A comprehensive genetic study of classic Hodgkin lymphoma using circulating tumor DNA

M. C. Pirosa; A. Bruscaggin; di Bergamo L. Terzi; M. Salehi; F. Jauk; G. Forestieri; S. Bocchetta; D. Piffaretti; R. Moia; V. Cristaldi; Trani M. di; G. A. Galimberti; K. Pini; V. Spina; C. Giordano; A. Condoluci; I. Romano; S. Annunziata; F. Bergesio; R. Boldorini; E. Borsatti; P. Bulian; E. Calabretta; S. Chauvie; F. Corrado; S. Crisci; M. Cuzzocrea; Filippi R. De; B. Gerber; M. Kurlapski; L. M. Larocca; E. Merlo; A. Rinaldi; M. Rodari; G. Romanowicz; G. M. Sacchetti; A. Stathis; G. Stussi; I. Zangrilli; A. Pinto; L. Mazzucchelli; V. Gattei; J. M. Zaucha; A. Santoro; Stefan Hohaus; F. Cavalli; A. Tzankov; C. Carlo-Stella; G. Gaidano; L. Ceriani; E. Zucca; D. Rossi

doi:10.1182/blood.2024027355

A comprehensive genetic study of classic Hodgkin lymphoma using circulating tumor DNA

M. C. Pirosa
, A. Bruscaggin
, di Bergamo L. Terzi
, M. Salehi
, F. Jauk
, G. Forestieri
, S. Bocchetta
, D. Piffaretti
, R. Moia
, V. Cristaldi
, Trani M. di
, G. A. Galimberti
, K. Pini
, V. Spina
, C. Giordano
, A. Condoluci
, I. Romano
, S. Annunziata
, F. Bergesio
, R. Boldorini

E. Borsatti, P. Bulian, E. Calabretta, S. Chauvie, F. Corrado, S. Crisci, M. Cuzzocrea, Filippi R. De, B. Gerber, M. Kurlapski, L. M. Larocca, E. Merlo, A. Rinaldi, M. Rodari, G. Romanowicz, G. M. Sacchetti, A. Stathis, G. Stussi, I. Zangrilli, A. Pinto, L. Mazzucchelli, V. Gattei, J. M. Zaucha, A. Santoro, Stefan Hohaus, F. Cavalli, A. Tzankov, C. Carlo-Stella, G. Gaidano, L. Ceriani, E. Zucca, D. Rossi^*

^*Autore corrispondente per questo lavoro

Risultato della ricerca: Contributo in rivista › Articolo

Abstract

This study analyzed the genetics of classic Hodgkin lymphoma (cHL) by using circulating tumor DNA (ctDNA). Two genetic subtypes were identified, differing in genetic instability mechanisms: one subtype (64% of cases) showed a higher mutation load and a higher fraction of mutations associated with activation-induced cytidine deaminase and microsatellite instability signatures, whereas the other subtype (36% of cases) exhibited chromosomal instability with more somatic copy number alterations. Whole-genome duplication was more common in cHL compared with other B-cell tumors and emerged as a prognostic biomarker for patients undergoing Adriamycin (doxorubicin)-bleomycin-vinblastine-dacarbazine–based therapy. Noncoding regulatory mutations, similar to those in diffuse large B-cell lymphoma, were highly prevalent in 86% of cHL. A recurrent somatic expression quantitative trait locus (seQTL) involving the BCL6 gene was found in 30% of cases. The seQTL of BCL6 aligned with accessible chromatin and increased H3K27 acetylation in cHL, disrupted PRDM1 binding, and co-occurred with BCL6 expression in cHL cells. Weak to strong expression of BCL6 was observed in 68% of cases, and BCL6 expression associated with gene repression similarly in cHL and germinal center B cells. After BCL6 degradation, the core set of genes directly bound and regulated by BCL6 was derepressed in cHL, and proliferation was impaired. The number and clonality of neoantigens was associated with tumor microenvironment type and response to checkpoint blockade. Finally, ctDNA analysis was suggested as a tool to distinguish ambiguous positron emission tomography/computed tomography–positive lesions after treatment.

Lingua originale	Inglese
pagine (da-a)	1207-1224
Numero di pagine	18
Rivista	Blood
Volume	146
Numero di pubblicazione	10
DOI	https://doi.org/10.1182/blood.2024027355
Stato di pubblicazione	Pubblicato - 2025

All Science Journal Classification (ASJC) codes

Biochimica
Immunologia
Ematologia
Biologia Cellulare

Keywords

lymphoma

OSS delle Nazioni Unite

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10.1182/blood.2024027355

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Pirosa, M. C., Bruscaggin, A., Terzi, D. B. L., Salehi, M., Jauk, F., Forestieri, G., Bocchetta, S., Piffaretti, D., Moia, R., Cristaldi, V., di, T. M., Galimberti, G. A., Pini, K., Spina, V., Giordano, C., Condoluci, A., Romano, I., Annunziata, S., Bergesio, F., ... Rossi, D. (2025). A comprehensive genetic study of classic Hodgkin lymphoma using circulating tumor DNA. Blood, 146(10), 1207-1224. https://doi.org/10.1182/blood.2024027355

