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571 research outputs found

Expression of myogenic regulatory factors in chicken embryos during somite and limb development

Author: Mohammed Rabeea Hazim
Mok Gi Fay
Sweetman Dylan
Publication venue: Wiley
Publication date: 16/07/2015
Field of study

The expression of the myogenic regulatory factors (MRFs), Myf5, MyoD, myogenin (Mgn) and MRF4 have been analysed during the development of chicken embryo somites and limbs. In somites, Myf5 is expressed first in somites and paraxial mesoderm at HH stage 9 followed by MyoD at HH stage 12, and Mgn and MRF4 at HH stage 14. In older somites, Myf5 and MyoD are also expressed in the ventrally extending myotome prior to Mgn and MRF4 expression. In limb muscles a similar temporal sequence is observed with Myf5 expression detected first in forelimbs at HH stage 22, MyoD at HH stage 23, Mgn at HH stage 24 and MRF4 at HH stage 30. This report describes the precise time of onset of expression of each MRF in somites and limbs during chicken embryo development, and provides a detailed comparative timeline of MRF expression in different embryonic muscle groups

Nottingham ePrints

Nottingham eTheses

Crossref

Repository@Nottingham

PubMed Central

University of East Anglia digital repository

P-selectin mobility undergoes a sol-gel transition as it diffuses from exocytosis sites into the cell membrane

Author: Babich V
Carter TD
Conte I
Hannah MJ
Hellen N
Knipe L
Le Trionnaire S
Martin-Almedina S
Mashanov GI
Mohammed A
Molloy J
Ogmen K
Torok K
Publication venue: Springer Nature
Publication date: 31/05/2022
Field of study

In response to vascular damage, P-selectin molecules are secreted onto the surface of cells that line our blood vessels. They then serve as mechanical anchors to capture leucocytes from the blood stream. Here, we track individual P-selectin molecules released at the surface of live endothelial cells following stimulated secretion. We find P-selectin initially shows fast, unrestricted diffusion but within a few minutes, movement becomes increasingly restricted and ~50% of the molecules become completely immobile; a process similar to a sol-gel transition. We find removal of the extracellular C-type lectin domain (ΔCTLD) and/or intracellular cytoplasmic tail domain (ΔCT) has additive effects on diffusive motion while disruption of the adapter complex, AP2, or removal of cell-surface heparan sulphate restores mobility of full-length P-selectin close to that of ΔCT and ΔCTLD respectively. We have found P-selectin spreads rapidly from sites of exocytosis and evenly decorates the cell surface, but then becomes less mobile and better-suited to its mechanical anchoring function

PubMed Central

St George's Online Research Archive

Lipophilic activated ester prodrug approach for drug delivery to the intestinal lymphatic system

Author: Al-Hayali Mohammed
Ali Joseph
Bradshaw Tracey D.
Chan Ting-Hoi
Chiang Manting
Cipolla Elena
Collins Hilary M.
Feng Wanshan
Fischer Peter M.
Gao Xizhe
Garces Aimie
Gershkovich Pavel
Heery David M.
Hume Amy
Kagan Leonid
Kim Min Gi
Kim Tae Hwan
Lau Chun Long
Lee Jong Bong
Malec Jed
McIntosh Tecashanell M.
Qin Chaolong
Shin Beom Soo
Soukarieh Fadi
Stocks Michael J.
Voronin Gregory
Yoo Sun Dong
Zgair Atheer
Publication venue: 'Elsevier BV'
Publication date: 28/09/2018
Field of study

The intestinal lymphatic system plays an important role in the pathophysiology of multiple diseases including lymphomas, cancer metastasis, autoimmune diseases, and human immunodeficiency virus (HIV) infection. It is thus an important compartment for delivery of drugs in order to treat diseases associated with the lymphatic system. Lipophilic prodrug approaches have been used in the past to take advantage of the intestinal lymphatic transport processes to deliver drugs to the intestinal lymphatics. Most of the approaches previously adopted were based on very bulky prodrug moieties such as those mimicking triglycerides (TG). We now report a study in which a lipophilic prodrug approach was used to efficiently deliver bexarotene (BEX) and retinoic acid (RA) to the intestinal lymphatic system using activated ester prodrugs. A range of carboxylic ester prodrugs of BEX were designed and synthesised and all of the esters showed improved association with chylomicrons, which indicated an improved potential for delivery to the intestinal lymphatic system. The conversion rate of the prodrugs to BEX was the main determinant in delivery of BEX to the intestinal lymphatics, and activated ester prodrugs were prepared to enhance the conversion rate. As a result, an 4-(hydroxymethyl)-1,3-dioxol-2-one ester prodrug of BEX was able to increase the exposure of the mesenteric lymph nodes (MLNs) to BEX 17-fold compared to when BEX itself was administered. The activated ester prodrug approach was also applied to another drug, RA, where the exposure of the MLNs was increased 2.4-fold through the application of a similar cyclic activated prodrug. Synergism between BEX and RA was also demonstrated in vitro by cell growth inhibition assays using lymphoma cell lines. In conclusion, the activated ester prodrug approach results in efficient delivery of drugs to the intestinal lymphatic system, which could benefit patients affected by a large number of pathological conditions

Nottingham ePrints

Nottingham eTheses

Repository@Nottingham

University of Melbourne Institutional Repository

Mapping geographical inequalities in access to drinking water and sanitation facilities in low-income and middle-income countries, 2000-17

