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Pan-cancer analysis of whole genomes

Author: A. -L. rv
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The ICGC/TCGA Pan-Cancer Analysis of Whole Genomes Consortium View Correspondence (jump link)
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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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First Measurement of the Hubble Constant from a Dark Standard Siren using the Dark Energy Survey Galaxies and the LIGO/Virgo Binary-Black-hole Merger GW170814

Author: Abbott BP
Abbott R
Abbott TD
Abbott TMC
Abdalla FB
Abraham S
Acernese F
Ackley K
Adams C
Adhikari RX
Adya VB
Affeldt C
Agathos M
Agatsuma K
Aggarwal N
Aguiar OD
Aiello L
Ain A
Ajith P
Allam S
Allen G
Allocca A
Aloy MA
Altin PA
Amato A
Ananyeva A
Anderson SB
Anderson WG
Angelova S
Annis J
Appert S
Arai K
Araya MC
Areeda JS
Arene M
Ascenzi S
Ashton G
Aston SM
Astone P
Aubin F
Aufmuth P
AultONeal K
Austin C
Avendano V
Avila S
Avila-Alvarez A
Babak S
Bacon P
Badaracco F
Bader MKM
Bae S
Baker PT
Baldaccini F
Ballardin G
Ballmer SW
Banagiri S
Barayoga JC
Barclay SE
Barish BC
Barker D
Barkett K
Barnum S
Barone F
Barr B
Barsotti L
Barsuglia M
Barta D
Bartlett J
Bartos I
Bassiri R
Basti A
Bawaj M
Bayley JC
Bazzan M
Bechtol K
Becsy B
Bejger M
Bell AS
Beniwal D
Berger E
Bergmann G
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Zimmerman A
Zucker ME
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Zweizig J
Publication venue: IOP PUBLISHING LTD
Publication date: 01/05/2019
Field of study

We present a multi-messenger measurement of the Hubble constant H 0 using the binary–black-hole merger GW170814 as a standard siren, combined with a photometric redshift catalog from the Dark Energy Survey (DES). The luminosity distance is obtained from the gravitational wave signal detected by the Laser Interferometer Gravitational-Wave Observatory (LIGO)/Virgo Collaboration (LVC) on 2017 August 14, and the redshift information is provided by the DES Year 3 data. Black hole mergers such as GW170814 are expected to lack bright electromagnetic emission to uniquely identify their host galaxies and build an object-by-object Hubble diagram. However, they are suitable for a statistical measurement, provided that a galaxy catalog of adequate depth and redshift completion is available. Here we present the first Hubble parameter measurement using a black hole merger. Our analysis results in

{H}_{0}={75}_{-32}^{+40}\,\mathrm{km}\,{{\rm{s}}}^{-1}\,{\mathrm{Mpc}}^{-1}

, which is consistent with both SN Ia and cosmic microwave background measurements of the Hubble constant. The quoted 68% credible region comprises 60% of the uniform prior range [20, 140] km s−1 Mpc−1, and it depends on the assumed prior range. If we take a broader prior of [10, 220] km s−1 Mpc−1, we find {H}_{0 {78}_{-24}^{+96}\,\mathrm{km}\,{{\rm{s}}}^{-1}\,{\mathrm{Mpc}}^{-1} (57% of the prior range). Although a weak constraint on the Hubble constant from a single event is expected using the dark siren method, a multifold increase in the LVC event rate is anticipated in the coming years and combinations of many sirens will lead to improved constraints on H 0

