https://orcid.org/0000-0002-7164-3930
Key Points
In patients with follicular lymphoma, both ctDNA and PET positivity after induction response are associated with shorter PFS.
Only combined ctDNA and PET identify patients at high risk of early relapse (POD24), linked to poor survival.
Abstract
Patients with follicular lymphoma who experience disease progression within 24 months of diagnosis (POD24) have a lower survival. Positron emission tomography (PET) response and circulating tumor DNA (ctDNA) minimal residual disease (MRD) assessment at end of induction (EOI) may allow their early identification. A representative cohort of 141 patients from the RELEVANCE phase 3 trial with both available serum samples for ctDNA testing and PET images at randomization and at EOI (week 24) was investigated. Twelve percent were POD24. ctDNA was analyzed using a customized 130-kilobase capture panel, with phased variant (PV) enriched regions representing 39% of the panel. ctDNA was detected in 140 patients (99.3%) at baseline. To optimize specificity, only PVs, found in 124 patients (88%), were considered for ctDNA MRD assessment at EOI. Median progression-free survival (PFS) from EOI was not reached (NR) for the 112 patients with undetected ctDNA at EOI vs 17.7 months (95% confidence interval [CI], 1.4 to NR) for patients with positive ctDNA (MRD+) (P = .0038). Similarly, median PFS was NR for the 104 patients with undetected disease on PET at EOI vs 28.3 months (95% CI, 2.9 to NR; P = .0002) for patients with PET positivity. Both tests had a negative predictive value (NPV) of >90% for POD24. The positive predictive value was 58.3% for ctDNA MRD and 45% for PET but increased to 85.7% when both parameters were combined, without alteration of NPV. These data show that the combination of PET response and ctDNA MRD at EOI allows an early prediction of POD24, which may lead to a preemptive treatment decision. This trial was registered at www.clinicaltrials.gov as #NCT01650701.
References
1.
Bachy
E
, Seymour
JF
, Feugier
P
, et al. Sustained progression-free survival benefit of rituximab maintenance in patients with follicular lymphoma: long-term results of the PRIMA study
. J Clin Oncol
. 2019
;37
(31
):2815
-2824
.2.
Gupta
G
, Garg
V
, Mallick
S
, Gogia
A
. Current trends in diagnosis and management of follicular lymphoma
. Am J Blood Res
. 2022
;12
(4
):105
-124
.3.
Casulo
C
, Dixon
JG
, Le-Rademacher
J
, et al. Validation of POD24 as a robust early clinical end point of poor survival in FL from 5225 patients on 13 clinical trials
. Blood
. 2022
;139
(11
):1684
-1693
.4.
Lansigan
F
, Barak
I
, Pitcher
B
, et al. The prognostic significance of PFS24 in follicular lymphoma following first line immunotherapy: a combined analysis of 3 CALGB trials
. Cancer Med
. 2019
;8
(1
):165
-173
.5.
Casulo
C
, Byrtek
M
, Dawson
KL
, et al. Early relapse of follicular lymphoma after rituximab plus cyclophosphamide, doxorubicin, vincristine, and prednisone defines patients at high risk for death: an analysis from the National LymphoCare Study
. J Clin Oncol
. 2015
;33
(23
):2516
-2522
.6.
Maurer
MJ
, Bachy
E
, Ghesquières
H
, et al. Early event status informs subsequent outcome in newly diagnosed follicular lymphoma
. Am J Hematol
. 2016
;91
(11
):1096
-1101
.7.
Seymour
JF
, Marcus
R
, Davies
A
, et al. Association of early disease progression and very poor survival in the GALLIUM study in follicular lymphoma: benefit of obinutuzumab in reducing the rate of early progression
. Haematologica
. 2019
;104
(6
):1202
-1208
.8.
Moccia
AA
, Schär
S
, Hayoz
S
, et al. Prognostic value of POD24 validation in follicular lymphoma patients initially treated with chemotherapy-free regimens in a pooled analysis of three randomized trials of the Swiss Group for Clinical Cancer Research (SAKK)
. Br J Haematol
. 2021
;192
(6
):1031
-1034
.9.
Solal-Céligny
P
, Roy
P
, Colombat
P
, et al. Follicular Lymphoma International Prognostic Index
. Blood
. 2004
;104
(5
):1258
-1265
.10.
