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Suffocating cancer: hypoxia-associated epimutations as targets for cancer therapy

Lower than normal levels of oxygen (hypoxia) is a hallmark of all solid tumours rendering them frequently resistant to both radiotherapy and chemotherapy regimes. Furthermore, tumour hypoxia and activation of the hypoxia inducible factor (HIF) transcriptional pathway is associated with poorer prognosis. Driven by both genetic and epigenetic changes, cancer cells do not only survive but thrive in hypoxic conditions. Detailed knowledge of these changes and their functional consequences is of great clinical utility and is already helping to determine phenotypic plasticity, histological tumour grading and overall prognosis and survival stratification in several cancer types. As epigenetic changes - contrary to genetic changes - are potentially reversible, they may prove to be potent therapeutic targets to add to the cancer physicians' armorarium in the future

Springer - Publisher Connector

arXiv.org e-Print Archive

UCL Discovery

Iron Behaving Badly: Inappropriate Iron Chelation as a Major Contributor to the Aetiology of Vascular and Other Progressive Inflammatory and Degenerative Diseases

Author: A Abbott
A Abou-Raya
A Aljandali
A Ambesi-Impiombato
A Aydin
A Balcerczyk
A Besarab
A Brzezinski
A Campbell
A Carrillo-Vico
A Cavalli
A Chattopadhyay
A Chattopadhyay
A Cherubini
A Dey
A Doms
A Donovan
A Donovan
A Dávalos
A Gaeta
A Garny
A Gnjec
A Gomes
A Gopalakrishnan
A Hald
A Henney
A Hirayama
A Hoffmann
A Huber
A Hugman
A Iannetti
A Ide-Ektessabi
A Jacobs
A Jeyabalan
A Kahvejian
A Karrar
A Kasztler
A Kibel
A Kocyigit
A Kotha
A Kumral
A Lass
A Lecube
A Lewén
A Lotery
A Maggio
A Malek
A Malik
A Mantovani
A Matsuzawa
A Mitra
A Monge
A Murakami
A Murakami
A Murakami
A Murakami
A Mutti
A Nijnik
A Nunomura
A Nunomura
A Patt
A Persson
A Pietrangelo
A Piga
A Pirat
A Post
A Pradhan
A Protti
A Rattner
A Ravati
A Rehman
A Reynolds
A Richmond
A Roetto
A Roetto
A Rostom
A Rumbold
A Russo
A Rötig
A Saltelli
A Saltelli
A Sandek
A Sassano
A Scalbert
A Scalbert
A Scalbert
A Sica
A Smahi
A Sola
A Stintzi
A Szewczyk
A Taguchi
A Tedgui
A Terman
A Terman
A Terman
A Undas
A Virdis
A Wagner
A Wagner
A Wagner
A Wagner
A Wojas-Pelc
A Wong
A Xu
A Yoritaka
A Yoshimura
A-L Barabási
AA Andreadis
AA Borisy
AA Farooqui
AA Qutub
AA Qutub
AA Vlessis
AB Nathens
AB Parsons
AB Parsons
AB Thompson
AB Thomson
AC Bayne
AC Bharti
AC Cave
AC Mello Filho
AD d'Hardemare
AD de Silva
Ad hoc committee on systemic lupus erythematosus response criteria for fatigue
ADL van der
AE Aust
AE Baue
AE Finefrock
AE Heazell
AE Heazell
AE Kartikasari
AEC Ihekwaba
AEC Ihekwaba
AF Tramontano
AH Berg
AH Koeppen
AH Koeppen
AH Tong
AI Bush
AI Bush
AI Bush
AI Bush
AI Faden
AJ Ghio
AJ Ghio
AJ Ghio
AJ Hulbert
AJ Kowaltowski
AJ Lusis
AJ Matthews
AJ Reyes
AJ van Oostrom
AJ Watson
AJ White
AJ Williams
AK Junk
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AL Hemdahl
AL Hopkins
AL Hopkins
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AL Mark
AL Sirén
AL Sirén
AL Sirén
AL Takeda
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AM Borzychowski
AM Choi
AM Dolga
AM Elneihoum
AM Elneihoum
AM Feist
AM Harvey
AM Jenkinson
AM Lin
AM Samuni
AM Snyder
AN Crowson
AN Tabah
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AP Breen
AP Liappis
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AR Kallianpur
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AR Ness
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AT McKie
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B Halliwell
B Halliwell
B Halliwell
B Halliwell
B Halliwell
B Halliwell
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B Pradines
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Publication venue
Publication date: 09/08/2008
Field of study

