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581 research outputs found

Assessing Heavy Episodic Drinking: A Random Survey of 18 to 34-Year-Olds in Four Cities in Four Different Continents

Author: Adan
Alfred Makanjuola
Anne Taylor
Babor
Bloomfield
Bridgette Bewick
Eleonora Dal Grande
Graeme Tucker
Hosmer
Ibanga
Paulo Alterwain
Qian Ling
Sudhinaraset
Valentina Kirzhanova
Publication venue: 'MDPI AG'
Publication date: 01/01/2019
Field of study

Background: Heavy episodic drinking (HED) can have health and social consequences. This study assesses the associations between HED and demographic, socioeconomic, motivation and effects indicators for people aged 18–34 years old living in four cities in different regions of the world. Method: Multistage random sampling was consistent across the four cities (Ilorin (Nigeria), Wuhan (China), Montevideo (Uruguay) and Moscow (Russia)). The questionnaire was forward/back translated and face-to-face interviewing was undertaken. A total of 6235 interviews were undertaken in 2014. Separate univariable and multivariable modelling was undertaken to determine the best predictors of HED. Results: HED prevalence was 9.0%. The best predictors differed for each city. The higher probability of HED in the final models included beliefs that they have reached adulthood, feeling relaxed as an effect of drinking alcohol, and forgetting problems as an effect of drinking alcohol. Lower probability of HED was associated with not being interested in alcohol as a reason for limiting alcohol, and the belief that drinking alcohol is too expensive or a waste of money. Conclusion: Although some indicators were common across the four cities, the variables included in the final models predominantly differed from city to city. The need for country-specific prevention and early intervention programs are warranted

Crossref

Adelaide Research & Scholarship

Directory of Open Access Journals

White Rose Research Online

Meta-analysis of lipid-traits in Hispanics identifies novel loci, population-specific effects and tissue-specific enrichment of eQTLs

Author: Below Jennifer E.
Bottinger Erwin
Candille Sophie
Cox Nancy J.
Cruz Miguel
Duan Qing
Gamazon Eric R.
Gottesman Omri
Hanis Craig L.
Ida Chen Y.-D.
Krithika S.
Li Yun
Loos Ruth J. F.
Lu Yingchang
Manichakul Ani
Morris Andrew P.
Parra Esteban J.
Peralta-Romero Jesus
Rich Stephen S.
Rotter Jerome I.
Tang Hua
Taylor Kent D.
Torres Jason
Valladares-Salgado Adan
Wang Xin-Qun
Publication venue: 'Springer Science and Business Media LLC'
Publication date: 01/01/2016
Field of study

We performed genome-wide meta-analysis of lipid traits on three samples of Mexican and Mexican American ancestry comprising 4,383 individuals and followed up significant and highly suggestive associations in three additional Hispanic samples comprising 7,876 individuals. Genome-wide significant signals were observed in or near CELSR2, ZNF259/APOA5, KANK2/DOCK6 and NCAN/MAU2 for total cholesterol, LPL, ABCA1, ZNF259/APOA5, LIPC and CETP for HDL cholesterol, CELSR2, APOB and NCAN/MAU2 for LDL cholesterol and GCKR, TRIB1, ZNF259/APOA5 and NCAN/MAU2 for triglycerides. Linkage disequilibrium and conditional analyses indicate that signals observed at ABCA1 and LIPC for HDL cholesterol and NCAN/MAU2 for triglycerides are independent of previously reported lead SNP associations. Analyses of lead SNPs from the European Global Lipids Genetics Consortium (GLGC) dataset in our Hispanic samples show remarkable concordance of direction of effects as well as strong correlation in effect sizes. A meta-analysis of the European GLGC and our Hispanic datasets identified five novel regions reaching genome-wide significance: two for total cholesterol (FN1 and SAMM50), two for HDL cholesterol (LOC100996634 and COPB1) and one for LDL cholesterol (LINC00324/CTC1/PFAS). The top meta-analysis signals were found to be enriched for SNPs associated with gene expression in a tissue-specific fashion, suggesting an enrichment of tissue-specific function in lipid-associated loci

