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37 research outputs found

Mars Pathfinder mission operations concepts

Author: Dias William C.
Nakata Albert Y.
Sturms Francis M., Jr.
Tai Wallace S.
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Field of study

The Mars Pathfinder Project plans a December 1996 launch of a single spacecraft. After jettisoning a cruise stage, an entry body containing a lander and microrover will directly enter the Mars atmosphere and parachute to a hard landing near the sub-solar latitude of 15 degrees North in July 1997. Primary surface operations last for 30 days. Cost estimates for Pathfinder ground systems development and operations are not only lower in absolute dollars, but also are a lower percentage of total project costs than in past planetary missions. Operations teams will be smaller and fewer than typical flight projects. Operations scenarios have been developed early in the project and are being used to guide operations implementation and flight system design. Recovery of key engineering data from entry, descent, and landing is a top mission priority. These data will be recorded for playback after landing. Real-time tracking of a modified carrier signal through this phase can provide important insight into the spacecraft performance during entry, descent, and landing in the event recorded data is never recovered. Surface scenarios are dominated by microrover activity and lander imaging during 7 hours of the Mars day from 0700 to 1400 local solar time. Efficient uplink and downlink processes have been designed to command the lander and microrover each Mars day

NASA Technical Reports Server

Large scale international replication and meta-analysis study confirms association of the 15q14 locus with myopia. The CREAM consortium

Author: A Fernandez-Medarde
Abhishek Nag
AH Kihara
AI Jobling
Alan F. Wright
Albert Hofman
Albert V. Smith
Alex W. Hewitt
Alireza Mirshahi
AM Solouki
Andres Metspalu
André G. Uitterlinden
Angela Döring
Anke Tönjes
B Lu
Barbara E. Klein
Beate St. Pourcain
Ben A. Oostra
BJ Curtin
Brian W. Fleck
C Jones
Caroline C. W. Klaver
Caroline Hayward
Cathy Williams
Chiea-Chuen Khor
Christian Wolfram
Christopher J. Hammond
Claire L. Simpson
Cornelia M. van Duijn
David A. Mackey
Dominiek D. G. Despriet
Dwight Stambolian
E-Shyong Tai
Eranga Vithana
Federico Murgia
Fernando Rivadeneira
Fumihiko Matsuda
George McMahon
Guðný Eiríksdóttir
H Hayashi
H Nakanishi
Harry Campbell
HM Wu
I Morgan
Igor Rudan
Isao Nakata
James F. Wilson
Jeremy A. Guggenheim
JH Kempen
Jie Jin Wang
JM Ip
Joan E. Bailey-Wilson
Johannes R. Vingerling
Jugnoo S. Rahi
K Striedinger
KA Rose
Karl J. Lackner
Kenji Yamashiro
Konrad Oexle
Kyoko Ohno-Matsui
Larry D. Atwood
Laura Portas
Lennart C. Karssen
Leonieke M. E. van Koolwijk
Leslie J. Raffel
Liang-Kee Goh
LL Lin
M Dirani
M Guldenagel
M He
M. Kamran Ikram
Mary Frances Cotch
Mika Kähönen
MR Deans
NA McBrien
Nagahisa Yoshimura
Najaf Amin
Norbert Pfeiffer
Olavi Pärssinen
Ozren Polasek
Paul Mitchell
Paul N. Baird
Paulus T. V. M. de Jong
PG Hysi
Phillippa M. Cumberland
Pirro G. Hysi
PN Baird
Priya Duggal
Q Wang
Qiao Fan
R Paffenholz
Raphaële Castagné
Reedik Mägi
René Höhn
RH Duparc
Robert Wojciechowski
Ryo Yamada
S Vitale
Sarayut Janmahasatian
Seang-Mei Saw
Shomi Bhattacharya
SM Saw
SM Saw
SM Saw
Sudha K. Iyengar
Taina Rantanen
Tanja Zeller
Terho Lehtimäki
Terri L. Young
Thomas Bettecken
Thomas Meitinger
Tien-Yin Wong
Timothy D. Spector
Tin Aung
TL Young
TL Young
Tõnu Esko
Veronique Vitart
Vilmundur Gudnason
Virginie J. M. Verhoeven
Wanting Tay
Xiaohui Li
Xin Zhou
Xueling Sim
Y Gao
Y Shi
Y Tano
Yi Lu
Yi-Ju Li
Yik-Ying Teo
YJ Li
Z Li
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2012
Field of study