The production of peroxide and superoxide is an inevitable consequence of aerobic metabolism, and while these particular "reactive oxygen species" (ROSs) can exhibit a number of biological effects, they are not of themselves excessively reactive and thus they are not especially damaging at physiological concentrations. However, their reactions with poorly liganded iron species can lead to the catalytic production of the very reactive and dangerous hydroxyl radical, which is exceptionally damaging, and a major cause of chronic inflammation. We review the considerable and wide-ranging evidence for the involvement of this combination of (su)peroxide and poorly liganded iron in a large number of physiological and indeed pathological processes and inflammatory disorders, especially those involving the progressive degradation of cellular and organismal performance. These diseases share a great many similarities and thus might be considered to have a common cause (i.e. iron-catalysed free radical and especially hydroxyl radical generation). The studies reviewed include those focused on a series of cardiovascular, metabolic and neurological diseases, where iron can be found at the sites of plaques and lesions, as well as studies showing the significance of iron to aging and longevity. The effective chelation of iron by natural or synthetic ligands is thus of major physiological (and potentially therapeutic) importance. As systems properties, we need to recognise that physiological observables have multiple molecular causes, and studying them in isolation leads to inconsistent patterns of apparent causality when it is the simultaneous combination of multiple factors that is responsible. This explains, for instance, the decidedly mixed effects of antioxidants that have been observed, etc...Comment: 159 pages, including 9 Figs and 2184 reference

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Pan-cancer analysis of whole genomes

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The ICGC/TCGA Pan-Cancer Analysis of Whole Genomes Consortium View Correspondence (jump link)
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Zhang H. b
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zi zj
zm Jayaseelan
Zou
Zou
zt Kim
zw Lewis
Ó. A. th
Ø. sk
Publication venue
Publication date: 11/12/2019
Field of study

Cancer is driven by genetic change, and the advent of massively parallel sequencing has enabled systematic documentation of this variation at the whole-genome scale(1-3). Here we report the integrative analysis of 2,658 whole-cancer genomes and their matching normal tissues across 38 tumour types from the Pan-Cancer Analysis of Whole Genomes (PCAWG) Consortium of the International Cancer Genome Consortium (ICGC) and The Cancer Genome Atlas (TCGA). We describe the generation of the PCAWG resource, facilitated by international data sharing using compute clouds. On average, cancer genomes contained 4-5 driver mutations when combining coding and non-coding genomic elements; however, in around 5% of cases no drivers were identified, suggesting that cancer driver discovery is not yet complete. Chromothripsis, in which many clustered structural variants arise in a single catastrophic event, is frequently an early event in tumour evolution; in acral melanoma, for example, these events precede most somatic point mutations and affect several cancer-associated genes simultaneously. Cancers with abnormal telomere maintenance often originate from tissues with low replicative activity and show several mechanisms of preventing telomere attrition to critical levels. Common and rare germline variants affect patterns of somatic mutation, including point mutations, structural variants and somatic retrotransposition. A collection of papers from the PCAWG Consortium describes non-coding mutations that drive cancer beyond those in the TERT promoter(4); identifies new signatures of mutational processes that cause base substitutions, small insertions and deletions and structural variation(5,6); analyses timings and patterns of tumour evolution(7); describes the diverse transcriptional consequences of somatic mutation on splicing, expression levels, fusion genes and promoter activity(8,9); and evaluates a range of more-specialized features of cancer genomes(8,10-18).Peer reviewe

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International Consensus Statement on Rhinology and Allergy: Rhinosinusitis

