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1.
Elife ; 52016 05 17.
Artigo em Inglês | MEDLINE | ID: mdl-27185408

RESUMO

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.


Assuntos
Doenças do Cão/genética , Variação Genética , Mitocôndrias/genética , Recombinação Genética , Seleção Genética , Tumores Venéreos Veterinários/genética , Animais , DNA Mitocondrial/química , DNA Mitocondrial/genética , Cães , Análise de Sequência de DNA
2.
Baez Ortega, Adrian; Gori, Kevin; Strakova, Andrea; Allen, Janice L; Allum, Karen M; Bansse Issa, Leontine; Bhutia, Thinlay N; Bisson, Jocelyn L; Briceño, Cristóbal; Castillo Domracheva, Artemio; Corrigan, Anne M; Cran, Hugh R; Crawford, Jane T; Davis, Eric; De Castro, Karina F; De Nardi, Andrigo B; De Vos, Anna P; Delgadillo Keenan, Laura; Donelan, Edward M; Espinoza Huerta, Adela R; Faramade, Ibikunle A; Fazil, Mohammed; Fotopoulou, Eleni; Fruean, Skye N; Gallardo Arrieta, Fanny; Glebova, Olga; Gouletsou, Pagona G; Hafelin Manrique, Rodrigo F; Henriques, Joaquim JGP; Horta, Rodrigo S; Ignatenko, Natalia; Kane, Yaghouba; King, Cathy; Koening, Debbie; Krupa, Ada; Kruzeniski, Steven; Kwon, Young-Mi; Lanza Perea, Marta; Lazyan, Mihran; López Quintana, Adriana M; Losfelt, Thibault; Marino, Gabriele; Martínez Castañedo, Simón; Martínez López, Mayra; Meyer, Michael; Migneco, Edward J; Nakanwagi, Berna; Neal, Karter B; Neuzing, Winifred; Leathlobhair, Maire Ni; Nixon, Sally J; Ortega Pacheco, Antonio; Pedraza Ordoñez, Francisco; Peleteiro, María C; Polak, Katherine; Pye, Ruth J; Reece, John F; Rojas Gutierrez, José; Sadia, Haleema; Schmeling, Sheila K; Shamanova, Olga; Sherlock, Alan; Stammnitz, Maximilian; Steenland Smith, Audrey E; Svitich, Alla; Tapia Martínez, Lester J; Thoya Ngoka, Ismail; Torres, Cristian G; Tudor, Elizabeth M; Van der Wel, Mirjam; Vitalaru, Bogdan A; Vural, Sevil A; Walkinton, Oliver; Wang, Jinhong; Wehrle Martínez, Alvaro S; Widdowson, Sophie AE; Stratton, Michael; Alexandrov, Ludmil B; Martincorena, Iñigo; Murchison, Elizabeth P.
Science ; 365: [7 p], agosto, 2019.
Artigo em Inglês | URUCAN | ID: bcc-5407

RESUMO

The canine transmissible venereal tumor (CTVT) is a cancer lineage that arose several millennia ago and survives by "metastasizing" between hosts through cell transfer. The somatic mutations in this cancer record its phylogeography and evolutionary history. We constructed a time-resolved phylogeny from 546 CTVT exomes and describe the lineage's worldwide expansion. Examining variation in mutational exposure, we identify a highly context-specific mutational process that operated early in the cancer's evolution but subsequently vanished, correlate ultraviolet-light mutagenesis with tumor latitude, and describe tumors with heritable hyperactivity of an endogenous mutational process. CTVT displays little evidence of ongoing positive selection, and negative selection is detectable only in essential genes. We illustrate how long-lived clonal organisms capture changing mutagenic environments, and reveal that neutral genetic drift is the dominant feature of long-term cancer evolution(AU)


Assuntos
Animais , Cães , Tumores Venéreos Veterinários/genética , Bibliografia Nacional , Uruguai
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