Association of gene mutations with time‐to‐first treatment in 384 treatment‐naive chronic lymphocytic leukaemia patients

Hu, Boyu; Patel, Keyur P.; Chen, Hsiang‐Chun; Wang, Xuemei; Luthra, Rajyalakshmi; Routbort, Mark J.; Kanagal‐Shamanna, Rashmi; Medeiros, L. Jeffrey; Yin, C. Cameron; Zuo, Zhuang; Ok, Chi Young; Loghavi, Sanam; Tang, Guilin; Tambaro, Francesco Paolo; Thompson, Philip A.; Burger, Jan A.; Jain, Nitin; Ferrajoli, Alessandra; Bose, Prithviraj; Estrov, Zeev; Keating, Michael J.; Wierda, William G.

doi:10.1111/bjh.16042

Cited by 28 publications

(28 citation statements)

References 49 publications

(98 reference statements)

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“…The percentage of del17p cells has an impact on the prognosis of CLL patients, and the low percentage of del17p cells predicts a better TTFT [66]. However, another study revealed that neither del17p, mutated p53, nor complex karyotypes is associated with TTFT, which suggests that they have limited roles in early CLL patients but may take effect in relapsed disease [47]. Besides chromosome aberrations above, del6q, del9p21, del10q23, total or partial trisomies of chromosomes 3, 8, 18, 19, and duplications in 2p24 also have an impact on prognosis in CLL [67].…”

Section: Chromosome Aberrationsmentioning

confidence: 99%

Recent progress of prognostic biomarkers and risk scoring systems in chronic lymphocytic leukemia

2020

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Chronic lymphocytic leukemia (CLL) is the most prevalent adult leukemia with high heterogeneity in the western world. Thus, investigators identified a number of prognostic biomarkers and scoring systems to guide treatment decisions and validated them in the context of immunochemotherapy. A better understanding of prognostic biomarkers, including serum markers, flow cytometry outcomes, IGHV mutation status, microRNAs, chromosome aberrations and gene mutations, have contributed to prognosis in CLL. Del17p/ TP53 mutation, NOTCH1 mutation, CD49d, IGHV mutation status, complex karyotypes and microRNAs were reported to be of predictive values to guide clinical decisions. Based on the biomarkers above, classic prognostic models, such as the Rai and Binet staging systems, MDACC nomogram, GCLLSG model and CLL-IPI, were developed to improve risk stratification and tailor treatment intensity. Considering the presence of novel agents, many investigators validated the conventional prognostic biomarkers in the setting of novel agents and only TP53 mutation status/del 17p and CD49d expression were reported to be of prognostic value. Whether other prognostic indicators and models can be used in the context of novel agents, further studies are required.

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Section: Chromosome Aberrationsmentioning

confidence: 99%

Recent progress of prognostic biomarkers and risk scoring systems in chronic lymphocytic leukemia

2020

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“…In addition, by taking advantage of the genetic heterogeneity of CLL, mutations of genes involved in CLL pathogenesis have been tested as biomarkers for identifying early stage CLL patients with a higher risk of progression and treatment requirement. These studies point to mutations of SF3B1, NOTCH1, ATM, U1, and XPO1 as molecular predictors of shorter TTFT [7,56,57]. Interestingly, TP53 disruption is not associated with a shorter TTFT, in line with the notion that TP53 disruption interacts with treatment with chemotherapeutic agents, but not with a watch and wait strategy that does not expose CLL cells carrying TP53 disruption to the positive selection pressure exerted by ineffective chemotherapy [55,56].…”

Section: Management Of Asymptomatic Cll Patientsmentioning

confidence: 70%

“…Recent studies have tried to identify the clinical and molecular features of early stage CLL patients managed with a watch and wait approach and who might manifest treatment requirement soon after diagnosis [6,[55][56][57][58]. The pattern of tumor growth of untreated CLL has been investigated by analyzing serial longitudinal samples collected between diagnosis and the time of treatment requirement [6].…”

Section: Management Of Asymptomatic Cll Patientsmentioning

confidence: 99%

“…These studies point to mutations of SF3B1, NOTCH1, ATM, U1, and XPO1 as molecular predictors of shorter TTFT [7,56,57]. Interestingly, TP53 disruption is not associated with a shorter TTFT, in line with the notion that TP53 disruption interacts with treatment with chemotherapeutic agents, but not with a watch and wait strategy that does not expose CLL cells carrying TP53 disruption to the positive selection pressure exerted by ineffective chemotherapy [55,56]. The precise role of gene mutations in sorting asymptomatic CLL patients with an imminent risk of treatment requirement still needs to be clarified and is the current subject of investigations.…”

Section: Management Of Asymptomatic Cll Patientsmentioning

confidence: 99%

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Precision Medicine Management of Chronic Lymphocytic Leukemia

