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2 research outputs found

Mitochondrial genetic diversity, selection and recombination in a canine transmissible cancer.

Author: Airikkala-Otter Ilona
Allen Janice L
Allum Karen M
Bansse-Issa Leontine
Bisson Jocelyn L
Castillo Domracheva Artemio
Corrigan Anne M
Cran Hugh R
Crawford Jane T
Cutter Stephen M
de Castro Karina F
De Nardi Andrigo B
de Vos Anna P
de Vos Johan P
Delgadillo Keenan Laura
Donelan Edward M
Faramade Ibikunle A
Flores Reynoso Erika
Fotopoulou Eleni
Fruean Skye N
Gallardo-Arrieta Fanny
Glebova Olga
Henriques Joaquim Jgp
Häfelin Manrique Rodrigo F
Ignatenko Natalia
Koenig Debbie
Lanza-Perea Marta
Lobetti Remo
Lopez Quintana Adriana M
Losfelt Thibault
Marino Gabriele
Martincorena Inigo
Martínez Castañeda Simón
Martínez-López Mayra F
Meyer Michael
Murchison Elizabeth P
Nakanwagi Berna
Neunzig Winifred
Nixon Sally J
Ní Leathlobhair Máire
Onsare Marsden M
Ortega-Pacheco Antonio
Peleteiro Maria C
Pye Ruth J
Reece John F
Rojas Gutierrez Jose
Sadia Haleema
Schmeling Sheila K
Shamanova Olga
Ssuna Richard K
Steenland-Smit Audrey E
Strakova Andrea
Svitich Alla
Thoya Ngoka Ismail
van der Wel Mirjam G
Vițălaru Bogdan A
Walkinton Oliver
Wang Guo-Dong
Wedge David C
Wehrle-Martinez Alvaro S
Widdowson Sophie Ae
Yin Ting-Ting
Publication venue: 'eLife Sciences Publications, Ltd'
Publication date: 01/01/2016
Field of study

Canine transmissible venereal tumour (CTVT) is a clonally transmissible cancer that originated approximately 11,000 years ago and affects dogs worldwide. Despite the clonal origin of the CTVT nuclear genome, CTVT mitochondrial genomes (mtDNAs) have been acquired by periodic capture from transient hosts. We sequenced 449 complete mtDNAs from a global population of CTVTs, and show that mtDNA horizontal transfer has occurred at least five times, delineating five tumour clades whose distributions track two millennia of dog global migration. Negative selection has operated to prevent accumulation of deleterious mutations in captured mtDNA, and recombination has caused occasional mtDNA re-assortment. These findings implicate functional mtDNA as a driver of CTVT global metastatic spread, further highlighting the important role of mtDNA in cancer evolution.Wellcome Trust Investigator Award, 102942/Z/13/A Elizabeth P Murchison Leverhulme Trust Philip Leverhulme Prize Elizabeth P Murchison Royal Society Research Grant, RG130615 Elizabeth P Murchiso

LAReferencia - Red Federada de Repositorios Institucionales de Publicaciones Científicas Latinoamericanas

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PubMed Central

Apollo (Cambridge)

Open Access Repository

Recurrent horizontal transfer identifies mitochondrial positive selection in a transmissible cancer

Author: Airikkala-Otter Ilona
Allen Janice L.
Allum Karen M.
Arnold Clara L.
Baez-Ortega Adrian
Bansse-Issa Leontine
Bhutia Thinlay N.
Bisson Jocelyn L.
Blank Kelli
Bolton Isobelle A. G.
Briceño Cristóbal
Castillo Domracheva Artemio
Chinnery Patrick F.
Corrigan Anne M.
Cran Hugh R.
Crawford Jane T.
Cutter Stephen M.
Davis Eric
de Castro Karina F.
De Nardi Andrigo B.
de Vos Anna P.
Delgadillo Keenan Laura
Donelan Edward M.
Espinoza Huerta Adela R.
Falkenberg Maria
Faramade Ibikunle A.
Fazil Mohammed
Fotopoulou Eleni
Fruean Skye N.
Gallardo-Arrieta Fanny
Glebova Olga
Gori Kevin
Gouletsou Pagona G.
Gustafsson Claes M.
Henriques Joaquim J. G. P.
Horta Rodrigo S.
Hughes Katherine
Häfelin Manrique Rodrigo F.
Ignatenko Natalia
Kane Yaghouba
King Cathy
Koenig Debbie
Krupa Ada
Kruzeniski Steven J.
Lanza-Perea Marta
Lazyan Mihran
Lopez Quintana Adriana M.
Losfelt Thibault
Marino Gabriele
Martínez Castañeda Simón
Martínez-López Mayra F.
Masuruli Bedan M.
Meyer Michael
Migneco Edward J.
Murchison Elizabeth P.
Nakanwagi Berna
Neal Karter B.
Neunzig Winifred
Nicholls Thomas J.
Nixon Sally J.
Ní Leathlobhair Máire
Ortega-Pacheco Antonio
Pedraza-Ordoñez Francisco
Peleteiro Maria C.
Polak Katherine
Pye Ruth J.
Ramirez-Ante Juan C.
Reece John F.
Rojas Gutierrez Jose
Sadia Haleema
Sampson Alexander T.
Schmeling Sheila K.
Shamanova Olga
Sherlock Alan G.
Steenland-Smit Audrey E.
Strakova Andrea
Svitich Alla
Tapia Martínez Lester J.
Thoya Ngoka Ismail
Torres Cristian G.
Tudor Elizabeth M.
van der Wel Mirjam G.
Vițălaru Bogdan A.
Vural Sevil A.
Walkinton Oliver
Wang Jinhong
Wehrle-Martinez Alvaro S.
Widdowson Sophie A. E.
Zvarich Irina
Publication venue: Nature Communications
Publication date: 01/01/2020
Field of study

Abstract: Autonomous replication and segregation of mitochondrial DNA (mtDNA) creates the potential for evolutionary conflict driven by emergence of haplotypes under positive selection for ‘selfish’ traits, such as replicative advantage. However, few cases of this phenomenon arising within natural populations have been described. Here, we survey the frequency of mtDNA horizontal transfer within the canine transmissible venereal tumour (CTVT), a contagious cancer clone that occasionally acquires mtDNA from its hosts. Remarkably, one canine mtDNA haplotype, A1d1a, has repeatedly and recently colonised CTVT cells, recurrently replacing incumbent CTVT haplotypes. An A1d1a control region polymorphism predicted to influence transcription is fixed in the products of an A1d1a recombination event and occurs somatically on other CTVT mtDNA backgrounds. We present a model whereby ‘selfish’ positive selection acting on a regulatory variant drives repeated fixation of A1d1a within CTVT cells

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