Simplified algorithm for genetic subtyping in diffuse large B-cell lymphoma

Shen, Rong; Fu, Di; Dong, Lei; Zhang, Muchen; Shi, Qingqing; Shi, Zi-Yang; Cheng, Shu; Wang, Li; Xu, Pengpeng; Zhao, Wei‐Li

doi:10.1038/s41392-023-01358-y

Cited by 20 publications

(30 citation statements)

References 48 publications

(103 reference statements)

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“…13 In the era of immunochemotherapy, non-GCB DLBCL, a high IPI score and MCD-like subtype are all predictors of a poor prognosis for patients with DLBCL. [23][24][25][26][27] Our study suggests that a therapeutic regimen containing BTKis, compared with the standard regimen, can significantly improve the CRR in DLBCL patients with the above high-risk factors. A subgroup analysis of 18 patients in the BTKi + R-CHOP treatment group suggested that there were no statistically significant differences in ORR, CRR and PFS between GCB versus non-GCB DLBCL, non-DEL versus DEL or IPI ≥3 versus <3.…”

Section: Discussionmentioning

confidence: 70%

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A single‐centre, real‐world study of BTK inhibitors for the initial treatment of MYD88^mut/CD79B^mut diffuse large B‐cell lymphoma

Deng,

Zhang,

Xiao

et al. 2024

Cancer Medicine

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BackgroundMCD (MYD88L265P/CD79Bmut) diffuse large B‐cell lymphoma has a poor prognosis. There is no published clinical research conclusion regarding zanubrutinib or orelabrutinib for the initial treatment of MCD DLBCL.AimsThis study aimed to analyse the efficacy and safety of Bruton's tyrosine kinase inhibitor (BTKi) (zanubrutinib or orelabrutinib) therapy for newly diagnosed DLBCL patients with MYD88mut and/or CD79Bmut.Materials and MethodsTwenty‐three newly diagnosed DLBCL patients with MYD88mut and/or CD79Bmut from June 2020 to June 2022 received BTKi combined with rituximab plus cyclophosphamide, doxorubicin, vincristine and prednisone (R‐CHOP) or rituximab + lenalidomide (R2). A control group of 17 patients with MYD88mut and/or CD79Bmut DLBCL who received the standard R‐CHOP therapy was also assessed. We retrospectively analysed clinical characteristics, safety, overall response rate (ORR), complete response (CR) rate and progression‐free survival (PFS) of the two groups.ResultsThe main clinical features were a high International Prognostic Index (IPI) score (≥3, 22/40, 55%) and a high rate of extranodal involvement (27/40,67.5%). Among the 23 DLBCL patients, 18 received BTKi + R‐CHOP, and five elderly DLBCL patients were treated with BTKi + R2. Compared with those in the control group (ORR 70.6%, CRR 52.9%, 1‐year PFS rate 41.2%), improved ORR, CRR and PFS results were observed in the BTKi + R‐CHOP group (100%, 94.4% and 88.9%, p = 0.019, 0.007, and 0.0001). In subgroup analyses based on genetic subtypes, cell origin, dual expression or IPI score, patients in the BTKi + R‐CHOP group had better PFS than patients in the control group. In the BTKi + R‐CHOP group, no significant difference was found in ORR, CRR and PFS based on subtype analysis, while BTKi‐type subgroups exhibited statistically significant differences in 1‐year PFS (p = 0.028). There were no significant differences in grade 3–4 haematological toxicity (p = 1) and grade 3–4 non‐haematological toxicity (p = 0.49) between the BTKi + R‐CHOP and R‐CHOP treatment groups. In the BTKi + R2 group, the ORR was 100%, the CRR was 80%, and the 1‐year PFS rate was 80%. The incidences of grade 3–4 haematologic toxicity and non‐haematological toxicity were both 40%. No bleeding or cardiovascular events of grade 3 or higher occurred in any patients.DiscussionThe efficacy of BTKi combined with R‐CHOP was similar to previous reports, which was significantly better than R‐CHOP alone. It is necessary to fully consider that 14 patients in the BTKi + R‐CHOP group received a BTKi as maintenance therapy when evaluating efficacy. Meanwhile, the addition of a BTKi may improve the prognosis of non‐GCB, DEL or high‐IPI‐score DLBCL patients with MYD88mut and/or CD79Bmut. In our study, five elderly DLBCL patients with MYD88mut and/or CD79Bmut were achieved better ORR, CRR, PFS than the historical data of R‐miniCHOP treatment and Ibrutinib + R2 treatment. However, the efficacy and benefit of BTKis for this type of DLBCL need to be further analysed using a larger sample size.ConclusionThis study suggests that newly diagnosed DLBCL patients with MYD88mut and/or CD79Bmut may benefit from BTKis according to real‐world clinical data.