Author: Abbastabar H
Abd-Allah F
Abdelalim A
Abdollahpour I
Abegaz KH
Abejie AN
Abreu LG
Abrigo MRM
Abualhasan A
Accrombessi MMK
Adamu AA
Adebayo OM
Adedeji IA
Adedoyin RA
Adekanmbi V
Adetokunboh OO
Adhikari TB
Afarideh M
Agudelo-Botero M
Ahmadi K
Ahmadi M
Ahmed AE
Ahmed MB
Akalu TY
Akanda AS
Al-Aly Z
Al-Mekhlafi HM
Alahdab F
Alam N
Alam S
Alamene GM
Alanzi TM
Albright J
Albujeer A
Alcalde-Rabanal JE
Alebel A
Alemu ZA
Ali M
Alijanzadeh M
Alipour V
Aljunid SM
Almasi A
Almasi-Hashiani A
Altirkawi KA
Alvis-Guzman N
Alvis-Zakzuk NJ
Amini S
Amit AML
Amul GGH
Andrei CL
Anjomshoa M
Ansariadi A
Antonio CAT
Antony B
Antriyandarti E
Arabloo J
Aref HMA
Aremu O
Armoon B
Arora A
Aryal KK
Arzani A
Asadi-Aliabadi M
Asmelash D
Atalay HT
Athari SM
Athari SS
Atre SR
Ausloos M
Awasthi S
Awoke N
Ayala Quintanilla BP
Ayano G
Ayanore MA
Aynalem YA
Azari S
Azman AS
Babaee E
Badawi A
Bagherzadeh M
Bakkannavar SM
Balakrishnan S
Banach M
Banoub JAM
Barac A
Barboza MA
Basu S
Baumann MM
Bay VD
Bayati M
Bedi N
Beheshti M
Behzadifar M
Behzadifar M
Bejarano Ramirez DF
Bell ML
Bennett DA
Benzian H
Berbada DA
Bernstein RS
Bhat AG
Bhattacharyya K
Bhaumik S
Bhutta ZA
Bijani A
Bikbov B
Bin Sayeed MS
Biswas RK
Blacker BF
Bohlouli S
Boufous S
Brady OJ
Briko AN
Briko NI
Britton GB
Brown A
Burugina Nagaraja S
Butt ZA
Bärnighausen TW
Campos-Nonato IR
Campuzano Rincon JC
Cano J
Car J
Carvalho F
Castañeda-Orjuela CA
Castro F
Cerin E
Chalise B
Chattu VK
Chin KL
Christopher DJ
Chu D-T
Cormier NM
Costa VM
Cromwell EA
Cámera LA
Cárdenas R
Dadi AFF
Dahiru T
Dahlawi SMA
Dandona L
Dandona R
Dang AK
Daoud F
Darwesh AM
Darwish AH
Daryani A
Das Gupta R
Das JK
Dash AP
Davis Weaver N
De la Hoz FP
De Neve J-W
Demissie DB
Demoz GT
Denova-Gutiérrez E
Deribe K
Desalew A
Deshpande A
Dharmaratne SD
Dhillon P
Dhimal M
Dhungana GP
Diaz D
Dipeolu IO
Do HT
Dolecek C
Doyle KE
Dubljanin E
Duraes AR
Dávila-Cervantes CA
Edinur HA
Effiong A
Eftekhari A
El Nahas N
El Sayed Zaki M
El Tantawi M
El-Jaafary SI
El-Khatib Z
Elhabashy HR
Elkout H
Elsharkawy A
Enany S
Endalew DA
Eshrati B
Eskandarieh S
Etemadi A
Ezekannagha O
Faraon EJA
Fareed M
Faro A
Farzadfar F
Fasil AF
Fazlzadeh M
Feigin VL
Fekadu W
Fentahun N
Fereshtehnejad S-M
Fernandes E
Filip I
Fischer F
Flohr C
Foigt NA
Folayan MO
Foroutan M
Franklin RC
Frostad JJ
Fukumoto T
Gad MM
Garcia GM
Gatotoh AM
Gayesa RT
Gebremedhin KB
Geramo YCD
Gesesew HA
Gezae KE
Ghashghaee A
Ghazi Sherbaf F
Gill PS
Gill TK
Ginindza TG
Girmay A
Gizaw Z
Goodridge A
Gopalani SV
Goulart AC
Goulart BNG
Grada A
Green MS
Gubari MIM
Gugnani HC
Guido D
Guimarães RA
Guo Y
Gupta R
Gupta R
Ha GH
Haagsma JA
Hafezi-Nejad N
Haile DH
Haile MT
Hall BJ
Hamidi S
Handiso DW
Haririan H
Hariyani N
Hasaballah AI
Hasan MM
Hasanzadeh A
Hassen HY
Hay SI
Hayelom DH
Hegazy MI
Heibati B
Heidari B
Hendrie D
Henok A
Herteliu C
Heydarpour F
Hidru HDD
Hird TR
Hoang CL
Hollerich GI
Hoogar P
Hossain N
Hosseinzadeh M
Househ M
Hu G
Humayun A
Hussain SA
Hussen MAA
Ibitoye SE
Ilesanmi OS
Ilic MD
Imani-Nasab MH
Iqbal U
Irvani SSN
Islam SMS
Ivers RQ
Iwu CJ
Jahanmehr N
Jakovljevic M
Jalali A
Jayatilleke AU
Jenabi E
Jha RP
Jha V
Ji JS
Johnson KB
Jonas JB
Jozwiak JJ
Kabir A
Kabir Z
Kanchan T
Karch A
Karki S
Kasaeian A
Kasahun GG
Kasaye HK
Kassa GG
Kassa GM
Kayode GA
Kebede MM
Keiyoro PN
Ketema DB
Khader YS
Khafaie MA
Khalid N
Khalilov R
Khan EA
Khan J
Khan MN
Khatab K
Khater AM
Khater MM
Khayamzadeh M
Khazaei M
Khosravi MH
Khubchandani J
Kiadaliri A
Kim YJ
Kimokoti RW
Kisa A
Kisa S
Kochhar S
Kolola T
Komaki H
Kosen S
Koul PA
Koyanagi A
Krishan K
Kuate Defo B
Kugbey N
Kumar GA
Kumar M
Kumar P
Kusuma D
La Vecchia C
Lacey B
Lal A
Lal DK
Lam H
Lami FH
Lansingh VC
Lasrado S
Lebedev G
Lee PH
LeGrand KE
Leili M
Lenjebo TL
Leshargie CT
Levine AJ
Lewycka S
Li S
Lindstedt PA
Linn S
Liu S
Lopez JCF
Lopukhov PD
Magdy Abd El Razek M
Mahadeshwara Prasad DR
Mahasha PW
Mahotra NB
Majeed A
Malekzadeh R
Malta DC
Mamun AA
Manafi N
Mansournia MA
Mapoma CC
Martinez G
Martini S
Martins-Melo FR
Mathur MR
Mayala BK
Mazidi M
McAlinden C
Meharie BG
Mehndiratta MM
Mehrabi Nasab E
Mehta KM
Mekonnen T
Mekonnen TC
Meles GG
Meles HG
Memiah PTN
Memish ZA
Mendoza W
Menezes RG
Mereta ST
Meretoja TJ
Mestrovic T
Metekiya WM
Metekiya WM
Miazgowski B
Miller TR
Miller-Petrie MK
Mini GK
Mirrakhimov EM
Moazen B
Mohajer B
Mohammad Gholi Mezerji N
Mohammad DK
Mohammad Y
Mohammadibakhsh R
Mohammed H
Mohammed JA
Mohammed S
Mohebi F
Mokdad AH
Moodley Y
Moradi G
Moradi M
Moradi-Joo M
Moraga P
Morales L
Mosapour A
Mosser JF
Mouodi S
Mousavi SM
Mozaffor M
Munro SB
Muriithi MK
Murray CJL
Musa KI
Mustafa G
Muthupandian S
Naderi M
Nagarajan AJ
Naghavi M
Naik G
Nangia V
Nascimento BR
Nazari J
Ndwandwe DE
Negoi I
Netsere HB
Ngunjiri JW
Nguyen CT
Nguyen HLT
Nguyen QP
Nigatu SG
Ningrum DNA
Nnaji CA
Nojomi M
Norheim OF
Noubiap JJ
Oancea B
Ogbo FA
Oh I-H
Olagunju AT
Olusanya BO
Olusanya JO
Onwujekwe OE
Ortega-Altamirano DV
Osarenotor O
Osei FB
Owolabi MO
P A M
Padubidri JR
Pakhale S
Pana A
Park E-K
Patel SK
Pathak A
Patle A
Paulos K
Pepito VCF
Perico N
Pervaiz A
Pescarini JM
Pesudovs K
Pham HQ
Pigott DM
Pilgrim T
Pirsaheb M
Poljak M
Pollock I
Postma MJ
Pourmalek F
Pourshams A
Prada SI
Preotescu L
Quintana H
Rabiee M
Rabiee N
Radfar A
Rafiei A
Rahim F
Rahimi S
Rahimi-Movaghar V
Rahman MA
Rahman MHU
Rajati F
Ranabhat CL
Rao PC
Rasella D
Rath GK
Rawaf S
Rawal L
Rawasia WF
Reiner RC
Remuzzi G
Renjith V
Renzaho AMN
Resnikoff S
Riahi SM
Ribeiro AI
Rickard J
Roever L
Ronfani L
Rubagotti E
Rubino S
Saad AM
Sabour S
Sadeghi E
Saeedi Moghaddam S
Safari Y
Sagar R
Sahraian MA
Sajadi SM
Salahshoor MR
Salam N
Saleem A
Salem H
Salem MR
Salimi Y
Salimzadeh H
Samy AM
Sanabria J
Santos IS
Santric-Milicevic MM
Sao Jose BP
Saraswathy SYI
Sarrafzadegan N
Sartorius B
Sathian B
Sathish T
Satpathy M
Sawhney M
Sayyah M
Sbarra AN
Schaeffer LE
Schwebel DC
Senbeta AM
Senthilkumaran S
Sepanlou SG
Serván-Mori E
Shafieesabet A
Shaheen AA
Shahid I
Shaikh MA
Shalash AS
Shams-Beyranvand M
Shamsi M
Shamsizadeh M
Shannawaz M
Sharafi K
Sharma R
Sheikh A
Shetty BSK
Shiferaw WS
Shigematsu M
Shin JI
Shiri R
Shirkoohi R
Shivakumar KM
Si S
Siabani S
Siddiqi TJ
Silva DAS
Singh A
Singh BBS
Singh JA
Singh NP
Singh V
Sinha DN
Sisay MM
Skiadaresi E
Smith DL
Soares Filho AM
Sobhiyeh MR
Sokhan A
Soriano JB
Sorrie MB
Soyiri IN
Spurlock EE
Sreeramareddy CT
Sudaryanto A
Sufiyan MB
Suleria HAR
Sykes BL
Tabarés-Seisdedos R
Tabuchi T
Tadesse DB
Tarigan IU
Taye B
Tefera YM
Tehrani-Banihashemi A
Tekelemedhin SW
Tekle MG
Temsah M-H
Tesfay BE
Tesfay FH
Tessema ZT
Thankappan KR
ThekkePurakkal AS
Thomas N
Thompson RL
Thomson AJ
Topor-Madry R
Tovani-Palone MR
Traini E
Tran BX
Tran KB
Ullah I
Unnikrishnan B
Usman MS
Uthman OA
Uzochukwu BSC
Valdez PR
Varughese S
Veisani Y
Violante FS
Vollmer S
W/hawariat FG
Waheed Y
Wallin MT
Wang Y
Wang Y-P
Wangdi K
Weiss DJ
Weldesamuel GT
Werkneh AA
Westerman R
Wiangkham T
Wiens KE
Wijeratne T
Wiysonge CS
Wolde HF
Wondafrash DZ
Wonde TE
Worku GT
Yadollahpour A
Yahyazadeh Jabbari SH
Yamada T
Yaseri M
Yatsuya H
Yeshaneh A
Yilma MT
Yip P
Yisma E
Yonemoto N
Younis MZ
Yousof H-ASA
Yu C
Yusefzadeh H
Zadey S
Zahirian Moghadam T
Zaidi Z
Zaman SB
Zamani M
Zandian H
Zar HJ
Zerfu TA
Zhang Y
Ziapour A
Zodpey S
Zuniga YMH
Publication venue
Publication date: 01/01/2020
Field of study

