Combinatorial targeting of nuclear export and translation of RNA inhibits aggressive B-cell lymphomas

Biljana Culjkovic-Kraljacic; Tharu M. Fernando; Rossella Marullo; Nieves Calvo-Vidal; Akanksha Verma; Shao Ning Yang; Fabrizio Tabb O; Marcello Gaudiano; Hiba Zahreddine; Rebecca L. Goldstein; Jayeshkumar Patel; Tony Taldone; Gabriela Chiosis; Marco Ladetto; Paola Ghione; Rodolfo Machiorlatti; Olivier Elemento; Giorgio Inghirami; Ari Melnick; Katherine L.B.Borden; Leandro Cerchietti

doi:10.1182/blood-2015-05-645069

Combinatorial targeting of nuclear export and translation of RNA inhibits aggressive B-cell lymphomas

Biljana Culjkovic-Kraljacic
, Tharu M. Fernando
, Rossella Marullo
, Nieves Calvo-Vidal
, Akanksha Verma
, Shao Ning Yang
, Fabrizio Tabb O
, Marcello Gaudiano
, Hiba Zahreddine
, Rebecca L. Goldstein
, Jayeshkumar Patel
, Tony Taldone
, Gabriela Chiosis
, Marco Ladetto
, Paola Ghione
, Rodolfo Machiorlatti
, Olivier Elemento
, Giorgio Inghirami
, Ari Melnick
, Katherine L.B.Borden

Leandro Cerchietti

Research output: Contribution to journal › Article › peer-review

Abstract

Aggressive double- And triple-hit (DH/TH) diffuse large B-cell lymphomas (DLBCLs) feature activation of Hsp90 stress pathways. Herein, we show that Hsp90 controls posttranscriptional dynamics of keymessengerRNA(mRNA) species including those encoding BCL6, MYC, and BCL2. Using a proteomics approach, we found that Hsp90 binds to andmaintains activity of eIF4E. eIF4E drives nuclear export and translation of BCL6, MYC, and BCL2 mRNA. eIF4E RNA-immunoprecipitation sequencing in DLBCL suggests that nuclear eIF4E controls an extended program that includes B-cell receptor signaling, cellular metabolism, and epigenetic regulation. Accordingly, eIF4E was required for survival of DLBCL including the most aggressive subtypes, DH/TH lymphomas. Indeed, eIF4E inhibition induces tumor regression in cell line and patient-derived tumorgrafts of TH-DLBCL, even in the presence of elevated Hsp90 activity. Targeting Hsp90 is typically limited by counterregulatory elevation of Hsp70B, which induces resistance to Hsp90 inhibitors. Surprisingly, we identify Hsp70mRNA as an eIF4E target. In this way, eIF4E inhibition can overcome drug resistance to Hsp90 inhibitors. Accordingly, rational combinatorial inhibition of eIF4E and Hsp90 inhibitors resulted in cooperative antilymphoma activity in DH/TH DLBCL in vitro and in vivo.

Original language	English
Pages (from-to)	858-868
Number of pages	11
Journal	Blood
Volume	127
Issue number	7
DOIs	https://doi.org/10.1182/blood-2015-05-645069
Publication status	Published - 18 Feb 2016
Externally published	Yes

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Culjkovic-Kraljacic, B., Fernando, T. M., Marullo, R., Calvo-Vidal, N., Verma, A., Yang, S. N., O, F. T., Gaudiano, M., Zahreddine, H., Goldstein, R. L., Patel, J., Taldone, T., Chiosis, G., Ladetto, M., Ghione, P., Machiorlatti, R., Elemento, O., Inghirami, G., Melnick, A., ... Cerchietti, L. (2016). Combinatorial targeting of nuclear export and translation of RNA inhibits aggressive B-cell lymphomas. Blood, 127(7), 858-868. https://doi.org/10.1182/blood-2015-05-645069

@article{a245a577f77a44179bfe1a0c3f328b95,

title = "Combinatorial targeting of nuclear export and translation of RNA inhibits aggressive B-cell lymphomas",

abstract = "Aggressive double- And triple-hit (DH/TH) diffuse large B-cell lymphomas (DLBCLs) feature activation of Hsp90 stress pathways. Herein, we show that Hsp90 controls posttranscriptional dynamics of keymessengerRNA(mRNA) species including those encoding BCL6, MYC, and BCL2. Using a proteomics approach, we found that Hsp90 binds to andmaintains activity of eIF4E. eIF4E drives nuclear export and translation of BCL6, MYC, and BCL2 mRNA. eIF4E RNA-immunoprecipitation sequencing in DLBCL suggests that nuclear eIF4E controls an extended program that includes B-cell receptor signaling, cellular metabolism, and epigenetic regulation. Accordingly, eIF4E was required for survival of DLBCL including the most aggressive subtypes, DH/TH lymphomas. Indeed, eIF4E inhibition induces tumor regression in cell line and patient-derived tumorgrafts of TH-DLBCL, even in the presence of elevated Hsp90 activity. Targeting Hsp90 is typically limited by counterregulatory elevation of Hsp70B, which induces resistance to Hsp90 inhibitors. Surprisingly, we identify Hsp70mRNA as an eIF4E target. In this way, eIF4E inhibition can overcome drug resistance to Hsp90 inhibitors. Accordingly, rational combinatorial inhibition of eIF4E and Hsp90 inhibitors resulted in cooperative antilymphoma activity in DH/TH DLBCL in vitro and in vivo.",