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Section: Discussionmentioning

confidence: 70%

“…Based on NGS and FISH results, the MCD-like, ST2-like, BN2-like, TP53mut subtypes were defined using the LymphPlex classification tool. 23 The last follow-up was on June 30, 2023.…”

Section: Patient Characteristicsmentioning

confidence: 99%

A single‐centre, real‐world study of BTK inhibitors for the initial treatment of MYD88^mut/CD79B^mut diffuse large B‐cell lymphoma

Deng,

Zhang,

Xiao

et al. 2024

Cancer Medicine

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“…A homemade pipeline was used to filter indels and SNVs detected by the above software 25 based on the following criteria: (1) variants with a mapping quality >30 were retained; (2) SNVs or indels with a mutation allele frequency <0.001 in the 1000 Genomes Project, ExAC-ALL, or ExAC East Asian databases were retained 26 ; (3) SNVs or indels with a variant allele frequency ≥1% and a read depth >10 were retained; (4) dbSNP (v147) sites in the COSMIC database were retained 27 ; (5) SNPs or indels, including stopgain, stoploss, frameshift, nonframeshift, and splicing sites, were retained; (6) missense mutations predicted as pathogenic at least by one in silico prediction tool (SIFT, Polyphen2_HDIV, Polyphen2_HVAR, LRT, MutationTaster, MutationAssessor, FATHMM, PROVEAN, FATHMM-MKL_coding, MetaSVM, or MetaLR) were retained; and 7 duplicate frameshift mutations in multiple samples, variants found in repetitive regions, and variants found in regions with poor coverage were excluded. Because the paired normal samples were not sequenced, all nonsilent SNVs/ indels yielded from the filtering pipeline were manually reviewed (see Table S2).…”

Section: Massive Parallel Sequencing and Variant Callingmentioning

confidence: 99%

The genetic landscape of histologically transformed marginal zone lymphomas

Li,

Yi,

Deng

et al. 2023

Cancer

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BackgroundMarginal zone lymphomas (MZLs) comprise a diverse group of indolent lymphoproliferative disorders; however, some patients develop histologic transformation (HT) with rapid progression to aggressive lymphoma.MethodsForty‐three MZLs with HT (HT‐MZLs), 535 MZLs, and 174 de novo diffuse large B‐cell lymphomas (DLBCLs) without rearrangements of MYC, BCL2, and BCL6 were collected. Among these, 22 HT‐MZLs, 39 MZLs, and 174 DLBCLs were subjected to 148‐gene targeted exome sequencing. The clinicopathologic features of patients who had HT‐MZL and their genetic alterations were compared with those of patients who had MZLs and DLBCLs.ResultsAll 43 HT‐MZLs corresponded to DLBCLs. No HT‐MZLs harbored BCL2 and MYC and/or BCL6 rearrangements. Bone marrow involvement and higher levels of lactate dehydrogenase were significantly more common in HT‐MZLs than in MZLs. Furthermore, upregulated BCL6, MUM1, C‐MYC, and Ki‐67 expression was observed more frequently in HT‐MZLs than in MZLs. TBL1XR1 was the most frequently altered gene (63.6%) in HT‐MZLs, followed by CCND3 (31.8%), CARD11, ID3, and TP53 (22.7%). A trend toward worse progression‐free survival in patients with TBL1XR1 mutations was observed. Compared with MZLs and non–germinal center B‐cell (GCB) type DLBCLs, significantly higher frequencies of TBL1XR1 and ID3 mutations were identified in HT‐MZLs. PIM1 mutations frequently occurred in DLBCLs and were significantly associated with TBL1XR1 mutations but were mutated less in HT‐MZLs that had TBL1XR1 mutations.ConclusionsThe current findings reveal the clinicopathologic and genetic features of HT‐MZLs, suggesting that these tumors might constitute a group distinct from MZL and de novo non–GCB type DLBCL. TBL1XR1 mutations may be considered a predictor of HT in MZL.