Anglia Ruskin Research

PubMed Central

Carolina Digital Repository

eScholarship - University of California

Fiber ball white matter modeling in focal epilepsy

Author: Adan Guleed
Biswas Shubhabrata
Bonilha Leonardo
Bryant Lorna
de Bezenac Christophe
Jensen Jens H
Keller Simon S
Kreilkamp Barbara AK
Marson Anthony G
McKinnon Emilie T
Taylor James A
Wieshmann Udo C
Publication venue: 'Wiley'
Publication date: 01/06/2021
Field of study

University of Liverpool Repository

Treatment outcomes and late toxicities in patients with embryonal central nervous system tumors

Author: A Gajjar
A Yancey
AC Paulino
AE Kiltie
AL Albright
C Hua
CM Brownstein
D Strother
DL Buscariollo
DR Copeland
EA Livesey
EC Halperin
EC Halperin
EC Halperin
Haruyasu Yoshida
Hiroaki Goto
Hiroko Yuki
I Ilveskoski
JM Hilden
JW Goldwein
K von Hoff
Kazumasa Odagiri
KF Ginn
L Adan
M Chintagumpala
M Massimino
Masaharu Hata
Masanori Adachi
MB Ranke
MD Ris
Motoko Omura
Noriko Aida
PM Zeltzer
PP Coradini
PR Brock
RE Taylor
RE Taylor
RI Jakacki
RK Mulhern
S Suwa
SN Chi
Susumu Ito
SY Kim
TE Merchant
TE Merchant
TE Merchant
Tetsu Niwa
TM Tekautz
Tomio Inoue
TS Hong
UH Athale
W Xu
YW Chen
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Genetic architecture of lipid traits in the Hispanic community health study/study of Latinos

Author: A Ko
Adan Valladares-Salgado
Alanna C. Morrison
Alex Reiner
Anne E. Justice
C Hill
C Lorenzo
Carl D. Langefeld
Carlos Jose Rodriguez
Cathy Laurie
CC Elbers
Charles Kooperberg
Chuan Gao
CJ Willer
D Weissglas-Volkov
Design of the Women’s Health Initiative clinical trial and observational study
Eimear Kenny
Eric A. Whitsel
Eric Boerwinkle
Esteban Parra
George Papanicolaou
Gregory A. Talavera
H Tada
J Wu
JE Below
Jennifer E. Below
Jill M. Norris
Kari E. North
Kent D. Taylor
L Dumitrescu
L Henkin
Leslie S. Emery
Lynne E. Wagenknecht
M Fenger
Mariaelisa Graff
ME Sweeney
Miguel Cruz
MO Goodarzi
N Zubair
Nicholette D. Palmer
PD Sorlie
PP Toth
Qing Duan
Ruth J. F. Loos
T Sofer
Tamar Sofer
Third Report of the National Cholesterol Education Program (NCEP)
WB Kannel
Y Wu
Yii-Der Ida Chen
Yun Li
Publication venue: 'Springer Science and Business Media LLC'
Publication date
Field of study

