Acute myeloid leukaemia with 8p11 (MYST3) rearrangement: an integrated cytologic, cytogenetic and molecular study by the groupe francophone de cytogénétique hématologique

Gervais, Carine; Murati, Anne; Hélias, Catherine; Struski, Stéphanie; Eischen, Alice; Lippert, Éric; Tigaud, Isabelle; Penther, Dominique; Bastard, Christian; Mugneret, Francine; Poppe, B; Speleman, Frank; Talmant, Pascaline; Akker, J. Vanden; Baranger, Laurence; Barin, Carole; Luquet, Isabelle; Nadal, Nathalie; Nguyen‐Khac, Florence; Maarek, Odile; Herens, Christian; Sainty, Danielle; Flandrin, Georges; Birnbaum, Daniel; Mj, Mozziconacci; Lessard, Michel

doi:10.1038/leu.2008.128

Cited by 65 publications

(80 citation statements)

References 37 publications

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“…44,45 With respect to the gender distribution, female patients represented 69% in our series (9/13 patients) which is supporting data from a previous study where 67% of cases were women. 9 We further could confirm the poor prognosis reported previously, 34,35,[44][45][46] as patients from our series demonstrated a median survival of 4.7 months only. For some part this negative outcome might be explained by the high incidence of t-AML cases in cases of t(8;16) with 54% in our cohort.…”

Section: Gene Expression Profiling In Aml With T(8;16) T Haferlach Et Alsupporting

confidence: 79%

“…As has been previously reported, 9 all cases examined in our series expressed the myeloid markers MPO, CD33, CD13, CD65 and CD15, but lacked the expression of the progenitor cell markers CD34, CD117 and CD133 (Supplementary Table 2). Furthermore, these cases displayed an expression pattern of the monocytic antigens CD14, CD64, CD11b as well as a coexpression of CD56 and CD4.…”

Section: Cytomorphology Cytogenetics Rt-pcr and Immunophenotypesupporting

confidence: 50%

“…We were able to add 13 new cases to the so far less than 100 reported cases in the Mitelman database (http://cgap.nci.nih.gov/Chromosomes/ Mitelman). 9 Also in our series of AML, the t(8;16) was observed to be very rare, that is, 0.2% of all cases in this study, compared to 0.4% according to Mitelman et al, 43 but its incidence in therapy-related AML was confirmed to be significantly higher, that is, 1.6% in this study. This is in line with data that described for many therapy-induced cases of the t(8;16) subtype the association to previous therapy with alkylating drugs in combination with topoisomerase-II-inhibitors, for example, anthracyclines or epipodophyllotoxins.…”

Section: Gene Expression Profiling In Aml With T(8;16) T Haferlach Et Almentioning

confidence: 42%

“…This rare translocation with less than 100 cases described so far, 9 is characterized by disruption and fusion of MYST3 (alias MOZ) and CREBBP (alias CBP) genes. MYST3 is localized on 8p11 and encodes the monocytic leukemia zinc finger protein, a histone acetyltransferase of the MYST family that modulates gene transcription through activation of the AML1 transcription factor complex.…”

Section: Introductionmentioning

confidence: 99%

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AML with translocation t(8;16)(p11;p13) demonstrates unique cytomorphological, cytogenetic, molecular and prognostic features