Myopia is a complex genetic disorder and a common cause of visual impairment among working age adults. Genome-wide association studies have identified susceptibility loci on chromosomes 15q14 and 15q25 in Caucasian populations of European ancestry. Here, we present a confirmation and meta-analysis study in which we assessed whether these two loci are also associated with myopia in other populations. The study population comprised 31 cohorts from the Consortium of Refractive Error and Myopia (CREAM) representing 4 different continents with 55,177 individuals; 42,845 Caucasians and 12,332 Asians. We performed a meta-analysis of 14 single nucleotide polymorphisms (SNPs) on 15q14 and 5 SNPs on 15q25 using linear regression analysis with spherical equivalent as a quantitative outcome, adjusted for age and sex. We calculated the odds ratio (OR) of myopia versus hyperopia for carriers of the top-SNP alleles using a fixed effects meta-analysis. At locus 15q14, all SNPs were significantly replicated, with the lowest P value 3.87 × 10 -12 for SNP rs634990 in Caucasians, and 9.65 × 10 -4 for rs8032019 in Asians. The overall meta-analysis provided P value 9.20 × 10 -23 for the top SNP rs634990. The risk of myopia versus hyperopia was OR 1.88 (95 % CI 1.64, 2.16, P < 0.001) for homozygous carriers of the risk allele at the top SNP rs634990, and OR 1.33 (95 % CI 1.19, 1.49, P < 0.001) for heterozygous carriers. SNPs at locus 15q25 did not replicate significantly (P value 5.81 × 10 -2 for top SNP rs939661). We conclude that common variants at chromosome 15q14 influence susceptibility for myopia in Caucasian and Asian populations world-wide. © The Author(s) 2012

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Impact of primary kidney disease on the effects of empagliflozin in patients with chronic kidney disease: secondary analyses of the EMPA-KIDNEY trial

Author: Abat S.
Abd Rahman R.
Abdul Cader R.
Abdul Hafidz M. I.
Abdul Wahab M. Z.
Abdul-Samad T.
Abdullah N. K.
Abe M.
Abraham N.
Acheampong S.
Achiri P.
Acosta J. A.
Adeleke A.
Adell V.
Adewuyi-Dalton R.
Adnan N.
Africano A.
Agharazii M.
Aguilar F.
Aguilera A.
Ahmad M.
Ahmad M. K.
Ahmad Miswan N.
Ahmad N. A.
Ahmad N. H.
Ahmad N. I.
Ahmad Rosdi H.
Ahmed I.
Ahmed S.
Aiello J.
Aitken A.
AitSadi R.
Aker S.
Akimoto S.
Akinfolarin A.
Akram S.
Al-Rabadi L.
Al-Zeer B.
Alberici F.
Albert C.
Aldrich L.
Alegata M.
Alexander L.
Alfaress S.
Alhadj Ali M.
Ali A.
Alicic R.
Aliu A.
Almaraz R.
Almasarwah R.
Almeida J.
Aloisi A.
Alscher D.
Alvarez P.
Amat M.
Ambrose C.
Ammar H.
An Y.
Andriaccio L.
Ansu K.
Apostolidi A.
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Araki H.
Araki S.
Arbi A.
Arechiga O.
Armstrong S.
Arnold T.
Aronoff S.
Arriaga W.
Arroyo J.
Arteaga D.
Asahara S.
Asai A.
Asai N.
Asano S.
Asawa M.
Asmee M. F.
Aucella F.
Augustin M.
Avery A.
Awad A.
Awang I. Y.
Awazawa M.
Axler A.
Ayub W.
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Baccaro R.
Badin C.
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Publication venue
Publication date: 01/01/2024
Field of study