author = "Biljana Culjkovic-Kraljacic and Fernando, \{Tharu M.\} and Rossella Marullo and Nieves Calvo-Vidal and Akanksha Verma and Yang, \{Shao Ning\} and O, \{Fabrizio Tabb\} and Marcello Gaudiano and Hiba Zahreddine and Goldstein, \{Rebecca L.\} and Jayeshkumar Patel and Tony Taldone and Gabriela Chiosis and Marco Ladetto and Paola Ghione and Rodolfo Machiorlatti and Olivier Elemento and Giorgio Inghirami and Ari Melnick and Katherine L.B.Borden and Leandro Cerchietti",

note = "Publisher Copyright: {\textcopyright} 2016 by The American Society of Hematology. {\textcopyright} 2016 by The American Society of Hematology.",

year = "2016",

month = feb,

day = "18",

doi = "10.1182/blood-2015-05-645069",

language = "English",

volume = "127",

pages = "858--868",

journal = "Blood",

issn = "0006-4971",

publisher = "Elsevier B.V.",

number = "7",

}

Culjkovic-Kraljacic, B, Fernando, TM, Marullo, R, Calvo-Vidal, N, Verma, A, Yang, SN, O, FT, Gaudiano, M, Zahreddine, H, Goldstein, RL, Patel, J, Taldone, T, Chiosis, G, Ladetto, M, Ghione, P, Machiorlatti, R, Elemento, O, Inghirami, G, Melnick, A, L.B.Borden, K & Cerchietti, L 2016, 'Combinatorial targeting of nuclear export and translation of RNA inhibits aggressive B-cell lymphomas', Blood, vol. 127, no. 7, pp. 858-868. https://doi.org/10.1182/blood-2015-05-645069

TY - JOUR

T1 - Combinatorial targeting of nuclear export and translation of RNA inhibits aggressive B-cell lymphomas

AU - Culjkovic-Kraljacic, Biljana

AU - Fernando, Tharu M.

AU - Marullo, Rossella

AU - Calvo-Vidal, Nieves

AU - Verma, Akanksha

AU - Yang, Shao Ning

AU - O, Fabrizio Tabb

AU - Gaudiano, Marcello

AU - Zahreddine, Hiba

AU - Goldstein, Rebecca L.

AU - Patel, Jayeshkumar

AU - Taldone, Tony

AU - Chiosis, Gabriela

AU - Ladetto, Marco

AU - Ghione, Paola

AU - Machiorlatti, Rodolfo

AU - Elemento, Olivier

AU - Inghirami, Giorgio

AU - Melnick, Ari

AU - L.B.Borden, Katherine

AU - Cerchietti, Leandro

PY - 2016/2/18

Y1 - 2016/2/18

N2 - Aggressive double- And triple-hit (DH/TH) diffuse large B-cell lymphomas (DLBCLs) feature activation of Hsp90 stress pathways. Herein, we show that Hsp90 controls posttranscriptional dynamics of keymessengerRNA(mRNA) species including those encoding BCL6, MYC, and BCL2. Using a proteomics approach, we found that Hsp90 binds to andmaintains activity of eIF4E. eIF4E drives nuclear export and translation of BCL6, MYC, and BCL2 mRNA. eIF4E RNA-immunoprecipitation sequencing in DLBCL suggests that nuclear eIF4E controls an extended program that includes B-cell receptor signaling, cellular metabolism, and epigenetic regulation. Accordingly, eIF4E was required for survival of DLBCL including the most aggressive subtypes, DH/TH lymphomas. Indeed, eIF4E inhibition induces tumor regression in cell line and patient-derived tumorgrafts of TH-DLBCL, even in the presence of elevated Hsp90 activity. Targeting Hsp90 is typically limited by counterregulatory elevation of Hsp70B, which induces resistance to Hsp90 inhibitors. Surprisingly, we identify Hsp70mRNA as an eIF4E target. In this way, eIF4E inhibition can overcome drug resistance to Hsp90 inhibitors. Accordingly, rational combinatorial inhibition of eIF4E and Hsp90 inhibitors resulted in cooperative antilymphoma activity in DH/TH DLBCL in vitro and in vivo.

AB - Aggressive double- And triple-hit (DH/TH) diffuse large B-cell lymphomas (DLBCLs) feature activation of Hsp90 stress pathways. Herein, we show that Hsp90 controls posttranscriptional dynamics of keymessengerRNA(mRNA) species including those encoding BCL6, MYC, and BCL2. Using a proteomics approach, we found that Hsp90 binds to andmaintains activity of eIF4E. eIF4E drives nuclear export and translation of BCL6, MYC, and BCL2 mRNA. eIF4E RNA-immunoprecipitation sequencing in DLBCL suggests that nuclear eIF4E controls an extended program that includes B-cell receptor signaling, cellular metabolism, and epigenetic regulation. Accordingly, eIF4E was required for survival of DLBCL including the most aggressive subtypes, DH/TH lymphomas. Indeed, eIF4E inhibition induces tumor regression in cell line and patient-derived tumorgrafts of TH-DLBCL, even in the presence of elevated Hsp90 activity. Targeting Hsp90 is typically limited by counterregulatory elevation of Hsp70B, which induces resistance to Hsp90 inhibitors. Surprisingly, we identify Hsp70mRNA as an eIF4E target. In this way, eIF4E inhibition can overcome drug resistance to Hsp90 inhibitors. Accordingly, rational combinatorial inhibition of eIF4E and Hsp90 inhibitors resulted in cooperative antilymphoma activity in DH/TH DLBCL in vitro and in vivo.

UR - https://www.scopus.com/pages/publications/84959372285

U2 - 10.1182/blood-2015-05-645069

DO - 10.1182/blood-2015-05-645069

M3 - Article

SN - 0006-4971

VL - 127

SP - 858

EP - 868

JO - Blood

JF - Blood

IS - 7

ER -

Combinatorial targeting of nuclear export and translation of RNA inhibits aggressive B-cell lymphomas

Abstract

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