Background Universal access to safe drinking water and sanitation facilities is an essential human right, recognised in the Sustainable Development Goals as crucial for preventing disease and improving human wellbeing. Comprehensive, high-resolution estimates are important to inform progress towards achieving this goal. We aimed to produce high-resolution geospatial estimates of access to drinking water and sanitation facilities. Methods We used a Bayesian geostatistical model and data from 600 sources across more than 88 low-income and middle-income countries (LMICs) to estimate access to drinking water and sanitation facilities on continuous continent-wide surfaces from 2000 to 2017, and aggregated results to policy-relevant administrative units. We estimated mutually exclusive and collectively exhaustive subcategories of facilities for drinking water (piped water on or off premises, other improved facilities, unimproved, and surface water) and sanitation facilities (septic or sewer sanitation, other improved, unimproved, and open defecation) with use of ordinal regression. We also estimated the number of diarrhoeal deaths in children younger than 5 years attributed to unsafe facilities and estimated deaths that were averted by increased access to safe facilities in 2017, and analysed geographical inequality in access within LMICs. Findings Across LMICs, access to both piped water and improved water overall increased between 2000 and 2017, with progress varying spatially. For piped water, the safest water facility type, access increased from 40.0% (95% uncertainty interval [UI] 39.4-40.7) to 50.3% (50.0-50.5), but was lowest in sub-Saharan Africa, where access to piped water was mostly concentrated in urban centres. Access to both sewer or septic sanitation and improved sanitation overall also increased across all LMICs during the study period. For sewer or septic sanitation, access was 46.3% (95% UI 46.1-46.5) in 2017, compared with 28.7% (28.5-29.0) in 2000. Although some units improved access to the safest drinking water or sanitation facilities since 2000, a large absolute number of people continued to not have access in several units with high access to such facilities (>80%) in 2017. More than 253 000 people did not have access to sewer or septic sanitation facilities in the city of Harare, Zimbabwe, despite 88.6% (95% UI 87.2-89.7) access overall. Many units were able to transition from the least safe facilities in 2000 to safe facilities by 2017; for units in which populations primarily practised open defecation in 2000, 686 (95% UI 664-711) of the 1830 (1797-1863) units transitioned to the use of improved sanitation. Geographical disparities in access to improved water across units decreased in 76.1% (95% UI 71.6-80.7) of countries from 2000 to 2017, and in 53.9% (50.6-59.6) of countries for access to improved sanitation, but remained evident subnationally in most countries in 2017. Interpretation Our estimates, combined with geospatial trends in diarrhoeal burden, identify where efforts to increase access to safe drinking water and sanitation facilities are most needed. By highlighting areas with successful approaches or in need of targeted interventions, our estimates can enable precision public health to effectively progress towards universal access to safe water and sanitation. Copyright (C) 2020 The Author(s). Published by Elsevier Ltd.Peer reviewe

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Global mortality associated with 33 bacterial pathogens in 2019: a systematic analysis for the Global Burden of Disease Study 2019

Author: Aali A
Abate SM
Abbasi-Kangevari M
Abbasi-Kangevari Z
Abd-Elsalam S
Abdulkader RS
Abebe G
Abedi A
Abhari AP
Abidi H
Aboagye RG
Absalan A
Acuna JM
Adane TD
Addo IY
Adegboye OA
Adnan M
Adnani QES
Afzal MS
Afzal S
Aghdam ZB
Aguilar GR
Ahinkorah BO
Ahmad A
Ahmad AR
Ahmad R
Ahmad S
Ahmad S
Ahmadi S
Ahmed A
Ahmed H
Ahmed JQ
Ajami M
Aji B
Akbarzadeh-Khiavi M
Akunna CJ
Al Hamad H
Al-Aly Z
Alahdab F
Aldeyab MA
Aleman AV
Alhalaiqa FAN
Alhassan RK
Ali BA
Ali HA
Ali L
Ali SS
Alimohamadi Y
Alipour V
Alizadeh A
Aljunid SM
Allel K
Almustanyir S
Ameyaw EK
Amit AML
Anandavelane N
Ancuceanu R
Andrei CL
Andrei T
Anggraini D
Ansar A
Anyasodor AE
Arabloo J
Aravkin AY
Areda D
Aripov T
Artamonov AA
Arulappan J
Aruleba RT
Asaduzzaman M
Ashraf T
Athari SS
Atlaw D
Attia S
Ausloos M
Avval AH
Awoke T
Ayana TM
Azadnajafabad S
Badar M
Badiye AD
Baghcheghi N
Bagherieh S
Baig AA
Bain LE
Bali AO
Banerjee I
Barac A
Bardhan M
Barone-Adesi F
Barqawi HJ
Barrow A
Baskaran P
Basu S
Batiha AMM
Bedi N
Belete MA
Belgaumi UI
Bender RG
Bhandari B
Bhandari D
Bhardwaj P
Bhaskar S
Bhattacharyya K
Bhattarai S
Bin Zaman S
Bitaraf S
Buonsenso D
Butt ZA
Cai J
Calina D
Camargos P
Camera LA
Cardenas R
Cevik M
Chadwick J
Charan J
Chaurasia A
Ching PR
Choudhari SG
Chowdhury EK
Chowdhury FR
Chu DT
Chukwu IS
Dadras O
Dagnaw FT
Dai XC
Darshan BB
Das Gupta R
Das S
Dastiridou A
de Sa ACMGN
de Sa ATN
Debela SA
Demisse FW
Demissie S
Dereje D
Derese M
Desai HD
Dessalegn FN
Dessalegni SAA
Desye B
Dhaduk K
Dhimal M
Dhingra S
Diao N
Diaz D
Djalalinia S
Dodangeh M
Dolecek C
Dongarwar D
Dora BT
Dorostkar F
dos Santos FLC
Dsouza HL
Dubljanin E
Dunachie SJ
Durojaiye OC
Edinur HA
Ejigu HB
Ekholuenetale M
Ekundayo TC
El-Abid H
Elhadi M
Elmonem MA
Emami A
Enyew DB
Erkhembayar R
Eshrati B
Etaee F
Fagbamigbe AF
Falahi S
Fallahzadeh A
Faraon EJA
Fatehizadeh A
Fekadu G
Fernandes JC
Ferrari A
Fetensa G
Filip I
Fischer F
Foroutan M
Gaal PA
Gadanya MA
Gaidhane AM
Ganesan B
Gebrehiwot M
Ghanbari R
Ghashghaee A
Gholamrezanezhad A
Gholizadeh A
Golechha M
Goleij P
Golinelli D
Goodridge A
Gray AP
Gunawardane DA
Guo Y
Gupta S
Gupta VB
Gupta VK
Guta A
Habibzadeh P
Halwani R
Han C
Hanif A
Hannan MA
Harapan H
Hassan S
Hassankhani H
Hay SI
Hayat K
Hayoon AG
Heibati B
Heidari G
Heidari M
Heidari-Soureshjani R
Herteliu C
Heyi DZ
Hezam K
Hoogar P
Horita N
Hossain MM
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Wool EE
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Yahya GATY
Yigit A
Yigit V
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Yonemoto N
Zahir M
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Zangiabadian M
Zare I
Zastrozhin MS
Zhang ZJ
Zheng P
Zhong CW
Zoladl M
Zumla A
Publication venue
Publication date: 01/01/2022
Field of study