Author: Aanaes K
Abadie WM
Abi Najm S
Abigail P
Abrahams JJ
Abrass LJ
Abreu CB
Abreu NA
Abshirini H
Abuzeid WM
Abuzeid WM
Achar P
Ackerhans M
Adam P
Adappa ND
Adappa ND
Adappa ND
Adappa ND
Adriaensen G
Agache I
Aghamohammadi A
Agius AM
Agyeman AA
Ahn CN
Ahn HJ
Ahn JC
Ahn SH
Ahovuo‐Saloranta A
Aitken M
Ajaiyeoba A
Akbari E
Akdis CA
Akira S
Akiyama K
Akiyama K
Akiyama K
Al Komser MK
Alam ES
Alandejani T
Alanin MC
Albritton FDT
Albu S
Albu S
Albu S
Aldini G
Alexander NS
Aljebab F
Alkire BC
Allen EK
Alobid I
Alobid I
Alobid I
Aloulah M
Alqudah M
Alromaih S
Alsaleh S
Alsharif S
Alt JA
Alt JA
Alt JA
Alt JA
Alt JA
Alves MP
Al‐Qudah M
Al‐Qudah M.
Al‐Qudah M.
Al‐Rawi MM
Al‐Shaikh S
Al‐Shemari H
Al‐Swiahb JN
Amali A
Amar YG
Amble FR
American Academy of Pediatrics Steering Committee on Quality Improvement and Management (AAP SCQIM)
Amin MR
Amine M
Amodu EJ
Anamika A
Anand V
Anderson DE
Anderson WC
Andhale S
Ankichetty SP
Annamalai S
Anon JB
Anselmo‐Lima WT
Antisdel JL
Antisdel JL
Antunes MB
Antunes MB
Anushiravani M
Anzai Y
Anzić SA
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Arild Danielsen K
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Chowdhury NI
Christensen DN
Christensen JM
Chu DK
Chung BJ
Chung SD
Church CA
Cirkovic I
Citardi MJ
Citardi MJ
Claeys S
Claeys S
Clarhed UKE
Clark DW
Clark NM
Clayman GL
Cleland EJ
Cleland EJ
Cleland EJ
Clement PA
Clinger JD
Clunes LA
Coates ML
Codispoti CD
Coey JG
Cohen NA
Cohen NA
Collins FS
Collins FS
Collins MM
Comert S
Conboy P
Conger BT
Conger BT
Conley DB
Cope EK
Copeland E
Cormier C
Cormier C
Cornelius RS
Cornet ME
Corradini C
Corriveau M‐N
Costa Carvalho BT
Costa ML
Costa ML
Costerton JW
Cottrell J
Craig JR
Craig JR.
Crawley BK
Criddle MW
Cronin MJ
Crosby DL
Cross JL
Crotty Alexander LE
Cryan JF
Cui XY
Cui YH
Cutler J
Cutler J
Cutting GR
Czerny MS
Côté DWJ
D'Anza B
Dabirmoghaddam P
Dahlen B
Dai Q
Dalgic A
Dalgorf DM
Dalm VA
Daramola OO
Darveaux J
Das A
Daudia AT
Dautremont JF
Davis GE
Dawson B
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De Boeck I
De Greve G
De Schryver E
De Schryver E
DeConde AS
DeConde AS
DeConde AS
DeConde AS
DeConde AS
DeConde AS
DeConde AS
DeConde AS
DeConde AS
DeConde AS
DeConde AS
Dejima K
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Delehaye E
Delemarre T
DelGaudio JM
DelGaudio JM
DelGaudio JM
DelGaudio JM
DelGaudio JM
Dellamonica P
DeMaria S
Demirhan A
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DeMuri GP
DeMuri GP
DeMuri GP
Den Beste KA
den Broek MF
Deng J
Denlinger LC
Derendorf H
Derry S
deShazo RD
Deshazo RD.
Desrosiers M
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Desrosiers MY
Detwiller KY
Deutsch PG
DeYoung K
Dhawale VS
Di Capite J
Di Cicco M
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DiBaise JK
Dietz CJ
Dietz de Loos D
Dietz de Loos DA
Dijkstra MD
Dilger AE
Dilidaer D
Dilokthornsakul P
Dingsor G
Divekar R
Divekar RD
Dixon AE
Dixon BJ
Djupesland PG
Djupesland PG
Djupesland PG
Do TQ
Dobzanski A
Doellman MS
Dogan M
Dolor RJ
Don DM
Dong D
Draf W
Drettner B
Druce HM
Du K
Dubin MG
Dubin MG
Dubin MG
Dubin MR
Duclos P
Dunbar J
Dunlop G
Durr ML
Dutta M
Dwyhalo KM
Dykewicz MS
Dykewicz MS
Ebbens FA
Ebbens FA
Ebell MH
Ebell MH
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Ebert CS
Ecevit MC
Eckhoff A
Ediriweera ER
Eggesbo HB.
Ehnhage A
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El Mograbi A
Elborn JS
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Eloy JA
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Eloy P
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El‐Shmaa NS
Emre IE
Endam LM
Endo Y
Erbek SS
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Error M
Esmaeilzadeh H
Esposito S
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Essaidi‐Laziosi M
Eviatar E
Eweiss AZ
Expert Panel on Neurologic I
Eyigor H
Ezzat W
Fabre C
Faghih Habibi A
Falagas ME
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Farag AA
Farrell PM
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Farzanegan B
Fastenberg JH
Feazel LM
Federspil PA
Feldman C
Ference EH
Ference EH
Ference EH
Ferguson BJ
Ferguson BJ
Ferguson BJ
Ferguson BJ
Ferguson JL
Fernandez IJ
Ferrara A
Filiaci F
Filiaci F
Flam JO
Fleissig E
Flyman S
Fokkens W
Fokkens WJ
Fokkens WJ
Fokkens WJ
Fokkens WJ
Fokkens WJ
Fong SA
Food Organization A, Organization WH
Foreman A
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Fortune DS
Forwith KD
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Fowler K
Fraczek M
Fraczek M. R‐NB
Frank DN
Frank S
Franklin JH
Freeman SB
Frenkiel S
Frerichs KA
Fried M
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Friedman M
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Fu T
Fujieda S
Fulde M
Furukawa CT.
Furukido K
Förster‐Ruhrmann U
Gabra N
Gabrielian ES
Gadkaree SK