Background: The EMPA KIDNEY trial showed that empagliflozin reduced the risk of the primary composite outcome of kidney disease progression or cardiovascular death in patients with chronic kidney disease mainly through slowing progression. We aimed to assess how effects of empagliflozin might differ by primary kidney disease across its broad population. Methods: EMPA-KIDNEY, a randomised, controlled, phase 3 trial, was conducted at 241 centres in eight countries (Canada, China, Germany, Italy, Japan, Malaysia, the UK, and the USA). Patients were eligible if their estimated glomerular filtration rate (eGFR) was 20 to less than 45 mL/min per 1·73 m2, or 45 to less than 90 mL/min per 1·73 m2 with a urinary albumin-to-creatinine ratio (uACR) of 200 mg/g or higher at screening. They were randomly assigned (1:1) to 10 mg oral empagliflozin once daily or matching placebo. Effects on kidney disease progression (defined as a sustained ≥40% eGFR decline from randomisation, end-stage kidney disease, a sustained eGFR below 10 mL/min per 1·73 m2, or death from kidney failure) were assessed using prespecified Cox models, and eGFR slope analyses used shared parameter models. Subgroup comparisons were performed by including relevant interaction terms in models. EMPA-KIDNEY is registered with ClinicalTrials.gov, NCT03594110. Findings: Between May 15, 2019, and April 16, 2021, 6609 participants were randomly assigned and followed up for a median of 2·0 years (IQR 1·5–2·4). Prespecified subgroupings by primary kidney disease included 2057 (31·1%) participants with diabetic kidney disease, 1669 (25·3%) with glomerular disease, 1445 (21·9%) with hypertensive or renovascular disease, and 1438 (21·8%) with other or unknown causes. Kidney disease progression occurred in 384 (11·6%) of 3304 patients in the empagliflozin group and 504 (15·2%) of 3305 patients in the placebo group (hazard ratio 0·71 [95% CI 0·62–0·81]), with no evidence that the relative effect size varied significantly by primary kidney disease (pheterogeneity=0·62). The between-group difference in chronic eGFR slopes (ie, from 2 months to final follow-up) was 1·37 mL/min per 1·73 m2 per year (95% CI 1·16–1·59), representing a 50% (42–58) reduction in the rate of chronic eGFR decline. This relative effect of empagliflozin on chronic eGFR slope was similar in analyses by different primary kidney diseases, including in explorations by type of glomerular disease and diabetes (p values for heterogeneity all >0·1). Interpretation: In a broad range of patients with chronic kidney disease at risk of progression, including a wide range of non-diabetic causes of chronic kidney disease, empagliflozin reduced risk of kidney disease progression. Relative effect sizes were broadly similar irrespective of the cause of primary kidney disease, suggesting that SGLT2 inhibitors should be part of a standard of care to minimise risk of kidney failure in chronic kidney disease. Funding: Boehringer Ingelheim, Eli Lilly, and UK Medical Research Council

Archivio istituzionale della ricerca - Alma Mater Studiorum Università di Bologna