Background Reducing the burden of death due to infection is an urgent global public health priority. Previous studies have estimated the number of deaths associated with drug-resistant infections and sepsis and found that infections remain a leading cause of death globally. Understanding the global burden of common bacterial pathogens (both susceptible and resistant to antimicrobials) is essential to identify the greatest threats to public health. To our knowledge, this is the first study to present global comprehensive estimates of deaths associated with 33 bacterial pathogens across 11 major infectious syndromes.Methods We estimated deaths associated with 33 bacterial genera or species across 11 infectious syndromes in 2019 using methods from the Global Burden of Diseases, Injuries, and Risk Factors Study (GBD) 2019, in addition to a subset of the input data described in the Global Burden of Antimicrobial Resistance 2019 study. This study included 343 million individual records or isolates covering 11 361 study-location-years. We used three modelling steps to estimate the number of deaths associated with each pathogen: deaths in which infection had a role, the fraction of deaths due to infection that are attributable to a given infectious syndrome, and the fraction of deaths due to an infectious syndrome that are attributable to a given pathogen. Estimates were produced for all ages and for males and females across 204 countries and territories in 2019. 95% uncertainty intervals (UIs) were calculated for final estimates of deaths and infections associated with the 33 bacterial pathogens following standard GBD methods by taking the 2.5th and 97.5th percentiles across 1000 posterior draws for each quantity of interest.Findings From an estimated 13.7 million (95% UI 10.9-17.1) infection-related deaths in 2019, there were 7.7 million deaths (5.7-10.2) associated with the 33 bacterial pathogens (both resistant and susceptible to antimicrobials) across the 11 infectious syndromes estimated in this study. We estimated deaths associated with the 33 bacterial pathogens to comprise 13.6% (10.2-18.1) of all global deaths and 56.2% (52.1-60.1) of all sepsis-related deaths in 2019. Five leading pathogens-Staphylococcus aureus, Escherichia coli, Streptococcus pneumoniae, Klebsiella pneumoniae, and Pseudomonas aeruginosa-were responsible for 54.9% (52.9-56.9) of deaths among the investigated bacteria. The deadliest infectious syndromes and pathogens varied by location and age. The age-standardised mortality rate associated with these bacterial pathogens was highest in the sub-Saharan Africa super-region, with 230 deaths (185-285) per 100 000 population, and lowest in the high-income super-region, with 52.2 deaths (37.4-71.5) per 100 000 population. S aureus was the leading bacterial cause of death in 135 countries and was also associated with the most deaths in individuals older than 15 years, globally. Among children younger than 5 years, S pneumoniae was the pathogen associated with the most deaths. In 2019, more than 6 million deaths occurred as a result of three bacterial infectious syndromes, with lower respiratory infections and bloodstream infections each causing more than 2 million deaths and peritoneal and intra-abdominal infections causing more than 1 million deaths.Interpretation The 33 bacterial pathogens that we investigated in this study are a substantial source of health loss globally, with considerable variation in their distribution across infectious syndromes and locations. Compared with GBD Level 3 underlying causes of death, deaths associated with these bacteria would rank as the second leading cause of death globally in 2019; hence, they should be considered an urgent priority for intervention within the global health community. Strategies to address the burden of bacterial infections include infection prevention, optimised use of antibiotics, improved capacity for microbiological analysis, vaccine development, and improved and more pervasive use of available vaccines. These estimates can be used to help set priorities for vaccine need, demand, and development. Copyright (c) 2022 The Author(s). Published by Elsevier Ltd. This is an Open Access article under the CC BY 4.0 license

Archivio della Ricerca - Università degli Studi di Siena

Measurement of inclusive very forward jet cross sections in proton-lead collisions at \sqrt{sNN} = 5:02 TeV

Author: Aarrestad TK
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Zanetti A
Zanetti M
Zarubin A
Zarucki M
Zeinali M
Zenaiev O
Zenz SC
Zeuner WD
Zevi Della Porta G
Zeyrek M
Zghiche A
Zhang A
Zhang F
Zhang H
Zhang J
Zhang S
Zhang Z
Zhao J
Zhaozhong S
Zhiltsov V
Zhokin A
Zhu DH
Zhu RY
Zhukov V
Zientek M
Zito G
Zobec J
Zolkapli Z
Zorbakir IS
Zorbilmez C
Zotto P
Zou D
Zucchetta A
Zumerle G
Publication venue: 'Springer Fachmedien Wiesbaden GmbH'
Publication date: 01/01/2019
Field of study

Measurements of differential cross sections for inclusive very forward jet production in proton-lead collisions as a function of jet energy are presented. The data were collected with the CMS experiment at the LHC in the laboratory pseudorapidity range −6.6 < η < −5.2. Asymmetric beam energies of 4 TeV for protons and 1.58 TeV per nucleon for Pb nuclei were used, corresponding to a center-of-mass energy per nucleon pair of \sqrt{sNN} = 5:02 TeV. Collisions with either the proton (p+Pb) or the ion (Pb+p) traveling towards the negative η hemisphere are studied. The jet cross sections are unfolded to stable-particle level cross sections with p_{T} ≳ 3 GeV, and compared to predictions from various Monte Carlo event generators. In addition, the cross section ratio of p+Pb and Pb+p data is presented. The results are discussed in terms of the saturation of gluon densities at low fractional parton momenta. None of the models under consideration describes all the data over the full jet-energy range and for all beam configurations. Discrepancies between the differential cross sections in data and model predictions of more than two orders of magnitude are observed

UCL Discovery

Measurements of differential cross-sections in top-quark pair events with a high transverse momentum top quark and limits on beyond the Standard Model contributions to top-quark pair production with the ATLAS detector at √s = 13 TeV