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Galletti B
Gan EC
Gan EC
Gan EC
Gan W
Gantz O
Gao WX
Garbutt JM
Garcia‐Rodriguez L
Garzaro M
Gehanno P
Gehanno P
Gelardi M
Gelber JT
Gentile VG
Georgalas C
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Geramas I
Gerber ME
Gerlinger I
Gevaert E
Gevaert P
Gevaert P
Gevaert P
Gevaert P
Gevaert P
Gevorgyan A
Ghegan MD
Ghegan MD
Giacchi RJ
Giacchi RJ
Gibbons MD
Giger R
Gilani S
Giles WC
Gillespie MB
Gion Y
Giotakis AI
Giuseppe M
Glicksman JT
Gliklich RE
Gliklich RE
Gliklich RE
Glowacki R
Gluck O
Goggin R
Goggin R
Goggin RK
Goggin RK
Goh BS
Golebski K
Gomez‐Rivera F
Gosepath J
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Gould J
Govindaraj S
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Grant MC
Grauvogel TD
Gray ML
Grayson JW
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Griggs ZH
Grobler A
Gross ND
Grzegorzek T
Grzeskowiak B
Gudis D
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Guilemany JM
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Gunel C
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Guttenplan MD
Guven DG
Gwaltney JJ
Gwaltney JM
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Gyawali BR
Głobińska A
Ha T
Ha TN
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Habermann W
Hadfield P
Hadfield PJ
Hadrup N
Hafner B
Haidar YM
Hait EJ
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Halbeisen FS
Halderman A
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Hansen FS
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Hardcastle T
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Hartwig S
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Harvey R
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Hashiba M
Hassanzad M
Hathorn IF
Hauer AJ
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Hauser LJ
Hauser LJ
Havas TE
Havel M
Haxel BR
Hayashi H
Hayes SM
Hays GC
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Heatley DG
Heaton CM
Hedman J
Heffler E
Hekiert AM
Hellings PW
Henmyr V
Henriquez OA
Hepworth E
Hermelingmeier KE
Hessler JL
Heymann PW
Hickner JM
Higashizawa T
Higgins Jr TS
Hilding AC.
Hintschich CA
Hirabayashi KE
Hirsch AG
Hirsch AG
Hirsch SD
Hirschberg A
Hirshoren N
Hissaria P
Ho J
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Hobson CE
Hoehle LP
Hoehle LP
Hoffmans R
Hofstra J
Hoggard M
Hoggard M
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Holcomb SS
Holmberg K
Holmstrom M
Holopainen E
Holy CE
Holzmann D
Hong HY
Hopkins C
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Hopkins C
Hopkins C
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Hopkins C
Hopkins C
Hopkins C
Hopkins C
Hopkins C AP
Hopkins C.
Horby P
Hosemann W
House LK
Houser SM
Howard BE
Howitt MR
Hox V
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Hoyle BD
Hoyt AE
Hoza J
Hsu CC
Hsu CL
Hsueh WD
Huang A
Huang SW
Huang WH
Huang Z
Huang Z
Huang Z
Huang Z
Huang Z
Huang ZZ
Huart C
Huck W
Hudon MA
Hueston WJ
Humphreys IM
Hunter B
Hunter E
Hunter TD
Husain Q
Hutcheson PS
Huttenhower C
Huvenne W
Hwang JW
Hwang PH
Hwang PH
Hwang PH
Hwang PH
Hwang SH
Hyo N
Ibrahim C
Iinuma T
Ikeda K
Ikeda K
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Ilhan AE
Illing EA
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Inanli S
Ingals EE
Iqbal IZ
Isaacs S
Itayem DA
Jackman AH
Jackson DJ
Jafari A
Jafari A
Jaffé A
Jain R
Jain R
Jain R
Jain R
Jain R
Jakobsson HE
Jamee M
Jameson M
Jang DW
Jang YJ
Jankowski R
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Jankowski R
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Jannert M
Jardeleza C
Jarvis D
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Jecker P
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Jen A
Jeney E
Jervis‐Bardy J
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Ji K
Jian L
Jiang RS
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Jiao J
Jiramongkolchai P
Joe SA
Johansson L
Johansson L
Jones NS
Jorissen M
Josephson GD
Joss TV
Jousimies‐Somer HR
Jung JH
Jung MS
Justice JM
Kakish KS
Kalaiarasi R
Kaldenbach T
Kalish L
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Kamen DL
Kamijyo A
Kanis JA
Kanjanaumporn J
Kanjanawasee D
Kanthakumar K
Kao SS
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Kaper NM
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Kaplan A
Karaaslan K
Karabayirli S
Karanfilov B
Karanth TK
Karawajczyk M
Karempelis P
Kari E
Karjalainen J
Karlsson G
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Karosi T
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Kashani S
Kasle DA
Kastl KG
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Kaszuba SM
Katle E‐J
Kato A
Kato K
Katsuta S
Kawai T
Kaya M
Kazak Z
Keith P
Keith PK
Keith PK
Keles GT
Kelly EA
Kemppainen T
Kemppainen TP
Kennedy DW