et al. 2009

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Balanced chromosomal rearrangements define distinct entities in acute myeloid leukemia (AML). Here, we present 13 AML cases with t(8;16)(p11;p13) with observed low incidence (13/6124 patients), but more frequent presentation in therapyrelated AML than in de novo AML (7/438 versus 6/5686, P ¼ 0.00001). Prognosis was poor with median overall survival of 4.7 months. Cytomorphology was characterized by parallel positive myeloperoxidase and non-specific esterase staining, therefore, French-American-British (FAB)-classification was impossible and origin of the AML with t(8;16) from an early stem cell with myeloid and monoblastic potential is hypothesized. Erythrophagocytosis was observed in 7/13 cases. Using gene expression profiling on 407 cases, patients with t(8;16) were compared to AML FAB subtypes with normal karyotype. Principal component analyses demonstrated that AML with t(8;16) were distinct from FAB subtypes M1, M4, M5a/b. When further compared to AML showing balanced rearrangements, that is, current WHO categories t(15;17), t(8;21), inv(16) and t(11q23)/MLL, AML with t(8;16) cases were clustered close to t(11q23)/MLL sharing commonly expressed genes. Subsequently, a pairwise comparison discriminated AML with t(8;16) from AML with t(11q23)/MLL, thus defining a highly unique signature for AML with t(8;16). In conclusion, AML with t(8;16) demonstrates unique cytomorphological, cytogenetic, molecular and prognostic features and is a specific subtype of AML.

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Section: Gene Expression Profiling In Aml With T(8;16) T Haferlach Et Alsupporting

confidence: 79%

Section: Cytomorphology Cytogenetics Rt-pcr and Immunophenotypesupporting

confidence: 50%

Section: Gene Expression Profiling In Aml With T(8;16) T Haferlach Et Almentioning

confidence: 42%

Section: Introductionmentioning

confidence: 99%

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AML with translocation t(8;16)(p11;p13) demonstrates unique cytomorphological, cytogenetic, molecular and prognostic features

et al. 2009

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“…90 So far, survival of a few months only was reported in most cases of MYST-rearranged AML, 87 and none of four patients reported by Quesnel et al 91 achieved CR after standard chemotherapy. Gervais et al 92 reported a mortality rate of 50% in the so far largest study of 30 cases with MYST3/8p11 rearrangements. Successful allo-SCT was reported in one case by Demuynck et al 93 Although the rare occurrence of the translocation has to be seen, there seems to be a clear indication to allo-SCT in the t(8;16).…”

Section: Cytogeneticsmentioning

confidence: 99%

Interactive diagnostics in the indication to allogeneic SCT in AML

Bacher

Haferlach

Schnittger

et al. 2009

Bone Marrow Transplant

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Owing to the heterogeneity of AML, the indication for allogeneic SCT (allo-SCT) requires an exact definition of the individual subentity and risk category. A comprehensive diagnostic approach is needed, which combines cytomorphology, cytogenetics, FISH, molecular genetics and immunophenotyping. Whereas the categorization in three prognostic karyotype groups is well established, rare recurrent aberrations as the unfavorable t(8;16)(p11;p13), inv(3)(q21q26) and t(6;9)(p23;q34) must also be considered. In normal karyotype, PCR analyses reveal prognostically relevant mutations in 485% of cases, and a molecular data set composed of the FLT3-ITD, MLL-PTD, NPM1 and CEBPA mutations was found able to guide the selection of patients for allo-SCT. Some novel markers as the WT1 mutations might further contribute to risk stratification in normal karyotype. The panel of minimal residual disease parameters is being expanded at this time, for example, by quantitative PCR for the NPM1 mutations. Immunophenotyping allows the definition of leukemia-associated phenotypes in nearly all cases, but its position in the indication to allo-SCT has to be validated. Thus, the optimization of the indication to allo-SCT is an ongoing process that should remain in continuous interaction with the increasing panel of known genetic markers and diagnostic methods.

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From chromosomes to genes

Panagopoulos¹

2015

Cancer Cytogenetics

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Acute myeloid leukaemia with 8p11 (MYST3) rearrangement: an integrated cytologic, cytogenetic and molecular study by the groupe francophone de cytogénétique hématologique

Cited by 65 publications

References 37 publications

AML with translocation t(8;16)(p11;p13) demonstrates unique cytomorphological, cytogenetic, molecular and prognostic features

AML with translocation t(8;16)(p11;p13) demonstrates unique cytomorphological, cytogenetic, molecular and prognostic features

Interactive diagnostics in the indication to allogeneic SCT in AML

From chromosomes to genes

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