Crossref

Genetic Drivers of Heterogeneity in Type 2 Diabetes Pathophysiology

Author: Adair Linda S
Adeyemo Adebowale
Aguilar-Salinas Carlos A
Ahlqvist Emma
Ahluwalia Tarunveer S
Ahsan Habibul
An Ping
Anand Sonia S
Arruda Ana Luiza
Becker Diane M
Below Jennifer E
Bertoni Alain
Bharadwaj Dwaipayan
Bielak Lawrence F
Bocher Ozvan
Boehnke Michael
Bonnefond Amélie
Bork-Jensen Jette
Bowden Donald W
Bragg Fiona
Brandslund Ivan
Broadaway K Alaine
Brody Jennifer A
Buchanan Thomas A
Burant Charles F
Butterworth Adam S
Cade Brian E
Canouil Mickaël
Chai Jin-Fang
Chambers John C
Chan Juliana C N
Chandak Giriraj R
Chang Kyong-Mi
Chang Li-Ching
Chee Miao-Li
Chen Chien-Hsiun
Chen Guanjie
Chen Ji
Chen Shyh-Huei
Chen Wei-Min
Chen Yii-Der Ida
Chen Yuan-Tsong
Chen Zhengming
Cheng Ching-Yu
Cho Yoon Shin
Choi Hyeok Sun
Chuang Lee-Ming
Collins Francis S
Cook James P
Cruz Miguel
Cui Jinrui
Cushman Mary
Danesh John
Das Swapan K
de Silva H Janaka
Dedoussis George
Denny Joshua C
Dimitrov Latchezar
Doumatey Ayo P
Du Shufa
Duan Qing
Dupuis Josee
Eckardt Kai-Uwe
Emery Leslie S
Engert James C
Evans Daniel S
Evans Michele K
Finer Sarah
Fischer Krista
Florez Jose C
Floyd James S
Ford Ian
Fornage Myriam
Franco Oscar H
Frayling Timothy M
Freedman Barry I
Froguel Philippe
Genter Pauline
Gerstein Hertzel C
Ghanbari Mohsen
Giedraitis Vilmantas
Gieger Christian
González-Villalpando Clicerio
González-Villalpando Maria Elena
Goodarzi Mark O
Gordon-Larsen Penny
Graff Mariaelisa
Grallert Harald
Grarup Niels
Gross Myron
Guare Lindsay A
Guo Xiuqing
Hackinger Sophie
Hai Yang
Haiman Christopher A
Hakaste Liisa
Han Sohee
Hanis Craig L
Hansen Torben
Hattersley Andrew T
Hatzikotoulas Konstantinos
Hayes M Geoffrey
Herder Christian
Horikoshi Momoko
Howard Annie-Green
Hsueh Willa
Huang Mengna
Huang Wei
Huerta-Chagoya Alicia
Hung Yi-Jen
Hwang Mi Yeong
Hwu Chii-Min
Ichihara Sahoko
Igase Michiya
Ikram Mohammad Arfan
Ingelsson Erik
Ingelsson Martin
Ipp Eli
Islam Md Tariqul
Isono Masato
Jang Hye-Mi
Jasmine Farzana
Jiang Guozhi
Jonas Jost B
Joo Yoonjung Yoonie
Jukema J Wouter
Jørgensen Torben
Kabagambe Edmond
Kadowaki Takashi
Kals Mart
Kamali Zoha
Kamanu Frederick K
Kandeel Fouad R
Kanoni Stavroula
Kardia Sharon L R
Kasturiratne Anuradhani
Kato Norihiro
Katsuya Tomohiro
Kaur Varinderpal
Kawaguchi Takahisa
Keaton Jacob M
Kho Abel N
Khor Chiea-Chuen
Kibriya Muhammad G
Kim Bong-Jo
Kim Duk-Hwan
Kim Young Jin
Koh Woon-Puay
Kooner Jaspal S
Kooperberg Charles
Kronenberg Florian
Kuusisto Johanna
Kwak Soo-Heon
Köttgen Anna
Laakso Markku
Lamri Amel
Lange Leslie A
Langenberg Claudia
Lee Jung-Jin
Lee Juyoung
Lee Kyung Min
Lee Myung-Shik
Lee Nanette R
Lee Simon S K
Leong Aaron
Li Liming
Li Yun
Li-Gao Ruifang
Ligthart Symen
Lim Victor J Y
Lin Kuang
Lind Lars
Lindgren Cecilia M
Linneberg Allan
Liu Ching-Ti
Liu Jianjun
Liu Simin
Liu Yongmei
Locke Adam E
Long Jirong
Loos Ruth J F
Lorenz Kim M
Louie Tin
Luan Jian\u27an
Luk Andrea O
Luo Xi
Lv Jun
Lynch Julie A
Lyssenko Valeriya
Läll Kristi
Ma Ronald C W
Maeda Shiro
Mahajan Anubha
Mamakou Vasiliki
Mandla Ravi
Mansuri Sohail Rafik
Marston Nicholas A
Matsuda Fumihiko
Matsuda Koichi
McCarthy Mark I
McKean-Cowdin Roberta
Meigs James B
Meitinger Thomas
Melander Olle
Melloni Giorgio E M
Mercader Josep M
Metspalu Andres
Millwood Iona Y
Mo Huan
Mohlke Karen L
Mook-Kanamori Dennis O
Moon Sanghoon
Morris Andrew D
Morris Andrew P
Motala Ayesha A
Moura Filipe A
Mägi Reedik
Nadler Jerry L
Nakatochi Masahiro
Nalls Michael A
Namba Shinichi
Nano Jana
Nayak Uma
Ng Maggie C Y
Nicolas Aude
Nongmaithem Suraj S
Noordam Raymond
North Kari E
Nousome Darryl
Ntalla Ioanna
Okada Yukinori
Orozco Lorena
Palmer Colin N A
Pan Ian
Pankow James S
Park Kyong-Soo
Parra Esteban J
Paré Guillaume
Patel Sanjay R
Patil Snehal
Pedersen Oluf
Pei Pei
Pereira Mark A
Peters Annette
Petty Lauren E
Peyser Patricia A
Pirie Fraser J
Polikowsky Hannah G
Porneala Bianca
Prasad Gauri
Preuss Michael H
Prins Bram Peter
Province Michael A
Psaty Bruce M
Rader Daniel J
Raffel Leslie J
Raffield Laura M
Rasmussen-Torvik Laura J
Rayner Nigel W
Redline Susan
Reiner Alexander P
Rich Stephen S
Ritchie Marylyn D
Roden Michael
Rohde Rebecca
Roll Katheryn
Rotimi Charles N
Rotter Jerome I
Ruff Christian T
Sabanayagam Charumathi
Sale Michèle M
Saleheen Danish
Sandow Kevin
Sankareswaran Alagu
Sarnowski Chloé
Sattar Naveed
Schroeder Philip
Schönherr Sebastian
Scott Robert A
Shahriar Mohammad
Shen Botong
Sheu Wayne H H
Shi Jinxiu
Shin Dong Mun
Shojima Nobuhiro
Shu Xiao-Ou
Sim Xueling
Smith Jennifer A
So Wing Yee
Sofer Tamar
Sonehara Kyuto
Southam Lorraine
Spracklen Cassandra N
Stančáková Alena
Stefansson Kari
Steinthorsdottir Valgerdur
Stilp Adrienne M
Strauch Konstantin
Sun Meng
Suzuki Ken
Tabara Yasuharu
Tai E-Shyong
Takeuchi Fumihiko
Taliun Daniel
Tam Claudia H T
Tan Jingyi
Taylor Henry J
Taylor Kent D
Thangam Manonanthini
Thorand Barbara
Thorleifsson Gudmar
Thorsteinsdottir Unnur
Tomlinson Brian
Tong Lin
Tran Tam C
Trompet Stella
Tsai Fuu-Jen
Tsao Philip S
Tuomi Tiinamaija
Tuomilehto Jaakko
Tusie-Luna Teresa
Udler Miriam S
Valladares-Salgado Adan
van Dam Rob M
van Dijk Ko Willems
van Heel David A
van Klinken Jan B
Vanderwerff Brett
Varma Rohit
Voight Benjamin F
Vujkovic Marijana
Wacher-Rodarte Niels
Walters Robin G
Wang Ya-Xing
Wareham Nicholas J
Wheeler Eleanor
Wickremasinghe Ananda R
Williamson Alice
Wilson James G
Witte Daniel R
Wong Tien-Yin
Wu Jer-Yuarn
Wuttke Matthias
Xiang Anny H
Yajnik Chittaranjan S
Yamamoto Ken
Yamamoto Kenichi
Yamauchi Toshimasa
Yanek Lisa R
Yao Jie
Yin Xianyong
Yokota Mitsuhiro
Yoon Kyungheon
Yu Canqing
Yuan Jian-Min
Yusuf Salim
Zawistowski Matthew
Zeggini Eleftheria
Zhang Liang
Zhang Weihua
Zheng Wei
Zonderman Alan B
Zöllner Sebastian
Publication venue: DigitalCommons@TMC
Publication date: 01/03/2024
Field of study