Kennedy DW
Kennedy DW
Kennedy DW
Kennedy DW
Kennedy DW
Kennedy DW
Kennedy JL
Kern RC
Kern RC
Kesimci E
Keswani A
Khalfoun S
Khalid AN
Khalid AN
Khalid AN
Khalil Y
Khalmuratova R
Khan A
Khan A
Khan AR
Khan MM
Khanwalkar AR
Khlifi R
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Khojastepour L
Khokar A
Khwaja S
Kidoguchi M
Kidwai S
Kieff DA
Kilty SJ
Kilty SJ
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Kilty SJ
Kim AS
Kim DH
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Kim DK
Kim DK
Kim DW
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Kim H
Kim HY
Kim JH
Kim JH
Kim JS
Kim JY
Kim J‐Y
Kim SH
Kim SH
Kim SH
Kim SJ
Kim ST
Kim ST
Kim SW
Kimmelman CP
King D
King JM
Kinsella JB
Kiris M
Kirsch CF
Kirtsreesakul V
Kirtsreesakul V
Kitagawa K
Kitz R
Klimek L
Klimek L
Kloepfer KM
Klossek J
Klossek JM
Klossek JM
Kluytmans J
Knott PD
Knott PD
Knowles MR
Ko MT
Kobayashi Y
Koch AK
Koch RM
Kofonow JM
Kohanski MA
Kohanski MA
Kohanski MA
Kohanski MA
Kohli P
Kolia NR
Kong IG
Kong IG
Konstantinidis I
Konstantinidis I
Korkmaz H
Koskinen A
Koteswara CM
Kounis NG
Koutsourelakis I
Kouzaki H
Kouzaki H
Kowalski ML
Kowalski ML
Krause HF
Kreindler JL
Kreindler JL
Krings JG
Kristin J
Kristjansson RP
Krivan G
Kroflic B
Krzeski A
Kuehnemund M
Kuiper JR
Kumar G
Kupferberg SB
Kuruvilla M
Labadie RF
Lacroix JS
Lacroix JS
Lacroix JS
Lai X
Lai Y
Laidlaw TM
Laidlaw TM
Laidlaw TM
Lal D
Lal D
Lal D
Lal D
Lal D
Lal D
Lam DH
Lam K
Lam M
Lam M
Lam WW
Lamblin C
LaMear WR
Lan F
Lanas A
Landry ML
Lane AP
Lang D
Langille M
Lanza DC
Lanza DC
Larivée N
Larsen K
Larsen KL
Larsen PL
Larsen PL
Lasso A
Laury AM
Lavigne F
Lavigne F
Lazar RH
Le Bon SD
Le PT
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Leason SR
Lechien JR
Lechien JR
Lechien JR
Lechien JR
Lechien JR
LeConte B
Lee HM
Lee IT
Lee J
Lee JM
Lee JM
Lee JS
Lee JT
Lee JT
Lee JT
Lee JT
Lee JY
Lee JY
Lee LN
Lee RJ
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Lee RJ
Lee RJ
Lee S
Lee SB
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Lee VS
Lee VS
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Legent F
Lehmann AE
Lehrer E
Leiman D
Lemiengre MB
Lemiengre MB
Lennard CM
Leo G
Leo G
Leo G
Leonard CG
Leonard DW
Leong JL
Leong JL
Leopold DA
Leung M‐K
Leung N
Leung R
Leung R
Leung R
Leung R
Leung RM
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Levetan CS
Levin TA
Levine SB
Levy JM
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Lewis K.
Leykin Y
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Li C
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Li CW
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Li J
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Liang J
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Lill C
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Lima JT
Lin DC
Lin J
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Lin L
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Lindbaek M
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Lindstrom DR
Little M
Little P
Litvack JR
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Liu CM
Liu CM
Liu J
Liu YF
Lloyd CM
Lobo BC
Loehrl TA
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Loftus CA
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Lombardi A
London NR
Longhini AB
Loo JL
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Losol P
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Louie JK
Low PM
Lowery AS
Lu J
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Lucuab‐Fegurgur DL
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Mace J
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Mainz JG
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Maitra S
Majima Y
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Makary CA
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Malik Z
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Marchica P
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Marple BF
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Marseglia GL
Marshall AH
Martinez‐Anton A
Marty FM
Marzban S
Maskell S
Mastalerz L
Masterson L
Masterson L
Matheny KE
Matsune S
Matsuno O
Matsuwaki Y
Mattos JL
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Maxfield AZ
May A
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Mazza JM
McAlister WH
McCormick J
McDonald VM
McErlean P
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McKinley SH
McMains KC
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McNally PA
McQuillan L
Mehan R VL
Melen I
Melroy C
Meltzer EO
Meltzer EO
Meltzer EO
Meltzer EO
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Melvin TA
Mendelsohn D
Menni C
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Merkley MA
Messerklinger W
Metson R
Metson R
Metson R
Mfuna EL
Mfuna Endam L
