Age-related phenotypic and oncogenic differences in T-cell acute lymphoblastic leukemias may reflect thymic atrophy

Asnafi, Vahid; Beldjord, Kheïra; Libura, M; Villarèse, Patrick; Millien, Corinne; Ballerini, Paola; Kühlein, Emilienne; Lafage‐Pochitaloff, Marina; Delabesse, Éric; Bernard, Olivier A.; Macintyre, Elizabeth

doi:10.1182/blood-2003-11-3944

Cited by 93 publications

(108 citation statements)

References 58 publications

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“…However, another implication of this disease mechanism is the expectation that HOX11 þ cancers would be especially sensitive to high doses of spindle poisons, which should promote catastrophic chromosomal abnormalities and induce cell death. Indeed, relative to other T-ALL subtypes, HOX11 þ T-ALLs have been demonstrated to be exceedingly responsive to combination chemotherapies (Asnafi et al, 2004;Ferrando et al, 2004), which typically employ spindle poisons in the treatment regimen. It may also explain the refractory nature of relapsed HOX11 þ T-ALLs to chemotherapy, which likely possess a complex karyotype, and the resultant need for bone marrow transplantation therapy for second-line treatment (Asnafi et al, 2005).…”

Section: Discussionmentioning

confidence: 99%

“…Clinically, patients with HOX11-positive lymphoblasts have a better prognosis when treated with modern combination chemotherapy than patients with T-ALLs involving activation of HOX11L2 (Ferrando et al, 2002(Ferrando et al, , 2004. The incidence of HOX11-positive lymphomas correlates with increasing age, indicating a longer latency for disease manifestation and suggesting the requirement of additional genetic events prior to malignancy (Asnafi et al, 2004).…”

Section: Introductionmentioning

confidence: 99%

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Dysregulated expression of mitotic regulators is associated with B-cell lymphomagenesis in HOX11-transgenic mice

et al. 2006

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Dysregulated expression of the homeobox gene, HOX11 is a frequent etiologic event in T-cell acute lymphoblastic leukemias. HOX11-transgenic mice (IgHl-HOX11 Tg )-expressing HOX11 in the B-cell compartment develop B-cell lymphomas with extended latency. The latency suggests that additional genetic events are required prior to the onset of malignant lymphoma. We report the identification of 17 HOX11 collaborating genes, revealed through their propensity to be targeted in a proviral insertional mutagenesis screen. Seven integrations disrupted genes in mitotic spindle checkpoint control, suggesting that cells with elevated HOX11 expression are especially sensitive to dysregulation of chromosome segregation during mitosis. IgHl-HOX11 Tg primary B-lymphocyte cultures exposed to the aneugenic agents, colchicine and colcemid, exhibited increased incidences of chromosome missegregation as assessed by cytokinesisblock micronucleus assays. Additionally, IgHl-HOX11 Tg cultures were shown to exhibit aberrant bypass of spindle checkpoint arrest, as assessed by the increased presence of cycling cells determined by assessment of DNA content and by BrdU immunolabelling. Western immunoblotting revealed elevated expression of the mitotic effector molecules, cyclin A, cyclin B1 and cdc20 in IgHl-HOX11 Tg cultures. Moreover, spontaneously arising lymphoid neoplasms in IgHl-HOX11 Tg mice frequently exhibit aberrant expression of mitotic regulators, concomitant with increased development of micronuclei, abnormal mitotic checkpoint control and increased incidences of abnormal karyotypes when expanded in culture. Collectively, these findings indicate that abnormal regulation of spindle checkpoint control as a result of HOX11 overexpression leads to a heightened predisposition for development of aneuploidy, contributing to oncogenesis.

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Section: Discussionmentioning

confidence: 99%

Section: Introductionmentioning

confidence: 99%

Dysregulated expression of mitotic regulators is associated with B-cell lymphomagenesis in HOX11-transgenic mice

et al. 2006

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“…Also, little is known about a correlation of molecular data and the immunologic subtypes as an already established prognostic factor. 9 Thus, we have retrospectively evaluated the incidence and prognostic impact of HOX11 and HOX11L2 expression in 286 immunologically well-characterized adult T-ALL patients.…”

Section: Introductionmentioning

confidence: 99%

“…6 However, available data are controversial regarding the clinical impact of aberrant HOX11 and HOX11L2 expression in childhood T-ALL, and few data are available in adult patients. [7][8][9][10] The pediatric and adult population might differ substantially in the activation status of these oncogenes. Also, little is known about a correlation of molecular data and the immunologic subtypes as an already established prognostic factor.…”