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“…The three antibodies CD10, BCL6, and MUM1 are used by Han's algorithm to classify DLBCL into germinal center B-cell-like (GCB) and nonGCB, which enables physicians to determine the prognosis of DLBCL patients (Alizadeh et al, 2000;Rosenwald et al, 2002). Next-generation sequencing was used to assess the genetic landscape of DLBCL (Chapuy et al, 2018;Schmitz et al, 2018;Shen et al, 2023;Wright et al, 2020). The LymphGen algorithm identi es seven distinct genetic subtypes, which is wildly acceptable, including MCD, BN2, N1, EZB-MYC +/− , ST2, and A53 (Shen et al, 2023).…”

Section: Introductionmentioning

confidence: 99%

“…Next-generation sequencing was used to assess the genetic landscape of DLBCL (Chapuy et al, 2018;Schmitz et al, 2018;Shen et al, 2023;Wright et al, 2020). The LymphGen algorithm identi es seven distinct genetic subtypes, which is wildly acceptable, including MCD, BN2, N1, EZB-MYC +/− , ST2, and A53 (Shen et al, 2023). Recently, a simpli ed 38-gene algorithm (termed 'LymphPlex') based on the information on mutations of 35 genes and rearrangements of three genes were established (Schmitz et al, 2018).…”

Section: Introductionmentioning

confidence: 99%

Genetic landscape and prognostic value of IRF4 alterations in Diffuse large B-cell lymphoma patients

Qin,

Chen,

Xie

et al. 2024

Preprint

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Objective: Diffuse large B-cell lymphoma (DLBCL) is the most common B-cell NHL with high heterogeneity. Patients with IRF4 alterations in various hematologic malignancies have a different prognosis. Methods: From January 1st, 2006 to December 31st, 2022, all enrolled novel DLBCL patients treated with R-CHOP or R-CHOP-like regimens underwent high-resolution sequencing based on probe capture, immunohistochemistry and fluorescence in situ hybridization. Publicity datasets were used to validate. Differential expression gene and connectivity map (CMap) analysis were used to screen the potential drugs to improve the clinical outcome. Results: By April 28th, 2023, 324 patients were enrolled, 164 had disease progressed or recurrence, while 160 hadn’t. The number of patients in each group who had mutations in TP53, MYD88, BCL2, IRF4, STAT3, BCOR, ID3, and CD79A varied significantly. TP53 and IRF4 mutations (mPFS of mutation vs. wildtype: 33.93 vs. 11.17 months, p=0.018, HR:0.60, 95%CI:0.35-1.01) were found to be significantly associated with poor survival, according to univariate and multivariable analysis. Subgroup analysis showed that for IRF4mut GCB/nonGCB and IRF4wt GCB/nonGCB patients had significantly different PFS (p=0.002, HR:2.92, 95%CI: 1.05-8.10). Pairwise comparisons analysis show that the IRF4mutnonGCB subtype is significantly associated with shorter PFS in both our cohort and validation cohort (p=0.001). According to CMap , IRF4mut patients may benefit from regimens containing lenalidomide, ibrutinib, or mitoxantrone as first- and subsequent-line treatment options. Conclusions: This study comprehensively described the genetic landscape of novel DLBCL. IRF4 mutation is an independent prognostic factor in DLBCL patients, and PFS is significantly shortened in IRF4mut nonGCB DLBCL subtype.

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Simplified algorithm for genetic subtyping in diffuse large B-cell lymphoma

Cited by 20 publications

References 48 publications

A single‐centre, real‐world study of BTK inhibitors for the initial treatment of MYD88^mut/CD79B^mut diffuse large B‐cell lymphoma

A single‐centre, real‐world study of BTK inhibitors for the initial treatment of MYD88^mut/CD79B^mut diffuse large B‐cell lymphoma

The genetic landscape of histologically transformed marginal zone lymphomas

Genetic landscape and prognostic value of IRF4 alterations in Diffuse large B-cell lymphoma patients

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Simplified algorithm for genetic subtyping in diffuse large B-cell lymphoma

Cited by 20 publications

References 48 publications

A single‐centre, real‐world study of BTK inhibitors for the initial treatment of MYD88mut/CD79Bmut diffuse large B‐cell lymphoma

A single‐centre, real‐world study of BTK inhibitors for the initial treatment of MYD88mut/CD79Bmut diffuse large B‐cell lymphoma

The genetic landscape of histologically transformed marginal zone lymphomas

Genetic landscape and prognostic value of IRF4 alterations in Diffuse large B-cell lymphoma patients

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A single‐centre, real‐world study of BTK inhibitors for the initial treatment of MYD88^mut/CD79B^mut diffuse large B‐cell lymphoma

A single‐centre, real‐world study of BTK inhibitors for the initial treatment of MYD88^mut/CD79B^mut diffuse large B‐cell lymphoma