Type 2 diabetes (T2D) is a heterogeneous disease that develops through diverse pathophysiological processes1,2 and molecular mechanisms that are often specific to cell type3,4. Here, to characterize the genetic contribution to these processes across ancestry groups, we aggregate genome-wide association study data from 2,535,601 individuals (39.7% not of European ancestry), including 428,452 cases of T2D. We identify 1,289 independent association signals at genome-wide significance (P \u3c 5 × 10-8) that map to 611 loci, of which 145 loci are, to our knowledge, previously unreported. We define eight non-overlapping clusters of T2D signals that are characterized by distinct profiles of cardiometabolic trait associations. These clusters are differentially enriched for cell-type-specific regions of open chromatin, including pancreatic islets, adipocytes, endothelial cells and enteroendocrine cells. We build cluster-specific partitioned polygenic scores5 in a further 279,552 individuals of diverse ancestry, including 30,288 cases of T2D, and test their association with T2D-related vascular outcomes. Cluster-specific partitioned polygenic scores are associated with coronary artery disease, peripheral artery disease and end-stage diabetic nephropathy across ancestry groups, highlighting the importance of obesity-related processes in the development of vascular outcomes. Our findings show the value of integrating multi-ancestry genome-wide association study data with single-cell epigenomics to disentangle the aetiological heterogeneity that drives the development and progression of T2D. This might offer a route to optimize global access to genetically informed diabetes care

