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10 research outputs found

Role of genetic testing for inherited prostate cancer risk: Philadelphia prostate cancer consensus conference 2017

Author: Abida W. (Wassim)
Andriole G.L. (Gerald)
Bangma C.H. (Chris)
Bekelman J.E. (Justin E.)
Benson M.C. (Mitchell C.)
Blanco A. (Amie)
Burnett A. (Arthur)
Catalona W.J. (William J.)
Cooney K.A. (Kathleen A.)
Cooperberg M.R. (Matthew)
Crawford D. (David)
Den R.B. (Robert B.)
Dicker A.P. (Adam P.)
Eggener S. (Scott)
Fleshner N.E. (Neil)
Freedman M.L. (Matthew L.)
Giri V.N. (Veda)
Gomella L.G. (Leonard G.)
Griend D.J.V. (Donald J. Vander)
Hamdy F. (Freddie)
Hoffman-Censits J. (Jean)
Hurwitz M.D. (Mark D.)
Hyatt C. (Colette)
Isaacs W.B. (William B.)
Kane C.J. (Christopher J.)
Kantoff P. (Philip)
Karnes R.J. (Jeffrey)
Karsh L.I. (Lawrence I.)
Kelly W.K. (William K.)
Klein E.A. (Eric A.)
Knudsen K.E. (Karen E.)
Lin D.W. (Daniel W.)
Loughlin K.R. (Kevin R.)
Lu-Yao G. (Grace)
Malkowicz S.B. (S. Bruce)
Mann M.J. (Mark J.)
Mark J.R. (James R.)
McCue P.A. (Peter A.)
Miner M.M. (Martin M.)
Morgan T. (Todd)
Moul J.W. (Judd W.)
Myers R.E. (Ronald E.)
Nielsen S.M. (Sarah M.)
Obeid E. (Elias)
Pavlovich C.P. (Christian P.)
Peiper S.C. (Stephen C.)
Penson D.F. (David F.)
Petrylak D.P. (Daniel P)
Pettaway C.A. (Curtis A.)
Pilarski R. (Robert)
Pinto P. (Peter)
Poage W. (Wendy)
Raj G.V. (Ganesh V.)
Rebbeck R. (Timothy)
Robson M. (Mark)
Rosenberg M.T. (Matt T.)
Sandler H. (Howard)
Sartor A.O. (Oliver)
Schaeffer E. (Edward)
Schwartz G.F. (Gordon F.)
Shahin M.S. (Mark S.)
Shore N.D. (Neal)
Shuch B. (Brian)
Soule H.R. (Howard R.)
Tomlins S.A. (Scott A)
Trabulsi E.J. (Edouard J.)
Uzzo R. (Robert)
Walsh P.C. (Patrick)
Weil C.J. (Carol J.)
Wender R. (Richard)
Publication venue: 'American Society of Clinical Oncology (ASCO)'
Publication date: 01/02/2018
Field of study

Purpose: Guidelines are limited for genetic testing for prostate cancer (PCA). The goal of this conference was to develop an expert consensus-dri

Erasmus University Digital Repository

Defining a standard set of patient-centered outcomes for men with localized prostate cancer

Background Value-based health care has been proposed as a unifying force to drive improved outcomes and cost containment. Objective To develop a standard set of multidimensional patient-centered health outcomes for tracking, comparing, and improving localized prostate cancer (PCa) treatment value. Design, setting, and participants We convened an international working group of patients, registry experts, urologists, and radiation oncologists to review existing data and practices. Outcome measurements and statistical analysis The group defined a recommended standard set representing who should be tracked, what should be measured and at what time points, and what data are necessary to make meaningful comparisons. Using a modified Delphi method over a series of teleconferences, the group reached consensus for the Standard Set. Results and limitations We recommend that the Standard Set apply to men with newly diagnosed localized PCa treated with active surveillance, surgery, radiation, or other methods. The Standard Set includes acute toxicities occurring within 6 mo of treatment as well as patient-reported outcomes tracked regularly out to 10 yr. Patient-reported domains of urinary incontinence and irritation, bowel symptoms, sexual symptoms, and hormonal symptoms are included, and the recommended measurement tool is the Expanded Prostate Cancer Index Composite Short Form. Disease control outcomes include overall, cause-specific, metastasis-free, and biochemical relapse-free survival. Baseline clinical, pathologic, and comorbidity information is included to improve the interpretability of comparisons. Conclusions We have defined a simple, easily implemented set of outcomes that we believe should be measured in all men with localized PCa as a crucial first step in improving the value of care. Patient summary Measuring, reporting, and comparing identical outcomes across treatments and treatment centers will provide patients and providers with information to make informed treatment decisions. We defined a set of outcomes that we recommend being tracked for every man being treated for localized prostate cancer

