A Quantitative Analysis of Subclonal and Clonal Gene Mutations before and after Therapy in Chronic Lymphocytic Leukemia

Amin, Nisar A.; Seymour, Erlene; Saiya-Cork, Kamlai; Parkin, Brian; Shedden, Kerby; Malek, Sami N.

doi:10.1158/1078-0432.ccr-15-3103

Cited by 63 publications

(53 citation statements)

References 50 publications

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“…The CLL cases selected for this study were highly characterized for known clinically relevant traits. In addition, the relapsed CLL samples were analyzed for gene mutations through whole exome sequencing (WES) and subsequent Sanger sequencing of all recurrently mutated genes as detected through WES, SNP 6.0 profiling of genomic copy number changes and deep panel-based gene re-sequencing of TP53, NOTCH1 and other genes as described(28). …”

Section: Resultsmentioning

confidence: 99%

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Cell-Intrinsic Determinants of Ibrutinib-Induced Apoptosis in Chronic Lymphocytic Leukemia

Amin

Balasubramanian

Saiya-Cork

et al. 2017

Clinical Cancer Research

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Purpose Ibrutinib, a Bruton’s tyrosine kinase (BTK) inhibitor, is approved for the treatment of relapsed CLL and CLL with del17p. Mechanistically, ibrutinib interferes with BCR signaling as well as multiple CLL cell to microenvironment interactions. Given the importance of ibrutinib in the management of CLL, a deeper understanding of factors governing sensitivity and resistance is warranted. Experimental Design We studied 48 longitudinally sampled paired CLL samples, 42 of which were procured before and after standard CLL chemotherapies, and characterized them for well-studied CLL molecular traits as well as by whole exome sequencing and SNP 6.0 array profiling. We exposed these samples to 0.25 μM – 5 μM of ibrutinib ex vivo and measured apoptosis fractions as well as BCR signaling by immunoblotting. We disrupted TP53 in HG3, PGA1 and PG-EBV cell lines and measured BCR signaling and ibrutinib responses. Results CLL samples demonstrated a surprisingly wide range of ex vivo sensitivities to ibrutinib with IC50 values ranging from 0.4 μM – 9.7 μM. Unmutated IGVH status, elevated ZAP70 expression and trisomy 12 were associated with heightened sensitivity to ibrutinib treatment. Five CLL samples were substantially more resistant to ibrutinib following relapse from chemotherapy; of these, three had acquired a del17p/TP53 mutated status. A validation sample of 15 CLL carrying TP53 mutations, of which 13 carried both del17p and a TP53 mutation confirmed substantially less sensitivity to ibrutinib-induced apoptosis. Conclusions This study identifies that CLL harboring del17p/TP53 mutated cells are substantially less sensitive to ibrutinib-induced apoptosis than del17p/TP53 wild type cells.

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Section: Resultsmentioning

confidence: 99%

“…Solution-based exome capture and HiSeq2000-based massively parallel sequencing and bioinformatic pipeline analysis of WES data was performed as described(28). …”

Section: Methodsmentioning

confidence: 99%

Cell-Intrinsic Determinants of Ibrutinib-Induced Apoptosis in Chronic Lymphocytic Leukemia

Amin

Balasubramanian

Saiya-Cork

et al. 2017

Clinical Cancer Research

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“…It was shown that 3-5% of CLL patients have acquired mutations in SAMHD1 at diagnosis (Clifford et al, 2014). However, SAMHD1 mutation frequency is increased in relapsed/refractory CLL (9-11%) without associated increase of other poor risk factors, such as 11q deletion or unmutated IGHV (Clifford et al, 2014;Amin et al, 2016). Two independent studies associated SAMHD1 mutations with resistance to standard CLL therapies (Clifford et al, 2014;Amin et al, 2016).…”