Author: Aad G
Abbott B
Abbott DC
Abeling K
Abhayasinghe DK
Abidi SH
Aboulhorma A
Abramowicz H
Abreu H
Abud AA
Abulaiti Y
Acharya BS
Achkar B
Adam L
Adamczyk L
Adamek L
Addepalli SV
Adelman J
Adiguzel A
Adorni S
Adye T
Affolder AA
Afik Y
Agaras MN
Agarwala J
Aggarwal A
Agheorghiesei C
Aguilar-Saavedra JA
Agullo PM
Ahmad A
Ahmadov F
Ahmed WS
Ai X
Aielli G
Aizenberg I
Akbiyik M
Akesson TPA
Akimov AV
Al Khoury K
Alberghi GL
Albert J
Albicocco P
Alderweireldt S
Aleksa M
Aleksandrov IN
Alexa C
Alexopoulos T
Alfonsi A
Alfonsi F
Alhroob M
Ali B
Ali S
Aliev M
Alimonti G
Allaire C
Allbrooke BMM
Allport PP
Aloisio A
Alonso F
Alpigiani C
Alves FLL
Alviggi MG
Ambler A
Ambroz L
Amelung C
Amidei D
Amoroso S
Amos KR
Amrouche CS
Ananiev V
Anastopoulos C
Andana RYG
Andari N
Andeen T
Anders JK
Andrean SY
Andreazza A
Angelidakis S
Angerami A
Anisenkov AV
Annovi A
Antel C
Anthony MT
Antipov E
Antonelli M
Antrim DJA
Anulli F
Aoki M
Aparo MA
Appelt C
Aranda CP
Aranzabal N
Araya ST
Arcangeletti C
Arce ATH
Arena E
Arguin JF
Argyropoulos S
Arling JH
Armbruster AJ
Arnaez O
Arnold H
Artoni G
Asada H
Asai K
Asai S
Asbah NA
Asimakopoulou EM
Assahsah J
Assamagan K
Astalos R
Astigarraga MEP
Atkin RJ
Atkinson M
Atlay NB
Atmani H
Atmasiddha PA
Augsten K
Auricchio S
Austrup VA
Avner G
Avolio G
Ayoub MK
Azuelos G
Babal D
Bachacou H
Bachas K
Bachiu A
Backman F
Badea A
Bagnaia P
Bahilo JJL
Bahmani M
Bailey AJ
Bailey VR
Baines JT
Bakalis C
Baker OK
Bakker PJ
Bakos E
Balaji S
Balasubramanian R
Baldin EM
Balek P
Ballabene E
Balli F
Baltes LM
Balunas WK
Balz J
Banas E
Bandieramonte M
Bandyopadhyay A
Bansal S
Barak L
Barberio EL
Barberis D
Barbero M
Barbour G
Barends KN
Barillari T
Barisits MS
Barkeloo J
Barklow T
Barnett RM
Baron P
Baroncelli A
Barone G
Barr AJ
Barreiro F
Barron U
Barrue RFC
Barsov S
Bartels F
Bartoldus R
Bartolini G
Barton AE
Bartos P
Basalaev A
Basan A
Baselga M
Bashta I
Bassalat A
Basso MJ
Basson CR
Bates RL
Batlamous S
Batley JR
Batool B
Battaglia M
Bauce M
Bauer F
Bauer P
Bayirli A
Beacham JB
Beau T
Beauchemin PH
Becherer F
Bechtle P
Beck HP
Becker K
Becot C
Beddall AJ
Bednyakov VA
Bee CP
Beemster LJ
Beermann TA
Begalli M
Begel M
Behera A
Behr JK
Beirer JF
Beisiegel F
Belfkir M
Bella G
Bella LA
Bellagamba L
Bellerive A
Bellos P
Beloborodov K
Belotskiy K
Belyaev NL
Benchekroun D
Benhammou Y
Benjamin DP
Benoit M
Bensinger JR
Bentvelsen S
Beresford L
Beretta M
Berge D
Berger N
Bergmann B
Beringer J
Berlendis S
Berlingen JM
Bernardi G
Bernius C
Bernlochner FU
Berry T
Berta P
Bertram IA
Bethke S
Betti A
Bevan AJ
Bhatta S
Bhattacharya DS
Bhattarai P
Bhopatkar VS
Bi R
Bi R
Bianchi RM
Biebel O
Bielski R
Biesuz NV
Biglietti M
Billoud TRV
Bindi M
Bingul A
Bini C
Biondi S
Biondini A
Birch-sykes CJ
Bird GA
Birman M
Bisanz T
Biswal JP
Biswas D
Bitadze A
Bjorke K
Bloch I
Blocker C
Blue A
Blumenschein U
Blumenthal J
Bobbink GJ
Bobrovnikov VS
Boehler M
Boeriu OEV
Bogavac D
Bogdanchikov AG
Bohm C
Boisvert V
Bokan P
Bolanos GR
Bold T
Bomben M
Bona M
Boonekamp M
Booth CD
Borbely AG
Borecka-Bielska HM
Borgna LS
Borissov G
Bortoletto D
Bosca SR
Boscherini D
Bosman M
Bostanabad MG
Bouaouda K
Boudreau J
Bouhova-Thacker EV
Boumediene D
Bouquet R
Bourdarios CA
Boveia A
Boyd J
Boye D
Boyko IR
Bracinik J
Brahimi N
Brandt G
Brandt O
Braren F
Brau B
Brau JE
Brendlinger K
Brener R
Brenner L
Brenner R
Bressler S
Bret MC
Brickwedde B
Britton D
Britzger D
Brock I
Brooijmans G
Brooks WK
Brost E
Bruers B
Bruncko D
Bruni A
Bruni G
Bruschi M
Bruscino N
Bryngemark L
Buanes T
Buat Q
Buchholz P
Buckley AG
Budagov IA
Bugge MK
Bulekov O
Bullard BA
Burdin S
Burgard CD
Burger AM
Burghgrave B
Burr JTP
Burton CD
Burzynski JC
Busch EL
Buscher V
Bussey PJ
Butler JM
Buttar CM
Butterworth JM
Buttinger W
Buzykaev AR
Bylund OB
Cabras G
Caforio D
Cai H
Cai Y
Cairo VMM
Cakir IT
Cakir O
Calace N
Calafiura P
Calderini G
Calfayan P
Callea G
Caloba LP
Calvet D
Calvet S
Calvet TP
Calvetti M
Camarda S
Camarri P
Camelia EA
Camerlingo MT
Cameron D
Camincher C
Campanelli M
Camplani A
Canale V
Canesse A
Cantero J
Cao Y
Capocasa F
Capriles FGD
Capua M
Carbone A
Cardarelli R
Cardenas JCJ
Cardillo F
Carducci G
Carli T
Carlino G
Carlson BT
Carlson EM
Carlson TI
Carminati L
Carnesale M
Caron S
Carquin E
Carra S
Carratta G
Carter JWS
Carter TM
Casadei D
Casado MP
Casha AF
Castiglia EG
Castillo FL
Castillo LRF
Castro NF
Catinaccio A
Catmore JR
Cavaliere V
Cavalli N
Cavasinni V
Celebi E
Celli F
Centonze MS
Cerny K
Cerqueira AS
Cerri A
Cerrito L
Cerutti F
Cervelli A
Cetin SA
Chadi Z
Chakraborty D
Chala M
Chan J
Chan WS
Chan WY
Chapman JD
Chargeishvili B
Charlton DG
Charman TP
Chatterjee M
Chekanov S
Chekulaev SV
Chelkov GA
Chen A
Chen B
Chen B
Chen C
Chen H
Chen H
Chen J
Chen J
Chen S
Chen SJ
Chen X
Chen X
Chen Y
Cheng CL
Cheng HC
Cheplakov A
Cheremushkina E
Cherepanova E
Cheu E
Cheung K
Chevalier L
Chiarella V
Chiarelli G
Chiodini G
Chisholm AS
Chitan A
Chiu YH
Chizhov MV
Choi K
Chomont AR
Chou Y
Chow YS
Chowdhury T
Christopher LD
Chu MC
Chu X
Chudoba J
Chwastowski JJ
Cieri D
Ciesla KM
Cindro V
Ciocio A
Cirotto F
Citron ZH
Citterio M
Ciubotaru DA
Ciungu BM
Clark A
Clark PJ
Clawson SE
Clement C
Clissa L
Coadou Y
Cobal M
Coccaro A
Codina EP
Coelli S
Cohen H
Coimbra AEC
Cole B
Collot J
Columbie JMC
Connell SH
Connelly IA
Conroy EI
Conventi F
Cooke HG
Cooper-Sarkar AM
Cormier F
Cornell SD
Corpe LD
Corradi M
Correia AMH
Corrigan EE
Corriveau F
Costa MJ
Costanza F
Costanzo D
Cote BM
Coutinho YA
Cowan G
Cowley JW
Cranmer K
Crepe-Renaudin S
Crescioli F
Cristinziani M
Cristoforetti M
Croft V
Crosetti G
Cueto A
Cui H
Cui Z
Cukierman AR
Cunningham WR
Curcio F
Czodrowski P
Czurylo MM
D'amen G
D'Amico V
D'Auria S
D'Eramo L
D'onofrio A
D'Onofrio M
D'uffizi M
Da Costa AMMJ
da Costa JBG
Da Via C
Dabrowski W
Dado T
Dahbi S
Dai T
Dallapiccola C
Dam M
Damazio DO
Damp J
Dandoy JR
Daneri MF
Danninger M
Dao V
Darbo G
Darmora S
Dattagupta A
David C
Davidek T
Davis DR
Davis-Purcell B
Dawson I
de Andrade LM
De Araujo MV
De Asmundis R
De Beurs M
De Carvalho ALM
De Castro S
De Groot N
de Jong P
De K
de la Hoz SG
De la Torre H
De Lima RT
De Maria A
De Regie JBD
de Renstrom PAB
De Sa RCL
De Salvo A
De Sanctis U
De Santis M
De Santo A
De Sousa MJDS
De Souza EEP
Dedovich DV
Degens J
Deiana AM
Del Peso J
Del Rio F
Delegido AJG
Deliot F
Delitzsch CM
Dell'Acqua A
Dell'Asta L
Della Pietra M
Della Volpe D
Delmastro M
Delsart PA
Demers S
Demichev M
Denisov SP
Derendarz D
Derue F
Dervan P
Desch K
Dette K
Deutsch C
Deviveiros PO
Di Bello FA
Di Ciaccio A
Di Ciaccio L
Di Domenico A
Di Donato C
Di Girolamo A
Di Gregorio G
Di Luca A
Di Micco B
Di Nardo R
Diaconu C
Dias BP
Dias FA
Diaz MA
Didenko M
Diehl EB
Dimitriadi C
Dimitrievska A
Ding W
Dingfelder J
Dinu IM
Dittmeier SJ
Dittus F
Djama F
Djobava T
Djuvsland JI
Do Vale TD
Dodsworth D
Doglioni C
Dolejsi J
Dolezal Z
Dominguez LP
Donadelli M
Donaldson CP
Dong B
Donini J
Donszelmann TC
Dopke J
Doria A
Dos Santos SPA
Dova MT
Doyle AT
Drechsler E
Dreyer E
Drobac AS
Du D
du Pree TA
Dubinin F
Dubovsky M
Duchovni E
Duckeck G
Ducu OA
Duda D
Dudarev A
Duflot L
Duhrssen M
Dulsen C
Dumitriu AE
Dunford M
Dungs S
Dunne K
Duperrin A
Duren M
Durglishvili A
Dutta B
Dwyer BL
Dyckes GI
Dyndal M
Dysch S
Dziedzic BS
Eckerova B
Eggleston MG
Ehrke LF
Eigen G
Einsweiler K
Ekelof T
El Ghazali Y
El Jarrari H
El Moursli RC
El Moussaouy A
Ellajosyula V
Ellert M
Ellinghaus F
Elliot AA
Ellis N
Elmsheuser J
Elsing M
Emeliyanov D
Emerman A
Enari Y
Ene I
Erdmann J
Ereditato A
Erland PA
Errenst M
Escalier M
Escobar C
Estabragh MR
Estevez MA
Etzion E
Evans G
Evans H
Evans MO
Ezhilov A
Ezzarqtouni S
Fabbri F
Fabbri L
Facini G
Fadeyev V
Fakhrutdinov RM
Falciano S
Falke PJ
Falke S
Faltova J
Fan Y
Fang Y
Fanourakis G
Fanti M
Faraj M
Farbin A
Farilla A
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Farrington SM
Fassi F
Fassouliotis D
Fawcett WJ
Fayard L
Fedin OL
Fedotov G
Feickert M
Feligioni L
Fell A
Fellers DE
Feng C
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Fenyuk AB
Ferguson SW
Fernandez SG
Ferrando J
Ferrari A
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Ferraz VA
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Filthaut F
Fiolhais MCN
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Fischer F
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Fortman AW
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Freeman PM
Freund WS
Freundlich EM
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Gagnon LG
Gajardo CMR
Gallardo GE
Gallas EJ
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Gama RG
Gan KK
Ganguly S
Gao J
Gao Y
Garcia B
Garcia BRM
Garcia C
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Garcia-Sciveres M
Gardner RW
Garg D
Garg RB
Gargiulo S
Garner CA
Garonne V
Garzon GOY
Gasiorowski SJ
Gaspar P
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Gavrilenko IL
Gavrilyuk A
Gay C
Gaycken G
Gazis EN
Geanta AA
Gee CM
Geisen J
Geisen M
Gemme C
Genest MH
Gentile S
George S
George WF
Geralis T
Gerlach LO
Gessinger-Befurt P
Ghosal A
Ghosh A
Ghosh A