DigitalCommons@The Texas Medical Center

Genetic drivers of heterogeneity in type 2 diabetes pathophysiology

Author: Adair Linda S.
Adeyemo Adebowale
Aguilar-Salinas Carlos A.
Ahlqvist Emma
Ahluwalia Tarunveer S.
Ahsan Habibul
An Ping
Anand Sonia S.
Arruda Ana Luiza
Becker Diane M.
Below Jennifer E.
Bertoni Alain
Bharadwaj Dwaipayan
Bielak Lawrence F.
Bocher Ozvan
Boehnke Michael
Bonnefond Amélie
Bork-Jensen Jette
Bowden Donald W.
Bragg Fiona
Brandslund Ivan
Broadaway K. Alaine
Brody Jennifer A.
Buchanan Thomas A.
Burant Charles F.
Butterworth Adam S.
Cade Brian E.
Canouil Mickaël
Chai Jin-Fang
Chambers John C.
Chan Juliana C. N.
Chandak Giriraj R.
Chang Kyong-Mi
Chang Li-Ching
Chee Miao-Li
Chen Chien-Hsiun
Chen Guanjie
Chen Ji
Chen Shyh-Huei
Chen Wei-Min
Chen Yii-Der Ida
Chen Yuan-Tsong
Chen Zhengming
Cheng Ching-Yu
Cho Yoon Shin
Choi Hyeok Sun
Chuang Lee-Ming
Collins Francis S.
Cook James P.
Cruz Miguel
Cui Jinrui
Cushman Mary
Dam Rob M. van
Danesh John
Das Swapan K.
de Silva H. Janaka
Dedoussis George
Denny Joshua C.
Dijk Ko Willems van
Dimitrov Latchezar
Doumatey Ayo P.
Du Shufa
Duan Qing
Dupuis Josee
Eckardt Kai-Uwe
Emery Leslie S.
Engert James C.
Evans Daniel S.
Evans Michele K.
Finer Sarah
Fischer Krista
Florez Jose C.
Floyd James S.
Ford Ian
Fornage Myriam
Franco Oscar H.
Frayling Timothy M.
Freedman Barry I.
Froguel Philippe
Genter Pauline
Gerstein Hertzel C.
Ghanbari Mohsen
Giedraitis Vilmantas
Gieger Christian
González-Villalpando Clicerio
González-Villalpando Maria Elena
Goodarzi Mark O.
Gordon-Larsen Penny
Graff Mariaelisa
Grallert Harald
Grarup Niels
Gross Myron
Guare Lindsay A.
Guo Xiuqing
Hackinger Sophie
Hai Yang
Haiman Christopher A.
Hakaste Liisa
Han Sohee
Hanis Craig L.
Hansen Torben
Hattersley Andrew T.
Hatzikotoulas Konstantinos
Hayes M. Geoffrey
Heel David A. van
Herder Christian
Horikoshi Momoko
Howard Annie-Green
Hsueh Willa
Huang Mengna
Huang Wei
Huerta-Chagoya Alicia
Hung Yi-Jen
Hwang Mi Yeong
Hwu Chii-Min
Ichihara Sahoko
Igase Michiya
Ikram Mohammad Arfan
Ingelsson Erik
Ingelsson Martin
Ipp Eli
Islam Md. Tariqul
Isono Masato
Jang Hye-Mi
Jasmine Farzana
Jiang Guozhi
Jonas Jost B.
Joo Yoonjung Yoonie
Jukema J. Wouter
Jørgensen Torben
Kabagambe Edmond
Kadowaki Takashi
Kals Mart
Kamali Zoha
Kamanu Frederick K.
Kandeel Fouad R.
Kanona Stavroula
Kanoni Stavroula
Kardia Sharon L. R.
Kasturiratne Anuradhani
Kato Norihiro
Katsuya Tomohiro
Kaur Varinderpal
Kawaguchi Takahisa
Keaton Jacob M.
Kho Abel N.
Khor Chiea-Chuen
Kibriya Muhammad G.
Kim Bong-Jo
Kim Duk-Hwan
Kim Young Jin
Klinken Jan B. van
Koh Woon-Puay
Kooner Jaspal S.
Kooperberg Charles
Kronenberg Florian
Kuusisto Johanna
Kwak Soo-Heon
Köttgen Anna
Laakso Markku
Lamri Amel
Lange Leslie A.
Langenberg Claudia
Lee Jung-Jin
Lee Juyoung
Lee Kyung Min
Lee Myung-Shik
Lee Nanette R.
Lee Simon S. K.
Leong Aaron
Li Liming
Li Yun
Li-Gao Ruifang
Ligthart Symen
Lim Victor J. Y.
Lin Kuang
Lind Lars
Lindgren Cecilia M.
Linneberg Allan
Liu Ching-Ti
Liu Jianjun
