Differential genomics and transcriptomics between tyrosine kinase inhibitor-sensitive and -resistant BCR-ABL-dependent chronic myeloid leukemia

Previously, it has been stated that the BCR-ABL fusion-protein is sufficient to induce Chronic Myeloid Leukemia (CML), but additional genomic-changes are required for disease progression. Hence, we profiled control and tyrosine kinase inhibitors (TKI) alone or in combination with other drug-treated...

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Autores principales: Singh, Neetu, Tripathi, Anil Kumar, Sahu, Dinesh Kumar, Mishra, Archana, Linan, Margaret, Argente, Bianca, Varkey, Julia, Parida, Niranjan, Chowdhry, Rebecca, Shyam, Hari, Alam, Nawazish, Dixit, Shivani, Shankar, Pratap, Mishra, Abhishek, Agarwal, Avinash, Yoo, Chris, Bhatt, Madan Lal Brahma, Kant, Ravi
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Impact Journals LLC 2018
Materias:
Research Paper
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6084383/
https://www.ncbi.nlm.nih.gov/pubmed/30100996
http://dx.doi.org/10.18632/oncotarget.25752
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author Singh, Neetu
Tripathi, Anil Kumar
Sahu, Dinesh Kumar
Mishra, Archana
Linan, Margaret
Argente, Bianca
Varkey, Julia
Parida, Niranjan
Chowdhry, Rebecca
Shyam, Hari
Alam, Nawazish
Dixit, Shivani
Shankar, Pratap
Mishra, Abhishek
Agarwal, Avinash
Yoo, Chris
Bhatt, Madan Lal Brahma
Kant, Ravi
author_facet Singh, Neetu
Tripathi, Anil Kumar
Sahu, Dinesh Kumar
Mishra, Archana
Linan, Margaret
Argente, Bianca
Varkey, Julia
Parida, Niranjan
Chowdhry, Rebecca
Shyam, Hari
Alam, Nawazish
Dixit, Shivani
Shankar, Pratap
Mishra, Abhishek
Agarwal, Avinash
Yoo, Chris
Bhatt, Madan Lal Brahma
Kant, Ravi
author_sort Singh, Neetu
collection PubMed
description Previously, it has been stated that the BCR-ABL fusion-protein is sufficient to induce Chronic Myeloid Leukemia (CML), but additional genomic-changes are required for disease progression. Hence, we profiled control and tyrosine kinase inhibitors (TKI) alone or in combination with other drug-treated CML-samples in different phases, categorized as drug-sensitive and drug-resistant on the basis of BCR-ABL transcripts, the marker of major molecular-response. Molecular-profiling was done using the molecular-inversion probe-based-array, Human Transcriptomics-Array2.0, and Axiom-Biobank genotyping-arrays. At the transcript-level, clusters of control, TKI-resistant and TKI-sensitive cases were correlated with BCR-ABL transcript-levels. Both at the gene- and exon-levels, up-regulation of MPO, TPX2, and TYMS and down-regulation of STAT6, FOS, TGFBR2, and ITK lead up-regulation of the cell-cycle, DNA-replication, DNA-repair pathways and down-regulation of the immune-system, chemokine- and interleukin-signaling, TCR, TGF beta and MAPK signaling pathways. A comparison between TKI-sensitive and TKI-resistant cases revealed up-regulation of LAPTM4B, HLTF, PIEZO2, CFH, CD109, ANGPT1 in CML-resistant cases, leading to up-regulation of autophagy-, protein-ubiquitination-, stem-cell-, complement-, TGFβ- and homeostasis-pathways with specific involvement of the Tie2 and Basigin signaling-pathway. Dysregulated pathways were accompanied with low CNVs in CP-new and CP-UT-TKI-sensitive-cases with undetectable BCR-ABL-copies. High CNVs (previously reported gain of 9q34) were observed in BCR-ABL-independent and -dependent TKI, non-sensitive-CP-UT/AP-UT/B-UT and B-new samples. Further, genotyping CML-CP-UT cases with BCR-ABL 0-to-77.02%-copies, the identified, rsID239798 and rsID9475077, were associated with FAM83B, a candidate for therapeutic resistance. The presence of BCR-ABL, additional genetic-events, dysregulated-signaling-pathways and rsIDs associated with FAM83B in TKI-resistant-cases can be used to develop a signature-profile that may help in monitoring therapy.