Erasmus University Digital Repository

Fine-mapping of prostate cancer susceptibility loci in a large meta-analysis identifies candidate causal variants

Author: Adolfsson J. (Jan)
Aguado M. (Miguel)
Ahmed M. (Mahbubl)
Aitken J. (Joanne)
Albanes D. (Demetrius)
Alcaraz A. (Antonio)
Aly M. (Markus)
Andriole G.L. (Gerald)
Anokian E. (Ezequiel)
Aukim-Hastie C. (Claire)
Auvinen A. (Anssi)
Bangma C.H. (Chris)
Barnett G. (Gill)
Batra J. (Jyotsna)
Benlloch S. (Sara)
Bentzen Sø. (Søren)
Berndt S.I. (Sonja)
Berry C. (Clare)
Bisbjerg R. (Rasmus)
Bohnert P. (Philipp)
Borre M. (M.)
Brenner H. (Hermann)
Broms M. (Michael)
Brook R.H.
Brown P. (Paul)
Burnet N. (Neil)
Bustamante M. (Mariona)
Butler L. (Lisa)
Calvo P. (Patricia)
Cancel-Tassin G. (Géraldine)
Cannon-Albright L.A. (Lisa)
Canzian F. (Federico)
Cao G. (Guangwen)
Carballo A. (Ana)
Cardoso M. (Marta)
Carracedo A. (Angel)
Carter B.D. (Brian D.)
Castaño-Vinyals G. (Gemma)
Castelao J.E. (Jose )
Cavalli-Bjoerkman C. (Carin)
Cecchini L. (Lluís)
Cenee S. (Sylvie)
Chambers S. (Suzanne)
Chanock S.J. (Stephen)
Christova S. (Svetlana)
Cieza-Borrella C. (Clara)
Claessens F.
Clements J. (Judith)
Conti G. (Giario)
Cook M. (Margaret)
Cox A. (Angela)
Cuk K. (Katarina)
Cussenot O. (Olivier)
Cybulski C. (Cezary)
Dadaev T. (Tokhir)
Davis M. (Michael)
De Langhe S. (Sofie)
De Meerleer G. (Gert)
De Ruyck K. (Kim)
Dearnaley D. (David)
Dierssen-Sotos T. (Trinidad)
Dikov T. (Tihomir)
Ding Y.C. (Yuan Chun)
Donovan J. (Jenny)
Drake B.F. (Bettina F.)
Dunning A.M. (Alison)
Easton D.F. (Douglas)
Eckert A. (Allison)
Eeles R.A. (Rosalind A.)
Eklund M. (Martin)
Elliott R. (Rebecca)
Evans A. (Andrew)
Fachal L. (Laura)
Feng N. (Ninghan)
Finelli A. (Antonio)
Fisher C. (Cyril)
Fitzgerald L.M. (Liesel M.)
Fleshner N.E. (Neil)
Freedman M. (Matthew)
Freeman L.E.B. (Laura E. Beane)
Gago-Dominguez M. (Manuela)
Gamulin M. (Marija)
Gapstur S.M. (Susan M.)
Gardiner R. (Robert)
George A. (Anne)
Geybels M.S. (Milan S.)
Giles G.G. (Graham G.)
Giovannucci E. (Edward)
Goh C. (Chee)
Gomez-Acebo I. (Ines)
Goodman P. (Phyllis)
Govindasami K. (Koveela)
Gracia-Lavedan E. (Esther)
Grindedal E.M. (Eli Marie)
Grönberg H. (Henrik)
Guo J. (Jianming)
Guo X. (Xin)
Guy M. (Michelle)
Gómez-Caamaño A. (Antonio)
Haiman C.A. (Christopher)
Hakansson N. (Niclas)
Hamdy F. (Freddie)
Hamilton R.J. (Robert J.)
Hayes V. (Vanessa)
Haynes A.-M. (Anne-Maree)
Hazel S. (Steve)
He W. (Weiyang)
Henderson B.E. (Brian)
Herkommer K. (Kathleen)
Hicks B. (Belynda)
Holleczek B. (B.)
Hoover R.N. (Robert)
Hopper J.L. (John L.)
Horvath L. (Lisa)
Hunter D. (David)
Hutchinson A. (Amy)
Imai T. (Takashi)
Ingles S.A. (Sue)
Iversen P. (Peter)
Jenster G.W. (Guido)
Johansson J.-E. (Jan-Erik)
John E.M. (Esther)
Joniau S. (Steven)
Kachakova D. (Darina)
Kaneva R. (Radka)
Karlsson A. (Ami)
Kastelan Z. (Zeljko)
Kedda M.-A. (Mary-Anne)
Kerns S.L. (Sarah L.)
Key T.J. (Tim J.)
Khaw K.-T. (Kay-Tee)
Kibel A. (Adam)
Kierzek A. (Andrzej)
Kim J. (Jongoh)
Klarskov P. (Peter)
Klim A. (Aleksandra)
Kluzniak W. (Wojciech)
Kogevinas M. (Manolis)
Kolb S. (Suzanne)
Kolonel L.N. (Laurence)
Kote-Jarai Z.
Koudou Y.A. (Yves Akoli)
Koutros S. (Stella)
Kraft P. (Peter)
Kujala P.M. (Paula)
Kulis T. (Tomislav)
Kulkarni G.S. (Girish S.)
Kwast Th.H. (Theo) van der
Lane A. (Athene)
Larkin S. (Samantha)
Le Marchand L. (Loic)