Liu Simin
Liu Yongmei
Locke Adam E.
Long Jirong
Loos Ruth J. F.
Lorenz Kim M.
Louie Tin
Luan Jian’an
Luk Andrea O.
Luo Xi
Lv Jun
Lynch Julie A.
Lyssenko Valeriya
Läll Kristi
Ma Ronald C. W.
Maeda Shiro
Mahajan Anubha
Mamakou Vasiliki
Mandla Ravi
Mansuri Sohail Rafik
Marston Nicholas A.
Matsuda Fumihiko
Matsuda Koichi
McCarthy Mark I.
McKean-Cowdin Roberta
Meigs James B.
Meitinger Thomas
Melander Olle
Melloni Giorgio E. M.
Mercader Josep M.
Metspalu Andres
Millwood Iona Y.
Mo Huan
Mohlke Karen L.
Mook-Kanamori Dennis O.
Moon Sanghoon
Morris Andrew D.
Morris Andrew P.
Motala Ayesha A.
Moura Filipe A.
Mägi Reedik
Nadler Jerry L.
Nakatochi Masahiro
Nalls Michael A.
Namba Shinichi
Nano Jana
Nayak Uma
Ng Maggie C. Y.
Nicolas Aude
Nongmaithem Suraj S.
Noordam Raymond
North Kari E.
Nousome Darryl
Ntalla Ioanna
Okada Yukinori
Orozco Lorena
Palmer Colin N. A.
Pan Ian
Pankow James S.
Park Kyong-Soo
Parra Esteban J.
Paré Guillaume
Patel Sanjay R.
Patil Snehal
Pedersen Oluf
Pei Pei
Pereira Mark A.
Peters Annette
Petty Lauren E.
Peyser Patricia A.
Pirie Fraser J.
Polikowsky Hannah G.
Porneala Bianca
Prasad Gauri
Preuss Michael H.
Prins Bram Peter
Province Michael A.
Psaty Bruce M.
Rader Daniel J.
Raffel Leslie J.
Raffield Laura M.
Rasmussen-Torvik Laura J.
Rayner Nigel W.
Redline Susan
Reiner Alexander P.
Rich Stephen S.
Ritchie Marylyn D.
Roden Michael
Rohde Rebecca
Roll Katheryn
Rotimi Charles N.
Rotter Jerome I.
Ruff Christian T.
Sabanayagam Charumathi
Sale Michèle M.
Saleheen Danish
Sandow Kevin
Sankareswaran Alagu
Sarnowski Chloé
Sattar Naveed
Schroeder Philip
Schönherr Sebastian
Scott Robert A.
Shahriar Mohammad
Shen Botong
Sheu Wayne H. H.
Shi Jinxiu
Shin Dong Mun
Shojima Nobuhiro
Shu Xiao-Ou
Sim Xueling
Smith Jennifer A.
So Wing Yee
Sofer Tamar
Sonehara Kyuto
Southam Lorraine
Spracklen Cassandra N.
Stančáková Alena
Stefansson Kari
Steinthorsdottir Valgerdur
Stilp Adrienne M.
Strauch Konstantin
Sun Meng
Suzuki Ken
Tabara Yasuharu
Tai E-Shyong
Takeuchi Fumihiko
Taliun Daniel
Tam Claudia H. T.
Tan Jingyi
Taylor Henry J.
Taylor Kent D.
Thangam Manonanthini
Thorand Barbara
Thorleifsson Gudmar
Thorsteinsdottir Unnur
Tomlinson Brian
Tong Lin
Tran Tam C.
Trompet Stella
Tsai Fuu-Jen
Tsao Philip S.
Tuomi Tiinamaija
Tuomilehto Jaakko
Tusie-Luna Teresa
Udler Miriam S.
Valladares-Salgado Adan
van Heel David A.
Vanderwerff Brett
Varma Rohit
Voight Benjamin F.
Vujkovic Marijana
Wacher-Rodarte Niels
Walters Robin G.
Wang Ya-Xing
Wareham Nicholas J.
Wheeler Eleanor
Wickremasinghe Ananda R.
Williamson Alice
Wilson James G.
Witte Daniel R.
Wong Tien-Yin
Wu Jer-Yuarn
Wuttke Matthias
Xiang Anny H.
Yajnik Chittaranjan S.
Yamamoto Ken
Yamamoto Kenichi
Yamauchi Toshimasa
Yanek Lisa R.
Yao Jie
Yin Xianyong
Yokota Mitsuhiro
Yoon Kyungheon
Yu Canqing
Yuan Jian-Min
Yusuf Salim
Zawistowski Matthew
Zeggini Eleftheria
Zhang Liang
Zhang Weihua
Zheng Wei
Zonderman Alan B.
Zöllner Sebastian
Publication venue
Publication date: 01/01/2024
Field of study