Moia

Patriarca

Schipani

et al. 2020

Cancers

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Chronic lymphocytic leukemia (CLL) is the most common type of leukemia in western countries, with an incidence of approximately 5.1/100,000 new cases per year. Some patients may never require treatment, whereas others relapse early after front line therapeutic approaches. Recent whole genome and whole exome sequencing studies have allowed a better understanding of CLL pathogenesis and the identification of genetic lesions with potential clinical relevance. Consistently, precision medicine plays a pivotal role in the treatment algorithm of CLL, since the integration of molecular biomarkers with the clinical features of the disease may guide treatment choices. Most CLL patients present at the time of diagnosis with an early stage disease and are managed with a watch and wait strategy. For CLL patients requiring therapy, the CLL treatment armamentarium includes both chemoimmunotherapy strategies and biological drugs. The efficacy of these treatment strategies relies upon specific molecular features of the disease. TP53 disruption (including both TP53 mutation and 17p deletion) is the strongest predictor of chemo-refractoriness, and the assessment of TP53 status is the first and most important decisional node in the first line treatment algorithm. The presence of TP53 disruption mandates treatment with biological drugs that inhibit the B cell receptor or, alternatively, the B-cell lymphoma 2 (BCL2) pathway and can, at least in part, circumvent the chemorefractoriness of TP53-disrupted patients. Beside TP53 disruption, the mutational status of immunoglobulin heavy variable (IGHV) genes also helps clinicians to improve treatment tailoring. In fact, patients carrying mutated IGHV genes in the absence of TP53 disruption experience a long-lasting and durable response to chemoimmunotherapy after fludarabine, cyclophosphamide, and rituximab (FCR) treatment with a survival superimposable to that of a matched general population. In contrast, patients with unmutated IGHV genes respond poorly to chemoimmunotherapy and deserve treatment with B cell receptor inhibitors. Minimal residual disease is also emerging as a relevant biomarker with potential clinical implications. Overall, precision medicine is now a mainstay in the management and treatment stratification of CLL. The identification of novel predictive biomarkers will allow further improvements in the treatment tailoring of this leukemia.

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“…An important question is how can this be added to by the more recent identification of recurrent genetic mutations in CLL. In the current paper, (Hu et al , ) the authors studied the impact on time from diagnosis to time to first treatment (TTFT) of detection of mutations in a 29 gene panel and looked for associations with a variety of standard prognostic factors in a cohort of 384 treatment naïve CLL. They demonstrate that mutated ATM ( P < 0·001), NOTCH1 ( P < 0·001) and SF3B1 ( P = 0·002) as well as unmutated IGHV ( P < 0·001), del(11q) ( P < 0·001) and trisomy 12 ( P < 0·001) by hierarchal FISH and advanced Rai ( P = 0·05) and Binet ( P < 0·001) stages were associated with shorter TTFT.…”

mentioning

confidence: 99%

Do we need to analyse everything at diagnosis in chronic lymphocytic leukaemia?

Gribben

2020

Br J Haematol

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Keywords: chronic lymphocytic leukaemia, heterogeneous disease, prognostic factors.Chronic lymphocytic leukaemia (CLL) is an extremely heterogeneous disease in terms of its clinical course and a variety of biomarkers have been described that have powerful prognostic and predictive outcome. An important question is how can this be added to by the more recent identification of recurrent genetic mutations in CLL. In the current paper, (Hu et al., 2019) the authors studied the impact on time from diagnosis to time to first treatment (TTFT) of detection of mutations in a 29 gene panel and looked for associations with a variety of standard prognostic factors in a cohort of 384 treatment na€ ıve CLL. They demonstrate that mutated ATM (P < 0Á001), NOTCH1 (P < 0Á001) and SF3B1 (P = 0Á002) as well as unmutated IGHV (P < 0Á001), del(11q) (P < 0Á001) and trisomy 12 (P < 0Á001) by hierarchal FISH and advanced Rai (P = 0Á05) and Binet (P < 0Á001) stages were associated with shorter TTFT. In a multivariable analysis, mutated ATM (P < 0Á001) and unmutated IGHV status (P < 0Á001) remained significant, and the authors suggest that these factors are therefore important in early leukemogenesis. Surprisingly, in this cohort and in contrast to previous studies, the very high-risk prognostic factors del(17p), mutated TP53 and complex karyotype were not associated with shorter TTFT and the authors suggest further that these factors may have less impact in early disease progression, but are more important in terms of response to chemotherapy and at later times in the clinical course of CLL.Up to 80% of CLL patients are now diagnosed incidentally and are asymptomatic at diagnosis. Many patients remain asymptomatic over decades and 20-30% have a life expectancy not significantly different from the general population (Rossi et al., 2013), while others progress rapidly to requirement for treatment with extensive lymphadenopathy, hepatosplenomegaly, and cytopoenias.

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Association of gene mutations with time‐to‐first treatment in 384 treatment‐naive chronic lymphocytic leukaemia patients

Cited by 28 publications

References 49 publications

Recent progress of prognostic biomarkers and risk scoring systems in chronic lymphocytic leukemia

Recent progress of prognostic biomarkers and risk scoring systems in chronic lymphocytic leukemia

Precision Medicine Management of Chronic Lymphocytic Leukemia

Do we need to analyse everything at diagnosis in chronic lymphocytic leukaemia?

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