<i>MYC</i> translocation‐negative classical Burkitt lymphoma cases: an alternative pathogenetic mechanism involving miRNA deregulation

Leucci, Eleonora; Cocco, Mario; Onnis, Anna; Falco, Giulia De; Cleef, Patricia van; Bellan, Cristiana; Rijk, Anke van; Nyagol, Joshua; Byakika, B; Lazzi, Stefano; Tosi, Piero; Krieken, J. Han van; Leoncini, Lorenzo

doi:10.1002/path.2410

Cited by 178 publications

(131 citation statements)

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“…14 In addition, rare cases that are otherwise characteristic of Burkitt lymphoma but lack MYC-IG rearrangement are acceptable for Burkitt lymphoma as these cases bear a Burkitt-like molecular signature, 13,14 and may upregulate MYC expression by alternative mechanisms possibly involving the modulation of microRNA. 22 Although the new diagnostic criteria are clearly outlined, the practical application is not always straightforward. For example, cases with features slightly deviating from the typical medium-sized monomorphous cytomorphology may be acceptable for Burkitt lymphoma, 14 whereas cases with greater cytomorphological variations would be classified as unclassifiable or diffuse large B-cell lymphoma.…”

Section: Discussionmentioning

confidence: 99%

Simple karyotype and bcl-6 expression predict a diagnosis of Burkitt lymphoma and better survival in IG-MYC rearranged high-grade B-cell lymphomas

et al. 2010

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Rearrangement of MYC with immunoglobulin genes is a hallmark of Burkitt lymphoma. However, this rearrangement is not entirely specific and is often accompanied by varying numbers of additional cytogenetic abnormalities. This study aimed to assess the impact of karyotypic complexity, in correlation with comprehensive immunophenotypic analyses on the diagnosis and clinical outcomes of 34 cases of MYC-IG rearranged lymphomas that included Burkitt lymphoma (twenty-two cases), diffuse large B-cell lymphoma (three cases), unclassifiable B-cell lymphoma with features intermediate between diffuse large B-cell lymphoma and Burkitt lymphoma (six cases), and plasmablastic lymphoma (three cases). Additional cytogenetic abnormalities were observed in 26 of 34 cases (76%), including four cases (12%) that harbored dual translocations involving BCL-2 or BCl-6. Burkitt lymphoma cases had a significantly lower number of additional abnormalities (mean of 1.7), compared with unclassified B-cell lymphoma (3.3), diffuse large B-cell lymphoma (21.7), and plasmablastic lymphoma (6.7). Cases with simple karyotype (p2 additional abnormalities) were more likely to have a diagnosis of Burkitt lymphoma (89 versus 33% in patients with 42 additional abnormalities, Po0.01) and express bcl-6 (95 versus 47%, Po0.01). In addition, Burkitt lymphoma, bcl-6 expression, and simple karyotype were individual predictors of better overall survival. However, in multivariate analyses, only bcl-6 expression remained an independent predictor, although survival could be further stratified by karyotypic complexity in bcl-6( þ ) patients. We conclude that simple karyotype and bcl-6 expression suggest a diagnosis of Burkitt lymphoma and may portend better overall survival. These results may be very useful in the diagnosis and stratification of MYC-IG rearranged high-grade B-cell lymphomas.

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Section: Discussionmentioning

confidence: 99%

Simple karyotype and bcl-6 expression predict a diagnosis of Burkitt lymphoma and better survival in IG-MYC rearranged high-grade B-cell lymphomas

et al. 2010

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“…Others have shown that classic Burkitt morphological features with a very high proliferation fraction should still be considered as a BL, even when there is a negative MYC translocation. 24 This group has found an alternative mechanism of c-MYC upregulation in these rare negative cases not identified by the commercial FISH probes. 24 Moreover, studies have shown that those cases morphologically diagnosed BL, with a very high proliferation index and negative c-MYC, who were treated with less aggressive chemotherapy for a DLBCL, tended to have worse outcomes.…”

Section: Discussionmentioning

confidence: 99%

Post‐transplant Burkitt lymphoma is a more aggressive and distinct form of post‐transplant lymphoproliferative disorder

Picarsic

Jaffe

Mazariegos

et al. 2011

Cancer

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BACKGROUND:Although the literature reports a low incidence of Burkitt lymphoma (BL) as a post‐transplant lymphoproliferative disorder (PTLD), this entity appears to be different from other monomorphic PTLDs (M‐PTLDs), both in its aggressive clinical presentation and its distinct pathologic profile.METHODS:Patients with BL, diagnosed in the post‐transplant setting, (patients aged ≤18 years) were retrieved from the pathology archives at Children's Hospital of Pittsburgh of the University of Pittsburgh Medical Center from 1982 to 2010. Clinical outcomes were obtained along with pathologic review.RESULTS:Twelve patients with pediatric BL in the post‐transplant setting (9 boys, 3 girls) were retrieved. The patients displayed a monomorphic population of small to intermediate‐sized, noncleaved, lymphoid elements with a “starry‐sky” pattern. The immunophenotype for patients available to the study was CD20+ (n = 9/10), CD10+ (n = 8/8), bcl‐6+ (n = 11/11), with a near 100% Ki‐67/MIB‐1 proliferation index (n = 7/7), and negative for TdT (n = 7/7). Most pretransplant Epstein‐Barr virus titers were negative (n = 8/10), with post‐transplant titers positive in all tested patients (n = 11), and with positive Epstein‐Barr–encoded RNA in situ hybridization in most cases (n = 9/11). The median time from transplantation to diagnosis was 52 months (range, 6‐107 months). Nine patients were currently alive after immediate antineoplastic chemotherapy, with median disease‐free time of 93 months from diagnosis (range, 2‐199 months).CONCLUSIONS:BL‐PTLD had a higher Epstein‐Barr virus incidence compared with sporadic and immunodeficiency‐associated BL and represented a distinct monomorphic PTLD. Although some M‐PTLDs can be managed less aggressively with decreased immunosuppression alone, immediate lymphoma‐specific chemotherapy was associated with a favorable outcome and was strongly recommended. Cancer 2011;. © 2011 American Cancer Society.

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“…An example is c-MYC, which seems to be regulated mainly by miR-34b/c. 53,54,46 This can presumably be explained by the enhanced complementarity between the miR-34b seed sequence and the seed-matching sequence in the c-MYC 3 0 -UTR, when compared with miR-34a (Table 1; Figure 2b). The induction of miR-34 genes allows p53 to regulate the expression of a large number of proteins, even after their transcripts have already been synthesized.…”

Section: Btg4mentioning

confidence: 99%

The miR-34 family in cancer and apoptosis

2009

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MYC translocation‐negative classical Burkitt lymphoma cases: an alternative pathogenetic mechanism involving miRNA deregulation

Cited by 178 publications

References 20 publications

Simple karyotype and bcl-6 expression predict a diagnosis of Burkitt lymphoma and better survival in IG-MYC rearranged high-grade B-cell lymphomas

Simple karyotype and bcl-6 expression predict a diagnosis of Burkitt lymphoma and better survival in IG-MYC rearranged high-grade B-cell lymphomas

Post‐transplant Burkitt lymphoma is a more aggressive and distinct form of post‐transplant lymphoproliferative disorder

The miR-34 family in cancer and apoptosis

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