Type 2 diabetes (T2D) is a heterogeneous disease that develops through diverse pathophysiological processes1,2 and molecular mechanisms that are often specific to cell type3,4. Here, to characterize the genetic contribution to these processes across ancestry groups, we aggregate genome-wide association study data from 2,535,601 individuals (39.7% not of European ancestry), including 428,452 cases of T2D. We identify 1,289 independent association signals at genome-wide significance (P < 5 × 10-8) that map to 611 loci, of which 145 loci are, to our knowledge, previously unreported. We define eight non-overlapping clusters of T2D signals that are characterized by distinct profiles of cardiometabolic trait associations. These clusters are differentially enriched for cell-type-specific regions of open chromatin, including pancreatic islets, adipocytes, endothelial cells and enteroendocrine cells. We build cluster-specific partitioned polygenic scores5 in a further 279,552 individuals of diverse ancestry, including 30,288 cases of T2D, and test their association with T2D-related vascular outcomes. Cluster-specific partitioned polygenic scores are associated with coronary artery disease, peripheral artery disease and end-stage diabetic nephropathy across ancestry groups, highlighting the importance of obesity-related processes in the development of vascular outcomes. Our findings show the value of integrating multi-ancestry genome-wide association study data with single-cell epigenomics to disentangle the aetiological heterogeneity that drives the development and progression of T2D. This might offer a route to optimize global access to genetically informed diabetes care.</p

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Test beam performance of a CBC3-based mini-module for the Phase-2 CMS Outer Tracker before and after neutron irradiation

Author: Abbaneo D.
Abbas M.
Adam W.
Agah A.
Agram J.-L.
Ahmad A.
Ahmed I.
Akpinar A.
Albergo S.
Albert E.
Albrecht A.
Alexander J.
Alhusseini M.
Alibordi M.
Allard Y.
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Šuša T.
Publication venue: Institute of Physics Publishing Ltd
Publication date: 05/05/2023
Field of study

The Large Hadron Collider (LHC) at CERN will undergo major upgrades to increase the instantaneous luminosity up to 5–7.5×10

^{34}

^{-2}

^{-1}

. This High Luminosity upgrade of the LHC (HL-LHC) will deliver a total of 3000–4000 fb-1 of proton-proton collisions at a center-of-mass energy of 13–14 TeV. To cope with these challenging environmental conditions, the strip tracker of the CMS experiment will be upgraded using modules with two closely-spaced silicon sensors to provide information to include tracking in the Level-1 trigger selection. This paper describes the performance, in a test beam experiment, of the first prototype module based on the final version of the CMS Binary Chip front-end ASIC before and after the module was irradiated with neutrons. Results demonstrate that the prototype module satisfies the requirements, providing efficient tracking information, after being irradiated with a total fluence comparable to the one expected through the lifetime of the experiment

KITopen

Combination of CMS searches for heavy resonances decaying to pairs of bosons or leptons

Author: Aarrestad TK
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Abbiendi G
Abbrescia M
Abdullah WAT Wan
Abdullin S
Abercrombie D
Acharya H
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Acosta JG
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Adams MR
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Adan D Perez
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Aguilar-Benitez M
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Publication venue: Elsevier
Publication date: 01/01/2019
Field of study