Section: Cell Cycle Apoptosis and Dna Damage And Synthesismentioning

confidence: 99%

“…However, SAMHD1 mutation frequency is increased in relapsed/refractory CLL (9-11%) without associated increase of other poor risk factors, such as 11q deletion or unmutated IGHV (Clifford et al, 2014;Amin et al, 2016). Two independent studies associated SAMHD1 mutations with resistance to standard CLL therapies (Clifford et al, 2014;Amin et al, 2016). Indeed, standard treatments may select pre-existing clones carrying SAMHD1 mutations (Amin et al, 2016).…”

Section: Cell Cycle Apoptosis and Dna Damage And Synthesismentioning

confidence: 99%

Chronic lymphocytic leukaemia genomics and the precision medicine era

2017

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Massive genomic analyses have underscored the diversity of chronic lymphocytic leukaemia (CLL) between patients. Genetic heterogeneity of tumour clones within a patient may fuel tumour evolution. Several recurrently deregulated intra-cellular pathways are candidates for targeted therapies that are very promising and are dramatically changing clinical patients' perspectives. In this review we present an overview of the genetic and epigenetic features of CLL and their clinical and biological implications.

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“…Whole‐exome sequencing (WES) has led to the discovery of mutations in genes such as SF3B1 , which encodes a protein that normally acts as part of the RNA spliceosome and mRNA processing machinery, with a reported mutational frequency in CLL between 10–15% (Wang et al , ; Wan & Wu, ). While functional loss or gain within the mutation is currently unclear, SF3B1 mutations cause deleterious effects on DNA damage repair and are associated with a shorter time‐to‐first treatment (TTFT) and overall survival (OS) (Jeromin et al , ; Te Raa et al , ; Amin et al , ; Nadeu et al , ). Additional examples include mutations in TP53, BIRC3, ATM, KRAS, POT1 and NOTCH1, which were all associated with reduced responses to treatment and shorter survival (Rossi et al , ; Cortese et al , ; Landau et al , ; Herling et al , ; Nadeu et al , ).…”

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confidence: 99%

Routine sequencing in CLL has prognostic implications and provides new insight into pathogenesis and targeted treatments

Patel

Chen

et al. 2019

Br J Haematol

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Summary Chronic lymphocytic leukaemia (CLL) is a genetically heterogeneous disease characterised by genomic alterations and gene mutations that may portend worse survival or resistance to treatments. A total of 680 blood or bone marrow samples underwent targeted sequencing of 29 genes previously identified as being mutated in CLL, which were correlated to known prognostic clinical characteristics. Overall, 400 (59%) patients were treatment‐naïve (TN) and 280 (41%) were relapsed/refractory (R/R). Most patients (70%) had ≥1 mutation, with TP53 (22%), SF3B1 (18%), NOTCH1 (13%) and ATM (13%) being the most commonly mutated genes. A higher proportion of R/R patients had mutations in SF3B1 (P = 0·01) and TP53 (P < 0·001). Patients with mutated IGHV CLL more often had mutations in KLHL6 (P = 0·001) and MYD88 (P < 0·001). Pairwise associations showed mutational co‐occurrences in the TN group including SF3B1/ATM [false discovery rate (FDR) < 0·05] and NOTCH1/POT1 (FDR < 0·01). Recurrent mutations resulting in premature truncation prior to the ubiquitination domains of NOTCH1 in its PEST domain and BIRC3 in its RING domain can produce proteins that constitutively activate CLL. Frequent missense mutations, such as K700E in SF3B1 and E571K in XPO1, have unknown function but are most likely to be activating mutations. Future directions include using these mutations to identify pathways for therapeutic targeting and rational drug design.

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A Quantitative Analysis of Subclonal and Clonal Gene Mutations before and after Therapy in Chronic Lymphocytic Leukemia

Cited by 63 publications

References 50 publications

Cell-Intrinsic Determinants of Ibrutinib-Induced Apoptosis in Chronic Lymphocytic Leukemia

Cell-Intrinsic Determinants of Ibrutinib-Induced Apoptosis in Chronic Lymphocytic Leukemia

Chronic lymphocytic leukaemia genomics and the precision medicine era

Routine sequencing in CLL has prognostic implications and provides new insight into pathogenesis and targeted treatments

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