Federico
M
, Bellei
M
, Marcheselli
L
, et al. Follicular Lymphoma International Prognostic Index 2: a new prognostic index for follicular lymphoma developed by the International Follicular Lymphoma Prognostic Factor project
. J Clin Oncol
. 2009
;27
:4555
-4562
.11.
Bachy
E
, Maurer
MJ
, Habermann
TM
, et al. A simplified scoring system in de novo follicular lymphoma treated initially with immunochemotherapy
. Blood
. 2018
;132
(1
):49
-58
.12.
Mir
F
, Mattiello
F
, Grigg
A
, et al. Follicular Lymphoma Evaluation Index (FLEX): a new clinical prognostic model that is superior to existing risk scores for predicting progression-free survival and early treatment failure after frontline immunochemotherapy
. Am J Hematol
. 2020
;95
(12
):1503
-1510
.13.
Pastore
A
, Jurinovic
V
, Kridel
R
, et al. Integration of gene mutations in risk prognostication for patients receiving first-line immunochemotherapy for follicular lymphoma: a retrospective analysis of a prospective clinical trial and validation in a population-based registry
. Lancet Oncol
. 2015
;16
(9
):1111
-1122
.14.
Rodríguez-Sevilla
JJ
, Fernández-Rodríguez
C
, Bento
L
, et al. Evaluation of 4 prognostic indices in follicular lymphoma treated in first line with immunochemotherapy
. Blood Adv
. 2023
;7
(8
):1606
-1614
.15.
Zanoni
L
, Bezzi
D
, Nanni
C
, et al. PET/CT in non-Hodgkin lymphoma: an update
. Semin Nucl Med
. 2023
;53
(3
):320
-351
.16.
Cottereau
AS
, Rebaud
L
, Trotman
J
, et al. Metabolic tumor volume predicts outcome in patients with advanced stage follicular lymphoma from the RELEVANCE trial
. Ann Oncol
. 2024
;35
(1
):130
-137
.17.
Dupuis
J
, Berriolo-Riedinger
A
, Julian
A
, et al. Impact of [(18)F]fluorodeoxyglucose positron emission tomography response evaluation in patients with high-tumor burden follicular lymphoma treated with immunochemotherapy: a prospective study from the Groupe d'Etudes des Lymphomes de l'Adulte and GOELAMS
. J Clin Oncol
. 2012
;30
(35
):4317
-4322
.18.
Trotman
J
, Fournier
M
, Lamy
T
, et al. Positron emission tomography-computed tomography (PET-CT) after induction therapy is highly predictive of patient outcome in follicular lymphoma: analysis of PET-CT in a subset of PRIMA trial participants
. J Clin Oncol
. 2011
;29
(23
):3194
-3200
.19.
Trotman
J
, Luminari
S
, Boussetta
S
, et al. Prognostic value of PET-CT after first-line therapy in patients with follicular lymphoma: a pooled analysis of central scan review in three multicentre studies
. Lancet Haematol
. 2014
;1
(1
):e17
-e27
.20.
Trotman
J
, Barrington
SF
, Belada
D
, et al. Prognostic value of end-of-induction PET response after first-line immunochemotherapy for follicular lymphoma (GALLIUM): secondary analysis of a randomised, phase 3 trial
. Lancet Oncol
. 2018
;19
(11
):1530
-1542
.21.
Roschewski
M
, Rossi
D
, Kurtz
DM
, Alizadeh
AA
, Wilson
WH
. Circulating tumor DNA in lymphoma: principles and future directions
. Blood Cancer Discov
. 2022
;3
(1
):5
-15
.22.
Kurtz
DM
, Scherer
F
, Jin
MC
, et al. Circulating tumor DNA measurements as early outcome predictors in diffuse large B-cell lymphoma
. J Clin Oncol
. 2018
;36
(28
):2845
-2853
.23.
Meriranta
L
, Alkodsi
A
, Pasanen
A
, et al. Molecular features encoded in the ctDNA reveal heterogeneity and predict outcome in high-risk aggressive B-cell lymphoma
. Blood
. 2022
;139
(12
):1863
-1877
.24.
Le Goff
E
, Blanc-Durand
P
, Roulin
L
, et al. Baseline circulating tumour DNA and total metabolic tumour volume as early outcome predictors in aggressive large B-cell lymphoma. A real-world 112-patient cohort
. Br J Haematol
. 2023
;202
(1
):54
-64
.25.
