Difference between revisions of "HAEM5:High grade B-cell lymphoma with 11q aberrations"

Haematolymphoid Tumours (WHO Classification, 5th ed.)

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editContent Update To WHO 5th Edition Classification Is In Process; Content Below is Based on WHO 4th Edition Classification

This page was converted to the new template on 2023-12-07. The original page can be found at HAEM4:Burkitt-Like Lymphoma with 11q Aberration.

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Primary Author(s)*

Lauren Shealy, MD, Medical University of South Carolina

Daynna Wolff, PhD, Medical University of South Carolina

WHO Classification of Disease

Definition / Description of Disease

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Synonyms / Terminology

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Epidemiology / Prevalence

• Males>females, with estimated ratio of 2.75:1 in one cohort^[1]
• Seems to have no racial predilection
• Increased incidence in post-transplant/immunodeficient individuals^[2], but never EBV-associated^{[1] [3]}
• Immunodeficiency can be congenital, HIV-associated, or iatrogenic in setting of transplant^{[3] [4]}
• Age range: 4^[1]-82^[5]
  • median age: 13.9 in a study limited to pediatric patient cohort ^[6], 49.5^[7]
  • mean age: 15^[8],15.5^[1]

Clinical Features

Sites of Involvement

• Nodal involvement ^[8]
  • cervical and abdominal lymphadenopathy predominant, with axillary, inguinal, tonsillar, and submandibular less commonly reported ^{[3] [1] [2] [8] [9]}
  • less common sites such as testes, parotid reported in association with immunodeficient patients ^[3]
• Rare bone marrow involvement^[10]
• CNS involvement is rare ^{[3] [1] [2] [8] [9]}

Morphologic Features

• Medium to large sheets of B-cells frequently with starry-sky background
• Diverse, having been morphologically classified as the following: ^{[6] [8]}
  • BLL, including atypical
  • HGBCL, NOS
  • DLBCL

• Course and increased number of apoptotic bodies (5-9) per macrophage^[7]
• Cytologic features often more blastoid ^[8]

Immunophenotype

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editv4:Immunophenotype

The content below was from the previous version of the page. Please incorporate above.

Flow Findings	Marker
Positive (universal)	CD10, CD20, CD19, CD22, BCL6 [9]
Positive (subset)	CD16/CD56 (present in 60%), CD8 (present in 40%) [9]
Negative (universal)	CD5, CD11C, CD23, CD200, BCL2 [9]
Negative (subset)	CD38 bright (absent 90%) [9]

Statistically significant differences in flow cytometry of BLL11q as compared to myc-positive Burkitt Lymphoma:^[9]

• less frequent CD45 depression ^[9]
• less frequent CD38 bright expression (10% as opposed to 91% in myc-postive BL) ^[9]
• CD16/CD56 (NK differentiation) positivity (60% of time as opposed to 0% in myc-positive BL) ^[9]
• CD 8 expression (40% as opposed to 4% in myc-positive BL) ^[9]

Immunohistochemistry:

• GCB phenotype ^{[6] [7][8]}

• Ki67 usually >90% ^{[6] [9][8] [1] [7]}
• LMO2 expression (46% to 70% as compared to 0% in myc-positive BL)^[8][9]
• MYC may be positive if using a 40% MYC^[8]

Chromosomal Rearrangements (Gene Fusions)

BLL-11q has no known gene fusions at this time.

Individual Region Genomic Gain / Loss / LOH

The table below represents the smallest reported minimal lost region and smallest reported minimal gain region. Other larger MGR and MLR have been reported.^{[10] [11]}

Characteristic Chromosomal Patterns

• Research up until this point has revealed no conservative breakpoints. ^[12]

Notably, no 1q21 abnormalities were found in myc-negative, 11q positive cases. ^[7][8]

Gene Mutations (SNV / INDEL)

• Studies suggest an overall unique mutational profile, with little to no overlap with commonly mutated genes in DLCBL and BL, respectively. Notably, recurrent mutations in BL such as ID3, TCF3, and CCND3 were not present. ^{[8] [14]}
• Mutations listed below where noted to be recurrent in BLL-11q cases. Bold genes have also been found recurrently mutated in DLCBL.
  • DDX3X^[8][14]
  • ETS1 coding mutations located a DNA-binding domain, combined with lower RNA expression in BLL-11q cases ^[8]
  • 7/15 cases showed mutations in GNA13^[14]
  • FOXO1^[14]
  • 3/15 cases showed a Y641 mutational hotspot mutation of EZH2 ^[14]
  • TTN^[14]

Recurrently mutated genes in BLL-11q with known mechanisms that may contribute to pathogenesis.

