2020
DOI: 10.21294/1814-4861-2020-19-3-78-88
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Association of the Combination of Stemness Gene Amplifications and Copy Number Aberrations of WNT-Signaling Genes in Breast Tumors With Metastasis

Abstract: We studied the association between the presence of 2 or more stemness gene amplifications as well as copy number aberrations (CNAs) of WNT signaling genes in residual breast tumor and metastasis. WNT pathway genes associated with metastasis were identified.Material and Methods. The study included 30 patients with breast cancer, who had 2 or more stemness gene amplifications in the residual tumor after neoadjuvant chemotherapy. Fifteen of the thirty patients devel… Show more

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Cited by 2 publications
(8 citation statements)
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“…The most important WNT signalling pathway genes responsible for its activation have previously been identified: 15 WNT signalling activator genes (WNT2B, SKP1, TCF7, PPP2CA, WNT8A, MAPK9, CCND3, PPP2R5D, WNT8B, CCND1, FZD2, WNT3, FZD9, WNT3, WNT9B) and 7 negative regulator genes (GSK3B, APC, CSNK2B, SFRP5, BTRC, TCF7L2, CSNK2A2), whose amplifications and deletions, respectively, should stimulate the WNT signalling pathway [32]. CNA-genetic landscape analysis of breast cancer tumour lines (BT-474, BT-549, MDA-MB-231, MDA-MD-468, MCF7, SK-BR-3 and T47D) revealed cultures with the ability/inability to dedifferentiate (due to amplifications of stemness genes [24]) and to the exit from postchemotherapy shock after chemotherapy exposure (due to CNA of WNT signalling pathway genes presented above).…”
Section: Resultsmentioning
confidence: 99%
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“…The most important WNT signalling pathway genes responsible for its activation have previously been identified: 15 WNT signalling activator genes (WNT2B, SKP1, TCF7, PPP2CA, WNT8A, MAPK9, CCND3, PPP2R5D, WNT8B, CCND1, FZD2, WNT3, FZD9, WNT3, WNT9B) and 7 negative regulator genes (GSK3B, APC, CSNK2B, SFRP5, BTRC, TCF7L2, CSNK2A2), whose amplifications and deletions, respectively, should stimulate the WNT signalling pathway [32]. CNA-genetic landscape analysis of breast cancer tumour lines (BT-474, BT-549, MDA-MB-231, MDA-MD-468, MCF7, SK-BR-3 and T47D) revealed cultures with the ability/inability to dedifferentiate (due to amplifications of stemness genes [24]) and to the exit from postchemotherapy shock after chemotherapy exposure (due to CNA of WNT signalling pathway genes presented above).…”
Section: Resultsmentioning
confidence: 99%
“…Cell lines with a presumed ability to dedifferentiate and to emerge from postchemotherapy shock after exposure to chemotherapy drugs were established for mechanistic culture studies. The ability to emerge from postchemotherapy shock was established using a scoring system that we developed earlier: one point was added to the total sum of points if WNT signalling activators were amplified or negative regulators were deleted, and vice versa; one point was subtracted from the total sum if WNT signalling activators were deleted or negative regulators were amplified [32].…”
Section: X For Peer Review 4 Of 16mentioning
confidence: 99%
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