CMS Collaboration: et al.A statistical combination of searches for heavy resonances decaying to pairs of bosons or leptons is presented. The data correspond to an integrated luminosity of 35.9 fb collected during 2016 by the CMS experiment at the LHC in proton-proton collisions at a center-of-mass energy of 13 TeV. The data are found to be consistent with expectations from the standard model background. Exclusion limits are set in the context of models of spin-1 heavy vector triplets and of spin-2 bulk gravitons. For mass-degenerate W′ and Z′ resonances that predominantly couple to the standard model gauge bosons, the mass exclusion at 95% confidence level of heavy vector bosons is extended to 4.5 TeV as compared to 3.8 TeV determined from the best individual channel. This excluded mass increases to 5.0 TeV if the resonances couple predominantly to fermions.Individuals have received support from the Marie-Curie program and the European Research Council and Horizon 2020 Grant, contract Nos. 675440, 752730, and 765710 (European Union); the Programa Estatal de Fomento de la Investigación Científica y Técnica de Excelencia María de Maeztu, grant MDM-2015-0509 and the Programa Severo Ochoa del Principado de Asturias

University of Liverpool Repository

eScholarship - University of California

ZORA

Digital.CSIC

Repository of the Vinča Nuclear Institute (VinaR)

ePubs: the open archive for STFC research publications

Helsingin yliopiston digitaalinen arkisto

MUSiC: a model-unspecific search for new physics in proton–proton collisions at √s=13TeV

Author: Aarrestad T. K.
Abbaneo D.
Abbiendi G.
Abbrescia M.
Abdelalim A. A.
Abdullah W. A. T. W.
Abdullin S.
Abercrombie D.
Acharya H.
Acosta D.
Acosta J. G.
Adam W.
Adams E.
Adams M. R.
Adams T.
Adan D. P.
Adloff C.
Adzic P.
Afanasiev S.
Agapitos A.
Agarwal G.
Aggleton R.
Agram J. -L.
Aguilar-Benitez M.
Ahmad A.
Ahmad M.
Ahmad W. H.
Ahmed A.
Ahuja S.
Akchurin N.
Akgun B.
Akpinar A.
Albajar C.
Albergo S.
Albert A.
Albrow M.
Aleksandrov A.
Alexander J.
Alhusseini M.
Alimena J.
Alison J.
Allen B.
Almond J.
Alonso A. G.
Alvarez C. R.
Alvarez J. D. R.
Alverson G.
Alves G. A.
Aly R.
Alyari M.
Amapane N.
Amaral S. M. S. D.
Ambrogi F.
Amendola C.
Amin N.
Amram O.
Amsler C.
Anagnostou G.
Anampa K. H.
Anderson D.
Andrea J.
Andreev V.
Andreev Y.
Andrews M. B.
Androsov K.
Ang L.
Angioni G. L. P.
Antchev G.
Antunovic Z.
Anuar A. A. B.
Apanasevich L.
Apollinari G.
Appelt E.
Apresyan A.
Apyan A.
Araujo M.
Arbelaez N. V.
Arcaro D.
Arcidiacono R.
Arenton M. W.
Argiro S.
Arneodo M.
Aruta C.
Asavapibhop B.
Asawatangtrakuldee C.
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Asghar M. I.
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Atakisi I. O.
Atanasov I.
Ather M. W.
Attikis A.
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Publication venue
Publication date: 01/01/2021
Field of study

Results of the Model Unspecific Search in CMS (MUSiC), using proton–proton collision data recorded at the LHC at a centre-of-mass energy of 13TeV, corresponding to an integrated luminosity of 35.9fb-1, are presented. The MUSiC analysis searches for anomalies that could be signatures of physics beyond the standard model. The analysis is based on the comparison of observed data with the standard model prediction, as determined from simulation, in several hundred final states and multiple kinematic distributions. Events containing at least one electron or muon are classified based on their final state topology, and an automated search algorithm surveys the observed data for deviations from the prediction. The sensitivity of the search is validated using multiple methods. No significant deviations from the predictions have been observed. For a wide range of final state topologies, agreement is found between the data and the standard model simulation. This analysis complements dedicated search analyses by significantly expanding the range of final states covered using a model independent approach with the largest data set to date to probe phase space regions beyond the reach of previous general searches

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