Alternative splicing of its 5′-UTR limits CD20 mRNA translation and enables resistance to CD20-directed immunotherapies

Aberrant skipping of coding exons in CD19 and CD22 compromises the response to immunotherapy in B-cell malignancies. Here, we showed that the MS4A1 gene encoding human CD20 also produces several messenger RNA (mRNA) isoforms with distinct 5′ untranslated regions. Four variants (V1-4) were detected u...

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Autores principales: Ang, Zhiwei, Paruzzo, Luca, Hayer, Katharina E., Schmidt, Carolin, Torres Diz, Manuel, Xu, Feng, Zankharia, Urvi, Zhang, Yunlin, Soldan, Samantha, Zheng, Sisi, Falkenstein, Catherine D., Loftus, Joseph P., Yang, Scarlett Y., Asnani, Mukta, King Sainos, Patricia, Pillai, Vinodh, Chong, Emeline, Li, Marilyn M., Tasian, Sarah K., Barash, Yoseph, Lieberman, Paul M., Ruella, Marco, Schuster, Stephen J., Thomas-Tikhonenko, Andrei
Formato: Online Artículo Texto
Lenguaje:English
Publicado: The American Society of Hematology 2023
Materias:
Immunobiology and Immunotherapy
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10667349/
https://www.ncbi.nlm.nih.gov/pubmed/37683180
http://dx.doi.org/10.1182/blood.2023020400
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author Ang, Zhiwei
Paruzzo, Luca
Hayer, Katharina E.
Schmidt, Carolin
Torres Diz, Manuel
Xu, Feng
Zankharia, Urvi
Zhang, Yunlin
Soldan, Samantha
Zheng, Sisi
Falkenstein, Catherine D.
Loftus, Joseph P.
Yang, Scarlett Y.
Asnani, Mukta
King Sainos, Patricia
Pillai, Vinodh
Chong, Emeline
Li, Marilyn M.
Tasian, Sarah K.
Barash, Yoseph
Lieberman, Paul M.
Ruella, Marco
Schuster, Stephen J.
Thomas-Tikhonenko, Andrei
author_facet Ang, Zhiwei
Paruzzo, Luca
Hayer, Katharina E.
Schmidt, Carolin
Torres Diz, Manuel
Xu, Feng
Zankharia, Urvi
Zhang, Yunlin
Soldan, Samantha
Zheng, Sisi
Falkenstein, Catherine D.
Loftus, Joseph P.
Yang, Scarlett Y.
Asnani, Mukta
King Sainos, Patricia
Pillai, Vinodh
Chong, Emeline
Li, Marilyn M.
Tasian, Sarah K.
Barash, Yoseph
Lieberman, Paul M.
Ruella, Marco
Schuster, Stephen J.
Thomas-Tikhonenko, Andrei
author_sort Ang, Zhiwei
collection PubMed
description Aberrant skipping of coding exons in CD19 and CD22 compromises the response to immunotherapy in B-cell malignancies. Here, we showed that the MS4A1 gene encoding human CD20 also produces several messenger RNA (mRNA) isoforms with distinct 5′ untranslated regions. Four variants (V1-4) were detected using RNA sequencing (RNA-seq) at distinct stages of normal B-cell differentiation and B-lymphoid malignancies, with V1 and V3 being the most abundant. During B-cell activation and Epstein-Barr virus infection, redirection of splicing from V1 to V3 coincided with increased CD20 positivity. Similarly, in diffuse large B-cell lymphoma, only V3, but not V1, correlated with CD20 protein levels, suggesting that V1 might be translation-deficient. Indeed, the longer V1 isoform contained upstream open reading frames and a stem-loop structure, which cooperatively inhibited polysome recruitment. By modulating CD20 isoforms with splice-switching morpholino oligomers, we enhanced CD20 expression and anti-CD20 antibody rituximab-mediated cytotoxicity in a panel of B-cell lines. Furthermore, reconstitution of CD20-knockout cells with V3 mRNA led to the recovery of CD20 positivity, whereas V1-reconstituted cells had undetectable levels of CD20 protein. Surprisingly, in vitro CD20-directed chimeric antigen receptor T cells were able to kill both V3- and V1-expressing cells, but the bispecific T-cell engager mosunetuzumab was only effective against V3-expressing cells. To determine whether CD20 splicing is involved in immunotherapy resistance, we performed RNA-seq on 4 postmosunetuzumab follicular lymphoma relapses and discovered that in 2 of them, the downregulation of CD20 was accompanied by a V3-to-V1 shift. Thus, splicing-mediated mechanisms of epitope loss extend to CD20-directed immunotherapies.