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Middleton PG
Miglani A
Miljkovic D
Miller AJ
Miller JD
Miller RS
Miller TR
Millien VO
Miloshev B
Min YG
Miraglia MDG
Mitchell E
Mitson‐Salazar A
Miłoński J
Mjösberg JM
Mo JH
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Mohapatra SSG
Moher D
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Moltke J
Mont MA
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Morawska L
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Morinaka S
Morita H
Moriyama H
Morrissey DK
Morrissey DK
Mortazavi N
Mortimore S
Mortuaire G
Mortuaire G
Mosges R
Moshaver A
Moss RB
Mostafa BE
Mostafa BE
Mostafa BED
Mozzanica F
Mrowka‐Kata K
Mueller SA
Mueller SK
Mueller SK
Mukerji SS
Mukherji SK
Mulligan JK
Mulligan JK
Mulligan JK
Mullol J
Mullol J
Munoz del Castillo F
Murphy J
Murr AH
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Musy PY
Mygind N
Mygind N
Myller J
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Nagata Y
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Namyslowski G
Nanayakkara JP
Nandapalan V
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Nayan S
Neher A
Neubauer PD
Neumark T
Newberry CI
Newton E
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Nguyen BK
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Nicolai P
Nimsakul S
Nino G
Ninomiya T
Nisa L
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Oakley GM
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Ocampo CJ
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Olson G
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Ooi EH
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Ooi ML
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Orb Q
Ordovas‐Montanes J
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Organization WH
Orlandi R
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Orlandi RR
Orlandi RR
Orlandi RR
Orlandi RR
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Orlandi RR
Ostovar A
Ou J
Ow R
Oyer SL
Ozdek A
Ozer AB
Ozkara S
Ozmen S
Ozturan A
Ozturk F
Paderno A
Palmer JN
Pang YT
Pant H
Pant H
Papagiannopoulos P
Papagiannopoulos P
Paramasivan S
Parasher AK
Parida PK
Parikh A
Parikh A
Parikh AA
Parikh SL
Parikh SR
Paris G.
Park D‐Y
Park M
Park SK
Park SK
Park SK
Park SM
Parma V
Parsek MR
Pasaje CF
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Passali D
Passali D
Passali D
Passàli D
Passàli D
Passàli D
Patel NA
Patel NN
Patel VS
Patel ZM
Patel ZM
Patou J
Patro SK
Pauli C
Pavlin JD
Payne SC
Payne SJ
Pearlman AN
Pearlman AN
Peng Y
Peng Y
Penttila M
Perez‐Novo CA
Peric A
Peric A
Perica A
Perić A
Perkasa MF
Perloff JR
Persson EK
Peters AT
Peña MT
Pfaar O
Pfaar O
Pfaar O
Pham V
Phillips KM
Phillips KM
Phillips KM
Phillips KM
Phillips KM
Phillips KM
Phillips KM
Philpott C
Philpott CM
Picado C
Piccirillo JF
Piccirillo JF
Pimenta F
Pincus RL
Pinther S
Pinto Bezerra Soter AC
Pinto JM
Pinto JM
Pipolo C
Plebani A
Plonk DP
Poachanukoon O
Poetker DM
Poetker DM
Poetker DM
Poetker DM
Poletti SC
Ponikau JU
Ponikau JU
Ponikau JU
Ponikau JU
Porter PC
Pothoven KL
Prajapati DP
Prickett KK
Prince AA
Principi N
Promsopa C
Psaltis AJ
Psaltis AJ
Pumhirun P
Pundir V
Pundir V
Purcell PL
Purkey MT
Purnell PR
Pynnonen M
Pynnonen MA
Pynnonen MA
Qualliotine JR
Quintanilla‐Dieck L
Quinti I
Qvarnberg Y
Rabago D
Rabago D
Rabbe R
Rachelefsky GS
Rachelefsky GS
Ragab A
Ragab A
Ragab S
Ragab S
Ragab SM
Raghunandhan S
Rahbar R
Rai G
Rains BM
Rains BM
Raithatha R
Rajan JP
Rajiv S
Ramadan HH
Ramadan HH
Ramadan HH
Ramadan HH.
Ramadan HH.
Ramakrishnan V
Ramakrishnan VR
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Ramanathan M
Ramanathan M
Ramanathan M
Ramanathan M
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Rameau A
Ramonell RP
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Ricciardolo FLM
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Richter JE
Rickert S
Riley CA
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Rogers GA
Roifman CM
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Rojita M
Roland LT
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Rom D
Roman RA
Rombaux P
Rondón C
Rosbe KW
Rose MA
Rosen PL
Rosenfeld RM
Rosenfeld RM
Rosenfeld RM
Rostkowska‐Nadolska B
Rostkowska‐Nadolska B
Rostkowska‐Nadolska BLM
Rotenberg BW
Roth M
Rowan NR
Rowan NR
Rowan NR
Rowe SM
Rowe‐Jones JM
Roxbury CR
Rozsasi A
Rudack C
Rudmik L
Rudmik L
Rudmik L
Rudmik L
Rudmik L
Rudmik L
Rudmik L
Rudmik L
Rudmik L
Rudmik L
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Rudmik L
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Rudmik L
Rudmik L
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Ziegler CGK
Zielinska‐Blizniewska H
Zou L
Zuckerman JD
Zurlo JJ
Zuskin E
Čulig J
Publication venue: 'Wiley'
Publication date: 01/01/2021
Field of study