Multi-messenger observations of a binary neutron star merger

Author: Aab A
Aartsen MG
Abbott BP
Abbott R
Abbott TD
Abbott TMC
Abdalla H
Abe F
Abeysekara AU
Abramo LR
Abramowski A
Abreu P
Acernese F
Acero F
Ackermann M
Ackley K
Ackley K
Adams C
Adams J
Adams SM
Adams T
Addesso P
Adhikari RX
Adya VB
Affeldt C
Afrough M
Agarwal B
Agathos M
Agatsuma K
Aggarwal N
Aglietta M
Agliozzo C
Agudo I
Aguiar OD
Aguilar JA
Aharonian F
Ahlers M
Ahrens M
Aiello L
Ain A
Ajith P
Akras S
Al Samarai I
Albert A
Albert A
Albuquerque IFM
Albury JM
Alcaniz JS
Alexander KD
Alfaro R
Alighieri S Di Serego
Allam S
Allekotte I
Allen B
Allen G
Allison J
Allison JR
Allocca A
Almela A
Altin PA
Altmann D
Alvarez C
Alvarez JD
Alvarez M Dovale
Alvarez-Muiz J
Amati L
Amato A
An T
Ananyeva A
Anastasi GA
Anchordoqui L
Andeen K
Anderson JP
Anderson SB
Anderson T
Anderson WG
Andrada B
Andre M
Andreoni I
Andreoni I
Andringa S
Angelova SV
Anghinolfi M
Angner EO
Angus CR
Annis J
Ansseau I
Antier S
Anton G
Antonelli LA
Antonelli LA
Anupama GC
Aoki K
Aoki W
Appert S
Aptekar RL
Arai K
Arakawa M
Aramo C
Araya MC
Arcavi I
Arceo R
Ardid M
Areeda JS
Aresu G
Argan A
Argelles C
Arnaud N
Array LWA Long Wavelength
Array MWA Murchison Widefield
Arrieta M
Arsene N
Arteaga-Velzquez JC
Artola R
Arun KG
Asakura Y
Asaoka Y
Ascenzi S
Ashall C
Ashley MCB
Ashton G
Asorey H
Assis P
Ast M
Aston SM
Astone P
Atallah DV
ATLAS
Atwood WB
Aubert J-J
Aubert P
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Auffenberg J
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Austin C
Avgitas T
Avila G
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Becker KH
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Belahcene I
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Bellm E
Belmont-Moreno E
Benetti S
Benkhali F Ait
Benoit-Levy A
BenZvi SY
Berat C
Berenji B
Berge D
Berger BK
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Bergmann G
Berisso M Gomez
Berley D
Bernal A
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Bernardini MG
Bernhard S
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Bero JJ
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Berry CPL
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Bertaina ME
Bertin E
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Bertolini A
Berton M
Bertou X
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Besson DZ
Beswick R
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Bhalerao V
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Biteau J
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Biwer C
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Blackburn JK
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Blackwell R
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Blair CD
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Blanchard P
Blanco A
Bland PA
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Blaufuss E
Blazek J
Bleve C
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Bohm C
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Bond IA
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CALTECH GROWTH JAGWAR
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Casentini C
Casey J
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Li ZJ
Li ZW
Liang XH
Liao JY
Lidman C
Liebling SL
Lien A
Lim G
Lim S-K
Lima M
Limatola L
Lin H
Link K
Linker SD
Linnemann JT
Lippert M
Lipunov VM
Lisi M
Littenberg TB
Liu CZ
Liu GQ
Liu HW
Liu J
Liu QR
Liu R
Liu SZ
Liu W
Liu XJ
Liu Y
Liu YN
Lnemann J
Lo Presti D
Lo RKL
Lockerbie NA
Lohse T
London LT
Longinotti AL
Longo F
Longo F
Loparco F
Lopes L
Lopes PAA
Lopez C
Lopez R
Lopez-Coto R
Lopez-Cruz O
Lord JE
Lorek R
Lorentz M
Lorenzini M
Loriette V
Lormand M
Loru S
Losurdo G
Lotze M
Loucatos S
Lough JD
Lourenco ACC
Lousto CO
Lovelace G
Lovellette MN
Lowe TB
Lu B
Lu FJ
Lu L
Lu XF
Lubrano P
Lucarelli F
Luce Q
Lucero A
Lumaca D
Luna-Garcia R
Lundgren AP
Luo T
Luszczak W
Lutovinov A
Luz RJ Barreira
Lyman JD
Lynch C
Lynch R
Lypova I
Lysenko AL
Ma B
Ma X
Ma Y
Macas R
Macfoy S
Machenschalk B
MacInnis M
Macleod DM
Macpherson D
Macri LM
Madore BF
Madsen J
Madsen K
Magaa-Sandoval F
Magee M
Magee RM
Maggi G
Magill JD
Magnier EA
Maguire K
Mahn KBM
Maia MAG
Maiorano E
Majorana E
Makhathini S
Makishima K
Maksimovic I
Malacari M
Maldera S
Malesani D
Mallamaci CC
Mallamaci M
Malone K
Malyshev D
Man N
Mancina S
Mandat D
Mandel I
Mandic V
Manfreda A
Mangano V
Mankiewicz L
Mansell GL
Manske M
Mantovani M
Mantsch P
Manulis I
Mao J
Mao J
Maoz D
Mapelli M
Marandon V
Marcelin M
March M
Marchesoni F
Marcote B
Marcowith A
Margiotta A
Margutti R
Mariaud C
Mariazzi AG
Marinelli A
Marinelli SS
Marion F
Maris IC
Marisaldi M
Markakis C
Markosyan AS
Markowitz A
Marongiu L
Maros E
Marquina A
Marriner J
Marrocchesi PS
Marsella G
Marsh P
Marshall FE
Marshall JL
Martelli F
Martellini L
Martello D
Martin IW
Martin RM
Martin S
Martin-Carrillo A
Martinez H
Martinez O
Martinez-Castellanos I
Martinez-Castro J
Martinez-Huerta H
Martinez-Mora JA
Martini P
Martynov DV
Maruyama R
Marx R
Mase K
Masetti N
Mason K
Massera E
Masserot A
Massinger TJ
Masso-Reid M
Mastrogiovanni S
Matas A
Mate S
Mathes HJ
Matheson T
Mathys S
Matichard F
Matone L
Matsubayashi K
Matsuoka M
Matthews J
Matthews JA
Matthiae G
Mattila S
Maunu R
Maurin G
Mavalvala N
Maxted N
Mayer M
Mayotte E
Mazaeva ED
Mazumder N
Mazur PO
Mazzali PA
Mazzali PA
Mazziotta MN
McBreen S
McBrien O
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McClelland DE
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McCuller L
McCully C
McEnery JE
McGuire SC
McIntyre G
McIver J
McMahon RG
McManus DJ
McNally F
McNeill L
Mcrae T
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Meacher D
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Meagher K
Medici M
Medina C
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Mehmet M
Mehner A
Meidam J
Meier M
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Melandri A
Melatos A
Mele R
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Melis A
Melis G
Melis K
Melo D
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Mendell G
Meng B
Menne T
Menshikov A
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Mereghetti S
Merenda K-D
Merilh EL
Merino G
Merzougui M
Meshkov S
Messenger C
Messick C
Metzdorff R
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Meures T
Meyer M
Meyer M
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Mezek G Kukec
Miao H
Miarecki S
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Mller A
Mockler D
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Mor K
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Mostaf M
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Mours B
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Mrka S
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Mukherjee D
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Nagai H
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Okita H
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Poe M
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Poh J
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Post A
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Poznanski D
Pradier T
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Pretz J
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Price PB
Prijatelj M
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Principe M
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Prokoph H
Prouza M
Prrer M
Przybylski GT
Pulone L
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Punch M
Puncken O
Punturo M
Puppo P
Qi H
Qi H
Qu JL
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Quel EJ
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Querel R
Quetschke V
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Quinn L
Quinn S
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Raab FJ
Raab S
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Reimer O
Reimer O
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Ren Z
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Reposeur T
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Resmi L
Rest A
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Rizzo M
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Roulet E
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Rowell G
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Rowlinson A
Roy R
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Rulten CB
Rumyantsev VV
Rusu F
Rutins G
Ryan K
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Saba A
Sachdev S
Sadecki T
Sadeghian L
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Sadler EM
Saffe C
Saffi SJ
Saftoiu A
Sahakian V
Sai N
Saito S
Saito T
Saito Y
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Sako M
Sako S
Salafia OS
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Sand DJ
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Schmidt T
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Schneider M
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Publication venue: 'American Astronomical Society'
Publication date: 01/01/2017
Field of study