Giacobbe B
Giagu S
Giangiacomi N
Giannelli MF
Giannetti P
Giannini A
Gibson SM
Gignac M
Gil DT
Gilbert BJ
Gillberg D
Gilles G
Gillwald NEK
Gimenez VC
Ginabat L
Gingrich DM
Giordani MP
Giraud PF
Giugliarelli G
Giugni D
Giuli F
Gkialas I
Gkountoumis P
Gladilin LK
Glasman C
Gledhill GR
Glisic M
Gnesi I
Go Y
Goblirsch-Kolb M
Godin D
Goldfarb S
Golling T
Gololo MGD
Golubkov D
Gombas JP
Gomes A
Goncalo R
Goncalves DO
Gonella G
Gonella L
Gongadze A
Goni RG
Gonnella F
Gonski JL
Gonzalez-Sevilla S
Goossens L
Gorasia NA
Gorbounov PA
Gordon HA
Gorini B
Gorini E
Gorisek A
Goshaw AT
Gostkin MI
Gottardo CA
Gouighri M
Goumarre V
Goussiou AG
Gouveia EDM
Govender N
Goy C
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Graham K
Gramstad E
Grancagnolo S
Grandi M
Gratchev V
Gravila PM
Gravili FG
Gray HM
Grefe C
Gregor IM
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Grinstein S
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Grivaz JF
Groh S
Gross E
Grosse-Knetter J
Grud C
Grummer A
Grundy JC
Guan L
Guan W
Gubbels C
Gudnadottir OS
Guescini F
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Guindon S
Guo F
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Gwilliam CB
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Hadavand HK
Haddad ES
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Haghighat SK
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Hall JJ
Hallewell GD
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Hamano K
Hamdaoui H
Hamer M
Hamity GN
Han J
Han K
Han L
Han L
Han S
Han YF
Hanagaki K
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Hangal DA
Hank MD
Hankache R
Hansen E
Hansen JB
Hansen JD
Hansen PH
Hara K
Harada D
Harenberg T
Harkusha S
Harris YT
Harrison PF
Hartman NM
Hartmann NM
Hasegawa Y
Hasib A
Haug S
Hauser R
Havranek M
Hawkes CM
Hawkings RJ
Hayashida S
Hayden D
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Hayes RL
Hays CP
Hays JM
Hayward HS
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Heidorn WD
Heilman J
Heim S
Heim T
Heinemann B
Heinlein JG
Heinrich JJ
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Hejbal J
Helary L
Held A
Helling CM
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Herde H
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Hinterkeuser F
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Hodkinson BH
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Hoffman ACA
Hohn D
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Hommels LBAH
Honan BP
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Hooberman BH
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Hryn'ova T
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Hubacek Z
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Huegging F
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Ibanez AP
Ibragimov I
Iconomidou-Fayard L
Iengo P
Iglesias JAS
Iguchi R
Iizawa T
Ikegami Y
Ilg A
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Imam H
Introzzi G
Iodice M
Ippolito V
Ishino M
Islam W
Issever C
Istin S
Ito H
Iuppa R
Ivina A
Izen JM
Izzo V
Jacka P
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Jacobs RM
Jaeger BP
Jagfeld CS
Jakel G
Jakobs K
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Jamieson J
Janas KW
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Jaspan AE
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Jeanneau F
Jeanty L
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Jenni P
Jezequel S
Jia J
Jia X
Jia Z
Jiang Y
Jiggins S
Jimenez YH
Jin S
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Jinnouchi O
Jivan H
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Johnson CA
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Jones TJ
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Ju X
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Kabana S
Kaczmarska A
Kado M
Kagan H
Kagan M
Kahn A
Kahn A
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Kakati N
Kalderon CW
Kamenshchikov A
Kang NJ
Kano Y
Kar D
Karava K
Kareem MJ
Karentzos E
Karkanias I
Karpov SN
Karpova ZM
Kartvelishvili V
Karyukhin AN
Kasimi E
Kato C
Katzy J
Kaur S
Kawade K
Kawagoe K
Kawaguchi T
Kawamoto T
Kawamura G
Kay EF
Kaya FI
Kazakos S
Kazanin VF
Ke Y
Keaveney JM
Keeler R
Kehris GV
Keller JS
Kelly AS
Kelsey D
Kempster JJ
Kendrick J
Kennedy KE
Kepka O
Kersevan BP
Kersten S
Khandoga M
Khanov A
Kharlamov AG
Kharlamova T
Khoda EE
Khoo TJ
Khoriauli G
Khramov E
Khubua J
Kiehn M
Kilgallon A
Kim E
Kim YK
Kimura N
Kirchhoff A
Kirchmeier D
Kirfel C
Kirk J
Kiryunin AE
Kishimoto T
Kisliuk DP
Kitsaki C
Kivernyk O
Klassen M
Klein C
Klein L
Klein M
Klein MH
Klein U
Klimek P
Klimentov A
Klimpel F
Klingl T
Klioutchnikova T
Klitzner FF
Kluit P
Kluth S
Kneringer E
Knight TM
Knue A
Kobayashi D
Kobayashi R
Kocian M
Kodama T
Kodys P
Koeck DM
Koenig PT
Koffas T
Kohler NM
Kolb M
Koletsou I
Komarek T
Koneke K
Kong AXY
Kono T
Konstantinidis N
Konya B
Kopeliansky R
Koperny S
Korcyl K
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Kortman B
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Kostecka WH
Kostyukhin VV
Kotsokechagia A
Kotwal A
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Kourkoumeli-Charalampidi A
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Kourlitis E
Kovanda O
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Kramarenko VA
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Kurochkin YA
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Kuutmann EB
Kuwertz ES
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Lakomiec IK
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Lambert JE
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Landon MPJ
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Lange JC
Langenberg RJ
Lankford AJ
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Lapertosa A
Laporte JF
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Latonova V
Latour BMD
Lau TS
Laudrain A
Laurier A
Lavorgna M
Lawlor SD
Lawrence Z
Lazzaroni M
Le B
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LeBlanc M
LeCompte T
Ledroit-Guillon F
Lee ACA
Lee GR
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Lefebvre B
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Leggett C
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Leite MAL
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Li X
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Liang Z
Liberatore M
Liberti B
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Lin K
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Lindley RE
Lindon JH
Linss A
Lipeles E
Lipniacka A
Liss TM
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Little JD
Liu B
Liu BX
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Liu JB
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Lloyd SL
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Lubatti HJ
Luci C
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Luehring F
Luise I
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Lundberg O
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Lyubushkin V
Lyubushkina T
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Maccarrone G
MacDonald JC
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Madden WDB
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McCormack WP
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McDougall AE
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Mckenzie RP
Mclaughlin DJ
McLean KD
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McNamara PC
McPherson RA
Mdhluli JE
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Milov A
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Minashvili IA
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Mineev M
Minegishi Y
Mino Y
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Mjornmark JU
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Norisam RRB
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Warburton A
Ward RJ
Warrack N
Watson AT
Watson MF
Watts G
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Webb AF
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Yao WM
Yap YC
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Yeletskikh I
Yexley MR
Yildiz HD
Yin P
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Zeissner SV
Zeitnitz C
Zeng JC
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Zenin O
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Zhao H
Zhao P
Zhao T
Zhao Y
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Zhemchugov A
Zheng Z
Zhong D
Zhou B
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Zhu C
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Zhu H
Zhu HL
Zhu J
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Zhuang X
Zhukov K
Zhulanov V
Zieminska D
Zimine NI
Zimmermann S
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Zorbas TG
Zormpa O
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Zwalinski L
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2022
Field of study