Leongamornlert D.A. (Daniel A.)
Lessel D. (Davor)
Lewis S.J. (Sarah J.)
Li J. (Jie)
Li M. (Meiling)
Lim J. (Jasmine)
Lin D.W. (Daniel W.)
Lin H.-Y. (Hui-Yi)
Lin J. (Ji)
Lindstrom S. (Sara)
Ling J. (Jin)
Livni N. (Naomi)
Llorca J. (Javier)
Lobato-Busto R. (Ramón)
Logothetis N.K. (Nikos)
Lophatananon A. (Artitaya)
Lu Y.-J. (Yong-Jie)
Lubinski J. (Jan)
Luedeke M. (Manuel)
Ma J. (Jing)
Machiela M.J. (Mitchell J.)
MacInnis R.J. (Robert J.)
Maehle L.
Maia S. (Sofia)
Maier C. (Christiane)
Mao X. (Xueying)
Marsden G. (Gemma)
Martin R.M. (Richard M.)
Martinez M.E. (Maria Elena)
Marzec J. (Jacek)
McDonnell S.K. (Shannon K.)
Menegaux F. (Florence)
Mengual L. (Lourdes)
Michael A. (Agnieszka)
Mijuskovic M. (Martina)
Milne R.L. (Roger)
Mitev V. (Vanio)
Mitkova A. (Atanaska)
Morgan A. (Angela)
Moya L. (Leire)
Mucci L. (Lorelei)
Muir K. (Kenneth)
Mulot C. (Claire)
Murtola T. (Teemu)
Neal D. (David)
Neuhausen S.L. (Susan)
Newcomb L.F. (Lisa F.)
Newcombe B.
Nielsen S.F. (Sune F.)
Nordestgaard B.G. (Børge)
Nordström T. (Tobias)
Olama A.A.A. (Ali Amin Al)
Ong A.T. (Aik T.)
Orntoft T.F. (Torben)
Ost P. (Piet)
Ostrander E.A. (Elaine)
Ostrer H. (Harry)
Pandha H. (Hardev)
Papargiris M. (Melissa)
Park H. (Hyun)
Park J.Y. (Jong Y.)
Parliament M. (Matthew)
Pashayan N. (Nora)
Paulo P. (Paula)
Pedersen J. (John)
Peleteiro P. (Paula)
Penney K.L. (Kathryn L.)
Pharoah P.D.P. (Paul)
Popov E. (Elenko)
Pow-Sang J. (Julio)
Ranu H. (Hardeep)
Razack A. (Azad)
Ren G. (Guoping)
Riboli E. (Elio)
Risbridger G. (Gail)
Riska S. (Shaun)
Roobol-Bouts M.J. (Monique)
Rosenstein B.S. (Barry S.)
Ruiz-Dominguez J.M. (José Manuel)
Rébillard X. (Xavier)
Røder M.A. (Martin Andreas)
Saito S. (Shiro)
Sanchez M. (Marie)
Saunders E.J. (Edward J.)
Saunders P. (Pamela)
Schaid D.J. (D.)
Schaik R.H.N. (Ron) van
Schleutker J. (Johanna)
Schnoeller T. (Thomas)
Schroder F.H. (F. H.)
Schumacher F.R. (Fredrick R)
Sellers T.F.
Sheng X. (Xin)
Siddiq A. (Afshan)
Silva M.P. (Maria P.)
Singhal S. (Sandeep)
Sipeky C. (Csilla)
Slavov C. (Chavdar)
Sorensen K.D. (Karina Dalsgaard)
Southey M.C. (Melissa C.)
Spurdle A. (Amanda)
Srinivasan S. (Srilakshmi)
Stampfer M.J. (Meir J.)
Stanford J.L. (Janet L.)
Stattin P. (Pär)
Steele L. (Linda)
Stegmaier C. (Christa)
Stern M.C. (Mariana C.)
Stevens V.L. (Victoria L.)
Sun Z. (Zan)
Szulkin R. (Robert)
Taari K. (Kimmo)
Talala K. (Kirsi)
Tammela T.L. (Teuvo)
Tan M.H. (Meng H.)
Tangen C.M. (Catherine M.)
Taylor R. (Renea)
Teixeira P.J.
Teo S.-H. (Soo-Hwang)
Thibodeau S.N. (Stephen N.)
Thierens H. (Hubert)
Thompson I.M. (Ian)
Thwaites A. (Alison)
Tilley W. (Wayne)
Tillmans L. (Lori)
Toi A. (Ants)
Townsend P.A. (Paul A.)
Travis S.P.L. (Simon)
Tretarre B. (Brigitte)
Truong T. (Thérèse)
Turman C. (Constance)
Usmani N. (Nawaid)
van den Broeck T. (Thomas)
Vega A. (Ana)
Vlahova A. (Aleksandrina)
Vogel W. (Walther)
Vogt A. (Aurelie)
Wakerell S. (Sarah)
Wang G. (Guomin)
Weinstein S. (Stephanie)
Weisher M. (Maren)
West C. (Catharine)
Whitmore I. (Ian)
Wiklund F. (Fredrik)
Wokolorczyk D. (Dominika)
Wolk K. (Kerstin)
Wu H. (Huihai)
Wu J. (Ji)
Wu Y. (Yudong)
Xu J. (Jianfeng)
Yeadon T. (Trina)
Yu Y. (Yongwei)
Zachariah B. (Babu)
Zhang H.-W. (Hong-Wei)
Zhang Y. (Yangling)
Zhang Z. (Zhuo)
Zhao S.-C. (Shan-Chao)
Zhou B. (Bo)
Zlotta A.R. (Alexandre)
Publication venue
Publication date: 01/01/2018
Field of study