@article{72c1544eb93a4351b4e1e40d6d8b6031,

title = "A comprehensive genetic study of classic Hodgkin lymphoma using circulating tumor DNA",

abstract = "This study analyzed the genetics of classic Hodgkin lymphoma (cHL) by using circulating tumor DNA (ctDNA). Two genetic subtypes were identified, differing in genetic instability mechanisms: one subtype (64\% of cases) showed a higher mutation load and a higher fraction of mutations associated with activation-induced cytidine deaminase and microsatellite instability signatures, whereas the other subtype (36\% of cases) exhibited chromosomal instability with more somatic copy number alterations. Whole-genome duplication was more common in cHL compared with other B-cell tumors and emerged as a prognostic biomarker for patients undergoing Adriamycin (doxorubicin)-bleomycin-vinblastine-dacarbazine–based therapy. Noncoding regulatory mutations, similar to those in diffuse large B-cell lymphoma, were highly prevalent in 86\% of cHL. A recurrent somatic expression quantitative trait locus (seQTL) involving the BCL6 gene was found in 30\% of cases. The seQTL of BCL6 aligned with accessible chromatin and increased H3K27 acetylation in cHL, disrupted PRDM1 binding, and co-occurred with BCL6 expression in cHL cells. Weak to strong expression of BCL6 was observed in 68\% of cases, and BCL6 expression associated with gene repression similarly in cHL and germinal center B cells. After BCL6 degradation, the core set of genes directly bound and regulated by BCL6 was derepressed in cHL, and proliferation was impaired. The number and clonality of neoantigens was associated with tumor microenvironment type and response to checkpoint blockade. Finally, ctDNA analysis was suggested as a tool to distinguish ambiguous positron emission tomography/computed tomography–positive lesions after treatment.",

keywords = "lymphoma, lymphoma",

author = "Pirosa, \{M. C.\} and A. Bruscaggin and Terzi, \{di Bergamo L.\} and M. Salehi and F. Jauk and G. Forestieri and S. Bocchetta and D. Piffaretti and R. Moia and V. Cristaldi and di, \{Trani M.\} and Galimberti, \{G. A.\} and K. Pini and V. Spina and C. Giordano and A. Condoluci and I. Romano and S. Annunziata and F. Bergesio and R. Boldorini and E. Borsatti and P. Bulian and E. Calabretta and S. Chauvie and F. Corrado and S. Crisci and M. Cuzzocrea and De, \{Filippi R.\} and B. Gerber and M. Kurlapski and Larocca, \{L. M.\} and E. Merlo and A. Rinaldi and M. Rodari and G. Romanowicz and Sacchetti, \{G. M.\} and A. Stathis and G. Stussi and I. Zangrilli and A. Pinto and L. Mazzucchelli and V. Gattei and Zaucha, \{J. M.\} and A. Santoro and Stefan Hohaus and F. Cavalli and A. Tzankov and C. Carlo-Stella and G. Gaidano and L. Ceriani and E. Zucca and D. Rossi",

year = "2025",

doi = "10.1182/blood.2024027355",

language = "English",

volume = "146",

pages = "1207--1224",

journal = "Blood",

issn = "0006-4971",

publisher = "Elsevier B.V.",

number = "10",

}

Pirosa, MC, Bruscaggin, A, Terzi, DBL, Salehi, M, Jauk, F, Forestieri, G, Bocchetta, S, Piffaretti, D, Moia, R, Cristaldi, V, di, TM, Galimberti, GA, Pini, K, Spina, V, Giordano, C, Condoluci, A, Romano, I, Annunziata, S, Bergesio, F, Boldorini, R, Borsatti, E, Bulian, P, Calabretta, E, Chauvie, S, Corrado, F, Crisci, S, Cuzzocrea, M, De, FR, Gerber, B, Kurlapski, M, Larocca, LM, Merlo, E, Rinaldi, A, Rodari, M, Romanowicz, G, Sacchetti, GM, Stathis, A, Stussi, G, Zangrilli, I, Pinto, A, Mazzucchelli, L, Gattei, V, Zaucha, JM, Santoro, A, Hohaus, S, Cavalli, F, Tzankov, A, Carlo-Stella, C, Gaidano, G, Ceriani, L, Zucca, E & Rossi, D 2025, 'A comprehensive genetic study of classic Hodgkin lymphoma using circulating tumor DNA', Blood, vol. 146, n. 10, pagg. 1207-1224. https://doi.org/10.1182/blood.2024027355

TY - JOUR

T1 - A comprehensive genetic study of classic Hodgkin lymphoma using circulating tumor DNA

AU - Pirosa, M. C.

AU - Bruscaggin, A.

AU - Terzi, di Bergamo L.

AU - Salehi, M.

AU - Jauk, F.

AU - Forestieri, G.

AU - Bocchetta, S.

AU - Piffaretti, D.

AU - Moia, R.

AU - Cristaldi, V.

AU - di, Trani M.

AU - Galimberti, G. A.

AU - Pini, K.

AU - Spina, V.