UCL Discovery

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
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Anzai Y
Anzić SA
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Arden KE
Arild Danielsen K
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Arslan HH
Asaka D
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Atighechi S
Atlas SJ
Au J
Aukema AA
Aurora R
Autio TJ
Autio TJ
Autio TJ
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Balikci HH
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Bhandarkar ND
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Bhatt JM
Bhattacharjee S
Bhattacharyya N
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Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
Bhattacharyya N
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Bhattacharyya N.
Bhattacharyya N.
Bhawana G
Bidder T
Biedlingmaier JF
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Biel MA
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Bilge T
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Blackwell DL
Blackwell KE
Blair C
Bleier BS
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Blount A
Boase S
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Bockmühl U
Boezaart AP
Bohman A
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Bohnhorst I
Boita MM
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Bomeli SR
Bondioni MP
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Bonnomet A
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Bosse Y
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Brandsted R
Braun JJ
Braun JJ
Braunstahl GJ
Braverman I
Brescia G
Brescia G
Brietzke SE
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Brodner D
Brook I
Brook I
Brook I
Brook I
Brook I.
Brook I.
Bross‐Soriano D
Brot C
Brown CL
Brown S
Brozek JL
Brozek JL
Brumund KT
Brunner JP
Buckley CE
Buehring I
Bugten V
Bukowy‐Bieryllo Z
Burgstaller JM
Burton BN
Bush A
Businco LD
Buysschaert ID
Byun JY
Cahill KN
Cai Y
Calhoun KH
Calixto NE
Callejas CA
Campbell AP
Campbell AP
Campbell RG
Campbell RG.
Candoni A
Cannady SB
Cannoni M
Canonica GW
Cantrell H.
Cao PP
Cao P‐P
Cao Y
Cao Y
Carlson‐Jones JA
Carlton DA
Carney AS
Carr TF
Carr TF
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Carroll WW
Carroll WW
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Casale M
Cassandro E
Castano R
Castelnuovo P
Castelnuovo P
Castro M
Catalano P
Catalano PJ
Catalano PJ
Caughey RJ
Caulley L
Cazzola M
Cekic B
Ceri H
Cervin A
Cervin A
Chaaban MR
Chaaban MR
Chaaban MR
Chakrabarti A
Chakrabarti A
Chalermwatanachai T
Chalton R
Chambers DW
Chan CL
Chan DK
Chan KO
Chan Y
Chandler JR
Chandra RK
Chandra RK
Chandra RK
Chandra RK
Chandy Z
Chang CC
Chang CC
Chang EH
Chang EH
Chang EH
Chang HS
Chang MT
Chang MT
Chang MT
Chang Y‐S
Chaudhary N
Che C
Chee L
Chen B
Chen B
Chen CF
Chen F
Chen FH
Chen H
Chen J‐B
Chen PH
Chen X
Chen YT
Cheng YK
Cheon YI
Chester AC
Chester AC
Chester AC
Chiarella SE
Chiesa‐Estomba CM
Chin D
Chinratanapisit S
Chiu A
Chiu AG
Chiu AG
Chiu AG
Cho DY
Cho DY
Cho DY
Cho DY
Cho DY
Cho DY
Cho DY
Cho DY
Cho DY
Cho GS
Cho HJ
Cho JH
Cho K
Cho KS
Cho KS
Cho SH
Cho SH
Cho SH
Chobillon MA
Choby G
Choby GW
Choi EB
Choi JH
Chong LY
Chong LY
Chong LY
Chow AW
Chowdhury NI
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
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Dalgorf DM
Dalm VA
Daramola OO
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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
Dejima K
Delehaye E
Delemarre T
DelGaudio JM
DelGaudio JM
DelGaudio JM
DelGaudio JM
DelGaudio JM
Dellamonica P
DeMaria S
Demirhan A
Demirhan A
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
Desrosiers M
Desrosiers M
Desrosiers M
Desrosiers MY
Detwiller KY
Deutsch PG
DeYoung K
Dhawale VS
Di Capite J
Di Cicco M
DiBaise JK
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
Eberhart LH
Ebert CS
Ecevit MC
Eckhoff A
Ediriweera ER
Eggesbo HB.
Ehnhage A
Ehnhage A
El Mograbi A
Elborn JS
Elhakim M
Eliashar R
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Eloy JA
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Eloy JA
Eloy P
Eluecque H
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El‐Hennawi DM
El‐Shmaa NS
Emre IE
Endam LM
Endo Y
Erbek SS
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Ernst FR
Error M
Esmaeilzadeh H
Esposito S
Esposito S
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
Farzal Z
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
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Fong SA
Food Organization A, Organization WH
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Furukido K
Förster‐Ruhrmann U
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Gabrielian ES
Gadkaree SK
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Galletti B
Gan EC
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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
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Gluck O
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Grzegorzek T
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Gyawali BR
Głobińska A
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Hadfield P
Hadfield PJ
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Haidar YM
Hait EJ
Hakansson K
Halbeisen FS
Halderman A
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Hansen JG
Hansen JG
Hansen JG
Hansen JG
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Harvey R
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Hassanzad M
Hathorn IF
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Hauptman G
Hauser LJ
Hauser LJ
Havas TE
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Hayashi H
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Heaton CM
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Heffler E
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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
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Hobson CE
Hoehle LP
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Hong HY
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Hopkins C
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Hopkins C
Hopkins C AP
Hopkins C.
Horby P
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House LK
Houser SM
Howard BE
Howitt MR
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Hoyle BD
Hoyt AE
Hoza J
Hsu CC
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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
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Hwang PH
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Iqbal IZ
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Jafari A
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Jakobsson HE
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Jameson M
Jang DW
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Jiramongkolchai P
Joe SA
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Jones NS
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Josephson GD
Joss TV
Jousimies‐Somer HR
Jung JH
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Kaldenbach T
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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

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