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spelling pubmed-60843832018-08-10 Differential genomics and transcriptomics between tyrosine kinase inhibitor-sensitive and -resistant BCR-ABL-dependent chronic myeloid leukemia Singh, Neetu Tripathi, Anil Kumar Sahu, Dinesh Kumar Mishra, Archana Linan, Margaret Argente, Bianca Varkey, Julia Parida, Niranjan Chowdhry, Rebecca Shyam, Hari Alam, Nawazish Dixit, Shivani Shankar, Pratap Mishra, Abhishek Agarwal, Avinash Yoo, Chris Bhatt, Madan Lal Brahma Kant, Ravi Oncotarget Research Paper Previously, it has been stated that the BCR-ABL fusion-protein is sufficient to induce Chronic Myeloid Leukemia (CML), but additional genomic-changes are required for disease progression. Hence, we profiled control and tyrosine kinase inhibitors (TKI) alone or in combination with other drug-treated CML-samples in different phases, categorized as drug-sensitive and drug-resistant on the basis of BCR-ABL transcripts, the marker of major molecular-response. Molecular-profiling was done using the molecular-inversion probe-based-array, Human Transcriptomics-Array2.0, and Axiom-Biobank genotyping-arrays. At the transcript-level, clusters of control, TKI-resistant and TKI-sensitive cases were correlated with BCR-ABL transcript-levels. Both at the gene- and exon-levels, up-regulation of MPO, TPX2, and TYMS and down-regulation of STAT6, FOS, TGFBR2, and ITK lead up-regulation of the cell-cycle, DNA-replication, DNA-repair pathways and down-regulation of the immune-system, chemokine- and interleukin-signaling, TCR, TGF beta and MAPK signaling pathways. A comparison between TKI-sensitive and TKI-resistant cases revealed up-regulation of LAPTM4B, HLTF, PIEZO2, CFH, CD109, ANGPT1 in CML-resistant cases, leading to up-regulation of autophagy-, protein-ubiquitination-, stem-cell-, complement-, TGFβ- and homeostasis-pathways with specific involvement of the Tie2 and Basigin signaling-pathway. Dysregulated pathways were accompanied with low CNVs in CP-new and CP-UT-TKI-sensitive-cases with undetectable BCR-ABL-copies. High CNVs (previously reported gain of 9q34) were observed in BCR-ABL-independent and -dependent TKI, non-sensitive-CP-UT/AP-UT/B-UT and B-new samples. Further, genotyping CML-CP-UT cases with BCR-ABL 0-to-77.02%-copies, the identified, rsID239798 and rsID9475077, were associated with FAM83B, a candidate for therapeutic resistance. The presence of BCR-ABL, additional genetic-events, dysregulated-signaling-pathways and rsIDs associated with FAM83B in TKI-resistant-cases can be used to develop a signature-profile that may help in monitoring therapy. Impact Journals LLC 2018-07-13 /pmc/articles/PMC6084383/ /pubmed/30100996 http://dx.doi.org/10.18632/oncotarget.25752 Text en Copyright: © 2018 Singh et al. http://creativecommons.org/licenses/by/3.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License 3.0 (http://creativecommons.org/licenses/by/3.0/) (CC BY 3.0), which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are credited.
spellingShingle Research Paper
Singh, Neetu
Tripathi, Anil Kumar
Sahu, Dinesh Kumar
Mishra, Archana
Linan, Margaret
Argente, Bianca
Varkey, Julia
Parida, Niranjan
Chowdhry, Rebecca
Shyam, Hari
Alam, Nawazish
Dixit, Shivani
Shankar, Pratap
Mishra, Abhishek
Agarwal, Avinash
Yoo, Chris
Bhatt, Madan Lal Brahma
Kant, Ravi
Differential genomics and transcriptomics between tyrosine kinase inhibitor-sensitive and -resistant BCR-ABL-dependent chronic myeloid leukemia
title Differential genomics and transcriptomics between tyrosine kinase inhibitor-sensitive and -resistant BCR-ABL-dependent chronic myeloid leukemia
title_full Differential genomics and transcriptomics between tyrosine kinase inhibitor-sensitive and -resistant BCR-ABL-dependent chronic myeloid leukemia
title_fullStr Differential genomics and transcriptomics between tyrosine kinase inhibitor-sensitive and -resistant BCR-ABL-dependent chronic myeloid leukemia
title_full_unstemmed Differential genomics and transcriptomics between tyrosine kinase inhibitor-sensitive and -resistant BCR-ABL-dependent chronic myeloid leukemia
title_short Differential genomics and transcriptomics between tyrosine kinase inhibitor-sensitive and -resistant BCR-ABL-dependent chronic myeloid leukemia
title_sort differential genomics and transcriptomics between tyrosine kinase inhibitor-sensitive and -resistant bcr-abl-dependent chronic myeloid leukemia
topic Research Paper
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC6084383/
https://www.ncbi.nlm.nih.gov/pubmed/30100996
http://dx.doi.org/10.18632/oncotarget.25752
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