhat AG
- Bhattacharyya K
- Bhattarai S
- Bhutta ZA
- Bibi S
- Bicer BK
- Biehl MH
- Bijani A
- Bikbov B
- Bilano V
- Bin Sayeed MS
- Bin Zaman S
- Biondi A
- Birihane BM
- Bisanzio D
- Bisignano C
- Biswas RK
- Bitew H
- Bjorge T
- Bockarie MJ
- Bohlouli S
- Bohluli M
- Bojia HA
- Bolla SR
- Boloor A
- Boon-Dooley AS
- Borges G
- Borzi AM
- Borzouei S
- Bose D
- Bosetti C
- Boston S
- Boufous S
- Bourne R
- Brady OJ
- Braithwaite D
- Brauer M
- Brayne C
- Breitborde NJK
- Breitner S
- Brenner H
- Breusov AV
- Briant PS
- Briggs AM
- Briko AN
- Briko NI
- Britton GB
- Brugha T
- Bryazka D
- Buchbinder R
- Bumgarner BR
- Burkart K
- Burnett RT
- Busse R
- Butt ZA
- Caetano dos Santos FL
- Cahill LE
- Cahuana-Hurtado L
- Cai T
- Callender CSKH
- Camera LA
- Campos-Nonato IR
- Cao J
- Car J
- Car LT
- Cardenas R
- Carreras G
- Carrero JJ
- Carvalho F
- Castaldelli-Maia JM
- Castaneda-Orjuela CA
- Castelpietra G
- Castle CD
- Castro E
- Castro F
- Catala-Lopez F
- Causey K
- Cederroth CR
- Cercy KM
- Cerin E
- Chalek J
- Chandan JS
- Chang AR
- Chang AY
- Chang J-C
- Chang K-L
- Charan J
- Charlson FJ
- Chattu VK
- Chaturvedi S
- Cherbuin N
- Chimed-Ochir O
- Chin KL
- Chirinos-Caceres JL
- Cho DY
- Choi J-YJ
- Christensen H
- Chu D-T
- Chung MT
- Chung S-C
- Cicuttini FM
- Ciobanu LG
- Cirillo M
- Cislaghi B
- Classen TKD
- Cohen AJ
- Collins EL
- Comfort H
- Compton K
- Conti S
- Cooper OR
- Corso B
- Cortesi PA
- Costa VM
- Cousin E
- Cowden RG
- Cowie BC
- Cromwell EA
- Croneberger AJ
- Cross DH
- Cross M
- Crowe CS
- Cruz JA
- Cummins S
- Cunningham M
- D'Amico E
- da Silva DD
- Dahlawi SMA
- Dai H
- Dai H
- Damasceno AAM
- Damiani G
- Dandona L
- Dandona R
- Daneshpajouhnejad P
- Dangel WJ
- Danielsson A-K
- Dargan PI
- Darshan BB
- Darwesh AM
- Daryani A
- Das Gupta R
- Das Neves J
- Das JK
- Dash AP
- Davey G
- Davila-Cervantes CA
- Davis AC
- Davitoiu DV
- Davletov K
- De Leo D
- De Neve J-W
- Dean FE
- DeCleene NK
- Deen A
- Defo BK
- Degenhardt L
- DeLang M
- Dellavalle RP
- Demeke FM
- Demoz GT
- Demsie DG
- Denova-Gutierrez E
- Dereje ND
- Deribe K
- Dervenis N
- Desai R
- Desalew A
- Dessie GA
- Deuba K
- Dharmaratne SD
- Dhungana GP
- Dianatinasab M
- Diaz D
- Dichgans M
- Didarloo A
- Dingels ZV
- Dippenaar IN
- Dirac MA
- Djalalinia S
- Do HT
- Dokova K
- Doku DT
- Dolecek C
- Dolgert AJ
- Dorostkar F
- Doshi CP
- Doshi PP
- Doshmangir L
- Douiri A
- Doxey MC
- Doyle KE
- Driscoll TR
- Dubljanin E
- Dunachie SJ
- Duncan BB
- Duraes AR
- Eagan AW
- Ebrahimi H
- Edvardsson D
- Effiong A
- Ehrlich JR
- El Nahas N
- El Sayed I
- El Tantawi M
- El-Jaafary SI
- Elbarazi I
- Elgendy IY
- Elhabashy HR
- Elsharkawy A
- Elyazar IRF
- Emamian MH
- Emmons-Bell S
- Erskine HE
- Eshrati B
- Eskandari K
- Eskandarieh S
- Esmaeilnejad S
- Esmaeilzadeh F
- Esteghamati A
- Esteghamati S
- Estep K
- Etemadi A
- Etisso AE
- Ezekannagha O
- Fanzo J
- Farag T
- Farahmand M
- Faraj A
- Faraon EJA
- Fareed M
- Faridnia R
- Farinha CSES
- Farioli A
- Faris PS
- Faro A
- Faruque M
- Farzadfar F
- Fattahi N
- Fazaeli AA
- Fazlzadeh M
- Feigin VL
- Feldman R
- Fereshtehnejad S-M
- Fernandes E
- Ferrara G
- Ferrara P
- Ferrari AJ
- Ferreira ML
- Feyissa GT
- Filip I
- Fischer F
- Fisher JL
- Fitzgerald R
- Flohr C
- Flor LS
- Foigt NA
- Folayan MO
- Fomenkov AA
- Force LM
- Fornari C
- Forooshani ZSD
- Foroutan M
