Toward a<i>NOTCH1/FBXW7/RAS/PTEN</i>–Based Oncogenetic Risk Classification of Adult T-Cell Acute Lymphoblastic Leukemia: A Group for Research in Adult Acute Lymphoblastic Leukemia Study

Trinquand, Amélie; Tanguy‐Schmidt, Aline; Abdelali, Raouf Ben; Lambert, Jérôme; Beldjord, Kheïra; Lengliné, Étienne; Gunzburg, Noémie de; Payet-Bornet, Dominique; Lhermitte, Ludovic; Mossafa, Hossein; Lhéritier, Véronique; Bond, Jonathan; Huguet, Françoise; Buzyn, Agnès; Leguay, Thibaud; Cahn, Jean‐Yves; Thomas, Xavier; Chalandon, Yves; Delannoy, André; Bonmati, Caroline; Maury, Sébastien; Nadel, Bertrand; Macintyre, Elizabeth; Ifrah, Norbert; Dombret, Hervé; Asnafi, Vahid

doi:10.1200/jco.2012.48.5292

Cited by 207 publications

(236 citation statements)

References 33 publications

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“…Currently, the 5-y survival rate of pediatric T-ALL has reached more than 80% (1). In adult T-ALL, while significant therapeutic progress has been made in advanced hematology/oncology centers with a 5-y survival rate of over 60% (2), there are still challenges to improve the clinical prognosis in many cases. A better understanding of T-ALL in an adult group may allow more rational disease stratification and precision therapy.…”

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confidence: 99%

“…On the other hand, fusion genes are also common (20-30% in T-ALL), generating overexpression of mRNAs with ORFs for wild-type protein (such as TAL1 in STIL-TAL1) (9, 10) or transcripts containing fusions between two truncated ORFs such as SET-NUP214 (11). A number of gene abnormalities in pathways regulating differentiation, proliferation, self-renewal, and survival of T-cell precursors are also found in high frequencies, such as mutations of NOTCH1, JAK-STAT, PI3K-AKT, or RAS-MAPK pathway genes and CDKN2A/2B deletions (2,5,(12)(13)(14)(15).…”

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confidence: 99%

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Identification of fusion genes and characterization of transcriptome features in T-cell acute lymphoblastic leukemia

Chen

Jiang

Zhong

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

106

138

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T-cell acute lymphoblastic leukemia (T-ALL) is a clonal malignancy of immature T cells. Recently, the next-generation sequencing approach has allowed systematic identification of molecular features in pediatric T-ALL. Here, by performing RNA-sequencing and other genomewide analysis, we investigated the genomic landscape in 61 adult and 69 pediatric T-ALL cases. Thirty-six distinct gene fusion transcripts were identified, with SET-NUP214 being highly related to adult cases. Among 18 previously unknown fusions, ZBTB16-ABL1, TRA-SALL2, and involvement of NKX2-1 were recurrent events. ZBTB16-ABL1 functioned as a leukemogenic driver and responded to the effect of tyrosine kinase inhibitors. Among 48 genes with mutation rates >3%, 6 were newly found in T-ALL. An aberrantly overexpressed short mRNA transcript of the SLC17A9 gene was revealed in most cases with overexpressed TAL1, which predicted a poor prognosis in the adult group. Up-regulation of HOXA, MEF2C, and LYL1 was often present in adult cases, while TAL1 overexpression was detected mainly in the pediatric group. Although most gene fusions were mutually exclusive, they coexisted with gene mutations. These genetic abnormalities were correlated with deregulated gene expression markers in three subgroups. This study may further enrich the current knowledge of T-ALL molecular pathogenesis.

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confidence: 99%

mentioning

confidence: 99%

Identification of fusion genes and characterization of transcriptome features in T-cell acute lymphoblastic leukemia

Chen

Jiang

Zhong

et al. 2017

Proc. Natl. Acad. Sci. U.S.A.

106

138

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“…In a French Group for Research in Adult ALL study of T-ALL patients, those with aberrations in RAS and/or PTEN had a significantly worse outcome compared to patients without such mutations. 36 This was not confirmed in the MRC UKALL2003 trial for pediatric T-ALL; RAS and/or PTEN aberrations also did not change the favorable outcome of patients with NOTCH1/FBWX7 mutations. 44 Taken together, these findings suggest that PTEN aberrations may represent a general, poor prognostic factor in T-ALL.…”

Section: Discussionmentioning

confidence: 88%

“…21 In diagnostic samples from patients with TALLMO, PTEN is frequently inactivated in the absence of NOTCH-activating mutations. 21,32,36,59 Thus, mutations in PTEN and NOTCH1/FBXW7 are frequently independent genetic events and only co-occur in a small number of patients' primary samples. In those patients who harbor both PTEN mutations and NOTCH1/FBXW7 mutations, the NOTCH1 mutations are usually weakly activating mutations.…”