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spelling pubmed-106673492023-09-11 Alternative splicing of its 5′-UTR limits CD20 mRNA translation and enables resistance to CD20-directed immunotherapies Ang, Zhiwei Paruzzo, Luca Hayer, Katharina E. Schmidt, Carolin Torres Diz, Manuel Xu, Feng Zankharia, Urvi Zhang, Yunlin Soldan, Samantha Zheng, Sisi Falkenstein, Catherine D. Loftus, Joseph P. Yang, Scarlett Y. Asnani, Mukta King Sainos, Patricia Pillai, Vinodh Chong, Emeline Li, Marilyn M. Tasian, Sarah K. Barash, Yoseph Lieberman, Paul M. Ruella, Marco Schuster, Stephen J. Thomas-Tikhonenko, Andrei Blood Immunobiology and Immunotherapy Aberrant skipping of coding exons in CD19 and CD22 compromises the response to immunotherapy in B-cell malignancies. Here, we showed that the MS4A1 gene encoding human CD20 also produces several messenger RNA (mRNA) isoforms with distinct 5′ untranslated regions. Four variants (V1-4) were detected using RNA sequencing (RNA-seq) at distinct stages of normal B-cell differentiation and B-lymphoid malignancies, with V1 and V3 being the most abundant. During B-cell activation and Epstein-Barr virus infection, redirection of splicing from V1 to V3 coincided with increased CD20 positivity. Similarly, in diffuse large B-cell lymphoma, only V3, but not V1, correlated with CD20 protein levels, suggesting that V1 might be translation-deficient. Indeed, the longer V1 isoform contained upstream open reading frames and a stem-loop structure, which cooperatively inhibited polysome recruitment. By modulating CD20 isoforms with splice-switching morpholino oligomers, we enhanced CD20 expression and anti-CD20 antibody rituximab-mediated cytotoxicity in a panel of B-cell lines. Furthermore, reconstitution of CD20-knockout cells with V3 mRNA led to the recovery of CD20 positivity, whereas V1-reconstituted cells had undetectable levels of CD20 protein. Surprisingly, in vitro CD20-directed chimeric antigen receptor T cells were able to kill both V3- and V1-expressing cells, but the bispecific T-cell engager mosunetuzumab was only effective against V3-expressing cells. To determine whether CD20 splicing is involved in immunotherapy resistance, we performed RNA-seq on 4 postmosunetuzumab follicular lymphoma relapses and discovered that in 2 of them, the downregulation of CD20 was accompanied by a V3-to-V1 shift. Thus, splicing-mediated mechanisms of epitope loss extend to CD20-directed immunotherapies. The American Society of Hematology 2023-11-16 2023-09-11 /pmc/articles/PMC10667349/ /pubmed/37683180 http://dx.doi.org/10.1182/blood.2023020400 Text en © 2023 by The American Society of Hematology. Licensed under Creative Commons Attribution-NonCommercial-NoDerivatives 4.0 International (CC BY-NC-ND 4.0), permitting only noncommercial, nonderivative use with attribution. All other rights reserved. https://creativecommons.org/licenses/by-nc-nd/4.0/This is an open access article under the CC BY-NC-ND license (http://creativecommons.org/licenses/by-nc-nd/4.0/).
spellingShingle Immunobiology and Immunotherapy
Ang, Zhiwei
Paruzzo, Luca
Hayer, Katharina E.
Schmidt, Carolin
Torres Diz, Manuel
Xu, Feng
Zankharia, Urvi
Zhang, Yunlin
Soldan, Samantha
Zheng, Sisi
Falkenstein, Catherine D.
Loftus, Joseph P.
Yang, Scarlett Y.
Asnani, Mukta
King Sainos, Patricia
Pillai, Vinodh
Chong, Emeline
Li, Marilyn M.
Tasian, Sarah K.
Barash, Yoseph
Lieberman, Paul M.
Ruella, Marco
Schuster, Stephen J.
Thomas-Tikhonenko, Andrei
Alternative splicing of its 5′-UTR limits CD20 mRNA translation and enables resistance to CD20-directed immunotherapies
title Alternative splicing of its 5′-UTR limits CD20 mRNA translation and enables resistance to CD20-directed immunotherapies
title_full Alternative splicing of its 5′-UTR limits CD20 mRNA translation and enables resistance to CD20-directed immunotherapies
title_fullStr Alternative splicing of its 5′-UTR limits CD20 mRNA translation and enables resistance to CD20-directed immunotherapies
title_full_unstemmed Alternative splicing of its 5′-UTR limits CD20 mRNA translation and enables resistance to CD20-directed immunotherapies
title_short Alternative splicing of its 5′-UTR limits CD20 mRNA translation and enables resistance to CD20-directed immunotherapies
title_sort alternative splicing of its 5′-utr limits cd20 mrna translation and enables resistance to cd20-directed immunotherapies
topic Immunobiology and Immunotherapy
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC10667349/
https://www.ncbi.nlm.nih.gov/pubmed/37683180
http://dx.doi.org/10.1182/blood.2023020400
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