On 2017 August 17 a binary neutron star coalescence candidate (later designated GW170817) with merger time 12:41:04 UTC was observed through gravitational waves by the Advanced LIGO and Advanced Virgo detectors. The Fermi Gamma-ray Burst Monitor independently detected a gamma-ray burst (GRB 170817A) with a time delay of ~1.7 s with respect to the merger time. From the gravitational-wave signal, the source was initially localized to a sky region of 31 deg2 at a luminosity distance of 40+8-8 Mpc and with component masses consistent with neutron stars. The component masses were later measured to be in the range 0.86 to 2.26 Mo. An extensive observing campaign was launched across the electromagnetic spectrum leading to the discovery of a bright optical transient (SSS17a, now with the IAU identification of AT 2017gfo) in NGC 4993 (at ~40 Mpc) less than 11 hours after the merger by the One- Meter, Two Hemisphere (1M2H) team using the 1 m Swope Telescope. The optical transient was independently detected by multiple teams within an hour. Subsequent observations targeted the object and its environment. Early ultraviolet observations revealed a blue transient that faded within 48 hours. Optical and infrared observations showed a redward evolution over ~10 days. Following early non-detections, X-ray and radio emission were discovered at the transient’s position ~9 and ~16 days, respectively, after the merger. Both the X-ray and radio emission likely arise from a physical process that is distinct from the one that generates the UV/optical/near-infrared emission. No ultra-high-energy gamma-rays and no neutrino candidates consistent with the source were found in follow-up searches. These observations support the hypothesis that GW170817 was produced by the merger of two neutron stars in NGC4993 followed by a short gamma-ray burst (GRB 170817A) and a kilonova/macronova powered by the radioactive decay of r-process nuclei synthesized in the ejecta