Section: Pten Is Not Linked a Priori To Resistance To Gamma-secretasementioning

confidence: 99%

“…With respect to T-ALL subtypes, we have shown that PTEN aberrations are strongly associated with TAL-or LMO-rearranged leukemia in children 21 and the same was observed in adult T-ALL cohorts. 36 The vast majority of PTEN aberrations are nonsense mutations in exon 7 (which truncate the Cterminal domain) and deletions that affect nearly the entire locus (Figure 1). Although truncated PTEN proteins that lack the lipid-binding C-terminal domain retain their phosphatase activity, they are highly unstable and are degraded rapidly.…”

Section: Pten Aberrations In T-cell Acute Lymphoblastic Leukemiamentioning

confidence: 99%

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The relevance of PTEN-AKT in relation to NOTCH1-directed treatment strategies in T-cell acute lymphoblastic leukemia

et al. 2016

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T-cell acute lymphoblastic leukemia (T-ALL) is a cancer of developing T cells in the thymus. T-ALL is characterized by chromosomal rearrangements. These rearrangements can lead to the aberrant activation of oncogenic transcription factors by placing their genes under the control of promoters and/or enhancers of Tcell receptor genes, the BCL11B gene, or other genes; occasionally, these rearrangements can give rise to oncogenic fusion proteins. The activated oncogenic transcription factors include TAL1 and LMO2 (and related family members), TLX1, TLX3, NKX2-1, HOXA, and MEF2C; in addition, certain oncogenic fusion proteins can directly activate the HOXA or MEF2C genes.1,2 Oncogenic proteins facilitate the developmental arrest of pre-leukemic immature T cells. We previously proposed that these chromosomal rearrangements should be classified as type A aberrations, as they are generally considered to be the driving oncogenic event associated with unique expression profiles.2 Based upon their gene expression signatures, T-ALL can be classified into the following four major subtypes: ETP-ALL, TLX, proliferative, and TALLMO. [3][4][5] Maturation arrest induces a pre-leukemic condition in which additional mutations can give rise to T-ALL.1,2 These secondary mutations are not necessarily clonal events and are often selected during disease progression or post-treatment T he tumor suppressor phosphatase and tensin homolog (PTEN) negatively regulates phosphatidylinositol 3-kinase (PI3K)-AKT signaling and is often inactivated by mutations (including deletions) in a variety of cancer types, including T-cell acute lymphoblastic leukemia. Here we review mutation-associated mechanisms that inactivate PTEN together with other molecular mechanisms that activate AKT and contribute to T-cell leukemogenesis. In addition, we discuss how Pten mutations in mouse models affect the efficacy of gamma-secretase inhibitors to block NOTCH1 signaling through activation of AKT. Based on these models and on observations in primary diagnostic samples from patients with T-cell acute lymphoblastic leukemia, we speculate that PTEN-deficient cells employ an intrinsic homeostatic mechanism in which PI3K-AKT signaling is dampened over time. As a result of this reduced PI3K-AKT signaling, the level of AKT activation may be insufficient to compensate for NOTCH1 inhibition, resulting in responsiveness to gamma-secretase inhibitors. On the other hand, de novo acquired PTEN-inactivating events in NOTCH1-dependent leukemia could result in temporary, strong activation of PI3K-AKT signaling, increased glycoly sis and glutaminolysis, and consequently gamma-secretase inhibitor resistance. Due to the central role of PTEN-AKT signaling and in the resistance to NOTCH1 inhibition, AKT inhibitors may be a promising addition to current treatment protocols for T-cell acute lymphoblastic leukemia.

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Acute Lymphoblastic Leukemia

Jabbour¹,

Jain²,

Kantarjian³

et al. 2022

Holland‐Frei Cancer Medicine

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Overview Acute lymphoblastic leukemia (ALL) is characterized by clonal proliferation of lymphoid progenitors. In the last decade, significant advances in understanding the disease pathogenesis, refining prognostic groups, and developing novel therapies that target specific subsets, have improved our treatment strategies and patient outcomes. Therapies targeting either specific transcripts (e.g., BCR‐ABL1 tyrosine kinase inhibitors) or specific leukemic cell surface antigens (e.g., CD20, CD22, and CD19 monoclonal antibodies, chimeric antigen receptor T‐cell therapies) produced major therapeutic breakthroughs. These novel therapies and combinations are transforming our strategies for adults with ALL and are resulting in significant improvements in survival. Many of these approaches focus on decreasing or eliminating the role of chemotherapy, with the goal of making these regimens more tolerable in older adults and decreasing the morbidity and mortality associated with myelosuppression‐related infections and other complications of intensive chemotherapy.

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Toward aNOTCH1/FBXW7/RAS/PTEN–Based Oncogenetic Risk Classification of Adult T-Cell Acute Lymphoblastic Leukemia: A Group for Research in Adult Acute Lymphoblastic Leukemia Study

Cited by 207 publications

References 33 publications

Identification of fusion genes and characterization of transcriptome features in T-cell acute lymphoblastic leukemia

Identification of fusion genes and characterization of transcriptome features in T-cell acute lymphoblastic leukemia

The relevance of PTEN-AKT in relation to NOTCH1-directed treatment strategies in T-cell acute lymphoblastic leukemia

Acute Lymphoblastic Leukemia

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