- Fox JT
- Francis JM
- Frank TD
- Franklin RC
- Freitas M
- Fu W
- Fukumoto T
- Fukutaki K
- Fuller JE
- Fullman N
- Furtado JM
- Gad MM
- Gaidhane AM
- Gakidou E
- Galles NC
- Gallus S
- Gamkrelidze A
- Garcia-Basteiro AL
- Gardner WM
- Geberemariyam BS
- Gebrehiwot AM
- Gebremedhin KB
- Gebremeskel GG
- Gebremeskel LG
- Gebresillassie BM
- Gebreslassie AAAA
- Gela JD
- Geramo YCD
- Geremew A
- Gesesew HA
- Gething PW
- Gezae KE
- Ghadimi M
- Ghadiri K
- Ghaffarifar F
- Ghafourifard M
- Ghajar A
- Ghamari F
- Ghashghaee A
- Ghiasvand H
- Ghith N
- Gholamian A
- Ghosh R
- Giampaoli S
- Gilani SA
- Gill PS
- Gill TK
- Gillum RF
- Ginawi IA
- Ginindza TG
- Gitimoghaddam M
- Giussani G
- Glagn M
- Glushkova EV
- Gnedovskaya EV
- Godinho MA
- Goharinezhad S
- Golechha M
- Goli S
- Gomez RS
- Gona PN
- Gopalani SV
- Goren E
- Gorini G
- Gorman TM
- Gottlich HC
- Goudarzi H
- Goudarzian AH
- Goulart AC
- Goulart BNG
- Grada A
- Greaves F
- Grivna M
- Grosso G
- Gubari MIM
- Gudi N
- Gugnani HC
- Guimaraes ALS
- Guimaraes RA
- Guled RA
- Gultie T
- Guo G
- Guo Y
- Gupta R
- Gupta R
- Gupta T
- Haagsma JA
- Hachinski V
- Haddock B
- Hafezi-Nejad N
- Hafiz A
- Hagins H
- Haile LM
- Haile TG
- Haj-Mirzaian A
- Haj-Mirzaian A
- Hall BJ
- Halvaei I
- Hamadeh RR
- Hameed S
- Hamidi S
- Hamilton EB
- Hammer MS
- Han C
- Han H
- Handiso DW
- Hanif A
- Hankey GJ
- Hanson SW
- Haririan H
- Haro JM
- Harvey JD
- Hasaballah AI
- Hasan MM
- Hasanpoor E
- Hasanzadeh A
- Hashemian M
- Hashi A
- Hassan A
- Hassan S
- Hassanipour S
- Hassankhani H
- Havmoeller RJ
- Hawariat FGW
- Hay RJ
- Hay SI
- Hayat K
- Hayoon AG
- Heibati B
- Heidari B
- Heidari G
- Heidari-Soureshjani R
- Hendrie D
- Henny K
- Henok A
- Henrikson HJ
- Henry NJ
- Herbert ME
- Herrera AMM
- Herteliu C
- Heydarpour F
- Hird TR
- Ho HC
- Hoek HW
- Hole MK
- Holla R
- Hollingsworth B
- Hoogar P
- Hopf KP
- Horita N
- Hosgood HD
- Hossain N
- Hosseini M
- Hosseinzadeh M
- Hostiuc M
- Hostiuc S
- Househ M
- Hoy DG
- Hsairi M
- Hsiao T
- Hsieh VC-R
- Hu G
- Hu K
- Huda TM
- Hugo FN
- Humayun A
- Hussain R
- Huynh CK
- Hwang B-F
- Iannucci VC
- Iavicoli I
- Ibeneme CU
- Ibitoye SE
- Ikeda N
- Ikuta KS
- Il Shin J
- Ilesanmi OS
- Ilic IM
- Ilic MD
- Imani-Nasab MH
- Inbaraj LR
- Ippolito H
- Iqbal U
- Irvani SSN
- Irvine CMS
- Islam M
- Islam MM
- Islam SMS
- Islami F
- Iso H
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- Publication venue
- Publication date
- 01/01/2020
- Field of study
Get PDFThe Global Burden of Diseases, Injuries, and Risk Factors Study (GBD) 2019 provides a rules-based synthesis of the available evidence on levels and trends in health outcomes, a diverse set of risk factors, and health system responses. GBD 2019 covered 204 countries and territories, as well as first administrative level disaggregations for 22 countries, from 1990 to 2019. Because GBD is highly standardised and comprehensive, spanning both fatal and non-fatal outcomes, and uses a mutually exclusive and collectively exhaustive list of hierarchical disease and injury causes, the study provides a powerful basis for detailed and broad insights on global health trends and emerging challenges. GBD 2019 incorporates data from 281 586 sources and provides more than 3.5 billion estimates of health outcome and health system measures of interest for global, national, and subnational policy dialogue. All GBD estimates are publicly available and adhere to the Guidelines on Accurate and Transparent Health Estimate Reporting. From this vast amount of information, five key insights that are important for health, social, and economic development strategies have been distilled. These insights are subject to the many limitations outlined in each of the component GBD capstone papers.Peer reviewe