Prostate cancer is a polygenic disease with a large heritable component. A number of common, low-penetrance prostate cancer risk loci have been identified through GWAS. Here we apply the Bayesian multivariate variable selection algorithm JAM to fine-map 84 prostate cancer susceptibility loci, using summary data from a large European ancestry meta-analysis. We observe evidence for multiple independent signals at 12 regions and 99 risk signals overall. Only 15 original GWAS tag SNPs remain among the catalogue of candidate variants identified; the remainder are replaced by more likely candidates. Biological annotation of our credible set of variants indicates significant enrichment within promoter and enhancer elements, and transcription factor-binding sites, including AR, ERG and FOXA1. In 40 regions at least one variant is colocalised with an eQTL in prostate cancer tissue. The refined set of candidate variants substantially increase the proportion of familial relative risk explained by these known susceptibility regions, which highlights the importance of fine-mapping studies and has implications for clinical risk profiling. © 2018 The Author(s).Prostate cancer is a polygenic disease with a large heritable component. A number of common, low-penetrance prostate cancer risk loci have been identified through GWAS. Here we apply the Bayesian multivariate variable selection algorithm JAM to fine-map 84 prostate cancer susceptibility loci, using summary data from a large European ancestry meta-analysis. We observe evidence for multiple independent signals at 12 regions and 99 risk signals overall. Only 15 original GWAS tag SNPs remain among the catalogue of candidate variants identified; the remainder are replaced by more likely candidates. Biological annotation of our credible set of variants indicates significant enrichment within promoter and enhancer elements, and transcription factor-binding sites, including AR, ERG and FOXA1. In 40 regions at least one variant is colocalised with an eQTL in prostate cancer tissue. The refined set of candidate variants substantially increase the proportion of familial relative risk explained by these known susceptibility regions, which highlights the importance of fine-mapping studies and has implications for clinical risk profiling. © 2018 The Author(s).Peer reviewe