AU - Giordano, C.

AU - Condoluci, A.

AU - Romano, I.

AU - Annunziata, S.

AU - Bergesio, F.

AU - Boldorini, R.

AU - Borsatti, E.

AU - Bulian, P.

AU - Calabretta, E.

AU - Chauvie, S.

AU - Corrado, F.

AU - Crisci, S.

AU - Cuzzocrea, M.

AU - De, Filippi R.

AU - Gerber, B.

AU - Kurlapski, M.

AU - Larocca, L. M.

AU - Merlo, E.

AU - Rinaldi, A.

AU - Rodari, M.

AU - Romanowicz, G.

AU - Sacchetti, G. M.

AU - Stathis, A.

AU - Stussi, G.

AU - Zangrilli, I.

AU - Pinto, A.

AU - Mazzucchelli, L.

AU - Gattei, V.

AU - Zaucha, J. M.

AU - Santoro, A.

AU - Hohaus, Stefan

AU - Cavalli, F.

AU - Tzankov, A.

AU - Carlo-Stella, C.

AU - Gaidano, G.

AU - Ceriani, L.

AU - Zucca, E.

AU - Rossi, D.

PY - 2025

Y1 - 2025

N2 - This study analyzed the genetics of classic Hodgkin lymphoma (cHL) by using circulating tumor DNA (ctDNA). Two genetic subtypes were identified, differing in genetic instability mechanisms: one subtype (64% of cases) showed a higher mutation load and a higher fraction of mutations associated with activation-induced cytidine deaminase and microsatellite instability signatures, whereas the other subtype (36% of cases) exhibited chromosomal instability with more somatic copy number alterations. Whole-genome duplication was more common in cHL compared with other B-cell tumors and emerged as a prognostic biomarker for patients undergoing Adriamycin (doxorubicin)-bleomycin-vinblastine-dacarbazine–based therapy. Noncoding regulatory mutations, similar to those in diffuse large B-cell lymphoma, were highly prevalent in 86% of cHL. A recurrent somatic expression quantitative trait locus (seQTL) involving the BCL6 gene was found in 30% of cases. The seQTL of BCL6 aligned with accessible chromatin and increased H3K27 acetylation in cHL, disrupted PRDM1 binding, and co-occurred with BCL6 expression in cHL cells. Weak to strong expression of BCL6 was observed in 68% of cases, and BCL6 expression associated with gene repression similarly in cHL and germinal center B cells. After BCL6 degradation, the core set of genes directly bound and regulated by BCL6 was derepressed in cHL, and proliferation was impaired. The number and clonality of neoantigens was associated with tumor microenvironment type and response to checkpoint blockade. Finally, ctDNA analysis was suggested as a tool to distinguish ambiguous positron emission tomography/computed tomography–positive lesions after treatment.

AB - This study analyzed the genetics of classic Hodgkin lymphoma (cHL) by using circulating tumor DNA (ctDNA). Two genetic subtypes were identified, differing in genetic instability mechanisms: one subtype (64% of cases) showed a higher mutation load and a higher fraction of mutations associated with activation-induced cytidine deaminase and microsatellite instability signatures, whereas the other subtype (36% of cases) exhibited chromosomal instability with more somatic copy number alterations. Whole-genome duplication was more common in cHL compared with other B-cell tumors and emerged as a prognostic biomarker for patients undergoing Adriamycin (doxorubicin)-bleomycin-vinblastine-dacarbazine–based therapy. Noncoding regulatory mutations, similar to those in diffuse large B-cell lymphoma, were highly prevalent in 86% of cHL. A recurrent somatic expression quantitative trait locus (seQTL) involving the BCL6 gene was found in 30% of cases. The seQTL of BCL6 aligned with accessible chromatin and increased H3K27 acetylation in cHL, disrupted PRDM1 binding, and co-occurred with BCL6 expression in cHL cells. Weak to strong expression of BCL6 was observed in 68% of cases, and BCL6 expression associated with gene repression similarly in cHL and germinal center B cells. After BCL6 degradation, the core set of genes directly bound and regulated by BCL6 was derepressed in cHL, and proliferation was impaired. The number and clonality of neoantigens was associated with tumor microenvironment type and response to checkpoint blockade. Finally, ctDNA analysis was suggested as a tool to distinguish ambiguous positron emission tomography/computed tomography–positive lesions after treatment.

KW - lymphoma

UR - https://publicatt.unicatt.it/handle/10807/325601

UR - https://www.scopus.com/inward/citedby.uri?partnerID=HzOxMe3b&scp=105008529546&origin=inward

UR - https://www.scopus.com/inward/record.uri?partnerID=HzOxMe3b&scp=105008529546&origin=inward

U2 - 10.1182/blood.2024027355

DO - 10.1182/blood.2024027355

M3 - Article

SN - 0006-4971

VL - 146

SP - 1207

EP - 1224

JO - Blood

JF - Blood

IS - 10

ER -

A comprehensive genetic study of classic Hodgkin lymphoma using circulating tumor DNA

Abstract

All Science Journal Classification (ASJC) codes

Keywords

OSS delle Nazioni Unite

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