Note: A more extensive list of mutations can be found in cBioportal (https://www.cbioportal.org/), COSMIC (https://cancer.sanger.ac.uk/cosmic), ICGC (https://dcc.icgc.org/) and/or other databases. When applicable, gene-specific pages within the CCGA site directly link to pertinent external content.

Epigenomic Alterations

• KMT2A has been found to be duplicated and occasionally amplified in numerous cases of BLL-11q^[12]
  • functions to methylate histones^[15]
• Found to have mutations in EP300, HIST1H1D, HIST1H2BC, CREBBP, KMT2C, EZH2, ARID1A, KMT2D^[8]

Genes and Main Pathways Involved

• Given the notable variations in size of the duplicated and deleted regions of BLL-11q, pathogenesis appears to be complex and remains to be elucidated. Still, it is presumed to be a a product of dosage effects produced by the more varied proximal duplications and more consistent terminal deletions.^[12]
• Genes found recurrently in minimal duplication region: IL10RA; TMPRSS4; SCN4B; AMICA1; MPZL3; CD3E; CD3D; UBE4A; ATP5L; KMT2A; TTC36, TMEM25, IFT46; ARCN1 ^{[10] [12]}
• Genes found recurrently in terminal deleted region: ETS1; FLT1; KCNJ5; C11orf45; TP53AIP1 ^{[10] [12]}
  • ETS1 and FLT1 are candidate tumor supressor genes thought to be involved in the pathogenesis of DLBCL ^{[10] [16]}

GENES with PROPOSED/KNOWN CANCER ASSOCIATIONS

Genetic Diagnostic Testing Methods

• Conventional cytogenetics (karyotyping) + FISH using MYC break-apart probe to rule out MYC translocation ^{[13] [3]}
• Chromosomal microarray analysis ^{[8] [3]}

Familial Forms

• None known

Additional Information

Put your text here

Links

HAEM5:Burkitt lymphoma

References

Notes

*Primary authors will typically be those that initially create and complete the content of a page.  If a subsequent user modifies the content and feels the effort put forth is of high enough significance to warrant listing in the authorship section, please contact the CCGA coordinators (contact information provided on the homepage).  Additional global feedback or concerns are also welcome.

*Citation of this Page: “High grade B-cell lymphoma with 11q aberrations”. Compendium of Cancer Genome Aberrations (CCGA), Cancer Genomics Consortium (CGC), updated 09/6/2024, https://ccga.io/index.php/HAEM5:High_grade_B-cell_lymphoma_with_11q_aberrations.

Other Sections

Cancer Sub-Classification/Subtype

Burkitt-like lymphoma with 11q aberration

Definition/Description of Disease

Rare aggressive mature B-cell lymphoma

Synonyms/Terminology

myc-negative Burkitt-like lymphoma (mnBLL, 11q)^[1]

non-myc Burkitt-like lymphoma (nmBLL)

BLL, 11q ^[2]

BLL-11q^[3]HAEM5:Burkitt lymphoma

Clinical Implications

• Look for 11q aberration if Myc negative lymphoma with morphology reminiscent of BL, DLBCL, or HGBCL ^[3]
• Attend to associated chromosomal and mutational abnormalities of other aggressive B-cell lymphomas, ensuring their absence before diagnosis of BLL-11q, since BLL-11q may represent ^{[2] [4] [5]}
• BLL-11q patients treated with R-CHOP (DLBCL treatment) have a higher risk of relapse than those treated with traditional BL treatment ^{[6] [7]}

Tentatively appears to portend a better prognosis with high likelihood of years of remission ^{[3] [8] [6][2]}

• 100% 2 year event free survival in pediatric cohort^[9]