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Ultralight vector dark matter search using data from the KAGRA O3GK run

Author: Abac A.G
Abbott R
Abe H
Abouelfettouh I
Acernese F
Ackley K
Adamcewicz C
Adhicary S
Adhikari N
Adhikari R.X
Adkins V.K
Adya V.B
Affeldt C
Agarwal D
Agathos M
Aguiar O.D
Aguilar I
Aiello L
Ain A
Ajith P
Akutsu T
Al-Jodah A
Al-Shammari S
Albanesi S
Alfaidi R.A
Allocca A
Alléné C
Altin P.A
Alvarez-Lopez S
Amato A
Amez-Droz L
Amorosi A
Amra C
Anand S
Ananyeva A
Anderson S.B
Anderson W.G
Andia M
Ando M
Andrade T
Andres N
Andrić T
Andrés-Carcasona M
Anglin J
Ansoldi S
Antelis J.M
Antier S
Aoumi M
Appavuravther E.Z
Appert S
Apple S.K
Arai K
Araya A
Araya M.C
Areeda J.S
Arellano F.E. Peña
Argianas L. Granda
Aritomi N
Armato F
Arnaud N
Arogeti M
Aronson S.M
Arun K.G
Ashton G
Aso Y
Assiduo M
Aston S.M
Astone P
Aubin F
Aultoneal K
Avallone G
Babak S
Badaracco F
Badger C
Bae S
Bagnasco S
Bagui E
Bai Y
Baier J.G
Bajpai R
Baka T
Ball M
Ballardin G
Ballmer S.W
Banagiri S
Banerjee B
Bankar D
Baral P
Barayoga J.C
Barish B.C
Barker D
Barneo P
Barone F
Barr B
Barsotti L
Barsuglia M
Barta D
Barthelmy S.D
Barton M.A
Bartos I
Basak S
Basalaev A
Bassiri R
Basti A
Bawaj M
Baxi P
Bayley J.C
Baylor A.C
Bazzan M
Bedakihale V.M
Beirnaert F
Bejger M
Belardinelli D
Bell A.S
Benedetto V
Beniwal D
Benoit W
Bentley J.D
Bera S
Berbel M
Bergamin F
Berger B.K
Bernuzzi S
Beroiz M
Bersanetti D
Bertolini A
Betzwieser J
Beveridge D
Bevins N
Bhandare R
Bhardwaj U
Bhatt R
Bhattacharjee D
Bhaumik S
Bhowmick S
Bianchi A
Bilenko I.A
Billingsley G
Binetti A
Bini S
Birnholtz O
Biscoveanu S
Bisht A
Bitossi M
Bizouard M.-A
Blackburn J.K
Blair C.D
Blair D.G
Bobba F
Bode N
Bogaert G
Boileau G
Boldrini M
Bolingbroke G.N
Bolliand A
Bonavena L.D
Bondarescu R
Bondu F
Bonilla E
Bonilla M.S
Bonino A
Bonnand R
Booker P
Borchers A
Boschi V
Bose S
Bossilkov V
Boudart V
Boumerdassi A
Bozzi A
Bradaschia C
Brady P.R
Braglia M
Branch A
Branchesi M
Breschi M
Briant T
Brillet A
Brinkmann M
Brockill P
Brockmueller E
Brooks A.F
Brown D.D
Brozzetti M.L
Brunett S
Bruno G
Bruntz R
Bryant J
Bucci F
Buchanan J
Bulashenko O
Bulik T
Bulten H.J
Buonanno A
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Cabourn Davies G.S
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Chaturvedi M
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Cheung H.T
Chia H.Y
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Chiang C
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Chincarini A
Chiofalo M.L
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Chua S.S.Y
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d'Emilio V
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d'Urso D
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Dal Canton T
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Danilishin S
Danzmann K
Darroch K.E
Dartez L.P
Dasgupta A
Datta S
Dattilo V