Cross-section measurements of top-quark pair production where the hadronically decaying top quark has transverse momentum greater than 355 GeV and the other top quark decays into ℓνb are presented using 139 fb−1 of data collected by the ATLAS experiment during proton-proton collisions at the LHC. The fiducial cross-section at s = 13 TeV is measured to be σ = 1.267 ± 0.005 ± 0.053 pb, where the uncertainties reflect the limited number of data events and the systematic uncertainties, giving a total uncertainty of 4.2%. The cross-section is measured differentially as a function of variables characterising the tt¯ system and additional radiation in the events. The results are compared with various Monte Carlo generators, including comparisons where the generators are reweighted to match a parton-level calculation at next-to-next-to-leading order. The reweighting improves the agreement between data and theory. The measured distribution of the top-quark transverse momentum is used to search for new physics in the context of the effective field theory framework. No significant deviation from the Standard Model is observed and limits are set on the Wilson coefficients of the dimension-six operators OtG and Otq(8), where the limits on the latter are the most stringent to date. [Figure not available: see fulltext.]

Archivio istituzionale della ricerca - Università di Trieste

Archivio istituzionale della ricerca - Università degli Studi di Udine

Archivio della Ricerca - Università di Pisa

Archivio della Ricerca - Università di Roma 3

ePubs: the open archive for STFC research publications

Improving topological cluster reconstruction using calorimeter cell timing in ATLAS

Author: Aad G
Abbott B
Abeling K
Abicht NJ
Abidi SH
Aboulhorma A
Abramowicz H
Abreu H
Abulaiti Y
Acharya BS
Adamczyk L
Addepalli SV
Addison MJ
Adelman J
Adiguzel A
Adye T
Affolder AA
Afik Y
Agaras MN
Agarwala J
Aggarwal A
Agheorghiesei C
Agullo P Martinez
Ahmad A
Ahmadov F
Ahmed WS
Ahuja S
Ai X
Aielli G
Aikot A
Aitbenchikh B
Aizenberg I
Akbiyik M
Akimov AV
Akiyama D
Akolkar NN
Aktas S
Alberghi GL
Albert J
Albicocco P
Albouy GL
Alderweireldt S
Aleksa M
Aleksandrov IN
Alexa C
Alexopoulos T
Alfonsi F
Algren M
Alhroob M
Ali B
Ali HMJ
Ali S
Alibocus SW
Aliev M
Alimonti G
Alkakhi W
Allaire C
Allbrooke BMM
Allen JF
Allport PP
Aloisio A
Alonso A Garcia
Alonso F
Alpigiani C
Alvarez IR Sotarriva
Alves FL Lucio
Alviggi MG
Aly M
Ambler A
Amelung C
Amerl M
Ames CG
Amidei D
Amos KR
Ananiev V
Anastopoulos C
Andana RY González
Andeen T
Anders JK
Andrean SY
Andreazza A
Angelidakis S
Angerami A
Anisenkov AV
Annovi A
Antel C
Anthony MT
Antipov E
Antonelli M
Anulli F
Aoki M
Aoki T
Aparo MA
Appelt C
Apyan A
Aranda C Padilla
Aranzabal N
Araya S Tapia
Arcangeletti C
Arce ATH
Arena E
Argos F Carrio
Arguin J-F
Argyropoulos S
Arling J-H
Arnaez O
Arnold H
Artoni G
Asada H
Asai K
Asai S
Asbah NA
Assamagan K
Astalos R
Astigarraga ME Pozo
Atashi S
Atkin RJ
Atkinson M
Atmani H
Atmasiddha PA
Augsten K
Auricchio S
Auriol AD
Austrup VA
Avolio G
Axiotis K
Azuelos G
Babal D
Bachacou H
Bachas K
Bachiu A
Backman F
Badea A
Baer TM
Bagnaia P
Bahmani M
Bailey AJ
Bailey VR
Baines JT
Baines L
Baker OK
Bakos E
Balakrishnan V
Balasubramanian R
Baldin EM
Balek P
Ballabene E
Balli F
Baltes LM
Balunas WK
Balz J
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Bandieramonte M
Bandyopadhyay A
Bansal S
Barak L
Barakat M
Barberio EL
Barberis D
Barbero M
Barel MZ
Barends KN
Barillari T
Barisits M-S
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Barsov S
Bartels F
Bartoldus R
Barton AE
Bartos P
Basan A
Baselga M
Bassalat A
Basso MJ
Basson CR
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Battulga D
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Beacham JB
Beau T
Beaucamp JY
Beauchemin PH
Becherer F
Bechtle P
Beck HP
Becker K
Beddall AJ
Bednyakov VA
Bee CP
Beemster LJ
Beermann TA
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Behera A
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Cheu E
Cheung K
Chevalier L
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Chiedde N
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de Jong P
de la Hoz S González
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de Renstrom PA Bruckman
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Zerwas D
Zhai M
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Zhao H
Zhao T
Zhao Y
Zhao Z
Zhemchugov A
Zheng J
Zheng K
Zheng X
Zheng Z
Zhong D
Zhou B
Zhou H
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Zhu CG
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Zhu Y
Zhuang X
Zhukov K
Zhulanov V
Zimine NI
Zinsser J
Ziolkowski M
Zoccoli A
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Zorbas TG
Zormpa O
Zou W
Zwalinski L
Åkesson TPA
Öncel ÖO
Ženiš T
Živković L
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 03/05/2024
Field of study