Section: Introductionmentioning

confidence: 99%

Thymic adult T-cell acute lymphoblastic leukemia stratified in standard- and high-risk group by aberrant HOX11L2 expression: experience of the German multicenter ALL study group

et al. 2008

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Adult T-cell acute lymphoblastic leukemia (T-ALL) continues to represent an unfavorable disease. Molecularly based treatment stratifications could help improve outcome. The prognostic impact of HOX11 and HOX11L2 expression has been an area of controversy. We have investigated 286 adult T-ALL patients enrolled into the German Multicenter ALL (GMALL) therapy protocols by comparative real-time RT-PCR. High HOX11 expression and HOX11L2 expression were predominantly seen in thymic T-ALL (P ¼ 0.031). In a multivariate analysis HOX11L2 expression proved to be an independent adverse risk factor for relapse-free survival (RFS) with a hazard ratio (HR) of 2.02 (P ¼ 0.023) and an HR for overall survival (OS) of 1.81 (P ¼ 0.021), both adjusted for the immunophenotype. HOX11 expression was found to have a favorable impact on RFS (HR 0.51; P ¼ 0.048) but did not exhibit a significant impact on OS. A subgroup analysis for thymic T-ALL revealed a more pronounced negative correlation of HOX11L2 expression with RFS (HR 3.26; P ¼ 0.002) and OS (HR 2.38; P ¼ 0.009). Although the prognostic impact of HOX11 in T-ALL is less clear, HOX11L2 expression identifies a small subset of high-risk patients, who are so far classified as standard-risk group. Thus, patients with aberrant HOX11L2 expression should be considered early as candidates for intensified treatment regimes.

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“…Un métabolisme primitif nécessite égale-ment que ces polymères soient capables de se replier dans des structures tertiaires stables ayant des fonctionnalités élaborées telles que la reconnaissance d'un ligand et la catalyse [5]. Parmi les systèmes étudiés, l'acide nucléique (3', 2')--L-thréose (ANT, Figure 1) pourrait jouer le rôle de précur-seur de l'ARN en raison de sa simplicité structurale -son squelette est constitué de thréoses qui ont un carbone de moins que les riboses de l'ARN -et de sa capacité à former des structures hélicoïdales stables avec des brins complémentaires d'ANT ou d'ARN [6][7][8].…”

Section: Cbfa2unclassified

Mécanisme d’action des oncogènes à homéodomaine TLX dans les LAL-T

Asnafi

Ferrier

2012

Med Sci (Paris)

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> Parmi les hémopathies, les leucémies aiguës lymphoblastiques T (LAL-T) représentent 15 à 25 % de l'ensemble des LAL et se caractérisent par un phénotype d'arrêt de maturation à un stade précoce de la différenciation lymphoïde T. Ces affections représen-tent ainsi un groupe hétérogène de leucémies aiguës dont le trait commun est un blocage de la différenciation cellulaire à un stade donné de la maturation thymique [1,2]. Leur pronostic, bien que nettement amélioré grâce aux progrès thérapeutiques récents, reste dans l'ensemble relativement médiocre, les taux de survie avoisinant 50 % à 5 ans chez l'adulte et environ 70 à 80 % chez l'enfant [3]. Dans ce contexte, l'identification de biomarqueurs susceptibles d'être utilisés pour la mise au point de thérapies ciblées représente un enjeu particulièrement important. Réarrangements V(D)J du TCR et différenciation des thymocytesL'oncogenèse des LAL-T est multigé-nique, avec coexistence de plusieurs dérégulations oncogéniques chez le même patient [4]. Parmi les sousgroupes identifiés, figure l'important groupe TLX marqué par la surexpression des oncogènes TLX1 ou TLX3. Ces gènes se caractérisent par la pré-sence d'une séquence d'ADN particulière, appelée homeobox, qui code pour un domaine protéique conservé ou homéodomaine, de structure hélice-tour-hélice. Cette structure a la propriété de se lier à l'ADN et d'interagir avec des protéines partenaires. Les facteurs de transcription à homéodomaine sont généralement impliqués dans l'organogenèse, la maintenance de l'homéostasie des tissus. Ils participent au contrôle de multiples fonctions cellulaires dont la croissance, la prolifération et l'apoptose [5]

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Age-related phenotypic and oncogenic differences in T-cell acute lymphoblastic leukemias may reflect thymic atrophy

Cited by 93 publications

References 58 publications

Dysregulated expression of mitotic regulators is associated with B-cell lymphomagenesis in HOX11-transgenic mice

Dysregulated expression of mitotic regulators is associated with B-cell lymphomagenesis in HOX11-transgenic mice

Thymic adult T-cell acute lymphoblastic leukemia stratified in standard- and high-risk group by aberrant HOX11L2 expression: experience of the German multicenter ALL study group

Mécanisme d’action des oncogènes à homéodomaine TLX dans les LAL-T

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