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Dave I
Davenport A
Davier M
Davies T.F
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de Matteis F
de Pietri R
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de Rossi C
de Simone R
de Souza Melo S. Assis
Deenadayalan M
Degallaix J
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Vermeulen S.M
Veske D
Vetrano F
Veutro A
Vibhute A.M
Viceré A
Vidal F.A. Ramis
Vidyant S
Viets A.D
Vijaykumar A
Vilkha A
Villa-Ortega V
Vincent E.T
Vinet J.-Y
Viret S
Virtuoso A
Vitale S
Vocca H
Voigt D
von Reis E.R.G
von Wrangel J.S.A
Vyatchanin S.P
Wade L.E
Wade M
Wagner K.J
Walet R.C
Walker M
Wallace G.S
Wallace L
Wang H
Wang J.Z
Wang W.H
Wang Z
Waratkar G
Ward R.L
Warner J
Was M
Washimi T
Washington N.Y
Watarai D
Wayt K.E
Weaver B
Weaving C.R
Webster S.A
Weinert M
Weinstein A.J
Weiss R
Weller C.M
Weller R.A
Wellmann F
Wen L
Wette K
Weßels P
Whelan J.T
White D.D
Whiting B.F
Whittle C
Wildberger J.B
Wilk O.S
Wilken D
Willetts K
Williams D
Williams M.J
Williams N.S
Willis J.L
Willke B
Wils M
Wipf C.C
Woan G
Woehler J
Wofford J.K
Wolfe N.E
Wong D
Wong H.T
Wong H.W.Y
Wong I.C.F
Wright J.L
Wright M
Wu C
Wu D.S
Wu H
Wysocki D.M
Xiao L
Xu V.A
Xu Y
Yaala M. Ben
Yadav N
Yamamoto H
Yamamoto K
Yamamoto M
Yamamoto T
Yamamoto T.S
Yamamura S
Yamazaki R
Yan S
Yan T
Yang F
Yang F.W
Yang K.Z
Yang L.-C
Yang Y
Yarbrough Z
Yeh S.-W
Yelikar A.B
Yeung S.M.C
Yin X
Yokoyama J
Yokozawa T
Yoo J
Yu H
Yuzurihara H
Zadrożny A
Zannelli A.J
Zanolin M
Zeeshan M
Zelenova T
Zendri J.-P
Zeoli M
Zerrad M
Zevin M
Zhang A.C
Zhang J
Zhang L
Zhang R
Zhang T
Zhang Y
Zhao C
Zhao Yue
Zhao Yuhang
Zheng Y
Zhong H
Zhong S
Zhou R
Zhu Z.-H
Zucker M.E
Zweizig J
Publication venue: HAL CCSD
Publication date: 23/04/2024
Field of study

International audienceAmong the various candidates for dark matter (DM), ultralight vector DM can be probed by laser interferometric gravitational wave detectors through the measurement of oscillating length changes in the arm cavities. In this context, KAGRA has a unique feature due to differing compositions of its mirrors, enhancing the signal of vector DM in the length change in the auxiliary channels. Here we present the result of a search for

U(1)_{B-L}

gauge boson DM using the KAGRA data from auxiliary length channels during the first joint observation run together with GEO600. By applying our search pipeline, which takes into account the stochastic nature of ultralight DM, upper bounds on the coupling strength between the

U(1)_{B-L}

gauge boson and ordinary matter are obtained for a range of DM masses. While our constraints are less stringent than those derived from previous experiments, this study demonstrates the applicability of our method to the lower-mass vector DM search, which is made difficult in this measurement by the short observation time compared to the auto-correlation time scale of DM