Background: The 5 years since the publication of the first International Consensus Statement on Allergy and Rhinology: Rhinosinusitis (ICAR‐RS) has witnessed foundational progress in our understanding and treatment of rhinologic disease. These advances are reflected within the more than 40 new topics covered within the ICAR‐RS‐2021 as well as updates to the original 140 topics. This executive summary consolidates the evidence‐based findings of the document. Methods: ICAR‐RS presents over 180 topics in the forms of evidence‐based reviews with recommendations (EBRRs), evidence‐based reviews, and literature reviews. The highest grade structured recommendations of the EBRR sections are summarized in this executive summary. Results: ICAR‐RS‐2021 covers 22 topics regarding the medical management of RS, which are grade A/B and are presented in the executive summary. Additionally, 4 topics regarding the surgical management of RS are grade A/B and are presented in the executive summary. Finally, a comprehensive evidence‐based management algorithm is provided. Conclusion: This ICAR‐RS‐2021 executive summary provides a compilation of the evidence‐based recommendations for medical and surgical treatment of the most common forms of RS

Ghent University Academic Bibliography

University of East Anglia digital repository

Body mass index, effect modifiers, and risk of pancreatic cancer: a pooled study of seven prospective cohorts

Author: A Ansary-Moghaddam
A Berrington de Gonzalez
A Berrington de Gonzalez
A Hofstetter
A Jessen
AD Rosenthal
AG Renehan
Amy Berrington de Gonzalez
Arthur Schatzkin
AV Patel
BA Calton
BT Ji
Bu-tian Ji
C Samanic
CA Eberle
Cari L. Meinhold
Catherine Schairer
D Li
D Spiegelman
D. Michal Freedman
Demetrius Albanes
DM Freedman
DS Michaud
DS Michaud
DS Michaud
EE Calle
EE Calle
F Wang
H Nawaz
H Obana
J Luo
J Luo
Jane A. Hoppin
Jarmo Virtamo
JD Boice Jr
JP Fryzek
JP Higgins
L Jiao
Laura E. Beane Freeman
Li Jiao
LN Anderson
M Wang
Martha S. Linet
MF Kuczmarski
Michael C. R. Alavanja
Michael F. Leitzmann
Mitchell H. Gail
Patricia Hartge
R DerSimonian
R Kaaks
Rachael Z. Stolzenberg-Solomon
RF Gillum
Richard B. Hayes
Ruth M. Pfeiffer
RZ Stolzenberg-Solomon
RZ Stolzenberg-Solomon
RZ Stolzenberg-Solomon
RZ Stolzenberg-Solomon
RZ Stolzenberg-Solomon
S Koutros
SA Smith-Warner
SC Gorber
SC Larsson
SC Larsson
SM Gapstur
SO Olusi
Stephanie J. Weinstein
SY Pan
T Ronnemaa
The ATBC Cancer Prevention Study Group
U Nothlings
W Zheng
Wei Zheng
Wen-Yi Huang
Wong-Ho Chow
Y Lin
Yikyung Park
Publication venue
Publication date: 01/01/2010
Field of study