Clusters of topologically connected calorimeter cells around cells with large absolute signal-to-noise ratio (topo-clusters) are the basis for calorimeter signal reconstruction in the ATLAS experiment. Topological cell clustering has proven performant in LHC Runs 1 and 2. It is, however, susceptible to out-of-time pile-up of signals from soft collisions outside the 25 ns proton-bunch-crossing window associated with the event’s hard collision. To reduce this effect, a calorimeter-cell timing criterion was added to the signal-to-noise ratio requirement in the clustering algorithm. Multiple versions of this criterion were tested by reconstructing hadronic signals in simulated events and Run 2 ATLAS data. The preferred version is found to reduce the out-of-time pile-up jet multiplicity by ∼50% for jet pT ∼ 20 GeV and by ∼80% for jet pT 50 GeV, while not disrupting the reconstruction of hadronic signals of interest, and improving the jet energy resolution by up to 5% for 20 < pT < 30 GeV. Pile-up is also suppressed for other physics objects based on topo-clusters (electrons, photons, τ -leptons), reducing the overall event size on disk by about 6% in early Run 3 pileup conditions. Offline reconstruction for Run 3 includes the timing requirement

UCL Discovery

Software Performance of the ATLAS Track Reconstruction for LHC Run 3

Author: Aad G
Abbott B
Abeling K
Abicht NJ
Abidi SH
Aboulhorma A
Abramowicz H
Abreu H
Abulaiti Y
Acharya BS
Adam Bourdarios C
Adamczyk L
Adamek L
Addepalli SV
Addison MJ
Adelman J
Adiguzel A
Adye T
Affolder AA
Afik Y
Agaras MN
Agarwala J
Aggarwal A
Agheorghiesei C
Agullo P Martinez
Ahmad A
Ahmadov F
Ahmed WS
Ahnen J Von
Ahuja S
Ai X
Aielli G
Aikot A
Aitbenchikh B
Aizenberg I
Akbiyik M
Akimov AV
Akiyama D
Akolkar NN
Alberghi GL
Albert J
Albicocco P
Albouy GL
Alderweireldt S
Aleksa M
Aleksandrov IN
Alexa C
Alexopoulos T
Alfonsi F
Algren M
Alhroob M
Ali B
Ali HMJ
Ali S
Alibocus SW
Aliev M
Alimonti G
Alkakhi W
Allaire C
Allbrooke BMM
Allen JF
Allendes Flores CA
Allport PP
Aloisio A
Alonso A Garcia
Alonso F
Alpigiani C
Alvarez Estevez M
Alvarez Fernandez A
Alvarez IR Sotarriva
Alves Cardoso M
Alves FL Lucio
Alviggi MG
Aly M
Amaral Coutinho Y
Ambler A
Amelung C
Amerl M
Ames CG
Amidei D
Amor Dos Santos SP
Amos KR
Ananiev V
Anastopoulos C
Andana RY González
Andeen T
Anders JK
Andrean SY
Andreazza A
Angelidakis S
Angerami A
Anisenkov AV
Annovi A
Antel C
Anthony MT
Antipov E
Antonelli M
Anulli F
Aoki M
Aoki T
Aparisi Pozo JA
Aparo MA
Aperio Bella L
Appelt C
Apyan A
Aranda C Padilla
Aranzabal N
Araya S Tapia
Arbiol Val SJ
Arcangeletti C
Arce ATH
Arena E
Argos F Carrio
Arguin J-F
Argyropoulos S
Arling J-H
Arnaez O
Arneman DR Van
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Artoni G
Asada H
Asai K
Asai S
Asbah NA
Assahsah J
Assamagan K
Astalos R
Astigarraga ME Pozo
Atashi S
Atkin RJ
Atkinson M
Atmani H
Atmasiddha PA
Augsten K
Auricchio S
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Avolio G
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Azuelos G
Babal D
Bachacou H
Bachas K
Bachiu A
Backman F
Badea A
Bagnaia P
Bahmani M
Bailey AJ
Bailey VR
Baines JT
Baines L
Baker OK
Bakos E
Bakshi Gupta D
Balakrishnan V
Balasubramanian R
Baldin EM
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Bazzano Hurrell LT
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Castiglia EG
Castillo FL
Castillo LR Flores
Castro NF
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Cavaliere V
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Cekmecelioglu YC
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Centeno G Löschcke
Centonze MS
Cepaitis V
Cerny K
Cerqueira AS
Cerri A
Cerrito L
Cerutti F
Cervato B
Cervelli A
Cesarini G
Cetin SA
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Chapman JD
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Charlton DG
Charman TP
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Chauhan C
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Chekulaev SV
Chelkov GA
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Cheng CL
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Chiarella V
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Chisholm AS
Chitan A
Chitishvili M
Chizhov MV
Choi A Cordeiro Oudot
Choi K
Chomont AR
Chou Y
Chow EYS
Chowdhury T
Chu KL
Chu MC
Chu X
Chudoba J
Chwastowski JJ
Ciaccio A Di
Ciaccio L Di
Cieri D
Ciesla KM
Cindro V
Ciocio A
Cirotto F
Citron ZH
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Clawson SE
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Cooper-Sarkar AM
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Czurylo MM
Da Costa AM Mendes Jacques
Da Cunha Sargedas De Sousa MJ
Da Fonseca Pinto JV
Da Silva G Gomes
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Damazio D Oliveira
Damp J
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Daneri MF
Danninger M
Dao V
Darbo G
Darmora S
Das SJ
David C
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Davis-Purcell B
Dawson I
Day-hall HA
De Abreu Farias PC Machado
De Acedo L Flores Sanz
de Andrade Filho L Manhaes
De Araujo M Verissimo
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De Biase N
De Carvalho AL Moreira
De Castro S
De Groot N
de Jong P
de la Hoz S González
De la Torre H
De Lima R Teixeira
De Maria A
De Moura Junior NMJ Nunes
De Sa R Coelho Lopes
De Salvo A
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De Simas Filho E Furtado
De Souza E Egidio Purcino
De Vivie De Regie JB
De K
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Degens J
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Dimitrievska A
Dingfelder J
Dinu I-M
Dittmeier SJ
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Domenico A Di
Dominguez L Pascual
Dona KM
Donadelli M
Donato C Di
Donell DM Mac
Dong B
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Donszelmann T Cuhadar
Dopke J
Doria A
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Drobac AS
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Publication venue: 'Springer Science and Business Media LLC'
Publication date: 02/04/2024
Field of study

Charged particle reconstruction in the presence of many simultaneous proton–proton (pp) collisions in the LHC is a challenging task for the ATLAS experiment’s reconstruction software due to the combinatorial complexity. This paper describes the major changes made to adapt the software to reconstruct high-activity collisions with an average of 50 or more simultaneous pp interactions per bunch crossing (pileup) promptly using the available computing resources. The performance of the key components of the track reconstruction chain and its dependence on pile-up are evaluated, and the improvement achieved compared to the previous software version is quantified. For events with an average of 60 pp collisions per bunch crossing, the updated track reconstruction is twice as fast as the previous version, without significant reduction in reconstruction efficiency and while reducing the rate of combinatorial fake tracks by more than a factor two

UCL Discovery