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Multi-messenger Observations of a Binary Neutron Star Merger

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Publication venue: 'American Astronomical Society'
Publication date: 28/10/2022
Field of study

On 2017 August 17 a binary neutron star coalescence candidate (later designated GW170817) with merger time 12:41:04 UTC was observed through gravitational waves by the Advanced LIGO and Advanced Virgo detectors. The Fermi Gamma-ray Burst Monitor independently detected a gamma-ray burst (GRB 170817A) with a time delay of ∼ 1.7 {{s}} with respect to the merger time. From the gravitational-wave signal, the source was initially localized to a sky region of 31 deg2 at a luminosity distance of {40}-8+8 Mpc and with component masses consistent with neutron stars. The component masses were later measured to be in the range 0.86 to 2.26 {M}ȯ . An extensive observing campaign was launched across the electromagnetic spectrum leading to the discovery of a bright optical transient (SSS17a, now with the IAU identification of AT 2017gfo) in NGC 4993 (at ∼ 40 {{Mpc}}) less than 11 hours after the merger by the One-Meter, Two Hemisphere (1M2H) team using the 1 m Swope Telescope. The optical transient was independently detected by multiple teams within an hour. Subsequent observations targeted the object and its environment. Early ultraviolet observations revealed a blue transient that faded within 48 hours. Optical and infrared observations showed a redward evolution over ∼10 days. Following early non-detections, X-ray and radio emission were discovered at the transient’s position ∼ 9 and ∼ 16 days, respectively, after the merger. Both the X-ray and radio emission likely arise from a physical process that is distinct from the one that generates the UV/optical/near-infrared emission. No ultra-high-energy gamma-rays and no neutrino candidates consistent with the source were found in follow-up searches. These observations support the hypothesis that GW170817 was produced by the merger of two neutron stars in NGC 4993 followed by a short gamma-ray burst (GRB 170817A) and a kilonova/macronova powered by the radioactive decay of r-process nuclei synthesized in the ejecta.</p

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