Kurtz
DM
, Soo
J
, Co Ting Keh
L
, et al. Enhanced detection of minimal residual disease by targeted sequencing of phased variants in circulating tumor DNA
. Nat Biotechnol
. 2021
;39
(12
):1537
-1547
.26.
Delfau-Larue
MH
, van der Gucht
A
, Dupuis
J
, et al. Total metabolic tumor volume, circulating tumor cells, cell-free DNA: distinct prognostic value in follicular lymphoma
. Blood Adv
. 2018
;2
(7
):807
-816
.27.
Hatipoğlu
T
, Esmeray Sönmez
E
, Hu
X
, et al. Plasma concentrations and cancer-associated mutations in cell-free circulating DNA of treatment-naive follicular lymphoma for improved non-invasive diagnosis and prognosis
. Front Oncol
. 2022
;12
:870487
.28.
Sarkozy
C
, Huet
S
, Carlton
VEH
, et al. The prognostic value of clonal heterogeneity and quantitative assessment of plasma circulating clonal IG-VDJ sequences at diagnosis in patients with follicular lymphoma
. Oncotarget
. 2017. Jan 31
;8
(5
):8765
-8774
.29.
Yoon
SE
, Shin
SH
, Nam
DK
, Cho
J
, Kim
WS
, Kim
SJ
. Feasibility of circulating tumor DNA analysis in patients with follicular lymphoma
. Cancer Res Treat
. 2024
;56
(3
):920
-935
.30.
Morschhauser
F
, Nastoupil
L
, Feugier
P
, et al. Six-year results from RELEVANCE: lenalidomide plus rituximab-chemotherapy followed by rituximab maintenance in untreated advanced follicular lymphoma
. J Clin Oncol
. 2022
;40
(28
):3239
-3245
.31.
Li
H
, Durbin
R
. Fast and accurate short read alignment with Burrows-Wheeler transform
. Bioinformatics
. 2009
;25
(14
):1754
-1760
.32.
Van der Auwera
GA
, Carneiro
MO
, Hartl
C
, et al. From FastQ data to high confidence variant calls: the Genome Analysis Toolkit best practices pipeline
. Curr Protoc Bioinformatics
. 2013
;43
(1110
):11.10.1
-11.10.33
.33.
Sater
V
, Viailly
PJ
, Lecroq
T
, et al. UMI-Varcal: a low-frequency variant caller for UMI-tagged paired-end sequencing data
. Methods Mol Biol
. 2022
;2493
:235
-245
.34.
Barrington
SF
, Mikhaeel
NG
, Kostakoglu
L
, et al. Role of imaging in the staging and response assessment of lymphoma: consensus of the International Conference on Malignant Lymphomas Imaging Working Group
. J Clin Oncol
. 2014
;32
(27
):3048
-3058
.35.
Cheson
BD
, Fisher
RI
, Barrington
SF
, et al. Recommendations for initial evaluation, staging, and response assessment of Hodgkin and non-Hodgkin lymphoma: the Lugano classification
. J Clin Oncol
. 2014
;32
(27
):3059
-3068
.36.
Jiménez-Ubieto
A
, Poza
M
, Martin-Muñoz
A
, et al. Real-life disease monitoring in follicular lymphoma patients using liquid biopsy ultra-deep sequencing and PET/CT
. Leukemia
. 2023
;37
(3
):659
-669
.37.
Barrington
SF
, Mir
F
, El-Galaly
TC
, et al. Follicular lymphoma treated with first-fine immunochemotherapy: a review of PET/CT in patients who did not achieve a complete metabolic response in the GALLIUM study
. J Nucl Med
. 2022
;63
(8
):1149
-1154
.38.
Pott
C
, Jurinovic
V
, Trotman
J
, et al. Minimal residual disease status predicts outcome in patients with previously untreated follicular lymphoma: a prospective analysis of the phase III GALLIUM study
. J Clin Oncol
. 2024
;42
(5
):550
-561
.39.
Fernández-Miranda
I
, Pedrosa
L
, Llanos
M
, et al. Monitoring of circulating tumor DNA predicts response to treatment and early progression in follicular lymphoma: results of a prospective pilot study
. Clin Cancer Res
. 2023
;29
(1
):209
-220
.© 2025 American Society of Hematology. Published by Elsevier Inc. All rights are reserved, including those for text and data mining, AI training, and similar technologies.
2025
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