Pan-cancer analysis of whole genomes
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- The ICGC/TCGA Pan-Cancer Analysis of Whole Genomes Consortium View Correspondence (jump link)
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- Zhang
- Zhang
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- Zhang H. b
- Zhao
- Zheng
- Zhou
- Zhou
- Zhu
- Zhu
- zi zj
- zm Jayaseelan
- Zou
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- zt Kim
- zw Lewis
- Ă. A. th
- Ă. sk
- Publication venue
- Publication date
- 11/12/2019
- Field of study
Get PDFCancer is driven by genetic change, and the advent of massively parallel sequencing has enabled systematic documentation of this variation at the whole-genome scale(1-3). Here we report the integrative analysis of 2,658 whole-cancer genomes and their matching normal tissues across 38 tumour types from the Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium of the International Cancer Genome Consortium (ICGC) and The Cancer Genome Atlas (TCGA). We describe the generation of the PCAWG resource, facilitated by international data sharing using compute clouds. On average, cancer genomes contained 4-5 driver mutations when combining coding and non-coding genomic elements; however, in around 5% of cases no drivers were identified, suggesting that cancer driver discovery is not yet complete. Chromothripsis, in which many clustered structural variants arise in a single catastrophic event, is frequently an early event in tumour evolution; in acral melanoma, for example, these events precede most somatic point mutations and affect several cancer-associated genes simultaneously. Cancers with abnormal telomere maintenance often originate from tissues with low replicative activity and show several mechanisms of preventing telomere attrition to critical levels. Common and rare germline variants affect patterns of somatic mutation, including point mutations, structural variants and somatic retrotransposition. A collection of papers from the PCAWG Consortium describes non-coding mutations that drive cancer beyond those in the TERT promoter(4); identifies new signatures of mutational processes that cause base substitutions, small insertions and deletions and structural variation(5,6); analyses timings and patterns of tumour evolution(7); describes the diverse transcriptional consequences of somatic mutation on splicing, expression levels, fusion genes and promoter activity(8,9); and evaluates a range of more-specialized features of cancer genomes(8,10-18).Peer reviewe
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
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- Ălvarez ĂMC
- Ăvalos Y
- Ănal G
- ĂstĂŒn S
- ÄoliÄ M
- ÄokiÄ J
- Ćœerovnik E
- Publication venue
- 'Informa UK Limited'
- Publication date
- 01/01/2021
- Field of study
Get PDFIn 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
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