Public Library of Science (PLOS)

Julkari

Vitamin D metabolic pathway genes and pancreatic cancer risk

Author: AC Ross
AE Millen
Alan A. Arslan
Alison Klein
Anne Zeleniuch-Jacquotte
Aruna Kamineni
Brian Henderson
C Moore
D Berry
D Campa
Demetrius Albanes
Dennis Maeder
Donghui Li
Elizabeth A. Holly
Emily White
Eric J. Duell
Eric J. Jacobs
Eric Klein
Federico Canzian
FP Boscoe
Geoffrey S. Tobias
Gianluca Severi
Gloria M. Petersen
GM Petersen
GM Zinser
Graham G. Giles
Hannah Arem
Harvey Risch
Herbert Yu
Irene Orlow
J Ahn
Jeffrey S Chang
Joshua N. Sampson
K Yu
Kai Yu
Kala Visvanathan
Kathy Helzlsouer
KJ Helzlsouer
KK Deeb
Kristin Moy
L Amundadottir
L Jiao
Laura Beane-Freeman
Laurence N. Kolonel
LN Anderson
M Kanemaru
M Porta
Manal Hassan
Marjorie L. McCullough
Melissa Austin
Michael Goggins
Michelle Brotzman
Michelle Cotterchio
Miquel Porta
Neal D. Freedman
Núria Malats
Paige Bracci
Patricia Hartge
Phyllis J. Goodman
Rachael Z. Stolzenberg-Solomon
Robert Hoover
RZ Stolzenberg-Solomon
RZ Stolzenberg-Solomon
S Kinoshita
Sara H. Olson
Satu Männistö
Steve Gallinger
Susan T. Mayne
T Mizoue
TJ Wang
Ulrike Peters
WB Grant
WB Grant
Wei Zheng
William R. Bamlet
Xiao-Ou Shu
Xiaoqin Xiong
Y Bao
Y Lin
Publication venue: 'Public Library of Science (PLoS)'
Publication date: 01/01/2015
Field of study

Evidence on the association between vitamin D status and pancreatic cancer risk is inconsistent. This inconsistency may be partially attributable to variation in vitamin D regulating genes. We selected 11 vitamin D-related genes (GC, DHCR7, CYP2R1, VDR, CYP27B1, CYP24A1, CYP27A1, RXRA, CRP2, CASR and CUBN) totaling 213 single nucleotide polymorphisms (SNPs), and examined associations with pancreatic adenocarcinoma. Our study included 3,583 pancreatic cancer cases and 7,053 controls from the genome-wide association studies of pancreatic cancer PanScans-I-III. We used the Adaptive Joint Test and the Adaptive Rank Truncated Product statistic for pathway and gene analyses, and unconditional logistic regression for SNP analyses, adjusting for age, sex, study and population stratification. We examined effect modification by circulating vitamin D concentration (≤50, >50 nmol/L) for the most significant SNPs using a subset of cohort cases (n = 713) and controls (n = 878). The vitamin D metabolic pathway was not associated with pancreatic cancer risk (p = 0.830). Of the individual genes, none were associated with pancreatic cancer risk at a significance level of p<0.05. SNPs near the VDR (rs2239186), LRP2 (rs4668123), CYP24A1 (rs2762932), GC (rs2282679), and CUBN (rs1810205) genes were the top SNPs associated with pancreatic cancer (p-values 0.008-0.037), but none were statistically significant after adjusting for multiple comparisons. Associations between these SNPs and pancreatic cancer were not modified by circulating concentrations of vitamin D. These findings do not support an association between vitamin D-related genes and pancreatic cancer risk. Future research should explore other pathways through which vitamin D status might be associated with pancreatic cancer risk.This project has been funded in whole or in part with federal funds from the National Cancer Institute, National Institutes of Health, under Contract No. HHSN261200800001E

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